WO2007130465A2 - Systems and methods for treating superficial venous malformations like spider veins - Google Patents

Systems and methods for treating superficial venous malformations like spider veins Download PDF

Info

Publication number
WO2007130465A2
WO2007130465A2 PCT/US2007/010652 US2007010652W WO2007130465A2 WO 2007130465 A2 WO2007130465 A2 WO 2007130465A2 US 2007010652 W US2007010652 W US 2007010652W WO 2007130465 A2 WO2007130465 A2 WO 2007130465A2
Authority
WO
WIPO (PCT)
Prior art keywords
light
reactive agent
energy
vein
prescribed form
Prior art date
Application number
PCT/US2007/010652
Other languages
French (fr)
Other versions
WO2007130465A3 (en
Inventor
Killian O'dowd
Anthony Jakubowski
Edward G. Mackay
Aidan Mulloy
Alan A. Creamer
Sherif Sultan
Original Assignee
Green Medical, Inc.
Priority date (The priority date is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the date listed.)
Filing date
Publication date
Priority claimed from US11/446,800 external-priority patent/US7465312B2/en
Application filed by Green Medical, Inc. filed Critical Green Medical, Inc.
Publication of WO2007130465A2 publication Critical patent/WO2007130465A2/en
Publication of WO2007130465A3 publication Critical patent/WO2007130465A3/en

Links

Classifications

    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61NELECTROTHERAPY; MAGNETOTHERAPY; RADIATION THERAPY; ULTRASOUND THERAPY
    • A61N5/00Radiation therapy
    • A61N5/06Radiation therapy using light
    • A61N5/0613Apparatus adapted for a specific treatment
    • A61N5/062Photodynamic therapy, i.e. excitation of an agent
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61NELECTROTHERAPY; MAGNETOTHERAPY; RADIATION THERAPY; ULTRASOUND THERAPY
    • A61N5/00Radiation therapy
    • A61N5/06Radiation therapy using light
    • A61N5/0601Apparatus for use inside the body
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61NELECTROTHERAPY; MAGNETOTHERAPY; RADIATION THERAPY; ULTRASOUND THERAPY
    • A61N5/00Radiation therapy
    • A61N5/06Radiation therapy using light
    • A61N5/0601Apparatus for use inside the body
    • A61N2005/0602Apparatus for use inside the body for treatment of blood vessels
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61NELECTROTHERAPY; MAGNETOTHERAPY; RADIATION THERAPY; ULTRASOUND THERAPY
    • A61N5/00Radiation therapy
    • A61N5/06Radiation therapy using light
    • A61N2005/0635Radiation therapy using light characterised by the body area to be irradiated
    • A61N2005/0643Applicators, probes irradiating specific body areas in close proximity
    • A61N2005/0644Handheld applicators
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61NELECTROTHERAPY; MAGNETOTHERAPY; RADIATION THERAPY; ULTRASOUND THERAPY
    • A61N5/00Radiation therapy
    • A61N5/06Radiation therapy using light
    • A61N2005/065Light sources therefor
    • A61N2005/0651Diodes
    • A61N2005/0652Arrays of diodes

Definitions

  • spider veins result from various dysfunctions in the veins.
  • Veins carry oxygen-poor blood from the body back to the heart .
  • Spider veins can be caused by the backup of blood, when one-way flap valves in veins become weak, causing blood to collect in veins. Spider veins can also arise due to other causes, e.g., hormone changes, inherited factors, and exposure to the sun. Spider veins are often red or blue and close to the surface of the skin. They can look like tree branches or spider webs with their short jagged lines. Spider veins can be found on the legs and face. They can cover either a very small or very large area of skin.
  • Sclerotherapy is a common treatment for spider veins. Sclerotherapy involves the injection of a solution into the vein that causes the vein walls to swell, stick together, and seal shut. This stops the flow of blood and the vein turns into scar tissue. Microsclerotherapy uses special solutions and injection techniques that can increase the success rate for removal of smaller spider veins. Sclerotherapy involves tedious, hard to learn injection techniques. It can lead to side effects like stinging or painful cramps where the injection was made, or temporary red raised patches of skin, or skin sores, or bruises. The treated vein can also become inflamed or develop lumps of clotted blood. Applying heat and taking aspirin or antibiotics can relieve inflammation. Lumps of coagulated blood can be drained.
  • Laser surgery can be used to treat larger spider veins in the legs. Laser surgery sends very strong bursts of light onto the vein, which makes the vein slowly fade and disappear. Laser surgery is more appealing to some patients because it does not use needles or incisions. Still, when the laser hits the skin, the patient can feel a heat sensation that can be quite painful. Laser surgery can cause redness or swelling of the skin, and can cause burns and scars. Depending on the severity of the veins, two to five treatments (15 to 20 minutes each) are generally needed to remove spider veins in the legs. Moreover, for spider veins larger than 3 mm, laser therapy is not very practical. Furthermore, the capital cost for purchasing trans-dermal lasers can be quite high, making the treatment relatively costly.
  • the invention provides devices, systems, methods, and protocols that provide minimally invasive, cost effective, and patient-friendly surgical and/or cosmetic surgical treatment of superficial venous malformations, e.g., spider veins.
  • the invention also provides devices, systems, methods, and protocols that provide minimally invasive, cost effective, and patient -friendly surgical treatment of diseases or dysfunctions in regions of the body that can be readily accessed by treatment agents carried by blood; e.g., cancers like breast and prostrate cancer; ear, nose, and throat conditions; periodontal disease; and diseases of the eye.
  • treatment agents carried by blood e.g., cancers like breast and prostrate cancer; ear, nose, and throat conditions; periodontal disease; and diseases of the eye.
  • the devices, systems and methods distribute a reactive agent at, in, or near an inner wall of a vein.
  • the reactive agent is characterized in that it can be controllably activated by the application of a prescribed form of energy.
  • the devices, systems, and methods activate the reactive agent by applying the prescribed form of energy to activate the reactive agent.
  • the activation of the agent causes localized injury to the inner wall of the vein.
  • the prescribed form of energy can comprise, e.g., electromagnetic radiation, and, more particularly, light energy.
  • the devices, systems, and methods distribute a light- reactive agent at, in, or near an inner wall of a vein.
  • the devices, systems, and methods activate the light- reactive agent by applying light energy at a wavelength that activates the light-reactive agent to cause localized injury to the inner wall of the vein.
  • the light energy is desirably non-thermal and is generated by a low voltage photoactivation device, comprising, e.g., one or more light-emitting diodes.
  • the light- reactive agent comprises LSIl (Talaporfin Sodium) that is administered intravenously.
  • the light -reactive agent comprises verteporfin that is administered intravenously.
  • Devices, systems, and methods that incorporate this aspect of the invention can treat superficial venous disease, like spider veins.
  • Fig. 1 is a perspective view of a system of devices for treating a superficial venous disease, such as spider veins using a light-reactive agent, the agent being suited for intravenous injection.
  • Fig. 2 is a perspective view of the system shown in Fig. 1 packaged as a kit, with directions for using the devices to treat a superficial venous disease.
  • Figs. 3A and 3B are side section views, taken generally alone line 3-3 in Fig. 1, showing alternative embodiments of the internal components of a photoactivation device that forms a part of the system shown in Fig. 1.
  • Figs. 4 to 14 show a representative method of using a system like that shown in Fig. 1 to treat spider veins .
  • Fig. 15 shows an alternative embodiment of a source of a light-reactive agent usable with the system shown in Fig. 1, the agent being in tablet or capsule form, for oral ingestion.
  • Fig. 16 shows an alternative embodiment of a source of a light-reactive agent usable with the system shown in Fig. 1, the agent being in cream form for topical application.
  • Fig. 17 shows an alternative embodiment of a source of a light-reactive agent usable with the system shown in Fig. 1, the agent being in a band aid form for topical application.
  • Figs. 18A, 18B, and 18C show alternative embodiments of a photoactivation device that can form a part of the system shown in Fig. 1.
  • Figs. 19 and 20 show the treatment of ears of
  • Fig. 21 shows visible alterations in the superficial venous anatomy of a rabbit ear treated as shown in Figs. 19 and 20 due to shrinkage of vein dimensions .
  • the systems, methods, and devices disclosed herein are directed to the distribution of a selected reactive agent at, in, or near an inner wall of a vein.
  • the selected reactive agent is characterized in that it can be reliably and controllably activating in situ by the application of a prescribed form of energy. Once distributed to the targeted site, the reactive agent can be activated in situ by applying the prescribed form of energy. The activation of the reactive agent causes localized injury to the inner wall of the vein.
  • the prescribed form of energy can comprise, e.g., electromagnetic radiation, and, more particularly, electromagnetic radiation in the wavelength spectrum comprising light energy.
  • the devices and system, and their associated methods of use, are particularly well suited for treating superficial venous diseases, such as spider veins .
  • Fig. i shows representative devices that together comprise a system 10 for treating a vascular disease or a dysfunction affecting the vascular system using light-reactive agents, i.e., reactive agents that are activated by light energy.
  • the devices and .system 10, and their associated methods of use, using light-reactive agents are particularly well suited for treating superficial venous diseases, such as spider veins. For this reason, the devices and system 10, and their associated methods of use will be described in this context .
  • the disclosed devices and system 10, and their associated methods of use are applicable for use in treating other diseases or dysfunctions elsewhere in the body that are not necessarily related to spider veins or their cause, but are nevertheless capable of treatment by light- reactive agents carried by blood.
  • Other conditions that can be treated by light reactive agents using the system 10 or a form of the system 10 include cancer, e.g., breast or prostrate cancer,- conditions of the ear, nose, or throat; periodontal disease; and conditions of the eye or sight (ophthalmology) .
  • the system 10 includes at least one source 12 of a selected light reactive agent 14.
  • the source 12 can be provided in various forms . For example, as shown in Fig.
  • the source 12 can comprise a conventional vial 16 containing the light reactive agent 14 in solution suited for intravenous injection.
  • the source 12 can comprise the light reactive agent 14 packaged with a carrier in tablet or capsule form for oral ingestion; or incorporated into a cream that can be applied topically to the skin.
  • the light reactive agent 14 can comprise any light-reactive drug suited for photodynamic therapy (PDT) .
  • PDT is a treatment that uses an agent or drug, also called a photosensitizer or photosensitizing agent, and light energy of a particular selected wavelength.
  • the photosensitizers which are inert by themselves, bind to proteins found in blood, e.g., lipoproteins. The proteins act as carriers, transporting the photosensitizers to cells targeted for treatment. When exposed to light of the particular wavelength (which varies according to the photosensitizer) , the photosensitizer reacts with oxygen.
  • the reaction transforms the oxygen into singlet oxygen and free radicals.
  • the singlet oxygen and free radicals disrupt normal cellular functions and cause cell death.
  • the light reactive agent 14 can be selected among a group of photosensitizers, depending upon type and location of tissue being treated, as well as the mode contemplated for its introduction into body tissue.
  • Each photosensitizer is activated by light of a specific wavelength. This wavelength determines how far the light can travel into the body. Thus, the physician can select a specific photosensitizer and wavelength (s) of light to treat different areas of the body.
  • the photosensitizer selected desirably possesses all or some of the following clinically relvant criteria: a commercially available pure chemical; low dark toxicity but strong photocytotoxicity; good selectivity toward target cells; long-wavelength absorbing; rapid removal from the body,- and ease of administration through various routes.
  • Candidate photosensitizers include, but are not limited, to: PHOTOFRIN ® (Porfimer sodium - Axcan Pharma, Inc.); FOSCAN ® (temoporfin, meta- tetrahydroxyphenylchlorin, mTHPC - Biolitec AG) ; VISUDYNE ® (verteporfin, benzoporphyrin derivative monoacid ring A, BPD-MA - Novartis Pharmaceuticals) ; LEVULAN ® (5 -aminolevulinic acid, ALA - DUSA Pharmaceuticals, Inc.); METVIX ® (methyl 1 aminolevulinate, MLA or M-ALA - Photocure, ASA); HPPH (2- [1-hexy- loxyethyl] -2-devinyl pyropheophorbide-a, PHOTOCCHLOR - Rosewell Park Cancer Institute) ; motexafin lutetium (MLu, luteti
  • the selected light reactive agent 14 is administered by the system 10 for delivery to a targeted tissue treatment site at, in, or near an inner wall of a vein.
  • the targeted tissue site is a sub-dermal region where one or more spider veins are present (this is shown Fig. 4 and will be described in greater detail later) .
  • the form for administration will depend upon the form of the source 12.
  • the light reactive agent 14 can be provided in tablet or capsule form 54 (see Fig. 15) , which can be ingested orally for absorption by the GI tract for systemic distribution by blood to the targeted tissue treatment site.
  • the tablet or capsule form 54 can incorporate time release features.
  • the tablet or capsule form 54 can also be in the form of an ionosphere to accelerate systemic distribution.
  • the light reactive agent 14 can be incorporated into a cream form 56 (see Fig. 16), and the light reactive agent 14 can be applied topically for percutaneous absorption by the skin to the targeted tissue treatment site.
  • the cream form 56 can be applied on exterior skin (e.g., an arm or a leg) or applied within the oral cavity (e.g., by swabbing the gums) .
  • the cream form 56 can also incorporate time release features.
  • the cream form 56 can be driven transdermally with the use of ultrasound, or can incorporate dimethyl sulfoxide (DMSO) or aloe cream or similar agent to accelerate transdermal delivery.
  • the light reactive agent 14 can be incorporated onto a platform form 58 (see Fig. 17) , such as, e.g., a band aid member placed on an exterior skin surface, or as a sub-lingual tab placed on or under the tongue.
  • the light reactive agent 14 can also be applied by pricking the skin.
  • Fig. 1 shows the light reactive agent 14 in solution in the vial 16.
  • Talaporfin Sodium together with a special array of light emitting diodes (LEDs) , has been tested by Light Sciences Oncology, Inc. in both preclinical and human clinical trials in the United States, Europe and Japan, and has shown efficacy in treating cancer (solid tumors) .
  • LSIl material can be activated by shining a LED array at a particular wavelength (664 nm) by a light source 12 into the affected area of tissue.
  • Fig. 1 shows the light reactive agent 14 in solution in the vial 16.
  • VISUDYNE ® material has been used, together with a special laser light, to treat abnormal blood vessel formation in the eye, called age-related macular degeneration (AMD) (which, if untreated, can lead to loss of eyesight) .
  • AMD age-related macular degeneration
  • VISUDYNE ® material can be activated by shining a pre-calculated dose of light at a particular wavelength (689 nm) by a low-energy laser or light source 12 into the affected area of tissue.
  • the device takes the form of a conventional hand-held syringe 18.
  • the syringe 18 draws the light reactive agent 14 in solution from the vial 16
  • the administration device can take the form of a conventional intravenous (IV) delivery catheter or set coupled to a syringe or other intravenous delivery device or pump.
  • IV intravenous
  • the system 10 includes a photoactivation device 20.
  • the photoactivation device 20 includes one or more light sources 22 (see Fig. 3) .
  • the light sources 22 have a wavelength or a range of wavelengths.
  • the photoactivation device 20 also includes means for controlling the intensity or a range of intensities, spot size or a range of spot sizes, and other operating characteristics of the light sources 22 that are conducive to activation the light reactive agent 14 in a desired manner.
  • the photoactivation device 20 comprises non-thermal light energy generated by a low-voltage source (not greater than 12 Volts) .
  • the photoactivation device 20 can take various forms, depending upon nature, location, and size of the targeted tissue region.
  • the photoactivation device 20 can, e.g., be mounted on an adjustable frame that is located above or below the targeted tissue region of an individual.
  • the photoactive device may, alternatively, deliver light through fiber optic cables (e.g., quartz fiber optic cables) and the like to areas inside the body.
  • a fiber optic cable can be inserted through an endoscope into a targeted internal tissue region (e.g., within a vessel or hollow organ) to treat a dysfunction.
  • the photoactivation device 20 may comprise a portable light source that applies light to surface tissue.
  • the light sources 22 can comprise, ' e.g., lasers, fluorescent, or incandescent lights.
  • the light sources 22 can also comprise light emitting diodes (LED's). LED' s can generate high energy light of desired wavelengths and can be assembled in a range of geometry and sizes.
  • the source of activating energy comprises a source of the electromagnetic radiation having the other prescribed wavelength.
  • the photoactivation device 20 is sized and configured to be held and manipulated in a single hand, so that it can be wanded or waved to apply light percutaneously to a tissue region where the spider vein or veins are located.
  • the photoactivation device 20 includes a low-energy light source 22 carried within a housing 24.
  • the housing 24 comprises a handle end 26 and a light transmitting end 28.
  • the handle end 26 is sized and configured to be conveniently gripped by a practitioner.
  • the handle end 26 encloses a control circuit 30 coupled to a self-contained low voltage (i.e., no more than 12 volts) , DC power ' source 32, such as a battery.
  • a self-contained low voltage i.e., no more than 12 volts
  • DC power ' source 32 such as a battery.
  • the battery 32 is desirably rechargeable, e.g., by a plug-in connector (not shown) , or, alternatively, the battery 32 can be configured to be removed and replaced through a lift-off cover (also not shown) .
  • the handle end 26 includes an on-off switch 34, which activates the control circuit 30.
  • the light source 22 comprises one or more light emitters 36, which are carried within the housing 24 for transmitting light from the light transmitting end 28 of the housing 24.
  • the light emitters 36 are coupled to the control circuit 30.
  • light can be applied to the skin in a tissue region where the spider vein or veins are located by holding the light transmitting end 28 of the housing 24 out of direct surface contact with the skin.
  • light can be applied to the skin in a tissue region where the spider vein or veins are located by placing the light transmitting end 28 of the housing 24 in direct surface contact with the skin.
  • direct surface contact between the skin and the light transmitting end 28 reflectance toward the operator is minimized.
  • the skin acts as a light guide, allowing output flux to be maximized without localized heating.
  • the light emitters 36 can be, e.g., light emitting diodes (LED's), emitting light in the wavelength (s) that activates the light reactive agent 14.
  • the light emitting diodes of a single photoactivation device 20 can be conditioned to deliver multiple wavelengths, so that the photoactivation device 20 can provide a universal platform for different light reactive agents 14.
  • the light reactive agent 14 is LSIl
  • at least one of the wavelengths is 664 nm.
  • the control circuit 30 may- comprise a printed circuit board on which the LED' s are mounted.
  • the light emitters 36 can be arranged in an array sized and configured to focus at common point. Small micro lenses (not shown) may be used to improve focus and adjust the focal distance.
  • the light emitters 36 are oriented to focus at a reflecting device 38 carried within the light transmitting end 28.
  • the reflecting device 38 reflects the light from the light emitters 36 out a portal 40 on the light transmitting end 28.
  • the reflecting device 38 may comprise, e.g., a surface mirror or a prism.
  • the common focal point for all the light emitters 36 may be slightly short of the reflecting device 38 or slightly beyond the reflecting device 38, so that the light from the reflecting device mirror will spread to cover an area, or spot size, beyond the portal 40.
  • the reflecting device 38 may be made adjustable to change the spot size during use.
  • the portal 40 is oriented at an angle to the main axis of the housing 24, preferably at about 90°.
  • the light transmitting end 28 could be mounted for pivoting through a range of angles relative to the main axis, and/or for rotation about the main axis, to permit virtually infinite alignment of the emitted light path with the targeted tissue treatment site.
  • the light- emitters 36 can comprise an array of light emitting diodes carried in the portal 40, for applying diffused light directly from the portal 40 without use of a reflecting device.
  • a removable transparent cover 42 can be provided to cover light transmitting end 28 during use.
  • the cover 42 can comprise/ e.g., plastic film encircled with an elastic material. The materials is selected to be substantially transparent to the wavelength of the light emitted. Following use for a given individual, the cover 42 can be removed and discarded, and replaced with a new cover for the next individual .
  • the photoactivation device 20 includes a carrier or platform 60 that is sized and configured to be placed upon surface tissue overlaying the treatment site.
  • the light emitters 36 comprise light emitting diodes, which can be arranged in various patterns on the platform 36.
  • the pattern of light emitters 36 can comprise a single linear or curvilinear array,- or as shown in Fig. 18B, the pattern of light emitters 36 can comprise a square or rectilinear array; or as shown in Fig. 18C, the pattern of light emitters 36 can comprise a circle or oval array.
  • the pattern can include linear or curvilinear or zigzag or symmetric or asymmetric arrays of light emitters 36, depending upon the topology of the targeted tissue region.
  • the carrier 60 may also be shaped to conform to the topology.
  • the carrier 60 may include one or more handles 64 and/or straps 66 (see Fig. 18C) , to facilitate stabilization and fixation of the carrier 60 at the targeted tissue treatment site.
  • a power cord 70 supplies power to the light emitters 36, which can be either from a battery source or a conventional 110 VAC source.
  • the pattern of light emitters 36 on the carrier 60 emit light in the wavelength (s) that activates the light reactive agent 14.
  • the light emitters 36 can be conditioned to deliver multiple wavelengths, so that the photoactivation device 20 can provide a universal platform for different light reactive agents 14.
  • the control circuit 30 may comprise a printed circuit board on which the LED' s are mounted.
  • the kit 44 comprises a sterile, wrapped assembly including an interior tray 46 made, e.g., from die cut cardboard, plastic sheet, or thermo-formed plastic material, which hold the contents.
  • the kit 44 also preferably includes directions 48 for using the contents of the kit 44 to carry out a desired procedure .
  • every component of the system 10 is contained within the kit 44.
  • various components can be provided in separate packaging. In this arrangement, the directions 48 still instruct use of the various components separately provided as a system 10.
  • the directions 48 can, of course vary. The directions may be physically present in the kit 44, but can also be supplied separately.
  • the directions 48 can be embodied in separate instruction manuals, or in video or audio tapes, CD's, and DVD's. The instructions for use can also be available through an internet web page.
  • the directions 48 instruct the practitioner how to use the system 10 to carry out the intended therapeutic treatment.
  • the directions 48 incorporate a method of treatment using the system 10.
  • Figs . 4 to 14 show a representative method of using the system 10 shown in Fig. 1 to treat a vascular condition such as spider veins, which the directions 48 can express in part or in its entirety. As Fig. 4 shows, the method identifies a site where the targeted condition exists, i.e., where the spider veins are present.
  • the spider veins are usually easily identifiable by a trained practitioner. They are often red or blue and close to the surface of the skin. They possess branches or "spider webs" with short jagged lines. Spider veins can be found on the legs and face. They can cover either a very small or very large area of skin.
  • the light reactive agent 14 is to be administered intravenously.
  • an appropriate injection site 52 is identified, as shown in Fig. 5.
  • the injection site 52 is where a selected light reactive agent 14 will administered intravenously by the system 10 for delivery to the targeted treatment site 50.
  • the injection site 52 offers venous access at a distance from the targeted treatment site 50 in an upstream blood flow direction (i.e., the injection site 52 is farther from the heart than the treatment site 50) .
  • the light reactive agent 14, when injected intravenously is allowed to become systemic and will be conveyed by venous blood flow toward the heart to the targeted treatment site 50.
  • the method prepares the light reactive agent 14 for introduction.
  • prescribed volume of the light reactive agent 14 is drawn into the syringe 18.
  • the volume to be injected in dependent upon the therapeutic dose that is prescribed, which is, in turn, dependent upon the concentration of the light reactive agent 14 in solution, as well as the morphology of the targeted treatment site 50.
  • VISUDYNE ® material is commercially reconstituted in saline or glucose solution at desired concentration of about verteporfin 2mg/mL.
  • a typical dose for a spider vein region can be in the order of 1 cc to 5 cc, but this dosage will of course depend upon the physiology of the individual, including the size and depth of the target treatment site 50, the skin type of the. individual, and the body size of the individual.
  • the dosage can be determined by clinical study by physical measurements and titration, or can be selected empirically based upon general anatomic considerations, or a combination of these and other considerations.
  • the method injects the light reactive agent 14 intravenously at the injection site 52.
  • the syringe 18 needle injects directly into a vein.
  • An IV catheter may be used, through which the light reactive agent 14 is injected by syringe or other suitable IV pumping device .
  • the rate of delivery is dependent upon the nature and dosage of the light reactive agent 14 as well as the physiology of the individual being treated. It is desirable to avoid discomfort to the individual, and the rate of delivery selected has this as its primary objective .
  • a period of time desirably occurs after injection (as the clocks C in Pigs. 7 and 8 indicate) , to allow the light reactive agent 14 to become systemic.
  • Fig. 9 shows, verteporfin V, once injected, attaches to lipoproteins LP in the plasma.
  • the lipoproteins LP carry the verteporin V to the targeted treatment site 50, as Fig. 10 shows. This exposes endothelium of the spider veins to the verteporin V carried by the lipoproteins LP.
  • the optimal time period to allow systemic distribution of the light reactive agent 14 in this manner to the targeted treatment site 50 following injection can be determined by clinical study by physical measurements, or can be selected empirically based upon general anatomic considerations, or a combination of these and other considerations.
  • the method operates the photoactivation device 20 to ⁇ apply light having prescribed characteristics to the targeted treatment site 50.
  • These prescribed characteristics include the wavelength and may also include, but are not necessarily limited to, a desired intensity, a desired spot size, and a desired duration of exposure.
  • the wavelength will depend upon the light reactive agent 14 selected.
  • the intensity, spot size, and duration of exposure of the applied light will depend upon the physiology of the individual being treated and the operating parameters of the system 10, e.g., upon the size of the treatment site 50; the depth of the treatment site 50; the skin type of the individual; the body size of the individual; the distance between the light transmitting end 28 of the housing 24 and the skin surface; the time of exposure; and the pattern of applying the light.
  • Optimal operating characteristics for the photoactivation device 20 can be determined by clinical study by physical measurements, or can be selected empirically based upon general anatomic considerations, or a combination of these and other considerations.
  • the photoactivation device 20 can apply light either without making direct contact with the skin or by making direct contact with the skin.
  • Fig. 12 shows, once verteporfin is activated by light in the .presence of oxygen, highly reactive, short-lived singlet oxygen and reactive oxygen radicals are generated.
  • the singlet oxygen and reactive oxygen radicals cause local damage to inner wall or endothelium of the veins. Cells outside of contact with the activated verteporfin, however, are left unaffected.
  • Treatment by the system 10 and method just described intentionally causes injury to the inner vein walls.
  • the clinically parameters above described i.e., the dosage, delivery time and rate, operating conditions of the photoactivation device 20, etc., the nature of the injury can be tightly controlled and localized.
  • the initial injury to the vein wall evokes a healing process (see Fig. 13) .
  • the vein heals shut over time.
  • the healing results in shrinkage of the spider vein, and eventually, complete obliteration of the spider veins in the targeted region, as Fig. 14 shows.
  • the superficial venous anatomy of the ears of New Zealand White Rabbits were treated by injecting light-reactive agent LSIl (Talaporfin Sodium) in doses selected to approximate a human dose, and thereafter exposing the superficial venous anatomy to light at a wavelength of 664 nm in dose periods ranging from 8 to 12 minutes. Visible alterations in the superficial venous anatomy due to shrinkage of veins in the treated regions were observed.
  • LSIl Light-reactive agent
  • New Zealand Rabbits were chosen because of their large ears having easily identifiable superficial venous anatomy (as Fig. 19 shows) .
  • a total of twelve rabbits were treated.
  • Each rabbit (weighing approximately six pounds) was intravaneously sedated for approximately 25 minutes using Ketamine and secured to a treatment table before being treated.
  • the ears were shaved clean of hair and skin prepped with alcohol .
  • LSIl (Talaporfin Sodium, from Light Sciences
  • the LSIl was administered intravenously by a syringe 18 and an IV administration line 68 into the superficial venous anatomy of one ear of each rabbit (the other ear serving as the Control) .
  • Different doses of LSIl (at a concentration of 0.125 mg per cc) were administered to different rabbits, at 0.25 mg/kg; 0.50 mg/kg,- 1.0 mg/kg; and 1.5 mg/kg, respectively.
  • the doses were selected to approximate a human dose of 3 mg/ml to 10 mg/ml (a dose of 0.2 to 0.5 mg/kg) .
  • the doses were administered to each rabbit's ear intravenously in a slow bolus method over a period of 5 minutes.
  • a light-applying carrier 60 of the type shown in Fig. 18A (with a linear array of three LED's) was laid on the head of the rabbit over the treated ear, which was held tight against the carrier (see Fig. 20) .
  • the light emitters 36 were operated at a wavelength of 664 nm.
  • the power source was standard 110 V AC current .
  • Fig. 21 is a drawing based upon a representative photograph of a control ear (Control) and a treated ear (Treated) of one of the treated rabbits.
  • Fig. 21 allows a side-by-side comparison between the superficial venous anatomy of a control ear and a treated ear (LSIl dose: 1.5mg/kg; Light Dose: 8 min of 664nm light) .
  • Fig. 21 demonstrates that treatment with the light -reactive agent LSIl (Talaporfin Sodium) in the manner described can serve to visibly alter the superficial venous anatomy, due to shrinkage of veins in the targeted region.
  • LSIl Light -reactive agent
  • the devices, systems, methods, and protocols that have been described can provide minimally invasive, cost effective, and patient-friendly treatment of diseases or dysfunctions in all regions of the body that can be readily accessed by treatment agents carried by blood; e.g., cancers like breast and prostrate cancer; ear, nose, and throat conditions; periodontal disease; and diseases of the eye.
  • treatment agents carried by blood e.g., cancers like breast and prostrate cancer; ear, nose, and throat conditions; periodontal disease; and diseases of the eye.

Abstract

Systems and methods treat superficial venous malformations, such as spider veins. The systems and methods distribute a reactive agent, e.g., a light-reactive agent such as talaporfin sodium or verteporf in, at or near an inner wall of a vein. The systems and methods activate the reactive agent by applying energy, e.g. non-thermal light energy at a wavelength that activates the reactive agent to cause localized injury to the inner wall of the vein.

Description

SYSTEMS AND METHODS FOR TREATING SUPERFICIAL VENOUS
MALFORMATIONS LIKE SPIDER VEINS Related Application
This application is a continuation-in-part of co-pending United States Patent Application Serial No. 11/446,800, filed June 5, 2006 and entitled "Systems and Methods for Treating Superficial Venous Malformations Like Spider Veins," which claims the benefit of United States Provisional Patent Application Serial No. 60/796,656, filed May 2, 2006, and entitled "Systems and Methods for Treating Superficial Venous Malformations Like Spider Veins," which are both incorporated herein by- reference . Background of the Invention As the large group of so-called baby-boomers advances in age, there are increasing demands for effective, non-invasive treatment of vascular diseases or dysfunctions affecting the vascular system. There are also increasing demands for non-invasive cosmetic surgery to repair conditions that have vascular origins.
For example, spider veins result from various dysfunctions in the veins. Veins carry oxygen-poor blood from the body back to the heart .
Spider veins can be caused by the backup of blood, when one-way flap valves in veins become weak, causing blood to collect in veins. Spider veins can also arise due to other causes, e.g., hormone changes, inherited factors, and exposure to the sun. Spider veins are often red or blue and close to the surface of the skin. They can look like tree branches or spider webs with their short jagged lines. Spider veins can be found on the legs and face. They can cover either a very small or very large area of skin.
Sclerotherapy is a common treatment for spider veins. Sclerotherapy involves the injection of a solution into the vein that causes the vein walls to swell, stick together, and seal shut. This stops the flow of blood and the vein turns into scar tissue. Microsclerotherapy uses special solutions and injection techniques that can increase the success rate for removal of smaller spider veins. Sclerotherapy involves tedious, hard to learn injection techniques. It can lead to side effects like stinging or painful cramps where the injection was made, or temporary red raised patches of skin, or skin sores, or bruises. The treated vein can also become inflamed or develop lumps of clotted blood. Applying heat and taking aspirin or antibiotics can relieve inflammation. Lumps of coagulated blood can be drained.
Laser surgery can be used to treat larger spider veins in the legs. Laser surgery sends very strong bursts of light onto the vein, which makes the vein slowly fade and disappear. Laser surgery is more appealing to some patients because it does not use needles or incisions. Still, when the laser hits the skin, the patient can feel a heat sensation that can be quite painful. Laser surgery can cause redness or swelling of the skin, and can cause burns and scars. Depending on the severity of the veins, two to five treatments (15 to 20 minutes each) are generally needed to remove spider veins in the legs. Moreover, for spider veins larger than 3 mm, laser therapy is not very practical. Furthermore, the capital cost for purchasing trans-dermal lasers can be quite high, making the treatment relatively costly. There is need for devices, systems, methods, and protocols that provide minimally invasive, cost effective, and patient-friendly surgical and/or cosmetic surgical treatment of superficial venous malformations, such as e.g., in the treatment of spider veins. There is also a need for devices, systems, methods, and protocols that provide minimally invasive, cost effective, and patient-friendly treatment of diseases or dysfunctions in any region of the body that can be readily accessed by treatment agents carried by blood; e.g., cancers like breast and prostrate cancer; ear, nose, and throat conditions; periodontal disease; and diseases of the eye. Summary of the Invention
The invention provides devices, systems, methods, and protocols that provide minimally invasive, cost effective, and patient-friendly surgical and/or cosmetic surgical treatment of superficial venous malformations, e.g., spider veins.
The invention also provides devices, systems, methods, and protocols that provide minimally invasive, cost effective, and patient -friendly surgical treatment of diseases or dysfunctions in regions of the body that can be readily accessed by treatment agents carried by blood; e.g., cancers like breast and prostrate cancer; ear, nose, and throat conditions; periodontal disease; and diseases of the eye.
According to one aspect of the invention, the devices, systems and methods distribute a reactive agent at, in, or near an inner wall of a vein. The reactive agent is characterized in that it can be controllably activated by the application of a prescribed form of energy. The devices, systems, and methods activate the reactive agent by applying the prescribed form of energy to activate the reactive agent. The activation of the agent causes localized injury to the inner wall of the vein. The prescribed form of energy can comprise, e.g., electromagnetic radiation, and, more particularly, light energy.
According to another aspect of the invention, the devices, systems, and methods distribute a light- reactive agent at, in, or near an inner wall of a vein. The devices, systems, and methods activate the light- reactive agent by applying light energy at a wavelength that activates the light-reactive agent to cause localized injury to the inner wall of the vein. The light energy is desirably non-thermal and is generated by a low voltage photoactivation device, comprising, e.g., one or more light-emitting diodes. In one embodiment, the light- reactive agent comprises LSIl (Talaporfin Sodium) that is administered intravenously. In another embodiment, the light -reactive agent comprises verteporfin that is administered intravenously. Devices, systems, and methods that incorporate this aspect of the invention can treat superficial venous disease, like spider veins.
The devices, systems, and methods improve the quality of patient care. The devices, systems, and methods eliminate side effects such as brusing, burning, and skin discoloration. The devices, systems, and methods do not require tedious, hard to learn injection techniques. They do not require high cost trans-dermal lasers. The devices, systems, and method are usable by by a large group of practitioners, such as dermatologists, phlebologists, vascular surgeons, and interventional radiologists . Brief Description of the Drawings Fig. 1 is a perspective view of a system of devices for treating a superficial venous disease, such as spider veins using a light-reactive agent, the agent being suited for intravenous injection.
Fig. 2 is a perspective view of the system shown in Fig. 1 packaged as a kit, with directions for using the devices to treat a superficial venous disease.
Figs. 3A and 3B are side section views, taken generally alone line 3-3 in Fig. 1, showing alternative embodiments of the internal components of a photoactivation device that forms a part of the system shown in Fig. 1.
Figs. 4 to 14 show a representative method of using a system like that shown in Fig. 1 to treat spider veins . Fig. 15 shows an alternative embodiment of a source of a light-reactive agent usable with the system shown in Fig. 1, the agent being in tablet or capsule form, for oral ingestion.
Fig. 16 shows an alternative embodiment of a source of a light-reactive agent usable with the system shown in Fig. 1, the agent being in cream form for topical application.
Fig. 17 shows an alternative embodiment of a source of a light-reactive agent usable with the system shown in Fig. 1, the agent being in a band aid form for topical application.
Figs. 18A, 18B, and 18C show alternative embodiments of a photoactivation device that can form a part of the system shown in Fig. 1. Figs. 19 and 20 show the treatment of ears of
New Zealand White Rabbits by injecting into the superficial venous anatomy light-reactive agent LSIl
(Talaporfin Sodium) in doses selected to approximate a human dose, and thereafter exposing the superficial venous anatomy to light at a wavelength of 664 nm in doses ranging from 8 to 12 minutes.
Fig. 21 shows visible alterations in the superficial venous anatomy of a rabbit ear treated as shown in Figs. 19 and 20 due to shrinkage of vein dimensions .
Description of the Preferred Embodiment
Although the disclosure hereof is detailed and exact to enable those skilled in the art to practice the invention, the physical embodiments herein disclosed merely exemplify the invention which may be embodied in other specific structures. While the preferred embodiment has -been described, the details may be changed without departing from the invention, which is defined by the claims . The systems, methods, and devices disclosed herein are directed to the distribution of a selected reactive agent at, in, or near an inner wall of a vein. The selected reactive agent is characterized in that it can be reliably and controllably activating in situ by the application of a prescribed form of energy. Once distributed to the targeted site, the reactive agent can be activated in situ by applying the prescribed form of energy. The activation of the reactive agent causes localized injury to the inner wall of the vein. The prescribed form of energy can comprise, e.g., electromagnetic radiation, and, more particularly, electromagnetic radiation in the wavelength spectrum comprising light energy. The devices and system, and their associated methods of use, are particularly well suited for treating superficial venous diseases, such as spider veins .
Fig. i shows representative devices that together comprise a system 10 for treating a vascular disease or a dysfunction affecting the vascular system using light-reactive agents, i.e., reactive agents that are activated by light energy. The devices and .system 10, and their associated methods of use, using light-reactive agents are particularly well suited for treating superficial venous diseases, such as spider veins. For this reason, the devices and system 10, and their associated methods of use will be described in this context .
Still, it should be appreciated that the disclosed devices and system 10, and their associated methods of use are applicable for use in treating other diseases or dysfunctions elsewhere in the body that are not necessarily related to spider veins or their cause, but are nevertheless capable of treatment by light- reactive agents carried by blood. Other conditions that can be treated by light reactive agents using the system 10 or a form of the system 10 include cancer, e.g., breast or prostrate cancer,- conditions of the ear, nose, or throat; periodontal disease; and conditions of the eye or sight (ophthalmology) . As Fig. 1 shows, the system 10 includes at least one source 12 of a selected light reactive agent 14. The source 12 can be provided in various forms . For example, as shown in Fig. 1, the source 12 can comprise a conventional vial 16 containing the light reactive agent 14 in solution suited for intravenous injection. Alternatively, the source 12 can comprise the light reactive agent 14 packaged with a carrier in tablet or capsule form for oral ingestion; or incorporated into a cream that can be applied topically to the skin. The light reactive agent 14 can comprise any light-reactive drug suited for photodynamic therapy (PDT) . PDT is a treatment that uses an agent or drug, also called a photosensitizer or photosensitizing agent, and light energy of a particular selected wavelength. The photosensitizers, which are inert by themselves, bind to proteins found in blood, e.g., lipoproteins. The proteins act as carriers, transporting the photosensitizers to cells targeted for treatment. When exposed to light of the particular wavelength (which varies according to the photosensitizer) , the photosensitizer reacts with oxygen.
The reaction transforms the oxygen into singlet oxygen and free radicals. The singlet oxygen and free radicals disrupt normal cellular functions and cause cell death.
The light reactive agent 14 can be selected among a group of photosensitizers, depending upon type and location of tissue being treated, as well as the mode contemplated for its introduction into body tissue. Each photosensitizer is activated by light of a specific wavelength. This wavelength determines how far the light can travel into the body. Thus, the physician can select a specific photosensitizer and wavelength (s) of light to treat different areas of the body.
The photosensitizer selected desirably possesses all or some of the following clinically relvant criteria: a commercially available pure chemical; low dark toxicity but strong photocytotoxicity; good selectivity toward target cells; long-wavelength absorbing; rapid removal from the body,- and ease of administration through various routes. Candidate photosensitizers include, but are not limited, to: PHOTOFRIN® (Porfimer sodium - Axcan Pharma, Inc.); FOSCAN® (temoporfin, meta- tetrahydroxyphenylchlorin, mTHPC - Biolitec AG) ; VISUDYNE® (verteporfin, benzoporphyrin derivative monoacid ring A, BPD-MA - Novartis Pharmaceuticals) ; LEVULAN® (5 -aminolevulinic acid, ALA - DUSA Pharmaceuticals, Inc.); METVIX® (methyl1 aminolevulinate, MLA or M-ALA - Photocure, ASA); HPPH (2- [1-hexy- loxyethyl] -2-devinyl pyropheophorbide-a, PHOTOCCHLOR - Rosewell Park Cancer Institute) ; motexafin lutetium (MLu, lutetiura(III) texaphyrin, LU-TEX, ANTRIN - Pharmacuclics Inc.); Npe6 (mono-L-aspartyl chlorine e6, taporfin sodium, talaporfin, LSIl - Light Science Oncology Inc., Snoqualπiie, Washington); and SnET2 (tin ethyl etiopurpurin, Sn etiopurpurin, rostaporfin, PHOTREX - Miravant Medical Technologies) .
In use, whatever the. form, the selected light reactive agent 14 is administered by the system 10 for delivery to a targeted tissue treatment site at, in, or near an inner wall of a vein. In the context of the illustrated embodiment, the targeted tissue site is a sub-dermal region where one or more spider veins are present (this is shown Fig. 4 and will be described in greater detail later) . The form for administration will depend upon the form of the source 12. The light reactive agent 14 can be provided in tablet or capsule form 54 (see Fig. 15) , which can be ingested orally for absorption by the GI tract for systemic distribution by blood to the targeted tissue treatment site. The tablet or capsule form 54 can incorporate time release features. The tablet or capsule form 54 can also be in the form of an ionosphere to accelerate systemic distribution.
Alternatively, the light reactive agent 14 can be incorporated into a cream form 56 (see Fig. 16), and the light reactive agent 14 can be applied topically for percutaneous absorption by the skin to the targeted tissue treatment site. The cream form 56 can be applied on exterior skin (e.g., an arm or a leg) or applied within the oral cavity (e.g., by swabbing the gums) . The cream form 56 can also incorporate time release features. The cream form 56 can be driven transdermally with the use of ultrasound, or can incorporate dimethyl sulfoxide (DMSO) or aloe cream or similar agent to accelerate transdermal delivery. Alternatively, the light reactive agent 14 can be incorporated onto a platform form 58 (see Fig. 17) , such as, e.g., a band aid member placed on an exterior skin surface, or as a sub-lingual tab placed on or under the tongue. The light reactive agent 14 can also be applied by pricking the skin.
It has been discovered that an injectable form of Talaporfin Sodium -- available 'from Light Sciences Oncology, Inc as LSIl -- can be intravenously administered to effectively treat spider veins using the system 10 shown in Fig. 1. Therefore, Fig. 1 shows the light reactive agent 14 in solution in the vial 16.
Talaporfin Sodium, together with a special array of light emitting diodes (LEDs) , has been tested by Light Sciences Oncology, Inc. in both preclinical and human clinical trials in the United States, Europe and Japan, and has shown efficacy in treating cancer (solid tumors) . LSIl material can be activated by shining a LED array at a particular wavelength (664 nm) by a light source 12 into the affected area of tissue.
It has also been discovered that an injectable form of the porphyrin-based photosensitizer called verteporfin -- commercially available from QLT, Inc. as VISUDYNE® material (verteporfin for injection) -- can be intravenously administered to effectively treat spider veins using the system 10 shown in Fig. l. Therefore, Fig. 1 shows the light reactive agent 14 in solution in the vial 16.
VISUDYNE® material has been used, together with a special laser light, to treat abnormal blood vessel formation in the eye, called age-related macular degeneration (AMD) (which, if untreated, can lead to loss of eyesight) . VISUDYNE® material can be activated by shining a pre-calculated dose of light at a particular wavelength (689 nm) by a low-energy laser or light source 12 into the affected area of tissue.
In the context of the illustrated embodiment, where the source 12 comprises an injectable solution of the light reactive agent 14, the device takes the form of a conventional hand-held syringe 18. The syringe 18 draws the light reactive agent 14 in solution from the vial 16
(as shown in Fig. 6) and injects the photodynamic material in solution into the vascular system for transport by the blood flow to the targeted tissue site (as shown in Fig. 7) . The injection site can be locally to tissue in the region to be treated, or directly into a vein or artery serving the region. Instead of a handheld syringe 18, the administration device can take the form of a conventional intravenous (IV) delivery catheter or set coupled to a syringe or other intravenous delivery device or pump.
As Fig. 1 also shows, the system 10 includes a photoactivation device 20. The photoactivation device 20 includes one or more light sources 22 (see Fig. 3) . The light sources 22 have a wavelength or a range of wavelengths. The photoactivation device 20 also includes means for controlling the intensity or a range of intensities, spot size or a range of spot sizes, and other operating characteristics of the light sources 22 that are conducive to activation the light reactive agent 14 in a desired manner. Desirably, the photoactivation device 20 comprises non-thermal light energy generated by a low-voltage source (not greater than 12 Volts) .
The photoactivation device 20 can take various forms, depending upon nature, location, and size of the targeted tissue region. The photoactivation device 20 can, e.g., be mounted on an adjustable frame that is located above or below the targeted tissue region of an individual. The photoactive device may, alternatively, deliver light through fiber optic cables (e.g., quartz fiber optic cables) and the like to areas inside the body. For example, a fiber optic cable can be inserted through an endoscope into a targeted internal tissue region (e.g., within a vessel or hollow organ) to treat a dysfunction. Alternatively, the photoactivation device 20 may comprise a portable light source that applies light to surface tissue.
The light sources 22 can comprise,' e.g., lasers, fluorescent, or incandescent lights. The light sources 22 can also comprise light emitting diodes (LED's). LED' s can generate high energy light of desired wavelengths and can be assembled in a range of geometry and sizes.
When the reactive agent is activated by another wavelength within the spectrum of electromagnetic energy, e.g., infrared and ultraviolet light, or X-rays and gamma-rays, the source of activating energy comprises a source of the electromagnetic radiation having the other prescribed wavelength. In one representative embodiment (see Figs. 1 and 3A/3B) , the photoactivation device 20 is sized and configured to be held and manipulated in a single hand, so that it can be wanded or waved to apply light percutaneously to a tissue region where the spider vein or veins are located.
In this embodiment (see Figs. 3A and 3B) , the photoactivation device 20 includes a low-energy light source 22 carried within a housing 24. The housing 24 comprises a handle end 26 and a light transmitting end 28. The handle end 26 is sized and configured to be conveniently gripped by a practitioner.
The handle end 26 encloses a control circuit 30 coupled to a self-contained low voltage (i.e., no more than 12 volts) , DC power' source 32, such as a battery. The battery 32 is desirably rechargeable, e.g., by a plug-in connector (not shown) , or, alternatively, the battery 32 can be configured to be removed and replaced through a lift-off cover (also not shown) . The handle end 26 includes an on-off switch 34, which activates the control circuit 30.
The light source 22 comprises one or more light emitters 36, which are carried within the housing 24 for transmitting light from the light transmitting end 28 of the housing 24. The light emitters 36 are coupled to the control circuit 30.
In use, light can be applied to the skin in a tissue region where the spider vein or veins are located by holding the light transmitting end 28 of the housing 24 out of direct surface contact with the skin. Alternatively, light can be applied to the skin in a tissue region where the spider vein or veins are located by placing the light transmitting end 28 of the housing 24 in direct surface contact with the skin. With direct surface contact between the skin and the light transmitting end 28, reflectance toward the operator is minimized. With direct surface contact between the skin and the light transmitting end 28, the skin acts as a light guide, allowing output flux to be maximized without localized heating. The light emitters 36 can be, e.g., light emitting diodes (LED's), emitting light in the wavelength (s) that activates the light reactive agent 14. The light emitting diodes of a single photoactivation device 20 can be conditioned to deliver multiple wavelengths, so that the photoactivation device 20 can provide a universal platform for different light reactive agents 14. In the illustrated embodiment, where the light reactive agent 14 is LSIl, at least one of the wavelengths is 664 nm. Where the light reactive agent 14 is verteporfin, at least one of the wavelengths is 689 nm. In this arrangement, the control circuit 30 may- comprise a printed circuit board on which the LED' s are mounted.
The light emitters 36 can be arranged in an array sized and configured to focus at common point. Small micro lenses (not shown) may be used to improve focus and adjust the focal distance. In the embodiment illustrated in Fig. 3A, the light emitters 36 are oriented to focus at a reflecting device 38 carried within the light transmitting end 28. The reflecting device 38 reflects the light from the light emitters 36 out a portal 40 on the light transmitting end 28. The reflecting device 38 may comprise, e.g., a surface mirror or a prism. The common focal point for all the light emitters 36 may be slightly short of the reflecting device 38 or slightly beyond the reflecting device 38, so that the light from the reflecting device mirror will spread to cover an area, or spot size, beyond the portal 40. The reflecting device 38 may be made adjustable to change the spot size during use.
Desirably, for ease of handling, the portal 40 is oriented at an angle to the main axis of the housing 24, preferably at about 90°. If desired, the light transmitting end 28 could be mounted for pivoting through a range of angles relative to the main axis, and/or for rotation about the main axis, to permit virtually infinite alignment of the emitted light path with the targeted tissue treatment site.
Alternatively, as shown in Fig. 3B, the light- emitters 36 can comprise an array of light emitting diodes carried in the portal 40, for applying diffused light directly from the portal 40 without use of a reflecting device.
As Fig. 1 shows, a removable transparent cover 42 can be provided to cover light transmitting end 28 during use. The cover 42 can comprise/ e.g., plastic film encircled with an elastic material. The materials is selected to be substantially transparent to the wavelength of the light emitted. Following use for a given individual, the cover 42 can be removed and discarded, and replaced with a new cover for the next individual .
In another representative embodiment (see Figs. 18A, 18B, and 18C), the photoactivation device 20 includes a carrier or platform 60 that is sized and configured to be placed upon surface tissue overlaying the treatment site. In this arrangement, the light emitters 36 comprise light emitting diodes, which can be arranged in various patterns on the platform 36. By way of example, as shown in Fig. 18A, the pattern of light emitters 36 can comprise a single linear or curvilinear array,- or as shown in Fig. 18B, the pattern of light emitters 36 can comprise a square or rectilinear array; or as shown in Fig. 18C, the pattern of light emitters 36 can comprise a circle or oval array. The pattern can include linear or curvilinear or zigzag or symmetric or asymmetric arrays of light emitters 36, depending upon the topology of the targeted tissue region. The carrier 60 may also be shaped to conform to the topology.
The carrier 60 may include one or more handles 64 and/or straps 66 (see Fig. 18C) , to facilitate stabilization and fixation of the carrier 60 at the targeted tissue treatment site. A power cord 70 supplies power to the light emitters 36, which can be either from a battery source or a conventional 110 VAC source.
As before stated, the pattern of light emitters 36 on the carrier 60 emit light in the wavelength (s) that activates the light reactive agent 14. The light emitters 36 can be conditioned to deliver multiple wavelengths, so that the photoactivation device 20 can provide a universal platform for different light reactive agents 14. In the illustrated embodiment, where the light reactive agent 14 is LSIl, at least one of the wavelengths is 664 nm. Where the light reactive agent 14 is verteporfin, at least one of the wavelengths is 689 nm. In this arrangement, the control circuit 30 may comprise a printed circuit board on which the LED' s are mounted. As Fig. 2 shows, the various components of the system 10 as just described can be consolidated for use in a functional kit 44. The kit 44 can take various forms. In the illustrated embodiment, the kit 44 comprises a sterile, wrapped assembly including an interior tray 46 made, e.g., from die cut cardboard, plastic sheet, or thermo-formed plastic material, which hold the contents. The kit 44 also preferably includes directions 48 for using the contents of the kit 44 to carry out a desired procedure . In the illustrated embodiment, every component of the system 10 is contained within the kit 44. Of course, various components can be provided in separate packaging. In this arrangement, the directions 48 still instruct use of the various components separately provided as a system 10.
The directions 48 can, of course vary. The directions may be physically present in the kit 44, but can also be supplied separately. The directions 48 can be embodied in separate instruction manuals, or in video or audio tapes, CD's, and DVD's. The instructions for use can also be available through an internet web page. The directions 48 instruct the practitioner how to use the system 10 to carry out the intended therapeutic treatment. The directions 48 incorporate a method of treatment using the system 10. Figs . 4 to 14 show a representative method of using the system 10 shown in Fig. 1 to treat a vascular condition such as spider veins, which the directions 48 can express in part or in its entirety. As Fig. 4 shows, the method identifies a site where the targeted condition exists, i.e., where the spider veins are present. This site is called the targeted treatment site 50. The spider veins are usually easily identifiable by a trained practitioner. They are often red or blue and close to the surface of the skin. They possess branches or "spider webs" with short jagged lines. Spider veins can be found on the legs and face. They can cover either a very small or very large area of skin.
In the illustrated embodiment, the light reactive agent 14 is to be administered intravenously. In this arrangement, an appropriate injection site 52 is identified, as shown in Fig. 5. The injection site 52 is where a selected light reactive agent 14 will administered intravenously by the system 10 for delivery to the targeted treatment site 50. Desirably, the injection site 52 offers venous access at a distance from the targeted treatment site 50 in an upstream blood flow direction (i.e., the injection site 52 is farther from the heart than the treatment site 50) . In this manner, the light reactive agent 14, when injected intravenously, is allowed to become systemic and will be conveyed by venous blood flow toward the heart to the targeted treatment site 50.
As Fig. 6 shows, the method prepares the light reactive agent 14 for introduction. In the illustrated embodiment , prescribed volume of the light reactive agent 14 is drawn into the syringe 18. The volume to be injected in dependent upon the therapeutic dose that is prescribed, which is, in turn, dependent upon the concentration of the light reactive agent 14 in solution, as well as the morphology of the targeted treatment site 50.
Typically, VISUDYNE® material is commercially reconstituted in saline or glucose solution at desired concentration of about verteporfin 2mg/mL. At this concentration, a typical dose for a spider vein region can be in the order of 1 cc to 5 cc, but this dosage will of course depend upon the physiology of the individual, including the size and depth of the target treatment site 50, the skin type of the. individual, and the body size of the individual. The dosage can be determined by clinical study by physical measurements and titration, or can be selected empirically based upon general anatomic considerations, or a combination of these and other considerations.
As Fig. 7 shows, the method injects the light reactive agent 14 intravenously at the injection site 52. In the illustrated embodiment, the syringe 18 needle injects directly into a vein. An IV catheter may be used, through which the light reactive agent 14 is injected by syringe or other suitable IV pumping device .
The rate of delivery is dependent upon the nature and dosage of the light reactive agent 14 as well as the physiology of the individual being treated. It is desirable to avoid discomfort to the individual, and the rate of delivery selected has this as its primary objective .
It is believed that, given the concentration and volume of the VISUDYNE® material being injected in the illustrated embodiment, an injection period of 20 to 30 seconds is acceptable.
A period of time desirably occurs after injection (as the clocks C in Pigs. 7 and 8 indicate) , to allow the light reactive agent 14 to become systemic. As Fig. 9 shows, verteporfin V, once injected, attaches to lipoproteins LP in the plasma. The lipoproteins LP carry the verteporin V to the targeted treatment site 50, as Fig. 10 shows. This exposes endothelium of the spider veins to the verteporin V carried by the lipoproteins LP. The optimal time period to allow systemic distribution of the light reactive agent 14 in this manner to the targeted treatment site 50 following injection can be determined by clinical study by physical measurements, or can be selected empirically based upon general anatomic considerations, or a combination of these and other considerations.
As Fig. 11 shows, after allowing a selected time period after injection to pass, the method operates the photoactivation device 20 to^ apply light having prescribed characteristics to the targeted treatment site 50. These prescribed characteristics include the wavelength and may also include, but are not necessarily limited to, a desired intensity, a desired spot size, and a desired duration of exposure. The wavelength will depend upon the light reactive agent 14 selected. The intensity, spot size, and duration of exposure of the applied light will depend upon the physiology of the individual being treated and the operating parameters of the system 10, e.g., upon the size of the treatment site 50; the depth of the treatment site 50; the skin type of the individual; the body size of the individual; the distance between the light transmitting end 28 of the housing 24 and the skin surface; the time of exposure; and the pattern of applying the light. Optimal operating characteristics for the photoactivation device 20 can be determined by clinical study by physical measurements, or can be selected empirically based upon general anatomic considerations, or a combination of these and other considerations. The photoactivation device 20 can apply light either without making direct contact with the skin or by making direct contact with the skin.
As Fig. 12 shows, once verteporfin is activated by light in the .presence of oxygen, highly reactive, short-lived singlet oxygen and reactive oxygen radicals are generated. The singlet oxygen and reactive oxygen radicals cause local damage to inner wall or endothelium of the veins. Cells outside of contact with the activated verteporfin, however, are left unaffected.
Treatment by the system 10 and method just described intentionally causes injury to the inner vein walls. By controlling the clinically parameters above described (i.e., the dosage, delivery time and rate, operating conditions of the photoactivation device 20, etc.,) the nature of the injury can be tightly controlled and localized.
The initial injury to the vein wall evokes a healing process (see Fig. 13) . During the healing process, the vein heals shut over time. The healing results in shrinkage of the spider vein, and eventually, complete obliteration of the spider veins in the targeted region, as Fig. 14 shows.
EXAMPLE
The superficial venous anatomy of the ears of New Zealand White Rabbits were treated by injecting light-reactive agent LSIl (Talaporfin Sodium) in doses selected to approximate a human dose, and thereafter exposing the superficial venous anatomy to light at a wavelength of 664 nm in dose periods ranging from 8 to 12 minutes. Visible alterations in the superficial venous anatomy due to shrinkage of veins in the treated regions were observed.
New Zealand Rabbits were chosen because of their large ears having easily identifiable superficial venous anatomy (as Fig. 19 shows) . A total of twelve rabbits were treated. Each rabbit (weighing approximately six pounds) was intravaneously sedated for approximately 25 minutes using Ketamine and secured to a treatment table before being treated. The ears were shaved clean of hair and skin prepped with alcohol . LSIl (Talaporfin Sodium, from Light Sciences
Oncology, Inc.) was selected as the light reactive agent 14. As Fig. 19 shows, the LSIl was administered intravenously by a syringe 18 and an IV administration line 68 into the superficial venous anatomy of one ear of each rabbit (the other ear serving as the Control) . Different doses of LSIl (at a concentration of 0.125 mg per cc) were administered to different rabbits, at 0.25 mg/kg; 0.50 mg/kg,- 1.0 mg/kg; and 1.5 mg/kg, respectively. The doses were selected to approximate a human dose of 3 mg/ml to 10 mg/ml (a dose of 0.2 to 0.5 mg/kg) .
The doses were administered to each rabbit's ear intravenously in a slow bolus method over a period of 5 minutes. After a pre-selected delay of ten minutes following the injection, a light-applying carrier 60 of the type shown in Fig. 18A (with a linear array of three LED's) was laid on the head of the rabbit over the treated ear, which was held tight against the carrier (see Fig. 20) . The light emitters 36 were operated at a wavelength of 664 nm. The power source was standard 110 V AC current .
For each LSIl dose, three different light doses - 8 minutes, 10 minutes, and 12 minutes - were applied. Twelve rabbits were treated according to the protocol (four different LSIl doses at three different light doses) .
At the conclusion of the light exposure, the treated ear was coated with aluminum oxide cream and a photograph taken. Fig. 21 is a drawing based upon a representative photograph of a control ear (Control) and a treated ear (Treated) of one of the treated rabbits. Fig. 21 allows a side-by-side comparison between the superficial venous anatomy of a control ear and a treated ear (LSIl dose: 1.5mg/kg; Light Dose: 8 min of 664nm light) . Fig. 21 demonstrates that treatment with the light -reactive agent LSIl (Talaporfin Sodium) in the manner described can serve to visibly alter the superficial venous anatomy, due to shrinkage of veins in the targeted region.
It should be appreciated that the devices, systems, methods, and protocols that have been described can provide minimally invasive, cost effective, and patient-friendly treatment of diseases or dysfunctions in all regions of the body that can be readily accessed by treatment agents carried by blood; e.g., cancers like breast and prostrate cancer; ear, nose, and throat conditions; periodontal disease; and diseases of the eye.
The foregoing is considered as illustrative only of the principles of the invention. Furthermore, since numerous modifications and changes will readily occur to those skilled in the art, it is not desired to limit the invention to the exact construction and operation shown and described. While the preferred embodiment has been described, the details may be changed without departing from the invention, which is defined by the claims.

Claims

I/We Claim:
1. A method for treating a spider vein comprising providing a reactive agent that is controllably activated by the application of a prescribed form of energy, distributing the reactive agent at, in, or near an inner wall of a spider vein, and activating the reactive agent by applying the prescribed form of energy that activates the reactive agent in situ to cause localized injury to the inner wall of the spider vein.
2. A method according to claim 1 wherein the prescribed form of energy comprises electromagnetic radiation.
3. A method according to claim 1 wherein the prescribed form of energy comprises light energy.
4. A method for treating a spider vein comprising providing a light-reactive agent, distributing the light-reactive agent at, in, or near an inner wall of a spider vein, and activating the light-reactive agent by applying light energy having a wavelength that activates the light-reactive agent to cause localized injury to the inner wall of the spider vein.
5. A method according to claim 4 wherein the light-reactive agent comprises verteporfin.
6. A method according to claim 4 wherein the light-reactive agent comprises talaporfin sodium.
7. A method according to claim 4 wherein the light-reactive agent is distributed by intravenous injection.
8. A method according to claim 4 wherein the light-reactive agent is distributed by ingestion.
9. A method according to claim 4 wherein the light-reactive agent is distributed by topical application.
10. A method according to claim 9 wherein the light-reactive agent is topically applied to exterior skin tissue.
11. A method according to claim 10 wherein the light-reactive agent is carried on a band aid member applied to skin tissue.
12. A method according to claim 9 wherein the light-reactive agent is topically applied to tissue within an oral cavity.
13. A method according to claim 9 wherein the light-reactive agent is applied by pricking tissue.
14. A method according to claim 4 wherein the light-reactive agent includes a time release component.
15. A method according to claim 4 wherein distribution of the light-reactive agent includes application of ultrasound.
16. A method according to claim 4 wherein distribution of the light-reactive agent includes use of dimethyl sulfoxide or aloe cream.
17. A method according to claim 4 wherein the light energy comprises light from at least one light emitting diode.
18. A method according to claim 4 wherein the light energy is applied by a handheld photoactivation device.
19. A method according to claim 18 wherein the photoactivation device is battery- powered.
20. A method according to claim 4 wherein light energy is applied by an array of
5 light emitters.
21. A method according to claim 20 wherein at least one of the light emitters comprises a light emitting diode.
22. A method according to claim 4
10 wherein light energy is applied by an array of light emitter carried by a platform.
23. A method according to claim 22 wherein the platform is sized and configured to be manually placed in contact with a tissue region. 15
24. A method according to claim 4 wherein light energy is applied via a fiber optic cable.
25. A method according to claim 24 wherein the fiber optic cable includes quartz. 20
26. A method according to claim 24 wherein the light energy comprises fluorescent light .
27. A method according to claim 24 wherein the light energy comprises
25 incandescent light.
28. A method according to claim 4 wherein the light energy comprises laser.
29. A system comprising a reactive agent that is controllably
■ 30 activated by the application of a prescribed form of energy, a device operating to emit the prescribed form of energy that activates the reactive agent, and directions for using the reactive agent and 35 the device to treat a spider vein condition.
30. A system comprising a light-reactive agent, a photoactivation device operating to emit light at a wavelength that activates the light-reactive agent , and directions for using the light-reactive agent and the photoactivation device to treat a. spider vein condition.
31. A system according to claim 30 wherein the light-reactive agent is verteporfin.
32. A system according to claim 30 wherein the light-reactive agent comprises talaporfin sodium.
33. A system according to claim 30 wherein the photoactivating device comprises a hand-held light source.
34. A system according to claim 30 wherein the photoactivation device includes at least one light emitting diode.
35. A system according to claim 30 wherein the photoactivation device includes an array of light emitters.
36. A system according to claim 35 wherein at least one of the light emitters comprises a light emitting diode.
37. A method according to claim 30 wherein the photoactivation device includes a platform and an array of light emitters carried by the platform.
38. A method according to claim 37 wherein the platform is sized and configured to be manually placed in contact with a tissue region.
39. A method for treating superficial venous malformations comprising providing a reactive agent that is controllably activated by the application of a prescribed form of energy, distributing the reactive agent at, in, or near an inner wall of a vein, and activating the reactive agent by applying the prescribed form of energy that activates the reactive agent in situ to cause localized injury to the inner wall of the vein.
40. A method according to claim 39 wherein the prescribed form of energy comprises electromagnetic radiation.
41. A method according to claim 39 wherein the prescribed form of energy comprises light energy.
42. A method according to claim 39 wherein the superficial venous malformation comprises a spider vein.
43. A system comprising a reactive agent that is controllably activated by the application of a prescribed form of energy, a device operating to emit the prescribed form of energy that activates the reactive agent, and directions for using the reactive agent and the device to treat a superficial venous malformation.
44. A system according to claim 43 wherein the prescribed form of energy comprises electromagnetic radiation.
45. A method according to claim 43 wherein the prescribed form of energy comprises light energy.
46. A system according to claim 43 wherein the superficial venous malformation comprises a spider vein.
47. A method for treating superficial venous malformations comprising providing a light-reactive agent, distributing the light-reactive agent at, in, or near an inner wall of a vein, and activating the light-reactive agent by- applying light energy from a light emitting diode having a wavelength that activates the light-reactive agent to cause localized injury to the inner wall of the vein.
48. A method according to claim 47 wherein the superficial venous malformation comprises a spider vein.
49. A system comprising a light-reactive agent, a photoactivation device comprising at least one light-emitting diode operating to emit light at a wavelength that activates the light-reactive agent, and directions for using the light-reactive agent and the photoactivation device to treat a superficial venous malformation.
50. A system according to claim 49 wherein the superficial venous malformation comprises a spider vein.
PCT/US2007/010652 2006-05-02 2007-05-02 Systems and methods for treating superficial venous malformations like spider veins WO2007130465A2 (en)

Applications Claiming Priority (5)

Application Number Priority Date Filing Date Title
US79665606P 2006-05-02 2006-05-02
US60/796,656 2006-05-02
US11/446,800 US7465312B2 (en) 2006-05-02 2006-06-05 Systems and methods for treating superficial venous malformations like spider veins
US11/446,800 2006-06-05
US11/799,583 US20070299431A1 (en) 2006-05-02 2007-05-02 Systems and methods for treating superficial venous malformations like spider veins

Publications (2)

Publication Number Publication Date
WO2007130465A2 true WO2007130465A2 (en) 2007-11-15
WO2007130465A3 WO2007130465A3 (en) 2008-12-04

Family

ID=42333362

Family Applications (1)

Application Number Title Priority Date Filing Date
PCT/US2007/010652 WO2007130465A2 (en) 2006-05-02 2007-05-02 Systems and methods for treating superficial venous malformations like spider veins

Country Status (2)

Country Link
US (2) US20070299431A1 (en)
WO (1) WO2007130465A2 (en)

Families Citing this family (21)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
WO2008124790A2 (en) 2002-07-10 2008-10-16 Angiodynamics, Inc. Device and method for endovascular treatment for causing closure of a blood vessel
US9895494B2 (en) * 2007-01-25 2018-02-20 DePuy Synthes Products, Inc. Syringe with energy delivery component and method of use
US20100311026A1 (en) 2009-06-03 2010-12-09 Tomes Jennifer E Catheter Tray, Packaging System, and Associated Methods
US9795761B2 (en) 2009-06-30 2017-10-24 Medline Industries, Inc. Medical kit, packaging system, instruction insert, and associated methods
US8448786B2 (en) 2009-06-30 2013-05-28 Medline Industries, Inc. Catheter tray, packaging system, instruction insert, and associated methods
US8678190B2 (en) 2009-06-30 2014-03-25 Medline Industries, Inc. Catheter tray, packaging system, instruction insert, and associated methods
US8631935B2 (en) 2009-06-03 2014-01-21 Medline Industries, Inc. Catheter tray, packaging system, and associated methods
USRE49724E1 (en) 2008-09-29 2023-11-14 Tom Kerber Device for photodynamical therapy of cancer
US10195459B2 (en) 2008-09-29 2019-02-05 Tom Kerber Device for photodynamical therapy of cancer
US20110184336A1 (en) * 2008-09-29 2011-07-28 Tom Kerber Device for photodynamical therapy of cancer
US10106295B2 (en) 2010-05-21 2018-10-23 Medline Industries, Inc. Stacked catheter tray, system, and associated methods
USD704856S1 (en) 2010-12-06 2014-05-13 Medline Industries, Inc. Medical tray
CA2862611C (en) 2011-02-24 2020-11-03 Eximo Medical Ltd. Hybrid catheter for tissue resection
JP2012196379A (en) * 2011-03-23 2012-10-18 Panasonic Corp Light irradiation type beauty apparatus
US8992513B2 (en) 2011-06-30 2015-03-31 Angiodynamics, Inc Endovascular plasma treatment device and method of use
MX2016004191A (en) 2013-10-16 2016-06-24 Bard Inc C R Catheter insertion tray with integrated instructions.
US11684420B2 (en) 2016-05-05 2023-06-27 Eximo Medical Ltd. Apparatus and methods for resecting and/or ablating an undesired tissue
US11896778B2 (en) 2017-03-31 2024-02-13 C. R. Bard, Inc. Catheter insertion-tray systems and methods thereof
US11490983B2 (en) 2018-04-24 2022-11-08 C. R. Bard, Inc. Catheterization packages and methods thereof
US11116937B2 (en) 2018-05-11 2021-09-14 Medline Industries, Inc. Foley catheter and corresponding single-layer tray packaging system
WO2019246307A1 (en) 2018-06-20 2019-12-26 C.R. Bard, Inc. Urinary catheter-insertion kits with integrated instructions for use and methods thereof

Citations (3)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US6050990A (en) * 1996-12-05 2000-04-18 Thermolase Corporation Methods and devices for inhibiting hair growth and related skin treatments
US6899723B2 (en) * 1999-01-15 2005-05-31 Light Sciences Corporation Transcutaneous photodynamic treatment of targeted cells
US6936044B2 (en) * 1998-11-30 2005-08-30 Light Bioscience, Llc Method and apparatus for the stimulation of hair growth

Family Cites Families (83)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US4111564A (en) * 1973-02-08 1978-09-05 Trice Jr James R Reference plane production
US5171749A (en) * 1987-01-20 1992-12-15 University Of British Columbia Wavelength-specific cytotoxic agents
US5283255A (en) * 1987-01-20 1994-02-01 The University Of British Columbia Wavelength-specific cytotoxic agents
US5298502A (en) * 1988-12-12 1994-03-29 Fmc Corporation Method and composition for photodynamic treatment and detection of tumors
CN1039283C (en) * 1988-12-12 1998-07-29 Fmc公司 Prodn. and use of porphyrins
CA2012175A1 (en) 1989-03-31 1990-09-30 Michael W. Berns Photochemical treatment of blood vessels
DE69029712T2 (en) * 1989-11-20 1997-05-28 Hamamatsu Photonics Kk Device for the diagnosis and treatment of cancer provided with a laser beam generator
US5258453A (en) * 1992-01-21 1993-11-02 University Of Utah Drug delivery system for the simultaneous delivery of drugs activatable by enzymes and light
CA2087902C (en) * 1992-02-05 2006-10-17 Narendra Raghunathji Desai Liposome compositions of porphyrin photosensitizers
CA2142711A1 (en) * 1992-08-17 1994-03-03 Anna M. Richter Method for destroying or inhibiting growth of unwanted cells or tissues
DK0680365T3 (en) * 1992-11-20 2000-06-05 Univ British Columbia Activation of photosensitizers
US5514669A (en) * 1993-09-29 1996-05-07 Medical College Of Ohio Use of photodynamic therapy to treat prostatic tissue
US5628744A (en) * 1993-12-21 1997-05-13 Laserscope Treatment beam handpiece
US5824080A (en) * 1995-09-28 1998-10-20 The General Hospital Corporation Photochemistry for the preparation of biologic grafts--allografts and xenografts
US7473251B2 (en) * 1996-01-05 2009-01-06 Thermage, Inc. Methods for creating tissue effect utilizing electromagnetic energy and a reverse thermal gradient
US5834503A (en) * 1996-06-14 1998-11-10 Qlt Phototherapeutics, Inc. Methods to treat arterial plaque
US5913884A (en) * 1996-09-19 1999-06-22 The General Hospital Corporation Inhibition of fibrosis by photodynamic therapy
US7390668B2 (en) * 1996-10-30 2008-06-24 Provectus Pharmatech, Inc. Intracorporeal medicaments for photodynamic treatment of disease
US6275726B1 (en) * 1997-05-15 2001-08-14 Board Of Regents, The University Of Texas System Methods of enhanced light transmission through turbid biological media
US6176854B1 (en) * 1997-10-08 2001-01-23 Robert Roy Cone Percutaneous laser treatment
US6579283B1 (en) * 1998-05-22 2003-06-17 Edward L. Tobinick Apparatus and method employing a single laser for removal of hair, veins and capillaries
US6663659B2 (en) * 2000-01-13 2003-12-16 Mcdaniel David H. Method and apparatus for the photomodulation of living cells
US6344050B1 (en) * 1998-12-21 2002-02-05 Light Sciences Corporation Use of pegylated photosensitizer conjugated with an antibody for treating abnormal tissue
US20020001567A1 (en) * 1998-12-21 2002-01-03 Photogen, Inc. Intracorporeal medicaments for high energy phototherapeutic treatment of disease
US6454789B1 (en) * 1999-01-15 2002-09-24 Light Science Corporation Patient portable device for photodynamic therapy
US6383471B1 (en) * 1999-04-06 2002-05-07 Lipocine, Inc. Compositions and methods for improved delivery of ionizable hydrophobic therapeutic agents
US6609014B1 (en) * 1999-04-14 2003-08-19 Qlt Inc. Use of PDT to inhibit intimal hyperplasia
US20020022032A1 (en) * 1999-04-23 2002-02-21 Curry Patrick Mark Immuno-adjuvant PDT treatment of metastatic tumors
US6102696A (en) * 1999-04-30 2000-08-15 Osterwalder; J. Martin Apparatus for curing resin in dentistry
US6210425B1 (en) * 1999-07-08 2001-04-03 Light Sciences Corporation Combined imaging and PDT delivery system
US6238426B1 (en) * 1999-07-19 2001-05-29 Light Sciences Corporation Real-time monitoring of photodynamic therapy over an extended time
US20040208855A1 (en) * 1999-11-17 2004-10-21 Allison Beth Anne Use of PDT to inhibit intimal hyperplasia
US6443976B1 (en) * 1999-11-30 2002-09-03 Akorn, Inc. Methods for treating conditions and illnesses associated with abnormal vasculature
US6319273B1 (en) * 1999-12-16 2001-11-20 Light Sciences Corporation Illuminating device for treating eye disease
US7166719B2 (en) * 2002-06-27 2007-01-23 Health Research, Inc. Fluorinated photosensitizers related to chlorins and bacteriochlorins for photodynamic therapy
AU2001224721A1 (en) 2000-01-10 2001-08-07 Super Dimension Ltd. Methods and systems for performing medical procedures with reference to projective images and with respect to pre-stored images
WO2001052814A1 (en) * 2000-01-21 2001-07-26 Miravant Medical Technologies Local drug delivery using photosensitizer-mediated and electromagnetic radiation-enhanced vascular permeability
WO2001068162A2 (en) 2000-03-16 2001-09-20 Biovar Life Support Inc. Control of life support systems
GB0007150D0 (en) 2000-03-24 2000-05-17 Lamellar Therapeutics Limited Immunotherapeutic methods and compositions
US20020095197A1 (en) * 2000-07-11 2002-07-18 Lardo Albert C. Application of photochemotherapy for the treatment of cardiac arrhythmias
US6580228B1 (en) * 2000-08-22 2003-06-17 Light Sciences Corporation Flexible substrate mounted solid-state light sources for use in line current lamp sockets
US7409366B1 (en) 2000-08-22 2008-08-05 Etp Holdings, Inc. Apparatus and method for adding liquidity to an ECN and improving executions of orders for securities
US7498034B2 (en) * 2000-11-06 2009-03-03 Cancer Research Technology Limited Imaging, diagnosis and treatment of disease
FR2818159B1 (en) 2000-12-15 2003-10-03 Franco Belge Combustibles PROCESS AND DEVICE FOR DECOLMATING A FILTER OF A PLANT FOR THE PRODUCTION OF URANIUM OXIDE FROM URANIUM HEXAFLUORIDE
US20020173780A1 (en) * 2001-03-02 2002-11-21 Altshuler Gregory B. Apparatus and method for photocosmetic and photodermatological treatment
ES2252423T3 (en) * 2001-01-22 2006-05-16 Eric Larsen PHOTODYNAMIC STIMULATION DEVICE.
US6887862B2 (en) * 2001-05-31 2005-05-03 Miravant Systems, Inc. Method for improving treatment selectivity and efficacy using intravascular photodynamic therapy
US6827926B2 (en) * 2001-05-31 2004-12-07 Miravant Pharmaceuticals, Inc. Metallotetrapyrrolic photosensitizing agents for use in photodynamic therapy
DE60219627T2 (en) * 2001-06-04 2008-02-07 The General Hospital Corp., Boston IDENTIFICATION AND THERAPY OF SENSITIVE PLAQUE WITH PHOTODYNAMIC COMPOUNDS
AU2002310351A1 (en) * 2001-06-11 2002-12-23 Cavalier Discovery Accelerators for increasing the rate of formation of free radicals and reactive oxygen species
WO2003007944A1 (en) * 2001-07-20 2003-01-30 Qlt, Inc. Treatment of macular edema with photodynamic therapy
WO2003011286A1 (en) * 2001-07-30 2003-02-13 The Research Foundation Of State University Of New York Core modified porphyrins
US6783541B2 (en) * 2001-11-21 2004-08-31 Miravant Medical Technologies, Inc. Methods for inhibiting or suppressing stenosis of arteriovenous access fistulas and grafts
IL148257A0 (en) * 2001-12-06 2002-09-12 Curelight Ltd Phototherapy for psoriasis and other skin disorders
US7762965B2 (en) * 2001-12-10 2010-07-27 Candela Corporation Method and apparatus for vacuum-assisted light-based treatments of the skin
EP1627662B1 (en) * 2004-06-10 2011-03-02 Candela Corporation Apparatus for vacuum-assisted light-based treatments of the skin
AU2003230808A1 (en) * 2002-04-05 2003-10-27 Candela Corporation High fluence rate activation of photosensitizers for dermatological applications
US20030233138A1 (en) * 2002-06-12 2003-12-18 Altus Medical, Inc. Concentration of divergent light from light emitting diodes into therapeutic light energy
US20040147501A1 (en) * 2002-07-08 2004-07-29 Dolmans Dennis E.J.G.J. Photodynamic therapy
WO2004004546A2 (en) * 2002-07-10 2004-01-15 Angiodynamics, Inc. Endovascular laser treatment device having a fiber tip spacer
EP1539067B1 (en) * 2002-07-17 2011-11-30 Novadaq Technologies Inc. Combined photocoagulation and photodynamic therapy
US20040171601A1 (en) * 2002-07-31 2004-09-02 Dai Fukumura Photodynamic and sonodynamic therapy
US7125406B2 (en) * 2002-09-13 2006-10-24 Given Kenna S Electrocautery instrument
US20060231107A1 (en) * 2003-03-07 2006-10-19 Glickman Randolph D Antibody-targeted photodynamic therapy
US10376711B2 (en) * 2003-03-14 2019-08-13 Light Sciences Oncology Inc. Light generating guide wire for intravascular use
US20080269846A1 (en) * 2003-03-14 2008-10-30 Light Sciences Oncology, Inc. Device for treatment of blood vessels using light
CA2523777C (en) * 2003-03-14 2016-05-10 Light Sciences Corporation Light generating device to intravascular use
US7153298B1 (en) * 2003-03-28 2006-12-26 Vandolay, Inc. Vascular occlusion systems and methods
WO2005004737A1 (en) 2003-06-30 2005-01-20 Candela Corporation Endovascular treatment of a blood vessel using a light source
WO2005007003A1 (en) * 2003-07-11 2005-01-27 Reliant Technologies, Inc. Method and apparatus for fractional photo therapy of skin
US7837675B2 (en) * 2004-07-22 2010-11-23 Shaser, Inc. Method and device for skin treatment with replaceable photosensitive window
WO2006036176A1 (en) * 2004-09-24 2006-04-06 Light Sciences Corporation Extended treatment of tumors through vessel occlusion with light activated drugs
US20060067889A1 (en) * 2004-09-27 2006-03-30 Light Sciences Corporation Singlet oxygen photosensitizers activated by target binding enhancing the selectivity of targeted PDT agents
JP2008526319A (en) * 2004-12-30 2008-07-24 ライト、サイエンシーズ、オンコロジー、インコーポレイテッド MEDICAL DEVICE USING FLEXIBLE OPTICAL STRUCTURE AND METHOD FOR MANUFACTURING THE SAME
US7891362B2 (en) * 2005-12-23 2011-02-22 Candela Corporation Methods for treating pigmentary and vascular abnormalities in a dermal region
US20070154538A1 (en) * 2005-12-29 2007-07-05 Ceramoptec Gmbh Removal of fat cells by PDT
US8658633B2 (en) * 2006-02-16 2014-02-25 Massachusetts Eye And Ear Infirmary Methods and compositions for treating conditions of the eye
US7465312B2 (en) * 2006-05-02 2008-12-16 Green Medical, Inc. Systems and methods for treating superficial venous malformations like spider veins
US8057464B2 (en) * 2006-05-03 2011-11-15 Light Sciences Oncology, Inc. Light transmission system for photoreactive therapy
US20070260229A1 (en) * 2006-05-05 2007-11-08 Luis Navarro Method and kit for treatment of varicose veins and other superficial venous pathology
US20080275432A1 (en) * 2006-05-11 2008-11-06 Ceramoptec Industries, Inc. Photodynamic foam composition and sclerosis treatment
KR101456839B1 (en) * 2006-06-30 2014-11-03 유로-셀티큐 에스.에이. Compositions and methods of making a photoactive agent
US20090137996A1 (en) * 2007-11-28 2009-05-28 Debenedictis Leonard C Nonablative and ablative tissue treatment method and device

Patent Citations (3)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US6050990A (en) * 1996-12-05 2000-04-18 Thermolase Corporation Methods and devices for inhibiting hair growth and related skin treatments
US6936044B2 (en) * 1998-11-30 2005-08-30 Light Bioscience, Llc Method and apparatus for the stimulation of hair growth
US6899723B2 (en) * 1999-01-15 2005-05-31 Light Sciences Corporation Transcutaneous photodynamic treatment of targeted cells

Also Published As

Publication number Publication date
US20070299431A1 (en) 2007-12-27
US8470010B2 (en) 2013-06-25
WO2007130465A3 (en) 2008-12-04
US20100210995A1 (en) 2010-08-19

Similar Documents

Publication Publication Date Title
US8470010B2 (en) Systems and methods for treating superficial venous malformations like spider veins
US8535360B2 (en) Systems and methods for treating superficial venous malformations like spider veins
Allison et al. Clinical PD/PDT in North America: an historical review
Wilson Photodynamic therapy for cancer: principles
Messmann et al. Enhancement of photodynamic therapy with 5-aminolaevulinic acid-induced porphyrin photosensitisation in normal rat colon by threshold and light fractionation studies
ES2454974T3 (en) Apparatus for optical inhibition of photodynamic therapy
EP0947222B1 (en) Method of activating photosensitive agents
Roberts et al. Photodynamic therapy of primary skin cancer: a review
KR101244434B1 (en) Laser, laser diode, LED, flexible OLED, with photodynamic, pneumodynamic, sonodynamic, RF alone or synergistic combination therapy for face and body, skin rejuvenation, skin whitening ,photobleaching, control of scar, acne, vascular lesion, precancerous skin lesion , local skin lesion, cellulite , fat reduction, stem cell therapy , hair removal, hair restoration, anti-aging, pain , wound healing in field of spa therapy ,dermatology and plastic surgery
US9149651B2 (en) Non-invasive vascular treatment systems, devices, and methods of using the same
DK2545962T3 (en) irradiation Facilities
US20050080465A1 (en) Device and method for treatment of external surfaces of a body utilizing a light-emitting container
KR20060126470A (en) Photodynamic therapy for local adipocyte reduction
US20140350454A1 (en) Irradiation apparatus
Allison et al. Clinical photodynamic therapy of head and neck cancers—A review of applications and outcomes
JP2002518147A (en) Irradiation of multiple treatment sites inside the tumor to enhance the effect of phototherapy
Allison et al. A clinical review of PDT for cutaneous malignancies
Lane New light on medicine
Qiang et al. Photodynamic therapy for malignant and non-malignant diseases: clinical investigation and application
KR20110138003A (en) Laser, laser diode, led, flexible oled, with photodynamic, pneumodynamic, sonodynamic, rf alone or synergistic combination therapy for face and body, skin rejuvenation, skin whitening ,photobleaching, control of scar, acne, vascular lesion, precancerous skin lesion , local skin lesion, cellulite , fat reduction, stem cell therapy , hair removal, hair restoration, anti-aging, pain , wound healing in field of spa therapy ,dermatology and plastic surgery
JP2007508089A (en) Mammal skin irradiation device
US20090326435A1 (en) Systems and methods for treating superficial venous malformations like varicose or spider veins
Kübler et al. An argon-dye laser system for photodynamic therapy and diagnosis
Theodossy et al. Anaesthetic considerations for patients receiving photodynamic therapy in head and neck surgery
Hendrich et al. Experimental photodynamic laser therapy for rheumatoid arthritis using photosan-3, 5-ALA-induced PPIX and BPD verteporfin in an animal model

Legal Events

Date Code Title Description
DPE2 Request for preliminary examination filed before expiration of 19th month from priority date (pct application filed from 20040101)
121 Ep: the epo has been informed by wipo that ep was designated in this application

Ref document number: 07776629

Country of ref document: EP

Kind code of ref document: A2

NENP Non-entry into the national phase

Ref country code: DE

122 Ep: pct application non-entry in european phase

Ref document number: 07776629

Country of ref document: EP

Kind code of ref document: A2

DPE2 Request for preliminary examination filed before expiration of 19th month from priority date (pct application filed from 20040101)