US20040158302A1

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Publication number: US20040158302A1
Application number: US10/749,719
Authority: US
Inventors: Victor Chornenky; Ali Jaafar
Original assignee: Individual
Current assignee: Individual
Priority date: 2000-05-10
Filing date: 2003-12-31
Publication date: 2004-08-12
Also published as: US6692486B2; US20020045848A1

Abstract

An apparatus and method for stabilization of aneurysm is disclosed. The apparatus comprises an ultraviolet radiation generator for generating UV radiation having a wavelength, strongly absorbed by the DNA and a catheter including means for delivering the ultraviolet radiation to the aneurysm. The distal end of the catheter is placed inside the aneurysm. Stabilization of the aneurysm is achieved by forming a mural arterial thrombus inside the aneurysm. To make irradiation possible, the blood is displaced from the aneurysm by a steady stream of UV radiation transparent fluid. The injury to the endothelium that triggers the thrombus formation is caused by UV radiation delivered to the aneurysm. In several days after intervention the thrombus becomes fully organized, leaving on the inside surface of the aneurysm a thick layer of fibrotic tissue that stabilizes the aneurysm.

Description

FIELD OF THE INVENTION

The present invention relates generally to apparatus and methods for the treatment of vascular disease and particularly to apparatus and method for treatment of cerebral aneurysms, arterial vascular malformations and arterial fistulas using lasers.[0001]

BACKGROUND INFORMATION

Cerebrovascular disease is the third leading cause of death in the United States ranking behind only coronary artery disease and cancer. This disease can take several forms, including but not limited to cerebral aneurysm, arterial venous malformations (AVMs) and arterial fistulas (collectively referred to hereafter as “aneurysms.”) One of the most important forms of this disease is the cerebral aneurysm, which manifest itself as a dilatation, or pouching of the arterial wall. As the disease progresses, the dilatation develops into a distended sac of thinned, stressed arterial tissue with a size of 5 to 10 mm in diameter. If not treated, an aneurysm continues to grow until it ruptures, causing a subarachnoid hemorrhage (that is, bleeding between the middle membrane covering of the brain and the brain itself), severe neurological complications, and, possibly, death.[0002]

The components of the arterial wall that are primarily responsible for its mechanical strength and elasticity are the structural proteins collagen and elastin. Collagen, which serves a protective function, is very extensible and breaks at a stress of about 500 megapascals. Collagen is the substance that gives the artery wall its high resistance to the hemodynamic forces created by the heart pumping the blood through the vessel. Elastin fibers, on the other hand, can stretch to about 250% of their original length and have about 20 times lower modulus of elasticity than collagen. These two proteins cooperate to provide vessels with sufficient strength and flexibility to withstand the continuous pounding and pressure of the blood as it flows through the vessel in response to the beat of the heart.[0003]

A fully developed cerebral aneurysm, however, consists almost entirely of collagen fibers, because the majority of the elastin fibers are fragmented by the distending forces of blood pulsating through the vessel in response to the rhythmic beat of the heart. This loss of elastin fibers is especially true for the top of aneurysm, where the tissue degradation is more advanced than in the base and the sidewalls of the aneurysm. Most ruptures consequently occur at the top, or dome, of the aneurysm. The aneurysm ruptures when its wall become too thin to withstand circumferential stresses imposed by pressure differential between the arterial lumen and the subarachnoid space outside the artery.[0004]

Each year about 30,000 North Americans are diagnosed with a ruptured aneurysm and more than half of them die within the first thirty (30) days thereafter. Diagnosis and successful treatment of an aneurysm prior to its rupture is therefore critical to improving the survivability of a patient to this disease. The fundamental objective in the management of an aneurysm that has not ruptured is to stabilize it, thus avoiding further dilatation or growth. Aneurysm stabilization is currently accomplished by:[0005]

1) Conventional neurosurgical intervention, which cuts off the blood flow from the vessel to the aneurysm by ligating its neck with a metal clip;[0006]

2) Endovascular embolization with metallic or other solid mechanical objects causing thrombosis—clotting—inside the aneurysm; and[0007]

3) Thrombus generation within the aneurysm by heating the blood with a catheter having an insulated heating coil at its distal end.[0008]

An example of the endovascular approach is given in U.S. Pat. No. 5,354,295 entitled “An Endovascular Electrolytically Detachable Wire And Tip For The Formation Of Thrombus In Arteries, Veins, Aneurysms, Vascular Malformations And Arteriovenous Fistulas” issued on Oct. 11, 1994 to Guido Guglielmi at al. In this patent a method of treatment of aneurysms is described, in which an aneurysm is packed with detachable platinum wires, causing blood stagnation and blood clot formation inside the aneurysm. The clot prevents arterial blood from reaching the cavity of the aneurysm and continuing to apply pressure to the wall of the aneurysm and helps to stabilize the aneurysm.[0009]

In U.S. Pat. No. 5,919,187, issued on Jul. 6, 1999 to Guido Guglielmi, and entitled “Method And Apparatus For Endovascular Thermal Thrombosis And Thermal Cancer Treatment,” a method and apparatus for endovascular thermal thrombosis is described. In this version of the endovascular approach to treatment, a thrombus is generated in an aneurysm, arteriovenous malformation (AVM) or fistula by heating the blood with a catheter having an insulated heating coil at its distal end.[0010]

The described methods are not applicable to aneurysms that do not have obviously defined necks (narrow openings between the artery and the aneurysm sac). Such aneurysms can't hold the wires or other emboli inside the cavity. Another shortcoming of the described methods is that the blood clot, formed by blood stagnation inside the cavity or its heating, is relatively weak. The fresh arterial blood, coming into the aneurysm can cause lysis (dissolution) of the clot inside the sac and create a chance that a piece of wire or a piece of clot can be displaced from the aneurysm into the blood stream and embolize distally.[0011]

A new treatment is needed that is free from these shortcomings and will improve the stabilization of aneurysms by improved methods and apparatus. The present invention provides an apparatus and method that stabilizes aneurysms of different shapes and produces a clot that is much more resistant to wash out by the blood flow.[0012]

SUMMARY OF THE INVENTION

The invention is an apparatus and method for forming a mural arterial thrombus, that is, a thrombus grown on and attached to the vascular wall inside a cerebral aneurysm, with emphasis on the formation of the arterial thrombus on the inner surface of the dome and the neck of the aneurysm.[0013]

In the present invention, formation of the desired arterial thrombus begins with an injury to the endothelium of the vascular wall of the aneurysm. This injury, which triggers the coagulation sequence within an aneurysm, is created by ultraviolet (UV) radiation delivered to the inner surface of the aneurysm by a micro catheter. The micro catheter comprises a steerable guide wire with an optical fiber in it. The proximal end of the optical fiber is coupled to a laser capable of producing (UV) radiation. The distal end of the guide wire, which emits UV radiation scattered in different directions, is placed inside the aneurysm. A dose of UV radiation, sufficient to cause complete necrosis of the endothelium and lead to the formation of the arteriala thrombus, is delivered to the whole surface of the aneurysm.[0014]

Preferrably, the blood is displaced from the aneurysm by a UV radiation transparent fluid, such as saline. Saline for this purpose may be delivered into the aneurysm from a pressurized saline bag or by a pump outside the patient via a plastic micro tube placed over the guide wire. In one implementation of the present invention a soft balloon, secured around the plastic micro tube, temporarily occludes the artery, thus ensuring better transparency inside the aneurysm. After delivery of the appropriate dose of UV radiation, the saline wash is terminated allowing blood to flow again into the aneurysm.[0015]

In another implementation of the invention an optical fiber (or multiple fibers) is placed inside the wall of the plastic micro tube delivering saline to the aneurysm. In this case a conventional guide wire is used for placing the tip of the micro catheter inside the aneurysm, and the blood flow in the feeding artery is not occluded even temporarily. The UV radiation is delivered to the aneurysm wall in the same manner as in the first implementation.[0016]

The foregoing method also may be used for the treatement of AVMs and arterial fistulas.[0017]

The foregoing objects of the invention will become apparent to those skilled in the art when the following detailed description of the invention is read in conjunction with the accompanying drawings and claims. Throughout the drawings, like numerals refer to similar or identical parts[0018]

BRIEF DESCRIPTION OF THE DRAWINGS

FIG. 1 illustrates an apparatus for treatment of cerebral aneurysms in accord with the present invention.[0019]

FIG. 2 is a cross-section taken along viewing plane[0020]2-2 of FIG. 1.

FIG. 3 presents a detailed view of the distal end of a catheter in accord with the present invention.[0021]

FIG. 4 depicts another embodiment of an apparatus for treatment of cerebral aneurysms in accord with the present invention.[0022]

FIG. 5 is a cross sectional view of the embodiment shown in FIG. 4 taken along viewing plane[0023]5-5.

FIGS. 6A, 6B, and[0024]6C shows several stages of treatment of an aneurysm.

FIG. 7 shows the treatment of arterial venous malformations using an apparatus in accord with the present invention.[0025]

DESCRIPTION OF PREFERRED EMBODIMENT

An apparatus[0026]10 for treatment of an aneurysm and in accord with the present invention is schematically shown in FIGS. 1 and 2. Apparatus10 comprises alaser12, asteerable guide wire14, and acatheter16.Catheter16 will be appropriately sized depending upon where in the patient's body a treatment will occur. For treatment of a cerebral aneurysm, which may require navigation through very small blood vessels in the brain,catheter16 will be a microtube in the form of an elongated tube and may include a substantially centrally disposedtubular passage18 defined by awall20 for receivingguide wire14.Catheter16 may, as shown in FIG. 1, also include anexpandable balloon21, which is used for occluding an artery during an interventional surgical procedure.Catheter16 may also include achannel22 disposed in thecatheter wall24 that is influid communication balloon21.

[0027]

Guide wire

14 has a tubular configuration and thus defines a tubular passage30 receiving anoptical fiber32. The rigid proximal end (not shown) of theguide wire14 is connectable to afiber optic connector34, which couples the output of theUV laser12 to thefiber32.Fiber32 is secured substantially coaxially at the center ofguide wire14. Theoptical fiber32 terminates anoptical tip36 disposed at the distal end thereof.

The proximal end of the[0028]

catheter

16 has two

hermetic fluid ports

40 and42 for receiving a fluid from external fluid sources, typically saline.Port40 communicates withballoon21 through thechannel22 in thewall24 ofcatheter16 and serves for inflation of the balloon through the flow of saline from an external source (not shown) through theport40, into thechannel22 and from there intoballoon21. The space between the external surface ofguide wire14 and thewall20 ofcatheter passage18 define a second channel for fluid flow. This second channel communicates withport42, which may also be fluidly connected to an external fluid source such as saline to provide a clear fluid distally ofballoon21 through theholes26.

Referring to FIG. 1, it will be observed that an[0029]

aneurysm

60 has formed at the branch of aparent artery62 into a pair ofdaughter arteries64. Theaneurysm60 includes aneck66, asac68 defining acavity70 lined with endothelial cells, which form the inner wall orsurface72 of an artery (and hence the sac), and adome74.

The catheter is placed in the blood vessel over the guide wire[0030]14 (0.009″ to 0.014″ in diameter). Theguide wire14 has a hollow tubular configuration and according to the present invention is made of a metallic material, though it will be understood that other materials now known or hereafter developed could also find use as a guide wire.

To provide the desired flexibility,[0031]

fiber

32 has diameter of about fifty (50) micrometers or less and preferably in a range of about twenty-five (25) to about fifty (50) micrometers.Fiber32 is preferably a multimode fiber made of fused silica adapted for the efficient transmission of UV radiation. Theoptical tip36 is transparent (or translucent) for the UV radiation and is made, for example, of sapphire or fused silica. The surface of theoptical tip36 is mated to thefiber32 and configured so as to diffuse UV light in the forward and side directions to better illuminate theinner surface72 of theaneurysm60. The UV radiation propagates in theoptical fiber32 from its proximal end to the distal end which is terminated with theoptical tip36. Theoptical tip36 scatters the radiation in different directions to the aneurysm'swall72. Theoptical tip36 is desirably positioned inside theaneurysm60 at different distances from theaneurysm wall72. During irradiation of thedome74 the distance between theoptical tip36 and the inner surface7 is short, ranging from about one down to zero mm while during irradiation of theneck66 theoptical tip36 is placed therewithin.

The laser can be pulsed or continues wave (CW), with the preferred form being a CW Ion Argon laser generating UV radiation with wavelength 257 nm, which is strongly absorbed by the DNA of the endothelial cells. Preferably, the energy source, regardless of its particular embodiment, should generate ultraviolet radiation in the range of about 240 to about 280 nanometers, corresponding to maximum UV absorption in DNA.[0032]

FIG. 3 represents enlarged view of the distal end of the catheter.[0033]

Guide wire

14 is illustrated as a lowprofile metal tube80 withfiber32 disposed thereinside with a spiral,thin wire82 around it, brazed at both ends to themetal tube80. Theoptical tip36 can be secured to the end of thetube80 andfiber32 with an epoxy orother glue84. Wash fluid flow through theholes26 and out of the open end86 of thecatheter16 is illustrated byarrows88.

FIGS. 4 and 5 show another implementation of the present invention. In the embodiment shown in the Figure, a[0034]

catheter

100 is used to deliver the necrotizing UV radiation to theaneurysm60.Catheter100 does not include an expandable balloon to occlude theartery62 and thus can have a simpler construction than the catheter shown in FIGS.1-3.Catheter100 comprises a single elongate tubular member including acentral passage102 defined by aninner wall104.Passage102 receives aguide wire106. Because there is no need to inflate a balloon, there is no need for a separate port and interwall fluid channel such aschannel22 as shown in FIG. 2. Thus,catheter100 includes a single hermetic fluid port10 that receives a wash fluid such as saline from an external source as indicated byarrow112.Port110 is in fluid communication withpassage102, thus providing a flow path from the external fluid source through theport110, through thepassage102 and out of theopen end114 of the distal end of thecatheter100.

[0035]

Catheter

100 further includes one or moreoptical fibers32 disposed within the catheter wall116. Each fiber will include anoptical tip36 at its distal end attached in any known manner. The UV radiation will be delivered to theinner surface72 of the aneurysm by thetips36, each of which will radiate in a substantially semispherical direction in the same manner as the embodiment shown in FIG. 1. UV radiation will be delivered to thefibers32 bylaser12 through theoptical coupler34.

A method of treatment of cerebral aneurysms comprises the steps of: a) inserting a fiber optic guide wire into an artery feeding an aneurysm, with the distal optical tip of the guide wire being placed inside the aneurysm; b) placing a balloon over the wire proximally to the optical tip of the guide wire; c) occluding the artery by inflating the balloon; d) clearing the optical field inside the artery and the aneurysm by delivering steady flow of fluid transparent or substantially transparent to UV radiation; e) activating a UV laser and delivering UV energy on the inside surface of the aneurysm in quantity sufficient for killing 99.9% or more of the endothelial cells on the irradiated surface of the aneurysm.[0036]

FIGS. 6A, 6B, and[0037]6C illustrate generally the treatment of an aneurysm. FIG. 6B shows anartery150 with ananeurysm152. Theaneurysm dome154 reveals athinner vessel wall156 as a result of the distention of thevessel150 at that location. Blood flow is indicated generally byarrow158.

FIG. 6B illustrates the aneurysm following treatment with the present invention. It will be observed that a necrotized[0038]

layer

160 of endothelial cells has been formed following treatment with UV radiation on the inside surface of the aneurysm.

FIG. 6C illustrates the[0039]

aneurysm

152 after the formation of a “real arterial thrombus”164. At the dome the thickness of the aneurysm's wall is the lowest and the probability of rupture is the highest (about 90% of all cerebral aneurysms are ruptured at the dome). Narrowing the neck of the aneurysm causes a decrease in the blood pressure within the aneurysm sac and thus assists in its stabilization. A “real arterial thrombus” significantly differs from a blood clot, as that term is usually used in the described methods of stabilization of aneurysms. The underlying core of the arterial thrombus consists of fibrin and aggregated platelets, which strongly adhere to each other and to the arterial wall. The color of the core is white, so an arterial thrombus is sometimes referred to as a “white thrombus”. The margin or exterior layer of the arterial thrombus consists of coagulated blood and is red. Arterial thrombi form at the site of an injury to the endothelium, which exposes the highly thrombogenic connective tissue underlying the endothelial layer to the blood flow. This connective tissue, primarily collagen, causes activation of platelets, leading to the formation of a thrombus.

Necrotic endothelial cells are not able to produce tissue plasmogen activator t-PA, major function of which is preventing thrombus formation on the vessel walls, and cannot stay attached to the the vessel wall surface. As they are flaked off and carried away by the blood flow, the highly thrombogenic underlying layer consisting of collagen is exposed. Platelets from blood, activated at the denuded from endothelium surface of the aneurysm, start aggregation and the whole sequence of arterial thrombus formation on the irradiated surface of the aneurysm is launched. In several days after intervention the thrombus, contracted in volume and ingrown by capilaries and fibroblasts, becomes organized. The fully organized thrombus on the inside surface of the aneurysm leaves a thick layer of fibrotic tissue, covered with a newly restored endothelial layer, thereby stabilizing the aneurysm against rupture and further thrombosis.[0040]

The energy fluence, required for causing necrosis of the endothelial cells, falls in the range of several units to several hundreds of mJ/cm2, that is, within a range of about 5 to about 1000 mJ/cm2. The time required for achieving full necrosis of endothelial cells with a milliwatt UV laser, falls in the range of about 10 seconds to several minutes. It will be understood that the time period over which irradiating of the aneurysm with UV energy occurs is inversely dependent upon the applied energy. As the power of the applied radiation decreases, the duration of time over which the energy must be applied to cause the desired cell death increases and vice versa. An Argon ion laser, generating UV radiation with wavelength 257 nanometers or a Nd-YAG laser generating radiation with a wavelength 256 nanometers (the fourth harmonic of the infrared wavelength 1.06 microns) is just two examples of UV radiation sources that can be used in accord with the present invention.[0041]

Without functioning endothelial cells the aneurysm's inner wall becomes highly thrombogenic, triggering formation of thrombus on it and coagulation of the blood in the sac of the aneurysm. After organization of the thrombus the inner wall of the aneurysm will be covered with a thick layer (several hundred microns) of a collagen rich fibrous tissue. For a normal artery the thickening of its wall is a negative event. It results in a loss of patency and flexibility of the vessel. But for an aneurysm the thickening of the wall decreases actual tensile stresses in it and arrests the growth of the aneurysm. It follows from a well-known fact that circumferential stress, responsible for the aneurysm rupture, is inversely proportional to the aneurysm wall thickness:[0042]

S=PR/2h

where[0043]

S=Circumferential Stress;[0044]

P=Blood Pressure;[0045]

R=Radius of the Aneurysm; and[0046]

h=Thickness of the Aneurysm Wall.[0047]

A several time increase in wall thickness causes a several time drop in the stresses. The formula is taken from “The Physics of Cerebrovascular Disease” by George J. Hademenos and Tarik F. Massoud, Springer-Verlag, 1998, ISBN 1-56396-558-5.[0048]

The critical thickness of a saccular aneurysm, at which a rupture Occurs, is around 40-50 microns. The thickness of a fibrous layer after full organization of thrombus reaches several hundred microns, thus warranting stabilization of the aneurysm after treatment with UV radiation.[0049]

FIG. 7 schematically illustrates treatment of an arterial venous malformation (AVM)[0050]120 in accord with the present invention. AVMs are massive blood formations wherein one or more feeding arteries provide blood to the mass, which is then drained by one or more draining arteries without the blood ever being supplied to the tissue, typically cerebral tissue. The formation of the AVM, then, results in starvation of the surrounding tissues because of the diversion of the fresh arterial blood from the tissue by the AVM. As shown in the figure,guide wire14 with anoptical fiber32 inside is advanced through afeeding artery122 toAVM120. Theoptical tip36 of thefiber32 is placed into a shunting arteriole124 of theAVM120. Theballoon21 inflates and occludes theartery122. Saline flow distally to theballoon21 clears thefeeder122 and proximal part ofAVM120 from blood. TheUV laser12 is turned on and the feeder's wall and adjacent vessels of the AVM are irradiated by UV radiation emitted by theoptical tip36. This procedure is repeated with all feeding arteries of the AVM. After blood flow is restored, arterial thrombi are formed in the AVM and adjacent feeders. The thrombus after organization causes stenosis or closing of the feeders, significantly decreasing blood flow through the AVM and out through the drainingvessels126

It will be understood that the present invention can also be used to treat arterial fistulas in the same manner as previously described with reference to aneurysms and AVMs.[0051]

It will be obvious to those skilled in the art that many modifications may be made within the scope of the present invention without departing from the spirit of thereof, and the invention includes all such modifications. For example, it will be understood that other sources of ultraviolet radiation now available or hereafter developed could provide the necessary ultraviolet radiation and that the use of a laser is not required by the present invention, though with current technology it is preferred.[0052]

Claims

What is claimed is:

1. An apparatus for treatment of cerebral aneurysms and AVMs, comprising: a laser generating ultraviolet radiation; a steerable guide wire having an optical fiber inside it, said fiber extended from the proximal to the distal end of the guide wire and at the proximal end coupled to the laser; an over-the-wire catheter having an occlusive balloon and a micro tube adapted for delivery of saline distally to the balloon for displacing blood from the aneurysm or AVM and clearing the optical field in front of the distal end of the optical fiber.

2. The apparatus ofclaim 1, in which the laser generates UV radiation in the range of 240 to 280 nanometers, corresponding to maximum UV absorption in DNA.

3. The apparatus ofclaim 1, in which the distal end of the fiber is coupled to an optical tip adapted for scattering UV radiation in different directions for complete irradiation of the inner surface of the aneurysm.

4. An apparatus for treatment of aneurysms comprising: a laser generating ultraviolet radiation; a steerable guide wire; an over-the-wire catheter having at least one optical fiber inside its wall, the proximal end of said fiber coupled to the laser, the distal end extended to the distal end of the micro catheter, said micro catheter adapted for delivery of saline for displacing blood from the aneurysm or AVM and clearing the optical field in front of the distal end of the optical fiber.

5. The apparatus ofclaim 4, in which the laser generates UV radiation in the range of 240 to 280 nanometers, corresponding to maximum UV absorption in DNA.

6. The apparatus ofclaim 4, in which the distal ends of the fibers are coupled to optical tips adapted for scattering UV radiation in different directions for complete irradiation of the inner surface of the aneurysm.

7. A method of treatment of aneurysms comprising the steps: inserting a fiber optic guide wire into the artery feeding an aneurysm, the distal tip of the guide wire being placed inside the aneurysm; placing a catheter with an occlusive balloon and micro tube over the wire, the distal end of the tube just proximally to the optical tip of the guide wire; occluding the artery by the balloon; clearing the optical field inside the artery and the aneurysm by delivering steady flow of saline; activating a UV laser and delivering UV radiation on the whole inside surface of the aneurysm in quantity sufficient for killing 99.9% or more of the endothelial cells on the irradiated surface of the aneurysm.

8. A method of treatment of cerebral aneurysms and AVMs, comprising the steps: inserting a guide wire into the artery feeding an aneurysm or AVM, the distal tip of the guide wire being placed inside the aneurysm or AVM; placing a micro tube catheter over the wire, the distal end of the tube just proximally to the tip of the guide wire; clearing the optical field inside the artery and the aneurysm by delivering steady flow of saline; activating a UV laser and delivering UV radiation on the whole inside surface of the aneurysm in quantity sufficient for killing 99.9% or more of the endotlhelial cells on the irradiated surface of the aneurysm.

9. Apparatus for treatment of aneurysms comprising: an ultraviolet radiation generator; and a catheter including means for delivering the ultraviolet radiation to the aneurysm.

10. The apparatus ofclaim 9 wherein said catheter includes a passage and where said means for delivering comprises: a guide wire received within said passage and movable therein, said guide wire having an optical fiber inside it, said fiber extended from the proximal to the distal end of the guide wire and at the distal end coupled to said generator.

11. The apparatus ofclaim 10 wherein said catheter further includes an over-the-wire catheter having an occlusive balloon and a micro tube adapted for delivery of an ultraviolet transparent wash fluid distally to the balloon for displacing blood from the aneurysm to clear the optical field in front of the distal end of the optical fiber.

12. The apparatus ofclaim 11 wherein said ultraviolet radiation generator generates UV radiation in the range of about 240 to about 280 nanometers:.

13. The apparatus ofclaim 10 wherein said fiber includes a distal end and said fiber distal end is coupled to an optical tip adapted for scattering UV radiation in different directions for complete irradiation of the inner surface of the aneurysm.

14. The apparatus ofclaim 10 wherein said guide wire is steerable.

15. The apparatus ofclaim 9 wherein said ultraviolet radiation generator is a laser.

16. The apparatus ofclaim 9 wherein said catheter includes a wall and a passage and a guide wire received within said passage and movable therein and wherein said means for delivering comprises at least one optical fiber, said at least one optical fiber disposed in said catheter wall.

17. The apparatus ofclaim 16 wherein said generator generates UV radiation in the range of about 240 to about 280 nanometers.

18. The apparatus ofclaim 17, wherein said at least one optical fiber has a distal end and wherein said apparatus further comprises an optical tip adapted for scattering UV radiation in different directions for complete irradiation of the inner surface of the aneurysm.

19. A method of treatment of an aneurysm, comprising the steps: inserting a fiber optic guide wire having an optical tip into the artery feeding the aneurysm, the distal tip of the guide wire being placed inside the aneurysm; and clearing the optical field inside the artery and the aneurysm by delivering a wash fluid transparent to UV radiation to displace the blood activating a UV laser and delivering UV radiation on the whole inside surface of the aneurysm in quantity sufficient for killing 99.9% or more of the enclotheliell cells on the irradiated surface of the aneurysm.

20. The method ofclaim 19 and further comprising: placing a catheter with an occlusive balloon just proximally to the optical tip of the guide wire; and occluding the artery by the balloon.

21. The method ofclaim 19 wherein the wash fluid is saline.