CN214050144U - End medicine coating balloon component and medical instrument comprising same - Google Patents

End medicine coating balloon component and medical instrument comprising same Download PDF

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Publication number
CN214050144U
CN214050144U CN202021059439.9U CN202021059439U CN214050144U CN 214050144 U CN214050144 U CN 214050144U CN 202021059439 U CN202021059439 U CN 202021059439U CN 214050144 U CN214050144 U CN 214050144U
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balloon
assembly
pharmaceutical composition
balloon assembly
catheter
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CN202021059439.9U
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Chinese (zh)
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丁海雁
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Qiwei Medical Technology Shenzhen Co ltd
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Individual
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Abstract

The application provides a medicine balloon subassembly is scribbled to tip and contains its medical instrument, the medicine balloon subassembly is scribbled to tip includes: a balloon catheter and a balloon disposed on the balloon catheter, the balloon having a front end and a rear end in a longitudinal direction, an outer surface of at least one of the front end and the rear end being provided with a pharmaceutical composition or a layer of a pharmaceutical composition, the layer of a pharmaceutical composition having a thickness of 1 to 100 microns, such as 10 to 75 microns. The tip medicine coating sacculus that this application is disclosed combines current apparatus to handle the fistula, can realize that interatrial fistula is continuous open, prevents that interatrial fistula is just closed naturally in short-term, reaches the effect that reduces heart preload, treatment heart failure for a long time.

Description

End medicine coating balloon component and medical instrument comprising same
Technical Field
The utility model belongs to the technical field of the medical treatment technique and specifically relates to a sacculus subassembly and contain its medical instrument are scribbled to tip.
Background
Interatrial septum fistulation is a well established technique in patients with advanced pediatric congenital heart disease, pulmonary hypertension. It is also applied to patients with diastolic dysfunction, heart failure and systolic dysfunction with continuous elevation of PCWP, and has a remarkable effect, but it is not formally developed clinically. The current research shows that the fistula can be naturally healed after 6 months no matter a stent is placed in the fistula or not after the interatrial fistula is made, so that the operation effect is greatly reduced. Therefore, how to avoid the natural closure of the fistula in a short period is the key to ensure the final treatment effect of the interatrial septum ostomy.
SUMMERY OF THE UTILITY MODEL
The heart medicine balloon is a new technology, and the medicine is uniformly distributed on the blood vessel wall by implanting the special balloon coated with paclitaxel, so as to inhibit the hyperplasia of the blood vessel endothelium and smooth muscle and prevent restenosis. The cardiac drug balloon can solve the problem of vascular stenosis without implanting a stent, and is an emerging treatment method. However, the existing drug balloons are designed for preventing the endothelial hyperplasia of coronary arteries and peripheral large blood vessels, and no balloon specially for healing the fistula, particularly the interatrial fistula with the thickness of only 2-3 mm is provided.
The application discloses give medicine and use sacculus subassembly combines current apparatus to handle the fistula, can realize that interatrial fistula is continuous open, solves the problem of interatrial fistula in short-term just closed naturally to reach the long-term purpose that reduces heart preload, treatment heart failure.
The technical scheme disclosed by the application comprises the following implementation modes:
embodiment 1, an end-on drug balloon assembly, comprising: a balloon catheter and a balloon disposed on the balloon catheter, the balloon having a front end and a rear end in a longitudinal direction, an outer surface of at least one of the front end and the rear end being provided with a pharmaceutical composition or a layer of a pharmaceutical composition, the layer of a pharmaceutical composition having a thickness of 1 to 100 microns, such as 10 to 75 microns.
Embodiment 2 the balloon assembly of embodiment 1, wherein the drug composition layer is disposed on an outer surface of only one of the leading end portion and the trailing end portion.
Embodiment 3 the balloon assembly of embodiment 1, wherein the balloon catheter has a guidewire through-hole and a pressurizing liquid channel, wherein the pressurizing liquid channel is in communication with the balloon interior.
Embodiment 4 the balloon assembly of embodiment 1, wherein the balloon is disposed at a front portion of the balloon catheter, the balloon front end being about 5 to 20mm from the balloon catheter front end.
Embodiment 5, the balloon assembly of embodiment 1 or 2, wherein the drug composition layer is disposed only on a portion having a diameter greater than 2mm where the outer surface of the balloon is disposed, and the drug composition layer is not disposed on the other outer surface of the balloon.
Embodiment 6 the balloon assembly of embodiment 1, wherein the longitudinal cut of the outer surface provided with the pharmaceutical composition does not have a concave arc-shaped profile, e.g., the longitudinal cut of the outer surface provided with the pharmaceutical composition has a circular arc shape, an elliptical arc shape, a parabolic shape, a linear shape, a polygonal shape, an irregular curved shape, or a combination of two or more thereof.
Embodiment 7 the balloon assembly of embodiment 1, wherein the pharmaceutical composition comprises at least one of paclitaxel and rapamycin, and optionally a pharmaceutical carrier.
Embodiment 8 the balloon assembly of any one of embodiments 1-7, wherein the balloon has a radial dimension when expanded of 6-25mm, e.g., 8 to 20mm, e.g., 10 to 20mm, e.g., 12 to 20mm, e.g., 14 to 20mm, e.g., 16 to 20mm, e.g., 18 to 20 mm.
Embodiment 9, the balloon assembly of any one of embodiments 1-7, wherein the balloon is a non-compliant balloon, a compliant balloon, or a semi-compliant balloon.
Embodiment 10, a medical device, in particular for percutaneous interatrial ostomy intervention, comprising a balloon assembly according to any of embodiments 1-9.
The technical scheme disclosed by the application also comprises the following scheme:
scheme 1, a balloon assembly for administration, comprising: the balloon catheter comprises a balloon catheter and a balloon arranged on the catheter, wherein the longitudinal section of the balloon has a concave arc-shaped profile when the balloon is fully expanded. In some aspects, a pharmaceutical composition or a layer of a pharmaceutical composition is disposed on an outer surface of the region having the concave arc-like profile. The thickness of the layer of the pharmaceutical composition is from 1 micron to 100 microns, for example from 10 to 75 microns.
Scheme 2, the balloon assembly for administration of claim 1, wherein the concave arc-like profile is formed in at least one of a longitudinal front portion, a longitudinal rear portion, and a longitudinal middle portion of the balloon.
Scheme 3, the balloon assembly for administration according to scheme 1, wherein the balloon catheter has a guide wire through hole and a pressurizing liquid channel, wherein the pressurizing liquid channel communicates with the inside of the balloon.
Scheme 4, the balloon assembly for administration according to scheme 1, wherein the balloon is disposed at the front of the balloon catheter, and the distance from the front end of the balloon to the front end of the balloon catheter is about 5 to 20 mm.
The balloon assembly for drug administration according to claim 5 or 1, wherein the concave arc-like profile is formed at a longitudinal front portion and/or a longitudinal rear portion of the balloon, and the concave arc-like profile starts from a position radially close to the balloon catheter to end at a radially middle portion of the balloon.
Scheme 6, the balloon assembly for administration according to scheme 1, wherein the longitudinal dimension of the balloon is 2/3 or less (1/2 or less) of its radial dimension, such that when the balloon is folded, the area with the concave arc-shaped profile is mostly folded inside, thereby avoiding loss of the drug during pushing of the balloon assembly.
Scheme 7 the balloon assembly for administration according to scheme 1, wherein the pharmaceutical composition comprises at least one of paclitaxel and rapamycin, and optionally a pharmaceutical carrier. The drug carrier comprises a hydrophilic drug carrier.
The balloon assembly for administration according to any one of claims 8 and 1 to 7, wherein the balloon assembly includes two balloons, the concave arc-shaped profile of one balloon is formed at a longitudinal front portion of the balloon, and the concave arc-shaped profile of the other balloon is formed at a longitudinal rear portion of the balloon.
Scheme 9, the balloon assembly for administration of any of schemes 1-8, wherein the balloon is a non-compliant balloon, a compliant balloon, or a semi-compliant balloon.
Scheme 10, a medical device, in particular for percutaneous interatrial ostomy intervention, comprising a balloon assembly according to any of schemes 1-9.
The technical scheme of this application combines current apparatus (for example cutting sacculus etc.) to handle the fistula, can realize dosing interatrial fistula and surrounding part, especially can make interatrial fistula continuously open, solves the problem that interatrial fistula is closed with regard to nature in short-term to reach the long-term purpose that reduces heart preload, treatment heart failure.
Drawings
To more clearly illustrate the technical solutions of the embodiments of the present disclosure, the drawings of the embodiments will be briefly introduced below, and it is apparent that the drawings in the following description relate only to some embodiments of the present disclosure and are not limiting to the present disclosure.
FIG. 1 shows a schematic view of the balloon assembly of example 1;
FIG. 2 shows a schematic view of the front end of the balloon assembly of example 1 with a drug composition disposed thereon;
fig. 3 shows a schematic view of the back end of the balloon assembly of example 2 with a drug composition disposed thereon;
FIG. 4 shows a schematic view of the front end of the balloon assembly of example 4 with a drug composition disposed thereon;
FIG. 5 shows a schematic view of another embodiment of the balloon assembly;
FIG. 6 shows a schematic view of another embodiment of the balloon assembly;
FIG. 7 shows a schematic view of another embodiment of the balloon assembly;
FIG. 8 shows a schematic view of another embodiment of the balloon assembly;
FIG. 9 shows a schematic view of another embodiment of the balloon assembly;
fig. 10 shows a schematic view of another embodiment of the balloon assembly.
Reference numerals: 1-balloon catheter, 11-balloon catheter front end, 12-balloon catheter front portion, 13-guide wire through hole, 14-pressurizing liquid channel, 2-balloon, 21-balloon front end, 22-front end portion, 23-back end portion, 3-pharmaceutical composition.
Detailed Description
In order to make the objects, technical solutions and advantages of the embodiments of the present disclosure more apparent, the technical solutions of the embodiments of the present disclosure will be described clearly and completely with reference to the drawings of the embodiments of the present disclosure. It is to be understood that the described embodiments are only a few embodiments of the present disclosure, and not all embodiments. All other embodiments, which can be derived by a person skilled in the art from the described embodiments of the disclosure without any inventive step, are within the scope of protection of the disclosure.
The following terms in this application have the specific meanings:
the direction along the catheter is defined herein as "longitudinal" and the direction perpendicular to the catheter is defined herein as "radial" and the balloon expands primarily in the radial direction.
In the present application, a portion which first reaches the region to be processed when used is defined as "front", and an orientation opposite to "front" is defined as "rear".
In this application, "end" and "section" and "end" are used to describe the balloon and various portions of the balloon catheter, where "end" refers to a defined end point or end surface, "section" is used to describe a range of regions, and "end" is used to describe a range of regions on the end surface.
For example, the "leading end" of a balloon catheter means that the balloon catheter first reaches the end point or end surface of the area to be treated when in operation, and the "leading end" of a balloon means that the balloon first reaches the end point or end surface of the area to be treated when in operation.
For example, the "front" of a balloon catheter refers to a range of the balloon catheter relative to the distal end of the operator, and the "longitudinal front", "longitudinal middle", and "longitudinal back" of the balloon refer to three regions of the balloon body ranging from the distal end to the proximal end relative to the operator in the direction of the balloon catheter, for example, the front refers to front 1/4, the back refers to back 1/4, and the middle refers between front 1/4 and back 1/4.
For example, the "leading end portion" of the balloon means that the balloon reaches the end face of the region to be treated first when it is operated, i.e., the region ranging from the leading end point of the balloon to the radially outermost end point of the balloon expansion. The "rear end portion" of the balloon means a portion opposite to the "front end portion", i.e., a region ranging from the radially outermost point of the balloon expansion to the balloon rear end point.
In the present application, each term has a meaning commonly understood in the art unless otherwise indicated or otherwise clearly understood from the context.
The application discloses sacculus subassembly is scribbled to tip, it includes: a balloon catheter and a balloon disposed on the balloon catheter, the balloon having a front end and a rear end in a longitudinal direction, an outer surface of at least one of the front end and the rear end being provided with a pharmaceutical composition or a layer of a pharmaceutical composition, the layer of a pharmaceutical composition having a thickness of 1 to 100 microns, such as 10 to 75 microns. Therefore, when the end part is contacted with the interatrial fistula and the surrounding area, the medicine can directly act on the area to be treated, so that the medicine can be conveniently applied to the fistula, and a better treatment effect is achieved. The application also provides a sacculus subassembly is scribbled to tip, and it includes: a balloon catheter and a balloon disposed on the balloon catheter, the balloon having a radial dimension when expanded of 6-25mm, such as 8 to 20mm, such as 10 to 20mm, such as 12 to 20mm, such as 14 to 20mm, such as 16 to 20mm, such as 18 to 20 mm. In some embodiments, the balloon has a leading end and a trailing end in the longitudinal direction, an outer surface of at least one of the leading end and the trailing end having disposed thereon a drug composition or a layer of a drug composition having a thickness of from 1 micron to 100 microns, such as from 10 to 75 microns. The present application uses parameters common in the art for the length of the balloon catheter, which is typically 1.8F-2.0F in diameter, and in some cases may be selected in the range of 1.0F to 6.0F. The unit F here has the meaning generally understood by those skilled in the art, 1F means a catheter having a circumference of 1 mm, 1.8F means a catheter having a circumference of 1.8 mm, and 2.0F means a catheter having a circumference of 2.0 mm.
In some embodiments, a pharmaceutical composition is disposed on an outer surface of only one of the front end portion and the back end portion. When the balloon is expanded in the heart, only the outer surface of one end part is loaded with the medicine, the end part loaded with the medicine acts on the fistula, and compared with the arrangement of the medicine compositions on the outer surfaces of the two end parts, the arrangement can reduce the medicine release amount to the maximum extent, thereby reducing the toxic and side effects.
In some embodiments, the balloon catheter has a guidewire through hole and a pressurizing liquid channel, wherein the pressurizing liquid channel is in communication with the balloon interior. The arrangement of the guide wire through hole can lead the balloon catheter to reach the selected area to be treated along the guide wire under the guide of the guide wire for treatment. The pressurizing liquid channel is used for injecting or extracting pressurizing liquid into or from the saccule, after the saccule reaches a target area, the pressurizing liquid is injected into the pressurizing liquid channel, the saccule is expanded under the action of hydraulic pressure, when the pressurizing liquid is extracted after administration treatment is finished, negative pressure is generated in the saccule, and the contraction and folding of the saccule are finished under the action of the negative pressure. Typically, for accurate positioning, markers (marker materials) are also provided inside the balloon, which are used to help an external device detect its position within the patient. In the present application, the selection of the balloon position marker is not particularly limited as long as the balloon position can be accurately positioned.
In some embodiments, the balloon is disposed at the front of the balloon catheter, and the distance from the front end of the balloon catheter is about 5 to 20 mm.
In some embodiments, the drug composition layer is disposed only on portions of the balloon having a diameter greater than 2mm where the outer surface of the balloon is disposed, and the drug composition layer is not disposed on other outer surfaces of the balloon. The "portion having a radius of more than 2 mm" as used herein refers to a specific outer surface area of the front end portion and/or the rear end portion, the perpendicular distance from any point in the specific outer surface area to the center line of the catheter being more than 2 mm. The drug composition is only arranged on the specific outer surface area, the specific outer surface area is overlapped with the drug administration area of the fistula to be treated and is in maximum contact with the drug administration area, the drug administration efficiency is improved, all the drugs act on the fistula, the minimal dose of drug application can be realized, and the toxicity generated by drug release in non-target areas is reduced. It should be understood that the above range for disposing the pharmaceutical composition is not a limitation on the end coating range of the balloon disclosed in the present invention, and one skilled in the art can select a suitable range for disposing the pharmaceutical composition according to actual needs, for example, a suitable end outer surface coating radius range, for example, greater than 2.5mm, for example, greater than 3mm, for example, greater than 3.5mm, for example, greater than 4mm, according to the fistula diameter. In interatrial fistulization intervention, the fistula expansion diameter that adopts trilateral fixed blade cutting sacculus is about 5mm, combines other sacculus to reach 12mm the most, according to congenital heart disease's clinical treatment experience, reaches the target size promptly when the fistula diameter is about 5 ~ 8mm, can effectively reduce left atrium pressure.
The shape of the longitudinal section of the outer surface provided with the pharmaceutical composition is not particularly limited, and in some embodiments, the longitudinal section of the outer surface provided with the pharmaceutical composition has a concave arc-shaped profile, a circular arc shape, an elliptical arc shape, a parabolic shape, a linear shape, a polygonal shape, an irregular curved shape, or a combination of two or more thereof. In some embodiments, the longitudinal cut of the outer surface provided with the pharmaceutical composition does not have a concave arc-shaped profile, e.g., the longitudinal cut of the outer surface provided with the pharmaceutical composition has a circular arc shape, an elliptical arc shape, a parabolic shape, a linear shape, a polygonal shape, an irregular curved shape, or a combination of two or more thereof. In the present application, the term "longitudinal section" refers to a section along the direction of the catheter, and the term "concave arc" refers to an arc surface of the balloon opposite to the direction of expansion of the balloon when the balloon is expanded. The arc shape, the elliptic arc shape and the parabola shape in the application all refer to a convex shape of the saccule which has the same expansion direction with the saccule when the saccule is expanded, and do not contain a concave arc shape. The different contour shapes of the longitudinal sections of the outer surface of the medicinal composition can enable the end part of the balloon to generate different fitting effects with the fistula and the area around the fistula. One skilled in the art can select different balloons depending on the surface shape of the stoma and the area surrounding the stoma.
In some embodiments, the pharmaceutical composition comprises at least one of paclitaxel and rapamycin, and optionally a pharmaceutical carrier. The drug carrier preferably comprises a hydrophilic drug carrier and/or a hydrophobic drug carrier. In some embodiments, the hydrophilic drug carrier is at least one selected from the group consisting of iopamidol and iopromide. The existing drug-coated balloon (DCB) interventional therapy technology attaches drugs for inhibiting cell proliferation on the surface of the balloon, attaches the drug surface to the interatrial fistula and the periphery by expanding the balloon, and transmits the drugs to a target point so as to achieve the effect of inhibiting smooth muscle proliferation. Paclitaxel and rapamycin have the function of inhibiting cell proliferation, and are widely applied to the field of coronary artery and peripheral interventional therapy in clinic, the two drugs are lipophilic drugs, the lipophilic drugs paclitaxel and/or rapamycin and the hydrophilic drug carrier iopamidol and/or iopromide are combined randomly to form the pharmaceutical composition, and the hydrophilic drug carrier can form a porous coating with a high contact surface between lipophilic drug molecules and a blood vessel wall, so that the dissolution and release of the lipophilic drug molecules are enhanced, and the drug delivery and the interaction between the lipophilic drug molecules and tissues can be changed. The pharmaceutical composition is loaded on the surface of the front end part and/or the rear end part of the balloon component disclosed in the application as a balloon coating, after the balloon is expanded, the front end part and/or the rear end part loaded with the pharmaceutical composition is completely contacted with an area to be treated, the target drug dose is uniformly and rapidly released, and clinical experience shows that the short contact time of 30 seconds to 70 seconds is enough to inhibit cell proliferation and prevent peripheral endothelial crawl and fistula natural healing.
In some embodiments, the balloon has a radial dimension when expanded of 6-25mm, such as 8 to 20mm, such as 10 to 20mm, such as 12 to 20mm, such as 14 to 20mm, such as 16 to 20mm, such as 18 to 20 mm. In the present application, the distance between two end points in the radial direction during the balloon expansion is the radial dimension, the size of the radial dimension determines the size of the drug-loaded region, and those skilled in the art can select an appropriate radial dimension according to the range of the region to be treated around the fistula. In addition, the larger radial dimension may ensure that the balloon end-loaded drug composition is encapsulated inside when the balloon is folded, thereby avoiding drug loss due to dissolution during the balloon assembly push.
In some embodiments, the balloon is a non-compliant balloon, a compliant balloon, or a semi-compliant balloon. Compliance of the balloon as described herein refers to the characteristic of the balloon profile or volume change that occurs with each increase in atmospheric pressure (atm) when the balloon is inflated, and is an indicator of the ability of the balloon to stretch. Three different types of balloons employed in this application possess different characteristics: the balloon diameter of the compliant balloon increases with increasing pressure, the compliant balloon dispersing the inflation pressure; the non-compliant balloon means that no matter how much the diameter of the pressure balloon is added, the diameter of the pressure balloon keeps unchanged after reaching the specified size, the expansion pressure of the non-compliant balloon is intensively acted on a treatment part, and the non-compliant balloon has weak adaptability to blood vessels; the semi-compliant balloon has a wide working range, can flexibly control the size of the balloon, and is mainly used for pre-expansion. In practical application, a person skilled in the art can select different balloons according to actual needs to achieve the optimal technical effect. The materials and methods for making the balloon assembly are not particularly limited and may be selected by one skilled in the art according to actual needs.
Another aspect of the present application provides a medical device comprising a balloon assembly according to any of the other embodiments described herein. In particular, another aspect of the present application provides a medical device for percutaneous interatrial ostomy intervention comprising a balloon assembly according to any of the other embodiments described herein.
In the present application, the material and method for producing the balloon assembly are not particularly limited as long as specific operational requirements can be satisfied.
The balloon and balloon catheter may be made from polyamide (e.g., nylon 66, nylon 12, etc.), polyether amide block copolymers. The method of preparing the balloon catheter may employ various methods known in the art. The balloon may be formed by blow molding. A marker material, typically a platinum iridium alloy, is disposed at the catheter in the balloon. The balloon and the catheter can be bonded together by hot melting, or can be bonded by using a suitable adhesive.
The application also discloses a method of treating an interatrial fistula, comprising:
1. make this application the sacculus and interatrial fistula go on contacting to administer to interatrial fistula and periphery.
2. Administration is made to both sides of the interatrial septum fistula.
The ranges described above may be used alone or in combination. The present application can be more easily understood by the following examples.
Examples
Example 1 [ circular arc, distal end portion coating agent ]
As shown in fig. 1, the present application discloses an end-dosing balloon assembly comprising: the balloon catheter comprises a balloon catheter 1 and a balloon 2, wherein the balloon 2 is arranged at the front part 12 of the balloon catheter, and the distance between the front end 21 of the balloon and the front end 11 of the balloon catheter is 5 mm. The balloon 2 has a front end 22 and a rear end 23 in the longitudinal direction, and the longitudinal section of the outer surfaces of the front end 22 and the rear end 23 is circular arc-shaped. The balloon 2 has a radial dimension of 18mm when expanded, the balloon catheter 1 has a diameter of 1.8F, the balloon catheter 1 has a guide wire through hole 13 and a pressurizing liquid channel 14, wherein the pressurizing liquid channel 14 communicates with the inside of the balloon 2.
As shown in fig. 2, a pharmaceutical composition 3 is disposed on an outer surface of the front end portion 22 of the balloon 2, and the pharmaceutical composition 3 is paclitaxel and iopromide. The pharmaceutical composition 3 forms a layer of the pharmaceutical composition having a thickness of about 50 microns.
In treatment, a guidewire is first placed through the atrial septum, creating a fistula of appropriate size in the septum. Then, the end-coating balloon assembly is arranged on the fistula along a guide wire, after the front part 12 of the balloon catheter is pushed to the far end to reach a target area by utilizing a PTCA technology, pressurizing liquid is injected into the balloon 2 through a pressurizing liquid channel 14, the balloon 2 is fully expanded under the action of hydraulic pressure, the pressure in the balloon 2 is kept, the surface of the area of the front end part 22 of the balloon is fully contacted with one surface of the atrial septum of the fistula to be treated, the medicine is rapidly released to the contacted area, after a preset expansion time is reached, the pressurizing liquid is extracted, the balloon 2 is deflated, and the balloon assembly is withdrawn to finish the treatment.
Example 2 [ circular arc, rear end portion coating agent ]
The end-coating balloon assembly disclosed in this embodiment is shown in fig. 3, and has the same structure as that of embodiment 1, except that a pharmaceutical composition 3 is disposed on the outer surface of the rear end portion 23 of the balloon 2, the pharmaceutical composition 3 is paclitaxel, rapamycin, and iopamidol, and the pharmaceutical composition 3 forms a pharmaceutical composition layer with a thickness of about 50 microns.
In treatment, a guidewire is first placed through the atrial septum, creating a fistula of appropriate size in the atrial septum. Then, the end-coating balloon assembly is arranged on the fistula along a guide wire, the front part 12 of the balloon catheter is pushed to the far end by utilizing the PTCA technology and penetrates through the fistula to reach a target area, pressurizing liquid is injected into the balloon 2 through a pressurizing liquid channel 14, the balloon 2 is fully expanded under the action of hydraulic pressure, the pressure in the balloon 2 is kept, the outer surface of the rear end part 23 is fully contacted with one surface of the fistula to be treated and quickly releases the medicine to the target area, after a preset expansion time is reached, the pressurizing liquid is extracted, the balloon 2 is deflated, and the balloon assembly is withdrawn to finish the treatment.
Example 3 [ circular arc, both ends applying medicine, example 1 and example 2 in combination ]
The end-coating balloon assembly disclosed in this embodiment is a combination of the two balloon assemblies disclosed in embodiments 1 and 2, wherein the outer surface of the front end portion 22 of the first balloon assembly is provided with the pharmaceutical composition 3 (i.e., the assembly of embodiment 1), the outer surface of the rear end portion 23 of the first balloon assembly is provided with the pharmaceutical composition 3 (i.e., the assembly of embodiment 2), and the pharmaceutical composition 3 is paclitaxel, rapamycin, or iopamidol.
In the treatment, the front part 12 of the balloon catheter of the first balloon component is pushed to the far end to reach a target area which does not pass through the fistula orifice in the same way as in example 1, the surface of the area of the front end part 22 is fully contacted with one side of the interatrial septum at the fistula orifice to be treated, the first balloon component is withdrawn after the treatment is finished, then the front part 12 of the balloon catheter of the second balloon component is pushed to the far end to pass through the fistula orifice to reach the target area in the same way as in example 2, the surface of the area of the rear end part 23 is fully contacted with the other side of the interatrial septum at the fistula orifice to be treated, and the second balloon component is withdrawn after the treatment is finished. Thereby completing the sequential treatment of the two sides of the atrial septum at the fistula. It should be noted that the stoma itself can be provided with a medication at each treatment.
Example 4 [ circular arc, partial coating of chemical on tip ]
The end-coating balloon assembly disclosed in this example is shown in fig. 4, and has the same structure as that of example 1, except that the pharmaceutical composition 3 is only disposed at a portion with a radius larger than 3mm at the outer surface of the front end portion 22, and the pharmaceutical composition 3 is rapamycin and iopamidol. The pharmaceutical composition 3 forms a layer of the pharmaceutical composition having a thickness of about 50 microns.
The operation method of the balloon assembly disclosed in the embodiment is consistent with that in embodiment 1, the end coating area disclosed in the embodiment is overlapped with the administration area of the fistula to be treated and is in maximum contact with the administration area, so that the administration efficiency is improved, all the medicines act on the fistula, the coating with the minimum dosage can be realized, and the toxicity generated by medicine release in a non-target area is reduced.
Example 5 [ the longitudinal section of the front end is straight, the longitudinal section of the rear end is elliptical arc, and part of the front end is coated with a drug ]
The end portion drug applying balloon assembly disclosed in this embodiment is shown in fig. 5, and the structure thereof is substantially the same as that of embodiment 1, except that the longitudinal section of the outer surface of the front end portion 22 is linear, and the longitudinal section of the outer surface of the rear end portion 23 is elliptical. The pharmaceutical composition (not shown in the figures) is only provided at the portion of the outer surface of the front end portion 22 having a radius larger than 3 mm.
The procedure in the treatment was in accordance with example 1.
Example 6 [ the longitudinal section of the front end is elliptical arc, the longitudinal section of the rear end is circular arc, and part of the front end is coated with a chemical ]
Fig. 6 shows an end-coating balloon assembly according to this embodiment, which is substantially the same as that of embodiment 1, except that the longitudinal section of the outer surface of the front end portion 22 is an elliptical arc, and the longitudinal section of the outer surface of the rear end portion 23 is an arc. The pharmaceutical composition (not shown in the figures) is only provided at the portion of the outer surface of the rear end portion 23 having a radius larger than 3 mm.
The procedure in the treatment was in accordance with example 1.
Example 7 [ longitudinal sections of front and rear end portions are both in the shape of an elliptical arc ]
The end-coating balloon assembly disclosed in this example is shown in fig. 7, and has a structure substantially identical to that of example 1, except that the longitudinal sections of the outer surfaces of the front end portion 22 and the rear end portion 23 are both elliptical arcs.
The pharmaceutical composition (not shown) can be disposed and treated in any manner from example 1 to example 4.
Example 8 [ longitudinal sections of front and rear end portions both in the shape of a trapezoid and in the shape of an elliptical arc ]
The end-coating balloon assembly disclosed in this example is shown in fig. 8, and its structure is substantially the same as that of example 1, except that the longitudinal sections of the outer surfaces of the front end portion 22 and the rear end portion 23 are a combination of trapezoidal and elliptical arcs.
The pharmaceutical composition (not shown) can be disposed and treated in any manner from example 1 to example 4.
Example 9 [ longitudinal sections of front and rear end portions are both trapezoidal ]
The end portion drug applying balloon assembly disclosed in this embodiment is shown in fig. 9, and has a structure substantially identical to that of embodiment 1, except that the longitudinal sections of the outer surfaces of the front end portion 22 and the rear end portion 23 are trapezoidal.
The pharmaceutical composition (not shown) can be disposed and treated in any manner from example 1 to example 4.
Example 10 [ both longitudinal sections of front end portion and rear end portion are doglegged ]
The end-coating balloon assembly disclosed in this example is shown in fig. 10, and its structure is substantially the same as that of example 1, except that the longitudinal sections of the outer surfaces of the front end portion 22 and the rear end portion 23 are both zigzag.
The pharmaceutical composition (not shown) can be disposed and treated in any manner from example 1 to example 4.
The present application also includes the following:
embodiment 1, an end-on drug balloon assembly, comprising: the balloon catheter comprises a balloon catheter and a balloon arranged on the balloon catheter, wherein the balloon is provided with a front end part and a rear end part in the longitudinal direction, and a pharmaceutical composition is arranged on the outer surface of at least one of the front end part and the rear end part.
Embodiment 2 the balloon assembly of embodiment 1, wherein an outer surface of only one of the leading end portion and the trailing end portion has a pharmaceutical composition disposed thereon.
Embodiment 3 the balloon assembly of embodiment 1, wherein the balloon catheter has a guidewire through-hole and a pressurizing liquid channel, wherein the pressurizing liquid channel is in communication with the balloon interior.
Embodiment 4 the balloon assembly of embodiment 1, wherein the balloon is disposed at a front portion of the balloon catheter, the balloon front end being about 5 to 20mm from the balloon catheter front end.
Embodiment 5, the balloon assembly of embodiment 1 or 2, wherein the pharmaceutical composition is disposed only on a portion of the outer surface where the pharmaceutical composition is disposed that has a diameter greater than 2mm, and the pharmaceutical composition is not disposed on the other outer face of the balloon.
Embodiment 6 the balloon assembly of embodiment 1, wherein the longitudinal cut of the outer surface provided with the pharmaceutical composition does not have a concave arc-shaped profile, e.g., the longitudinal cut of the outer surface provided with the pharmaceutical composition has a circular arc shape, an elliptical arc shape, a parabolic shape, a linear shape, a polygonal shape, an irregular curved shape, or a combination of two or more thereof.
Embodiment 7 the balloon assembly of embodiment 1, wherein the pharmaceutical composition comprises at least one of paclitaxel and rapamycin, and optionally a pharmaceutical carrier.
Embodiment 8 the balloon assembly of any one of embodiments 1-7, wherein the balloon has a radial dimension when expanded of 6-25mm, e.g., 8 to 20mm, e.g., 10 to 20mm, e.g., 12 to 20mm, e.g., 14 to 20mm, e.g., 16 to 20mm, e.g., 18 to 20 mm.
Embodiment 9, the balloon assembly of any one of embodiments 1-7, wherein the balloon is a non-compliant balloon, a compliant balloon, or a semi-compliant balloon.
Embodiment 10, a medical device, in particular for percutaneous interatrial ostomy intervention, comprising a balloon assembly according to any of embodiments 1-9.
The above description is intended to be exemplary of the present disclosure, and not to limit the scope of the present disclosure, which is defined by the claims appended hereto.

Claims (17)

1. An end-coated balloon assembly is characterized by comprising a balloon catheter and a balloon arranged on the balloon catheter, wherein the balloon is provided with a front end part and a rear end part in the longitudinal direction, a medicine composition or a medicine composition layer is arranged on the outer surface of at least one of the front end part and the rear end part, the thickness of the medicine composition layer is 1-100 micrometers, and the longitudinal section of the outer surface provided with the medicine composition does not have a concave arc-shaped profile.
2. The balloon assembly of claim 1 wherein only one of the leading end portion and the trailing end portion has the drug composition layer disposed on an outer surface thereof.
3. The balloon assembly of claim 1 wherein the balloon catheter has a guidewire through hole and a pressurized fluid channel, wherein the pressurized fluid channel is in communication with the balloon interior.
4. The balloon assembly of claim 1 wherein the balloon is disposed at a forward portion of the balloon catheter, and wherein the distance from the forward end of the balloon catheter is about 5 to 20 mm.
5. The balloon assembly of claim 1 wherein the drug composition layer is disposed only on portions of the outer surface where the drug composition is disposed that have a diameter greater than 2mm, and the other outer surface of the balloon is not disposed with the drug composition layer.
6. The balloon assembly of claim 1 wherein the longitudinal cut of the outer surface on which the pharmaceutical composition is disposed has a circular arc shape, an elliptical arc shape, a parabolic shape, a linear shape, a polygonal shape, a curved shape, or a combination of two or more thereof.
7. The balloon assembly of claim 1 wherein the pharmaceutical composition comprises at least one of paclitaxel and rapamycin, and optionally a pharmaceutical carrier.
8. The balloon assembly of any of claims 1-7 wherein the balloon has a radial dimension of 6-25mm when inflated.
9. The balloon assembly of any one of claims 1-7, wherein the balloon is a non-compliant balloon, a compliant balloon, or a semi-compliant balloon.
10. The balloon assembly of claim 1 wherein the drug composition layer has a thickness of 10 to 75 microns.
11. The balloon assembly of claim 8 wherein the radial dimension of the balloon when inflated is 8 to 20 mm.
12. The balloon assembly of claim 8 wherein the radial dimension of the balloon when inflated is 10 to 20 mm.
13. The balloon assembly of claim 8 wherein the radial dimension of the balloon when inflated is 12 to 20 mm.
14. The balloon assembly of claim 8 wherein the radial dimension of the balloon when inflated is 14 to 20 mm.
15. The balloon assembly of claim 8 wherein the radial dimension of the balloon when inflated is 16 to 20 mm.
16. The balloon assembly of claim 8 wherein the radial dimension of the balloon when inflated is 18 to 20 mm.
17. A medical device for use in percutaneous interatrial ostomy interventions comprising a balloon assembly according to any one of claims 1-16.
CN202021059439.9U 2020-06-10 2020-06-10 End medicine coating balloon component and medical instrument comprising same Active CN214050144U (en)

Priority Applications (1)

Application Number Priority Date Filing Date Title
CN202021059439.9U CN214050144U (en) 2020-06-10 2020-06-10 End medicine coating balloon component and medical instrument comprising same

Applications Claiming Priority (1)

Application Number Priority Date Filing Date Title
CN202021059439.9U CN214050144U (en) 2020-06-10 2020-06-10 End medicine coating balloon component and medical instrument comprising same

Publications (1)

Publication Number Publication Date
CN214050144U true CN214050144U (en) 2021-08-27

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Family Applications (1)

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Country Status (1)

Country Link
CN (1) CN214050144U (en)

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