CN103341202A - Chitosan sponge surgical dressing and preparation method thereof - Google Patents

Chitosan sponge surgical dressing and preparation method thereof Download PDF

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CN103341202A
CN103341202A CN2013102370085A CN201310237008A CN103341202A CN 103341202 A CN103341202 A CN 103341202A CN 2013102370085 A CN2013102370085 A CN 2013102370085A CN 201310237008 A CN201310237008 A CN 201310237008A CN 103341202 A CN103341202 A CN 103341202A
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chitosan
sponge
insulation
medical dressing
incubated
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CN103341202B (en
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贾峻峰
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JIANGSU DIWO BIOLOGICAL PRODUCTS CO Ltd
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JIANGSU DIWO BIOLOGICAL PRODUCTS CO Ltd
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Abstract

The invention discloses a chitosan sponge surgical dressing and a preparation method thereof. The chitosan sponge surgical dressing includes, by mass, 0.1% to 10% of water-soluble chitosan or a salt thereof, 0.001% to 5% of a foaming agent and 0.05% to 8% of a humectant. The chitosan sponge surgical dressing provided by the invention has a good foaming effect, high adsorption capacity, powerful moisture retention, softness and good plasticity and fills a gap in excellent surgical dressings.

Description

A kind of chitosan sponge body medical dressing and preparation method thereof
Technical field
The present invention relates to the crosslinking technological in tissue engineering bracket material, particularly a kind of chitosan sponge body medical dressing and preparation method thereof.
Background technology
Dressing is a kind of medical material that temporary covering wound uses that is used for, and its topmost function is to control transudate and the protection wound of wound, to avoid the pollution of antibacterial and grit, to provide being beneficial to the environment of wound healing.Select suitable dressing to cover on wound, can assist Bleeding control, protect from infection and absorb secretions, thereby promote wound healing.Now dressing plays the protection wound surface, prevents that body fluid and protein run off, prevent the effect that the antibacterial intrusion causes inflammation, and proliferative cell is provided support.The wound of skin is clinical common disease, when large defect or short time appear in skin, is difficult in the situation of healing, of crucial importance in the dressing of wound surface coverage.For a comparatively long period of time, using the most general surgical wound dressings is medical absorbent cotton and gauze.It can play certain facilitation to the treatment of wound, but has very large deficiency.For example, when it uses, the wound surface granulation tissue causes adhesion to growth in dressing; During releasing, easily cause secondary insult; Easily cause that due to the wound surface hydrops antibacterial infects.Along with the progress in epoch and scientific and technological development, progressively developed into the wound dressing of the high-tech constituent content of today by traditional gauze, breakthrough variation has occurred in the component of dressing and kind in the nearly more than ten years.Clinical need to propose requirements at the higher level to the research and development of dressing, also becomes the power that carries out the new pattern compress exploitation.Therefore, develop a kind of new pattern compress, make it can not only flap coverage, can also help wound healing, prevent bacteria attack, reduce superelevation metabolism and the malnutrition of wound area, alleviate wound pain, accelerating wound, have become scientific research personnel's main direction.Therefore, extremely important to improve its quality and water absorbing properties to the crosslinking Treatment of dressing.The matrix material that is generally used for dressing has two classes: natural macromolecular material and synthesized polymer material.Natural macromolecular material mainly contains collagen, gelatin, chitosan, starch, chondroitin sulfate, alginic acid, cellulose etc.Artificial macromolecular material commonly used comprises Polyethylene Glycol (PEG), polyurethane (PU), polyvinylpyrrolidone (PVP) etc.In general, natural polymer has excellent biocompatibility and degradability, and synthetic macromolecule has good physical and mechanical properties, processing characteristics and chemical stability.These material controllabilitys are good, and practicality is high, have advantage and disadvantage separately, therefore as biomaterial, in organizational project and regenerative medicine field, obtained application widely.
Natural polysaccharide molecule (as chitosan, starch, alginic acid etc.) is the ideal material of medical dressing, they have good biocompatibility on the one hand, there is on the other hand the multiple active function groups reacted on its strand, can carry out chemical modification by modified methods such as grafting easily, can effectively improve the Performance and quality of material.At present a lot of spongy body dressing, all based on this class material, if it is crosslinked to avoid using poisonous chemical reagent to carry out, such as adopting bimolecular conjugation reaction cross-linking method, is expected to obtain the polysaccharide spongy body medical dressing of high swelling ratio and good biocompatibility.Chitosan, starch, Sargassum acid are natural biologic material, can in human body, be degraded to the glucosamine of safety non-toxic, also can not cause immunogenic response, thereby have good biocompatibility; Chitosan is the unique positively charged glucosamine of occurring in nature simultaneously, because of its unique physics and chemistry structure, make the chitosan substance by and erythrocyte membrane between charge effect coagulation erythrocyte stop blooding, and hemostatic mechanism need not depend on clotting mechanism, so can also mediate solidifying of heparinization patient blood, this has unique effect for hemostasis in surgical operation.Chitosan has good biocompatibility, and bioadhesive and multiple biological activity are nontoxic without immune prototype, but plurality of enzymes biodegradation in body, and catabolite is nontoxic and can be absorbed fully by human body, is the ideal carrier of medicament slow release.In addition, chitosan also has performance antibacterial, wound healing.
Chitosan has good biocompatibility with it, biodegradability, and hemostasis and promote the characteristics such as wound healing, just becoming the focus of domestic and international research hemostatic material.At present simple chitosan hemostatic material exists poor toughness and the inapparent problem of haemostatic effect.This can be by with other materials or thereby medicine is compound improves toughness and shorten bleeding stopping period, as waited " preparation research of new field emergency trauma dressing " (health care equipment quietly in pass, 2007,28 (9): reported 1-3.) that chitosan and alginic acid calcium salt composite fibre hemostatic material bleeding stopping period are 127.8+33.6s(family's rabbit back both sides 2cm * 2cm wound); The average bleeding stopping period that application number 200610048015.0, denomination of invention are " a kind of new and effective Chinese medicine/chitosan compound hemostatic material " disclosed chitosan and Chinese medicine (Radix Notoginseng or the Pseudobulbus Bletillae (Rhizoma Bletillae)) compound hemostatic material is that the inboard tremulous pulse of 165~177s(Mus thigh section applies the pressure hemostasis).The biocompatibility that utilizes chitosan, hemostatic technical scheme of making medical dressing are also arranged in prior art.In actual applications, chitosan is generally made sponge for hemostasis after crosslinked foaming, as patent CN1071587A discloses, a kind ofly with acetic acid, dissolves chitosan, mixes the production technology that becomes sponge after collagen with formaldehyde crosslinking; Patent CN131021A discloses a kind of by acid dissolving chitosan, the production technology that glutaraldehyde cross-linking becomes sponge postlyophilization final vacuum drying to form; The production technology that Chinese patent CN 200510024503.3 discloses a kind of " after adopting the carboxymethyl chitosan glycerol adding, with the environment-protective ion exchanger, being cross-linked into the sponge postlyophilization ".The product that these techniques are produced has all been used cross-linking agent, and it is residual has certain toxicity to human body, and be not foamed into sponge, can not be applied to hemostasis, suck blood and the purposes such as imbibition.
Yet chitosan can not dissolve in neutral aqueous solution, foam performance is not good enough, and preparing sponge with it often needs it is dissolved in acid solution, is regulated the operations such as pH value, washing in the sponge production process again.The solubility limits of chitosan in water its range of application.Carboxymethyl chitosan is as the derivant of chitosan, the advantage that had both retained chitosan, improved again water solublity greatly, simultaneously owing to having introduced carboxymethyl group, made it possess more biological activitys and more good biocompatibility, have multiple use in medicine and other fields.Therefore also there is document to disclose the application for chitosan derivatives, as: Chinese patent CN 200510024503 discloses a kind of carboxymerhyl chitosan sponge with water-swelling property, in the technical scheme of this disclosure of the invention, utilize the carboxymethyl chitosan sugar aqueous solution that contains carboxymethyl chitosan, chitosan powder or chitin powder, glycerol plasticizer and environment-protective ion cross-linking agent to prepare sponge, but in this technical scheme, sponge is because foaming is insufficient, hole is few and unstable, easily harden, absorbability is poor, and the embrittlement that easily hardens in using; The China that application number is 20110136324.4 applies for a patent and discloses a kind of sthptic sponge, and this sponge is by molecular sieve and chitosan is compound obtains, and has utilized chitosan anthemorrhagic performance preferably in technical scheme.But in technique scheme only biocompatibility, the biodegradability from chitosan set about, conscientiously do not consider absorption property and soft plasticity when medical bio bressing is used.
Summary of the invention
The object of the invention is to provide the chitosan sponge body that a kind of foaming effect is good, absorbability is high, moisture retention is strong, soft plasticity is strong medical dressing, to solve the deficiency of medical biological dressing in prior art.
For achieving the above object, technical scheme disclosed by the invention is as follows: a kind of chitosan sponge body medical dressing comprises: water-soluble chitosan or its salt, foaming agent and three kinds of components of wetting agent, and the content of described three kinds of components is respectively by mass percentage:
Water-soluble chitosan or its salt 0.1%-10%;
Foaming agent 0.001%-5%;
Wetting agent 0.05%-8%.
Preferably, the content of described three kinds of components is respectively by mass percentage:
Water-soluble chitosan or its salt 2%-7%;
Foaming agent 0.1%-2%;
Wetting agent 1%-5%.
Preferably, water-soluble chitosan described in the present invention or its salt are selected from least one in using carboxyl chitosan, carboxymethyl chitosan, chitosan hydrochlorate, chitosan acetate, chitosan glutamate salt.Wherein, in preparation process, take carboxymethyl chitosan as best.It is that raw material is made that traditional medical sponge adopts chitin more, and chitin is owing to existing acetylamino and carboxyl, and intermolecular hydrogen bond is stronger, and poorly water-soluble need add chemical cosolvent while making medical sponge, is unfavorable for that human body is used; In the present invention, adopt dissolubility preferably water-soluble chitosan be that primary raw material is made medical sponge, in manufacturing process, without adding cosolvent, reduce the injury that in medical sponge, residual chemical substance causes human body.
Preferably, described in the present invention, medical foaming agent is selected from least one in tween, poloxamer, span, fatty acid glyceride, Span.Poloxamer described in the present invention is as emulsifying agent and stabilizing agent, with the chitosan emulsifying that mixes, the breast grain produced is few, absorbance is high, emulsifying effectiveness is outstanding, physicochemical property is stable, can tolerate-65 ℃ of freezings and+50 ° of ℃ of high temperature dryings, and be shaped to loose porous, constitutionally stable sponge shape.Span described in the present invention can be used as emulsifying agent, stabilizing agent, dispersant, wetting agent, cosolvent, softening agent, and in the chitosan dissolved, span, as senior emulsifying agent, plays the effect of the chitosan that is uniformly dispersed simultaneously.The stability of span, wettability, soft effect, after standing freezing and high temperature drying, not modification of physicochemical property, be shaped chitosan sponge, and soft porous is stable again simultaneously.Tween described in the present invention, Chinese is the polyoxyethylene sorbitan fatty acid ester, soluble in water.Tween has the effect of emulsifying diffusion, solubilising, moistening and stabilizing agent, to human body without injury, there is no zest, in the dissolving of chitosan and sponge molding, play the effects such as softening agent, stabilizing agent, foaming agent, wetting agent, do not change physicochemical property after high low temperature.Fatty acid glyceride described in the present invention, have emulsifying, lubricating function, and non-stimulated to skin and mucosa, safe and reliable, biodegradation is nontoxic.Span described in the present invention is non-ionic surface active agent, soft additive, emulsifying agent, dispersant, cosolvent.Above-mentioned foaming agent can make the sponge foaming porous, through not modification of high-low temperature difference, Stability Analysis of Structures.
Through experimentation of the present invention, showing in above-mentioned foaming agent, is more preferably poloxamer.
Preferably, the wetting agent described in the present invention is selected from least one in glycerol, propylene glycol, Polyethylene Glycol.Glycerol described in the present invention, colourless, transparent odorless, be a kind of Organic substance, can be used as softening agent, lytic agent, wetting agent, desiccant.The moisture absorption of glycerol and performance of keeping humidity, not dry not embrittlement after the assurance chitosan sponge is shaped, soft flexible.Polyethylene Glycol described in the present invention, nontoxic non-stimulated, good water solublity, with many organic matter components, the good compatibility is arranged, good lubricant, wetting agent, dispersant, glutinous stick, antistatic additive, solubilizing agent and softening agent, to cold and hot stable, safety and stability very while being heated to 150 ℃.Slightly possesses water absorption simultaneously.Be good adjuvant, make the intercommunication network structure of sponge stable, through cold and hot not modification, the sponge after shaping is loose porous, soft full of elasticity.Propylene glycol described in the present invention, nontoxic, zest is less than glycerol, and solubility property is good, viscosity, good hygroscopicity, intersolubility is good, emulsify well.Can make the chitosan sponge loose porous, have more elasticity.
Above-mentioned each component can be made into chitosan sponge body medical dressing through certain proportioning, but finds through long term test, and water-soluble chitosan, foaming agent and three kinds of components of wetting agent can reach preferably product effect by a certain percentage.According to the introduction of each detailed composition of above-mentioned each component, chitosan sponge body medical dressing of the present invention, preferred, comprise the component of following mass percent:
Carboxymethyl chitosan 2%-7%
Poloxamer 1%-2%
Polyethylene Glycol 2%-5%.
Preferably, the chitosan sponge body medical dressing described in the present invention can comprise the component of following mass percent:
Carboxymethyl chitosan 2%-7%
Tween 1%-2%
Polyethylene Glycol 2%-5%.
The above-mentioned proportioning that a kind of chitosan sponge body medical dressing is provided, the invention also discloses a kind of preparation method of chitosan sponge body medical dressing, it is characterized in that, operating procedure is as follows:
Step 1: prepare solution: after getting appropriate foaming agent and fully soaking, be placed in agitator even with the stirring at low speed of rotating speed 100-180 r/min, then add wetting agent in foaming agent solution, middling speed with 180-400r/min in agitator stirs, add wherein while stirring water-soluble chitosan or its salt to be uniformly dissolved to it, make again the high-speed stirred of agitator with rotating speed 400-700 r/min, solution foaming is expanded, the solution that must foam;
Step 2: pre-freeze: by above-mentioned foaming in good solution Implanted Silicon sealing rubber die dish, and be placed in pre-freeze 1h~24h in the fast freezing case of-70 ℃~-20 ℃, obtain the sponge semi-finished product ;
Step 3: by the sponge semi-finished product in step 2, put in vacuum freeze drier, make described sponge semi-finished product between temperature-20 ℃~+ 50 ℃, vacuum is less than under the condition of 30 handkerchiefs, segmentation is distilled and is incubated, and distillation and insulation are not less than 10 hours total time.
Described in above-mentioned preparation process 3, segmentation is distilled and is incubated, and comprises once distillation and insulation, secondary distillation and insulation, three distillations and the insulation carried out successively;
Once distil and be incubated under the condition that is-18 ℃~-10 ℃ in temperature by the sponge semi-finished product in step 2, the 20min-90min that wherein distils, insulation 5h-10h; Carry out continuously secondary distillation and insulation after once distilling and being incubated, temperature when secondary distillation and insulation is between-8 ℃~+ 3 ℃ again, and the 15min-70min that wherein distils, be incubated 1h-3h; Carry out continuously three distillations and insulation in the secondary distillation and after being incubated, temperature when three distillations and insulation is between+30 ℃~+ 50 ℃, and the 10min-70min that wherein distils, be incubated 1h-3h; Described segmentation is distilled and the temperature, the time that are incubated have all preset by the computerized control system of described vacuum freeze drier.Carry out distillation and the insulation under different temperatures by the bubble loss of thick fluid mould to after pre-freeze in the present invention, make sponge progressively be elevated and be incubated, product is loose porous, and aperture is even, and hole count is intensive, and the fragility of product and toughness are all better.
Chitosan sponge body medical dressing of the present invention mainly refers to bio-sponge.
In above-mentioned preparation method, during preparation, foaming agent, purified water are added in container in proportion, according to dissimilar foaming agent, determine different invading the bubble time, as poloxamer, after adding purified water in proportion, soak 1 hour.During preparation, adopt the rustless steel agitator should be standby high, in, end 3-5 shelves speed regulator (during low-speed running rotating speed 180-400r/min when rotating speed 100-180r/min, middling speed running, while running up rotating speed 400-700r/min), add foaming agent to stir; After foaming agent dissolves fully, wetting agent will be added in solution, middling speed stir treat 2-3 time even to solution, in solution, add water-soluble chitosan to become expanding foam solution to being uniformly dissolved while stirring, high-speed stirred again, when the volume of expanding foam solution expands to original 2-8 times, by expanding foam solution Implanted Silicon sealing rubber die dish, put into as early as possible fast freezing case, make its quick pre-freeze more than 1 hour; After pre-freeze is steeped to the loss of thick fluid mould completely, put it into and distilled in vacuum freeze drier and be incubated immediately, sublimation drying is more than 10 hours.Increase the link of the demoulding after pre-freeze in production process of the present invention, saved significantly the time of sublimation drying, saved the energy, improved productivity ratio; Complete after the product depanning, cracky is not cracked; Product is the sticking mould dish not, makes the depanning speed, raises labour efficiency.
The present invention compared with prior art has following advantage:
At first, the preparation of traditional bio-sponge product, the general stainless steel mould dish that uses prepares sponge, be difficult to the demoulding after quick-freezing, and the freezing crisp easy fracture of goods ice after the demoulding, after drying because of the poor flexibility of bio-sponge, being difficult for resilience after pressing resets, be difficult to cut, the time-consuming material that takes, be difficult to accomplish large production.And, along with the raising of medical level, some bio-sponge products need to make various moulding according to operation, as hollow cylindrical etc., if utilize the words of stainless steel mould dish can't process.The controlling technology that uses squeezing to be shaped when preparing bio-sponge in the present invention, utilize sticky glutinous, nontoxic silica gel to be processed into the mould of required product moulding, with compressed air, expanding foam solution is pushed to injection molding in case of necessity, and then freeze forming, take out the silica gel mould, due to the not sticky glutinous characteristic of silica gel mould, the easily demoulding of finished product.For the flat bulk product without specific (special) requirements, dissolving can be stirred to the water-soluble chitosan foamed and directly pour required block structure silica gel mould dish into, the freezing rear demoulding gets final product.
Secondly, in the present invention, utilize water-soluble chitosan to be combined with foaming agent and form the more powerful mesh structural porous structure of intercommunication, under certain proportioning, product possesses better adsorptivity, and the imbibition ability of product is significantly improved; Utilize properly mixed wetting agent, make product possess better elasticity and flexibility, product sticks the wound mouth, and absorbability is lasting, has more comfortableness simultaneously.Adopt the controlled casting process of silica gel mould dish, in product vacuum lyophilization process, more can tolerate the not modification of high temperature drying of ultralow low temperature and Geng Gao, product shaping is good simultaneously, form the stable mesh structural porous structure of intercommunication, when medical care or surface injury are used, docile more, absorbability is stronger; Operation can better parcel and support blood vessels or histoorgan in using, and plasticity is stronger.
Finally, by test, will utilize bio-sponge prepared with prior art by bio-sponge prepared by the technology of the present invention to compare, and find, bio-sponge prepared by the present invention has following advantage: good stability, put for a long time not easy to change, be out of shape; Foam performance is good, and product is loose porous, and the intercommunication network structure is stable; Have more elasticity, more soft, supportive and the toughness of product are improved; Better physical stability, can tolerate cryotherapy and high temperature drying and not modification forms more stable mesh structural porous structure; Possesses antistatic behaviour.
In a word, the invention has the beneficial effects as follows: chitosan sponge body medical dressing foaming effect of the present invention is good, absorbability is high, moisture retention is strong, soft plasticity is strong.
The accompanying drawing explanation
Fig. 1 (a) compares the electron microscope photo scanning of middle matched group one for the liquid absorbency rate of test example one biological sponge;
Fig. 1 (b) compares the electron microscope photo scanning of middle matched group two for the liquid absorbency rate of test example one biological sponge;
Fig. 1 (c) compares the electron microscope photo scanning of middle test group for the liquid absorbency rate of test example one biological sponge;
The cell adhesion of the chitin-sodium alginate spongy body medical dressing that Fig. 2 is different proportion.
The specific embodiment
Below in conjunction with accompanying drawing, preferred embodiment of the present invention is described in detail, thereby so that advantages and features of the invention can be easier to be it will be appreciated by those skilled in the art that, protection scope of the present invention is made to more explicit defining.
Reagent source used in the following embodiment preparation of the present invention: carboxymethyl chitosan, chitosan acetate, using carboxyl chitosan, poloxamer, tween, Span, Polyethylene Glycol, glycerol, propylene glycol: analytical pure is purchased from Chinese Medicine group;
Instrument used: rustless steel high speed agitator, scanning electron microscope (INCAX-AC T250).
Embodiment mono-: a kind of chitosan sponge body medical dressing, be specially medical sponge, and it comprises the component of following mass percent: 2% carboxymethyl chitosan, 1% poloxamer, 2% Polyethylene Glycol.Its preparation method is: after poloxamer is added to purified water, soak 1 hour; Then soaked poloxamer is utilized the rustless steel agitator with the stirring at low speed of rotating speed 100 r/min 2 times, then reduce to the stirring at low speed of rotating speed 180 r/min 2 times; After poloxamer dissolves fully, Polyethylene Glycol will be added in solution, with the middling speed of 300r/min stir 3 times even to solution, then in solution, add carboxymethyl chitosan to make expanding foam solution to being uniformly dissolved while stirring, make again the high-speed stirred of rustless steel agitator with 700r/min, when the volume of expanding foam solution expands to original 4-5 times, by expanding foam solution Implanted Silicon sealing rubber die dish, put into as early as possible fast freezing case, make its quick pre-freeze 2 hours; After pre-freeze is steeped to the loss of thick fluid mould completely, put it into immediately in vacuum freeze drier, once distil successively and insulation, secondary distillation and insulation, three distillations and insulation; By computerized control system, a sublimation temperature of vacuum freeze drier is preset as to-10 ℃, distillation time 90min, insulation 10h; The secondary sublimation temperature is preset as-8 ℃, distillation time 70min, insulation 1h; Three sublimation temperatures are preset as+and 50 ℃, distillation time 70min, insulation 1h.
Embodiment bis-: a kind of chitosan sponge body medical dressing, be specially medical sponge, and it comprises the component of following mass percent: 7% carboxymethyl chitosan, 2% poloxamer, 5% Polyethylene Glycol.Its preparation method is: after poloxamer is added to purified water, soak 3 hours; Then utilize the rustless steel agitator to stir under the speed of 150 r/min soaked poloxamer; After poloxamer dissolves fully, Polyethylene Glycol will be added in solution ,be stirred to solution even under the speed of 400 r/min, then in solution, add carboxymethyl chitosan to make expanding foam solution to being uniformly dissolved while stirring, under the speed of 700 r/min, stir again, when the volume of expanding foam solution expands to original 4-5 times, by in expanding foam solution Implanted Silicon sealing rubber die dish, put into as early as possible fast freezing case, make its quick pre-freeze 5 hours; After pre-freeze is steeped to the loss of thick fluid mould completely, put it into immediately in vacuum freeze drier, once distil successively and insulation, secondary distillation and insulation, three distillations and insulation; By computerized control system, a sublimation temperature of vacuum freeze drier is preset as to-15 ℃, distillation time 20min, insulation 5h; The secondary sublimation temperature is preset as-5 ℃, distillation time 15min, insulation 2h; Three sublimation temperatures are preset as+and 30 ℃, distillation time 10min, insulation 3h.
Embodiment tri-: a kind of chitosan sponge body medical dressing, be specially medical sponge, and it comprises the component of following mass percent: 3.5% carboxymethyl chitosan, 1% poloxamer, 2.5% Polyethylene Glycol.Its preparation method is: after poloxamer is added to purified water, soak 3 hours; Then utilize the rustless steel agitator to stir under the speed of 180 r/min soaked poloxamer; After poloxamer dissolves fully, Polyethylene Glycol will be added in solution ,be stirred to solution even under the speed of 300 r/min, then in solution, add carboxymethyl chitosan to make expanding foam solution to being uniformly dissolved while stirring, under the speed of 600 r/min, stir again, when the volume of expanding foam solution expands to original 4-5 times, by in expanding foam solution Implanted Silicon sealing rubber die dish, put into as early as possible fast freezing case, make its quick pre-freeze 15 hours; After pre-freeze is steeped to the loss of thick fluid mould completely, put it into immediately in vacuum freeze drier, once distil successively and insulation, secondary distillation and insulation, three distillations and insulation; By computerized control system, a sublimation temperature of vacuum freeze drier is preset as to-18 ℃, distillation time 80min, insulation 8h; The secondary sublimation temperature is preset as-8 ℃, distillation time 50min, insulation 1h; Three sublimation temperatures are preset as+and 40 ℃, distillation time 70min, insulation 2h.
Embodiment tetra-: a kind of chitosan sponge body medical dressing, be specially medical sponge, and it comprises the component of following mass percent: 2% carboxymethyl chitosan, 1% tween, 5% Polyethylene Glycol.Its preparation method is: after poloxamer is added to purified water, soak 3 hours; Then utilize the rustless steel agitator to stir under the speed of 160 r/min soaked tween; After tween dissolves fully, Polyethylene Glycol will be added in solution ,be stirred to solution even under the speed of 200 r/min, then in solution, add carboxymethyl chitosan to make expanding foam solution to being uniformly dissolved while stirring, under the speed of 700 r/min, stir again, when the volume of expanding foam solution expands to original 4-5 times, by in expanding foam solution Implanted Silicon sealing rubber die dish, put into as early as possible fast freezing case, make its quick pre-freeze 10 hours; After pre-freeze is steeped to the loss of thick fluid mould completely, put it into immediately in vacuum freeze drier, once distil successively and insulation, secondary distillation and insulation, three distillations and insulation; By computerized control system, a sublimation temperature of vacuum freeze drier is preset as to-12 ℃, distillation time 50min, insulation 6h; The secondary sublimation temperature is preset as+and 1 ℃, distillation time 60min, insulation 3h; Three sublimation temperatures are preset as+and 45 ℃, distillation time 30min, insulation 2h.
Embodiment five: a kind of chitosan sponge body medical dressing, be specially medical sponge, and it comprises the component of following mass percent: 4% chitosan acetate, 2% tween, 8% Polyethylene Glycol.Its preparation method is: after poloxamer is added to purified water, soak 3 hours; Then utilize the rustless steel agitator to stir under the speed of 170 r/min soaked tween; After tween dissolves fully, Polyethylene Glycol will be added in solution ,be stirred to solution even under the speed of 300 r/min, then in solution, add chitosan acetate to make expanding foam solution to being uniformly dissolved while stirring, under the speed of 400 r/min, stir again, when the volume of expanding foam solution expands to original 4-5 times, by in expanding foam solution Implanted Silicon sealing rubber die dish, put into as early as possible fast freezing case, make its quick pre-freeze 10 hours; After pre-freeze is steeped to the loss of thick fluid mould completely, put it into immediately in vacuum freeze drier, once distil successively and insulation, secondary distillation and insulation, three distillations and insulation; By computerized control system, a sublimation temperature of vacuum freeze drier is preset as to-16 ℃, distillation time 40min, insulation 7h; The secondary sublimation temperature is preset as+and 2 ℃, distillation time 50min, insulation 2h; Three sublimation temperatures are preset as+and 35 ℃, distillation time 50min, insulation 2h.
Embodiment six: a kind of chitosan sponge body medical dressing, it comprises the component of following mass percent: 0.1% water soluble shells is poly-, 0.001% foaming agent, 0.05% wetting agent.Its preparation method reference example one.
Embodiment seven: a kind of chitosan sponge body medical dressing, it comprises the component of following mass percent: 10% water-soluble chitosan, 5% foaming agent, 8% wetting agent.Its preparation method reference example one.
Embodiment eight: a kind of chitosan sponge body medical dressing, it comprises the component of following mass percent: 5% water-soluble chitosan, 3% foaming agent, 4% wetting agent.Its preparation method reference example one.
Embodiment nine: a kind of chitosan sponge body medical dressing, it comprises the component of following mass percent: 8% water-soluble chitosan, 1.5% foaming agent, 6% wetting agent.Its preparation method reference example one.
Embodiment ten: a kind of chitosan sponge body medical dressing, it comprises the component of following mass percent: 7% water-soluble chitosan, 0.1% foaming agent, 1% wetting agent.Its preparation method reference example one.
Embodiment 11: a kind of chitosan sponge body medical dressing, it comprises the component of following mass percent: 2% water-soluble chitosan, 2% foaming agent, 5% wetting agent.Its preparation method reference example one.
Embodiment 12: a kind of chitosan sponge body medical dressing, be specially medical sponge, and it comprises the component of following mass percent: 6% chitosan acetate, this dish of 4%, 7% glycerol.Its preparation method reference example one.
Embodiment 13: a kind of chitosan sponge body medical dressing, be specially medical sponge, and it comprises the component of following mass percent: 3% using carboxyl chitosan, 1.5% Span, 1% propylene glycol.Its preparation method reference example one.
Embodiment 14: a kind of chitosan sponge body medical dressing, be specially medical sponge, and it comprises the component of following mass percent: 9% chitosan glutamate salt, 4.5% fatty acid glyceride, 3% propylene glycol.Its preparation method reference example one.
The comparative experimental example of the product below prepared for the product that adopts technical scheme disclosed in this invention to prepare and prior art:
1 test example one: the liquid absorbency rate of bio-sponge is compared
1.1 test procedure:
Test group: press the medical sponge of above-described embodiment one preparation,
Matched group one: do not add poloxamer, all the other components are constant, still press the medical sponge of embodiment mono-preparation;
Matched group two: do not add Polyethylene Glycol, all the other components are constant, still press the medical sponge of embodiment mono-preparation;
Matched group three: according to the medical sponge of embodiment bis-preparations in CN 200510024503.
test method:by the above-mentioned liquid absorption of respectively organizing medical sponge of centrifugal determination.Utilize scanning electron microscope scanning respectively to organize the medical sponge structure, accompanying drawing 1 means that scanning electron microscope amplifies the medical sponge photo of 200 times, and in figure, scale means 100 μ m.
Blockage by test group and the about 1cm of each matched group medical bio-sponge clip length of side, nearly weigh 0.028g, put into respectively approximately 25 ℃, the beaker of 2ml purified water are housed, place 5 minutes, then put into centrifuge, under the rotating speed of 500rpm, after centrifugal 10min, take out sample, residual liquid is measured respectively, each sampling test 5 times, calculate the residual liquid meansigma methods that weighs every 0.1g sample.
1.2 result of the test: the pick up test data of table 1 medical sponge of the present invention
Figure 2013102370085100002DEST_PATH_IMAGE001
With matched group one, compare: *, there is significant difference P<0.05; With matched group two, compare, , there is significant difference P<0.05; With matched group three, compare: , there is significant difference P<0.05.
From above-mentioned test data, can find out, test group is compared with matched group one, matched group two and matched group three each groups, and the liquid absorbency rate of test group has significant difference.The pick up of the medical sponge of matched group three prepared than prior art by the liquid absorbency rate of the medical sponge that utilizes the present invention to prepare is good, differs maximum multiplying power and reaches 2.05 times.The electron microscope photo scanning that Fig. 1 (a) is matched group one, the electron microscope photo scanning that Fig. 1 (b) is matched group two, the electron microscope photo scanning that Fig. 1 (c) is test group, in observation by Fig. 1 (a), Fig. 1 (b) and three groups of electron microscope photo scannings of Fig. 1 (c) and table 1, data analysis can obtain: the network structure of the medical sponge of test group is stable, loose porous, therefore evenly, adsorbance is large in water suction; The network structure of the medical sponge of matched group one, matched group two and matched group three is even not, and pore size is uneven, unstable, therefore absorption is even not, absorbability is slightly poor.
test example two: the stability test of bio-sponge
2.1 test method:
Test group: press the medical sponge of above-described embodiment two preparations,
Matched group one: do not add Polyethylene Glycol, all the other components are constant, still press the medical sponge of embodiment bis-preparations;
Matched group two: commercial medical chitosan bio-sponge.
Get respectively and respectively organize medical sponge equivalent, carry out accelerated stability test, the study on the stability data are as shown in table 2.
2.1.1 accelerated stability test condition and detecting step:
accelerated test:chitosan bio-sponge dressing (calling sponge in the following text) acceleration environment: 40 ± 1 ℃, humidity: 60% ± 10%RH, investigation time=RT/Q10(40-25)/10=2 * 12/21.5=8.48 month=8 first quarter moons.
detect:device therefor is pHS-25C type acidometer, during detection first the phosphate standard buffer solution with pH=6.86 position, then with the Potassium Hydrogen Phthalate standard buffer solution of pH=4.00, carry out the oblique adjusting rate, finally survey the pH value of solution to be measured.
loss on drying detects:device therefor is baking oven, and during detection, sample thief is appropriate, 60 ° be dried to constant weight after, calculate loss on drying by less loss weight and sampling amount.
steriling test:key instrument: ZW-808A type germ collector, MJ-1608 mold incubator, HH.BII-500-BS electro-heating standing-temperature cultivator, YX280A rustless steel steam autoclave, constant temperature roaster, centrifuge, biological microscope, vacuum shelf, standard P H color comparator, totally-enclosed filtration system etc.
the steriling test method:clean environment under 10000 grades, in the way flow air section or shielding system of 100 grades, at first prepare culture medium, checks the suitability, sterilizing, the sensitivity of culture medium: prepare diluent, flushing liquor: verification experimental verification method, then judged result.Then the steriling test test sample, process and inoculation medium, then cultivates and observe, last judged result.This test all samples and reference substance, the equal well-grown of positive control pipe, negative control pipe asepsis growth, all test sample pipes are all clarified, asepsis growth.
2.2 it is as follows that test data records result:
The stability test data of table 2 bio-sponge
Figure 161724DEST_PATH_IMAGE002
conclusion: test group:sponge is stored in relative humidity and is no more than 80%, and temperature is-5 ℃~30 ℃, non-corrosiveness gas and draughty indoor, and outward appearance, pH value, loss on drying variation do not occur and can keep aseptic condition in product.
matched group 1:sponge is stored in relative humidity and is no more than 80%, and temperature is-5 ℃~30 ℃, non-corrosiveness gas and draughty indoor, and product produces outward appearance in the allowed band value, and yellowing phenomenon, loss on drying have phenomenon of losing water in the allowed band value a little.PH value does not occur product changes and can keep aseptic condition.
matched group 2:sponge is stored in relative humidity and is no more than 80%, and temperature is-5 ℃~30 ℃, non-corrosiveness gas and draughty indoor, and product produces outward appearance in the allowed band value, and yellowing phenomenon, loss on drying have phenomenon of losing water in the allowed band value a little.PH value does not occur product changes and can keep aseptic condition.
Contrast learns, the stability of test group medical sponge is better than the stability of the medical sponge of matched group 1 and matched group 2.
test example three: the sticky stickiness test of the skin of bio-sponge
3.1 test method:
Test group: the biological sponge of getting the embodiment of the present invention three preparations;
Matched group: get the bio-sponge that commercially available traditional handicraft is manufactured;
Test procedure: respectively get the appropriate also noting marker of test group and matched group bio-sponge, put into respectively same beaker, use the purified water moistening, room temperature was invaded bubble after 24 hours, took out respectively two kinds of samples.Perusal hands touch pinches two kinds of products: the test group product becomes evenly cotton-shaped, with hands, touches and pinches without sticky stickiness, and comfortable feel, prove and can contact with wound face evenly, simultaneously not sticky glutinous skin; The matched group product occurs that sponge is cotton-shaped inhomogeneous, slightly is with little microlith, with hands, touches and pinches, and product subsurface has sticky glutinous sticky feeling, illustrate while using, with wound, contact evenly not, and easy gluing sticks skin.
test example four: the cell adhesion of bio-sponge detects
4.1 test method:
Test group: the bio-sponge of getting the embodiment of the present invention three preparations;
Matched group one: get the bio-sponge that commercially available traditional handicraft is manufactured;
Matched group two: do not add Polyethylene Glycol, all the other components are constant, still press the bio-sponge of embodiment tri-preparations;
Matched group three: do not add poloxamer, all the other components are constant, still press the bio-sponge of embodiment tri-preparations;
Get the bio-sponge equivalent of above-mentioned each group through the 60Coradiation sterilizing, be cut into respectively circle and size and 24 well culture plate (Nunc tM, Denmark) aperture is consistent, and each group bio-sponge is paved with respectively to each culture plate bottom.All inoculating quantity on the bio-sponge surface is 5 * 10 4the human body fibroblast, and all add 3 milliliters of culture fluid (DMEM culture medium+10% calf serum+100 unit/ml penicillin/streptomycin), be put under 37 ℃ to hatch after 4 hours and take out, repeatedly rinse to remove the cell do not adhered to by phosphate buffered solution, then the phosphate buffered solution that adds 20 microlitre 0.5wt%MTT, be placed under 37 ℃ to hatch after 4 hours and add 200 microlitre dimethyl sulfoxide, after vibration evenly, adopt microplate reader (Biorad, Model 550) to measure respectively the absorbance of purple material in 570 nm places.Concrete data are participated in accompanying drawing 2, and the superficial cell adhesion value of test group is very low, with matched group one, matched group two and matched group three, compares, and the superficial cell adhesiveness of test group, lower than other three groups of matched groups, has significant difference.
Chitosan sponge body medical dressing prepared by the present invention is the sponge loose structure, and average pore size is 100 microns left and right, and mutually runs through, and is conducive to the absorption (Fig. 1 (C)) of ventilative and moisture.Other chitosan sponges in the prior art of comparing, chitosan sponge of the present invention loose porous, hole is not only intensive and hole size is even, pore size is moderate, the water absorbing capacity of chitosan sponge dressing of the present invention is extremely strong, can absorb the liquid (table 1) that is equivalent to 17 ~ 25 times of own wts.The stability of chitosan sponge body medical dressing of the present invention is better, can store that in 8.5 months, outward appearance does not occur product, loss on drying changes and keep aseptic condition (table 2).The sticky stickiness test of the skin of chitosan bio-sponge of the present invention shows that product can contact evenly with wound face, and not sticky glutinous skin, and the wounded is without sense of discomfort.Because the cell adhesion of dressing is that the sponge design needs a very important problem of considering.The dressing caused because material is incorrect adheres to granulation tissue, thereby causes the secondary damage brought when dressing removes, and comprises the adhesion to granulation, to the epithelial cell of migration, fibroblastic infringement of hypertrophy, even more serious than not using dressing.The superficial cell adhesion value of the test group in test example four of the present invention is very low, significantly lower than other three groups of matched groups (Fig. 2), the hydrophilic that dressing of the present invention is described is high, water absorbing capacity is strong, thereby is unfavorable for the adhesion of cell, and such dressing is unlikely causes the tissue adhesion.
The foregoing is only embodiments of the invention; not thereby limit the scope of the claims of the present invention; every equivalent structure or conversion of equivalent flow process that utilizes description of the present invention and accompanying drawing content to do; or directly or indirectly be used in other relevant technical fields, all in like manner be included in scope of patent protection of the present invention.

Claims (9)

1. a chitosan sponge body medical dressing, is characterized in that, it comprises: water-soluble chitosan or its salt, foaming agent and three kinds of components of wetting agent, and the content of described three kinds of components is respectively by mass percentage:
Water-soluble chitosan or its salt 0.1%-10%;
Foaming agent 0.001%-5%;
Wetting agent 0.05%-8%.
2. chitosan sponge body medical dressing according to claim 1, is characterized in that, the content of described three kinds of components is respectively by mass percentage:
Water-soluble chitosan or its salt 2%-7%;
Foaming agent 0.1%-2%;
Wetting agent 1%-5%.
3. chitosan sponge body medical dressing according to claim 2, it is characterized in that, described water-soluble chitosan or its salt are selected from least one in using carboxyl chitosan, carboxymethyl chitosan, chitosan hydrochlorate, chitosan acetate, chitosan glutamate salt.
4. chitosan sponge body medical dressing according to claim 3, is characterized in that, described medical foaming agent is selected from least one in tween, poloxamer, span, fatty acid glyceride, Span.
5. chitosan sponge body medical dressing according to claim 4, is characterized in that, described wetting agent is selected from least one in glycerol, propylene glycol, Polyethylene Glycol.
6. chitosan sponge body medical dressing according to claim 5, is characterized in that, comprises the component of following mass percent:
Carboxymethyl chitosan 2%-7%
Poloxamer 1%-2%
Polyethylene Glycol 2%-5%.
7. chitosan sponge body medical dressing according to claim 5, is characterized in that, comprises the component of following mass percent:
Carboxymethyl chitosan 2%-7%
Tween 1%-2%
Polyethylene Glycol 2%-5%.
8. the preparation method of a chitosan sponge body medical dressing, is characterized in that, operating procedure is as follows:
Step 1: prepare solution: after getting appropriate foaming agent and fully soaking, be placed in agitator even with the stirring at low speed of rotating speed 100-180 r/min, then add wetting agent in foaming agent solution, middling speed with 180-400r/min in agitator stirs, add wherein while stirring water-soluble chitosan or its salt to be uniformly dissolved to it, make again the high-speed stirred of agitator with rotating speed 400-700 r/min, solution foaming is expanded, the solution that must foam;
Step 2: pre-freeze: by above-mentioned foaming in good solution Implanted Silicon sealing rubber die dish, be placed in pre-freeze 1h~24h in the fast freezing case of-70 ℃~-20 ℃, obtain the sponge semi-finished product;
Step 3: by the sponge semi-finished product in step 2, put in vacuum freeze drier, make described sponge semi-finished product between temperature-20 ℃~+ 50 ℃, vacuum is less than under the condition of 30 handkerchiefs, segmentation is distilled and is incubated, and distillation and insulation are not less than 10 hours total time.
9. the preparation method of chitosan sponge body medical dressing according to claim 8, is characterized in that, the segmentation described in step 3 is distilled and is incubated, and comprises once distillation and insulation, secondary distillation and insulation, three distillations and the insulation carried out successively;
Once distil and be incubated under the condition that is-18 ℃~-10 ℃ in temperature by the sponge semi-finished product in step 2, the 20min-90min that wherein distils, insulation 5h-10h; Carry out continuously secondary distillation and insulation after once distilling and being incubated, temperature when secondary distillation and insulation is between-8 ℃~+ 3 ℃ again, and the 15min-70min that wherein distils, be incubated 1h-3h; Carry out continuously three distillations and insulation in the secondary distillation and after being incubated, temperature when three distillations and insulation is between+30 ℃~+ 50 ℃, and the 10min-70min that wherein distils, be incubated 1h-3h;
Described segmentation is distilled and the temperature, the time that are incubated have all preset by the computerized control system of described vacuum freeze drier.
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CN104189940A (en) * 2014-08-28 2014-12-10 青岛美科医疗器械有限公司 Antibacterial liquid dressing containing chitosan hydrochloride and preparation method thereof
CN105194716A (en) * 2015-10-16 2015-12-30 柏为(武汉)医疗科技有限公司 Absorbable hemostatic medical polymer material and preparation method thereof
CN107652477A (en) * 2017-10-18 2018-02-02 德清舒华泡沫座椅有限公司 A kind of environment-friendly antibacterial sponge and its preparation technology
CN107722336A (en) * 2017-10-18 2018-02-23 德清舒华泡沫座椅有限公司 The antibacterial sponge and its preparation technology of a kind of environment-friendly degradable
WO2018204565A1 (en) * 2017-05-03 2018-11-08 Warner Babcock Institute For Green Chemistry, Llc Cushion
CN112023110A (en) * 2020-08-06 2020-12-04 西安交通大学 Active antibacterial dressing based on bamboo fungus egg extract
CN114533937A (en) * 2022-02-14 2022-05-27 北京冠合医疗科技有限公司 Biodegradable temperature-sensitive embolic gel and preparation method and application thereof

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CN103012836A (en) * 2013-01-05 2013-04-03 吴斌 Preparation method of polysaccharide sponge for material dressing

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CN102416194A (en) * 2011-11-11 2012-04-18 汤小国 Novel chitosan hemostatic sponge and preparation method thereof
CN103012836A (en) * 2013-01-05 2013-04-03 吴斌 Preparation method of polysaccharide sponge for material dressing

Cited By (8)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
CN104189940A (en) * 2014-08-28 2014-12-10 青岛美科医疗器械有限公司 Antibacterial liquid dressing containing chitosan hydrochloride and preparation method thereof
CN105194716A (en) * 2015-10-16 2015-12-30 柏为(武汉)医疗科技有限公司 Absorbable hemostatic medical polymer material and preparation method thereof
WO2018204565A1 (en) * 2017-05-03 2018-11-08 Warner Babcock Institute For Green Chemistry, Llc Cushion
CN107652477A (en) * 2017-10-18 2018-02-02 德清舒华泡沫座椅有限公司 A kind of environment-friendly antibacterial sponge and its preparation technology
CN107722336A (en) * 2017-10-18 2018-02-23 德清舒华泡沫座椅有限公司 The antibacterial sponge and its preparation technology of a kind of environment-friendly degradable
CN112023110A (en) * 2020-08-06 2020-12-04 西安交通大学 Active antibacterial dressing based on bamboo fungus egg extract
CN112023110B (en) * 2020-08-06 2021-11-19 西安交通大学 Active antibacterial dressing based on bamboo fungus egg extract
CN114533937A (en) * 2022-02-14 2022-05-27 北京冠合医疗科技有限公司 Biodegradable temperature-sensitive embolic gel and preparation method and application thereof

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