Bandages

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  • 文章类型: Journal Article
    背景:糖尿病伤口面临重大挑战,特别是在细菌感染和延迟愈合方面。因此,解决局部细菌问题和促进伤口加速愈合至关重要。在这次调查中,我们利用静电纺丝来制造包封MXene包封的微凝胶和壳聚糖/明胶聚合物的微凝胶/纳米纤维膜。
    结果:薄膜敷料促进了近红外(NIR)下的程序化光热疗法(PPT)和轻度光热疗法(MPTT),展示快速和广泛的抗菌和生物膜破坏能力。PPT效果在52°C下在5分钟内实现快速灭菌,并在10分钟内分散成熟的生物膜。同时,通过调整NIR功率以引起局部温和加热(42°C),敷料刺激成纤维细胞增殖和迁移,显着增强血管化。此外,体内实验成功验证了薄膜敷料,强调其在解决糖尿病伤口的复杂性方面的巨大潜力。
    结论:负载MXene微凝胶的纳米纤维敷料采用温度协调的光热疗法,有效地融合了高温灭菌和低温促进伤口愈合的优点。它表现得很快,广谱抗菌和生物膜破坏能力,特殊的生物相容性,对促进细胞增殖和血管化具有显著的作用。这些结果肯定了我们的纳米纤维敷料的功效,强调其在解决糖尿病伤口因感染而难以愈合的挑战方面的巨大潜力。
    BACKGROUND: Diabetic wounds present significant challenges, specifically in terms of bacterial infection and delayed healing. Therefore, it is crucial to address local bacterial issues and promote accelerated wound healing. In this investigation, we utilized electrospinning to fabricate microgel/nanofiber membranes encapsulating MXene-encapsulated microgels and chitosan/gelatin polymers.
    RESULTS: The film dressing facilitates programmed photothermal therapy (PPT) and mild photothermal therapy (MPTT) under near-infrared (NIR), showcasing swift and extensive antibacterial and biofilm-disrupting capabilities. The PPT effect achieves prompt sterilization within 5 min at 52 °C and disperses mature biofilm within 10 min. Concurrently, by adjusting the NIR power to induce local mild heating (42 °C), the dressing stimulates fibroblast proliferation and migration, significantly enhancing vascularization. Moreover, in vivo experimentation successfully validates the film dressing, underscoring its immense potential in addressing the intricacies of diabetic wounds.
    CONCLUSIONS: The MXene microgel-loaded nanofiber dressing employs temperature-coordinated photothermal therapy, effectively amalgamating the advantageous features of high-temperature sterilization and low-temperature promotion of wound healing. It exhibits rapid, broad-spectrum antibacterial and biofilm-disrupting capabilities, exceptional biocompatibility, and noteworthy effects on promoting cell proliferation and vascularization. These results affirm the efficacy of our nanofiber dressing, highlighting its significant potential in addressing the challenge of diabetic wounds struggling to heal due to infection.
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  • 文章类型: Journal Article
    功能性无机纳米材料(NMs)被广泛用作生物活性材料和药物储库。在皮肤损伤部位缺乏稳定形式的NMs应用,可能会阻碍清创术的移除,提高pH值,诱导组织毒性,并限制它们在皮肤修复中的使用。这需要克服上述限制的创新伤口敷料的出现。这项研究的首要目的是利用锶掺杂的中孔硅颗粒(PSiSr)赋予基于聚(乳酸-羟基乙酸共聚物)/明胶(PG)的纤维敷料(PG@PSiSr)的多功能性,以进行切除伤口处理。
    使用化学合成方法合成了中孔硅颗粒(PSi)和PSiSr。使用静电纺丝将PSi和PSiSr两者结合到PG纤维中。一系列的结构,形态学,孔径分布,并对PG@PSi和PG@PSiSr膜进行了累积pH研究。细胞相容性,血液相容性,Transwell迁移,划痕伤口愈合,并在体外测试了这些复合敷料的血管生成特性。通过大鼠皮下植入模型评估复合敷料在体内的生物相容性,而通过在大鼠全层切除缺损模型中的植入可以识别它们的伤口愈合潜力。
    PG@PSiSr膜可以持续释放硅离子(Si4)和锶离子(Sr2)长达192小时,并显着促进人脐静脉内皮细胞(HUVEC)和NIH-3T3成纤维细胞的迁移。PG@PSiSr膜也显示出更好的细胞相容性,血液相容性,并在体外显著形成HUVECs的小管样网络。此外,PG@PSisr膜还促进宿主细胞的浸润并促进胶原蛋白的沉积,同时减少大鼠皮下植入模型中炎性细胞的积累,如评估的长达14天。在大鼠全层切除伤口模型中移植的膜的进一步评估显示伤口快速闭合(PG@SiSr与对照,96.1%vs71.7%),再上皮化,伴随皮肤附件形成的炎症反应较少(例如,血管,腺体,毛囊,等。).
    总而言之,我们成功地制备了PSisr颗粒,并使用静电纺丝制备了PG@PSisr敷料。PSiSr介导的治疗性离子释放,如Si4+和Sr2+,可以改善PLGA/凝胶敷料的功能,以进行有效的伤口修复,这也可能对其他软组织修复学科产生影响。
    UNASSIGNED: Functional inorganic nanomaterials (NMs) are widely exploited as bioactive materials and drug depots. The lack of a stable form of application of NMs at the site of skin injury, may impede the removal of the debridement, elevate pH, induce tissue toxicity, and limit their use in skin repair. This necessitates the advent of innovative wound dressings that overcome the above limitations. The overarching objective of this study was to exploit strontium-doped mesoporous silicon particles (PSiSr) to impart multifunctionality to poly(lactic-co-glycolic acid)/gelatin (PG)-based fibrous dressings (PG@PSiSr) for excisional wound management.
    UNASSIGNED: Mesoporous silicon particles (PSi) and PSiSr were synthesized using a chemo-synthetic approach. Both PSi and PSiSr were incorporated into PG fibers using electrospinning. A series of structure, morphology, pore size distribution, and cumulative pH studies on the PG@PSi and PG@PSiSr membranes were performed. Cytocompatibility, hemocompatibility, transwell migration, scratch wound healing, and delineated angiogenic properties of these composite dressings were tested in vitro. The biocompatibility of composite dressings in vivo was assessed by a subcutaneous implantation model of rats, while their potential for wound healing was discerned by implantation in a full-thickness excisional defect model of rats.
    UNASSIGNED: The PG@PSiSr membranes can afford the sustained release of silicon ions (Si4+) and strontium ions (Sr2+) for up to 192 h as well as remarkably promote human umbilical vein endothelial cells (HUVECs) and NIH-3T3 fibroblasts migration. The PG@PSiSr membranes also showed better cytocompatibility, hemocompatibility, and significant formation of tubule-like networks of HUVECs in vitro. Moreover, PG@PSiSr membranes also facilitated the infiltration of host cells and promoted the deposition of collagen while reducing the accumulation of inflammatory cells in a subcutaneous implantation model in rats as assessed for up to day 14. Further evaluation of membranes transplanted in a full-thickness excisional wound model in rats showed rapid wound closure (PG@SiSr vs control, 96.1% vs 71.7%), re-epithelialization, and less inflammatory response alongside skin appendages formation (eg, blood vessels, glands, hair follicles, etc.).
    UNASSIGNED: To sum up, we successfully fabricated PSiSr particles and prepared PG@PSiSr dressings using electrospinning. The PSiSr-mediated release of therapeutic ions, such as Si4+ and Sr2+, may improve the functionality of PLGA/Gel dressings for an effective wound repair, which may also have implications for the other soft tissue repair disciplines.
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  • 文章类型: Journal Article
    皮肤是人体中最大的器官,需要适当的敷料以促进受伤后的愈合。可移动部件上的伤口,比如肘部,膝盖,手腕,脖子,通常经历延迟和低效的愈合由于频繁的运动。为了更好地适应可移动的伤口,已经成功开发了多种功能性水凝胶并将其用作柔性伤口敷料。一方面,机械性能,如附着力,可拉伸性,和自我修复,使这些水凝胶适用于移动伤口并促进愈合过程;另一方面,生物活动,如抗菌和抗氧化性能,可以进一步加速伤口愈合过程。在这次审查中,我们专注于基于水凝胶的可移动伤口敷料的最新进展,并提出了这种敷料的挑战和观点。
    Skin is the largest organ in the human body and requires proper dressing to facilitate healing after an injury. Wounds on movable parts, such as the elbow, knee, wrist, and neck, usually undergo delayed and inefficient healing due to frequent movements. To better accommodate movable wounds, a variety of functional hydrogels have been successfully developed and used as flexible wound dressings. On the one hand, the mechanical properties, such as adhesion, stretchability, and self-healing, make these hydrogels suitable for mobile wounds and promote the healing process; on the other hand, the bioactivities, such as antibacterial and antioxidant performance, could further accelerate the wound healing process. In this review, we focus on the recent advances in hydrogel-based movable wound dressings and propose the challenges and perspectives of such dressings.
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  • 文章类型: Journal Article
    本研究旨在开发一种新型明胶氧化银材料,用于释放一氧化氮生物纳米复合伤口敷料,化学,和抗菌性能的糖尿病伤口的治疗。明胶-氧化银纳米颗粒(Ag2O-NP)生物纳米复合材料是使用壳聚糖和明胶聚合物与氧化银纳米颗粒通过冷冻干燥方法制备的。使用扫描电子显微镜(SEM)和X射线衍射(XRD)分析对样品进行了表征。结果表明,Ag2O-NP纳米颗粒增加了孔隙率,孔径减小,提高了弹性模量。Ag2O-NP伤口敷料对金黄色葡萄球菌和大肠杆菌表现出最有效的抗菌性能。在样本中,含有氧化银纳米颗粒的伤口敷料表现出优异的物理和机械性能,孔隙率为48%,抗拉强度为3.2MPa,弹性模量为51.7MPa。制造的伤口敷料的空空间与总体积的体积比在40%至60%的范围内。并行,考虑到糖尿病的并发症及其对血管系统的影响,研究的另一方面集中在开发一种能够释放一氧化氮气体以再生受损血管并加速糖尿病伤口愈合的全介导伤口敷料。壳聚糖,一种生物相容性和生物可降解的聚合物,被选为伤口敷料的基质,和β-甘油磷酸盐(GPβ),三聚磷酸盐(TPP),和过2介导的藻酸盐(AL)用作交联剂。在扫描电子显微镜测试中,壳聚糖-海藻酸盐(CS-AL)伤口敷料在孔数和均匀性方面表现出最佳特征。它还表现出优异的吸水率(3854%)和最小的透气性。此外,CS-AL样品在14天后表现出80%的降解率,表明其作为伤口敷料的适用性。伤口敷料装载有S-亚硝基谷胱甘肽(GSNO)粉末,通过油脂测试确认一氧化氮气体的成功释放,在540nm的波长处显示峰值。随后的研究表明,用高糖处理人脐静脉内皮细胞(HUVECs)导致PER2和SIRT1的表达降低,而PER2的表达增加,这可能随后增强SIRT1的表达并促进细胞增殖活性。然而,用改性材料处理细胞后,观察到PER2和SIRT1的表达增加,导致细胞增殖活性的部分恢复。这项综合研究成功开发了per2介导的生物纳米复合伤口敷料,机械,化学,和抗菌性能。氧化银纳米颗粒的掺入增强了抗菌活性,而从敷料释放的一氧化氮气体证明了减轻高葡萄糖水平引起的血管内皮细胞损伤的能力。这些进步显示出通过解决与糖尿病相关的并发症并增强整体伤口愈合来促进糖尿病伤口愈合过程的有希望的潜力。
    This study aimed to develop a novel Gelatin silver oxide material for releasing nitric oxide bionanocomposite wound dressing with enhanced mechanical, chemical, and antibacterial properties for the treatment of diabetic wounds. The gelatin- silver oxide nanoparticles (Ag2O-NP) bio nanocomposite was prepared using chitosan and gelatin polymers incorporated with silver oxide nanoparticles through the freeze-drying method. The samples were characterized using scanning electron microscopy (SEM) and X-ray diffraction (XRD) analysis. Results showed that the Ag2O-NP nanoparticles increased porosity, decreased pore size, and improved elastic modulus. The Ag2O-NP wound dressing exhibited the most effective antibacterial properties against Staphylococcus aureus and Escherichia coli. Among the samples, the wound dressing containing silver oxide nanoparticles demonstrated superior physical and mechanical properties, with 48% porosity, a tensile strength of 3.2 MPa, and an elastic modulus of 51.7 MPa. The fabricated wound dressings had a volume ratio of empty space to total volume ranging from 40% to 60%. In parallel, considering the complications of diabetes and its impact on the vascular system, another aspect of the research focused on developing a per2mediated wound dressing capable of releasing nitric oxide gas to regenerate damaged vessels and accelerate diabetic wound healing. Chitosan, a biocompatible and biodegradable polymer, was selected as the substrate for the wound dressing, and beta-glycerophosphate (GPβ), tripolyphosphate (TPP), and per2mediated alginate (AL) were used as crosslinkers. The chitosan-alginate (CS-AL) wound dressing exhibited optimal characteristics in terms of hole count and uniformity in the scanning electron microscope test. It also demonstrated superior water absorption (3854%) and minimal air permeability. Furthermore, the CS-AL sample exhibited an 80% degradation rate after 14 days, indicating its suitability as a wound dressing. The wound dressing was loaded with S-nitrosoglutathione (GSNO) powder, and the successful release of nitric oxide gas was confirmed through the grease test, showing a peak at a wavelength of 540 nm. Subsequent investigations revealed that the treatment of human umbilical vein endothelial cells (HUVECs) with high glucose led to a decrease in the expression of PER2 and SIRT1, while the expression of PER2 increased, which may subsequently enhance the expression of SIRT1 and promote cell proliferation activity. However, upon treatment of the cells with the modified materials, an increase in the expression of PER2 and SIRT1 was observed, resulting in a partial restoration of cell proliferative activity. This comprehensive study successfully developed per2-mediated bio-nanocomposite wound dressings with improved physical, mechanical, chemical, and antibacterial properties. The incorporation of silver oxide nanoparticles enhanced the antimicrobial activity, while the released nitric oxide gas from the dressing demonstrated the ability to mitigate vascular endothelial cell damage induced by high glucose levels. These advancements show promising potential for facilitating the healing process of diabetic wounds by addressing complications associated with diabetes and enhancing overall wound healing.
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  • 文章类型: Journal Article
    滥用抗生素正在增加目前耐药细菌伤口感染的发生率,在全球范围内产生巨大的医疗保健负担。在这里,我们通过将天然植物提取物TA作为非抗生素和交联剂包埋在羧甲基壳聚糖(CMCS)和聚乙烯吡咯烷酮(PVP)中,以促进伤口愈合,制备了一种pH响应性CMCS/PVP/TA(CPT)多功能水凝胶敷料。CPT水凝胶表现出优异的自愈性,自适应,和粘附性能,以满足不同的伤口要求。重要的是,这种水凝胶表现出pH敏感性,并通过在细菌感染(碱性)的情况下释放TA而表现出良好的抗抗性细菌活性和抗氧化活性。此外,CPT水凝胶显示出凝血能力,并能在30s内迅速止血。生物相容性水凝胶通过增厚肉芽组织有效加速全层皮肤缺损模型中的伤口愈合,增加胶原蛋白沉积,血管增生,和M2型巨噬细胞极化。总之,这项研究表明,多功能CPT水凝胶为感染的皮肤伤口愈合提供了潜在应用的候选材料。
    Antibiotic abuse is increasing the present rate of drug-resistant bacterial wound infections, producing a significant healthcare burden globally. Herein, we prepared a pH-responsive CMCS/PVP/TA (CPT) multifunctional hydrogel dressing by embedding the natural plant extract TA as a nonantibiotic and cross-linking agent in carboxymethyl chitosan (CMCS) and polyvinylpyrrolidone (PVP) to prompt wound healing. The CPT hydrogel demonstrated excellent self-healing, self-adaptive, and adhesion properties to match different wound requirements. Importantly, this hydrogel showed pH sensitivity and exhibited good activity against resistant bacteria and antioxidant activity by releasing TA in case of bacterial infection (alkaline). Furthermore, the CPT hydrogel exhibited coagulant ability and could rapidly stop bleeding within 30 s. The biocompatible hydrogel effectively accelerated wound healing in a full-thickness skin defect model by thickening granulation tissue, increasing collagen deposition, vascular proliferation, and M2-type macrophage polarization. In conclusion, this study demonstrates that multifunctional CPT hydrogel offers a candidate material with potential applications for infected skin wound healing.
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  • 文章类型: Journal Article
    感染伤口的修复是一个复杂的病理生理过程。目前关于感染伤口治疗的研究主要集中在感染治疗上。而血管损伤和免疫失衡引起的延迟愈合的相关因素却普遍被忽视。在这项研究中,细胞外基质(ECM)样动态和多功能透明质酸(HA)水凝胶,免疫调节,血管生成能力被设计为伤口敷料,用于治疗感染的皮肤伤口。水凝胶敷料中的动态网络基于巯基和生物活性金属离子之间形成的可逆金属-配体配位。在我们的设计中,抗菌银和免疫调节锌离子用于与巯基化HA和血管生成肽协调。除了感染伤口所需的生物活性外,水凝胶还可以表现出自我修复和可注射的能力。感染皮肤伤口模型的动物实验表明,水凝胶敷料能够实现微创注射和无缝皮肤伤口覆盖,然后通过有效的细菌杀灭促进伤口愈合。持续的炎症抑制,改善血管形成。总之,具有伤口感染所需的生物活性和ECM样动态结构的金属离子配位水凝胶代表了一类用于治疗感染和慢性炎症伤口的组织仿生伤口敷料。
    The repair of infected wounds is a complex physiopathologic process. Current studies on infected wound treatment have predominantly focused on infection treatment, while the factors related to delayed healing caused by vascular damage and immune imbalance are commonly overlooked. In this study, an extracellular matrix (ECM)-like dynamic and multifunctional hyaluronic acid (HA) hydrogel with antimicrobial, immunomodulatory, and angiogenic capabilities was designed as wound dressing for the treatment of infected skin wounds. The dynamic network in the hydrogel dressing was based on reversible metal-ligand coordination formed between sulfhydryl groups and bioactive metal ions. In our design, antibacterial silver and immunomodulatory zinc ions were employed to coordinate with sulfhydrylated HA and a vasculogenic peptide. In addition to the desired bioactivities for infected wounds, the hydrogel could also exhibit self-healing and injectable abilities. Animal experiments with infected skin wound models indicated that the hydrogel dressings enabled minimally invasive injection and seamless skin wound covering and then facilitated wound healing by efficient bacterial killing, continuous inflammation inhibition, and improved blood vessel formation. In conclusion, the metal ion-coordinated hydrogels with wound-infection-desired bioactivities and ECM-like dynamic structures represent a class of tissue bionic wound dressings for the treatment of infected and chronic inflammation wounds.
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  • 文章类型: Journal Article
    深层和不规则伤口的严重出血在院前和手术环境中构成了重大挑战。为了解决这个问题,我们使用Fe3O4开发了一种新型的基于壳聚糖的止血敷料,该敷料具有磁性靶向机制,称为牛血清白蛋白修饰的Fe3O4嵌入多孔α-酮戊二酸/壳聚糖(BSA/Fe3O4@KA/CS)。该敷料通过将药剂磁性引导至伤口部位来增强止血。体外,BSA/Fe3O4@KA/CS的止血功效与商业壳聚糖(Celox™)相当,并且不会因修饰而降低。在体内,与Celox™相比,BSA/Fe3O4@KA/CS表现出优异的止血性能和减少的失血。BSA/Fe3O4@KA/CS的止血机制包括通过水吸收浓缩固体血液成分,粘附于血细胞,和内源性凝血途径的激活。磁场靶向在将敷料引导至深度出血部位时至关重要。此外,安全性评估证实了BSA/Fe3O4@KA/CS的生物相容性和生物降解性。总之,我们介绍了一种利用磁性引导对壳聚糖进行有效止血的新方法,将BSA/Fe3O4@KA/CS定位为处理各种伤口的有希望的候选者。
    Severe bleeding from deep and irregular wounds poses a significant challenge in prehospital and surgical settings. To address this issue, we developed a novel chitosan-based hemostatic dressing with a magnetic targeting mechanism using Fe3O4, termed bovine serum albumin-modified Fe3O4 embedded in porous α-ketoglutaric acid/chitosan (BSA/Fe3O4@KA/CS). This dressing enhances hemostasis by magnetically guiding the agent to the wound site. In vitro, the hemostatic efficacy of BSA/Fe3O4@KA/CS is comparable to that of commercial chitosan (Celox™) and is not diminished by the modification. In vivo, BSA/Fe3O4@KA/CS demonstrated superior hemostatic performance and reduced blood loss compared to Celox™. The hemostatic mechanism of BSA/Fe3O4@KA/CS includes the concentration of solid blood components through water absorption, adherence to blood cells, and activation of the endogenous coagulation pathway. Magnetic field targeting is crucial in directing the dressing to deep hemorrhagic sites. Additionally, safety assessments have confirmed the biocompatibility and biodegradability of BSA/Fe3O4@KA/CS. In conclusion, we introduce a novel approach to modify chitosan using magnetic guidance for effective hemostasis, positioning BSA/Fe3O4@KA/CS as a promising candidate for managing various wounds.
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  • 文章类型: Journal Article
    目前,伤口敷料在临床应用中主要用于浅表皮肤伤口。然而,这些敷料具有显著的局限性,包括差的生物相容性和有限的促进伤口愈合的能力。为了解决这个问题,本研究以醛聚乙二醇为交联剂,设计了一种具有增强生物相容性的羧甲基壳聚糖-甲基丙烯酸明胶水凝胶,可以促进伤口愈合和血管生成。CSDG水凝胶表现出酸敏感性,具有高达300%的溶胀率。此外,它表现出优异的抗外部应力,承受高达160kPa的压力和80%的自变形。与市售壳聚糖伤口凝胶相比,CSDG水凝胶表现出优异的生物相容性,抗菌性能,和止血能力。体内外实验结果表明,CSDG水凝胶通过上调CD31、IL-6、和VEGF,从而促进伤口的快速愈合。总之,本研究成功制备了CSDG水凝胶伤口敷料,为开发基于天然大分子的水凝胶敷料提供了新的途径和方法。 .
    At present, wound dressings in clinical applications are primarily used for superficial skin wounds. However, these dressings have significant limitations, including poor biocompatibility and limited ability to promote wound healing. To address the issue, this study used aldehyde polyethylene glycol as the cross-linking agent to design a carboxymethyl chitosan-methacrylic acid gelatin hydrogel with enhanced biocompatibility, which can promote wound healing and angiogenesis. The CSDG hydrogel exhibits acid sensitivity, with a swelling ratio of up to 300%. Additionally, it exhibited excellent resistance to external stress, withstanding pressures of up to 160 kPa and self-deformation of 80%. Compared to commercially available chitosan wound gels, the CSDG hydrogel demonstrates excellent biocompatibility, antibacterial properties, and hemostatic ability. Bothin vitroandin vivoresults showed that the CSDG hydrogel accelerated blood vessel regeneration by upregulating the expression of CD31, IL-6, FGF, and VEGF, thereby promoting rapid healing of wounds. In conclusion, this study successfully prepared the CSDG hydrogel wound dressings, providing a new approach and method for the development of hydrogel dressings based on natural macromolecules.
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  • 文章类型: Journal Article
    背景:医用敷料旨在促进伤口愈合并减少感染。本项目旨在研究天然棕色棉敷料对大肠杆菌感染创面愈合的影响。
    方法:在本研究中,以脱脂白色棉纱布为对照组,以脱脂棕色棉纱布和脱脂漂白棕色棉纱布作为实验1组和实验2组,通过建立以大肠杆菌为感染生物的大鼠感染创面模型,探讨其对动物感染后创面损伤的修复效果。
    结果:通过分析伤口愈合状况,研究了促进感染伤口愈合的能力,宏观伤口愈合率,苏木精-伊红染色,Masson染色,用Elisa法检测炎症因子的分泌情况。结果显示在伤口愈合的第14天,3组敷料的宏观创面愈合率均大于98%;实验组1的胶原含量达到49.85±5.84%,实验组2的胶原含量达到53.48±5.32%,高于对照组;棕色棉纱布通过缩短炎症期来促进皮肤创面愈合。三种炎症因子THF-α的表达,IL-2、IL-8和三种细胞因子MMP-3、MMP-8、MMP-9均低于对照组。
    结论:天然棕色棉纱布对感染创面有较好的修复和促进愈合作用。开辟了天然棕色棉纱布在沾染创面医治中的运用。
    BACKGROUND: Medical dressings are designed to promote wound healing and reduce infection. The aim of project is to investigate the effect of natural brown colored cotton dressings on the healing of infected wounds in E.coli animals.
    METHODS: In this study, degreased white cotton gauze was used as the control group, with degreased brown cotton gauze and degreased bleached brown cotton gauze as the experimental group 1 and experimental group 2, to investigate the effect on the repair of post-infectious wound damage in animals by establishing an infected wound model in rats with E.coli as the infecting organism.
    RESULTS: The ability to promote healing of infected wounds was investigated by analyzing the wound healing status, macroscopic wound healing rate, hematoxylin-eosin staining, Masson staining, secretion of inflammatory factors by Elisa assay. The result showed that at day 14 of wound healing, the macroscopic wound healing rate was greater than 98% for all three groups of dressings; the collagen content reached 49.85 ± 5.84% in the experimental group 1 and 53.48 ± 5.32% in the experimental group 2, which was higher than the control group; brown cotton gauze promotes skin wound healing by shortening the inflammatory period in both groups. The expression of three inflammatory factors THF-α, IL-2, and IL-8 and three cytokines MMP-3, MMP-8, and MMP-9 were lower than that of the control group.
    CONCLUSIONS: It was found that natural brown cotton gauze has better repairing and promoting healing effect on infected wounds. It opens up the application of natural brown cotton gauze in the treatment of infected wounds.
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  • 文章类型: Journal Article
    不断升级的全球健康问题源于细菌感染引起的慢性伤口,对个人构成重大威胁。因此,开发水凝胶敷料以促进及时的伤口监测和有效的伤口管理是当务之急。为此,将pH敏感型溴百里酚蓝(BTB)和pH响应型药物盐酸四环素(TH)引入多糖基水凝胶中,实现伤口监测与控制治疗的一体化。多糖基水凝胶是通过席夫碱反应通过在氧化海藻酸钠(OSA)骨架上交联羧甲基壳聚糖(CMCS)形成的。BTB用作pH指示剂,通过视觉颜色变化来监测伤口感染。TH可以通过席夫碱键的pH响应动态释放,为慢性感染的伤口提供有效的治疗和长期抗菌活性。此外,聚乳酸纳米纤维(PLA)的引入提高了水凝胶的力学性能。多功能水凝胶具有优异的机械性能,自我修复,可注射,抗菌性能和生物相容性。此外,正在考虑的多面水凝胶敷料在促进慢性感染伤口的愈合过程中表现出值得注意的能力。因此,这项研究为智能和快速的细菌感染监测和动态治疗平台的发展提供了新的视角。
    The escalating global health concern arises from chronic wounds induced by bacterial infections, posing a significant threat to individuals. Consequently, an imperative exist for the development of hydrogel dressings to facilitate prompt wound monitoring and efficacious wound management. To this end, pH-sensitive bromothymol blue (BTB) and pH-responsive drug tetracycline hydrochloride (TH) were introduced into the polysaccharide-based hydrogel to realize the integration of wound monitoring and controlled treatment. Polysaccharide-based hydrogels were formed via a Schiff base reaction by cross-linking carboxymethyl chitosan (CMCS) on an oxidized sodium alginate (OSA) skeleton. BTB was used as a pH indicator to monitor wound infection through visual color changes visually. TH could be dynamically released through the pH response of the Schiff base bond to provide effective treatment and long-term antibacterial activity for chronically infected wounds. In addition, introducing polylactic acid nanofibers (PLA) enhanced the mechanical properties of hydrogels. The multifunctional hydrogel has excellent mechanical, self-healing, injectable, antibacterial properties and biocompatibility. Furthermore, the multifaceted hydrogel dressing under consideration exhibits noteworthy capabilities in fostering the healing process of chronically infected wounds. Consequently, the research contributes novel perspectives towards the advancement of intelligent and expeditious bacterial infection monitoring and dynamic treatment platforms.
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