负压封闭引流技术促进慢性复杂创面的愈合

目的:探讨负压封闭引流技术(VSD)对慢性复杂创面愈合的治疗效果。方法:选取各类慢性复杂性创面患者共65例,病程均超过3个月,将65例患者随机分为VSD组(35例)及对照组(30例)。VSD组定期更换VSD辅料;2周后视创面愈合情况,选择继续VSD治疗,或行II期修复治疗(直接拉拢缝合,皮片移植,或皮瓣移植修复)。对照组的治疗采用常规换药,即以凡士林油纱布及无菌纱布覆盖创面,内置引流条,每12 h换药一次。两组创面于治疗前及治疗后各个时间点分别对比创面愈合率及创面组织细菌计数。结果:VSD治疗组患者全部愈合,治愈率达100%,对照组30例患者中治愈率为86.7%。两组治愈率相比无明显统计学差异(P0.05)。VSD治疗组平均愈合时间为22±3.3天,对照组平均愈合时间为35±5.8天,两组愈合时间的差异具有统计学意义(P0.01)。治疗后相同检测时间点VSD组创面细菌含量显著低于对照组,两组创面细菌含量的差异具有统计学意义(P0.05)。结论:负压封闭引流技术(VSD)在提高慢性复杂创面的愈合率及清除创面细菌方面具有显著的效果。     

基于"湿性愈合"理论的新型敷料在糖尿病足溃疡创面处理中的应用

目的:观察基于"湿性愈合"理论的新型敷料用于糖尿病足溃疡创面的处理的治疗效果。方法:首先评估糖尿病足溃疡创面,然后根据不同情况采用不同新型敷料,应用湿性伤口愈合理论对48例糖尿病足溃疡的患者进行临床研究,选取48例传统方法处理的同类患者作为对照。结果:结果显示湿性愈合组患者出院时的创面愈合率较对照组明显提高,治疗周期明显缩短(P<0.05),换药次数明显减少(P<0.05)。结论:基于"湿性愈合"理论的新型敷料在糖尿病足溃疡创面的处理中取得了良好效果,值得进一步研究与应用。     

封闭负压引流对兔糖尿病溃疡创面组织愈合影响的观察

目的:探讨封闭负压引流(VAC)对兔糖尿病溃疡创面组织愈合的影响及其可能机制。方法:采用四氧嘧啶法建立兔糖尿病溃疡模型,设空白对照组和实验组(对照组创面采用常规包扎治疗处理,实验组创面则采用VAC处理),观察和比较两组动物的创面肉眼观、愈合时间,在致伤前、致伤后3 d、7 d、14 d取创面软组织,检测和比较两组动物的创面组织含水量、血流量以及血浆ET-1和NO含量。结果:与对照组比较,实验组动物的创面肿胀及分泌物得到明显控制,创面坏死组织的清除与肉芽组织的生长明显加快,平均愈合时间明显缩短(P0.05);致伤后3 d、7 d和14 d,创面组织含水量与血浆ET-1含量明显下降(P0.05),创面组织血流量与血浆NO含量明显增加(P0.05)。结论:VAC对兔糖尿病溃疡创面组织的愈合可起到积极的促进作用,这可能与其增加血浆NO含量及降低ET-1的含量有关,其具体机制尚有待于进一步的研究。     

红光促进难治性创面愈合的研究

目的:探讨红光照射对难治性创面的创缘组织中血管内皮细胞生长因子(vascular endothelial growth factor,VEGF)的表达及治疗难治性创面的临床效果。方法:收集2008年6月-2010年12月因难治性创面入住笔者单位治疗的40例患者,按治疗方法分为红光照射治疗组20例和常规治疗组20例。常规治疗组患者创面以0.5%碘伏与水胶体敷料换药。治疗组在常规治疗的基础上加用红光照射。于治疗后第7天、14天、21天切取创缘组织,研究红光照射对创缘组织中VEGF的影响,并比较两组患者的创面愈合率和愈合时间。结果:临床实验中,治疗组创缘组织中的VEGF含量明显高于对照组(P<0.01);治疗组创面愈合率明显高于对照组(P<0.01);治疗组的愈合时间低于对照组(P<0.05)。结论:红光照射能显著提高创缘组织中VEGF含量,减少创面愈合时间,促进愈合。     

封闭负压引流联合局部给氧治疗兔耳缺血性创面的实验研究

目的:观察封闭负压引流联合局部给氧促进兔耳缺血性创面愈合的效果。方法:28只大耳白兔,双耳背各造成直径2.5cm全层皮肤缺损,结扎中央血管神经束及后边缘动静脉,形成缺血创面。56个创面随机分为七组:A组(-50mmHg负压同时给氧,浓度为40%±5%,每日4小时)、B组(持续-50mmHg负压4小时继之局部给氧1小时)、C组(负压治疗4min,停止1min,每日4小时,之后给氧1小时),D组(-50mmHg负压治疗每日4小时)、E组(-125mmHg负压治疗每日4小时)、F组(单纯给40%±5%氧1小时)和G组(空白对照)。在创面形成第0、1、3、5、7、10、14、18天拍照,测量创面面积,计算创面愈合率及创面愈合时间;在各时相点切取创面标本,组织学观察创面肉芽、上皮生长、水肿和炎细胞,Ki67免疫组化标记增殖细胞并计算增殖指数,TUNEL法计算凋亡指数。结果:负压给氧组在相同时相点创面愈合率高于单纯负压、氧疗或空白组(P<0.05),创面肉芽生长快,水肿和炎症轻,细胞增殖指数高于对照组(P<0.05),而细胞凋亡指数显著低于对照组(P<0.05)。结论:负压联合局部给氧能显著促进兔耳缺血创面的愈合。     

壳聚糖复合KGF 2突变体温敏敷料联合简易负压吸引法对压力性损伤的疗效

目的探究壳聚糖复合角质细胞生长因子(keratinocyte growth factor-2,KGF-2)突变体温敏敷料联合简易负压吸引法对长期卧床老年患者大面积压力性损伤的治疗效果。方法选择2016年1月至2018年12月我院普外科收治的90名大面积压力性损伤患者,随机分为对照组与观察组,各45例。对照组患者采用简易负压吸引联合传统泡沫敷料治疗,观察组患者在此基础上联合壳聚糖复合KGF-2突变体温敏敷料填充。比较两组患者的伤口愈合效果以及创面细菌检出率。结果观察组患者的伤口愈合总有效率(93.3%)明显高于对照组(75.6%),差异有统计学意义(χ~2=5.41,P=0.003)。观察组患者细菌检出率(8.89%)显著低于对照组(35.56%),差异有统计学意义(χ~2=3.02,P=0.003)。结论壳聚糖复合KGF-2突变体温敏敷料联合简易负压吸引法能显著促进长期卧床老年患者大面积压力性损伤创面愈合,降低交叉感染的风险,具有较好的临床应用效果。     

负压封闭引流治疗厌氧菌感染创面的临床观察

目的:观察负压封闭引流联合双氧水冲洗治疗厌氧菌感染创面的临床治疗效果。方法:收集我院收治的创面厌氧菌感染患者60例,随机分为两组。其中,对照组(30例)患者采用常规换药治疗创面厌氧菌感染,VSD组(30例)患者给予负压封闭引流并辅以双氧水冲洗治疗。观察并比较两组患者厌氧菌清除率,以及创面愈合情况。结果:VSD组创面厌氧菌感染率明显低于对照组,创面愈合效果优于对照组,差异有统计学意义(P0.01)。结论:负压封闭引流不仅能够有效控制感染创面厌氧菌生长,而且可以有效促进创面愈合,对临床具有指导意义。     

糖尿病足溃疡的危险因素探讨及亲水性纤维含银敷料促进患者伤口愈合的临床对照研究

摘要 目的：探讨糖尿病足溃疡（DFU）的危险因素,并研究亲水性纤维含银敷料促进患者伤口愈合的应用价值。方法：选取2017年8月-2020年12月期间我院收治的糖尿病患者230例。230例糖尿病患者中发生DFU的79例,纳为DFU组,剩余151例未发生DFU,纳为无DFU组。DFU组的患者采用随机数字表法分为治疗1组39例和治疗2组40例,治疗1组给予传统纱布敷料,治疗2组给予亲水性纤维含银敷料。采用多因素Logistic回归分析DFU发生的危险因素。观察治疗1组、治疗2组的临床疗效和临床指标。结果：DFU组、无DFU组在性别、年龄、户籍地、糖尿病病程、并发下肢血管病变、并发周围神经病变、足底有胼胝、血红蛋白（Hb）、C反应蛋白（CRP）、白蛋白（ALB）、总胆固醇（TC）、纤维蛋白原（FIB）、红细胞沉降率（ESR）、高密度脂蛋白（HDL）、 胱抑C（CysC）、 低密度脂蛋白（LDL）、脂蛋白a[Lp(a)]、糖化血红蛋白（HbAlc）方面对比差异有统计学意义（P<0.05）。男性、糖尿病病程、并发下肢血管病变、并发周围神经病变、足底有胼胝、ALB、ESR、CysC、CRP、Lp(a)、HbAlc均是DFU发生的危险因素（P<0.05）。治疗2组的临床总有效率明显高于治疗1组（P<0.05）。治疗2组的创面愈合时间、出现明显肉芽时间、住院时间短于治疗1组,住院费用高于治疗1组（P<0.05）。结论：DFU的发生受到多种因素影响,包括男性、糖尿病病程、并发下肢血管病变等,因此临床应加强对这些因素的预防和控制。此外,亲水性纤维含银敷料可促进DFU患者创面愈合,疗效显著。     

负压创面治疗技术对皮肤移植成活的临床观察及实验研究

目的:采用负压固定移植皮片方法,观察负压创面治疗技术(negative-pressure wound therapy,NPWT)对游离皮片成活的影响,初步探讨微血管形成与皮肤成活之间的关系。方法:采用回顾性研究的方法,对65例皮肤缺损的患者,根据皮肤移植术后皮片固定方法的不同,分为两组,其中I组为NPWT治疗组,有35例患者,刃厚游离皮片移植术后行创面负压吸引治疗;II组为常规治疗组,有30例患者,刃厚游离皮片移植术后用打包或加压包扎的方式固定。Balb/c小鼠20只,按皮片移植后不同固定加压方式,分为实验组:负压创面治疗技术使用组(10只),对照组:打包加压组(10只),于皮片移植术后第5天,大体观察移植皮片颜色、有无水疱、有无皮下积液及质地,计算并比较皮片成活率,以免疫组化染色标记毛细血管内皮,检测皮片中微血管情况。结果:临床观察表明:I组术后皮片成活时间平均较II组缩短,有统计学差异(P<0.01),I组术后住院治疗时间平均较II组缩短5天,有统计学差异(P<0.01),I组术后抗生素费用、换药次数及换药费用较II组减少,有统计学差异(P<0.01)。动物实验结果表明:术后第5天,实验组小鼠移植皮片中微血管增生较对照组明显增多(P<0.05)。结论:与常规打包或加压包扎固定皮片的方式相比,负压创面治疗技术的应用可以缩短皮片成活时间,缩短患者住院治疗时间,减少抗生素的使用及换药次数,促进移植皮片中毛细血管增生,提高皮片成活率。     

负压吸引治疗法在手显微外科的临床应用概况

<正>负压吸引治疗方法主要包括负压封闭引流(vacuum sealing drainage,VSD)、真空辅助闭合(vacuum-assisted closure,VAC)和负压创面治疗法(negative pressure wound therapy,NPWT),目前已广泛应用于医学各领域。临床上主要用于手显微外科、创伤骨科、普外科、烧伤科、整形外科、胸外科的急性损伤和慢性创面愈合方面以及压力性溃疡(褥疮)、糖尿病足等难治性创面的治疗。本文就负压吸引技术在手显微外科相关疾病治疗研究进展作一综述如下。     

外科新三联疗法治疗糖尿病足的临床观察

目的:观察外科新三联疗法(外科换药-威伐激光-成纤维细胞生长因子)治疗糖尿病足溃疡的临床疗效和安全性。方法:将57例糖尿病足溃疡患者随机分为2组。对照组28例,采用外科换药辅以成纤维细胞生长因子外敷治疗;治疗组29例,在对照组治疗的基础上配合威伐激光照射治疗。疗程为8周,观察两组患者的治疗有效率、愈合时间和不良反应的发生情况。结果:治疗组和对照组的有效率分别为86.21%、57.14%,治疗组显著高于对照组(P0.05);且治疗组溃疡的愈合时间(39.40±2.24天)较对照组(50.67±2.31天)明显缩短(P0.01)。此外,两组患者均无明显的不良反应发生。结论:外科新三联疗法(外科换药-威伐激光-成纤维细胞生长因子)是治疗糖尿病足溃疡的有效方法,且安全性好。     

Circulating fibrocyte mobilization in negative pressure wound therapy

Non‐healing diabetic wounds are difficult to treat. They also create heavy financial burdens for both patients and society. Negative pressure wound therapy (NPWT) has been adopted to treat intractable wounds and has proved to be effective. However, the mechanisms that underlie the effects of this treatment are not entirely understood. Circulating fibrocytes are unique haematopoietic‐derived stem cells that have been reported to play a pivotal role in wound healing. Here, we have investigated the effect of NPWT on fibrocyte mobilization and the role of fibrocyte mobilization in the healing of diabetic wounds during NPWT. We show that the NPWT group exhibited 2.6‐fold to 12.1‐fold greater numbers of tail vein‐injected PKH‐26‐labelled fibrocytes in the diabetic wound sites compared with the control group. We also demonstrate that the full‐thickness skin wounds treated with NPWT exhibit significantly reduced mRNA and protein expression, blood vessel density and proliferating cells when exogenous fibrocyte mobilization is inhibited. We speculate that systemic mobilization of fibrocytes during NPWT may be a mechanism for healing intractable wounds in a diabetic rat model experiment and that enhancement of cell mobilization may represent a potential treatment idea for intractable wound healing across all fields of surgery.     

Negative pressure wound therapy reduces the motility of <Emphasis Type="Italic">Pseudomonas aeruginosa</Emphasis> and enhances wound healing in a rabbit ear biofilm infection model

Pseudomonas aeruginosa motility, virulence factors and biofilms are known to be detrimental to wound healing. The efficacy of negative pressure wound therapy (NPWT) against P. aeruginosa has been little studied, either in vitro or in vivo. The present study evaluated the effect of negative pressure (NP) on P. aeruginosa motility in vitro, and the effect of NPWT on virulence factors and biofilms in vivo. P. aeruginosa motility was quantified under different levels of NP (atmospheric pressure, ? 75, ? 125, ? 200 mmHg) using an in vitro model. Swimming, swarming and twitching motility were significantly inhibited by NP (? 125 and ? 200 mmHg) compared with atmospheric pressure (p = 0.05). Virulence factors and biofilm components were quantified in NPWT and gauze treated groups using a rabbit ear biofilm model. Biofilm structure was studied with fluorescence microscopy and scanning electron microscopy. Additionally, viable bacterial counts and histological wound healing parameters were measured. Compared with the control, NPWT treatment resulted in a significant reduction in expression of all virulence factors assayed including exotoxin A, rhamnolipid and elastase (p = 0.01). A significant reduction of biofilm components (eDNA) (p = 0.01) was also observed in the NPWT group. The reduction of biofilm matrix was verified by fluorescence- and scanning electron-microscopy. NPWT lead to better histologic parameters (p = 0.01) and decreased bacterial counts (p = 0.05) compared with the control. NPWT treatment was demonstrated to be an effective strategy to reduce virulence factors and biofilm components, which may explain the increased wound healing observed.     

A pilot randomised controlled trial of negative pressure wound therapy to treat grade III/IV pressure ulcers [ISRCTN69032034

ABSTRACT: BACKGROUND: Negative pressure wound therapy (NPWT) is widely promoted as a treatment for full thickness wounds, however there is a lack of high-quality research evidence regarding its clinical and cost effectiveness. A trial of NPWT for the treatment grade III/IV pressure ulcers would be worthwhile but premature without assessing whether such a trial is feasible. The aim of this pilot randomised controlled trial was to assess the feasibility of conducting a future full trial of NPWT for the treatment of grade III and IV pressure ulcers and to pilot all aspects of the trial. METHODS: This was a two centre (acute and community), pilot randomised controlled trial. Eligible participants were randomised to receive either NPWT or Standard Care (SC) (spun hydrocolloid, alginate or foam dressings). The primary outcome measure was time to healing of the reference pressure ulcer. Secondary outcome measures included recruitment rates, frequency of treatment visits, resources used and duration of follow-up. RESULTS: 312 patients were screened for eligibility into this trial over a 12-month recruitment period and 12/312 participants (3.8%) were randomised; six to NPWT and six to SC. Only one reference pressure ulcer healed (NPWT group) during follow up (time to healing 79 days). The mean number of treatment visits per week was 3.1 (NPWT) and 5.7 (SC). 6/6 TNP and 1/6 SC participants withdrew from their allocated trial treatment. The mean duration of follow-up was 3.8 (NPWT) and 5.0 (SC) months. CONCLUSIONS: This pilot trial yielded vital information for the planning of any future full study including a projected recruitment rate, required duration of follow up and extent of research nurse support required. Data were also used to inform cost-effectiveness and value of information analyses which were conducted alongside the pilot trial.     

负压创面治疗技术对皮肤移植成活的临床观察及实验研究

目的：采用负压固定移植皮片方法,观察负压创面治疗技术（negative-pressure wound therapy,NPWT）对游离皮片成活的影响,初步探讨微血管形成与皮肤成活之间的关系。方法：采用回顾性研究的方法,对65例皮肤缺损的患者,根据皮肤移植术后皮片固定方法的不同,分为两组,其中Ⅰ组为NPWT治疗组,有35例患者,刃厚游离皮片移植术后行创面负压吸引治疗;Ⅱ组为常规治疗组。有30例患者,刃厚游离皮片移植术后用打包或加压包扎的方式固定。Balb／c小鼠20只,按皮片移植后不同固定加压方式,分为实验组：负压创面治疗技术使用组（10只）,对照组：打包加压组（10只）,于皮片移植术后第5天,大体观察移植皮片颜色、有无水疱、有无皮下积液及质地,计算并比较皮片成活率,以免疫组化染色标记毛细血管内皮,检测皮片中微血管情况。结果：临床观察表明：Ⅰ组术后皮片成活时间平均较Ⅱ组缩短,有统计学差异（P〈0．01）,Ⅰ组术后住院治疗时间平均较Ⅱ组缩短5天,有统计学差异（P〈0．01）,Ⅰ组术后抗生素费用、换药次数及换药费用较Ⅱ组减少,有统计学差异（P〈0．01）。动物实验结果表明：术后第5天,实验组小鼠移植皮片中微血管增生较对照组明显增多（P〈0．05）。结论：与常规打包或加压包扎固定皮片的方式相比,负压创面治疗技术的应用可以缩短皮片成活时间,缩短患者住院治疗时间,减少抗生素的使用及换药次数,促进移植皮片中毛细血管增生,提高皮片成活率。     

Negative-Pressure Wound Therapy Enhances Local Inflammatory Responses in Acute Infected Soft-Tissue Wound

Clinical studies found that negative-pressure wound therapy (NPWT) displayed significant clinical benefits in the healing of infected wounds. However, the effect of NPWT on local inflammatory responses in acute infected soft-tissue wound has not been investigated thoroughly. The purpose of this study was to test the impact of NPWT on local expression of proinflammatory cytokines, amount of neutrophils, and bacterial bioburden in wound from acute infected soft-tissue wounds. Full-thickness wounds were created on the back of rabbits, and were inoculated with Staphylococcus aureus strain ATCC29213. The wounds were treated with sterile saline-moistened gauze dressings and NPWT with continuous negative pressure (?125 mmHg). Wound samples were harvested on days 0 (6 h after bacterial inoculation), 2, 4, 6, and 8 at the center of wound beds before irrigation for real-time PCR analysis of gene expression of IL-1β, IL-8, and TNF-α. Wound biopsies were examined histologically for neutrophil quantification in different layers of tissue. Quantitative bacterial cultures at the same time point were analyzed for bacterial clearance. Application of NPWT to acute infected wounds in rabbits was compared with treatment with sterile saline-moistened gauze, over an 8-day period. NPWT-treated wounds exhibited earlier and greater peaking of IL-1β and IL-8 expression and decrease in TNF-α expression over the early 4 days (P < 0.05). Furthermore, histologic examination revealed that significantly increased neutrophil count was observed in the shallow layer in wound biopsies of NPWT treatment at day 2 (P < 0.001). In addition, there was a statistically significant decrease of bacteria load from baseline (day 0) at days 2 and 8 in NPWT group (P < 0.05). In conclusion, this study demonstrates that NPWT of acute infected soft-tissue wounds leads to increased local IL-1β and IL-8 expression in early phase of inflammation, which may trigger accumulation of neutrophils and thus accelerate bacterial clearance. Meanwhile, the success of NPWT in the treatment of acute wounds can attenuate the expression of TNF-α, and the result may partly explain how NPWT can avoid significantly impairing wound healing.     

Negative pressure wound therapy promotes muscle‐derived stem cell osteogenic differentiation through MAPK pathway

Negative pressure wound therapy (NPWT) has been revealed to be effective in the treatment of open fractures, although the underlying mechanism is not clear. This article aimed to investigate the effects of NPWT on muscle‐derived stem cell (MDSC) osteoblastic differentiation and the related potential mechanism. The cell proliferation rate was substantially increased in NPWT‐treated MDSCs in comparison with a static group for 3 days. There was no observable effect on the apoptosis of MDSC treated with NPWT compared with the control group for 3 days. The expression levels of HIF‐1α, BMP‐2, COL‐I, OST and OPN were increased on days 3, 7 and 14, but the expression level of Runx2 was increased on days 3 and 7 in the NPWT group. Pre‐treatment, the specific inhibitors were added into the MDSCs treated with NPWT and the control group. ALP activity and mineralization were reduced by inhibiting the ERK1/2, p38 and JNK pathways. The expression levels of Runx2, COL‐I, OST and OPN genes and proteins were also decreased using the specific MAPK pathway inhibitors on days 3, 7 and 14. There were no significant effects on the expression of BMP‐2 except on day 3. However, the expressions of the HIF‐1α gene and protein slightly increased when the JNK pathway was inhibited. Therefore, NPWT promotes the proliferation and osteogenic differentiation of MDSCs through the MAPK pathway.