首页> 美国卫生研究院文献>Tissue Engineering and Regenerative Medicine >Effect of Palmitoyl-Pentapeptide (Pal-KTTKS) on Wound Contractile Process in Relation with Connective Tissue Growth Factor and α-Smooth Muscle Actin Expression
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Effect of Palmitoyl-Pentapeptide (Pal-KTTKS) on Wound Contractile Process in Relation with Connective Tissue Growth Factor and α-Smooth Muscle Actin Expression

机译:棕榈酰五肽(Pal-KTTKS)对伤口收缩过程的影响与结缔组织生长因子和α-平滑肌肌动蛋白的表达有关

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摘要

To evaluate whether Palmitoyl-pentapeptide (Pal-KTTKS), a lipidated subfragment of type 1 pro-collagen (residues 212–216), plays a role in fibroblast contractility, the effect of Pal-KTTKS on the expression of pro-fibrotic mediators in hypertropic scarring were investigated in relation with trans-differentiation of fibroblast to myofibroblast, an icon of scar formation. α-SMA was visualized by immunofluorescence confocal microscopy with a Cy-3-conjugated monoclonal antibody. The extent of α-SMA-positive fibroblasts was determined in collagen lattices and in cell culture study. Pal-KTTKS (0–0.5 µM) induced CTGF and α-SMA protein levels were determined by western blot analysis and fibroblast contractility was assessed in three-dimensional collagen lattice contraction assay. In confocal analysis, fibroblasts were observed as elongated and spindle shapes while myofibroblast observed as squamous, enlarged cells with pronounced stress fibers. Without Pal-KTTKS treatment, three quarters of the fibroblasts differentiates into the myofibroblast; α-SMA-positive stress fibers per field decreased twofold with 0.1 µM Pal-KTTKS treatment (75 ± 7.1 vs 38.6 ± 16.1%, n = 3, p < 0.05). The inhibitory effect was not significant in 0.5 µM Pal-KTTKS treatment. Stress fiber level and collagen contractility correlates with α-SMA expression level. In conclusion, Pal-KTTKS (0.1 µM) reduces α-SMA expression and trans-differentiation of fibroblasts to myofibroblast. The degree of reduction is dose-dependent. An abundance of myofibroblast and fibrotic scarring is correlated with excessive levels of α-SMA and collagen contractility. Delicate balance between the wound healing properties and pro-fibrotic abilities of pentapeptide KTTKS should be considered for selecting therapeutic dose for scar prevention.
机译:为了评估棕榈酰五肽(Pal-KTTKS)(一种脂化的1型胶原蛋白的亚片段)(残基212-216)是否在成纤维细胞的收缩中起作用,Pal-KTTKS对促成纤维细胞中促纤维化介质表达的影响研究了与成纤维细胞向成肌纤维细胞的转分化有关的增生性瘢痕形成,成肌纤维细胞是瘢痕形成的标志。通过与Cy-3偶联的单克隆抗体的免疫荧光共聚焦显微镜观察α-SMA。在胶原蛋白晶格和细胞培养研究中确定了α-SMA阳性成纤维细胞的程度。通过蛋白质印迹分析确定了Pal-KTTKS(0–0.5 µM)诱导的CTGF和α-SMA蛋白水平,并通过三维胶原蛋白晶格收缩测定法评估了成纤维细胞的收缩性。在共聚焦分析中,观察到成纤维细胞呈细长形和纺锤形,而成肌纤维细胞则呈鳞状,扩大的细胞,具有明显的应力纤维。没有Pal-KTTKS处理,四分之三的成纤维细胞分化为肌成纤维细胞。使用0.1μMPal-KTTKS处理后,每个视野的α-SMA阳性应力纤维减少了两倍(75±7.1对38.6±16.1%,n = 3,p <0.05)。在0.5μMPal-KTTKS处理中抑制作用不明显。应激纤维水平和胶原蛋白收缩性与α-SMA表达水平相关。总之,Pal-KTTKS(0.1 µM)降低了α-SMA的表达以及成纤维细胞向成肌纤维细胞的转分化。减少程度是剂量依赖性的。大量的成肌纤维细胞和纤维化瘢痕形成与过度水平的α-SMA和胶原蛋白收缩性相关。五肽KTTKS的伤口愈合特性与促纤维化能力之间应达到微妙的平衡,以选择预防疤痕的治疗剂量。

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