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Evaluation of recombinant CXCL8((3-73))K11R/G31P in muscle fibrosis and Trichinella larvae encapsulation in a murine model of trichinellosis

机译:重组CXCL8((3-73))K11R / G31P在旋毛虫病小鼠模型中的肌肉纤维化和旋毛虫幼虫包封的评估

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Trichinella spiralis (T. spiralis) larvae in raw or inadequately cooked meat can cause chronic infections in a wide range of hosts including humans. During the development inside the skeletal muscles, T. spiralis larvae infect muscle cells accompanying with the infiltration of host inflammatory cells, eventually create a new type of cell known as nurse cell developing a surrounding vascular network to support the larvae development. Controlling of host inflammatory responses and angiogenesis influences both the nurse cell differentiation and the parasite larvae development. CXCL8 is a chemokine that acts on G-protein coupled receptors, of which activation contributes to fibrosis and angiogenesis. CXCL8((3_73))K11R/G31P (G31P) has been reported as a CXCL8 analogue. The aim of this study is to investigate the effect of G31P in inflammatory responses and the development of T. spiralis larvae in muscle tissues of mice infected with T. spiralis. The level of inflammatory factors and the morphology of T. spiralis larvae in infected tissues were investigated through ELISA and electron-microscopy analysis. G31P up-regulated IFN-gamma and down-regulated CXCL8 level, and impaired the encapsulation of T. spiralis larvae in vivo. The results showed that G31P influenced the development of T. spiralis larvae in muscle tissues. (C) 2016 Elsevier B.V. All rights reserved.
机译:生的或煮熟的肉中的旋毛虫幼虫可在包括人类在内的许多宿主中引起慢性感染。在骨骼肌内部发育过程中,螺旋螺旋体幼虫会感染肌肉细胞,并伴随宿主炎症细胞的浸润,最终形成一种称为护士细胞的新型细胞,从而发展出周围的血管网络来支持幼虫的发育。宿主炎症反应和血管生成的控制影响护士细胞分化和寄生虫幼虫的发展。 CXCL8是一种作用于G蛋白偶联受体的趋化因子,其激活有助于纤维化和血管生成。据报道CXCL8((3_73))K11R / G31P(G31P)是CXCL8类似物。这项研究的目的是调查G31P在感染螺旋藻的小鼠肌肉组织中的炎症反应和螺旋藻幼虫的发育中的作用。通过ELISA和电子显微镜分析研究了感染组织中炎症因子的水平和螺旋体幼虫的形态。 G31P上调IFN-γ和下调CXCL8水平,并削弱了螺旋体幼虫在体内的封装。结果表明,G31P影响了螺旋组织幼虫在肌肉组织中的发育。 (C)2016 Elsevier B.V.保留所有权利。

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