结缔组织生长因子参与人和大鼠急性坏死性胰腺炎的胰腺修复及组织重塑。
Connective tissue growth factor is involved in pancreatic repair and tissue remodeling in human and rat acute necrotizing pancreatitis.
作者信息
di Mola Fabio F, Friess Helmut, Riesle Erick, Koliopanos Alexander, Büchler Peter, Zhu Zhaowen, Brigstock David R, Korc Murray, Büchler Markus W
机构信息
Department of General Surgery, University of Heidelberg, Germany.
出版信息
Ann Surg. 2002 Jan;235(1):60-7. doi: 10.1097/00000658-200201000-00008.
OBJECTIVE
To analyze the involvement of connective tissue growth factor (CTGF) in the transforming growth factor-beta (TGF-beta) pathway during acute necrotizing pancreatitis (ANP) in humans and rats.
SUMMARY BACKGROUND DATA
Connective tissue growth factor is involved in several fibrotic diseases and has a critical role in fibrogenesis and tissue remodeling after injury.
METHODS
Normal human pancreas tissue samples were obtained through an organ donor program from five individuals without a history of pancreatic disease. Human ANP tissues were obtained from eight persons undergoing surgery for this disease. In rats, ANP was induced by intraductal infusion of taurocholate. The expression of CTGF was studied by Northern blot analysis, in situ hybridization, and immunohistochemistry in both human and rat pancreatic tissue samples.
RESULTS
Northern blot analysis revealed enhanced CTGF mRNA expression in human ANP tissue samples compared with normal controls. In addition, a concomitant increase in TGF-beta1 was present. By in situ hybridization, CTGF mRNA was localized in the remaining acinar and ductal cells and in fibroblasts. In regions of intense damage adjacent to areas of necrosis, CTGF mRNA signals were most intense. Inflammatory cells were devoid of any CTGF mRNA signals. By immunohistochemistry, CTGF protein was localized at high levels in the same cell types as CTGF mRNA. In ANP in rats, concomitantly enhanced mRNA levels of CTGF, TGF-beta1, and collagen type 1 were present, with a biphasic peak pattern on days 2 to 3 and day 7 after induction of ANP.
CONCLUSIONS
These data indicate that CTGF participates in tissue remodeling in ANP. The expression of CTGF predominantly in the remaining acinar and ductal cells indicates that extracellular matrix synthesis after necrosis is at least partly regulated by the remaining pancreatic parenchyma and only to a minor extent by inflammatory cells. Blockage of CTGF, a downstream mediator of TGF-beta in fibrogenesis, might be useful as a target to influence and reduce fibrogenesis in this disorder.
目的
分析结缔组织生长因子(CTGF)在人类和大鼠急性坏死性胰腺炎(ANP)期间转化生长因子-β(TGF-β)通路中的作用。
总结背景数据
结缔组织生长因子参与多种纤维化疾病,在损伤后的纤维生成和组织重塑中起关键作用。
方法
通过器官捐赠计划从五名无胰腺疾病病史的个体获取正常人类胰腺组织样本。从八名接受该疾病手术的患者获取人类ANP组织。在大鼠中,通过导管内注入牛磺胆酸盐诱导ANP。采用Northern印迹分析、原位杂交和免疫组织化学方法研究人类和大鼠胰腺组织样本中CTGF的表达。
结果
Northern印迹分析显示,与正常对照相比,人类ANP组织样本中CTGF mRNA表达增强。此外,TGF-β1也随之增加。通过原位杂交,CTGF mRNA定位于剩余的腺泡和导管细胞以及成纤维细胞中。在坏死区域附近的严重损伤区域,CTGF mRNA信号最强。炎症细胞未检测到任何CTGF mRNA信号。通过免疫组织化学,CTGF蛋白定位于与CTGF mRNA相同的细胞类型中且水平较高。在大鼠ANP中,CTGF、TGF-β1和I型胶原的mRNA水平同时增强,在诱导ANP后第2至3天和第7天呈双相峰值模式。
结论
这些数据表明CTGF参与ANP的组织重塑。CTGF主要在剩余的腺泡和导管细胞中表达,表明坏死后细胞外基质的合成至少部分受剩余胰腺实质调节,而炎症细胞的调节作用较小。CTGF作为TGF-β在纤维生成中的下游介质,阻断其作用可能是影响和减少该疾病纤维生成的一个有用靶点。
Zotero 插件