胰腺星状细胞:胰腺肿瘤微环境的最高管理者。

N. Stanishevska
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Activation triggers for PSC are Yes-associated protein, TGF-β1, miRNA let-7d, IL-8, MCP1, TGF-β2, IGFBP2, and others. 10 actively expressed genes were identified: TP53, SRC, IL6, JUN, ISG15, CAD, STAT1, OAS3, OAS1, VIM during co-cultivation of a cancer cell line (PCC) with PSC. PSC deactivation is associated with speckle-type mediator POZ (SPOP) acting through nuclear factor-kappaB, transretinoic acid (ATRA). Exhibiting their activity, PSCs express several stem cell markers, α-SMA (α-actin of smooth muscle cells), vimentin, α ITGA 11 (collagen type I receptor), α5 integrin receptor ITGA5 (fibronectin receptor), hyaluronic acid, hyaluronan synthase 2 (HAS2), hyaluronidase 1 (HYAL1), BAG3 , matrix metallopeptidase 2 (MMP2), Nodal protein, miR-1246 and miR-1290, miR-210, CCN2 (connective tissue growth factor), TRPV1, SP and CGRP (Calcitonin gene-related peptide) and many other factors. Сonclusion. 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引用次数: 0

摘要

星状胰腺细胞作为基质成分的产生细胞,积极地与癌细胞相互作用,决定了癌细胞之间基质屏障的形成,从而提供肿瘤化疗耐药。目的对星状细胞在胰腺肿瘤间质微环境形成中的作用、星状细胞功能调控和实现的分子机制等方面的最新研究进展进行综述。方法采用复合材料分析法对数据进行处理。结果。星状胰腺细胞(PSC)表现出两种表型和功能状态:不活跃和活跃。PSC的激活是由肿瘤细胞通过多种分子介质进行的。PSC的激活触发因子有yes相关蛋白、TGF-β1、miRNA let-7d、IL-8、MCP1、TGF-β2、IGFBP2等。在PCC与PSC共培养过程中,共鉴定出10个活性表达基因:TP53、SRC、IL6、JUN、ISG15、CAD、STAT1、OAS3、OAS1、VIM。PSC失活与斑点型介质POZ (SPOP)通过核因子κ b、转维甲酸(ATRA)作用有关。PSCs表现出活性,表达多种干细胞标志物α- sma(平滑肌细胞α-肌动蛋白)、vimentin、α ITGA 11(胶原I型受体)、α5整合素受体ITGA5(纤维连接蛋白受体)、透明质酸、透明质酸合成酶2 (HAS2)、透明质酸酶1 (HYAL1)、BAG3、基质金属肽酶2 (MMP2)、结蛋白、miR-1246和miR-1290、miR-210、结缔组织生长因子CCN2、TRPV1、SP和降钙素基因相关肽CGRP等多种因子。Сonclusion。星状胰腺细胞是腺间基质的产生者,受多种因子(TNF-α、IL-6、MCP-1、ATP、HMGB1等)的激活,包括胰腺肿瘤细胞产生的因子,具有增殖、迁移和抑制肿瘤细胞凋亡的调节作用。肿瘤组织中α ITGA 11 (I型胶原受体)、α5整合素受体ITGA5(纤维连接蛋白受体)、金属肽酶、Nodal蛋白、miR-1246、miR-1290、miR-210的表达增加,表明这些细胞被激活。PSC活性状态的维持是由肿瘤细胞提供的,其中星状胰腺细胞在肿瘤过程的进展中是伙伴。对psc -肿瘤细胞系统相互作用机制的进一步研究为揭示胰腺肿瘤发病机制的影响杠杆创造了前景。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Pancreatic stellate cells: the top managers of the pancreatic tumor microenvironment.
Background Stellate pancreatocytes, being cells - producers of stromal components, actively interact with cancer cells, determine the formation of a stromal barrier between the latter and thereby provide tumor chemoresistance. Objective The review is devoted to the analysis of recent data on the role of stellate pancreatocytes in the formation of the stromal microenvironment of pancreatic tumors, molecular mechanisms through which the regulation and realization of stellate cell functions is carried out. Methods Data processing was carried out by the method of complex material analysis. Results. Stellate pancreatocytes (PSC) exhibit phenotypically and functionally two states: inactive and active. PSC activation is carried out by cells of the developing tumor through a variety of molecular mediators. Activation triggers for PSC are Yes-associated protein, TGF-β1, miRNA let-7d, IL-8, MCP1, TGF-β2, IGFBP2, and others. 10 actively expressed genes were identified: TP53, SRC, IL6, JUN, ISG15, CAD, STAT1, OAS3, OAS1, VIM during co-cultivation of a cancer cell line (PCC) with PSC. PSC deactivation is associated with speckle-type mediator POZ (SPOP) acting through nuclear factor-kappaB, transretinoic acid (ATRA). Exhibiting their activity, PSCs express several stem cell markers, α-SMA (α-actin of smooth muscle cells), vimentin, α ITGA 11 (collagen type I receptor), α5 integrin receptor ITGA5 (fibronectin receptor), hyaluronic acid, hyaluronan synthase 2 (HAS2), hyaluronidase 1 (HYAL1), BAG3 , matrix metallopeptidase 2 (MMP2), Nodal protein, miR-1246 and miR-1290, miR-210, CCN2 (connective tissue growth factor), TRPV1, SP and CGRP (Calcitonin gene-related peptide) and many other factors. Сonclusion. Stellate pancreatocytes, being producers of the interacinar stroma, are activated by various factors (TNF-α, IL-6, MCP-1, ATP, and HMGB1, etc.), including factors produced by tumor cells of the pancreas, and act as regulators of proliferation, migration, and suppression apoptosis of the latter. An increase in the expression of α ITGA 11 (type I collagen receptor), α5 integrin receptor ITGA5 (fibronectin receptor), metallopeptidases, Nodal protein, miR-1246, miR-1290, and miR-210 is observed in tumor tissue, that indicates the activation of these cells. The maintenance of the active state of PSC is provided by tumor cells, for which stellate pancreatocytes are partners in the progression of the neoplastic process. Further study of the mechanisms of interaction in the PSC-tumor cell system creates the prospect of revealing levers of influence on the pathogenesis of pancreatic tumors.
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