参与胰腺星状细胞活性及与胰腺癌细胞相互作用的信号通路

N. Stanishevska
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The Нedgehog signaling pathway provides interaction between PSC and tumor cells, which involves the leading mediator of this pathway - sHH (sonic hedgehog), the overexpression of which is recorded in the tumor tissue of the pancreas and ensures the formation of the tumor stroma. Stellate pancreatocytes also trigger the HGF / c-Met / survivin signaling pathway for invasion and metastasis. The activation of the PSCs themselves may be mediated by serotonin via the RhoA / ROCK signaling pathway. While the proliferation and migration of these cells, activated by alcohol, HNE (human neutrophil elastase), PDGF, IL-33 PSC are regulated by the MAP kinase and PI3K pathways. The Wnt signaling pathway promotes collagen accumulation. Through the AMPK / mTOR pathway, factor FTY720 induces apoptosis and inhibits the autophagy of stellate pancreatocytes. The interaction of PSC and tumor cells is also mediated through Notch and TGF-β, and through the Hippo signaling pathway with the participation of YAP / TAZ factors, it is possible to suppress the fibrotic activity of PSC. The interaction of stellate pancreatocytes and tumor cells is reflected in a direct correlation between a decrease in autophagy and apoptosis of stellate pancreatocytes and suppression of invasion and migration of tumor cells. This interaction can be mediated by ERK1 / 2 kinase. Among the factors secreted by tumor cells and causing PSC activation are: growth factor β1 (TGF-β1), PAI-1 protein, translation initiation factor 4E (eIF4E), sHH (involving PSC in pain deployment), Exo-Pan and Exo-Mia exosomes (engaging PSCs in carcinogenesis). Deactivation is mediated by colony stimulating factor 1 (CSF1R, cytokine). 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引用次数: 0

摘要

背景。星状胰腺细胞的激活、增殖和迁移能力是由一系列信号分子机制保证的,这些机制支持肿瘤细胞与PSC的相互作用,并决定肿瘤的发生过程。本综述是一系列致力于对星状胰腺细胞的作用和功能的现代理解的文章的延续,即它们参与与癌细胞的相互作用和提供星状胰腺细胞-癌细胞系统协同作用的信号分子途径。方法。数据处理采用复合材料分析方法。结果。Нedgehog信号通路提供PSC与肿瘤细胞之间的相互作用,其中涉及该通路的主要介质- sHH (sonic hedgehog),其过表达在胰腺肿瘤组织中被记录下来,并确保肿瘤间质的形成。星状胰腺细胞也可触发HGF / c-Met / survivin信号通路,参与细胞的侵袭和转移。PSCs本身的激活可能是由血清素通过RhoA / ROCK信号通路介导的。而这些细胞在酒精、HNE(人中性粒细胞弹性酶)、PDGF、IL-33 PSC的激活下,其增殖和迁移受MAP激酶和PI3K通路的调控。Wnt信号通路促进胶原蛋白积累。FTY720因子通过AMPK / mTOR通路诱导星状胰腺细胞凋亡,抑制自噬。PSC与肿瘤细胞的相互作用也是通过Notch和TGF-β介导的,并且通过Hippo信号通路在YAP / TAZ因子的参与下,有可能抑制PSC的纤维化活性。星状胰腺细胞与肿瘤细胞的相互作用体现在星状胰腺细胞自噬和凋亡的减少与肿瘤细胞侵袭和迁移的抑制之间的直接相关性。这种相互作用可以通过ERK1 / 2激酶介导。肿瘤细胞分泌导致PSC活化的因子有:生长因子β1 (TGF-β1)、PAI-1蛋白、翻译起始因子4E (eIF4E)、sHH(参与PSC疼痛部署)、Exo-Pan和Exo-Mia外泌体(参与PSC癌变)。失活是由集落刺激因子1 (CSF1R)介导的。反过来,星状胰腺细胞分泌趋化因子CXCL1,刺激肿瘤细胞的迁移和侵袭,具有多个mirna的外泌体,刺激癌细胞的增殖和迁移。Сonclusion。星状胰腺细胞的激活是实现其纤维化功能所必需的,是通过RhoA / ROCK信号通路通过血清素介导的。Hippo通路(激活)和AMPK / mTOR(抑制自噬和激活凋亡)也参与星状胰腺细胞活性的调节。肿瘤细胞与星状胰腺细胞通过Hedgehog、Notch和TGF-β信号通路相互作用;调控癌细胞的侵袭和转移提供了HGF / c-Met / survivin信号通路。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Signaling pathways involved in pancreatic stellate cells activity and interaction with pancreatic cancer cells
Background. The activation, proliferation and migration capabilities of stellate pancreatocytes are guaranteed by a number of signaling molecular mechanisms that support the interaction of tumor cells with the PSC and determine the neoplastic process. Objective The review is a continuation of aт articles series devoted to the modern understanding of the role and functions of stellate pancreatocytes, namely, their involvement in interaction with cancer cells and signaling molecular pathways that provide synergism of the stellate pancreatocyte-cancer cell system. Methods. Data processing was carried out by the method of complex material analysis. Results. The Нedgehog signaling pathway provides interaction between PSC and tumor cells, which involves the leading mediator of this pathway - sHH (sonic hedgehog), the overexpression of which is recorded in the tumor tissue of the pancreas and ensures the formation of the tumor stroma. Stellate pancreatocytes also trigger the HGF / c-Met / survivin signaling pathway for invasion and metastasis. The activation of the PSCs themselves may be mediated by serotonin via the RhoA / ROCK signaling pathway. While the proliferation and migration of these cells, activated by alcohol, HNE (human neutrophil elastase), PDGF, IL-33 PSC are regulated by the MAP kinase and PI3K pathways. The Wnt signaling pathway promotes collagen accumulation. Through the AMPK / mTOR pathway, factor FTY720 induces apoptosis and inhibits the autophagy of stellate pancreatocytes. The interaction of PSC and tumor cells is also mediated through Notch and TGF-β, and through the Hippo signaling pathway with the participation of YAP / TAZ factors, it is possible to suppress the fibrotic activity of PSC. The interaction of stellate pancreatocytes and tumor cells is reflected in a direct correlation between a decrease in autophagy and apoptosis of stellate pancreatocytes and suppression of invasion and migration of tumor cells. This interaction can be mediated by ERK1 / 2 kinase. Among the factors secreted by tumor cells and causing PSC activation are: growth factor β1 (TGF-β1), PAI-1 protein, translation initiation factor 4E (eIF4E), sHH (involving PSC in pain deployment), Exo-Pan and Exo-Mia exosomes (engaging PSCs in carcinogenesis). Deactivation is mediated by colony stimulating factor 1 (CSF1R, cytokine). In turn, stellate pancreatocytes secrete the chemokine CXCL1, which stimulates the migration and invasion of tumor cells, exosomes with multiple miRNAs, which stimulate the proliferation and migration of cancer cells. Сonclusion. The activation of stellate pancreatocytes, which is necessary for the implementation of their fibrotic functions, is mediated through the RhoA / ROCK signaling pathway via serotonin. The Hippo pathway (activation) and AMPK / mTOR (suppression of autophagy and activation of apoptosis) are also involved in the regulation of the activity of stellate pancreatocytes. The interaction between the tumor cell and stellate pancreatocyte occurs through the Hedgehog, Notch, and TGF-β signaling pathways; regulation of invasion and metastasis of cancer cells provides the HGF / c-Met / survivin signaling pathway.
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