Laminin-511 Activates the Human Induced Pluripotent Stem Cell Survival via α6β1 Integrin-Fyn-RhoA-ROCK Signaling.

IF 2.5 3区医学 Q3 CELL & TISSUE ENGINEERING Stem cells and development Pub Date : 2022-11-01 DOI:10.1089/scd.2022.0010

Yoshiki Nakashima, Masayoshi Tsukahara

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引用次数: 2

Abstract

In human induced pluripotent stem cells (hiPSCs), laminin-511/α6β1 integrin interacts with E-cadherin, an intercellular adhesion molecule, to induce the activation of the phosphatidylinositol 3-kinase (PI3K)-dependent signaling pathway. The interaction between laminin-511/α6β1 integrin and E-cadherin, an intercellular adhesion molecule, results in protection against apoptosis through the proto-oncogene tyrosine-protein kinase Fyn(Fyn)-RhoA-ROCK signaling pathway and the Ras homolog gene family member A (RhoA)/Rho kinase (ROCK) signaling pathway (the major pathway for cell death). In this article, the impact of laminin-511 on hiPSC on α6β1 integrin-Fyn-RhoA-ROCK signaling is discussed and explored along with validation experiments. PIK3CA mRNA (mean [standard deviation {SD}]: iMatrix-511, 1.00 [0.61]; collagen+MFGE8, 0.023 [0.02]; **P < 0.01; n = 6) and PIK3R1 mRNA (mean [SD]: iMatrix-511, 1.00 [0.79]; collagen+MFGE8, 0.040 [0.06]; *P < 0.05; n = 6) were upregulated by iMatrix-511 resulting from an increased expression of Integrin α6 mRNA (mean [SD]: iMatrix-511, 1.00 [0.42]; collagen+MFGE8, 0.23 [0.05]; **P < 0.01; n = 6). The iMatrix-511 increased the expression of p120-Catenin mRNA (mean [SD]: iMatrix-511, 1.00 [0.71]; collagen+MFGE8, 0.025 [0.03]; **P < 0.01; n = 6) and RAC1 mRNA (mean [SD]: iMatrix-511, 1.00 [0.28]; collagen+MFGE8, 0.39 [0.15]; **P < 0.01; n = 6) by increasing the expression of E-cadherin mRNA (mean [SD]: iMatrix-511, 1.00 [0.38]; collagen+MFGE8, 0.16 [0.11]; **P < 0.01; n = 6). As a result, iMatrix-511 increased the expression of P190 RhoGAP (GTPase-activating proteins) mRNA, such as ARHGAP1 mRNA (mean [SD]: iMatrix-511, 1.00 [0.57]; collagen+MFGE8, 0.032 [0.03]; **P < 0.01; n = 6), ARHGAP4 mRNA (mean [SD]: iMatrix-511, 1.00 [0.56]; collagen+MFGE8, 0.039 [0.049]; **P < 0.01; n = 6), and ARHGAP5 mRNA (mean [SD]: iMatrix-511, 1.00 [0.39]; collagen+MFGE8, 0.063 [0.043]; **P < 0.01; n = 6). Western blotting showed that phospho-Rac1 remained in the cytoplasm and phospho-Fyn showed nuclear transition in iPSCs cultured on iMatrix-511. Proteome analysis showed that PI3K signaling was enhanced and cytoskeletal actin was activated in iPSCs cultured on iMatrix-511. In conclusion, laminin-511 strongly activated the cell survival by promoting α6β1 integrin-Fyn-RhoA-ROCK signaling in hiPSCs.

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Laminin-511通过α6β1 Integrin-Fyn-RhoA-ROCK信号激活人诱导多能干细胞存活

在人诱导多能干细胞(hiPSCs)中，层粘连蛋白-511/α6β1整合素与细胞间粘附分子E-cadherin相互作用，诱导磷脂酰肌醇3-激酶(PI3K)依赖信号通路的激活。层粘连蛋白-511/α6β1整合素与细胞间粘附分子E-cadherin相互作用，通过原癌基因酪氨酸-蛋白激酶Fyn(Fyn)-RhoA-ROCK信号通路和Ras同源基因家族成员A (RhoA)/Rho激酶(ROCK)信号通路(细胞死亡的主要途径)对细胞凋亡起到保护作用。本文结合验证实验，探讨了hiPSC中laminin-511对α6β1 integrin-Fyn-RhoA-ROCK信号传导的影响。PIK3CA mRNA(均值[标准差{SD}]: iMatrix-511, 1.00 [0.61];胶原+MFGE8, 0.023 [0.02];**P n = 6)和PIK3R1 mRNA (mean [SD]: iMatrix-511, 1.00 [0.79];胶原+MFGE8, 0.040 [0.06];*P n = 6)， iMatrix-511上调了Integrin α6 mRNA的表达(平均值[SD]: iMatrix-511, 1.00 [0.42];胶原+MFGE8, 0.23 [0.05];**P n = 6)。iMatrix-511增加了p120-Catenin mRNA的表达(平均[SD]: iMatrix-511, 1.00 [0.71];胶原+MFGE8, 0.025 [0.03];**P n = 6)和RAC1 mRNA (mean [SD]: iMatrix-511, 1.00 [0.28];胶原+MFGE8, 0.39 [0.15];**P n = 6)通过增加E-cadherin mRNA的表达(mean [SD]: iMatrix-511, 1.00 [0.38];胶原+MFGE8, 0.16 [0.11];**P n = 6)。结果，iMatrix-511增加了P190 RhoGAP (gtpase激活蛋白)mRNA的表达，如ARHGAP1 mRNA (mean [SD]: iMatrix-511, 1.00 [0.57];胶原+MFGE8, 0.032 [0.03];* * P n = 6), ARHGAP4 mRNA(意味着(SD): imatrix - 511, 1.00 (0.56);胶原+MFGE8, 0.039 [0.049];**P n = 6)， ARHGAP5 mRNA (mean [SD]: iMatrix-511, 1.00 [0.39];胶原+MFGE8, 0.063 [0.043];**P n = 6)。Western blot结果显示，在iMatrix-511上培养的iPSCs中，phospho-Rac1保留在细胞质中，phospho-Fyn出现核转移。蛋白质组学分析显示，在iMatrix-511上培养的iPSCs中，PI3K信号通路增强，细胞骨架肌动蛋白被激活。综上所述，laminin-511通过促进hipsc中α6β1 integrin-Fyn-RhoA-ROCK信号通路，强烈激活细胞存活。

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来源期刊

Stem cells and development 医学-细胞与组织工程

CiteScore

7.80

自引率

2.50%

发文量

审稿时长

3 months

期刊介绍： Stem Cells and Development is globally recognized as the trusted source for critical, even controversial coverage of emerging hypotheses and novel findings. With a focus on stem cells of all tissue types and their potential therapeutic applications, the Journal provides clinical, basic, and translational scientists with cutting-edge research and findings. Stem Cells and Development coverage includes: Embryogenesis and adult counterparts of this process Physical processes linking stem cells, primary cell function, and structural development Hypotheses exploring the relationship between genotype and phenotype Development of vasculature, CNS, and other germ layer development and defects Pluripotentiality of embryonic and somatic stem cells The role of genetic and epigenetic factors in development