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首页> 外文期刊>Tissue engineering, Part A >APRIL and BAFF proteins increase proliferation of human adipose-derived stem cells through activation of Erk1/2 MAP kinase
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APRIL and BAFF proteins increase proliferation of human adipose-derived stem cells through activation of Erk1/2 MAP kinase

机译:APRIL和BAFF蛋白通过激活Erk1 / 2 MAP激酶增强人脂肪干细胞的增殖

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Human adipose-derived stem cells (hASC) are mesenchymal stem cells with reduced immunogenicity and the ability to modulate immune responses. APRIL and BAFF proteins are overexpressed in inflammatory and autoimmune diseases for which allogeneic hASC therapy is currently under clinical investigation. Modification of hASC properties by the tissue microenvironment could be a critical factor in patient outcome and is still not well understood. Our aim was to characterize the APRIL/BAFF system in hASC by analyzing the ligand and receptor expression patterns, the effects mediated by APRIL and BAFF on hASC, and the underlying signaling. We found that hASC express the tumor necrosis factor proteins APRIL (a proliferation-inducing ligand) and BAFF (B cell-activator factor) as well as their receptors TACI (transmembrane activator and calcium-modulator and cyclophilin ligand interactor), BCMA (B cell maturation antigen) and the BAFF-specific receptor (BAFF-R). APRIL and BAFF secretion was differentially enhanced by CXCL12 and interferon (IFN)-γ, implicated in hASC-mediated migration and immunosuppression, respectively. In addition, APRIL and BAFF induced rapid phosphorylation of extracellular signal-regulated kinases 1/2 (ERK1/2) and Akt kinases and promoted an increase in hASC proliferation, without affecting the immunosuppressive capacity of these cells. The use of specific chemical inhibitors indicated that the PI3K transduction pathway is involved in hASC basal growth and that APRIL-and BAFF-mediated effects are ERK-dependent. These results provide new information about the molecular mechanisms that underlie APRIL and BAFF secretion and signaling in hASC, and are of special relevance for the use of allogeneic hASC as therapeutic tools.
机译:人脂肪来源的干细胞(hASC)是具有降低的免疫原性和调节免疫反应能力的间充质干细胞。 APRIL和BAFF蛋白在同种异体hASC治疗目前正在临床研究中的炎性和自身免疫性疾病中过表达。组织微环境对hASC特性的改变可能是影响患者预后的关键因素,目前尚不清楚。我们的目的是通过分析配体和受体表达模式,APRIL和BAFF介导的对hASC的作用以及潜在的信号传导来表征hASC中的APRIL / BAFF系统。我们发现,hASC表达肿瘤坏死因子蛋白APRIL(一种诱导增殖的配体)和BAFF(B细胞激活因子),以及它们的受体TACI(跨膜激活剂和钙调节剂以及亲环蛋白配体相互作用子),BCMA(B细胞)成熟抗原)和BAFF特异性受体(BAFF-R)。 CPRI12和干扰素-γ分别增强了APRIL和BAFF的分泌,分别与hASC介导的迁移和免疫抑制有关。此外,APRIL和BAFF诱导细胞外信号调节激酶1/2(ERK1 / 2)和Akt激酶的快速磷酸化,并促进hASC增殖的增加,而不会影响这些细胞的免疫抑制能力。使用特定的化学抑制剂表明,PI3K转导途径与hASC的基础生长有关,而APRIL和BAFF介导的作用是ERK依赖性的。这些结果提供了有关hASC中APRIL和BAFF分泌和信号传导基础的分子机制的新信息,并且对于使用同种异体hASC作为治疗工具特别相关。

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