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嘌呤能信号在干细胞分化和组织再生中的作用。

Perspectives of purinergic signaling in stem cell differentiation and tissue regeneration.

机构信息

Departamento de Bioquímica , Instituto de Química, Universidade São Paulo, Av. Prof. Lineu Prestes, 748-Bloco 8S/Room 0858, CEP: 05508-900, São Paulo, SP, Brazil.

出版信息

Purinergic Signal. 2012 Sep;8(3):523-37. doi: 10.1007/s11302-011-9282-3. Epub 2011 Dec 6.

Abstract

Replacement of lost or dysfunctional tissues by stem cells has recently raised many investigations on therapeutic applications. Purinergic signaling has been shown to regulate proliferation, differentiation, cell death, and successful engraftment of stem cells originated from diverse origins. Adenosine triphosphate release occurs in a controlled way by exocytosis, transporters, and lysosomes or in large amounts from damaged cells, which is then subsequently degraded into adenosine. Paracrine and autocrine mechanisms induced by immune responses present critical factors for the success of stem cell therapy. While P1 receptors generally exert beneficial effects including anti-inflammatory activity, P2 receptor-mediated actions depend on the subtype of stimulated receptors and localization of tissue repair. Pro-inflammatory actions and excitatory tissue damages mainly result from P2X7 receptor activation, while other purinergic receptor subtypes participate in proliferation and differentiation, thereby providing adequate niches for stem cell engraftment and novel mechanisms for cell therapy and endogenous tissue repair. Therapeutic applications based on regulation of purinergic signaling are foreseen for kidney and heart muscle regeneration, Clara-like cell replacement for pulmonary and bronchial epithelial cells as well as for induction of neurogenesis in case of neurodegenerative diseases.

摘要

干细胞替代丢失或功能失调的组织最近引起了许多关于治疗应用的研究。嘌呤能信号转导已被证明可调节来自不同来源的干细胞的增殖、分化、细胞死亡和成功植入。三磷酸腺苷(adenosine triphosphate,ATP)通过胞吐作用、转运体和溶酶体以受控方式释放,或者大量从受损细胞中释放,然后被降解为腺苷。免疫反应引起的旁分泌和自分泌机制是干细胞治疗成功的关键因素。虽然 P1 受体通常发挥有益作用,包括抗炎活性,但 P2 受体介导的作用取决于受刺激受体的亚型和组织修复的定位。促炎作用和兴奋组织损伤主要由 P2X7 受体激活引起,而其他嘌呤能受体亚型参与增殖和分化,从而为干细胞植入提供适当的小生境,并为细胞治疗和内源性组织修复提供新的机制。基于嘌呤能信号转导调节的治疗应用被预见可用于肾脏和心肌再生、Clara 样细胞替代肺和支气管上皮细胞,以及在神经退行性疾病的情况下诱导神经发生。

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