Calcium Signaling Initiated by Agonists in Mesenchymal Stromal Cells from the Human Adipose Tissue

P. Kotova, O. A. Rogachevskaja, M. Bystrova, E. N. Kochkina, D. S. Ivashin, S. Kolesnikov
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引用次数: 2

Abstract

Mesenchymal stromal cells (MSCs) from different sources represent a heterogeneous population of proliferating non-differentiated cells that contain multipotent stem cells capable of originating a variety of mesenchymal cell lineages. By using Ca 2+ imaging and the Ca 2+ dye Fluo -4 , we studied MSCs from the human adipose tissue and examined Ca 2+ signaling initiated by a variety of GPCR ligands, focusing primarily on adrenergic and purinergic agonists. Being characterized by a relative change of Fluo -4 fluorescence, ago-nist-induced Ca 2+ responses were generated in an “all-or-nothing” fashion. Specifically, at relatively low doses, agonists elicited undetectable responses but initiated quite simi- lar Ca 2+ transients at all concentrations above the threshold. The inhibitory analysis and Ca 2+ /IP 3 uncaging pointed at the phosphoinositide cascade as a pivotal pathway responsible for agonist transduction and implicated Ca 2+ -induced Ca 2+ release (CICR) in shaping agonists-dependent Ca 2+ signals. Altogether, our data suggest that agonist transduction in MSCs includes two fundamentally different stages: an agonist initially triggers a local, gradual, and relatively small Ca 2+ signal, which next stimulates CICR to accomplish transduction with a large and global Ca 2+ transient. By involving the trigger-like mechanism CICR, a cell is capable of generating Ca 2+ responses of virtually universal shape and magnitude at different agonist concentrations above the threshold.
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人脂肪组织间充质间质细胞中激动剂引发的钙信号传导
来自不同来源的间充质基质细胞(MSCs)代表了一种异质性的增殖非分化细胞群,其中包含能够产生多种间充质细胞系的多能干细胞。通过ca2 +成像和ca2 +染料Fluo -4,我们研究了来自人类脂肪组织的MSCs,并检测了多种GPCR配体引发的ca2 +信号,主要关注肾上腺素能和嘌呤能激动剂。ago-nist诱导的ca2 +响应以“全有或全无”的方式产生,其特征是Fluo -4荧光的相对变化。具体来说,在相对较低的剂量下,激动剂引起了无法检测到的反应,但在高于阈值的所有浓度下,都引发了非常相似的ca2 +瞬态。抑制分析和ca2 + / ip3的释放表明,磷酸肌苷级联是激动剂转导的关键途径,并涉及ca2 +诱导的ca2 +释放(CICR)在形成激动剂依赖的ca2 +信号中。总之,我们的数据表明,激动剂在MSCs中的转导包括两个基本不同的阶段:激动剂最初触发局部、渐进和相对较小的ca2 +信号,然后刺激CICR以大的全局ca2 +瞬时信号完成转导。通过触发机制CICR,细胞能够在超过阈值的不同激动剂浓度下产生几乎普遍形状和大小的ca2 +反应。
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