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甘油磷酸肌醇 -4 - 磷酸通过蛋白酪氨酸激酶依赖的Vav激活增强SDF - 1α刺激的T细胞趋化性。

Glycerophosphoinositol-4-phosphate enhances SDF-1alpha-stimulated T-cell chemotaxis through PTK-dependent activation of Vav.

作者信息

Patrussi Laura, Mariggio' Stefania, Paccani Silvia Rossi, Capitani Nagaja, Zizza Pasquale, Corda Daniela, Baldari Cosima T

机构信息

Department of Evolutionary Biology, University of Siena, Via Aldo Moro 2, 53100, Siena, Italy.

出版信息

Cell Signal. 2007 Nov;19(11):2351-60. doi: 10.1016/j.cellsig.2007.07.014. Epub 2007 Jul 28.

Abstract

Glycerophosphoinositols (GPIs) are water-soluble phosphoinosite metabolites produced by all cell types, whose levels increase in response to a variety of extracellular stimuli, and are particularly high in Ras-transformed cells. GPIs are released to the extracellular space, wherefrom they can be taken up by other cells through a specific transporter. Exogenous GPIs affect a plethora of cellular functions. Among these compounds the most active is GroPIns4P, which affects cAMP levels and PKA-dependent functions through the inhibition of heterotrimeric Gs proteins. GroPIns4P has also recently been found to promote actin cytoskeleton reorganization by inducing Rho and Rac activation through an as yet unidentified mechanism. Here we have assessed the potential effects of GroPIns4P on T-cells. We found that GroPIns4P enhances CXCR4-dependent chemotaxis. This activity results from the capacity of GroPIns4P to activate the Rho GTPase exchange factor, Vav, through an Lck-dependent pathway which also results in activation of the stress kinases JNK and p38. GroPIns4P was also found to activate with a delayed kinetics the Lck-dependent activation of ZAP-70, Shc and Erk1/2. The activities of GroPIns4P were found to be dependent on its capacity to inhibit cAMP production and PKA activation. Collectively, the data provide the first evidence of a role of glycerophosphoinositols as modulators of T-cell signaling and establish a mechanistic basis for the effects of this phosphoinositide derivative on F-actin dynamics.

摘要

甘油磷酸肌醇(GPIs)是所有细胞类型都能产生的水溶性磷酸肌醇代谢产物,其水平会因各种细胞外刺激而升高,在Ras转化细胞中含量尤其高。GPIs会释放到细胞外空间,其他细胞可通过特定转运蛋白从该空间摄取它们。外源性GPIs会影响大量细胞功能。在这些化合物中,活性最强的是GroPIns4P,它通过抑制异源三聚体Gs蛋白来影响cAMP水平和PKA依赖性功能。最近还发现,GroPIns4P可通过一种尚未明确的机制诱导Rho和Rac激活,从而促进肌动蛋白细胞骨架重组。在此,我们评估了GroPIns4P对T细胞的潜在影响。我们发现,GroPIns4P可增强CXCR4依赖性趋化作用。这种活性源于GroPIns4P通过Lck依赖性途径激活Rho GTPase交换因子Vav的能力,该途径还会导致应激激酶JNK和p38的激活。还发现GroPIns4P能以延迟动力学激活ZAP-70、Shc和Erk1/2的Lck依赖性激活。发现GroPIns4P的活性取决于其抑制cAMP产生和PKA激活的能力。总体而言,这些数据首次证明了甘油磷酸肌醇作为T细胞信号调节剂的作用,并为这种磷酸肌醇衍生物对F-肌动蛋白动力学的影响建立了机制基础。

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