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在粘菌盘基网柄菌发育过程中 TgrB1-TgrC1 细胞黏附复合物的组装。

Assembly of the TgrB1-TgrC1 cell adhesion complex during Dictyostelium discoideum development.

机构信息

*Department of Biochemistry, University of Toronto, Toronto, ON, Canada, M5S 1A8.

出版信息

Biochem J. 2014 Apr 15;459(2):241-9. doi: 10.1042/BJ20131594.

Abstract

In Dictyostelium discoideum, TgrB1 and TgrC1 are partners of a heterophilic cell-adhesion system. To investigate its assembly process, the split GFP complementation assay was used to track the oligomeric status of both proteins. The ability of TgrC1 to form cis-homodimers spontaneously was demonstrated by fluorescence complementation studies and confirmed by chemical cross-linking. In contrast, TgrB1 failed to form cis-homodimers in the absence of TgrC1. Treatment of cell aggregates with antibodies against TgrB1 or TgrC1 did not affect TgrC1 dimerization, but inhibited TgrB1 dimer formation, suggesting that TgrB1 cis-homodimerization is dependent on trans-interaction with TgrC1. When TgrB1 and TgrC1 conjugated with the complementary halves of GFP were co-expressed in cells, cis-heterodimers were not detected. However, weak FRET signals were detected in cells expressing TgrB1-RFP and TgrC1-GFP, suggesting that TgrB1 dimers and TgrC1 dimers were arranged juxtapose to each other in the adhesion complex. The results of the present study suggest that the assembly process is initiated upon trans-interaction of monomeric TgrB1 with TgrC1 homodimers on adjacent cells, which triggers the formation of TgrB1 dimers. The homodimerization of TgrB1 in turn induces the clustering of TgrB1 and TgrC1, and the coalescence of TgrB1-TgrC1 clusters results in the formation of large adhesion complexes.

摘要

在盘基网柄菌(Dictyostelium discoideum)中,TgrB1 和 TgrC1 是异源细胞粘附系统的伴侣。为了研究其组装过程,使用分裂 GFP 互补测定法来跟踪两种蛋白质的寡聚状态。荧光互补研究证明了 TgrC1 形成顺式同源二聚体的能力,并通过化学交联得到了证实。相比之下,在没有 TgrC1 的情况下,TgrB1 未能形成顺式同源二聚体。用针对 TgrB1 或 TgrC1 的抗体处理细胞聚集体不会影响 TgrC1 二聚体化,但会抑制 TgrB1 二聚体形成,表明 TgrB1 顺式同源二聚化依赖于与 TgrC1 的反式相互作用。当 TgrB1 和 TgrC1 与 GFP 的互补半部分缀合并在细胞中共同表达时,未检测到顺式异源二聚体。然而,在表达 TgrB1-RFP 和 TgrC1-GFP 的细胞中检测到弱的 FRET 信号,表明 TgrB1 二聚体和 TgrC1 二聚体在粘附复合物中彼此相邻排列。本研究的结果表明,组装过程是由单体 TgrB1 与相邻细胞上的 TgrC1 同源二聚体的反式相互作用引发的,这触发了 TgrB1 二聚体的形成。TgrB1 的同源二聚化继而诱导 TgrB1 和 TgrC1 的聚集,并且 TgrB1-TgrC1 簇的合并导致大的粘附复合物的形成。

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