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可变剪接调节果蝇 Ubx 蛋白的功能。

Alternative splicing modulates Ubx protein function in Drosophila melanogaster.

机构信息

Department of Zoology, University of Cambridge, Cambridge CB2 3EJ, UK.

出版信息

Genetics. 2010 Mar;184(3):745-58. doi: 10.1534/genetics.109.112086. Epub 2009 Dec 28.

Abstract

The Drosophila Hox gene Ultrabithorax (Ubx) produces a family of protein isoforms through alternative splicing. Isoforms differ from one another by the presence of optional segments-encoded by individual exons-that modify the distance between the homeodomain and a cofactor-interaction module termed the "YPWM" motif. To investigate the functional implications of Ubx alternative splicing, here we analyze the in vivo effects of the individual Ubx isoforms on the activation of a natural Ubx molecular target, the decapentaplegic (dpp) gene, within the embryonic mesoderm. These experiments show that the Ubx isoforms differ in their abilities to activate dpp in mesodermal tissues during embryogenesis. Furthermore, using a Ubx mutant that reduces the full Ubx protein repertoire to just one single isoform, we obtain specific anomalies affecting the patterning of anterior abdominal muscles, demonstrating that Ubx isoforms are not functionally interchangeable during embryonic mesoderm development. Finally, a series of experiments in vitro reveals that Ubx isoforms also vary in their capacity to bind DNA in presence of the cofactor Extradenticle (Exd). Altogether, our results indicate that the structural changes produced by alternative splicing have functional implications for Ubx protein function in vivo and in vitro. Since other Hox genes also produce splicing isoforms affecting similar protein domains, we suggest that alternative splicing may represent an underestimated regulatory system modulating Hox gene specificity during fly development.

摘要

果蝇的 Hox 基因 Ultrabithorax(Ubx)通过选择性剪接产生了一系列蛋白同工型。同工型之间的差异在于存在可选片段——由单个外显子编码——这些片段改变了同源域和一个称为“YPWM”基序的辅助因子相互作用模块之间的距离。为了研究 Ubx 选择性剪接的功能意义,我们在这里分析了单个 Ubx 同工型对胚胎中胚层中天然 Ubx 分子靶标 decapentaplegic(dpp)基因的激活的体内影响。这些实验表明,Ubx 同工型在胚胎发生过程中在中胚层组织中激活 dpp 的能力不同。此外,使用一种 Ubx 突变体,该突变体将完整的 Ubx 蛋白谱减少到仅一种同工型,我们获得了影响前腹肌肉模式形成的特定异常,证明 Ubx 同工型在胚胎中胚层发育过程中不能互换。最后,一系列体外实验表明,Ubx 同工型在辅助因子 Extradenticle(Exd)存在的情况下结合 DNA 的能力也不同。总之,我们的结果表明,选择性剪接产生的结构变化对 Ubx 蛋白在体内和体外的功能具有功能意义。由于其他 Hox 基因也产生影响类似蛋白结构域的剪接同工型,我们认为选择性剪接可能代表了一个被低估的调节系统,可在果蝇发育过程中调节 Hox 基因的特异性。

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