Department of Functional Genomics, Institute of Molecular Biology and Genetics, 150 Zabolotnogo Street, Kyiv 03680, Ukraine.
Gene. 2011 Oct 10;485(2):120-9. doi: 10.1016/j.gene.2011.06.021. Epub 2011 Jun 25.
Intersectin 1 (ITSN1) is an evolutionarily conserved adaptor protein engaged in clathrin-mediated endocytosis, cell signaling and actin cytoskeleton rearrangements. Two major ITSN1 isoforms were initially described, the ubiquitous short isoform (ITSN1-s) and the long isoform (ITSN1-l) expressed predominantly in neurons. Numerous alternative splicing events for ITSN1 pre-mRNA were later identified. Here we describe a novel isoform ITSN1-22a with an alternative C-terminus encoded by exon 22a. This exon is only found in placental mammals. The transcript of ITSN1-22a is detected in a wide range of human and mouse tissues. We show here that two alternative splicing events affect the coding sequence of the ITSN1-22a isoform. Moreover, alternative polyadenylation of these transcripts was demonstrated in human tissues. The protein encoded by the ITSN1-22a transcript possesses two EH domains, a coiled-coil region, an SH3A domain and a specific C-terminal domain (CTD) but lacks four SH3 domains in comparison with ITSN1-s. The level of ITSN1-22a protein varies in different mouse tissues and human cell lines. The highest amounts of this isoform occur in mouse brain, spleen, lung and the human B cell line DG75. ITSN1-22a binds via its CTD to the SH3 domain of the endocytic protein amphiphysin 1 and the SH3A domain of ITSN1. Furthermore association in vivo and codistribution of ITSN1-22a and ITSN1-s were demonstrated suggesting that these isoforms could function in concert. We have revealed differential binding of ITSN1-s and ITSN1-22a to the ubiquitin ligase Cbl. Both isoforms possess the SH3A domain capable of binding to Cbl; however ITSN1-22a in contrast to ITSN1-s did not interact with Cbl in vivo. In vitro binding experiments demonstrated that the CTD of ITSN1-22a negatively regulated its binding to Cbl; at the same time interaction with another partner, dynamin 1 was not affected by the presence of the CTD. These data suggest that intramolecular interaction within ITSN1-22a could specifically regulate its binding to protein partners. Thus, this novel mammalian ITSN1 isoform possesses a significantly altered domain structure and performs specific protein-protein interactions.
衔接蛋白 1(ITSN1)是一种进化上保守的衔接蛋白,参与网格蛋白介导的内吞作用、细胞信号转导和肌动蛋白细胞骨架重排。最初描述了两种主要的 ITSN1 同工型,普遍存在的短同工型(ITSN1-s)和主要在神经元中表达的长同工型(ITSN1-l)。后来,人们发现了 ITSN1 前体 mRNA 的许多选择性剪接事件。在这里,我们描述了一种新型的同工型 ITSN1-22a,其 C 末端由外显子 22a 编码。该外显子仅存在于胎盘哺乳动物中。在广泛的人类和小鼠组织中检测到 ITSN1-22a 的转录本。我们在这里表明,两个选择性剪接事件影响 ITSN1-22a 同工型的编码序列。此外,在人类组织中证明了这些转录物的可变多聚腺苷酸化。由 ITSN1-22a 转录本编码的蛋白质具有两个 EH 结构域、一个卷曲螺旋区、一个 SH3A 结构域和一个特异的 C 末端结构域(CTD),但与 ITSN1-s 相比,它缺少四个 SH3 结构域。在不同的小鼠组织和人类细胞系中,ITSN1-22a 蛋白的水平不同。这种同工型在小鼠大脑、脾脏、肺和人类 B 细胞系 DG75 中的含量最高。ITSN1-22a 通过其 CTD 与内吞蛋白 amphiphysin 1 的 SH3 结构域和 ITSN1 的 SH3A 结构域结合。此外,体内关联和 ITSN1-22a 和 ITSN1-s 的共定位表明这些同工型可能协同发挥作用。我们发现 ITSN1-s 和 ITSN1-22a 与泛素连接酶 Cbl 的不同结合。这两种同工型都具有能够与 Cbl 结合的 SH3A 结构域;然而,与 ITSN1-s 不同的是,ITSN1-22a 体内并未与 Cbl 相互作用。体外结合实验表明,ITSN1-22a 的 CTD 负调控其与 Cbl 的结合;同时,与另一个伙伴 dynamin 1 的相互作用不受 CTD 的影响。这些数据表明,ITSN1-22a 内的分子内相互作用可以特异性调节其与蛋白质伙伴的结合。因此,这种新型的哺乳动物 ITSN1 同工型具有明显改变的结构域结构,并执行特定的蛋白质-蛋白质相互作用。
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