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Human canonical CD157/Bst1 is an alternatively spliced isoform masking a previously unidentified primate-specific exon included in a novel transcript

机译:人类规范CD157 / Bst1是一种选择性剪接的亚型,掩盖了新转录本中先前未鉴定的灵长类特异性外显子

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CD157/Bst1 is a dual-function receptor and β-NAD+-metabolizing ectoenzyme of the ADP-ribosyl cyclase family. Expressed in human peripheral blood neutrophils and monocytes, CD157 interacts with extracellular matrix components and regulates leukocyte diapedesis via integrin-mediated signalling in inflammation. CD157 also regulates cell migration and is a marker of adverse prognosis in epithelial ovarian cancer and pleural mesothelioma. One form of CD157 is known to date: the canonical sequence of 318 aa from a 9-exon transcript encoded by BST1 on human chromosome 4. Here we describe a second BST1 transcript, consisting of 10 exons, in human neutrophils. This transcript includes an unreported exon, exon 1b, located between exons 1 and 2 of BST1. Inclusion of exon 1b in frame yields CD157-002, a novel proteoform of 333 aa: exclusion of exon 1b by alternative splicing generates canonical CD157, the dominant proteoform in neutrophils and other tissues analysed here. In comparative functional analyses, both proteoforms were indistinguishable in cell surface localization, specific mAb binding, and behaviour in cell adhesion and migration. However, NAD glycohydrolase activity was detected in canonical CD157 alone. Comparative phylogenetics indicate that exon 1b is a genomic innovation acquired during primate evolution, pointing to the importance of alternative splicing for CD157 function.
机译:CD157 / Bst1是双功能受体,是ADP-核糖基环化酶家族的β-NAD+代谢型外切酶。在人类外周血中性粒细胞和单核细胞中表达的CD157与细胞外基质成分相互作用,并通过整联蛋白介导的炎症信号调节白细胞渗尿。 CD157还调节细胞迁移,是上皮性卵巢癌和胸膜间皮瘤不良预后的标志。迄今为止已知一种形式的CD157:来自BST1在人染色体4上编码的9外显子转录本的318aa的规范序列。在这里,我们描述了人类嗜中性白细胞中由10个外显子组成的第二BST1转录本。此成绩单包括一个未报告的外显子,外显子1b,位于BST1的外显子1和2之间。在框架中包含外显子1b会产生CD157-002,一种新的333aa蛋白质形式:通过选择性剪接排除外显子1b会产生规范CD157,这是中性粒细胞和此处分析的其他组织中的主要蛋白形式。在比较功能分析中,两种蛋白形式在细胞表面定位,特异性mAb结合以及细胞黏附和迁移行为方面均无法区分。但是,仅在规范CD157中检测到NAD糖水解酶活性。比较的系统发育学表明,外显子1b是在灵长类动物进化过程中获得的基因组创新,指出了CD157功能的可变剪接的重要性。

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