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Identification of a new isoform of the murine Sh2d1a gene and its functional implications

机译:小鼠Sh2d1a基因新同种型的鉴定及其功能含义

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Signaling lymphocytic activation molecule (SLAM)-associated protein (SAP) is a Src homology (SH) domain 2-containing intracellular adaptor protein that is predominantly expressed in the hematopoietic system by T lymphocytes and NK cells. SAP protein is encoded by the SH2D1A gene located on the X chromosome. Loss-of-function mutations in SAP cause the X-linked lymphoproliferative disease (XLP), a severe immunodeficiency characterized by heightened susceptibility to Epstein-Barr virus and impaired humoral immunity. Normal individuals express several functional and non-functional isoforms of SAP as a result of alternative splicing. In this study, we identify a cryptic exon in the murine Sh2d1a gene. At the mRNA level, the new isoform of SAP (SAP-2) that includes this new exon is widely expressed in lymphoid tissues by C57BL/6 and 129 strains of inbred mice. SAP-2 accounts for approximately 1%–3% of total SAP transcripts, and it is dynamically regulated during lymphocyte activation. At the protein level, the SAP-2 isoform is a 144 amino-acid protein. Compared to the dominant 126 aminoacid SAP-1 isoform, the additional 18 amino acids are inserted into a structural region that is critical for phosphotyrosine binding. Our functional analysis in vitro indicates that SAP-2 is a non-functional isoform due to decreased protein stability. Thus, both human and mouse have multiple SAP splice isoforms that may or may not function. Modulation of relative proportions of these isoforms is potentially a mechanism whereby cells can regulate SAP-mediated biological activities.
机译:信号淋巴细胞活化分子(SLAM)相关蛋白(SAP)是一种包含Src同源性(SH)结构域2的细胞内衔接蛋白,主要在T细胞和NK细胞的造血系统中表达。 SAP蛋白由位于X染色体上的SH2D1A基因编码。 SAP中功能丧失的突变会导致X连锁淋巴组织增生性疾病(XLP),这是一种严重的免疫缺陷,其特征在于对爱泼斯坦-巴尔病毒的敏感性增强和体液免疫力受损。正常个体由于选择性剪接而表达了几种功能性和非功能性SAP同工型。在这项研究中,我们确定了小鼠Sh2d1a基因中的一个隐性外显子。在mRNA水平上,C57BL / 6和129个近交系小鼠在淋巴组织中广泛表达了包括该新外显子的SAP新同种型(SAP-2)。 SAP-2约占总SAP笔录的1%–3%,并且在淋巴细胞激活过程中受到动态调节。在蛋白质水平上,SAP-2同工型是144个氨基酸的蛋白质。与主要的126个氨基酸的SAP-1同种型相比,将其他18个氨基酸插入对磷酸酪氨酸结合至关重要的结构区域。我们的体外功能分析表明,由于蛋白质稳定性下降,SAP-2是一种无功能的同工型。因此,人和小鼠都具有可能起作用或可能不起作用的多个SAP剪接同工型。这些同工型的相对比例的调节可能是细胞可以调节SAP介导的生物活性的机制。

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