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免疫球蛋白超家族的一个新成员和一个V-ATP酶G亚基是人类主要组织相容性复合体中靠近肿瘤坏死因子基因座的新基因预测产物。

A new member of the Ig superfamily and a V-ATPase G subunit are among the predicted products of novel genes close to the TNF locus in the human MHC.

作者信息

Neville M J, Campbell R D

机构信息

Medical Research Council Immunochemistry Unit, Department of Biochemistry, University of Oxford, United Kingdom.

出版信息

J Immunol. 1999 Apr 15;162(8):4745-54.

Abstract

It is becoming increasingly apparent that many of the genes in the class III region of the human MHC encode proteins involved in the immune and inflammatory responses. Furthermore, genetic studies have indicated that genes within the class III region, particularly the telomeric segment containing the TNF gene, could contribute to susceptibility to diseases of immune-related etiology. We have sequenced an 82-kb segment of DNA around the TNF gene to identify candidate disease susceptibility genes in this region. The 10 known genes in this region have been precisely positioned with the order allograft inflammatory factor 1, G1, 1C7, leukocyte-specific transcript 1 (B144), lymphotoxin B, TNF, lymphotoxin A, NB6, IKBL, BAT1 (centromere to telomere), and their genomic structures have been defined. Comparison of the G1 genomic region with previously described cDNA and genomic sequences, together with the results of reverse transcriptase-PCR, indicates that three alternative transcripts, G1, allograft inflammatory factor 1, and IFN-gamma-responsive transcript, are all derived from this gene. The completion of the sequence of 1C7 (D6S2570) has revealed that this gene encodes a putative novel member of the Ig superfamily. A number of alternatively spliced transcripts of 1C7 were identified by reverse transcriptase-PCR, all of which are expressed in immune-related cell lines. Alternative splicing within the Ig domain-encoding region was seen to result in possible set switching between an IgV domain and an IgC2 domain. Lastly, a previously unidentified gene, homologous to a number of V-ATPase G subunits, has been located 1 kb telomeric of IKBL.

摘要

越来越明显的是,人类主要组织相容性复合体(MHC)Ⅲ类区域中的许多基因编码参与免疫和炎症反应的蛋白质。此外,遗传学研究表明,Ⅲ类区域内的基因,特别是包含肿瘤坏死因子(TNF)基因的端粒片段,可能与免疫相关病因的疾病易感性有关。我们对TNF基因周围一段82 kb的DNA片段进行了测序,以确定该区域中候选的疾病易感基因。该区域中的10个已知基因已被精确定位,顺序为同种异体移植炎症因子1、G1、1C7、白细胞特异性转录本1(B144)、淋巴毒素B、TNF、淋巴毒素A、NB6、IKBL、BAT1(从着丝粒到端粒),并且它们的基因组结构已被确定。将G1基因组区域与先前描述的cDNA和基因组序列进行比较,以及逆转录酶 - PCR的结果表明,三种可变转录本G1、同种异体移植炎症因子1和干扰素 - γ反应性转录本均源自该基因。1C7(D6S2570)序列的完成揭示该基因编码免疫球蛋白超家族的一个假定新成员。通过逆转录酶 - PCR鉴定出1C7的许多可变剪接转录本,所有这些转录本均在免疫相关细胞系中表达。在免疫球蛋白结构域编码区域内的可变剪接导致免疫球蛋白V结构域和免疫球蛋白C2结构域之间可能的类别转换。最后,一个与多个V - ATP酶G亚基同源的先前未鉴定的基因已定位在IKBL端粒1 kb处。

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