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小鼠淋巴毒素β基因的克隆与表达分析

Cloning and expression analysis of the murine lymphotoxin beta gene.

作者信息

Pokholok D K, Maroulakou I G, Kuprash D V, Alimzhanov M B, Kozlov S V, Novobrantseva T I, Turetskaya R L, Green J E, Nedospasov S A

机构信息

Biological Carcinogenesis and Development Program, Program Resources, Inc./DynCorp. Frederick, MD 21702-1201.

出版信息

Proc Natl Acad Sci U S A. 1995 Jan 31;92(3):674-8. doi: 10.1073/pnas.92.3.674.

Abstract

Tumor necrosis factor alpha (TNF-alpha) and soluble lymphotoxin (LT) (also called LT-alpha or TNF-beta) are cytokines with similar biological activities that are encoded by related and closely linked genes. TNF-alpha, a mediator of the inflammatory response, exists in soluble and transmembrane forms. LT-alpha can be secreted or retained at the cell surface by binding to a 33-kDa transmembrane subunit, LT-beta. The recently cloned human LT-beta gene encodes another TNF family member and is linked to the TNF/LT locus within the major histocompatibility complex locus. The cell surface LT is a heterotrimer consisting of LT-alpha and LT-beta, whose physiological function is not yet clearly defined. We now report the sequence analysis of the genomic region and cDNA of murine LT-beta gene, which is closely associated with the TNF-alpha and LT-alpha genes within the murine major histocompatibility complex locus. Unlike the TNF-alpha, LT-alpha, and human LT-beta genes, which contain four exons, the murine LT-beta contains three exons and encodes a 244-amino acid polypeptide with a 66-amino acid insert that is absent from the human homologue. In situ hybridization demonstrates constitutive expression of LT-beta in lymphoid and hematopoietic tissues. LT-beta transcription is maximal in the thymic medulla and in splenic white pulp. LT-beta mRNA is also detected in the skin and in specific regions of the brain. The LT-beta promoter region contains putative Ets-binding sites, suggesting that the expression of LT-beta may be regulated in part by Ets transcription factors whose pattern of lymphoid expression overlaps that of LT-beta.

摘要

肿瘤坏死因子α(TNF-α)和可溶性淋巴毒素(LT)(也称为LT-α或TNF-β)是具有相似生物学活性的细胞因子,它们由相关且紧密连锁的基因编码。TNF-α是炎症反应的介质,以可溶性和跨膜形式存在。LT-α可以通过与一个33 kDa的跨膜亚基LT-β结合而分泌或保留在细胞表面。最近克隆的人LT-β基因编码另一个TNF家族成员,并与主要组织相容性复合体基因座内的TNF/LT基因座相连。细胞表面的LT是由LT-α和LT-β组成的异源三聚体,其生理功能尚未明确界定。我们现在报告小鼠LT-β基因的基因组区域和cDNA的序列分析,该基因与小鼠主要组织相容性复合体基因座内的TNF-α和LT-α基因密切相关。与包含四个外显子的TNF-α、LT-α和人LT-β基因不同,小鼠LT-β包含三个外显子,编码一个244个氨基酸的多肽,其中有一个66个氨基酸的插入片段,而人同源物中没有该片段。原位杂交显示LT-β在淋巴和造血组织中组成性表达。LT-β转录在胸腺髓质和脾白髓中最高。在皮肤和大脑的特定区域也检测到LT-β mRNA。LT-β启动子区域包含假定的Ets结合位点,表明LT-β的表达可能部分受Ets转录因子调节,其淋巴样表达模式与LT-β的表达模式重叠。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6a1d/42682/fda85d10ed27/pnas01481-0037-a.jpg

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