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人类泛素结合酶基因UBE2L3的特征分析

Characterization of a human ubiquitin-conjugating enzyme gene UBE2L3.

作者信息

Moynihan T P, Ardley H C, Leek J P, Thompson J, Brindle N S, Markham A F, Robinson P A

机构信息

Molecular Medicine Unit, University of Leeds, Clinical Sciences Building, St. James's University Hospital, Leeds LS9 7TF, UK.

出版信息

Mamm Genome. 1996 Jul;7(7):520-5. doi: 10.1007/s003359900155.

Abstract

Ubiquitin-conjugating enzymes (E2s) are essential components of the post-translational protein ubiquitination pathway, mediating the transfer of activated ubiquitin to substrate proteins. We have identified a human gene, UBE2L3, localized on Chromosome (Chr) 22q11. 2-13.1, encoding an E2 almost identical to that encoded by the recently described human L-UBC (UBE2L1) gene present on Chr 14q24.3. Using chromosome-specific vectorette PCR, we have determined the intron/exon structure of UBE2L3. In contrast to the intronless UBE2L1 gene, the coding sequence of UBE2L3 is interrupted by three large introns. UBE2L3-derived mRNA appears to be the predominant species in most tissues rather than the transcript from UBE2L1 or another homologous gene UBE2L2, which maps to Chr 12q12. We also present additional evidence that these genes are members of a larger multigene family. The primary sequence of the protein encoded by UBE2L3 is identical to partial peptide sequence derived from the rabbit E2 'E2-F1,' suggesting that we have identified the human homolog of this protein. This latter E2 has been demonstrated to participate in transcription factor NF-kappaB maturation, c-fos degradation, and human papilloma virus-mediated p53 degradation in vitro.

摘要

泛素结合酶(E2s)是翻译后蛋白质泛素化途径的重要组成部分,介导活化的泛素转移至底物蛋白。我们鉴定出一个人类基因UBE2L3,定位于染色体(Chr)22q11.2 - 13.1,其编码的一种E2与位于Chr 14q24.3上最近描述的人类L-UBC(UBE2L1)基因所编码的E2几乎相同。利用染色体特异性载体PCR,我们确定了UBE2L3的内含子/外显子结构。与无内含子的UBE2L1基因不同,UBE2L3的编码序列被三个大的内含子打断。在大多数组织中,源自UBE2L3的mRNA似乎是主要类型,而非源自UBE2L1或另一个同源基因UBE2L2(定位于Chr 12q12)的转录本。我们还提供了额外证据,表明这些基因是一个更大的多基因家族的成员。UBE2L3编码的蛋白质的一级序列与源自兔E2“E2-F1”的部分肽序列相同,这表明我们鉴定出了该蛋白质的人类同源物。后者的E2已被证明在体外参与转录因子NF-κB成熟、c-fos降解以及人乳头瘤病毒介导的p53降解。

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