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Mta表达需要一种出乎意料不稳定的线粒体编码蛋白。

An unexpectedly labile mitochondrially encoded protein is required for Mta expression.

作者信息

Han A C, Rodgers J R, Rich R R

机构信息

Howard Hughes Medical Institute Laboratory, Baylor College of Medicine, Houston, TX 77030.

出版信息

Immunogenetics. 1989;29(4):258-64. doi: 10.1007/BF00717910.

Abstract

Maternally transmitted antigen (Mta) is a mouse major histocompatibility antigen recognized by cytotoxic T lymphocytes. A role for mitochondria in expression of this class I-like cell surface antigen has been previously established. We now show that a labile product of mitochondrial protein synthesis is required for Mta expression. Reexpression of Mta determinants after enzymatic removal occurred within 24 h, and the regeneration process was sensitive to chloramphenicol (CAP), a selective inhibitor of mitochondrial protein synthesis. Additionally, target cells treated with CAP for as little as 18 h showed diminished expression of Mta. The estimated half-life for Mtf products ranged from 6 to 15 h, less than the half-lives of known mitochondrial translation products. This suggests that the Mtf product is not generated by the normal turnover of stable mitochondrial respiratory proteins. Instead, these results indicate the existence of either labile unknown mitochondrially encoded peptides or a rapid turnover pathway for known mitochondrial products.

摘要

母系传播抗原(Mta)是一种可被细胞毒性T淋巴细胞识别的小鼠主要组织相容性抗原。线粒体在这类I类细胞表面抗原的表达中所起的作用此前已得到证实。我们现在表明,Mta表达需要线粒体蛋白质合成的一种不稳定产物。酶解去除后,Mta决定簇在24小时内重新表达,并且再生过程对氯霉素(CAP)敏感,氯霉素是线粒体蛋白质合成的选择性抑制剂。此外,用CAP处理仅18小时的靶细胞显示Mta表达减少。Mtf产物的估计半衰期为6至15小时,短于已知线粒体翻译产物的半衰期。这表明Mtf产物不是由稳定的线粒体呼吸蛋白的正常周转产生的。相反,这些结果表明存在不稳定的未知线粒体编码肽或已知线粒体产物的快速周转途径。

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