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通过非典型翻译起始产生的卡波西肉瘤相关疱疹病毒潜伏相关核抗原 1 的复杂替代细胞质蛋白异构体。

Complex alternative cytoplasmic protein isoforms of the Kaposi's sarcoma-associated herpesvirus latency-associated nuclear antigen 1 generated through noncanonical translation initiation.

机构信息

Cancer Virology Program, University of Pittsburgh, Pittsburgh, Pennsylvania, USA.

出版信息

J Virol. 2013 Mar;87(5):2744-55. doi: 10.1128/JVI.03061-12. Epub 2012 Dec 19.

Abstract

Kaposi's sarcoma-associated herpesvirus (KSHV) latency associated-nuclear antigen 1 (LANA1) protein is constitutively expressed in all KSHV-infected cells, as well as in all forms of KSHV-associated malignancies. LANA1 is a multifunctional KSHV oncoprotein containing multiple repeat sequences that is important for viral episome maintenance and the regulation of cellular and viral gene expression. We characterize here multiple LANA1 isoforms and show that ∼50% of LANA1 is naturally generated as N-terminally truncated shoulder proteins that are detected on SDS-PAGE as faster-migrating shoulder bands designated LANA1(S). Higher-molecular-weight LANA1(S) isoforms initiate downstream at noncanonical sites within the N-terminal region, whereas lower-molecular-weight LANA1(S) isoforms initiate downstream within the central repeat 1 domain. LANA1(S) proteins lack an N-terminal nuclear localization signal motif, and some isoforms differ from full-length, canonical LANA1 by localizing to perinuclear and cytoplasmic sites. Although LANA1 has until now been assumed to be solely active in the nucleus, this finding indicates that this major KSHV oncoprotein may have cytoplasmic activities as well. KSHV overcomes its limited genetic coding capacity by generating alternatively initiated protein isoforms that may have distinct biological functions.

摘要

卡波西肉瘤相关疱疹病毒(KSHV)潜伏相关核抗原 1(LANA1)蛋白在所有 KSHV 感染的细胞中以及所有形式的 KSHV 相关恶性肿瘤中持续表达。LANA1 是一种多功能的 KSHV 癌蛋白,含有多个重复序列,对病毒外显子的维持以及细胞和病毒基因表达的调节都很重要。我们在这里对多个 LANA1 亚型进行了表征,并表明约 50%的 LANA1 是天然产生的 N 端截短的肩蛋白,在 SDS-PAGE 上作为更快迁移的肩带被检测到,称为 LANA1(S)。较高分子量的 LANA1(S)亚型在 N 端区域的非典型位点起始下游,而较低分子量的 LANA1(S)亚型在中央重复 1 结构域内起始下游。LANA1(S)蛋白缺乏 N 端核定位信号基序,一些亚型与全长、典型的 LANA1 不同,定位于核周和细胞质部位。尽管 LANA1 迄今为止一直被认为仅在核内具有活性,但这一发现表明这种主要的 KSHV 癌蛋白也可能具有细胞质活性。KSHV 通过产生具有不同生物学功能的替代起始蛋白亚型来克服其有限的遗传编码能力。

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