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Complement Regulation by Kaposis Sarcoma-Associated Herpesvirus ORF4 Protein

机译:卡波西氏肉瘤相关疱疹病毒ORF4蛋白的补体调节

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摘要

Kaposi's sarcoma-associated herpesvirus (KSHV) is associated with three types of human tumor: Kaposi's sarcoma, multicentric Castleman's disease, and primary effusion lymphoma. The virus encodes a number of proteins that participate in disrupting the immune response, one of which was predicted by sequence analysis to be encoded by open reading frame 4 (ORF4). The predicted ORF4 protein shares homology with cellular proteins referred to as regulators of complement activation. In the present study, the transcription profile of the ORF4 gene was characterized, revealing that it encodes at least three transcripts, by alternative splicing mechanisms, and three protein isoforms. Functional studies revealed that each ORF4 protein isoform inhibits complement and retains a C-terminal transmembrane domain. Consistent with the complement-regulating activity, we propose to name the proteins encoded by the ORF4 gene collectively as KSHV complement control protein (KCP). KSHV ORF4 is the most complex alternatively spliced gene encoding a viral complement regulator described to date. KCP inhibits the complement component of the innate immune response, thereby possibly contributing to the in vivo persistence and pathogenesis of this virus.
机译:卡波西氏肉瘤相关疱疹病毒(KSHV)与三种类型的人类肿瘤有关:卡波西氏肉瘤,多中心Castleman病和原发性积液性淋巴瘤。该病毒编码许多参与破坏免疫反应的蛋白质,其中一种蛋白质通过序列分析预测为开放阅读框4(ORF4)编码。预测的ORF4蛋白与称为补体激活调节剂的细胞蛋白具有同源性。在本研究中,对ORF4基因的转录谱进行了表征,揭示了它通过可变剪接机制和至少三种蛋白同工型编码至少三个转录本。功能研究表明,每种ORF4蛋白同工型均能抑制补体并保留C端跨膜结构域。与补体调节活性一致,我们建议将由ORF4基因编码的蛋白统称为KSHV补体控制蛋白(KCP)。迄今为止,KSHV ORF4是编码病毒补体调节剂的最复杂的可变剪接基因。 KCP抑制先天免疫应答的补体成分,从而可能有助于这种病毒的体内持久性和发病机理。

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