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来自毁灭褶翅小蜂杆状病毒的PTP-H2和PTP-H3定位于粘着斑,并且在昆虫免疫细胞中具有抗吞噬作用。

PTP-H2 and PTP-H3 from Microplitis demolitor Bracovirus localize to focal adhesions and are antiphagocytic in insect immune cells.

作者信息

Pruijssers Andrea J, Strand Michael R

机构信息

Department of Entomology and Center for Emerging and Tropical Diseases, University of Georgia, Athens, Georgia 30602, USA.

出版信息

J Virol. 2007 Feb;81(3):1209-19. doi: 10.1128/JVI.02189-06. Epub 2006 Nov 22.

Abstract

Viruses in the family Polydnaviridae are symbiotically associated with parasitoid wasps. Wasps inject polydnaviruses (PDVs) when laying an egg into their insect host, and expression of viral gene products causes several physiological alterations, including immunosuppression, that allow the wasp's progeny to develop. As with other PDVs, most Microplitis demolitor bracovirus (MdBV) genes are related variants that form gene families. The largest MdBV gene family includes 13 members that encode predicted proteins related to protein tyrosine phosphatases (PTPs). Sequence analysis during the present study indicated that five PTP family members (PTP-H2, -H3, -N1, and -N2) have fully conserved catalytic domains, whereas other family members exhibited replacements, deletions, or rearrangements of amino acids considered essential for tyrosine phosphatase activity. Expression studies indicated that most MdBV PTP genes are expressed in virus-infected host insects, with transcript abundance usually being highest in hemocytes. MdBV-infected hemocytes also exhibited higher levels of tyrosine phosphatase activity than noninfected hemocytes. We produced expression constructs for four of the most abundantly expressed PTP family members and conducted functional studies with hemocyte-like Drosophila S2 cells. These experiments suggested that recombinant PTP-H2 and PTP-H3 are functional tyrosine phosphatases whereas PTP-H1 and PTP-J1 are not. PTP-H2 and -H3 localized to focal adhesions in S2 cells, and coexpression with another MdBV gene product, Glc1.8, resulted in complete inhibition of phagocytosis.

摘要

多DNA病毒科的病毒与寄生蜂存在共生关系。寄生蜂在将卵产入昆虫宿主时会注入多DNA病毒(PDV),病毒基因产物的表达会引起多种生理变化,包括免疫抑制,从而使寄生蜂的后代得以发育。与其他PDV一样,大多数毁灭褶翅小蜂杆状病毒(MdBV)基因是形成基因家族的相关变体。最大的MdBV基因家族包括13个成员,它们编码与蛋白酪氨酸磷酸酶(PTP)相关的预测蛋白。本研究期间的序列分析表明,五个PTP家族成员(PTP-H2、-H3、-N1和-N2)具有完全保守的催化结构域,而其他家族成员则出现了被认为对酪氨酸磷酸酶活性至关重要的氨基酸替换、缺失或重排。表达研究表明,大多数MdBV PTP基因在病毒感染的宿主昆虫中表达,转录本丰度通常在血细胞中最高。感染MdBV的血细胞也比未感染的血细胞表现出更高水平的酪氨酸磷酸酶活性。我们构建了四个表达量最高的PTP家族成员的表达载体,并对类血细胞的果蝇S2细胞进行了功能研究。这些实验表明,重组PTP-H2和PTP-H3是有功能的酪氨酸磷酸酶,而PTP-H1和PTP-J1则不是。PTP-H2和-H3定位于S2细胞中的粘着斑,与另一种MdBV基因产物Glc1.8共表达会导致吞噬作用完全受到抑制。

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