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棉铃虫褶翅小蜂杆状病毒抑制粉纹夜蛾血细胞的吞噬作用。

Microplitis demolitor bracovirus inhibits phagocytosis by hemocytes from Pseudoplusia includens.

作者信息

Strand Michael R, Beck Markus H, Lavine Mark D, Clark Kevin D

机构信息

Department of Entomology, University of Georgia, Athens, Georgia, USA.

出版信息

Arch Insect Biochem Physiol. 2006 Mar;61(3):134-45. doi: 10.1002/arch.20107.

Abstract

The braconid wasp Microplitis demolitor carries Microplitis demolitor bracovirus (MdBV) and parasitizes the larval stage of several noctuid moths. A key function of MdBV in parasitism is suppression of the host's cellular immune response. Prior studies in the host Pseudoplusia includens indicated that MdBV blocks encapsulation by preventing two types of hemocytes, plasmatocytes and granulocytes, from adhering to foreign targets. The other main immune response mediated by insect hemocytes is phagocytosis. The goal of this study was to determine which hemocyte types were phagocytic in P. includens and to assess whether MdBV infection affects this defense response. Using the bacterium Escherichia coli and inert polystyrene beads as targets, our results indicated that the professional phagocyte in P. includens is granulocytes. The phagocytic responses of granulocytes were very similar to those of High Five cells that prior studies have suggested are a granulocyte-like cell line. MdBV infection dose-dependently disrupted phagocytosis in both cell types by inhibiting adhesion of targets to the cell surface. The MdBV glc1.8 gene encodes a cell surface glycoprotein that had previously been implicated in disruption of adhesion and encapsulation responses by immune cells. Knockdown of glc1.8 expression by RNA interference (RNAi) during the current study rescued the ability of MdBV-infected High Five cells to phagocytize targets. Collectively, these results indicate that glc1.8 is a key virulence determinant in disruption of both adhesion and phagocytosis by insect immune cells.

摘要

茧蜂科黄蜂毁侧沟茧蜂携带毁侧沟茧蜂杆状病毒(MdBV),并寄生于几种夜蛾的幼虫阶段。MdBV在寄生过程中的一个关键功能是抑制宿主的细胞免疫反应。先前对宿主甘蓝夜蛾的研究表明,MdBV通过阻止两种血细胞,即浆血细胞和颗粒血细胞,黏附于外来目标来阻断包囊形成。昆虫血细胞介导的另一种主要免疫反应是吞噬作用。本研究的目的是确定甘蓝夜蛾中哪些血细胞类型具有吞噬作用,并评估MdBV感染是否会影响这种防御反应。以大肠杆菌和惰性聚苯乙烯珠作为目标,我们的结果表明,甘蓝夜蛾中的专职吞噬细胞是颗粒血细胞。颗粒血细胞的吞噬反应与先前研究表明的类似颗粒血细胞系的High Five细胞的吞噬反应非常相似。MdBV感染通过抑制目标与细胞表面的黏附,剂量依赖性地破坏了这两种细胞类型的吞噬作用。MdBV的glc1.8基因编码一种细胞表面糖蛋白,此前曾被认为与免疫细胞破坏黏附和包囊反应有关。在本研究中,通过RNA干扰(RNAi)敲低glc1.8的表达,挽救了MdBV感染的High Five细胞吞噬目标的能力。总体而言,这些结果表明,glc1.是昆虫免疫细胞破坏黏附和吞噬作用的关键毒力决定因素。

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