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热休克蛋白70-4(Hsc70-4):一种在……中双链RNA内化的意外介质 。 (原文句末不完整)

Hsc70-4: An unanticipated mediator of dsRNA internalization in .

作者信息

Fletcher Sabrina J, Bardossy Eugenia S, Tomé-Poderti Lorena, Moss Thomas, Mongelli Vanesa, Frangeul Lionel, Blanc Hervé, Verdier Yann, Vinh Joelle, Mukherjee Shaeri, Saleh Maria-Carla

机构信息

Viruses and RNAi Unit, Institut Pasteur, Université Paris Cité, CNRS UMR3569, F-75015 Paris, France.

Department of Microbiology and Immunology, The George William Hooper Foundation, University of California, San Francisco, San Francisco, CA 94143, USA.

出版信息

Sci Adv. 2025 May 16;11(20):eadv1286. doi: 10.1126/sciadv.adv1286.

Abstract

The small interfering RNA pathway is the primary antiviral defense mechanism in invertebrates and plants. This systemic mechanism relies on the recognition, transport, and internalization of double-stranded RNA (dsRNA). Our aim was to identify cell surface proteins that bind extracellular dsRNA and mediate its internalization in cells. We used coimmunoprecipitation coupled with proteomics analysis and found that silencing heat shock cognate protein 70-4 (Hsc70-4), a constitutively expressed heat shock protein, impairs dsRNA internalization. Unexpectedly, despite lacking a predicted transmembrane domain, Hsc70-4 localizes to the cell membrane via lipid interactions. Antibody blocking experiments revealed an extracellular domain on Hsc70-4 that is essential for dsRNA internalization. Intriguingly, this dsRNA-specific binding capacity of Hsc70-4 functions independently of its chaperone activity. These findings not only highlight Hsc70-4 as a previously uncharacterized and essential component in the dsRNA internalization process but also offer promising insights for advancing RNA interference-based technologies to combat pests and vector-borne diseases.

摘要

小干扰RNA途径是无脊椎动物和植物中的主要抗病毒防御机制。这种系统性机制依赖于双链RNA(dsRNA)的识别、运输和内化。我们的目标是鉴定结合细胞外dsRNA并介导其在细胞内内化的细胞表面蛋白。我们使用了免疫共沉淀结合蛋白质组学分析,发现沉默热休克同源蛋白70-4(Hsc70-4),一种组成性表达的热休克蛋白,会损害dsRNA的内化。出乎意料的是,尽管缺乏预测的跨膜结构域,Hsc70-4通过脂质相互作用定位于细胞膜。抗体阻断实验揭示了Hsc70-4上一个对dsRNA内化至关重要的细胞外结构域。有趣的是,Hsc70-4的这种dsRNA特异性结合能力独立于其伴侣活性发挥作用。这些发现不仅突出了Hsc70-4作为dsRNA内化过程中一个以前未被表征的重要组成部分,而且为推进基于RNA干扰的技术以对抗害虫和媒介传播疾病提供了有希望的见解。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c277/12083535/2335206b9d3c/sciadv.adv1286-f1.jpg

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