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外源性热休克蛋白70与巨噬细胞脂筏微区结合,并刺激抗原的吞噬、加工和MHC-II呈递。

Exogenous heat shock protein 70 binds macrophage lipid raft microdomain and stimulates phagocytosis, processing, and MHC-II presentation of antigens.

作者信息

Wang Ruibo, Kovalchin Joseph T, Muhlenkamp Peggy, Chandawarkar Rajiv Y

机构信息

Division of Plastic Surgery, University of Connecticut Health Center MC 1601, 263 Farmington Ave, Farmington CT 06030-1601, USA.

出版信息

Blood. 2006 Feb 15;107(4):1636-42. doi: 10.1182/blood-2005-06-2559. Epub 2005 Nov 1.

Abstract

The extracellular presence of endotoxin-free heat shock protein 70 (HSP70) enhances the rate and capacity of macrophage-mediated phagocytosis at 6 times the basal rate. It is protein-specific, dose- and time-dependent and involves the internalization of inert microspheres, Gram-positive and -negative bacteria and fungi. Structurally, exogenous HSP70 binds the macrophage plasma membrane, specifically on its lipid raft-microdomain. Disruption of lipid rafts, HSP70-LR interaction, or denaturing HSP70 abrogates the HSP-mediated increase in phagocytosis. Further, HSP70-mediated phagocytosis directly enhances the processing and presentation of internalized antigens via the endocytic MHC class-II pathway to CD4+ T lymphocytes. Modulating the HSP70-LR interaction presents an opportunity to intervene at the level of host-pathogen interface: a therapeutic tool for emerging infections, especially when conventional treatment with antibiotics is ineffective (antibiotic resistance) or unavailable (rapidly spreading, endemic). These results identify a new role for HSP70, a highly conserved molecule in stimulating phagocytosis: a primordial macrophage function, thereby influencing both innate and adaptive immune responses.

摘要

无内毒素热休克蛋白70(HSP70)在细胞外的存在使巨噬细胞介导的吞噬作用速率和能力提高至基础速率的6倍。这具有蛋白质特异性、剂量和时间依赖性,且涉及惰性微球、革兰氏阳性和阴性细菌以及真菌的内化。在结构上,外源性HSP70与巨噬细胞质膜结合,特别是在其脂筏微结构域上。破坏脂筏、HSP70与脂筏的相互作用或使HSP70变性可消除HSP介导的吞噬作用增强。此外,HSP70介导的吞噬作用通过内吞性MHC II类途径直接增强内化抗原向CD4 + T淋巴细胞的加工和呈递。调节HSP70与脂筏的相互作用为在宿主-病原体界面水平进行干预提供了一个机会:这是一种针对新发感染的治疗工具,尤其是在常规抗生素治疗无效(抗生素耐药)或无法使用(快速传播的地方流行病)时。这些结果确定了HSP70在刺激吞噬作用中的新作用:一种原始的巨噬细胞功能,从而影响先天性和适应性免疫反应。

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