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表面活性蛋白A和D的抗流感活性机制:与血清凝集素的比较

Mechanisms of anti-influenza activity of surfactant proteins A and D: comparison with serum collectins.

作者信息

Hartshorn K L, White M R, Shepherd V, Reid K, Jensenius J C, Crouch E C

机构信息

Department of Medicine, Boston University School of Medicine, Massachusetts, USA.

出版信息

Am J Physiol. 1997 Dec;273(6):L1156-66. doi: 10.1152/ajplung.1997.273.6.L1156.

Abstract

The present study provides the first direct comparison of anti-influenza A virus (IAV) activities of the collectins surfactant protein (SP) A and SP-D, mannose-binding lectin (MBL), and conglutinin. SP-D, MBL, and conglutinin inhibited IAV hemagglutination activity with a greater potency than and by a distinct mechanism from SP-A. Although isolated trimeric SP-D carbohydrate recognition domains inhibited hemagglutination activity, preparations of SP-D also containing the collagen domain and NH2 terminus caused greater inhibition. In contrast to SP-A (or nonmultimerized SP-D), absence of the N-linked attachment did not effect interactions of multimerized SP-D with IAV. SP-D, SP-A, and conglutinin caused viral precipitation through formation of massive viral aggregates, whereas MBL formed aggregates of smaller size that did not precipitate. All of the collectins enhanced IAV binding to neutrophils; however, in the case of MBL, this effect was modest compared with the binding enhancement induced by SP-D or conglutinin. These studies clarify the structural requirements for viral inhibition by SP-D and reveal significant differences in the mechanisms of anti-IAV activity among the collectins.

摘要

本研究首次对凝集素表面活性蛋白(SP)A、SP-D、甘露糖结合凝集素(MBL)和胶固素的抗甲型流感病毒(IAV)活性进行了直接比较。SP-D、MBL和胶固素抑制IAV血凝活性的效力高于SP-A,且作用机制不同。虽然分离的三聚体SP-D糖识别结构域可抑制血凝活性,但含有胶原结构域和NH2末端的SP-D制剂抑制作用更强。与SP-A(或非多聚化的SP-D)不同,N-连接附着的缺失并不影响多聚化SP-D与IAV的相互作用。SP-D、SP-A和胶固素通过形成大量病毒聚集体导致病毒沉淀,而MBL形成的聚集体较小,不会沉淀。所有凝集素均增强IAV与中性粒细胞的结合;然而,就MBL而言,与SP-D或胶固素诱导的结合增强相比,这种作用较小。这些研究阐明了SP-D抑制病毒的结构要求,并揭示了凝集素之间抗IAV活性机制的显著差异。

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