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重组人肺表面活性蛋白D和SP-D多聚体与甲型流感病毒的相互作用。

Interactions of recombinant human pulmonary surfactant protein D and SP-D multimers with influenza A.

作者信息

Hartshorn K, Chang D, Rust K, White M, Heuser J, Crouch E

机构信息

Department of Medicine, Boston University School of Medicine, Massachusetts 02118, USA.

出版信息

Am J Physiol. 1996 Nov;271(5 Pt 1):L753-62. doi: 10.1152/ajplung.1996.271.5.L753.

DOI:10.1152/ajplung.1996.271.5.L753
PMID:8944718
Abstract

To further study the structure and function of surfactant protein D (SP-D), recombinant human SP-D (rhSP-D) was isolated from the culture medium of Chinese hamster ovary (CHO)-K1 cells stably transfected with a full-length hSP-D cDNA. Although a significant fraction of the secreted rhSP-D was recovered as dodecamers similar to recombinant rat SP-D (rrSP-D), a major fraction accumulated as multimers of dodecamers indistinguishable from human proteinosis SP-D. As previously shown for the rat protein, rhSP-D agglutinated specific strains of influenza A virus (IAV), inhibited viral hemagglutinin activity, and protected neutrophils (PMN) from deactivation by IAV. However, the potency of rhSP-D multimers was severalfold greater than for purified dodecamers, comparable to natural, proteinosis hSP-D. Although rhSP-D multimers were also more potent than the serum collectins in mediating viral aggregation and protection of PMN, they were less potent than conglutinin in inhibiting infectivity in vitro. These studies establish that the propensity of hSP-D to form multimers of dodecamers is determined by its primary structure and demonstrate carbohydrate recognition domain valency-dependent interactions of SP-D with IAV.

摘要

为了进一步研究表面活性蛋白D(SP-D)的结构和功能,从稳定转染全长人SP-D cDNA的中国仓鼠卵巢(CHO)-K1细胞的培养基中分离出重组人SP-D(rhSP-D)。尽管分泌的rhSP-D中有很大一部分以类似于重组大鼠SP-D(rrSP-D)的十二聚体形式回收,但主要部分以与人类蛋白沉积症SP-D无法区分的十二聚体多聚体形式积累。如先前对大鼠蛋白的研究所示,rhSP-D凝集甲型流感病毒(IAV)的特定毒株,抑制病毒血凝素活性,并保护中性粒细胞(PMN)免受IAV的失活作用。然而,rhSP-D多聚体的效力比纯化的十二聚体高几倍,与天然的、蛋白沉积症的人SP-D相当。尽管rhSP-D多聚体在介导病毒聚集和保护PMN方面也比血清凝集素更有效,但在体外抑制感染性方面比凝聚素效力更低。这些研究表明,hSP-D形成十二聚体多聚体的倾向由其一级结构决定,并证明了SP-D与IAV的碳水化合物识别结构域价态依赖性相互作用。

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