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首页> 外文期刊>The Biochemical Journal >Salivary agglutinin and lung scavenger receptor cysteine-rich glycoprotein 340 have broad anti-influenza activities and interactions with surfactant protein D that vary according to donor source and sialylation
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Salivary agglutinin and lung scavenger receptor cysteine-rich glycoprotein 340 have broad anti-influenza activities and interactions with surfactant protein D that vary according to donor source and sialylation

机译:唾液凝集素和肺清道夫受体富含半胱氨酸的糖蛋白340具有广泛的抗流感活性,并且与表面活性剂D的相互作用随供体来源和唾液酸化而变化。

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摘要

We previously found that scavenger receptor cysteine-rich gp-340 (glycoprotein-340), isolated from lung or saliva, directly inhibits human IAVs (influenza A viruses). We now show that salivary gp-340 has broad antiviral activity against human, equine and porcine IAV strains. Although lung and salivary gp-340 are identical in protein sequence, salivary gp-340 from one donor had significantly greater antiviral activity against avian-like IAV strains which preferentially bind sialic acids in alpha(2,3) linkage. A greater density of alpha(2,3)-linked sialic acids was present on the salivary gp-340 from this donor as compared with salivary gp-340 from another donor or several preparations of lung gp-340. Hence, the specificity of sialic acid linkages on gp-340 is an important determinant of anti-IAV activity. Gp-340 binds to SP-D (surfactant protein D), and we previously showed that lung gp-340 has cooperative interactions with SP-D in viral neutralization and aggregation assays. We now report that salivary gp-340 can, in some cases, strongly antagonize certain antiviral activities of SP-D. This effect was associated with greater binding of salivary gp-340 to the carbohydrate recognition domain of SP-D as compared with the binding of lung gp-340. These findings may relate to interindividual variations in innate defence against highly pathogenic IAV and to effects of aspiration of oral contents on SP-D-mediated lung functions.
机译:我们先前发现,从肺或唾液中分离出来的富含清除剂受体的半胱氨酸gp-340(糖蛋白-340)直接抑制人IAV(甲型流感病毒)。我们现在显示唾液gp-340对人,马和猪IAV株具有广泛的抗病毒活性。尽管肺和唾液gp-340的蛋白质序列相同,但是来自一个供体的唾液gp-340对禽类IAV株具有更大的抗病毒活性,该禽类IAV株优先结合唾液酸的alpha(2,3)键。与来自另一个供体或肺gp-340的几种制剂的唾液gp-340相比,来自该供体的唾液gp-340上存在更高密度的与α(2,3)连接的唾液酸。因此,gp-340上唾液酸键的特异性是抗IAV活性的重要决定因素。 Gp-340与SP-D(表面活性蛋白D)结合,并且我们先前显示,肺gp-340在病毒中和和聚集测定中与SP-D具有协同相互作用。我们现在报告唾液gp-340在某些情况下可以强烈拮抗SP-D的某些抗病毒活性。与肺gp-340的结合相比,该效果与唾液gp-340与SP-D的碳水化合物识别结构域的结合更大有关。这些发现可能与针对高致病性IAV的先天防御之间的个体差异以及吸入内含物对SP-D介导的肺功能的影响有关。

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