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首页> 外文期刊>American Journal of Physiology >Viral aggregating and opsonizing activity in collectin trimers
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Viral aggregating and opsonizing activity in collectin trimers

机译:收集修剪器中的病毒聚集和Opsonizing活动

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Collectins are collagenous lectins present in blood, respiratory lining fluid, and other mucosal secretions that play important roles in innate defense against infection. The collectin, surfactant protein D (SP-D), limits infection by viruses and bacteria in the respiratory tract, eye, and female genital tract. Multimeric SP-D has strong antiviral activity and is a potent viral and bacterial agglutinin and opsonin; however, trimers composed of the neck and carbohydrate recognition domain (hSP-D-NCRD) of SP-D lack these activities. We now show that, in contrast, a trimeric neck and CRD construct of bovine serum collectin CL-46 induces aggregation of influenza A virus (IAV) and potently increases IAV uptake by neutrophils. CL-46-NCRD showed calcium-dependent and sugar-sensitive binding to both neutrophils and IAV. Replacement of specific residues of the CRD of human SP-D with those found in bovine serum collectins conferred opsonizing activity. The most effective substitution involved replacement of arginine 343 with valine (hSP-D-NCRD/R343V). hSP-D-NCRD/R343V greatly increased viral uptake by neutrophils and monocytes and also potentiated neutrophil respiratory burst responses. These effects were further increased by cross-linking of hSP-D-NCRD/R343V trimers with MAbs directed against areas of the hSP-D-NCRD not involved in viral binding. Unlike the wild-type human SP-D hSP-D-NCRD, hSP-D-NCRD/R343V also induced viral aggregation. These results indicate that collectins can act as opsonins for IAV even in the absence of the collagen domain or higher order multimerization. This may involve increased affinity of individual CRDs for glycoconjugates displayed on host cells or the viral envelope.
机译:收集素是存在于血液,呼吸道衬里流体和其他粘膜分泌物中的胶凝胶,其在对抗感染先生防御中起重要作用。收集蛋白,表面活性剂蛋白D(SP-D),限制病毒和细菌在呼吸道,眼睛和女性生殖道中的感染。多聚体SP-D具有强烈的抗病毒活性,是一种有效的病毒和细菌凝集素和Opsonin;然而,由SP-D的颈部和碳水化合物识别结构域(HSP-D-NCRD)组成的三聚体缺乏这些活动。现在我们现在表明,相比之下,牛血清收集蛋白CL-46的三聚体颈部和CRD构建体诱导流感病毒(IAV)的聚集,并且效果增加了中性粒细胞的IAV吸收。 CL-46-NCRD显示出钙依赖性和糖敏感的含有嗜中性粒细胞和IAV的结合。用牛血清收集素发现的人替换人SP-D CRD的特定残留物。最有效的替代涉及用缬氨酸(HSP-D-NCRD / R343V)替代精氨酸343。 HSP-D-NCRD / R343V通过中性粒细胞和单核细胞大大增加了病毒吸收,并且还具有增强的中性粒细胞呼吸爆发反应。通过将HSP-D-NCRD / R343V三蛋白交联进一步增加了这些效果,所述MAb针对不参与病毒结合的HSP-D-NCRD区域。与野生型人SP-D HSP-D-NCRD不同,HSP-D-NCRD / R343V也诱导病毒聚集。这些结果表明,即使在没有胶原结构域或更高阶的多尺度的情况下,Collectins也可以作为IAV的opsonins。这可能涉及在宿主细胞或病毒包络上显示的糖缀合物的单个CRD的亲和力增加。

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