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Porcine, murine and human sialoadhesin (Sn/Siglec-1/CD169): portals for porcine reproductive and respiratory syndrome virus entry into target cells

机译:猪,鼠和人唾液酸粘附素(sn / siglec-1 / CD169):猪生殖和呼吸综合征病毒进入靶细胞的门户

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摘要

Porcine sialoadhesin (pSn; a sialic acid-binding lectin) and porcine CD163 (pCD163) are molecules that facilitate infectious entry of porcine reproductive and respiratory syndrome virus (PRRSV) into alveolar macrophages. In this study, it was shown that murine Sn (mSn) and human Sn (hSn), like pSn, can promote PRRSV infection of pCD163-expressing cells. Intact sialic acid-binding domains are crucial, since non-sialic acid-binding mutants of pSn, mSn and hSn did not promote infection. Endodomain-deletion mutants of pSn, mSn and hSn promoted PRRSV infection less efficiently, but also showed markedly reduced expression levels, making further research into the potential role of the Sn endodomain in PRRSV receptor activity necessary. These data further complement our knowledge on Sn as an important PRRSV receptor, and suggest - in combination with other published data - that species differences in the main PRRSV entry mediators Sn and CD163 do not account for the strict host species specificity displayed by the virus.
机译:猪唾液酸粘附素(pSn;唾液酸结合凝集素)和猪CD163(pCD163)是促进猪生殖和呼吸综合症病毒(PRRSV)感染性进入肺泡巨噬细胞的分子。在这项研究中,已显示鼠Sn(mSn)和人Sn(hSn)像pSn一样,可以促进PRCDV感染表达pCD163的细胞。完整的唾液酸结合域至关重要,因为pSn,mSn和hSn的非唾液酸结合突变体不会促进感染。 pSn,mSn和hSn的内切域缺失突变体不太有效地促进PRRSV感染,但也显示出明显降低的表达水平,因此有必要进一步研究Sn内切域在PRRSV受体活性中的潜在作用。这些数据进一步补充了我们对Sn作为重要的PRRSV受体的认识,并与其他已发表的数据一起表明,主要PRRSV进入介体Sn和CD163中的物种差异不能解释该病毒显示的严格宿主物种特异性。

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