Stead Family Department of Pediatrics, Carver College of Medicine, The University of Iowa, Iowa City, Iowa, United States of America.
Department of Internal Medicine, Carver College of Medicine, The University of Iowa, Iowa City, Iowa, United States of America.
PLoS Pathog. 2021 Aug 12;17(8):e1009458. doi: 10.1371/journal.ppat.1009458. eCollection 2021 Aug.
Measles virus (MeV) is the most contagious human virus. Unlike most respiratory viruses, MeV does not directly infect epithelial cells upon entry in a new host. MeV traverses the epithelium within immune cells that carry it to lymphatic organs where amplification occurs. Infected immune cells then synchronously deliver large amounts of virus to the airways. However, our understanding of MeV replication in airway epithelia is limited. To model it, we use well-differentiated primary cultures of human airway epithelial cells (HAE) from lung donors. In HAE, MeV spreads directly cell-to-cell forming infectious centers that grow for ~3-5 days, are stable for a few days, and then disappear. Transepithelial electrical resistance remains intact during the entire course of HAE infection, thus we hypothesized that MeV infectious centers may dislodge while epithelial function is preserved. After documenting by confocal microscopy that infectious centers progressively detach from HAE, we recovered apical washes and separated cell-associated from cell-free virus by centrifugation. Virus titers were about 10 times higher in the cell-associated fraction than in the supernatant. In dislodged infectious centers, ciliary beating persisted, and apoptotic markers were not readily detected, suggesting that they retain functional metabolism. Cell-associated MeV infected primary human monocyte-derived macrophages, which models the first stage of infection in a new host. Single-cell RNA sequencing identified wound healing, cell growth, and cell differentiation as biological processes relevant for infectious center dislodging. 5-ethynyl-2'-deoxyuridine (EdU) staining located proliferating cells underneath infectious centers. Thus, cells located below infectious centers divide and differentiate to repair the dislodged infected epithelial patch. As an extension of these studies, we postulate that expulsion of infectious centers through coughing and sneezing could contribute to MeV's strikingly high reproductive number by allowing the virus to survive longer in the environment and by delivering a high infectious dose to the next host.
麻疹病毒(MeV)是最具传染性的人类病毒。与大多数呼吸道病毒不同,MeV 在进入新宿主时并不直接感染上皮细胞。MeV 通过携带它的免疫细胞穿过上皮细胞,然后在淋巴器官中扩增。受感染的免疫细胞随后同步将大量病毒输送到气道。然而,我们对 MeV 在气道上皮细胞中的复制的理解是有限的。为了模拟它,我们使用来自肺供体的分化良好的人呼吸道上皮细胞(HAE)原代培养物。在 HAE 中,MeV 直接在细胞间传播,形成感染中心,这些中心生长约 3-5 天,稳定几天,然后消失。上皮细胞跨上皮电阻在整个 HAE 感染过程中保持完整,因此我们假设 MeV 感染中心可能在保留上皮功能的情况下脱落。在用共聚焦显微镜记录感染中心逐渐从 HAE 上脱落之后,我们回收了顶端冲洗液,并通过离心将细胞相关和无细胞病毒分离。与上清液相比,细胞相关病毒滴度高约 10 倍。在脱落的感染中心中,纤毛跳动持续,并且不易检测到凋亡标志物,表明它们保留了功能代谢。细胞相关的 MeV 感染原代人单核细胞衍生的巨噬细胞,该细胞模拟了新宿主感染的第一阶段。单细胞 RNA 测序确定了伤口愈合、细胞生长和细胞分化是与感染中心脱落相关的生物学过程。5-乙炔基-2'-脱氧尿苷(EdU)染色定位在感染中心下方的增殖细胞。因此,位于感染中心下方的细胞分裂和分化以修复脱落的感染上皮斑块。作为这些研究的延伸,我们假设通过咳嗽和打喷嚏将感染中心排出可以使病毒在环境中存活更长时间,并向新宿主输送更高的传染性剂量,从而有助于 MeV 极高的繁殖数。
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