论文标题

SARS-COV-2进入基因在人类气道中最高表达的鼻腔和纤毛细胞

SARS-CoV-2 Entry Genes Are Most Highly Expressed in Nasal Goblet and Ciliated Cells within Human Airways

论文作者

Sungnak, Waradon, Huang, Ni, Bécavin, Christophe, Berg, Marijn, Network, HCA Lung Biological

论文摘要

SARS-COV-2冠状病毒是导致Covid-19冠状病毒病的病因学剂,是全球威胁。为了更好地理解病毒性朝向主义,我们评估了冠状病毒受体ACE2的RNA表达以及病毒蛋白蛋白启动蛋白酶蛋白酶TMPRSS2被认为控制了由人类细胞联合体产生的健康个体的单细胞RNA序列(SCRNA-SEQ)数据集中的病毒进入。我们发现ACE2以及蛋白酶TMPRSS2在呼吸道和肠道上皮细胞中差异表达。对呼吸树中上皮细胞的深入分析表明,鼻皮细胞,特别是杯状细胞/分泌细胞和纤毛细胞,显示了分析的所有上皮细胞的最高ACE2表达。病毒受体/入门相关蛋白朝上气道的偏斜表达可能与增强的传播率相关。最后,我们表明,与ACE2气道上皮表达相关的许多顶部基因都是先天免疫相关的抗病毒基因,高度富集在鼻上皮细胞中。这种与免疫途径的关联可能对感染和病毒病理学有临床意义,并突出了鼻皮妇在病毒感染中的特定意义。我们的发现强调了人类细胞图集作为参考数据集的可用性的重要性。在这种情况下,将数据汇编的分析指向鼻食和纤毛细胞作为早期病毒靶标和SARS-COV-2感染的潜在储层特别相关的作用。反过来,这是剖析病毒传播和制定预防和治疗临床策略的生物学框架。

The SARS-CoV-2 coronavirus, the etiologic agent responsible for COVID-19 coronavirus disease, is a global threat. To better understand viral tropism, we assessed the RNA expression of the coronavirus receptor, ACE2, as well as the viral S protein priming protease TMPRSS2 thought to govern viral entry in single-cell RNA-sequencing (scRNA-seq) datasets from healthy individuals generated by the Human Cell Atlas consortium. We found that ACE2, as well as the protease TMPRSS2, are differentially expressed in respiratory and gut epithelial cells. In-depth analysis of epithelial cells in the respiratory tree reveals that nasal epithelial cells, specifically goblet/secretory cells and ciliated cells, display the highest ACE2 expression of all the epithelial cells analyzed. The skewed expression of viral receptors/entry-associated proteins towards the upper airway may be correlated with enhanced transmissivity. Finally, we showed that many of the top genes associated with ACE2 airway epithelial expression are innate immune-associated, antiviral genes, highly enriched in the nasal epithelial cells. This association with immune pathways might have clinical implications for the course of infection and viral pathology, and highlights the specific significance of nasal epithelia in viral infection. Our findings underscore the importance of the availability of the Human Cell Atlas as a reference dataset. In this instance, analysis of the compendium of data points to a particularly relevant role for nasal goblet and ciliated cells as early viral targets and potential reservoirs of SARS-CoV-2 infection. This, in turn, serves as a biological framework for dissecting viral transmission and developing clinical strategies for prevention and therapy.

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