Igenomix Foundation, INCLIVA Health Research Institute, Valencia, Spain.
Department of Obstetrics & Gynecology, Beth Israel Deaconess Medical Center, Harvard University, Boston, MA, USA.
Hum Reprod. 2021 Sep 18;36(10):2709-2719. doi: 10.1093/humrep/deab183.
Are SARS-CoV-2 canonical cell entry machinery, consisting of ACE2, TMPRSS2, NRP1 and LY6E, or alternative potential cell entry machinery, consisting of BSG, ANPEP, CD209, CLEC4G, TMPRSS4, TMPRSS11A, FURIN, CTSB, CTSL and IFITM1, expressed in the human endometrium across the menstrual cycle?
Analysis of cell entry factors for SARS-CoV-2 by single-cell RNA-sequencing (scRNAseq) in the preconceptional human endometrium reveals low risk of infection.
Gene expression datasets from bulk endometrial tissue show no significant expression of the SARS-CoV-2 receptor ACE2 and TMPRSS2. This is in contrast to reported expression of ACE2 at the single-cell level in the decidua and trophoblast cells at the maternal-fetal interface in early pregnancy, as well as vertical transmission of SARS-CoV-2 during pregnancy.
STUDY DESIGN, SIZE, DURATION: This analysis of SARS-CoV-2 cell entry machinery gene expression was conducted by scRNAseq in 73 181 human endometrial cells isolated from endometrial biopsies obtained from 27 donors across the menstrual cycle.
PARTICIPANTS/MATERIALS, SETTING, METHODS: ScRNAseq examined the expression of genes encoding cell entry machinery for SARS-CoV-2. The raw data were from a previously published dataset.
ScRNAseq analysis showed no significant expression of ACE2 in stromal or unciliated epithelial cells in any phase of the menstrual cycle. TMPRSS2 was expressed in epithelial cells during the early proliferative and mid-secretory phases. Interestingly, the expression of NRP1 was observed in both stromal and epithelial cells across all phases of the menstrual cycle, and LY6E was highly expressed in stromal cells. In the mid-secretory phase, coexpression of ACE2 and TMPRSS2 was detected in 0.07% of luminal epithelial cells. No cells simultaneously expressed ACE2, NRP1 and TMPRSS2 at the time of embryo implantation. Focusing on non-canonical cell entry machinery, BSG was highly expressed in all cell types across the menstrual cycle and may interact with CTSB or CTSL proteases, but viral infection using this machinery has not yet been confirmed.
All raw data in this study can be found at NCBI's Gene Expression Omnibus (series accession code GSE111976) and Sequence Read Archive (accession code SRP135922).
LIMITATIONS, REASONS FOR CAUTION: Our findings at the single-cell level imply low efficiency of SARS-CoV-2 endometrial infection using canonical receptors in a cohort of healthy reproductive-age women; however, infection of endometrial cells can only be assessed in the presence of the virus. All samples were processed for scRNAseq, so no samples are remaining to analyze protein expression or spatial transcriptomics.
Our results offer a useful resource to guide reproductive decisions when assessing risk of endometrial infection by SARS-CoV-2 during the preconceptional period in asymptomatic COVID-19 carriers.
STUDY FUNDING/COMPETING INTEREST(S): This study was jointly supported by the March of Dimes, Chan Zuckerberg Biohub and MINECO/FEDER (SAF-2015-67164-R, to C.S.) (Spanish Government), and the European Union's Horizon 2020 Framework Programme for Research and Innovation (Grant agreement 874867). W.W. was supported by the Stanford Bio-X Graduate Bowes Fellowship and Chan Zuckerberg Biohub. F.V. was supported by the Miguel Servet Program Type II of ISCIII (CPII18/00020) and the FIS project (PI18/00957). A patent disclosure has been filed for the study with the title 'Methods for assessing endometrial transformation' and the global patent number 'EP 3807648 A2' under the inventors S.R.Q., C.S., W.W. and F.V. C.S. is the Founder and Head of the Scientific Advisory Board of Igenomix SL. S.R.Q is the Director of Mirvie. I.M. is partially employed by Igenomix SL. B.R. has no interests to declare.
在受孕前的人类子宫内膜中,SARS-CoV-2 的经典细胞进入机制(包括 ACE2、TMPRSS2、NRP1 和 LY6E)或替代潜在的细胞进入机制(包括 BSG、ANPEP、CD209、CLEC4G、TMPRSS4、TMPRSS11A、FURIN、CTSB、CTSL 和 IFITM1)是否表达?
通过对受孕前人类子宫内膜进行单细胞 RNA 测序(scRNAseq)分析 SARS-CoV-2 的细胞进入因子,揭示了低感染风险。
来自大块子宫内膜组织的基因表达数据集显示 SARS-CoV-2 受体 ACE2 和 TMPRSS2 没有明显表达。这与在妊娠早期母体-胎儿界面的蜕膜和滋养层细胞中报道的 ACE2 在单细胞水平上的表达以及妊娠期间 SARS-CoV-2 的垂直传播形成对比。
研究设计、大小和持续时间:这项关于 SARS-CoV-2 细胞进入机制基因表达的分析通过 scRNAseq 在 27 名供体整个月经周期中从子宫内膜活检中分离的 73181 个人类子宫内膜细胞中进行。
参与者/材料、设置、方法:scRNAseq 检查了编码 SARS-CoV-2 细胞进入机制的基因表达。原始数据来自先前发表的数据集。
scRNAseq 分析显示,在月经周期的任何阶段,基质或无纤毛上皮细胞中均无 ACE2 的显著表达。TMPRSS2 在早期增殖期和中期分泌期表达于上皮细胞。有趣的是,NRP1 的表达在整个月经周期的基质和上皮细胞中均有观察到,LY6E 在基质细胞中高度表达。在中期分泌期,腔上皮细胞中同时表达 ACE2 和 TMPRSS2 的比例为 0.07%。在胚胎植入时,没有细胞同时表达 ACE2、NRP1 和 TMPRSS2。关注非经典细胞进入机制,BSG 在整个月经周期的所有细胞类型中均高度表达,可能与 CTSB 或 CTSL 蛋白酶相互作用,但尚未证实使用该机制的病毒感染。
本研究的所有原始数据均可在 NCBI 的基因表达综合数据库(系列注册号 GSE111976)和序列读取档案(访问号 SRP135922)中找到。
局限性、谨慎的原因:我们在单细胞水平上的发现表明,在一组健康的生殖年龄女性中,使用经典受体,SARS-CoV-2 子宫内膜感染的效率较低;然而,只有在存在病毒的情况下才能评估子宫内膜细胞的感染。所有样本均被处理用于 scRNAseq,因此没有剩余样本可用于分析蛋白质表达或空间转录组学。
我们的研究结果为评估无症状 COVID-19 携带者受孕前期间 SARS-CoV-2 子宫内膜感染的风险提供了有用的资源。
研究资金/利益冲突:这项研究由 March of Dimes、Chan Zuckerberg Biohub 和 MINECO/FEDER(西班牙政府)联合资助,并得到了欧盟地平线 2020 研究与创新计划的支持(授予协议 874867)。WW 得到了斯坦福生物-X 研究生鲍尔斯奖学金和 Chan Zuckerberg Biohub 的支持。FV 得到了 ISCIII 的 Miguel Servet 计划第二型(CPII18/00020)和 FIS 项目(PI18/00957)的支持。一项名为“评估子宫内膜转化的方法”的专利已由 S.R.Q.、C.S.、WW 和 F.V. 的发明者提交全球专利号“EP 3807648 A2”。C.S. 是 Igenomix SL 的创始人和科学顾问委员会主席。S.R.Q. 是 Mirvie 的董事。I.M. 部分受雇于 Igenomix SL。BR. 没有利益冲突。
