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COVID-19 and Vertical Transmission: Assessing the Expression of ACE2 / TMPRSS2 in the Human Fetus and Placenta to Assess the Risk of SARS-CoV-2 Infection

27 Pages Posted: 5 Jul 2021

See all articles by Max Arran Beesley

Max Arran Beesley

University College London

Joseph R. Davidson

University College London

Francesco Panariello

Telethon Institute of Genetics and Medicine (TIGEM) - Armenise/Harvard Laboratory of Integrative Genomics

Soichi Shibuya

University College London

Dominic Scaglioni

University College London

Brendan C. Jones

University College London

Katarzyna Maksym

University College London

Olumide Ogunbiyi

NIHR Great Ormond Street Biomedical Research Centre

Neil J. Sebire

University College London

Davide Cacchiarelli

Telethon Institute of Genetics and Medicine (TIGEM) - Armenise/Harvard Laboratory of Integrative Genomics

Anna L. David

University College London

Paolo De Coppi

University College London - Great Ormond Street Institute of Child Health; NIHR Great Ormond Street Biomedical Research Centre; Great Ormond Street Hospital for Children

Mattia Francesco Maria Gerli

University College London - Great Ormond Street Institute of Child Health; University College London - UCL Division of Surgery and Interventional Science

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Abstract

Background: While pregnant women have been identified as a potentially at-risk group concerning COVID-19 infection, little is known regarding the susceptibility of the fetus to infection. Co-expression of ACE2 and TMPRSS2 has been identified as a pre-requisite for infection, and expression across different tissues is known to vary between children and adults. However, the expression of these proteins in the fetus is unknown.

Methods: We performed a retrospective analysis of single cell data repositories. This data was then validated at both gene and protein level by performing qRT-PCR and two-colour immunohistochemistry on a library of second-trimester human fetal tissues.

Findings: TMPRSS2 is present at both gene and protein level in the predominantly epithelial fetal tissues analysed. ACE2 is present at significant levels, only in the fetal intestine and kidney and is not expressed in the fetal lung. The placenta is also negative for the two proteins both during development and at term.

Interpretation: This dataset indicates that the lungs are unlikely to be a viable route of SARS-CoV2 fetal infection. The fetal kidney, despite presenting both the proteins required for the infection, is anatomically protected from the exposure to the virus. However, the GI tract is likely to be susceptible to infection due to its high co-expression of both proteins, as well as its exposure to potentially infected amniotic fluid.

Funding Information: This work was made possible by an MRC / UKRI COVID-19 Rapid response initiative grant (MR/V028480/1).

Declaration of Interests: The authors declare no conflicts of interest related to this work or its developments. DC is founder, shareholder, and consultant of Next Generation Diagnostic SRL.

Ethics Approval Statement: Human fetal tissues were obtained with consent through the Human Developmental Biology Resource (HDBR; REC 18/LO/0822 – IRAS 244325; Project ID 2000478). Placental samples were obtained at delivery of an uncomplicated, full-term pregnancy (median 39 weeks PCW [Range 38+1 -39+4] for 6 patients recruited through the EVERREST Prospective Study as normal controls (National Research Ethics reference 13/LO/1254), NCT02097667 registered 31st October 2013[10].

Keywords: COVID-19, SARS-CoV2, ACE2, TMPRSS2, Vertical Transmission, Fetal Infection

Suggested Citation

Beesley, Max Arran and Davidson, Joseph R. and Panariello, Francesco and Shibuya, Soichi and Scaglioni, Dominic and Jones, Brendan C. and Maksym, Katarzyna and Ogunbiyi, Olumide and Sebire, Neil J. and Cacchiarelli, Davide and David, Anna L. and De Coppi, Paolo and Gerli, Mattia Francesco Maria, COVID-19 and Vertical Transmission: Assessing the Expression of ACE2 / TMPRSS2 in the Human Fetus and Placenta to Assess the Risk of SARS-CoV-2 Infection. Available at SSRN: https://ssrn.com/abstract=3880389 or http://dx.doi.org/10.2139/ssrn.3880389

Max Arran Beesley

University College London ( email )

Gower Street
London, WC1E 6BT
United Kingdom

Joseph R. Davidson

University College London ( email )

Gower Street
London, WC1E 6BT
United Kingdom

Francesco Panariello

Telethon Institute of Genetics and Medicine (TIGEM) - Armenise/Harvard Laboratory of Integrative Genomics ( email )

Soichi Shibuya

University College London ( email )

Gower Street
London, WC1E 6BT
United Kingdom

Dominic Scaglioni

University College London ( email )

Gower Street
London, WC1E 6BT
United Kingdom

Brendan C. Jones

University College London ( email )

Gower Street
London, WC1E 6BT
United Kingdom

Katarzyna Maksym

University College London ( email )

Gower Street
London, WC1E 6BT
United Kingdom

Olumide Ogunbiyi

NIHR Great Ormond Street Biomedical Research Centre ( email )

London
United Kingdom

Neil J. Sebire

University College London ( email )

Gower Street
London, WC1E 6BT
United Kingdom

Davide Cacchiarelli

Telethon Institute of Genetics and Medicine (TIGEM) - Armenise/Harvard Laboratory of Integrative Genomics ( email )

Anna L. David

University College London ( email )

Gower Street
London, WC1E 6BT
United Kingdom

Paolo De Coppi

University College London - Great Ormond Street Institute of Child Health ( email )

30 Guilford Street
London, England WC1N 1EH
United Kingdom

NIHR Great Ormond Street Biomedical Research Centre

London
United Kingdom

Great Ormond Street Hospital for Children

London
United Kingdom

Mattia Francesco Maria Gerli (Contact Author)

University College London - Great Ormond Street Institute of Child Health ( email )

30 Guilford Street
London, England WC1N 1EH
United Kingdom

University College London - UCL Division of Surgery and Interventional Science

London
United Kingdom