Preferential uptake of SARS-CoV-2 by pericytes potentiates vascular damage and permeability in an organoid model of the microvasculature

Abdullah Khan; Jasmeet Reyat; Harriet Hill; Joshua Bourne; Martina Colicchia; Maddy L Newby; Joel D Allen; Max Crispin; Esther Youd; Paul Murray; Graham Taylor; Zania Stamataki; Alex Richter; Adam Cunningham; Matthew Pugh; Julie Rayes

doi:10.1093/cvr/cvac097

Preferential uptake of SARS-CoV-2 by pericytes potentiates vascular damage and permeability in an organoid model of the microvasculature

Abdullah Khan, Jasmeet Reyat, Harriet Hill, Joshua Bourne, Martina Colicchia, Maddy L Newby, Joel D Allen, Max Crispin, Esther Youd, Paul Murray, Graham Taylor, Zania Stamataki, Alex Richter, Adam Cunningham, Matthew Pugh, Julie Rayes

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Abstract

Aims: Thrombotic complications and vasculopathy have been extensively associated with severe COVID-19 infection; however, the mechanisms inducing endotheliitis and the disruption of endothelial integrity in the microcirculation are poorly understood. We hypothesized that within the vessel wall, pericytes preferentially take up viral particles and mediate the subsequent loss of vascular integrity.

Methods and results: Immunofluorescence of post-mortem patient sections was used to assess pathophysiological aspects of COVID-19 infection. The effects of COVID-19 on the microvasculature were assessed using a vascular organoid model exposed to live viral particles or recombinant viral antigens. We find increased expression of the viral entry receptor angiotensin-converting enzyme 2 on pericytes when compared to vascular endothelium and a reduction in the expression of the junctional protein CD144, as well as increased cell death, upon treatment with both live virus and/or viral antigens. We observe a dysregulation of genes implicated in vascular permeability, including Notch receptor 3, angiopoietin-2, and TEK. Activation of vascular organoids with interleukin-1β did not have an additive effect on vascular permeability. Spike antigen was detected in some patients’ lung pericytes, which was associated with a decrease in CD144 expression and increased platelet recruitment and von Willebrand factor (VWF) deposition in the capillaries of these patients, with thrombi in large vessels rich in VWF and fibrin.

Conclusion: Together, our data indicate that direct viral exposure to the microvasculature modelled by organoid infection and viral antigen treatment results in pericyte infection, detachment, damage, and cell death, disrupting pericyte-endothelial cell crosstalk and increasing microvascular endothelial permeability, which can promote thrombotic and bleeding complications in the microcirculation.

Original language	English
Article number	cvac097
Pages (from-to)	1-12
Number of pages	12
Journal	Cardiovascular Research
DOIs	https://doi.org/10.1093/cvr/cvac097
Publication status	Published - 16 Jun 2022

Bibliographical note

Final Version of Record not yet available as of 26/08/2022

© The Author(s) 2022. Published by Oxford University Press on behalf of European Society of Cardiology.

Keywords

SARS-CoV-2
COVID-19
Endothelial permeability
Thrombosis
Organoids
Vasculopathy

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10.1093/cvr/cvac097Licence: Creative Commons: Attribution (CC BY)

Khan2022_Preferential_uptake_of_SARS-CoV-2Final published version, 1.98 MBLicence: Creative Commons: Attribution (CC BY)

Engineering a novel human bone marrow organoid to target myelofibrosis
Khan, A.
THE WELLCOME TRUST
1/05/20 → 30/04/24
Project: Research

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Khan, A., Reyat, J., Hill, H., Bourne, J., Colicchia, M., Newby, M. L., Allen, J. D., Crispin, M., Youd, E., Murray, P., Taylor, G., Stamataki, Z., Richter, A., Cunningham, A., Pugh, M., & Rayes, J. (2022). Preferential uptake of SARS-CoV-2 by pericytes potentiates vascular damage and permeability in an organoid model of the microvasculature. Cardiovascular Research, 1-12. Article cvac097. https://doi.org/10.1093/cvr/cvac097

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title = "Preferential uptake of SARS-CoV-2 by pericytes potentiates vascular damage and permeability in an organoid model of the microvasculature",

abstract = "Aims: Thrombotic complications and vasculopathy have been extensively associated with severe COVID-19 infection; however, the mechanisms inducing endotheliitis and the disruption of endothelial integrity in the microcirculation are poorly understood. We hypothesized that within the vessel wall, pericytes preferentially take up viral particles and mediate the subsequent loss of vascular integrity.Methods and results: Immunofluorescence of post-mortem patient sections was used to assess pathophysiological aspects of COVID-19 infection. The effects of COVID-19 on the microvasculature were assessed using a vascular organoid model exposed to live viral particles or recombinant viral antigens. We find increased expression of the viral entry receptor angiotensin-converting enzyme 2 on pericytes when compared to vascular endothelium and a reduction in the expression of the junctional protein CD144, as well as increased cell death, upon treatment with both live virus and/or viral antigens. We observe a dysregulation of genes implicated in vascular permeability, including Notch receptor 3, angiopoietin-2, and TEK. Activation of vascular organoids with interleukin-1β did not have an additive effect on vascular permeability. Spike antigen was detected in some patients{\textquoteright} lung pericytes, which was associated with a decrease in CD144 expression and increased platelet recruitment and von Willebrand factor (VWF) deposition in the capillaries of these patients, with thrombi in large vessels rich in VWF and fibrin.Conclusion: Together, our data indicate that direct viral exposure to the microvasculature modelled by organoid infection and viral antigen treatment results in pericyte infection, detachment, damage, and cell death, disrupting pericyte-endothelial cell crosstalk and increasing microvascular endothelial permeability, which can promote thrombotic and bleeding complications in the microcirculation.",

keywords = "SARS-CoV-2, COVID-19, Endothelial permeability, Thrombosis, Organoids, Vasculopathy",

author = "Abdullah Khan and Jasmeet Reyat and Harriet Hill and Joshua Bourne and Martina Colicchia and Newby, {Maddy L} and Allen, {Joel D} and Max Crispin and Esther Youd and Paul Murray and Graham Taylor and Zania Stamataki and Alex Richter and Adam Cunningham and Matthew Pugh and Julie Rayes",

note = "Final Version of Record not yet available as of 26/08/2022 {\textcopyright} The Author(s) 2022. Published by Oxford University Press on behalf of European Society of Cardiology.",

year = "2022",

month = jun,

day = "16",

doi = "10.1093/cvr/cvac097",

language = "English",

pages = "1--12",

journal = "Cardiovascular Research",

issn = "0008-6363",

publisher = "Oxford University Press",

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Khan, A, Reyat, J, Hill, H, Bourne, J, Colicchia, M, Newby, ML, Allen, JD, Crispin, M, Youd, E, Murray, P, Taylor, G , Stamataki, Z , Richter, A , Cunningham, A , Pugh, M & Rayes, J 2022, 'Preferential uptake of SARS-CoV-2 by pericytes potentiates vascular damage and permeability in an organoid model of the microvasculature', Cardiovascular Research, pp. 1-12. https://doi.org/10.1093/cvr/cvac097

TY - JOUR

T1 - Preferential uptake of SARS-CoV-2 by pericytes potentiates vascular damage and permeability in an organoid model of the microvasculature

AU - Khan, Abdullah

AU - Reyat, Jasmeet

AU - Hill, Harriet

AU - Bourne, Joshua

AU - Colicchia, Martina

AU - Newby, Maddy L

AU - Allen, Joel D

AU - Crispin, Max

AU - Youd, Esther

AU - Murray, Paul

AU - Taylor, Graham

AU - Stamataki, Zania

AU - Richter, Alex

AU - Cunningham, Adam

AU - Pugh, Matthew

AU - Rayes, Julie

N1 - Final Version of Record not yet available as of 26/08/2022 © The Author(s) 2022. Published by Oxford University Press on behalf of European Society of Cardiology.

PY - 2022/6/16

Y1 - 2022/6/16

N2 - Aims: Thrombotic complications and vasculopathy have been extensively associated with severe COVID-19 infection; however, the mechanisms inducing endotheliitis and the disruption of endothelial integrity in the microcirculation are poorly understood. We hypothesized that within the vessel wall, pericytes preferentially take up viral particles and mediate the subsequent loss of vascular integrity.Methods and results: Immunofluorescence of post-mortem patient sections was used to assess pathophysiological aspects of COVID-19 infection. The effects of COVID-19 on the microvasculature were assessed using a vascular organoid model exposed to live viral particles or recombinant viral antigens. We find increased expression of the viral entry receptor angiotensin-converting enzyme 2 on pericytes when compared to vascular endothelium and a reduction in the expression of the junctional protein CD144, as well as increased cell death, upon treatment with both live virus and/or viral antigens. We observe a dysregulation of genes implicated in vascular permeability, including Notch receptor 3, angiopoietin-2, and TEK. Activation of vascular organoids with interleukin-1β did not have an additive effect on vascular permeability. Spike antigen was detected in some patients’ lung pericytes, which was associated with a decrease in CD144 expression and increased platelet recruitment and von Willebrand factor (VWF) deposition in the capillaries of these patients, with thrombi in large vessels rich in VWF and fibrin.Conclusion: Together, our data indicate that direct viral exposure to the microvasculature modelled by organoid infection and viral antigen treatment results in pericyte infection, detachment, damage, and cell death, disrupting pericyte-endothelial cell crosstalk and increasing microvascular endothelial permeability, which can promote thrombotic and bleeding complications in the microcirculation.

AB - Aims: Thrombotic complications and vasculopathy have been extensively associated with severe COVID-19 infection; however, the mechanisms inducing endotheliitis and the disruption of endothelial integrity in the microcirculation are poorly understood. We hypothesized that within the vessel wall, pericytes preferentially take up viral particles and mediate the subsequent loss of vascular integrity.Methods and results: Immunofluorescence of post-mortem patient sections was used to assess pathophysiological aspects of COVID-19 infection. The effects of COVID-19 on the microvasculature were assessed using a vascular organoid model exposed to live viral particles or recombinant viral antigens. We find increased expression of the viral entry receptor angiotensin-converting enzyme 2 on pericytes when compared to vascular endothelium and a reduction in the expression of the junctional protein CD144, as well as increased cell death, upon treatment with both live virus and/or viral antigens. We observe a dysregulation of genes implicated in vascular permeability, including Notch receptor 3, angiopoietin-2, and TEK. Activation of vascular organoids with interleukin-1β did not have an additive effect on vascular permeability. Spike antigen was detected in some patients’ lung pericytes, which was associated with a decrease in CD144 expression and increased platelet recruitment and von Willebrand factor (VWF) deposition in the capillaries of these patients, with thrombi in large vessels rich in VWF and fibrin.Conclusion: Together, our data indicate that direct viral exposure to the microvasculature modelled by organoid infection and viral antigen treatment results in pericyte infection, detachment, damage, and cell death, disrupting pericyte-endothelial cell crosstalk and increasing microvascular endothelial permeability, which can promote thrombotic and bleeding complications in the microcirculation.

KW - SARS-CoV-2

KW - COVID-19

KW - Endothelial permeability

KW - Thrombosis

KW - Organoids

KW - Vasculopathy

U2 - 10.1093/cvr/cvac097

DO - 10.1093/cvr/cvac097

M3 - Article

C2 - 35709328

SN - 0008-6363

SP - 1

EP - 12

JO - Cardiovascular Research

JF - Cardiovascular Research

M1 - cvac097

ER -

Preferential uptake of SARS-CoV-2 by pericytes potentiates vascular damage and permeability in an organoid model of the microvasculature

Abstract

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Keywords

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Engineering a novel human bone marrow organoid to target myelofibrosis

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