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A systems genomics approach uncovers molecular associates of RSV severity

View ORCID ProfileMatthew N McCall, View ORCID ProfileChin-Yi Chu, Lu Wang, Lauren Benoodt, Juilee Thakar, Anthony Corbett, Jeanne Holden-Wiltse, Christopher Slaunwhite, Alex Grier, Steven Gill, Ann R. Falsey, View ORCID ProfileDavid J Topham, View ORCID ProfileMary Caserta, Edward Walsh, View ORCID ProfileXing Qiu, Thomas J. Mariani
doi: https://doi.org/10.1101/2020.12.18.423266
Matthew N McCall
1 University of Rochester Medical Center;
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Chin-Yi Chu
2 University of Rochester;
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Lu Wang
1 University of Rochester Medical Center;
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Lauren Benoodt
1 University of Rochester Medical Center;
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Juilee Thakar
1 University of Rochester Medical Center;
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Anthony Corbett
1 University of Rochester Medical Center;
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Jeanne Holden-Wiltse
1 University of Rochester Medical Center;
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Christopher Slaunwhite
1 University of Rochester Medical Center;
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Alex Grier
1 University of Rochester Medical Center;
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Steven Gill
3 University of Rochester School of Medicine and Dentistry
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Ann R. Falsey
1 University of Rochester Medical Center;
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David J Topham
1 University of Rochester Medical Center;
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Mary Caserta
1 University of Rochester Medical Center;
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Edward Walsh
3 University of Rochester School of Medicine and Dentistry
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Xing Qiu
2 University of Rochester;
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Thomas J. Mariani
2 University of Rochester;
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  • For correspondence: tom_mariani@urmc.rochester.edu
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Abstract

Globally, RSV infection results in millions of hospitalizations and thousands of deaths each year. Specific factors that contribute to disease severity, such as premature birth and certain comorbidities, are well established. Additionally, genetic variants resulting in alterations in the adaptive and innate immune response appear to be associated with RSV severity. While previous studies focused on a single aspect of the disease, we jointly modeled the association of disparate data modalities with RSV severity. To investigate the host response to respiratory syncytial virus (RSV) infection in infants, we performed a systems-level study of RSV pathophysiology, incorporating high-throughput measurements of the peripheral innate and adaptive immune systems and the airway epithelium and microbiota. Specifically, we developed and employed a novel multi-omic data integration method based on multilayered principal component analysis, penalized regression, and feature weight back-propagation. Our novel approach enabled us to identify cell type specific and shared cellular pathways associated with RSV severity. Of particular interest was the association between RSV severity, activation of pathways controlling Th17 and acute phase response signaling, and inhibition of B cell receptor signaling, which were present in both airway and immune cells. These data identify specific aspects of dysregulation between the humoral and mucosal response to RSV that may play a critical role in determining illness severity.

Competing Interest Statement

ARF is currently receiving funding from Merck Sharpe and Dohme, Pfizer, Janssen, Astra Zeneca and BioFire and personal fees for DSMB from Novavax. The others authors do not have any competing interests to report.

Copyright 
The copyright holder for this preprint is the author/funder, who has granted bioRxiv a license to display the preprint in perpetuity. It is made available under a CC-BY-NC 4.0 International license.
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Posted December 19, 2020.
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A systems genomics approach uncovers molecular associates of RSV severity
Matthew N McCall, Chin-Yi Chu, Lu Wang, Lauren Benoodt, Juilee Thakar, Anthony Corbett, Jeanne Holden-Wiltse, Christopher Slaunwhite, Alex Grier, Steven Gill, Ann R. Falsey, David J Topham, Mary Caserta, Edward Walsh, Xing Qiu, Thomas J. Mariani
bioRxiv 2020.12.18.423266; doi: https://doi.org/10.1101/2020.12.18.423266
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A systems genomics approach uncovers molecular associates of RSV severity
Matthew N McCall, Chin-Yi Chu, Lu Wang, Lauren Benoodt, Juilee Thakar, Anthony Corbett, Jeanne Holden-Wiltse, Christopher Slaunwhite, Alex Grier, Steven Gill, Ann R. Falsey, David J Topham, Mary Caserta, Edward Walsh, Xing Qiu, Thomas J. Mariani
bioRxiv 2020.12.18.423266; doi: https://doi.org/10.1101/2020.12.18.423266

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