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High-throughput phenotyping reveals expansive genetic and structural underpinnings of immune variation.

Authors :
Abeler-Dörner L
Laing AG
Lorenc A
Ushakov DS
Clare S
Speak AO
Duque-Correa MA
White JK
Ramirez-Solis R
Saran N
Bull KR
Morón B
Iwasaki J
Barton PR
Caetano S
Hng KI
Cambridge E
Forman S
Crockford TL
Griffiths M
Kane L
Harcourt K
Brandt C
Notley G
Babalola KO
Warren J
Mason JC
Meeniga A
Karp NA
Melvin D
Cawthorne E
Weinrick B
Rahim A
Drissler S
Meskas J
Yue A
Lux M
Song-Zhao GX
Chan A
Ballesteros Reviriego C
Abeler J
Wilson H
Przemska-Kosicka A
Edmans M
Strevens N
Pasztorek M
Meehan TF
Powrie F
Brinkman R
Dougan G
Jacobs W Jr
Lloyd CM
Cornall RJ
Maloy KJ
Grencis RK
Griffiths GM
Adams DJ
Hayday AC
Source :
Nature immunology [Nat Immunol] 2020 Jan; Vol. 21 (1), pp. 86-100. Date of Electronic Publication: 2019 Dec 16.
Publication Year :
2020

Abstract

By developing a high-density murine immunophenotyping platform compatible with high-throughput genetic screening, we have established profound contributions of genetics and structure to immune variation (http://www.immunophenotype.org). Specifically, high-throughput phenotyping of 530 unique mouse gene knockouts identified 140 monogenic 'hits', of which most had no previous immunologic association. Furthermore, hits were collectively enriched in genes for which humans show poor tolerance to loss of function. The immunophenotyping platform also exposed dense correlation networks linking immune parameters with each other and with specific physiologic traits. Such linkages limit freedom of movement for individual immune parameters, thereby imposing genetically regulated 'immunologic structures', the integrity of which was associated with immunocompetence. Hence, we provide an expanded genetic resource and structural perspective for understanding and monitoring immune variation in health and disease.

Details

Language :
English
ISSN :
1529-2916
Volume :
21
Issue :
1
Database :
MEDLINE
Journal :
Nature immunology
Publication Type :
Academic Journal
Accession number :
31844327
Full Text :
https://doi.org/10.1038/s41590-019-0549-0