Somatic Reversion of Pathogenic DOCK8 Variants Alters Lymphocyte Differentiation and Function to Effectively Cure DOCK8 Deficiency

Overview

Journal J Clin Invest

Specialty General Medicine

Date 2020 Dec 8

PMID 33290277

Citations 14

Authors

Bethany A Pillay

Mathieu Fusaro

Paul E Gray

Aaron L Statham

Leslie Burnett

Liliana Bezrodnik

Alisa Kane

Winnie Tong

Chrystelle Abdo

Sarah Winter

Samuel Chevalier

Romain Levy

Cecile Masson

Yohann Schmitt

Christine Bole

Marion Malphettes

Elizabeth Macintyre

Jean-Pierre de Villartay

John B Ziegler

Joanne M Smart

Jane Peake

Asghar Aghamohammadi

Lennart Hammarstrom

Hassan Abolhassani

Capucine Picard

Alain Fischer

Sylvain Latour

Benedicte Neven

Stuart G Tangye

Cindy S Ma

Affiliations

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Abstract

Inborn errors of immunity cause monogenic immune dysregulatory conditions such as severe and recurrent pathogen infection, inflammation, allergy, and malignancy. Somatic reversion refers to the spontaneous repair of a pathogenic germline genetic variant and has been reported to occur in a number of inborn errors of immunity, with a range of impacts on clinical outcomes of these conditions. DOCK8 deficiency due to biallelic inactivating mutations in DOCK8 causes a combined immunodeficiency characterized by severe bacterial, viral, and fungal infections, as well as allergic disease and some cancers. Here, we describe the clinical, genetic, and cellular features of 3 patients with biallelic DOCK8 variants who, following somatic reversion in multiple lymphocyte subsets, exhibited improved clinical features, including complete resolution of infection and allergic disease, and cure over time. Acquisition of DOCK8 expression restored defective lymphocyte signalling, survival and proliferation, as well as CD8+ T cell cytotoxicity, CD4+ T cell cytokine production, and memory B cell generation compared with typical DOCK8-deficient patients. Our temporal analysis of DOCK8-revertant and DOCK8-deficient cells within the same individual established mechanisms of clinical improvement in these patients following somatic reversion and revealed further nonredundant functions of DOCK8 in human lymphocyte biology. Last, our findings have significant implications for future therapeutic options for the treatment of DOCK8 deficiency.

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