Immunogenetics associated with severe coccidioidomycosis

与严重球孢子菌病相关的免疫遗传学

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作者:Amy P Hsu ,Agnieszka Korzeniowska ,Cynthia C Aguilar ,Jingwen Gu ,Eric Karlins ,Andrew J Oler ,Gang Chen ,Glennys V Reynoso ,Joie Davis ,Alexandria Chaput ,Tao Peng ,Ling Sun ,Justin B Lack ,Derek J Bays ,Ethan R Stewart ,Sarah E Waldman ,Daniel A Powell ,Fariba M Donovan ,Jigar V Desai ,Nima Pouladi ,Debra A Long Priel ,Daisuke Yamanaka ,Sergio D Rosenzweig ,Julie E Niemela ,Jennifer Stoddard ,Alexandra F Freeman ,Christa S Zerbe ,Douglas B Kuhns ,Yves A Lussier ,Kenneth N Olivier ,Richard C Boucher ,Heather D Hickman ,Jeffrey Frelinger ,Joshua Fierer ,Lisa F Shubitz ,Thomas L Leto ,George R Thompson 3rd ,John N Galgiani ,Michail S Lionakis ,Steven M Holland

Abstract

Disseminated coccidioidomycosis (DCM) is caused by Coccidioides, pathogenic fungi endemic to the southwestern United States and Mexico. Illness occurs in approximately 30% of those infected, less than 1% of whom develop disseminated disease. To address why some individuals allow dissemination, we enrolled patients with DCM and performed whole-exome sequencing. In an exploratory set of 67 patients with DCM, 2 had haploinsufficient STAT3 mutations, and defects in β-glucan sensing and response were seen in 34 of 67 cases. Damaging CLEC7A and PLCG2 variants were associated with impaired production of β-glucan-stimulated TNF-α from PBMCs compared with healthy controls. Using ancestry-matched controls, damaging CLEC7A and PLCG2 variants were overrepresented in DCM, including CLEC7A Y238* and PLCG2 R268W. A validation cohort of 111 patients with DCM confirmed the PLCG2 R268W, CLEC7A I223S, and CLEC7A Y238* variants. Stimulation with a DECTIN-1 agonist induced DUOX1/DUOXA1-derived hydrogen peroxide [H2O2] in transfected cells. Heterozygous DUOX1 or DUOXA1 variants that impaired H2O2 production were overrepresented in discovery and validation cohorts. Patients with DCM have impaired β-glucan sensing or response affecting TNF-α and H2O2 production. Impaired Coccidioides recognition and decreased cellular response are associated with disseminated coccidioidomycosis.

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