Literature DB >> 27776107

RASGRP1 deficiency causes immunodeficiency with impaired cytoskeletal dynamics.

Elisabeth Salzer1,2, Deniz Cagdas3, Miroslav Hons4, Emily M Mace5, Wojciech Garncarz1,2, Özlem Yüce Petronczki1,2, René Platzer6, Laurène Pfajfer1,2, Ivan Bilic1, Sol A Ban1, Katharina L Willmann1, Malini Mukherjee5, Verena Supper6, Hsiang Ting Hsu5, Pinaki P Banerjee5, Papiya Sinha5, Fabienne McClanahan7, Gerhard J Zlabinger8, Winfried F Pickl9, John G Gribben7, Hannes Stockinger6, Keiryn L Bennett1, Johannes B Huppa6, Loïc Dupré1,2,10, Özden Sanal3, Ulrich Jäger11, Michael Sixt4, Ilhan Tezcan3, Jordan S Orange5, Kaan Boztug1,2,12,13.   

Abstract

RASGRP1 is an important guanine nucleotide exchange factor and activator of the RAS-MAPK pathway following T cell antigen receptor (TCR) signaling. The consequences of RASGRP1 mutations in humans are unknown. In a patient with recurrent bacterial and viral infections, born to healthy consanguineous parents, we used homozygosity mapping and exome sequencing to identify a biallelic stop-gain variant in RASGRP1. This variant segregated perfectly with the disease and has not been reported in genetic databases. RASGRP1 deficiency was associated in T cells and B cells with decreased phosphorylation of the extracellular-signal-regulated serine kinase ERK, which was restored following expression of wild-type RASGRP1. RASGRP1 deficiency also resulted in defective proliferation, activation and motility of T cells and B cells. RASGRP1-deficient natural killer (NK) cells exhibited impaired cytotoxicity with defective granule convergence and actin accumulation. Interaction proteomics identified the dynein light chain DYNLL1 as interacting with RASGRP1, which links RASGRP1 to cytoskeletal dynamics. RASGRP1-deficient cells showed decreased activation of the GTPase RhoA. Treatment with lenalidomide increased RhoA activity and reversed the migration and activation defects of RASGRP1-deficient lymphocytes.

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Year:  2016        PMID: 27776107      PMCID: PMC6400263          DOI: 10.1038/ni.3575

Source DB:  PubMed          Journal:  Nat Immunol        ISSN: 1529-2908            Impact factor:   25.606


  69 in total

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