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Literature DB >> 32647003

HEM1 deficiency disrupts mTORC2 and F-actin control in inherited immunodysregulatory disease.

Sarah A Cook¹, William A Comrie^1,2, M Cecilia Poli^3,4,5, Morgan Similuk⁶, Andrew J Oler⁷, Aiman J Faruqi¹, Douglas B Kuhns⁸, Sheng Yang⁹, Alexander Vargas-Hernández^3,4, Alexandre F Carisey^3,4, Benjamin Fournier^10,11, D Eric Anderson¹², Susan Price¹³, Margery Smelkinson¹⁴, Wadih Abou Chahla¹⁵, Lisa R Forbes^3,4, Emily M Mace¹⁶, Tram N Cao^3,4, Zeynep H Coban-Akdemir^17,18, Shalini N Jhangiani^18,19, Donna M Muzny^18,19, Richard A Gibbs^17,18,19, James R Lupski^17,18,19, Jordan S Orange¹⁶, Geoffrey D E Cuvelier²⁰, Moza Al Hassani²¹, Nawal Al Kaabi²¹, Zain Al Yafei²¹, Soma Jyonouchi^22,23, Nikita Raje^24,25, Jason W Caldwell²⁶, Yanping Huang^27,28, Janis K Burkhardt²⁷, Sylvain Latour^10,11, Baoyu Chen⁹, Gehad ElGhazali²¹, V Koneti Rao¹³, Ivan K Chinn^3,4, Michael J Lenardo²⁹.

Abstract

Immunodeficiency often coincides with hyperactive immune disorders such as autoimmunity, lymphoproliferation, or atopy, but this coincidence is rarely understood on a molecular level. We describe five patients from four families with immunodeficiency coupled with atopy, lymphoproliferation, and cytokine overproduction harboring mutations in NCKAP1L, which encodes the hematopoietic-specific HEM1 protein. These mutations cause the loss of the HEM1 protein and the WAVE regulatory complex (WRC) or disrupt binding to the WRC regulator, Arf1, thereby impairing actin polymerization, synapse formation, and immune cell migration. Diminished cortical actin networks caused by WRC loss led to uncontrolled cytokine release and immune hyperresponsiveness. HEM1 loss also blocked mechanistic target of rapamycin complex 2 (mTORC2)-dependent AKT phosphorylation, T cell proliferation, and selected effector functions, leading to immunodeficiency. Thus, the evolutionarily conserved HEM1 protein simultaneously regulates filamentous actin (F-actin) and mTORC2 signaling to achieve equipoise in immune responses.

Entities: Chemical

Mesh：

Substances：

Year: 2020 PMID： 32647003 PMCID： PMC8383235 DOI： 10.1126/science.aay5663

Source DB: PubMed Journal: Science ISSN： 0036-8075 Impact factor: 47.728

42 in total

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8. Genetic errors of immunity distinguish pediatric nonmalignant lymphoproliferative disorders.

Authors: Lisa R Forbes; Olive S Eckstein; Nitya Gulati; Erin C Peckham-Gregory; Nmazuo W Ozuah; Joseph Lubega; Nader K El-Mallawany; Jennifer E Agrusa; M Cecilia Poli; Tiphanie P Vogel; Natalia S Chaimowitz; Nicholas L Rider; Emily M Mace; Jordan S Orange; Jason W Caldwell; Juan C Aldave-Becerra; Stephen Jolles; Francesco Saettini; Hey J Chong; Asbjorg Stray-Pedersen; Helen E Heslop; Kala Y Kamdar; R Helen Rouce; Donna M Muzny; Shalini N Jhangiani; Richard A Gibbs; Zeynep H Coban-Akdemir; James R Lupski; Kenneth L McClain; Carl E Allen; Ivan K Chinn
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Authors: Klemens Rottner; Theresia E B Stradal; Baoyu Chen
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