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S-nitrosylation-triggered unfolded protein response maintains hematopoietic progenitors in Drosophila

Authors
Cho, BumsikShin, MingyuChang, EunjiSon, SeoghoShin, IncheolShim, Jiwon
Issue Date
Apr-2024
Publisher
Cell Press
Keywords
blood progenitor; Drosophila; EGFR; hematopoiesis; hemocyte; Ire1/Xbp1; lymph gland; nitric oxide; S-nitrosylation; unfolded protein response
Citation
Developmental Cell, v.59, no.8, pp 1075 - 1090.e6
Indexed
SCIE
SCOPUS
Journal Title
Developmental Cell
Volume
59
Number
8
Start Page
1075
End Page
1090.e6
URI
https://scholarworks.bwise.kr/hanyang/handle/2021.sw.hanyang/195291
DOI
10.1016/j.devcel.2024.02.013
ISSN
1534-5807
1878-1551
Abstract
The Drosophila lymph gland houses blood progenitors that give rise to myeloid-like blood cells. Initially, blood progenitors proliferate, but later, they become quiescent to maintain multipotency before differentiation. Despite the identification of various factors involved in multipotency maintenance, the cellular mechanism controlling blood progenitor quiescence remains elusive. Here, we identify the expression of nitric oxide synthase in blood progenitors, generating nitric oxide for post-translational S-nitrosylation of protein cysteine residues. S-nitrosylation activates the Ire1-Xbp1-mediated unfolded protein response, leading to G2 cell-cycle arrest. Specifically, we identify the epidermal growth factor receptor as a target of S-nitrosylation, resulting in its retention within the endoplasmic reticulum and blockade of its receptor function. Overall, our findings highlight developmentally programmed S-nitrosylation as a critical mechanism that induces protein quality control in blood progenitors, maintaining their undifferentiated state by inhibiting cell-cycle progression and rendering them unresponsive to paracrine factors.
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