Abstract
AbstractIt has remained unknown how cells reduce cystine taken up from the extracellular space, which is a required step for further utilization of cysteine in key processes such as protein or glutathione synthesis. Here, we show that the thioredoxin-related protein of 14 kDa (TRP14, encoded by TXNDC17) is the rate-limiting enzyme for intracellular cystine reduction. When TRP14 is genetically knocked out, cysteine synthesis through the transsulfuration pathway becomes the major source of cysteine in human cells, and knockout of both pathways becomes lethal in C. elegans subjected to proteotoxic stress. TRP14 can also reduce cysteinyl moieties on proteins, rescuing their activities as here shown with cysteinylated peroxiredoxin 2. Txndc17 knockout mice were, surprisingly, protected in an acute pancreatitis model, concomitant with activation of Nrf2-driven antioxidant pathways and upregulation of transsulfuration. We conclude that TRP14 is the evolutionarily conserved enzyme principally responsible for intracellular cystine reduction in C. elegans, mice, and humans.
Funder
MEC | Agencia Estatal de Investigación
Ministry of Economy and Competitiveness from Spain
The Knut and Allice Wallenberg Foundations
Swedish Cancer Society
Swedish Research Council
National Tumor Laboratory Project
Hungarian Thematic Excellence Programme
The National Research. Development and Innovation Office
United States National Institutes of Health
Hungarian LKH Foundation and Hungarian Magyar Tudományos Akadémia
Conserjería de Economía, Conocimiento, Empresas y Universidad, Junta de Andalucía, Spain
MEC | Instituto de Salud Carlos III
Hungary Ministry of Culture and Innovation
Hungarian Thematic Excellence Program
HUN-REN Hungarian Research Network
Hungarian Academy of Sciences
Publisher
Springer Science and Business Media LLC
Cited by
1 articles.
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