| Literature DB >> 33571427 |
Shang Ma1, Adrienne E Dubin1, Yunxiao Zhang1, Seyed Ali Reza Mousavi1, Yu Wang1, Adam M Coombs1, Meaghan Loud1, Immacolata Andolfo2, Ardem Patapoutian3.
Abstract
Iron overload causes progressive organ damage and is associated with arthritis, liver damage, and heart failure. Elevated iron levels are present in 1%-5% of individuals; however, iron overload is undermonitored and underdiagnosed. Genetic factors affecting iron homeostasis are emerging. Individuals with hereditary xerocytosis, a rare disorder with gain-of-function (GOF) mutations in mechanosensitive PIEZO1 ion channel, develop age-onset iron overload. We show that constitutive or macrophage expression of a GOF Piezo1 allele in mice disrupts levels of the iron regulator hepcidin and causes iron overload. We further show that PIEZO1 is a key regulator of macrophage phagocytic activity and subsequent erythrocyte turnover. Strikingly, we find that E756del, a mild GOF PIEZO1 allele present in one-third of individuals of African descent, is strongly associated with increased plasma iron. Our study links macrophage mechanotransduction to iron metabolism and identifies a genetic risk factor for increased iron levels in African Americans.Entities:
Keywords: African American; Ion channel; PIEZO1; erythropoiesis; human genetics; iron metabolism; macrophage; mechanotransduction; phagocytosis
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Year: 2021 PMID: 33571427 PMCID: PMC7927959 DOI: 10.1016/j.cell.2021.01.024
Source DB: PubMed Journal: Cell ISSN: 0092-8674 Impact factor: 41.582