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Manganese homeostasis: from rare single-gene disorders to complex phenotypes and diseases
Nathan Katz, Daniel J. Rader
Nathan Katz, Daniel J. Rader
Published November 4, 2019
Citation Information: J Clin Invest. 2019;129(12):5082-5085. https://doi.org/10.1172/JCI133120.
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Manganese homeostasis: from rare single-gene disorders to complex phenotypes and diseases

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Abstract

Manganese (Mn) participates in a variety of distinct physiological processes, including acting as a cofactor for several enzymes and metalloenzymes, in addition to playing a role in immune function, endocrine function, hematopoiesis, and oxidative stress regulation. Mn homeostasis is tightly regulated via intestinal absorption and hepatobiliary and intestinal excretion. In this issue of the JCI, Mercadante and colleagues explored the role of the metal transporter Slc30a10 in vivo using a mouse model system. The authors used whole-body and tissue-specific gene knockouts to show that Slc30a10 is paramount for Mn excretion in the liver and small intestines. These findings provide further insights into mechanisms for Mn homeostasis as well as potential targets for addressing Mn-associated disorders or environmental exposures.

Authors

Nathan Katz, Daniel J. Rader

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Single-gene Mendelian disorders of Mn homeostasis

Single-gene Mendelian disorders of Mn homeostasis


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