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Intestine-specific deletion of metal transporter Zip14 (Slc39a14) causes brain manganese overload and locomotor defects of manganism

Am J Physiol Gastrointest Liver Physiol. 2020; 
Aydemir TB, Thorn TL, Ruggiero CH, Pompilus M, Febo M, Cousins RJ.
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Catalog Antibody … 137 Visualization was by chemiluminescence (SuperSignal, Thermo Fisher) and digital imaging 138 (Protein Simple) Rabbit anti-mouse ZIP14 antibody was custom made by Genscript Antibodies 139 for GAPDH and actin were obtained from Cell Signalling 140 … Get A Quote

摘要

Impaired manganese (Mn) homeostasis can result in excess Mn accumulation in specific brain regions and neuropathology. Maintaining Mn homeostasis and detoxification is dependent on effective Mn elimination. Specific metal transporters control Mn homeostasis. Human carriers of mutations in the metal transporter ZIP14 and whole-body Zip14 KO (WB-KO) mice display similar phenotypes, including spontaneous systemic and brain Mn overload, and motor dysfunction. Initially, it was believed that Mn accumulation due to ZIP14 mutations caused by impaired hepatobiliary Mn elimination. However, liver-specific Zip14 KO mice (L-KO) did not show systemic Mn accumulation or motor deficits. ZIP14 is highly expressed in the small... More

关键词

detoxification; manganism; neuroinflammation; parkinsonism; transport