Solute Carrier Family SLC41, What Do We Really Know About It?

Overview

Journal Wiley Interdiscip Rev Membr Transp Signal

Specialty Biology

Date 2013 Dec 17

PMID 24340240

Citations 10

Authors

Andrea Fleig

Monika Schweigel-Rontgen

Martin Kolisek

Affiliations

Soon will be listed here.

Abstract

The 41 family of solute carriers (SLC41) comprises three members A1, A2 and A3, which are distantly homologous to bacterial Mg channel MgtE. SLC41A1 was recently characterized as being an Na/Mg exchanger (NME; a predominant cellular Mg efflux system). Little is known about the exact function of SLC41A2 and SLC41A3, although, these proteins have also been linked to Mg transport in human (animal) cells. The molecular biology (including membrane topology, cellular localization, transcriptomics and proteomics) of SLC41A2 and SLC41A3 compared with SLC41A1 has only been poorly explored. Significantly more data with regard to function, functional regulation, involvement in cellular signalling, complex-forming ability, spectrum of binding partners and involvement in the pathophysiology of human diseases are available for SLC41A1. Three recent observations namely the identification of the null mutation, c.698G>T, in SLC41A1 underlying the nephronophthisis-like phenotype, the recognition of a putative link between SLC41A1 and Parkinson's disease, and the observation that nearly 55% of preeclamptic placental samples overexpress marks the protein as a possible therapeutic target of these diseases. A potential role of the SLC41 family of Mg transporters in the pathophysiology of human diseases is further substantiated by the finding that SLC41A3 knockout mice develop abnormal locomotor coordination.

Citing Articles

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A Comprehensive Prognostic and Immune Analysis of SLC41A3 in Pan-Cancer.

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SLC41A1 and TRPM7 in magnesium homeostasis and genetic risk for Parkinson's disease.

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