Human genetic adaptation related to cellular zinc homeostasis

Author:

Roca-Umbert Ana,Garcia-Calleja JorgeORCID,Vogel-González Marina,Fierro-Villegas Alejandro,Ill-Raga Gerard,Herrera-Fernández Víctor,Bosnjak Anja,Muntané Gerard,Gutiérrez Esteban,Campelo FelixORCID,Vicente Rubén,Bosch ElenaORCID

Abstract

SLC30A9 encodes a ubiquitously zinc transporter (ZnT9) and has been consistently suggested as a candidate for positive selection in humans. However, no direct adaptive molecular phenotype has been demonstrated. Our results provide evidence for directional selection operating in two major complementary haplotypes in Africa and East Asia. These haplotypes are associated with differential gene expression but also differ in the Met50Val substitution (rs1047626) in ZnT9, which we show is found in homozygosis in the Denisovan genome and displays accompanying signatures suggestive of archaic introgression. Although we found no significant differences in systemic zinc content between individuals with different rs1047626 genotypes, we demonstrate that the expression of the derived isoform (ZnT9 50Val) in HEK293 cells shows a gain of function when compared with the ancestral (ZnT9 50Met) variant. Notably, the ZnT9 50Val variant was found associated with differences in zinc handling by the mitochondria and endoplasmic reticulum, with an impact on mitochondrial metabolism. Given the essential role of the mitochondria in skeletal muscle and since the derived allele at rs1047626 is known to be associated with greater susceptibility to several neuropsychiatric traits, we propose that adaptation to cold may have driven this selection event, while also impacting predisposition to neuropsychiatric disorders in modern humans.

Funder

Ministerio de Ciencia e Innovación

Unidad de Excelencia María de Maeztu

Severo Ochoa

Direcció General de Recerca, Generalitat de Catalunya

Fundació Cellex, Fundació Mir-Puig, and Generalitat de Catalunya

FPI-MCIN/AEI PhD

Instituto de Salud Carlos III

Publisher

Public Library of Science (PLoS)

Subject

Cancer Research,Genetics (clinical),Genetics,Molecular Biology,Ecology, Evolution, Behavior and Systematics

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