Sex Chromosomes and Gonads Shape the Sex-Biased Transcriptomic Landscape in Tlr7-Mediated Demyelination During Aging

Author:

Lopez-Lee ChloeORCID,Kodama Lay,Fan Li,Wong Man Ying,Foxe Nessa R.,Jiaz Laraib,Yu Fangmin,Ye Pearly,Zhu Jingjie,Norman Kendra,Torres Eileen Ruth,Kim Rachel D.,Mousa Gergey Alzaem,Dubal DenaORCID,Liddelow ShaneORCID,Luo Wenjie,Gan Li

Abstract

AbstractDemyelination occurs in aging and associated diseases, including Alzheimer’s disease. Several of these diseases exhibit sex differences in prevalence and severity. Biological sex primarily stems from sex chromosomes and gonads releasing sex hormones. To dissect mechanisms underlying sex differences in demyelination of aging brains, we constructed a transcriptomic atlas of cell type-specific responses to illustrate how sex chromosomes, gonads, and their interaction shape responses to demyelination. We found that sex-biased oligodendrocyte and microglial responses are driven by interaction of sex chromosomes and gonads prior to myelin loss. Post demyelination, sex chromosomes mainly guide microglial responses, while gonadal composition influences oligodendrocyte signaling. Significantly, ablation of the X-linked gene Toll-like receptor 7 (Tlr7), which exhibited sex-biased expression during demyelination, abolished the sex-biased responses and protected against demyelination.One-sentence summaryCell type-specific processes underlying aged demyelination are sex-biased and mediated byTlr7.

Publisher

Cold Spring Harbor Laboratory

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