Loss of Inpp5d has disease-relevant and sex-specific effects on glial transcriptomes

Inpp5d 的缺失对神经胶质细胞转录组具有疾病相关和性别特异性的影响

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作者:Luke C Dabin, Holly Kersey, Byungwook Kim, Dominic J Acri, Daniel Sharify, Audrey Lee-Gosselin, Cristian A Lasagna-Reeves, Adrian L Oblak, Bruce T Lamb, Jungsu Kim

Discussion

Our data suggest that the normal function of Inpp5d is entangled with mechanisms involved in neurodegeneration. We report the effect of Inpp5d loss without pathology and show that this has dramatic effects on gene expression. Our study provides a critical reference for researchers of neurodegeneration, allowing separation of disease-specific changes mediated by Inpp5d in disease from baseline effects of Inpp5d loss. Highlights: Loss of Inpp5d has different effects in male and female mice. Genes dysregulated by Inpp5d loss relate to neurodegeneration. Total loss of Inpp5d in female mice collapses a conserved gene co-expression module. Loss of microglial Inpp5d affects the transcriptome of other cell types.

Methods

We performed single-cell RNA sequencing to study the effect of Inpp5d loss on wild-type mouse brain transcriptomes.

Results

Loss of Inpp5d has sex-specific effects on the brain transcriptome. Affected genes are enriched for multiple neurodegeneration terms. Network analyses reveal a gene co-expression module centered around Inpp5d in female mice. Inpp5d loss alters Pleotrophin (PTN), Prosaposin (PSAP), and Vascular Endothelial Growth Factor A (VEGFA) signaling probability between cell types.

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