The inactive X chromosome drives sex differences in microglial inflammatory activity in human glioblastoma

Author:

Tharp Marla E.ORCID,Han Claudia Z.ORCID,Balak Chris D.ORCID,Fitzpatrick Conor,O’Connor Carolyn,Preissl Sebastian,Buchanan Justin,Nott AlexiORCID,Escoubet Laure,Mavrommatis Konstantinos,Gupta Mihir,Schwartz Marc S.,Hoi Sang U,Jones Pamela S.,Levy Michael L.,Gonda David D.,Ben-Haim Sharona,Ciacci Joseph,Barba David,Khalessi Alexander,Coufal Nicole G.ORCID,Chen Clark C.,Glass Christopher K.ORCID,Page David C.ORCID

Abstract

SummaryBiological sex is an important risk factor in cancer, but the underlying cell types and mechanisms remain obscure. Since tumor development is regulated by the immune system, we hypothesize that sex-biased immune interactions underpin sex differences in cancer. The male-biased glioblastoma multiforme (GBM) is an aggressive and treatment-refractory tumor in urgent need of more innovative approaches, such as considering sex differences, to improve outcomes. GBM arises in the specialized brain immune environment dominated by microglia, so we explored sex differences in this immune cell type. We isolated adult human TAM-MGs (tumor-associated macrophages enriched for microglia) and control microglia and found sex-biased inflammatory signatures in GBM and lower-grade tumors associated with pro-tumorigenic activity in males and anti-tumorigenic activity in females. We demonstrated that genes expressed or modulated by the inactive X chromosome facilitate this bias. Together, our results implicate TAM-MGs, specifically their sex chromosomes, as drivers of male bias in GBM.

Publisher

Cold Spring Harbor Laboratory

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