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17 β-Estradiol Impedes Aortic Root Dilation and Rupture in Male Marfan Mice

Louis Saddic, Sean Escopete, Lior Zilberberg, Shannon Kalsow, Divya Gupta, Mansoureh Eghbali, Sarah J. Parker

2023International Journal of Molecular Sciences11 citationsDOIOpen Access PDF

Abstract

Marfan syndrome causes a hereditary form of thoracic aortic aneurysms with worse outcomes in male compared to female patients. In this study, we examine the effects of 17 β-estradiol on aortic dilation and rupture in a Marfan mouse model. Marfan male mice were administered 17 β-estradiol, and the growth in the aortic root, along with the risk of aortic rupture, was measured. Transcriptomic profiling was used to identify enriched pathways from 17 β-estradiol treatments. Aortic smooth muscle cells were then treated with cytokines to validate functional mechanisms. We show that 17 β-estradiol decreased the size and rate of aortic root dilation and improved survival from rupture. The Marfan transcriptome was enriched in inflammatory genes, and the addition of 17 β-estradiol modulated a set of genes that function through TNFα mediated NF-κB signaling. In addition, 17 β-estradiol suppressed the induction of these TNFα induced genes in aortic smooth muscle cells in vitro in an NF-κB dependent manner, and 17 β-estradiol decreased the formation of adventitial inflammatory foci in aortic roots in vivo. In conclusion, 17 β-estradiol protects against the dilation and rupture of aortic roots in Marfan male mice through the inhibition of TNFα-NF-κB signaling.

Topics & Concepts

Marfan syndromeTranscriptomeMedicineInternal medicineIn vivoAortic rootCardiologyEndocrinologyAortaBiologyGene expressionGeneBiotechnologyBiochemistryAortic Disease and Treatment ApproachesAortic aneurysm repair treatmentsConnective tissue disorders research
17 β-Estradiol Impedes Aortic Root Dilation and Rupture in Male Marfan Mice | Litcius