Estradiol-driven metabolism in transwomen associates with reduced circulating extracellular vesicle microRNA-224/452

跨性别女性中雌二醇驱动的代谢与循环细胞外囊泡 microRNA-224/452 减少有关

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作者:Barend W Florijn, Jacques M G J Duijs, Maartje Klaver, Eline N Kuipers, Sander Kooijman, Jurrien Prins, Huayu Zhang, Hetty C M Sips, Wendy Stam, Maaike Hanegraaf, Ronald W A L Limpens, Rienk Nieuwland, Bas B van Rijn, Ton J Rabelink, Patrick C N Rensen, Martin den Heijer, Roel Bijkerk, Anton Jan van

Conclusion

This study identified an estradiol-drive post-transcriptional network that could potentially offer a mechanistic understanding of metabolism following gender-affirming estradiol therapy.

Methods

Following plasma miR-sequencing (seq) in a transwomen discovery (n = 20) and validation cohort (n = 30), we identified miR-224 and miR-452. Subsequent systemic silencing of these miRs in male C57Bl/6 J mice (n = 10) was followed by RNA-seq-based gene expression analysis of brown and white adipose tissue in conjunction with mechanistic studies in cultured adipocytes.

Objective

Sex steroid hormones like estrogens have a key role in the regulation of energy homeostasis and metabolism. In transwomen, gender-affirming hormone therapy like estradiol (in combination with antiandrogenic compounds) could affect metabolism as well. Given that the underlying pathophysiological mechanisms are not fully understood, this study assessed circulating estradiol-driven microRNAs (miRs) in transwomen and their regulation of genes involved in metabolism in mice.

Results

Estradiol in transwomen lowered plasma miR-224 and -452 carried in extracellular vesicles (EVs) while their systemic silencing in mice and cultured adipocytes increased lipogenesis (white adipose) but reduced glucose uptake and mitochondrial respiration (brown adipose). In white and brown adipose tissue, differentially expressed (miR target) genes are associated with lipogenesis (white adipose) and mitochondrial respiration and glucose uptake (brown adipose).

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