Aranda Gloria, Fernández-Rebollo Eduardo, Pradas-Juni Marta, Hanzu Felicia Alexandra, Kalko Susana G, Halperin Irene, Mora Mireia
Group of Endocrine Disorders, IDIBAPS, Barcelona, Spain; Department of Endocrinology and Nutrition, Hospital Clinic, Barcelona, Spain.
Spanish Biomedical Research Centre in Diabetes and Associated Metabolic Disorders (CIBERDEM), Barcelona, Spain.
J Steroid Biochem Mol Biol. 2017 Sep;172:20-28. doi: 10.1016/j.jsbmb.2017.05.010. Epub 2017 May 21.
Cross-sex hormone therapy (CHT) is critical for phenotypical and physiological transition in adults with gender dysphoria (GD). However, the impact of the CHT onto the molecular level/epigenetic regulation has not been comprehensively addressed. We postulate that CHT in GD could drive changes at the androgen receptor (AR), estrogen receptor alpha (ESR1) and estrogen receptor beta (ESR2), affecting their DNA methylation pattern and mRNA expression that may influence in the phenotypical changes associated to CHT. We carried out a prospective observational study on individuals with a diagnosis of GD. 18 subjects (no previous CHT): 12 female to male (FtoM) and 6 male to female (MtoF). An Epityper Mass array TM method was used to study the DNA methylation and Real-time PCR quantitative reverse transcription PCR (qRT-PCR) was used to quantify the gene expression. The analysis of AR, ESR1 and ESR2 receptor was performed at baseline, 6 and 12 months after CHT. No differences in DNA methylation of ESR were found in MtoF, while DNA methylation was increased in FtoM at 6 and 12 months of CHT. The AR showed a significant increase of methylation in MtoF group after 12 months of estrogenic treatment. Regarding the expression analysis, AR expression was significantly decreased in FtoM upon CHT treatment. AR, ESR1 and ESR2 methylation were correlated with anthropometric, metabolic and hormonal parameters in FtoM and MtoF. Our results support that CHT is associated to epigenetic changes that might affect the response to treatment with sex steroids.
跨性别激素疗法(CHT)对于患有性别焦虑症(GD)的成年人的表型和生理转变至关重要。然而,CHT对分子水平/表观遗传调控的影响尚未得到全面探讨。我们推测,GD患者的CHT可能会导致雄激素受体(AR)、雌激素受体α(ESR1)和雌激素受体β(ESR2)发生变化,影响它们的DNA甲基化模式和mRNA表达,这可能会影响与CHT相关的表型变化。我们对诊断为GD的个体进行了一项前瞻性观察研究。18名受试者(未接受过CHT):12名女性变男性(FtoM)和6名男性变女性(MtoF)。采用Epityper Mass array TM方法研究DNA甲基化,采用实时PCR定量逆转录PCR(qRT-PCR)定量基因表达。在基线、CHT后6个月和12个月对AR、ESR1和ESR2受体进行分析。在MtoF中未发现ESR的DNA甲基化有差异,而在CHT治疗6个月和12个月时,FtoM的DNA甲基化增加。在接受雌激素治疗12个月后,MtoF组的AR甲基化显著增加。关于表达分析,CHT治疗后FtoM中的AR表达显著降低。FtoM和MtoF中的AR、ESR1和ESR2甲基化与人体测量、代谢和激素参数相关。我们的结果支持CHT与表观遗传变化有关,这些变化可能会影响对性类固醇治疗的反应。
