A recent expansive investigation has unveiled critical insights into the complex interplay between hormone therapy and autoimmune disease incidence among postmenopausal women, a demographic already disproportionately affected by these immune system disorders. The study, presented at the 2025 Annual Meeting of The Menopause Society in Orlando, exposes an elevated risk of developing autoimmune conditions linked to hormone therapy use, although the relationship is nuanced and demands further exploration.
Autoimmune diseases represent a significant public health challenge, with a steadily increasing global prevalence over recent decades. Women bear the brunt of this burden, exhibiting up to a fourfold greater likelihood of diagnosis compared with men. This striking sex disparity has spurred considerable scientific inquiry into the immunomodulatory role of sex hormones, especially as incidence rates shift conspicuously during and after the menopausal transition.
Dr. Xuezhi (Daniel) Jiang and colleagues conducted a landmark retrospective analysis involving nearly 1.8 million postmenopausal women, averaging 60.5 years of age. Utilizing data from the TriNetX global health research network, the study meticulously examined the association between hormone replacement therapies and the onset of various autoimmune diseases over different durations—5 years, 10 years, and across the entire postmenopausal period. The longitudinal design and sheer scale provide an unprecedented lens on this critical health intersection.
Results indicate that hormone therapy users exhibited a statistically significant increase in the incidence of autoimmune diseases compared to non-users, except in the cases of Graves’ disease and autoimmune hepatitis, where no meaningful elevation in risk was observed. These findings add a pivotal dimension to understanding how exogenous hormone modulation influences immune regulation in aging women.
The underlying biological mechanisms remain to be conclusively defined but may involve hormone-driven alterations in immune cell function. Estrogen, for instance, has been shown to exhibit both pro-inflammatory and anti-inflammatory effects contingent on context, receptor subtype, and immune cell populations. The postmenopausal hormonal milieu is markedly altered from that of reproductive years, potentially reshaping immune surveillance and tolerance in ways that predispose to autoimmunity when supplemented with exogenous hormones.
Critically, the research clarifies that while the relative risk elevation is statistically compelling, the absolute risks remain modest and highly variable depending on the specific autoimmune condition. This suggests that hormone therapy continues to be a viable and effective intervention for alleviating severe menopausal symptoms such as vasomotor instability, with benefits potentially outweighing risks for many patients, particularly when therapy is individualized under clinical guidance.
However, the retrospective observational design inherently limits causal inference, necessitating well-designed prospective studies to validate these associations, elucidate causal pathways, and define the temporal dynamics of hormone exposure and autoimmune pathogenesis. Such research would significantly advance clinicians’ ability to perform precise risk-benefit assessments tailored to each woman’s health profile.
Dr. Stephanie Faubion, medical director for The Menopause Society, emphasizes the paramount importance of personalized medicine when considering hormone therapy. The decision to commence or continue hormone replacement must integrate comprehensive evaluation of individual risk factors, symptomatology, and personal preferences. The current findings enrich the dialogue surrounding these decisions and reinforce the need for vigilant monitoring and informed consent.
The study also sheds light on the broader epidemiological trend of rising autoimmune disease prevalence, underscoring the necessity for interdisciplinary research that integrates endocrinology, immunology, and women’s health. Environmental exposures and psychosocial stressors have long been implicated in autoimmune pathophysiology, and their interactions with hormonal influences constitute a fertile ground for future investigation.
As the medical community grapples with optimizing menopause management, findings like these advocate for sustained support of hormone therapy research, enhanced patient education, and updated clinical guidelines that reflect emerging evidence. Healthcare providers must remain adaptable, integrating new knowledge to balance symptom relief with long-term health preservation.
The implications extend beyond individual patient care to public health policy and research funding priorities. Understanding hormone therapy’s full impact on autoimmune disease development could inform screening protocols, preventive strategies, and therapeutic innovations that ultimately improve quality of life for millions of aging women worldwide.
In summary, this comprehensive study marks a significant advancement in unraveling the multifaceted relationship between hormone therapy and autoimmune diseases in postmenopausal women. It highlights the complexity of immune-hormonal interactions and the imperative for nuanced clinical approaches. While hormone therapy remains a cornerstone in menopause symptom management, these findings motivate a reevaluation of risk practices and reaffirm the urgency for continued scientific inquiry.
Subject of Research: Association between hormone therapy and autoimmune disease risk in postmenopausal women
Article Title: Association of Hormone Therapy with Autoimmune Disease Risk in Postmenopausal Women: A TriNetX-Based Analysis
News Publication Date: October 21, 2025
Web References: https://menopause.org
Keywords: autoimmune diseases, hormone therapy, postmenopausal women, menopause management, immune regulation, estrogen, clinical risk assessment