Light micrograph of a cross-section of an ovary revealing cysts caused by endometriosis
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Recent extensive research into the biology of endometriosis has revealed novel mechanisms through which this chronic condition significantly impacts women’s health, paving the way for enhanced treatment options. This landmark study analyzed data from over 1 million women and identified specific genes linked to endometriosis among individuals of African descent, a group historically underrepresented in previous research.
According to Shefali Setia Verma from the University of Pennsylvania, “We identified approximately 300 genes that warrant further investigation in this field.”
Understanding Endometriosis: Endometriosis is a chronic and often debilitating condition characterized by the growth of tissue similar to the endometrium in locations outside the uterus, forming painful lesions. It affects approximately 10% of women of reproductive age, often leading to symptoms such as fatigue, severe pain, and fertility issues. Furthermore, endometriosis has been linked to cardiovascular diseases, although the underlying biological mechanisms remain inadequately understood.
To address this, Setia-Verma and her team employed a “multi-omics” approach, combining analyses of genes, proteins, microbiomes, and symptoms associated with endometriosis to create a comprehensive understanding of the condition. The researchers examined data from 14 global biobanks, compiling information from over 1 million women.
The team’s initial analysis uncovered 58 genomic regions related to endometriosis, with 27 of these being previously unidentified. Detailed scrutiny led to the identification of 314 genes associated with the disorder. Notably, this study highlighted three genetic regions linked to endometriosis detectable solely in individuals with African ancestry.
Among the most strongly associated genes, many were found to be involved in immune response, inflammation, and cellular motility. This is particularly significant as endometriosis involves cells growing inappropriately, suggesting the condition may relate to the biological processes governing cell migration rather than just misplaced tissue growth. “This insight may lead to the development of treatments targeting cell movement,” adds Setia Verma.
The association with inflammation and immune response may also clarify why endometriosis affects broader health issues, including cardiovascular disease, arthritis, and depression. Persistent inflammation going untreated can result in various long-term complications. In the UK, for example, the average time for a diagnosis is 9 years. Dr. Setia Verma stresses, “Untreated pain and inflammation can lead to a range of chronic symptoms.”
The insights from this study have crucial implications for treatment approaches. Current therapies for endometriosis predominantly target hormonal pathways since estrogen can stimulate lesion growth and associated inflammation. However, if inflammation is a principal factor in symptomatology and broader health concerns, addressing these inflammatory pathways may provide a more effective therapeutic strategy, according to Setia Verma.
The researchers discovered links between specific genes and proteins related to endometriosis, cardiovascular disease, and the regulation of blood cholesterol and fats. “This essentially indicates an increased cardiovascular disease risk for individuals with endometriosis,” remarks Setia Verma.
Another insightful finding was that individuals with endometriosis often exhibit reduced levels of Bifidobacteria, beneficial bacteria crucial for gut health and immune system support. “This sheds light on how endometriosis contributes to broader systemic health risks beyond reproductive issues,” states Setia Verma. This warrants further exploration into the role of Bifidobacteriaceae as a potential target for innovative therapies.
The strength of this study lies in its diverse participant demographic. Nilfel Ramioglu from Oxford University notes, “Most endometriosis research has focused on individuals of European descent, which limits the applicability of findings and exacerbates inequalities in women’s health research.” Ramioglu emphasizes that these efforts signify vital progress toward inclusive advancements in endometriosis research. However, additional research is essential for drawing definitive conclusions. As she asserts, “While this kind of study identifies biological pathways needing exploration, further validation is necessary to establish whether targeting these pathways leads to improved patient outcomes.”
Source: www.newscientist.com
