TIM‐3 Expression in Endometriosis

Author:

Lourenço Reis José1ORCID,Martins Catarina23,Ângelo‐Dias Miguel23,Rosa Natacha Nurdine4,Borrego Luís Miguel235,Lima Jorge123ORCID

Affiliation:

1. Department of Obstetrics and Gynecology LUZ SAÚDE Hospital da Luz Lisboa Lisboa Portugal

2. CHRC, NOVA Medical School Faculdade de Ciências Médicas, NMS|FCM Universidade Nova de Lisboa Lisboa Portugal

3. Immunology Department NOVA Medical School|Faculdade de Ciências Médicas NMS|FCM Universidade Nova de Lisboa Lisboa Portugal

4. UCD School of Medicine University College Dublin Dublin Ireland

5. Department of Imunoallergy LUZ SAÚDE, Hospital da Luz Lisboa Portugal

Abstract

ABSTRACTProblemEndometriosis is a prevalent chronic gynecological disease linked to immune dysfunction. The protein T‐cell immunoglobulin and mucin domain‐containing protein 3 (TIM‐3) plays a crucial role in immune system balance. Malfunction of TIM‐3 may result in excessive immune activation and inflammatory tissue damage. Given TIM‐3's established role in the development of cancer and autoimmune diseases, we decided to study its role in women suffering from endometriosis.Study MethodWe included a total of 62 female patients, all of whom had undergone laparoscopic surgery. Of these, 47 had endometriosis and 15 did not. During surgery, we collected peritoneal fluid (PF) and peripheral blood (PB) samples from every patient for analysis using flow cytometry. To mark the samples, we used a panel of monoclonal antibodies and examined TIM‐3 expression in their immune cells.ResultsEndometriosis patients in PB demonstrated a significantly lower percentage of CD56+ T cells with TIM‐3 expression. As endometriosis progressed through its stages, this expression lessened. This decrease was particularly notable in women with stage III/IV endometriosis. Additionally, both women diagnosed with intestinal endometriosis and those with recent endometriosis diagnoses showed a significantly reduced percentage of CD56+ T cells expressing TIM‐3.ConclusionsPatients with endometriosis exhibit diminished TIM‐3 expression within circulating T cells. This warrants further investigation to discern whether it contributes to the progression of endometriosis, potentially through the amplification of autoreactive T cells and inflammation.

Publisher

Wiley

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