Deeply infiltrating endometriosis: pathogenetic implications of the anatomical distribution

doi:10.1093/humrep/del079

Hum. Reprod. Advance Access originally published online on March 16, 2006
Human Reproduction 2006 21(7):1839-1845; doi:10.1093/humrep/del079

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© The Author 2006. Published by Oxford University Press on behalf of the European Society of Human Reproduction and Embryology. All rights reserved. For Permissions, please email: journals.permissions@oxfordjournals.org

Deeply infiltrating endometriosis: pathogenetic implications of the anatomical distribution

Charles Chapron¹^{, 2}^{, 5}, Nicolas Chopin¹, Bruno Borghese¹, Hervé Foulot¹, Bertrand Dousset³, Marie Cécile Vacher-Lavenu⁴, Marco Vieira¹, Wael Hasan¹ and Alexandre Bricou¹

¹ Service de Gynécologie Obstérique II, Unité de Chirurgie Gynécologique ² Institut Cochin, IFR ³ Service de Chirurgie Digestive and ⁴ Sevice Central d’Anatomie et Cytologie Pathologiques, Université Paris V, Assistance Publique – Hôpitaux de Paris (AP-HP), Groupe Hospitalier Universitaire (GHU) Ouest, CHU Cochin, Paris, France

⁵ To whom correspondence should be addressed at: Département de Chirurgie Gynécologique, Service de Gynécologie Obstérique II, Clinique Universitaire Baudelocque, 123 Boulevard Port-Royal, CHU Cochin – Saint Vincent de Paul, 75014 Paris, France. E-mail: charles.chapron{at}cch.ap-hop-paris.fr

BACKGROUND: To investigate whether knowledge of the anatomicaldistribution of histologically proven deeply infiltrating endometriosis(DIE) lesions contributes to understanding the pathogenesis.METHODS: Observational study between June 1992 and December2004 (retrospective study between 1992 and 2000; prospectivestudy between 2001 and 2004). Continuous series of 426 patientssuffering from pelvic pain who underwent complete surgical exeresisof DIE. DIE lesions were classified according to four differentpossibilities: (i) Firstly, DIE lesions were classified as locatedin the anterior or posterior pelvic compartment. (ii) Secondly,DIE were classified as left, median and right. (iii) Thirdly,DIE lesions were classified as pelvic or abdominal. (iv) Fourthly,DIE lesions that could present in a right and/or left locationwere classified as unilateral or bilateral. RESULTS: These 426patients presented 759 histologically proven DIE lesions: bladder(48 lesions; 6.3%); uterosacral (USL) (400 lesions; 52.7%);vagina (123 lesions; 16.2%); ureter (16 lesions; 2.1%) and intestine(172, 22.7%). DIE lesions are significantly more often locatedin the pelvis (n = 730 lesions) than in the abdomen (n = 29lesions) (P < 0.0001). Pelvic DIE lesions are significantlymore often located in the posterior compartment of the pelvis[682 DIE lesions (93.4%) versus 48 DIE lesions (6.6%); P <0.0001]. Pelvic DIE lesions are significantly more frequentlylocated on the left side. For patients with unilateral pelvicDIE lesions, the anatomical distribution is significantly differentin the three groups: left (172 lesions; 32.0%), median (284lesions; 52.8%) and right (82 lesions; 15.2%) (P < 0.0001).For patients with lateral lesions, left DIE lesions (172 lesions;67.8%) were found significantly more frequently than right DIElesions (82 lesions; 32.2%) (P < 0.0001). A similar predispositionwas observed when we included patients with bilateral pelvicDIE lesions (P = 0.0031). The same significantly asymmetricdistribution is observed for total (pelvic and abdominal) DIElesions. CONCLUSIONS: Our results demonstrate that distributionof DIE lesions is asymmetric. It is possible that this is relatedto the anatomical difference between the left and right hemipelvisand to the flow of peritoneal fluid. These findings supportthe hypothesis that retrograde menstruation of regurgitatedendometrial cells is implicated in the pathogenesis of DIE.

Key words: anatomical distribution/deeply infiltrating endometriosis/implantation/pathogenesis/retrograde menstruation

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