Molecular mechanisms and biological plausibility underlying the malignant transformation of endometriosis: a critical analysis

doi:10.1093/humupd/dmi037

Human Reproduction Update Advance Access originally published online on September 19, 2005
Human Reproduction Update 2006 12(1):77-89; doi:10.1093/humupd/dmi037

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© The Author 2005. 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@oupjournals.org

Molecular mechanisms and biological plausibility underlying the malignant transformation of endometriosis: a critical analysis

Paola Viganó¹, Edgardo Somigliana, Ilda Chiodo, Annalisa Abbiati and Paolo Vercellini

Department of Obstetrics, Gynecology and Neonatology, Fondazione ‘Policlinico–Mangiagalli–Regina Elena’, Milan, Italy

^¹ To whom correspondence should be addressed at: Department of Obstetrics, Gynecology and Neonatology, Fondazione ‘Policlinico–Mangiagalli–Regina Elena’, Via Commenda 12, 20122 Milan, Italy. E-mail: paola.vigano{at}unimi.it

Submitted on June 1, 2005; accepted on July 29, 2005

Although population-based studies have unequivocally reportedan increased risk of ovarian cancer in women with endometriosis,the biological evidence supporting the idea of endometriosisas a preneoplastic condition is scanty and not well substantiated.The fundamental features of human neoplasms (monoclonal growth,genetic changes, mutations in tumour suppressor genes and replicativeadvantage) have been evaluated in endometriotic lesions butresults obtained are discordant. It is plausible that ectopicglands may expand monoclonally but the entity of this phenomenonis debated. According to some allelotyping studies, from one-thirdto one-half of endometriosis lesions would harbour somatic geneticchanges in chromosomal regions supposed to contain genes involvedin ovarian tumourigenesis, especially for the endometrioid histotype.These findings would be consistent with the progression modelfor carcinogenesis from the benign precursor to ovarian cancerbut they could not be unequivocally replicated. Gene mutationalstudies are rare in this context. A single group has found missensemutations and deletions of PTEN gene in about 20% of ovarianendometriotic cysts. Moreover, in a model of genetically engineeredmice harbouring an oncogenic allele of K-ras resulting in benignlesions reminiscent of endometriosis, a conditional deletionof PTEN caused the progression towards the endometrioid tumour.Based on these data, the causal link between endometriosis andovarian endometrioid/clear cell carcinomas remains to be definedboth in terms of entity of association and of undelying molecularmechanisms.

Key words: endometriosis / malignant transformation of endometriosis / molecular mechanisms

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