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Unravelling the two entities of endometrioid ovarian cancer: A single center clinical experience
Abstract
Objective
Due
to the increasing prevalence of the benign condition, ovarian carcinoma
arising from endometriosis is emerging as a relevant clinical entity
with an unclear biological signature. We have investigated clinical and
histologic features of endometriosis-associated endometrioid ovarian
cancer using an institutional retrospective database.
Methods
Patients
diagnosed with endometrioid ovarian cancer at our institution were
divided into two groups according to the fulfillment or not of Sampson's
and Scott's criteria for the detection of endometriosis-associated
ovarian cancer. Clinical and histological data were reported and
compared. Survival analysis was obtained using the log-rank test in an
unadjusted Kaplan-Meier method. Multivariate analysis was performed
using the Cox proportional hazards regression model to establish
independent factors associated with endometriosis-associated
endometrioid ovarian cancer and to identify predictors of survival.
Results
Patients
with endometriosis-associated endometrioid ovarian cancer were
significantly younger, had a lower disease stage (77% vs 38%; p = 0.003), a less prevalent high grade tumor (38% vs 82%; p = 0.002)
and a higher prevalence of squamous and mucinous metaplasia.
The rate
of endometrial cancer diagnosis was significantly higher in women with
endometriosis-associated endometrioid ovarian cancer (33%) than in other
patients (11%) (p = 0.04) with a 92% concordance between
ovarian and endometrial histologic tumor grade. A significant difference
in survival rate could not be demonstrated between patients with or
without endometriosis.
Conclusions
The
analysis of a retrospective endometrioid ovarian cancer database may
allow to suggest a molecular, morphological and clinical parallelism
between endometrial and endometrioid ovarian cancer.
Highlights
►
Endometriosis-associated endometrioid ovarian tumors possess a
different biologic signature when compared to cancers not associated
with the disease.
► Clinical course and molecular alterations of type I and type II endometrial tumors are similar to those detected respectively in endometriosis-associated and non-associated endometrioid ovarian tumor.
► Clinical course and molecular alterations of type I and type II endometrial tumors are similar to those detected respectively in endometriosis-associated and non-associated endometrioid ovarian tumor.
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