Abstract
Accurate diagnosis of ovarian
clear cell carcinoma (CCC) is important because of its poor prognosis
with chemoresistance and a high recurrent rate. The clinicopathologic
characteristics and prognostic significance of the cell cycle regulator
[early mitotic inhibitor-1 (Emi1)] and galactoside-binding protein
(Galectin-3) were evaluated. Among 155 CCCs from 18 hospitals in Korea
between 1995 and 2006, 129 pure CCCs were selected with consensus using
immunohistochemical stains for hepatocyte nuclear factor-1β, Wilms'
tumor protein, and estrogen receptor. The expressions of Emi1,
Galectin-3, p53, and Ki-67 labeling index were analyzed with
clinicopathologic parameters and the patient's survival. The mean age of
the patients was 49.6 yr; the tumors were bilateral in 10.9%, and the
average size was 12 cm. Adenofibromatous component was found in 7%, and
endometriosis in 48.1% of the cases. Psammoma body was seen in 16.3%.
Disease-free survival and overall survival rates were 78.3% and 79.1%,
respectively. The International Federation of Obstetrics and Gynecology
(FIGO) stage was the most important prognostic indicator. Emi1
expression (>5%) was seen in 23.3% of CCCs, and associated with high
FIGO grades and poor overall survival (P<0.05). High Galectin-3
(≥80%) expression was seen in 59.7% of CCCs, and associated with FIGO
stages III and IV, and high Ki-67 labeling index. High Ki-67 labeling
index (≥50%) and p53 expression (≥50%) were seen in 27.1% and 18.6% of
CCCs, respectively, but there was no clinicopathologic and prognostic
significance. On the basis of the fact that the expression of Emi1 in
CCC was correlated with a high histologic grade and worse overall
survival, target therapy using inhibitors of Emi1 may be tried in the
management of CCC patients with Emi1 expression.
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