Prognostic impact of CD133 expression in Endometrial Cancer Patients

被引:0
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作者
G. Mancebo
J. M. Sole-Sedeno
O. Pino
E. Miralpeix
S. Mojal
L. Garrigos
B. Lloveras
P. Navarro
J. Gibert
M. Lorenzo
I. Aran
R. Carreras
F. Alameda
机构
[1] Passeig Marítim,Obstetrics and Gynaecology Department of Hospital Universitari del Mar
[2] 25-29,Oncology Department of Hospital Universitari de la Vall d’Hebron
[3] Passeig de la Vall d’Hebron,Pathology Department of Hospital Universitari del Mar.
[4] 119-129,Universitat Autónoma de Barcelona
[5] Passeig Marítim,Universitat Pompeu Fabra
[6] 25-29,Department of Statistics, IMIM
[7] Plaza Cívica,Hospital del Mar Medical Research Institute
[8] Campus de la UAB,Cancer Research Programme, IMIM
[9] Doctor Aiguader,Hospital del Mar Medical Research Institute
[10] 80,undefined
[11] Doctor Aiguader,undefined
[12] 88,undefined
[13] Doctor Aiguader,undefined
[14] 88,undefined
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Scientific Reports | / 7卷
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摘要
To assess the impact of CD133 expression on the prognosis of endometrioid endometrial carcinoma (EEC). We retrospectively assessed CD133 expression in tissue microarray of 116 surgically treated FIGO I-III EEC. Tumors with ≥10% of CD133-expressing cells were considered CD133-positive (CD133+). On the basis of CD133 expression, clinical and pathological parameters, progression-free survival (PFS) and overall survival (OS) were evaluated. Of the EEC studied 85.2% showed CD133-expressing cells. Only 61% (n = 66) of EEC presented ≥10% of CD133 expressing cells and were considered CD133+. The mean OS for CD133+ tumour patients was 161 months (95% CI, 154–168) as compared with 146 months (95% CI, 123–160) for those with CD133- tumors (p = 0.012). The mean PFS for CD133+ tumour was 159 months (95% CI, 149–168) as compared with 147 months (95% CI, 132-161) in those with a CD133-tumour (p = 0.014). CD133+ tumours were less likely to have vascular invasion (p = 0.010) and more likely to be well differentiated (p = 0.034). C133+ tumours predicted favorable OS and PFS of EEC patients, with a Hazard Ratio 4.731 (95% CI, 1.251–17.89; p = 0.022). CD133+ tumor status correlates with favorable prognosis of EEC. Our findings are in agreement with studies addressing brain and colorectal tumours.
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