Expression of endothelin 1 and endothelin A receptor in HPV-associated cervical carcinoma: new potential targets for anticancer therapy

被引:51
作者
Venuti, A
Salani, D
Manni, V
Poggiali, F
Bagnato, A
机构
[1] Regina Elena Canc Inst, Virol Lab, I-00158 Rome, Italy
[2] Regina Elena Canc Inst, Lab Mol Pathol & Ultrastruct, I-00158 Rome, Italy
关键词
ETAR antagonists; genital tumors; tumor growth; papillomavirus; autocrine loop;
D O I
10.1096/fj.00-0024com
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
Human papillomaviruses (HPV) are associated with cervical cancer and interact with growth factors that may enhance malignant transformation of cervical carcinoma cells. Endothelin-1 (ET-1) is released from HPV transfected keratinocytes and induces increased growth response in these cell lines in comparison with normal cells. In the present study several cervical carcinoma cell Lines have been analyzed to investigate the expression of ET-1 and its receptors as well as their involvement in tumor growth, All HPV-positive cancer cells secreted ET-1 and expressed mRNA for ET-1 and its receptors, whereas a HPV-negative carcinoma cell line expressed only the ETBR mRNA and didn't secrete ET-1, Binding studies showed that HPV-associated cells expressed an increased number of functional ETAR. ET-1 stimulated a marked dose-dependent increase in [H-3]-thymidine incorporation with respect to the normal cells whereas ET-3 and ETBR agonists had no effect, In HPV-positive cancer cells, a specific antagonist of ETAR inhibited the proliferation induced by ET-1 and substantially reduced the basal growth rate of unstimulated cervical tumor cells, whereas the ETBR antagonist had no effect, These results demonstrate that ET-1 participates in the progression of neoplastic growth in HPV-associated carcinoma, in which ETAR are increased and could be targeted for antitumor therapy.-Venuti, A., Salani, D., Manni, V., Poggiali, F., Bagnato, A. Expression of endothelin 1 and endothelin A receptor in HPV-associated cervical carcinoma: new potential targets for anticancer therapy.
引用
收藏
页码:2277 / 2283
页数:7
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