Hormonal Treatment of Human Hepatocellular Carcinoma

Overview

Journal Ann N Y Acad Sci

Specialty Science

Date 2007 Jan 31

PMID 17261772

Citations 20

Authors

Massimo Di Maio

Ermelinda De Maio

Alessandro Morabito

Roberta DAniello

Gianfranco De Feo

Ciro Gallo

Francesco Perrone

Affiliations

Soon will be listed here.

Abstract

Animal models of experimental liver carcinogenesis and epidemiological studies in humans suggest a relationship between sex hormones and hepatocellular carcinoma (HCC). In 1997, a systematic review of the existing, small randomized trials evaluating the antiestrogen tamoxifen yielded a positive result, but the large randomized CLIP-1 trial showed no survival advantage from the addition of tamoxifen to best supportive care. A possible explanation for the negative results is the lack of patient selection, but the expression of estrogen (ER) and progesterone (PgR) receptors in HCC does not clearly affect the survival outcome of the patients treated with tamoxifen. In the last years, it has been proposed that negative results might be due to the fact that tamoxifen in HCC could act via an ER-independent pathway, which requires much higher doses than those usually administered, but a double-blind Asian randomized trial conducted to assess possible dose-response effect showed no efficacy for tamoxifen, with an inversely negative impact with increasing dose. According to the results of large trials and of the Cochrane systematic review, neither further trials are warranted with tamoxifen in HCC, nor should any use in clinical practice be considered. Interesting results have been obtained when the type of hormonal treatment (tamoxifen or megestrol) has been chosen according to the presence of wild-type or variant ER, but these results should be confirmed in large randomized trials. Negative results have been obtained with antiandrogen therapy. In conclusion, hormonal treatment should not be a part of the current management of HCC patients.

Citing Articles

Anti-Hepatocellular Carcinoma Effect and Molecular Mechanism of the Estrogen Signaling Pathway.

Guo Y, Wu G, Yi J, Yang Q, Jiang W, Lin S Front Oncol. 2022; 11:763539.

PMID: 35096574 PMC: 8789654. DOI: 10.3389/fonc.2021.763539.

SERMs (selective estrogen receptor modulator), acting as estrogen receptor β agonists in hepatocellular carcinoma cells, inhibit the transforming growth factor-α-induced migration via specific inhibition of AKT signaling pathway.

Matsushima-Nishiwaki R, Yamada N, Hattori Y, Hosokawa Y, Tachi J, Hori T PLoS One. 2022; 17(1):e0262485.

PMID: 35007301 PMC: 8746762. DOI: 10.1371/journal.pone.0262485.

Estrogen Receptor-α Suppresses Liver Carcinogenesis and Establishes Sex-Specific Gene Expression.

OBrien M, Pitot H, Chung S, Lambert P, Drinkwater N, Bilger A Cancers (Basel). 2021; 13(10).

PMID: 34068249 PMC: 8153146. DOI: 10.3390/cancers13102355.

Olaparib and enzalutamide synergistically suppress HCC progression via the AR-mediated miR-146a-5p/BRCA1 signaling.

Zhao J, Sun Y, Lin H, Chou F, Xiao Y, Jin R FASEB J. 2020; 34(4):5877-5891.

PMID: 32134529 PMC: 7243671. DOI: 10.1096/fj.201903045RR.

Genetic Predisposition to Hepatocarcinogenesis in Inbred and Outbred Mouse Lines Selected for High or Low Inflammatory Response.

de Carvalho L, Borrego A, Jensen J, Koury Cabrera W, Santos A, Ribeiro O J Immunol Res. 2019; 2019:5298792.

PMID: 31049358 PMC: 6462334. DOI: 10.1155/2019/5298792.