Hepatitis B virus (HBV) induced hepatocellular carcinoma (HCC) occurs predominantly in male patients. Aided by the capture-NGS, our recent study showed that the insertional mutagenesis to active TERT oncogene occurs preferentially in the male HCC. Meanwhile, the TERT promoter mutations at -124G>A and -146G>A, the most frequent somatic mutation identified in HCC, also occurred preferentially in male HCC. We have previously identified androgen and estrogen effects on the transcription of HBV via targeting to viral enhancer I, leading to higher viral titer in male carriers. This study proposed to investigate if sex hormones can also through the HBV integrated in the host genome or frequent TERT promoter mutations to regulate the expression of TERT oncogenes, as a mechanism contributing to male HCC. We propose to approach this by the cell culture based TERT-promoter-Luc reporter assay, containing the HBV integration or -124G>A or -146G>A mutations at promoter region. We first found a significantly higher Luc activity from HBV/TERT-Luc than that from WT/TERT-Luc construct, which can be further increased by AR but suppressed by ER pathway. Knockdown of HNF4Α abolished the difference, indicating the critical role of HNF4Α in this regulation. Next, we found a significant elevation in both G(-124)A and G(-146)A-Luc constructs relative to the WT-TERT-Luc, which is dependent on the GABPα. The effect of AR and ERα pathway was examined, showing the reporter activity to be further elevated by AR, in a ligand independent manner, which however was not affected by the ERα pathway. Interestingly, or results showed that HNF4Αalso contributed to the activation of G(-124)A-TERT-Luc. The function of AR however is independent of HNF4Α. Our study thus supported the involvement of sex hormones in regulating the transcription of TERT through HBV integration or frequent TERT promoter mutations.