Telomerase-dependent Oncolytic Adenovirus for Cancer Treatment

Overview

Journal Gene Ther

Date 2003 Jul 15

PMID 12858189

Citations 33

Authors

T-G Huang

M J Savontaus

K Shinozaki

B V Sauter

S L C Woo

Affiliations

Soon will be listed here.

Abstract

Conditionally replicative adenovirus (CRAD) is an attractive anticancer agent as it can selectively replicate in tumor cells. Expression of telomerase reverse transcriptase (TERT) is a unique tumor cell characteristic, being absent in normal postmitotic cells. Thus, we constructed a TERT promoter regulated CRAD for tumor-specific oncolysis by replacing the endogenous adenovirus E1A promoter with that of human TERT (Adv-TERTp-E1A). We showed that its replication was severely attenuated in TERT-negative cells, but that it replicated almost as efficiently as wild-type adenovirus in TERT-positive cells. Accordingly, Adv-TERTp-E1A conferred cytopathicity to TERT-positive, but not TERT-negative, cells. In vivo replication of Adv-TERTp-E1A after local administration into a xenograft model of human hepatocellular carcinoma in nude mice was demonstrated by an increase in adenovirus titers in tumor extracts by several orders of magnitude between 6 h and 3 days postvector injection. Furthermore, significant inhibition of tumor growth with substantial necrotic tumor areas staining positively for adenovirus was observed with Adv-TERTp-E1A, but not with a control replication-deficient adenovirus. There was also the absence of hepatotoxicity in tumor-bearing animals after intratumoral delivery of the CRAD. The results indicate that the TERT promoter-driven CRAD is capable of tumor-selective replication and oncolysis in vitro and in vivo, and can be utilized as an adjuvant treatment agent for cancer.

Citing Articles

A Review of Telomere Attrition in Cancer and Aging: Current Molecular Insights and Future Therapeutic Approaches.

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Establishment of a Simple and Efficient Reverse Genetics System for Canine Adenoviruses Using Bacterial Artificial Chromosomes.

Matsugo H, Kobayashi-Kitamura T, Kamiki H, Ishida H, Takenaka-Uema A, Murakami S Viruses. 2020; 12(7).

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Tumor-targeting oncolytic virus elicits potent immunotherapeutic vaccine responses to tumor antigens.

Luo Y, Lin C, Zou Y, Ju F, Ren W, Lin Y Oncoimmunology. 2020; 9(1):1726168.

PMID: 32117591 PMC: 7028326. DOI: 10.1080/2162402X.2020.1726168.

A SIRPα-Fc fusion protein enhances the antitumor effect of oncolytic adenovirus against ovarian cancer.

Huang Y, Lv S, Liu P, Ye Z, Yang H, Li L Mol Oncol. 2020; 14(3):657-668.

PMID: 31899582 PMC: 7053234. DOI: 10.1002/1878-0261.12628.

Telomere Gene Therapy: Polarizing Therapeutic Goals for Treatment of Various Diseases.

Hong J, Yun C Cells. 2019; 8(5).

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