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Query: UMLS:C0001486 (
Adenovirus
)
3,125
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Adenovirus
serotype 5 (Ad5) is frequently used as an effective vector for induction of therapeutic transgenes in cancer gene therapy or of tumor cell lysis in oncolytic virotherapy. Ad5 can infect target cells through binding with the coxsackie and adenovirus receptor (CAR). Thus, the infectious ability of Ad5-based vectors depends on the CAR expression level in target cells. There are conventional methods to evaluate the CAR expression level in human target cells, including flow cytometry, western blotting and immunohistochemistry. Here, we show a simple system for detection and assessment of functional CAR expression in human tumor cells, using the green fluorescent protein (GFP)-expressing telomerase-specific replication-competent adenovirus
OBP
-401.
OBP
-401 infection induced detectable GFP expression in CAR-expressing tumor cells, but not in CAR-negative tumor cells, nor in CAR-positive normal fibroblasts, 24 h after infection.
OBP
-401-mediated GFP expression was significantly associated with CAR expression in tumor cells.
OBP
-401 infection detected tumor cells with low CAR expression more efficiently than conventional methods.
OBP
-401 also distinguished CAR-positive tumor tissues from CAR-negative tumor and normal tissues in biopsy samples. These results suggest that GFP-expressing telomerase-specific replication-competent adenovirus is a very potent diagnostic tool for assessment of functional CAR expression in tumor cells for Ad5-based antitumor therapy.
...
PMID:A simple detection system for adenovirus receptor expression using a telomerase-specific replication-competent adenovirus. 2224 Nov 76
Oncolytic viruses engineered to replicate in tumour cells but not in normal cells could be used as tumour-specific vectors carrying the therapeutic genes. We previously developed a telomerase-specific oncolytic adenovirus,
OBP
-301, that causes cell death in human cancer cells with telomerase activities. Here, we further modified
OBP
-301 to express the wild-type p53 tumour suppressor gene (
OBP
-702), and investigated whether
OBP
-702 induces stronger antitumour activity than
OBP
-301. The antitumour effect of
OBP
-702 was compared to that of
OBP
-301 on
OBP
-301-sensitive (H358 and H460) and
OBP
-301-resistant (T.Tn and HSC4) human cancer cells.
OBP
-702 suppressed the viability of both
OBP
-301-sensitive and
OBP
-301-resistant cancer cells more efficiently than
OBP
-301.
OBP
-702 caused increased apoptosis compared to
OBP
-301 or a replication-deficient adenovirus expressing the p53 gene (Ad-p53) in H358 and T.Tn cells.
Adenovirus
E1A-mediated p21 and MDM2 downregulation was involved in the apoptosis caused by
OBP
-702. Moreover,
OBP
-702 significantly suppressed tumour growth in subcutaneous tumour xenograft models compared to monotherapy with
OBP
-301 or Ad-p53. Our data demonstrated that
OBP
-702 infection expressed adenovirus E1A and then inhibited p21 and MDM2 expression, which in turn efficiently induced apoptotic cell death. This novel apoptotic mechanism suggests that the p53-expressing
OBP
-702 is a promising antitumour reagent for human cancer and could improve the clinical outcome.
...
PMID:A novel apoptotic mechanism of genetically engineered adenovirus-mediated tumour-specific p53 overexpression through E1A-dependent p21 and MDM2 suppression. 2224 27
We evaluated the antitumor effect of a telomerase-specific replication-selective adenovirus (Telomelysin,
OBP
-301) for adenoid cystic carcinoma (ACC) in vitro and in vivo.
Adenovirus
E1 gene expression was controlled by human telomerase reverse transcription (hTERT). Infection of ACC cells by
OBP
-301 induced high E1A mRNA expression and subsequent oncolytic cell death in a dose-dependent manner. Using
OBP
-401 (TelomeScan), a genetically engineered adenovirus that carries the GFP gene under the control of the cytomegalovirus (CMV) promoter at the deleted E3 region of
OBP
-301, ACC cells expressed bright GFP fluorescence as early as 12 h after
OBP
-401 infection. The fluorescence intensity gradually increased in a time-dependent manner, followed by rapid cell death due to the cytopathic effect of
OBP
-401, as evidenced by the floating, highly light-refractive cells using phase-contrast microscopy. Effects of intratumorally injected
OBP
-401 against established Acc2 xenograft tumors were seen in BALB/c nu/nu mice. The levels of GFP expression following ex vivo infection of
OBP
-401 may be of value as a positive predictive marker for the outcome of telomerase-specific virotherapy. Our data clearly indicated that telomerase-specific oncolytic adenoviruses have significant therapeutic potential against human ACC in vitro and in vivo. These results suggest that treatment with
OBP
-301 and
OBP
-401 may improve the quality of life of oral cancer patients.
...
PMID:Antitumor effects of telomerase-specific replication-selective oncolytic viruses for adenoid cystic carcinoma cell lines. 2406 18
Adenovirus
serotype 5 (Ad5) is widely and frequently used as a virus vector in cancer gene therapy and oncolytic virotherapy. Oncolytic virotherapy is a novel antitumor treatment for inducing lytic cell death in tumor cells without affecting normal cells. Based on the Ad5 genome, we have generated three types of telomerase-specific replication-competent oncolytic adenoviruses:
OBP
-301 (Telomelysin), green fluorescent protein (GFP)-expressing
OBP
-401 (TelomeScan), and tumor suppressor
p53
-armed
OBP
-702. These viruses drive the expression of the adenoviral
E1A
and
E1B
genes under the control of the
hTERT
(human telomerase reverse transcriptase-encoding gene) promoter, providing tumor-specific virus replication. This review focuses on the therapeutic potential of three
hTERT
promoter-driven oncolytic adenoviruses against bone and soft-tissue sarcoma cells with telomerase activity.
OBP
-301 induces the antitumor effect in monotherapy or combination therapy with chemotherapeutic drugs via induction of autophagy and apoptosis.
OBP
-401 enables visualization of sarcoma cells within normal tissues by serving as a tumor-specific labeling reagent for fluorescence-guided surgery via induction of GFP expression.
OBP
-702 exhibits a profound antitumor effect in
OBP
-301-resistant sarcoma cells via activation of the p53 signaling pathway. Taken together, telomerase-specific oncolytic adenoviruses are promising antitumor reagents that are expected to provide novel therapeutic options for the treatment of bone and soft-tissue sarcomas.
...
PMID:Bone and Soft-Tissue Sarcoma: A New Target for Telomerase-Specific Oncolytic Virotherapy. 3208 83
