Expression of mouse telomerase reverse transcriptase during development, differentiation and proliferation

Greenberg, Roger A.; Allsopp, Richard; Chin, Lynda; Morin, Gregg B.; DePinho, Ronald A.

doi:10.1038/sj.onc.1201933

Cited by 305 publications

(253 citation statements)

References 26 publications

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“…(b) Graph of mTERT and c-myc hybridization signals normalized to b-actin and 28S rRNA respectively, and plotted as a function of time of exposure to HMBA. Open circle, Myc56MEL; closed circle, MEL; solid line, mTERT; dotted line, c-myc; quantitation of expression=the relative ratio of TERT or myc signal to actin or 28S, respectively HMBA-exposure of parental MEL cultures was associated with a rapid 3 ± 4-fold decline in both cmyc and TERT mRNA levels by 4 h post-induction as reported previously (Greenberg et al, 1998). In contrast, c-myc and TERT expression in the HMBAtreated Myc56MEL cultures remained at pre-induction levels in two separate experiments.…”

Section: Coordinate Regulation Of C-myc and Tert Gene Expressionsupporting

confidence: 61%

“…Upon hexamethylene bisacetamide (HMBA) induction of MEL cell di erentiation, c-Myc and TERT exhibit highly regulated and strikingly similar patterns of gene expression (Lachman and Skoultchi, 1984;Greenberg et al, 1998). To examine more closely the relationship between c-Myc and TERT gene expression, we measured steady state c-myc and TERT mRNA levels following HMBA treatment in parental MEL cultures and in Myc56MEL cells, a well characterized MEL clonal derivative that constitutively expresses c-Myc (Dmitrovsky et al, 1986).…”

Section: Coordinate Regulation Of C-myc and Tert Gene Expressionmentioning

confidence: 99%

“…In addition, exposure of three di erent human leukemic cell lines to antisense c-myc oligonucleotides results in down-regulation of telomerase activity (Fujimoto and Takahashi, 1997); whereas Nmyc gene ampli®cation in neuroblastoma is associated with high telomerase activity (Hiyama et al, 1995). These observations, together with highly similar expression pro®les for mTERT and c-myc during mouse erythroleukemia (MEL) cell di erentiation and mitogen-stimulated lymphocyte proliferation (Greenberg et al, 1998;Lachman and Skoultchi, 1984;Reed et al, 1986), imply a potential link between increased Myc transactivation activity and up-regulation of TERT gene expression in normal proliferating and transformed cells. Indeed, recent evidence has shown that enforced expression of c-Myc in normal human ®broblasts or normal human mammary epithelial cells leads to increased expression of hTERT (Wang et al, 1998).…”

Section: Introductionmentioning

confidence: 95%

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Telomerase reverse transcriptase gene is a direct target of c-Myc but is not functionally equivalent in cellular transformation

et al. 1999

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Section: Coordinate Regulation Of C-myc and Tert Gene Expressionsupporting

confidence: 61%

Section: Coordinate Regulation Of C-myc and Tert Gene Expressionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 95%

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Telomerase reverse transcriptase gene is a direct target of c-Myc but is not functionally equivalent in cellular transformation

et al. 1999

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“…Alignment of the first 300 bp of the mTERT and hTERT promoter sequences reveals a number of conserved regions. 52 Relative to the A in the initiation codon, there is an Ebox at position À314 in the hTERT promoter and at À32 in the mouse promoter. In addition, there are two SP1-binding sites located at À168 and À134, which are highly conserved between mouse and human.…”

Section: Discussionmentioning

confidence: 99%

“…Unlike humans, in which the expression of hTERT is limited to a small number of normal tissues, 25 mTERT expression is widely expressed at low levels in many adult tissues. 52 Despite the difference in expression pattern, adenoviral vectors using the hTERT promoter to drive LacZ or HSV-thymidine kinase genes had undetectable transgene expression in the livers of mice, 28,30,33 suggesting that activity of the hTERT promoter is low in normal mouse liver. This was not attributable to the inability of the hTERT promoter to use the mouse transcriptional machinery, since LacZ expression was seen in the mouse lung carcinoma cell line M109.…”

Section: Discussionmentioning

confidence: 99%

Antitumor efficacy and tumor-selective replication with a single intravenous injection of OAS403, an oncolytic adenovirus dependent on two prevalent alterations in human cancer

et al. 2004

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A potentially promising treatment of metastatic cancer is the systemic delivery of oncolytic adenoviruses. This requires engineering viruses which selectively replicate in tumors. We have constructed such an oncolytic adenovirus, OAS403, in which two early region genes are under the control of tumor-selective promoters that play a role in two key pathways involved in tumorigenesis. The early region E1A is controlled by the promoter for the E2F-1 gene, a transcription factor that primarily upregulates genes for cell growth. The E4 region is under control of the promoter for human telomerase reverse transcriptase, a gene upregulated in most cancer cells. OAS403 was evaluated in vitro on a panel of human cells and found to elicit tumor-selective cell killing. Also, OAS403 was less toxic in human hepatocyte cultures, as well as in vivo when compared to an oncolytic virus that lacked selective E4 control. A single intravenous injection of 3 Â 10 12 vp/kg in a Hep3B xenograft mouse tumor model led to significant antitumor efficacy. Additionally, systemic administration in a pre-established LNCaP prostate tumor model resulted in over 80% complete tumor regressions at a tolerable dose. Vector genome copy number was measured in tumors and livers at various times following tail vein injection and showed a selective time-dependent increase in tumors but not livers over 29 days. Furthermore, efficacy was significantly improved when OAS403 treatment was combined with doxorubicin. This virus holds promise for the treatment of a broad range of human cancers including metastatic disease.

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Leben am Ende der Chromosomen: Telomere und Telomerase

Cech¹

2000

Angewandte Chemie

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An zellulären Alterungsprozessen und Krebs ist die Telomerase beteiligt, das Enzym, das die Enden linearer Chromosomen repliziert. Die molekularen Komponenten, die den katalytisch wirksamen Kern dieses Ribonucleoprotein‐Enzyms bilden (gezeigt ist ein Ausschnitt des aktiven Zentrums mit gebundenen Substraten), wurden kürzlich in einer Reihe von Organismen einschließlich des Menschen identifiziert. Damit sind für Chemiker die Voraussetzungen für die Entwicklung von Telomeraseinhibitoren geschaffen, die als Chemotherapeutika zur Behandlung von Krebs eingesetzt werden könnten.

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Expression of mouse telomerase reverse transcriptase during development, differentiation and proliferation

Cited by 305 publications

References 26 publications

Telomerase reverse transcriptase gene is a direct target of c-Myc but is not functionally equivalent in cellular transformation

Telomerase reverse transcriptase gene is a direct target of c-Myc but is not functionally equivalent in cellular transformation

Antitumor efficacy and tumor-selective replication with a single intravenous injection of OAS403, an oncolytic adenovirus dependent on two prevalent alterations in human cancer

Leben am Ende der Chromosomen: Telomere und Telomerase

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