The ornithine decarboxylase gene is a transcriptional target of c-Myc.

Bello-Fernández, Concha; Packham, Graham; Cleveland, John L.

doi:10.1073/pnas.90.16.7804

Cited by 670 publications

(527 citation statements)

References 20 publications

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“…Because very few in situ DNA binding sites for any of these proteins have been characterized (Grandori et al, 1996) and because the E-boxes of acknowledged cmyc transcriptional targets have not been examined for binding by N-myc and L-myc, it is not yet completely clear how in vitro binding site preferences might be related to those favored in vivo. Recent results have shown that L-myc is incapable of activating the ornithine decarboxylase (ODC) promoter (HL Zhang and EVP, unpublished observations), a generally accepted c-myc-responsive target (Bello-Fernandez et al, 1993). This could be explained by preferential DNA binding, by di erential requirements for transcriptional co-activators, or by di erences in strengths of the myc protein transcriptional activation domains (TADs) (Barrett et al, 1992).…”

Section: Erential E Ects Of Myc Proteins On Dna Binding Transcripmentioning

confidence: 99%

“…Others, however, have not observed such an e ect (Henriksson et al, 1993;Lutterbach and Hann, 1994). Under conditions that may be more physiological, we have stably expressed a double Thr 58 /Ser 62 ?Ala c-myc mutant and measured levels of ornithine decarboxylase (ODC), an enzyme whose gene is generally accepted as being c-myc inducible (Bello-Fernandez et al, 1993). We have observed that this mutant cannot up-regulate endogenous ODC enzyme activity whereas wild-type c-myc does so by fourfold (CEN and EVP, unpublished).…”

Section: Burkitt's Lymphoma (Bl)mentioning

confidence: 99%

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MYC oncogenes and human neoplastic disease

1999

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c-myc, N-myc and L-myc are the three members of the myc oncoprotein family whose role in the pathogenesis of many human neoplastic diseases has received wide empirical support. In this review, we ®rst summarize data, derived mainly from non-clinical studies, indicating that these oncoproteins actually serve quite di erent roles in vivo. This concept necessarily lies at the heart of the basis for the observation that the deregulated expression of each MYC gene is reproducibly associated with only certain naturally occurring malignancies in humans and that these genes are not interchangeable with respect to their aberrant functional consequences. We also review evidence implicating each of the above MYC genes in speci®c neoplastic diseases and have attempted to identify unresolved questions which deserve further basic or clinical investigation. We have made every attempt to review those diseases for which signi®cant and con®rmatory evidence, based on studies with primary tumor material, exists to implicate MYC members in their causation and/or progression.

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Section: Erential E Ects Of Myc Proteins On Dna Binding Transcripmentioning

confidence: 99%

Section: Burkitt's Lymphoma (Bl)mentioning

confidence: 99%

MYC oncogenes and human neoplastic disease

1999

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“…c-Myc has been demonstrated to enhance transcription of a number of direct target genes including aprothymosin , ornithine decarboxylase (Bello-Fernandez et al, 1993;Wagner et al, 1993), cdc25A (Galaktionov et al, 1996), and MrDb (Grandori et al, 1996). In addition, c-Myc has been demonstrated to repress transcription of the growth arrest genes gas1 (Lee et al, 1997) and gadd45 (Marhin et al, 1997).…”

Section: Introductionmentioning

confidence: 99%

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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“…As another possibility, the transcriptional targets of c-Myc might be regulated by Pim-1 kinase, since c-Myc is considered to induce apoptosis by activating the transcription of its target genes (Henriksson and LuÈ scher, 1996). To date, ECA39 (Benvenisty et al, 1992), ornithine decarboxylase (ODC) (Bello-Fernandez et al, 1993), p53 (Reisman et al, 1993), a-prothymosin (Gaubatz et al, 1994), cad (Miltenberger et al, 1995), and Cdc25A (Galaktionov et al, 1996) have been shown to be the genes transcriptionally activated by c-Myc. Among them, Cdc25A cell-cycle phosphatase has only recently been recognized as a candidate mediator molecule of c-Mycmediated apoptosis.…”

Section: Discussionmentioning

confidence: 99%

Pim-1 kinase stimulates c-Myc-mediated death signaling upstream of caspase-3 (CPP32)-like protease activation

Mochizuki¹,

Kitanaka²,

Noguchi³

et al. 1997

Oncogene

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Pim-1 oncoprotein is a serine/threonine kinase that can closely cooperate with c-Myc in lymphomagenesis, as does Bcl-2. Although the molecular mechanism of this cooperative transformation remains unknown, it is speculated that, similar to Bcl-2, Pim-1 contributes to transformation by inhibiting apoptosis. In this study, therefore, we examined the e ect of Pim-1 expression on c-Myc-mediated apoptosis of Rat-1 ®broblasts triggered by serum deprivation. Our results showed that, rather than inhibiting apoptosis, Pim-1 expression stimulated cMyc-mediated apoptosis in Rat-1 ®broblasts. Pim-1 stimulated c-Myc-mediated apoptosis through an enhancement of the c-Myc-mediated activation of caspase-3 (CPP32)-like proteases, since the suppression of this activity by a speci®c caspase inhibitor abolished the apoptosis stimulation by Pim-1. A kinase-defective Pim-1 mutant failed to stimulate c-Myc-mediated apoptosis, and Pim-1 expression alone in the absence of c-Myc overexpression did not induce apoptosis of serumdeprived Rat-1 cells, indicating that the kinase activity of Pim-1 and the activated c-Myc signaling pathway were required for apoptosis stimulation by Pim-1. Together, these results suggest that Pim-1 oncoprotein stimulates as a serine/threonine kinase the death signaling elicited by c-Myc at a step upstream of caspase-3-like protease activation in Rat-1 ®broblasts. Our results also suggest that Pim-1 kinase might function cooperatively with c-Myc through the phosphorylation of a factor(s) which regulates the common signaling pathway involved in c-Myc-mediated apoptosis and transformation.

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The ornithine decarboxylase gene is a transcriptional target of c-Myc.

Cited by 670 publications

References 20 publications

MYC oncogenes and human neoplastic disease

MYC oncogenes and human neoplastic disease

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

Pim-1 kinase stimulates c-Myc-mediated death signaling upstream of caspase-3 (CPP32)-like protease activation

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