<i>Increased Expression of N</i>-myc <i>in Human Small Cell Lung Cancer Biopsies Predicts Lack of Response to Chemotherapy and Poor Prognosis</i>

Funa, Keiko; Steinholtz, Lena; E, Nõu; Bergh, Jonas

doi:10.1093/ajcp/88.2.216

Cited by 94 publications

(26 citation statements)

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“…In addition to the infrequent L-MYC ampli®cation in SCLC discussed above, both C-MYC and N-MYC ampli®cation and overexpression have also been observed (Little et al, 1983;Saksela et al, 1984;Nau et al, 1986;Funa et al, 1987;Johnson et al, 1987Johnson et al, , 1992Gu et al, 1988;Takahashi et al, 1989;Noguchi et al, 1990;Makela et al, 1992;Rygaard et al, 1993). The frequency of ampli®cation/overexpression for either gene has generally ranged from 2 ± 30% of all tumors, xenografts or cell lines and the extent of ampli®cation has ranged from 5 ± 4100-fold.…”

Section: Small Cell Lung Cancer (Sclc)mentioning

confidence: 96%

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: Small Cell Lung Cancer (Sclc)mentioning

confidence: 96%

MYC oncogenes and human neoplastic disease

1999

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“…DNA amplification of N-myc occurs in a subset of rhabdomyosarcoma, a pediatric soft-tissue sarcoma, and is predominantly found in the alveolar subset and rarely in the more common embryonal subtype (30), although N-myc mRNA and protein expression is found in the vast majority of all rhabdomyosarcoma cases regardless of histology (31). N-myc is amplified in 15% to 20% of small-cell lung cancers (32,33) and is associated with poor response to chemotherapy, rapid tumor growth, and shorter survival (34). N-myc amplification rarely occurs in other lung cancer histologies.…”

Section: N-myc and Human Cancermentioning

confidence: 99%

The N-myc Oncogene: Maximizing its Targets, Regulation, and Therapeutic Potential

Beltran

2014

Molecular Cancer Research

124

116

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N-myc (MYCN), a member of the Myc family of basic-helix-loop-helix-zipper (bHLHZ) transcription factors, is a central regulator of many vital cellular processes. As such, N-myc is well recognized for its classic oncogenic activity and association with human neuroblastoma. Amplification and overexpression of N-myc has been described in other tumor types, particularly those of neural origin and neuroendocrine tumors. This review outlines N-myc's contribution to normal development and oncogenic progression. In addition, it highlights relevant transcriptional targets and mechanisms of regulation. Finally, the clinical implications of N-Myc as a biomarker and potential as a target using novel therapeutic approaches are discussed. Mol Cancer Res; 12(6); 815-22. Ó2014 AACR. IntroductionThe N-myc gene was first reported in 1983, when Schwab and colleagues (1) and Kohl and colleagues (2) discovered that there were a subset of human neuroblastoma cell lines harboring multiple copies of a DNA sequence related to the C-myc oncogene (MYC), and this region was designated Nmyc (MYCN). Genomic amplification of N-myc resulted in overexpression of N-myc at the mRNA level, and rat embryo cells transfected with N-myc demonstrated oncogenic properties. These findings were first to bring attention to N-myc as a putative oncogene.

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“…Initially 661 bp PstI fragment of bovine 0-PPT cDNA (15) containing the sequence from exon 3 to 6 was subcloned into transcription vector Riboprobe Gemini (Promega). RNA probe was transcribed by using SP 6 RNA polymerase and '3-UTP as previously described (17). ISH on carcinoid tumor tissue was performed as previously described ( 17) using the probe with high specific activity at 5-9 x lo8 cpm/pg.…”

Section: Application Of Ish In Detection Of Peptide and Hormone Mrnamentioning

confidence: 99%

“…RNA probe was transcribed by using SP 6 RNA polymerase and '3-UTP as previously described (17). ISH on carcinoid tumor tissue was performed as previously described ( 17) using the probe with high specific activity at 5-9 x lo8 cpm/pg. Strong hybridization signals on the tumor cells was obtained with lo6 cpm/section (Fig.…”

Section: Application Of Ish In Detection Of Peptide and Hormone Mrnamentioning

confidence: 99%

IN Situ Hybridization for Detection OF Hormone and Peptide mRNA in Carcinoid Tumors

Funa

1991

Acta Oncologica

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Increased Expression of N-myc in Human Small Cell Lung Cancer Biopsies Predicts Lack of Response to Chemotherapy and Poor Prognosis

Cited by 94 publications

References 0 publications

MYC oncogenes and human neoplastic disease

MYC oncogenes and human neoplastic disease

The N-myc Oncogene: Maximizing its Targets, Regulation, and Therapeutic Potential

IN Situ Hybridization for Detection OF Hormone and Peptide mRNA in Carcinoid Tumors

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