Differential expression of N-myc in phenotypically distinct subclones of a human neuroblastoma cell line

Differential expression of N-myc in phenotypically distinct subclones of a human neuroblastoma cell line

Neuroblastomas are malignant childhood neoplasms that arise from derivatives of the neural crest. We report the characterization of a new neuroblastoma cell line, designated NBL-W, derived from the primary tumor of a patient with stage IVS disease (S. L. Cohn, C. V. Herst, H. S. Maurer, and S. T. Ro...

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Veröffentlicht in:Cancer research (Chicago, Ill.) Ill.), 1991-12, Vol.51 (23), p.6338-6345
Hauptverfasser: FOLEY, J, COHN, S. L, SALWEN, H. R, CHAGNOVICH, D, COWAN, J, MASON, K. L, PARYSEK, L. M
Format: Artikel
Sprache:eng
Schlagworte:
Biological and medical sciences
Cell Differentiation - drug effects
Gene Expression Regulation, Neoplastic - genetics
Genes, myc - genetics
Humans
Intermediate Filaments - chemistry
Karyotyping
Medical sciences
Nerve Growth Factors
Neural Crest - enzymology
Neuroblastoma - chemistry
Neuroblastoma - genetics
Neuroblastoma - pathology
Neurology
Phenotype
RNA, Messenger - analysis
RNA, Neoplasm - analysis
Tretinoin
Tumor Cells, Cultured - chemistry
Tumor Cells, Cultured - pathology
Tumors of the nervous system. Phacomatoses
Vimentin - analysis
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Zusammenfassung:Neuroblastomas are malignant childhood neoplasms that arise from derivatives of the neural crest. We report the characterization of a new neuroblastoma cell line, designated NBL-W, derived from the primary tumor of a patient with stage IVS disease (S. L. Cohn, C. V. Herst, H. S. Maurer, and S. T. Rosen, J. Clin. Oncol., 5: 1441-1444, 1987) according to the criteria of Evans [A. E. Evans, G. J. D'Angio, and J. Randolf, Cancer (Phila.), 27: 374-378, 1971]. Neurite-bearing (N) and substrate-adherent (S) cell lines have been subcloned from the parent line. N and S cells can interconvert, and both cell types label with the neural crest cell surface marker antibody, HNK-1. Cells in the subcloned lines and in the parent line have been shown by Southern blot analysis to contain approximately 100 copies of the N-myc gene. Cytogenetic analysis shows a homogeneously staining region present on chromosome 19. Although these subclones are of identical genotype, the S cells express lower amounts of N-myc mRNA and protein as compared to the N cells. N cells express several neuronal proteins including the neurotransmitter-processing enzymes tyrosine hydroxylase and dopamine beta-hydroxylase, the neuronal intermediate filament proteins peripherin and NF66/alpha-internexin, and the neural cell adhesion molecule. S cells generally lack neuronal markers but express the mesenchymal intermediate filament protein vimentin, and a small subset of the S cells express glial fibrillary acidic protein. Some S cells were labeled weakly with neural cell adhesion molecule antibody; others were negative. S cells did not express the glial marker S-100 or a melanocyte marker, tyrosinase. Thus, S cells express the neural crest marker HNK-1 but do not express a set of antigens characteristic of any known cell type derived from the neural crest. These results are consistent with the suggestion that differential N-myc expression may be involved in the interconversion of N and S cells but indicate that the S cell phenotype need not represent a highly differentiated neural crest derivative.
ISSN:0008-5472
1538-7445