Identification of Subsets of Neuroblastomas by Combined Histopathologic and N-myc Analysis

Identification of Subsets of Neuroblastomas by Combined Histopathologic and N-myc Analysis

Background: Neuroblastomas show different histopathologic phenotypes, and the tumor cells can carry normal or multiple copies of the N-myc proto-oncogene (MYCN). Studies of the N-myc gene and histopathology of untreated primary neuroblastomas have demonstrated that both these factors are important i...

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Veröffentlicht in:JNCI : Journal of the National Cancer Institute 1995-10, Vol.87 (19), p.1470-1476
Hauptverfasser: Shimada, Hiroyuki, Stram, Daniel O., Chatten, Jane, Joshi, Vijay V., Hachitanda, Yoichi, Brodeur, Garrett M., Lukens, John N., Matthay, Katherine K., Seeger, Robert C.
Format: Artikel
Sprache:eng
Schlagworte:
Biological and medical sciences
Chi-Square Distribution
Child
Child, Preschool
Disease Progression
Gene Amplification
Genes
Genes, myc
Health risk assessment
Humans
Medical research
Medical sciences
Neoplasm Staging
Neuroblastoma - classification
Neuroblastoma - genetics
Neuroblastoma - pathology
Neurology
Pathology
Phenotype
Prognosis
Survival Analysis
Tumors
Tumors of the nervous system. Phacomatoses
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Zusammenfassung:Background: Neuroblastomas show different histopathologic phenotypes, and the tumor cells can carry normal or multiple copies of the N-myc proto-oncogene (MYCN). Studies of the N-myc gene and histopathology of untreated primary neuroblastomas have demonstrated that both these factors are important in risk assessment. Purpose: Our purpose was to determine if there are any associations between N-myc gene copy number, histopathologic features, clinical stage, and progression-free survival (PFS) and if joint analyses of histopathology and N-myc gene copy number improve risk assessment. Methods: The histopathologic phenotype and N-myc gene copy number were determined for 232 biopsy/surgery specimens obtained from untreated primary neuroblastoma patients. Tumors were classified as having favorable or unfavorable histology on the basis of Schwannian stroma (rich versus poor), neuroblastic differentiation (differentiating versus undifferentiated), and mitosis-karyorrhexis (fragmenting nucleus) index (MKI; high, intermediate, or low) in the context of age at diagnosis (Shimada classification). N-myc gene amplification was considered significant when the gene copy number was at least 10-fold higher than normal as determined by Southern blot analysis. Otherwise, tumors were classified as nonamplified for N-myc. Results: Among 19 stroma-rich tumors, 11 had grossly visible neuroblastic nodules, and two of these had N-myc amplification. Of 213 stroma-poor tumors, 51 had N-myc amplification, all of which were undifferentiated, and 45 (88% of 51) had high MKI. This histologic phenotype was present in less than 10% of tumors with nonamplified N-myc. Of 162 stroma-poor tumors that showed nonamplified N-myc, 45 (28%) were differentiating and 121 (75%) had low MKI. Neuroblastomas of clinical stages I, II, and IV-S nearly always had favorable histology and no amplification of N-myc. Stage III (regional) and particularly stage IV (metastatic) tumors, however, frequently had unfavorable histologic features with or without N-myc amplification. The estimated PFS at the end of 4 years after diagnosis was 83% for patients whose tumors had favorable histology and no N-myc amplification. The estimated PFS for the patients whose neuroblastomas had unfavorable histology, however, was 29% without and 13% with N-myc amplification, respectively. Subsets of patients with stage II, III, or IV disease were identified by both histologic evaluation and N-myc analysis. Multivariate Cox regressio
ISSN:0027-8874
1460-2105
DOI:10.1093/jnci/87.19.1470