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Unfavorable DNA ploidy and Ha-ras p21 findings in neuroblastomas detected through mass screening

Authors :
Kusafuka, Takeshi
Nagahara, Noboru
Oue, Takaharu
Imura, Kenji
Nakamura, Tetsuro
Kobayashi, Yasutsugu
Komoto, Yosuke
Fukuzawa, Masahiro
Okada, Akira
Nakayama, Masahiro
Source :
Cancer. August 15, 1995, Vol. 76 Issue 4, p695, 5 p.
Publication Year :
1995

Abstract

Background. Urinary mass screening has been available for 6-month-old infants throughout Japan since 1985. It is still controversial as to whether the program contributes to the detection of unfavorable neuroblastomas destined to present clinically when a patient reaches an older age. DNA diploidy and tetraploidy, low expression of Ha-ras p21, and an amplified N-myc gene status relate to an unfavorable prognosis. The authors examined these biologic indicators in neuroblastomas detected by urinary mass screening. Patients and Methods. Seventy-eight neuroblastomas detected by mass screening were studied for DNA ploidy using DNA flow cytometry, Ha-ras p21 expression using immunostaining, and N-myc gene copy number using slot-blot or Southern blot hybridization methods. Results. Of 73 tumors with analyzable DNA flow cytometric results, 18 (24.7%) had diploidy (n = 7) or tetraploidy (n = 11). Twenty-eight (40.0%) of 70 tumors examined showed low-to-absent expression of Ha-ras p21. DNA diploid and tetraploid status correlated significantly with the low-to-absent expression of Ha-ras p21 (P = 0.00021). Fourteen (20.0%) of the 70 patients had both of these two unfavorable prognostic markers. N-myc amplification was not detected in 41 of 41 tumors studied. All 78 patients were alive 8-92 months after completion of treatment. Conclusions. At least 20.0% of neuroblastomas detected by mass screening have unfavorable biologic prognostic markers. These patients may benefit from early detection and immediate treatment. However, the biologic features associated with a poor prognosis are not predictive of poor outcome in individual patients, and, therefore, should not be used to justify more intensive therapies. Cancer 1995; 76:695-9. Key words: neuroblastoma, mass screening, DNA ploidy, Ha-ras p21, N-myc.

Details

ISSN :
0008543X
Volume :
76
Issue :
4
Database :
Gale General OneFile
Journal :
Cancer
Publication Type :
Periodical
Accession number :
edsgcl.17290011