Deletions in Chromosome Arms 3p and 11q Are New Prognostic Markers in Localized and 4s Neuroblastoma

Overview

Journal Clin Cancer Res

Specialty Oncology

Date 2003 Jan 23

PMID 12538451

Citations 39

Authors

Ruediger Spitz

Barbara Hero

Karen Ernestus

Frank Berthold

Affiliations

Soon will be listed here.

Abstract

Purpose: To find new nonrandom chromosomal changes in neuroblastoma (NB) with a potential to forecast the patient's outcome, alterations in chromosome arms 3p and 11q were investigated.

Experimental Design: Frequency and prognostic potential of 3p and 11q alterations in 144 NBs were analyzed using interphase fluorescence in situ hybridization with DNA probes for 3p26 and 11q23. Aberrations were defined as deletion (monosomy of a specific region) or imbalance (at least two intact and additional 3p26- or 11q23-deleted chromosomes).

Results: Forty-two of 144 cases (29%) displayed 11q alterations (21% deletions, 8% imbalances). Most aberrations were associated with stage 4 disease (28 of 59, 47%) but were also present in localized and 4s tumors (14 of 85, 16%; P = 0.007). Patients with 11q deletion/imbalance were significantly older at diagnosis (P < 0.001). Changes in 3p were detected in 26 of 144 (18%) samples (15% deletions, 3% imbalances). These alterations were also associated with stage 4 [20 of 59 (34%) versus 6 of 85 (7%) in stages 1-3 and 4s, P = 0.007], and the median age was increased (P < 0.001). Aberrations in both chromosomes were highly associated with each other (P < 0.001). MYCN amplification (MNA) was detected in 10% and 12% of tumors with 11q and 3p alterations, and changes in 1p36 occurred in 13% and 26% of the 3p- and 11q-aberrant tumors. MYCN amplification and 11q deletion/imbalance tended to show an inverse correlation (P = 0.07) as well as 1p and 3p deletion/imbalance (P = 0.07). Patients with 3p and 11q abnormalities in localized/4s tumors showed an inferior outcome compared with those without these alterations (P = 0.002 and P = 0.0027, respectively), in particular in MYCN single copy tumors (P < 0.0001 and P = 0.0006, respectively).

Conclusion: Alterations in 3p and 11q are frequent nonrandom aberrations in NB and define a new high-risk subgroup in MYCN single copy stage 1-3 and 4s disease.

Citing Articles

Clinical Response to a PARP Inhibitor and Chemotherapy in a Child with BARD1-Mutated Refractory Neuroblastoma: A Case Report.

Cupit-Link M, Hagiwara K, Zhang J, Federico S Res Sq. 2023; .

PMID: 37645774 PMC: 10462232. DOI: 10.21203/rs.3.rs-3250117/v1.

IGF2BP1 induces neuroblastoma via a druggable feedforward loop with MYCN promoting 17q oncogene expression.

Hagemann S, Misiak D, Bell J, Fuchs T, Lederer M, Bley N Mol Cancer. 2023; 22(1):88.

PMID: 37246217 PMC: 10226260. DOI: 10.1186/s12943-023-01792-0.

Mitochondria-associated gene expression perturbation predicts clinical outcomes and shows potential for targeted therapy in neuroblastoma.

Chai C, Chen Y, Luo Y, Zhang H, Ye Z, He X Front Pediatr. 2023; 11:1094926.

PMID: 37025299 PMC: 10070980. DOI: 10.3389/fped.2023.1094926.

MYCN mRNA degradation and cancer suppression by a selective small-molecule inhibitor in MYCN-amplified neuroblastoma.

Liu T, Gu L, Wu Z, Albadari N, Li W, Zhou M Front Oncol. 2022; 12:1058726.

PMID: 36505784 PMC: 9730801. DOI: 10.3389/fonc.2022.1058726.

Impact of 11q Loss of Heterozygosity Status on the Response of High-Risk Neuroblastoma With MYCN Amplification to Neoadjuvant Chemotherapy.

Lu X, Qu L, Duan X, Zuo W, Sai K, Rui G Front Pediatr. 2022; 10:898918.

PMID: 35757140 PMC: 9226623. DOI: 10.3389/fped.2022.898918.