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与神经母细胞瘤新治疗策略相关的预后标志物的不断演变的意义

Evolving significance of prognostic markers associated with new treatment strategies in neuroblastoma.

作者信息

Mora Jaume, Gerald William L, Cheung Nai-Kong V

机构信息

Department of Oncology, Hospital Sant Joan de Deu de Barcelona, Passeig de Sant Joan de Deu num 2, Barcelona 08950, Spain.

出版信息

Cancer Lett. 2003 Jul 18;197(1-2):119-24. doi: 10.1016/s0304-3835(03)00094-6.

Abstract

The striking differences in the natural history of clinical subgroups of neuroblastoma (NB), and the evolving therapeutic approaches for each, makes it imperative for prognostic markers to be reevaluated within individual clinical categories. At least one third of NB cases present without distant metastasis and cytotoxic therapy does not alter the natural history. We carried out a retrospective analysis of archived tumor samples. Fifty-seven of these patients had local-regional (LR) NB and were managed conservatively, initially treated with surgery alone. Among the biologic and clinical features analyzed including age, stage, histology, ploidy, MYCN, and 1p36, 1p22, 11q, 14q, 9p and 19q loss of heterozygosity (LOH) in multivariate analysis, diploidy was one of the most significant factors associated with progression-free survival and stage 4 progression. Clonal ploidy heterogeneity was common in LR NB. A predominant near-triploid clonal population was found in most cases of non-progressing LR NB tumors whereas progressing LR NB cases had a predominant diploid clone. We also reviewed the prognostic factors among 84 stage 4 NB cases treated with the N5, N6 or N7 protocols at MSKCC from 1987 to 1999. Traditional markers such as lactate dehydrogenase (LDH), ferritin, age and MYCN status were not prognostic in the univariate analysis. 11q23 and 1p22 LOH were correlated with better survival. These results highlight the evolving significance of prognostic analysis in homogeneous clinical groups undergoing similar treatments. To further characterize the gene expression profile between local-regional and metastatic NB, we carried out Microarray analysis of 41 NB tumors and 12 NB cell lines, using the Affymetrix Genechip Human Genome U95 Set. Distinct gene expression patterns between metastatic and non-metastatic NB tumors have been identified. Validation of these results and further mechanistic studies may shed new light on the biology of metastasis in human NB.

摘要

神经母细胞瘤(NB)临床亚组的自然病史存在显著差异,且针对各亚组的治疗方法也在不断演变,这使得有必要在各个临床类别中重新评估预后标志物。至少三分之一的NB病例在无远处转移的情况下发病,细胞毒性疗法并不会改变其自然病史。我们对存档的肿瘤样本进行了回顾性分析。其中57例患者患有局部区域(LR)NB,采用保守治疗,最初仅接受手术治疗。在分析的生物学和临床特征中,包括年龄、分期、组织学、倍性、MYCN以及1p36、1p22、11q、14q、9p和19q杂合性缺失(LOH),在多变量分析中,二倍体是与无进展生存期和4期进展相关的最重要因素之一。克隆倍性异质性在LR NB中很常见。在大多数无进展的LR NB肿瘤病例中发现了占主导地位的近三倍体克隆群体,而进展期LR NB病例则有一个占主导地位的二倍体克隆。我们还回顾了1987年至1999年在纪念斯隆凯特琳癌症中心(MSKCC)接受N5、N6或N7方案治疗的84例4期NB病例的预后因素。在单变量分析中,传统标志物如乳酸脱氢酶(LDH)、铁蛋白、年龄和MYCN状态并无预后价值。11q23和1p22 LOH与更好的生存率相关。这些结果凸显了在接受相似治疗的同质临床组中预后分析的不断演变的重要性。为了进一步表征局部区域NB和转移性NB之间的基因表达谱,我们使用Affymetrix Genechip Human Genome U95 Set对41例NB肿瘤和12例NB细胞系进行了微阵列分析。已确定转移性和非转移性NB肿瘤之间存在不同的基因表达模式。对这些结果的验证以及进一步的机制研究可能会为人类NB转移生物学提供新的见解。

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