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对局限性神经母细胞瘤患者和健康供体的骨髓和外周血样本进行多个靶分子监测。

Multiple target molecular monitoring of bone marrow and peripheral blood samples from patients with localized neuroblastoma and healthy donors.

机构信息

Laboratory of Oncology, Gaslini Institute, Genoa, Italy.

出版信息

Pediatr Blood Cancer. 2012 Jan;58(1):43-9. doi: 10.1002/pbc.22960. Epub 2011 Jan 19.

DOI:10.1002/pbc.22960
PMID:21254375
Abstract

BACKGROUND

Multiple target molecular monitoring of minimal residual disease in neuroblastoma (NB) patients may increase sensitivity and overcome tumor heterogeneity. However, multiple target analysis is costly and time consuming, thus improvement with respect to single target monitoring needs to be achieved.

PROCEDURES

Italian patients with localized NB were evaluated at diagnosis for TH, GD2-s, DDC, DCX, ELAV-4, STX, and Phox2b mRNA expressions. Patients with metastatic NB were tested as positive controls, together with NB primary tumors and cell lines, while healthy donors were tested as negative controls.

RESULTS

All NB-related markers but Phox2b were expressed in healthy donors, and in a high percentage of patients with localized NB without association with clinical events. The introduction of cut-off levels increased marker specificity, although the percentage of positive results was only slightly modified. While TH positivity in PB samples significantly associated with a worse prognosis, a paradox association was found for GD2-s mRNA expression. No correlation and agreement between quantitative and qualitative results obtained with the two assays were found. In the set of samples tested for all markers, no pattern of expression was found to be associated with a specific clinical situation.

CONCLUSION

These findings suggest that positive molecular results may not reflect the presence of disease, and that correlation among different markers is small in condition of low tumor burden. Thus, to reduce cost and amount of precious samples, in addition to TH, whose prognostic value was confirmed, only Phox2b warrants further evaluation in multi-center, prospective studies for high risk patients.

摘要

背景

神经母细胞瘤(NB)患者微小残留病的多靶点分子监测可能会提高敏感性并克服肿瘤异质性。然而,多靶点分析成本高且耗时,因此需要改进单靶点监测。

方法

意大利局部 NB 患者在诊断时评估 TH、GD2-s、DDC、DCX、ELAV-4、STX 和 Phox2b mRNA 表达。转移性 NB 患者作为阳性对照进行检测,同时检测 NB 原发肿瘤和细胞系,而健康供体作为阴性对照进行检测。

结果

所有 NB 相关标志物(Phox2b 除外)均在健康供体中表达,且在很大比例的局部 NB 患者中表达,与临床事件无关。引入截断值后增加了标志物的特异性,尽管阳性结果的百分比仅略有改变。虽然 PB 样本中的 TH 阳性与预后不良显著相关,但 GD2-s mRNA 表达存在矛盾关联。两种检测方法获得的定量和定性结果之间没有相关性和一致性。在测试所有标志物的样本集中,没有发现任何表达模式与特定的临床情况相关。

结论

这些发现表明,阳性分子结果可能并不能反映疾病的存在,而且在肿瘤负荷较低的情况下,不同标志物之间的相关性较小。因此,为了降低成本和珍贵样本的数量,除了 TH(其预后价值已得到证实)外,仅 Phox2b 需要在多中心前瞻性研究中进一步评估高危患者。

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