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短端粒:尤因肉瘤复发的一种新型潜在预测指标。

Short telomeres: a novel potential predictor of relapse in Ewing sarcoma.

作者信息

Avigad Smadar, Naumov Inna, Ohali Anat, Jeison Marta, Berco Gili Halevy, Mardoukh Jacques, Stark Batia, Ash Shifra, Cohen Ian J, Meller Isaac, Kollender Yehuda, Issakov Josephine, Yaniv Isaac

机构信息

Molecular Oncology, Felsenstein Medical Research Center, Petach Tikva, Israel.

出版信息

Clin Cancer Res. 2007 Oct 1;13(19):5777-83. doi: 10.1158/1078-0432.CCR-07-0308.

Abstract

PURPOSE

Despite advances in therapy, >50% of patients with Ewing sarcoma will relapse. The current prognostic factors are not optimal for risk prediction. Studies have shown that telomere length could predict outcome in different malignancies. Our aim was to evaluate whether telomere length could be a better prognostic factor in Ewing sarcoma and correlate the results with clinical variables, outcome, and chromosomal instability.

EXPERIMENTAL DESIGN

Telomere length was determined in the primary tumor and peripheral blood of 32 patients with Ewing sarcoma. Chromosomal instability was evaluated by combining classical cytogenetics, comparative genomic hybridization and random aneuploidy. Telomere length was correlated to clinical variables, chromosomal instability, and outcome.

RESULTS

In 75% of the tumors, changes in telomere length, when compared with the corresponding peripheral blood lymphocytes, were noted. The majority of changes consisted of a reduction in telomere length. Patients harboring shorter telomeres had a significantly adverse outcome (P = 0.015). Chromosomal instability was identified in 65% of tumors, significantly correlating with short telomeres (P = 0.0094). Using multivariate analysis, telomere length remained the only significant prognostic variable (P = 0.034). Patients with short telomeres had a 5.3-fold risk of relapse as compared to those with unchanged or longer telomeres.

CONCLUSION

We have shown that tumors with telomere length reduction result in genomic instability. In addition, telomere length reduction was the only significant predictor of outcome. We suggest that reduction of telomere length in tumor cells at diagnosis could serve as a prognostic marker in Ewing sarcoma.

摘要

目的

尽管治疗取得了进展,但超过50%的尤因肉瘤患者会复发。目前的预后因素在风险预测方面并不理想。研究表明,端粒长度可预测不同恶性肿瘤的预后。我们的目的是评估端粒长度是否可能是尤因肉瘤中更好的预后因素,并将结果与临床变量、预后和染色体不稳定性相关联。

实验设计

测定了32例尤因肉瘤患者原发肿瘤和外周血中的端粒长度。通过结合经典细胞遗传学、比较基因组杂交和随机非整倍体分析评估染色体不稳定性。将端粒长度与临床变量、染色体不稳定性和预后相关联。

结果

在75%的肿瘤中,观察到与相应外周血淋巴细胞相比端粒长度的变化。大多数变化包括端粒长度的缩短。端粒较短的患者预后明显较差(P = 0.015)。在65%的肿瘤中发现了染色体不稳定性,与短端粒显著相关(P = 0.0094)。使用多变量分析,端粒长度仍然是唯一显著的预后变量(P = 0.034)。与端粒长度不变或较长的患者相比,端粒较短的患者复发风险高5.3倍。

结论

我们已经表明,端粒长度缩短的肿瘤会导致基因组不稳定。此外,端粒长度缩短是唯一显著的预后预测指标。我们建议,诊断时肿瘤细胞中端粒长度的缩短可作为尤因肉瘤的预后标志物。

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