首页> 外文期刊>JAMA: the Journal of the American Medical Association >Association of telomere length of peripheral blood leukocytes with hematopoietic relapse, malignant transformation, and survival in severe aplastic anemia.
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Association of telomere length of peripheral blood leukocytes with hematopoietic relapse, malignant transformation, and survival in severe aplastic anemia.

机译:造血复发,恶性转化和严重血栓性贫血中的恶性转化和存活的外周血白细胞的端粒长度。

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CONTEXT: Critically short telomeres produce apoptosis, cell senescence, and chromosomal instability in tissue culture and animal models. Variations in telomere length have been reported in severe aplastic anemia but their clinical significance is unknown. OBJECTIVE: To investigate the relationship between telomere length and clinical outcomes in severe aplastic anemia. DESIGN, SETTING, AND PATIENTS: Single institution analysis of 183 patients with severe aplastic anemia who were treated in sequential prospective protocols at the National Institutes of Health from 2000 to 2008. The pretreatment leukocyte age-adjusted telomere length of patients with severe aplastic anemia consecutively enrolled in immunosuppression protocols with antithymocyte globulin plus cyclosporine for correlation with clinical outcomes were analyzed. MAIN OUTCOME MEASURES: Hematologic response, relapse, clonal evolution, and survival. RESULTS: There was no relationship between hematologic response and telomere length with response rates of 56.5% of 46 patients in the first, 54.3% of 46 in the second, 60% of 45 in the third, and 56.5% of 46 in the fourth quartiles. Multivariate analysis demonstrated that telomere length was associated with relapse, clonal evolution, and mortality. Evaluated as a continuous variable, telomere length inversely correlated with the probability of hematologic relapse (hazard ratio [HR], 0.16; 95% confidence interval [CI], 0.03-0.69; P = .01). The probability of clonal evolution was higher in patients in the first quartile (24.5%; 95% CI, 8.7%-37.5%) than in quartiles 2 through 4 (8.4%; 95% CI, 3.2%-13.3%; P = .009), and evolution to monosomy 7 or complex cytogenetics was more common in the first quartile (18.8%; 95% CI, 3.5%-31.6%) than in quartiles 2 through 4 (4.5%; 95% CI, 0.5%-8.2%; P = .002). Survival between these 2 groups differed, with 66% (95% CI, 52.9%-82.5%) surviving 6 years in the first quartile compared with 83.8% (95% CI, 77.3%-90.9%) in quartiles 2 through 4 (P = .008). CONCLUSION: In a cohort of patients with severe aplastic anemia receiving immunosuppressive therapy, telomere length was unrelated to response but was associated with risk of relapse, clonal evolution, and overall survival.
机译:背景:批判性短端粒产生凋亡,细胞衰老和组织培养和动物模型中的染色体不稳定性。在严重的血栓性贫血中报道了端粒长度的变化,但它们的临床意义是未知的。目的:探讨严重血栓性贫血中端粒长度与临床结果的关系。设计,设定和患者:2000年至2008年国家卫生研究院持续预期障碍患者的单一机构分析。2000年至2008年的序贯审理课程。连续增殖贫血患者的预处理白细胞年龄调整后长度分析了患有Antithymocyte球蛋白加环孢菌素的免疫抑制方案分析了与临床结果相关的免疫抑制方案。主要观察指标:血液学反应,复发,克隆演化和生存。结果:血液学反应和端粒长度之间没有关系,反应率为46例患者的响应率为46例,占46例的54.3%,第三个中的60%占45%,第四个四分位数的56.5%占46%的56.5% 。多变量分析表明,端粒长度与复发,克隆演化和死亡率有关。作为连续变量评估,端粒长度与血液学复发概率(危险比[HR],0.16; 95%置信区间[CI],0.03-0.69; P = .01)相反。在第一个四分位数(24.5%; 95%CI,8.7%-37.5%)中克隆演化的概率高于四分位数2至4(8.4%; 95%CI,3.2%-13.3%; P =。 009),并在第一个四分位数(18.8%; 95%CI,3.5%-31.6%)中比四分位数2至4(4.5%; 95%CI,0.5%-8.2)更常见的009或复杂细胞遗传学的进化更常见%; p = .002)。这些2组之间的存活率不同,66%(95%CI,52.9%-82.5%)在第一个四分位数中存活6年,与83.8%(95%CI,77.3%-90.9%)相比,在2到4(P = .008)。结论:在接受免疫抑制治疗的严重血栓性贫血患者队列中,端粒长度与反应无关,但与复发,克隆演化和整体存活风险有关。

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