化疗诱导儿童急性淋巴细胞白血病B患者血浆抗氧化改变,与疾病预后相关

Q4 Immunology and Microbiology
Matheus Ricardo Garbim , Geise Ellen Broto , Fausto Celso Trigo , Vanessa Jacob Victorino , Stefania Tagliari de Oliveira , Décio Sabbatini Barbosa , Carolina Panis
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引用次数: 1

摘要

儿童急性淋巴细胞白血病(ALL)是最常见的儿童癌症,细胞毒性化疗仍然是主要的治疗选择。化疗药物通过氧化应激产生作用,但其临床意义尚不清楚。在化疗期间,本研究评估了34例诊断为b细胞ALL (B-ALL)患者外周血样本的抗氧化谱。在诊断(D0)和诱导、巩固和维持阶段采集外周血样本。采用高灵敏度化学发光技术测定血浆总抗氧化能力(TRAP)。在诱导期(28.68 ~ 1194.71 μM Trolox, p = 0.0178)和高危组(年龄>10年和/或白细胞计数和/或>诊断时50,000个白细胞/m3),低风险患者(253.79 ~ 1194.71 μM Trolox, p = 0.0314)。与存活患者相比,死亡患者的TRAP也减少(392.42-1194.71 μM Trolox, p = 0.0278)。巩固期(56.14-352.05 μM Trolox, p=<0.0001)和维持期(30.48-672.99 μM Trolox, p=<0.0001)患者的TRAP水平与诱导期(28.68-1390.26 μM Trolox)患者相比显著降低,达到与治愈期(64.82-437.82 μM Trolox)患者相近的水平。这些发现表明,化疗期间B-ALL总抗氧化能力的变化是一个与疾病预后相关的参数。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Chemotherapy induces plasmatic antioxidant changes in pediatric patients with acute lymphoid leukemia B that correlate to disease prognosis

Chemotherapy induces plasmatic antioxidant changes in pediatric patients with acute lymphoid leukemia B that correlate to disease prognosis

Pediatric acute lymphoid leukemias (ALL) is the most common childhood cancer, and cytotoxic chemotherapy remains the primary treatment option. Chemotherapic drugs act by oxidative stress generation, but their clinical meaning is poorly understood. During the chemotherapy schedule, this study evaluated the antioxidant profile of peripheral blood samples from 34 patients diagnosed with type B-cell ALL (B-ALL). Peripheral blood samples were collected at diagnosis (D0) and during the induction, consolidation, and maintenance phases. The plasma total antioxidant capacity (TRAP) was determined using the high-sensitivity chemiluminescence technique. Antioxidant levels were higher on D0 compared to day 7 after treatment starting (D7) in the induction phase (28.68–1194.71 μM Trolox, p = 0.0178) and in the high-risk group (age > ten years and/or with white blood cell counts and/or > 50,000 white blood cells/m3 at diagnosis) concerning low-risk patients (253.79–1194.71 μM Trolox, p = 0.0314). Reduced TRAP was also detected in patients who died compared to those who survived (392.42–1194.71 μM Trolox, p = 0.0278). Patients under consolidation (56.14–352.05 μM Trolox, p=<0.0001) and maintenance (30.48–672.99 μM Trolox, p=<0.0001) showed a significant reduction in TRAP levels compared to those from the induction phase (28.68–1390.26 μM Trolox), reaching levels similar to cured patients out of treatment (64.82–437.82 μM Trolox). These findings suggest that the variation of the total antioxidant capacity in B-ALL during chemotherapy is a parameter that correlates to some predictors of disease prognosis.

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