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首页> 外文期刊>Biological research for nursing >Influence of Nitrosative Stress on Fatigue During Childhood Leukemia Treatment
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Influence of Nitrosative Stress on Fatigue During Childhood Leukemia Treatment

机译:氮胁迫对儿童白血病治疗期间疲劳的影响

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摘要

The focus on a cure for childhood leukemia over the last three decades has resulted in survival rates of more than 80%. However, efforts to manage leukemia-treatment symptoms have not kept pace with new therapies. Symptom toxicity during treatment can result in complications, treatment delays, and therapy dose reductions. Compromise in therapy can negatively influence the quality of life and, even more notably, jeopardize chances for long-term survival. This study examined biologic mechanisms that influence fatigue caused by increased reactive oxidative species (ROS) or actual failure of the antioxidant defense system due to genetic variation by investigating reactive nitrosative species, a downstream consequence of ROS. The specific aims of this study were to characterize the trajectory of nitrosative stress during acute lymphoblastic leukemia treatment and evaluate the influence of nitrosative stress on fatigue. A repeated measures design was used to evaluate the fatigue experienced by 186 children and adolescents, 3-18 years of age, with a diagnosis of leukemia during the most intense phase of treatment. An established biomarker of nitrosative stress, protein 3-nitrotyrosine (3NT) residues in the cerebral spinal fluid, was evaluated at diagnosis, postinduction, and consolidation phases of treatment. Higher fatigue was associated with higher 3NT levels at the beginning of treatment. Two distinct groups of children experienced either consistently high or consistently low 3NT levels across the treatment trajectory, from diagnosis to 12 months postinduction. Findings from this study support continued exploration into the phenotypic biochemical mechanisms that influence a reactive response to childhood cancer treatment.
机译:在过去三十年中,对儿童白血病治愈的重点导致生存率超过80%。然而,努力管理白血病治疗症状的症状并没有与新疗法保持速度。治疗过程中的症状毒性可导致并发症,治疗延迟和治疗剂量减少。治疗中的妥协可以对生命的质量产生负面影响,更容易发生,危及长期存活的机会。该研究检查了通过研究反应性亚硝化物种,ROS下游后果导致抗氧化物质(ROS)增加或抗氧化防御系统的实际失败影响的生物机制。本研究的具体目的是在急性淋巴细胞白血病治疗期间表征亚硝化胁迫的轨迹,并评估氮粘性应激对疲劳的影响。重复措施设计用于评估186名儿童和青少年的疲劳,3-18岁,在最强烈的治疗期间诊断白血病。在诊断,后导和固结阶段评估脑脊髓中亚硝基胁迫,蛋白质3-硝基荧光蛋白(3NT)残基的亚硝基胁迫,蛋白质3-硝基荧光蛋白(3NT)残留物。在治疗开始时,较高的疲劳与较高的3NT水平相关。两种不同的儿童群体在治疗轨迹中始终如一地高或始终如一的3NT水平,从诊断到12个月后诊断。本研究的调查结果支持持续探索对影响儿童癌症治疗的活性反应的表型生化机制。

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