Describing the evolution of myeloid-derived leucocytes in treated B-lineage paediatric acute lymphoblastic leukaemia with a data-driven granulocyte-monocyte-blast model.

IF 0.8 4区 数学 Q4 BIOLOGY
Larisse Bolton, Thomas M Acho, David K Stones, Cang Hui
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引用次数: 0

Abstract

Acute lymphoblastic leukaemia (ALL) is associated with a compromised myeloid system. Understanding the state of granulopoiesis in a patient during treatment, places the clinician in an advantageous position. Mathematical models are aids able to present the clinician with insight into the behaviour of myeloid-derived leucocytes. The main objective of this investigation was to determine whether a proposed model of ALL during induction therapy would be a usable descriptor of the system. The model assumes the co-occurrence of the independent leukaemic and normal marrow populations. It is comprised of four delay-differential equations, capturing the fundamental characteristics of the blood and bone marrow myeloid leucocytes and B-lineage lymphoblasts. The effect of treatment was presumed to amplify cell loss within both populations. Clinical data was used to inform the construction, calibration and examination of the model. The model is promising-presenting a good foundation for the development of a clinical supportive tool. The predicted parameters and forecasts aligned with clinical expectations. The starting assumptions were also found to be sound. A comparative investigation highlighted the differing responses of similarly diagnosed patients during treatment and further testing on patient data emphasized patient specificity. Model examination recommended the explicit consideration of the suppressive effects of treatment on the normal population production. Additionally, patient-related factors that could have resulted in such different responses between patients need to be considered. The parameter estimates require refinement to incorporate the action of treatment. Furthermore, the myeloid populations require separate consideration. Despite the model providing explanation, incorporating these recommendations would enhance both model usability and predictive capacity.

用数据驱动的粒细胞-单核细胞-母细胞模型描述治疗的b系儿科急性淋巴细胞白血病中骨髓来源的白细胞的进化。
急性淋巴细胞白血病(ALL)与骨髓系统受损有关。了解患者在治疗过程中的颗粒生成状态,使临床医生处于有利地位。数学模型可以帮助临床医生深入了解骨髓源性白细胞的行为。本研究的主要目的是确定在诱导治疗期间提出的ALL模型是否可以作为该系统的可用描述符。该模型假定独立的白血病群体和正常骨髓群体同时出现。它由四个延迟微分方程组成,捕获了血液和骨髓骨髓性白细胞和b系淋巴细胞的基本特征。据推测,治疗的效果会在两个人群中放大细胞损失。使用临床数据来指导模型的构建、校准和检验。该模型很有前景,为临床辅助工具的开发提供了良好的基础。预测参数和预测符合临床期望。开始的假设也被认为是合理的。一项比较调查强调了类似诊断的患者在治疗期间的不同反应,对患者数据的进一步测试强调了患者的特异性。模型检验建议明确考虑处理对正常种群生产的抑制作用。此外,需要考虑可能导致患者之间不同反应的患者相关因素。参数估计需要改进以纳入处理的作用。此外,髓系人群需要单独考虑。尽管模型提供了解释,但纳入这些建议将提高模型的可用性和预测能力。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
CiteScore
2.20
自引率
0.00%
发文量
15
审稿时长
>12 weeks
期刊介绍: Formerly the IMA Journal of Mathematics Applied in Medicine and Biology. Mathematical Medicine and Biology publishes original articles with a significant mathematical content addressing topics in medicine and biology. Papers exploiting modern developments in applied mathematics are particularly welcome. The biomedical relevance of mathematical models should be demonstrated clearly and validation by comparison against experiment is strongly encouraged. The journal welcomes contributions relevant to any area of the life sciences including: -biomechanics- biophysics- cell biology- developmental biology- ecology and the environment- epidemiology- immunology- infectious diseases- neuroscience- pharmacology- physiology- population biology
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