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首页> 外文期刊>PLoS Computational Biology >Computational Biomarker Pipeline from Discovery to Clinical Implementation: Plasma Proteomic Biomarkers for Cardiac Transplantation
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Computational Biomarker Pipeline from Discovery to Clinical Implementation: Plasma Proteomic Biomarkers for Cardiac Transplantation

机译:从发现到临床实施的计算生物标志物管道:用于心脏移植的血浆蛋白质组学生物标志物

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Recent technical advances in the field of quantitative proteomics have stimulated a large number of biomarker discovery studies of various diseases, providing avenues for new treatments and diagnostics. However, inherent challenges have limited the successful translation of candidate biomarkers into clinical use, thus highlighting the need for a robust analytical methodology to transition from biomarker discovery to clinical implementation. We have developed an end-to-end computational proteomic pipeline for biomarkers studies. At the discovery stage, the pipeline emphasizes different aspects of experimental design, appropriate statistical methodologies, and quality assessment of results. At the validation stage, the pipeline focuses on the migration of the results to a platform appropriate for external validation, and the development of a classifier score based on corroborated protein biomarkers. At the last stage towards clinical implementation, the main aims are to develop and validate an assay suitable for clinical deployment, and to calibrate the biomarker classifier using the developed assay. The proposed pipeline was applied to a biomarker study in cardiac transplantation aimed at developing a minimally invasive clinical test to monitor acute rejection. Starting with an untargeted screening of the human plasma proteome, five candidate biomarker proteins were identified. Rejection-regulated proteins reflect cellular and humoral immune responses, acute phase inflammatory pathways, and lipid metabolism biological processes. A multiplex multiple reaction monitoring mass-spectrometry (MRM-MS) assay was developed for the five candidate biomarkers and validated by enzyme-linked immune-sorbent (ELISA) and immunonephelometric assays (INA). A classifier score based on corroborated proteins demonstrated that the developed MRM-MS assay provides an appropriate methodology for an external validation, which is still in progress. Plasma proteomic biomarkers of acute cardiac rejection may offer a relevant post-transplant monitoring tool to effectively guide clinical care. The proposed computational pipeline is highly applicable to a wide range of biomarker proteomic studies.
机译:定量蛋白质组学领域的最新技术进步刺激了对各种疾病的大量生物标志物发现研究,为新的治疗方法和诊断方法提供了途径。但是,固有的挑战限制了将候选生物标记物成功转化为临床用途的成功,因此凸显了对从生物标记物发现过渡到临床实施的可靠分析方法的需求。我们已经开发了用于生物标记研究的端到端计算蛋白质组学管道。在发现阶段,管道将重点放在实验设计,适当的统计方法和结果质量评估的不同方面。在验证阶段,管道将重点放在将结果迁移到适合外部验证的平台上,并基于确证的蛋白质生物标记物开发分类器评分。在临床实施的最后阶段,主要目标是开发和验证适合临床部署的分析方法,并使用开发的分析方法校准生物标志物分类器。拟议中的管道用于心脏移植的生物标志物研究,旨在开发微创临床试验以监测急性排斥反应。从人血浆蛋白质组的非靶向筛选开始,鉴定了五种候选生物标记蛋白。排斥调节蛋白反映细胞和体液免疫反应,急性期炎症途径和脂质代谢生物学过程。针对五个候选生物标记物开发了多重多重反应监测质谱(MRM-MS)分析,并通过酶联免疫吸附(ELISA)和免疫比浊法(INA)进行了验证。基于确证蛋白质的分类器评分表明,开发的MRM-MS测定法为外部验证提供了合适的方法,该方法仍在进行中。急性心脏排斥反应的血浆蛋白质组学生物标志物可提供相关的移植后监测工具,以有效指导临床护理。拟议的计算流程高度适用于广泛的生物标志物蛋白质组学研究。

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