Disentangling Predictors of COPD Mortality with Probabilistic Graphical Models

Tyler C. Lovelace, Min Hyung Ryu, Minxue Jia, Peter Castaldi, Frank C Sciurba, Craig P. Hersh, Panayiotis Benos
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Abstract

Chronic Obstructive Pulmonary Disease (COPD) is a leading cause of mortality. Predicting mortality risk in COPD patients can be important for disease management strategies. Although scores for all-cause mortality have been developed previously, there is limited research on factors that may directly affect COPD-specific mortality. We used probabilistic (causal) graphs to analyze clinical baseline COPDGene data, including demographics, spirometry, quantitative chest imaging, and symptom features, as well as gene expression data (from year-5). We identified factors linked to all-cause and COPD-specific mortality. Although many were similar, there were differences in certain comorbidities (all-cause mortality model only) and forced vital capacity (COPD-specific mortality model only). Using our results, we developed VAPORED, a 7-variable COPD-specific mortality risk score, which we validated using the ECLIPSE 3-yr mortality data. We showed that the new model is more accurate than the existing ADO, BODE, and updated BODE indices. Additionally, we identified biological signatures linked to all-cause mortality, including a plasma cell mediated component. Finally, we developed a web page to help clinicians calculate mortality risk using VAPORED, ADO, and BODE indices. Given the importance of predicting COPD-specific and all-cause mortality risk in COPD patients, we showed that probabilistic graphs can identify the features most directly affecting them, and be used to build new, more accurate models of mortality risk. Novel biological features affecting mortality were also identified. This is an important step towards improving our identification of high-risk patients and potential biological mechanisms that drive COPD mortality.
用概率图形模型分解慢性阻塞性肺病死亡率的预测因素
慢性阻塞性肺病(COPD)是导致死亡的主要原因。预测慢性阻塞性肺病患者的死亡风险对疾病管理策略非常重要。虽然之前已经开发出了全因死亡率评分,但对可能直接影响慢性阻塞性肺病特异性死亡率的因素的研究还很有限。我们使用概率(因果)图分析了临床基线 COPDGene 数据,包括人口统计学、肺活量测定、胸部定量成像和症状特征,以及基因表达数据(第 5 年)。我们确定了与全因死亡率和慢性阻塞性肺病特异性死亡率相关的因素。虽然许多因素相似,但某些合并症(仅全因死亡率模型)和强迫生命容量(仅慢性阻塞性肺病特异性死亡率模型)存在差异。根据我们的研究结果,我们开发了 VAPORED,这是一个由 7 个变量组成的慢性阻塞性肺病特异性死亡风险评分,我们使用 ECLIPSE 3 年死亡率数据对其进行了验证。结果表明,新模型比现有的 ADO、BODE 和更新的 BODE 指数更准确。此外,我们还确定了与全因死亡率相关的生物特征,包括浆细胞介导的成分。最后,我们开发了一个网页,帮助临床医生使用 VAPORED、ADO 和 BODE 指数计算死亡风险。鉴于预测慢性阻塞性肺病患者的特异性和全因死亡风险的重要性,我们证明概率图可以识别最直接影响患者的特征,并用于建立新的、更准确的死亡风险模型。我们还发现了影响死亡率的新生物特征。这是我们朝着更好地识别高危患者和导致慢性阻塞性肺病死亡率的潜在生物机制迈出的重要一步。
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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