对接受硼替佐米诱导、大剂量治疗和自体干细胞移植的多发性骨髓瘤患者进行定量综合生存期预测

IF 5.3 2区 医学 Q1 ONCOLOGY JCO precision oncology Pub Date : 2024-07-01 DOI:10.1200/PO.23.00613
Manuela Hummel, Thomas Hielscher, Martina Emde-Rajaratnam, Hans Salwender, Susanne Beck, Christof Scheid, Uta Bertsch, Hartmut Goldschmidt, Anna Jauch, Jérôme Moreaux, Anja Seckinger, Dirk Hose
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引用次数: 0

摘要

目的:鉴于多发性骨髓瘤患者生存期的高度异质性,定量预测单个患者的生存期,而不是像目前的模型(如修订版国际分期系统(R-ISS)、R2-ISS或梅奥-2022-评分)那样将患者归入2至4个风险组,将对临床非常有用:我们的目的是开发一种定量预测工具,用于预测个体患者的 3-5 年总生存(OS)概率。我们将已确定的临床和分子风险因素整合到一个综合预后模型中,并评估和验证了该模型相对于R-ISS、R2-ISS和Mayo-2022-score的风险识别能力:结果:在 Cox 回归模型的基础上建立了一个用于估计 OS 概率的提名图。通过给每个预后因素打分并将所有分数相加,可以将患者的个体风险状况转化为 3-5 年的 OS 概率。外部对该提名图的判别和校准进行了验证。在验证队列中,预后指数没有明显的偏差或过度拟合。基于重采样的外部评估显示校准效果良好。该模型的c指数在训练队列(0.76)和验证队列(0.75)中相似,且明显高于R-ISS(P < .001)或R2-ISS(P < .01):总之,我们开发并验证了基于个人定量提名图的 OS 预测。综合分子预后因素的连续风险评估优于单独的 R-ISS、R2-ISS 或 Mayo-2022 评分。
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Quantitative Integrative Survival Prediction in Multiple Myeloma Patients Treated With Bortezomib-Based Induction, High-Dose Therapy and Autologous Stem Cell Transplantation.

Purpose: Given the high heterogeneity in survival for patients with multiple myeloma, it would be clinically useful to quantitatively predict the individual survival instead of attributing patients to two to four risk groups as in current models, for example, revised International Staging System (R-ISS), R2-ISS, or Mayo-2022-score.

Patients and methods: Our aim was to develop a quantitative prediction tool for individual patient's 3-/5-year overall survival (OS) probability. We integrated established clinical and molecular risk factors into a comprehensive prognostic model and evaluated and validated its risk discrimination capabilities versus R-ISS, R2-ISS, and Mayo-2022-score.

Results: A nomogram for estimating OS probabilities was built on the basis of a Cox regression model. It allows one to translate the individual risk profile of a patient into 3-/5-year OS probabilities by attributing points to each prognostic factor and summing up all points. The nomogram was externally validated regarding discrimination and calibration. There was no obvious bias or overfitting of the prognostic index on the validation cohort. Resampling-based and external evaluation showed good calibration. The c-index of the model was similar on the training (0.76) and validation cohort (0.75) and significantly higher than for the R-ISS (P < .001) or R2-ISS (P < .01).

Conclusion: In summary, we developed and validated individual quantitative nomogram-based OS prediction. Continuous risk assessment integrating molecular prognostic factors is superior to R-ISS, R2-ISS, or Mayo-2022-score alone.

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