肝细胞癌BCLC B期和C期血小板计数升高（bbb200 × 10^9 / L）的预后意义：一项回顾性多中心分析

IF 4.2 3区医学 Q2 ONCOLOGY

Journal of Hepatocellular Carcinoma Pub Date : 2025-05-05 eCollection Date: 2025-01-01 DOI:10.2147/JHC.S511263

Stefan Munker, Isaac Rodriguez, Kathrin Bernhart, Najib Ben Khaled, Merve Findik, Lisa Katrin Siegmund, Liangtao Ye, Florian P Reiter, Daniel Roessler, Daniel Nasseh, Lorenz Balcar, Katharina Pomej, Bernhard Scheiner, Christel Weiss, Matthias Pinter, Max Seidensticker, Julia Mayerle, Alexander B Philipp, Enrico N De Toni

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引用次数: 0

摘要

在肝细胞癌（HCC）中，与肝功能下降或门静脉高压症相关的合并症通常限制了治疗选择。传统上，低血小板计数被认为是HCC的不良预后因素，特别是在早期阶段。然而，最近的证据表明，在晚期，血小板计数升高也可能预示更糟糕的结果，提示一种依赖于阶段的预后影响。目的：本研究评估血小板计数在BCLC分期中的预后作用，并对门静脉高压进行调整，以改善个体化患者管理。方法：回顾性分析1112例不同肿瘤分期HCC患者的血小板计数。检测各种血小板计数临界值（X至Y × 10^9/L）以确定最佳预后阈值。为了分离血小板水平对门静脉高压症的影响，在多变量分析中纳入脾脏直径作为调整变量，并考虑静脉曲张状态（约三分之二的患者）。采用优化的截止值，采用单因素和多因素Cox比例风险模型进行生存分析。执行引导以进行内部验证。结果：血小板计数在84 ~ 200 × 10^9/L之间与较差的生存率相关（HR = 0.66, 95% CI = 0.57 ~ 0.78, p < 0.0001）。Bootstrapping显示了最终模型的鲁棒性。亚组分析显示，多变量分析（包括脾直径）中血小板计数升高（bbb200 × 10^9/L）， BCLC B期和C期患者的生存率较低，但A期患者的生存率不高。结论：血小板计数对HCC的预后影响具有分期依赖性。诊断时血小板计数高于200/µL的临界值与较差的预后相关。使用这个临界值可以提高BCLC B和C患者的生存预测，并可能用于风险分层和指导治疗决策。需要进一步的外部验证来确认这些发现并评估其临床适用性。

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Prognostic Significance of Elevated Platelet Count (>200 x 10^9 per L) in BCLC Stages B and C of Hepatocellular Carcinoma: A Retrospective Multicenter Analysis.

Introduction: In hepatocellular carcinoma (HCC) comorbidities related to decreased liver function or to portal hypertension often limit treatment options. Traditionally, low platelet count has been considered a negative prognostic factor in HCC, especially in early stages. However, recent evidence suggests that elevated platelet count may also predict worse outcomes in advanced stages, suggesting a stage-dependent prognostic impact.

Aim: This study evaluated the prognostic role of platelet counts across BCLC stages, adjusted for portal hypertension, to improve individualized patient management.

Methods: In this retrospective, multicenter study, platelet count of 1112 patients with HCC in different tumor stages was analyzed. Various platelet count cutoffs (X to Y × 10^9/L) were tested to identify the optimal prognostic threshold. To isolate the effect of platelet levels from portal hypertension, spleen diameter was incorporated as an adjustment variable in multivariate analyses, with variceal status considered when available (in about two thirds of patients). Using an optimized cut-off, survival analysis was performed using univariate and multivariate Cox proportional hazards models. Bootstrapping was performed for internal validation.

Results: Platelet count outside 84-200 × 10^9/L was associated with poorer survival (HR = 0.66, 95% CI = 0.57-0.78, p < 0.0001). Bootstrapping showed robustness of the final model. Subgroup analysis revealed worse survival in BCLC stages B and C but not stage A for elevated platelet counts (>200 × 10^9/L) in multivariate analysis (including spleen diameter).

Conclusion: Platelet counts showed a stage-dependent prognostic impact in HCC. A platelet count above a cutoff of 200/µL at diagnosis was associated with poorer prognosis. Using this cutoff may improve survival prediction in BCLC B and C patients with potential usage for risk stratification and guidance of treatment decisions. Further external validation is required to confirm these findings and evaluate their clinical applicability.

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