泛免疫炎症值在鼻咽癌同期化放疗后三联征预测中的价值

IF 2.3 4区 医学 Q3 BIOTECHNOLOGY & APPLIED MICROBIOLOGY International Journal of Biological Markers Pub Date : 2024-03-01 Epub Date: 2024-01-08 DOI:10.1177/03936155231223198
Efsun Somay, Busra Yilmaz, Erkan Topkan, Beyza Sirin Ozdemir, Duriye Ozturk, Ali Ayberk Besen, Huseyin Mertsoylu, Ugur Selek
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引用次数: 0

摘要

目的:放射诱导的三联症(RIT)是同期化放疗(C-CRT)罕见但严重的副作用之一,很难准确预测。我们旨在研究接受 C-CRT 的局部晚期鼻咽癌(LA-NPC)患者在治疗前的泛免疫炎症值(PIV)是否能预测 RIT:方法: 回顾性分析了接受C-CRT治疗且最大张口度(MMO)大于35毫米的LA-NPC患者的数据。C-CRT后的任何MMO小于或等于35毫米均视为RIT。所有 PIV 值均使用全血细胞计数检测结果计算:PIV = (血小板 × 单核细胞 × 中性粒细胞) ÷ 淋巴细胞。采用接收者操作特征分析法来分析治疗前 PIV 读数与 RIT 状态之间可能存在的关联。使用逻辑回归分析检验了干扰变量与 RIT 率之间的独立关系:该研究共有 223 名参与者,其中 46 人(20.6%)被诊断为 RIT,从 C-CRT 到 RIT 的中位时间为 10 个月(范围:5-18 个月)。采用接收器操作特征曲线分析法对 C-CRT 前的 PIV 水平和 RIT 率进行了分析,830 为最佳临界值(曲线下面积:92.1%;灵敏度:87%):92.1%;灵敏度:87.5%;特异性:85.5%;尤登指数:0.730):0.730).PIV>830队列中的RIT发生率明显高于PIV≤830队列(60.3% vs. 5%;危险比5.79;P P = 0.004)、咀嚼仪剂量V58Gy≥%32(P = 0.003)和PIV>830(P 结论:PIV≤830队列中的RIT发生率明显高于PIV≤830队列(60.3% vs. 5%;危险比5.79;P P = 0.004):C-CRT前PIV升高是一个独特的生物标记,可独立预测接受C-CRT的LA-NPC的RIT率升高。
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Worth of pan-immune-inflammation value in trismus prediction after concurrent chemoradiotherapy for nasopharyngeal carcinomas.

Objective: Radiation-induced trismus (RIT), one of the rare but serious side effects of concurrent chemoradiotherapy (C-CRT), is difficult to predict with high accuracy. We aimed to examine whether the pretreatment pan-immune-inflammation value (PIV) measures predict RIT in patients with locally advanced nasopharyngeal carcinoma (LA-NPC) receiving C-CRT.

Methods: Data of patients with LA-NPC who underwent C-CRT and had maximum mouth openings (MMO) > 35 mm were reviewed. Any MMO of 35 mm or less after C-CRT was considered RIT. All PIV values were computed using the complete blood count test results: PIV = (Platelets × Monocytes × Neutrophils) ÷ Lymphocytes. The receiver operating characteristic analysis was employed to dissect a possible association between pre-treatment PIV readings and RIT status. Confounding variables were tested for their independent relationship with the RIT rates using logistic regression analysis.

Results: The research comprised 223 participants, and RIT was diagnosed in 46 (20.6%) at a median time from C-CRT to RIT of 10 months (range: 5-18 months). Pre-C-CRT PIV levels and RIT rates were analyzed using receiver operating characteristic curve analysis, with 830 being the optimal cutoff (area under the curve: 92.1%; sensitivity: 87.5%; specificity: 85.5%; Youden index: 0.730). RIT was significantly more prevalent in the PIV > 830 cohort than its PIV ≤ 830 counterpart (60.3% vs. 5%; hazard ratio 5.79; P < 0.001). Multivariate logistic regression analysis revealed that advanced T-stage (P = 0.004), masticatory apparatus dose V58Gy≥%32 (P = 0.003), and PIV > 830 (P < 0.001) were independently linked with significantly elevated rates of RIT.

Conclusion: The presence of elevated pre-C-CRT PIV is a unique biological marker that independently predicts increased RIT rates in LA-NPC undergoing C-CRT.

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来源期刊
International Journal of Biological Markers
International Journal of Biological Markers 医学-生物工程与应用微生物
CiteScore
4.10
自引率
0.00%
发文量
43
期刊介绍: IJBM is an international, online only, peer-reviewed Journal, which publishes original research and critical reviews primarily focused on cancer biomarkers. IJBM targets advanced topics regarding the application of biomarkers in oncology and is dedicated to solid tumors in adult subjects. The clinical scenarios of interests are screening and early diagnosis of cancer, prognostic assessment, prediction of the response to and monitoring of treatment.
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