评估血浆 D-二聚体水平对实体恶性肿瘤的预后、疾病进展和存活率的影响

Rucha Kalwaghe, Pravinkumar Ghongade, Anupama Gupta
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引用次数: 0

摘要

背景:D-二聚体是一种纤维蛋白降解产物(FDP),是血凝块被纤维蛋白溶解降解后存在于血液中的一种小的蛋白质片段。目的:评估 D-二聚体水平与实体恶性肿瘤患者的预后、疾病进展和生存期的关系。背景和设计:2021 年 2 月至 2023 年 2 月进行的横断面分析研究。材料与方法记录 100 例实体恶性肿瘤病例的数据,包括干预前的 D-二聚体水平及其随访值、肿瘤分级、TNM[肿瘤大小(T)、结节(N)和转移(M)]分期、疾病进展和患者状态。统计分析:Kaplan-Meier 曲线和对数秩。结果85%的癌症病例中发现 D-二聚体水平增高。76.3%的口腔癌、82%的乳腺癌、100%的消化道癌和卵巢癌病例出现高 D-二聚体水平。据统计,T1 + T2 阶段的 D-二聚体水平低于 T3 + T4 阶段的 D-二聚体水平。(χ2 = 5.40, P = 0.002)。实体恶性肿瘤淋巴结 N0 期与 N1 + N2 期(χ2 = 5.82,P = 0.0001)以及无转移期(Mo)与 M1 期(χ2 = 3.02,P = 0.003)的 D-二聚体水平有显著差异。随着实体恶性肿瘤的复发和进展,D-二聚体呈线性明显增加。死亡患者的 D-二聚体高于存活患者(t = 3.75,P = 0.0001)。D 二聚体升高与死亡率升高有关(P = 0.023,奇数比 = 3.73,生存系数 = 1.31,标准误差 = 0.578)。结论D-二聚体是一种很有前景的预后生物标志物,可预测癌症患者的不良临床结局、癌症复发、进展、转移和不良生存。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Assessment of plasma D-dimer level for prognosis, disease progression, and survival in solid malignancies
Background: D-dimer is a fibrin degradation product (FDP), a small protein fragment present in the blood after a blood clot is degraded by fibrinolysis. Aim: To evaluate the association of D-dimer level with prognosis, disease progression and survival of patients in cases of solid malignancies. Setting and Design: Analytical cross sectional study conducted from February 2021 to February 2023. Materials and Methods: Data regarding 100 solid malignancy cases including their preintervention D-dimer levels and its value at follow up, grading, TNM [Tumor size (T), node (N), and metastases (M)] staging of tumor, disease progression and patient status were recorded. Statistical Analysis: Kaplan–Meier curve and Log Rank. Results: Amplified D-dimer level was noted in 85% cancer cases. 76.3% of oral cancer, 82% of breast cancer, 100% cases of digestive tract and ovarian cancer were presented with high D-dimer level. D-dimer in T1 + T2 stage was statistically lower than the D-dimer level of T3 + T4 stage. (χ2 = 5.40, P = 0.002). Comparison of Lymph node in N0 versus N1 + N2 stage (χ2 = 5.82, P = 0.0001) as well as no metastases stage (Mo) versus M1 stages (χ2 = 3.02, P = 0.003) of solid malignancies had significant difference in D-dimer level. D-dimer increased significantly and linearly with recurrence and advancement of solid malignancy. Dead patient had higher D-dimer than alive patients (t = 3.75, P = 0.0001). Increased D-dimer was associated with elevated mortality (P = 0.023, odd ratio = 3.73, survival coefficient = 1.31 with standard error = 0.578). Conclusion: D-dimer is a promising prognostic biomarker which can predict poor clinical outcomes in cancer patients, cancer recurrence, progression, metastases, poor survival.
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