凝血因子Ⅷ联合血栓弹力图对急性白血病化疗骨髓抑制患者出血风险的预测价值

doi:10.3969/j.issn.1671-7171.2023.06.014

摘要
图/表
参考文献
相关文章 (15)

全文: PDF (1238 KB) HTML (1 KB)
输出: BibTeX | EndNote (RIS)

摘要【目的】探讨凝血因子Ⅷ(FⅧ)联合血栓弹力图(TEG)对急性白血病化疗骨髓抑制患者出血风险的预测价值。【方法】检测86例急性白血病化疗骨髓抑制患者的FⅧ水平及TEG参数[凝固时间(K值)、反应时间(R值)、血栓形成的最大幅度(MA值)及血凝块聚合速率(Angle值)],根据患者骨髓抑制后48 h内出血情况将其分为出血组和无出血组,以Logistic多因素回归分析患者出血的相关因素,以受试者工作特征(ROC)曲线评估TEG相关指标及FⅧ水平对患者出血的预测价值。【结果】 86例患者中,51例出血(出血组),占比59.30%;35例患者未出血(无出血组),占比40.70%。出血组感染例数占比高于无出血组,且MA值及FⅧ水平均低于无出血组(P<0.05);Logistic多因素回归分析结果显示,合并感染、MA值及FⅧ水平降低均为急性白血病化疗骨髓抑制患者出血的危险因素(P<0.05);ROC分析显示,MA值、FⅧ水平及二者联合预测患者出血的曲线下面积(AUC)分别为0.744、0.724及0.848,MA值、FⅧ水平单一预测患者出血的效能低于二者联合检测(P<0.05)。【结论】合并感染的急性白血病骨髓抑制患者随着MA值及FⅧ水平的降低,出血发生率明显升高;MA值及FⅧ水平对患者的出血风险具有一定的临床预测价值。

	服务

	把本文推荐给朋友
	加入我的书架
	加入引用管理器
	E-mail Alert
	RSS
	作者相关文章
	刘仁美
	张新滨

关键词 ：白血病, 急性病, 血液凝固因子, 血栓弹力描记术, 抗肿瘤联合化疗方案, 骨髓疾病/病因学

Abstract：【Objective】 To explore the predictive value of coagulation factor Ⅷ (FⅧ) combined with thromboelastography (TEG) on the bleeding risk of patients with acute leukemia chemotherapy and myelosuppression. 【Methods】 A total of 86 patients with acute leukemia chemotherapy and myelosuppression were tested for the coagulation FⅧ level and TEG parameters [coagulation time (K value),reaction time (R value),maximum thrombosis (MA value) and blood clot aggregation rate (Angle value)]. According to the bleeding within 48 hours after bone marrow suppression,patients were divided into the bleeding group and no bleeding group. Logistic multivariate regression analysis was used to explore the related factors of bleeding in patients with acute leukemia chemotherapy for myelosuppression,and receiver operating characteristic curve (ROC) was used to determine the predictive value of TEG-related indicators and FⅧ levels in patients.【Results】 Among 86 patients with acute leukemia bone marrow suppression during chemotherapy,51 patients had bleeding (the bleeding group),accounting for 59.30% (51/86); the remaining 35 patients had no bleeding (non-bleeding group),accounting for 40.70% (35/86). The proportion of infected cases in the bleeding group was higher than that in the non-bleeding group,and the MA value and FⅧ level were lower than those in the bleeding group (P<0.05). Logistic multivariate regression analysis showed that co-infection and reduced-MA value and FⅧ level were risk factors for bleeding in patients (P<0.05). ROC analysis showed that the bleeding risk by the area under the curve (AUC) of MA value,FⅧ level and the combination of the two parameters were 0.744,0.724,and 0.848,respectively. MA value and FⅧ level alone predict the bleeding risk in patients,however,their predictive powers were lower than the combination of the two (P<0.05). 【Conclusion】 With the decrease of MA value and FⅧ level,the incidence of bleeding in acute leukemia myelosuppressed patients with co-infection increased significantly; MA value and FⅧ level have a certain clinical predictive value for bleeding in patients.

Key words： Leukemia Acute Disease Blood Coagulation Factors Thrombelastography Antineoplastic Combined Chemotherapy Protocols Bone Marrow Diseases/ET

收稿日期: 2022-09-08

中图分类号:

R733.712

引用本文:

刘仁美, 张新滨. 凝血因子Ⅷ联合血栓弹力图对急性白血病化疗骨髓抑制患者出血风险的预测价值[J]. 医学临床研究, 2023, 40(6): 848-851.
LIU Ren-mei, ZHANG Xin-bin. Predictive Value of Coagulation Factor Ⅷ Combined with Thromboelastography on Bleeding Risk of Patients with Acute Leukemia Chemotherapy and Myelosuppression. JOURNAL OF CLINICAL RESEARCH, 2023, 40(6): 848-851.

链接本文:

http://journal07.magtech.org.cn/yxlcyj/CN/10.3969/j.issn.1671-7171.2023.06.014 或 http://journal07.magtech.org.cn/yxlcyj/CN/Y2023/V40/I6/848

[1] van GALEN P,HOVESTADT V,WADSWORTH I M,et al.Single-cell rna-seq reveals aml hierarchies relevant to disease progression and immunity[J].Cell,2019,176(6):1265-1281.
[2] MOUSSA A D,ROUAS R,NAJAR M,et al. Identification of acute myeloid leukemia bone marrow circulating MicroRNAs[J].Int J Mol Sci,2020,21(19):134-136.
[3] BEZZERRI V,API M,ALLEGRI M,et al. Nonsense suppression therapy:new hypothesis for the treatment of inherited bone marrow failure syndromes[J].Int J Mol Sci,2020,21(13):71-72.
[4] NEPSTAD I,HATFIELD K J,GRONNINGSAETER I S,et al. The PI3K-Akt-mTOR signaling pathway in human acute myeloid leukemia (AML) cells[J].Int J Mol Sci,2020,21(8):37-39.
[5] ERBANI J,TAY J,BARBIER V,et al. Acute myeloid leukemia chemo-resistance is mediated by e-selectin receptor CD162 in bone marrow niches[J].Front Cell Dev Biol,2020,8(1):668.
[6] VALENT P,SADOVNIK I,EISENWORT G,et al. Immunotherapy-based targeting and elimination of leukemic stem cells in AML and CML[J].Int J Mol Sci,2019,20(17):112.
[7] OLSON L B,NAQVI I A,TURNER D J,et al. Key Pathogenic factors in coronavirus disease 2019-associated coagulopathy and acute lung injury highlighted in a patient with copresentation of acute myelocytic leukemia:a case report[J].A A Pract,2021,15(4):e1432.
[8] 王艳芝,谭榜云,李琳,等. 急性白血病患者化疗后骨髓抑制期血浆凝血因子Ⅷ水平及其对出血事件的影响[J].中华血液学杂志,2020,41(1):59-63.
[9] 中华医学会血液学分会白血病淋巴瘤学组. 成人急性髓系白血病(非急性早幼粒细胞白血病)中国诊疗指南(2017年版)[J].中华血液学杂志,2017,38(3):177-182.
[10] 张之南,沈悌. 血液病诊断及疗效标准[M].3版.北京:科学出版社,2007.
[11] 侯明,秦平. 成人原发免疫性血小板减少症诊治的中国专家共识(2016版)解读[J].临床血液学杂志,2016,29(4):523-527.
[12] 李静,张养民,陈丽娜,等. 血栓弹力图对急性白血病患者出血风险的评估及诊断价值[J].中国医刊,2019,54(3):263-266.
[13] 董娟,陈永玲,邹惠安,等. F11 rs2289252基因多态性与急性白血病患者出血相关性分析[J].微循环学杂志,2019,29(1):28-32.
[14] ALI S,DUNMORE H M,KARRES D,et al. The EMA review of mylotarg (Gemtuzumab Ozogamicin) for the treatment of acute myeloid leukemia[J].Oncologist,2019,24(5):e171-e179.