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不同给药方案中氟嘧啶的心脏毒性:一项前瞻性研究。

Cardiotoxicity of fluoropyrimidines in different schedules of administration: a prospective study.

作者信息

Kosmas Christos, Kallistratos Manolis S, Kopterides Petros, Syrios John, Skopelitis Helias, Mylonakis Nicolaos, Karabelis Athanasios, Tsavaris Nicolas

机构信息

Department of Medicine, 2nd Division of Medical Oncology, "Metaxa" Cancer Hospital, Piraues, 21 Apolloniou Street, 16341 Athens, Greece.

出版信息

J Cancer Res Clin Oncol. 2008 Jan;134(1):75-82. doi: 10.1007/s00432-007-0250-9. Epub 2007 Jul 17.

Abstract

BACKGROUND

Cardiotoxicity associated with 5-Fluorouracil (5FU) administration has been infrequently reported in literature, albeit various series of acute coronary syndromes have recorded a low but definite incidence of the above toxicity. In the present study, patients undergoing 5FU-based and oral capecitabine (Xeloda-based chemotherapy were tested for the potential development of cardiac-related symptoms during their administration.

PATIENTS AND METHODS

Six hundred and forty-four patients entered the study. Those experiencing any cardiac-related symptoms during 5FU infusion or oral capecitabine were subjected to ECG and serum cardiac enzymes determination. If cardiotoxicity was confirmed, 5FU infusion or oral capecitabine were interrupted, sublingual nitrates administered and cardiac monitoring initiated, while patients with >two-fold enzyme elevation were followed in a coronary care unit for at least 72 h. Cases with acute myocardial infarction were excluded from further 5FU or oral capecitabine treatment.

RESULTS

Overall 26 patients (4.03%) developed symptoms and/or ECG abnormalities due to 5FU and capecitabine. Patients with continuous 5FU infusion presented a higher incidence of cardiotoxicity [14/209; 6.7%, 95% confidence interval (CI) = 3.3-10.1%] than the remaining (7/317; 2.3%, 95% CI = 0.8-3.3%) (P < 0.012). Specifically, an increased incidence of cardiac-related events was encountered in patients with continuous 24-h 5FU + LV infusion for 5 days (12.5%, 95% CI = 2.3-22.7%) rather than in patients with the same schedule without LV (5.3%, 95% CI = 1.95-8.67%) (P < 0.027), as well as in patients with short 5FU + LV administration (2.4%, 95% CI = 0.9-3.9%) (P < 0.019). Overall, 3/54 patients (5.5%, 95% CI = -0.6-11.1%) on oral capecitabine developed cardiac-related events. Seven out of the 20 patients suffered an acute myocardial infarction, 6 developed ischemia only, while 4 more patients had ECG consistent with coronary vasospasm and 3 with conduction disturbances, of which one subsequently died. Patients administered oral capecitabine had a similar incidence of cardiac-related events; 1/22 (4.5%) patients with advanced breast cancer and 2/32 (6.2%) with colorectal cancer.

CONCLUSIONS

The present study supports the toxic effect of 5-FU on the myocardium, which is largely schedule-dependent, whereas a low but finite risk of such toxicity has been observed with oral capecitabine. A high level of alertness is required when using fluoropyrimidines (i.v. 5FU or oral capecitabine), while their toxic effect on the coronary endothelium and myocardium merits further investigation.

摘要

背景

尽管各类急性冠状动脉综合征系列研究记录了与5-氟尿嘧啶(5FU)给药相关的心脏毒性发生率较低但确切存在,但文献中对此类心脏毒性的报道并不常见。在本研究中,对接受基于5FU和口服卡培他滨(希罗达)化疗的患者在给药期间发生心脏相关症状的可能性进行了检测。

患者与方法

644例患者进入本研究。在5FU静脉输注或口服卡培他滨期间出现任何心脏相关症状的患者接受心电图和血清心肌酶测定。如果确诊为心脏毒性,则中断5FU静脉输注或口服卡培他滨,给予舌下含服硝酸盐并开始心脏监测,而酶升高超过两倍的患者在冠心病监护病房至少随访72小时。急性心肌梗死患者被排除在进一步的5FU或口服卡培他滨治疗之外。

结果

总体而言,26例患者(4.03%)因5FU和卡培他滨出现症状和/或心电图异常。持续静脉输注5FU的患者心脏毒性发生率[14/209;6.7%,95%置信区间(CI)=3.3 - 10.1%]高于其余患者(7/317;2.3%,95%CI = 0.8 - 3.3%)(P < 0.012)。具体而言,连续24小时5FU + 左亚叶酸钙输注5天的患者心脏相关事件发生率增加(12.5%,95%CI = 2.3 - 22.7%),高于相同给药方案但无左亚叶酸钙的患者(5.3%,95%CI = 1.95 - 8.67%)(P < 0.027),以及5FU + 左亚叶酸钙短期给药的患者(2.4%,95%CI = 0.9 - 3.9%)(P < 0.019)。总体而言,口服卡培他滨的54例患者中有3例(5.5%,95%CI = -0.6 - 11.1%)发生心脏相关事件。20例患者中有7例发生急性心肌梗死,6例仅出现缺血,另有4例患者心电图符合冠状动脉痉挛,3例有传导障碍,其中1例随后死亡。接受口服卡培他滨治疗的患者心脏相关事件发生率相似;晚期乳腺癌患者中1/22(4.5%),结直肠癌患者中2/32(6.2%)。

结论

本研究支持5 - FU对心肌的毒性作用,这种毒性在很大程度上取决于给药方案,而口服卡培他滨也存在低但有限的此类毒性风险。使用氟嘧啶(静脉注射5FU或口服卡培他滨)时需要高度警惕,而它们对冠状动脉内皮和心肌的毒性作用值得进一步研究。

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