接受中等剂量持续输注白细胞介素-2治疗的患者发生中心静脉置管相关感染和血栓形成

Central venous device-related infection and thrombosis in patients treated with moderate dose continuous-infusion interleukin-2.

作者信息

Eastman M E, Khorsand M, Maki D G, Williams E C, Kim K, Sondel P M, Schiller J H, Albertini M R

机构信息

Department of Medicine, University of Wisconsin, Madison, WI 53792, USA.

出版信息

Cancer. 2001 Feb 15;91(4):806-14.

PMID:11241250

Abstract

BACKGROUND

This study was performed to determine the incidence of central venous device-related blood stream infection and thrombosis in patients treated with moderate dose continuous-infusion interleukin-2 (IL-2).

METHODS

The records of 160 consecutive patients treated at the University of Wisconsin Hospital and Clinics, between June 1990 and June 1997, with moderate dose continuous-infusion IL-2 (IL-2 [1.5-3.0 x 10(6) U/m(2)/day] Hoffman-LaRoche, Nutley, NJ or IL-2 [4.5 x 10(6) U/m(2)/day] Chiron Corporation, Berkley, CA) were reviewed retrospectively. The majority of patients had metastatic melanoma (78 patients) or renal cell carcinoma (70 patients). All of the patients had a surgically implanted central venous device placed before starting IL-2 therapy; 89% of these were cuffed Hickman catheters. Eighty-four patients received 1 mg of warfarin per day as prophylaxis against device-related thrombosis; none received periinsertion prophylactic antibiotics.

RESULTS

Twenty-one patients (13%) developed central venous device-related bloodstream infection (DRBSI) during the study period, a rate of 2 DRBSI per 1000 device-days. DRBSIs were associated with the type of immunotherapy given with IL-2 (P = 0.01) and with thrombosis (odds ratio, 4.1; 95% confidence interval, 1.5-11.4; P = 0.008) but not with patient gender, type of cancer, duration of the central device, or site of device placement. Twenty-six patients (16%) developed central venous device-related thrombosis (DRT) during immunotherapy. Low dose warfarin did not appear to prevent thrombosis. Device-related thrombosis was associated with DRBSI but not with patient gender, type of cancer, type of device, duration or location of device, or concomitant immunotherapy.

CONCLUSIONS

Central venous DRBSI and DRT are significant complications that can occur during moderate dose continuous-infusion IL-2 therapy. The risk of DRBSI appears lower than the risk reported with high dose IL-2 therapy by previous investigators. The risk of DRT appears to be higher than the risk reported for patients with similar devices but not given IL-2. Low dose warfarin did not prevent DRT when started after device placement.

摘要

背景

本研究旨在确定接受中等剂量持续输注白细胞介素-2（IL-2）治疗的患者中心静脉置管相关血流感染和血栓形成的发生率。

方法

回顾性分析1990年6月至1997年6月在威斯康星大学医院和诊所连续接受治疗的160例患者的记录，这些患者接受中等剂量持续输注IL-2（IL-2[1.5 - 3.0×10(6) U/m(2)/天]，霍夫曼-罗氏公司，新泽西州纽特里；或IL-2[4.5×10(6) U/m(2)/天]，基龙公司，加利福尼亚州伯克利）治疗。大多数患者患有转移性黑色素瘤（78例）或肾细胞癌（70例）。所有患者在开始IL-2治疗前均通过手术植入中心静脉置管；其中89%为带袖套的希克曼导管。84例患者每天接受1毫克华法林以预防置管相关血栓形成；无人接受置管时预防性使用抗生素。

结果

在研究期间，21例患者（13%）发生了中心静脉置管相关血流感染（DRBSI），发生率为每1000个置管日2例DRBSI。DRBSI与IL-2联合使用的免疫治疗类型有关（P = 0.01），与血栓形成有关（比值比，4.1；95%置信区间，1.5 - 11.4；P = 0.008），但与患者性别、癌症类型、中心静脉置管持续时间或置管部位无关。26例患者（16%）在免疫治疗期间发生了中心静脉置管相关血栓形成（DRT）。低剂量华法林似乎不能预防血栓形成。置管相关血栓形成与DRBSI有关，但与患者性别、癌症类型、置管类型、置管持续时间或部位以及联合免疫治疗无关。