Cornett Wendy R, McCall Linda M, Petersen Rebecca P, Ross Merrick I, Briele Henry A, Noyes R Dirk, Sussman Jeffrey J, Kraybill William G, Kane John M, Alexander H Richard, Lee Jeffrey E, Mansfield Paul F, Pingpank James F, Winchester David J, White Richard L, Chadaram Vijaya, Herndon James E, Fraker Douglas L, Tyler Douglas S
The University of Texas M.D. Anderson Cancer Center, Houston, TX, USA.
J Clin Oncol. 2006 Sep 1;24(25):4196-201. doi: 10.1200/JCO.2005.05.5152.
To determine in a randomized prospective multi-institutional trial whether the addition of tumor necrosis factor alpha (TNF-alpha) to a melphalan-based hyperthermic isolated limb perfusion (HILP) treatment would improve the complete response rate for locally advanced extremity melanoma.
Patients with locally advanced extremity melanoma were randomly assigned to receive melphalan or melphalan plus TNF-alpha during standard HILP. Patient randomization was stratified according to disease/treatment status and regional nodal disease status.
The intervention was completed in 124 patients of the 133 enrolled. Grade 4 adverse events were observed in 14 (12%) of 129 patients, with three (4%) of 64 in the melphalan-alone arm and 11 (16%) of 65 in the melphalan-plus-TNF-alpha arm (P = .0436). There were two toxicity-related lower extremity amputations in the melphalan-plus-TNF-alpha arm, and one disease progression-related upper extremity amputation in the melphalan-alone arm. There was no treatment-related mortality in either arm of the study. One hundred sixteen patients were assessable at 3 months postoperatively. Sixty-four percent of patients (36 of 58) in the melphalan-alone arm and 69% of patients (40 of 58) in the melphalan-plus-TNF-alpha arm showed a response to treatment at 3 months, with a complete response rate of 25% (14 of 58 patients) in the melphalan-alone arm and 26% (15 of 58 patients) in the melphalan-plus-TNF-alpha arm (P = .435 and P = .890, respectively).
In locally advanced extremity melanoma treated with HILP, the addition of TNF-alpha to melphalan did not demonstrate a significant enhancement of short-term response rates over melphalan alone by the 3-month follow-up, and TNF-alpha plus melphalan was associated with a higher complication rate.
在一项随机前瞻性多机构试验中,确定在基于美法仑的热灌注隔离肢体治疗(HILP)中添加肿瘤坏死因子α(TNF-α)是否会提高局部晚期肢体黑色素瘤的完全缓解率。
局部晚期肢体黑色素瘤患者在标准HILP期间被随机分配接受美法仑或美法仑加TNF-α治疗。患者随机分组根据疾病/治疗状态和区域淋巴结疾病状态进行分层。
133名入组患者中有124名完成了干预。129名患者中有14名(12%)出现4级不良事件,美法仑单药组64名患者中有3名(4%),美法仑加TNF-α组65名患者中有11名(16%)(P = 0.0436)。美法仑加TNF-α组有2例与毒性相关的下肢截肢,美法仑单药组有1例与疾病进展相关的上肢截肢。研究的两组均无治疗相关死亡。术后3个月有116名患者可评估。美法仑单药组64%(58名中的36名)患者和美法仑加TNF-α组69%(58名中的40名)患者在3个月时显示对治疗有反应,美法仑单药组完全缓解率为25%(58名患者中的14名),美法仑加TNF-α组为26%(58名患者中的15名)(分别为P = 0.435和P = 0.890)。
在接受HILP治疗的局部晚期肢体黑色素瘤中,在美法仑基础上加用TNF-α在3个月随访时未显示出比单用美法仑显著提高短期缓解率,且TNF-α加美法仑与更高的并发症发生率相关。
