Koppe Manuel J, Oyen Wim J G, Bleichrodt Robert P, Verhofstad Albert A, Goldenberg David M, Boerman Otto C
Department of Surgery, Radboud University Nijmegen Medical Center, Nijmegen, The Netherlands.
Cancer Biother Radiopharm. 2006 Oct;21(5):506-14. doi: 10.1089/cbr.2006.21.506.
Gemcitabine has been shown to exert a radiosensitizing effect in various epithelial cancers. The aim of the present studies was to investigate whether the efficacy of radioimmunotherapy (RIT) using the (131)I-labeled anti-CEA monoclonal antibody (MAb) MN-14 could be enhanced by coadministration of gemcitabine in nude mice with small (1-3 mm) peritoneal metastases of colonic origin.
Firstly, the maximum tolerated dose (MTD) of gemcitabine was determined, when administered intraperitoneally at two different dosing schedules (0.11-3.0 mg/mouse/administration on days 0, 3, 6, and 9, or 0.022-0.60 mg/mouse/administration on days 0, 1, 2, 3, and 4). In two separate therapy studies in which these two administration regimens were applied, the efficacy of gemcitabine monotherapy was compared to that of RIT alone (125 muCi (131)I-MN-14/mouse) or RIT combined with gemcitabine.
When administered every 3rd day for a total of 4 administrations, or daily for 5 consecutive days, the gemcitabine was considered safe at 0.33 mg/mouse/administration and 0.066 mg/mouse/administration, respectively. In the first therapy study, median survival of the control mice was 39 days. Gemcitabine monotherapy at 0.11 mg or 0.33 mg/mouse/administration every 3rd day (total, 4 administrations) resulted in a median survival of 52 and 57 days, respectively (p = 0.0003, compared to controls). RIT alone resulted in a median survival of 66 days (p < 0.0001, compared to controls). The combination of RIT and gemcitabine coadministration resulted in a median survival of 73 and 94 days, respectively (p = 0.12, for trend). In the second therapy study, median survival of the control mice was 48 days, which was similar to the median survival of the mice treated with daily administrations of gemcitabine monotherapy at 0.022 mg/mouse/administration on 5 consecutive days (49 days; p = 0.17). RIT alone resulted in a significantly improved median survival of 66 days (p= = 0.0010, compared to controls). Combination therapy using RIT and gemcitabine resulted in a median survival of 64 days, which did not differ significantly from the survival of the mice treated with RIT alone (p = 0.43).
At the dose regimens employed, gemcitabine did not enhance the efficacy of RIT of experimental small-volume peritoneal carcinomatosis of colonic origin.
吉西他滨已被证明在多种上皮性癌症中具有放射增敏作用。本研究的目的是探讨在患有小(1 - 3毫米)结肠源性腹膜转移瘤的裸鼠中,联合使用吉西他滨是否能增强使用(131)I标记的抗CEA单克隆抗体(MAb)MN - 14的放射免疫疗法(RIT)的疗效。
首先,确定吉西他滨的最大耐受剂量(MTD),采用两种不同的给药方案经腹腔给药(第0、3、6和9天,0.11 - 3.0毫克/小鼠/次给药;或第0、1、2、3和4天,0.022 - 0.60毫克/小鼠/次给药)。在两项分别应用这两种给药方案的治疗研究中,将吉西他滨单药治疗的疗效与单独使用RIT(125微居里(131)I - MN - 14/小鼠)或RIT联合吉西他滨的疗效进行比较。
当每3天给药1次,共给药4次,或连续5天每日给药时,吉西他滨在剂量分别为0.33毫克/小鼠/次和0.066毫克/小鼠/次时被认为是安全的。在第一项治疗研究中,对照小鼠的中位生存期为39天。每3天以0.11毫克或0.33毫克/小鼠/次给药(共4次给药)的吉西他滨单药治疗导致中位生存期分别为52天和57天(与对照组相比,p = 0.0003)。单独使用RIT导致中位生存期为66天(与对照组相比,p < 0.0001)。RIT与吉西他滨联合给药导致中位生存期分别为73天和94天(趋势p = 0.12)。在第二项治疗研究中,则对照小鼠的中位生存期为48天,这与连续5天每日以0.022毫克/小鼠/次进行吉西他滨单药治疗的小鼠的中位生存期(49天;p = 0.17)相似。单独使用RIT导致中位生存期显著提高至66天(与对照组相比,p = 0.0010)。使用RIT和吉西他滨的联合治疗导致中位生存期为64天,与单独接受RIT治疗的小鼠的生存期无显著差异(p = 0.43)。
在所采用的剂量方案下,吉西他滨并未增强对实验性小体积结肠源性腹膜癌病的RIT疗效。
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