Janik J, Kopp W C, Smith J W, Longo D L, Alvord W G, Sharfman W H, Fenton R G, Sznol M, Steis R G, Creekmore S P
Biological Response Modifiers Program, Program Resources, Inc/DynCorp, National Cancer Institute-Frederick Cancer Research and Development Center, MD.
J Clin Oncol. 1993 Jan;11(1):125-35. doi: 10.1200/JCO.1993.11.1.125.
This phase I study was conducted to determine the maximum-tolerated dose (MTD) and the immunologic properties of levamisole in cancer patients when administered alone and in combination with interferon gamma (IFN-gamma).
Twenty patients with advanced cancer and 36 patients with completely resected melanoma (n = 33) or renal cell cancer (n = 3) received levamisole orally every other day for six doses at 1.0, 2.5, 5.0, or 10.0 mg/kg. Ten days later, patients restarted levamisole and began IFN-gamma 0.1 mg/m2 by subcutaneous injection every other day. Blood samples were collected for measurement of neopterin and soluble interleukin-2 receptor (sIL-2R), and for flow-cytometric analysis.
The MTD of levamisole was 5 mg/kg, and this was not changed by the addition of IFN-gamma. Dose-related increases in serum levels of neopterin and sIL-2R were noted. Multiple doses of > or = 5 mg/kg of levamisole were required to elicit immune changes, which were more prominent in patients with minimal tumor burdens. Increased expression of CD64 and class I and class II major histocompatibility antigens on monocytes was also observed. The combination of IFN-gamma and levamisole did not result in greater immunologic effects than those observed in previous trials of IFN-gamma alone.
Levamisole induces dose-related immunologic changes in patients with large or minimal tumor burdens. These changes may be involved in the beneficial effects noted in recent adjuvant trials of levamisole. Ongoing clinical trials should correlate immune changes with response, and trials exploring different schedules of administration using higher, more immunologically active, doses of levamisole should be performed.
本I期研究旨在确定单独使用及与γ干扰素(IFN-γ)联合使用时,左旋咪唑在癌症患者中的最大耐受剂量(MTD)及其免疫特性。
20例晚期癌症患者以及36例黑色素瘤完全切除患者(n = 33)或肾细胞癌患者(n = 3)每隔一天口服一次左旋咪唑,共六剂,剂量分别为1.0、2.5、5.0或10.0mg/kg。十天后,患者重新开始服用左旋咪唑,并开始每隔一天皮下注射0.1mg/m²的IFN-γ。采集血样以检测新蝶呤和可溶性白细胞介素-2受体(sIL-2R),并进行流式细胞术分析。
左旋咪唑的MTD为5mg/kg,添加IFN-γ后未发生改变。观察到新蝶呤和sIL-2R血清水平呈剂量相关增加。需要多次服用≥5mg/kg的左旋咪唑才能引发免疫变化,在肿瘤负荷最小的患者中这种变化更为显著。还观察到单核细胞上CD64以及I类和II类主要组织相容性抗原的表达增加。IFN-γ与左旋咪唑联合使用并未产生比先前单独使用IFN-γ的试验中观察到的更大免疫效应。
左旋咪唑在肿瘤负荷大或小的患者中均可诱导剂量相关的免疫变化。这些变化可能与近期左旋咪唑辅助试验中观察到的有益效果有关。正在进行的临床试验应将免疫变化与反应相关联,并且应该进行探索使用更高、免疫活性更强的剂量的左旋咪唑的不同给药方案的试验。
