Bang Soo-Mee, Lee Jae Hoon, Yoon Sung-Soo, Park Seonyang, Min Chang-Ki, Kim Chun-Choo, Suh Cheolwon, Sohn Sang Kyun, Min Yoo-Hong, Lee Je-Jung, Kim Kihyun, Seong Chu-Myong, Yoon Hwi-Joong, Cho Kyung Sam, Jo Deog-Yeon, Lee Kyung Hee, Lee Na-Ri, Kim Chul Soo
Gachon Medical School, Incheon, Korea.
Int J Hematol. 2006 May;83(4):309-13. doi: 10.1532/IJH97.A30512.
The proteasome inhibitor bortezomib has demonstrated clinical activity in patients with multiple myeloma (MM). Adverse events, including thrombocytopenia and peripheral neuropathy, have affected 30% to 60% of patients overall, and interrupted therapy in 10% to 20%. No prior toxicity data are available for Asian patients who have used bortezomib for MM. We used National Cancer Institute Common Terminology Criteria for Adverse Events, version 3.0, to review the clinical records of patients with an MM diagnosis from 25 centers in Korea. The included patients were treated with bortezomib alone or in combination with other agents, including thalidomide. Ninety-five MM patients were treated. The patients had a median age of 60 years (range, 42-77 years). The median number of previous treatments was 3 (range, 0-10), and 39% of the patients had been treated with 4 or more major classes of agents, including thalidomide (67%), and autologous stem cell transplantation (51%). Regimens included bortezomib only in 38 patients (40%), bortezomib plus dexamethasone in 34 patients (36%), and bortezomib plus a thalidomide-containing regimen in 23 patients (24%). The analysis of patient response to therapy revealed a complete response (CR) or a near-CR in 31 patients (33%) and a partial response in 30 patients (32%), for an objective response rate of 65% in 93 patients. The most common adverse events reported were thrombocytopenia (47%), sensory neuropathy (42%), anemia (31%), and leukopenia (31%). Thirteen patients (14%) stopped therapy because of adverse events (neuropathy, 8; infection, 4; diarrhea, 1). Neuropathy greater than grade 2 was more frequent in patients who received 4 or more prior therapy regimens (17/37) than in those who received 3 or fewer (14/58). In addition, therapy including thalidomide was significantly correlated with neuropathy of grades 1 to 3 (P = .001). We identified 6 therapy-related deaths (6%) within 20 days after the last dose of bortezomib. The causes of death were infection in 3 patients, disease progression in 2 patients, and suicide in 1 patient. The incidences of thrombocytopenia and neurotoxicity were similar; however, gastrointestinal toxicities were relatively low in Korean patients compared with those reported in Western studies. Significant neuropathy was associated with the number of prior regimens and combination with thalidomide. These findings provide useful information for clinicians and patients using bortezomib.
蛋白酶体抑制剂硼替佐米已在多发性骨髓瘤(MM)患者中展现出临床活性。不良事件,包括血小板减少症和周围神经病变,总体上影响了30%至60%的患者,并有10%至20%的患者中断治疗。此前尚无使用硼替佐米治疗MM的亚洲患者的毒性数据。我们采用美国国立癌症研究所不良事件通用术语标准3.0版,回顾了韩国25个中心诊断为MM的患者的临床记录。纳入的患者接受了单独的硼替佐米治疗或与其他药物联合治疗,包括沙利度胺。95例MM患者接受了治疗。患者的中位年龄为60岁(范围42 - 77岁)。既往治疗的中位次数为3次(范围0 - 10次),39%的患者接受过4种或更多主要类型的药物治疗,包括沙利度胺(67%)和自体干细胞移植(51%)。治疗方案包括仅用硼替佐米的38例患者(40%)、硼替佐米加地塞米松的34例患者(36%)以及硼替佐米加含沙利度胺方案的23例患者(24%)。对患者治疗反应的分析显示,31例患者(33%)达到完全缓解(CR)或接近CR,30例患者(32%)达到部分缓解,93例患者的客观缓解率为65%。报告的最常见不良事件为血小板减少症(47%)、感觉神经病变(42%)、贫血(31%)和白细胞减少症(31%)。13例患者(14%)因不良事件停止治疗(神经病变,8例;感染,4例;腹泻,1例)。接受4种或更多既往治疗方案的患者(17/37)中2级以上神经病变比接受3种或更少治疗方案的患者(14/58)更常见。此外,含沙利度胺的治疗与1至3级神经病变显著相关(P = .001)。我们在最后一剂硼替佐米后20天内确定了6例与治疗相关的死亡(6%)。死亡原因分别为感染3例、疾病进展2例和自杀1例。血小板减少症和神经毒性的发生率相似;然而,与西方研究报道相比,韩国患者的胃肠道毒性相对较低。显著的神经病变与既往治疗方案的数量以及与沙利度胺联合使用有关。这些发现为使用硼替佐米的临床医生和患者提供了有用信息。
