Chen Christine I, Kouroukis C Tom, White Darrell, Voralia Michael, Stadtmauer Edward, Stewart A Keith, Wright John J, Powers Jean, Walsh Wendy, Eisenhauer Elizabeth
Princess Margaret Hospital, Toronto, Ontario, Canada.
J Clin Oncol. 2007 Apr 20;25(12):1570-5. doi: 10.1200/JCO.2006.07.8659. Epub 2007 Mar 12.
To evaluate the efficacy and toxicity of single-agent bortezomib in Waldenström's macroglobulinemia (WM).
Symptomatic WM patients, untreated or previously treated, received bortezomib 1.3 mg/m2 intravenously days 1, 4, 8, and 11 on a 21-day cycle until two cycles past complete response (CR), stable disease (SD) attained, progression (PD), or unacceptable toxicity. Responses were based on both paraprotein levels and bidimensional disease measurements.
Twenty-seven patients were enrolled. A median of six cycles (range, two to 39) of bortezomib were administered. Twenty-one patients had a decrease in immunoglobulin M (IgM) of at least 25%, with 12 patients (44%) reaching at least 50% IgM reduction. Using both IgM and bidimensional criteria, responses included seven partial responses (PRs; 26%), 19 SDs (70%), and one PD (4%). Total response rate was 26%. IgM reductions were prompt, with nodal responses lagging. Hemoglobin levels increased by at least 10 g/L in 18 patients (66%). Most nonhematologic toxicities were grade 1 to 2, but 20 patients (74%) developed new or worsening peripheral neuropathy (five patients with grade 3, no grade 4), a common cause for dose reduction. Onset of neuropathy was within two to four cycles and reversible in the majority. Hematologic toxicities included grade 3 to 4 thrombocytopenia in eight patients (29.6%) and neutropenia in five (19%). Toxicity led to treatment discontinuation in 12 patients (44%), most commonly because of neuropathy.
Bortezomib has efficacy in WM, but neurotoxicity can be dose limiting. The slower response in nodal disease may require prolonged therapy, perhaps with a less intensive dosing schedule to avoid early discontinuation because of toxicity. Future studies of bortezomib in combination with other agents are warranted.
评估单药硼替佐米治疗华氏巨球蛋白血症(WM)的疗效和毒性。
有症状的WM患者,无论未经治疗或先前接受过治疗,均接受硼替佐米1.3mg/m²静脉注射,于第1、4、8和11天给药,每21天为一个周期,直至达到完全缓解(CR)、疾病稳定(SD)、疾病进展(PD)或出现不可接受的毒性后两个周期。疗效基于副蛋白水平和二维疾病测量结果。
入组27例患者。硼替佐米的给药中位周期数为6个周期(范围为2至39个周期)。21例患者的免疫球蛋白M(IgM)降低至少25%,其中12例患者(44%)的IgM降低至少50%。根据IgM和二维标准,疗效包括7例部分缓解(PR;26%)、19例疾病稳定(SD;70%)和1例疾病进展(PD;4%)。总缓解率为26%。IgM迅速降低,淋巴结反应滞后。18例患者(66%)的血红蛋白水平至少升高10g/L。大多数非血液学毒性为1至2级,但20例患者(74%)出现新的或加重的周围神经病变(5例为3级,无4级),这是剂量减少的常见原因。神经病变在2至4个周期内出现,大多数情况下可逆转。血液学毒性包括8例患者(29.6%)出现3至4级血小板减少和5例患者(19%)出现中性粒细胞减少。毒性导致12例患者(44%)停止治疗,最常见的原因是神经病变。
硼替佐米对WM有效,但神经毒性可能限制剂量。淋巴结疾病的反应较慢可能需要延长治疗时间,或许采用强度较低的给药方案以避免因毒性而早期停药。有必要对硼替佐米与其他药物联合进行进一步研究。
