National Institute of Neoplastic Diseases (INEN), Lima, Peru.
Anticancer Drugs. 2012 Mar;23(3):335-41. doi: 10.1097/CAD.0b013e32834e74d6.
The objective of the study was to evaluate the safety, pharmacokinetics, and antitumor activity of ispinesib, a kinesin spindle protein inhibitor. Patients with locally advanced or metastatic breast cancer who had received only prior neoadjuvant or adjuvant chemotherapy were treated with escalating doses of ispinesib administered as a 1-h infusion on days 1 and 15 every 28 days until toxicity or progression of disease. Doses were escalated until dose-limiting toxicity was observed in two out of six patients during cycle 1. A total of 16 patients were treated at three dose levels: 10 mg/m (n=3), 12 mg/m (n=6), and 14 mg/m (n=7). Forty-four percent of the patients had locally advanced disease and 56% had metastatic disease; 50% were estrogen receptor positive, 44% were progesterone receptor positive, 25% human epidermal growth factor 2 were positive, and 31% triple (estrogen receptor, progesterone receptor, human epidermal growth factor 2) negative. Sixty-nine percent of patients were chemo-naive. The maximum tolerated dose was 12 mg/m and dose-limiting toxicity was grade 3 increased aspartate aminotransferase and alanine aminotransferase. The most common toxicities included neutropenia (88%; 38% grade 3 and 44% grade 4), increased alanine aminotransferase (56%), anemia (38%), increased aspartate aminotransferase (31%), and diarrhea (31%). No neuropathy, mucositis, or alopecia was reported. Among the 15 patients evaluable for antitumor activity, there were three partial responses, one confirmed by the response evaluation criteria in solid tumors (7% response rate). Nine patients (60%) had stable disease lasting at least 42 days, with four (27%) lasting for at least 90 days. Disease stabilization (partial responses+stable disease) was observed in 11 (73.3%) patients. In conclusion, ispinesib was well tolerated when administered on days 1 and 15 every 28 days. Limited activity was observed with this schedule in patients with previously untreated advanced breast cancer.
研究目的在于评估伊匹司他(一种驱动蛋白纺锤体蛋白抑制剂)的安全性、药代动力学和抗肿瘤活性。入组患者为既往仅接受过新辅助或辅助化疗的局部晚期或转移性乳腺癌患者,采用伊匹司他 1 小时静脉输注,剂量爬坡,第 1 天和第 15 天给药,每 28 天为一个周期,直至毒性或疾病进展。当 1 个周期内 6 例患者中有 2 例出现剂量限制性毒性时,即停止剂量递增。共 16 例患者接受了 3 个剂量水平的治疗:10mg/m2(n=3)、12mg/m2(n=6)和 14mg/m2(n=7)。44%的患者为局部晚期疾病,56%的患者为转移性疾病;50%的患者雌激素受体阳性,44%的孕激素受体阳性,25%的患者人类表皮生长因子 2 阳性,31%的患者三重(雌激素受体、孕激素受体、人类表皮生长因子 2)阴性。69%的患者为化疗初治。最大耐受剂量为 12mg/m2,剂量限制性毒性为 3 级氨基转移酶升高。最常见的毒性包括中性粒细胞减少症(88%;38%为 3 级,44%为 4 级)、丙氨酸氨基转移酶升高(56%)、贫血(38%)、天门冬氨酸氨基转移酶升高(31%)和腹泻(31%)。未报告神经病变、粘膜炎或脱发。在 15 例可评估抗肿瘤活性的患者中,有 3 例部分缓解,其中 1 例经实体瘤反应评价标准确认(7%的缓解率)。9 例(60%)患者疾病稳定至少 42 天,其中 4 例(27%)至少稳定 90 天。11 例(73.3%)患者疾病稳定(部分缓解+疾病稳定)。结论:伊匹司他在第 1 天和第 15 天,每 28 天给药,耐受性良好。在未经治疗的晚期乳腺癌患者中,该方案观察到有限的活性。
