Reyno L M, Egorin M J, Eisenberger M A, Sinibaldi V J, Zuhowski E G, Sridhara R
Division of Medical Oncology, University of Maryland Cancer Center, Baltimore 21201, USA.
J Clin Oncol. 1995 Sep;13(9):2187-95. doi: 10.1200/JCO.1995.13.9.2187.
We used population pharmacokinetic-parameter estimates and designed a fixed dosing schedule to maintain plasma suramin concentrations between 100 and 300 micrograms/mL and then evaluated its performance.
On day 1, patients received a 200-mg test dose and 1,000-mg/m2 loading dose. On days 2, 3, 4, and 5, patients received 1-hour infusions of 400, 300, 250, and 200 mg/m2, respectively. Subsequent 1-hour infusions of 275 mg/m2 were given on days 8, 11, 15, 19, 22, 29, 36, 43, 50, 57, 67, and 78. Therapy was discontinued for dose-limiting toxicity (DLT) or progressive disease (PD). Patients were to be removed from the fixed dosing schedule if, after day 5, three consecutive peak plasma suramin concentrations were greater than 300 micrograms/mL.
Forty-two patients, including 40 with hormone-refractory prostate cancer (HRPC), received 700 infusions. Forty patients were assessable for toxicity; 38 were assessable for response. Two patients with preexisting pulmonary disease died early of respiratory insufficiency. Treatment was discontinued in five patients due to DLT and in seven due to PD. No patient had treatment discontinued due to repeated peak plasma suramin concentrations > or = 300 micrograms/mL. The fixed dosing schedule was precise, unbiased, and well tolerated. DLT consisted of grade 4 nephrotoxicity (n = 2), neurotoxicity (n = 2), and corticosteroid-induced psychosis (n = 1). Three patients, who received all 18 doses of suramin per protocol, developed severe, but not dose-limiting, malaise, fatigue, and lethargy. Twenty-four of 36 assessable patients with elevated serum prostate-specific antigen (PSA) levels had a > or = 50% reduction, lasting more than 4 weeks, and 18 had a > or = 75% reduction, lasting more than 4 weeks. Twelve of 23 (52%) symptomatic HRPC patients noted a subjective improvement in pain. There were no measurable responses in four patients with measurable disease. The estimated median survival time in 38 assessable patients with HRPC was 18.8 months. The estimated median time to progression in 35 patients, for whom data were available, was 10.1 months.
This easily implemented schedule allowed suramin to be administered safely as an intermittent bolus injection. Toxicity was manageable and reversible.
我们使用群体药代动力学参数估计值并设计了一个固定给药方案,以维持苏拉明血浆浓度在100至300微克/毫升之间,然后评估其效果。
第1天,患者接受200毫克试验剂量和1000毫克/平方米的负荷剂量。在第2、3、4和5天,患者分别接受400、300、250和200毫克/平方米的1小时静脉输注。随后在第8、11、15、19、22、29、36、43、50、57、67和78天给予275毫克/平方米的1小时静脉输注。因剂量限制性毒性(DLT)或疾病进展(PD)而停止治疗。如果在第5天后,连续三次血浆苏拉明峰值浓度大于300微克/毫升,则将患者从固定给药方案中剔除。
42例患者,包括40例激素难治性前列腺癌(HRPC)患者,接受了700次输注。40例患者可评估毒性;38例可评估反应。2例原有肺部疾病的患者因呼吸功能不全早期死亡。5例患者因DLT停止治疗,7例因PD停止治疗。没有患者因血浆苏拉明峰值浓度反复≥300微克/毫升而停止治疗。固定给药方案精确、无偏差且耐受性良好。DLT包括4级肾毒性(n = 2)、神经毒性(n = 2)和皮质类固醇诱发的精神病(n = 1)。3例按照方案接受了全部18剂苏拉明的患者出现了严重但非剂量限制性的不适、疲劳和嗜睡。36例血清前列腺特异性抗原(PSA)水平升高的可评估患者中,24例PSA水平降低≥50%,持续超过4周,18例降低≥75%,持续超过4周。23例有症状的HRPC患者中有12例(52%)主观疼痛有所改善。4例有可测量疾病的患者没有可测量的反应。38例可评估的HRPC患者的估计中位生存时间为18.8个月。35例有可用数据的患者的估计中位进展时间为10.1个月。
这个易于实施的方案允许将苏拉明作为间歇性推注安全给药。毒性可控且可逆。
