Phase I/II Clinical Trial of Weekly Intraperitoneal Paclitaxel (IP-PTX) with Monthly Intravenous Carboplatin (IV-CBDCA) for Minimal Residual Disease of Ovarian, Tubal, and Peritoneal Carcinoma

Journal of Cancer Biology and Therapeutics Pub Date : 2019-06-11 DOI:10.18314/GJCT.V5I1.1809

T. S, Terai Y, Tanimura K, Miyamoto T, Omichi M, Takeuchi K

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Abstract

We conducted weekly intraperitoneal administration of paclitaxel (IP-PTX) with monthly intravenous administration of carboplatin (IV-CBDCA), as a prospective phase 1/2 setting. The purpose of this study was to assess the pharmacokinetics and to decide the recommended dose (RD) according to modified Fibonacci method. Patients aged 20-75 years old with histological confirmed mullerian cancers (epithelial ovarian cancer; EOC, fallopian tubal cancer; FTC, and primary peritoneal cancer; PPC) from stage IC to IV or the patients with recurrent disease with small residual disease (including retention of ascetic fluid, para-aortic nodes recurrence after optimal debulked after interval debulking surgery; IDS) were eligible. The protocol regimen consisted of IP-PTX on day1 (D1), 8, and 15, at a starting dose level 1(DL1) of 45 mg/m2, with 15 mg/ m2 incremental, and IV-CBDCA was fixed dose AUC 5.0 mg/mL.min on D1, monthly. The accrual period was from August 2000 until September 2005. As for result, twelve patients were enrolled. No dose limiting toxicity (DLT) was observed in DL1. In dose level 2 (DL2, 60 mg/m2), one grade 3 (G3) hypersensitive reaction to CBDCA was detected. Further 5 patients had been enrolled but additional DLT was not identified. The RD was decided as DL2, which was the same dose of RD in weekly IP-PTX reported by Francis et al. The serum AUCs of PTX in DL1 and DL2 were 1605 nM.min and 2365 nM.min, respectively. By serum CA125, five complete responses were observed out of 8 evaluable patients by Rustin’s criteria. In conclusion, the combination of weekly IP-PTX and monthly IV-CBDCA at AUC 5.0 mg/mL.min was feasible and the recommended dose of IP-PTX was 60 mg/m2. The therapy was moderate effective for optimal debulking mullerian carcinomas. From our pharmacokinetic results, as for the patients with extra-pelvic lesions, additional IV-PTX would be necessary like GOG 172 experimental arm.

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每周一次腹腔注射紫杉醇(IP-PTX)联合每月静脉注射卡铂(IV-CBDCA)治疗卵巢、输卵管和腹膜癌微小残留疾病的I/II期临床试验

作为前瞻性1/2期研究，我们每周腹腔注射紫杉醇(IP-PTX)，每月静脉注射卡铂(IV-CBDCA)。本研究的目的是根据改进的斐波那契方法评估药代动力学并确定推荐剂量(RD)。年龄20-75岁组织学证实的苗勒管癌(上皮性卵巢癌;EOC，输卵管癌;FTC和原发性腹膜癌;PPC)从IC期到IV期或复发性疾病伴小残留疾病(包括腹水潴留、间隔减容手术后最佳减容后主动脉旁淋巴结复发)的患者;IDS)均符合条件。方案方案包括IP-PTX在第1天(D1)，第8天和第15天，起始剂量水平1(DL1)为45 mg/m2，增量为15 mg/m2, IV-CBDCA为固定剂量AUC 5.0 mg/mL。D1上的最小值，每月。应计期间为2000年8月至2005年9月。结果12例患者入组。DL1未见剂量限制性毒性(DLT)。在剂量水平2 (DL2, 60 mg/m2)下，检测到1例CBDCA 3级(G3)超敏反应。另外5名患者入组，但没有发现额外的DLT。确定RD为DL2，与Francis等报道的每周IP-PTX中RD的剂量相同。PTX在DL1和DL2的AUCs为1605 nM。min和2365 nM。分别为最小值。经血清CA125检测，8例可按Rustin标准评估的患者中有5例完全缓解。综上所述，每周使用IP-PTX和每月使用IV-CBDCA, AUC为5.0 mg/mL。min可行，IP-PTX推荐剂量为60 mg/m2。该疗法对最佳减体积苗勒管癌效果中等。从我们的药代动力学结果来看，对于盆腔外病变的患者，像GOG 172实验组一样，需要额外的IV-PTX。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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Journal of Cancer Biology and Therapeutics

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