Lorus Therapeutics Inc., 2 Meridian Road., Toronto, ON M9W 4Z7, Canada.
Cancer Chemother Pharmacol. 2011 Jul;68(1):193-205. doi: 10.1007/s00280-010-1473-z. Epub 2010 Oct 1.
GTI-2040, a 20-mer phosphorothioate oligonucleotide, was designed to hybridize to the mRNA sequence of human ribonucleotide reductase R2. GTI-2040 has been shown to inhibit human cancer cell proliferation by downregulation of R2 expression in vitro and to significantly inhibit tumor growth in xenograft models of human cancer in mice. As part of the safety evaluation for human clinical trials, the toxicity and toxicokinetics of GTI-2040 were determined in Sprague-Dawley rats and rhesus monkeys.
GTI-2040 was administered to rats at 2, 10, and 50 mg/kg/day by bolus intravenous injection every second day for 21 days with a 21-day recovery. In monkeys, an acute study was performed with single, escalating doses of GTI-2040 ranging from 10 to 80 mg/kg given as a 24-h continuous intravenous infusion. As well, a 21-day, continuous intravenous infusion study with GTI-2040 was conducted in monkeys at 2, 10, and 50 mg/kg/day, with a 3-week recovery. Blood sampling was done to measure GTI-2040 plasma concentrations, metabolites, and pharmacokinetic parameters, and tissues were collected to assess the distribution of GTI-2040 and/or metabolites.
The toxicities of GTI-2040 in both rats and monkeys were typical for the phosphorothioate oligonucleotide class of compounds. In monkeys, there was a dose-related increase in GTI-2040 plasma levels with concomitant increase in complement activation and prolongation of activated partial thromboplastin time. In both rats and monkeys, the tissues having the highest concentrations of GTI-2040 (kidney, liver, spleen) had the largest dose-related toxic effects. Adverse effects were diminished or absent in the recovery animals.
GTI-2040 was well tolerated when infused over 24 h at doses up to 80 mg/kg in monkeys. In rats and monkeys, GTI-2040 was reasonably well tolerated and showed reversible toxicities when administered at doses up to 50 mg/kg/day for 21 days. The no observed adverse effect dose level for GTI-2040 in both animal species was 2 mg/kg/day. There were no apparent sequence-specific effects related to the interaction of GTI-2040 with the R2 component of the mRNA expressing ribonucleotide reductase.
GTI-2040 是一种 20 个碱基的硫代磷酸寡核苷酸,设计用于与人类核核苷酸还原酶 R2 的 mRNA 序列杂交。体外实验表明,GTI-2040 通过下调 R2 表达抑制人类癌细胞增殖,并显著抑制荷瘤小鼠中人类癌症的肿瘤生长。作为人体临床试验安全性评估的一部分,在 Sprague-Dawley 大鼠和恒河猴中确定了 GTI-2040 的毒性和毒代动力学。
在大鼠中,GTI-2040 以 2、10 和 50mg/kg/天的剂量通过每两天静脉注射一次 21 天,21 天恢复期。在猴子中,进行了单次递增剂量的急性研究,GTI-2040 的剂量范围为 10 至 80mg/kg,连续 24 小时静脉输注。此外,在猴子中进行了为期 21 天的连续静脉输注研究,GTI-2040 的剂量为 2、10 和 50mg/kg/天,恢复期为 3 周。采集血样以测量 GTI-2040 血浆浓度、代谢物和药代动力学参数,并采集组织以评估 GTI-2040 和/或代谢物的分布。
GTI-2040 在大鼠和猴子中的毒性均为典型的硫代磷酸寡核苷酸类化合物。在猴子中,随着 GTI-2040 血浆水平的剂量相关性增加,补体激活增加,活化部分凝血活酶时间延长。在大鼠和猴子中,GTI-2040 浓度最高的组织(肾脏、肝脏、脾脏)具有最大的剂量相关性毒性作用。在恢复期动物中,不良反应减轻或消失。
在猴子中,GTI-2040 以高达 80mg/kg 的剂量连续 24 小时输注时耐受性良好。在大鼠和猴子中,GTI-2040 以高达 50mg/kg/天的剂量连续 21 天给药时耐受性良好,表现出可逆毒性。在这两种动物物种中,GTI-2040 的无观察到不良效应剂量水平为 2mg/kg/天。没有明显的与 GTI-2040 与表达核核苷酸还原酶的 mRNA 的 R2 成分相互作用相关的序列特异性效应。
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