喜树碱
结合
化学
抗体-药物偶联物
抗体
单克隆抗体
体外
细胞毒性
序号38
生物
作者
Ryan Lyski,Lauren Bou,Uland Y. Lau,David W. Meyer,Julia H. Cochran,Nicole M. Okeley,Kim K. Emmerton,Francisco Zapata,Jessica K. Simmons,Esther S. Trueblood,David Ortiz,Margo Zaval,Katie Snead,Steven Jin,Lauren Farr,Maureen Ryan,Peter D. Senter,Scott C. Jeffrey
出处
期刊:Molecular Cancer Therapeutics
[American Association for Cancer Research]
日期:2021-02-01
卷期号:20 (2): 329-339
标识
DOI:10.1158/1535-7163.mct-20-0526
摘要
We have developed a highly active and well-tolerated camptothecin (CPT) drug-linker designed for antibody-mediated drug delivery in which the lead molecule consists of a 7-aminomethyl-10,11-methylenedioxy CPT (CPT1) derivative payload attached to a novel hydrophilic protease-cleavable valine-lysine-glycine tripeptide linker. A defined polyethylene glycol stretcher was included to improve the properties of the drug-linker, facilitating high antibody-drug conjugate (ADC) drug loading, while reducing the propensity for aggregation. A CPT1 ADC with 8 drug-linkers/mAb displayed a pharmacokinetic profile coincident with parental unconjugated antibody and had high serum stability. The ADCs were broadly active against cancer cells in vitro and in mouse xenograft models, giving tumor regressions and complete responses at low (≤3 mg/kg, single administration) doses. Pronounced activities were obtained in both solid and hematologic tumor models and in models of bystander killing activity and multidrug resistance. Payload release studies demonstrated that two CPTs, CPT1 and the corresponding glycine analog (CPT2), were released from a cAC10 ADC by tumor cells. An ADC containing this drug-linker was well tolerated in rats at 60 mg/kg, given weekly four times. Thus, ADCs comprised of this valine-lysine-glycine linker with CPT drug payloads have promise in targeted drug delivery.
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