UMR7292 GICC CNRS-Université de Tours, Team IMT, 31 Avenue Monge, 37200 Tours, France.
Org Biomol Chem. 2018 Mar 14;16(11):1882-1889. doi: 10.1039/c7ob02780j.
Herein we describe the synthesis and evaluation of four novel HER2-targeting, cathepsin B-sensitive antibody-drug conjugates bearing a monomethylauristatin E (MMAE) cytotoxic payload, constructed via the conjugation of cleavable linkers to trastuzumab using a site-specific bioconjugation methodology. These linkers vary by both cleavable trigger motif and hydrophilicity, containing one of two cathepsin B sensitive dipeptides (Val-Cit and Val-Ala), and engendered with either hydrophilic or hydrophobic character via application of a PEG spacer. Through evaluation of physical properties, in vitro cytotoxicity, and receptor affinity of the resulting antibody-drug conjugates (ADCs), we have demonstrated that while both dipeptide triggers are effective, the increased hydrophobicity of the Val-Ala pair limits its utility within this type of linker. In addition, while PEGylation augments linker hydrophilicity, this change does not translate to more favourable ADC hydrophilicity or potency. While all described structures demonstrated excellent and similar in vitro cytotoxicity, the ADC with the ValCitPABMMAE linker shows the most promising combination of in vitro potency, structural homogeneity, and hydrophilicity, warranting further evaluation into its therapeutic potential.
在此,我们描述了四种新型 HER2 靶向、组织蛋白酶 B 敏感的抗体药物偶联物的合成和评估,这些偶联物通过使用特异性生物缀合方法将可切割接头连接到曲妥珠单抗上,携带单甲基奥瑞他汀 E(MMAE)细胞毒性有效载荷。这些接头在可切割触发基序和亲水性方面各不相同,包含两种组织蛋白酶 B 敏感二肽(缬氨酸-瓜氨酸和缬氨酸-丙氨酸)中的一种,并通过应用 PEG 间隔物赋予亲水性或疏水性。通过评估所得抗体药物偶联物(ADC)的物理性质、体外细胞毒性和受体亲和力,我们证明了虽然两种二肽触发物都有效,但 Val-Ala 对的增加疏水性限制了其在这种类型接头中的应用。此外,虽然 PEG 化增加了接头的亲水性,但这种变化并没有转化为更有利的 ADC 亲水性或效力。虽然所有描述的结构都表现出优异的体外细胞毒性,但具有 ValCitPABMMAE 接头的 ADC 表现出最有前途的体外效力、结构均一性和亲水性组合,值得进一步评估其治疗潜力。
