Hong E Erica, Erickson Hans, Lutz Robert J, Whiteman Kathleen R, Jones Gregory, Kovtun Yelena, Blanc Veronique, Lambert John M
†ImmunoGen, Inc., 830 Winter Street, Waltham, Massachusetts 02451, United States.
§Sanofi, 13 quai Jules Guesde, Vitry sur Seine, 94403 France.
Mol Pharm. 2015 Jun 1;12(6):1703-16. doi: 10.1021/acs.molpharmaceut.5b00175. Epub 2015 Apr 27.
Coltuximab ravtansine (SAR3419) is an antibody-drug conjugate (ADC) targeting CD19 created by conjugating a derivative of the potent microtubule-acting cytotoxic agent, maytansine, to a version of the anti-CD19 antibody, anti-B4, that was humanized as an IgG1 by variable domain resurfacing. Four different linker-maytansinoid constructs were synthesized (average ∼3.5 maytansinoids/antibody for each) to evaluate the impact of linker-payload design on the activity of the maytansinoid-ADCs targeting CD19. The ADC composed of DM4 (N(2')-deacetyl-N(2')-[4-mercapto-4-methyl-1-oxopentyl]maytansine) conjugated to antibody via the N-succinimidyl-4-(2-pyridyldithio)butyrate (SPDB) linker was selected for development as SAR3419. A molar ratio for DM4/antibody of between 3 and 5 was selected for the final design of SAR3419. Evaluation of SAR3419 in Ramos tumor xenograft models showed that the minimal effective single dose was about 50 μg/kg conjugated DM4 (∼2.5 mg/kg conjugated antibody), while twice this dose gave complete regressions in 100% of the mice. SAR3419 arrests cells in the G2/M phase of the cell cycle, ultimately leading to apoptosis after about 24 h. The results of in vitro and in vivo studies with SAR3419 made with DM4 that was [(3)H]-labeled at the C20 methoxy group of the maytansinoid suggest a mechanism of internalization and intracellular trafficking of SAR3419, ultimately to lysosomes, in which the antibody is fully degraded, releasing lysine-N(ε)-SPDB-DM4 as the initial metabolite. Subsequent intracellular reduction of the disulfide bond between linker and DM4 generates the free thiol species, which is then converted to S-methyl DM4 by cellular methyl transferase activity. We provide evidence to suggest that generation of S-methyl DM4 in tumor cells may contribute to in vivo tumor eradication via bystander killing of neighboring tumor cells. Furthermore, we show that S-methyl DM4 is converted to the sulfoxide and sulfone derivatives in the liver, suggesting that hepatic catabolism of the payload to less cytotoxic maytansinoid species contributes to the overall therapeutic window of SAR3419. This compound is currently in phase II clinical evaluation for the treatment of diffuse large B cell lymphoma.
科图昔单抗拉凡他辛(SAR3419)是一种靶向CD19的抗体药物偶联物(ADC),它通过将强效微管作用细胞毒性剂美登素的衍生物与抗CD19抗体抗B4的一个版本偶联而成,该抗B4抗体通过可变域重铺技术人源化为IgG1。合成了四种不同的连接子-美登素类似物构建体(每种平均约3.5个美登素类似物/抗体),以评估连接子-载荷设计对靶向CD19的美登素类似物-ADC活性的影响。由DM4(N(2')-去乙酰基-N(2')-[4-巯基-4-甲基-1-氧代戊基]美登素)通过N-琥珀酰亚胺基-4-(2-吡啶二硫基)丁酸酯(SPDB)连接子与抗体偶联而成的ADC被选为SAR3419进行开发。在SAR3419的最终设计中,DM4/抗体的摩尔比选择为3至5。在拉莫斯肿瘤异种移植模型中对SAR3419的评估表明,最小有效单剂量约为50μg/kg偶联的DM4(约2.5mg/kg偶联的抗体),而该剂量的两倍可使100%的小鼠完全消退。SAR3419使细胞停滞在细胞周期的G2/M期,最终在约24小时后导致细胞凋亡。用在美登素类似物的C20甲氧基处用[(3)H]标记的DM4对SAR3419进行的体外和体内研究结果表明,SAR3419的内化和细胞内运输机制最终是进入溶酶体,在溶酶体中抗体被完全降解,释放出赖氨酸-N(ε)-SPDB-DM4作为初始代谢产物。随后连接子与DM4之间的二硫键在细胞内还原生成游离硫醇物种,然后通过细胞甲基转移酶活性将其转化为S-甲基DM4。我们提供的证据表明,肿瘤细胞中S-甲基DM4的生成可能通过对邻近肿瘤细胞的旁观者杀伤作用促进体内肿瘤的根除。此外,我们表明S-甲基DM向肝脏中的亚砜和砜衍生物转化,这表明载荷在肝脏中分解代谢为细胞毒性较小的美登素类似物物种有助于SAR3419的整体治疗窗。该化合物目前正在进行治疗弥漫性大B细胞淋巴瘤的II期临床评估。
