Literature DB >> 27197308

A New Triglycyl Peptide Linker for Antibody-Drug Conjugates (ADCs) with Improved Targeted Killing of Cancer Cells.

Rajeeva Singh1, Yulius Y Setiady2, Jose Ponte2, Yelena V Kovtun2, Katharine C Lai2, E Erica Hong2, Nathan Fishkin2, Ling Dong2, Gregory E Jones2, Jennifer A Coccia2, Leanne Lanieri2, Karen Veale2, Juliet A Costoplus2, Anna Skaletskaya2, Rabih Gabriel2, Paulin Salomon2, Rui Wu2, Qifeng Qiu2, Hans K Erickson2, John M Lambert2, Ravi V J Chari2, Wayne C Widdison1.   

Abstract

A triglycyl peptide linker (CX) was designed for use in antibody -: drug conjugates (ADC), aiming to provide efficient release and lysosomal efflux of cytotoxic catabolites within targeted cancer cells. ADCs comprising anti-epithelial cell adhesion molecule (anti-EpCAM) and anti-EGFR antibodies with maytansinoid payloads were prepared using CX or a noncleavable SMCC linker (CX and SMCC ADCs). The in vitro cytotoxic activities of CX and SMCC ADCs were similar for several cancer cell lines; however, the CX ADC was more active (5-100-fold lower IC50) than the SMCC ADC in other cell lines, including a multidrug-resistant line. Both CX and SMCC ADCs showed comparable MTDs and pharmacokinetics in CD-1 mice. In Calu-3 tumor xenografts, antitumor efficacy was observed with the anti-EpCAM CX ADC at a 5-fold lower dose than the corresponding SMCC ADC in vivo Similarly, the anti-EGFR CX ADC showed improved antitumor activity over the respective SMCC conjugate in HSC-2 and H1975 tumor models; however, both exhibited similar activity against FaDu xenografts. Mechanistically, in contrast with the charged lysine-linked catabolite of SMCC ADC, a significant fraction of the carboxylic acid catabolite of CX ADC could be uncharged in the acidic lysosomes, and thus diffuse out readily into the cytosol. Upon release from tumor cells, CX catabolites are charged at extracellular pH and do not penetrate and kill neighboring cells, similar to the SMCC catabolite. Overall, these data suggest that CX represents a promising linker option for the development of ADCs with improved therapeutic properties. Mol Cancer Ther; 15(6); 1311-20. ©2016 AACR. ©2016 American Association for Cancer Research.

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Year:  2016        PMID: 27197308     DOI: 10.1158/1535-7163.MCT-16-0021

Source DB:  PubMed          Journal:  Mol Cancer Ther        ISSN: 1535-7163            Impact factor:   6.261


  8 in total

1.  Expanding the Reach of Antibody-Drug Conjugates.

Authors:  Ravi V J Chari
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Journal:  Sci Rep       Date:  2022-06-10       Impact factor: 4.996

Review 3.  Advances in Liver Cancer Stem Cell Isolation and their Characterization.

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Review 4.  Antibody-Drug Conjugates (ADCs) for Personalized Treatment of Solid Tumors: A Review.

Authors:  John M Lambert; Charles Q Morris
Journal:  Adv Ther       Date:  2017-03-30       Impact factor: 3.845

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Review 6.  Antibody-drug conjugates: Recent advances in linker chemistry.

Authors:  Zheng Su; Dian Xiao; Fei Xie; Lianqi Liu; Yanming Wang; Shiyong Fan; Xinbo Zhou; Song Li
Journal:  Acta Pharm Sin B       Date:  2021-04-06       Impact factor: 11.413

7.  Synthesis and Evaluation of Small Molecule Drug Conjugates Harnessing Thioester-Linked Maytansinoids.

Authors:  Chen-Fu Lo; Tai-Yu Chiu; Yu-Tzu Liu; Li-Rung Huang; Teng-Kuang Yeh; Kuan-Hsun Huang; Kuan-Liang Liu; Chia-Yu Hsu; Ming-Yu Fang; Yu-Chen Huang; Tsu-An Hsu; Chiung-Tong Chen; Lun Kelvin Tsou
Journal:  Pharmaceutics       Date:  2022-06-21       Impact factor: 6.525

Review 8.  Recent Developments in ADC Technology: Preclinical Studies Signal Future Clinical Trends.

Authors:  Penelope M Drake; David Rabuka
Journal:  BioDrugs       Date:  2017-12       Impact factor: 5.807

  8 in total

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