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Synthesis and evaluation of pyrrolobenzodiazepine dimer antibody-drug conjugates with dual β-glucuronide and dipeptide triggers
被引:13
作者:

Gregson, Stephen J.
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QMB Innovat Ctr, Spirogen, 42 New Rd, London E1 2AX, England QMB Innovat Ctr, Spirogen, 42 New Rd, London E1 2AX, England

Barrett, Allison M.
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AstraZeneca, One MedImmune Way, Gaithersburg, MD 20878 USA QMB Innovat Ctr, Spirogen, 42 New Rd, London E1 2AX, England

Patel, Neki V.
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QMB Innovat Ctr, Spirogen, 42 New Rd, London E1 2AX, England QMB Innovat Ctr, Spirogen, 42 New Rd, London E1 2AX, England

Kang, Gyoung-Dong
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QMB Innovat Ctr, Spirogen, 42 New Rd, London E1 2AX, England QMB Innovat Ctr, Spirogen, 42 New Rd, London E1 2AX, England

Schiavone, Davide
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AstraZeneca, Granta Pk, Cambridge CB21 6GH, England QMB Innovat Ctr, Spirogen, 42 New Rd, London E1 2AX, England

Sult, Erin
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AstraZeneca, One MedImmune Way, Gaithersburg, MD 20878 USA QMB Innovat Ctr, Spirogen, 42 New Rd, London E1 2AX, England

Barry, Conor S.
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QMB Innovat Ctr, Spirogen, 42 New Rd, London E1 2AX, England QMB Innovat Ctr, Spirogen, 42 New Rd, London E1 2AX, England

Vijayakrishnan, Balakumar
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QMB Innovat Ctr, Spirogen, 42 New Rd, London E1 2AX, England QMB Innovat Ctr, Spirogen, 42 New Rd, London E1 2AX, England

Adams, Lauren R.
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QMB Innovat Ctr, Spirogen, 42 New Rd, London E1 2AX, England QMB Innovat Ctr, Spirogen, 42 New Rd, London E1 2AX, England

Masterson, Luke A.
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QMB Innovat Ctr, Spirogen, 42 New Rd, London E1 2AX, England QMB Innovat Ctr, Spirogen, 42 New Rd, London E1 2AX, England

D'Hooge, Francois
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QMB Innovat Ctr, Spirogen, 42 New Rd, London E1 2AX, England QMB Innovat Ctr, Spirogen, 42 New Rd, London E1 2AX, England

Snaith, Mike
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AstraZeneca, Granta Pk, Cambridge CB21 6GH, England QMB Innovat Ctr, Spirogen, 42 New Rd, London E1 2AX, England

Harper, Jay
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AstraZeneca, One MedImmune Way, Gaithersburg, MD 20878 USA QMB Innovat Ctr, Spirogen, 42 New Rd, London E1 2AX, England

Hartley, John A.
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QMB Innovat Ctr, Spirogen, 42 New Rd, London E1 2AX, England QMB Innovat Ctr, Spirogen, 42 New Rd, London E1 2AX, England

Howard, Philip W.
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h-index: 0
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QMB Innovat Ctr, Spirogen, 42 New Rd, London E1 2AX, England QMB Innovat Ctr, Spirogen, 42 New Rd, London E1 2AX, England
机构:
[1] QMB Innovat Ctr, Spirogen, 42 New Rd, London E1 2AX, England
[2] AstraZeneca, One MedImmune Way, Gaithersburg, MD 20878 USA
[3] AstraZeneca, Granta Pk, Cambridge CB21 6GH, England
关键词:
Antibody-drug conjugate;
beta-Glucuronidase;
Prodrug;
Pyrrolobenzodiazepine;
Serum stability;
SPECTRUM ANTITUMOR-ACTIVITY;
CROSS-LINKING AGENT;
IN-VITRO EVALUATION;
SJG-136;
NSC-694501;
SELECTIVE THERAPY;
PRODRUG;
CANCER;
POTENT;
EFFICACY;
DESIGN;
D O I:
10.1016/j.ejmech.2019.06.044
中图分类号:
R914 [药物化学];
学科分类号:
100701 ;
摘要:
Antibody-drug conjugates (ADCs) containing pyrrolobenzodiazepine (PBD) dimers are currently being evaluated in human oncology clinical trials with encouraging results. To further improve the therapeutic window, next-generation PBD drug-linker design has focused on the inclusion of additional tumor-selective triggers and use of lower-potency PBDs. beta-Glucuronidase is a well-known target for discovery prodrugs due to increased presence in tumor cells and microenvironment. In this study, a beta-glucuronidase cleavable cap was investigated at the PBD NW-position and compared with corresponding free imine ADCs. SG3600 (glucuronide) ADCs showed in vitro and in vivo efficacy/tolerability comparable to SG3400 (imine) ADCs, and good 50% inhibitory concentration differentials were observed in vitro between control non-antigen-targeted ADCs and targeted ADCs. Dependence on beta-glucuronidase for SG3600 activity was demonstrated through CRISPRCas9 knockdown studies and addition of exogenous beta-glucuronidase. SG3600 showed better serum stability, improved conjugation efficiency and was able to reach high drug-to-antibody ratio without aggregation. (C) 2019 Elsevier Masson SAS. All rights reserved.
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页码:591 / 607
页数:17
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