DNA sequence-selective G-A cross-linking ADC payloads for use in solid tumour therapies

George Procopiou; Paul J.M. Jackson; Daniella di Mascio; Jennifer L. Auer; Chris Pepper; Khondaker Miraz Rahman; Keith R. Fox; David E. Thurston

doi:10.1038/s42003-022-03633-0

DNA sequence-selective G-A cross-linking ADC payloads for use in solid tumour therapies

George Procopiou, Paul J.M. Jackson, Daniella di Mascio, Jennifer L. Auer, Chris Pepper, Khondaker Miraz Rahman, Keith R. Fox, David E. Thurston

Institute of Pharmaceutical Science

Research output: Contribution to journal › Article › peer-review

2 Citations (Scopus)

Abstract

Antibody-Drug Conjugates (ADCs) are growing in importance for the treatment of both solid and haematological malignancies. There is a demand for new payloads with novel mechanisms of action that may offer enhanced therapeutic efficacy, especially in patients who develop resistance. We report here a class of Cyclopropabenzindole-Pyridinobenzodiazepine (CBI-PDD) DNA cross-linking payloads that simultaneously alkylate guanine (G) and adenine (A) bases in the DNA minor groove with a defined sequence selectivity. The lead payload, FGX8-46 (6), produces sequence-selective G-A cross-links and affords cytotoxicity in the low picomolar region across a panel of 11 human tumour cell lines. When conjugated to the antibody cetuximab at an average Drug-Antibody Ratio (DAR) of 2, an ADC is produced with significant antitumour activity at 1 mg/kg in a target-relevant human tumour xenograft mouse model with an unexpectedly high tolerability (i.e., no weight loss observed at doses as high as 45 mg/kg i.v., single dose).

Original language	English
Article number	741
Pages (from-to)	741
Number of pages	1
Journal	Communications Biology
Volume	5
Issue number	1
DOIs	https://doi.org/10.1038/s42003-022-03633-0
Publication status	Published - 29 Jul 2022

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title = "DNA sequence-selective G-A cross-linking ADC payloads for use in solid tumour therapies",

abstract = "Antibody-Drug Conjugates (ADCs) are growing in importance for the treatment of both solid and haematological malignancies. There is a demand for new payloads with novel mechanisms of action that may offer enhanced therapeutic efficacy, especially in patients who develop resistance. We report here a class of Cyclopropabenzindole-Pyridinobenzodiazepine (CBI-PDD) DNA cross-linking payloads that simultaneously alkylate guanine (G) and adenine (A) bases in the DNA minor groove with a defined sequence selectivity. The lead payload, FGX8-46 (6), produces sequence-selective G-A cross-links and affords cytotoxicity in the low picomolar region across a panel of 11 human tumour cell lines. When conjugated to the antibody cetuximab at an average Drug-Antibody Ratio (DAR) of 2, an ADC is produced with significant antitumour activity at 1 mg/kg in a target-relevant human tumour xenograft mouse model with an unexpectedly high tolerability (i.e., no weight loss observed at doses as high as 45 mg/kg i.v., single dose).",

author = "George Procopiou and Jackson, {Paul J.M.} and {di Mascio}, Daniella and Auer, {Jennifer L.} and Chris Pepper and Rahman, {Khondaker Miraz} and Fox, {Keith R.} and Thurston, {David E.}",

note = "Funding Information: All authors except C.P. are either paid employees/consultants (G.P., P.J.M.J., D.E.T.) or recipients of grants funded by Femtogenix Ltd (D.d.M, K.R.F.). G.P., P.J.M.J., K.M.R and D.E.T. hold shares and/or share options in the company. C.P declares no competing interests. Publisher Copyright: {\textcopyright} 2022, The Author(s).",

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AU - Jackson, Paul J.M.

AU - di Mascio, Daniella

AU - Auer, Jennifer L.

AU - Pepper, Chris

AU - Rahman, Khondaker Miraz

AU - Fox, Keith R.

AU - Thurston, David E.

N1 - Funding Information: All authors except C.P. are either paid employees/consultants (G.P., P.J.M.J., D.E.T.) or recipients of grants funded by Femtogenix Ltd (D.d.M, K.R.F.). G.P., P.J.M.J., K.M.R and D.E.T. hold shares and/or share options in the company. C.P declares no competing interests. Publisher Copyright: © 2022, The Author(s).

PY - 2022/7/29

Y1 - 2022/7/29

N2 - Antibody-Drug Conjugates (ADCs) are growing in importance for the treatment of both solid and haematological malignancies. There is a demand for new payloads with novel mechanisms of action that may offer enhanced therapeutic efficacy, especially in patients who develop resistance. We report here a class of Cyclopropabenzindole-Pyridinobenzodiazepine (CBI-PDD) DNA cross-linking payloads that simultaneously alkylate guanine (G) and adenine (A) bases in the DNA minor groove with a defined sequence selectivity. The lead payload, FGX8-46 (6), produces sequence-selective G-A cross-links and affords cytotoxicity in the low picomolar region across a panel of 11 human tumour cell lines. When conjugated to the antibody cetuximab at an average Drug-Antibody Ratio (DAR) of 2, an ADC is produced with significant antitumour activity at 1 mg/kg in a target-relevant human tumour xenograft mouse model with an unexpectedly high tolerability (i.e., no weight loss observed at doses as high as 45 mg/kg i.v., single dose).

AB - Antibody-Drug Conjugates (ADCs) are growing in importance for the treatment of both solid and haematological malignancies. There is a demand for new payloads with novel mechanisms of action that may offer enhanced therapeutic efficacy, especially in patients who develop resistance. We report here a class of Cyclopropabenzindole-Pyridinobenzodiazepine (CBI-PDD) DNA cross-linking payloads that simultaneously alkylate guanine (G) and adenine (A) bases in the DNA minor groove with a defined sequence selectivity. The lead payload, FGX8-46 (6), produces sequence-selective G-A cross-links and affords cytotoxicity in the low picomolar region across a panel of 11 human tumour cell lines. When conjugated to the antibody cetuximab at an average Drug-Antibody Ratio (DAR) of 2, an ADC is produced with significant antitumour activity at 1 mg/kg in a target-relevant human tumour xenograft mouse model with an unexpectedly high tolerability (i.e., no weight loss observed at doses as high as 45 mg/kg i.v., single dose).

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DNA sequence-selective G-A cross-linking ADC payloads for use in solid tumour therapies

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