Potent Cyclic Peptide Inhibitors of FXIIa Discovered by mRNA Display with Genetic Code Reprogramming

Daniel J. Ford; Nisharnthi M. Duggan; Sarah E. Fry; Jorge Ripoll-Rozada; Stijn M. Agten; Wenyu Liu; Leo Corcilius; Tilman M. Hackeng; Rene Van Oerle; Henri M.H. Spronk; Anneliese S. Ashhurst; Vishnu Mini Sasi; Joe A. Kaczmarski; Colin J. Jackson; Pedro José Barbosa Pereira; Toby Passioura; Hiroaki Suga; Richard J. Payne

doi:10.1021/acs.jmedchem.1c00651

Potent Cyclic Peptide Inhibitors of FXIIa Discovered by mRNA Display with Genetic Code Reprogramming

Daniel J. Ford, Nisharnthi M. Duggan, Sarah E. Fry, Jorge Ripoll-Rozada, Stijn M. Agten, Wenyu Liu, Leo Corcilius, Tilman M. Hackeng, Rene Van Oerle, Henri M.H. Spronk, Anneliese S. Ashhurst, Vishnu Mini Sasi, Joe A. Kaczmarski, Colin J. Jackson, Pedro José Barbosa Pereira, Toby Passioura, Hiroaki Suga, Richard J. Payne^*

^*Corresponding author for this work

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

15 Citations (Scopus)

Abstract

The contact system comprises a series of serine proteases that mediate procoagulant and proinflammatory activities via the intrinsic pathway of coagulation and the kallikrein-kinin system, respectively. Inhibition of Factor XIIa (FXIIa), an initiator of the contact system, has been demonstrated to lead to thrombo-protection and anti-inflammatory effects in animal models and serves as a potentially safer target for the development of antithrombotics. Herein, we describe the use of the Randomised Nonstandard Peptide Integrated Discovery (RaPID) mRNA display technology to identify a series of potent and selective cyclic peptide inhibitors of FXIIa. Cyclic peptides were evaluated in vitro, and three lead compounds exhibited significant prolongation of aPTT, a reduction in thrombin generation, and an inhibition of bradykinin formation. We also describe our efforts to identify the critical residues for binding FXIIa through alanine scanning, analogue generation, and via in silico methods to predict the binding mode of our lead cyclic peptide inhibitors.

Original language	English
Pages (from-to)	7853-7876
Number of pages	24
Journal	Journal of Medicinal Chemistry
Volume	64
Issue number	11
DOIs	https://doi.org/10.1021/acs.jmedchem.1c00651
Publication status	Published - 10 Jun 2021

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Ford, D. J., Duggan, N. M., Fry, S. E., Ripoll-Rozada, J., Agten, S. M., Liu, W., Corcilius, L., Hackeng, T. M., Van Oerle, R., Spronk, H. M. H., Ashhurst, A. S., Mini Sasi, V., Kaczmarski, J. A., Jackson, C. J., Pereira, P. J. B., Passioura, T., Suga, H., & Payne, R. J. (2021). Potent Cyclic Peptide Inhibitors of FXIIa Discovered by mRNA Display with Genetic Code Reprogramming. Journal of Medicinal Chemistry, 64(11), 7853-7876. https://doi.org/10.1021/acs.jmedchem.1c00651

@article{00c34211aba1467ab4abaf872d3b3d63,

title = "Potent Cyclic Peptide Inhibitors of FXIIa Discovered by mRNA Display with Genetic Code Reprogramming",

abstract = "The contact system comprises a series of serine proteases that mediate procoagulant and proinflammatory activities via the intrinsic pathway of coagulation and the kallikrein-kinin system, respectively. Inhibition of Factor XIIa (FXIIa), an initiator of the contact system, has been demonstrated to lead to thrombo-protection and anti-inflammatory effects in animal models and serves as a potentially safer target for the development of antithrombotics. Herein, we describe the use of the Randomised Nonstandard Peptide Integrated Discovery (RaPID) mRNA display technology to identify a series of potent and selective cyclic peptide inhibitors of FXIIa. Cyclic peptides were evaluated in vitro, and three lead compounds exhibited significant prolongation of aPTT, a reduction in thrombin generation, and an inhibition of bradykinin formation. We also describe our efforts to identify the critical residues for binding FXIIa through alanine scanning, analogue generation, and via in silico methods to predict the binding mode of our lead cyclic peptide inhibitors.",

author = "Ford, \{Daniel J.\} and Duggan, \{Nisharnthi M.\} and Fry, \{Sarah E.\} and Jorge Ripoll-Rozada and Agten, \{Stijn M.\} and Wenyu Liu and Leo Corcilius and Hackeng, \{Tilman M.\} and \{Van Oerle\}, Rene and Spronk, \{Henri M.H.\} and Ashhurst, \{Anneliese S.\} and \{Mini Sasi\}, Vishnu and Kaczmarski, \{Joe A.\} and Jackson, \{Colin J.\} and Pereira, \{Pedro Jos{\'e} Barbosa\} and Toby Passioura and Hiroaki Suga and Payne, \{Richard J.\}",

note = "Publisher Copyright: {\textcopyright} 2021 American Chemical Society.",

year = "2021",

month = jun,

day = "10",

doi = "10.1021/acs.jmedchem.1c00651",

language = "English",

volume = "64",

pages = "7853--7876",

journal = "Journal of Medicinal Chemistry",

issn = "0022-2623",

publisher = "American Chemical Society",

number = "11",

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Ford, DJ, Duggan, NM, Fry, SE, Ripoll-Rozada, J, Agten, SM, Liu, W, Corcilius, L, Hackeng, TM, Van Oerle, R, Spronk, HMH, Ashhurst, AS, Mini Sasi, V, Kaczmarski, JA, Jackson, CJ, Pereira, PJB, Passioura, T, Suga, H & Payne, RJ 2021, 'Potent Cyclic Peptide Inhibitors of FXIIa Discovered by mRNA Display with Genetic Code Reprogramming', Journal of Medicinal Chemistry, vol. 64, no. 11, pp. 7853-7876. https://doi.org/10.1021/acs.jmedchem.1c00651

TY - JOUR

T1 - Potent Cyclic Peptide Inhibitors of FXIIa Discovered by mRNA Display with Genetic Code Reprogramming

AU - Ford, Daniel J.

AU - Duggan, Nisharnthi M.

AU - Fry, Sarah E.

AU - Ripoll-Rozada, Jorge

AU - Agten, Stijn M.

AU - Liu, Wenyu

AU - Corcilius, Leo

AU - Hackeng, Tilman M.

AU - Van Oerle, Rene

AU - Spronk, Henri M.H.

AU - Ashhurst, Anneliese S.

AU - Mini Sasi, Vishnu

AU - Kaczmarski, Joe A.

AU - Jackson, Colin J.

AU - Pereira, Pedro José Barbosa

AU - Passioura, Toby

AU - Suga, Hiroaki

AU - Payne, Richard J.

PY - 2021/6/10

Y1 - 2021/6/10

N2 - The contact system comprises a series of serine proteases that mediate procoagulant and proinflammatory activities via the intrinsic pathway of coagulation and the kallikrein-kinin system, respectively. Inhibition of Factor XIIa (FXIIa), an initiator of the contact system, has been demonstrated to lead to thrombo-protection and anti-inflammatory effects in animal models and serves as a potentially safer target for the development of antithrombotics. Herein, we describe the use of the Randomised Nonstandard Peptide Integrated Discovery (RaPID) mRNA display technology to identify a series of potent and selective cyclic peptide inhibitors of FXIIa. Cyclic peptides were evaluated in vitro, and three lead compounds exhibited significant prolongation of aPTT, a reduction in thrombin generation, and an inhibition of bradykinin formation. We also describe our efforts to identify the critical residues for binding FXIIa through alanine scanning, analogue generation, and via in silico methods to predict the binding mode of our lead cyclic peptide inhibitors.

AB - The contact system comprises a series of serine proteases that mediate procoagulant and proinflammatory activities via the intrinsic pathway of coagulation and the kallikrein-kinin system, respectively. Inhibition of Factor XIIa (FXIIa), an initiator of the contact system, has been demonstrated to lead to thrombo-protection and anti-inflammatory effects in animal models and serves as a potentially safer target for the development of antithrombotics. Herein, we describe the use of the Randomised Nonstandard Peptide Integrated Discovery (RaPID) mRNA display technology to identify a series of potent and selective cyclic peptide inhibitors of FXIIa. Cyclic peptides were evaluated in vitro, and three lead compounds exhibited significant prolongation of aPTT, a reduction in thrombin generation, and an inhibition of bradykinin formation. We also describe our efforts to identify the critical residues for binding FXIIa through alanine scanning, analogue generation, and via in silico methods to predict the binding mode of our lead cyclic peptide inhibitors.

UR - https://www.scopus.com/pages/publications/85108021293

U2 - 10.1021/acs.jmedchem.1c00651

DO - 10.1021/acs.jmedchem.1c00651

M3 - Article

SN - 0022-2623

VL - 64

SP - 7853

EP - 7876

JO - Journal of Medicinal Chemistry

JF - Journal of Medicinal Chemistry

IS - 11

ER -

Potent Cyclic Peptide Inhibitors of FXIIa Discovered by mRNA Display with Genetic Code Reprogramming

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