Development of supramolecular anticoagulants with on-demand reversibility

Author:

Dockerill MillicentORCID,Ford Daniel J.,Angerani Simona,Alwis Imala,Dowman Luke J.,Ripoll-Rozada JorgeORCID,Smythe Rhyll E.ORCID,Liu Joanna S. T.,Pereira Pedro José BarbosaORCID,Jackson Shaun P.ORCID,Payne Richard J.ORCID,Winssinger NicolasORCID

Abstract

AbstractDrugs are administered at a dosing schedule set by their therapeutic index, and termination of action is achieved by clearance and metabolism of the drug. In some cases, such as anticoagulant drugs or immunotherapeutics, it is important to be able to quickly reverse the drug’s action. Here, we report a general strategy to achieve on-demand reversibility by designing a supramolecular drug (a noncovalent assembly of two cooperatively interacting drug fragments held together by transient hybridization of peptide nucleic acid (PNA)) that can be reversed with a PNA antidote that outcompetes the hybridization between the fragments. We demonstrate the approach with thrombin-inhibiting anticoagulants, creating very potent and reversible bivalent direct thrombin inhibitors (Ki = 74 pM). The supramolecular inhibitor effectively inhibited thrombus formation in mice in a needle injury thrombosis model, and this activity could be reversed by administration of the PNA antidote. This design is applicable to therapeutic targets where two binding sites can be identified.

Publisher

Springer Science and Business Media LLC

Cited by 4 articles. 订阅此论文施引文献 订阅此论文施引文献,注册后可以免费订阅5篇论文的施引文献,订阅后可以查看论文全部施引文献

1. Xeno Nucleic Acids as Functional Materials: From Biophysical Properties to Application;Advanced Healthcare Materials;2024-07-22

2. Designing reversible anticoagulants;Nature Reviews Drug Discovery;2024-05-31

3. Designing drugs with reversible activity;Nature Biotechnology;2024-04-30

4. Impact of charges on the hybridization kinetics and thermal stability of PNA duplexes;Organic & Biomolecular Chemistry;2024

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