Dynamic Combinatorial Optimization of In Vitro and In Vivo Heparin Antidotes

Daniel Carbajo; Yolanda Pérez; Marta Guerra-Rebollo; Eva Prats; Jordi Bujons; Ignacio Alfonso

doi:10.1021/acs.jmedchem.1c02054

Dynamic Combinatorial Optimization of In Vitro and In Vivo Heparin Antidotes

Daniel Carbajo, Yolanda Pérez, Marta Guerra-Rebollo, Eva Prats, Jordi Bujons, Ignacio Alfonso^*

^*Autor/a de correspondencia de este trabajo

Producción científica: Artículo en revista indizada › Artículo › revisión exhaustiva

11 Citas (Scopus)

Resumen

Heparin-like macromolecules are widely used in clinics as anticoagulant, antiviral, and anticancer drugs. However, the search of heparin antidotes based on small synthetic molecules to control blood coagulation still remains a challenging task due to the physicochemical properties of this anionic polysaccharide. Here, we use a dynamic combinatorial chemistry approach to optimize heparin binders with submicromolar affinity. The recognition of heparin by the most amplified members of the dynamic library has been studied with different experimental (SPR, fluorescence, NMR) and theoretical approaches, rendering a detailed interaction model. The enzymatic assays with selected library members confirm the correlation between the dynamic covalent screening and the in vitro heparin inhibition. Moreover, both ex vivo and in vivo blood coagulation assays with mice show that the optimized molecules are potent antidotes with potential use as heparin reversal drugs. Overall, these results underscore the power of dynamic combinatorial chemistry targeting complex and elusive biopolymers.

Idioma original	Inglés
Páginas (desde-hasta)	4865-4877
Número de páginas	13
Publicación	Journal of Medicinal Chemistry
Volumen	65
N.º	6
DOI	https://doi.org/10.1021/acs.jmedchem.1c02054
Estado	Publicada - 24 mar 2022

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title = "Dynamic Combinatorial Optimization of In Vitro and In Vivo Heparin Antidotes",

abstract = "Heparin-like macromolecules are widely used in clinics as anticoagulant, antiviral, and anticancer drugs. However, the search of heparin antidotes based on small synthetic molecules to control blood coagulation still remains a challenging task due to the physicochemical properties of this anionic polysaccharide. Here, we use a dynamic combinatorial chemistry approach to optimize heparin binders with submicromolar affinity. The recognition of heparin by the most amplified members of the dynamic library has been studied with different experimental (SPR, fluorescence, NMR) and theoretical approaches, rendering a detailed interaction model. The enzymatic assays with selected library members confirm the correlation between the dynamic covalent screening and the in vitro heparin inhibition. Moreover, both ex vivo and in vivo blood coagulation assays with mice show that the optimized molecules are potent antidotes with potential use as heparin reversal drugs. Overall, these results underscore the power of dynamic combinatorial chemistry targeting complex and elusive biopolymers.",

keywords = "Reversal activity, Chemistry, Anticoagulants, Sulfate, Binding, Amber, Simulations, Antagonist, Design, Surfen",

author = "Daniel Carbajo and Yolanda P{\'e}rez and Marta Guerra-Rebollo and Eva Prats and Jordi Bujons and Ignacio Alfonso",

note = "Funding Information: This work was supported by the Spanish Ministry of Science and Innovation, Spanish Research Agency (10.13039/501100011033), and European Social Fund (MCI/AEI/FEDER, RTI2018-096182-B-I00, CSIC13-4E-2076) as well as AGAUR (2017 SGR 208). The authors acknowledge the assistance from the ICTS {"}NANBIOSIS{"}in some key experiments: SPR carried out in the Unit U2, Custom Antibody Service (CAbS, CIBER-BBN) and DLS performed by the Nanostructured Liquid Characterization Unit, both located at IQAC-CSIC. We acknowledge support of the publication fee by the CSIC Open Access Publication Support Initiative through its Unit of Information Resources for Research (URICI). Funding Information: This work was supported by the Spanish Ministry of Science and Innovation, Spanish Research Agency (10.13039/501100011033), and European Social Fund (MCI/AEI/FEDER, RTI2018-096182-B-I00, CSIC13-4E-2076), as well as AGAUR (2017 SGR 208). The authors acknowledge the assistance from the ICTS “NANBIOSIS” in some key experiments: SPR carried out in the Unit U2, Custom Antibody Service (C, CIBER-BBN) and DLS performed by the Nanostructured Liquid Characterization Unit, both located at IQAC-CSIC. We acknowledge support of the publication fee by the CSIC Open Access Publication Support Initiative through its Unit of Information Resources for Research (URICI). AbS Publisher Copyright: {\textcopyright} 2022 American Chemical Society.",

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AU - Prats, Eva

AU - Bujons, Jordi

AU - Alfonso, Ignacio

N1 - Funding Information: This work was supported by the Spanish Ministry of Science and Innovation, Spanish Research Agency (10.13039/501100011033), and European Social Fund (MCI/AEI/FEDER, RTI2018-096182-B-I00, CSIC13-4E-2076) as well as AGAUR (2017 SGR 208). The authors acknowledge the assistance from the ICTS "NANBIOSIS"in some key experiments: SPR carried out in the Unit U2, Custom Antibody Service (CAbS, CIBER-BBN) and DLS performed by the Nanostructured Liquid Characterization Unit, both located at IQAC-CSIC. We acknowledge support of the publication fee by the CSIC Open Access Publication Support Initiative through its Unit of Information Resources for Research (URICI). Funding Information: This work was supported by the Spanish Ministry of Science and Innovation, Spanish Research Agency (10.13039/501100011033), and European Social Fund (MCI/AEI/FEDER, RTI2018-096182-B-I00, CSIC13-4E-2076), as well as AGAUR (2017 SGR 208). The authors acknowledge the assistance from the ICTS “NANBIOSIS” in some key experiments: SPR carried out in the Unit U2, Custom Antibody Service (C, CIBER-BBN) and DLS performed by the Nanostructured Liquid Characterization Unit, both located at IQAC-CSIC. We acknowledge support of the publication fee by the CSIC Open Access Publication Support Initiative through its Unit of Information Resources for Research (URICI). AbS Publisher Copyright: © 2022 American Chemical Society.

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Y1 - 2022/3/24

N2 - Heparin-like macromolecules are widely used in clinics as anticoagulant, antiviral, and anticancer drugs. However, the search of heparin antidotes based on small synthetic molecules to control blood coagulation still remains a challenging task due to the physicochemical properties of this anionic polysaccharide. Here, we use a dynamic combinatorial chemistry approach to optimize heparin binders with submicromolar affinity. The recognition of heparin by the most amplified members of the dynamic library has been studied with different experimental (SPR, fluorescence, NMR) and theoretical approaches, rendering a detailed interaction model. The enzymatic assays with selected library members confirm the correlation between the dynamic covalent screening and the in vitro heparin inhibition. Moreover, both ex vivo and in vivo blood coagulation assays with mice show that the optimized molecules are potent antidotes with potential use as heparin reversal drugs. Overall, these results underscore the power of dynamic combinatorial chemistry targeting complex and elusive biopolymers.

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Dynamic Combinatorial Optimization of In Vitro and In Vivo Heparin Antidotes

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