Fluorine Modifications Contribute to Potent Antiviral Activity against Highly Drug-Resistant HIV-1 and Favorable Blood-Brain Barrier Penetration Property of Novel Central Nervous System- Targeting HIV-1 Protease Inhibitors In Vitro

Masayuki Amano; Ravikiran S. Yedidi; Pedro Miguel Salcedo-Gómez; Hironori Hayashi; Kazuya Hasegawa; Cuthbert D. Martyr; Arun K. Ghosh; Hiroaki Mitsuya

doi:10.1128/aac.01715-21

Fluorine Modifications Contribute to Potent Antiviral Activity against Highly Drug-Resistant HIV-1 and Favorable Blood-Brain Barrier Penetration Property of Novel Central Nervous System- Targeting HIV-1 Protease Inhibitors In Vitro

Masayuki Amano, Ravikiran S. Yedidi, Pedro Miguel Salcedo-Gómez, Hironori Hayashi, Kazuya Hasegawa, Cuthbert D. Martyr, Arun K. Ghosh, Hiroaki Mitsuya

Disaster Medical Science Division

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Abstract

To date, there are no specific treatment regimens for HIV-1-related central nervous system (CNS) complications, such as HIV-1-associated neurocognitive disorders (HAND). Here, we report that two newly generated CNS-targeting HIV-1 protease (PR) inhibitors (PIs), GRL-08513 and GRL-08613, which have a P1-3,5-bis-fluorophenyl or P1-para-monofluorophenyl ring and P2-tetrahydropyrano-tetrahydrofuran (Tp-THF) with a sulfonamide isostere, are potent against wild-type HIV-1 strains and multiple clinically isolated HIV-1 strains (50% effective concentration [EC50]: 0.0001 to ;0.0032 mM). As assessed with HIV-1 variants that had been selected in vitro to propagate at a 5 mM concentration of each HIV-1 PI (atazanavir, lopinavir, or amprenavir), GRL-08513 and GRL-08613 efficiently inhibited the replication of these highly PI-resistant variants (EC50: 0.003 to ;0.006 mM). GRL-08513 and GRL-08613 also maintained their antiviral activities against HIV-2ROD as well as severely multidrug- resistant clinical HIV-1 variants. Additionally, when we assessed with the in vitro blood-brain barrier (BBB) reconstruction system, GRL-08513 and GRL-08613 showed the most promising properties of CNS penetration among the evaluated compounds, including the majority of FDA-approved combination antiretroviral therapy (cART) drugs. In the crystallographic analysis of compound-PR complexes, it was demonstrated that the Tp-THF rings at the P2 moiety of GRL-08513 and GRL-08613 form robust hydrogen bond interactions with the active site of HIV-1 PR. Furthermore, both the P1-3,5-bis-fluorophenyl- and P1-para-monofluorophenyl rings sustain greater contact surfaces and form stronger van der Waals interactions with PR than is the case with darunavir-PR complex. Taken together, these results strongly suggest that GRL-08513 and GRL-08613 have favorable features for patients infected with wildtype/ multidrug-resistant HIV-1 strains and might serve as candidates for a preventive and/or therapeutic agent for HAND and other CNS complications.

Original language	English
Article number	e01715-21
Journal	Antimicrobial agents and chemotherapy
Volume	66
Issue number	2
DOIs	https://doi.org/10.1128/aac.01715-21
Publication status	Published - 2022 Feb

Keywords

Blood-brain barrier
Central nervous system infections
HIV-1
HIV-1-associated neurocognitive disorders
Protease inhibitors

ASJC Scopus subject areas

Pharmacology
Pharmacology (medical)
Infectious Diseases

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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Amano, M., Yedidi, R. S., Salcedo-Gómez, P. M., Hayashi, H., Hasegawa, K., Martyr, C. D., Ghosh, A. K., & Mitsuya, H. (2022). Fluorine Modifications Contribute to Potent Antiviral Activity against Highly Drug-Resistant HIV-1 and Favorable Blood-Brain Barrier Penetration Property of Novel Central Nervous System- Targeting HIV-1 Protease Inhibitors In Vitro. Antimicrobial agents and chemotherapy, 66(2), [e01715-21]. https://doi.org/10.1128/aac.01715-21

Fluorine Modifications Contribute to Potent Antiviral Activity against Highly Drug-Resistant HIV-1 and Favorable Blood-Brain Barrier Penetration Property of Novel Central Nervous System- Targeting HIV-1 Protease Inhibitors In Vitro. / Amano, Masayuki; Yedidi, Ravikiran S.; Salcedo-Gómez, Pedro Miguel et al.

In: Antimicrobial agents and chemotherapy, Vol. 66, No. 2, e01715-21, 02.2022.

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

Amano, M, Yedidi, RS, Salcedo-Gómez, PM, Hayashi, H, Hasegawa, K, Martyr, CD, Ghosh, AK & Mitsuya, H 2022, 'Fluorine Modifications Contribute to Potent Antiviral Activity against Highly Drug-Resistant HIV-1 and Favorable Blood-Brain Barrier Penetration Property of Novel Central Nervous System- Targeting HIV-1 Protease Inhibitors In Vitro', Antimicrobial agents and chemotherapy, vol. 66, no. 2, e01715-21. https://doi.org/10.1128/aac.01715-21

Amano M, Yedidi RS, Salcedo-Gómez PM, Hayashi H, Hasegawa K, Martyr CD et al. Fluorine Modifications Contribute to Potent Antiviral Activity against Highly Drug-Resistant HIV-1 and Favorable Blood-Brain Barrier Penetration Property of Novel Central Nervous System- Targeting HIV-1 Protease Inhibitors In Vitro. Antimicrobial agents and chemotherapy. 2022 Feb;66(2):e01715-21. doi: 10.1128/aac.01715-21

Amano, Masayuki ; Yedidi, Ravikiran S. ; Salcedo-Gómez, Pedro Miguel et al. / Fluorine Modifications Contribute to Potent Antiviral Activity against Highly Drug-Resistant HIV-1 and Favorable Blood-Brain Barrier Penetration Property of Novel Central Nervous System- Targeting HIV-1 Protease Inhibitors In Vitro. In: Antimicrobial agents and chemotherapy. 2022 ; Vol. 66, No. 2.

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title = "Fluorine Modifications Contribute to Potent Antiviral Activity against Highly Drug-Resistant HIV-1 and Favorable Blood-Brain Barrier Penetration Property of Novel Central Nervous System- Targeting HIV-1 Protease Inhibitors In Vitro",

abstract = "To date, there are no specific treatment regimens for HIV-1-related central nervous system (CNS) complications, such as HIV-1-associated neurocognitive disorders (HAND). Here, we report that two newly generated CNS-targeting HIV-1 protease (PR) inhibitors (PIs), GRL-08513 and GRL-08613, which have a P1-3,5-bis-fluorophenyl or P1-para-monofluorophenyl ring and P2-tetrahydropyrano-tetrahydrofuran (Tp-THF) with a sulfonamide isostere, are potent against wild-type HIV-1 strains and multiple clinically isolated HIV-1 strains (50% effective concentration [EC50]: 0.0001 to ;0.0032 mM). As assessed with HIV-1 variants that had been selected in vitro to propagate at a 5 mM concentration of each HIV-1 PI (atazanavir, lopinavir, or amprenavir), GRL-08513 and GRL-08613 efficiently inhibited the replication of these highly PI-resistant variants (EC50: 0.003 to ;0.006 mM). GRL-08513 and GRL-08613 also maintained their antiviral activities against HIV-2ROD as well as severely multidrug- resistant clinical HIV-1 variants. Additionally, when we assessed with the in vitro blood-brain barrier (BBB) reconstruction system, GRL-08513 and GRL-08613 showed the most promising properties of CNS penetration among the evaluated compounds, including the majority of FDA-approved combination antiretroviral therapy (cART) drugs. In the crystallographic analysis of compound-PR complexes, it was demonstrated that the Tp-THF rings at the P2 moiety of GRL-08513 and GRL-08613 form robust hydrogen bond interactions with the active site of HIV-1 PR. Furthermore, both the P1-3,5-bis-fluorophenyl- and P1-para-monofluorophenyl rings sustain greater contact surfaces and form stronger van der Waals interactions with PR than is the case with darunavir-PR complex. Taken together, these results strongly suggest that GRL-08513 and GRL-08613 have favorable features for patients infected with wildtype/ multidrug-resistant HIV-1 strains and might serve as candidates for a preventive and/or therapeutic agent for HAND and other CNS complications.",

keywords = "Blood-brain barrier, Central nervous system infections, HIV-1, HIV-1-associated neurocognitive disorders, Protease inhibitors",

author = "Masayuki Amano and Yedidi, {Ravikiran S.} and Salcedo-G{\'o}mez, {Pedro Miguel} and Hironori Hayashi and Kazuya Hasegawa and Martyr, {Cuthbert D.} and Ghosh, {Arun K.} and Hiroaki Mitsuya",

note = "Funding Information: We thank the synchrotron beamline staff at SPring-8 for their support in X-ray diffraction data collection and acknowledge support by the Platform Project for Supporting in Drug Discovery and Life Science Research from the Ministry of Education, Culture, Sports, Science and Technology (MEXT). The synchrotron radiation experiments were performed at BL41XU of SPring-8 with the approval of the Japan Synchrotron Radiation Research Institute (JASRI) (proposal no. 2014A1001). This work utilized the computational resources of the NIH HPC Biowulf cluster (https://hpc.nih.gov). We also thank Kenji Maeda (NCGM Research Institute, Japan) for his support in the acquisition of research materials. We declare no competing financial interests. Funding Information: This work was supported in part by a grant for a global education and research center aimed at the control of AIDS (Global Center of Excellence, supported by Monbu-Kagakusho), by a grant from Promotion of AIDS Research from the Ministry of Health, Welfare, and Labor of Japan, by a grant from the Cooperative Research Project on Clinical and Epidemiological Studies of Emerging and Reemerging Infectious Diseases (Renkei Jigyo: no. 78, Kumamoto University) of Monbu-Kagakusho (H.M.), by a grant from the Research Program on HIV/AIDS from the Japan Agency for Medical Research and Development, AMED (JP20fk0310113, H.M.), by a grant for JSPS KAKENHI (grant number 17K19577, 17H0422, 20K2160, and 20H03727, H.M.), by a grant from the National Center for Global Health and Medicine (H.M.), by the Intramural Research Program of Center for Cancer Research, National Cancer Institute, National Institutes of Health (H.M.), and by a grant from the National Institutes of Health (AI150466, A.K.G.). Publisher Copyright: {\textcopyright} 2022 American Society for Microbiology.",

year = "2022",

month = feb,

doi = "10.1128/aac.01715-21",

language = "English",

volume = "66",

journal = "Antimicrobial Agents and Chemotherapy",

issn = "0066-4804",

publisher = "American Society for Microbiology",

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TY - JOUR

T1 - Fluorine Modifications Contribute to Potent Antiviral Activity against Highly Drug-Resistant HIV-1 and Favorable Blood-Brain Barrier Penetration Property of Novel Central Nervous System- Targeting HIV-1 Protease Inhibitors In Vitro

AU - Amano, Masayuki

AU - Yedidi, Ravikiran S.

AU - Salcedo-Gómez, Pedro Miguel

AU - Hayashi, Hironori

AU - Hasegawa, Kazuya

AU - Martyr, Cuthbert D.

AU - Ghosh, Arun K.

AU - Mitsuya, Hiroaki

N1 - Funding Information: We thank the synchrotron beamline staff at SPring-8 for their support in X-ray diffraction data collection and acknowledge support by the Platform Project for Supporting in Drug Discovery and Life Science Research from the Ministry of Education, Culture, Sports, Science and Technology (MEXT). The synchrotron radiation experiments were performed at BL41XU of SPring-8 with the approval of the Japan Synchrotron Radiation Research Institute (JASRI) (proposal no. 2014A1001). This work utilized the computational resources of the NIH HPC Biowulf cluster (https://hpc.nih.gov). We also thank Kenji Maeda (NCGM Research Institute, Japan) for his support in the acquisition of research materials. We declare no competing financial interests. Funding Information: This work was supported in part by a grant for a global education and research center aimed at the control of AIDS (Global Center of Excellence, supported by Monbu-Kagakusho), by a grant from Promotion of AIDS Research from the Ministry of Health, Welfare, and Labor of Japan, by a grant from the Cooperative Research Project on Clinical and Epidemiological Studies of Emerging and Reemerging Infectious Diseases (Renkei Jigyo: no. 78, Kumamoto University) of Monbu-Kagakusho (H.M.), by a grant from the Research Program on HIV/AIDS from the Japan Agency for Medical Research and Development, AMED (JP20fk0310113, H.M.), by a grant for JSPS KAKENHI (grant number 17K19577, 17H0422, 20K2160, and 20H03727, H.M.), by a grant from the National Center for Global Health and Medicine (H.M.), by the Intramural Research Program of Center for Cancer Research, National Cancer Institute, National Institutes of Health (H.M.), and by a grant from the National Institutes of Health (AI150466, A.K.G.). Publisher Copyright: © 2022 American Society for Microbiology.

PY - 2022/2

Y1 - 2022/2

N2 - To date, there are no specific treatment regimens for HIV-1-related central nervous system (CNS) complications, such as HIV-1-associated neurocognitive disorders (HAND). Here, we report that two newly generated CNS-targeting HIV-1 protease (PR) inhibitors (PIs), GRL-08513 and GRL-08613, which have a P1-3,5-bis-fluorophenyl or P1-para-monofluorophenyl ring and P2-tetrahydropyrano-tetrahydrofuran (Tp-THF) with a sulfonamide isostere, are potent against wild-type HIV-1 strains and multiple clinically isolated HIV-1 strains (50% effective concentration [EC50]: 0.0001 to ;0.0032 mM). As assessed with HIV-1 variants that had been selected in vitro to propagate at a 5 mM concentration of each HIV-1 PI (atazanavir, lopinavir, or amprenavir), GRL-08513 and GRL-08613 efficiently inhibited the replication of these highly PI-resistant variants (EC50: 0.003 to ;0.006 mM). GRL-08513 and GRL-08613 also maintained their antiviral activities against HIV-2ROD as well as severely multidrug- resistant clinical HIV-1 variants. Additionally, when we assessed with the in vitro blood-brain barrier (BBB) reconstruction system, GRL-08513 and GRL-08613 showed the most promising properties of CNS penetration among the evaluated compounds, including the majority of FDA-approved combination antiretroviral therapy (cART) drugs. In the crystallographic analysis of compound-PR complexes, it was demonstrated that the Tp-THF rings at the P2 moiety of GRL-08513 and GRL-08613 form robust hydrogen bond interactions with the active site of HIV-1 PR. Furthermore, both the P1-3,5-bis-fluorophenyl- and P1-para-monofluorophenyl rings sustain greater contact surfaces and form stronger van der Waals interactions with PR than is the case with darunavir-PR complex. Taken together, these results strongly suggest that GRL-08513 and GRL-08613 have favorable features for patients infected with wildtype/ multidrug-resistant HIV-1 strains and might serve as candidates for a preventive and/or therapeutic agent for HAND and other CNS complications.

AB - To date, there are no specific treatment regimens for HIV-1-related central nervous system (CNS) complications, such as HIV-1-associated neurocognitive disorders (HAND). Here, we report that two newly generated CNS-targeting HIV-1 protease (PR) inhibitors (PIs), GRL-08513 and GRL-08613, which have a P1-3,5-bis-fluorophenyl or P1-para-monofluorophenyl ring and P2-tetrahydropyrano-tetrahydrofuran (Tp-THF) with a sulfonamide isostere, are potent against wild-type HIV-1 strains and multiple clinically isolated HIV-1 strains (50% effective concentration [EC50]: 0.0001 to ;0.0032 mM). As assessed with HIV-1 variants that had been selected in vitro to propagate at a 5 mM concentration of each HIV-1 PI (atazanavir, lopinavir, or amprenavir), GRL-08513 and GRL-08613 efficiently inhibited the replication of these highly PI-resistant variants (EC50: 0.003 to ;0.006 mM). GRL-08513 and GRL-08613 also maintained their antiviral activities against HIV-2ROD as well as severely multidrug- resistant clinical HIV-1 variants. Additionally, when we assessed with the in vitro blood-brain barrier (BBB) reconstruction system, GRL-08513 and GRL-08613 showed the most promising properties of CNS penetration among the evaluated compounds, including the majority of FDA-approved combination antiretroviral therapy (cART) drugs. In the crystallographic analysis of compound-PR complexes, it was demonstrated that the Tp-THF rings at the P2 moiety of GRL-08513 and GRL-08613 form robust hydrogen bond interactions with the active site of HIV-1 PR. Furthermore, both the P1-3,5-bis-fluorophenyl- and P1-para-monofluorophenyl rings sustain greater contact surfaces and form stronger van der Waals interactions with PR than is the case with darunavir-PR complex. Taken together, these results strongly suggest that GRL-08513 and GRL-08613 have favorable features for patients infected with wildtype/ multidrug-resistant HIV-1 strains and might serve as candidates for a preventive and/or therapeutic agent for HAND and other CNS complications.

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KW - Central nervous system infections

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KW - HIV-1-associated neurocognitive disorders

KW - Protease inhibitors

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Fluorine Modifications Contribute to Potent Antiviral Activity against Highly Drug-Resistant HIV-1 and Favorable Blood-Brain Barrier Penetration Property of Novel Central Nervous System- Targeting HIV-1 Protease Inhibitors In Vitro

Abstract

Keywords

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UN SDGs

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