Characterization of Histone Deacetylase 8 (HDAC8) Selective Inhibition Reveals Specific Active Site Structural and Functional Determinants

Martin Marek; Tajith B. Shaik; Tino Heimburg; Alokta Chakrabarti; Julien Lancelot; Elizabeth Ramos-Morales; Cyrielle Da Veiga; Dmitrii Kalinin; Jelena Melesina; Dina Robaa; Karin Schmidtkunz; Takayoshi Suzuki; Ralph Holl; Eric Ennifar; Raymond J. Pierce; Manfred Jung; Wolfgang Sippl; Christophe Romier

doi:10.1021/acs.jmedchem.8b01087

Characterization of Histone Deacetylase 8 (HDAC8) Selective Inhibition Reveals Specific Active Site Structural and Functional Determinants

Martin Marek
, Tajith B. Shaik
, Tino Heimburg
, Alokta Chakrabarti
, Julien Lancelot
, Elizabeth Ramos-Morales
, Cyrielle Da Veiga
, Dmitrii Kalinin
, Jelena Melesina
, Dina Robaa
, Karin Schmidtkunz
, Takayoshi Suzuki
, Ralph Holl
, Eric Ennifar
, Raymond J. Pierce
, Manfred Jung
, Wolfgang Sippl
, Christophe Romier

Research output: Contribution to a Journal (Peer & Non Peer) › Article › peer-review

101 Citations (Scopus)

Abstract

Metal-dependent histone deacetylases (HDACs) are key epigenetic regulators that represent promising therapeutic targets for the treatment of numerous human diseases. Yet the currently FDA-approved HDAC inhibitors nonspecifically target at least several of the 11 structurally similar but functionally different HDAC isozymes, which hampers their broad usage in clinical settings. Selective inhibitors targeting single HDAC isozymes are being developed, but precise understanding in molecular terms of their selectivity remains sparse. Here, we show that HDAC8-selective inhibitors adopt a L-shaped conformation required for their binding to a HDAC8-specific pocket formed by HDAC8 catalytic tyrosine and HDAC8 L1 and L6 loops. In other HDAC isozymes, a L1-L6 lock sterically prevents L-shaped inhibitor binding. Shielding of the HDAC8-specific pocket by protein engineering decreases potency of HDAC8-selective inhibitors and affects catalytic activity. Collectively, our results unravel key HDAC8 active site structural and functional determinants important for the design of next-generation chemical probes and epigenetic drugs.

Original language	English
Pages (from-to)	10000-10016
Number of pages	17
Journal	Journal of Medicinal Chemistry
Volume	61
Issue number	22
DOIs	https://doi.org/10.1021/acs.jmedchem.8b01087
Publication status	Published - 21 Nov 2018
Externally published	Yes

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Marek, M., Shaik, T. B., Heimburg, T., Chakrabarti, A., Lancelot, J., Ramos-Morales, E., Da Veiga, C., Kalinin, D., Melesina, J., Robaa, D., Schmidtkunz, K., Suzuki, T., Holl, R., Ennifar, E., Pierce, R. J., Jung, M., Sippl, W., & Romier, C. (2018). Characterization of Histone Deacetylase 8 (HDAC8) Selective Inhibition Reveals Specific Active Site Structural and Functional Determinants. Journal of Medicinal Chemistry, 61(22), 10000-10016. https://doi.org/10.1021/acs.jmedchem.8b01087

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title = "Characterization of Histone Deacetylase 8 (HDAC8) Selective Inhibition Reveals Specific Active Site Structural and Functional Determinants",

abstract = "Metal-dependent histone deacetylases (HDACs) are key epigenetic regulators that represent promising therapeutic targets for the treatment of numerous human diseases. Yet the currently FDA-approved HDAC inhibitors nonspecifically target at least several of the 11 structurally similar but functionally different HDAC isozymes, which hampers their broad usage in clinical settings. Selective inhibitors targeting single HDAC isozymes are being developed, but precise understanding in molecular terms of their selectivity remains sparse. Here, we show that HDAC8-selective inhibitors adopt a L-shaped conformation required for their binding to a HDAC8-specific pocket formed by HDAC8 catalytic tyrosine and HDAC8 L1 and L6 loops. In other HDAC isozymes, a L1-L6 lock sterically prevents L-shaped inhibitor binding. Shielding of the HDAC8-specific pocket by protein engineering decreases potency of HDAC8-selective inhibitors and affects catalytic activity. Collectively, our results unravel key HDAC8 active site structural and functional determinants important for the design of next-generation chemical probes and epigenetic drugs.",

author = "Martin Marek and Shaik, \{Tajith B.\} and Tino Heimburg and Alokta Chakrabarti and Julien Lancelot and Elizabeth Ramos-Morales and \{Da Veiga\}, Cyrielle and Dmitrii Kalinin and Jelena Melesina and Dina Robaa and Karin Schmidtkunz and Takayoshi Suzuki and Ralph Holl and Eric Ennifar and Pierce, \{Raymond J.\} and Manfred Jung and Wolfgang Sippl and Christophe Romier",

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doi = "10.1021/acs.jmedchem.8b01087",

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Marek, M, Shaik, TB, Heimburg, T, Chakrabarti, A, Lancelot, J, Ramos-Morales, E, Da Veiga, C, Kalinin, D, Melesina, J, Robaa, D, Schmidtkunz, K, Suzuki, T, Holl, R, Ennifar, E, Pierce, RJ, Jung, M, Sippl, W & Romier, C 2018, 'Characterization of Histone Deacetylase 8 (HDAC8) Selective Inhibition Reveals Specific Active Site Structural and Functional Determinants', Journal of Medicinal Chemistry, vol. 61, no. 22, pp. 10000-10016. https://doi.org/10.1021/acs.jmedchem.8b01087

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AU - Marek, Martin

AU - Shaik, Tajith B.

AU - Heimburg, Tino

AU - Chakrabarti, Alokta

AU - Lancelot, Julien

AU - Ramos-Morales, Elizabeth

AU - Da Veiga, Cyrielle

AU - Kalinin, Dmitrii

AU - Melesina, Jelena

AU - Robaa, Dina

AU - Schmidtkunz, Karin

AU - Suzuki, Takayoshi

AU - Holl, Ralph

AU - Ennifar, Eric

AU - Pierce, Raymond J.

AU - Jung, Manfred

AU - Sippl, Wolfgang

AU - Romier, Christophe

PY - 2018/11/21

Y1 - 2018/11/21

N2 - Metal-dependent histone deacetylases (HDACs) are key epigenetic regulators that represent promising therapeutic targets for the treatment of numerous human diseases. Yet the currently FDA-approved HDAC inhibitors nonspecifically target at least several of the 11 structurally similar but functionally different HDAC isozymes, which hampers their broad usage in clinical settings. Selective inhibitors targeting single HDAC isozymes are being developed, but precise understanding in molecular terms of their selectivity remains sparse. Here, we show that HDAC8-selective inhibitors adopt a L-shaped conformation required for their binding to a HDAC8-specific pocket formed by HDAC8 catalytic tyrosine and HDAC8 L1 and L6 loops. In other HDAC isozymes, a L1-L6 lock sterically prevents L-shaped inhibitor binding. Shielding of the HDAC8-specific pocket by protein engineering decreases potency of HDAC8-selective inhibitors and affects catalytic activity. Collectively, our results unravel key HDAC8 active site structural and functional determinants important for the design of next-generation chemical probes and epigenetic drugs.

AB - Metal-dependent histone deacetylases (HDACs) are key epigenetic regulators that represent promising therapeutic targets for the treatment of numerous human diseases. Yet the currently FDA-approved HDAC inhibitors nonspecifically target at least several of the 11 structurally similar but functionally different HDAC isozymes, which hampers their broad usage in clinical settings. Selective inhibitors targeting single HDAC isozymes are being developed, but precise understanding in molecular terms of their selectivity remains sparse. Here, we show that HDAC8-selective inhibitors adopt a L-shaped conformation required for their binding to a HDAC8-specific pocket formed by HDAC8 catalytic tyrosine and HDAC8 L1 and L6 loops. In other HDAC isozymes, a L1-L6 lock sterically prevents L-shaped inhibitor binding. Shielding of the HDAC8-specific pocket by protein engineering decreases potency of HDAC8-selective inhibitors and affects catalytic activity. Collectively, our results unravel key HDAC8 active site structural and functional determinants important for the design of next-generation chemical probes and epigenetic drugs.

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JF - Journal of Medicinal Chemistry

IS - 22

ER -

Characterization of Histone Deacetylase 8 (HDAC8) Selective Inhibition Reveals Specific Active Site Structural and Functional Determinants

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