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A bump-and-hole approach to engineer controlled selectivity of BET bromodomain chemical probes

A bump-and-hole approach to engineer controlled selectivity of BET bromodomain chemical probes
A bump-and-hole approach to engineer controlled selectivity of BET bromodomain chemical probes
Small molecules are useful tools for probing the biological function and therapeutic potential of individual proteins, but achieving selectivity is challenging when the target protein shares structural domains with other proteins. The Bromo and Extra-Terminal (BET) proteins have attracted interest because of their roles in transcriptional regulation, epigenetics, and cancer. The BET bromodomains (protein interaction modules that bind acetyl-lysine) have been targeted by potent small-molecule inhibitors, but these inhibitors lack selectivity for individual family members. We developed an ethyl derivative of an existing small-molecule inhibitor, I-BET/JQ1, and showed that it binds leucine/alanine mutant bromodomains with nanomolar affinity and achieves up to 540-fold selectivity relative to wild-type bromodomains. Cell culture studies showed that blockade of the first bromodomain alone is sufficient to displace a specific BET protein, Brd4, from chromatin. Expansion of this approach could help identify the individual roles of single BET proteins in human physiology and disease.
0036-8075
638-641
Baud, M.G.J
8752d519-3d33-43b6-9a77-ab731d410c2e
Lin-Shiao, E.
471154b1-8312-46a4-8c86-2d59538eabf4
Cardote, T.
49751a34-b457-433a-a1f5-b0b62b24f384
Tallant, C.
a98ac34a-4a5c-40f6-9444-6aaf3f3e1e2e
Pschibul, A.
9c2579b3-47e5-48ae-a591-4ff7a0e2ec66
Chan, K.-H.
87d77c74-fcc0-4255-b0a9-e97a4b695e9f
Zengerle, M.
6843f52d-8e5d-4bd1-b67a-ec7c2c7c6093
Garcia, J.R.
9b4f5fb5-91a8-4b4d-b012-a530de365cf2
Kwan, T.T.- L.
3bacbbb0-c477-4af9-85ab-489768cfdc82
Ferguson, F.M.
af922633-1722-436e-9dc5-51aa4ac04312
Ciulli, A.
8a04c43e-58ae-49e3-9c2f-72aae3b2e014
Baud, M.G.J
8752d519-3d33-43b6-9a77-ab731d410c2e
Lin-Shiao, E.
471154b1-8312-46a4-8c86-2d59538eabf4
Cardote, T.
49751a34-b457-433a-a1f5-b0b62b24f384
Tallant, C.
a98ac34a-4a5c-40f6-9444-6aaf3f3e1e2e
Pschibul, A.
9c2579b3-47e5-48ae-a591-4ff7a0e2ec66
Chan, K.-H.
87d77c74-fcc0-4255-b0a9-e97a4b695e9f
Zengerle, M.
6843f52d-8e5d-4bd1-b67a-ec7c2c7c6093
Garcia, J.R.
9b4f5fb5-91a8-4b4d-b012-a530de365cf2
Kwan, T.T.- L.
3bacbbb0-c477-4af9-85ab-489768cfdc82
Ferguson, F.M.
af922633-1722-436e-9dc5-51aa4ac04312
Ciulli, A.
8a04c43e-58ae-49e3-9c2f-72aae3b2e014

Baud, M.G.J, Lin-Shiao, E., Cardote, T., Tallant, C., Pschibul, A., Chan, K.-H., Zengerle, M., Garcia, J.R., Kwan, T.T.- L., Ferguson, F.M. and Ciulli, A. (2014) A bump-and-hole approach to engineer controlled selectivity of BET bromodomain chemical probes. Science, 346 (6209), 638-641. (doi:10.1126/science.1249830).

Record type: Article

Abstract

Small molecules are useful tools for probing the biological function and therapeutic potential of individual proteins, but achieving selectivity is challenging when the target protein shares structural domains with other proteins. The Bromo and Extra-Terminal (BET) proteins have attracted interest because of their roles in transcriptional regulation, epigenetics, and cancer. The BET bromodomains (protein interaction modules that bind acetyl-lysine) have been targeted by potent small-molecule inhibitors, but these inhibitors lack selectivity for individual family members. We developed an ethyl derivative of an existing small-molecule inhibitor, I-BET/JQ1, and showed that it binds leucine/alanine mutant bromodomains with nanomolar affinity and achieves up to 540-fold selectivity relative to wild-type bromodomains. Cell culture studies showed that blockade of the first bromodomain alone is sufficient to displace a specific BET protein, Brd4, from chromatin. Expansion of this approach could help identify the individual roles of single BET proteins in human physiology and disease.

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More information

Accepted/In Press date: 1 October 2014
Published date: 31 October 2014
Organisations: Faculty of Natural and Environmental Sciences

Identifiers

Local EPrints ID: 400504
URI: http://eprints.soton.ac.uk/id/eprint/400504
ISSN: 0036-8075
PURE UUID: 26503bf0-ca9d-47dd-98bd-e7d2a709a89d
ORCID for M.G.J Baud: ORCID iD orcid.org/0000-0003-3714-4350

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Date deposited: 16 Sep 2016 15:33
Last modified: 15 Mar 2024 03:54

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Contributors

Author: M.G.J Baud ORCID iD
Author: E. Lin-Shiao
Author: T. Cardote
Author: C. Tallant
Author: A. Pschibul
Author: K.-H. Chan
Author: M. Zengerle
Author: J.R. Garcia
Author: T.T.- L. Kwan
Author: F.M. Ferguson
Author: A. Ciulli

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