Structural Insights into BET Client Recognition of Endometrial and Prostate Cancer-Associated SPOP Mutants

Michael Sebastian Ostertag; Wiebke Hutwelker; Oliver Plettenburg; Michael Sattler; Grzegorz Maria Popowicz

doi:10.1016/j.jmb.2019.04.017

Structural Insights into BET Client Recognition of Endometrial and Prostate Cancer-Associated SPOP Mutants

J Mol Biol. 2019 May 17;431(11):2213-2221. doi: 10.1016/j.jmb.2019.04.017. Epub 2019 Apr 23.

Authors

Michael Sebastian Ostertag¹, Wiebke Hutwelker², Oliver Plettenburg², Michael Sattler³, Grzegorz Maria Popowicz⁴

Affiliations

¹ Institute of Structural Biology, Helmholtz Zentrum München, Ingolstädter Landstr. 1, 85764 Neuherberg, Germany; Center for Integrated Protein Science Munich at Chair of Biomolecular NMR Spectroscopy, Department Chemie, Technische Universität München, Lichtenbergstrasse 4, 85747 Garching, Germany.
² Institute of Medicinal Chemistry, Helmholtz Zentrum München, Ingolstädter Landstr. 1, 85764 Neuherberg, Germany; Institute of Organic Chemistry, Leibniz Universität Hannover, Schneiderberg 1b, 30167 Hannover, Germany.
³ Institute of Structural Biology, Helmholtz Zentrum München, Ingolstädter Landstr. 1, 85764 Neuherberg, Germany; Center for Integrated Protein Science Munich at Chair of Biomolecular NMR Spectroscopy, Department Chemie, Technische Universität München, Lichtenbergstrasse 4, 85747 Garching, Germany. Electronic address: sattler@helmholtz-muenchen.de.
⁴ Institute of Structural Biology, Helmholtz Zentrum München, Ingolstädter Landstr. 1, 85764 Neuherberg, Germany; Center for Integrated Protein Science Munich at Chair of Biomolecular NMR Spectroscopy, Department Chemie, Technische Universität München, Lichtenbergstrasse 4, 85747 Garching, Germany. Electronic address: grzegorz.popowicz@helmholtz-muenchen.de.

PMID: 31026449
DOI: 10.1016/j.jmb.2019.04.017

Abstract

BET proteins such as BRD3 are oncogenic transcriptional coactivators. SPOP binding triggers their proteasomal degradation. In both endometrial and prostate cancers, SPOP mutations occur in the MATH domain, but with opposed influence on drug susceptibility. In prostate cancer, SPOP mutations presumably cause increased BET levels, decreasing BET inhibitor drug susceptibility. As opposed, in endometrial cancer, decreased BET levels concomitant with higher BET inhibitor drug susceptibility were observed. Here, we present the to our knowledge first co-crystal structure of SPOP and a bromodomain containing protein (BRD3). Our structural and biophysical data confirm the suggested loss-of-function in prostate cancer-associated SPOP mutants and provide mechanistic explanation. As opposed to previous literature, our data on endometrial cancer-associated SPOP mutants do not show altered binding behavior compared to wild-type SPOP, indicating a more complex regulatory mechanism. SPOP mutation screening may thus be considered a valuable personalized medicine tool for effective antitumor therapy.

Keywords: BET protein; SPOP; cancer; ubiquitination; x-ray crystallograpgy.

MeSH terms

Crystallography, X-Ray
Endometrial Neoplasms / genetics
Endometrial Neoplasms / metabolism*
Female
Humans
Male
Models, Molecular
Nuclear Proteins / chemistry
Nuclear Proteins / genetics
Nuclear Proteins / metabolism*
Prostatic Neoplasms / genetics
Prostatic Neoplasms / metabolism*
Protein Conformation
Repressor Proteins / chemistry
Repressor Proteins / genetics
Repressor Proteins / metabolism*
Transcription Factors / chemistry
Transcription Factors / metabolism*
Ubiquitination

Substances

BRD3 protein, human
Nuclear Proteins
Repressor Proteins
SPOP protein, human
Transcription Factors