Structure–Activity Relationships of Cbx7 Inhibitors, Including Selectivity Studies against Other Cbx Proteins

Simhadri, Chakravarthi; Gignac, Michael C.; Anderson, Cameron J.; Milosevich, Natalia; Dheri, Aman; Prashar, Nishant; Flemmer, Robert T.; Dev, Amarjot; Henderson, Trevor G.; Douglas, Sarah F.; Wulff, Jeremy E.; Hof, Fraser

doi:10.1021/acsomega.6b00120

Cited by 18 publications

(23 citation statements)

References 38 publications

(52 reference statements)

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“…Expression of chromodomain of Cbx7 and its purification, and conducting FP experiments and data analysis of the compounds were performed in similar manner as described in the published reports . Addgene plasmid 25241 for CBX7, deposited by C. Arrowsmith, Structural Genomics Consortium, Toronto (Canada), and encoding for Cbx7 chromodomain residues 7–62, was used for all biochemical binding studies.…”

Section: Methodsmentioning

confidence: 99%

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Rational Adaptation of L3MBTL1 Inhibitors to Create Small‐Molecule Cbx7 Antagonists

et al. 2019

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Chromobox homolog 7 (Cbx7) is an epigenetic modulator that is an important driver of multiple cancers. It is a methyl reader protein that operates by recognizing and binding to methylated lysine residues on specific partners. Herein we report our efforts to create low‐molecular‐weight inhibitors of Cbx7 by making rational structural adaptations to inhibitors of a different methyl reader protein, L3MBTL1, inhibitors that had previously been reported to be inactive against Cbx7. We evaluated each new inhibitor for Cbx7 inhibition by fluorescence polarization assay, and also confirmed the binding of selected inhibitors to Cbx7 by saturation‐transfer difference NMR spectroscopy. This work identified multiple small‐molecule inhibitors with modest (IC50: 257–500 μm) potency.

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Section: Methodsmentioning

confidence: 99%

“…Successful approaches to Cbx7 inhibition have been driven by peptide‐based approaches– and high‐throughput screening for small‐molecule inhibitor approaches . Small‐molecule Cbx7 antagonists MS35472 and MS351 have been shown to de‐repress the p16 gene in PC3 prostate cancer cells …”

Section: Introductionmentioning

confidence: 99%

Rational Adaptation of L3MBTL1 Inhibitors to Create Small‐Molecule Cbx7 Antagonists

et al. 2019

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“…chromodomain is the most similar to CBX7 (similarity score of 90%), 3,14 both bind the native histone substrate with similar affinity, 3 and almost all CBX7 ligands reported to date have had similar affinities for CBX4. 9,10,12,13 Interestingly, both 10 and 11 show significantly weaker binding to CBX4 compared to CBX7. Future efforts on selective inhibition of CBX7 may benefit from extended engagement of the peptide-binding groove.…”

Section: Selective Inhibition Of Cbx7 Over Cbx4mentioning

confidence: 99%

“…9,11,12 We have previously reported a peptide-driven approach to identify a series of submicromolar inhibitors targeting CBX4/CBX7 and CBX6. [12][13][14] Potent peptidic inhibitors of CBX4/CBX7 have also been identified by the Frye group and have shown activity in cellular based studies. 9,15 The first small molecule inhibitors of any CBX protein also targeted CBX7.…”

Section: Introductionmentioning

confidence: 99%

Pan-Specific and Partially Selective Dye-Labeled Peptidic Inhibitors of the Polycomb Paralog Proteins

Milosevich¹,

McFarlane²,

Gignac³

et al. 2019

Preprint

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Epigenetic regulation of gene expression is in part controlled by post-translational modifications on histone proteins. Histone methylation is a key epigenetic mark that controls gene transcription and repression. There are five human polycomb paralog proteins (Cbx2/4/6/7/8) which use their chromodomains to recognize trimethylated lysine 27 on Histone 3 (H3K27me3). Recognition of the methyllysine side chain is achieved through multiple cation-pi interactions within an 'aromatic cage' motif. Despite high structural similarity within the chromodomains of this protein family, they each have unique functional roles and are linked to different cancers. Selective inhibition of different CBX proteins is highly desirable for both fundamental studies and potential therapeutic applications. We will report on a series of peptidic inhibitors that selectively target certain polycomb paralogs. We have identified peptidic scaffolds with sub-micromolar potency, and will report examples that are pan-specific and that are partially selective for individual members within the family. These results highlight important structure-activity relationships that allow for selectivity to be achieved through interactions outside of the methyllysine binding aromatic cage motif.

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“…The 12 new azapeptide analogues of ligand 1 were evaluated for their affinity for CBX7 in a competitive fluorescence polarization assay that measured the displacement of a dye‐labeled peptide ligand, as previously reported . Most of the new analogues were not measurably active in the assay up to the limits of their most concentrated solutions (0.8–1.8 mM).…”

Section: Chemistrymentioning

confidence: 99%

Aza‐amino acid scanning of chromobox homolog 7 (CBX7) ligands

Traoré

Gignac

Doan

et al. 2017

Journal of Peptide Science

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An aza-amino acid scan of peptide inhibitors of the chromobox homolog 7 (CBX7) was performed to study the conformational requirements for affinity to the methyllysine reader protein. Twelve azapeptide analogues were prepared using three different approaches employing respectively N-(Fmoc)aza-amino acid chlorides and submonomer azapeptide synthesis to install systematically aza-residues at the first four residues of the peptide, as well as to provide aza-lysine residues possessing saturated and unsaturated side chains. The aza-peptide ligands were evaluated in a chromobox homolog 7 binding assay, providing useful insight into structural requirements for affinity. Copyright © 2017 European Peptide Society and John Wiley & Sons, Ltd.

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Structure–Activity Relationships of Cbx7 Inhibitors, Including Selectivity Studies against Other Cbx Proteins

Cited by 18 publications

References 38 publications

Rational Adaptation of L3MBTL1 Inhibitors to Create Small‐Molecule Cbx7 Antagonists

Rational Adaptation of L3MBTL1 Inhibitors to Create Small‐Molecule Cbx7 Antagonists

Pan-Specific and Partially Selective Dye-Labeled Peptidic Inhibitors of the Polycomb Paralog Proteins

Aza‐amino acid scanning of chromobox homolog 7 (CBX7) ligands

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