R. Al-Awar scite author profile

R. Al-Awar

5Publications

24Citation Statements Received

9Citation Statements Given

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Discovery of an MLLT1/3 YEATS Domain Chemical Probe

Moustakim

Christott²,

Monteiro³

et al. 2018

Preprint

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<p>YEATS domain (YD) containing proteins are an emerging</p> <p>class of epigenetic targets in drug discovery. Dysregulation of these modified lysine binding proteins has been linked to the onset and progression of cancers. We herein report the discovery and characterisation of the first small molecule chemical probe, SGC-iMLLT, for the YD of MLLT1 (ENL/YEATS1) and MLLT3 (AF9/YEATS3). SGC-iMLLT is a potent and selective inhibitor of MLLT1/3 -histone interactions. Excellent selectivity over other human YD proteins (YEATS2/4) and bromodomains was observed. Furthermore, our probe displays cellular target engagement of MLLT1 and MLLT3. The first small molecule X-ray co-crystal structures with the MLLT1 YD are also reported. This first in class probe molecule can be used to understand MLLT1/3 associated biology and the therapeutic potential of small molecule YD inhibitors.</p>

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287 The discovery and optimization of small molecule antagonists of the WDR5–MLL interaction

Al-Awar¹,

Getlik²,

Smil³

et al. 2014

European Journal of Cancer

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Crystal structure of human WDR5 in complex with compound 9h

Dong¹,

Dombrovski²,

Smil³

et al. 2015

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Crystal structure of murine IRE1 in complex with MKC9989 inhibitor

Sanches¹,

Duffy²,

Talukdar³

et al. 2014

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Gent-11. Small Molecule Epigenetic Screen Identifies Novel Ezh2 and Hdac Inhibitors That Target Glioblastoma Brain Tumor-Initiating Cells

Grinshtein

Rioseco

Marcellus³

et al. 2016

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R. Al-Awar

Discovery of an MLLT1/3 YEATS Domain Chemical Probe

287 The discovery and optimization of small molecule antagonists of the WDR5–MLL interaction

Crystal structure of human WDR5 in complex with compound 9h

Crystal structure of murine IRE1 in complex with MKC9989 inhibitor

Gent-11. Small Molecule Epigenetic Screen Identifies Novel Ezh2 and Hdac Inhibitors That Target Glioblastoma Brain Tumor-Initiating Cells

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