Discovery of potent BET bromodomain 1 stereoselective inhibitors using DNA-encoded chemical library selections

Modukuri, Ram K.; Yu, Zhifeng; Tan, Zhi; Ta, Hai Minh; Ucisik, Melek N.; Jin, Zhuang; Anglin, Justin L.; Sharma, Kiran; Nyshadham, Pranavanand; Li, Feng; Riehle, Kevin; Faver, John C.; Duong, Kevin; Nagarajan, Sureshbabu; Simmons, Nicholas; Palmer, Stephen; Teng, Mingxing; Young, Damian W.; Yi, Joanna; Kim, Choel; Matzuk, Martin M.

doi:10.1073/pnas.2122506119

Cited by 22 publications

(19 citation statements)

References 35 publications

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“…DECL selection was performed as previously described. − Briefly, 53 different DECLs (total of 4.17 billion molecules) were combined and incubated with 0.2 μM of BMPR2-His kinase domain in 150 μL of a selection buffer (25 mM Tris–HCl pH 7.5, 150 mM NaCl, 10 mM MgCl2,1 mM CHAPS, 1 mM TCEP, 10 mM imidazole, and 0.1 mg/mL Sheared Salmon Sperm DNA). The same library pool without protein was incubated under the same conditions as the NTC to assess background binding of DECL molecules to the affinity resin.…”

Section: Methodsmentioning

confidence: 99%

“…To address the bias of count data caused by factors such as sample size and library diversity, we developed an in-house normalized z -score to quantify the enrichment of n-synthons. , A higher z -score indicates a more significant enrichment in the selection. The normalized z -score is calculated on the basis of modeling the selection data as binomial distribution. , The DNA sequencing process is considered as a random sampling process, and the z -score indicates the probability of observing k times out of n independent samples. The normalized z -score is calculated as follows: z n = p 0 − p normali p normali ( 1 − p i ) where p 0 is observed populations of n-synthons, whereas p i represents the expected populations of n-synthons.…”

Section: Methodsmentioning

confidence: 99%

“…The discovery of kinase inhibitors has relied on high-throughput screening and other strategies to identify hit compounds as starting points. Compound optimization is then achieved using concerted medicinal chemistry to generate more potent and selective lead-like compounds. − This pathway can be tremendously time-consuming and is greatly facilitated by structure. Recent studies have also used DNA-encoded chemistry technology (DEC-Tec) as a strategy to find kinase-selective leads. − To uncover kinase inhibitors with specificity for BMPR2, we used DEC-Tec to screen our multibillion compound library collection of small molecules using the kinase domain of BMPR2.…”

Section: Introductionmentioning

confidence: 99%

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Discovery of Highly Potent and BMPR2-Selective Kinase Inhibitors Using DNA-Encoded Chemical Library Screening

Modukuri

Monsivais

et al. 2023

J. Med. Chem.

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The discovery of monokinase-selective inhibitors for patients is challenging because the 500+ kinases encoded by the human genome share highly conserved catalytic domains. Until now, no selective inhibitors unique for a single transforming growth factor β (TGFβ) family transmembrane receptor kinase, including bone morphogenetic protein receptor type 2 (BMPR2), have been reported. This dearth of receptor-specific kinase inhibitors hinders therapeutic options for skeletal defects and cancer as a result of an overactivated BMP signaling pathway. By screening 4.17 billion "unbiased" and "kinase-biased" DNA-encoded chemical library molecules, we identified hits CDD-1115 and CDD-1431, respectively, that were low-nanomolar selective kinase inhibitors of BMPR2. Structure−activity relationship studies addressed metabolic lability and high-molecular-weight issues, resulting in potent and BMPR2-selective inhibitor analogs CDD-1281 (IC 50 = 1.2 nM) and CDD-1653 (IC 50 = 2.8 nM), respectively. Our work demonstrates that DNA-encoded chemistry technology (DEC-Tec) is reliable for identifying novel first-in-class, highly potent, and selective kinase inhibitors.

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Section: Methodsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Discovery of Highly Potent and BMPR2-Selective Kinase Inhibitors Using DNA-Encoded Chemical Library Screening

Modukuri

Monsivais

et al. 2023

J. Med. Chem.

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“…While this manuscript was in review, the reverse of this selection experiment was also performed by the same group to identify BD1-selective molecule CDD-787 with over 500-fold selectivity (see Table 3 below). 107 The binding pose of CDD-1102 in a crystal structure with BRDT-BD1 shows unique features of molecular recognition. Whereas traditional K ac mimics directly interact with the carboxamide nitrogen of a conserved asparagine residue and through a conserved water molecule to a tyrosine residue deeper in the binding pocket (Asn351 and Try308 in BRDT), CDD-1102 does not directly interact with the carboxamide of Asn351 and displaces the conserved water (Figure 27B).…”

Section: Cdd-1102mentioning

confidence: 99%

Recent progress and structural analyses of domain‐selective BET inhibitors

Divakaran

Harki

Pomerantz

2023

Medicinal Research Reviews

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Epigenetic mechanisms for controlling gene expression through heritable modifications to DNA, RNA, and proteins, are essential processes in maintaining cellular homeostasis. As a result of their central role in human diseases, the proteins responsible for adding, removing, or recognizing epigenetic modifications have emerged as viable drug targets. In the case of lysine‐ε‐N‐acetylation (Kac), bromodomains serve as recognition modules (“readers”) of this activating epigenetic mark and competition of the bromodomain‐Kac interaction with small‐molecule inhibitors is an attractive strategy to control aberrant bromodomain‐mediated gene expression. The bromodomain and extra‐terminal (BET) family proteins contain eight similar bromodomains. These BET bromodomains are among the more commonly studied bromodomain classes with numerous pan‐BET inhibitors showing promising anticancer and anti‐inflammatory efficacy. However, these results have yet to translate into Food and Drug Administration‐approved drugs, in part due to a high degree of on‐target toxicities associated with pan‐BET inhibition. Improved selectivity within the BET‐family has been proposed to alleviate these concerns. In this review, we analyze the reported BET‐domain selective inhibitors from a structural perspective. We highlight three essential characteristics of the reported molecules in generating domain selectivity, binding affinity, and mimicking Kac molecular recognition. In several cases, we provide insight into the design of molecules with improved specificity for individual BET‐bromodomains. This review provides a perspective on the current state of the field as this exciting class of inhibitors continue to be evaluated in the clinic.

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“…After tagged barcode amplification and sequencing, the optimal binder can be thus identified in the selection of DELs. 20–25 Generally, the encoded libraries are constructed via iterative steps of combinatory synthesis and enzymatic encoding ligation. 26–30 Numerous reaction toolkits, which must be DNA-compatible, have been thereby developed and employed to construct encoded libraries, and the building blocks (BBs) for library construction should be conveniently accessible or commercially available to expand the chemical diversities to more complicated molecular architectures beyond encoding early-stage peptide-like libraries.…”

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confidence: 99%

Incorporation of viridicatin alkaloid-like scaffolds into DNA-encoded chemical libraries

et al. 2023

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Discovery of potent BET bromodomain 1 stereoselective inhibitors using DNA-encoded chemical library selections

Cited by 22 publications

References 35 publications

Discovery of Highly Potent and BMPR2-Selective Kinase Inhibitors Using DNA-Encoded Chemical Library Screening

Discovery of Highly Potent and BMPR2-Selective Kinase Inhibitors Using DNA-Encoded Chemical Library Screening

Recent progress and structural analyses of domain‐selective BET inhibitors

Incorporation of viridicatin alkaloid-like scaffolds into DNA-encoded chemical libraries

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