Cation–π interactions in CREBBP bromodomain inhibition: an electrostatic model for small-molecule binding affinity and selectivity

“…The bottom pyridine ring of the CBP complex rotates 90°, as CBP lacks the Trp for a pi–pi interaction in the LPF pocket. However, XP-524 forms a cation–pi interaction with Arg-1173, a key interaction in the design of potent EP300/CBP inhibitors ( 26 – 28 ). Contrastingly, JQ-1 is not able to capture this important cation–pi interaction, as the chlorophenyl ring of JQ-1 clashes with Arg-1173, thereby blocking the binding of JQ-1 to CBP and the ability of JQ-1 to act as an EP300/CBP inhibitor ( Fig.…”

Section: Resultsmentioning

confidence: 99%

XP-524 is a dual-BET/EP300 inhibitor that represses oncogenic KRAS and potentiates immune checkpoint inhibition in pancreatic cancer

Principe

Xiong

et al. 2022

Proc. Natl. Acad. Sci. U.S.A.

View full text Add to dashboard Cite

Pancreatic ductal adenocarcinoma (PDAC) is associated with extensive dysregulation of the epigenome and epigenetic regulators, such as bromodomain and extraterminal motif (BET) proteins, have been suggested as potential targets for therapy. However, single-agent BET inhibition has shown poor efficacy in clinical trials, and no epigenetic approaches are currently used in PDAC. To circumvent the limitations of the current generation of BET inhibitors, we developed the compound XP-524 as an inhibitor of the BET protein BRD4 and the histone acetyltransferase EP300/CBP, both of which are ubiquitously expressed in PDAC tissues and cooperate to enhance tumorigenesis. XP-524 showed increased potency and superior tumoricidal activity than the benchmark BET inhibitor JQ-1 in vitro, with comparable efficacy to higher-dose JQ-1 combined with the EP300/CBP inhibitor SGC-CBP30. We determined that this is in part due to the epigenetic silencing of KRAS in vitro, with similar results observed using ex vivo slice cultures of human PDAC tumors. Accordingly, XP-524 prevented KRAS-induced, neoplastic transformation in vivo and extended survival in two transgenic mouse models of aggressive PDAC. In addition to the inhibition of KRAS/MAPK signaling, XP-524 also enhanced the presentation of self-peptide and tumor recruitment of cytotoxic T lymphocytes, though these lymphocytes remained refractory from full activation. We, therefore, combined XP-524 with an anti–PD-1 antibody in vivo, which reactivated the cytotoxic immune program and extended survival well beyond XP-524 in monotherapy. Pending a comprehensive safety evaluation, these results suggest that XP-524 may benefit PDAC patients and warrant further exploration, particularly in combination with immune checkpoint inhibition.

show abstract

“…Gap between corrected and raw complexation energy is equal to BSSE energy. In all CP calculations empirical dispersion method, D2 version of Grimme's dispersion correction [35], was applied with B3LYP and WB97XD by defining the values of the functional-specific global parameters for non-covalent interactions [36,37].…”

Section: Methodsmentioning

confidence: 99%

Complexation Energies and Electronic-Structural Properties of Adamantane Derivatives: A DFT Study

Karakaya

2019

Adıyaman University Journal of Science

View full text Add to dashboard Cite

This article is an investigation related to the complexation energies, binding abilities, frontier molecular orbital's energy gaps and dipole moments on dimeric forms of 1-adamantanol, 1-adamantanemethylamine and 1-adamantanecarboxylic acid as the adamantane derivatives. All the optimizations, counterpoise corrections and complexation energy computations have been achieved by density functional theory with B3LYP and WB97XD functionals. In all counterpoise calculations have been used the empirical dispersion method with B3LYP and WB97XD for non-covalent interactions. The more favorable complexation energies have been obtained by B3LYP with the addition of dispersion correction. In addition, the images mapped with total density and electrostatic potential have been obtained in this study.

show abstract

Cation–π interactions in CREBBP bromodomain inhibition: an electrostatic model for small-molecule binding affinity and selectivity

Cited by 27 publications

References 81 publications

Cation–π interactions in protein–ligand binding: theory and data-mining reveal different roles for lysine and arginine

Cation–π interactions in protein–ligand binding: theory and data-mining reveal different roles for lysine and arginine

XP-524 is a dual-BET/EP300 inhibitor that represses oncogenic KRAS and potentiates immune checkpoint inhibition in pancreatic cancer

Complexation Energies and Electronic-Structural Properties of Adamantane Derivatives: A DFT Study

Contact Info

Product

Resources

About