In silico tools to aid medicinal chemistry: optimising bromodomain inhibitors

In silico tools to aid medicinal chemistry: optimising bromodomain inhibitors

<p>Development of ligands for bromodomains has expanded our understanding of gene regulation and epigenetic links to disease. These acetylated lysine ‘reader’ domains are found within larger macromolecules that are involved in gene transcription and degradation. This thesis looks to employ...

وصف كامل

التفاصيل البيبلوغرافية
المؤلف الرئيسي:	Bluck, J
مؤلفون آخرون:	Biggin, P
التنسيق:	أطروحة
منشور في:	2019

مواد مشابهة

Epigenetic mechanisms in silico: understanding demethylation and rational design of bromodomain inhibitors
حسب: Coelho, W
منشور في: (2017)

Development of small molecule CREBBP bromodomain ligands using medicinal chemistry-based approaches
حسب: Moroglu, M
منشور في: (2020)

Emerging tools to investigate bromodomain functions
حسب: Kougnassoukou Tchara, P, وآخرون
منشور في: (2019)

Developing inhibitors of bromodomain-histone interactions
حسب: Hewings, D
منشور في: (2014)

Small-molecule bromodomain inhibitors for cancer therapy
حسب: Qi, J, وآخرون
منشور في: (2010)

BET bromodomain ligands: Probing the WPF shelf to improve BRD4 bromodomain affinity and metabolic stability
حسب: Jennings, L, وآخرون
منشور في: (2018)

Dual kinase-bromodomain inhibitors for rationally designed polypharmacology.
حسب: Ciceri, P, وآخرون
منشور في: (2014)

Targeting low-druggability bromodomains: fragment based screening and inhibitor design against the BAZ2B bromodomain.
حسب: Ferguson, F, وآخرون
منشور في: (2013)

Chemical probes and inhibitors of bromodomains outside the BET family
حسب: Moustakim, M, وآخرون
منشور في: (2016)

Developing small molecule inhibitors of bromodomain-histone interactions
حسب: Wilson, B, وآخرون
منشور في: (2015)

Development of small molecule inhibitors of the bromodomain-histone interaction
حسب: Rooney, TPC
منشور في: (2014)

Discovery of BET bromodomain inhibitors and their role in target validation
حسب: Mueller, S, وآخرون
منشور في: (2014)

Bromodomain Protein Inhibitors Reorganize the Chromatin of Synovial Fibroblasts
حسب: Monika Krošel, وآخرون
منشور في: (2023-04-01)

Bromodomain inhibitors and cancer therapy: From structures to applications
حسب: Montserrat Pérez-Salvia, وآخرون
منشور في: (2017-05-01)

Enhanced efficacy of histone deacetylase inhibitor combined with bromodomain inhibitor in glioblastoma
حسب: Wei Meng, وآخرون
منشور في: (2018-10-01)

Pyronaridine as a Bromodomain-Containing Protein 4-<i>N</i>-Terminal Bromodomain (BRD4-BD1) Inhibitor: <i>In Silico</i> Database Mining, Molecular Docking, and Molecular Dynamics Simulation
حسب: Mahmoud A. A. Ibrahim, وآخرون
منشور في: (2023-07-01)

Bromodomain-peptide displacement assays for interactome mapping and inhibitor discovery.
حسب: Philpott, M, وآخرون
منشور في: (2011)

Bromodomain-peptide displacement assays for interactome mapping and inhibitor discovery.
حسب: Philpott, M, وآخرون
منشور في: (2011)

Corrigendum: Dual kinase-bromodomain inhibitors for rationally designed polypharmacology.
حسب: Ciceri, P, وآخرون
منشور في: (2014)

Chemical Space Expansion of Bromodomain Ligands Guided by in Silico Virtual Couplings (AutoCouple)
حسب: Laurent Batiste, وآخرون
منشور في: (2018-02-01)

Development of selective CBP/P300 benzoxazepine bromodomain inhibitors
حسب: Popp, T, وآخرون
منشور في: (2016)

Developing small molecule inhibitors of the CREBBP bromodomain-histone interaction
حسب: Rooney, T, وآخرون
منشور في: (2012)

BET Bromodomain Inhibitors: Novel Design Strategies and Therapeutic Applications
حسب: Kenneth K. W. To, وآخرون
منشور في: (2023-03-01)

Bromodomain Inhibitors as Therapeutics for Herpesvirus-Related Disease: All BETs Are Off?
حسب: Ian J. Groves, وآخرون
منشور في: (2020-07-01)

Optimisation of Financial Risk with the Aid of Hedging Tools
حسب: Jaroslav Slepecky
منشور في: (2002-12-01)

BROMODOMAIN INHIBITORS REDUCE TH17-TYPE RESPONSES IN SPONDYLOARTHRITIS IN VITRO
حسب: Hammitzsch, A, وآخرون
منشور في: (2014)

Synthesis and biological investigation of (+)-JD1, an organometallic BET bromodomain inhibitor
حسب: Hassell-Hart, S, وآخرون
منشور في: (2019)

Bioactivation of Isoxazole-Containing Bromodomain and Extra-Terminal Domain (BET) Inhibitors
حسب: Noah R. Flynn, وآخرون
منشور في: (2021-06-01)

BET Bromodomain Inhibition Synergizes with PARP Inhibitor in Epithelial Ovarian Cancer
حسب: Sergey Karakashev, وآخرون
منشور في: (2017-12-01)

Chemical tools to probe the role of bromodomains in the parasite Trypanosoma cruzi
حسب: Laurin, CMC
منشور في: (2019)

Resistance to BET Bromodomain Inhibitors Is Mediated by Kinome Reprogramming in Ovarian Cancer
حسب: Alison M. Kurimchak, وآخرون
منشور في: (2016-08-01)

RVX-208, an inhibitor of BET transcriptional regulators with selectivity for the second bromodomain.
حسب: Picaud, S, وآخرون
منشور في: (2013)

RVX-208, an inhibitor of BET transcriptional regulators with selectivity for the second bromodomain
حسب: Picaud, S, وآخرون
منشور في: (2013)

Benzodiazepines and benzotriazepines as protein interaction inhibitors targeting bromodomains of the BET family.
حسب: Filippakopoulos, P, وآخرون
منشور في: (2012)

Response and resistance to BET bromodomain inhibitors in triple-negative breast cancer
حسب: Shu, Shaokun, وآخرون
منشور في: (2017)

Cracking the histone code: Developing inhibitors of bromodomain-acetyl-lysine interactions
حسب: Conway, S
منشور في: (2013)

Benzodiazepines and benzotriazepines as protein interaction inhibitors targeting bromodomains of the BET family
حسب: Filippakopoulos, P, وآخرون
منشور في: (2012)

The design and synthesis of 5-and 6-isoxazolylbenzimidazoles as selective inhibitors of the BET bromodomains
حسب: Hay, D, وآخرون
منشور في: (2013)

Effect of BET missense mutations on bromodomain function, inhibitor binding and stability
حسب: Lori, L, وآخرون
منشور في: (2016)

Bromodomain inhibitor treatment leads to overexpression of multiple kinases in cancer cells
حسب: Darshan S. Chandrashekar, وآخرون
منشور في: (2024-11-01)