A Novel Selective JAK2 Inhibitor Identified Using Pharmacological Interactions

Lin, Tony Eight; HuangFu, Wei-Chun; Chao, Min Wu; Sung, Tzu-Ying; Chang, Chao-Di; Chen, Yiying; Hsieh, Jui-Hua; Tu, Huang‐Ju; Huang, Han-Pang; Pan, Shiow‐Lin; Hsu, Kai‐Cheng

doi:10.3389/fphar.2018.01379

Cited by 27 publications

(28 citation statements)

References 60 publications

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“…In this study, this aberration was observed in six patients including two normal-like TN and three basal-like TN tumours highlighting the genomic similarities between triple-negative molecular phenotypes across FMCs and HBCs. Tumours carrying this mutation are characterised by the co-gain of PD-L1, PD-L2, and JAK2, and might benefit from immune checkpoint targeted therapies 57,78,79 or adjuvant therapy with JAK2-specific inhibitors 80,81 . Interestingly, the Jak-STAT signalling pathway was the only KEGG pathway enriched with amplified genes in the basal-like TN subtype.…”

Section: Discussionmentioning

confidence: 99%

Analysis of Copy-Number Variations and Feline Mammary Carcinoma Survival

Granados-Soler

Bornemann-Kolatzki²,

Beck³

et al. 2020

Sci Rep

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Feline mammary carcinomas (FMCs) are highly malignant. As the disease-free survival (DFS) and overall survival (OS) are short, prognostication is crucial. Copy-number variations (CNVs) analysis by nextgeneration sequencing serves to identify critical cancer-related genomic regions. Thirty-three female cats with FMCs were followed during two years after surgery. Tumours represented tubulopapillary and solid carcinomas encompassing six molecular subtypes. Regardless of the histopathological diagnosis, molecular subtypes showed important differences in survival. Luminal A tumours exhibited the highest DFS (p = 0.002) and cancer-specific OS (p = 0.001), and the lowest amount of CNVs (p = 0.0001). In contrast, basal-like triple-negative FMCs had the worst outcome (DFS, p < 0.0001; and OS, p < 0.00001) and were the most aberrant (p = 0.05). In the multivariate analysis, copy-number losses (CNLs) in chromosome B1 (1-23 Mb) harbouring several tumour-repressors (e.g. CSMD1, MTUS1, MSR1, DBC2, and TUSC3) negatively influenced DFS. Whereas, copy-number gains (CNGs) in B4 (1-29 Mb) and F2 (64-82.3 Mb) comprising epithelial to mesenchymal transition genes and metastasis-promoting transcription factors (e.g. GATA3, VIM, ZEB1, and MYC) negatively influenced DFS and cancer-specific OS. These data evidence an association between specific CNVs in chromosomes B1, B4 and F2, and poor prognosis in FMCs.

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Section: Discussionmentioning

confidence: 99%

Analysis of Copy-Number Variations and Feline Mammary Carcinoma Survival

Granados-Soler

Bornemann-Kolatzki²,

Beck³

et al. 2020

Sci Rep

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“…The docking pose of the 30 known BTK inhibitors was analysed to identify possible binding interactions. This study recognises a binding interaction if a residue was observed to form an interaction with ≥ 50% of the BTK inhibitors 17 . The calculation for binding interactions is as follows: where the binding interaction score, S ( i ), for a compound, i , equals the number of binding interactions the compound forms, N ( i ), plus the docking score , D ( i ), of a compound i generated using LeadIT.…”

Section: Methodsmentioning

confidence: 87%

“…For our study, a binding interaction was considered if ≥ 50% of the 30 diverse BTK inhibitors formed an interaction with a binding site residue 17 . As a result, two hydrogen-bonding and four hydrophobic interactions were identified ( Figure 1(A,B) ).…”

Section: Resultsmentioning

confidence: 99%

“…Compounds were then removed if they exhibited Pan Assay Interference Compounds (PAINS) structures. PAINS structures often display false positives in high-throughput screens 17 . The Lipinski Rule of Five estimates pharmacokinetics of compounds in the human body 20 .…”

Section: Methodsmentioning

confidence: 99%

“…For example, small-molecule kinase inhibitors targeting the ATP binding site typically form hydrogen bonds with hinge residues 16 . Filtering compounds based on both their docking scores and binding interactions has proven a useful strategy to not only better understand the protein-ligand binding mechanism, but to improve the hit rate for potential inhibitors 17 . Herein, we identified binding interactions within the BTK binding site by docking known BTK inhibitors.…”

Section: Introductionmentioning

confidence: 99%

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Structure-based virtual screening and biological evaluation of novel small-molecule BTK inhibitors

Lin

Sung

Chao

et al. 2021

Journal of Enzyme Inhibition and Medicinal Chemistry

Self Cite

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Bruton tyrosine kinase (BTK) is linked to multiple signalling pathways that regulate cellular survival, activation, and proliferation. A covalent BTK inhibitor has shown favourable outcomes for treating B cell malignant leukaemia. However, covalent inhibitors require a high reactive warhead that may contribute to unexpected toxicity, poor selectivity, or reduced effectiveness in solid tumours. Herein, we report the identification of a novel noncovalent BTK inhibitor. The binding interactions (i.e. interactions from known BTK inhibitors) for the BTK binding site were identified and incorporated into a structure-based virtual screening (SBVS). Top-rank compounds were selected and testing revealed a BTK inhibitor with >50% inhibition at 10 µM concentration. Examining analogues revealed further BTK inhibitors. When tested across solid tumour cell lines, one inhibitor showed favourable inhibitory activity, suggesting its potential for targeting BTK malignant tumours. This inhibitor could serve as a basis for developing an effective BTK inhibitor targeting solid cancers.

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3D‐QSAR, Molecular Docking and Molecular Dynamics Analysis of 1,2,3,4‐Tetrahydroquinoxalines as BRD4/BD2 Inhibitors

Quan

et al. 2022

ChemistrySelect

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BRD4 plays an indispensable role in cell cycle regulation, affecting processes such as cell proliferation, apoptosis and transcription. In this article, a three-dimensional quantitative conformational relationship (3D-QSAR) was used to investigate the molecular simulations related to 45 tetrahydrooxazole BRD4/BD2 selective inhibitors. 3D-QSAR models were developed based on two different analytical methods, COMFA and COMSIA. All CoMSIA field combinations were compared together and the best CoMSIA model was selected based on external validation and model prediction results. Both CoMSIA (S + E + H + D (q 2 = 0.808, r 2 = 0.99)) and CoMFA models (q 2 = 0.779;,r 2 = 0.962) predicted the internal and external well.Twenty small molecules with higher inhibitory activity than the template compound were designed by 3D-QSAR model prediction and quantum chemistry analysis, screened by molecular docking and ADMET methods, and five novel compounds were found to have better predicted activity and binding affinity. Molecular dynamics simulations showed that PRO70, PRO371, TYR428, ASN429 and VAL435 are important residues that can interact with the ligands. Moreover, further structural optimization of the more active candidate compounds will provide an essential theoretical basis of the synthesis and design of novel BRD4/BD2 inhibitors.

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A Novel Selective JAK2 Inhibitor Identified Using Pharmacological Interactions

Cited by 27 publications

References 60 publications

Analysis of Copy-Number Variations and Feline Mammary Carcinoma Survival

Analysis of Copy-Number Variations and Feline Mammary Carcinoma Survival

Structure-based virtual screening and biological evaluation of novel small-molecule BTK inhibitors

3D‐QSAR, Molecular Docking and Molecular Dynamics Analysis of 1,2,3,4‐Tetrahydroquinoxalines as BRD4/BD2 Inhibitors

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