&lt;p&gt;Novel HDAC/Tubulin Dual Inhibitor: Design, Synthesis and Docking Studies of α-Phthalimido-Chalcone Hybrids as Potential Anticancer Agents with Apoptosis-Inducing Activity&lt;/p&gt;

Mourad, Ahmed A.E.; Mourad, M.; Jones, Peter G.

doi:10.2147/dddt.s256756

Cited by 25 publications

(19 citation statements)

References 44 publications

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“…Chalcones have been shown to exhibit anticancer activity through their inhibitory potential against various targets, such as 5α-reductase [ 187 ], aromatase [ 188 ], histone deacetylase inhibitors (HDAC) [ 189 , 190 ], proteasome [ 191 , 192 ], JAK/STAT signaling pathways [ 193 ], cell division cycle 25 (CD25) [ 194 ], cathepsin-K [ 72 , 195 ], topoisomerase-II [ 196 , 197 ], Wnt [ 198 , 199 ], ROS/MAPK [ 200 ], p38 [ 201 , 202 ] and mTOR [ 203 , 204 ]. However, these studies are not covered in this review because not enough evidence has been provided to indicate that these proteins or pathways are direct targets of chalcones.…”

Section: Representative Mechanisms Of Anticancer Action Of Chalconesmentioning

confidence: 99%

Chalcone Derivatives: Role in Anticancer Therapy

et al. 2021

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Chalcones (1,3-diaryl-2-propen-1-ones) are precursors for flavonoids and isoflavonoids, which are common simple chemical scaffolds found in many naturally occurring compounds. Many chalcone derivatives were also prepared due to their convenient synthesis. Chalcones as weandhetic analogues have attracted much interest due to their broad biological activities with clinical potentials against various diseases, particularly for antitumor activity. The chalcone family has demonstrated potential in vitro and in vivo activity against cancers via multiple mechanisms, including cell cycle disruption, autophagy regulation, apoptosis induction, and immunomodulatory and inflammatory mediators. It represents a promising strategy to develop chalcones as novel anticancer agents. In addition, the combination of chalcones and other therapies is expected to be an effective way to improve anticancer therapeutic efficacy. However, despite the encouraging results for their response to cancers observed in clinical studies, a full description of toxicity is required for their clinical use as safe drugs for the treatment of cancer. In this review, we will summarize the recent advances of the chalcone family as potential anticancer agents and the mechanisms of action. Besides, future applications and scope of the chalcone family toward the treatment and prevention of cancer are brought out.

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Section: Representative Mechanisms Of Anticancer Action Of Chalconesmentioning

confidence: 99%

Chalcone Derivatives: Role in Anticancer Therapy

et al. 2021

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“…It has been reported that the combination of SAHA and vincristine (a tubulin inhibitor) could achieve synergistic effects in leukemia, which provides a theoretical basis for designing dual tubulin/HDAC inhibitors. Several groups have reported the discovery of novel tubulin/HDAC dual inhibitors in recent years. ,− For instance, Diana and co-workers designed dual tubulin/HDAC inhibitors that demonstrated potent anticancer activities . Despite these advancements, the therapeutic value of dual tubulin/HADC inhibitors (in particular, dual inhibitors with HDAC-isoform-selectivity) remains to be further explored.…”

Section: Introductionmentioning

confidence: 99%

Efficient Synthesis and Bioevaluation of Novel Dual Tubulin/Histone Deacetylase 3 Inhibitors as Potential Anticancer Agents

Peng

Chen

et al. 2021

J. Med. Chem.

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Novel dual HDAC3/tubulin inhibitors were designed and efficiently synthesized by combining the pharmacophores of SMART (tubulin inhibitor) and MS-275 (HDAC inhibitor), among which compound 15c was found to be the most potent and balanced HDAC3/tubulin dual inhibitor with high HDAC3 activity (IC 50 = 30 nM) and selectivity (SI > 1000) as well as excellent antiproliferative potency against various cancer cell lines, including an HDAC-resistant gastric cancer cell line (YCC3/7) with IC 50 values in the range of 30−144 nM. Compound 15c inhibited B16-F10 cancer cell migration and colony formation. In addition, 15c demonstrated significant in vivo antitumor efficacy in a B16-F10 melanoma tumor model with a better TGI (70.00%, 10 mg/kg) than that of the combination of MS-275 and SMART. Finally, 15c presented a safe cardiotoxicity profile and did not cause nephro-/ hepatotoxicity. Collectively, this work shows that compound 15c represents a novel tubulin/HDAC3 dual-targeting agent deserving further investigation as a potential anticancer agent.

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“…The results of PLIP analysis of training set compounds and simulated hits showed a concrete relationship between the salient chemical features (Hypo 1) present in training set compounds (FDA approved drugs) and molecular interactions observed in simulated hits in complex with HDAC3. The structural information for five drug molecules such as TSA (5EEF, 16), LBH (5EF8, 1), JNJ-26481585 (6HSK, 2), ACY-1215 (5WGL, 1), and SHH (4LXZ, 11) was retrieved from the crystal structures whereas, for NVP-LAQ824, MS-275 and VPA drugs were obtained from the earlier docking studies 58 – 60 . Total 31 co-crystal structures of these five drugs were downloaded from the protein data bank and analyzed for protein–ligand interactions profiles using PLIP online server and DS.…”

Section: Resultsmentioning

confidence: 99%

Identification of novel leads as potent inhibitors of HDAC3 using ligand-based pharmacophore modeling and MD simulation

Kumbhar

Nimal

Barale

et al. 2022

Sci Rep

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In the landscape of epigenetic regulation, histone deacetylase 3 (HDAC3) has emerged as a prominent therapeutic target for the design and development of candidate drugs against various types of cancers and other human disorders. Herein, we have performed ligand-based pharmacophore modeling, virtual screening, molecular docking, and MD simulations to design potent and selective inhibitors against HDAC3. The predicted best pharmacophore model ‘Hypo 1’ showed excellent correlation (R2 = 0.994), lowest RMSD (0.373), lowest total cost value (102.519), and highest cost difference (124.08). Hypo 1 consists of four salient pharmacophore features viz. one hydrogen bond acceptor (HBA), one ring aromatic (RA), and two hydrophobic (HYP). Hypo 1 was validated by Fischer's randomization with a 95% of confidence level and the external test set of 60 compounds with a good correlation coefficient (R2 = 0.970). The virtual screening of chemical databases, drug-like properties calculations followed by molecular docking resulted in identifying 22 representative hit compounds. Performed 50 ns of MD simulations on top three hits were retained the salient π-stacking, Zn2+ coordination, hydrogen bonding, and hydrophobic interactions with catalytic residues from the active site pocket of HDAC3. Total binding energy calculated by MM-PBSA showed that the Hit 1 and Hit 2 formed stable complexes with HDAC3 as compared to reference TSA. Further, the PLIP analysis showed a close resemblance between the salient pharmacophore features of Hypo 1 and the presence of molecular interactions in co-crystallized FDA-approved drugs. We conclude that the screened hit compounds may act as potent inhibitors of HDAC3 and further preclinical and clinical studies may pave the way for developing them as effective therapeutic agents for the treatment of different cancers and neurodegenerative disorders.

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<p>Novel HDAC/Tubulin Dual Inhibitor: Design, Synthesis and Docking Studies of α-Phthalimido-Chalcone Hybrids as Potential Anticancer Agents with Apoptosis-Inducing Activity</p>

Cited by 25 publications

References 44 publications

Chalcone Derivatives: Role in Anticancer Therapy

Chalcone Derivatives: Role in Anticancer Therapy

Efficient Synthesis and Bioevaluation of Novel Dual Tubulin/Histone Deacetylase 3 Inhibitors as Potential Anticancer Agents

Identification of novel leads as potent inhibitors of HDAC3 using ligand-based pharmacophore modeling and MD simulation

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