HDAC4 Inhibitors with Cyclic Linker and Non‐hydroxamate Zinc Binding Group: Design, Synthesis, HDAC Screening and <i>in</i> <i>vitro</i> Cytotoxicity evaluation.

Tilekar, Kalpana; Hess, Jessica D.; Upadhyay, Neha; Schweipert, Markus; Flath, Felix; Gutierrez, Denisse A.; Loiodice, Fulvio; Lavecchia, Antonio; Meyer‐Almes, Franz‐Josef; Aguilera, Renato J.; Ramaa, C. S.

doi:10.1002/slct.202102061

Cited by 9 publications

(9 citation statements)

References 61 publications

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“…The authors attributed the preference to bind HDAC4 to the carbonyl group of the TZD warhead. It was noted that previously described N-substituted TZD analogs were inactive, highlighting the importance of the NH group for HDAC4 selectivity [161]. Interestingly, compound 88 showed inhibitory activity of 750 nM and 12 µM toward HDAC4 and HDAC8, respectively, supporting prior studies suggesting a chelation of HDAC8 via the amide carbonyl.…”

Section: Thiazolidinedione (Tzd) Warheadssupporting

confidence: 62%

“…Additional evaluation of 85 in CCRF-CEM tumor xenografts led to significant tumor regression [160]. Follow-up studies by Tilekar et al [161] identified TZD derivatives with a pyridine linker, replacing the naphthyl group. The most potent compound of the series 87 showed a potency of 4.9 µM toward HDAC4 and greater than 10-fold selectivity over HDAC8.…”

Section: Thiazolidinedione (Tzd) Warheadsmentioning

confidence: 99%

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Non-Hydroxamate Zinc-Binding Groups as Warheads for Histone Deacetylases

Frühauf

Meyer‐Almes

2021

Molecules

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Histone deacetylases (HDACs) remove acetyl groups from acetylated lysine residues and have a large variety of substrates and interaction partners. Therefore, it is not surprising that HDACs are involved in many diseases. Most inhibitors of zinc-dependent HDACs (HDACis) including approved drugs contain a hydroxamate as a zinc-binding group (ZBG), which is by far the biggest contributor to affinity, while chemical variation of the residual molecule is exploited to create more or less selectivity against HDAC isozymes or other metalloproteins. Hydroxamates have a propensity for nonspecificity and have recently come under considerable suspicion because of potential mutagenicity. Therefore, there are significant concerns when applying hydroxamate-containing compounds as therapeutics in chronic diseases beyond oncology due to unwanted toxic side effects. In the last years, several alternative ZBGs have been developed, which can replace the critical hydroxamate group in HDACis, while preserving high potency. Moreover, these compounds can be developed into highly selective inhibitors. This review aims at providing an overview of the progress in the field of non-hydroxamic HDACis in the time period from 2015 to present. Formally, ZBGs are clustered according to their binding mode and structural similarity to provide qualitative assessments and predictions based on available structural information.

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Section: Thiazolidinedione (Tzd) Warheadssupporting

confidence: 62%

Section: Thiazolidinedione (Tzd) Warheadsmentioning

confidence: 99%

Non-Hydroxamate Zinc-Binding Groups as Warheads for Histone Deacetylases

Frühauf

Meyer‐Almes

2021

Molecules

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“…This study evaluated 223 TZD ligand analogs including newly synthesized compounds PB1-PB9 and GB1-GB36 with different substitution patterns (Table S1). Many of the TZD ligands have been published very recently to be HDAC4 or HDAC8 inhibitors [18,19,25]. This large ensemble of TZD ligands was utilized to derive a SAR and identify ligand moieties crucial for binding to the catalytic domain of human wild type histone deacetylase 4 (cdHDAC4 wt ).…”

Section: Chemistry Synthesis Of Compounds Pb1-pb9 and Gb1-gb36mentioning

confidence: 99%

“…Furthermore, some TZD ligands are capable to inhibit aldose reductase (ALR2), protein tyrosine phosphatase 1B (PTP1B) and α-glucosidase [18]. Very recently, we reported on TZD-containing ligands, which are capable to inhibit HDAC4 [18,19]. Enzyme activity assays of the HDAC family demonstrated activity of TZD ligands against HDAC4 or HDAC8 depending on the substitution pattern.…”

Section: Introductionmentioning

confidence: 99%

Mechanistic Insights into Binding of Ligands with Thiazolidinedione Warhead to Human Histone Deacetylase 4

et al. 2021

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Recently, we have reported that non-hydroxamate thiazolidinedione (TZD) analogs are capable of inhibiting human deacetylase 4 (HDAC4). This study aims at the dissection of the molecular determinants and kinetics of the molecular recognition of TZD ligands by HDAC4. For this purpose, a structure activity relationship analysis of 225 analogs was combined with a comprehensive study of the enzyme and binding kinetics of a variety of HDAC4 mutant variants. The experimental data were rationalized by docking to the two major conformations of HDAC4. TZD ligands are competitive inhibitors and bind via a two-step mechanism involving principal molecular recognition and induced fit. The residence time of 24 g is (34 ± 3) min and thus much larger than that of the canonical pan-HDAC inhibitor SAHA ((5 ± 2) min). Importantly, the binding kinetics can be tuned by varying the structure of the CAP group.

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“…incorporated a common pharmacophoric feature, which is a heterocyclic ring, "2,4-thiazolidinedione (TZD)" as a central or peripheral moiety that significantly contributed to antitumor activity by targeting single or multiple cancer hallmarks. [5][6][7][8][9][10][11][12][13][14][15] However, we also published compounds without the TZD nucleus showing good antiproliferative activity (Figure 1). [16][17][18][19][20][21][22][23][24][25] Interestingly, there are countless pieces of literature demonstrating compounds with anticancer activity incorporating various heterocyclic rings.…”

Section: Introductionmentioning

confidence: 96%

Design, in silico studies, synthesis, and in vitro anticancer assessment of new naphthylidene isoxazolidinedione derivatives

Upadhyay,

Tilekar,

Oak

et al. 2024

Vietnam Journal of Chemistry

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Cancer is the most destructive and fatal disease, representing an urgent medical challenge to the world. The discovery of a new anticancer candidate may help reduce or eliminate this alarming disease to a greater extent. On similar lines, in silico research was carried out on novel naphthylidene isoxazolidinedione derivatives that were logically conceived, synthesized, purified, and structurally characterized. In vitro biological evaluation revealed the most active compound 4d with an inhibitory concentration of 42.87 µm against K562 and 47.42 µm on A549 cells. The anticancer activity of this naphthylidene isoxazolidinedione derivative was evident by cell cycle and apoptosis assays, which showed arrest of the G2/M phase (65.6%) of the K562 cells and induction of apoptosis with 21.47% apoptotic cells as compared to 0.2% of untreated cells, respectively.

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HDAC4 Inhibitors with Cyclic Linker and Non‐hydroxamate Zinc Binding Group: Design, Synthesis, HDAC Screening and in vitro Cytotoxicity evaluation.

Cited by 9 publications

References 61 publications

Non-Hydroxamate Zinc-Binding Groups as Warheads for Histone Deacetylases

Non-Hydroxamate Zinc-Binding Groups as Warheads for Histone Deacetylases

Mechanistic Insights into Binding of Ligands with Thiazolidinedione Warhead to Human Histone Deacetylase 4

Design, in silico studies, synthesis, and in vitro anticancer assessment of new naphthylidene isoxazolidinedione derivatives

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