New Multi-Targeted Antiproliferative Agents: Design and Synthesis of IC261-Based Oxindoles as Potential Tubulin, CK1 and EGFR Inhibitors

Fareed, Momen R.; Shoman, Mai E.; Hamed, Mohammed I. A.; Badr, Mohamed; Bogari, Hanin A.; Elhady, Sameh S.; Ibrahim, Tarek S.; Abuo‐Rahma, Gamal El‐Din A.; Ali, Taha F. S.

doi:10.3390/ph14111114

Cited by 13 publications

(11 citation statements)

References 82 publications

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“…Vanillin or alkylated vanillin derivatives reacted with different oxindole derivatives, yielding compounds 5a–c and 6a–o , respectively. The resulted compounds were a mixture of E and Z isomers and used without separation as the previous literature reported that the E isomer is mainly the major isomer − with the possibility of interconversion between the two isomers in methanol within 2 days. , Compounds’ identities were confirmed by comparing mp and NMR data to those we had previously reported …”

Section: Resultsmentioning

confidence: 85%

Vanillin-Based Indolin-2-one Derivative Bearing a Pyridyl Moiety as a Promising Anti-Breast Cancer Agent via Anti-Estrogenic Activity

et al. 2023

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The structure-based design introduced indoles as an essential motif in designing new selective estrogen receptor modulators employed for treating breast cancer. Therefore, here, a series of synthesized vanillin-substituted indolin-2-ones were screened against the NCI-60 cancer cell panel followed by in vivo, in vitro, and in silico studies. Physicochemical parameters were evaluated with HPLC and SwissADME tools. The compounds demonstrated promising anti-cancer activity for the MCF-7 breast cancer cell line (GI = 6–63%). The compound with the highest activity (6j) was selective for the MCF-7 breast cancer cell line (IC50 = 17.01 μM) with no effect on the MCF-12A normal breast cell line supported by real-time cell analysis. A morphological examination of the used cell lines confirmed a cytostatic effect of compound 6j. It inhibited both in vivo and in vitro estrogenic activity, triggering a 38% reduction in uterine weight induced by estrogen in an immature rat model and hindering 62% of ER-α receptors in in vitro settings. In silico molecular docking and molecular dynamics simulation studies supported the stability of the ER-α and compound 6j protein–ligand complex. Herein, we report that indolin-2-one derivative 6j is a promising lead compound for further pharmaceutical formulations as a potential anti-breast cancer drug.

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Section: Resultsmentioning

confidence: 85%

Vanillin-Based Indolin-2-one Derivative Bearing a Pyridyl Moiety as a Promising Anti-Breast Cancer Agent via Anti-Estrogenic Activity

et al. 2023

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“…The biological findings suggest compounds 61 and 62 are suitable leads for development of novel therapeutics for colon cancer, along with improved physicochemical and pharmacokinetic features. [68] 2.20 Mechanistic investigations showed that 63 substantially reduced tubulin polymerization, dose-dependently triggered cell death, and arrested cell division in the G2/M phase. Since 63 was a microtubule polymerization inhibitor, the outcomes of molecular docking and bioactive activities were comparable with those of colchicine.…”

Section: -Benzylideneindolin-2-one Derivativesmentioning

confidence: 99%

Section: Indole Derivatives As Potent Inhibitors Of Cbsmentioning

confidence: 99%

Indole derivatives targeting colchicine binding site as potential anticancer agents

Goel

Jaiswal

Jain

2023

Archiv der Pharmazie

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Microtubules are appealing as intracellular targets for anticancer activity due to their importance in cell division. Three important binding sites are present on the tubulin protein: taxane, vinca, and colchicine binding sites (CBS). Many USFDA‐approved drugs such as paclitaxel, ixabepilone, vinblastine, and combretastatin act by altering the dynamics of the microtubules. Additionally, a large number of compounds have been synthesized by medicinal chemists around the globe that target different tubulin binding sites. Although CBS inhibitors have proved their cytotoxic potential, no CBS‐targeting drug had been able to reach the market. Several studies have reported design, synthesis, and biological evaluation of indole derivatives as potential anticancer agents. These compounds have been shown to inhibit cancer cell proliferation, induce apoptosis, and disrupt microtubule formation. Moreover, the binding affinity of these compounds to the CBS has been demonstrated using molecular docking studies and competitive binding assays. The present work has reviewed indole derivatives as potential colchicine‐binding site inhibitors. The structure–activity relationship studies have revealed the crucial pharmacophoric features required for the potent and selective binding of indole derivatives to the CBS. The development of these compounds with improved efficacy and reduced toxicity could potentially lead to the development of novel and effective cancer therapies.

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“…Compounds were mixtures of E and Z isomers (see Supporting Information: S1). No separation was made since previous literature reported that the E isomer is mainly the major isomer [24][25][26] and acknowledged the interconversion between the two isomers in methanol within 2 days. [21,27] 2.2 | Pharmacology/biology 2.2.1 | One-dose screening against FLT3 ITDmutated MV4-11 and FLT3 WT THP-1 acute myeloid leukemia cells…”

Section: Chemistrymentioning

confidence: 99%

Discovery of oxindole‐based FLT3 inhibitors as a promising therapeutic lead for acute myeloid leukemia carrying the oncogenic ITD mutation

Bender

Shoman

Ali

et al. 2022

Archiv der Pharmazie

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FMS-like tyrosine kinase 3 (FLT3) mutations occur in approximately 30% of acute myeloid leukemia (AML) patients. In the current study, the oxindole chemotype is employed as a structural motif for the design of new FLT3 inhibitors as potential hits for AML irradiation.Cell-based screening was performed with 18 oxindole derivatives and 5a-c inhibited 68%-73% and 83%-91% of internal tandem duplication (ITD)-mutated MV4-11 cell growth for 48-and 72-h treatments while only 0%-2% and 27%-39% in wild-type THP-1 cells. The most potent compound 5a inhibited MV4-11 cells with IC 50 of 4.3 μM at 72 h while it was 8.7 μM in THP-1 cells, thus showing two-fold selective inhibition against the oncogenic ITD mutation. The ability of 5a to modulate cell death was examined. High-throughput protein profiling revealed low levels of the growth factors IGFBP-2 and -4 with the blockage of various apoptotic inhibitors such as Survivin. p21 with cellular stress mechanisms was characterized by increased expression of HSP proteins along with TNF-β. Mechanistically, compounds 5a and 5b inhibited FLT3 kinase with IC 50 values of 2.49 and 1.45 μM, respectively. Theoretical docking studies supported

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New Multi-Targeted Antiproliferative Agents: Design and Synthesis of IC261-Based Oxindoles as Potential Tubulin, CK1 and EGFR Inhibitors

Cited by 13 publications

References 82 publications

Vanillin-Based Indolin-2-one Derivative Bearing a Pyridyl Moiety as a Promising Anti-Breast Cancer Agent via Anti-Estrogenic Activity

Vanillin-Based Indolin-2-one Derivative Bearing a Pyridyl Moiety as a Promising Anti-Breast Cancer Agent via Anti-Estrogenic Activity

Indole derivatives targeting colchicine binding site as potential anticancer agents

Discovery of oxindole‐based FLT3 inhibitors as a promising therapeutic lead for acute myeloid leukemia carrying the oncogenic ITD mutation

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