Hedgehog Antagonist Pyrimidine–Indole Hybrid Molecule Inhibits Ciliogenesis through Microtubule Destabilisation

Khatra, Harleen; Khan, Pragya Paramita; Pattanayak, Sankha; Bhadra, Jhuma; Rather, Bilal A.; Chakrabarti, Saikat; Saha, Taniya; Sinha, Surajit

doi:10.1002/cbic.201700631

Cited by 8 publications

(9 citation statements)

References 52 publications

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“…Our earlier report [19] suggested that substitution can be incorporated very easily at 1 or 2-position of indole in PIH (P) without changing much in the biological activity. Accordingly, for the synthesis of water soluble derivatives of PIH (P) we then decided to incorporate water soluble moiety in the indole part at this position keeping the hydrazine part of the molecule intact.…”

Section: Chemistrymentioning

confidence: 97%

“…For the synthesis of N-alkylated indole derivative the reaction was started from 2methylindole-3-carboxaldehyde (3 B). [19] The indole was alkylated with triethylene glycol 2-bromoethyl methyl ether to get N-alkylated indole derivative (4 C). These three indole derivatives were reacted with hydrazine derivative to get the final compounds 6 A, 6 B and 6 C. In accordance with our earlier report, [19] all the compounds were characterized by spectroscopic methods and found to be single-isomers with the appearance of a single set of peaks in 1 HNMR.…”

Section: Chemistrymentioning

confidence: 99%

“…[19] The indole was alkylated with triethylene glycol 2-bromoethyl methyl ether to get N-alkylated indole derivative (4 C). These three indole derivatives were reacted with hydrazine derivative to get the final compounds 6 A, 6 B and 6 C. In accordance with our earlier report, [19] all the compounds were characterized by spectroscopic methods and found to be single-isomers with the appearance of a single set of peaks in 1 HNMR. Comparing with the previously reported hydrazone derivatives of E-conformers for antiproliferative activity, [21] we believed the most stable Eisomer was formed in our case.…”

Section: Chemistrymentioning

confidence: 99%

“…[15][16][17][18] In our laboratory, the mechanism of action of a small molecule based on pyrimidine indole hybrid (PIH (P)) structure was delineated and found to inhibit ciliogenesis by inhibiting the polymerization of tubulin subunits. [19] This result encouraged us to study the anticancer activity of PIH (P). For any drug to achieve the required pharmacological response, one of the important parameters to be taken into consideration is its solubility in water.…”

Section: Introductionmentioning

confidence: 99%

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Evaluation of a Tubulin‐Targeted Pyrimidine Indole Hybrid Molecule as an Anticancer Agent

et al. 2020

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Several small molecules targeting microtubule dynamics have been developed because microtubules are considered to be one of the most successful cancer chemotherapeutic targets. In this regard, taxol is most worthy to mention which stabilizes microtubule polymer thereby causing defectsinmitotic spindle assembly, chromosome segregation and cell division resulting in cancer inhibition. In this direction, we have earlier reported a small molecule called Pyrimidine-Indole-Hybrid (PIH (P)) which was found to inhibit ciliogenesis by inhibiting both the acetylation and polymerization of tubulin subunits. Here, we have evaluated the anticancer activities of PIH (P) and its water soluble derivatives. Three water soluble derivatives of PIH (P) namely 6 A, 6B and 6 C were synthesized. Among PIH (P) series of compounds, PIH (P) and 6 C were found to be the most potent compounds showing anti-proliferative and cytoskeletal disrupting activities against MCF-7 cells. Not only that, PIH (P) and 6 C also showed a promising effect in preventing cancer cell migration, invasion and colony-formation and helped to reduce spheroid formation by several-folds. They have potential to inhibit the activity of proteins (N-Cadherin, Vimentin) responsible for Epithelial to Mesenchymal Transition (EMT). Hence, this class of compound could be a new antimitotic agent that is different from taxol with respect to mechanism, particularly by destabilizing tubulin rather than causing stabilization.

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Section: Chemistrymentioning

confidence: 97%

Section: Chemistrymentioning

confidence: 99%

Section: Chemistrymentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Evaluation of a Tubulin‐Targeted Pyrimidine Indole Hybrid Molecule as an Anticancer Agent

et al. 2020

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“…Inspired from the interesting Hh signaling antagonist potency of pyrimidine-indole hybrid (PIH) structure, 54 Khatra et al 55 have designed a small compound library of PIH series 3k (Figure 3B) and identified their distinct modes of action as Hh inhibitors. All the new compounds were screened in Shh-Light 2 cells at 1.0 mM concentration.…”

Section: Recent Advances In Design Of Hh Pathway Inhibitorsmentioning

confidence: 99%

Design of Hedgehog pathway inhibitors for cancer treatment

Bariwal

Kumar

Dong

et al. 2018

Medicinal Research Reviews

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Hedgehog (Hh) signaling is involved in the initiation and progression of various cancers and is essential for embryonic and postnatal development. This pathway remains in the quiescent state in adult tissues but gets activated upon inflammation and injuries. Inhibition of Hh signaling pathway using natural and synthetic compounds has provided an attractive approach for treating cancer and inflammatory diseases. While the majority of Hh pathway inhibitors target the transmembrane protein Smoothened (SMO), some small molecules that target the signaling cascade downstream of SMO are of particular interest. Substantial efforts are being made to develop new molecules targeting various components of the Hh signaling pathway. Here, we have discussed the discovery of small molecules as Hh inhibitors from the diverse chemical background. Also, some of the recently identified natural products have been included as a separate section. Extensive structure-activity relationship (SAR) of each chemical class is the focus of this review. Also, clinically advanced molecules are discussed from the last 5 to 7 years. Nanomedicine-based delivery approaches for Hh pathway inhibitors are also discussed concisely.

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Cananginone Abrogates EMT in Breast Cancer Cells through Hedgehog Signaling

Sinha

Bose

Das

et al. 2022

Chemistry & Biodiversity

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Cananginones, a family of linear acetogenins found as secondary metabolites in the plant kingdom, show cytotoxicity against several types of cancer cells. We aimed to investigate the efficacy of cananginone and its mechanism as an anti-cancer agent. Our initial screening of Cananginone against HepG2, PC3, A549, and MCF7 cells showed anti-cancer activities and is more potent against MCF7 cells, consistent with the previous report. Next, cell-based assays have revealed that cananginone abrogates cancer stem cell renewal as well as Epithelial-Mesenchymal Transition (EMT) and increased the ROS level beyond the threshold level thus reducing the viability of cancer cells. In the connection of Hh-Gli to EMT, our study indicated that cananginone inhibits Gli1 in a noncanonical pathway. Presumably, this is the first report on the inhibitory activity of cananginone in the Hh pathway and is different from Hh-antagonists cyclopamine and GANT 61 considering the mechanism.

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Hedgehog Antagonist Pyrimidine–Indole Hybrid Molecule Inhibits Ciliogenesis through Microtubule Destabilisation

Cited by 8 publications

References 52 publications

Evaluation of a Tubulin‐Targeted Pyrimidine Indole Hybrid Molecule as an Anticancer Agent

Evaluation of a Tubulin‐Targeted Pyrimidine Indole Hybrid Molecule as an Anticancer Agent

Design of Hedgehog pathway inhibitors for cancer treatment

Cananginone Abrogates EMT in Breast Cancer Cells through Hedgehog Signaling

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