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  2. Hedgehog Antagonist Pyrimidine-Indole Hybrid Molecule Inhibits Ciliogenesis through Microtubule Destabilisation

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

  • Chembiochem. 2018 Apr 4;19(7):723-735. doi: 10.1002/cbic.201700631.
Harleen Khatra 1 Pragya Paramita Khan 1 Sankha Pattanayak 1 Jhuma Bhadra 1 Bilal Rather 2 Saikat Chakrabarti 2 Taniya Saha 3 Surajit Sinha 1
Affiliations

Affiliations

  • 1 Department of Organic Chemistry, Indian Association for the Cultivation of Science, Jadavpur, Kolkata, 700032, India.
  • 2 Structural Biology and Bio-Informatics Division, CSIR-Indian Institute of Chemical Biology, Jadavpur, Kolkata, 700 032, India.
  • 3 Division of Molecular Medicine, Bose Institute, Kolkata, 700 009, India.
Abstract

One of the crucial regulators of embryonic patterning and tissue development is the Hedgehog-glioma (Hh-Gli) signalling pathway; its uncontrolled activation has been implicated in different types of Cancer in adult tissues. Primary cilium is one of the important factors required for the activation of Hh signalling, as it brings the critical components together for key protein-protein interactions required for Hh pathway regulation. Most of the synthetic and natural small molecule modulators of the pathway primarily antagonise Smoothened (Smo) or Other effectors like Hh ligand or Gli. Here, we report a previously described Hh antagonist, with a pyrimidine-indole hybrid (PIH) core structure, as an inhibitor of ciliogenesis. The compound is unique in its mode of action, as it shows perturbation of microtubule dynamics in both cell-based assays and in vivo systems (zebrafish embryos). Further studies revealed that the probable targets are α-tubulin and its acetylated form, found in the cytoplasm and primary cilia. PIH also showed axonal defasiculation in developing zebrafish embryos. We thus propose that PIH antagonises Hh signalling by repressing cilia biogenesis and disassembling α-tubulin from its stabilised form.

Keywords

Hedgehog inhibitors; ciliogenesis; microtubule destabilizers; small molecules; zebrafish.

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