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Work in the Ruiz i
Work in the Ruiz i Altaba lab was funded by grants from the Swiss National Science Foundation, the Ligue Suisse Contre le Cancer, the European FP7 Marie-Curie Initial Training Network HEALING, a James McDonnell Foundation 21st Century Science Initiative in Brain Cancer-Research Award and funds from the Départment d’Instruction Publique of the Republic and Canton of Geneva.
Introduction
The core components of Hedgehog (Hh) signaling pathway are composed of three Hh ligands- Sonic Hh (Shh), India Hh (Ihh) and Desert Hh (Dhh), a 12-pass transmembrane receptor Patched1 (Ptch), a G-protein-coupled receptor-like 7-pass transmembrane protein Smoothened (Smo) and three zinc-finger transcription factors (Gli1, Gli2, and Gli3). In the absence of an Hh ligand, Ptch represses signal transduction by inhibiting Smo from entering the cilium. Upon ligand binding, Smo enters the cilium and transduces the Hh signal, activating the cytoplasmic Gli transcription factors and promoting their translocation to the nucleus. Gli activation induces the transcription of downstream target genes, such as Gli1, Ptch1 and Hh-interacting protein (Hhip). On the other hand, Suppressor of fused (Sufu) inhibits Gli activator activity in the absence of pyk2 inhibitor by interacting with Gli proteins [1,2]. This pathway participates in numerous biological processes throughout embryonic development and exerts important regulatory functions in the adults. However, the uncontrolled excessive activation of Hh pathway is linked to a number of human malignant tumors, especially medulloblastoma (MB), basal cell carcinoma (BCC), and rhabdomyosarcoma (RMS) [3]. Aberrant activation of the Hh pathway can result from abnormal up-regulation of the Hh ligands, loss of Ptch, Smo mutations, and gene amplification/chromosomal translocation of Gli1 or Gli2 [4,5]. Based on these findings, Hh pathway has attracted a great deal of interest as a therapeutic target for malignancy. To date, two Hh pathway inhibitors, GDC-0449 (vismodegib) and LDE-225 (sonidegib), have been approved by the United States Food and Drug Administration (FDA) for the treatment of metastatic or locally advanced BCC in 2012 and 2015, respectively [6]. And more than ten Hh pathway inhibitors have entered clinical trials for the treatment of a wide range of cancers (refer to http://www.clinicaltrials.gov/). There are also a number of small molecules inhibiting Hh signaling been discovered [7].
However, most of Hh pathway inhibitors mentioned above are Smo antagonists, which are only effective on ligand-dependent cancers [[8], [9], [10]]. Furthermore, severe side effects and acquired drug resistances to Smo antagonists have been observed in cell culture, animal experiments and clinical trials [[11], [12], [13], [14]]. Smo mutations, loss of function of Sufu or Gli2 amplification, upregulation of noncanonical and synergistic Gli signaling were identified as the causes of these drug resistances [[15], [16], [17], [18], [19]]. Therefore, there continues to be a high demand for new effective Hh pathway inhibitors that target other components such as Gli.
Natural products (NP), including semi-synthetic NPs and NP derived small-molecular compounds, with great characteristics of high chemical diversity and biochemical specificity, provide a large reservoir of pharmaceutical material for the development of new drugs, including anticancer agents [20]. Cyclopamine, the first Hh pathway inhibitor, was identified from the plant Veratrum californicum in 1970s [21,22]. From the same genus plant V. grandiflorum, we have also discovered three new steroidal alkaloids as potent Hh inhibitors [23]. In recent years, several other chemotypes of NPs, such as isoflavone, chalcone, phenylpropanoid, diterpenoid and triterpene have been demonstrated to inhibit the activation of Hh pathway by direct or indirect mechanisms [[24], [25], [26]]. Therefore, the mining of novel Hh pathway inhibitors from the pool of naturally occurring small-molecules is still of great interest.