Histone Deacetylase 6 Represents a Novel Drug Target in the Oncogenic Hedgehog Signaling Pathway

Dhanyamraju, Pavan Kumar; Holz, Philipp Simon; Finkernagel, Florian; Fendrich, Volker; Lauth, Matthias

doi:10.1158/1535-7163.mct-14-0481

Cited by 44 publications

(37 citation statements)

References 80 publications

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“…In a previous report it was observed that, in addition to HDAC1/2, HDAC6 is also upregulated in SHH-MB and its targeting leads to a substantial anti-tumor effect in mouse models of SHH-MB29. Interestingly, HDAC6 seems to exert its function independently of Gli acetylation, by acting at both receptor and downstream level, most likely by affecting Gli2/3 stability.…”

Section: Discussionmentioning

confidence: 94%

“…Indeed, HDAC1/2 deacetylate and enhance Gli1 transcriptional activity, thus suggesting that, by blocking these enzymes, MGCD0103 may inhibit Hh function via Gli1 acetylation. Since in a recent work it was also observed that HDAC6 inhibits Hh signaling by acting both upstream and downstream of Sufu29, we first tested at what level the inhibitory effect of MGCD0103 occurs. To this end, we used the Sufu −/− MEF cells, where the absence of the cytoplasmic inhibitor Sufu causes an increase of Hh target gene expression, independently of the receptor (Ptch1/Smo) activation30.…”

Section: Resultsmentioning

confidence: 99%

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Selective targeting of HDAC1/2 elicits anticancer effects through Gli1 acetylation in preclinical models of SHH Medulloblastoma

Coni

Mancuso

Magno

et al. 2017

Sci Rep

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SHH Medulloblastoma (SHH-MB) is a pediatric brain tumor characterized by an inappropriate activation of the developmental Hedgehog (Hh) signaling. SHH-MB patients treated with the FDA-approved vismodegib, an Hh inhibitor that targets the transmembrane activator Smoothened (Smo), have shown the rapid development of drug resistance and tumor relapse due to novel Smo mutations. Moreover, a subset of patients did not respond to vismodegib because mutations were localized downstream of Smo. Thus, targeting downstream Hh components is now considered a preferable approach. We show here that selective inhibition of the downstream Hh effectors HDAC1 and HDAC2 robustly counteracts SHH-MB growth in mouse models. These two deacetylases are upregulated in tumor and their knockdown inhibits Hh signaling and decreases tumor growth. We demonstrate that mocetinostat (MGCD0103), a selective HDAC1/HDAC2 inhibitor, is a potent Hh inhibitor and that its effect is linked to Gli1 acetylation at K518. Of note, we demonstrate that administration of mocetinostat to mouse models of SHH-MB drastically reduces tumor growth, by reducing proliferation and increasing apoptosis of tumor cells and prolongs mouse survival rate. Collectively, these data demonstrate the preclinical efficacy of targeting the downstream HDAC1/2-Gli1 acetylation in the treatment of SHH-MB.

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Section: Discussionmentioning

confidence: 94%

Section: Resultsmentioning

confidence: 99%

Selective targeting of HDAC1/2 elicits anticancer effects through Gli1 acetylation in preclinical models of SHH Medulloblastoma

Coni

Mancuso

Magno

et al. 2017

Sci Rep

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“…These findings suggest that selective inhibition of HDAC6 can represents a new therapeutic approach in the treatment of Hh-dependent malignancies. Indeed, the specific HDAC6 antagonist, ACY-1215 [70] ( Figures 1 and 2 and Table 1), reduced strikingly in vivo tumor growth. Hence, HDAC6, despite exerting a dichotomous role (it is required to achieve full pathway activity, but it has also been described to repress basal Hh target gene transcription) is a critical player in Hh pathway regulation, promoting the maximum expression of a subset of GLI target genes [70].…”

Section: Hdac Inhibitors (Hdacis)mentioning

confidence: 98%

“…Indeed, the specific HDAC6 antagonist, ACY-1215 [70] ( Figures 1 and 2 and Table 1), reduced strikingly in vivo tumor growth. Hence, HDAC6, despite exerting a dichotomous role (it is required to achieve full pathway activity, but it has also been described to repress basal Hh target gene transcription) is a critical player in Hh pathway regulation, promoting the maximum expression of a subset of GLI target genes [70]. Since the upregulation of HDACs has been documented in various types of tumors, the development of novel potent and selective HDACi is ongoing.…”

Section: Hdac Inhibitors (Hdacis)mentioning

confidence: 98%

Targeting GLI factors to inhibit the Hedgehog pathway

Infante

Alfonsi

Botta

et al. 2015

Trends in Pharmacological Sciences

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Hedgehog (Hh) signaling has emerged in recent years as an attractive target for anticancer therapy because its aberrant activation is implicated in several cancers. Major progress has been made in the development of SMOOTHENED (SMO) antagonists, although they have shown several limitations due to downstream SMO pathway activation or the occurrence of drug-resistant SMO mutations. Recently, particular interest has been elicited by the identification of molecules able to hit glioma-associated oncogene (GLI) factors, the final effectors of the Hh pathway, which provide a valid tool to overcome anti-SMO resistance. Here, we review results achieved in developing GLI antagonists, explaining their mechanisms of action and highlighting their therapeutic potential. We also underline the relevance of structural details in their discovery and optimization.

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“…A similar induction of GLI1 was observed in MEFs treated with the pan-HDACi trichostatin A. 34 The canonical role of GLI1 is as a key transcription factor and effector molecule in the Hedgehog signaling pathway. 25 As SMO inhibition did not sensitize to vorinostat-induced apoptosis, GLI1 appears to function through a noncanonical pathway in this system.…”

Section: Discussionmentioning

confidence: 60%

A genome scale RNAi screen identifies GLI1 as a novel gene regulating vorinostat sensitivity

et al. 2016

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Vorinostat is an FDA-approved histone deacetylase inhibitor (HDACi) that has proven clinical success in some patients; however, it remains unclear why certain patients remain unresponsive to this agent and other HDACis. Constitutive STAT (signal transducer and activator of transcription) activation, overexpression of prosurvival Bcl-2 proteins and loss of HR23B have been identified as potential biomarkers of HDACi resistance; however, none have yet been used to aid the clinical utility of HDACi. Herein, we aimed to further elucidate vorinostat-resistance mechanisms through a functional genomics screen to identify novel genes that when knocked down by RNA interference (RNAi) sensitized cells to vorinostat-induced apoptosis. A synthetic lethal functional screen using a whole-genome protein-coding RNAi library was used to identify genes that when knocked down cooperated with vorinostat to induce tumor cell apoptosis in otherwise resistant cells. Through iterative screening, we identified 10 vorinostatresistance candidate genes that sensitized specifically to vorinostat. One of these vorinostat-resistance genes was GLI1, an oncogene not previously known to regulate the activity of HDACi. Treatment of vorinostat-resistant cells with the GLI1 smallmolecule inhibitor, GANT61, phenocopied the effect of GLI1 knockdown. The mechanism by which GLI1 loss of function sensitized tumor cells to vorinostat-induced apoptosis is at least in part through interactions with vorinostat to alter gene expression in a manner that favored apoptosis. Upon GLI1 knockdown and vorinostat treatment, BCL2L1 expression was repressed and overexpression of BCL2L1 inhibited GLI1-knockdown-mediated vorinostat sensitization. Taken together, we present the identification and characterization of GLI1 as a new HDACi resistance gene, providing a strong rationale for development of GLI1 inhibitors for clinical use in combination with HDACi therapy.

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Histone Deacetylase 6 Represents a Novel Drug Target in the Oncogenic Hedgehog Signaling Pathway

Cited by 44 publications

References 80 publications

Selective targeting of HDAC1/2 elicits anticancer effects through Gli1 acetylation in preclinical models of SHH Medulloblastoma

Selective targeting of HDAC1/2 elicits anticancer effects through Gli1 acetylation in preclinical models of SHH Medulloblastoma

Targeting GLI factors to inhibit the Hedgehog pathway

A genome scale RNAi screen identifies GLI1 as a novel gene regulating vorinostat sensitivity

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