Preclinical validation of AR42, a novel histone deacetylase inhibitor, as treatment for vestibular schwannomas

Authors

Abraham Jacob, The Ohio State University
Janet Oblinger, The University of Arizona
Matthew L. Bush, The University of Arizona
Victoria Brendel, The University of Arizona
Griffin Santarelli, The University of ToledoFollow
Abhik R. Chaudhury, The Ohio State University
Samuel Kulp, The Ohio State University
Krista M.D. La Perle, The Ohio State University
Ching Shih Chen, The Ohio State University
Long Sheng Chang, The University of Arizona
D. Bradley Welling, The University of Arizona

Document Type

Article

Abstract

Objectives/Hypothesis: Recent studies indicate that vestibular schwannomas (VSs) rely on phosphatidylinositol 3-kinase/AKT activation to promote cell proliferation and survival; therefore, targeting AKT may provide new therapeutic options. We have previously shown that AR42, a novel histone deacetylase inhibitor, potently suppresses VS growth in vitro at doses correlating with AKT inactivation. The objectives of the current study were translational: 1) to examine the end biologic effects of AR42 on tumor growth in vivo, 2) to validate AKT as its in vivo molecular target, 3) to determine whether AR42 penetrates the blood-brain barrier (BBB), and 4) to study the pharmacotoxicity profile of AR42. Study Design: In vivo mouse studies. Methods: AR42 was dosed orally in murine schwannoma allografts and human VS xenografts. Magnetic resonance imaging was used to quantify changes in tumor volume, and intracellular molecular targets were analyzed using immunohistochemistry. BBB penetration was assayed, and both blood-chemistry measurements and histology studies were used to evaluate toxicity. Results: Growth of schwannoma implants was dramatically decreased by AR42 at doses correlating with AKT dephosphorylation, cell cycle arrest, and apoptosis. AR42 penetrated the BBB, and wild-type mice fed AR42 for 6 months behaved normally and gained weight appropriately. Blood-chemistry studies and organ histology performed after 3 and 6 months of AR42 treatment demonstrated no clinically significant abnormalities. Conclusions: AR42 suppresses schwannoma growth at doses correlating with AKT pathway inhibition. This orally bioavailable drug penetrates the BBB, is well tolerated, and represents a novel candidate for translation to human VS clinical trials. © 2011 The American Laryngological, Rhinological, and Otological Society, Inc.

Publication Date

1-1-2012

Publication Title

Laryngoscope

ISSN

0023852X

E-ISSN

15314995

Volume

122

Issue

1

First Page

174

Last Page

189

PubMed ID

22109824

Digital Object Identifier (DOI)

10.1002/lary.22392

Recommended Citation

Jacob, Abraham; Oblinger, Janet; Bush, Matthew L.; Brendel, Victoria; Santarelli, Griffin; Chaudhury, Abhik R.; Kulp, Samuel; La Perle, Krista M.D.; Chen, Ching Shih; Chang, Long Sheng; and Welling, D. Bradley, "Preclinical validation of AR42, a novel histone deacetylase inhibitor, as treatment for vestibular schwannomas" (2012). Neurology. 600.
https://scholar.barrowneuro.org/neurology/600