TY - JOUR
T1 - Early phase clinical studies of AR-42, a histone deacetylase inhibitor, for neurofibromatosis type 2-associated vestibular schwannomas and meningiomas
AU - Welling, D. Bradley
AU - Collier, Katharine A.
AU - Burns, Sarah S.
AU - Oblinger, Janet L.
AU - Shu, Edina
AU - Miles-Markley, Beth A.
AU - Hofmeister, Craig C.
AU - Makary, Mina S.
AU - Slone, H. Wayne
AU - Blakeley, Jaishri O.
AU - Mansouri, S. Alireza
AU - Neff, Brian A.
AU - Jackler, Robert K.
AU - Mortazavi, Amir
AU - Chang, Long Sheng
N1 - Funding Information:
The authors thank our patients who participated. We also thank the OSUCCC PhASR core for PK analysis. We express appreciation to Edwin M. Choy, MD, PhD, Dominic J. Reda, PhD, and Christopher Moertel, MD, our Data Safety & Monitoring Board; Christine Finn, PharmD consultant; and Arno Therapeutics. This work was supported by the U.S. Department of Defense (W81XWH‐14‐1‐0167 to D. Bradley Welling, W81XWH‐18‐1‐0547 to Long‐Sheng Chang); National Cancer Institute of the National Institutes of Health (U01CA076576, R01CA201382 to Amir Mortazavi and Craig C. Hofmeister); the Galloway Family; Advocure NF2; The Ohio State University Comprehensive Cancer Center (P30CA16058); and The Ohio State University Center for Clinical and Translational Science to Long‐Sheng Chang. The content is solely the responsibility of the authors and does not represent official views of the sponsors.
Funding Information:
D. Bradley Welling is a consultant for CereXis, Science 24/7, NFBio, NF2 Biosolutions, and Mulberry Bio. Craig C. Hofmeister has received research grants from Takeda and Oncolytics Biotech; research and personal grants from Janssen, BMS, Sanofi, Nektar, Karyopharm, Imbrium, and Oncopeptides, all outside the submitted work. Amir Mortazavi is on the advisory board for Seattle Genetics and Pfizer and is on the scientific advisory board for Debiopharm Group. His institution (but not him) has received research funding from Acerta Pharma, Genentech, Roche, Merck, Novartis, Seattle Genetics, Astellas Pharma, Mirati Therapeutics, and Bristol‐Myers Squibb. The other authors declare no potential conflict of interest. The Ohio State University (OSU) holds the patent on the investigational drug AR‐42 (US 10/597022). The Technology Commercialization Office has licensed AR‐42 (now called REC‐2282) to Recursion Pharmaceuticals using the institution's standard terms, conditions, and approval process, in which no author participated. To assure absence of institutional conflict of interest in assessment of response and attribution of toxicity, both were reviewed by the Cancer Therapy Evaluation Program of the National Cancer Institute prior to reporting results for the phase I study. Safety issues related to dose increases and attribution of response were monitored by The OSU Data Safety Monitoring Committee and The OSU Cancer Center Institutional Review Board for the phase 1 pilot. A separate Data Safety and Monitoring Board of Massachusetts Eye and Ear oversaw pilot study 2.
Funding Information:
The authors thank our patients who participated. We also thank the OSUCCC PhASR core for PK analysis. We express appreciation to Edwin M. Choy, MD, PhD, Dominic J. Reda, PhD, and Christopher Moertel, MD, our Data Safety & Monitoring Board; Christine Finn, PharmD consultant; and Arno Therapeutics. This work was supported by the U.S. Department of Defense (W81XWH-14-1-0167 to D. Bradley Welling, W81XWH-18-1-0547 to Long-Sheng Chang); National Cancer Institute of the National Institutes of Health (U01CA076576, R01CA201382 to Amir Mortazavi and Craig C. Hofmeister); the Galloway Family; Advocure NF2; The Ohio State University Comprehensive Cancer Center (P30CA16058); and The Ohio State University Center for Clinical and Translational Science to Long-Sheng Chang. The content is solely the responsibility of the authors and does not represent official views of the sponsors.
Publisher Copyright:
© 2021 The Authors. Laryngoscope Investigative Otolaryngology published by Wiley Periodicals LLC on behalf of The Triological Society.
PY - 2021/10
Y1 - 2021/10
N2 - Objectives: Two pilot studies of AR-42, a pan-histone deacetylase inhibitor, in human neurofibromatosis type 2 (NF2), vestibular schwannomas (VS), and meningiomas are presented. Primary endpoints included safety, and intra-tumoral pharmacokinetics (PK) and pharmacodynamics (PD). Methods: Pilot 1 is a subset analysis of a phase 1 study of AR-42 in solid tumors, which included NF2 or sporadic meningiomas. Tumor volumes and treatment-related adverse events (TRAEs) are reported (NCT01129193). Pilot 2 is a phase 0 surgical study of AR-42 assessing intra-tumoral PK and PD. AR-42 was administered for 3 weeks pre-operatively. Plasma and tumor drug concentrations and p-AKT expression were measured (NCT02282917). Results: Pilot 1: Five patients with NF2 and two with sporadic meningiomas experienced a similar incidence of TRAEs to the overall phase I trial. The six evaluable patients had 15 tumors (8 VS, 7 meningiomas). On AR-42, tumor volume increased in six, remained stable in eight, and decreased in one tumor. The annual percent growth rate decreased in eight, remained stable in three, and increased in four tumors. Pilot 2: Four patients with sporadic VS and one patient with meningioma experienced no grade 3/4 toxicities. Expression of p-AKT decreased in three of four VS. All tumors had higher AR-42 concentrations than plasma. Conclusions: AR-42 is safe. Tumor volumes showed a mixed response, but most slowed growth. On a 40-mg regimen, drug concentrated in tumors and growth pathways were suppressed in most tumors, suggesting this may be a well-tolerated and effective dose. A phase 2 study of AR-42 for NF2-associated tumors appears warranted. Level of Evidence: 1b, 4.
AB - Objectives: Two pilot studies of AR-42, a pan-histone deacetylase inhibitor, in human neurofibromatosis type 2 (NF2), vestibular schwannomas (VS), and meningiomas are presented. Primary endpoints included safety, and intra-tumoral pharmacokinetics (PK) and pharmacodynamics (PD). Methods: Pilot 1 is a subset analysis of a phase 1 study of AR-42 in solid tumors, which included NF2 or sporadic meningiomas. Tumor volumes and treatment-related adverse events (TRAEs) are reported (NCT01129193). Pilot 2 is a phase 0 surgical study of AR-42 assessing intra-tumoral PK and PD. AR-42 was administered for 3 weeks pre-operatively. Plasma and tumor drug concentrations and p-AKT expression were measured (NCT02282917). Results: Pilot 1: Five patients with NF2 and two with sporadic meningiomas experienced a similar incidence of TRAEs to the overall phase I trial. The six evaluable patients had 15 tumors (8 VS, 7 meningiomas). On AR-42, tumor volume increased in six, remained stable in eight, and decreased in one tumor. The annual percent growth rate decreased in eight, remained stable in three, and increased in four tumors. Pilot 2: Four patients with sporadic VS and one patient with meningioma experienced no grade 3/4 toxicities. Expression of p-AKT decreased in three of four VS. All tumors had higher AR-42 concentrations than plasma. Conclusions: AR-42 is safe. Tumor volumes showed a mixed response, but most slowed growth. On a 40-mg regimen, drug concentrated in tumors and growth pathways were suppressed in most tumors, suggesting this may be a well-tolerated and effective dose. A phase 2 study of AR-42 for NF2-associated tumors appears warranted. Level of Evidence: 1b, 4.
KW - AR-42
KW - histone deacetylase inhibitor
KW - meningioma
KW - neurofibromatosis type 2
KW - vestibular schwannoma
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U2 - 10.1002/lio2.643
DO - 10.1002/lio2.643
M3 - Article
C2 - 34667843
AN - SCOPUS:85113164573
SN - 0023-852X
VL - 6
SP - 1008
EP - 1019
JO - Laryngoscope investigative otolaryngology
JF - Laryngoscope investigative otolaryngology
IS - 5
ER -