TY - JOUR
T1 - An open-label study evaluating the safety, behavioral, and electrophysiological outcomes of low-dose ketamine in children with ADNP syndrome
AU - Kolevzon, Alexander
AU - Levy, Tess
AU - Barkley, Sarah
AU - Bedrosian-Sermone, Sandra
AU - Davis, Matthew
AU - Foss-Feig, Jennifer
AU - Halpern, Danielle
AU - Keller, Katherine
AU - Kostic, Ana
AU - Layton, Christina
AU - Lee, Rebecca
AU - Lerman, Bonnie
AU - Might, Matthew
AU - Sandin, Sven
AU - Siper, Paige M.
AU - Sloofman, Laura G.
AU - Walker, Hannah
AU - Zweifach, Jessica
AU - Buxbaum, Joseph D.
N1 - Funding Information:
We are extremely grateful to the families who participated and to the ADNP Kids Research Foundation and the Foundation for Mood Disorders for their support. Support for mediKanren was provided by the National Center for Advancing Translational Sciences, National Institutes of Health, through the Biomedical Data Translator Program, awards OT2TR003435 and OT2TR002517. Any opinions expressed in this document are those of the Translator community at large and do not necessarily reflect the views of NCATS, individual Translator team members, or affiliated organizations and institutions. ClinicalTrials.gov Identifier: NCT04388774, Low-Dose Ketamine in Children with ADNP Syndrome, https://clinicaltrials.gov/ct2/show/NCT04388774. Alexander Kolevzon is on the scientific advisory boards of Ovid Therapeutics, Ritrova Therapeutics, and Jaguar Therapeutics and consults to Acadia, Alkermes, GW Pharmaceuticals, Neuren Pharmaceuticals, Clinilabs Drug Development Corporation, and Scioto Biosciences. Paige M. Siper and Mount Sinai licensed the Sensory Assessment for Neurodevelopmental Disorders (SAND) developed by PMS to Stoelting, Co. Sandra Sermone is on the board of directors of ADNP Kids Research Foundation, has patent applications filed for ketamine and ketamine/NAP for the treatment of ADNP syndrome and related neurological conditions, and is a parent of a child with ADNP syndrome. Matthew Davis is on the scientific advisory board of ADNP Kids Research Foundation, has patent applications filed for ketamine and ketamine/NAP for the treatment of ADNP syndrome and related neurological conditions, and is a parent of a child with ADNP syndrome. Joseph D. Buxbaum consults for BridgeBio Pharma. The remainder of the authors declare no competing interests.
Funding Information:
We are extremely grateful to the families who participated and to the ADNP Kids Research Foundation and the Foundation for Mood Disorders for their support. Support for mediKanren was provided by the National Center for Advancing Translational Sciences , National Institutes of Health , through the Biomedical Data Translator Program, awards OT2TR003435 and OT2TR002517 . Any opinions expressed in this document are those of the Translator community at large and do not necessarily reflect the views of NCATS, individual Translator team members, or affiliated organizations and institutions.
Publisher Copyright:
© 2022 The Author(s)
PY - 2022/10/13
Y1 - 2022/10/13
N2 - Activity-dependent neuroprotective protein (ADNP) syndrome is a rare genetic condition associated with intellectual disability and autism spectrum disorder. Preclinical evidence suggests that low-dose ketamine may induce expression of ADNP and that neuroprotective effects of ketamine may be mediated by ADNP. The goal of the proposed research was to evaluate the safety, tolerability, and behavioral outcomes of low-dose ketamine in children with ADNP syndrome. We also sought to explore the feasibility of using electrophysiological markers of auditory steady-state response and computerized eye tracking to assess biomarker sensitivity to treatment. This study utilized a single-dose (0.5 mg/kg), open-label design, with ketamine infused intravenously over 40 min. Ten children with ADNP syndrome ages 6 to 12 years were enrolled. Ketamine was generally well tolerated, and there were no serious adverse events. The most common adverse events were elation/silliness (50%), fatigue (40%), and increased aggression (40%). Using parent-report instruments to assess treatment effects, ketamine was associated with nominally significant improvement in a wide array of domains, including social behavior, attention deficit and hyperactivity, restricted and repetitive behaviors, and sensory sensitivities, a week after administration. Results derived from clinician-rated assessments aligned with findings from the parent reports. Overall, nominal improvement was evident based on the Clinical Global Impressions - Improvement scale, in addition to clinician-based scales reflecting key domains of social communication, attention deficit and hyperactivity, restricted and repetitive behaviors, speech, thinking, and learning, activities of daily living, and sensory sensitivities. Results also highlight the potential utility of electrophysiological measurement of auditory steady-state response and eye-tracking to index change with ketamine treatment. Findings are intended to be hypothesis generating and provide preliminary support for the safety and efficacy of ketamine in ADNP syndrome in addition to identifying useful endpoints for a ketamine clinical development program. However, results must be interpreted with caution given limitations of this study, most importantly the small sample size and absence of a placebo-control group.
AB - Activity-dependent neuroprotective protein (ADNP) syndrome is a rare genetic condition associated with intellectual disability and autism spectrum disorder. Preclinical evidence suggests that low-dose ketamine may induce expression of ADNP and that neuroprotective effects of ketamine may be mediated by ADNP. The goal of the proposed research was to evaluate the safety, tolerability, and behavioral outcomes of low-dose ketamine in children with ADNP syndrome. We also sought to explore the feasibility of using electrophysiological markers of auditory steady-state response and computerized eye tracking to assess biomarker sensitivity to treatment. This study utilized a single-dose (0.5 mg/kg), open-label design, with ketamine infused intravenously over 40 min. Ten children with ADNP syndrome ages 6 to 12 years were enrolled. Ketamine was generally well tolerated, and there were no serious adverse events. The most common adverse events were elation/silliness (50%), fatigue (40%), and increased aggression (40%). Using parent-report instruments to assess treatment effects, ketamine was associated with nominally significant improvement in a wide array of domains, including social behavior, attention deficit and hyperactivity, restricted and repetitive behaviors, and sensory sensitivities, a week after administration. Results derived from clinician-rated assessments aligned with findings from the parent reports. Overall, nominal improvement was evident based on the Clinical Global Impressions - Improvement scale, in addition to clinician-based scales reflecting key domains of social communication, attention deficit and hyperactivity, restricted and repetitive behaviors, speech, thinking, and learning, activities of daily living, and sensory sensitivities. Results also highlight the potential utility of electrophysiological measurement of auditory steady-state response and eye-tracking to index change with ketamine treatment. Findings are intended to be hypothesis generating and provide preliminary support for the safety and efficacy of ketamine in ADNP syndrome in addition to identifying useful endpoints for a ketamine clinical development program. However, results must be interpreted with caution given limitations of this study, most importantly the small sample size and absence of a placebo-control group.
KW - ADNP
KW - ASD
KW - Helsmoortel-Van der Aa syndrome
KW - autism spectrum disorder
KW - ketamine
UR - http://www.scopus.com/inward/record.url?scp=85137328920&partnerID=8YFLogxK
U2 - 10.1016/j.xhgg.2022.100138
DO - 10.1016/j.xhgg.2022.100138
M3 - Article
AN - SCOPUS:85137328920
SN - 2666-2477
VL - 3
JO - Human Genetics and Genomics Advances
JF - Human Genetics and Genomics Advances
IS - 4
M1 - 100138
ER -