Nature Search

Carvone derived cannabidiol enantiomers as novel anticonvulsants

Rochelle M. Hines
April Contreras
Dustin J. Hines
ResearchOpen Access24 Sept 2025
Neuropsychopharmacology

P: 1-12
Human ARHGEF9 intellectual disability syndrome is phenocopied by a mutation that disrupts collybistin binding to the GABA_A receptor α2 subunit

Dustin J. Hines
April Contreras
Rochelle M. Hines
ResearchOpen Access12 May 2022
Molecular Psychiatry

Volume: 27, P: 1275
Autism-related traits in myotonic dystrophy type 1 model mice are due to MBNL sequestration and RNA mis-splicing of autism-risk genes

Sznajder et al. identified a molecular link between autism and myotonic dystrophy, showing that a tandem repeat mutation in a single gene can disrupt splicing of multiple autism-related genes during brain development, leading to autism-like traits.

Łukasz J. Sznajder
Mahreen Khan
Ryan K. C. Yuen
ResearchOpen Access21 Apr 2025
Nature Neuroscience

Volume: 28, P: 1199-1212
Developmental seizures and mortality result from reducing GABA_A receptor α2-subunit interaction with collybistin

The inhibitory synaptic protein collybistin (CB) and GABA_AR-α subunits are thought to interact, but strength and specificity are unclear. Here the authors study the CB–α2 interaction and show that a mouse mutated in the CB-binding region of α2 displays a loss of specific synapses and seizure.

Rochelle M. Hines
Hans Michael Maric
Stephen J. Moss
ResearchOpen Access07 Aug 2018
Nature Communications

Volume: 9, P: 1-15
Mutations in NONO lead to syndromic intellectual disability and inhibitory synaptic defects

Via exome sequencing, the authors identified mutations in the NONO protein, a member of the DBHS family, as a likely cause of severe intellectual disability. Using animal and cell models, they found that nearly one-third of NONO-regulated transcripts were synaptosomal and that NONO depletion directly affected inhibitory synaptic structure.

Dennis Mircsof
Maéva Langouët
Laurence Colleaux
Research16 Nov 2015
Nature Neuroscience

Volume: 18, P: 1731-1736
Human ARHGEF9 intellectual disability syndrome is phenocopied by a mutation that disrupts collybistin binding to the GABA_A receptor α2 subunit

Dustin J. Hines
April Contreras
Rochelle M. Hines
ResearchOpen Access15 Feb 2022
Molecular Psychiatry

Volume: 27, P: 1729-1741
Behavioral arrest and a characteristic slow waveform are hallmark responses to selective 5-HT_2A receptor activation

April Contreras
Matthew Khumnark
Dustin J. Hines
ResearchOpen Access21 Jan 2021
Scientific Reports

Volume: 11, P: 1-12
Neural Basis of Benzodiazepine Reward: Requirement for α2 Containing GABA_A Receptors in the Nucleus Accumbens

Elif Engin
Konstantin I Bakhurin
Uwe Rudolph
Research19 Feb 2014
Neuropsychopharmacology

Volume: 39, P: 1805-1815

Search

Carvone derived cannabidiol enantiomers as novel anticonvulsants

Human ARHGEF9 intellectual disability syndrome is phenocopied by a mutation that disrupts collybistin binding to the GABA_A receptor α2 subunit

Autism-related traits in myotonic dystrophy type 1 model mice are due to MBNL sequestration and RNA mis-splicing of autism-risk genes

Developmental seizures and mortality result from reducing GABA_A receptor α2-subunit interaction with collybistin

Mutations in NONO lead to syndromic intellectual disability and inhibitory synaptic defects

Human ARHGEF9 intellectual disability syndrome is phenocopied by a mutation that disrupts collybistin binding to the GABA_A receptor α2 subunit

Behavioral arrest and a characteristic slow waveform are hallmark responses to selective 5-HT_2A receptor activation

Neural Basis of Benzodiazepine Reward: Requirement for α2 Containing GABA_A Receptors in the Nucleus Accumbens

Search

Quick links

Search

Filter By:

Search

Quick links