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Optimizing clozapine for chemogenetic neuromodulation of somatosensory cortex

Jongwook Cho, Seungjun Ryu, Sunwoo Lee, Junsoo Kim, Hyoung-Ihl Kim

2020Scientific Reports25 citationsDOIOpen Access PDF

Abstract

Abstract Clozapine (CLZ) has been proposed as an agonist for Designer Receptors Exclusively Activated by Designer Drugs (DREADDs), to replace Clozapine-N-oxide (CNO); however, there are no reliable guidelines for the use of CLZ for chemogenetic neuromodulation. We titrated the optimal dose of CLZ required to evoke changes in neural activity whilst avoiding off-target effects. We also performed [ 18 F]Fluoro-deoxy-glucose micro positron emission tomography (FDG-microPET) scans to determine the global effect of CLZ-induced hM3D(Gq) DREADD activation in the rat brain. Our results show that low doses of CLZ (0.1 and 0.01 mg/kg) successfully induced neural responses without off-target effects. CLZ at 1 mg/kg evoked a stronger and longer-lasting neural response but produced off-target effects, observed as changes in locomotor behavior and FDG-microPET imaging. Unexpectedly, FDG-microPET imaging failed to demonstrate an increase in regional glucose metabolism in the stimulated cortex during CLZ chemogenetic neuromodulation. Therefore, caution should be used when interpreting FDG-PET images in the context of cortical chemogenetic activation.

Topics & Concepts

NeuromodulationClozapineSomatosensory systemContext (archaeology)Positron emission tomographyMedicineNeuroscienceAgonistPharmacologyPsychologyInternal medicineReceptorSchizophrenia (object-oriented programming)BiologyPaleontologyPsychiatryTranscranial Magnetic Stimulation StudiesNeurological disorders and treatmentsNeuroscience and Neural Engineering
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