Deschloroclozapine, a potent and selective chemogenetic actuator enables rapid neuronal and behavioral modulations in mice and monkeys

Author:

Nagai YujiORCID,Miyakawa NaohisaORCID,Takuwa Hiroyuki,Hori Yukiko,Oyama Kei,Ji Bin,Takahashi Manami,Huang Xi-PingORCID,Slocum Samuel T.,DiBerto Jeffrey F.,Xiong Yan,Urushihata Takuya,Hirabayashi Toshiyuki,Fujimoto AtsushiORCID,Mimura Koki,English Justin G.ORCID,Liu Jing,Inoue Ken-ichi,Kumata Katsushi,Seki Chie,Ono Maiko,Shimojo Masafumi,Zhang Ming-Rong,Tomita Yutaka,Nakahara Jin,Suhara TetsuyaORCID,Takada Masahiko,Higuchi Makoto,Jin Jian,Roth Bryan L.,Minamimoto TakafumiORCID

Abstract

AbstractThe chemogenetic technology Designer Receptors Exclusively Activated by Designer Drugs (DREADDs) affords remotely reversible control of cellular signaling, neuronal activity and behavior. Although the combination of muscarinic-based DREADDs with clozapine-N-oxide (CNO) has been widely used, sluggish kinetics, metabolic liabilities, and potential off-target effects of CNO represent areas for improvement. Here we provide a new high affinity and selective agonist deschloroclozapine (DCZ) for muscarinic-based DREADDs. Positron emission tomography revealed that DCZ selectively bound to and occupied DREADDs in both mice and monkeys. Systemic delivery of low doses of DCZ (1 or 3 μg/kg) enhanced neuronal activity via hM3Dq within minutes in mice and monkeys. Intramuscular injections of DCZ (100 μg/kg) reversibly induced spatial working memory deficits in monkeys expressing hM4Di in the prefrontal cortex. DCZ represents the most potent, selective, metabolically stable and fast-acting DREADD agonist reported with utility in both mice and non-human primates for a variety of applications.

Publisher

Cold Spring Harbor Laboratory

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