Lrrc7 mutant mice model developmental emotional dysregulation that can be alleviated by mGluR5 allosteric modulation

LRRC7 has been identified as a candidate gene for severe childhood emotional dysregulation. Direct experimental evidence for a role of LRRC7 in the disease is needed, as is a better understanding of its impact on neuronal structure and signaling, and hence potential treatment targets. Here, we gener...

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Veröffentlicht in:	Translational psychiatry 2019-10, Vol.9 (1), p.244-12, Article 244
Hauptverfasser:	Chong, Chi Ho, Li, Qi, Mak, Priscilla Hoi Shan, Ng, Cypress Chun Pong, Leung, Eva Hin Wa, Tan, Vicky Huiqi, Chan, Anthony Kin Wang, McAlonan, Grainne, Chan, Siu Yuen
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Schlagworte:	13/109 631/378 631/378/340 64/110 82/29 82/80 96/1 Animals Anxiety Behavior, Animal - drug effects Behavioral Sciences Benzamides - pharmacology Biological Psychology Disease Models, Animal Female Male Medicine Medicine & Public Health Mice Mutation Neurons - physiology Neurosciences Pharmacotherapy Psychiatry Pyrazoles - pharmacology Receptor, Metabotropic Glutamate 5 - physiology Sialoglycoproteins - genetics Signal Transduction
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description	LRRC7 has been identified as a candidate gene for severe childhood emotional dysregulation. Direct experimental evidence for a role of LRRC7 in the disease is needed, as is a better understanding of its impact on neuronal structure and signaling, and hence potential treatment targets. Here, we generated and analyzed an Lrrc7 mutant mouse line. Consistent with a critical role of LRRC7 in emotional regulation, mutant mice had inappropriate juvenile aggressive behavior and significant anxiety-like behavior and social dysfunction in adulthood. The pivotal role of mGluR5 signaling was demonstrated by rescue of behavioral defects with augmentation of mGluR5 receptor activity by 3-Cyano- N -(1,3-diphenyl-1 H -pyrazol-5-yl)benzamide (CDPPB). Intra-peritoneal injection of CDPPB alleviated abnormal juvenile behavior, as well as anxiety-like behavior and hypersociability at adulthood. Furthermore, mutant primary neurons had impaired neurite outgrowth which was rescued by CDPPB treatment. In conclusion, Lrrc7 mutant mice provide a valuable tool to model childhood emotional dysregulation and persistent mental health comorbidities. Moreover, our data highlight an important role of LRRC7 in mGluR5 signaling, which is a potential new treatment target for anxiety and social dysfunction.
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Direct experimental evidence for a role of LRRC7 in the disease is needed, as is a better understanding of its impact on neuronal structure and signaling, and hence potential treatment targets. Here, we generated and analyzed an Lrrc7 mutant mouse line. Consistent with a critical role of LRRC7 in emotional regulation, mutant mice had inappropriate juvenile aggressive behavior and significant anxiety-like behavior and social dysfunction in adulthood. The pivotal role of mGluR5 signaling was demonstrated by rescue of behavioral defects with augmentation of mGluR5 receptor activity by 3-Cyano- N -(1,3-diphenyl-1 H -pyrazol-5-yl)benzamide (CDPPB). Intra-peritoneal injection of CDPPB alleviated abnormal juvenile behavior, as well as anxiety-like behavior and hypersociability at adulthood. Furthermore, mutant primary neurons had impaired neurite outgrowth which was rescued by CDPPB treatment. In conclusion, Lrrc7 mutant mice provide a valuable tool to model childhood emotional dysregulation and persistent mental health comorbidities. 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Direct experimental evidence for a role of LRRC7 in the disease is needed, as is a better understanding of its impact on neuronal structure and signaling, and hence potential treatment targets. Here, we generated and analyzed an Lrrc7 mutant mouse line. Consistent with a critical role of LRRC7 in emotional regulation, mutant mice had inappropriate juvenile aggressive behavior and significant anxiety-like behavior and social dysfunction in adulthood. The pivotal role of mGluR5 signaling was demonstrated by rescue of behavioral defects with augmentation of mGluR5 receptor activity by 3-Cyano- N -(1,3-diphenyl-1 H -pyrazol-5-yl)benzamide (CDPPB). Intra-peritoneal injection of CDPPB alleviated abnormal juvenile behavior, as well as anxiety-like behavior and hypersociability at adulthood. Furthermore, mutant primary neurons had impaired neurite outgrowth which was rescued by CDPPB treatment. In conclusion, Lrrc7 mutant mice provide a valuable tool to model childhood emotional dysregulation and persistent mental health comorbidities. Moreover, our data highlight an important role of LRRC7 in mGluR5 signaling, which is a potential new treatment target for anxiety and social dysfunction.</abstract><cop>London</cop><pub>Nature Publishing Group UK</pub><pmid>31582721</pmid><doi>10.1038/s41398-019-0580-9</doi><tpages>12</tpages><orcidid>https://orcid.org/0000-0001-7262-1293</orcidid><oa>free_for_read</oa></addata></record>
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subjects	13/109 631/378 631/378/340 64/110 82/29 82/80 96/1 Animals Anxiety Behavior, Animal - drug effects Behavioral Sciences Benzamides - pharmacology Biological Psychology Disease Models, Animal Female Male Medicine Medicine & Public Health Mice Mutation Neurons - physiology Neurosciences Pharmacotherapy Psychiatry Pyrazoles - pharmacology Receptor, Metabotropic Glutamate 5 - physiology Sialoglycoproteins - genetics Signal Transduction
title	Lrrc7 mutant mice model developmental emotional dysregulation that can be alleviated by mGluR5 allosteric modulation
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