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The mouse as a model for neuropsychiatric drug development.

Authors :
Howe, James R
Howe, James R
Bear, Mark F
Golshani, Peyman
Klann, Eric
Lipton, Stuart A
Mucke, Lennart
Sahin, Mustafa
Silva, Alcino J
Howe, James R
Howe, James R
Bear, Mark F
Golshani, Peyman
Klann, Eric
Lipton, Stuart A
Mucke, Lennart
Sahin, Mustafa
Silva, Alcino J
Source :
Current biology : CB; vol 28, iss 17, R909-R914; 0960-9822
Publication Year :
2018

Abstract

Much has been written about the validity of mice as a preclinical model for brain disorders. Critics cite numerous examples of apparently effective treatments in mouse models that failed in human clinical trials, raising the possibility that the two species' neurobiological differences could explain the high translational failure rate in psychiatry and neurology (neuropsychiatry). However, every stage of translation is plagued by complex problems unrelated to neurobiological conservation. Therefore, although these case studies are intriguing, they cannot alone determine whether these differences observed account for translation failures. Our analysis of the literature indicates that most neuropsychiatric treatments used in humans are at least partially effective in mouse models, suggesting that neurobiological differences are unlikely to be the main cause of neuropsychiatric translation failures.

Details

Database :
OAIster
Journal :
Current biology : CB; vol 28, iss 17, R909-R914; 0960-9822
Notes :
application/pdf, Current biology : CB vol 28, iss 17, R909-R914 0960-9822
Publication Type :
Electronic Resource
Accession number :
edsoai.on1391609131
Document Type :
Electronic Resource