TY - JOUR
T1 - Comprehensive analysis of the 16p11.2 deletion and null cntnap2 mouse models of autism spectrum disorder
AU - Brunner, Daniela
AU - Kabitzke, Patricia
AU - He, Dansha
AU - Cox, Kimberly
AU - Thiede, Lucinda
AU - Hanania, Taleen
AU - Sabath, Emily
AU - Alexandrov, Vadim
AU - Saxe, Michael
AU - Peles, Elior
AU - Mills, Alea
AU - Spooren, Will
AU - Ghosh, Anirvan
AU - Feliciano, Pamela
AU - Benedetti, Marta
AU - Clayton, Alice Luo
AU - Biemans, Barbara
N1 - Publisher Copyright: © 2015 Brunner et al.
PY - 2015/8/14
Y1 - 2015/8/14
N2 - Autism spectrum disorder comprises several neurodevelopmental conditions presenting symptoms in social communication and restricted, repetitive behaviors. A major roadblock for drug development for autism is the lack of robust behavioral signatures predictive of clinical efficacy. To address this issue, we further characterized, in a uniform and rigorous way, mousemodels of autism that are of interest because of their construct validity and wide availability to the scientific community.We implemented a broad behavioral battery that included but was not restricted to core autism domains, with the goal of identifying robust, reliable phenotypes amenable for further testing. Here we describe comprehensive findings from two known mouse models of autism, obtained at different developmental stages, using a systematic behavioral test battery combining standard tests as well as novel, quantitative, computer-vision based systems. The first mousemodel recapitulates a deletion in human chromosome 16p11.2, found in 1% of individuals with autism. The second mouse model harbors homozygous null mutations in Cntnap2, associated with autism and Pitt-Hopkins-like syndrome. Consistent with previous results, 16p11.2 heterozygous null mice, also known as Del(7Slx1b-Sept1)4Aam weighed less than wild type littermates displayed hyperactivity and no social deficits. Cntnap2 homozygous null mice were also hyperactive, froze less during testing, showed a mild gait phenotype and deficits in the three-chamber social preference test, although less robust than previously published. In the open field test with exposure to urine of an estrous female, however, the Cntnap2 null mice showed reduced vocalizations. In addition, Cntnap2 nullmice performed slightly better in a cognitive procedural learning test. Although finding and replicating robust behavioral phenotypes in animalmodels is a challenging task, such functional readouts remain important in the development of therapeutics and we anticipate both our positive and negative findings will be utilized as a resource for the broader scientific community.
AB - Autism spectrum disorder comprises several neurodevelopmental conditions presenting symptoms in social communication and restricted, repetitive behaviors. A major roadblock for drug development for autism is the lack of robust behavioral signatures predictive of clinical efficacy. To address this issue, we further characterized, in a uniform and rigorous way, mousemodels of autism that are of interest because of their construct validity and wide availability to the scientific community.We implemented a broad behavioral battery that included but was not restricted to core autism domains, with the goal of identifying robust, reliable phenotypes amenable for further testing. Here we describe comprehensive findings from two known mouse models of autism, obtained at different developmental stages, using a systematic behavioral test battery combining standard tests as well as novel, quantitative, computer-vision based systems. The first mousemodel recapitulates a deletion in human chromosome 16p11.2, found in 1% of individuals with autism. The second mouse model harbors homozygous null mutations in Cntnap2, associated with autism and Pitt-Hopkins-like syndrome. Consistent with previous results, 16p11.2 heterozygous null mice, also known as Del(7Slx1b-Sept1)4Aam weighed less than wild type littermates displayed hyperactivity and no social deficits. Cntnap2 homozygous null mice were also hyperactive, froze less during testing, showed a mild gait phenotype and deficits in the three-chamber social preference test, although less robust than previously published. In the open field test with exposure to urine of an estrous female, however, the Cntnap2 null mice showed reduced vocalizations. In addition, Cntnap2 nullmice performed slightly better in a cognitive procedural learning test. Although finding and replicating robust behavioral phenotypes in animalmodels is a challenging task, such functional readouts remain important in the development of therapeutics and we anticipate both our positive and negative findings will be utilized as a resource for the broader scientific community.
UR - http://www.scopus.com/inward/record.url?scp=84942906846&partnerID=8YFLogxK
U2 - 10.1371/journal.pone.0134572
DO - 10.1371/journal.pone.0134572
M3 - مقالة
SN - 1932-6203
VL - 10
JO - PLoS ONE
JF - PLoS ONE
IS - 8
M1 - e0134572
ER -