| Literature DB >> 25755142 |
Jacob Ellegood1, Nobuhiro Nakai2, Jin Nakatani3, Mark Henkelman1,4, Toru Takumi2,5, Jason Lerch1,4.
Abstract
Paternally and maternally inherited deletions and duplications of human chromosome 15q11-13 are relatively common in the human population. Furthermore, duplications in the 15q region are often associated with autism. Both maternal and paternal interstitial 15q11-13 duplication mouse models have been previously created, where several behavioral differences were found in the paternal duplication (patDp/+) mouse but not in the maternal duplication (matDp/+). These included decreased sociability, behavioral inflexibility, abnormal ultrasonic vocalizations, decreased spontaneous activity, and increased anxiety. Similarly, in the current study, we found several anatomical differences in the patDp/+ mice that were not seen in the matDp/+ mice. Regional differences that are evident only in the paternal duplication are a smaller dentate gyrus and smaller medial striatum. These differences may be responsible for the behavioral inflexibility. Furthermore, a smaller dorsal raphe nucleus could be responsible for the reported serotonin defects. This study highlights consistency that can be found between behavioral and anatomical phenotyping.Entities:
Keywords: 15q11-13 duplication; animal models; copy number variation; molecular genetics; neuroanatomy; structural MRI
Mesh:
Year: 2015 PMID: 25755142 DOI: 10.1002/aur.1469
Source DB: PubMed Journal: Autism Res ISSN: 1939-3806 Impact factor: 5.216