2016
An essential role for UBE2A/HR6A in learning and memory and mGLUR-dependent long-term depression
Publication
Publication
Human Molecular Genetics , Volume 25 - Issue 1 p. 1- 8
UBE2A deficiency syndrome (also known as X-linked intellectual disability type Nascimento) is an intellectual disability syndrome characterized by prominent dysmorphic features, impaired speech and often epilepsy. The syndrome is caused by Xq24 deletions encompassing the UBE2A (HR6A) gene or by intragenic UBE2A mutations. UBE2A encodes an E2 ubiquitinconjugating enzyme involved in DNA repair and female fertility. A recent study in Drosophila showed that dUBE2A binds to the E3 ligase Parkin, which is required for mitochondrial function and responsible for juvenile Parkinson's disease. In addition, these studies showed impairments in synaptic transmission in dUBE2A mutant flies. However, a causal role of UBE2A in of cognitive deficits has not yet been established. Here, we show that Ube2a knockout mice have a major deficit in spatial learning tasks, whereas other tested phenotypes, including epilepsy and motor coordination, were normal. Results from electrophysiological measurements in the hippocampus showed no deficits in synaptic transmission nor in the ability to induce long-term synaptic potentiation. However, a small but significant deficit was observed in mGLUR-dependent long-term depression, a pathway previously implied in several other mouse models for neurodevelopmental disorders. Our results indicate a causal role of UBE2A in learning and mGLUR-dependent long-term depression, and further indicate that the Ube2a knockout mouse is a good model to study the molecular mechanisms underlying UBE2A deficiency syndrome.
Additional Metadata | |
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doi.org/10.1093/hmg/ddv436, hdl.handle.net/1765/89831 | |
Human Molecular Genetics | |
Organisation | Department of Neuroscience |
Bruinsma, C., Savelberg, S. M. C., Kool, M., Jolfaei, M. A., van Woerden, G., Baarends, W., & Elgersma, Y. (2016). An essential role for UBE2A/HR6A in learning and memory and mGLUR-dependent long-term depression. Human Molecular Genetics, 25(1), 1–8. doi:10.1093/hmg/ddv436 |