Date : 06.19.2009

Generation of a severe memory-deficit mutant mouse by exclusively eliminating the kinase activity of CaMKIIα

Category : Press Release
 National Institute for Physiological Sciences, Japan
 

Ca2+⁄calmodulin-dependent protein kinase IIα (CaMKIIα) is an enzyme that adds phosphates to a variety of protein substrates to modify their functions. CaMKIIα is enriched in the hippocampus, the memory center of the brain, and is believed to be an essential mediator of activity-dependent synaptic plasticity and memory functions. However, the causative role of the enzymatic activity of CaMKIIα in such processes has not been demonstrated yet, because this enzyme has multiple protein functions other than the kinase activity. A Japanese research group, led by Dr Yoko Yamagata of the National Institute for Physiological Sciences, Japan, has successfully generated a novel kinase-dead mutant mouse of the CaMKIIα gene that completely and exclusively lacks its kinase activity. They examined hippocampal synaptic plasticity and behavioral learning of the mouse, and found a severe deficit in both processes. They reported their findings in the Journal of Neuroscience, published on June 10, 2009.

The research group successfully generated a novel CaMKIIα (K42R) knock-in mouse that completely lacks the kinase activity of CaMKIIα, and examined the effects on structural, functional, and behavioral expression of synaptic memory. In the K42R brain, tetanus-induced long-term potentiation (LTP), a proposed cellular mechanism of memory, and sustained postsynaptic spine enlargement, a structural basis for LTP, were both impaired, whereas dynamic postsynaptic movement of CaMKIIα protein was preserved. In addition, the K42R mouse showed a severe deficit in inhibitory avoidance learning, a form of memory dependent on the hippocampus. The research group concluded that the mutant mouse could not form memories and did not remember the events that had just happened.

"We demonstrated that the mutant mouse has a severe memory deficit because of the lack of the kinase activity of CaMKIIα. This finding supports the idea that the kinase activity of CaMKIIα is essential to memory functions. Such a memory-deficit mutant mouse could serve as an animal model to study the molecular mechanisms of memory, and be a useful tool for the development and screening of therapeutic reagents for memory-deficit disorders. It may also help open a new therapeutic approach to memory dysfunctions in patients.", said Dr Yamagata.

This research was carried out in collaboration with Profs. Shigeo Okabe, Toshiya Manabe, Yuchio Yanagawa, Keiji Imoto, Kunihiko Obata and others. Dr Yoko Yamagata and Prof Yuchio Yanagawa have applied for a patent on this technology through Japan Science and Technology Agency (JST).

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Kinase-Dead Knock-In Mouse Reveals an Essential Role of Kinase Activity of Ca2+⁄Calmodulin-Dependent Protein Kinase IIα in Dendritic Spine Enlargement, Long-Term Potentiation, and Learning
Yoko Yamagata, Shizuka Kobayashi, Tatsuya Umeda, Akihiro Inoue, Hiroyuki Sakagami, Masahiro Fukaya, Masahiko Watanabe, Nobuhiko Hatanaka, Masako Totsuka, Takeshi Yagi, Kunihiko Obata, Keiji Imoto, Yuchio Yanagawa, Toshiya Manabe, and Shigeo Okabe
Journal of Neuroscience, 29: 7607-7618, 2009