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[Structure and function of neural plasticity-related gene products].

作者信息

Yamagata K, Sugiura H, Suzuki K

机构信息

Department of Molecular Neurobiology, Tokyo Metropolitan Institute for Neuroscience, Fuchu, Japan.

出版信息

Nihon Shinkei Seishin Yakurigaku Zasshi. 1998 Aug;18(4):133-6.

PMID:9866829
Abstract

We have isolated novel immediate early genes (IEGs) from the hippocampus by differential cloning techniques. These mRNAs are induced by synaptic activity and translated into proteins that may affect neural function. We have analyzed a variety of "effector" immediate early genes. These mRNAs encode: 1) cytoplasmic proteins, such as cyclooxygenase-2, a small G protein, Rheb, and a cytoskeleton-associated protein, Arc; 2) membrane-bound proteins, such as the cell adhesion protein Arcadlin, and a neurite-outgrowth protein, Neuritin; and 3) a secreted protein, Narp. We hypothesize that physiological stimulation induces "effector" proteins that might strengthen synaptic connections of activated synapses. In contrast, pathological conditions such as epilepsy or drug addiction may accelerate overproduction of these gene products, which cause abnormal synapse formation. Gene targeting and in vivo gene transfer techniques are required to prove this hypothesis.

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