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PMID:16527258
Citation |
Nakanishi, K, Ida, M, Suzuki, H, Kitano, C, Yamamoto, A, Mori, N, Araki, M and Taketani, S (2006) Molecular characterization of a transport vesicle protein Neurensin-2, a homologue of Neurensin-1, expressed in neural cells. Brain Res. 1081:1-8 |
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Abstract |
We have isolated and characterized a novel cDNA encoding a small neuronal membrane protein showing high sequence homology to Neuro-p24/Neurensin-1, a protein containing a microtubule-associated domain at the carboxyl-terminus and exclusively localized to small vesicles of neurons. The newly identified Neurensin-2 constitutes two-membrane spanning domains but not the microtubule-binding domain, with a molecular mass of 28 kDa. Neurensin-2 mRNA is expressed only in brain, whereas the protein expressed in various neurons including those of the thalamus/hypothalamus and hippocampus, of postnatally developing mice. While the levels of Neurensin-1 mRNA and protein in retinoic acid-exposed mouse neuroblastoma Neuro2a cells increased, those of Neurensin-2 mRNA and protein remained unchanged. When the Neurensin-2 cDNA was transfected into Neuro2a cells, Neurensin-2 was expressed in small vesicles including lysosomes in the perinuclear region. On the cotransfection of Neurensin-1 and -2 cDNA into Neuro2a cells, Neurensin-2 was mainly found in small vesicles of the cell body and Neurensin-1 in those of growth cones. In nerve growth factor-stimulated PC12 cells, the intracellular localization of these proteins also differed. Furthermore, immunochemical staining of mouse brain revealed that Neurensin-1 and -2 had a similar distribution in many regions such as the Diagonal band, hippocampus, amygdaloid nucleus, and habenula nucleus, but differed in the intracellular localization as follows: Neurensin-1 was found mainly in neuritic processes, while Neurensin-2 was found in cell bodies. Thus, both Neurensin-1, and -2 are localized in small vesicles in neural cells, but their localizations of the vesicles are not always the same by each other, suggesting that they are under separate regulation. |
Links |
PubMed Online version:10.1016/j.brainres.2006.01.085 |
Keywords |
Animals; Blotting, Northern/methods; Blotting, Western/methods; Brain/cytology; Brain/metabolism; Cell Line; Cercopithecus aethiops; Cloning, Molecular/methods; DNA Fragmentation/physiology; Gene Expression/drug effects; Gene Expression/physiology; Humans; Immunohistochemistry/methods; Mice; Nerve Growth Factor/pharmacology; Nerve Tissue Proteins/genetics; Nerve Tissue Proteins/metabolism; Neurons/drug effects; Neurons/metabolism; Sequence Alignment/methods; Sequence Homology, Amino Acid; Transfection/methods; Vesicular Transport Proteins/genetics; Vesicular Transport Proteins/metabolism |
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