Literature DB >> 26131110

Amyloid-β immunization enhances neurogenesis and cognitive ability in neonatal mice.

Hongguang Chen1, Min Wang2, Aihong Jiao1, Guotai Tang1, Wei Zhu1, Peng Zou1, Tuo Li1, Guangqiang Cui1, Peiyou Gong1.   

Abstract

Whether Aβ actually has a physiological as well as a pathological role is not known. In order to investigate the effect of endogenous Aβ, wild type C57BL/6 mice were immunized with human or mouse derived Aβ1-42. The anti-Aβ antibody concentrations were increased in both treated groups. Compared to the human Aβ1-42 treated group, level of serum Aβ significantly decreased in mouse Aβ1-42 treated group. Western blot results revealed that these two derived Aβ1-42 had no cross-reaction. The new dentate granule survival cells increased in Aβ1-42 immunization groups, indicated by more BrdU+/NeuN+ and BrdU+/DCX+ cells as compared to PBS-treated group, accompanied by behavioral performance improving in a hippocampus-dependent learning task. Immunohistochemical analysis showed that BrdU+/Iba1+ cells also increased, however new born astrocytes (BrdU+/GFAP+) were unaffected in all treated mice. Interestingly, according the results of ELISA analysis both vaccines up-regulated IL-4 and IFN-γ levels in the brains and sera, but the TNF-α level did not changed. Of note, human Aβ1-42 immunization in neonatal mice enhanced neurogenesis and cognitive ability, might via Aβ immune response rather than cleaning endogenous Aβ.

Entities:  

Keywords:  Amyloid-β; cognitive function; immunization; neonatal mice; neurogenesis

Year:  2015        PMID: 26131110      PMCID: PMC4483988     

Source DB:  PubMed          Journal:  Int J Clin Exp Med        ISSN: 1940-5901


  43 in total

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