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Amyloid-β Processing in Aged S100B Transgenic Mice Is Sex Dependent
Authors:Krista Minia Wartchow  Leticia Rodrigues  Izabela Swierzy  Michael Buchfelder  Diogo Onofre de Souza  Carlos-Alberto Gonalves  Andrea Kleindienst
Affiliation:1.Department of Biochemistry, Federal University of Rio Grande do Sul, Porto Alegre 90035-003, Brazil; (K.M.W.); (L.R.); (D.O.d.S.); (C.-A.G.);2.Department of Neurosurgery, Friedrich-Alexander University, 91054 Erlangen, Germany; (I.S.); (M.B.)
Abstract:(1) Background: Calcium-binding protein S100B is involved in neuroregeneration but has also been associated with neurodegeneration. These contrasting effects may result from concentration or duration of exposure. We investigated the effect of long-term increased S100B levels on amyloid-β processing in one-year-old transgenic (tg) mice with 12 copies of the murine S100B gene with specific consideration of sex and specific brain regions. (2) Methods: S100B and amyloid-β 42 (Aβ42) were quantified in serum, cerebrospinal fluid (CSF), adipose tissue, and different brain regions by ELISA in wild-type (wt) and S100Btg mice (each n = 7 per group). Thioflavin T (ThT) and Aβ immunostaining were performed for visualization of Aβ deposition. (3) Results: S100B in serum, CSF, and brain was significantly increased in S100Btg mice of both sexes. Aβ42 was significantly increased in the hippocampus of male S100Btg mice (p = 0.0075), and the frontal cortex of female S100Btg mice (p = 0.0262). ThT and Aβ immunostaining demonstrated Aβ deposition in different brain regions in S100Btg mice of both sexes and female wt. (4) Conclusion: Our data validate this experimental model for studying the role of S100B in neurodegeneration and indicate that Aβ processing is sex-dependent and brain region-specific, which deserves further investigation of signaling pathways and behavioral responses.
Keywords:Alzheimer’  s disease  amyloid-β  processing  S100B  transgenic mice  neurodegeneration
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