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W3017286941 endingPage "100069" @default.
W3017286941 startingPage "100069" @default.
W3017286941 abstract "Female and male mice of the BTBR T+Itpr3tf/J (BTBR) strain have behaviors that resemble autism spectrum disorder. In comparison to C57BL/6 (B6) mice, BTBR mice have elevated humoral immunity, in that they have naturally high serum IgG levels and generate high levels of IgG antibodies, including autoantibodies to brain antigens. This study focused on the specificities of autoantibodies and the immune cells and their transcription factors that might be responsible for the autoantibodies. BTBR IgG autoantibodies bind to neurons better than microglia and with highest titer to nuclear antigens. Two of the antigens identified were alpha-enolase (ENO1) and dihydrolipoyllysine-residue succinyltransferase component of 2-oxoglutarate dehydrogenase complex, mitochondrial (DLST). Surprisingly based on IgG levels, the blood and spleens of BTBR mice have more CD4+ and CD8+ T cells, but fewer B cells than B6 mice. The high levels of autoantibodies in BTBR relates to their splenic T follicular helper (Tfh) cell levels, which likely are responsible for the higher number of plasma cells in BTBR mice than B6 mice. BTBR mice have increased gene expression of interleukin-21 receptor (Il-21r) and Paired Box 5 (Pax5), which are known to aid B cell differentiation to plasma cells, and an increased Lysine Demethylase 6B (Kdm6b)/DNA Methyltransferase 1 (Dnmt1) ratio, which increases gene expression. Identification of gene expression and immune activities of BTBR mice may aid understanding of mechanisms associated with autism since neuroimmune network interactions have been posited and induction of autoantibodies may drive the neuroinflammation associated with autism." @default.
W3017286941 created "2020-04-24" @default.
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W3017286941 date "2020-04-01" @default.
W3017286941 modified "2023-10-16" @default.
W3017286941 title "Immunity and autoantibodies of a mouse strain with autistic-like behavior" @default.
W3017286941 cites W1498689470 @default.
W3017286941 cites W1515976390 @default.
W3017286941 cites W1535504388 @default.
W3017286941 cites W1759851510 @default.
W3017286941 cites W1942336078 @default.
W3017286941 cites W1964358779 @default.
W3017286941 cites W1966773673 @default.
W3017286941 cites W1968659204 @default.
W3017286941 cites W1975859542 @default.
W3017286941 cites W1979856142 @default.
W3017286941 cites W1985533946 @default.
W3017286941 cites W1992748173 @default.
W3017286941 cites W1995335058 @default.
W3017286941 cites W1996087940 @default.
W3017286941 cites W1996518201 @default.
W3017286941 cites W2003863298 @default.
W3017286941 cites W2004265420 @default.
W3017286941 cites W2005377557 @default.
W3017286941 cites W2006918320 @default.
W3017286941 cites W2011730338 @default.
W3017286941 cites W2017983301 @default.
W3017286941 cites W2021202989 @default.
W3017286941 cites W2021227276 @default.
W3017286941 cites W2032917789 @default.
W3017286941 cites W2035570187 @default.
W3017286941 cites W2037250871 @default.
W3017286941 cites W2039231543 @default.
W3017286941 cites W2040039050 @default.
W3017286941 cites W2043927799 @default.
W3017286941 cites W2046517086 @default.
W3017286941 cites W2052424568 @default.
W3017286941 cites W2070438913 @default.
W3017286941 cites W2071797996 @default.
W3017286941 cites W2071959000 @default.
W3017286941 cites W2082109123 @default.
W3017286941 cites W2082450387 @default.
W3017286941 cites W2088275003 @default.
W3017286941 cites W2089955605 @default.
W3017286941 cites W2105371617 @default.
W3017286941 cites W2117086716 @default.
W3017286941 cites W2124064142 @default.
W3017286941 cites W2127634492 @default.
W3017286941 cites W2128144325 @default.
W3017286941 cites W2129026301 @default.
W3017286941 cites W2133202761 @default.
W3017286941 cites W2133937538 @default.
W3017286941 cites W2141668423 @default.
W3017286941 cites W2163643314 @default.
W3017286941 cites W2167538265 @default.
W3017286941 cites W2207583083 @default.
W3017286941 cites W2466729104 @default.
W3017286941 cites W2514407728 @default.
W3017286941 cites W2526262022 @default.
W3017286941 cites W2531275645 @default.
W3017286941 cites W2560140650 @default.
W3017286941 cites W2590554940 @default.
W3017286941 cites W2604448707 @default.
W3017286941 cites W2614349964 @default.
W3017286941 cites W2616162660 @default.
W3017286941 cites W2789943585 @default.
W3017286941 cites W2792610442 @default.
W3017286941 cites W2801318701 @default.
W3017286941 cites W2801425434 @default.
W3017286941 cites W2801551952 @default.
W3017286941 cites W2803895816 @default.
W3017286941 cites W2804693820 @default.
W3017286941 cites W2861106439 @default.
W3017286941 cites W2891625674 @default.
W3017286941 cites W2895714451 @default.
W3017286941 cites W2906413783 @default.
W3017286941 cites W2946450286 @default.
W3017286941 cites W2969932277 @default.
W3017286941 cites W2991468577 @default.
W3017286941 cites W2994115498 @default.
W3017286941 cites W2998750038 @default.
W3017286941 doi "https://doi.org/10.1016/j.bbih.2020.100069" @default.
W3017286941 hasPubMedCentralId "https://www.ncbi.nlm.nih.gov/pmc/articles/8474232" @default.
W3017286941 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/34589851" @default.
W3017286941 hasPublicationYear "2020" @default.
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