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W2056576239 startingPage "12048" @default.
W2056576239 abstract "Amyloid precursor protein (APP) is commonly associated with Alzheimer disease, but its physiological function remains unknown. Nav1.6 is a key determinant of neuronal excitability in vivo. Because mouse models of gain of function and loss of function of APP and Nav1.6 share some similar phenotypes, we hypothesized that APP might be a candidate molecule for sodium channel modulation. Here we report that APP colocalized and interacted with Nav1.6 in mouse cortical neurons. Knocking down APP decreased Nav1.6 sodium channel currents and cell surface expression. APP-induced increases in Nav1.6 cell surface expression were Go protein-dependent, enhanced by a constitutively active Go protein mutant, and blocked by a dominant negative Go protein mutant. APP also regulated JNK activity in a Go protein-dependent manner. JNK inhibition attenuated increases in cell surface expression of Nav1.6 sodium channels induced by overexpression of APP. JNK, in turn, phosphorylated APP. Nav1.6 sodium channel surface expression was increased by T668E and decreased by T668A, mutations of APP695 mimicking and preventing Thr-668 phosphorylation, respectively. Phosphorylation of APP695 at Thr-668 enhanced its interaction with Nav1.6. Therefore, we show that APP enhances Nav1.6 sodium channel cell surface expression through a Go-coupled JNK pathway.Background: Loss-of-function amyloid precursor protein (APP) and Nav1.6 transgenic mice share similar phenotypes.Results: APP interacts with Nav1.6 and enhances its cell surface expression through a Go-coupled JNK pathway.Conclusion: APP regulates Nav1.6 function, likely through a Go-coupled JNK pathway.Significance: This finding advances the current understanding of APP functions and has implications for novel therapies for neurodegenerative disorders. Amyloid precursor protein (APP) is commonly associated with Alzheimer disease, but its physiological function remains unknown. Nav1.6 is a key determinant of neuronal excitability in vivo. Because mouse models of gain of function and loss of function of APP and Nav1.6 share some similar phenotypes, we hypothesized that APP might be a candidate molecule for sodium channel modulation. Here we report that APP colocalized and interacted with Nav1.6 in mouse cortical neurons. Knocking down APP decreased Nav1.6 sodium channel currents and cell surface expression. APP-induced increases in Nav1.6 cell surface expression were Go protein-dependent, enhanced by a constitutively active Go protein mutant, and blocked by a dominant negative Go protein mutant. APP also regulated JNK activity in a Go protein-dependent manner. JNK inhibition attenuated increases in cell surface expression of Nav1.6 sodium channels induced by overexpression of APP. JNK, in turn, phosphorylated APP. Nav1.6 sodium channel surface expression was increased by T668E and decreased by T668A, mutations of APP695 mimicking and preventing Thr-668 phosphorylation, respectively. Phosphorylation of APP695 at Thr-668 enhanced its interaction with Nav1.6. Therefore, we show that APP enhances Nav1.6 sodium channel cell surface expression through a Go-coupled JNK pathway. Background: Loss-of-function amyloid precursor protein (APP) and Nav1.6 transgenic mice share similar phenotypes. Results: APP interacts with Nav1.6 and enhances its cell surface expression through a Go-coupled JNK pathway. Conclusion: APP regulates Nav1.6 function, likely through a Go-coupled JNK pathway. Significance: This finding advances the current understanding of APP functions and has implications for novel therapies for neurodegenerative disorders." @default.
W2056576239 created "2016-06-24" @default.
W2056576239 creator A5006062838 @default.
W2056576239 creator A5009880272 @default.
W2056576239 creator A5028296024 @default.
W2056576239 creator A5090357799 @default.
W2056576239 date "2015-05-01" @default.
W2056576239 modified "2023-10-16" @default.
W2056576239 title "Amyloid Precursor Protein Enhances Nav1.6 Sodium Channel Cell Surface Expression" @default.
W2056576239 cites W1497914507 @default.
W2056576239 cites W1520091697 @default.
W2056576239 cites W1527604508 @default.
W2056576239 cites W1537888364 @default.
W2056576239 cites W1550589316 @default.
W2056576239 cites W1584834830 @default.
W2056576239 cites W1606121092 @default.
W2056576239 cites W1967391569 @default.
W2056576239 cites W1974841170 @default.
W2056576239 cites W1979612107 @default.
W2056576239 cites W1981008691 @default.
W2056576239 cites W1985245021 @default.
W2056576239 cites W1991625887 @default.
W2056576239 cites W1991691364 @default.
W2056576239 cites W1992496728 @default.
W2056576239 cites W1997032548 @default.
W2056576239 cites W1997220636 @default.
W2056576239 cites W1998634339 @default.
W2056576239 cites W1999466646 @default.
W2056576239 cites W2003391115 @default.
W2056576239 cites W2009266927 @default.
W2056576239 cites W2010718593 @default.
W2056576239 cites W2012862746 @default.
W2056576239 cites W2018499368 @default.
W2056576239 cites W2020978754 @default.
W2056576239 cites W2027533965 @default.
W2056576239 cites W2030249003 @default.
W2056576239 cites W2032301313 @default.
W2056576239 cites W2034201162 @default.
W2056576239 cites W2036395998 @default.
W2056576239 cites W2036435819 @default.
W2056576239 cites W2041622179 @default.
W2056576239 cites W2047559774 @default.
W2056576239 cites W2048685634 @default.
W2056576239 cites W2055366845 @default.
W2056576239 cites W2059437215 @default.
W2056576239 cites W2060995405 @default.
W2056576239 cites W2064241002 @default.
W2056576239 cites W2065857917 @default.
W2056576239 cites W2066116456 @default.
W2056576239 cites W2069584842 @default.
W2056576239 cites W2073509272 @default.
W2056576239 cites W2073894712 @default.
W2056576239 cites W2076485183 @default.
W2056576239 cites W2079173805 @default.
W2056576239 cites W2084020188 @default.
W2056576239 cites W2090477486 @default.
W2056576239 cites W2101190305 @default.
W2056576239 cites W2104835101 @default.
W2056576239 cites W2133147654 @default.
W2056576239 cites W2145996232 @default.
W2056576239 cites W2147408978 @default.
W2056576239 cites W2148635311 @default.
W2056576239 cites W2149117501 @default.
W2056576239 cites W2155783312 @default.
W2056576239 cites W2159332152 @default.
W2056576239 cites W2161335932 @default.
W2056576239 cites W2161665590 @default.
W2056576239 cites W2163179531 @default.
W2056576239 cites W2163301650 @default.
W2056576239 cites W2169920915 @default.
W2056576239 doi "https://doi.org/10.1074/jbc.m114.617092" @default.
W2056576239 hasPubMedCentralId "https://www.ncbi.nlm.nih.gov/pmc/articles/4424341" @default.
W2056576239 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/25767117" @default.
W2056576239 hasPublicationYear "2015" @default.
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