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• W2883676941 abstract "OPRM1 A118G, a functional human mu-opioid receptor (MOR) polymorphism, is associated with drug dependence and altered stress responsivity in humans as well as altered MOR signaling. MOR signaling can regulate many cellular processes, including gene expression, and many of the long-term, stable effects of drugs and stress may stem from changes in gene expression in diverse brain regions. A mouse model bearing an equivalent polymorphism (Oprm1 A112G) was previously generated and studied. Mice homozygous for the G112 allele show differences in opioid- and stress-related phenotypes.The current study examines the expression of 24 genes related to drug and stress responsivity in the caudoputamen, nucleus accumbens, hypothalamus, hippocampus, and amygdala of drug-naïve, stress-minimized, male and female mice homozygous for either the G112 variant allele or the wild-type A112 allele.We detected nominal genotype-dependent changes in gene expression of multiple genes. We also detected nominal sex-dependent as well as sex-by-genotype interaction effects on gene expression. Of these, four genotype-dependent differences survived correction for multiple testing: Avp and Gal in the hypothalamus and Oprl1 and Cnr1 in the hippocampus.Changes in the regulation of these genes by mu-opioid receptors encoded by the G112 allele may be involved in some of the behavioral and molecular consequences of this polymorphism observed in mice." @default.
• W2883676941 created "2018-08-03" @default.
• W2883676941 creator A5039487284 @default.
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• W2883676941 creator A5091075235 @default.
• W2883676941 date "2018-07-19" @default.
• W2883676941 modified "2023-09-26" @default.
• W2883676941 title "Oprm1 A112G, a single nucleotide polymorphism, alters expression of stress-responsive genes in multiple brain regions in male and female mice" @default.
• W2883676941 cites W1489720543 @default.
• W2883676941 cites W1507267321 @default.
• W2883676941 cites W1703928389 @default.
• W2883676941 cites W1931216733 @default.
• W2883676941 cites W1951822496 @default.
• W2883676941 cites W1962839343 @default.
• W2883676941 cites W1968677614 @default.
• W2883676941 cites W1969886388 @default.
• W2883676941 cites W1971084467 @default.
• W2883676941 cites W1976960945 @default.
• W2883676941 cites W1978715208 @default.
• W2883676941 cites W1981891173 @default.
• W2883676941 cites W1989254187 @default.
• W2883676941 cites W1992364990 @default.
• W2883676941 cites W1994549739 @default.
• W2883676941 cites W2002074672 @default.
• W2883676941 cites W2002642921 @default.
• W2883676941 cites W2003547326 @default.
• W2883676941 cites W2004136481 @default.
• W2883676941 cites W2008257668 @default.
• W2883676941 cites W2008264529 @default.
• W2883676941 cites W2010051841 @default.
• W2883676941 cites W2010129023 @default.
• W2883676941 cites W2010945696 @default.
• W2883676941 cites W2011863697 @default.
• W2883676941 cites W2012743573 @default.
• W2883676941 cites W2013796305 @default.
• W2883676941 cites W2014887176 @default.
• W2883676941 cites W2014898651 @default.
• W2883676941 cites W2016264450 @default.
• W2883676941 cites W2017514322 @default.
• W2883676941 cites W2022724702 @default.
• W2883676941 cites W2030865965 @default.
• W2883676941 cites W2037628352 @default.
• W2883676941 cites W2039322090 @default.
• W2883676941 cites W2039877085 @default.
• W2883676941 cites W2040925146 @default.
• W2883676941 cites W2043364141 @default.
• W2883676941 cites W2044153999 @default.
• W2883676941 cites W2046181038 @default.
• W2883676941 cites W2054447293 @default.
• W2883676941 cites W2058213757 @default.
• W2883676941 cites W2060163580 @default.
• W2883676941 cites W2060644077 @default.
• W2883676941 cites W2060903877 @default.
• W2883676941 cites W2062079462 @default.
• W2883676941 cites W2064447463 @default.
• W2883676941 cites W2064453868 @default.
• W2883676941 cites W2066848874 @default.
• W2883676941 cites W2067645781 @default.
• W2883676941 cites W2076942602 @default.
• W2883676941 cites W2077312848 @default.
• W2883676941 cites W2077879821 @default.
• W2883676941 cites W2079317155 @default.
• W2883676941 cites W2080253238 @default.
• W2883676941 cites W2083332683 @default.
• W2883676941 cites W2085879736 @default.
• W2883676941 cites W2089869714 @default.
• W2883676941 cites W2097200639 @default.
• W2883676941 cites W2102675531 @default.
• W2883676941 cites W2104786490 @default.
• W2883676941 cites W2108747869 @default.
• W2883676941 cites W2111916508 @default.
• W2883676941 cites W2116354423 @default.
• W2883676941 cites W2122926414 @default.
• W2883676941 cites W2129143684 @default.
• W2883676941 cites W2135432300 @default.
• W2883676941 cites W2135665752 @default.
• W2883676941 cites W2140584456 @default.
• W2883676941 cites W2142371956 @default.
• W2883676941 cites W2152268051 @default.
• W2883676941 cites W2164012002 @default.
• W2883676941 cites W2164732590 @default.
• W2883676941 cites W2172323892 @default.
• W2883676941 cites W2227607890 @default.
• W2883676941 cites W2464717012 @default.
• W2883676941 cites W2586082674 @default.
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• W2883676941 doi "https://doi.org/10.1007/s00213-018-4965-x" @default.
• W2883676941 hasPubMedCentralId "https://www.ncbi.nlm.nih.gov/pmc/articles/6132675" @default.
• W2883676941 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/30027498" @default.
• W2883676941 hasPublicationYear "2018" @default.
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