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W2048802677 endingPage "1321" @default.
W2048802677 startingPage "1308" @default.
W2048802677 abstract "Antagonism of group I metabotropic glutamate receptors (mGluR1 and mGluR5) reduces behavioral effects of drugs of abuse, including cocaine. However, the underlying mechanisms remain poorly understood. Activation of mGluR5 increases protein synthesis at synapses. Although mGluR5-induced excessive protein synthesis has been implicated in the pathology of fragile X syndrome, it remains unknown whether group I mGluR-mediated protein synthesis is involved in any behavioral effects of drugs of abuse. We report that group I mGluR agonist DHPG induced more pronounced initial depression of inhibitory postsynaptic currents (IPSCs) followed by modest long-term depression (I-LTD) in dopamine neurons of rat ventral tegmental area (VTA) through the activation of mGluR1. The early component of DHPG-induced depression of IPSCs was mediated by the cannabinoid CB1 receptors, while DHPG-induced I-LTD was dependent on protein synthesis. Western blotting analysis indicates that mGluR1 was coupled to extracellular signal-regulated kinase (ERK) and mammalian target of rapamycin (mTOR) signaling pathways to increase translation. We also show that cocaine conditioning activated translation machinery in the VTA via an mGluR1-dependent mechanism. Furthermore, intra-VTA microinjections of mGluR1 antagonist JNJ16259685 and protein synthesis inhibitor cycloheximide significantly attenuated or blocked the acquisition of cocaine-induced conditioned place preference (CPP) and activation of translation elongation factors. Taken together, these results suggest that mGluR1 antagonism inhibits de novo protein synthesis; this effect may block the formation of cocaine–cue associations and thus provide a mechanism for the reduction in CPP to cocaine." @default.
W2048802677 created "2016-06-24" @default.
W2048802677 creator A5013660755 @default.
W2048802677 creator A5014461610 @default.
W2048802677 creator A5038690033 @default.
W2048802677 creator A5049815313 @default.
W2048802677 creator A5056391726 @default.
W2048802677 creator A5065351411 @default.
W2048802677 date "2013-01-24" @default.
W2048802677 modified "2023-10-12" @default.
W2048802677 title "Metabotropic Glutamate Receptor I (mGluR1) Antagonism Impairs Cocaine-Induced Conditioned Place Preference via Inhibition of Protein Synthesis" @default.
W2048802677 cites W1487132131 @default.
W2048802677 cites W1567696719 @default.
W2048802677 cites W1608785134 @default.
W2048802677 cites W1845377771 @default.
W2048802677 cites W1963919233 @default.
W2048802677 cites W1964310366 @default.
W2048802677 cites W1966901093 @default.
W2048802677 cites W1968950270 @default.
W2048802677 cites W1969661654 @default.
W2048802677 cites W1969724443 @default.
W2048802677 cites W1981832344 @default.
W2048802677 cites W1986435336 @default.
W2048802677 cites W1987105275 @default.
W2048802677 cites W1987827006 @default.
W2048802677 cites W1991973951 @default.
W2048802677 cites W1993051284 @default.
W2048802677 cites W1993109240 @default.
W2048802677 cites W1993386709 @default.
W2048802677 cites W1994926162 @default.
W2048802677 cites W1999537989 @default.
W2048802677 cites W2003472138 @default.
W2048802677 cites W2009162050 @default.
W2048802677 cites W2010333198 @default.
W2048802677 cites W2010533815 @default.
W2048802677 cites W2011223687 @default.
W2048802677 cites W2012303490 @default.
W2048802677 cites W2017197221 @default.
W2048802677 cites W2019372876 @default.
W2048802677 cites W2024613165 @default.
W2048802677 cites W2025348599 @default.
W2048802677 cites W2030657755 @default.
W2048802677 cites W2033726788 @default.
W2048802677 cites W2037060024 @default.
W2048802677 cites W2037513419 @default.
W2048802677 cites W2038098576 @default.
W2048802677 cites W2039869230 @default.
W2048802677 cites W2040301525 @default.
W2048802677 cites W2044161108 @default.
W2048802677 cites W2045401053 @default.
W2048802677 cites W2046316453 @default.
W2048802677 cites W2049511526 @default.
W2048802677 cites W2053929792 @default.
W2048802677 cites W2054528757 @default.
W2048802677 cites W2054559819 @default.
W2048802677 cites W2058019798 @default.
W2048802677 cites W2058535388 @default.
W2048802677 cites W2059956308 @default.
W2048802677 cites W2060053691 @default.
W2048802677 cites W2069705491 @default.
W2048802677 cites W2070942862 @default.
W2048802677 cites W2073561166 @default.
W2048802677 cites W2073917895 @default.
W2048802677 cites W2077529232 @default.
W2048802677 cites W2077594514 @default.
W2048802677 cites W2080120821 @default.
W2048802677 cites W2080252952 @default.
W2048802677 cites W2080451230 @default.
W2048802677 cites W2081234982 @default.
W2048802677 cites W2081620736 @default.
W2048802677 cites W2085215186 @default.
W2048802677 cites W2086236919 @default.
W2048802677 cites W2087343899 @default.
W2048802677 cites W2092491372 @default.
W2048802677 cites W2106042714 @default.
W2048802677 cites W2106214171 @default.
W2048802677 cites W2117922300 @default.
W2048802677 cites W2122230301 @default.
W2048802677 cites W2122531239 @default.
W2048802677 cites W2122592499 @default.
W2048802677 cites W2124178069 @default.
W2048802677 cites W2127186613 @default.
W2048802677 cites W2129927715 @default.
W2048802677 cites W2130634332 @default.
W2048802677 cites W2131832591 @default.
W2048802677 cites W2134736026 @default.
W2048802677 cites W2134906491 @default.
W2048802677 cites W2136381335 @default.
W2048802677 cites W2137769667 @default.
W2048802677 cites W2139810677 @default.
W2048802677 cites W2140192917 @default.
W2048802677 cites W2143034003 @default.
W2048802677 cites W2143960888 @default.
W2048802677 cites W2144761196 @default.
W2048802677 cites W2151571360 @default.
W2048802677 cites W2157405529 @default.
W2048802677 cites W2162507760 @default.
W2048802677 cites W2172184241 @default.