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this intended switch in AMPAR properties, mice lacking all GluR-B, however, show a widespread impairment in behavior, including lethargy, motor coordination problems, and deficits in exploratory activity [51], which preclude detailed behavioral analyses. Similarly, mice expressing (in the entire brain) a substantial part of the GluR-B population in the Q/R site-unedited form become seizure-prone and die prematurely [53]. Some of these problems can be partially overcome by use of spatially and temporally restricted expression systems [54–56], in particular the Cre-lox system, with Cre-recombinase expression in defined brain areas of gene-targeted mice carrying GluR-B alleles marked by loxP sites for Cre-mediated recombination [55,57]. Indeed, restricting the expression of Q/R site-unedited GluR-B to forebrain resulted in almost normal lifespan and an only weakly seizure-prone phenotype [58]. Mice with forebrain-specific GluR-B depletion appeared almost completely normal throughout life with no developmental abnormalities, thus permitting a detailed, quantitative investigation of olfactory behavior."}
2_test
{"project":"2_test","denotations":[{"id":"16216087-8938126-84723726","span":{"begin":216,"end":218},"obj":"8938126"},{"id":"16216087-7502080-84723727","span":{"begin":431,"end":433},"obj":"7502080"},{"id":"16216087-8980238-84723728","span":{"begin":551,"end":553},"obj":"8980238"},{"id":"16216087-8980237-84723728","span":{"begin":551,"end":553},"obj":"8980237"},{"id":"16216087-12040087-84723728","span":{"begin":551,"end":553},"obj":"12040087"},{"id":"16216087-8980237-84723729","span":{"begin":747,"end":749},"obj":"8980237"},{"id":"16216087-2783482-84723730","span":{"begin":750,"end":752},"obj":"2783482"},{"id":"16216087-15548671-84723731","span":{"begin":910,"end":912},"obj":"15548671"},{"id":"T76144","span":{"begin":216,"end":218},"obj":"8938126"},{"id":"T84875","span":{"begin":431,"end":433},"obj":"7502080"},{"id":"T5085","span":{"begin":551,"end":553},"obj":"8980238"},{"id":"T5467","span":{"begin":551,"end":553},"obj":"8980237"},{"id":"T11439","span":{"begin":551,"end":553},"obj":"12040087"},{"id":"T27507","span":{"begin":747,"end":749},"obj":"8980237"},{"id":"T56644","span":{"begin":750,"end":752},"obj":"2783482"},{"id":"T25849","span":{"begin":910,"end":912},"obj":"15548671"}],"text":"Concerning this intended switch in AMPAR properties, mice lacking all GluR-B, however, show a widespread impairment in behavior, including lethargy, motor coordination problems, and deficits in exploratory activity [51], which preclude detailed behavioral analyses. Similarly, mice expressing (in the entire brain) a substantial part of the GluR-B population in the Q/R site-unedited form become seizure-prone and die prematurely [53]. Some of these problems can be partially overcome by use of spatially and temporally restricted expression systems [54–56], in particular the Cre-lox system, with Cre-recombinase expression in defined brain areas of gene-targeted mice carrying GluR-B alleles marked by loxP sites for Cre-mediated recombination [55,57]. Indeed, restricting the expression of Q/R site-unedited GluR-B to forebrain resulted in almost normal lifespan and an only weakly seizure-prone phenotype [58]. Mice with forebrain-specific GluR-B depletion appeared almost completely normal throughout life with no developmental abnormalities, thus permitting a detailed, quantitative investigation of olfactory behavior."}
craft-ca-core-ex-dev
{"project":"craft-ca-core-ex-dev","denotations":[{"id":"T2196","span":{"begin":35,"end":40},"obj":"GO_EXT:0004971"},{"id":"T2197","span":{"begin":53,"end":57},"obj":"NCBITaxon:10088"},{"id":"T2198","span":{"begin":70,"end":74},"obj":"GO_EXT:0008066"},{"id":"T2199","span":{"begin":70,"end":76},"obj":"PR_EXT:000008234"},{"id":"T2200","span":{"begin":119,"end":127},"obj":"GO_PATO_EXT:biological_behavior"},{"id":"T2201","span":{"begin":149,"end":154},"obj":"GO_EXT:biological_movement_or_translocation_process"},{"id":"T2202","span":{"begin":245,"end":255},"obj":"GO_PATO_EXT:biological_behavior"},{"id":"T2203","span":{"begin":277,"end":281},"obj":"NCBITaxon:10088"},{"id":"T2204","span":{"begin":282,"end":292},"obj":"GO:0010467"},{"id":"T2205","span":{"begin":308,"end":313},"obj":"UBERON:0000955"},{"id":"T2206","span":{"begin":341,"end":345},"obj":"GO_EXT:0008066"},{"id":"T2207","span":{"begin":341,"end":347},"obj":"PR_EXT:000008234"},{"id":"T2208","span":{"begin":366,"end":367},"obj":"CHEBI_SO_EXT:glutamine"},{"id":"T2209","span":{"begin":368,"end":369},"obj":"CHEBI_SO_EXT:arginine"},{"id":"T2210","span":{"begin":377,"end":383},"obj":"SO_EXT:sequence_alteration_process"},{"id":"T2211","span":{"begin":414,"end":417},"obj":"GO:0016265"},{"id":"T2212","span":{"begin":531,"end":541},"obj":"GO:0010467"},{"id":"T2213","span":{"begin":581,"end":584},"obj":"SO_EXT:0000346"},{"id":"T2214","span":{"begin":602,"end":613},"obj":"GO_EXT:recombinase"},{"id":"T2215","span":{"begin":614,"end":624},"obj":"GO:0010467"},{"id":"T2216","span":{"begin":636,"end":647},"obj":"UBERON:0002616"},{"id":"T2217","span":{"begin":651,"end":655},"obj":"SO_EXT:0000704"},{"id":"T2218","span":{"begin":665,"end":669},"obj":"NCBITaxon:10088"},{"id":"T2219","span":{"begin":679,"end":683},"obj":"GO_EXT:0008066"},{"id":"T2220","span":{"begin":679,"end":685},"obj":"PR_EXT:000008234"},{"id":"T2221","span":{"begin":686,"end":693},"obj":"SO_EXT:0001023"},{"id":"T2222","span":{"begin":694,"end":700},"obj":"CHEBI_SO_EXT:molecular_label_or_mark_or_tag_process"},{"id":"T2223","span":{"begin":704,"end":714},"obj":"SO_EXT:0000346"},{"id":"T2224","span":{"begin":732,"end":745},"obj":"GO_SO_EXT:sequence_rearrangement_process"},{"id":"T2225","span":{"begin":779,"end":789},"obj":"GO:0010467"},{"id":"T2226","span":{"begin":793,"end":794},"obj":"CHEBI_SO_EXT:glutamine"},{"id":"T2227","span":{"begin":795,"end":796},"obj":"CHEBI_SO_EXT:arginine"},{"id":"T2228","span":{"begin":804,"end":810},"obj":"SO_EXT:sequence_alteration_process"},{"id":"T2229","span":{"begin":811,"end":815},"obj":"GO_EXT:0008066"},{"id":"T2230","span":{"begin":811,"end":817},"obj":"PR_EXT:000008234"},{"id":"T2231","span":{"begin":821,"end":830},"obj":"UBERON:0001890"},{"id":"T2232","span":{"begin":857,"end":865},"obj":"UBERON:0000104"},{"id":"T2233","span":{"begin":915,"end":919},"obj":"NCBITaxon:10088"},{"id":"T2234","span":{"begin":925,"end":934},"obj":"UBERON:0001890"},{"id":"T2235","span":{"begin":944,"end":948},"obj":"GO_EXT:0008066"},{"id":"T2236","span":{"begin":944,"end":950},"obj":"PR_EXT:000008234"},{"id":"T2237","span":{"begin":1006,"end":1010},"obj":"UBERON:0000104"},{"id":"T2238","span":{"begin":1106,"end":1115},"obj":"GO:0007608"},{"id":"T2239","span":{"begin":1116,"end":1124},"obj":"GO_PATO_EXT:biological_behavior"}],"text":"Concerning this intended switch in AMPAR properties, mice lacking all GluR-B, however, show a widespread impairment in behavior, including lethargy, motor coordination problems, and deficits in exploratory activity [51], which preclude detailed behavioral analyses. Similarly, mice expressing (in the entire brain) a substantial part of the GluR-B population in the Q/R site-unedited form become seizure-prone and die prematurely [53]. Some of these problems can be partially overcome by use of spatially and temporally restricted expression systems [54–56], in particular the Cre-lox system, with Cre-recombinase expression in defined brain areas of gene-targeted mice carrying GluR-B alleles marked by loxP sites for Cre-mediated recombination [55,57]. Indeed, restricting the expression of Q/R site-unedited GluR-B to forebrain resulted in almost normal lifespan and an only weakly seizure-prone phenotype [58]. Mice with forebrain-specific GluR-B depletion appeared almost completely normal throughout life with no developmental abnormalities, thus permitting a detailed, quantitative investigation of olfactory behavior."}
craft-ca-core-dev
{"project":"craft-ca-core-dev","denotations":[{"id":"T1992","span":{"begin":53,"end":57},"obj":"NCBITaxon:10088"},{"id":"T1993","span":{"begin":70,"end":76},"obj":"PR:000008234"},{"id":"T1994","span":{"begin":277,"end":281},"obj":"NCBITaxon:10088"},{"id":"T1995","span":{"begin":282,"end":292},"obj":"GO:0010467"},{"id":"T1996","span":{"begin":308,"end":313},"obj":"UBERON:0000955"},{"id":"T1997","span":{"begin":341,"end":347},"obj":"PR:000008234"},{"id":"T1998","span":{"begin":414,"end":417},"obj":"GO:0016265"},{"id":"T1999","span":{"begin":531,"end":541},"obj":"GO:0010467"},{"id":"T2000","span":{"begin":581,"end":584},"obj":"SO:0000346"},{"id":"T2001","span":{"begin":614,"end":624},"obj":"GO:0010467"},{"id":"T2002","span":{"begin":636,"end":647},"obj":"UBERON:0002616"},{"id":"T2003","span":{"begin":651,"end":655},"obj":"SO:0000704"},{"id":"T2004","span":{"begin":665,"end":669},"obj":"NCBITaxon:10088"},{"id":"T2005","span":{"begin":679,"end":685},"obj":"PR:000008234"},{"id":"T2006","span":{"begin":686,"end":693},"obj":"SO:0001023"},{"id":"T2007","span":{"begin":704,"end":714},"obj":"SO:0000346"},{"id":"T2008","span":{"begin":779,"end":789},"obj":"GO:0010467"},{"id":"T2009","span":{"begin":811,"end":817},"obj":"PR:000008234"},{"id":"T2010","span":{"begin":821,"end":830},"obj":"UBERON:0001890"},{"id":"T2011","span":{"begin":857,"end":865},"obj":"UBERON:0000104"},{"id":"T2012","span":{"begin":915,"end":919},"obj":"NCBITaxon:10088"},{"id":"T2013","span":{"begin":925,"end":934},"obj":"UBERON:0001890"},{"id":"T2014","span":{"begin":944,"end":950},"obj":"PR:000008234"},{"id":"T2015","span":{"begin":1006,"end":1010},"obj":"UBERON:0000104"},{"id":"T2016","span":{"begin":1106,"end":1115},"obj":"GO:0007608"}],"text":"Concerning this intended switch in AMPAR properties, mice lacking all GluR-B, however, show a widespread impairment in behavior, including lethargy, motor coordination problems, and deficits in exploratory activity [51], which preclude detailed behavioral analyses. Similarly, mice expressing (in the entire brain) a substantial part of the GluR-B population in the Q/R site-unedited form become seizure-prone and die prematurely [53]. Some of these problems can be partially overcome by use of spatially and temporally restricted expression systems [54–56], in particular the Cre-lox system, with Cre-recombinase expression in defined brain areas of gene-targeted mice carrying GluR-B alleles marked by loxP sites for Cre-mediated recombination [55,57]. Indeed, restricting the expression of Q/R site-unedited GluR-B to forebrain resulted in almost normal lifespan and an only weakly seizure-prone phenotype [58]. Mice with forebrain-specific GluR-B depletion appeared almost completely normal throughout life with no developmental abnormalities, thus permitting a detailed, quantitative investigation of olfactory behavior."}