Dibutyltin Disrupts Glucocorticoid Receptor Function and Impairs Glucocorticoid-Induced Suppression of Cytokine Production 英文参考文献.docVIP

下载本文档

1
0
约4.85万字
约 11页
2017-05-11 发布于上海
举报
版权申诉

Dibutyltin Disrupts Glucocorticoid Receptor Function and Impairs Glucocorticoid-Induced Suppression of Cytokine Production 英文参考文献.doc

1、本文档共11页，可阅读全部内容。
2、原创力文档（book118）网站文档一经付费（服务费），不意味着购买了该文档的版权，仅供个人/单位学习、研究之用，不得用于商业用途，未经授权，严禁复制、发行、汇编、翻译或者网络传播等，侵权必究。
3、本站所有内容均由合作方或网友上传，本站不对文档的完整性、权威性及其观点立场正确性做任何保证或承诺！文档内容仅供研究参考，付费前请自行鉴别。如您付费，意味着您自己接受本站规则且自行承担风险，本站不退款、不进行额外附加服务；查看《如何避免下载的几个坑》。如果您已付费下载过本站文档，您可以点击这里二次下载。
4、如文档侵犯商业秘密、侵犯著作权、侵犯人身权等，请点击“版权申诉”（推荐），也可以打举报电话：400-050-0827(电话支持时间：9:00-18:30)。
5、该文档为VIP文档，如果想要下载，成为VIP会员后，下载免费。
6、成为VIP后，下载本文档将扣除1次下载权益。下载后，不支持退款、换文档。如有疑问请联系我们。
7、成为VIP后，您将拥有八大权益，权益包括：VIP文档下载权益、阅读免打扰、文档格式转换、高级专利检索、专属身份标志、高级客服、多端互通、版权登记。
8、VIP文档为合作方或网友上传，每下载1次，网站将根据用户上传文档的质量评分、类型等，对文档贡献者给予高额补贴、流量扶持。如果你也想贡献VIP文档。上传文档

Dibutyltin Disrupts Glucocorticoid Receptor Function and Impairs Glucocorticoid-Induced Suppression of Cytokine Production 英文参考文献

DibutyltinDisruptsGlucocorticoidReceptorFunction andImpairsGlucocorticoid-InducedSuppressionof CytokineProduction ChristelGumy1,2,CharlieChandsawangbhuwana3,AnnaA.Dzyakanchuk1,DeniseV.Kratschmar1, MichaelE.Baker3*,AlexOdermatt1* 1Division of Molecular and Systems Toxicology, Department of Pharmaceutical Sciences, University of Basel, Basel, Switzerland, 2Department of Nephrology and Hypertension,UniversityofBerne,Berne,Switzerland,3DepartmentofMedicine,UniversityofCaliforniaSanDiego,LaJolla,California,UnitedStatesofAmerica Abstract Background: Organotins are highly toxic and widely distributed environmental chemicals. Dibutyltin (DBT) is used as stabilizerintheproductionofpolyvinylchlorideplastics,anditisalsothemajormetaboliteformedfromtributyltin(TBT)in vivo.DBTisimmunotoxic,however,theresponsibletargetsremaintobedefined.Duetotheimportanceofglucocorticoids inimmune-modulation,weinvestigatedwhetherDBTcouldinterferewithglucocorticoidreceptor(GR)function. Methodology:WeusedHEK-293cellstransientlytransfectedwithhumanGRaswellasratH4IIEhepatomacellsandnative humanmacrophagesandhumanTHP-1macrophagesexpressingendogenousreceptortostudyorganotineffectsonGR function.Dockingoforganotinswasusedtoinvestigatethebindingmechanism. PrincipalFindings:WefoundthatnanomolarconcentrationsofDBT,butnototherorganotinstested,inhibitligandbinding toGRanditstranscriptionalactivity.DockinganalysisindicatedthatDBTinhibitsGRactivationallostericallybyinsertinginto asiteclosetothesteroid-bindingpocket,whichdisruptsakeyinteractionbetweentheA-ringoftheglucocorticoidandthe GR. DBT inhibited glucocorticoid-induced expression of phosphoenolpyruvate carboxykinase (PEPCK) and tyrosine- aminotransferase (TAT) and abolished the glucocorticoid-mediated transrepression of TNF-a-induced NF-kB activity. Moreover, DBT abrogated the glucocorticoid-mediated suppression of interleukin-6 (IL-6) and TNF-a production in lipopolysaccharide(LPS)-stimulatednativehumanmacrophagesandhumanTHP-1macrophages. Conclusions:DBT