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A potential mechanism underlying atypical antipsychotics-induced lipid disturbances
by
Yao, J K
, Tang, M M
, Xu, P
, Xue, Y
, Tan, Q Y
, Deng, Y
, Cai, H L
, Jiang, P
, Li, H D
, Dang, R L
in
631/154
/ 631/154/436/108
/ Animals
/ Antipsychotic Agents - blood
/ Antipsychotic Agents - pharmacology
/ Antipsychotics
/ Behavioral Sciences
/ Biological Psychology
/ Blotting, Western
/ Cholesterol - blood
/ Clozapine - pharmacology
/ Corticosterone - blood
/ Disease Models, Animal
/ Fatty Acids, Nonesterified - blood
/ Insulin - blood
/ Lipid Metabolism - drug effects
/ Lipogenesis - drug effects
/ Liver - drug effects
/ Male
/ Medicine
/ Medicine & Public Health
/ Neurosciences
/ Original
/ original-article
/ Pharmacotherapy
/ Polymerase Chain Reaction
/ Progesterone - blood
/ Psychiatry
/ Rats
/ Rats, Sprague-Dawley
/ Risperidone - pharmacology
/ Signal Transduction - drug effects
/ Triglycerides - blood
2015
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A potential mechanism underlying atypical antipsychotics-induced lipid disturbances
by
Yao, J K
, Tang, M M
, Xu, P
, Xue, Y
, Tan, Q Y
, Deng, Y
, Cai, H L
, Jiang, P
, Li, H D
, Dang, R L
in
631/154
/ 631/154/436/108
/ Animals
/ Antipsychotic Agents - blood
/ Antipsychotic Agents - pharmacology
/ Antipsychotics
/ Behavioral Sciences
/ Biological Psychology
/ Blotting, Western
/ Cholesterol - blood
/ Clozapine - pharmacology
/ Corticosterone - blood
/ Disease Models, Animal
/ Fatty Acids, Nonesterified - blood
/ Insulin - blood
/ Lipid Metabolism - drug effects
/ Lipogenesis - drug effects
/ Liver - drug effects
/ Male
/ Medicine
/ Medicine & Public Health
/ Neurosciences
/ Original
/ original-article
/ Pharmacotherapy
/ Polymerase Chain Reaction
/ Progesterone - blood
/ Psychiatry
/ Rats
/ Rats, Sprague-Dawley
/ Risperidone - pharmacology
/ Signal Transduction - drug effects
/ Triglycerides - blood
2015
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While trying to remove the title from your shelf something went wrong :( Kindly try again later!
Do you wish to request the book?
A potential mechanism underlying atypical antipsychotics-induced lipid disturbances
by
Yao, J K
, Tang, M M
, Xu, P
, Xue, Y
, Tan, Q Y
, Deng, Y
, Cai, H L
, Jiang, P
, Li, H D
, Dang, R L
in
631/154
/ 631/154/436/108
/ Animals
/ Antipsychotic Agents - blood
/ Antipsychotic Agents - pharmacology
/ Antipsychotics
/ Behavioral Sciences
/ Biological Psychology
/ Blotting, Western
/ Cholesterol - blood
/ Clozapine - pharmacology
/ Corticosterone - blood
/ Disease Models, Animal
/ Fatty Acids, Nonesterified - blood
/ Insulin - blood
/ Lipid Metabolism - drug effects
/ Lipogenesis - drug effects
/ Liver - drug effects
/ Male
/ Medicine
/ Medicine & Public Health
/ Neurosciences
/ Original
/ original-article
/ Pharmacotherapy
/ Polymerase Chain Reaction
/ Progesterone - blood
/ Psychiatry
/ Rats
/ Rats, Sprague-Dawley
/ Risperidone - pharmacology
/ Signal Transduction - drug effects
/ Triglycerides - blood
2015
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A potential mechanism underlying atypical antipsychotics-induced lipid disturbances
Journal Article
A potential mechanism underlying atypical antipsychotics-induced lipid disturbances
2015
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Overview
Previous findings suggested that a four-protein complex, including sterol-regulatory element-binding protein (SREBP), SREBP-cleavage-activating protein (SCAP), insulin-induced gene (INSIG) and progesterone receptor membrane component 1 (PGRMC1), within the endoplasmic reticulum appears to be an important regulator responsible for atypical antipsychotic drug (AAPD)-induced lipid disturbances. In the present study, effects of typical antipsychotic drug and AAPDs as well as treatment outcome of steroid antagonist mifepristone (MIF) on the PGRMC1/INSIG/SCAP/SREBP pathway were investigated in rat liver using real-time quantitative polymerase chain reaction (qPCR) and western blot analysis. In addition, serum triacylglycerol, total cholesterol, free fatty acids and various hormones including progesterone, corticosterone and insulin were measured simultaneously. Following treatment with clozapine or risperidone, both lipogenesis and cholesterogenesis were enhanced via inhibition of PGRMC1/INSIG-2 and activation of SCAP/SREBP expressions. Such metabolic disturbances, however, were not demonstrated in rats treated with aripiprazole (ARI) or haloperidol (HAL). Moreover, the add-on treatment of MIF was effective in reversing the AAPD-induced lipid disturbances by upregulating the expression of PGRMC1/INSIG-2 and subsequent downregulation of SCAP/SREBP. Taken together, our findings suggest that disturbances in lipid metabolism can occur at an early stage of AAPD treatment before the presence of weight gain. Such metabolic defects can be modified by an add-on treatment of steroid antagonist MIF enhancing the PGRMC1 pathway. Thus, it is likely that PGRMC1/INSIG-2 signaling may be a therapeutic target for AAPD-induced weight gain.
Publisher
Nature Publishing Group UK,Nature Publishing Group
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