TY - JOUR
T1 - Hyperleptinemia contributes to antipsychotic drug–associated obesity and metabolic disorders
AU - Zhao, Shangang
AU - Lin, Qian
AU - Xiong, Wei
AU - Li, Li
AU - Straub, Leon
AU - Zhang, Dinghong
AU - Zapata, Rizaldy
AU - Zhu, Qingzhang
AU - Sun, Xue Nan
AU - Zhang, Zhuzhen
AU - Funcke, Jan Bernd
AU - Li, Chao
AU - Chen, Shiuhwei
AU - Zhu, Yi
AU - Jiang, Nisi
AU - Li, Guannan
AU - Xu, Ziying
AU - Wyler, Steven C.
AU - Wang, May Yun
AU - Bai, Juli
AU - Han, Xianlin
AU - Kusminski, Christine M.
AU - Zhang, Ningyan
AU - An, Zhiqiang
AU - Elmquist, Joel K.
AU - Osborn, Olivia
AU - Liu, Chen
AU - Scherer, Philipp E.
N1 - Publisher Copyright:
© 2023 American Association for the Advancement of Science. All rights reserved.
PY - 2023/11/15
Y1 - 2023/11/15
N2 - Despite their high degree of effectiveness in the management of psychiatric conditions, exposure to antipsychotic drugs, including olanzapine and risperidone, is frequently associated with substantial weight gain and the development of diabetes. Even before weight gain, a rapid rise in circulating leptin concentrations can be observed in most patients taking antipsychotic drugs. To date, the contribution of this hyperleptinemia to weight gain and metabolic deterioration has not been defined. Here, with an established mouse model that recapitulates antipsychotic drug–induced obesity and insulin resistance, we not only confirm that hyperleptinemia occurs before weight gain but also demonstrate that hyperleptinemia contributes directly to the development of obesity and associated metabolic disorders. By suppressing the rise in leptin through the use of a monoclonal leptin-neutralizing antibody, we effectively prevented weight gain, restored glucose tolerance, and preserved adipose tissue and liver function in antipsychotic drug–treated mice. Mechanistically, suppressing excess leptin resolved local tissue and systemic inflammation typically associated with antipsychotic drug treatment. We conclude that hyperleptinemia is a key contributor to antipsychotic drug–associated weight gain and metabolic deterioration. Leptin suppression may be an effective approach to reducing the undesirable side effects of antipsychotic drugs.
AB - Despite their high degree of effectiveness in the management of psychiatric conditions, exposure to antipsychotic drugs, including olanzapine and risperidone, is frequently associated with substantial weight gain and the development of diabetes. Even before weight gain, a rapid rise in circulating leptin concentrations can be observed in most patients taking antipsychotic drugs. To date, the contribution of this hyperleptinemia to weight gain and metabolic deterioration has not been defined. Here, with an established mouse model that recapitulates antipsychotic drug–induced obesity and insulin resistance, we not only confirm that hyperleptinemia occurs before weight gain but also demonstrate that hyperleptinemia contributes directly to the development of obesity and associated metabolic disorders. By suppressing the rise in leptin through the use of a monoclonal leptin-neutralizing antibody, we effectively prevented weight gain, restored glucose tolerance, and preserved adipose tissue and liver function in antipsychotic drug–treated mice. Mechanistically, suppressing excess leptin resolved local tissue and systemic inflammation typically associated with antipsychotic drug treatment. We conclude that hyperleptinemia is a key contributor to antipsychotic drug–associated weight gain and metabolic deterioration. Leptin suppression may be an effective approach to reducing the undesirable side effects of antipsychotic drugs.
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U2 - 10.1126/scitranslmed.ade8460
DO - 10.1126/scitranslmed.ade8460
M3 - Article
C2 - 37992151
AN - SCOPUS:85177985472
SN - 1946-6234
VL - 15
JO - Science translational medicine
JF - Science translational medicine
IS - 723
M1 - eade8460
ER -