Ameliorating antipsychotic-induced weight gain by betahistine: Mechanisms and clinical implications

Jiamei Lian; Xu-Feng Huang; Nagesh Pai; Chao Deng

doi:10.1016/j.phrs.2016.02.011

Ameliorating antipsychotic-induced weight gain by betahistine: Mechanisms and clinical implications

Pharmacol Res. 2016 Apr:106:51-63. doi: 10.1016/j.phrs.2016.02.011. Epub 2016 Feb 15.

Authors

Jiamei Lian¹, Xu-Feng Huang¹, Nagesh Pai², Chao Deng³

Affiliations

¹ Illawarra Health and Medical Research Institute, Wollongong 2522, NSW, Australia; School of Medicine, University of Wollongong, Wollongong, 2522, NSW, Australia.
² School of Medicine, University of Wollongong, Wollongong, 2522, NSW, Australia.
³ Illawarra Health and Medical Research Institute, Wollongong 2522, NSW, Australia; School of Medicine, University of Wollongong, Wollongong, 2522, NSW, Australia. Electronic address: chao@uow.edu.au.

PMID: 26892184
DOI: 10.1016/j.phrs.2016.02.011

Abstract

Second generation antipsychotic drugs (SGAs) cause substantial body weight gain/obesity and other metabolic side-effects such as dyslipidaemia. Their antagonistic affinity to the histaminergic H1 receptor (H1R) has been identified as one of the main contributors to weight gain/obesity side-effects. The effects and mechanisms of betahistine (a histaminergic H1R agonist and H3 receptor antagonist) have been investigated for ameliorating SGA-induced weight gain/obesity in both animal models and clinical trials. It has been demonstrated that co-treatment with betahistine is effective in reducing weight gain, associated with olanzapine in drug-naïve patients with schizophrenia, as well as in the animal models of both drug-naïve rats and rats with chronic, repeated exposure to olanzapine. Betahistine co-treatment can reduce food intake and increase the effect of thermogenesis in brown adipose tissue by modulating hypothalamic H1R-NPY-AMPKα (NPY: neuropeptide Y; AMPKα: AMP-activated protein kinase α) pathways, and ameliorate olanzapine-induced dyslipidaemia through modulation of AMPKα-SREBP-1-PPARα-dependent pathways (SREBP-1: Sterol regulatory element binding protein 1; PPARα: Peroxisome proliferator-activated receptor-α) in the liver. Although reduced locomotor activity was observed from antipsychotic treatment in rats, betahistine did not affect locomotor activity. Importantly, betahistine co-treatment did not influence the effects of antipsychotics on serotonergic receptors in the key brain regions for antipsychotic therapeutic efficacy. However, betahistine co-treatment reverses the upregulated dopamine D2 binding caused by chronic olanzapine administration, which may be beneficial in reducing D2 supersensitivity often observed in chronic antipsychotic treatment. Therefore, these results provide solid evidence supporting further clinical trials in treating antipsychotics-induced weight gain using betahistine in patients with schizophrenia and other mental disorders.

Keywords: Antipsychotic drug; Aripiprazole (PubChem CID: 60795); Betahistine; Betahistine (PubChem CID: 68643); Chemical compound studied in this article; Clozapine (PubChem CID:2818); Haloperidol (PubChem CID: 3559); Histamine receptor; Locomotor activity; Olanzapine (PubChem CID: 4585); Risperidone (PubChem CID: 5073); Therapeutic efficacy; Weight gain.

Publication types

Research Support, Non-U.S. Gov't
Review

MeSH terms

AMP-Activated Protein Kinases / metabolism
Animals
Antipsychotic Agents / adverse effects*
Benzodiazepines / adverse effects
Betahistine / pharmacology*
Betahistine / therapeutic use*
Histamine Agonists / pharmacology*
Histamine Agonists / therapeutic use*
Humans
Olanzapine
Receptors, Histamine H1 / metabolism
Weight Gain / drug effects*

Substances

Antipsychotic Agents
Histamine Agonists
Receptors, Histamine H1
Benzodiazepines
AMP-Activated Protein Kinases
Olanzapine
Betahistine