Effect of histaminergic manipulation on weight in obese adults: a randomized placebo controlled trial

Barak, Nir; Greenway, Frank L.; Fujioka, Ken; Aronne, Louis J.; Kushner, Robert F.

doi:10.1038/ijo.2008.135

Cited by 37 publications

(37 citation statements)

References 30 publications

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“…These clinical findings correspond with the results of animal studies, in which it was demonstrated that the co-treatment with betahistine partially reduced olanzapine-induced weight gain sideeffects [169]. It is worthy to note that histaminergic modulation may counterbalance druginduced overfeeding and weight gain, however it may be ineffective when there is no drugdependent alteration as showed in clinical trials in obese (otherwise health) subjects [172,171]. Therefore, it is not clear whether it could be useful as a weight-loss medication in obese non-medicated people.…”

Section: Clinical Trials For Co-treatment Of Betahistine and Olanzapisupporting

confidence: 74%

“…Barak and colleagues conducted a multicentre randomized, placebo-controlled weight loss trial using betahistine (16,32,48 mg/day) in 281 obese adults for a 12-week treatment [171]. The overall results revealed that betahistine did not induce significant weight loss in obese participants at the above dosages, while the prevalence of adverse events was low.…”

Section: Clinical Trials For Co-treatment Of Betahistine and Olanzapimentioning

confidence: 99%

“…The overall results revealed that betahistine did not induce significant weight loss in obese participants at the above dosages, while the prevalence of adverse events was low. However, further subgroup analysis revealed that the non-Hispanics women ≤ 50 years old, treated by betahistine (48 mg/day) lost ~4.24 kg body weight, compared with the placebo group (~1.65 kg) (p=0.005) [171] (Table 1). Another randomized placebo-controlled double-blind trial reported that 24 hours treatment of betahistine (48, 96, or 144 mg/day) had no effect on food intake or appetites [172], suggesting that long term administration may be the essential factor to reveal the effect of betahistine on energy intake [172] (Table 1).…”

Section: Clinical Trials For Co-treatment Of Betahistine and Olanzapimentioning

confidence: 99%

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

Lian

Huang

Pai

et al. 2016

Pharmacological Research

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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 olanzapineinduced 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.

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Section: Clinical Trials For Co-treatment Of Betahistine and Olanzapisupporting

confidence: 74%

Section: Clinical Trials For Co-treatment Of Betahistine and Olanzapimentioning

confidence: 99%

Section: Clinical Trials For Co-treatment Of Betahistine and Olanzapimentioning

confidence: 99%

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

Lian

Huang

Pai

et al. 2016

Pharmacological Research

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“…43 In 2008, a study reported a significant weight reduction in women aged less than 50 years who received 48 mg betahistine/day rather than a placebo throughout a 12-week randomized controlled trial. 44 In 2012; a review regarded betahistine as one of the drug candidates for future role as a centrally acting anti-obesity medications. 45 In this study, administration of betahistine (along with low calorie diet and medium intensity exercise) caused a significant reduction in FPG, HbA1c%, Cpeptide, IR and functioning Beta Cell percent.…”

Section: Discussionmentioning

confidence: 99%

Role of betahistine in glycemic control of obese subjects: a placebo- controlled clinical trial

Al-Anbari

Sahib

Al-Mukhtar

2016

Int J Basic Clin Pharmacol

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Background: Poor glycemic control, insulin resistance and abnormal beta cell function are of the most important complications that associated with obesity, targeting of such complications with pharmacological agents depending on the already existing central mechanism may decrease the incidence of morbidity and mortality among obese subjects. Betahistine is an anti-vertigo drug, commonly prescribed to patients with balance disorders or to improve vertigo symptoms associated with Meniere's disease. The aim of this study was to investigate the effect of betahistine on glycemic status, insulin resistance and pancreatic function in obese subjects.Methods: A randomized, placebo controlled trial was carried out on 72 obese subjecta of both sexes with age range of 18-50 years who allocated into two groups: Group A: 48 patients treated with 144mg /day in three divided every eight hours for twelve weeks. Group B: 24 patients treated with placebo for twelve weeks to serve as control. For each group, demographic data, liver and renal function tests beside the studied parameters were investigated at baseline and after 12 weeks.Results: Administration of betahistine to obese subjects resulted in improvement in fasting blood glucose, glycosylated hemoglobin, insulin resistance and beta cell percent values after twelve weeks compared to baseline values and placebo treated group.Conclusions: Administration of betahistine in a dose of 144mg /day for twelve weeks to obese subjects effectively improve glycemic control, insulin resistance and beta cell functions in these subjects, indicating the beneficial effect of betahistine in slowing or reversing the long term progress of obesity complications without incidence of any serious adverse effects, indicating its efficacy and safety.

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“…21 While claims have been made that Betahistine is associated with weight loss, these appear to be unfounded. 22 …”

Section: Marketed Preparations Of H 3 R Antagonist Betahistinementioning

confidence: 99%

Untitled

2015

IJPSR

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ABSTRACT:The histamine H3 receptor is an G protein-coupled receptor that regulates neurotransmission in the central nervous system and plays a major role in cognitive and homeostatic functions. The third histamine receptor was discovered in 1983 by a traditional pharmacological approach, consisting of assessing the inhibitory effect of histamine on its own release from depolarized rat brain slices. Histamine H3 receptors are found mostly in central nervous system also to some extent in peripheral tissues and involved in the regulation of release of various neurotransmitters in brain. They have been implicated in diverse potential therapeutic applications such as sleep wake disorders, attentiondeficient hyperactivity disorder, epilepsy, cognitive impairment and obesity. This review is aimed to provide an overview of marketed preparations and also experimental H3 receptor antagonists under pipeline of drug discovery and development.

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Effect of histaminergic manipulation on weight in obese adults: a randomized placebo controlled trial

Cited by 37 publications

References 30 publications

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

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

Role of betahistine in glycemic control of obese subjects: a placebo- controlled clinical trial

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