Phenylpiracetam: molecular mechanisms of effects in obesity

O. Gromova, I. Torshin, L. B. Lazebnik
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Abstract

Metabolic syndrome (MS), including hyperlipidemia and obesity, is a proven risk factor not only for cerebrovascular diseases. Obesity is a dangerous comorbid condition in patients, complicating cerebrovascular pathology, asthenic conditions, diabetes mellitus, liver disease, alcoholism and other diseases accompanied by dysmetabolic disorders. Fundamental and clinical studies of the nootropic fonturacetam (Actitropil) have shown that the drug can be used not only for a wide range of cerebrovascular diseases, asthenia, etc., but also for obesity. The mechanisms of action of fonturacetam in producing pharmacological effects that reduce excess appetite and prevent the accumulation of excess body weight were studied in chemoreactomic analysis. Regulation of the metabolic effectiveness of Phenylpiracetam is based on multi-level correction of target transmitters and receptors that control the metabolism of fats and carbohydrates (influence on leptin, cannabinoid receptors, adrenoreceptors, peroxisome receptors). Phenylpiracetam activates the adrenaline, adenosine, glucagon-like peptide, sphingosine phosphate and peroxisome proliferators (PPARG) receptors and inhibits the cannabinoid, opioid, histamine, glutamate, nociceptin, orexin, neuropeptide Y receptors. The resulting pharmacological properties indicate important pathophysiological effects of phenylpiracetam for the treatment of obesity. A decrease in the rate of fat mass gain when taking Phenylpiracetam is noted due to an improvement in the quality of night sleep. Chemoreactomic analysis of Actitropil indicated new molecular mechanisms of the pharmacological action of the molecule, which reduces excess appetite and prevents the accumulation of excess body weight. Phenylpiracetam (Actitropil) is distinguished by a balance of effectiveness, a high safety profile with no addiction to the drug and safety. Thus, Phenylpiracetam is a racetam that exhibits nootropic, antiasthenic and lipotropic effects.
苯基吡拉西坦:肥胖症的分子作用机制
代谢综合征(MS),包括高脂血症和肥胖症,已被证实不仅是脑血管疾病的危险因素。肥胖是一种危险的并发症,会并发脑血管病变、虚弱、糖尿病、肝病、酗酒和其他伴有代谢紊乱的疾病。对促智药 fonturacetam(Actitropil)的基础和临床研究表明,该药物不仅可用于治疗各种脑血管疾病、气喘等,还可用于治疗肥胖症。通过化学反应组学分析,研究了囟素在产生降低过剩食欲和防止体重过重积累的药理作用方面的作用机制。苯基吡拉西坦对新陈代谢效果的调节是基于对控制脂肪和碳水化合物新陈代谢的目标递质和受体的多层次校正(对瘦素、大麻素受体、肾上腺素受体、过氧化物酶受体的影响)。苯吡拉西坦能激活肾上腺素、腺苷、胰高血糖素样肽、磷酸鞘磷脂和过氧物酶体(PPARG)受体,抑制大麻素、阿片、组胺、谷氨酸、神经肽 Y 受体。由此产生的药理特性表明,苯基吡拉西坦对治疗肥胖症具有重要的病理生理作用。服用苯基吡拉西坦后,由于夜间睡眠质量的改善,脂肪量增加的速度有所下降。对 Actitropil 进行的化学反应组学分析表明,该分子的药理作用具有新的分子机制,可以降低过剩的食欲,防止体重超标。苯吡拉西坦(Actitropil)的显著特点是兼顾有效性、高安全性、无药物成瘾性和安全性。因此,苯基吡拉西坦是一种赛坦类药物,具有促智、抗疲劳和促脂作用。
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