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New molecular targets in the pathophysiology of obesity and available treatment options under investigation

机译:新的分子病理生理学的目标肥胖和可用的治疗方案调查

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摘要

The pharmacotherapy of obesity has historically recorded an overall poor safety and efficacy profile largely because of the complex mechanisms involved in the pathophysiology of obesity. It is hoped that a better understanding of the regulation of body weight will lead us to the development of effective and safer drugs. Recent advances in our understanding of the regulation of energy homeostasis has allowed the design of novel anti-obesity drugs targeting specific molecules crucial for the modulation of energy balance, including drugs that induce satiety, modulate nutrient absorption or influence metabolism or lipogenesis. Almost a decade after the Food and Drug Administration approved the first weight loss medication, it recently approved two novel anti-obesity drugs Belviq (lorcaserin) and Qsymia (topiramate and phentermine), thus signalling the beginning of a new era in the pharmacotherapy of obesity. It is believed that the next generation of weight-loss drugs will be based on combination treatments with gut hormones in a manner that mimics the changes underlying surgically induced weight loss thus introducing the so called 'bariatric pharmacotherapy'. An in-depth understanding of the interrelated physiological and behavioural effects of these new molecules together with the development of new treatment paradigms is needed so that future disappointments in the field of obesity pharmacotherapy may be avoided.
机译:肥胖历来的药物治疗记录整个可怜的安全性和有效性形象很大程度上是由于复杂的机制参与肥胖的病理生理学。希望更好的理解监管的体重将会引领我们开发有效的和安全的药物。我们理解的进步的监管能量的体内平衡的设计小说针对特定抗肥胖药物分子能量的调制的关键平衡,包括药物诱导饱腹感,调节营养吸收或影响新陈代谢和脂肪生成。美国食品和药物管理局的批准第一次减肥药物,它最近批准了两种新颖的抗肥胖药物Belviq(lorcaserin)和Qsymia(托吡酯和芬特明),因此信号的开始肥胖的药物治疗的新时代。相信下一代的减肥将基于联合治疗的药物与肠道激素的方式模仿改变底层减肥手术引起的因此引入所谓的减肥药物治疗”。相关的生理和行为这些新的分子结合的影响开发新的治疗模式是必要的这领域的未来的失望肥胖的药物治疗可以避免。

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