Cardiovascular effects of antiobesity drugs: are the new medicines all the same?

Mauro Cataldi, Angelo Cignarelli, Francesco Giallauria, Giovanna Muscogiuri, Luigi Barrea, Silvia Savastano, Annamaria Colao, on behalf of Obesity Programs of nutrition, Education, Research and Assessment (OPERA) Group
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引用次数: 5

Abstract

Waiting for a definite answer from well-designed randomized prospective clinical trials, the impact of the new antiobesity drugs -liraglutide, bupropion/naltrexone, phentermine/topiramate and lorcaserin- on cardiovascular outcomes remains uncertain. What has been learned from previous experience with older medicines is that antiobesity drugs may influence cardiovascular health not only causing weight reduction but also through direct actions on the cardiovascular system. Therefore, in the present review, we examine what is known, mainly from preclinical investigations, about the cardiovascular pharmacology of the new antiobesity medicines with the aim of highlighting potential mechanistic differences. We will show that the two active substances of the bupropion/naltrexone combination both exert beneficial and unwanted cardiovascular effects. Indeed, bupropion exerts anti-inflammatory effects but at the same time it does increase heart rate and blood pressure by potentiating catecholaminergic neurotransmission, whereas naltrexone reduces TLR4-dependent inflammation and has potential protective effects in stroke but also impairs cardiac adaption to ischemia and the beneficial opioid protective effects mediated in the endothelium. On the contrary, with the only exception of a small increase in heat rate, liraglutide only exerts favorable cardiovascular effects by protecting myocardium and brain from ischemic damage, improving heart contractility, lowering blood pressure and reducing atherogenesis. As far as the phentermine/topiramate combination is concerned, no direct cardiovascular beneficial effect is expected for phentermine (as this drug is an amphetamine derivative), whereas topiramate may exert cardioprotective and neuroprotective effects in ischemia and anti-inflammatory and antiatherogenic actions. Finally, lorcaserin, a selective 5HT2C receptor agonist, does not seem to exert significant direct effects on the cardiovascular system though at very high concentrations this drug may also interact with other serotonin receptor subtypes and exert unwanted cardiovascular effects. In conclusion, the final effect of the new antiobesity drugs on cardiovascular outcomes will be a balance between possible (but still unproved) beneficial effects of weight loss and “mixed” weight-independent drug-specific effects. Therefore comparative studies will be required to establish which one of the new medicines is more appropriate in patients with specific cardiovascular diseases.
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抗肥胖药物对心血管的影响:新药都一样吗?
新的抗肥胖药物--利拉鲁肽、安非他明/纳曲酮、芬特明/托吡酯和氯卡塞林--对心血管结果的影响仍有待设计完善的随机前瞻性临床试验给出明确答案。从以往使用老药的经验中可以看出,抗肥胖药物不仅能减轻体重,还能直接作用于心血管系统,从而影响心血管健康。因此,在本综述中,我们将主要通过临床前研究,对新的抗肥胖药物的心血管药理学进行研究,以突出潜在的机理差异。我们将说明,安非他酮/纳曲酮复方制剂的两种活性物质都会对心血管产生有益或有害的影响。事实上,安非他酮具有抗炎作用,但同时也会通过增强儿茶酚胺能神经递质而增加心率和血压;而纳曲酮可减少 TLR4 依赖性炎症,对中风具有潜在的保护作用,但同时也会损害心脏对缺血的适应性以及内皮介导的有益的阿片类药物保护作用。相反,利拉鲁肽除了能使发热率略有增加外,只能通过保护心肌和大脑免受缺血性损伤、改善心脏收缩力、降低血压和减少动脉粥样硬化的发生来发挥有利的心血管效应。至于芬特明/托吡酯联合用药,预计芬特明不会对心血管产生直接的有益影响(因为这种药物是一种苯丙胺衍生物),而托吡酯则可能在缺血时发挥保护心脏和神经的作用,并具有抗炎和抗动脉粥样硬化的作用。最后,选择性 5HT2C 受体激动剂洛卡西林(lorcaserin)似乎对心血管系统没有明显的直接影响,但在浓度非常高的情况下,这种药物也可能与其他血清素受体亚型相互作用,对心血管产生不必要的影响。总之,新型抗肥胖药物对心血管结果的最终影响将在减轻体重可能产生的(但仍未得到证实的)有益影响与 "混合的 "不依赖体重的药物特异性影响之间取得平衡。因此,需要进行比较研究,以确定哪种新药更适合特定心血管疾病患者。
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