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Experimental therapies targeting apolipoprotein C-III for the treatment of hyperlipidemia - spotlight on volanesorsen

机译:靶向载脂蛋白C-III的实验疗法治疗高脂血症 - 染色菌

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Introduction: Despite the substantial reduction in cardiovascular morbidity and mortality after the management of dyslipidemia with statins, residual risk remains even after achieving low-density lipoprotein cholesterol targets. This residual risk appears to be partly attributed to low levels of high-density lipoprotein cholesterol (HDL-C) and high levels of triglycerides (TG). Apolipoprotein C3 (APOC3) is a key regulator of TG metabolism and its targeting may reduce TG levels and cardiovascular risk. Areas covered: We discuss APOC3-targeted experimental treatments for dyslipidemia. There is an emphasis on volanesorsen because it the agent in the most advanced stage of development. M580, a retinoic acid receptor-alpha specific agonist, an agent in early-stage development is briefly covered. Preclinical data suggest that this agent decreases APOC3 mRNA levels and reduces total cholesterol, TG levels and hepatic lipid accumulation. Expert opinion: The effects of this novel therapeutic approach on cardiovascular morbidity and mortality should be determined in randomized controlled trials. The cost of volanesorsen, the unfavorable safety profile and the need for subcutaneous administration present barriers to long-term use. AM580 may hold promise in the management of hypertriglyceridemia but further investigations are necessary to evaluate safety and efficacy.
机译:介绍:尽管在使用他汀类药物的血脂血症管理后心血管发病率和死亡率显着降低,但仍然在实现低密度脂蛋白胆固醇靶标后,残留风险仍然存在。这种残余风险似乎部分归因于低水平的高密度脂蛋白胆固醇(HDL-C)和高水平的甘油三酯(TG)。载脂蛋白C3(APOC3)是TG代谢的关键调节剂,其靶向可降低TG水平和心血管风险。所涵盖的地区:我们讨论血脂血症的Apoc3针对靶向实验治疗方法。强调valaneSorsen,因为它是在最先进的发展阶段的代理人。 M580,一种视黄酸受体-α特异性激动剂,简要介绍了早期发育的试剂。临床前数据表明该试剂降低了Apoc3 mRNA水平并降低了总胆固醇,TG水平和肝脂肪积累。专家意见:这种新型治疗方法对心血管发病率和死亡率的影响应在随机对照试验中确定。 ValaneSorsen的成本,不利的安全性剖面和对皮下给药的需要存在长期使用的障碍。 AM580可能在高甘油脂血症管理中持有承诺,但进一步调查是评估安全性和疗效的必要条件。

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