Bureau of Medicine and Surgery, US Navy, Washington, DC, USA.
Am J Clin Nutr. 2010 Jan;91(1):262S-266S. doi: 10.3945/ajcn.2009.28449D. Epub 2009 Nov 18.
Since the early 1970s, pharmaceutical biochemists have sought to exploit the scientific findings that were uncovered when they studied the basis for the function and mode of action of fibric acid derivatives. In the early 1970s, little was known of peroxisome proliferator-activated receptors (PPARs), even in concept. Since then, however, the development of bioactive small molecules in medicinal science has resulted in tools developed to be inserted into the PPAR-binding domain, which has resulted in the recognition of literally thousands of possible biological effects of binding configurations. In diabetes care, the first of the marketed agents from these discoveries and developments was introduced in 1996. It was potent and did its job well. However, the use of this early form of thiazolidinedione sometimes, although rarely, led to fulminant liver failure, and ultimately the drug was removed from the market. Subsequent thiazolidinediones have been developed, and 2 have been relatively successful. However, they are not without their problems. This article describes the history of the development of these drugs, identifies the valuable attributes that they possess, and gives a clear rationale as to why a quest for a "safer" PPAR agonist is still being sought.
自 20 世纪 70 年代初以来,药物生物化学家一直在努力利用他们在研究纤维酸衍生物的功能和作用模式基础时所发现的科学发现。在 20 世纪 70 年代初,人们对过氧化物酶体增殖物激活受体(PPAR)知之甚少,甚至在概念上也是如此。然而,从那时起,医学科学中生物活性小分子的发展导致了开发出用于插入 PPAR 结合域的工具,从而导致识别出成百上千种可能的结合构型的生物学效应。在糖尿病治疗中,这些发现和开发的首批市售药物于 1996 年推出。它功效强大,效果很好。然而,这种早期形式的噻唑烷二酮的使用有时(尽管很少)会导致暴发性肝衰竭,最终该药物被从市场上撤出。随后开发了其他噻唑烷二酮类药物,其中 2 种相对成功。然而,它们并非没有问题。本文描述了这些药物的开发历史,确定了它们所具有的有价值的属性,并清楚地说明了为什么仍在寻找“更安全”的 PPAR 激动剂。
