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Prodrugs--from serendipity to rational design.

机译:前药-从偶然到合理的设计。

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The prodrug concept has been used to improve undesirable properties of drugs since the late 19th century, although it was only at the end of the 1950s that the actual term prodrug was introduced for the first time. Prodrugs are inactive, bioreversible derivatives of active drug molecules that must undergo an enzymatic and/or chemical transformation in vivo to release the active parent drug, which can then elicit its desired pharmacological effect in the body. In most cases, prodrugs are simple chemical derivatives that are only one or two chemical or enzymatic steps away from the active parent drug. However, some prodrugs lack an obvious carrier or promoiety but instead result from a molecular modification of the prodrug itself, which generates a new active compound. Numerous prodrugs designed to overcome formulation, delivery, and toxicity barriers to drug utilization have reached the market. In fact, approximately 20% of all small molecular drugs approved during the period 2000 to 2008 were prodrugs. Although the development of a prodrug can be very challenging, the prodrug approach represents a feasible way to improve the erratic properties of investigational drugs or drugs already on the market. This review introduces in depth the rationale behind the use of the prodrug approach from past to present, and also considers the possible problems that can arise from inadequate activation of prodrugs.
机译:从19世纪末开始,前药概念就一直被用来改善药物的不良特性,尽管直到1950年代末才首次引入实际术语“前药”。前药是活性药物分子的无活性的,生物可逆的衍生物,必须在体内进行酶促和/或化学转化以释放出活性母体药物,然后才能在体内引发其所需的药理作用。在大多数情况下,前药是简单的化学衍生物,与活性母体药物仅相距一两个化学或酶促步骤。但是,某些前药缺乏明显的载体或原基,而是由前药本身的分子修饰产生的,从而产生新的活性化合物。旨在克服配方,递送和药物利用毒性障碍的多种前药已投放市场。实际上,在2000年至2008年期间批准的所有小分子药物中,约有20%是前药。尽管前药的开发可能非常具有挑战性,但前药方法代表了一种改善研究药物或市场上已有药物的不稳定特性的可行方法。这篇综述深入地介绍了从前到现在使用前药方法的基本原理,并且还考虑了前药活化不足可能引起的问题。

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