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Functional Selectivity, Ligand-Directed Trafficking, Conformation-Specific Agonism: What's In A Name?

机译:功能选择性,配体定向贩运,特定形式的激动性:名字叫什么?

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Research on the design of compounds to selectively affect specific subsets of signals downstream of receptors has burgeoned lately, and several reports discussed at Experimental Biology 2005 indicate progress is being made in the understanding of what makes a drug functionally selective. Different conformations adopted by receptors after associating with specific ligands can determine which intracellular signaling pathways get activated and which do not. The appeal of such specific compounds is enormous when one considers that many disease states might require the subtle manipulation of some (or even one) but not all downstream events stemming from specific receptor activation. Additionally, a better understanding of functional selectivity would likely improve the drug delivery process: if compounds are screened through several functional assays appropriately designed to look for compounds exhibiting a high degree of selectivity, then many potential lead compounds might not be as frequently overlooked.
机译:最近,有关选择性地影响受体下游信号的特定子集的化合物设计的研究蓬勃发展,2005年《实验生物学》上讨论的几份报告表明,在了解什么使药物具有功能选择性方面正在取得进展。受体与特定的配体缔合后所采用的不同构象可以确定哪些细胞内信号通路被激活,哪些没有。当人们认为许多疾病状态可能需要对某些(或什至一种)但并非所有下游事件(由于特定受体激活而引起)进行微妙的操纵时,这种特殊化合物的吸引力是巨大的。此外,对功能选择性的更好理解可能会改善药物的递送过程:如果通过适当设计以寻找表现出高选择性的化合物的几种功能试验筛选化合物,那么许多潜在的先导化合物可能不会被经常忽视。

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