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MECHANISM-BASED INACTIVATION OF RIBONUCLEASE A

机译:基于机理的核糖核酸酶A的失活

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The first example of a mechanism-based inhibitor of a phosphodiesterase is reported. Although the inactivation brought about by the fluoride 4 is not complete, this compound provides a useful starting point for the synthesis of other more potent inhibitors of ribonuclease A, as well as inhibitors of other nucleases. In addition, an inexpensive method is described for the synthesis of phosphate diesters that cannot be synthesized using standard phosphoramidite methodology. Phosphitylation of the target alcohol with a dialkyl chlorophosphite, followed by activation of the resulting trialkyl phosphite with It, yields an iodophosphate. The resulting iodophosphate can then be coupled to a second alcohol, phenol, or enolate to give a phosphate triester, which after subsequent deprotection affords the desired phosphate diester. The novel phosphorylation chemistry presented should greatly facilitate the synthesis of other similar mechanism-based phosphodiesterase inhibitors. [References: 45]
机译:报道了基于机理的磷酸二酯酶抑制剂的第一个例子。尽管氟化物4导致的灭活作用还不完全,但该化合物为合成其他更有效的核糖核酸酶A抑制剂以及其他核酸酶抑制剂提供了有用的起点。另外,描述了一种廉价的方法用于合成不能使用标准亚磷酰胺方法合成的磷酸二酯。将目标醇用亚磷酸二烷基酯进行磷酸化,然后用It将其活化,生成亚磷酸三烷基酯,得到碘代磷酸盐。然后可以将所得的碘代磷酸酯与第二种醇,苯酚或烯醇酸酯偶联以产生磷酸酯三酯,其在随后的脱保护之后提供所需的磷酸二酯。提出的新型磷酸化化学应极大地促进其他类似的基于机理的磷酸二酯酶抑制剂的合成。 [参考:45]

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