Chemical Biology Laboratory, Molecular Discovery Program, Center for Cancer Research, National Cancer Institute, National Institutes of Health, Frederick, Maryland 21702, United States.
J Org Chem. 2011 Nov 4;76(21):8885-90. doi: 10.1021/jo201599c. Epub 2011 Oct 3.
We had previously reported that Mitsunobu-based introduction of alkyl substituents onto the imidazole N(π)-position of a key histidine residue in phosphothreonine-containing peptides can impart high binding affinity against the polo-box domain of polo-like kinase 1. Our current paper investigates the mechanism leading to this N(π)-alkylation and provides synthetic methodologies that permit the facile synthesis of histidine N(π)-modified peptides. These agents represent new and potentially important tools for biological studies.
我们之前曾报道过,基于 Mitsunobu 的方法在含有磷酸苏氨酸的肽中关键组氨酸残基的咪唑 N(π)-位上引入烷基取代基,可以赋予与 polo 样激酶 1 的 polo 盒结构域高的结合亲和力。我们当前的论文研究了导致这种 N(π)-烷基化的机制,并提供了允许方便地合成组氨酸 N(π)-修饰肽的合成方法。这些试剂代表了用于生物学研究的新的、潜在重要的工具。
