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An improved reversibly dimerizing mutant of the FK506-binding protein FKBP

机译:一种改进的可逆二聚的突变FK506-binding蛋白质FKBP

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摘要

FK506-binding protein (FKBP) is a monomer that binds to FK506, rapamycin, and related ligands. The F36M substitution, in which Phe36 in the ligand-binding pocket is changed to Met, leads to formation of antiparallel FKBP dimers, which can be dissociated into monomers by ligand binding. This FKBP(M) mutant has been employed in the mammalian secretory pathway to generate aggregates that can be dissolved by ligand addition to create cargo waves. However, when testing this approach in yeast, we found that dissolution of FKBP(M) aggregates was inefficient. An improved reversibly dimerizing FKBP formed aggregates that dissolved more readily. This FKBP(L,V) mutant carries the F36L mutation, which increases the affinity of ligand binding, and the I90V mutation, which accelerates ligand-induced dissociation of the dimers. The FKBP(L,V) mutant expands the utility of reversibly dimerizing FKBP.
机译:FK506-binding蛋白质(FKBP)是一个单体结合吸收FK506,雷帕霉素,和相关的配体。F36M替换,Phe36配体结合口袋改为相遇,导致可以形成反平行的FKBP二聚体由配体结合分离成单体。这FKBP (M)突变体被雇佣的哺乳动物产生分泌途径总量,可以通过配体溶解除了创建货物波。在酵母测试这种方法,我们发现解散FKBP (M)聚集效率低下。FKBP形成聚合物溶解更多很容易。突变,增加配体的亲和力绑定,I90V突变,加速ligand-induced离解的二聚体。FKBP (L, V)突变体膨胀的效用可逆二聚FKBP。

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