FKBP12 physically and functionally interacts with aspartokinase in Saccharomyces cerevisiae

被引：33

作者：

Alarcon, CM

Heitman, J

机构：

[1] DUKE UNIV, MED CTR, DEPT GENET, DURHAM, NC 27710 USA

[2] DUKE UNIV, MED CTR, DEPT PHARMACOL, DURHAM, NC 27710 USA

[3] DUKE UNIV, MED CTR, HOWARD HUGHES MED INST, DURHAM, NC 27710 USA

来源：

MOLECULAR AND CELLULAR BIOLOGY | 1997年 / 17卷 / 10期

关键词：

D O I：

10.1128/MCB.17.10.5968

中图分类号：

Q5 [生物化学]; Q7 [分子生物学];

学科分类号：

071010 ; 081704 ;

摘要：

The peptidyl-prolyl isomerase FKBP12 was originally identified as the intracellular receptor for the immunosuppressive drugs FK506 (tacrolimus) and rapamycin (sirolimus). Although peptidyl-prolyl isomerases have been implicated in catalyzing protein folding, the cellular functions of FKBP12 in Saccharomyces cerevisiae and other organisms are largely unknown. Using the yeast two-h,brid system, we identified aspartokinase, an enzyme that catalyzes an intermediate step in threonine and methionine biosynthesis, as an in vivo binding target of FKBP12. Aspartokinase also binds FKBP12 in vitro, and drugs that bind the FKBP12 active site, or mutations in FKBP12 surface and active site residues, disrupt the FKBP12-aspartokinase complex in vivo and in vitro. fpr1 mutants lacking FKBP12 are viable, are not threonine or methionine auxotrophs, and express wild-type levels of aspartokinase protein and activity; thus, FKBP12 is not essential for aspartokinase activity. The activity of aspartokinase is regulated by feedback inhibition by product, and genetic analyses reveal that FKBP12 is important for this feedback inhibition, possibly by catalyzing aspartokinase conformational changes in response to product binding.

引用

页码：5968 / 5975

页数：8

共 60 条

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