Small Molecule Gated Split-Tyrosine Phosphatases and Orthogonal Split-Tyrosine Kinases

被引：19

作者：

Camacho-Soto, Karla ^{[1
]}

Castillo-Montoya, Javier ^{[1
]}

Tye, Blake ^{[1
]}

Ogunleye, Luca O. ^{[1
]}

Ghosh, Indraneel ^{[1
]}

机构：

[1] Univ Arizona, Dept Chem & Biochem, Tucson, AZ 85721 USA

来源：

JOURNAL OF THE AMERICAN CHEMICAL SOCIETY | 2014年 / 136卷 / 49期

关键词：

PROTEIN-PROTEIN INTERACTIONS; FRAGMENT COMPLEMENTATION ASSAYS; AFFINITY-BASED PROBES; LIVING CELLS; SIGNAL-TRANSDUCTION; DRUG DISCOVERY; IN-VIVO; BIVALENT INHIBITORS; HUMAN GENOME; SPECIFICITY;

D O I：

10.1021/ja5080745

中图分类号：

O6 [化学];

学科分类号：

0703 ;

摘要：

Protein kinases phosphorylate client proteins, while protein phosphatases catalyze their dephosphorylation and thereby in concert exert reversible control over numerous signal transduction pathways. We have recently reported the design and validation of split-protein kinases that can be conditionally activated by an added small molecule chemical inducer of dimerization (CID), rapamycin. Herein, we provide the rational design and validation of three split-tyrosine phosphatases (PTPs) attached to FKBP and FRB, where catalytic activity can be modulated with rapamycin. We further demonstrate that the orthogonal CIDs, abscisic acid and gibberellic acid, can be used to impart control over the activity of split-tyrosine kinases (PTKs). Finally, we demonstrate that designed split-phosphatases and split-kinases can be activated by orthogonal CIDs in mammalian cells. In sum, we provide a methodology that allows for post-translational orthogonal small molecule control over the activity of user defined split-PTKs and split-PTPs. This methodology has the long-term potential for both interrogating and redesigning phosphorylation dependent signaling pathways.

引用

页码：17078 / 17086

页数：9

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