A peptide library approach identifies a specific inhibitor for the ZAP-70 protein tyrosine kinase

Kiyotaka Nishikawa; Sansana Sawasdikosol; David A. Fruman; Jack Lai; Zhou Songyang; Steven J. Burakoff; Michael B. Yaffe; Lewis C. Cantley

doi:10.1016/S1097-2765(05)00085-7

A peptide library approach identifies a specific inhibitor for the ZAP-70 protein tyrosine kinase

Kiyotaka Nishikawa, Sansana Sawasdikosol, David A. Fruman, Jack Lai, Zhou Songyang, Steven J. Burakoff, Michael B. Yaffe, Lewis C. Cantley

Research output: Contribution to journal › Article › peer-review

9 Scopus citations

Abstract

We utilized a novel peptide library approach to identify specific inhibitors of ZAP-70, a protein Tyr kinase involved in T cell activation. By screening more than 6 billion peptides oriented by a common Tyr residue for their ability to bind to ZAP-70, we determined a consensus optimal peptide. A Phe-for-Tyr substituted version of the peptide inhibited ZAP-70 protein Tyr kinase activity by competing with protein substrates (K(I) of 2 μM). The related protein Tyr kinases, Lck and Syk, were not significantly inhibited by the peptide. When introduced into intact T cells, the peptide blocked signaling downstream of ZAP-70, including ZAP-70-dependent gene induction, without affecting upstream Tyr phosphorylation. Thus, screening Tyr-oriented peptide libraries can identify selective peptide inhibitors of protein Tyr kinases.

Original language	English
Pages (from-to)	969-974
Number of pages	6
Journal	Molecular Cell
Volume	6
Issue number	4
DOIs	https://doi.org/10.1016/S1097-2765(05)00085-7
State	Published - 2000
Externally published	Yes

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@article{225b1c4faa674efcbbe1c48985dcc62a,

title = "A peptide library approach identifies a specific inhibitor for the ZAP-70 protein tyrosine kinase",

abstract = "We utilized a novel peptide library approach to identify specific inhibitors of ZAP-70, a protein Tyr kinase involved in T cell activation. By screening more than 6 billion peptides oriented by a common Tyr residue for their ability to bind to ZAP-70, we determined a consensus optimal peptide. A Phe-for-Tyr substituted version of the peptide inhibited ZAP-70 protein Tyr kinase activity by competing with protein substrates (K(I) of 2 μM). The related protein Tyr kinases, Lck and Syk, were not significantly inhibited by the peptide. When introduced into intact T cells, the peptide blocked signaling downstream of ZAP-70, including ZAP-70-dependent gene induction, without affecting upstream Tyr phosphorylation. Thus, screening Tyr-oriented peptide libraries can identify selective peptide inhibitors of protein Tyr kinases.",

author = "Kiyotaka Nishikawa and Sansana Sawasdikosol and Fruman, {David A.} and Jack Lai and Zhou Songyang and Burakoff, {Steven J.} and Yaffe, {Michael B.} and Cantley, {Lewis C.}",

note = "Funding Information: We thank Michael Berne (Tufts University) for peptide synthesis and sequencing. This reseach was supported by NIH grant GM56203 to L. C. C. and AI7258 to S. J. B.",

year = "2000",

doi = "10.1016/S1097-2765(05)00085-7",

language = "English",

volume = "6",

pages = "969--974",

journal = "Molecular Cell",

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number = "4",

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T1 - A peptide library approach identifies a specific inhibitor for the ZAP-70 protein tyrosine kinase

AU - Nishikawa, Kiyotaka

AU - Sawasdikosol, Sansana

AU - Fruman, David A.

AU - Lai, Jack

AU - Songyang, Zhou

AU - Burakoff, Steven J.

AU - Yaffe, Michael B.

AU - Cantley, Lewis C.

N1 - Funding Information: We thank Michael Berne (Tufts University) for peptide synthesis and sequencing. This reseach was supported by NIH grant GM56203 to L. C. C. and AI7258 to S. J. B.

PY - 2000

Y1 - 2000

N2 - We utilized a novel peptide library approach to identify specific inhibitors of ZAP-70, a protein Tyr kinase involved in T cell activation. By screening more than 6 billion peptides oriented by a common Tyr residue for their ability to bind to ZAP-70, we determined a consensus optimal peptide. A Phe-for-Tyr substituted version of the peptide inhibited ZAP-70 protein Tyr kinase activity by competing with protein substrates (K(I) of 2 μM). The related protein Tyr kinases, Lck and Syk, were not significantly inhibited by the peptide. When introduced into intact T cells, the peptide blocked signaling downstream of ZAP-70, including ZAP-70-dependent gene induction, without affecting upstream Tyr phosphorylation. Thus, screening Tyr-oriented peptide libraries can identify selective peptide inhibitors of protein Tyr kinases.

AB - We utilized a novel peptide library approach to identify specific inhibitors of ZAP-70, a protein Tyr kinase involved in T cell activation. By screening more than 6 billion peptides oriented by a common Tyr residue for their ability to bind to ZAP-70, we determined a consensus optimal peptide. A Phe-for-Tyr substituted version of the peptide inhibited ZAP-70 protein Tyr kinase activity by competing with protein substrates (K(I) of 2 μM). The related protein Tyr kinases, Lck and Syk, were not significantly inhibited by the peptide. When introduced into intact T cells, the peptide blocked signaling downstream of ZAP-70, including ZAP-70-dependent gene induction, without affecting upstream Tyr phosphorylation. Thus, screening Tyr-oriented peptide libraries can identify selective peptide inhibitors of protein Tyr kinases.

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U2 - 10.1016/S1097-2765(05)00085-7

DO - 10.1016/S1097-2765(05)00085-7

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AN - SCOPUS:0033636260

SN - 1097-2765

VL - 6

SP - 969

EP - 974

JO - Molecular Cell

JF - Molecular Cell

IS - 4

ER -

A peptide library approach identifies a specific inhibitor for the ZAP-70 protein tyrosine kinase

Abstract

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