Phage-peptide display identifies the interferon-responsive, death-activated protein kinase family as a novel modifier of MDM2 and p21WAF1.

Burch LR; Scott M; Pohler E; Meek D; Hupp T

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Phage-peptide display identifies the interferon-responsive, death-activated protein kinase family as a novel modifier of MDM2 and p21WAF1.

机译：噬菌体肽展示将干扰素应答，死亡激活的蛋白激酶家族鉴定为MDM2和p21WAF1的新型修饰剂。

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Phage-peptide display is a versatile tool for identifying novel protein-protein interfaces. Our previous work highlighted the selection of phage-peptides that bind to specific isoforms of MDM2 protein and in this work we subjected the putative MDM2-binding proteins to phage-peptide display to expand further on putative protein interaction maps. One peptide that bound MDM2 had significant homology to members of the death-activated protein kinase (DAPK) family, an enzyme family of no known direct link to the p53 pathway. We examined whether a nuclear member of the DAPK family named DAPK3 or ZIP kinase had direct links to the p53 pathway. ZIP kinase was cloned, purified, and the enzyme was able to phosphorylate MDM2 at Ser166, a site previously reported to be modified by Akt kinase, thus demonstrating that ZIP kinase is a bona fide MDM2-binding protein. Native ZIP kinase fractions were then subjected to phage-peptide display and one ZIP kinase consensus peptide motif was identified in p21(WAF1). ZIP kinase phosphorylates p21(WAF1) at Thr145 and alanine-substituted mutations in the p21(WAF1) phosphorylation site alter its ability to be phosphorylated by ZIP kinase. Thus, although ZIP kinase consensus sites were then defined as containing a minimal RKKx(T/S) consensus motif, alternate contacts in ZIP kinase binding are implicated, since amino acid residues surrounding the phospho-acceptor site can effect the specific activity of the kinase. Transfected ZIPK can promote the phosphorylation of p21(WAF1) at Thr145 in vivo and can increase the half-life of p21(WAF1), while the half-life of p21(WAF1[T145A]) is not effected by ZIP kinase. Thus, phage-peptide display identified an interferon-responsive protein kinase family as a novel modifier of two components of the p53 pathway, MDM2 and p21(WAF1), and underscores the utility of phage-peptide display for gaining novel insights into biochemical pathways.

机译：噬菌体肽展示是鉴定新型蛋白质-蛋白质界面的多功能工具。我们以前的工作重点是选择与MDM2蛋白的特定同工型结合的噬菌体肽，在这项工作中，我们对假定的MDM2结合蛋白进行了噬菌体肽展示，以在假定的蛋白相互作用图上进一步扩展。结合MDM2的一种肽与死亡激活蛋白激酶（DAPK）家族的成员具有显着同源性，该家族是一种未知的直接连接至p53途径的酶家族。我们检查了DAPK家族的核心成员DAPK3或ZIP激酶是否与p53途径有直接联系。 ZIP激酶被克隆，纯化，并且该酶能够在Ser166磷酸化MDM2，Ser166是先前报道过被Akt激酶修饰的位点，因此证明ZIP激酶是真正的MDM2结合蛋白。然后对天然ZIP激酶馏分进行噬菌体肽展示，并在p21（WAF1）中鉴定出一个ZIP激酶共有肽基序。 ZIP激酶在Thr145处磷酸化p21（WAF1），而p21（WAF1）磷酸化位点的丙氨酸取代突变会改变其被ZIP激酶磷酸化的能力。因此，尽管随后将ZIP激酶共有位点定义为包含最小的RKKx（T / S）共有基序，但由于在磷酸受体位点周围的氨基酸残基可影响该激酶的比活性，因此涉及ZIP激酶结合中的其他接触。转染的ZIPK可以在体内促进Thr145上p21（WAF1）的磷酸化，并可以延长p21（WAF1）的半衰期，而p21（WAF1 [T145A]）的半衰期不受ZIP激酶的影响。因此，噬菌体肽展示将干扰素反应性蛋白激酶家族鉴定为p53途径两个成分MDM2和p21（WAF1）的新型修饰物，并强调了噬菌体肽展示在获取生化途径方面的新颖见解的实用性。

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《Journal of Molecular Biology》 |2004年第1期|共14页
作者
Burch LR; Scott M; Pohler E; Meek D; Hupp T;
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正文语种 eng
中图分类基础医学;
关键词
ZIP kinase; Peptides; Bacteriophages; oncoprotein p21; Family; 肽类; 噬菌体; 家庭;

机译：ZIP kinase;Peptides;Bacteriophages;oncoprotein p21;Family;肽类;噬菌体;家庭;

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1. Phage-peptide display identifies the interferon-responsive, death-activated protein kinase family as a novel modifier of MDM2 and p21WAF1. [J] . Burch LR, Scott M, Pohler E, Journal of Molecular Biology . 2004,第1期

机译：噬菌体肽展示将干扰素应答，死亡激活的蛋白激酶家族鉴定为MDM2和p21WAF1的新型修饰剂。
2. Functional study of a novel interferon-responsive gene, GRAMD1B, identified in multiplex MS families [J] . Osiceanu A. M., Esposito F., Zauli A., The FEBS journal . 2014,第Suppla1期

机译：在多重MS家族中鉴定的新型干扰素应答基因GRAMD1B的功能研究
3. AN UNUSUAL PROTEIN KINASE DISPLAYING CHARACTERISTICS OF BOTH THE SERINE/THREONINE AND TYROSINE FAMILIES IS ENCODED BY THE ARABIDOPSIS THALIANA GENE ATN1 [J] . Tregear JW., Schwebeldugue N., Kreis M., Plant Science . 1996,第1a2期

机译：拟南芥基因ATN1编码丝氨酸/苏氨酸和酪氨酸家族的异常蛋白激酶表现特征
4. Identification of Calcium-dependent Protein Kinase (CDPK): a Multi-functional Gene Family in Rafflesia cantleyi [C] . Safoora Amini, Hoe-Han Goh, Kiew-Lian Wan UKM FST Postgraduate Colloquium . 2016

机译：依赖钙依赖性蛋白激酶（CDPK）：Rafflesia Cantleyi的多功能基因家族
5. Screening lytic phage display libraries for proteins which interact withcAMP-dependent protein kinase regulatory subunit type I-alpha. [D] . Bianco, Robert A. 2002

机译：筛选裂解噬菌体展示文库中与cAMP依赖性蛋白激酶调节亚基I-alpha相互作用的蛋白。
6. Phage display identifies thioredoxin and superoxide dismutase as novel protein kinase C-interacting proteins: thioredoxin inhibits protein kinase C-mediated phosphorylation of histone. [O] . J A Watson, M G Rumsby, R G Wolowacz 1999

机译：噬菌体展示将硫氧还蛋白和超氧化物歧化酶鉴定为新型蛋白激酶C相互作用蛋白：硫氧还蛋白抑制蛋白激酶C介导的组蛋白磷酸化。
7. Phage display identifies thioredoxin and superoxide dismutase as novel protein kinase C-interacting proteins: thioredoxin inhibits protein kinase C-mediated phosphorylation of histone. [O] . Watson, J A, Rumsby, M G, Wolowacz, R G 1999

机译：噬菌体展示将硫氧还蛋白和超氧化物歧化酶鉴定为新型蛋白激酶C相互作用蛋白：硫氧还蛋白抑制蛋白激酶C介导的组蛋白磷酸化。

Phage-peptide display identifies the interferon-responsive, death-activated protein kinase family as a novel modifier of MDM2 and p21WAF1.

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