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A three-hybrid system for detecting small ligand-protein receptor interactions.一种用于检测小分子配体-蛋白质受体相互作用的三杂交系统。
Proc Natl Acad Sci U S A. 1996 Nov 12;93(23):12817-21. doi: 10.1073/pnas.93.23.12817.
2
A novel FK506 binding protein can mediate the immunosuppressive effects of FK506 and is associated with the cardiac ryanodine receptor.一种新型FK506结合蛋白可介导FK506的免疫抑制作用,并与心肌兰尼碱受体相关。
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3
Identification of an 11-kDa FKBP12-rapamycin-binding domain within the 289-kDa FKBP12-rapamycin-associated protein and characterization of a critical serine residue.在289 kDa FKBP12-雷帕霉素相关蛋白中鉴定出一个11 kDa FKBP12-雷帕霉素结合结构域并对一个关键丝氨酸残基进行表征。
Proc Natl Acad Sci U S A. 1995 May 23;92(11):4947-51. doi: 10.1073/pnas.92.11.4947.
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A GAL4-based yeast three-hybrid system for the identification of small molecule-target protein interactions.一种基于GAL4的酵母三杂交系统,用于鉴定小分子-靶蛋白相互作用。
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FAP48, a new protein that forms specific complexes with both immunophilins FKBP59 and FKBP12. Prevention by the immunosuppressant drugs FK506 and rapamycin.FAP48是一种新蛋白,它能与免疫亲和素FKBP59和FKBP12形成特定复合物。免疫抑制剂FK506和雷帕霉素可起到预防作用。
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A chimeric thyroid hormone receptor constitutively bound to DNA requires retinoid X receptor for hormone-dependent transcriptional activation in yeast.一种与DNA组成型结合的嵌合甲状腺激素受体在酵母中进行激素依赖性转录激活需要视黄酸X受体。
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Stabilization in vitro of the untransformed glucocorticoid receptor complex of S49 lymphocytes by the immunophilin ligand FK506.免疫亲和素配体FK506对S49淋巴细胞未转化糖皮质激素受体复合物的体外稳定作用。
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Only in the presence of immunophilins can cyclosporin and FK506 disrupt in vivo binding of calcineurin A to its autoinhibitory domain yet strengthen interaction between calcineurin A and B subunits.只有在免疫亲和素存在的情况下,环孢素和FK506才能在体内破坏钙调神经磷酸酶A与其自身抑制域的结合,但同时增强钙调神经磷酸酶A与B亚基之间的相互作用。
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Dimeric ligands define a role for transcriptional activation domains in reinitiation.二聚体配体确定了转录激活结构域在重新起始中的作用。
Nature. 1996 Aug 29;382(6594):822-6. doi: 10.1038/382822a0.
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Targets of immunophilin-immunosuppressant complexes are distinct highly conserved regions of calcineurin A.免疫亲和素-免疫抑制剂复合物的作用靶点是钙调神经磷酸酶A的不同高度保守区域。
EMBO J. 1995 Jun 15;14(12):2772-83. doi: 10.1002/j.1460-2075.1995.tb07277.x.

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Mechanistic studies of a signaling pathway activated by the organic dimerizer FK1012.由有机二聚体FK1012激活的信号通路的机制研究。
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Cdi1, a human G1 and S phase protein phosphatase that associates with Cdk2.Cdi1,一种与Cdk2相关的人类G1期和S期蛋白磷酸酶。
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一种用于检测小分子配体-蛋白质受体相互作用的三杂交系统。

A three-hybrid system for detecting small ligand-protein receptor interactions.

作者信息

Licitra E J, Liu J O

机构信息

Center for Cancer Research, Massachusetts Institute of Technology, Cambridge 02139, USA.

出版信息

Proc Natl Acad Sci U S A. 1996 Nov 12;93(23):12817-21. doi: 10.1073/pnas.93.23.12817.

DOI:10.1073/pnas.93.23.12817
PMID:8917502
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC24003/
Abstract

Small ligand-receptor interactions underlie many fundamental processes in biology and form the basis for pharmacological intervention of human diseases in medicine. We report herein a genetic system, named the yeast three-hybrid system, for detecting ligand-receptor interactions in vivo. This system is adapted from the yeast two-hybrid system with which a third synthetic hybrid ligand is combined. The feasibility of this system was demonstrated using as the hybrid ligand a heterodimer of covalently linked dexamethasone and FK506. Yeast expressing fusion proteins of the hormone binding domain of the rat glucocorticoid receptor fused to the LexA DNA-binding domain and FKBP12 fused to a transcriptional activation domain activated reporter genes when plated on medium containing the dexamethasone-FK506 heterodimer. The reporter gene activation is completely abrogated in a competitive manner by the presence of excess FK506. Using this system, we screened a Jurkat cDNA library fused to the transcriptional activation domain in yeast expressing the hormone binding domain of rat glucocorticoid receptor-LexA DNA binding domain fusion protein in the presence of dexamethasone-FK506 heterodimer. We isolated overlapping clones of human FKBP12. These results demonstrate that the three-hybrid system can be used to discover receptors for small ligands and to screen for new ligands to known receptors.

摘要

小分子配体 - 受体相互作用是生物学中许多基本过程的基础,也是医学上人类疾病药物干预的基础。我们在此报告一种用于在体内检测配体 - 受体相互作用的遗传系统,名为酵母三杂交系统。该系统是在酵母双杂交系统的基础上改编而来,加入了第三个合成杂交配体。使用共价连接的地塞米松和FK506异二聚体作为杂交配体,证明了该系统的可行性。当将表达与LexA DNA结合结构域融合的大鼠糖皮质激素受体激素结合结构域的融合蛋白和与转录激活结构域融合的FKBP12的酵母接种在含有地塞米松 - FK506异二聚体的培养基上时,报告基因被激活。过量FK506的存在以竞争方式完全消除了报告基因的激活。使用该系统,我们在存在地塞米松 - FK506异二聚体的情况下,筛选了与表达大鼠糖皮质激素受体 - LexA DNA结合结构域融合蛋白的激素结合结构域的酵母中的转录激活结构域融合的Jurkat cDNA文库。我们分离出了人FKBP12的重叠克隆。这些结果表明,三杂交系统可用于发现小分子配体的受体,并筛选已知受体的新配体。