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Kinase Screening and Profiling

Overview of attention for book
Kinase Screening and Profiling
Humana Press

Table of Contents

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    Book Overview
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    Chapter 1 HTRF Kinase Assay Development and Methods in Inhibitor Characterization
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    Chapter 2 Application of Eukaryotic Elongation Factor-2 Kinase (eEF-2K) for Cancer Therapy: Expression, Purification, and High-Throughput Inhibitor Screening
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    Chapter 3 Recombinant Kinase Production and Fragment Screening by NMR Spectroscopy.
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    Chapter 4 Bioluminescence Methods for Assaying Kinases in Quantitative High-Throughput Screening (qHTS) Format Applied to Yes1 Tyrosine Kinase, Glucokinase, and PI5P4Kα Lipid Kinase
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    Chapter 5 Using Bioluminescent Kinase Profiling Strips to Identify Kinase Inhibitor Selectivity and Promiscuity
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    Chapter 6 Measuring Activity of Phosphoinositide Lipid Kinases Using a Bioluminescent ADP-Detecting Assay.
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    Chapter 7 A High-Throughput Radiometric Kinase Assay
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    Chapter 8 A High-Content Assay to Screen for Modulators of EGFR Function
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    Chapter 9 Monitoring Protein Kinase Expression and Phosphorylation in Cell Lysates with Antibody Microarrays
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    Chapter 10 From Enzyme to Whole Blood: Sequential Screening Procedure for Identification and Evaluation of p38 MAPK Inhibitors.
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    Chapter 11 Genetically Encoded Fluorescent Indicators to Visualize Protein Phosphorylation in Living Cells
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    Chapter 12 Characterization of an Engineered Src Kinase to Study Src Signaling and Biology
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    Chapter 13 Screening One-Bead-One-Compound Peptide Libraries for Optimal Kinase Substrates
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    Chapter 14 Determination of the Substrate Specificity of Protein Kinases with Peptide Micro- and Macroarrays
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    Chapter 15 Rapid Identification of Protein Kinase Phosphorylation Site Motifs Using Combinatorial Peptide Libraries
Attention for Chapter 12: Characterization of an Engineered Src Kinase to Study Src Signaling and Biology
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Chapter title
Characterization of an Engineered Src Kinase to Study Src Signaling and Biology
Chapter number 12
Book title
Kinase Screening and Profiling
Published in
Methods in molecular biology, January 2016
DOI 10.1007/978-1-4939-3073-9_12
Pubmed ID
Book ISBNs
978-1-4939-3072-2, 978-1-4939-3073-9
Authors

Leanna R. Gentry, Andrei V. Karginov, Klaus M. Hahn, Channing J. Der

Abstract

Pharmacologic inhibitors of protein kinases comprise the vast majority of approved signal transduction inhibitors for cancer treatment. An important facet of their clinical development is the identification of the key substrates critical for their driver role in cancer. One approach for substrate identification involves evaluating the phosphorylation events associated with stable expression of an activated protein kinase. Another involves genetic or pharmacologic inhibition of protein kinase expression or activity. However, both approaches are limited by the dynamic nature of signaling, complicating whether phosphorylation changes are primary or secondary activities of kinase function. We have developed rapamycin-regulated (RapR) protein kinases as molecular tools that allow for the study of spatiotemporal regulation of signaling. Here we describe the application of this technology to the Src tyrosine kinase and oncoprotein (RapR-Src). We describe how to achieve stable expression of this tool in cell lines and how to subsequently activate the tool and determine its function in signaling and morphology.

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Mendeley readers

Mendeley readers

The data shown below were compiled from readership statistics for 11 Mendeley readers of this research output. Click here to see the associated Mendeley record.

Geographical breakdown

Country Count As %
Canada 1 9%
Unknown 10 91%

Demographic breakdown

Readers by professional status Count As %
Other 3 27%
Professor > Associate Professor 2 18%
Researcher 2 18%
Student > Bachelor 1 9%
Student > Ph. D. Student 1 9%
Other 0 0%
Unknown 2 18%
Readers by discipline Count As %
Biochemistry, Genetics and Molecular Biology 3 27%
Medicine and Dentistry 3 27%
Agricultural and Biological Sciences 2 18%
Unknown 3 27%