Phosphoserine/threonine binding domains: molecular integrators of protein kinase signaling in cell cycle control and cancer

Yaffe, Michael

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Introduction
pSer/pThr binding domains in cell signaling
Protein phosphorylation
Historical perspective on tyrosine kinase signaling
SH2 domains bind ligands via pTyr and pTyr+3
The human kinome
Ser and Thr kinases differ from Tyr kinases
The new 'dogma' of signal transduction
The concept
14-3-3 proteins are pSer/pThr-binding proteins
Identifying new phospho-binding domains
Recognizing overlapping consensus motifs
The biology supports the biochemistry
Architecture of polo-like kinases
Structural basis for phospho-dependent binding
Residues interacting with the phospho-peptide
What does the Polo-box domain do in cells?
The PBD targets Plk1 to mitotic substrates
In the absence of a ligand, PBD inhibits Plk2
Synergy between Cdk activity and the Plk1 PBD
Identifying new pSer/pThr-binding domains (1)
The DNA damage response pathway
"High-throughput" analysis
Screening 96,000 proteins
Pax2-transactivation domain interacting protein
The BRCT domains
A subset of tandem BRCT domains
pS+3 position- based phosphopeptides selection
Basis for tandem BRCT-phosphopeptide binding
Ser-1655 and Lys-1702 mediate interactions
Cancer-associated mutations in BRCA1 BRCT
Eliminating phosphopeptide binding function
ATM amplification involves H2AX phosphorylation
The phosphorylated C-terminus of H2AX
BRCT domains are 'tuned' to bind to gamma H2AX
Structural basis for MDC1 BRCT: H2AX binding
Mutants cause loss of MDC1 foci after IR
Identifying new pSer/pThr-binding domains (2)
Proteins that contain pSer/pThr binding domains
Coordination of mitotic signaling complexes
Evolutionary difference
pSer/pThr binding domains control cell cycle
Conclusions
Acknowledgements

Topics Covered

Protein phosphorylation
Historical perspective on signaling by tyrosine kinases
The human kinome
How can phosphorylation control enzyme activity
The new 'dogma' of signal transduction by serine/threonine kinases
New phospho-binding domains
Polo family kinases together with cyclin-dependent kinases play many roles throughout mitosis
Architecture of polo-like kinases
Structural basis for phospho-dependent binding
What does the polo-box domain do in cells
A proteomic approach to identifying new phospho-Ser/Thr-binding domains
The DNA damage response pathway
BRCA1
Cancer associated mutations

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Chemical Biology

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Oncology

Talk Citation

Yaffe, M. (2008, August 14). Phosphoserine/threonine binding domains: molecular integrators of protein kinase signaling in cell cycle control and cancer [Video file]. In The Biomedical & Life Sciences Collection, Henry Stewart Talks. Retrieved April 19, 2024, from https://hstalks.com/bs/941/.
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Publication History

Published on August 14, 2008

Financial Disclosures

Dr. Michael Yaffe has not informed HSTalks of any commercial/financial relationship that it is appropriate to disclose.

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Phosphoserine/threonine binding domains: molecular integrators of protein kinase signaling in cell cycle control and cancer

Dr. Michael Yaffe – Massachusetts Institute of Technology, USA

Published on August 14, 2008 86 min

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Transcript

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0:00

Hello. I'm Michael Yaffe from the MIT Center for Cancer Research and the Departments of Biology and Biological Engineering. And the title of my talk is "Phosphoserine and Phosphothreonine Binding Domains Molecular Integrators of Protein Kinase Signaling in Cell Cycle Control and Cancer".

0:18

What I'd like to tell you about is how phosphoserine and phosphothreonine binding domains are involved in orchestrating cells signaling with a particular focus on cell cycle control and the response to cells to DNA damage. It's well established that in response to various types of stimuli, such as growth factor stimulation or DNA damage, protein kinase has become activated in cells and phosphorylate, a subset of proteins within the cell and these phosphorylated substrates then are believed to be responsible for many of the molecular effects that follow after the initial stimulus. Some of these molecular effects include things like cell cycle checkpoints, DNA damage repair, or the decision of a cell to undergo apoptosis or withdraw from the cell cycle and senensence. There is also integration of the cell cycle and the DNA damage checkpoint pathways so that it appears not only due to cell cycle checkpoints inactivate progression through the cell cycle, but progression through the cell cycle may be required in order to activate DNA damage checkpoints. The unique aspect of our approach to this problem has been making the claim that phosphorylation of substrates by protein kinases alone may not be enough to elicit the particular molecular effects that are observed. Instead, it appears to be the interaction of the phosphorylated substrates with specific phosphoserine, phosphothreonine or phosphotyrosine-binding domains that coordinates the action of the protein kinase with the molecular effect that we observe. Therefore, it becomes important for us to not only identify the phosphopeptide-binding domains and their substrates, but to also use systems biology approaches to understand the activation of different protein kinases as a function of time, in order to understand how signalling networks are coordinated in time and space. It's well established that protein phosphorylation

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Phosphoserine/threonine binding domains: molecular integrators of protein kinase signaling in cell cycle control and cancer

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Phosphoserine/threonine binding domains: molecular integrators of protein kinase signaling in cell cycle control and cancer

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Phosphoserine/threonine binding domains: molecular integrators of protein kinase signaling in cell cycle control and cancer