The regulation of MAP kinase signalling by dual-specificity protein phosphatases

Keyse, Steve M.

We noted you are experiencing viewing problems

Check with your IT department that JWPlatform, JWPlayer and Amazon AWS & CloudFront are not being blocked by your network. The relevant domains are *.jwplatform.com, *.jwpsrv.com, *.jwpcdn.com, jwpltx.com, jwpsrv.a.ssl.fastly.net, *.amazonaws.com and *.cloudfront.net. The relevant ports are 80 and 443.
Check the following talk links to see which ones work correctly:
Auto Mode
HTTP Progressive Download Send us your results from the above test links at access@hstalks.com and we will contact you with further advice on troubleshooting your viewing problems.
No luck yet? More tips for troubleshooting viewing issues
Contact HST Support access@hstalks.com

Please review our troubleshooting guide for tips and advice on resolving your viewing problems.
For additional help, please don't hesitate to contact HST support access@hstalks.com

We hope you have enjoyed this limited-length demo

Request free trial
Recommend to your librarian

Share
Share This Lecture
Messaging

Outlook

Gmail

Yahoo!

WhatsApp
Social

Facebook

X

LinkedIn

VKontakte
Permalink
Replay Talk

This is a limited length demo talk; you may login or review methods of obtaining more access.

Slides
Topics
Links
Citation

Printable Handouts

PDF

Navigable Slide Index

Introduction
MAPK/SAPK cascades in mammalian cells
Duration, strength of p-ERK determine cell fate
The activation and inactivation of MAP kinases
MKPs share basic structural features
The MAP-kinase phosphatases families
DUSP6/MKP-3: key properties
MKP-3 catalytic activation on binding to ERK2
MKP catalytic activity requires a general acid
Acid loop displaced in the absence of substrate
MKP-3 is expressed in FGF sites
Removal of AER abrogates MKP-3 expression
Inhibition of FGF or MEK1/2 abolishes MKP-3
How do FGF induce DUSP6/MKP-3 expression?
Inhibition of MAPK suppresses MKP-3 by FGFs
Deletion analysis of the MKP-3 gene promoter
In silico analysis of the DUSP6/MKP-3 promoter
Mutated Ets abolishes the FGF response
Ets1 and Ets2 bind to MKP-3 gene promoter
Murine MKP-3 promoter directs expression of GFP
DUSP6/MKP-3 summary
The dual-specificity MAPK phosphatase family
MKP-1 inactivates ERK, p38-alpha and JNK
DUSP1/MKP-1 are inducible by UV-radiation
MKP-1 is abolished in p38-alpha knockout mice
MKP-1 unaffected by loss of p38-alpha or JNK
UV induction of MKP-1 is rescued by p38-alpha
p38-alpha is essential for induction of MKP-1
UV induction of MKP-1 mediated by MSK 1/2
MKP-1 promoter activity, p38, MSK 1/2 and CREB
Deletion of MKP-1 increases ERK, p38 and JNK
Cells lacking MKP-1 are acutely sensitive to UV
Cell death when lacking MKP-1 isn't due to p38
MKP-1(-) cell death rescued by MKP-1 mutant
JNK1/2(-) cells not sensitised to UV
Cross-talk between p38-alpha and JNK pathways
Concluding remarks
Acknowledgements

Topics Covered

Signal transduction
Mechanisms of MAP kinase inactivation
Dual-specificity MAP kinase phosphatases
Fibroblast growth factor signalling

Links

Series:

Protein Phosphorylation

Categories:

Biochemistry

Talk Citation

Keyse, S.M. (2011, March 16). The regulation of MAP kinase signalling by dual-specificity protein phosphatases [Video file]. In The Biomedical & Life Sciences Collection, Henry Stewart Talks. Retrieved April 24, 2024, from https://hstalks.com/bs/1973/.
Export Citation (RIS)

Publication History

Published on March 16, 2011

Financial Disclosures

Prof. Steve M. Keyse has not informed HSTalks of any commercial/financial relationship that it is appropriate to disclose.

Embed in course/own notesEmbed Lecture

The regulation of MAP kinase signalling by dual-specificity protein phosphatases

Prof. Steve M. Keyse – University of Dundee, UK

Published on March 16, 2011 49 min

Review
Share
Share This Talk
Messaging

Outlook

Gmail

Yahoo!

WhatsApp
Social

Facebook

X

LinkedIn

VKontakte
Permalink
Add to

A selection of talks on Biochemistry

45 min

Prof. George Chaconas
University of Calgary, Canada

34 min

Dr. Monika Winter
Northumbria University, UK

26 min

Dr. Mel Bedi
Wayne State University, USA

24 min

Prof. Henry Jay Forman
University of California, Merced, USA

34 min

Prof. Demet Araç
The University of Chicago, USA

48 min

Prof. Emeritus Richard R. Burgess
University of Wisconsin-Madison, USA

49 min

Dr. Stephen R. Hammes
University of Rochester Medical Center, USA

39 min

Prof. Juliet Gerrard
University of Auckland, New Zealand

37 min

Dr. Francisco R. M. Laurindo
University of São Paulo School of Medicine, Brazil

22 min

Dr. Kathleen Knights
Flinders University, Australia

45 min

Dr. Christine Beedham
Department of Clinical Sciences, University of Bradford, UK

31 min

Dr. Daniel Wacker
Icahn School of Medicine at Mount Sinai, USA

40 min

Prof. Antonio Baici
University of Zurich, Switzerland

33 min

Prof. José Cuezva
Universidad Autónoma de Madrid, Spain

40 min

Prof. Monika Fuxreiter
University of Debrecen, Hungary

36 min

Prof. Keith Willison
Imperial College London, UK

Transcript

Please wait while the transcript is being prepared...

0:00

Hi, my name's Steve Keyse, and I'm based at the University of Dundee in Scotland; And the subject of my talk today, is "The Regulation of Mitogen-activated Protein Kinase Signalling by Dual-Specificity Protein Phosphatases.

0:15

This next slide shows an overview, the mitogen and stress-activated protein kinase signalling cascades in mammalian cells. These highly conserve signal transduction pathways, serve to respond to a series of environmental cues which range from growth factors and hormones, through to cellular stresses such as pro-inflammatory cytokines and DNA damaging agents, and elicit a wide variety of physiological responses in cells, which range from increases in the rate of cell growth or cell differentiation, changes in morphology and motility, mediation of inflammatory responses, cell cycle arrest, and even cell death. These pathways are divided into three major families: the so-called classical Ras-MAP kinase pathway which is largely responsible for the response to growth factors and hormones, and is thought primarily to influence cell growth, differentiation and survival. There are two so-called stress-activated MAP kinase pathways exemplified by the c-Jun amino-terminal kinases or JNKs, and the p38 MAP kinases, which respond primarily to cellular stress and pro-inflammatory cytokines, and are thought to be responsible for exit from the cell cycle, and responses to damage such as cell death.

Show

Hide

Share
Share This Talk
Messaging

Outlook

Gmail

Yahoo!

WhatsApp
Social

Facebook

X

LinkedIn

VKontakte
Permalink
More actions

The regulation of MAP kinase signalling by dual-specificity protein phosphatases

Embed in course/own notes

See Options

Login via your organisation

We noted you are experiencing viewing problems

We hope you have enjoyed this limited-length demo

Share This Lecture

Messaging

Social

Permalink

Printable Handouts

Navigable Slide Index

Topics Covered

Links

Series:

Categories:

Talk Citation

Publication History

Financial Disclosures

The regulation of MAP kinase signalling by dual-specificity protein phosphatases

Share This Talk

Messaging

Social

Permalink

A selection of talks on Biochemistry

Transcript

Share This Talk

Messaging

Social

Permalink

The regulation of MAP kinase signalling by dual-specificity protein phosphatases