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The Wnt Signaling Pathway (β Catenin )

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Dickinson Lab Lab
Dickinson Lab Lab
1  sur  12
Jonathan Fletcher Dr. Amanda Dickinson’s Developmental Biology Fall 2011
Normal Cellular Conditions  Wnt ligand is not present  Dishevelled is inactive  GSK3 destruction complex prevents the dissociation of β-Catenin  Β-TrCP then targets β-Catenin for proteosomal destruction  No transcription of Wnt genes occur under normal conditions
Normal Conditions (Wnt -) FRZ DSH Β-TrCP
Presence of Wnt ligand  Wnt Ligand is present and interacts with Frizzled transmembrane receptors (Logan and Nusse 2004)  LRP associates with the Wnt/Frizzled protein complex. LRP is required for signaling in many Wnt pathways. (Wehrli et al. 2000)  Frizzled then activates Dishevelled (Logan and Nusse 2004)  Once activated Dishevelled inhibits the GSK3 destruction complex enzyme (Logan and Nusse 2004)  β-Catenin is now free to dissociate from the APC protein and enter the nucleus (Behrans et al. 1996)  Once in the nucleus β-Catenin can associate with an LEF or TCF DNA- Binding protein, becoming a transcription factor (Behrans et al. 1996)  This complex binds to and activates the Wnt responsive genes (Behrans et al. 1996; Cadigan and Nusse 1997)
Conditions with Wnt present ( Wnt+) Wnt LRP FRZ DSH LEF/TCF B-Cat Wnt –responsive genes
Things can go wrong: Cancer!  The APC protein also functions  This can lead to uncontrolled as a tumor suppressor (Korinek proliferation et al 1997)  Ultimately can lead to tumor  Colon cancer may occur when formation, more APC genes are mutated (Korinek mutations, invasion and et al 1997) metastasis.  APC can no longer keep β- Catenin out of the nucleus (Korinek et al. 1997; He et al. 1998)  Once inside the nucleus β- Catenin can bind with other proteins including SMADs, CtBP, Groucho and CBP to upregulate proteins for cell division.
If APC is mutated (Oncogenes) FRZ When APC is mutated the Gsk3 APC complex becomes DSH unlinked from Wnt Signaling (Does not matter if Wnt is present or not… It will still release B- Catenin) CtBP TCF 1 B-Cat Cyclins, c-Myc, Pro-tumorigenic genes SMAD
Wnt Role In Development  Wnt proteins now recognized as a major developmentally important family of proteins. (Cadigan and Nusse 1997)  They are important in embryonic induction (Cadigan and Nusse 1997)  They are extremely important in the generation of cell polarity (Cadigan and Nusse 1997)  They also function in the specification of the cells fate(Cadigan and Nusse 1997)
Legend  DSH- Dishevelled Protein  FRZ- Frizzled Receptor  CBP- CREB binding Protein  Wnt- Wingless/Integrated protein  Groucho-Non-DNA binding co-repressor ( named after comedian)  SMAD- The name is a combination of the drosophila protein, mothers againstdecapentaplegic (MAD) and the C. elegans protein SMA.  CtBP-1-Carboxyl terminal binding protein  c-MYC- myelocytomatosis oncogene  LEF- Lymphoid Enhancer Factor  TCF- DNA binding protein  APC-Adenomatous polyposis coli  GSK-3- Glycogen synthase kinase 3  LRP- arrow  Axin-Negative regulator of Wnt  β-Cat- Beta Catenin Protein  Β-TrCP-beta transduction repeat containing protein
References  www.familyguy.wikia.com/wiki/peter_griffin  http://www.ccalliance.org/colorectal_cancer/staging.html  www.bioportal.kobic.re.kr/Pdcase/pathway.jsp?pathway=h_wntPathway  Jürgen Behrens, Boris-Alexander Jerchow, Martin Würtele, Jan Grimm, Christian Asbrand, Ralph Wirtz, Michael Kühl, Doris Wedlich and Walter Birchmeier. Functional Interaction of an Axin Homolog, Conductin, with β-Catenin, APC, and GSK3β. Science 24 April 1998: Vol. 280 no. 5363 pp. 596-599  Logan CY, Nusse R. The Wnt signaling pathway in development and disease. Annual Review Cell Development Biology. 2004:20:781-810  Cadigan KM, Nusse R.Wnt signaling: a common theme in animal development. Genes Dev. 1997 Dec 15:11 (24) 3286-305  Wehrli M, Dougan ST, Caldwell K, O’Keefe L. Schwartz S, Vaizel-Ohayon D, Schejter E, Tomlinson A, DiNardo S. Arrow encodes an LDL-receptor-related protein essential for Wingless signaling. Nature. 2000. 407 (6803): 527-530  Vladmir Korinek, Nick Barker, Patrice J. Morin, Dick Van Wichen, Roel de Weger, Kenneth W. Kinzler, Bert Vogelstein and Hans Clever. 1997. Constituitive Transcriptional Activation by a Beta-catenin- Tcf Complex in APC -/- Colon Carcinoma. Science 21 Vol. 275 No. 5307 pp. 1784-1787
Brownies!!! The Wnt Way!!!!! Wnt Cell FRZ Membrane APC DSH Active Inhibition GSk3 Β-Catenin Axin Transcription LEF/TCF
Thank You!!!  Dr. Amanda Dickinson, PhD  Ryan Lab for not eating these delicious brownies before I could get them down the hall!

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The Wnt Signaling Pathway (β Catenin )

  • 1. Jonathan Fletcher Dr. Amanda Dickinson’s Developmental Biology Fall 2011
  • 2. Normal Cellular Conditions  Wnt ligand is not present  Dishevelled is inactive  GSK3 destruction complex prevents the dissociation of β-Catenin  Β-TrCP then targets β-Catenin for proteosomal destruction  No transcription of Wnt genes occur under normal conditions
  • 3. Normal Conditions (Wnt -) FRZ DSH Β-TrCP
  • 4. Presence of Wnt ligand  Wnt Ligand is present and interacts with Frizzled transmembrane receptors (Logan and Nusse 2004)  LRP associates with the Wnt/Frizzled protein complex. LRP is required for signaling in many Wnt pathways. (Wehrli et al. 2000)  Frizzled then activates Dishevelled (Logan and Nusse 2004)  Once activated Dishevelled inhibits the GSK3 destruction complex enzyme (Logan and Nusse 2004)  β-Catenin is now free to dissociate from the APC protein and enter the nucleus (Behrans et al. 1996)  Once in the nucleus β-Catenin can associate with an LEF or TCF DNA- Binding protein, becoming a transcription factor (Behrans et al. 1996)  This complex binds to and activates the Wnt responsive genes (Behrans et al. 1996; Cadigan and Nusse 1997)
  • 5. Conditions with Wnt present ( Wnt+) Wnt LRP FRZ DSH LEF/TCF B-Cat Wnt –responsive genes
  • 6. Things can go wrong: Cancer!  The APC protein also functions  This can lead to uncontrolled as a tumor suppressor (Korinek proliferation et al 1997)  Ultimately can lead to tumor  Colon cancer may occur when formation, more APC genes are mutated (Korinek mutations, invasion and et al 1997) metastasis.  APC can no longer keep β- Catenin out of the nucleus (Korinek et al. 1997; He et al. 1998)  Once inside the nucleus β- Catenin can bind with other proteins including SMADs, CtBP, Groucho and CBP to upregulate proteins for cell division.
  • 7. If APC is mutated (Oncogenes) FRZ When APC is mutated the Gsk3 APC complex becomes DSH unlinked from Wnt Signaling (Does not matter if Wnt is present or not… It will still release B- Catenin) CtBP TCF 1 B-Cat Cyclins, c-Myc, Pro-tumorigenic genes SMAD
  • 8. Wnt Role In Development  Wnt proteins now recognized as a major developmentally important family of proteins. (Cadigan and Nusse 1997)  They are important in embryonic induction (Cadigan and Nusse 1997)  They are extremely important in the generation of cell polarity (Cadigan and Nusse 1997)  They also function in the specification of the cells fate(Cadigan and Nusse 1997)
  • 9. Legend  DSH- Dishevelled Protein  FRZ- Frizzled Receptor  CBP- CREB binding Protein  Wnt- Wingless/Integrated protein  Groucho-Non-DNA binding co-repressor ( named after comedian)  SMAD- The name is a combination of the drosophila protein, mothers againstdecapentaplegic (MAD) and the C. elegans protein SMA.  CtBP-1-Carboxyl terminal binding protein  c-MYC- myelocytomatosis oncogene  LEF- Lymphoid Enhancer Factor  TCF- DNA binding protein  APC-Adenomatous polyposis coli  GSK-3- Glycogen synthase kinase 3  LRP- arrow  Axin-Negative regulator of Wnt  β-Cat- Beta Catenin Protein  Β-TrCP-beta transduction repeat containing protein
  • 10. References  www.familyguy.wikia.com/wiki/peter_griffin  http://www.ccalliance.org/colorectal_cancer/staging.html  www.bioportal.kobic.re.kr/Pdcase/pathway.jsp?pathway=h_wntPathway  Jürgen Behrens, Boris-Alexander Jerchow, Martin Würtele, Jan Grimm, Christian Asbrand, Ralph Wirtz, Michael Kühl, Doris Wedlich and Walter Birchmeier. Functional Interaction of an Axin Homolog, Conductin, with β-Catenin, APC, and GSK3β. Science 24 April 1998: Vol. 280 no. 5363 pp. 596-599  Logan CY, Nusse R. The Wnt signaling pathway in development and disease. Annual Review Cell Development Biology. 2004:20:781-810  Cadigan KM, Nusse R.Wnt signaling: a common theme in animal development. Genes Dev. 1997 Dec 15:11 (24) 3286-305  Wehrli M, Dougan ST, Caldwell K, O’Keefe L. Schwartz S, Vaizel-Ohayon D, Schejter E, Tomlinson A, DiNardo S. Arrow encodes an LDL-receptor-related protein essential for Wingless signaling. Nature. 2000. 407 (6803): 527-530  Vladmir Korinek, Nick Barker, Patrice J. Morin, Dick Van Wichen, Roel de Weger, Kenneth W. Kinzler, Bert Vogelstein and Hans Clever. 1997. Constituitive Transcriptional Activation by a Beta-catenin- Tcf Complex in APC -/- Colon Carcinoma. Science 21 Vol. 275 No. 5307 pp. 1784-1787
  • 11. Brownies!!! The Wnt Way!!!!! Wnt Cell FRZ Membrane APC DSH Active Inhibition GSk3 Β-Catenin Axin Transcription LEF/TCF
  • 12. Thank You!!!  Dr. Amanda Dickinson, PhD  Ryan Lab for not eating these delicious brownies before I could get them down the hall!