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MyoD functions as a transcriptional activator only as a heterodimer with E proteins, which are a sub-family of bHLH proteins. This interaction takes place in the bHLH domain of both proteins. In one experiment, forced binding of E12 to MyoD that had been inhibited using E protein fragments substantially restored MyoD's activity <ref>doi: 10.1101/gad.1765109</ref>. The myogenic ability of MyoD is inhibited by the presence of another bHLH protein known as Twist. Twist inhibits MyoD by competitively binding E proteins and preventing MyoD-E protein heterodimers from forming <ref>Hamamori, Y., Wu, H. Y., Sartorelli, V., & Kedes, L. The basic domain of myogenic basic helix-loop-helix (bHLH) proteins is the novel target for direct inhibition by another bHLH protein, Twist. Molecular and Cellular Biology. '''1997'''. 17. 6563–6573.</ref>.
MyoD functions as a transcriptional activator only as a heterodimer with E proteins, which are a sub-family of bHLH proteins. This interaction takes place in the bHLH domain of both proteins. In one experiment, forced binding of E12 to MyoD that had been inhibited using E protein fragments substantially restored MyoD's activity <ref>doi: 10.1101/gad.1765109</ref>. The myogenic ability of MyoD is inhibited by the presence of another bHLH protein known as Twist. Twist inhibits MyoD by competitively binding E proteins and preventing MyoD-E protein heterodimers from forming <ref>Hamamori, Y., Wu, H. Y., Sartorelli, V., & Kedes, L. The basic domain of myogenic basic helix-loop-helix (bHLH) proteins is the novel target for direct inhibition by another bHLH protein, Twist. Molecular and Cellular Biology. '''1997'''. 17. 6563–6573.</ref>.
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The protein IFRD1 is an activating cofactor of MyoD. This protein and MyoD cooperatively activate muscle-specific enhancers. This same cofactor also represses NF-κB, which has been shown to inhibit MyoD mRNA translation <ref>PMID: 21127072</ref>
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The protein IFRD1 is an activating cofactor of MyoD. This protein and MyoD cooperatively activate muscle-specific enhancers. This same cofactor also represses NF-κB, which has been shown to inhibit MyoD mRNA translation <ref>PMID: 21127072</ref>.
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NFATc1 is a transcription factor that inhibits MyoD activity. This is inhibition is accomplished through physically obstructing MyoD's activation domain, preventing transcriptional activity. This process functions to convert fast-twitch muscle to slow-twitch muscle <ref>PMID: 24183602</ref>.
MyoD is degraded by ubiquination of its N-terminal Lys residue. Data suggests that this occurs through attachment of ubiquitin at the N-terminal residue, followed by synthesis of a polyubiquitin chain on an internal Lys residue, which sufficiently disrupts MyoD's structure to cause degradation. This process is a major pathway of selective protein degradation in eukaryotic cells <ref>DOI: 10.1093/emboj/17.20.5964</ref>.
MyoD is degraded by ubiquination of its N-terminal Lys residue. Data suggests that this occurs through attachment of ubiquitin at the N-terminal residue, followed by synthesis of a polyubiquitin chain on an internal Lys residue, which sufficiently disrupts MyoD's structure to cause degradation. This process is a major pathway of selective protein degradation in eukaryotic cells <ref>DOI: 10.1093/emboj/17.20.5964</ref>.

Revision as of 02:08, 13 October 2015

Function and Classification

MyoD, along with Myf5, is responsible for muscle cell differentiation and establishment of the myogenic lineage. It is a member of the basic helix loop helix (bHLH) family and myogenic factors subfamily of proteins [1].

Crystal Structure of MyoD bHLH Domain

Drag the structure with the mouse to rotate

References

[1] [2] [3] [4] [5] http://www.ncbi.nlm.nih.gov/pmc/articles/PMC232510/


  1. Phospho Site Plus. http://www.phosphosite.org/proteinAction.do?id=3637&showAllSites=true (accessed October 6, 2015)
  2. Jones S. An overview of the basic helix-loop-helix proteins. Genome Biol. 2004;5(6):226. Epub 2004 May 28. PMID:15186484 doi:http://dx.doi.org/10.1186/gb-2004-5-6-226
  3. Weintraub, H., Dwarki, V. J., Verma, I., Davis, R., Hollenberg, S., Snider, L., Lassar, A., Tapscott, S. J. Muscle-specific transcriptional activation by MyoD. Genes & Dev. 1991. 5. 1377-1386
  4. Gerber, A. N., Klesert, T. R., Berstrom, D. A., Tapscott, S. J. Two domains of MyoD mediate transcriptional activation of genes in repressive chromatin: a mechanism for lineage determination in myogenesis. Genes & Dev. 1997. 11. 436-450
  5. Kophengnavong, T., Michnowicz, J. E., & Blackwell, T. K. Establishment of Distinct MyoD, E2A, and Twist DNA Binding Specificities by Different Basic Region-DNA Conformations. Molecular and Cellular Biology, 2000, 20. 261–272.
  6. Jones S. An overview of the basic helix-loop-helix proteins. Genome Biol. 2004;5(6):226. Epub 2004 May 28. PMID:15186484 doi:http://dx.doi.org/10.1186/gb-2004-5-6-226
  7. Weintraub, H., Dwarki, V. J., Verma, I., Davis, R., Hollenberg, S., Snider, L., Lassar, A., Tapscott, S. J. Muscle-specific transcriptional activation by MyoD. Genes & Dev. 1991. 5. 1377-1386
  8. Yang Z, MacQuarrie KL, Analau E, Tyler AE, Dilworth FJ, Cao Y, Diede SJ, Tapscott SJ. MyoD and E-protein heterodimers switch rhabdomyosarcoma cells from an arrested myoblast phase to a differentiated state. Genes Dev. 2009 Mar 15;23(6):694-707. doi: 10.1101/gad.1765109. PMID:19299559 doi:http://dx.doi.org/10.1101/gad.1765109
  9. Hamamori, Y., Wu, H. Y., Sartorelli, V., & Kedes, L. The basic domain of myogenic basic helix-loop-helix (bHLH) proteins is the novel target for direct inhibition by another bHLH protein, Twist. Molecular and Cellular Biology. 1997. 17. 6563–6573.
  10. Micheli L, Leonardi L, Conti F, Maresca G, Colazingari S, Mattei E, Lira SA, Farioli-Vecchioli S, Caruso M, Tirone F. PC4/Tis7/IFRD1 stimulates skeletal muscle regeneration and is involved in myoblast differentiation as a regulator of MyoD and NF-kappaB. J Biol Chem. 2011 Feb 18;286(7):5691-707. doi: 10.1074/jbc.M110.162842. Epub 2010, Dec 2. PMID:21127072 doi:http://dx.doi.org/10.1074/jbc.M110.162842
  11. Federation AJ, Bradner JE, Meissner A. The use of small molecules in somatic-cell reprogramming. Trends Cell Biol. 2014 Mar;24(3):179-87. doi: 10.1016/j.tcb.2013.09.011. Epub, 2013 Oct 31. PMID:24183602 doi:http://dx.doi.org/10.1016/j.tcb.2013.09.011
  12. Breitschopf K, Bengal E, Ziv T, Admon A, Ciechanover A. A novel site for ubiquitination: the N-terminal residue, and not internal lysines of MyoD, is essential for conjugation and degradation of the protein. EMBO J. 1998 Oct 15;17(20):5964-73. PMID:9774340 doi:http://dx.doi.org/10.1093/emboj/17.20.5964
  13. Arnold, H. H.; Braun, T. Targeted inactivation of myogenic factor genes reveals their role during mouse myogenesis: a review. Int. J. Dev. Biol. 1996. 40. 345-353

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Anthony Milto

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