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===Histone Methylation===
===Histone Methylation===
[[Image:human_nucleosome_ray_trace.png|200 px| right| thumb|Human nucleosome]]
[[Image:human_nucleosome_ray_trace.png|200 px| right| thumb|Human nucleosome]]
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Histone proteins aid in the packing of DNA for the purpose of compacting the genome in the nucleus of the cell and regulating physical accessibility of genes for transcription. The protein itself is an octamer made of heterodimer core proteins H2a, H2b, H3, and H4, with H1 and H5 acting as linker proteins. About 145-157 base pairs wind around a histone core protein. <ref name="DesJarlais">PMID: 26745824</ref> Modifications to histone core proteins can affect the accessibility of genes in the genome and their ability to be transcribed. Some of these modifications include methylation/demethylation, acetylation/deacetylation, and ubiquitination/deubiquitination. (2)
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Histone proteins aid in the packing of DNA for the purpose of compacting the genome in the nucleus of the cell and regulating physical accessibility of genes for transcription. The protein itself is an octamer made of heterodimer core proteins H2a, H2b, H3, and H4, with H1 and H5 acting as linker proteins. About 145-157 base pairs wind around a histone core protein. <ref name="DesJarlais">PMID: 26745824</ref> Modifications to histone core proteins can affect the accessibility of genes in the genome and their ability to be transcribed. Some of these modifications include methylation/demethylation, acetylation/deacetylation, and ubiquitination/deubiquitination. <ref name="Lun">DOI: 10.1016/j.apsb.2013.04.007</ref>
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Specifically, histone methylation is associated with gene activation. (3) Many domain families fall under the Histone methylase family, one of these enzymes being the <scene name='81/811092/Set7_rotate/4'>SET7 domain</scene> family, which can target H3, H4, or H2a; each of these methylation sites can have different effects on gene expression within the genome. Typically, methylation of some of these sites are always present on both active and inactive genes, extra methylations required for activity. (4) Some tumor related genes such as p53 are site specifically methylated to promote biological function (5), whereas hypomethylation of CpG is linked to tumor genesis. (2) A particular enzyme in the SET7 domain family is lysine methyltransferase, which acts on the histone by adding a methyl group to Lys4 on H3; the addition results in promotion of gene unwinding and gene transcription. (4,3)
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Specifically, histone methylation is associated with gene activation. <ref name="Dong">PMID: 23566087</ref> Many domain families fall under the Histone methylase family, one of these enzymes being the <scene name='81/811092/Set7_rotate/4'>SET7 domain</scene> family, which can target H3, H4, or H2a; each of these methylation sites can have different effects on gene expression within the genome. Typically, methylation of some of these sites are always present on both active and inactive genes, extra methylations required for activity. <ref name="Xiao">doi:10.1038/nature01378</ref> Some tumor related genes such as p53 are site specifically methylated to promote biological function (5), whereas hypomethylation of CpG is linked to tumor genesis. <ref name="Lun" /> A particular enzyme in the SET7 domain family is lysine methyltransferase, which acts on the histone by adding a methyl group to Lys4 on H3; the addition results in promotion of gene unwinding and gene transcription. (4,3)
==KMT Structure==
==KMT Structure==
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<references/>
<references/>
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2. Lu, D. Epigenetic modification enzymes: catalytic mechanisms and inhibitors. Acta Pharmaceutica Sinica B 2013, 3: 141-149.
 
3. Dong, X.; Weng, Z. The correlation between histone modifications and gene expression. Epigenomics 2013, 5: 113-6.
3. Dong, X.; Weng, Z. The correlation between histone modifications and gene expression. Epigenomics 2013, 5: 113-6.

Revision as of 01:38, 10 April 2019

Lysine Methyl Transferase, Homo Sapiens

Lysine Methyl Transferase

Drag the structure with the mouse to rotate

References

  1. DesJarlais R, Tummino PJ. Role of Histone-Modifying Enzymes and Their Complexes in Regulation of Chromatin Biology. Biochemistry. 2016 Mar 22;55(11):1584-99. doi: 10.1021/acs.biochem.5b01210. Epub , 2016 Jan 26. PMID:26745824 doi:http://dx.doi.org/10.1021/acs.biochem.5b01210
  2. 2.0 2.1 doi: https://dx.doi.org/10.1016/j.apsb.2013.04.007
  3. Dong X, Weng Z. The correlation between histone modifications and gene expression. Epigenomics. 2013 Apr;5(2):113-6. doi: 10.2217/epi.13.13. PMID:23566087 doi:http://dx.doi.org/10.2217/epi.13.13
  4. Xiao B, Jing C, Wilson JR, Walker PA, Vasisht N, Kelly G, Howell S, Taylor IA, Blackburn GM, Gamblin SJ. Structure and catalytic mechanism of the human histone methyltransferase SET7/9. Nature. 2003 Feb 6;421(6923):652-6. Epub 2003 Jan 22. PMID:12540855 doi:10.1038/nature01378


3. Dong, X.; Weng, Z. The correlation between histone modifications and gene expression. Epigenomics 2013, 5: 113-6.

4. Xiao, B.; Jing, C.; Wilson, J.; Walker, P.; Vasisht, N.; et al. Structure and catalytic mechanism of the human histone methyltranferase SET7/9. Letters to Nature 2003, 412: 652-655.

5. Del Rizzo, P. A.; Trievel, R.C. Substrate and product specificities of SET domain methyltransferases. Epigenetics 2011, 6: 1059-1067

6. Mao, X.; Qiao, Z.; Fan, C.; Guo, A.; Yu, X.; Jin, F. Expression pattern and methylation of estrogen receptor α in breast intraductal proliferative lesions. Oncology Reports 2016, 36: 1868-1874.

7. Tamura, R., Doi, S., Nakashima, A., Sasaki, K., Maeda, K., Ueno, T., & Masaki, T. (2018). Inhibition of the H3K4 methyltransferase SET7/9 ameliorates peritoneal fibrosis. PloS one, 13(5), e0196844. doi:10.1371/journal.pone.0196844

8. Schluckebier et al. (1997), Differential binding of S-andeosylmethionine S-adenosylhomocysteine and Sinefungin to adenine-specific DNA methyltransferase M. TaqI; J. Mol. Biol., 265 56

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Madeleine Wilson

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