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Pentatricopeptide repeat (PPR) proteins are a family of sequence specific RNA-binding proteins which participate in organelle RNA metabolism. Although the mechanisms of RNA binding and the functions of PPR proteins are not fully understood, PPR proteins are thought to assist in RNA editing,^[1] translation,^[2] and organelle biogenesis.^[3] They make up the majority of RNA-binding factors in plant organelles. PPR proteins are characterized by a series of tandem-repeat amino acid consensus sequences which form α-helix . These hairpin structures accumulate to form a α-solenoid tertiary structure. PPR proteins belong to one of two classes: P-class and PLS-class, with the P-class containing 35 amino acid repeats and the PLS-class containing 31-36 amino acid repeats. PPR10 is a well-characterized P-class PPR protein found in the chloroplast of Zea mays.^[2]

1 Function
2 Mechanism
3 Synthetic Applications
4 References

Function

In the Zea mays plastid, PPR10 binds specifically to the ssRNA oligonucleotides ATPH (17 nucleotides: 5'-GUAUUCUUUAAUUAUUUC-3') and SPAJ (18 nucleotides: 5'-GUAUUCUUUAAUUAUUUC-3') where it has been shown to shield the transcripts from ribonucleases. In addition to stabilizing these RNA sequences, PPR10 increases the rate at which they are translated.^[2]

Mechanism

The primary factor in the ability of PPR10 to bind RNA bases in a modular fashion lies in the hydrogen bonding of an AA residue at position 6 of each repeat with a specific base. For example, in the structure to the right, Through van der Waals interactions, Val210 and Arg175 (both orange) also contribute to the specific binding of guanine in this example. These residues force G1 into a conformation where it forms a hydrogen bond to Thr178. The example of PPR10 binding G1 of ATPH exemplifies the general rules by which PPR proteins bind specific nucleotides: firstly, a residue at the 6 position of one repeat forms a hydrogen bond with the base. The identity of this residue determines whether the repeat will bind a purine (adenine and guanine) or pyrimidine (cytosine and uracil). It appears that serine and threonine at position 6 are specific for purines, and asparagine at position 6 is specific for pyrimidines.^[4] Secondly, a residue at position 1 of the next repeat (1') completes the specificity of the interaction. Through van der Waals interactions, this residue determines between A/G and C/U. Other amino acids further contribute to this mechanism, but the previously described rules always apply when PPR proteins bind RNA sequences with modularity.^[5]

Synthetic Applications

There is potential. . .

References

↑ Okuda K, Nakamura T, Sugita M, Shimizu T, Shikanai T. A pentatricopeptide repeat protein is a site recognition factor in chloroplast RNA editing. J Biol Chem. 2006 Dec 8;281(49):37661-7. Epub 2006 Oct 2. PMID:17015439 doi:http://dx.doi.org/10.1074/jbc.M608184200
↑ ^2.0 ^2.1 ^2.2 Prikryl J, Rojas M, Schuster G, Barkan A. Mechanism of RNA stabilization and translational activation by a pentatricopeptide repeat protein. Proc Natl Acad Sci U S A. 2011 Jan 4;108(1):415-20. doi: 10.1073/pnas.1012076108., Epub 2010 Dec 20. PMID:21173259 doi:http://dx.doi.org/10.1073/pnas.1012076108
↑ Lurin C, Andres C, Aubourg S, Bellaoui M, Bitton F, Bruyere C, Caboche M, Debast C, Gualberto J, Hoffmann B, Lecharny A, Le Ret M, Martin-Magniette ML, Mireau H, Peeters N, Renou JP, Szurek B, Taconnat L, Small I. Genome-wide analysis of Arabidopsis pentatricopeptide repeat proteins reveals their essential role in organelle biogenesis. Plant Cell. 2004 Aug;16(8):2089-103. Epub 2004 Jul 21. PMID:15269332 doi:http://dx.doi.org/10.1105/tpc.104.022236
↑ Barkan A, Rojas M, Fujii S, Yap A, Chong YS, Bond CS, Small I. A combinatorial amino acid code for RNA recognition by pentatricopeptide repeat proteins. PLoS Genet. 2012;8(8):e1002910. doi: 10.1371/journal.pgen.1002910. Epub 2012 Aug , 16. PMID:22916040 doi:http://dx.doi.org/10.1371/journal.pgen.1002910
↑ Yagi Y, Nakamura T, Small I. The potential for manipulating RNA with pentatricopeptide repeat proteins. Plant J. 2014 Jun;78(5):772-82. doi: 10.1111/tpj.12377. Epub 2014 Jan 29. PMID:24471963 doi:http://dx.doi.org/10.1111/tpj.12377

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@@ Line 6: / Line 6: @@
 ==Mechanism==
-The primary factor in the ability of PPR10 to bind RNA bases in a modular fashion lies in the hydrogen bonding of an AA residue at position 6 of each repeat with a specific base. For example, in the structure to the right, <scene name='69/696301/G1binding/1'>threonine residue 178 (blue) forms a hydrogen bond to G1 (green) of ATPH.</scene> Through van der Waals interactions, Val210 and Arg175 (both orange) also contribute to the specific binding of guanine in this example. These residues force G1 into a conformation where it forms a hydrogen bond to Thr178. The example of PPR10 binding G1 of ATPH exemplifies the general rules by which PPR proteins bind specific nucleotides: firstly, a residue at the 6 position of one repeat forms a hydrogen bond with the base. The identity of this residue determines whether the repeat will bind a purine or pyrimidine (serine and threonine bind purine, and asparagine binds pyrimidine).<ref>doi:10.1371/journal.pgen.1002910</ref>
+The primary factor in the ability of PPR10 to bind RNA bases in a modular fashion lies in the hydrogen bonding of an AA residue at position 6 of each repeat with a specific base. For example, in the structure to the right, <scene name='69/696301/G1binding/1'>threonine residue 178 (blue) forms a hydrogen bond to G1 (green) of ATPH.</scene> Through van der Waals interactions, Val210 and Arg175 (both orange) also contribute to the specific binding of guanine in this example. These residues force G1 into a conformation where it forms a hydrogen bond to Thr178. The example of PPR10 binding G1 of ATPH exemplifies the general rules by which PPR proteins bind specific nucleotides: firstly, a residue at the 6 position of one repeat forms a hydrogen bond with the base. The identity of this residue determines whether the repeat will bind a purine (adenine and guanine) or pyrimidine (cytosine and uracil). It appears that serine and threonine at position 6 are specific for purines, and asparagine at position 6 is specific for pyrimidines.<ref>doi:10.1371/journal.pgen.1002910</ref> Secondly, a residue at position 1 of the next repeat (1') completes the specificity of the interaction. Through van der Waals interactions, this residue determines between A/G and C/U. Other amino acids further contribute to this mechanism, but the previously described rules always apply when PPR proteins bind RNA sequences with modularity.<ref name = "engineering">DOI:10.1111/tpj.12377</ref>
 ==Synthetic Applications==

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