Difference between revisions of "Team:XJTLU-CHINA/PeptideProduction"
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| + | <h1>Anti-Microbial Peptide</h1> | ||
| + | <p style="font-size:20px"> | ||
| + | Anti-microbial peptide (AMP) is a part of the innate immune system of most multi-cellular organisms to counter microbial | ||
| + | infections (Margitta and Torsten, 1999). The cationic and amphipathic α-helix structure is the most wildly | ||
| + | conformation in those peptides but some hydrophobic α-helical peptides which possess antimicrobial activity. | ||
| + | This year we choose three different cationic antimicrobial peptides which encompass α-helical conformation | ||
| + | in our project. | ||
| + | </p> | ||
| + | <p style="font-size:20px"> | ||
| + | Figure 1 shows the molecular mechanism of cationic AMPs α-helical structure. Most of cationic AMPs associate with lipid group | ||
| + | of bacteria membrane. The α-helical structure disrupt the packing of lipid molecules such that the membrane | ||
| + | becomes leaky (Rocca et al., 1999). | ||
| + | </p> | ||
| + | </div> | ||
| + | |||
| + | <div class="fig" align="center"> | ||
| + | <figure> | ||
| + | <img width="650px" src="https://static.igem.org/mediawiki/2017/9/99/Peptide_Production_1.png"> | ||
| + | <figcaption>Figure 1: The interaction mechanism of cationic α-helical structure of Anti-microbial peptides. The α-helical | ||
| + | structure insert into the bacteria Lipid bilayer in aqueous solution. Following insertion of the peptide, | ||
| + | the bilayer membrane permeability may be varied.</figcaption> | ||
| + | </figure> | ||
| + | </div> | ||
| + | |||
| + | <div class="para"> | ||
| + | <h1>LL-37</h1> | ||
| + | <p style="font-size:20px"> | ||
| + | LL-37 is the only cathelicidin-derived antimicrobial peptide found in humans (Dürr, Sudheendra and Ramamoorthy, 2006). Mature | ||
| + | LL-37 has 37 amino acid residues starting with two leucines (NH2-LLGDFFRKSKEKIGKEFKRIVQRIKDFLRNLVPRTES-COOH). | ||
| + | The peptide is cleaved from a larger protein, hCAP-18 by extracellular proteolysis of proteinase 3 from the | ||
| + | C-terminal end of hCAP18 (Patricia, 2010; Ramos, Domingues, and Gama, 2011). The peptide composed of two | ||
| + | mainly parts: from residue Leu2 to Leu31 is α-helical structure (Fig 2b) and 6 residues form loop structure | ||
| + | (Fig 2a). | ||
| + | </p> | ||
| + | <p style="font-size:20px"> | ||
| + | Ramos, Domingues, and Gama (2011) also reported that LL-37 has additional roles such as regulating the inflammatory response | ||
| + | to wound or infection sites, binding and neutralizing LPS, and wound closure apart from anti-microbial property | ||
| + | (Figure 2c). | ||
| + | </p> | ||
| + | </div> | ||
| + | |||
| + | <div class="fig" align="center"> | ||
| + | <figure> | ||
| + | <img width="650px" src="https://static.igem.org/mediawiki/2017/d/de/Peptide_Production_2a.png"> | ||
| + | <figcaption>Figure 2a: LL-37 structure and residues(PDB 2K6O)</figcaption> | ||
| + | </figure> | ||
| + | <figure> | ||
| + | <img width="650px" src="https://static.igem.org/mediawiki/2017/2/29/Peptide_Production_2b.png"> | ||
| + | <figcaption>Figure 2b: LL-37 secondary structure prediction (predicted by http://www.compbio.dundee.ac.uk/jpred/index.html | ||
| + | ). | ||
| + | </figcaption> | ||
| + | </figure> | ||
| + | <figure> | ||
| + | <img width="650px" src="https://static.igem.org/mediawiki/2017/3/3b/Peptide_Production_2c.png"> | ||
| + | <figcaption>Figure 2c: Biological functions of LL-37 (Ramos, Domingues, and Gama, 2011)</figcaption> | ||
| + | </figure> | ||
| + | </div> | ||
</div> | </div> | ||
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Revision as of 08:57, 30 October 2017
Peptide Production
Anti-Microbial Peptide
Anti-microbial peptide (AMP) is a part of the innate immune system of most multi-cellular organisms to counter microbial infections (Margitta and Torsten, 1999). The cationic and amphipathic α-helix structure is the most wildly conformation in those peptides but some hydrophobic α-helical peptides which possess antimicrobial activity. This year we choose three different cationic antimicrobial peptides which encompass α-helical conformation in our project.
Figure 1 shows the molecular mechanism of cationic AMPs α-helical structure. Most of cationic AMPs associate with lipid group of bacteria membrane. The α-helical structure disrupt the packing of lipid molecules such that the membrane becomes leaky (Rocca et al., 1999).
LL-37
LL-37 is the only cathelicidin-derived antimicrobial peptide found in humans (Dürr, Sudheendra and Ramamoorthy, 2006). Mature LL-37 has 37 amino acid residues starting with two leucines (NH2-LLGDFFRKSKEKIGKEFKRIVQRIKDFLRNLVPRTES-COOH). The peptide is cleaved from a larger protein, hCAP-18 by extracellular proteolysis of proteinase 3 from the C-terminal end of hCAP18 (Patricia, 2010; Ramos, Domingues, and Gama, 2011). The peptide composed of two mainly parts: from residue Leu2 to Leu31 is α-helical structure (Fig 2b) and 6 residues form loop structure (Fig 2a).
Ramos, Domingues, and Gama (2011) also reported that LL-37 has additional roles such as regulating the inflammatory response to wound or infection sites, binding and neutralizing LPS, and wound closure apart from anti-microbial property (Figure 2c).
