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10.1186/2191-0855-3-45

http://scihub22266oqcxt.onion/10.1186/2191-0855-3-45
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C3751704!3751704!23945047
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suck abstract from ncbi


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pmid23945047      AMB+Express 2013 ; 3 (ä): 45
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  • Overexpression of an antimicrobial peptide derived from C elegans using an aggregation-prone protein coexpression system #MMPMID23945047
  • Tomisawa S; Hojo E; Umetsu Y; Ohki S; Kato Y; Miyazawa M; Mizuguchi M; Kamiya M; Kumaki Y; Kikukawa T; Kawano K; Demura M; Aizawa T
  • AMB Express 2013[]; 3 (ä): 45 PMID23945047show ga
  • Antibacterial factor 2 (ABF-2) is a 67-residue antimicrobial peptide derived from the nematode Caenorhabditis elegans. Although it has been reported that ABF-2 exerts in vitro microbicidal activity against a range of bacteria and fungi, the structure of ABF-2 has not yet been solved. To enable structural studies of ABF-2 by NMR spectroscopy, a large amount of isotopically labeled ABF-2 is essential. However, the direct expression of ABF-2 in Escherichia coli is difficult to achieve due to its instability. Therefore, we applied a coexpression method to the production of ABF-2 in order to enhance the inclusion body formation of ABF-2. The inclusion body formation of ABF-2 was vastly enhanced by coexpression of aggregation-prone proteins (partner proteins). By using this method, we succeeded in obtaining milligram quantities of active, correctly folded ABF-2. In addition, 15?N-labeled ABF-2 and a well-dispersed heteronuclear single quantum coherence (HSQC) spectrum were also obtained successfully. Moreover, the effect of the charge of the partner protein on the inclusion body formation of ABF-2 in this method was investigated by using four structurally homologous proteins. We concluded that a partner protein of opposite charge enhanced the formation of an inclusion body of the target peptide efficiently.
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