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Purification and Biochemical Characterization of a New Protease Inhibitor from <i>Conyza dioscoridis</i> with Antimicrobial, Antifungal and Cytotoxic Effects
oleh: Aida Karray, Mona Alonazi, Slim Smaoui, Philippe Michaud, Dina Soliman, Abir Ben Bacha
Format: | Article |
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Diterbitkan: | MDPI AG 2020-11-01 |
Deskripsi
The main objective of the current study was the extraction, purification, and biochemical characterization of a protein protease inhibitor from <i>Conyza</i><i>dioscoridis</i>. Antimicrobial potential and cytotoxic effects were also examined. The protease inhibitor was extracted in 0.1 M phosphate buffer (pH 6–7). Then, the protease inhibitor, named PDInhibitor, was purified using ammonium sulfate precipitation followed by filtration through a Sephadex G-50 column and had an apparent molecular weight of 25 kDa. The N-terminal sequence of PDInhibitor showed a high level of identity with those of the Kunitz family. PDInhibitor was found to be active at pH values ranging from 5.0 to 11.0, with maximal activity at pH 9.0. It was also fully active at 50 °C and maintained 90% of its stability at over 55 °C. The thermostability of the PDInhibitor was clearly enhanced by CaCl<sub>2</sub> and sorbitol, whereas the presence of Ca<sup>2+</sup> and Zn<sup>2+</sup> ions, Sodium taurodeoxycholate (NaTDC), Sodium dodecyl sulfate (SDS), Dithiothreitol (DTT), and β-ME dramatically improved the inhibitory activity. A remarkable affinity of the protease inhibitor with available important therapeutic proteases (elastase and trypsin) was observed. PDInhibitor also acted as a potent inhibitor of commercial proteases from <i>Aspergillus oryzae</i> and of Proteinase K. The inhibitor displayed potent antimicrobial activity against gram+ and gram- bacteria and against fungal strains. Interestingly, PDInhibitor affected several human cancer cell lines, namely HCT-116, MDA-MB-231, and Lovo. Thus, it can be considered a potentially powerful therapeutic agent.