AI Article Synopsis

  • - RNase He1, derived from the mushroom Hericium erinaceus, shares a high similarity with RNase Po1 from Pleurotus ostreatus, particularly in the crucial catalytic sequence, but has a lower optimal pH for activity and minimal effect on human tumor cells.
  • - Researchers created RNase He1 mutants by changing specific amino acids to investigate ways to enhance its pH and antitumor properties, using RNase Po1 as a template.
  • - The modified recombinant RNase He1 exhibited improved enzyme activity and successfully inhibited the growth of human leukemia cells, showcasing its potential for developing cancer-fighting treatments based on RNase activity.

Article Abstract

RNase He1 from Hericium erinaceus, a member of the RNase T1 family, has high identity with RNase Po1 from Pleurotus ostreatus with complete conservation of the catalytic sequence. However, the optimal pH for RNase He1 activity is lower than that of RNase Po1, and the enzyme shows little inhibition of human tumor cell proliferation. Hence, to investigate the potential antitumor activity of recombinant RNase He1 and to possibly enhance its optimum pH, we generated RNase He1 mutants by replacing 12 Asn/Gln residues with Asp/Glu residues; the amino acid sequence of RNase Po1 was taken as reference. These mutants were then expressed in Escherichia coli. Using site-directed mutagenesis, we successfully modified the optimal pH for enzyme activity and generated a recombinant RNase He1 that inhibited the proliferation of cells in the human leukemia cell line. These properties are extremely important in the production of anticancer biologics that are based on RNase activity.

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Source
http://dx.doi.org/10.1080/09168451.2014.972327DOI Listing

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