AI Article Synopsis

  • Researchers designed a chimeric DNA-RNA hammerhead ribozyme targeting SARS-CoV based on a sequence from mouse hepatitis virus (MHV) to develop a specific treatment for SARS.
  • The ribozyme successfully cleaved MHV and SARS-CoV RNA in laboratory tests and inhibited MHV multiplication by approximately 60% in DBT cells, showcasing its effectiveness.
  • The study suggests that this synthetic ribozyme could be a potential treatment option for managing SARS infections.

Article Abstract

Objective: Severe acute respiratory syndrome (SARS) is a severe pulmonary infectious disease caused by a novel coronavirus. To develop an effective and specific medicine targeting the SARS-coronavirus (CoV), a chimeric DNA-RNA hammerhead ribozyme was designed and synthesized using a sequence homologous with the mouse hepatitis virus (MHV).

Method: Chimeric DNA-RNA hammerhead ribozyme targeting MHV and SARS-CoV were designed and synthesized.To confirm its activity, in vitro cleavage reactions were performed with the synthesized ribozyme. Effects of the chimeric ribozyme were evaluated on multiplication of MHV. Effects of the chimeric ribozyme on expression of SARS-CoV were evaluated in cultured 3T3 cells.

Result: The synthetic ribozyme cleaved the synthetic target MHV and SARS-CoV RNA into fragments of predicted length. The chimeric DNA-RNA hammerhead ribozyme targeting SARS-CoV significantly inhibited multiplication of MHV in DBT cells by about 60%. The chimeric DNA-RNA hammerhead ribozyme targeting SARS-CoV significantly inhibited the expression of SARS-CoV RNA in 3T3 cells transfected with the recombinant plasmid. The chimeric DNA-RNA ribozyme targeting SARS-CoV significantly inhibited MHV viral activity and expression of recombinant SARS RNA in vitro.

Conclusion: These findings indicate that the synthetic chimeric DNA-RNA ribozyme could provide a feasible treatment for SARS.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC7179559PMC
http://dx.doi.org/10.1159/000215946DOI Listing

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