<span style="font-family:""><span style="font-family:Verdana;">For just about 30 years, researchers have considered the likelihood to utilize </span><span style="font...<span style="font-family:""><span style="font-family:Verdana;">For just about 30 years, researchers have considered the likelihood to utilize </span><span style="font-family:Verdana;">nucleic acids as antiviral therapeutics. In principle, small single-stranded</span><span style="font-family:Verdana;"> nuc</span><span style="font-family:Verdana;">leotide sequence (oligonucleotide) could hybridize to a particular gene or</span><span style="font-family:Verdana;"> mes</span><span style="font-family:Verdana;">senger RNA and diminish transcription or translation, respectively, in this</span><span style="font-family:Verdana;"> manner decreasing the amount of protein that is synthesized. Until now, an incredible number of antisense oligonucleotides, double-stranded oligonucleotides, aptamers, ribozymes, deoxyribozymes, interfering RNAs, chimeric RNA</span></span><span style="font-family:Verdana;">-</span><span style="font-family:""><span style="font-family:Verdana;">DNA molecules, antibody genes has been created artificially and ap</span><span style="font-family:Verdana;">plied effectively for comprehension and manipulating biological processe</span><span style="font-family:Verdana;">s and in clinical preliminaries to treat a variety of diseases. Their versatility and potency make them similarly fit candidates for fighting viral infections. However, troubles with their efficiency, off-target effects, toxicity, delivery, and stability halted the development of nucleic acid-based therapeutics that can be utilized in the clinic. The potential for nucleic acid therapeutic agents is significant and is quite recently beginning to be realized. In this review, we have summarized some of the recent advancements made in the area of nucleic acid based therapeutics and focused on the methods of their delivery and associated challenges.展开更多
文摘<span style="font-family:""><span style="font-family:Verdana;">For just about 30 years, researchers have considered the likelihood to utilize </span><span style="font-family:Verdana;">nucleic acids as antiviral therapeutics. In principle, small single-stranded</span><span style="font-family:Verdana;"> nuc</span><span style="font-family:Verdana;">leotide sequence (oligonucleotide) could hybridize to a particular gene or</span><span style="font-family:Verdana;"> mes</span><span style="font-family:Verdana;">senger RNA and diminish transcription or translation, respectively, in this</span><span style="font-family:Verdana;"> manner decreasing the amount of protein that is synthesized. Until now, an incredible number of antisense oligonucleotides, double-stranded oligonucleotides, aptamers, ribozymes, deoxyribozymes, interfering RNAs, chimeric RNA</span></span><span style="font-family:Verdana;">-</span><span style="font-family:""><span style="font-family:Verdana;">DNA molecules, antibody genes has been created artificially and ap</span><span style="font-family:Verdana;">plied effectively for comprehension and manipulating biological processe</span><span style="font-family:Verdana;">s and in clinical preliminaries to treat a variety of diseases. Their versatility and potency make them similarly fit candidates for fighting viral infections. However, troubles with their efficiency, off-target effects, toxicity, delivery, and stability halted the development of nucleic acid-based therapeutics that can be utilized in the clinic. The potential for nucleic acid therapeutic agents is significant and is quite recently beginning to be realized. In this review, we have summarized some of the recent advancements made in the area of nucleic acid based therapeutics and focused on the methods of their delivery and associated challenges.
