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Broad-spectrum and virus-specific nucleic acid-based antivirals against influenza.

机译:广谱和基于病毒的核酸特异性抗流感病毒。

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摘要

Rapid increase in drug-resistant influenza virus isolates, and pandemic threat posed by highly pathogenic avian influenza A and swine flu viruses provide clear and compelling reasons for fast tracking development of novel antiviral drugs. Nucleic acid-based drugs represent a promising class of novel antiviral agents that can be designed to target various seasonal, pandemic and avian influenza viruses. Nucleic acids can be designed to elicit broad-spectrum antiviral responses in the host, by suppressing viral gene expression, or by inducing cleavage or degradation of viral RNA. Immunomodulating nucleic acids, such as double stranded RNA and CpG oligonucleotides, can be potent anti-influenza agents that work by eliciting protective innate and adaptive immunity in the host. By activating the toll-like receptor signaling pathways, these drugs can activate the host's antiviral and inflammatory defenses to combat influenza viruses. Antisense oligonucleotides, small interfering RNAs (siRNA), and nanoRNAs represent sequence specific gene-silencing approaches that could be deployed to suppress or inhibit viral protein gene expression. Lastly, catalytic nucleic acids such as DNAzymes and/or ribozymes can suppress viral replication by repeatedly cleaving viral mRNAs and template RNAs. In summary, nucleic acid-based antiviral agents are versatile, diverse and could complement existing antiviral drugs in combating influenza.
机译:耐药流感病毒分离株的迅速增加,以及高致病性甲型禽流感和猪流感病毒构成的大流行威胁,为快速跟踪新型抗病毒药物的开发提供了明确而令人信服的理由。基于核酸的药物代表了有前途的一类新型抗病毒药,可以设计成针对各种季节性,大流行和禽流感病毒。可通过抑制病毒基因表达或诱导病毒RNA裂解或降解来设计核酸,以在宿主中引发广谱抗病毒反应。免疫调节核酸,例如双链RNA和CpG寡核苷酸,可能是有效的抗流感药物,可通过在宿主体内引起保护性先天性和适应性免疫而发挥作用。通过激活toll样受体信号传导途径,这些药物可以激活宿主的抗病毒和炎性防御能力,以对抗流感病毒。反义寡核苷酸,小干扰RNA(siRNA)和nanoRNA代表了序列特异性基因沉默方法,可用于抑制或抑制病毒蛋白基因表达。最后,催化核酸(例如DNA酶和/或核酶)可以通过反复切割病毒mRNA和模板RNA来抑制病毒复制。总之,基于核酸的抗病毒剂用途广泛,种类繁多,并且可以补充现有的抗病毒药物来对抗流感。

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