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Inhibition of HSV-1 ocular infection with morpholino oligomers targeting ICP0 and ICP27.

机译:靶向ICP0和ICP27的吗啉代低聚物对HSV-1眼部感染的抑制作用。

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摘要

Alternative therapies are needed for HSV-1 infections in patients refractory to treatment with Acyclovir (ACV) and its derivatives. Peptide-conjugated phosphorodiamidate morpholino oligomers (PPMO) are single-stranded DNA analogues that enter cells readily and reduce target gene expression through steric blockage of complementary RNA. When applied before or soon after infection PPMO targeting the translation-start-site regions of HSV-1 ICP0 or ICP27 mRNA reduced HSV-1 plaque formation by 70-98% in vitro. The ICP0 PPMO also reduced ACV-resistant HSV-1 (strain 615.9) plaque formation by 70-90%, while an equivalent dose of ACV produced only 40-50% inhibition when the treatment was applied between 1 and 3hpi. Seven daily topical treatments of 100microg ICP0 PPMO caused no gross or microscopic damage to the corneas of uninfected mice. Topical application of 10microg ICP0 PPMO to the eyes of HSV-1 infected mice reduced the incidence of eye disease by 37.5-50% compared to controls. This study demonstrates that topically applied PPMO holds promise as an antiviral drug candidate against HSV-1 ocular infection.
机译:对于使用阿昔洛韦(ACV)及其衍生物难以治疗的患者,HSV-1感染需要替代疗法。肽缀合的二氨基磷酸二酰胺吗啉代寡聚体(PPMO)是单链DNA类似物,可轻易进入细胞并通过位阻互补RNA减少目标基因的表达。当在感染前或感染后不久应用PPMO靶向HSV-1 ICP0或ICP27 mRNA的翻译起始位点区域时,体外可降低70-98%的HSV-1斑块形成。 ICP0 PPMO还可以将抗ACV的HSV-1(615.9株)噬菌斑形成减少70-90%,而当等剂量的ACV在治疗后1至3hpi内仅产生40-50%的抑制作用。每天进行100microg ICP0 PPMO的七次局部治疗不会对未感染小鼠的角膜造成任何严重或微观的损害。与对照组相比,向HSV-1感染小鼠的眼睛局部施用10microg ICP0 PPMO可将眼部疾病的发生率降低37.5-50%。这项研究表明,局部应用PPMO有望作为抗HSV-1眼部感染的抗病毒药物。

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