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一种与单纯疱疹病毒1型立即早期前体mRNA 4和5的剪接连接互补的寡聚(核苷甲基膦酸酯)的抗病毒作用。

Antiviral effect of an oligo(nucleoside methylphosphonate) complementary to the splice junction of herpes simplex virus type 1 immediate early pre-mRNAs 4 and 5.

作者信息

Smith C C, Aurelian L, Reddy M P, Miller P S, Ts'o P O

出版信息

Proc Natl Acad Sci U S A. 1986 May;83(9):2787-91. doi: 10.1073/pnas.83.9.2787.

Abstract

Selective inhibition of regulatory immediate early (IE) genes of herpes simplex virus type 1 (HSV-1) should inhibit virus growth. Treatment of HSV-1-infected cells with the oligo(nucleoside methylphosphonate) d(TpCCTCCTG) (deoxynucleoside methylphosphonate residues in italic), which is complementary to the acceptor splice junction of HSV-1 IE pre-mRNA 4 and 5, before (1-24 hr) or at the time of infection caused a dose-dependent inhibition in virus replication. Virus titers were decreased 50% and 90% in cells treated with 25 microM and 75 microM oligomer, respectively; at 300 microM, a 99% reduction in virus production was observed. Viral DNA synthesis was reduced 70-75% and there was a 90% reduction in synthesis of viral proteins, including other IE species and viral functional (130-kDa major DNA-binding) and structural (glycoprotein gB) proteins. In the same concentration range, d(TpCCTCCTG) caused a minimal reduction (0-30%) in protein synthesis and growth rates (less than 40%) of uninfected cells. The data suggest that oligo(nucleoside methylphosphonate)s may be effective in antiviral chemotherapy.

摘要

对单纯疱疹病毒1型(HSV-1)调节性即刻早期(IE)基因的选择性抑制应能抑制病毒生长。在感染前(1 - 24小时)或感染时,用与HSV-1 IE前体mRNA 4和5的受体剪接接头互补的寡聚(核苷甲基膦酸酯)d(TpCCTCCTG)(斜体为脱氧核苷甲基膦酸酯残基)处理HSV-1感染的细胞,会导致病毒复制呈剂量依赖性抑制。用25 microM和75 microM寡聚物处理的细胞中病毒滴度分别降低了50%和90%;在300 microM时,观察到病毒产量降低了99%。病毒DNA合成减少了70 - 75%,包括其他IE种类以及病毒功能性(130 kDa主要DNA结合)和结构性(糖蛋白gB)蛋白在内的病毒蛋白合成减少了90%。在相同浓度范围内,d(TpCCTCCTG)对未感染细胞的蛋白质合成和生长速率造成的降低最小(0 - 30%)。数据表明寡聚(核苷甲基膦酸酯)可能在抗病毒化疗中有效。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b869/323391/c71025ee818e/pnas00313-0019-a.jpg

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