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Amino Acid Substitutions in the Thymidine Kinase Gene of Induced Acyclovir-Resistant Herpes Simplex Virus Type 1

机译:诱导诱导的Acyclovir耐药疱疹病毒型肾小序激酶基因的氨基酸取代1

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Acyclovir (ACV) is an antiviral drug of choice in healthcare setting to treat infections caused by herpes viruses, including, but not limited to genital herpes, cold sores, shingles and chicken pox. Acyclovir resistance has emerged significantly due to extensive use and misuse of this antiviral in human, especially in immunocompromised patients. However, it remains unclear about the amino acid substitutions in thymidine (TK) gene, which specifically confer the resistance-associated mutation in herpes simplex virus. Hence, acyclovir-resistant HSV-1 was selected at high concentration (2.0 - 4.5 μg/mL), and the TK-gene was subjected to sequencing and genotypic characterization. Genotypic sequences comparison was done using HSV-1 17 (GenBank Accesion no. X14112) for resistance-associated mutation determination whereas HSV-1 KOS, HSV-1 473/08 and HSV clinical isolates sequences were used for polymorphismassociated mutation. The result showed that amino acid substitutions at the non-conserved region (UKM-1: Gln34Lys, UKM-2: Arg32Ser & UKM-5: Arg32Cys) and ATP-binding site (UKM-3: Tyr53End & UKM-4: Ile54Leu) of the TKgene. These discoveries play an important role to extend another dimension to the evolution of acyclovir-resistant HSV-1 and suggest that selection at high ACV concentration induced ACV-resistant HSV-1 evolution. These findings also expand the knowledge on the type of mutations among acyclovir-resistant HSV-1. In conclusion, HSV-1 showed multiple strategies to exhibit acyclovir resistance, including amino acid substitutions in the TK gene.
机译:Acyclovir(ACV)是医疗保健设定中的抗病毒药物,以治疗疱疹病毒引起的感染,包括但不限于生殖器疱疹,唇疱疹,带状疱疹和鸡痘。由于在人类的广泛使用和滥用这种抗病毒,尤其是免疫因素患者,Acyclovir抗性显着出现。然而,它仍然不清楚胸苷(TK)基因中的氨基酸取代,其在单纯疱疹病毒中特别赋予抗性相关突变。因此,在高浓度(2.0-4.5μg/ ml)中选择抗抗菌致抗性HSV-1,并且TK-基因经受测序和基因型表征。基因型序列使用HSV-1 17(Genbank Accesion No.X14112)进行对抗性相关的突变测定进行的,而HSV-1 KOS,HSV-1 473/08和HSV临床分离序列用于多晶类突变。结果表明,非保守区氨基酸取代(UKM-1:GLN34LY,UKM-2:ARG32SER&UKM-5:ARG32CYS)和ATP结合位点(UKM-3:TYR53END&UKM-4:ILE54LEU) Tkgene。这些发现发挥着重要作用,使另一尺寸延伸到Acyclovir抗性HSV-1的演变,并表明在高ACV浓度下选择诱导ACV抗性HSV-1进化。这些调查结果还扩展了抗性抗性HSV-1之间的突变类型的知识。总之,HSV-1显示出具有Acyclovir抗性的多种策略,包括TK基因中的氨基酸取代。

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