Mousavi-Jazi Mehrdad, Schloss Lottie, Wahren Britta, Brytting Maria
Swedish Institute for Infectious Disease Control, Microbiology and Tumorbiology Center, Karolinska Institute, Stockholm, Sweden.
J Clin Virol. 2003 Apr;26(3):301-6. doi: 10.1016/s1386-6532(02)00046-x.
In vitro selection of viruses with decreased drug susceptibility is a useful tool for mapping drug resistance-associated alterations, evaluating cross-resistance profiles, and elucidating molecular mechanisms of antiviral activity.
To provide data on mechanisms of selective drug action and features of drug resistance that may be clinically important.
Foscarnet (PFA) and ganciclovir (GCV) were used to induce mutants of the human cytomegalovirus (HCMV) Towne strain.
Three new mutations, selected in the presence of PFA, were identified with single base substitutions resulting in T419M, Q578H, and L773V in conserved regions of the HCMV DNA polymerase. None of these mutations have been reported previously. These mutations conferred resistance to PFA but did not change the susceptibility to GCV. A mutant was selected in the presence of GCV. This GCV-selected mutant had no mutation in the UL54 but had an amino acid alteration at codon M460V of UL97, which conferred resistance to GCV. All the mutants had the same growth phenotype as the parental laboratory strain Towne.
We have determined three novel alterations in HCMV DNA polymerase inducing reduced susceptibility to PFA. None of these alterations changed the growth phenotype of the parental virus.
体外筛选药物敏感性降低的病毒是一种有用的工具,可用于绘制耐药性相关改变、评估交叉耐药谱以及阐明抗病毒活性的分子机制。
提供有关选择性药物作用机制和可能具有临床重要性的耐药特征的数据。
膦甲酸钠(PFA)和更昔洛韦(GCV)用于诱导人巨细胞病毒(HCMV)Towne株的突变体。
在PFA存在下筛选出的三个新突变被鉴定为单碱基替换,导致HCMV DNA聚合酶保守区域中的T419M、Q578H和L773V。这些突变以前均未被报道过。这些突变赋予了对PFA的抗性,但未改变对GCV的敏感性。在GCV存在下筛选出一个突变体。这个GCV筛选出的突变体在UL54中没有突变,但在UL97的密码子M460V处有一个氨基酸改变,赋予了对GCV的抗性。所有突变体的生长表型与亲本实验室株Towne相同。
我们确定了HCMV DNA聚合酶中的三个新改变,导致对PFA的敏感性降低。这些改变均未改变亲本病毒的生长表型。
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