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对接受抗病毒药物治疗的猫进行1型猫疱疹病毒突变及耐药性发展的监测。

Surveillance for feline herpesvirus type 1 mutation and development of resistance in cats treated with antiviral medications.

作者信息

Lewin Andrew C, Ineck Nikole E, Mironovich Melanie A, Marino Morgan E, Liu Chin-Chi, Emelogu Ugochi, Mills Erinn P, Camacho-Luna Pilar, Carter Renee T

机构信息

Department of Veterinary Clinical Sciences, School of Veterinary Medicine, Louisiana State University, Baton Rouge, LA, United States.

出版信息

Front Vet Sci. 2023 May 18;10:1197249. doi: 10.3389/fvets.2023.1197249. eCollection 2023.

Abstract

Feline herpesvirus type 1 (FHV-1) commonly causes ocular surface disease in cats and is treated with antiviral medications targeting viral DNA polymerase (UL30/42). Herein, we describe a method to assess the FHV-1 genome for mutation development and to assess the functional impact of mutations, if present. Fourteen shelter-housed domestic cats with FHV-1 ocular surface disease were assigned to one of four treatment groups: placebo ( = 3), cidofovir 0.5% ophthalmic solution ( = 3), famciclovir oral solution ( = 5), or ganciclovir 0.15% ophthalmic solution ( = 3). Swabs were collected before (day 1) and after (day 8) 1 week of twice-daily treatments to isolate viable FHV-1. Viral DNA was extracted for sequencing using Illumina MiSeq with subsequent genomic variant detection between paired day 1 and day 8 isolates. Plaque reduction assay was performed on paired isolates demonstrating non-synonymous variants. A total of 171 synonymous and 3 non-synonymous variants were identified in day 8 isolates. No variants were detected in viral UL23, UL30, or UL42 genes. Variant totals were not statistically different in animals receiving antiviral or placebo ( = 0.4997). A day 8 isolate from each antiviral treatment group contained a single non-synonymous variant in ICP4 (transcriptional regulator). These 3 isolates demonstrated no evidence of functional antiviral resistance when IC was assessed. Most (10/14 pairs) day 1 and 8 viral isolate pairs from the same host animal were near-identical. While functional variants were not detected in this small sample, these techniques can be replicated to assess FHV-1 isolates suspected of having developed resistance to antiviral medications.

摘要

猫疱疹病毒1型(FHV-1)通常会引发猫的眼表疾病,针对该病毒的治疗采用靶向病毒DNA聚合酶(UL30/42)的抗病毒药物。在此,我们描述了一种评估FHV-1基因组突变发展情况以及评估突变(若存在)功能影响的方法。14只患有FHV-1眼表疾病的收容所饲养家猫被分配到四个治疗组之一:安慰剂组(n = 3)、0.5%西多福韦眼药水组(n = 3)、泛昔洛韦口服溶液组(n = 5)或0.15%更昔洛韦眼药水组(n = 3)。在每日两次治疗1周前(第1天)和治疗1周后(第8天)采集拭子以分离存活的FHV-1。提取病毒DNA用于使用Illumina MiSeq进行测序,随后检测第1天和第8天配对分离株之间的基因组变异。对显示非同义变异的配对分离株进行蚀斑减少试验。在第8天的分离株中总共鉴定出171个同义变异和3个非同义变异。在病毒UL23、UL30或UL42基因中未检测到变异。接受抗病毒药物或安慰剂的动物的变异总数无统计学差异(P = 0.4997)。每个抗病毒治疗组的第8天分离株在ICP4(转录调节因子)中均含有一个单一的非同义变异。在评估IC时,这3个分离株未显示出功能性抗病毒耐药的证据。来自同一宿主动物的大多数(10/14对)第1天和第8天病毒分离株对几乎完全相同。虽然在这个小样本中未检测到功能性变异,但这些技术可重复用于评估怀疑对抗病毒药物产生耐药性的FHV-1分离株。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/45d7/10232796/b8f657a98ce9/fvets-10-1197249-g001.jpg

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