局部用替诺福韦可预防感染沙眼衣原体和阴道毛滴虫的猕猴发生阴道猿猴免疫缺陷病毒感染。

Topical tenofovir protects against vaginal simian HIV infection in macaques coinfected with Chlamydia trachomatis and Trichomonas vaginalis.

作者信息

Makarova Natalia, Henning Tara, Taylor Andrew, Dinh Chuong, Lipscomb Jonathan, Aubert Rachael, Hanson Debra, Phillips Christi, Papp John, Mitchell James, McNicholl Janet, Garcia-Lerma Gerardo J, Heneine Walid, Kersh Ellen, Dobard Charles

机构信息

aLaboratory Branch, Division of HIV/AIDS Prevention bDivision of Sexually Transmitted Disease Prevention, Centers of Disease Control and Prevention (CDC) Atlanta, Georgia cTotal Solutions, Inc., Madison, Alabama, USA.

出版信息

AIDS. 2017 Mar 27;31(6):745-752. doi: 10.1097/QAD.0000000000001389.

DOI:10.1097/QAD.0000000000001389

PMID:28060011

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC11513895/

Abstract

BACKGROUND

Chlamydia trachomatis and Trichomonas vaginalis, two prevalent sexually transmitted infections, are known to increase HIV risk in women and could potentially diminish preexposure prophylaxis efficacy, particularly for topical interventions that rely on local protection. We investigated in macaques whether coinfection with Chlamydia trachomatis/Trichomonas vaginalis reduces protection by vaginal tenofovir (TFV) gel.

METHODS

Vaginal TFV gel dosing previously shown to provide 100 or 74% protection when applied either 30 min or 3 days before simian HIV(SHIV) challenge was assessed in pigtailed macaques coinfected with Chlamydia trachomatis/Trichomonas vaginalis and challenged twice weekly with SHIV162p3 for up to 10 weeks (two menstrual cycles). Three groups of six macaques received either placebo or 1% TFV gel 30 min or 3 days before each SHIV challenge. We additionally assessed TFV and TFV diphosphate concentrations in plasma and vaginal tissues in Chlamydia trachomatis/Trichomonas vaginalis coinfected (n = 4) and uninfected (n = 4) macaques.

RESULTS

Chlamydia trachomatis/Trichomonas vaginalis coinfections were maintained during the SHIV challenge period. All macaques that received placebo gel were SHIV infected after a median of seven challenges (one menstrual cycle). In contrast, no infections were observed in macaques treated with TFV gel 30 min before SHIV challenge (P < 0.001). Efficacy was reduced to 60% when TFV gel was applied 3 days before SHIV challenge (P = 0.07). Plasma TFV and TFV diphosphate concentrations in tissues and vaginal lymphocytes were significantly higher in Chlamydia trachomatis/Trichomonas vaginalis coinfected compared with Chlamydia trachomatis/Trichomonas vaginalis uninfected macaques.

CONCLUSION

Our findings in this model suggest that Chlamydia trachomatis/Trichomonas vaginalis coinfection may have little or no impact on the efficacy of highly effective topical TFV modalities and highlight a significant modulation of TFV pharmacokinetics.

摘要

背景

沙眼衣原体和阴道毛滴虫是两种常见的性传播感染病原体，已知它们会增加女性感染艾滋病毒的风险，并可能降低暴露前预防的效果，特别是对于依赖局部保护的局部干预措施。我们在猕猴中研究了沙眼衣原体/阴道毛滴虫合并感染是否会降低阴道替诺福韦（TFV）凝胶的保护作用。

方法

在感染沙眼衣原体/阴道毛滴虫的猪尾猕猴中，评估了先前显示在猿猴免疫缺陷病毒（SHIV）攻击前30分钟或3天应用时可提供100%或74%保护作用的阴道TFV凝胶给药情况，这些猕猴每周接受两次SHIV162p3攻击，持续长达10周（两个月经周期）。三组六只猕猴在每次SHIV攻击前30分钟或3天分别接受安慰剂或1%TFV凝胶。我们还评估了感染沙眼衣原体/阴道毛滴虫（n = 4）和未感染（n = 4）的猕猴血浆和阴道组织中的TFV和二磷酸替诺福韦浓度。

结果

在SHIV攻击期间，维持了沙眼衣原体/阴道毛滴虫合并感染。所有接受安慰剂凝胶的猕猴在中位七次攻击（一个月经周期）后均感染了SHIV。相比之下，在SHIV攻击前30分钟用TFV凝胶治疗的猕猴未观察到感染（P < 0.001）。当在SHIV攻击前3天应用TFV凝胶时，疗效降至60%（P = 0.07）。与未感染沙眼衣原体/阴道毛滴虫的猕猴相比，感染沙眼衣原体/阴道毛滴虫的猕猴组织和阴道淋巴细胞中的血浆TFV和二磷酸替诺福韦浓度显著更高。

结论

我们在该模型中的发现表明，沙眼衣原体/阴道毛滴虫合并感染可能对高效局部TFV治疗方式的疗效影响很小或没有影响，并突出了TFV药代动力学的显著调节。

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