Modeling HIV infection and therapies in humanized mice

Nischang, Marc; Gers-Huber, Gustavo; Audigé, Annette; Akkina, Ramesh; Speck, Roberto F.

doi:10.4414/smw.2012.13618

Cited by 23 publications

(18 citation statements)

References 134 publications

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“…A second approach was to genetically engineer rodents so that their cells express the human version of the CD4 receptor and the chemokine co-receptors to which HIV-1 binds to enter target cells (Nischang, Gers-Huber et al 2012). The envelope glycoprotein 120 (gp120) on the surface of the HIV-1 virus interacts with target cell receptors to begin the cell entry process.…”

Section: Animal Models Of Hiv-1mentioning

confidence: 99%

The HIV-1 transgenic rat model of neuroHIV

Vigorito

Connaghan

Chang

2015

Brain, Behavior, and Immunity

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Despite the ability of current combination anti-retroviral therapy (cART) to limit the progression of HIV-1 to AIDS, HIV-positive individuals continue to experience neuroHIV in the form of HIV-associated neurological disorders (HAND), which can range from subtle to substantial neurocognitive impairment. NeuroHIV may also influence substance use, abuse, and dependence in HIV-positive individuals. Because of the nature of the virus, variables such as mental health co-morbidities make it difficult to study the interaction between HIV and substance abuse in human populations. Several rodent models have been developed in an attempt to study the transmission and pathogenesis of the HIV-1 virus. The HIV-1 transgenic (HIV-1Tg) rat is a reliable model of neuroHIV because it mimics the condition of HIV-infected patients on cART. Research using this model supports the hypothesis that the presence of HIV-1 viral proteins in the central nervous system increases the sensitivity and susceptibility of HIV-positive individuals to substance abuse.

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Section: Animal Models Of Hiv-1mentioning

confidence: 99%

The HIV-1 transgenic rat model of neuroHIV

Vigorito

Connaghan

Chang

2015

Brain, Behavior, and Immunity

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“…The hu-HSC humanized mouse model such as RAG-hu employs engraftment of human hematopoietic stem cells (HSC) into newborn immunodeficient (Rag1 −/− or Rag2 −/− γc −/− ) mice whereas the BLT mouse model is derived by transplantation of human fetal thymus tissue, liver tissue and HSC (Akkina, 2013; Denton and Garcia, 2011). Both models harbor human immune cells in mucosal sites such as vaginal and rectal tissue, and are susceptible to HIV infection via these routes thus mimicking key aspects of viral mucosal transmission (Berges et al, 2008; Denton and Garcia, 2012; Nischang et al, 2012). Both topical and systemic PrEP strategies employing ARVs have been successfully tested using these models (Chateau et al, 2013; Denton et al, 2011; Neff et al, 2011; Neff et al, 2010).…”

Section: Introductionmentioning

confidence: 99%

HIV pre-exposure prophylaxis: Mucosal tissue drug distribution of RT inhibitor Tenofovir and entry inhibitor Maraviroc in a humanized mouse model

Veselinović¹,

Yang²,

LeCureux³

et al. 2014

Virology

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Pre-exposure prophylaxis (PrEP) strategies utilizing anti-retroviral drugs show considerable promise for HIV prevention. However there is insufficient pharmacokinetic (PK) data on drug concentrations required for protection at the relevant mucosal tissues where the infection is initiated. Here we evaluated the utility of a humanized mouse model to derive PK data on two leading drugs, the RT inhibitor tenofovir (TFV) and CCR5 inhibitor maraviroc (MVC). Following oral dosing, both the drugs and the intracellular active TFV-diphosphate could be detected in vaginal, rectal and intestinal tissues. The drug exposures (AUC24hr) were found to be higher in vaginal tissue compared to plasma with even higher levels detected in rectal and intestinal tissues. The overall trends of drug concentrations seen in humanized mice reflect those seen in the human thus establishing the utility of this model complementing the present non-human primate (NHP) models for future pre-clinical evaluations of promising HIV PrEP drug candidates.

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“…Humanized (hu) mice, which are generated by the transplantation of CD34 ϩ cells, are of particular value in this context. These mice excel in their multilineage hematopoiesis (10), are highly permissive to HIV (11), and allow for the gene engineering of human CD34 ϩ cells before transplantation (12). Indeed, various anti-HIV moieties have been investigated in hu mice as gene therapy options, including cellular factors, boosting the anti-HIV immune response, and the HIV genome itself (12).…”

mentioning

confidence: 99%

Lentivector Knockdown of CCR5 in Hematopoietic Stem and Progenitor Cells Confers Functional and Persistent HIV-1 Resistance in Humanized Mice

Myburgh

Ivic

Pepper

et al. 2015

J Virol

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Gene-engineered CD34؉ hematopoietic stem and progenitor cells (HSPCs) can be used to generate an HIV-1-resistant immune system. However, a certain threshold of transduced HSPCs might be required for transplantation into mice for creating an HIVresistant immune system. In this study, we combined CCR5 knockdown by a highly efficient microRNA (miRNA) lentivector with pretransplantation selection of transduced HSPCs to obtain a rather pure population of gene engineered CD34

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Modeling HIV infection and therapies in humanized mice

Cited by 23 publications

References 134 publications

The HIV-1 transgenic rat model of neuroHIV

The HIV-1 transgenic rat model of neuroHIV

HIV pre-exposure prophylaxis: Mucosal tissue drug distribution of RT inhibitor Tenofovir and entry inhibitor Maraviroc in a humanized mouse model

Lentivector Knockdown of CCR5 in Hematopoietic Stem and Progenitor Cells Confers Functional and Persistent HIV-1 Resistance in Humanized Mice

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