Benjamin Atkinson’s research while affiliated with University of Maryland, Baltimore and other places

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Publications (1)


Humanized mouse models for preclinical evaluation of HIV cure strategies
  • Literature Review

May 2022

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25 Reads

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3 Citations

Aids Reviews

Sally Fraker

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Benjamin Atkinson

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Alonso Heredia

Although the world is currently focused on the COVID-19 pandemic, HIV/AIDS remains a significant threat to public health. To date, the HIV/AIDS pandemic has claimed the lives of over 36 million people, while nearly 38 million people are currently living with the virus. Despite the undeniable success of antiretroviral therapy (ART) in controlling HIV, the medications are not curative. Soon after initial infection, HIV integrates into the genome of infected cells as a provirus, primarily, within CD4+ T lymphocytes and tissue macrophages. When not actively transcribed, the provirus is referred to as a latent reservoir because it is hidden to the immune system and ART. Following ART discontinuation, HIV may emerge from the replication-competent proviruses and resumes the infection of healthy cells. Thus, these latent reservoirs are a major obstacle to an HIV cure, and their removal remains a priority. A vital aspect in the development of curative therapies is the demonstration of efficacy in an animal model, such as the humanized mouse model. Therefore, optimization, standardization, and validation of the humanized mouse model are a priority. The purpose of this review article is to provide an update on existing humanized mouse models, highlighting the advantages and disadvantages of each as they pertain to HIV cure studies and to review the approaches to curative therapies that are under investigation.

Citations (1)


... These studies mirror reports of individuals infected with Nef-defective HIV-1 in which viral loads remain low in the absence of antiretroviral therapy (Deacon et al., 1995;Kirchhoff et al., 1995;Zou et al., 2012). Similar observations have been made in HIV-1 infected humanized immune system mice, in which immunodeficient animals are reconstituted with human CD4 + T cells and other host cell targets for HIV-1 (Chen et al., 2022;Fraker et al., 2022). In these animals, wild-type HIV-1 infection results in plasma viremia and depletion of CD4 + T cells while Nef-defective HIV-1 replicates poorly and does not cause CD4 + T cell loss (Watkins et al., 2015;Zou et al., 2012). ...

Reference:

PROTAC-mediated Degradation of HIV-1 Nef Efficiently Restores Cell-surface CD4 and MHC-I Expression and Blocks HIV-1 Replication
Humanized mouse models for preclinical evaluation of HIV cure strategies
  • Citing Article
  • May 2022

Aids Reviews