Evaluation of Four Humanized NOD-Derived Mouse Models for Dengue Virus-2 Infection

Author:

Gutierrez-Barbosa Hernando12ORCID,Medina-Moreno Sandra1,Perdomo-Celis Federico3ORCID,Davis Harry1,Chua Joel V.1ORCID,Zapata Juan C.1ORCID

Affiliation:

1. Institute of Human Virology, University of Maryland School of Medicine, Baltimore, MD 21201, USA

2. Facultad de Biología, Universidad de Antioquia, Bogotá 050010, Colombia

3. Instituto de Genética Humana, Facultad de Medicina, Pontificia Universidad Javeriana, Bogotá 110231, Colombia

Abstract

Dengue is a significant public health problem with no specific viral treatment. One of the main challenges in studying dengue is the lack of adequate animal models recapitulating human immune responses. Most studies on humanized mice use NOD-scid IL2R gamma null (NSG) mice, which exhibit poor hematopoiesis for some cell populations. This study compares three humanized (hu) NOD-derived mouse models for dengue virus-2 (DENV-2) infection in the context of human cytokine expression. Three mouse strains (hu-NSG, hu-EXL, and hu-SGM3) received xenotransplants of human CD34+ fetal cord blood cells from a single donor, and one mouse strain received human peripheral blood mononuclear cells (hu-SGM3-PBMCs). All models exhibited infectious viruses in blood confirmed by plaque assay, but mice expressing human cytokines showed higher viremia compared to conventional NSG mice. The hu-SGM3-PBMCs model developed lethal infections, showing a significant increase in viremia and clinical signs. A detectable human cytokine response was observed in all the DENV-2-infected humanized mouse models. In conclusion, humanized NOD-derived mouse models expressing human cytokines offer a relevant platform for the study of dengue pathogenesis and antiviral therapies.

Funder

the Institute of Human Virology, University of Maryland School of Medicine

Publisher

MDPI AG

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