Humanized Mice Engrafted With Human HSC Only or HSC and Thymus Support Comparable HIV-1 Replication, Immunopathology, and Responses to ART and Immune Therapy

Humanized Mice Engrafted With Human HSC Only or HSC and Thymus Support Comparable HIV-1 Replication, Immunopathology, and Responses to ART and Immune Therapy

Immunodeficient mice reconstituted with human immune tissues and cells (humanized mice) are relevant and robust models for the study of HIV-1 infection, immunopathogenesis, and therapy. In this study, we performed a comprehensive comparison of human immune reconstitution and HIV-1 infection, immunop...

Full description

Bibliographic Details
Main Authors: Liang Cheng, Jianping Ma, Guangming Li, Lishan Su
Format: Article
Language:English
Published: Frontiers Media S.A. 2018-04-01
Series:Frontiers in Immunology
Subjects:
humanized mice
NRG-hu HSC
NRG-hu Thy/HSC
HIV-1 replication
HIV-1 immunopathology
combined antiretroviral therapy
Online Access:http://journal.frontiersin.org/article/10.3389/fimmu.2018.00817/full
id doaj-b1eebbfee6604a619b141ee85c019435
record_format Article
spelling doaj-b1eebbfee6604a619b141ee85c0194352020-11-24T21:33:59ZengFrontiers Media S.A.Frontiers in Immunology1664-32242018-04-01910.3389/fimmu.2018.00817343425Humanized Mice Engrafted With Human HSC Only or HSC and Thymus Support Comparable HIV-1 Replication, Immunopathology, and Responses to ART and Immune TherapyLiang Cheng0Liang Cheng1Jianping Ma2Guangming Li3Lishan Su4Lishan Su5Lineberger Comprehensive Cancer Center, University of North Carolina at Chapel Hill, Chapel Hill, NC, United StatesDepartment of Microbiology and Immunology, University of North Carolina at Chapel Hill, Chapel Hill, NC, United StatesLineberger Comprehensive Cancer Center, University of North Carolina at Chapel Hill, Chapel Hill, NC, United StatesLineberger Comprehensive Cancer Center, University of North Carolina at Chapel Hill, Chapel Hill, NC, United StatesLineberger Comprehensive Cancer Center, University of North Carolina at Chapel Hill, Chapel Hill, NC, United StatesDepartment of Microbiology and Immunology, University of North Carolina at Chapel Hill, Chapel Hill, NC, United StatesImmunodeficient mice reconstituted with human immune tissues and cells (humanized mice) are relevant and robust models for the study of HIV-1 infection, immunopathogenesis, and therapy. In this study, we performed a comprehensive comparison of human immune reconstitution and HIV-1 infection, immunopathogenesis and therapy between immunodeficient NOD/Rag2−/−/γc−/− (NRG) mice transplanted with human HSCs (NRG-hu HSC) and mice transplanted with HSCs and thymus fragments (NRG-hu Thy/HSC) from the same donors. We found that similar human lymphoid and myeloid lineages were reconstituted in NRG-hu HSC and NRG-hu Thy/HSC mice, with human T cells more predominantly reconstituted in NRG-hu Thy/HSC mice, while NRG-hu HSC mice supported more human B cells and myeloid cells reconstitution. HIV-1 replicated similarly and induced similar T cell depletion, immune activation, and dysfunction in NRG-hu HSC and NRG-hu Thy/HSC mice. Moreover, combined antiretroviral therapy (cART) inhibited HIV-1 replication efficiently with similar persistent HIV-1 reservoirs in both models. Finally, we found that blocking type-I interferon signaling under cART treatment transiently activated HIV-1 reservoirs, enhanced T cell recovery and reduced HIV-1 reservoirs in both HIV-1 infected NRG-hu HSC and NRG-hu Thy/HSC mice. In summary, we report that NRG-hu Thy/HSC and NRG-hu HSC mice support similar HIV-1 infection and similar HIV-1 immunopathology; and HIV-1 replication responds similarly to cART and IFNAR blockade therapies. The NRG-hu HSC mouse model reconstituted with human HSC only is sufficient for the study of HIV-1 infection, pathogenesis, and therapy.http://journal.frontiersin.org/article/10.3389/fimmu.2018.00817/fullhumanized miceNRG-hu HSCNRG-hu Thy/HSCHIV-1 replicationHIV-1 immunopathologycombined antiretroviral therapy
collection DOAJ
language English
format Article
sources DOAJ
author Liang Cheng
Liang Cheng
Jianping Ma
Guangming Li
Lishan Su
Lishan Su
spellingShingle Liang Cheng
Liang Cheng
Jianping Ma
Guangming Li
Lishan Su
Lishan Su
Humanized Mice Engrafted With Human HSC Only or HSC and Thymus Support Comparable HIV-1 Replication, Immunopathology, and Responses to ART and Immune Therapy
Frontiers in Immunology
humanized mice
NRG-hu HSC
NRG-hu Thy/HSC
HIV-1 replication
HIV-1 immunopathology
combined antiretroviral therapy
author_facet Liang Cheng
Liang Cheng
Jianping Ma
Guangming Li
Lishan Su
Lishan Su
author_sort Liang Cheng
title Humanized Mice Engrafted With Human HSC Only or HSC and Thymus Support Comparable HIV-1 Replication, Immunopathology, and Responses to ART and Immune Therapy
title_short Humanized Mice Engrafted With Human HSC Only or HSC and Thymus Support Comparable HIV-1 Replication, Immunopathology, and Responses to ART and Immune Therapy
title_full Humanized Mice Engrafted With Human HSC Only or HSC and Thymus Support Comparable HIV-1 Replication, Immunopathology, and Responses to ART and Immune Therapy
title_fullStr Humanized Mice Engrafted With Human HSC Only or HSC and Thymus Support Comparable HIV-1 Replication, Immunopathology, and Responses to ART and Immune Therapy
title_full_unstemmed Humanized Mice Engrafted With Human HSC Only or HSC and Thymus Support Comparable HIV-1 Replication, Immunopathology, and Responses to ART and Immune Therapy
title_sort humanized mice engrafted with human hsc only or hsc and thymus support comparable hiv-1 replication, immunopathology, and responses to art and immune therapy
publisher Frontiers Media S.A.
series Frontiers in Immunology
issn 1664-3224
publishDate 2018-04-01
description Immunodeficient mice reconstituted with human immune tissues and cells (humanized mice) are relevant and robust models for the study of HIV-1 infection, immunopathogenesis, and therapy. In this study, we performed a comprehensive comparison of human immune reconstitution and HIV-1 infection, immunopathogenesis and therapy between immunodeficient NOD/Rag2−/−/γc−/− (NRG) mice transplanted with human HSCs (NRG-hu HSC) and mice transplanted with HSCs and thymus fragments (NRG-hu Thy/HSC) from the same donors. We found that similar human lymphoid and myeloid lineages were reconstituted in NRG-hu HSC and NRG-hu Thy/HSC mice, with human T cells more predominantly reconstituted in NRG-hu Thy/HSC mice, while NRG-hu HSC mice supported more human B cells and myeloid cells reconstitution. HIV-1 replicated similarly and induced similar T cell depletion, immune activation, and dysfunction in NRG-hu HSC and NRG-hu Thy/HSC mice. Moreover, combined antiretroviral therapy (cART) inhibited HIV-1 replication efficiently with similar persistent HIV-1 reservoirs in both models. Finally, we found that blocking type-I interferon signaling under cART treatment transiently activated HIV-1 reservoirs, enhanced T cell recovery and reduced HIV-1 reservoirs in both HIV-1 infected NRG-hu HSC and NRG-hu Thy/HSC mice. In summary, we report that NRG-hu Thy/HSC and NRG-hu HSC mice support similar HIV-1 infection and similar HIV-1 immunopathology; and HIV-1 replication responds similarly to cART and IFNAR blockade therapies. The NRG-hu HSC mouse model reconstituted with human HSC only is sufficient for the study of HIV-1 infection, pathogenesis, and therapy.
topic humanized mice
NRG-hu HSC
NRG-hu Thy/HSC
HIV-1 replication
HIV-1 immunopathology
combined antiretroviral therapy
url http://journal.frontiersin.org/article/10.3389/fimmu.2018.00817/full
work_keys_str_mv AT liangcheng humanizedmiceengraftedwithhumanhsconlyorhscandthymussupportcomparablehiv1replicationimmunopathologyandresponsestoartandimmunetherapy
AT liangcheng humanizedmiceengraftedwithhumanhsconlyorhscandthymussupportcomparablehiv1replicationimmunopathologyandresponsestoartandimmunetherapy
AT jianpingma humanizedmiceengraftedwithhumanhsconlyorhscandthymussupportcomparablehiv1replicationimmunopathologyandresponsestoartandimmunetherapy
AT guangmingli humanizedmiceengraftedwithhumanhsconlyorhscandthymussupportcomparablehiv1replicationimmunopathologyandresponsestoartandimmunetherapy
AT lishansu humanizedmiceengraftedwithhumanhsconlyorhscandthymussupportcomparablehiv1replicationimmunopathologyandresponsestoartandimmunetherapy
AT lishansu humanizedmiceengraftedwithhumanhsconlyorhscandthymussupportcomparablehiv1replicationimmunopathologyandresponsestoartandimmunetherapy
_version_ 1725951014287179776

Similar Items