Nanoparticles containing siRNA to silence CD4 and CCR5 reduce expression of these receptors and inhibit HIV-1 infection in human female reproductive tract tissue explants

Nanoparticles containing siRNA to silence CD4 and CCR5 reduce expression of these receptors and inhibit HIV-1 infection in human female reproductive tract tissue explants

Human Immunodeficiency Virus-type 1 (HIV- 1) binds to CD4 and CCR5 receptors on target cells in the human female reproductive tract. We sought to determine whether reducing levels of messenger RNA (mRNA) transcripts that encode these receptors in female reproductive tract cells could protect mucosal...

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Bibliographic Details
Main Authors: Susan K. Eszterhas, Nicole O. Ilonzo, Jennifer E. Crozier, Stela Celaj, Alexandra L. Howell
Format: Article
Language:English
Published: MDPI AG 2011-09-01
Series:Infectious Disease Reports
Subjects:
heterosexual transmission, women, virus infection, HIV-1, nanoparticles.
Online Access:http://www.pagepress.org/journals/index.php/idr/article/view/2370
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spelling doaj-47df71c52ccb4948949caf2d9af73dd92021-01-02T13:54:07ZengMDPI AGInfectious Disease Reports2036-74302036-74492011-09-0132e11e1110.4081/idr.2011.23701629Nanoparticles containing siRNA to silence CD4 and CCR5 reduce expression of these receptors and inhibit HIV-1 infection in human female reproductive tract tissue explantsSusan K. Eszterhas0Nicole O. Ilonzo1Jennifer E. Crozier2Stela Celaj3Alexandra L. Howell4V.A. Medical Center, White River Junction, VT; Department of Microbiology & Immunology, Dartmouth Medical School, Lebanon, NHDepartment of Microbiology & Immunology, Dartmouth Medical School, Lebanon, NHV.A. Medical Center, White River Junction, VTDepartment of Microbiology & Immunology, Dartmouth Medical School, Lebanon, NHV.A. Medical Center, White River Junction, VT; Department of Microbiology & Immunology, Dartmouth Medical School, Lebanon, NHHuman Immunodeficiency Virus-type 1 (HIV- 1) binds to CD4 and CCR5 receptors on target cells in the human female reproductive tract. We sought to determine whether reducing levels of messenger RNA (mRNA) transcripts that encode these receptors in female reproductive tract cells could protect mucosal tissue explants from HIV- 1 infection. Explants prepared from the endometrium, endocervix, and ectocervix of hysterectomy tissues from HIV-1 sero-negative women were exposed to nanoparticles containing CD4- and CCR5-specific short-interfering RNA (siRNA) sequences. Explants were then exposed two days later to HIV-1, and HIV-1 reverse transcripts were measured five days post-infection. Explants treated with nanoparticles containing CD4- and CCR5-specific siRNA showed reduced levels of CD4 and CCR5 transcripts, and significantly lower levels of HIV-1 reverse transcripts compared to those treated with an irrelevant siRNA. In female reproductive tract explants and in peripheral blood cell cultures, siRNA transfection induced the secretion of IFN-alpha (IFN-α), a potent antiviral cytokine. In female mice, murine-specific Cd4-siRNA nanoparticles instilled within the uterus significantly reduced murine Cd4 transcripts by day 3. Our findings demonstrate that siRNA nanoparticles reduce expression of HIV-1 infectivity receptors in human female reproductive tract tissues and also inhibit HIV-1 infection. Murine studies demonstrate that nanoparticles can penetrate the reproductive tract tissues in vivo and silence gene expression. The induction of IFN-α after siRNA transfection can potentially contribute to the antiviral effect. These findings support the therapeutic development of nanoparticles to deliver siRNA molecules to silence host cell receptors in the female reproductive tract as a novel microbicide to inhibit mucosal HIV-1 transmission.http://www.pagepress.org/journals/index.php/idr/article/view/2370heterosexual transmission, women, virus infection, HIV-1, nanoparticles.
collection DOAJ
language English
format Article
sources DOAJ
author Susan K. Eszterhas
Nicole O. Ilonzo
Jennifer E. Crozier
Stela Celaj
Alexandra L. Howell
spellingShingle Susan K. Eszterhas
Nicole O. Ilonzo
Jennifer E. Crozier
Stela Celaj
Alexandra L. Howell
Nanoparticles containing siRNA to silence CD4 and CCR5 reduce expression of these receptors and inhibit HIV-1 infection in human female reproductive tract tissue explants
Infectious Disease Reports
heterosexual transmission, women, virus infection, HIV-1, nanoparticles.
author_facet Susan K. Eszterhas
Nicole O. Ilonzo
Jennifer E. Crozier
Stela Celaj
Alexandra L. Howell
author_sort Susan K. Eszterhas
title Nanoparticles containing siRNA to silence CD4 and CCR5 reduce expression of these receptors and inhibit HIV-1 infection in human female reproductive tract tissue explants
title_short Nanoparticles containing siRNA to silence CD4 and CCR5 reduce expression of these receptors and inhibit HIV-1 infection in human female reproductive tract tissue explants
title_full Nanoparticles containing siRNA to silence CD4 and CCR5 reduce expression of these receptors and inhibit HIV-1 infection in human female reproductive tract tissue explants
title_fullStr Nanoparticles containing siRNA to silence CD4 and CCR5 reduce expression of these receptors and inhibit HIV-1 infection in human female reproductive tract tissue explants
title_full_unstemmed Nanoparticles containing siRNA to silence CD4 and CCR5 reduce expression of these receptors and inhibit HIV-1 infection in human female reproductive tract tissue explants
title_sort nanoparticles containing sirna to silence cd4 and ccr5 reduce expression of these receptors and inhibit hiv-1 infection in human female reproductive tract tissue explants
publisher MDPI AG
series Infectious Disease Reports
issn 2036-7430
2036-7449
publishDate 2011-09-01
description Human Immunodeficiency Virus-type 1 (HIV- 1) binds to CD4 and CCR5 receptors on target cells in the human female reproductive tract. We sought to determine whether reducing levels of messenger RNA (mRNA) transcripts that encode these receptors in female reproductive tract cells could protect mucosal tissue explants from HIV- 1 infection. Explants prepared from the endometrium, endocervix, and ectocervix of hysterectomy tissues from HIV-1 sero-negative women were exposed to nanoparticles containing CD4- and CCR5-specific short-interfering RNA (siRNA) sequences. Explants were then exposed two days later to HIV-1, and HIV-1 reverse transcripts were measured five days post-infection. Explants treated with nanoparticles containing CD4- and CCR5-specific siRNA showed reduced levels of CD4 and CCR5 transcripts, and significantly lower levels of HIV-1 reverse transcripts compared to those treated with an irrelevant siRNA. In female reproductive tract explants and in peripheral blood cell cultures, siRNA transfection induced the secretion of IFN-alpha (IFN-α), a potent antiviral cytokine. In female mice, murine-specific Cd4-siRNA nanoparticles instilled within the uterus significantly reduced murine Cd4 transcripts by day 3. Our findings demonstrate that siRNA nanoparticles reduce expression of HIV-1 infectivity receptors in human female reproductive tract tissues and also inhibit HIV-1 infection. Murine studies demonstrate that nanoparticles can penetrate the reproductive tract tissues in vivo and silence gene expression. The induction of IFN-α after siRNA transfection can potentially contribute to the antiviral effect. These findings support the therapeutic development of nanoparticles to deliver siRNA molecules to silence host cell receptors in the female reproductive tract as a novel microbicide to inhibit mucosal HIV-1 transmission.
topic heterosexual transmission, women, virus infection, HIV-1, nanoparticles.
url http://www.pagepress.org/journals/index.php/idr/article/view/2370
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