James A. Daucher scite author profile

Chemokines were originally characterized by their ability to direct migration and induce activation of selected leukocyte populations. The beta-chemokines MIP-1 alpha, MIP-beta, and RANTES have been implicated in the suppression of viral replication by CD8+ T cells from HIV-infected individuals. The present study was undertaken to evaluate the effect of beta-chemokines on HIV replication in cocultures of dendritic cells (DCs) and CD4+ T cells, and an in vitro model of the lymphoid microenvironment. In the acute infection system, where DCs from uninfected individuals are pulsed with HIV and cocultured with autologous CD4+ T cells, no inhibition of replication of monocytotropic or T cell tropic viral isolates by MIP-1 alpha, MIP-1 beta, and RANTES, alone or in combination, was observed. In contrast, in an endogenous infection system, where the DCs and CD4+ T cells were obtained from HIV-infected subjects, addition of recombinant beta-chemokines suppressed HIV replication. However, neutralizing antibodies to beta-chemokines did not affect the suppressive activity of CD8+ T cells from HIV-infected donors in either system, suggesting that CD8+ T cell-mediated suppression is not due exclusively to beta-chemokines. Furthermore, no significant differences in secretion of MIP-1 alpha, MIP-1 beta, and RANTES by purified CD8+ T cells were noted in uninfected versus HIV-infected donors, regardless of the stage of disease. These results indicate that HIV suppression by CD8+ T cells derived from HIV-infected donors is a multifactorial phenomenon and not limited to the action of MIP-1 alpha, MIP-1 beta, and RANTES.

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Adaptations of the Rat Vagina in Pregnancy to Accommodate Delivery

Daucher

Clark

Stolz

et al. 2007

Obstetrics & Gynecology

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Cytokine Regulation of HIV Replication Induced by Dendritic Cell–CD4-Positive T Cell Interactions

Weissman

Daucher²,

Barker³

et al. 1996

AIDS Research and Human Retroviruses

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It has been established that human immunodeficiency virus (HIV) replication occurs throughout the course of disease in the lymphoid tissue. We have developed a model system to study the effect of cytokines and other agents on HIV replication using cocultures of DCs and T cells that reflect the cell-to-cell interactions that occur in the microenvironment of lymphoid tissue. Dendritic cells from peripheral blood, when pulsed with small amounts of HIV, induce infection in autologous, unstimulated CD4-positive T cells. Using this system, cytokines, anti-cytokine antibodies, and inhibitors of cellular activation were added to cultures and the effects on cellular proliferation and activation and HIV production were measured. Cytokines that increased T cell proliferation, such as IL-2 and IL-4, enhanced HIV replication, while the effect of IL-12 was more complex. HIV production was inhibited by blocking endogenously produced IL-2, as well as by adding IL-10, which blocks IL-2 secretion, antigen-presenting cell function, and T cell activation. Proinflammatory cytokines induced modest enhancement of viral replication in cocultures of HIV-pulsed DCs and CD4-positive T cells. Thus, using a model of HIV replication that more closely mimics the in vivo microenvironment of lymphoid tissue may allow a better analysis of the effect of cytokines and cytokine networks, as well as agents that modify immune activation on HIV replication.

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Humidified Compared With Dry, Heated Carbon Dioxide at Laparoscopy to Reduce Pain

Beste

Daucher

Holbert

2006

Obstetrics & Gynecology

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James A. Daucher

Multifactorial Nature of Noncytolytic CD8⁺T Cell-Mediated Suppression of HIV Replication: β-Chemokine-Dependent and -Independent Effects

Adaptations of the Rat Vagina in Pregnancy to Accommodate Delivery

Cytokine Regulation of HIV Replication Induced by Dendritic Cell–CD4-Positive T Cell Interactions

Humidified Compared With Dry, Heated Carbon Dioxide at Laparoscopy to Reduce Pain

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James A. Daucher

Multifactorial Nature of Noncytolytic CD8+T Cell-Mediated Suppression of HIV Replication: β-Chemokine-Dependent and -Independent Effects

Adaptations of the Rat Vagina in Pregnancy to Accommodate Delivery

Cytokine Regulation of HIV Replication Induced by Dendritic Cell–CD4-Positive T Cell Interactions

Humidified Compared With Dry, Heated Carbon Dioxide at Laparoscopy to Reduce Pain

Contact Info

Product

Resources

About

Multifactorial Nature of Noncytolytic CD8⁺T Cell-Mediated Suppression of HIV Replication: β-Chemokine-Dependent and -Independent Effects