world-immunology-cancer-summit-2019-keynote

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December 09-10, 2019 | Barcelona, Spain

Volume 02

Journal of Immune Disorders & Therapy

J Immune Disord Ther, Volume 02

World Immunology 2019 & Cancer Summit 2019

December 09-10, 2019

WORLD CONGRESS ON

IMMUNOLOGY AND CANCER

Killing of latently HIV-infected CD4 T cells by autologous CD8 T cells is modulated by Nef

he role of HIV-specific CD8 T cell activity in the course of HIV infection and the way it affects the virus that resides in the

latent reservoir resting memory cells is debated. The PBMC of HIV-infected patients contain HIV-specific CD8 T cells and

their potential targets, CD4 T cells latently infected by HIV. CD4 T cells and CD8 T cells procured from PBMC of HIV-infected

patients were co-incubated and analyzed: Formation of CD8 T cells and HIV-infected CD4 T cell conjugates and apoptosis of

these CD4 T cells were observed by fluorescence microscopy with

in situ

PCR of HIV LTR DNA and quantified by imaging

flow cytometry using anti-human activated caspase 3 antibody and TUNEL assay. The conjugation activity and apoptosis were

found to be much higher in patients with acute HIV infection or AIDS compared to patients in chronic infection on antiretroviral

therapy (ART) or not. Patients on ART had low grade conjugation and apoptosis of

isolated CD69, CD25 and HLA-DR-negative CD4 T cells (latent reservoir cells) by

CD8 T cells. We demonstrate in HIV-infected patients, that CD8 T cells conjugate with

and kill HIV-infected CD4 T cells, including HIV-infected resting memory CD4 T cells,

throughout the course of HIV infection. We propose that in HIV-infected patients CD4

T cell annihilation is caused in part by ongoing activity of HIV-specific CD8 T cells.

HIV Nef protein interacts with ASK 1 and inhibits its pro-apoptotic death signaling by

Fas/FasL, thus protecting HIV-infected cells from CD8 T cells killing. A peptide that

interrupts Nef-ASK1 interaction that had been delivered into CD4 T cells procured from

patients on ART resulted in the increase of their apoptosis inflicted by autologous CD8 T

cells. We suggest that elimination of the HIV-infected latent reservoir CD4 T cells can be

achieved by Nef inhibition.

Biography

David Hassin, MD, specializations in internal medicine, infectious diseases and AIDS medicine. Research experience: 1) adenovirus in vitro

DNA replication. 2) DNA amplification of SV40 DNA in cells transformed by SV40 exposed to carcinogens. 3) The study of cytotoxic T lym-

phocytes (CTL) in mice infected by mengovirus (picornavirus). 4) The physiological effect of CTL on myocytes

in vitro

. 5) The study of Fas/

Fas ligand and perforin granzyme activity of CTL interacting with allogeneic cells in a mouse model. 6) Killing of latently HIV-infected CD4 T

cells by autologous CD8 T cells.

David Hassin

Ben- Gurion University of the Negev, Israel

Figure 1. Inhibition of HIV Nef interaction with

ASK1 in the CD4 T cells procured from patients

on ART results in increased susceptibility to

killing by autologous CD8 T cells