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Persistent HIV-1 infection in duodenal mucosa and memory CD8+ T cell differentiation Liliana Belmonte 1 PhD; Alberto Zalar 2 MD; Patricia Baré 1 PhD; Noel.

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Presentation on theme: "Persistent HIV-1 infection in duodenal mucosa and memory CD8+ T cell differentiation Liliana Belmonte 1 PhD; Alberto Zalar 2 MD; Patricia Baré 1 PhD; Noel."— Presentation transcript:

1 Persistent HIV-1 infection in duodenal mucosa and memory CD8+ T cell differentiation Liliana Belmonte 1 PhD; Alberto Zalar 2 MD; Patricia Baré 1 PhD; Noel Badano 1 PhD st; Valentina Araya 2 MD; Eduardo Piskorz 2 MD; Maria Inés Figueroa 3 MD; Cecilia Parodi 1 PhD, Beatriz Ruibal-Ares 1 MD, Pedro Cahn 3 MD, PhD; Maria Marta de E de Bracco 1 PhD. Laboratory of Immunology and Virology 1, Academia Nacional de Medicina, Buenos Aires, Argentina. Gastroenterology 2 and Infectious Diseases 3 Units, Hospital Juan A Fernandez, Buenos Aires, Argentina.

2 Introduction Despite the clinical improvement associated with HAART, current antiviral drugs are not able to eradicate HIV due to the persistence of virus in tissue reservoirs. Viral reservoirs therefore represent a potentially life-long site of replication-competent forms of HIV that cannot be suppressed by current antiretroviral treatment

3 The objectives of the study were: ¤ To verify if HIV-1 persists in the intestine of HIV+ patients in spite of successful antiretroviral treatment (HAART) ¤ To identify the cells that harbour HIV-1 in the duodenal mucosa

4 Material and Methods A.- Distal duodenal biopsies were obtained from 13 patients with chronic HIV-1 infection under HAART: 9 males, 4 females, 9 males, 4 females, 7 with pVL < 50 copies/ml, Median CD4 cell count 354 cell/mm 3 (31-563) 7 with pVL < 50 copies/ml, Median CD4 cell count 354 cell/mm 3 (31-563) 6 with pVL>100.000 copies/ml, Median CD4 cell count 58 cell/mm 3 (7-198) 6 with pVL>100.000 copies/ml, Median CD4 cell count 58 cell/mm 3 (7-198) Distal duodenal biopsies from 10 HIV-1 seronegative individuals were used as control (C). B.- A biopsy was labeled as “HIV +” if HIV-DNA was detected by standard PCR (using primers SK145 and SKCC1B to define a sequence of 155 nucleotides within the highly conserved region of the HIV-1 gag gene) C.- The phenotype of leukocytes present in the tissue was assessed by flow cytometry using anti CD4, CD64, CD27, CD28, CD45RO. HIV-1 detection was performed by intracellular staining with KC57 antibody (anti-p24).

5 CD4 depletion in duodenal mucosa n:13 n:10

6 CD8+ T cells in duodenal mucosa n:13 n:10

7 Characteristics of duodenal CD8+ T cell population p=0.001 p=0.027 % % % % % p=NS

8 Patients ND pVL (n=7) Patients pVL > 100.000 copies/ml (n=6) HIV + Biopsies 44 HIV- Biopsies Biopsies32 Lack of correlation of pVL with HIV persistence in duodenal mucosa p=0.72, chi-square test

9 p24 positivity in duodenal CD64+ cells Control Biopsy HIV- biopsy (by PCR) HIV+ biopsy (by PCR) Control isotype p24 expression KC57 FITC Median FI KC57: 193 Median FI isotype: 52 Median FI KC57: 56 Median FI isotype: 47 Median FI KC57: 45 Median FI isotype: 35

10 p24 positivity in duodenal CD68+ Macrophages HIV+ biopsy (by PCR) Control Biopsy Control isotype p24 expression Median FI KC57: 158 Median FI isotype: 54 Median FI KC57: 67 Median FI isotype: 57

11 Conclusions  As reported in other segments of the GI tract, we found that CD4 T cells were depleted in duodenal mucosa of HIV patients when compared to controls, while no differences were observed in the proportion of CD8 T cells in both groups.  However, the persistence of HIV in the duodenal tissue affects the differentiation pattern of CD8 T cells. Thus, the proportion of fully differentiated CD8+ T cells was higher in the absence of HIV in the duodenum of HIV patients.

12 Conclusions  HIV-DNA could be detected in the duodenal mucosa both in patients who failed treatment and in those with undetectable pVL.  Concerning the nature of cells that harbour HIV infection, we have shown that macrophages may host persistent HIV infection and could be considered as a reservoir of HIV even after HAART.


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