Microbial translocation predicts disease progression of HIV-infected antiretroviral-naive patients with high CD4+ cell count

Giulia Marchetti¹, Alessandro Cozzi-Lepri, Esther Merlini, Giusi M Bellistrì, Antonella Castagna, Massimo Galli, Gabriella Verucchi, Andrea Antinori, Andrea Costantini, Andrea Giacometti, Antonino di Caro, Antonella D'arminio Monforte; ICONA Foundation Study Group

Collaborators, Affiliations

Collaborators

ICONA Foundation Study Group:
M Moroni, G Angarano, A Antinori, G Carosi, R Cauda, A d'Arminio Monforte, G Di Perri, M Galli, R Iardino, G Ippolito, A Lazzarin, C F Perno, P L Viale, F Von Schlosser, A d'Arminio Monforte, A Ammassari, M Andreoni, A Antinori, C Balotta, P Bonfanti, S Bonora, M Borderi, M R Capobianchi, A Castagna, F Ceccherini-Silberstein, A Cozzi-Lepri, A d'Arminio Monforte, A De Luca, M Gargiulo, C Gervasoni, E Girardi, M Lichtner, S Lo Caputo, G Madeddu, F Maggiolo, S Marcotullio, L Monno, R Murri, C Mussini, M Puoti, C Torti, A Cozzi-Lepri, I Fanti, T Formenti, M Montroni, A Giacometti, A Costantini, A Riva, U Tirelli, F Martellotta, G Angarano, L Monno, N Ladisa, F Suter, F Maggiolo, P L Viale, G Verucchi, B Piergentili, G Carosi, G Cristini, C Torti, C Minardi, D Bertelli, T Quirino, C Abeli, P E Manconi, P Piano, J Vecchiet, K Falasca, G Carnevale, S Lorenzotti, L Sighinolfi, F Leoncini, F Mazzotta, M Pozzi, S Lo Caputo, G Cassola, G Viscoli, A Alessandrini, R Piscopo, G Mazzarello, C Mastroianni, V Belvisi, P Bonfanti, C Molteni, A Chiodera, P Castelli, M Galli, A Lazzarin, G Rizzardini, M Puoti, A d'Arminio Monforte, A L Ridolfo, A Foschi, A Castagna, S Salpietro, S Merli, L Carenzi, M C Moioli, P Cicconi, T Formenti, R Esposito, C Mussini, A Gori, V Pastore, N Abrescia, A Chirianni, M De Marco, C Ferrari, R Borghi, F Baldelli, B Belfiori, G Parruti, F Sozio, G Magnani, M A Ursitti, Reggio Emilia, M Arlotti, P Ortolani, R Cauda, M Andreoni, A Antinori, G Antonucci, P Narciso, V Tozzi, V Vullo, A De Luca, M Zaccarelli, L Gallo, R Acinapura, P De Longis, L Ceccarelli, R Libertone, M P Trotta, A Miccoli, A M Cattelan, M S Mura, G Madeddu, P Caramello, G Di Perri, G C Orofino, M Sciandra, E Raise, F Ebo, G Pellizzer, D Buonfrate

Affiliation

¹ Department of Medicine, Surgery and Dentistry, Clinic of Infectious Diseases, 'San Paolo' Hospital, University of Milan, Italy. giulia.marchetti@unimi.it

PMID: 21505312
DOI: 10.1097/QAD.0b013e3283471d10

Microbial translocation predicts disease progression of HIV-infected antiretroviral-naive patients with high CD4+ cell count

Giulia Marchetti et al. AIDS. 2011.

. 2011 Jul 17;25(11):1385-94.

doi: 10.1097/QAD.0b013e3283471d10.

Authors

Collaborators

ICONA Foundation Study Group:
M Moroni, G Angarano, A Antinori, G Carosi, R Cauda, A d'Arminio Monforte, G Di Perri, M Galli, R Iardino, G Ippolito, A Lazzarin, C F Perno, P L Viale, F Von Schlosser, A d'Arminio Monforte, A Ammassari, M Andreoni, A Antinori, C Balotta, P Bonfanti, S Bonora, M Borderi, M R Capobianchi, A Castagna, F Ceccherini-Silberstein, A Cozzi-Lepri, A d'Arminio Monforte, A De Luca, M Gargiulo, C Gervasoni, E Girardi, M Lichtner, S Lo Caputo, G Madeddu, F Maggiolo, S Marcotullio, L Monno, R Murri, C Mussini, M Puoti, C Torti, A Cozzi-Lepri, I Fanti, T Formenti, M Montroni, A Giacometti, A Costantini, A Riva, U Tirelli, F Martellotta, G Angarano, L Monno, N Ladisa, F Suter, F Maggiolo, P L Viale, G Verucchi, B Piergentili, G Carosi, G Cristini, C Torti, C Minardi, D Bertelli, T Quirino, C Abeli, P E Manconi, P Piano, J Vecchiet, K Falasca, G Carnevale, S Lorenzotti, L Sighinolfi, F Leoncini, F Mazzotta, M Pozzi, S Lo Caputo, G Cassola, G Viscoli, A Alessandrini, R Piscopo, G Mazzarello, C Mastroianni, V Belvisi, P Bonfanti, C Molteni, A Chiodera, P Castelli, M Galli, A Lazzarin, G Rizzardini, M Puoti, A d'Arminio Monforte, A L Ridolfo, A Foschi, A Castagna, S Salpietro, S Merli, L Carenzi, M C Moioli, P Cicconi, T Formenti, R Esposito, C Mussini, A Gori, V Pastore, N Abrescia, A Chirianni, M De Marco, C Ferrari, R Borghi, F Baldelli, B Belfiori, G Parruti, F Sozio, G Magnani, M A Ursitti, Reggio Emilia, M Arlotti, P Ortolani, R Cauda, M Andreoni, A Antinori, G Antonucci, P Narciso, V Tozzi, V Vullo, A De Luca, M Zaccarelli, L Gallo, R Acinapura, P De Longis, L Ceccarelli, R Libertone, M P Trotta, A Miccoli, A M Cattelan, M S Mura, G Madeddu, P Caramello, G Di Perri, G C Orofino, M Sciandra, E Raise, F Ebo, G Pellizzer, D Buonfrate

Affiliation

¹ Department of Medicine, Surgery and Dentistry, Clinic of Infectious Diseases, 'San Paolo' Hospital, University of Milan, Italy. giulia.marchetti@unimi.it

PMID: 21505312
DOI: 10.1097/QAD.0b013e3283471d10

Abstract

Objectives: We investigated the significance of microbial translocation measured on average 3 years after HIV seroconversion in driving disease progression in HIV untreated patients with high CD4(+) cell count.

Design: We included ICONA patients with documented last HIV-negative and first HIV-positive test, at least one plasma sample stored while antiretroviral therapy (ART)-naive and CD4(+) cell count greater than 200 cells/μl.

Methods: Microbial translocation [lipopolysaccharide (LPS), sCD14 and EndoCAb] and immune activation (IL-6 and TNF-α) were measured. Correlation between immune activation, microbial translocation, CD4(+) and plasma HIV-RNA was evaluated by linear regression and nonparametric Spearman's rho. The independent predictive value of these markers on time to progression to the combined endpoint of AIDS, death, CD4(+) cell count less than 200 cells/μl or start of antiretroviral therapy (ART) was assessed using survival analysis.

Results: We analysed 1488 biomarker measures from 379 patients. A median of 3.1 years after the estimated seroconversion date [interquartile range (IQR) 1.6-5.4], median (IQR) markers values were LPS, 110 pg/ml (IQR 75-215), sCD14, 3.3 μg/ml (2.2-4.8), IL-6, 1.1 pg/ml (0.6-1.9) and TNF-α, 2.4 pg/ml (1.8-3.4). Two hundred and sixty progression events were recorded over a median of 1.6 years from the first sample (2% AIDS, 84% ART initiation, 12% CD4(+) cell count less than 200 cells/μl and 2% death). LPS was the only biomarker associated with this primary composite outcome independently of age, HIV-RNA and CD4(+) (relative hazard = 1.40 per loge higher, 95% confidence interval 1.18-1.66, P < 0.001).

Conclusion: Circulating LPS in the first years of chronic HIV infection is a strong predictor of disease progression independent of CD4(+) cell count and HIV viraemia and may be considered a candidate biomarker for HIV monitoring and evaluation in clinical trials.

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Bacterial translocation: a useful biomarker for immune activation and disease progression.
Bentwich Z. Bentwich Z. AIDS. 2011 Jul 17;25(11):1439-41. doi: 10.1097/QAD.0b013e328348a8df. AIDS. 2011. PMID: 21712658 No abstract available.

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Microbial translocation predicts disease progression of HIV-infected antiretroviral-naive patients with high CD4+ cell count

Collaborators

Affiliation

Microbial translocation predicts disease progression of HIV-infected antiretroviral-naive patients with high CD4+ cell count

Authors

Collaborators

Affiliation

Abstract

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Full Text Sources

Medical

Research Materials