4.0 Article

Immune Reconstitution in HIV plus Subjects on Lopinavir/Ritonavir-Based HAART According to the Severity of Pre-Therapy CD4+

Journal

CURRENT HIV RESEARCH
Volume 10, Issue 7, Pages 597-605

Publisher

BENTHAM SCIENCE PUBL LTD
DOI: 10.2174/157016212803306032

Keywords

HAART; immune depression; immune reconstitution; late presenter; microbial translocation; T-cell activation

Funding

  1. Abbott Italia

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Background: We aimed to assess the impact of TDF/FTC +LPV/r-based HAART on the quality of immune reconstitution and on microbial translocation (MT) in HIV-infected antiretroviral-naive late presenting patients. Methods: 40 HIV+ antiretroviral-naive patients starting a first TDF/FTC+LPV/r HAART with CD4+<= 350 cell/mu L (20 severe immune depression patients -SID CD4+<= 100/mu L; 20 moderate immune depression patients -MID, CD4+ 200-350/mu L) were followed for 12 months (T12). CD38+CD8+, CD45R0+CD38+CD8+, CD95+CD4+/CD8+, CD127+CD4+/CD8+, pStat5 signalling (flow cytometry), plasma IL-7, sCD14 (ELISA), LPS (LAL) were tested at T0 and T12. Results: By T12, both study groups displayed significant CD4+ increase and HIV-RNA reduction (p<.01). Despite similar CD38+CD8+ reduction in both SID (p=.039) and MID (p=.007), SID displayed a significant rise in CD45R0+CD38+CD8+ (p=.039). MID displayed significant increase of CD95+CD4+ (p=.002), with higher baseline and T12 levels (p=.024; p=.002), suggesting reduced commitment to apoptosis. At T12, different IL-7/IL-7R profile was shown according to pre-therapy immune depression. As compared to SID, MID increased circulating IL-7 (p=.049) displaying higher baseline and T12 CD127+CD4+ (p=.0001; p=.004) and CD127+CD8+ (p=.006; p=.009). By T12, only MID displayed significant reduction in LPS (p=.020) and sCD14 (p=.005). Conclusions: In antiretroviral-naive late presenters, we show different immune reconstitution quality and MT upon 12 months TDF/FTC+LPV/r-containing HAART according to the severity of pre-therapy immune depression. Despite equal T-cell activation decline, only MID patients tend to reduce pro-apoptotic T-lymphocytes, with a gain in circulating IL-7 and higher CD127+ central-memory T-cells, and a possible control over MT.

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