Primary HIV infection features colonic damage and neutrophil inflammation yet containment of microbial translocation

原发性 HIV 感染的特征是结肠损伤和中性粒细胞炎症,但微生物易位受到抑制

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作者:Camilla Tincati, Valeria Bono, Elvira Stefania Cannizzo, Delfina Tosi, Federica Savi, Camilla Falcinella, Anna Casabianca, Chiara Orlandi, Carmelo Luigiano, Matteo Augello, Stefano Rusconi, Antonio Muscatello, Alessandra Bandera, Andrea Calcagno, Andrea Gori, Silvia Nozza, Giulia Marchetti; Italian

Conclusion

Early HIV infection features higher HIV DNA in the gut, yet comparable mucosal alterations to those observed in chronic infection. In contrast, microbial translocation is contained in primary HIV infection, likely because of a partial preservation of E-cadherin and mucosal immune subsets, namely γδ T-cells.

Methods

Fifteen people with primary HIV infection (P-HIV) and 13 with chronic HIV infection (C-HIV) c-ART-naive participants were cross-sectionally studied. Gut biopsies were analysed in terms of gut reservoirs (total, integrated and unintegrated HIV DNA); tight junction proteins (E-cadherin, Zonula Occludens-1), CD4 + expression, neutrophil myeloperoxidase (histochemical staining); collagen deposition (Masson staining). Flow cytometry was used to assess γδ T-cell frequency (CD3 + panγδ+Vδ1+/Vδ2+). In plasma, we measured microbial translocation (LPS, sCD14, EndoCAb) and gut barrier function (I-FABP) markers (ELISA).

Results

P-HIV displayed significantly higher tissue HIV DNA, yet neutrophil infiltration and collagen deposition in the gut were similar in the two groups. In contrast, microbial translocation markers were significantly lower in P-HIV compared with C-HIV. A trend to higher mucosal E-cadherin, and gut γδ T-cells was also observed in P-HIV.

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