Advanced baseline immunosuppression is associated with elevated levels of plasma markers of fungal translocation and inflammation in long-term treated HIV-infected Tanzanians

被引:4
作者
Barabona, Godfrey [1 ]
Mahiti, Macdonald [2 ]
Toyoda, Mako [1 ]
Kamori, Doreen [2 ]
Masoud, Salim [2 ]
Judicate, George P. [1 ]
Sunguya, Bruno [1 ,2 ]
Lyamuya, Eligius [1 ,2 ]
Ueno, Takamasa [1 ,2 ]
机构
[1] Kumamoto Univ, Joint Res Ctr Human Retrovirus Infect, 2-2-1 Chuo Ku, Kumamoto 8600811, Japan
[2] Muhimbili Univ Hlth & Allied Sci, Dar Es Salaam, Tanzania
关键词
HIV/AIDS; chronic inflammation; HIV treatment in low-income counties; 1-3-beta-D-Glucan; IMMUNE ACTIVATION; DISEASE; RISK;
D O I
10.1186/s12981-021-00381-9
中图分类号
R51 [传染病];
学科分类号
100401 ;
摘要
Background: For over a decade, antiretroviral therapy (ART) in resource-limited countries was only recommended for patients with advanced HIV disease. We investigated this group of patients in order to determine any relationship between degree of immunosuppression during treatment initiation and the subsequent levels of inflammatory biomarkers, reservoir size and plasma marker of fungal translocation after achieving long-term virological control. Methods: We analyzed 115 virally suppressed (female 83.5%) and 40 untreated (female 70%) subjects from Dar es Salaam, Tanzania. The size of HIV latent reservoir (proviral DNA copy) was determined using quantitative PCR. Inflammatory biomarkers; IL-6, IL-10, and soluble CD14 (sCD14), were measured using multiplex cytometric beads array. Antibody titers for Cytomegalovirus (CMV) and Epstein Barr virus (EBV), plasma level of 1-3-beta-D-Glucan (BDG) was measured using ELISA. High-sensitivity C-reactive protein (hsCRP) was measured using nephelometric method. Results: The median age was 36 (IQR 32-44) and 47 (IQR 43-54) years in untreated and virally suppressed patients respectively. Median duration of treatment for virally suppressed patients was 9 years (IQR 7-12) and median baseline CD4 count was 147 cells/mm(3) (IQR 65-217). Virally suppressed patients were associated with significantly lower plasma levels of IL-10, sCD14 and BDG (P < 0.05) when compared to untreated patients. However, plasma level of IL-6 was similar between the groups. Baseline advanced level of immunosuppression (CD4 < 100cells/cm(3)) was associated with significantly higher plasma level of IL-6 (P = 0.02), hsCRP (P = 0.036) and BDG (P = 0.0107). This relationship was not seen in plasma levels of other tested markers. Degree of baseline immunosuppression was not associated with the subsequent proviral DNA copy. In addition, plasma levels of inflammatory marker were not associated with sex, CMV or EBV antibody titers, treatment duration or regimen. Conclusions: Our data suggest that advanced immunosuppression at ART initiation is associated with severity of inflammation and elevated fungal translocation marker despite long term virological control. Further studies are needed to evaluate the potential increased burden of non-AIDS comorbidities that are linked to elevated inflammatory and fungal translocation markers as a result of the policy of HIV treatment at CD4 count < 200 cells/cm(3) implemented for over a decade in Tanzania.
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