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Original Article
129 (
5
); 548-554
doi:
10.25259/IJMR_20091295_548

Incomplete immunological recovery following anti-tuberculosis treatment in HIV-infected individuals with active tuberculosis

Tuberculosis Research Centre (ICMR), Chennai, India

Reprint requests: Dr Soumya Swaminathan, Deputy Director Sr. Grade, HIV/AIDS Division, Tuberculosis Research Centre (ICMR) Mayor V.R. Ramanathan Road, Chetput, Chennai 600 031, India e-mail: doctorsoumya@yahoo.com

Licence
This open access article is licensed under Creative Commons Attribution 4.0 International (CC BY 4.0). http://creativecommons.org/licenses/by/4.0

Abstract

Background & objectives:

Mycobacterium tuberculosis infection has been shown to result in increased HIV replication and disease progression in HIV-infected individuals through increased immune activation. The objective of this study was to correlate plasma levels of immune activation markers with the presence of tuberculosis (TB) in HIV-infected and uninfected individuals, and to study the changes following anti-tuberculosis treatment.

Methods:

Plasma markers of immune activation - neopterin, beta-2-microglobulin (β2M) and soluble tumour necrosis factor alpha receptor type I (sTNFα-RI) were measured by ELISA in 42 HIV positive TB patients (HIV+TB+) undergoing a six-month course of TB chemotherapy. Thirty seven HIV+ persons without active TB, 38 TB patients without HIV infection, and 62 healthy volunteers served as controls.

Results:

Plasma levels of all three markers were elevated in HIV+ individuals, more so in those with active TB. When HIV+ individuals were further categorized based on CD4+ T cell counts, HIV+TB+ patients with CD4+ T cells counts < 200 cells/μl were found to have the highest levels at baseline with a steep fall in neopterin and sTNFa-RI during treatment, but in most instances the levels did not drop to normal. β2M levels remained persistently high despite completing TB treatment.

Interpretation & conclusions:

The findings of the study suggest that both HIV and TB act synergistically to activate the host immune system. Although ATT was effective in clearing M. tuberculosis infection, a high proportion of HIV+ TB patients continued to have levels well above the normal range, indicating that underlying immune activation persists despite TB treatment. None of the markers were specific enough to be used to assess cure of TB.

Keywords

Anti-tuberculosis treatment
HIV-1
immune activation
Mycobacterium tuberculosis -neopterin
sTNFα-RI
β-2-microglobulin

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