Tuberculous Meningitis Clinical Trial
Official title:
Diagnosis of Tuberculous Meningitis by a Secretory Antigenic Target 6 (ESAT-6) in CSF
Early and reliable diagnosis of tuberculous meningitis (TBM) still poses a great challenge. One of the underlying difficulties is due to the fact that tubercle bacilli are mainly not present in the cerebrospinal fluid (CSF) but in the phagocytotic macrophages. The present study was designed to demonstrate early secretory antigenic target 6 (ESAT-6), a mycobacterium-specific antigens, in the macrophages in infected CSF samples and compare the efficiency of this antigen in the laboratory diagnosis of TBM.
Tuberculosis is a disease that carries a global health burden, and tuberculous meningitis
(TBM) is one of the most serious clinical manifestations of extrapulmonary tuberculosis. The
failure to promptly recognize and treat patients with TBM enables the disease to exact a
devastating toll around the globe despite the availability of effective chemotherapy.
Therefore, accurate and timely identification of infected individuals and subsequent prompt
initiation of effective anti-tuberculosis chemotherapy are essential in reducing the
mortality of TBM.1 However, the disease is often difficult to diagnose with certainty,
especially at early stages,2 as the presenting clinical and cerebrospinal fluid (CSF)
features of TBM are non-specific and have to be differentiated from a plethora of other
infectious meningitides such as viral, bacterial or cryptococcal meningitis, which
frequently result in diagnostic confusion. Consequently, TBM is often diagnosed when
irreversible neurologic damages have already taken place and immediate anti-tuberculosis
therapy is therefore recommended regardless of the results of individual tests if TBM is
seriously contemplated.
The confirmation of TBM depends on the demonstration of Mycobacterium tuberculosis in the
CSF by bacteriological methods. Smear acid-fast bacillus microscopy is rapid and
inexpensive, but has a very low sensitivity (10-20%),3 and culture also lacks sensitivity
and is time-consuming. A number of strategies have been attempted to improve the laboratory
diagnosis of TBM. Nucleic acid amplification tests (NAAT) show potential roles in confirming
the diagnosis of TBM, but they, too, suffer from the problem of overall low sensitivity
(0.46-0.66), partly due to a low bacillary load in the CSF.4-5 Immunodiagnostic methods have
also been evaluated, but the heterogeneity of immune responses in TBM patients at the
different stages of the infection poses a major obstacle to the detection of mycobacterial
antibodies in CSF samples.6-7 In general, patients at the chronic stages of TBM have a
myriad of antibody responses to all major antigens of Mycobacterium tuberculosis, while
patients at the early stages have scarcely any detectable antibody response. In addition,
interpretation of mycobacterial antibodies in the CSF must take into account the
contribution of antibodies from the plasma, therefore, jeopardizing the use of these
antibody-based immunodiagnostic methods in the location where they are most needed.7 One
approach to provide direct evidence of existing infection is the detection of the presence
of specific antigens in the circulating CSF. The first generation of these tests employed
non-specific antigens as exemplified by bacille Calmette-Guerin (BCG) or purified protein
derivative (PPD).8-10 Genomic analysis and antigen mining of Mycobacterium tuberculosis have
yielded novel, more specific antigens, such as early secretory antigenic target 6 (ESAT-6),
38-kD antigen, and Ag85 complex.11 Nevertheless, the diagnostic efficiency of this
antigen-based approach is still unsatisfactory.5-6 Mycobacterium tuberculosis belongs to the
group of intracellular bacteria, which replicate within resting macrophages. During the
early stages of the central nervous system (CNS) infection, the tubercle bacilli in the CSF
are immediately phagocytosed by the macrophages,12-13 leading to the scarcity of
mycobacterial markers in the circulating CSF. Thus, no such tests have yet become available
for early diagnosis of active TBM with the requisite sensitivity and specificity.
The investigators hypothesized that, in contrast to the scarcity of mycobacterial markers in
the circulating CSF, macrophages in infected CSF may carry a high load of mycobacterial
antigens, which could lend themselves to the development a cell-based diagnostic approach
for TBM. Here, the investigators sought to develop a smear immunocytochemical method to
improve the accuracy of early diagnosis of TBM by examining early secretory antigenic target
6 (ESAT-6), a mycobacterium-specific antigens, in the macrophages in CSF specimens from
patients with TBM and patients with infectious meningitis other than TBM. The investigators
also compared the efficiency of this cell-based approach for detecting mycobacterial
antigens with microbiological and NAAT method in the laboratory diagnosis of TBM. Further,
on the basis of the clinical presentations, CSF and etiological findings in this study, the
investigators proposed novel diagnostic criteria for TBM.
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