key: cord-0899859-illrdtko
authors: Datta, Sumona; Evans, Carlton A
title: The uncertainty of tuberculosis diagnosis
date: 2020-05-18
journal: Lancet Infect Dis
DOI: 10.1016/s1473-3099(20)30400-x
sha: 9b3abae31e993474ce9cc7c98f8c4106e383d234
doc_id: 899859
cord_uid: illrdtko

nan

Tuberculosis is estimated to affect 10 million people each year, but this statistic is remarkably uncertain: 30% are countries' estimates of undiagnosed, untreated, or unreported cases. Furthermore, about half of tuber culosis diagnoses globally are uncertain because they rely entirely on the nonspecific clinical features of tuberculosis, without any laboratory confirmation. 1 Laboratory tests for tuberculosis generally perform poorly and are scarcely available in resourceconstrained settings where most cases of tuberculosis occur. 1 Consequently, when assessing a patient who is unwell with symptoms such as prolonged productive cough for whom rapid laboratory tests for tuberculosis are unavailable or negative, it is often difficult to discern whether the patient has tuberculosis or a more common disease such as a bacterial pneumonia. In this situation, some guidelines recommend a trial of antibiotics, a widely practiced approach entailing a few days of broadspectrum antibiotics that are inactive against tuberculosis. This approach assumes that symptom persistence despite a trial of antibiotics implies that tuberculosis is probable, and that improvement on a trial of antibiotics rules out tuberculosis. 2 However, these assumptions have been the subject of remarkably little research and are undermined by issues such as antibiotic resistance and the placebo effect.

In a systematic review and metaanalysis in The Lancet Infectious Diseases, Titus Divala and colleagues 3 evaluated a trial of antibiotics as if it were a diagnostic test for tuberculosis. After screening 9410 publications, they identified eight studies in which patients with initially negative rapid tuberculosis tests were treated with a trial of antibiotics, the response to which was compared with the subsequent results of more sensitive laboratory testing for tuberculosis. Of the 2786 patients who had a trial of antibiotics, overall 608 patients (22% [range 4-65]) were later found to have laboratoryproven tuberculosis. The crude results of these eight studies are summarised in the figure, which shows that whether patients' symptoms persisted on a trial of antibiotics did not usefully predict laboratoryproven tuberculosis. For example, overall, 1307 (47% [range 6-76]) of 2786 patients had symptoms that persisted despite a trial of antibiotics, implying that they had tuberculosis, but remarkably only 454 (35% [range 11-84]) of 1307 patients with persistent symptoms were later found to have laboratoryconfirmed tuberculosis. Furthermore, 154 patients (25% [range 3-85]) of 608 patients later found to have laboratoryconfirmed tuberculosis paradoxically improved on a trial of anti biotics, an improvement that should have ruled out this tuberculosis diagnosis. These crude percentages are complementary to the rigorous random effects metaanalysis reported by Divala and colleagues, which suggested that a trial of antibiotics had pooled sensitivity of 67% (95% CI 42-85) and specificity of 73% (58-85) versus mycobacteriology tests. This poor performance of a trial of antibiotics has important implications for policy and practice. 3 The methods and results of these eight studies varied so greatly that the combined statistics and pooled metaanalyses have questionable precision. 4 Despite this variability, the trial of antibiotics performed poorly for ruling tuberculosis in or out in each of the eight studies. These findings are approximations because tuberculosis laboratory testing might be false positive, 5 and because falsenegative laboratory tests in patients who have tuberculosis are frequent. 6 Furthermore, molecular testing was only included in the initial rapid testing in one of these eight studies, 7 but it has since become widely used for diagnosing tuberculosis. 1 None of these issues are likely to challenge Divala and colleagues' conclusion that a trial of antibiotics is unreliable for informing tuberculosis diagnosis. Importantly, broadspectrum antibiotics might still be necessary, not to inform tuberculosis diagnosis, but rather because the patient's illness requires anti biotic treatment, ideally guided by laboratory testing. 8 However, there is compelling evidence that broad spectrum antibiotic therapy for patients with a suspected respiratory tract infection might often be safely withheld initially, potentially reducing the risk of sideeffects and antibiotic resistance. 9 Divala and colleagues' findings show that a trial of antibiotics should not generally be used to decide whether to commence tuberculosis therapy in patients with negative, pending, or unavailable laboratory tests for tuberculosis. But what should health systems, clinicians, and patients do instead? When should empirical treatment be commenced rather than doing additional tests or waiting to see how the illness evolves? There is an urgent need for operational research to address this knowledge gap, which will depend on local epidemiology, the severity of the patient's illness, and the availability of repeat and more accurate laboratory tests.

More than a century after Robert Koch identified Mycobacterium tuberculosis, why do policy and practice still often include nonevidencebased algorithms for people with tuberculosis? Why are we clarifying the poor diagnostic reliability of a trialofantibiotics for tuberculosis only after they have been used millions of times during several decades? Both questions are answered in part by the chronic severe underfunding of tuberculosis research. 1, 10 The coronavirus disease 2019 (COVID19) emergency and resultant socioeconomic crisis will inevitably worsen the global tuberculosis pandemic by increasing tuberculosis risk factors and social determinants, and challenging health systems and access to them. It is striking that long before mortality attributed to COVID19 approaches 1·5 million-the number of deaths caused by tuberculosis each yearthere has been unprecedented investment in research that is rapidly defining how best to care for people with suspected COVID19. This should be an inspiration to the fight for tuberculosis elimination. Similar urgency and investment are also desperately needed to inform improved care for people suspected of having the most frequent infectious cause of death, tuberculosis. 

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