Practical management of suspected hypersensitivity reactions to anti-tuberculosis drugs.
William Hywel BerminghamRashmeet BhogalSowmya Arudi NagarajanLeman MutluReham Mohamed El-ShabrawyRamesh MadhanUma Maheswari KrishnaswamyMandakolathur Ramaswamy MuraliSanath Thushara KudagammanaRajeev ShresthaStevent SumantriDevasahayam Jesudas ChristopherPadukudru Anand MaheshMartin DedicoatMamidipudi Thirumala KrishnaPublished in: Clinical and experimental allergy : journal of the British Society for Allergy and Clinical Immunology (2022)
Tuberculosis (TB) is the commonest cause of death by a single infectious agent globally and ranks amongst the top ten causes of global mortality. The incidence of TB is highest in Low-Middle Income countries (LMICs). Prompt institution of, and compliance with, therapy are cornerstones for a favourable outcome in TB and to mitigate the risk of multiple drug resistant (MDR)-TB, which is challenging to treat. There is some evidence that adverse drug reactions (ADRs) and hypersensitivity reactions (HSRs) to anti-TB drugs occur in over 60% and 3%-4% of patients respectively. Both ADRs and HSRs represent significant barriers to treatment adherence and are recognised risk factors for MDR-TB. HSRs to anti-TB drugs are usually cutaneous and benign, occur within few weeks after commencement of therapy and are likely to be T-cell mediated. Severe and systemic T-cell mediated HSRs and IgE mediated anaphylaxis to anti-TB drugs are relatively rare, but important to recognise and treat promptly. T-cell-mediated HSRs are more frequent amongst patients with co-existing HIV infection. Some patients develop multiple sensitisation to anti-TB drugs. Whilst skin tests, patch tests and in vitro diagnostics have been used in the investigation of HSRs to anti-TB drugs, their predictive value is not established, they are onerous, require specialist input of an allergist and are resource-dependent. This is compounded by the global, unmet demand for allergy specialists, particularly in low-income countries (LICs)/LMICs and now the challenging circumstances of the severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) pandemic. This narrative review provides a critical analysis of the limited published evidence on this topic and proposes a cautious and pragmatic approach to optimise and standardise the management of HSRs to anti-TB drugs. This includes clinical risk stratification and a dual strategy involving sequential re-challenge and rapid drug desensitisation. Furthermore, a concerted international effort is needed to generate real-time data on ADRs, HSRs, safety and clinical outcomes of these interventions.
Keyphrases
- mycobacterium tuberculosis
- sars cov
- drug resistant
- adverse drug
- drug induced
- end stage renal disease
- respiratory syndrome coronavirus
- multidrug resistant
- ejection fraction
- type diabetes
- chronic kidney disease
- newly diagnosed
- risk factors
- prognostic factors
- coronavirus disease
- randomized controlled trial
- emergency department
- stem cells
- pulmonary embolism
- mental health
- metabolic syndrome
- peritoneal dialysis
- pseudomonas aeruginosa
- hiv infected
- machine learning
- cardiovascular events
- early onset
- bone marrow
- adipose tissue
- smoking cessation
- data analysis
- insulin resistance
- human immunodeficiency virus