Using IGRAs for the diagnosis of
M. tuberculosis infection in children under 5 is controversial. First, there is concern about the reduced sensitivity of IGRAs. A study from the United States showed that the sensitivity of IGRAs was low in the diagnosis of laboratory-confirmed ATBI among children under 5 years of age, with 58.7% positivity in the 2–4-years-old group and 51.9% positivity in the under-2-years-old group
[39]. Despite this, there is a high level of concordance between IGRAs and the TST in the diagnosis of ATBI
[33]. Different studies had different conclusions regarding the value of IGRAs and the TST for diagnosing LTBI. A cohort study of BCG-vaccinated children younger than 5 years showed that there was a high discordance (12.3%) between IGRAs and the TST, mostly TST+/IGRA−
[40]; another study showed that for high-risk children aged 2–5 years old, IGRAs’ positivity was lower than that of the TST
[41]. None of the TST+/IGRA− children developed into ATBI during the follow-up even without prophylactic treatment, demonstrating the false positivity of the TST that came from the cross-reaction with BCG
[40][41][42][40,41,42]. Using the TST as a standard, a meta-analysis showed that IGRAs had higher sensitivity and specificity, with the pooled sensitivity and specificity of ELISA being 84.1 and 89.5%, respectively, and the pooled sensitivity and specificity of ELISPOT were 93.1 and 76.7%, respectively
[43]. An IFN-γ-inducible protein 10 (IP-10) assay compared with current IGRAs will improve the diagnosis of LTBI in patients younger than 5 years
[44]. Another reason to hesitate to use IGRAs is that younger age will significantly increase indeterminate results due to the low mitogen response caused by immunologic immaturity
[45][46][45,46]. Indeterminate results in children under 2 years old can reach up to 40%. In addition, iron deficiency anemia, helminths, and malaria infection, which are common in children under 5 years old, may also increase the indeterminate rates
[45]. However, the largest study found less than 1% of results were indeterminate, where the
resea
rcheuthors included more than 5000 IGRA results in children under 2 years old
[47].
At present, an increasing number of guidelines approve the application of IGRAs in the diagnosis of LTBI in children. When high specificity is required (e.g., BCG-vaccinated children in low-risk areas), IGRAs are a better choice. When sensitivity is the first consideration (e.g., children about to receive immunomodulatory biologics), a TST and IGRA need to be performed simultaneously, and any positive result should be regarded as infection. However, for the diagnosis of ATBI in children, IGRAs are thought to be a complementary diagnostic technology
[48][49][48,49].