Specific human gene expression in response to infection is an effective marker for diagnosis of latent and active tuberculosis.

Publication date: Nov 06, 2024

RNA sequencing and microarray analysis revealed transcriptional markers expressed in whole blood can differentiate active pulmonary TB (ATB) from other respiratory diseases (ORDs), and latent TB infection (LTBI) from healthy controls (HC). Here we describe a streamlined reverse transcriptase quantitative polymerase chain reaction (RT-qPCR) assay that could be applied at near point-of-care for diagnosing and distinguishing ATB from ORDs and LTBI from HC. A literature review was undertaken to identify the most plausible host-gene markers (HGM) of TB infection. Primers, and dual labelled hydrolysis probes were designed and analytically evaluated for accuracy in an in-vitro model of infection using a lung fibroblast cell-line. Best performing genes were multiplexed into panels of 2-4 targets and taken forward for clinical evaluation. Mycobacteria Growth Indicator Tube and QuantiFERON-TB Gold Plus were used as reference tests for ATB and LTBI respectively. A total of 16 HGM were selected and incorporated into five multiplex RT-qPCR panels. PCR assay efficiency of all evaluated targets was ≥ 90% with a median analytical sensitivity of 292 copies/ul [IQR: 215. 0-358. 3 copies/ul], and a median limit of quantification of 61. 7 copies/ul [IQR: 29. 4-176. 3 copies/ul]. Clinically, ATB was characterised by higher gene expression than ORDs, while LTBI was associated with lower gene expression than HC, Kruskal-Wallis p 

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Concepts Keywords
Higher Active tuberculosis
Mycobacteria Adult
Pcr Biomarkers
Pulmonary Biomarkers
Tuberculosis Diagnosis
Female
Host gene expression
Humans
Latent Tuberculosis
Latent tuberculosis
Male
Mycobacterium tuberculosis
Reverse transcriptase-quantitative PCR
Tuberculosis
Tuberculosis, Pulmonary

Semantics

Type Source Name
disease MESH infection
disease MESH tuberculosis
pathway KEGG Tuberculosis
disease MESH respiratory diseases
disease IDO assay
disease IDO host
disease IDO cell
drug DRUGBANK Gold
disease IDO blood
disease MESH latent infection
disease MESH Latent tuberculosis
disease MESH morbidity
drug DRUGBANK Coenzyme M
disease MESH COVID 19 pandemic
drug DRUGBANK BCG vaccine
disease IDO ribonucleic acid
drug DRUGBANK Cefaclor
disease IDO colony
drug DRUGBANK Phenol
drug DRUGBANK Ethanol
drug DRUGBANK Water
disease IDO reagent
drug DRUGBANK Fluorescein
disease IDO nucleic acid
disease IDO bacteria
drug DRUGBANK Sodium hydroxide
drug DRUGBANK Phosphate ion
drug DRUGBANK Amphotericin B
drug DRUGBANK Nalidixic acid
drug DRUGBANK Trimethoprim
disease MESH Tuberculosis Pulmonary

Original Article

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