Drug Resistance in Tuberculous Lymphadenitis: Molecular Characterization

Author:

Assefa Gebeyehu12ORCID,Desta Kassu2,Araya Shambel2ORCID,Girma Selfu1ORCID,Hailu Elena1ORCID,Mihret Adane1ORCID,Hailu Tsegaye1,Tilahun Melaku1ORCID,Diriba Getu3ORCID,Dagne Biniyam3ORCID,Atnafu Abay1ORCID,Endalafer Nigatu1,Abera Adugna3,Bekele Shiferaw1,Mengistu Yordanos4,Bobosha Kidist1ORCID,Aseffa Abraham1ORCID

Affiliation:

1. Armauer Hansen Research Institute, AHRI, Addis Ababa, Ethiopia

2. Department of Medical Laboratory Sciences, College of Health Sciences, Addis Ababa University, Addis Ababa, Ethiopia

3. Ethiopian Public Health Institute, EPHI, Addis Ababa, Ethiopia

4. Haramaya University, Harar, Ethiopia

Abstract

Background. Drug-resistant tuberculosis (TB) epidemic in high-TB-incidence countries, particularly Ethiopia, remains a significant challenge. As a result, we investigated the drug resistance, common gene mutation, and molecular characterization of mycobacterial isolates from patients with suspected tuberculous lymphadenitis (TBLN). Methodology. A cross-sectional study of 218 FNA samples from TBLN patients inoculated on Lowenstein-Jensen media was carried out. The culture isolates were identified as MTB by polymerase chain reaction (PCR) and the difference-9 (RD9) test region. In addition, the GenoType MTBDRplus assay tested the first and second-line MTB drugs, and the spoligotyping strain-dependent polymorphism test was determined. Results. Among the 50 culture-positive isolates, 14% (7/50) had drug resistance caused by a gene mutation. Out of these, 4 (8%) isolates were mono-resistant to isoniazid drug, which is caused by a gene mutation in katG in the region of interrogated at codon 315 in the amino acid sequence of S315T1, and 3 (6%) isolates were resistant to both rifampicin and isoniazid drugs. The mutation was observed for katG (at codon 315 with a change in the sequence of amino acid S315T) and rpoB (at codon 530–533 with a change in the sequence of amino acid S531L (S450L)) genes. The most prevalent spoligotypes were orphan and SIT53 strains. Conclusion. The predominance of INH mono-resistance poses a critical risk for the potential development of MDR-TB, as INH mono-resistance is a typical pathway to the occurrence of MDR-TB. The orphan and SIT53 (T) strains were the most common in the study area, and a drug-resistant strain caused by a common gene mutation could indicate the transmission of clonal-resistant strains in the community.

Funder

AHRI core budget

Publisher

Hindawi Limited

Subject

General Earth and Planetary Sciences,General Engineering,General Environmental Science

Reference42 articles.

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