Prevalence and Genotypic Characterization of Extended-Spectrum Beta-Lactamases Produced by Gram Negative Bacilli at a Tertiary Care Hospital in Rural South Western Uganda.

Moses A Bwanga F Boum Y Bazira J
British microbiology research journal 2014 Dec ; 4(12); 1541-1550. doi: 10.9734/BMRJ/2014/9792. Epub 2018 11 13
Antibiotics ESBL Uganda resistance patterns sensitivity patterns

Abstract

AIM: To determine the prevalence and genotypic characterisation of extended spectrum beta-lactamases produced by gram negative bacilli isolated at Mbarara Regional Referral Hospital (MRRH).

SAMPLES: Gram negative clinical isolates.

STUDY DESIGN: Laboratory-based descriptive cross-sectional study.

PLACE AND DURATION OF THE STUDY: MRRH, June and August 2012.

METHODS: Gram negative clinical isolates were sub cultured, and identified using biochemical tests. They were screened for ESBL by using oxyimino-cephalosporins and confirmed by double disc synergy Genotyping was performed using the PCR for TEM, SHV and CTX-M. Susceptibility pattern for the extended spectrum beta-lactamases, (ESBL) - positive isolates to other antibiotic classes was performed by the Kirby Bauer Technique.

RESULTS: A total of 484 isolates were included in the study. The commonest ESBL producers were (34%), followed by unidentified (19.3%) spp. (12.7%). Phenotypically, 88/484 were ESBL producers while genotypically 213/ 484 possessed ESBL genes. The ESBL genes were (146; 70%), (72; 34%) and (100; 47%). 87of 213 isolates expressed more than one ESBL gene. Of these 36 (7.4%) produced / 28 (5.8%) CTX-M /TEM, 4 (0.8%) SHV/ TEM and 19 (3.9%) CTX-M/SHVTEM. Sixty two (16%) were phenotypically and genotypically positive, 12 (3%) of the isolates were phenotypically positive but genotypically negative and 140 (37%) isolates were phenotypically negative but genotypically positive. The ESBL producers were highly susceptible to imipenem (95%), nitrofurantoin (66%) but less susceptible to ampicillin (4%) and ticarcillin (7%).

CONCLUSION: ESBL production among the Gram-negative clinical isolates at MRRH is very high with several isolates possessing multiple genes. The ESBL producers are highly susceptible to imipenem, but very resistant to ciprofloxacin.