| Literature DB >> 22860144 |
Emmanuelle Cambau1, Aurélie Chauffour-Nevejans, Liana Tejmar-Kolar, Masanori Matsuoka, Vincent Jarlier.
Abstract
BACKGROUND: Although leprosy is efficiently treated by multidrug therapy, resistance to first-line (dapsone, rifampin) and to second-line drugs (fluoroquinolones) was described worldwide. Since Mycobacterium leprae is not growing in vitro, phenotypic susceptibility testing requires a one year experiment in the mouse model and this is rarely performed. Genetics on antibiotic resistance provide the basis for molecular tests able to detect for antibiotic resistance in leprosy. METHODOLOGY/PRINCIPALEntities:
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Year: 2012 PMID: 22860144 PMCID: PMC3409109 DOI: 10.1371/journal.pntd.0001739
Source DB: PubMed Journal: PLoS Negl Trop Dis ISSN: 1935-2727
Probes and primers used in the GenoType Leprae DR test for molecular detection of antileprosy resistance.
| Antibiotic | Gene | Probe | Targeted codon(s) or mutation |
| Rifampin |
| WT1 | 432 |
| WT2 | 438–441 | ||
| WT3 | 451 | ||
| WT4 | 456–458 | ||
| MUT1 | S456L | ||
| MUT2 | H451Y | ||
| Ofloxacin |
| WT | 89–91 |
| MUT | A91V | ||
| Dapsone |
| WT | 53–55 |
| MUT | P55L |
na, non applicable.
numbering system used in the M. leprae genome of strain NT (sequence NC 002677 in GenBank).
List of mutations present in the M. leprae resistant strains.
| Mutations in the region determining resistance in the following genes (N strains) | ||
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|
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| S456L (10) | P55L (8) | A91V (4) |
| S456F (1) | P55R (3) | |
| S456M + L458V (1) | T53I (7) | |
| H451Y (1) | T53A (3) | |
| G432S + H451D (1) | T53V (1) | |
| T433I + D441Y (1) | ||
| Q438V (1) | ||
Figure 1Mutations conferring resistance in Mycobacterium leprae are detected by the GenoType LepraeDR DNA strip test.
Lane 1 is a negative control (only the CC band). Lanes 2 to 11 showed various profiles for resistant strains: lane 2, rpoB mutation S456L with wild type gyrA and folP1 alleles; lane 3, wild type rpoB and gyrA alleles with a folP1 mutation to be defined; lane 4, rpoB mutation S456L with a wild type gyrA allele but a mutation in folP1; lane 5, rpoB mutation (Q438V) with wild type gyrA and folP1 alleles; lane 6, wild type rpoB and gyrA alleles with a P55L mutation in folP1; lane 7, rpoB mutation S456L with a A91V gyrA mutation and a P55L mutation in folP; lane 8 and lane 9, wild type rpoB and gyrA alleles with a P55L mutation in folP1 ; lane 10 and lane 11, rpoB mutation S456L with wild type gyrA and folP1 alleles. The numbering system used is that of the Mycobacterium leprae genome strain NT (n°NC 002677).
Figure 2Mycobacterium leprae susceptible strains showed a wild type profile in the GenoType LepraeDR test.
Lane 1 to 16 (except lane 8) showed wild type profiles for susceptible M. leprae strains. Lane 8 showed a multiresistant profile with mutations in rpoB, gyrA and folP1 genes. Lanes 17 and 18 showed result of negative controls.
Concordance of results for the DNA strip test (GenoType LepraeDR) and the susceptibility phenotypic and genotypic pattern of antibiotic resistance for the M. leprae strains studied.
|
| N diagnosis tests with interpretable results | Concordance GenoType LepraeDR N strains (%) | |||
| In vivo susceptibility testing | PCR sequencing | DNA strip test | versus in vivo Susceptibility testing | versus PCR sequencing | |
| Total tested for at least one antibiotic | 84 | 120 | 120 | 84 (100%) | 120 (98%) |
| Rifampin resistant | 13 | 16 | 16 | 13 (100%) | 16 (100%) |
| Rifampin susceptible | 71 | 104 | 104 | 71 (100%) | 102 |
| Dapsone resistant | 8 | 22 | 22 | 8 (100%) | 22 (100%) |
| Dapsone susceptible | 48 | 98 | 98 | 48 (100%) | 98 (100%) |
| Ofloxacin resistant | 1 | 4 | 4 | 1 | 4 |
| Ofloxacin susceptible | 4 | 56 | 56 | 4 | 56 (100%) |
For strains growing in vivo and yielding interpretable susceptibility results. Tests were stopped for dapsone due to new regulation for antibiotic animal feeding. Tests for ofloxacin were restricted to patient with previous treatment by fluoroquinolones.
including two strains with a mutation at codon 447: Ser447Cys for one strain and a silent mutation for the second strain (see text for details).