Overexpression Of Both Erg11 And Abc2 Genes Might Be Responsible For Itraconazole Resistance In Clinical Isolates Of Candida Krusei

ObjectiveTo study the main molecular mechanisms responsible for itraconazole resistance in clinical isolates of Candida krusei.MethodsThe 14 alpha-demethylases encoded by ERG11 gene in the 16 C. krusei clinical isolates were amplified by polymerase chain reaction (PCR), and their nucleotide sequences were determined to detect point mutations. Meanwhile, ERG11 and efflux transporters (ABC1 and ABC2) genes were determined by quantitative real-time reverse transcription polymerase chain reaction (qRT-PCR) for their expression in itraconazole-resistant (R), itraconazole-susceptible dose dependent (SDD) and itraconazole-susceptible (S) C. krusei at the mRNA level.ResultsWe found 7-point mutations in ERG11 gene of all the C. krusei clinical isolates, including 6 synonymous mutations and 1 missense mutation (C44T). However, the missense mutation was found in the three groups. The mRNA levels of ERG11 gene in itraconazole-resistant isolates showed higher expression compared with itraconazole-susceptible dose dependent and itraconazole-susceptible ones (P = 0.015 and P = 0.002 respectively). ABC2 gene mRNA levels in itraconazole-resistant group was significantly higher than the other two groups, and the levels of their expression in the isolates appeared to increase with the decrease of susceptibility to itraconazole (P = 0.007 in SDD compared with S, P = 0.016 in SDD with R, and P<0.001 in S with R respectively). While ABC1 gene presented lower expression in itraconazole resistant strains. However, the mRNA levels of ERG11, ABC1 and ABC2 in a C. krusei (CK10) resistant to both itraconazole and voriconazole were expressed highest in all the itraconazole-resistant isolates.ConclusionsThere are ERG11 gene polymorphisms in clinical isolates of C. krusei. ERG11 gene mutations may not be involved in the development of itraconazole resistance in C. krusei. ERG11 and ABC2 overexpression might be responsible for the acquired itraconazole resistance of these clinical isolates.