Multilocus Sequence Typing (MLST) Genotypes of Candida glabrata Bloodstream Isolates in Korea: Association With Antifungal Resistance, Mutations in Mismatch Repair Gene (Msh2), and Clinical Outcomes.

Candida glabrata bloodstream infection (BSI) isolates from a particular geographic area have been reported to comprise a relatively small number of the major sequence types (STs) by multilocus sequence typing (MLST) analysis. Yet little is known about the characteristics of major ST strains of C. glabrata. To address this question in Korea, we investigated antifungal resistance and non-synonymous mutations of the mismatch repair gene (msh2 mutations) in C. glabrata BSI isolates, as well as associated clinical characteristics, and compared the results according to MLST genotype. We assessed a total of 209 C. glabrata BSI isolates from seven hospitals in Korea for 2 years (2009 and 2014). Clinical features of candidemia and their outcomes were analyzed for 185 available cases. According to MLST, ST7 (47.8%) was the most common type, followed by ST3 (22.5%); the remainder represented 28 types of minor STs (29.7%). Fluconazole-resistance (FR) rates for ST7, ST3, and other strains were 9.0% (9/100), 8.5% (4/47), and 4.8% (3/62), respectively, and all were susceptible to amphotericin B and micafungin. All ST7 isolates harbored the V239L mutation in msh2, known to confer hypermutability, while 91.5% of ST3 isolates did not harbor the msh2 mutation. Overall, isolates of the same ST had identical msh2 mutations, with the exception of nine isolates. The msh2 mutations were identified in 68.8% (11/16) of the FR isolates and 67.4% (130/193) of the fluconazole susceptible-dose dependent isolates. There was no significant difference in all clinical characteristics between ST3 and ST7. However, the 30-day mortality of C. glabrata candidemia due to the two major ST (ST3 or ST7) strains was significantly higher than that of candidemia due to other minor ST strains (45.1 vs. 25.0%, p < 0.05). Multivariate logistic regression analysis also showed that two major STs (ST3 and ST7) were independent predictors of 30-day mortality. This study showed for the first time that two STs (ST7 and ST3) were predominant among BSI isolates in Korea, and that C. glabrata BSI isolates belonging to two major MLST genotypes are characterized by higher mortality. In addition, most msh2 mutations align with MLST genotype, irrespective of FR.

Introduction

Candida glabrata is a commensal yeast in the human gastrointestinal tract, genitourinary tract, or oral cavity, but can cause serious bloodstream infections (BSI) in hospitalized patients. Compared with other common Candida species, C. glabrata has intrinsically low susceptibility to azole drugs, especially to fluconazole, but it can develop antifungal resistance rapidly in response to exposure to azoles or echinocandins (Pfaller et al., 2003; Barberino et al., 2006; Jensen et al., 2015). The frequency of BSI due to C. glabrata has increased significantly over the past two decades, and C. glabrata has become the second most commonly isolated bloodstream fungal pathogen in Europe and North America, with 10–30% of isolates being fluconazole resistant (FR) (Pfaller et al., 2007). However, geographic variation has been observed in both the frequency of isolation and fluconazole resistance among C. glabrata (Pfaller et al., 2010). C. glabrata is the fourth most common cause of candidemia, accounting for 14.2% of all cases of candidemia in Korea, and the incidence of C. glabrata candidemia and fluconazole resistance varies among hospitals (Won et al., 2015). Although the use of fluconazole is associated with an increased risk of BSIs caused by C. glabrata (Chow et al., 2008; Jensen et al., 2015; Won et al., 2015), many questions regarding the epidemiology of C. glabrata BSI remain unanswered (Lott et al., 2010).

Candida glabrata is a haploid organism in which a single DNA repair mutation is sufficient to cause an associated mutator phenotype and subsequent emergence of resistance-conferring mutations (Healey et al., 2016b). A recent study suggested that elevated levels of both triazole and multi-drug resistance associated with C. glabrata are at least partially due to the presence of loss-of-function mutations in the mismatch repair gene (msh2 mutations) (Healey et al., 2016b). Other factors may also play a role, especially in the setting of low echinocandin and polyene resistance, as reported in France, where fluconazole resistance was not associated with the MSH2 genotype pointing to other potential underlying factors (Dellière et al., 2016). Yet, genotype and MSH2 status can be an important factor, as a recent multilocus sequence typing (MLST) study of clinical C. glabrata strains showed that different sequence types (STs) may carry different msh2 alleles, suggesting that some determinants of drug resistance or virulence may also vary among STs (Healey et al., 2016a). MLST studies of C. glabrata BSI isolates conducted in the United States or China have indicated that C. glabrata BSI isolates comprise a relatively small number of the major STs, although these major STs may vary geographically (Lott et al., 2010, 2012; Hou et al., 2017). It is possible that major ST strains of C. glabrata possess higher virulence traits to cause BSIs than do other isolates, or different clinical characteristics. Until now, few studies have evaluated the microbiological and clinical characteristics of major ST strains of C. glabrata from a multicenter BSI surveillance study. The objectives of this study were to detect the major MLST genotypes among C. glabrata BSI isolates in Korean hospitals, and to evaluate whether C. glabrata BSI strains belonging to the major MLST genotypes have different clinical characteristics, and they display different rates of antifungal resistance or msh2 mutations.

Materials and Methods

Microorganisms

A total of 209 non-duplicate isolates of C. glabrata recovered from blood cultures were included in this study. These isolates were recovered from seven Korean university hospitals during nationwide surveillance studies. Of the 209 BSI isolates, 94 were collected from September 2009 to August 2010 (period 1), and 115 were collected from January to December 2014 (period 2). All isolates were collected from blood cultures by routine methods in use in each laboratory. All C. glabrata isolates were submitted to Chonnam National University Hospital for testing. Species identification was based on colony morphology on CHROMagar Candida (BBL, Becton Dickinson, Sparks, MD, United States) at 35°C, and a commercial identification system (API 20C; bioMérieux, Marcy L’Etoile, France, or the Vitek 2 system; Vitek 2 ID-YST, bioMérieux). The isolates which did not belong to common STs in this study were re-identified by sequencing of the internal transcribed spacer (ITS) of ribosomal DNA and matrix-assisted laser desorption/ionization-time of flight mass spectrometry (MALDI–TOF Biotyper, Bruker Daltonics, Billerica, MA, United States) to differentiate from cryptic species within the C. glabrata complex (Lee et al., 2017). All isolates were confirmed as C. glabrata.

Antifungal Susceptibility Testing

In vitro testing of susceptibility to fluconazole, voriconazole, amphotericin B, and micafungin was performed on all isolates using the Clinical and Laboratory Standards Institute (CLSI) broth microdilution (BMD) method, according to document M27-A3; minimum inhibitory concentrations (MICs) were determined after 24 h of incubation (Clinical Laboratory Standards Institute [CLSI], 2008). Species-specific clinical breakpoints proposed by the CLSI document M27-S4 were used for the categorical interpretation for fluconazole and micafungin MICs (Clinical and Laboratory Standards Institute [CLSI], 2012). In addition, the epidemiologic cutoff values (ECVs) were used for the threshold for resistance to voriconazole and amphotericin B, as the CLSI has not set clinical breakpoints for these two antifungal agents against C. glabrata (Pfaller and Diekema, 2012). Two reference strains, Candida parapsilosis ATCC 22019 and Candida krusei ATCC 6258, were included in each antifungal susceptibility test as quality control isolates.

MLST

MLST was performed using a procedure described previously (Dodgson et al., 2003). The six genes selected for MLST analysis were FKS, LEU2, NMT1, TRP1, UGP1, and URA3. The reaction products were analyzed using an ABI Prism 3130xl Genetic Analyzer (Applied Biosystems). The allele profiles of the strains were defined according to the six MLST loci. Each unique allele profile was designated as a ST, determined using the MLST database.[1]

Sequence Analysis of the msh2 Gene

Candida glabrata genomic DNA was extracted as previously described (Dodgson et al., 2003), using the DNeasy Mini kit (Qiagen Inc., Valencia, CA, United States), and used as the template for amplification of the full-length msh2 gene. Primers used for amplification and sequencing of msh2 were as follows (Healey et al., 2016b): for amplification, 5′-CGATGAGCCGATCACTTTAC-3′ (CgMSH2u273F) and 5′-ACTTATCGAGGCACTCAGTC-3′ (CgMSH2d145R); for sequencing, 5′-ACCTAGCATCTCTTGTTCAC-3′ (CgMSH2c846R), 5′-CCTGGTCAATCTCATACACC-3′ (CgMSH2c1626R), 5′-CCATGCAAGTCCAAAACCATC-3′ (CgMSH2c2340R), and 5′-ACTTATCGAGGCACTCAGTC-3′ (CgMSH2d145R). Amplification conditions were as follows: an initial denaturation step for 3 min at 95°C, followed by 29 cycles of denaturation for 40 s at 95°C, annealing for 90 s at 56°C, elongation for 3 min at 72°C, and a final elongation step for 10 min at 72°C. Polymerase chain reaction (PCR) products were purified using a PCR purification kit (GeneAll Biotechnology, Seoul, Korea) according to the manufacturer’s recommendations. PCR products were sequenced using the abovementioned PCR primer pairs. Sequencing of both strands was performed using the ABI PRISM 3730XL Analyzer (Applied Biosystems, Foster City, CA, United States). Nucleotide sequences were analyzed using the MegAlign software package (DNAStar Inc., Madison, WI, United States) and compared with that of the database strain, CBS138/ XM_447585.

Clinical Data Analysis

Clinical information including demographics, clinical status at positive culture, and therapy-related factors, and outcome of fungemia were collected retrospectively from 185 available patients with C. glabrata BSI (Kim et al., 2009; Choi et al., 2016). Clinical status at positive culture examined within 30 days before the candidemia occurrence included prior surgery, total parenteral nutrition use, prior antifungal exposure, immunosuppressive therapy, and neutropenia (defined as an absolute neutrophil count of 500/mm3). Severe sepsis, which was recently termed “sepsis” after the Sepsis-3 definition, was defined as life-threatening organ dysfunction caused by a dysregulated host response to infection and organ dysfunction identified as an acute change in total Sequential Organ Failure Assessment (SOFA) score (≥ 2 points) following infection (Singer et al., 2016). The “Candida score” was determined by variables including total parenteral nutrition, surgery, multifocal Candida colonization, and severe sepsis (Leon et al., 2006). The age-adjusted Charlson comorbidity index (ACCI) was calculated using the algorithm proposed by Charlson et al., in which 19 comorbid conditions are weighted and scored, with additional points added for age (Charlson et al., 1987; Hall et al., 2004). Patient outcome (survival or death) was assessed as all-cause mortality at 7, 30, 60, 90, and 120 days after the first positive blood culture result. This study was approved by the Institutional Review Board of Chonnam National University Hospital (IRB CNUH-2014-290). A waiver of the requirement for informed consent was granted given the retrospective nature of the project. Patient information was anonymized and de-identified prior to the analysis, and no information that could lead to patient identification was used.

Statistical Analysis

Quantitative variables are expressed as means and standard deviation, and categorical variables as counts and percentages. Comparison of categorical variables between groups was performed using the χ2 or Fisher’s exact t-test. The independent t-test was used to compare continuous variables between two groups, the Mann–Whitney U test to compare continuous variables with non-normal distributions, and one-way analysis of variance (ANOVA) to compare variables among more than three groups, as appropriate (Jung et al., 2016). The predictive factors for 30-day mortality were analyzed using univariate and multivariate logistic regression analysis (Agresti, 2013). Variables with p < 0.1 in univariate analyses were included in multivariate regression models. The Cox proportional hazard model was used to evaluate potential risk factors for 30-day mortality by the hazard ratio (HR). The Kaplan–Meier method was used to calculate 120-day survival probability in subgroup analyses. All statistical analyses were performed using SPSS software (ver. 18.0; SPSS Inc., Chicago, IL, United States), and significance was determined at a level of p < 0.05.

Results

MLST and Antifungal Susceptibility

MLST results and the prevalence of FR among 209 BSI isolates of C. glabrata from 209 patients of seven Korean hospitals (hospitals A–G) spanning two time periods: September 2009 to August 2010 (period 1; n = 94), and January to December 2014 (period 2; n = 115) are shown in Table . Overall, 30 unique STs among the 209 clinical isolates were obtained. A total of 191 isolates belonged to the 12 previously described STs (2, 3, 6, 7, 10, 12, 19, 22, 26, 46, 55, and 59), whereas 18 isolates belonged to 18 new STs. Twenty STs were each derived from a single isolate, and ten STs were shared by 189 isolates (90.4%). ST7 (100 isolates, 47.8%) was the most common type, followed by ST3 (47 isolates, 22.5%), ST22 (12 isolates, 5.7%), and ST10 (9 isolates, 4.3%). ST7 represented 50.0% (47/94) and 46.1% (53/115) of all C. glabrata BSI isolates obtained during study periods 1 and 2, respectively, and ST3 represented 17.0% (16/94) and 27.0% (31/115) of all C. glabrata BSI isolates obtained during study periods 1 and 2, respectively. The major two ST types, ST7 and ST3, were found in all 7 hospitals through the study periods, however, the other STs were scattered in some hospitals. Overall, two major STs (ST7 and ST3) comprised 70.3% (147/209) of all C. glabrata BSI isolates obtained during the study periods. Of the 209 isolates, 16 (7.7%) were resistant to both fluconazole (MIC ≥ 64 μg/ml) and voriconazole (MIC > 0.5 μg/ml). All isolates were susceptible to amphotericin B (≤ 2 μg/ml) and micafungin (≤ 0.06 μg/ml). The FR rates were not significantly different among ST7, ST3, and other minor ST isolates, at 9.0% (9/100), 8.5% (4/47), and 4.8% (3/62), respectively. The FR rates were 5.3% (5/94) and 9.6% (11/115) during periods 1 and 2, respectively.

Mutations in msh2

Non-synonymous mutations in the mismatch repair gene (msh2 mutations) according to MLST genotype and fluconazole and voriconazole susceptibilities are described in Table . All 16 FR isolates and one FS (MIC, 32 μg/ml) isolate were resistant to voriconazole. Msh2 mutations occurred in 65.1% (136/209) of the C. glabrata BSI isolates from Korean hospitals. Msh2 mutations were detected in 68.8% (11/16) of FR isolates and 67.4% (130/193) of fluconazole susceptible-dose dependent (FS) isolates. Among the 189 BSI isolates that shared 10 STs (excluding 20 STs unique to a single isolate), isolates of the same ST harbored identical msh2 mutations, with the exception of seven isolates: ST7 (three isolates), and ST3 (four isolates) showed an additional mutation compared with their ST strains. All 100 isolates of ST7 (nine FR and 91 FS) harbored the V239L mutation, associated with prominent hypermutability, and three isolates showed additional msh2 mutations (V63F, V615A, or G204A). Among the 47 ST3 isolates, only four FS isolates harbored E7K (two isolates), Y167N (one isolate), or S118N (one isolate) mutations, and no non-synonymous mutations were found in 91.5% (43/47) of the ST3 isolates. All 12 ST22 isolates possessed the E456D mutation and all 9 ST10 isolates possessed the P208S/N890I mutation. No mutations were observed in any of the isolates of ST55 (five isolates), ST6 (four isolates), ST26 (four isolates), or ST59 (two isolates). Two isolates of ST12 harbored the E456D mutation. Overall, the MSH2 sequence analysis revealed that the majority of isolates harbored the V239L (112 isolates, 53.6%), followed by no mutation (69 isolates, 33.0%), E456D (15 isolates, 7.2%), and P208S/N890I (9 isolates, 4.3%), respectively. Msh2 mutations were found in 100% (100/100), 8.5% (4/47), and 59.7% (37/62) of ST7, ST3, and other isolates, respectively.

Clinical Characteristics and Mortality

A total of 185 patients were assessed to obtain data to predict clinical outcomes. Among all 185 patients, overall cumulative mortality occurred in 19.5, 39.5, and 47.0% at 7, 30, and 60 days after positive blood culture. Table summarizes the clinical characteristics of 185 patients infected with ST3, ST7, or the other minor ST BSI strains of C. glabrata. There were no significant differences among these three groups with respect to age, sex, or clinical status at positive culture. However, significant differences were found among the three groups in 30-day mortality rate (43.3, 48.8, and 25.0% for ST7, ST3, and minor STs, respectively; p = 0.035), and 60-day mortality rate (53.3% vs. 53.5% vs. 30.8%, p = 0.022, respectively), respectively. There were no significant differences among clinical characteristics between ST3 and ST7. When two major ST strains (ST7 and ST3) and other minor strains were considered, there were significant difference between two groups in neutropenia (two major STs vs. the minor STs; 9.0% vs. 0.0%, p = 0.025), 30-day mortality rate (two major STs vs. the minor STs; 45.1% vs. 25.0%, p = 0.012), 60-day mortality rate (two major STs vs. the minor STs; 53.4% vs. 30.8%, p = 0.006) and 120-day mortality rate (two major STs vs. the minor STs; 56.4% vs. 36.5%, p = 0.015; Table ).

Table shows the results of univariate and multivariate logistic regression analyses performed to identify risk factors for 30-day mortality. Based on the full multivariate model, the major STs (odd ratio [OR]: 4.058; 95% confidence interval [CI]: 1.349-12.201; p = 0.013), severe sepsis (OR: 9.886; 95% CI: 2.472-39.540; p = 0.001), and lack of antifungal therapy (OR: 2.850; 95% CI: 1.026–7.918; p = 0.044) were independent predictors of 30-day mortality. The adjusted Cox proportional hazard model revealed that stains with the two major STs (HR: 2.706; 95% CI: 1.236–5.921; p = 0.013) and severe sepsis (HR: 4.577; 95% CI: 1.884–11.119; p = 0.001) were significantly associated with 30-day mortality, in addition to lack of antifungal therapy (HR: 3.164; 95% CI: 1.733–5.777: p < 0.001), respectively (Figure ). Kaplan–Meier survival analysis showed that the differences in mortality between patients with two major STs and those with other minor STs were sustained (p = 0.0067; log-rank tests). Patients with the two major STs experienced shorter survival than those with other minor STs (p = 0.0184 for 120-day survival; p = 0.0231 for 90-day survival; p = 0.0115 for 60-day survival; p = 0.0215 for 30-day survival; p = 0.0405 for 7-day survival; log-rank tests; Figure ). There were no significant differences in clinical characteristics, including mortality rate, according to the msh2 mutation type.

Hazard ratios (HRs) for 30-day mortality according to various factors. Lines indicate HRs and their 95% confidence intervals (CIs) for all variables suggested as prognostic factors for 30-day mortality by univariate analysis (p < 0.1) (Table ). Asterisks indicate p < 0.05 in adjusted HRs. Abbreviations: Major STs, major sequence types (ST7 or ST3) by multilocus sequence typing (MLST; ACCI, age-adjusted Charlson comorbidity index; ICU, intensive care unit.

Survival analysis for candidemia patients. Patients with bloodstream infections were grouped according to MLST type (ST3, ST7, or Other STs) and censored at death or day 120. There was a significant difference in mortality rate between the curves.

Discussion

To our knowledge, this is the first study to report that two major ST (ST7 and ST3) strains, comprising 70.3% of all C. glabrata BSI isolates from Korean hospitals, are linked to higher mortality in candidemia patients. The rates of antifungal resistance were not significantly different among ST7, ST3, and other strains. Of the two major STs, ST7 isolates harbored the same V239L substitution in msh2, which is associated with hypermutability, whereas nearly all ST3 isolates lacked msh2 mutations. Overall, we found that occurrences of most msh2 mutations were associated with specific MLST genotypes, irrespective of FR. The present study highlights that MLST genotypes are associated not only with particular msh2 mutations but also with the prediction of mortality in candidemia patients with C. glabrata.

To date, only a few studies have investigated the MLST genotypes of BSI isolates of C. glabrata collected by multicenter surveillance (Lott et al., 2010, 2012; Hou et al., 2017). MLST of 230 BSI isolates in three United States cities showed that three STs (ST3, ST16, and ST19) were the most abundant, together comprising 51% of all BSI isolates (Lott et al., 2010). The prevalence of ST16 among BSI isolates of C. glabrata in Atlanta-area hospitals increased significantly between 1992 and 1993 (4%) and 2008 (40%). An increase was also observed for ST3, from 19 to 28%, but the prevalence of ST19 did not change (Lott et al., 2010). A recent study from China showed that ST7 and ST3 were the most common STs (68.0 and 9.0% of all 200 BSI isolates, respectively; Hou et al., 2017). In the present study, ST7 and ST3 were the predominant genotypes (47.8 and 22.5% of all BSI isolates, respectively) among 209 BSI isolates. During the two study periods, the prevalence of ST7 remained unchanged at 4.5-year intervals (50.0 and 46.1%, respectively), but that of ST3 increased (17 and 27%, respectively), suggesting that ST3 strains evolved for optimal adaptation to new environments as causative agents of BSI in Korea. No ST16 strain was isolated in either of two studies in China (Hou et al., 2017) or Korea (present study). Collectively, our results support the notion that the major MLST genotypes of C. glabrata BSI isolates vary both geographically and over time.

Clinical characteristics of the specific MLST genotypes of C. glabrata BSI isolates has not previously been reported. In the present study, cumulative mortalities of C. glabrata BSI at 7 and 30 days after the first episode of candidemia were 19.5 and 39.5%, respectively, which is similar to previous reports (Lortholary et al., 2014; Ding et al., 2015). Notably, we found a significant difference in the 30-day mortality of C. glabrata candidemia due to the two major ST (ST3 or ST7) strains and in that of candidemia due to other minor ST strains (45.1% vs. 25.0%). There were no significant differences in all clinical characteristics between ST3 and ST7. We could not find significant differences in other clinical features between patients with either of the two major STs or other minor STs, except for neutropenia. Although neutropenia may have an impact on the mortality of C. glabrata fungemia (Wu et al., 2017), only 12 patients (6.5%) had neutropenia in the present study. We found the same results that two major STs were associated with higher 30-day mortality than other minor STs, even after we removed the data for the 12 patients with neutropenia.

Multivariate logistic regression identified the two major STs, severe sepsis, and lack of antifungal therapy as independent variables associated with a higher 30-day mortality rate. The adjusted Cox proportional hazard model also revealed that the two major STs and severe sepsis were significantly associated with 30-day mortality, in addition to lack of antifungal therapy. Proper administration of antifungal agents (Bassetti et al., 2017) or therapeutic measures such as antifungal treatment within the first 48 h (Garnacho-Montero et al., 2017), severe sepsis and septic shock (Puig-Asensio et al., 2014; Garnacho-Montero et al., 2017) have been reported as variables independently associated with 30-day mortality of candidemia. However, candidemia due to the two major ST strains of C. glabrata was more likely to be fatal than candidemia due to other strains in our cohort. The Kaplan–Meier survival analysis also showed that the differences in mortality between the major STs and the other minor STs were sustained from 30 to 120 days after positive blood culture. Although it is difficult to establish that the death of a patient was attributable solely to candidemia, a link between the presence of two ST strains and increased mortality seems the likely explanation for our data.

A recent study reported that msh2 mutations varied according to MLST genotypes; however, only 48 clinical isolates were tested (Healey et al., 2016a). In our work, we compared msh2 mutations by MLST genotype using 209 BSI isolates from seven hospitals during a 2-year period, and demonstrated that most isolates of the same ST harbored identical msh2 mutations. Among the 189 BSI isolates that shared 10 STs (excluding 20 STs unique to a single isolate) in the present study, isolates of the same ST harbored identical msh2 mutations, with the exception of nine isolates that showed an additional mutation compared to their ST strains. In a previous report, strains harboring V239L/A942T or V239L in msh2 were identified in centers in the United States, Switzerland, Qatar, and India, but the majority of strains isolated from United States medical centers exhibited E231G/L269F or P208S/N890I mutations (Healey et al., 2016a). In the present study, the majority of isolates (53.6%) harbored V239L, followed by no mutation (33.0%), E456D (7.2%), and P208S/N890I (4.3%). Our data suggest that geographic differences in the frequency of msh2 mutations in clinical C. glabrata isolates (Healey et al., 2016b) may reflect differences in the distribution of the major MLSTs of C. glabrata among hospitals or geographic locales.

It has been reported that msh2 mutations are more frequent among FR (65%) and multidrug resistant (62%) C. glabrata isolates than among FS isolates (52%) (Healey et al., 2016b). However, among the 209 BSI isolates in the current study, the frequency of msh2 mutations was similar between FS (67.4%, 130/193) and FR (68.8%, 11/16), which is consistent with the findings of a recent study (Dellière et al., 2016). In the present study, the rate of msh2 mutations was different among ST7 (100%), ST3 (8.5%), and other (58.1%) strains, but FR rates did not differ significantly among ST7 (9.0%), ST3 (8.5%), and other (4.8%) strains. It is possible that not all msh2 mutations are equal and they may not all contribute to the acquisition of fluconazole resistance. Notably, V239L and P208S/N890I, but not E456D or E7K, were shown to confer partial loss of msh2 function (Dellière et al., 2016; Healey et al., 2016b); how the other msh2 polymorphisms identified within our study influence phenotype has yet to be determined. However, a more recent study has shown the absence of azole or echinocandin resistance in C. glabrata isolates in India despite background prevalence of strains with defects in DNA mismatch repair pathway; albeit, isolates were collected from patients with limited antifungal exposure. Notably, 49% of tested strains in India contained partial loss of msh2 mutation (Singh et al., 2018). Also, Healey et al. showed that additional mechanisms of DNA repair, including other MMR genes, and other cellular systems may influence the mutagenic potential of C. glabrata strains (Dellière et al., 2016). Taken together, these data suggest that msh2 mutations in C. glabrata isolates occur independently of FR acquisition, and the msh2 mutation alone is not responsible for the acquisition or increased prevalence of FR in specific STs.

Clinical outcomes of fungemia are dependent on the fungus (virulence and susceptibility), host status (severity of the underlying condition), and therapy (timing in relation to infection stage, antifungal drug choice and dosing; Arendrup, 2013). In the present study, we found that two MLST genotypes more frequently caused BSI infections than other genotypes in Korea, and mortality at 30 days was higher for BSI with two major ST strains than for BSI with other strains, suggesting that the pathogenic potential of C. glabrata, with respect to significant morbidity and mortality, may partly depend on the MLST genotype. The most likely explanation for our results is that the two major ST strains may be more virulent than other minor ST strains in Korean patients. Therefore, some of the virulence traits of C. glabrata which include growth at 37°C, high stress resistance, resistance to starvation, drug resistance, high adherence or presence of several auxotrophies (Gabaldon and Carrete, 2016) require investigation for strains of major MLST genotypes. In addition, further study of major MLST genotypes of C. glabrata BSI isolates and their expansion over time will contribute significantly to our understanding of incidence rates and patient outcomes of C. glabrata BSI, and their antifungal resistance in particular geographic locations.

Author Contributions

SK, WL, M-NK, KL, HL, and YU participated in isolate and clinical data collection. SB, EW, and MC carried out the experimental studies and performed the statistical analysis. KH and DP helped draft the manuscript. SB, EW, and JS conceived the study, participated in study design and data analysis, and were responsible for writing and submission of the final manuscript. All authors read and approved the manuscript.

Conflict of Interest Statement

The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest.

Table 1

Multilocus sequence typing (MLST) and fluconazole resistance (FR) status of 209 Candida glabrata bloodstream isolates from seven Korean hospitals.

Sequence type (ST) by MLST	Total (%), all periods	FR (%), all periods	Period†	No. of isolates (No. of FR isolates) in hospital							Subtotal (%), each period	Subtotal FR (%), each period
				A	B	C	D	E	F	G
7	100 (47.8)	9 (9.0)	1	16	12 (2)	2	3	3	3 (1)	8	47 (50.0)	3 (6.4)
			2	23 (1)	9 (3)	4	6 (2)	3	4	4	53 (46.1)	6 (11.3)
3	47 (22.5)	4 (8.5)	1	6	1	1	3	1	3	1	16 (17.0)
			2	9 (2)	9 (2)	5	2			6	31 (27.0)	4 (12.9)
22	12 (5.7)		1	2				2			4 (4.3)
			2		2	1		2		3	8 (7.0)
10	9 (4.3)		1	1	2	1		1			5 (5.3)
			2	1	3						4 (3.5)
55	5 (2.4)	1 (20.0)	1	1		1	1				3 (3.2)
			2	2 (1)							2 (1.7)	1 (50.0)
2	4 (1.9)	2 (50.0)	1		1				2 (2)		3 (3.2)	2 (66.7)
			2	1							1 (0.9)
6	4 (1.9)		1	1		1					2 (2.1)
			2						2		2 (1.7)
26	4 (1.9)		1			2					2 (2.1)
			2					1		1	2 (1.7)
12	2 (1.0)		1							1	1 (1.1)
			2	1							1 (0.9)
59	2 (1.0)		1	2							2 (2.1)
			2								0 (0.0)
Others‡	20 (9.6)		1	3	3			1		2	9 (9.6)
			2	5	2			2	1	1	11 (9.6)
Total	209 (100)	16 (7.7)	1	32	19	8	7	8	9	12	94 (100)	5 (5.3)
			2	42	25	10	8	8	7	15	115 (100)	11 (9.6)

Table 2

Non-synonymous mutations in the mismatch repair gene (msh2 mutations) in 209 C. glabrata bloodstream isolates according to MLST genotye, fluconazole and voriconazole susceptibilities.

MLST		Msh2 mutation∗	No. of isolates§				Total
ST	Allele profile†		Fluconazole susceptible-dose dependent	Fluconazole resistant	Voriconazole susceptible	Voriconazole resistant
7	3-4-4-3-3-4	V239L	88	9	87	10	100
		V63F, V239L	1		1
		V239L, V615A	1		1
		G204A, V239L	1		1
3	5-7-8-7-3-6	None	39	4	39	4	47
		E7K	2		2
		Y167N	1		1
		S118N	1		1
22	7-5-6-3-1-8	E456D	12		12		12
10	8-4-3-5-1-2	P208S, N890I	9		9		9
55	3-6-22-2-3-9	None	4	1	4	1	5
2	1-2-2-1-1-1	V239L, A942T	2	2	2	2	4
6	2-5-7-5-1-2	None	4		4		4
26	7-4-3-4-1-8	None	4		4		4
12	7-5-6-12-1-8	E456D	2		2		2
59	7-13-17-9-3-19	None	2		2		2
Others‡		V239L	9		9		9
		E456D	1		1		1
		None	10		10		10
Total			193	16	192	17	209

Table 3

Clinical characteristics of C. glabrata bloodstream isolates belonging to two major STs (ST7 and ST3) and other minor STs.

Variables	Two major MLST types			Other minor STs
	ST7	ST3	Total of two major STs
No. of patients	90	43	133	52
Demographics
Age, years, mean ± SD	68.2 ± 14.91	66.2 ± 14.22	67.5 ± 14.67	67.2 ± 12.23
Male, No. (%)	47 (52.2)	20 (46.5)	67 (50.4)	27 (51.9)
Clinical status at positive culture
Prior fungal therapy, No. (%)	12 (13.3)	8 (18.6)	20 (15.0)	3 (5.8)
Total parenteral nutrition, No. (%)	41 (45.6)	20 (46.5)	61 (45.9)	21 (40.4)
Prior surgery (1 months), No. (%)	24 (26.7)	9 (20.9)	33 (24.8)	13 (25.0)
Severe sepsis, No. (%)	46 (51.1)	20 (46.5)	66 (49.6)	27 (51.9)
Neutropenia (< 500 cell/mm3), No. (%)	7 (7.8)	5 (11.6)	12 (9.0)†	0 (0.0)
Immunosuppressive therapy, No. (%)	22 (24.4)	8 (18.6)	30 (22.6)	8 (15.4)
ICU admission, No. (%)	19 (21.1)	12 (27.9)	31 (23.3)	9 (17.3)
Urine catheter, No. (%)	54 (60.0)	26 (60.5)	80 (60.2)	30 (57.7)
CVC use, No. (%)	52 (57.8)	31 (72.1)	83 (62.4)	26 (50.0)
Candida score, mean ± SD	1.5 ± 0.91	1.3 ± 0.86	1.4 ± 0.90	1.5 ± 1.35
ACCI, mean ± SD	6.6 ± 3.10	7.3 ± 2.89	6.9 ± 3.04	6.0 ± 2.81
Therapy after positive culture
Antifungal therapy	64 (71.1)	28 (65.1)	92 (69.2)	33 (63.5)
Removal of CVC, No. (%)	40 (44.4)	26 (60.5)	66 (49.6)	24 (46.2)
Clinical outcome
7-day all-cause mortality, No. (%)	18 (20.0)	11 (25.6)	29 (21.8)	7 (13.5)
30-day all-cause mortality, No. (%)	39 (43.3)	21 (48.8)	60 (45.1)†	13 (25.0)
60-day all-cause mortality, No. (%)	48 (53.3)	23 (53.5)	71 (53.4)†	16 (30.8)
90-day all-cause mortality, No. (%)	50 (55.6)	24 (55.8)	74 (55.6)†	19 (36.5)
120-day all-cause mortality, No. (%)	51 (56.7)	24 (55.8)	75 (56.4)†	19 (36.5)

Table 4

Univariate and multivariate logistic regression analyses of prognostic factors for 30-day mortality.

Characteristic	Survivors (N = 112)	Non-survivors (N = 73)	Univariate analysis	Multivariate analysis†
			p-value	Odd ratio (95% CI)	p-value
Demographics
Age, years, mean ± SD	66.8 ± 14.99	68.4 ± 12.34
Male, No. (%)	51 (45.5)	43 (58.9)	0.075	2.413 (0.934-6.229)	0.069
Clinical status at positive culture
Prior antifungal exposure, No. (%)	11 (9.8)	12 (16.4)	0.195
Intensive care unit admission, No. (%)‡	17 (15.2)	23 (31.5)	0.02	1.238 (0.403-3.800)	0.71
Total parenteral nutrition, No. (%)	46 (41.1)	36 (49.3)	0.253
Immunosuppressive therapy, No. (%)	25 (22.3)	13 (17.8)	0.455
Neutropenia, No. (%)	5 (4.5)	7 (9.6)	0.172
Prior surgery, No. (%)	31 (27.7)	15 (20.5)	0.269
Severe sepsis, No. (%)‡	41 (36.6)	52 (71.2)	< 0.001	9.886 (2.472-39.540)	0.001
CVC use, No. (%)	66 (58.9)	43 (58.9)	0.97
Urine catheter, No. (%)‡	60 (53.6)	50 (68.5)	0.036	1.973 (0.573-6.792)	0.281
Candida score, mean ± SD‡	1.3 ± 0.85	1.7 ± 1.24	0.009	0.729 (0.359-1.480)	0.381
ACCI, mean ± SD‡	6.3 ± 2.84	7.2 ± 3.16	0.045	1.053 (0.889-1.246)	0.551
Therapy after positive culture
Removal of CVC, No. (%)	52 (46.4)	38 (52.1)	0.246
Lack of antifungal therapy, No. (%)‡	29 (25.9)	31 (42.5)	0.019	2.850 (1.026-7.918)	0.044
C. glabrata isolate
Major STs (ST 7 or ST 3)‡	73 (65.2)	60 (82.2)	0.01	4.058 (1.349-12.201)	0.013
Fluconazole resistance	6 (5.4)	7 (9.6)	0.277