Among patients with WRN. doi:10.1371/journal.pone.0057661.t{Warfarin-Related Nephropathy in Korean PatientsWRN. The more severe clinical picture of patients with atrial fibrillation, such as old age, more comorbidities, and worse renal function at baseline and after follow-up than patients without atrial fibrillation denied the MK 8931 site possibility that protective effect was due to the benign clinical characteristic of patients with atrial fibrillation. Collectively, our findings suggest that caution is required in prescribing and monitoring warfarin treatment in patients with a low pre-treated serum albumin level, especially if patients have CHD, regardless of basal renal function. Recently, there have been increasing concerns that AKI can lead to chronic kidney disease and can accelerate the progression of pre-existing chronic kidney disease [16?8]. Consistent with these notions, our study also demonstrated that after the mean follow-up period of 14 months, the sCr level was still higher and the eGFR remained lower in patients with WRN compared to those without WRN, despite no significant difference in the basal sCr level. The renal function after follow-up was also worse in dead patients than live patients only in WRN group. Similar to the previous study [3], this study also found that WRN was associated with a substantial increase in the mortality rate, especially in the early period after WRN. However, contrary to the previous study, which showed no significant difference in mortality from the 6 months 1662274 after WRN, increased mortality persisted even 5 years after WRN. The results of the present study correspond well with previous studies that reported that AKI was associated with an increased risk for long-term mortality after 58-49-1 site several years of follow-up [19,20]. There were several limitations to the current study. First, our study was a retrospective study using only medical records; thus some essential information was often unavailable. Second, the criteria for determination of baseline laboratory findings were suboptimal. Any time within 6 months before INR .3.0 could become “baseline”, so the intervals from “baseline” laboratory findings to the event of INR .3.0 were inconsistent between enrolled patients. Third, the progression of underlying CKD during the “baseline” 6 months rather than WRN could be the cause of elevated sCr in some patients, although we excluded this possibility of progression of CKD by calculating the slope of the 1/ sCr level using the sCr level measured at 12 months, 6 months, and 3 months before INR .3.0 in patients who had available data. Fourth, although we defined AKI based on AKIN criteria published in 2007 [9], the required time frame “elevation of sCr .0.3 mg/dL within 48 hours” could not be satisfied in all patients. Fifth, we could not analyze the association between WRN and hematuria, proteinuria, and albuminuria due to lots of missing data related to urinalysis. Sixth, our study could not provide any data to an important question about unique susceptibility of glomerular capillary to warfarin observed in this study i.e. how glomerular hemorrhage could occur alone, without other significant systemic bleedings? Finally, the most importantly the current study could not totally exclude the effect of acute illness rather than warfarin itself on the deterioration of renal function in WRN group, although we demonstrated no significant differencein the frequency of advers events and prescription of therape.Among patients with WRN. doi:10.1371/journal.pone.0057661.t{Warfarin-Related Nephropathy in Korean PatientsWRN. The more severe clinical picture of patients with atrial fibrillation, such as old age, more comorbidities, and worse renal function at baseline and after follow-up than patients without atrial fibrillation denied the possibility that protective effect was due to the benign clinical characteristic of patients with atrial fibrillation. Collectively, our findings suggest that caution is required in prescribing and monitoring warfarin treatment in patients with a low pre-treated serum albumin level, especially if patients have CHD, regardless of basal renal function. Recently, there have been increasing concerns that AKI can lead to chronic kidney disease and can accelerate the progression of pre-existing chronic kidney disease [16?8]. Consistent with these notions, our study also demonstrated that after the mean follow-up period of 14 months, the sCr level was still higher and the eGFR remained lower in patients with WRN compared to those without WRN, despite no significant difference in the basal sCr level. The renal function after follow-up was also worse in dead patients than live patients only in WRN group. Similar to the previous study [3], this study also found that WRN was associated with a substantial increase in the mortality rate, especially in the early period after WRN. However, contrary to the previous study, which showed no significant difference in mortality from the 6 months 1662274 after WRN, increased mortality persisted even 5 years after WRN. The results of the present study correspond well with previous studies that reported that AKI was associated with an increased risk for long-term mortality after several years of follow-up [19,20]. There were several limitations to the current study. First, our study was a retrospective study using only medical records; thus some essential information was often unavailable. Second, the criteria for determination of baseline laboratory findings were suboptimal. Any time within 6 months before INR .3.0 could become “baseline”, so the intervals from “baseline” laboratory findings to the event of INR .3.0 were inconsistent between enrolled patients. Third, the progression of underlying CKD during the “baseline” 6 months rather than WRN could be the cause of elevated sCr in some patients, although we excluded this possibility of progression of CKD by calculating the slope of the 1/ sCr level using the sCr level measured at 12 months, 6 months, and 3 months before INR .3.0 in patients who had available data. Fourth, although we defined AKI based on AKIN criteria published in 2007 [9], the required time frame “elevation of sCr .0.3 mg/dL within 48 hours” could not be satisfied in all patients. Fifth, we could not analyze the association between WRN and hematuria, proteinuria, and albuminuria due to lots of missing data related to urinalysis. Sixth, our study could not provide any data to an important question about unique susceptibility of glomerular capillary to warfarin observed in this study i.e. how glomerular hemorrhage could occur alone, without other significant systemic bleedings? Finally, the most importantly the current study could not totally exclude the effect of acute illness rather than warfarin itself on the deterioration of renal function in WRN group, although we demonstrated no significant differencein the frequency of advers events and prescription of therape.