Abstract
A retrospective review was performed to assess the risk factors and outcomes of BK virus infection and nephropathy (BKVN), an early complication in pediatric kidney allograft recipients. The study investigated the incidence, risk factors, and clinical outcomes of BK viremia and BKVN in a Korean population of pediatric patients who received renal transplantation from 2001–2015 at the Seoul National University Hospital. BKVN was defined as biopsy-proven BKVN or plasma BK viral loads >10,000 copies/mL for >3 weeks. BK viremia was defined as a BK viral load >100 copies/mL in blood. Among 168 patients assessed for BK virus status, 30 patients (17.9%) tested positive for BK viremia at a median of 12.6 months after transplantation. BKVN was diagnosed in six patients (3.6%) at a median of 13.4 months after transplantation. Three of the six BKVN patients had Alport syndrome (p = 0.003), despite this disease comprising only 6% of the study population. Every patient with BK viremia and Alport syndrome developed BKVN, while only 11.1% of patients with BK viremia progressed to BKVN in the absence of Alport syndrome. Multivariate analysis revealed that Alport syndrome was associated with BKVN development (hazard ratio 13.2, p = 0.002). BKVN treatment included the reduction of immunosuppression, leflunomide, and intravenous immunoglobulin. No allografts were lost in the two years following the diagnosis of BKVN. In summary, the incidence of BKVN in pediatric kidney allograft recipients was similar to findings in previous reports, but was higher in patients with underlying Alport syndrome.
Highlights
BK virus (BKV) is a polyomavirus that resides in the urogenital tract as a latent infection [1]
BK virus nephropathy (BKVN) is considered to be an early complication of kidney transplantation that often occurs in the first year of transplantation; 95% of BKVN develops within two years of transplantation according to the organization Kidney Disease: Improving Global Outcomes (KDIGO), but it may develop as late as in the fifth year [9,10,11]
We retrospectively reviewed the medical records of all pediatric kidney allograft recipients who underwent transplantation at the Seoul National University Hospital between January 2001 and July 2015
Summary
BK virus (BKV) is a polyomavirus that resides in the urogenital tract as a latent infection [1]. Reactivation of a latent infection is frequently observed [1,3] as BK virus nephropathy (BKVN) or hemorrhagic cystitis [1,4]. While hemorrhagic cystitis frequently develops in patients with hematologic stem cell transplantation, BKVN is essentially a complication of kidney transplantation [2,5]. The prevalence of BKVN in adult kidney allograft recipients is 1% to 10% [2,5,6] and has been reported to be 2% to 8% in pediatric renal transplant recipients [7,8]. Risk factors for BKVN in children have not yet been studied sufficiently. To gain a better understanding of BKVN in pediatric kidney transplantation recipients, the clinical characteristics and risk factors for BK virus infection and BKVN in pediatric kidney allograft recipients was assessed in this study
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