Clinical study of different immune induction and BK virus infection after renal transplantation

Lizhong Han, Hao Zhong, Zhizhong Liu, Yanhui Feng, Guixia Sun

Abstract


Objective: To monitor the incidence of BK virus infection in hematuria of renal transplant recipients induced by different immunizations.

Methods: A total of 109 patients who underwent renal transplantation in Baogang Hospital of Inner Mongolia from January 2019 to December 2022 were analyzed retrospectively. The results of BK virus DNA detection in urine and blood were observed after operation. They were divided into three groups according to different immunosuppressive induction regimens; 35 patients in group A, 42 patients in group B, and 32 patients in group C (basiliximab). To explore the effect of different immune induction regimens on BK virus infection in renal transplant recipients.

Results: The positive rate of urine BK virus in all patients in 1 month after operation was 10.09% (11/109), which was significantly higher than that of blood BK virus 0% (0/109), and the difference had a statistical significance (p < .05). The positive rate of urine BK virus in all patients in 6 months after operation was 31.19% (34/109), which was significantly higher than that of blood BK virus 3.67% (4/109), and the difference had a statistical significance (p < .05). The positive rate of urine BK virus in all patients in 12 months after operation was 35.79% (39/109), which was significantly higher than that of blood BK virus 5.50% (6/109), and the difference had a statistical significance (p < .05). The urinary BK virus infection rate was increased significantly from 1 month to 6 months after operation, but was not increased significantly from 6 months to 12 months after operation. There was a statistically significant difference between the two groups (p < .05). The BK virus infection rate in renal transplant recipients induced by basiliximab within the first month was significantly lower than that in patients using polyclonal antibodies, but the urinary BK virus infection rate after one year was not significantly different from that in patients using polyclonal antibodies.

Conclusions: There are slight differences in BK virus infection after early renal transplantation with different immune induction therapies, but there is no significant difference in the long-term. It is recommended to strengthen the early monitoring of BK virus after renal transplantation, timely adjust  immunosuppressive regimens to achieve the early detection and early treatment.


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DOI: https://doi.org/10.5430/dcc.v9n4p12

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