S-M Ji1, Q-W Wang, J-S Chen, G-Z Sha, Z-H Liu, L-S Li. 1. Research Institute of Nephrology, Jinling Hospital, and Nanjing University School of Medicine, People's Republic of China. jishuming@vip.163.com
Abstract
OBJECTIVE: In this study, the effects of Triptergium Wilfordii Hook F.(T II) were assessed on human kidney allograft rejection and long-term survival. METHODS: This study compared treatment with T II(T II group, n=121) to that without T II(control group, n=102) among adult first cadaveric renal transplant recipients. The T II cohort of 121 recipients were divided into a regular dosage group (n=82) and a double dosage group (n=39). No antibody induction was administered to any patient. RESULTS: Biopsy-proven early acute allograft rejection occurred in 4.1% of patients in the T II group versus 24.5% of patients in the control group. No rejection or repeated rejections occurred in the double dosage group at 3 months after transplantation. Acute rejection episodes were milder in the T II than the control group. The incidence of CD25+ cells>10/ mm3 in the allografts at 3 months after transplantation was lower in the T II group than the control group, 15% and 50%, respectively. All patients tolerated T II well over the 5 years of this study. The 5-year graft survival censored for death with function was 96.7% in the T II group and 80.4% in the control group. CONCLUSION: T II was effective to prevent renal allograft rejection and increase long-term renal allograft survival among adult cadaveric renal transplant recipients.
OBJECTIVE: In this study, the effects of Triptergium Wilfordii Hook F.(T II) were assessed on human kidney allograft rejection and long-term survival. METHODS: This study compared treatment with T II(T II group, n=121) to that without T II(control group, n=102) among adult first cadaveric renal transplant recipients. The T II cohort of 121 recipients were divided into a regular dosage group (n=82) and a double dosage group (n=39). No antibody induction was administered to any patient. RESULTS: Biopsy-proven early acute allograft rejection occurred in 4.1% of patients in the T II group versus 24.5% of patients in the control group. No rejection or repeated rejections occurred in the double dosage group at 3 months after transplantation. Acute rejection episodes were milder in the T II than the control group. The incidence of CD25+ cells>10/ mm3 in the allografts at 3 months after transplantation was lower in the T II group than the control group, 15% and 50%, respectively. All patients tolerated T II well over the 5 years of this study. The 5-year graft survival censored for death with function was 96.7% in the T II group and 80.4% in the control group. CONCLUSION: T II was effective to prevent renal allograft rejection and increase long-term renal allograft survival among adult cadaveric renal transplant recipients.
Authors: Raphaela Goldbach-Mansky; Mildred Wilson; Roy Fleischmann; Nancy Olsen; Joel Silverfield; Phillip Kempf; Alan Kivitz; Yvonne Sherrer; Frank Pucino; Gyorgy Csako; Rene Costello; Tuyet Hang Pham; Christopher Snyder; Désirée van der Heijde; Xuelian Tao; Robert Wesley; Peter E Lipsky Journal: Ann Intern Med Date: 2009-08-18 Impact factor: 25.391
Authors: Xu Lengnan; Zhao Ban; Wang Haitao; Liu Lili; Chen Aiqun; Wang Huan; Zeng Ping; Mao Yonghui Journal: Biomed Res Int Date: 2020-06-10 Impact factor: 3.411