Chinese Journal of Tissue Engineering Research ›› 2010, Vol. 14 ›› Issue (5): 789-793.doi: 10.3969/j.issn.1673-8225.2010.05.008

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Correlation of urine monocyte chemoattractant protein-1 and acute rejection after renal transplantation

Xing Li1, Zhang Zhu2, Cai Wen-li1, Qu Qing-shan1, Miao Shu-zhai1, Wang Kai1   

  1. 1 Department of Organ Transplantation of Nephropathy, Zhengzhou People’s Hospital, Zhengzhou   450003, Henan Province, China; 2 Department of Nephropathy Transplantation, First Affiliated Hospital, Henan University of Chinese Medicine, Zhengzhou   450000, Henan Province, China
  • Online:2010-01-29 Published:2010-01-29
  • About author:Xing Li★, Master, Attending physician, Department of Organ Transplantation of Nephropathy, Zhengzhou People’s Hospital, Zhengzhou 450003, Henan Province, China xingli0809@yahoo.cn

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Abstract:

BACKGROUND: Presently, acute rejection following renal transplantation remains a risk factor for chronic rejection and graft function injury. How to non-invasive, rapid and exact diagnosis and prompt treatment is important.
OBJECTIVE: To investigate early diagnosis and post-treatment expression of urine monocyte chemoattractant protein-1 (MCP-1) in the acute rejection after renal transplantation, through detecting the association of the urine MCP-1 variation according to some cases of nephridial tissue biopsy.
METHODS: We selected 62 chronic renal failure patients who received renal homotransplantations in the Department of Renal Transplantation of Zhengzhou People’s Hospital from October 2008 to February 2009. The stable renal function group contained 42 patients with stable renal function following renal transplantation. Acute rejection group contained 20 patients with acute rejection following renal transplantation. We chose 10 patients who examined no abnormalities in the Medical Examination Center of Zhengzhou People’s Hospital to detect their urine sample as control group. All patients following renal transplantation underwent conventional immunosuppression. In addition, patients in the acute rejection group were treated with antilymphocyte globulin or methylprednisolone reinforced impact therapy. MCP-1 mass concentration changes were measured by double antibodies sandwich enzyme linked immurosorbent assay.
RESULTS AND CONCLUSION: Compared with control group, no significant change was determined in urine MCP-1 mass concentration in the stable renal function group (P > 0.05). The urine MCP-1 mass concentration was significantly increased in the acute rejection group (P < 0.01). Compared with pretreatment, urine MCP-1 mass concentration was significantly decreased following treatment in 20 patients from the acute rejection group (P < 0.01). Of them, 17 cases had relieved clinical symptom, and normal auxiliary examination, and their urine MCP-1 mass concentration was close to the control group; 3 cases were inefficient, whose urine MCP-1 mass concentration was greater than the control group. Eight cases received nephridial tissue biopsy, and kidney pathology demonstrated acute rejection of transplanted kidney, which was similar to urine MCP-1 mass concentration in the acute rejection group prior to treatment (P > 0.05). These indicated that the level of MCP-1 in urine can non-invasively diagnose acute rejection following renal transplantation in an early phase, and monitor therapeutic efficacy. This may be associated with renal pathological injury during acute rejection following renal transplantation.

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