Urine samples from 156 patients who received renal transplants between June 2006 and December 2009 were examined in our center. A total of 49 patients had biopsy-confirmed phenotypes of acute rejection (AR) with an elevated serum creatinine level of ≥25% above baseline within 6 months of transplant, while 58 patients had stable grafts and no abnormal histological findings (NO-AR) in protocol biopsies performed 2–3 months following transplantation. Fresh first-morning mid-flow urine samples from patients were collected every 2 weeks during the first 2 months following transplantation. Urine samples were similarly collected from the 10 patients with biopsy-proven acute tubular necrosis (ATN), 29 patients with chronic allograft nephropathy (CAN) and 10 patients with subclinical rejection (SCR). Urine samples were not collected on the day of biopsy. All subjects received primary grafts from deceased donors. Detailed demographic characteristics of these groups are summarized in Table I, with no significant differences identified between groups (P>0.05; Table I). Patients with signs of infection or malignant tumor were excluded from the study. Urine samples were also collected from 40 healthy individuals as controls (average age: 39.6±6.8 years; male/female: 24/16). Normal controls were recruited from the medical examination center of our center. The study was approved by the Ethics Committee of The First Affiliated Hospital of College of Medicine of Zhejiang University (Zhejiang, China) in accordance with the Declaration of Helsinki, and all of the study participants provided written informed consent.

Details of immune suppressive protocols used in Chinese renal allograft recipients have been previously reported by this group (19). All subjects who were recruited to participate in the present study were receiving a combination of three immunosuppressive drugs at the time of transplantation, composed of a calcineurin inhibitor (tacrolimus or cyclosporine, tacrolimus: trough level 5–10 ng/ml, or cyclosporin: Trough level 200–300 ng/ml for six months following the transplant), prednisone (in tapering doses from 80–10 mg/day within the first month after transplant), and azathioprine or mycophenolatemofetil. A3 day course of intravenous methylprednisolone (6 mg/kg) was used as anti-rejection therapy following clinical and biopsy-proven diagnosis of acute rejection. Steroid-resistant acute rejection (SRAR) was defined as lack of response to steroid treatment (graft function had no improvement or worsened) and was treated with OKT3 (5 mg/day) for 5–7 days. In addition, plasma exchange therapy was performed in patients diagnosed with humoral rejection. A single experienced renal pathologist who was unaware of the results of the study used Banff 97 classification (20,21) to evaluate all biopsy specimens.

Fresh urine samples were immediately centrifuged for 10 min at 1,600 × g at 4°C, then the supernatant was aliquoted and stored at −80°C until required. Urinary creatinine and protein were measured for the purpose of calibration; sTim-3 levels determined by ELISA were expressed per millimole of urinary creatinine to correct for differences in urine concentration.

sTim-3 was measured in urine samples using a commercial human sTim-3 ELISA kit (catalog no. T133-90; Groundwork Biotechnology Diagnosticate, Ltd., San Diego, CA, USA). Undiluted urine samples were tested in duplicate according to the manufacturer's protocol.

Statistical analysis was performed using SPSS version 16.0 (SPSS, Inc., Chicago, IL, USA). Parameters between groups were compared using the Mann-Whitney or Kruskal-Wallis test and post hoc tests for nonparametric continuous data. To measure the sensitivity and specificity of urinary sTim-3 in distinguishing between AR and NO-AR patients, a conventional receiver operating characteristic (ROC) curve was generated. ROC curves were also used to determine the sensitivities and specificities for sTim-3 measurements to diagnose SCR and predict the outcome following acute rejection. The diagnostic and predictive value of this model was investigated by the area under the ROC curve. Youden's index, defined as sensitivity + specificity-1, was used for the computation of the diagnostic threshold. Results were expressed in the text as mean ± standard error of the mean unless otherwise stated. P<0.05 was considered to indicate a statistically significant difference.

In the 58NO-AR patients, the level of urinary sTim-3 did not change significantly during the first 8 weeks following transplantation, with a value of 1,732±182 ng/mmol creatinine at 2 weeks, 1,504±154.1 ng/mmol creatinine at 4 weeks, 1,515±87.2 ng/mmol creatinine at 6 weeks and 1,415±144.4 ng/mmol creatinine at 8 weeks (Fig. 1).

All patients diagnosed with AR (n=49) were treated with intravenous methylprednisolone. Among them, 18 patients with reversible creatinine increases were classified as SSAR, while 31 patients showing no improvement following steroids were classified as SRAR. Patients with SRAR were further treated with OKT3, plasma exchange or both. A total of 47 patients were successfully controlled. Anti-rejection treatment appeared to be unsuccessful in 2 patients. In these cases, graft function deteriorated rapidly, with grafts failing within 3 months of the transplant procedure.

A total of 31 of the 49 patients with AR also had urine samples taken before or after the occurrence of AR. The concentration of urinary sTim-3 in patients during the period of AR (4,221±529.6, 95%CI: 3,123–5,266 ng/mmol creatinine) was significantly higher than during stable renal function, both before the occurrence of AR (1,507±229.3, 95%CI: 1,239–2,065 ng/mmol creatinine; P<0.001) and after AR reversion (1,493±210, 95%CI: 1,267–1,960 ng/mmol creatinine; P<0.001).

Compared with those without rejection (patients with NO-AR, ATN or healthy controls), patients with AR had significantly higher levels of urinary sTim-3 (Fig. 2): 4,356±440.4, 95%CI: 3,473–5,242 ng/mmol creatinine in patients with AR; 1,430±106.2, 95%CI: 1,118–1,548 ng/mmol creatinine in patients with NO-AR (P<0.001 vs. AR); 2,060±217, 95% CI: 1,679–2,680 ng/mmol creatinine in patients with ATN (P=0.02 vs. AR); and 1,269±99.3, 95% CI: 1,068–1,469 ng/mmol creatinine in healthy controls (P<0.001 vs. AR).Urinary sTim-3levels in patients with AR were also higher than in patients with CAN (3,920±543.5, 95%CI: 3,473–5,242 ng/mmol creatinine), however, the difference was not statistically significant (P=0.058 vs. AR; Fig. 2). Urinary sTim-3 concentrations in patients with NO-AR and in the 40 healthy controls were extremely similar, both remaining at relatively low levels, as depicted in Fig. 2.

A ROC curve was performed to determine the discriminatory power of sTim-3 levels for diagnosis of acute rejection (Fig. 3). The area under ROC curve was 0.88 (95% CI: 0.809–0.951). The optimal cutoff level for sTim-3 was 1,836 ng/mmol creatinine, with a sensitivity and specificity of 89.8 and 82.8%, respectively (P<0.001). When the cutoff level was set at 2,764 ng/mmol creatinine, the corresponding specificity was 91.4%.

Among the 49 patients with AR, 37 were diagnosed as cellular rejection and 12 were humoral rejection according to antibody-mediated rejection criteria. Patients with cellular rejection excreted sTim-3 (4,010±490.7, 95% CI: 3,010–4,985 ng/mmol creatinine) less than those with humoral rejection (5,091±961.5 ng/mmol creatinine, 95% CI: 3,012–7,210 ng/mmol creatinine), but this effect was not statistically significant (P=0.15).

The 31 patients with SRAR had significantly greater urinary sTim-3 concentrations (5,660±616.5, 95% CI: 4,387–6,890 ng/mmol creatinine) than the 18 patients with SSAR (2,753±386.7, 95% CI: 1,930–3,576 ng/mmol creatinine) and 58 patients with NO-AR (P<0.001; Fig. 4). Patients with SSAR excreted significantly more urinarys TIM-3 than NO-AR patients (P=0.009; Fig. 4). The ROC curve demonstrated the sensitivity and specificity of various cutoff levels for urinarys Tim-3 to predict the incidence of SRAR (Fig. 5). The area under the ROC curve was 0.86 (95% CI: 0.744–0.976, P<0.001). The cutoff point that optimized the combined sensitivity and specificity for sTim-3 was 3,242.9 ng/mmol creatinine. At this threshold, the sensitivity was 83.9% and the specificity was 88.9% (P<0.001).

The 2 patients with graft loss appeared to have higher urinary sTim-3 concentrations than the 47 patients with reversible acute rejection (6,496±1,488, 95% CI: 2,981–10,065 ng/mmol creatinine vs. 4,252±445.1, 95% CI: 3,356–5,249 ng/mmol creatinine), but the difference between these two groups was not statistically significant (P=0.17). A negative association between urinary sTim-3 concentration and estimated glomerular filtration rate (eGFR) was also identified (Fig. 6). As demonstrated in Fig. 6, patients with a high average urinary sTim-3 concentration within 2 months of transplantation (>4,000 ng/mmol creatinine; n=99) had a significantly lower eGFR than the group with low average sTim-3 levels (<2,000 ng/mmol creatinine; n=57): 3 months after transplantation, eGFR in the group with lower average sTim-3 was 80.2±2.2 ml/min 1.73 m² vs. 59.4±5.9 ml/min 1.73 m² in the group with higher sTim-3 levels (P<0.001); 85.2±2.6 ml/min 1.73 m² in the group with lower average sTim-3 vs. 60.9±8.6 ml/min 1.73 m² in the group with higher sTim-3 levels 6 months after transplantation (P<0.001); and 86.6±3.6 ml/min 1.73 m²in the group with lower average sTim-3 vs. 60.9±8.6 ml/min 1.73 m² in the group with higher sTim-3 levels 12 months after transplantation (P<0.001).

A total of 10 patients were diagnosed with subclinical rejection (SCR) in protocol biopsy according to Banff 97 classification; urinary sTim-3 levels were determined to be suitable as an indicator in these patients too. Patients with SCR excreted urinary sTim-3 at a significantly higher level (3,783±760.9, 95% CI: 2,087–5,478 ng/mmol creatinine) than patients with NO-AR (1,430±106.2, 95% CI: 1,118–1,548 ng/mmol creatinine; P<0.001; Fig. 7). However, there was no significant difference in urinary sTim-3 concentrations between patients with SCR and AR (P=0.72; Fig. 7).

A ROC curve was used to present the sensitivity and specificity of urinary sTim-3 levels as an indicator of SCR (Fig. 8). The area under the ROC curve was 0.934 (95% CI: 0.87–0.99; P<0.001). The cutoff point that maximized the combined sensitivity and specificity for sTim-3 was 1,857 ng/mmol creatinine. At this threshold, the corresponding sensitivity and specificity was 90 and 82.8%, respectively (P<0.001).