| Literature DB >> 26892933 |
Tung-Min Yu1,2, Che-Chen Lin3,4, Kuo-Hsiung Shu2, Ya-Wen Chuang2, Shih-Ting Huang2, Cheng-Hsu Chen2, Ming-Ju Wu2, Mu-Chi Chung2, Chao-Hsiang Chang3,5, Chi-Yuan Li3,6, Chi-Jung Chung7,8.
Abstract
Data regarding the risk of various liver diseases among different hepatitis viruses in kidney transplantation have not yet been identified.We selected individuals with kidney transplantation (ICD-9-CM V420 or 996.81) from 2000-2009 from the catastrophic illness registry of National Health Insurance Research Database (NHIRD)as the study cohort. The two end-points in the study included overall death, and post-transplant occurrence of hepatic disease. After adjustment for other risk factors, the risk of mortality was increased in patients with HBV infection (N = 352) and with HCV infection (N = 275) compared to those with neither HBV nor HCV infection (N = 3485). In addition,renal transplant recipients with HBV alone,HCV alone, and both with HBV and HCVinfectionrespectively had an approximately 10-fold hazard ratio (HR) = 9.84, 95% confidence interval (CI): 4.61-21.0, 4-fold increased risk (HR = 4.40, 95% CI: 1.85-10.5)and 5-fold increased risk (HR = 4.63, 95% CI: 1.06-20.2)of hepatocellular carcinoma (HCC)compared to those with neither HBV nor HCV infection. Our findings showed a significant risk of de novo liver disease in recipients with hepatitis virus infection. Based on our findings, we reinforce the importance and impact of hepatitis virus in renal transplantation.Entities:
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Year: 2016 PMID: 26892933 PMCID: PMC4759529 DOI: 10.1038/srep21312
Source DB: PubMed Journal: Sci Rep ISSN: 2045-2322 Impact factor: 4.379
Demographic and clinical information in kidney transplantation cohort classified by status of hepatitis virus infection.
| Group 1 (B–/C–) | Group 2 (B + /C–) | Group3 (B–/C + ) | Group4 (B + /C + ) | |||
|---|---|---|---|---|---|---|
| Number | 3485 | 336 | 262 | 50 | ||
| Gender | 0.0036 | |||||
| Female | 1718 (49.3) | 137 (40.8) | 121 (46.2) | 17 (34.0) | ||
| Male | 1767 (50.7) | 199 (59.2) | 141 (53.8) | 33 (66.0) | ||
| Age at kidney transplantation | 0.0031 | |||||
| 18 to 40 years | 1076 (30.9) | 112 (33.3) | 67 (25.6) | 6 (12.0) | ||
| 40 to 65 years | 2264 (65) | 217 (64.6) | 190 (72.5) | 41 (82.0) | ||
| 65 + years | 145 (4.2) | 7 (2.1) | 5 (1.9) | 3 (6.0) | ||
| Date of kidney transplantation | 0.0031 | |||||
| 2000 to 2005 | 2181 (62.6) | 179 (53.3) | 174 (66.4) | 29 (58.0) | ||
| 2006 to 2009 | 1304 (37.4) | 157 (46.7) | 88 (33.6) | 21 (42.0) | ||
| Comorbidity at recruitment | ||||||
| Diabetes | 631 (18.1) | 43 (12.8) | 67 (25.6) | 11 (22.0) | 0.0008 | |
| Hypertension | 2419 (69.4) | 243 (72.3) | 180 (68.7) | 32 (64.0) | 0.5589 | |
| Chronic glomerulonephritis | 1148 (32.9) | 133 (39.6) | 79 (30.2) | 14 (28.0) | 0.0465 | |
| Heart failure | 249 (7.1) | 12 (3.6) | 21 (8.0) | 4 (8.0) | 0.0820 | |
| Coronary artery disease | 312 (9) | 25 (7.4) | 26 (9.9) | 4 (8.0) | 0.7330 | |
| Immunosuppresants | ||||||
| 3449 (99.0) | 334 (99.4) | 261 (99.6) | 49 (98.0) | 0.5447 | ||
| Cyclosporin | 1645 (47.2) | 155 (46.1) | 176 (67.2) | 32 (64.0) | <0.0001 | |
| Tacrolimus | 2649 (76) | 278 (82.7) | 195 (74.4) | 37 (74.0) | 0.0366 | |
| Sirolimus | 1509 (43.3) | 137 (40.8) | 130 (49.6) | 21 (42.0) | 0.1640 | |
| mycophenolatemofetil | 3215 (92.3) | 314 (93.5) | 250 (95.4) | 44 (88.0) | 0.1431 | |
| Lamivudine | 64 (1.8) | 151 (44.9) | 4 (1.5) | 13 (26.0) | <0.0001 | |
| Median follow-up of mortality, years (SD) | 5.6 (2.8) | 4.9 (2.8) | 5.6 (2.9) | 5.4 (2.8) | 0.0001 | |
Hazard ratios of mortality and subsequent hepatic diseasesstratified by virus status inkidney transplantation population.
| Group 1 (B–/C–) | Group 2 (B + /C–) | Group 3 (B–/C + ) | Group 4 (B + /C + ) | |||||||||
|---|---|---|---|---|---|---|---|---|---|---|---|---|
| Event | PY | Rate | Event | PY | Rate | Event | PY | Rate | Event | PY | Rate | |
| 335 | 19480 | 17.2 | 52 | 1631 | 31.9 | 51 | 1456 | 35.0 | 6 | 269 | 22.3 | |
| Crude HR | ref | 1.88 (1.40–2.52) | 2.04 (1.52–2.73) | 1.31 (0.58–2.93) | ||||||||
| Adjusted HR | ref | 2.99 (2.13–4.18) | 2.05 (1.52–2.76) | 1.36 (0.61–3.07) | ||||||||
| 225 | 18578 | 12.1 | 24 | 1564 | 15.3 | 45 | 1323 | 34.0 | 6 | 244 | 24.6 | |
| Crude HR | ref | 1.31 (0.86–2.00) | 2.87 (2.08–3.95) | 2.11 (0.94–4.74) | ||||||||
| Adjusted HR | ref | 1.47 (0.90–2.38) | 2.49 (1.79–3.44) | 2.32 (1.02–5.28) | ||||||||
| 68 | 19330 | 3.52 | 46 | 1552 | 29.6 | 35 | 1393 | 25.1 | 4 | 256 | 15.7 | |
| Crude HR | ref | 8.35 (5.74–12.2) | 7.16 (4.76–10.8) | 4.41 (1.61–12.1) | ||||||||
| Adjusted HR | ref | 7.08 (4.43–11.3) | 7.14 (4.70–10.9) | 2.96 (1.06–8.24) | ||||||||
| 23 | 19330 | 1.19 | 17 | 1552 | 11.0 | 7 | 1393 | 5.03 | 2 | 256 | 7.83 | |
| Crude HR | ref | 9.22 (4.92–17.3) | 4.25 (1.82–9.91) | 6.53 (1.54–27.7) | ||||||||
| Adjusted HR | ref | 9.84 (4.61–21.0) | 4.40 (1.85–10.5) | 4.63 (1.06–20.2) | ||||||||
| 21 | 19330 | 1.09 | 15 | 1552 | 9.67 | 24 | 1393 | 17.2 | 0 | 256 | 0 | |
| Crude HR | ref | 8.92 (4.59–17.3) | 15.9 (8.87–28.6) | — | ||||||||
| Adjusted HR | ref | 5.86 (2.42–14.2) | 18.0 (9.78–33.2) | — | ||||||||
| 24 | 19330 | 1.24 | 14 | 1552 | 9.02 | 4 | 1393 | 2.87 | 2 | 256 | 7.83 | |
| Crude HR | ref | 7.01 (3.62–13.6) | 2.30 (0.80–6.62) | 6.18 (1.46–26.1) | ||||||||
| Adjusted HR | ref | 5.63 (2.47–12.8) | 2.06 (0.71–6.00) | 4.6 (1.05–20.1) | ||||||||
Rate was calculated per 1000 person-years. Overall hepatic diseases including hepatocellular carcinoma (ICD-9 code 155.0), hepatic failure (ICD 570), andliver cirrhosis (ICD 571.5). Adjusted HRs were adjusted for age, sex, diabetes mellitus, hypertension, heart failure, coronary artery disease, chronic glomerulonephritis, Sirolimus, mycophenolate, Cyclosporin, Tacrolimus and Lamivudine.
Predictors of mortality and subsequent hepatic disease in kidney transplantation population.
| Death | Overall liver diseases | |||
|---|---|---|---|---|
| Crude HR | Adjusted HR | Crude HR | Adjusted HR | |
| Hepatitis virus status | ||||
| Group 1 (B–/C–) | ref | ref | ref | ref |
| Group 2 (B + /C–) | 1.88 (1.40–2.52) | 2.90 (2.07–4.05) | 8.35 (5.74–12.2) | 6.76 (4.24–10.8) |
| Group 3 (B–/C + ) | 2.04 (1.52–2.73) | 1.98 (1.47–2.67) | 7.16 (4.76–10.8) | 6.57 (4.31–10.0) |
| Group 4 (B + /C + ) | 1.31 (0.58–2.93) | 1.32 (0.58–2.97) | 4.41 (1.61–12.1) | 2.82 (1.01–7.88) |
| Gender | ||||
| Female | ref | ref | ref | ref |
| Male | 1.30 (1.08–1.57) | 1.23 (1.01–1.48) | 1.90 (1.36–2.66) | 1.83 (1.30–2.58) |
| Age at kidney transplantation | ||||
| 18 to 40 years | ref | ref | ref | ref |
| 40 to 65 years | 2.64 (2.04–3.42) | 2.48 (1.91–3.24) | 2.60 (1.69–3.99) | 2.69 (1.73–4.18) |
| 65 + years | 6.14 (4.15–9.10) | 5.63 (3.74–8.48) | 2.43 (1.00–5.93) | 2.73 (1.08–6.87) |
| Comorbidity | ||||
| Diabetes | ||||
| No | ref | ref | ref | ref |
| Yes | 1.82 (1.47–2.26) | 1.34 (1.07–1.69) | 0.99 (0.64–1.52) | 0.84 (0.53–1.34) |
| Hypertension | ||||
| No | ref | ref | ref | ref |
| Yes | 1.14 (0.93–1.40) | 1.01 (0.82–1.24) | 0.69 (0.50–0.95) | 0.60 (0.43–0.84) |
| Chronic glomerulonephritis | ||||
| No | ref | ref | ref | ref |
| Yes | 0.87 (0.71–1.07) | 0.84 (0.68–1.04) | 0.76 (0.53–1.09) | 0.86 (0.59–1.27) |
| Congestive Heart failure | ||||
| No | ref | ref | ref | ref |
| Yes | 1.81 (1.33–2.46) | 1.76 (1.28–2.41) | 1.55 (0.90–2.69) | 1.72 (0.97–3.04) |
| Coronary artery disease | ||||
| No | ref | ref | ref | ref |
| Yes | 1.99 (1.52–2.61) | 1.39 (1.04–1.85) | 1.6 (0.98–2.62) | 1.42 (0.84–2.41) |
| Cyclosporin use | ||||
| No | ref | ref | ref | ref |
| Yes | 1.18 (0.97–1.42) | 1.02 (0.81–1.27) | 1.18 (0.85–1.63) | 1.27 (0.88–1.83) |
| Tacrolimus use | ||||
| No | ref | ref | ref | ref |
| Yes | 0.8 (0.65–0.98) | 0.81 (0.64–1.03) | 1.41 (0.94–2.11) | 1.46 (0.93–2.31) |
| Sirolimus | ||||
| No | ref | ref | ref | ref |
| Yes | 1.09 (0.91–1.32) | 1.20 (0.99–1.45) | 0.89 (0.65–1.23) | 0.82 (0.59–1.13) |
| mycophenolate | ||||
| No | ref | ref | ref | ref |
| Yes | 0.72 (0.53–0.98) | 0.73 (0.53–1.01) | 0.55 (0.34–0.89) | 0.47 (0.29–0.78) |
| Lamivudine | ||||
| No | ref | ref | ref | ref |
| Yes | 0.84 (0.54–1.30) | 0.48 (0.29–0.79) | 4.28 (2.87–6.38) | 1.59 (0.95–2.65) |
Adjusted HRs were adjusted for age, sex, diabetes mellitus, hypertension, heart failure, coronary artery disease, chronic glomerulonephritis, Sirolimus, mycophenolate, Cyclosporin,Tacrolimus and Lamivudine.
Figure 1Comparison of patient survival stratified by virus status.
Figure 2Comparison of kidney graft survival stratified by virus status.
Figure 3Cumulative incidence rates of subsequent hepatic diseases stratified by virus status: (A) overall hepatic diseases, (B) hepatocellular carcinoma, (C) liver cirrhosis, and (D) hepatic failure.