| Literature DB >> 34596918 |
Özgür Muhammet Koc1,2,3,4, Marleen Pierco5, Kathleen Remans5, Thijs Van den Hende5, Jef Verbeek5, Hannah Van Malenstein5, Schalk Van der Merwe5, Geert Robaeys1,2,5, Diethard Monbaliu6, Jacques Pirenne6, Bart Van den Bosch7, Fabienne Dobbels8, Frederik Nevens5.
Abstract
Telemedicine gained interest in liver transplant patients but focused until now on the early post-operative period. This prospective cohort study assessed feasibility, safety, and clinical beneficial effects of a telemedicine based remote monitoring program (TRMP) for the chronic follow-up of adult liver transplant recipients. Between November 2017 and August 2019, a total of 87 of the 115 selected patients (76%) started the TRMP. Over the 2 years study period, none of the patients switched to standard follow-up: 39/87 (45%) continued to do this autonomously and 48/87 (55%) stopped to report their data personally but communicated their lab values to the nurse. The other 28/115 (11%) patients who did not accept the TRMP continued the standard follow-up. There was no difference in educational level between the three groups. Remote monitoring did not result in an increase in liver graft rejection and need of hospitalization. TRMP was associated with a higher number of tacrolimus level determinations and tacrolimus blood level concentrations could be kept lower. In conclusion, our results show that in patients with a stable clinical condition there is a high willingness to participate in TRMP and that this approach is safe. Remote monitoring allowed a stringent follow-up of tacrolimus levels.Entities:
Keywords: kidney injury; liver transplant; remote monitoring; tacrolimus levels; telemedicine
Mesh:
Substances:
Year: 2021 PMID: 34596918 PMCID: PMC9285405 DOI: 10.1111/ctr.14494
Source DB: PubMed Journal: Clin Transplant ISSN: 0902-0063 Impact factor: 3.456
FIGURE 1Mynexuzhealth, a telemedicine based remote monitoring program (TRMP)
FIGURE 2Flowchart of the study. TRMP: telemedicine based remote monitoring program
Baseline characteristics (n = 115)
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| Median age at inclusion, years | 59.1 ± 12.17 | 67.2 ± 17.20 | 66.0 ± 11.77 | .006 |
| Male sex, | 24 (61.5) | 29 (60.4) | 14 (50.0) | .592 |
| Caucasian race, | 39 (100.0) | 48 (100.0) | 28 (100.0) | … |
| Distance to hospital ( miles) | 77.5 ± 93.0 | 68.2 ± 47.8 | 44.2 ± 33.3 | .006 |
| Educational level, | ||||
| Low | 11 (28.2) | 11 (25.0) | 10 (38.5) | .335 |
| Moderate | 15 (38.5) | 20 (45.5) | 13 (50.0) | |
| High | 13 (33.3) | 13 (29.5) | 3 (11.5) | |
| Active alcohol abuse, | 0 (.0) | 1 (2.1) | 2 (7.1) | .254 |
| Active smoking, | 1 (2.6) | 1 (2.1) | 2 (7.1) | .557 |
| BMI ≥ 25 kg/m2 | 18 (50.0) | 33 (68.8) | 21 (75.0) | .081 |
| Median years from LT to inclusion | 6.4 ± 8.42 | 7.4 ± 12.92 | 7.0 ± 9.28 | .740 |
| Primary indication for LT, | .167 | |||
| Acute hepatic failure | 5 (12.8) | 2 (4.2) | 0 (.0) | |
| Cirrhosis | 17 (43.6) | 36 (75.0) | 20 (71.4) | |
| HCC | 2 (5.1) | 1 (2.1) | 1 (3.6) | |
| Cholestatic diseases | 6 (15.4) | 4 (8.3) | 2 (7.1) | |
| Metabolic diseases | 4 (10.3) | 1 (2.1) | 2 (7.1) | |
| Others | 5 (12.8) | 4 (8.3) | 3 (10.7) | |
| Etiologies leading to LT, | .339 | |||
| Alcohol | 8 (20.5) | 14 (29.2) | 9 (32.1) | |
| NASH | 4 (10.3) | 10 (20.8) | 4 (14.3) | |
| HCV | 4 (10.3) | 3 (6.3) | 5 (17.9) | |
| Others | 23 (59.0) | 21 (43.8) | 10 (35.7) | |
| Immunosuppressive therapy, | .368 | |||
| TAC | 16 (41.0) | 21 (43.8) | 10 (35.7) | |
| TAC+MMF | 10 (25.6) | 9 (18.8) | 12 (42.9) | |
| TAC+EVR | 7 (17.9) | 7 (14.6) | 2 (7.1) | |
| Others | 6 (15.4) | 11 (22.9) | 4 (14.3) | |
| Possible nephrotoxic drug use, | .205 | |||
| None | 16 (41.0) | 10 (20.8) | 10 (35.7) | |
| One drug | 14 (35.9) | 18 (37.5) | 11 (39.3) | |
| Two or more drugs | 9 (23.1) | 20 (41.7) | 7 (25.0) | |
| Median creatinine level (mg/dl) | 1.0 ± .35 | 1.1 ± .36 | 1.0 ± .38 | .729 |
| GFR categories (ml/min/1.73m2), | .465 | |||
| G1 ≥ 90 | 9 (23.1) | 8 (16.7) | 3 (10.7) | |
| G2 60 – 89 | 18 (46.2) | 19 (39.6) | 16 (57.1) | |
| G3a 45 – 59 | 9 (23.1) | 12 (25.0) | 4 (14.3) | |
| G3b 30 – 44 | 3 (7.7) | 9 (18.8) | 5 (17.9) | |
| Median glucose level (mg/dl) | 97.0 ± 17.25 | 101.0 ± 35.00 | 104.0 ± 31.25 | .115 |
| Median LDL cholesterol level (mg/dl) | 88.0 ± 39.50 | 91.0 ± 36.50 | 95.5 ± 29.25 | .506 |
| Arterial hypertension , | 16 (41.0) | 32 (66.7) | 12 (42.9) | .031 |
| Diabetes mellitus, | 9 (23.1) | 20 (41.7) | 10 (35.7) | .185 |
| Cardiovascular disease, | 6 (15.4) | 8 (16.7) | 3 (10.7) | .845 |
| Non‐liver malignancy, | 3 (7.7) | 5 (10.4) | 3 (10.7) | .851 |
Data are n (%) or median ± interquartile range, IQR.
Abbreviations: TRMP, telemedicine based remote monitoring program; BMI, body mass index; NASH, non‐alcoholic steatohepatitis; HCV, hepatitis C virus; TAC, tacrolimus; EVR, everolimus; MMF, mycophenolate mofetil; GFR, glomerular filtration rate.
Outcomes at end of study follow‐up (n = 115)
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| Median follow‐up, years | 2.0 ± .93 | 2.1 ± .89 | 2.4 ± .44 | .034 |
| Median outpatient visits | 2.0 ± 1.00 | 2.0 ± 3.00 | 5.0 ± 2.00 | <.001 |
| Median emergency visits | .0 ± .00 | .0 ± .00 | .0 ± .00 | .595 |
| Median hospitalizations | .0 ± .00 | .0 ± .00 | .0 ± .00 | .451 |
| Median number of TAC level determinations | 8.0 ± 6.00 | 7.0 ± 7.00 | 6.0 ± 3.00 | .013 |
| Median TAC levels outside target level | 1.0 ± 2.25 | 1.0 ± 2.50 | 1.0 ± 2.00 | .819 |
| Median TAC concentration | 4.7 ± 1.72 | 4.6 ± 1.74 | 4.4 ± 2.76 | .707 |
| Liver graft rejection | 1 (2.6) | 0 (.0) | 1 (3.6) | .337 |
| Re‐transplantation | 0 (.0) | 0 (.0) | 0 (.0) | … |
| Acute kidney injury | 0 (.0) | 3 (6.3) | 4 (14.3) | .048 |
| Chronic kidney disease progression | 1 (2.6) | 3 (6.3) | 2 (7.1) | .658 |
| Median last creatinine level (mg/dl) | 1.0 ± .29 | 1.1 ± .32 | 1.0 ± .29 | .524 |
| Disease recurrence | 0 (.0) | 1 (2.1) | 1 (3.6) | .714 |
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| 1 (2.6) | 0 (.0) | 1 (3.6) | .337 |
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| 2 (5.1) | 0 (.0) | 2 (7.1) | .162 |
| Community acquired infections | 2 (5.1) | 4 (8.3) | 6 (21.4) | .106 |
| Mortality | 0 (.0) | 1 (2.1) | 0 (.0) | 1.000 |
Data are n (%) or median ± interquartile range, IQR.
Abbreviation: TAC: tacrolimus.
Outcomes within 12 months prior versus after the use of TRMP (n = 69)
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| Median outpatient visits | 2.0 ± 1.00 | 1.0 ± .00 | < .001 | 2.0 ± 1.00 | 1.0 ± 1.00 | < .001 |
| Median emergency visits | .0 ± .00 | .0 ± .00 | 1.000 | .0 ± .00 | .0 ± .00 | .414 |
| Median hospitalizations | .0 ± .00 | .0 ± .00 | 1.000 | .0 ± .00 | .0 ± .00 | .518 |
| Median number of TAC level determinations | 3.0 ± 3.00 | 4.5 ± 3.75 | < .001 | 2.0 ± 1.00 | 4.0 ± 2.75 | .003 |
| Median TAC levels outside target level | 1.0 ± 1.00 | 1.0 ± 2.00 | .524 | 1.0 ± 1.00 | 1.0 ± 1.00 | .171 |
| Median TAC concentration | 5.1 ± 2.16 | 4.7 ± 2.23 | .038 | 5.4 ±2.5 | 4.4 ± 2.01 | .002 |
| Liver graft rejection | 2 (6.5) | 1 (3.2) | 1.000 | 2 (5.7) | 0 (.0) | … |
| Acute kidney injury | 0 (.0) | 0 (.0) | … | 5 (13.9) | 0 (.0) | … |
| Chronic kidney disease progression | 0 (.0) | 0 (.0) | … | 1 (2.8) | 0 (.0) | … |
Data are n (%) or median ± interquartile range, IQR.
Abbreviation: TAC: tacrolimus.