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434
Low Dose Tenofovir Disoproxil Fumarate
Improves Kidney Function and Sustains
Virologic Suppression in Renally Compromised
Chronic Hepatitis B Patients
Kin Seng Liem1,2, Scott K. Fung3, David KH Wong1, Alirezah
Zahirieh4, Hemant A. Shah1, Colina K. Yim1, Jordan J. Feld1,5,
Bettina E. Hansen1,2,6 and Harry L. A. Janssen1, (1)Toronto
Centre for Liver Disease, University Health Network, (2)
Dept. of Gastroenterology & Hepatology, Erasmus University
Medical Center Rotterdam, (3)University of Toronto, Toronto,
on, Canada, (4)Sunnybrook Health Sciences Center, (5)
Mclaughlin-Rotman Centre for Global Health, (6)Institute of
Health Policy, Management, and Evaluation, University of
Toronto
Background: Tenofovir disoproxil fumarate (TDF) therapy
effectively inhibits viral replication in patients with chronic
hepatitis B (CHB), but renal impairment can occur. Viral
breakthrough and renal function were studied in renally
impaired patients on reduced dose TDF and in patients on
full dose TDF. Methods: CHB patients with full and reduced
dose TDF (due to GFR [Cockcroft-Gault] <50mL/min/1.73m2
± serum phosphate <0.8mmol/L) from a North-American
hospital were evaluated. Viral breakthrough (confirmed
HBV DNA>1 log IU/mL above nadir on-therapy [AASLD])
and biochemical breakthrough (confirmed ALT>1.5x ULN)
were assessed from 1 month after starting (reduced) TDF
dose (baseline) till end of follow-up (EOF). Renal function
was calculated by Chronic Kidney Disease (CKD)-EPI and
grouped as CKD stage 1-5. Outcome was compared between
full and reduced dose TDF, and between before and after
dose reduction among patients who started on full dose
TDF. Results: Of 739 patients on TDF, 67 (9%) had reduced
dose vs. 672 (91%) full dose. At baseline the mean (SD) age
was 68 (11) vs. 45 (13) years, 63% vs.70% was male, mean
duration on TDF was 3 (2) vs. 5 (3) years for reduced vs. full
dose of TDF. Low dose patients had a baseline HBV DNA of
1.4 log (71% undetectable), 75% received TDF 300mg Q48hr
(range 75mg - 300mg Q48hr), mean CKD-EPI was 50 (20)
mL, 22% had hypophosphatemia, 46% had CKD stage G3b
or worse and 14% had decompensated cirrhosis. During a
mean follow-up of 3 (2) years, all patients continued to have
viral suppression except for 1 dialysis patient on TDF 300mg/
week who had a viral breakthrough (HBV DNA peak 3.6 log)
that resolved 4 months after dose increase to Q72hr without
decompensation and 1 patient on full dose TDF (resolved
naturally). Another reduced dose patient had a transient
ALT increase (peak 2x ULN) without rise in HBV DNA. The
CKD-EPI decline observed during full dose TDF reversed in
the first year of lower dosing and remained stable thereafter
(+2.0 (13) mL at EOF vs. baseline; p=0.28), with 50 (75%)
patients reaching CKD-EPI>50mL and 11/15 (73%) patients
normalizing serum phosphate. None developed Fanconi
syndrome or lactic acidosis. TDF was further dose reduced or
switched to ETV/LAM in 11% of patients and dose increased
due to improved GFR in 14%. Conclusion: Low dose TDF
could preserve renal function and sustain viral suppression in
most renally impaired CHB patients, even with advanced liver
disease. This useful, yet simple strategy could be especially
feasible in resource limited settings. |
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发表于 2018-10-21 16:28