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TENOFOVIR ALAFENAMIDE FUMARATE IS EFFECTIVE AND
HAS SUPERIOR RENAL SAFETY MAINLY AMONG STAGE 2
CHRONIC KIDNEY DISEASE (CKD): REAL-WORLD STUDY FROM
THE CANADIAN HEPATITIS B NETWORK (CANHEPB)
Mina S. Farag1,2, Scott K Fung1, Edward Tam3, Karen E.
Doucette4, Alexander Wong5, Alnoor Ramji6, Brian Conway7,
Curtis Cooper8, Keith Tsoi9, Carla S. Coffin10, Bettina E.
Hansen1,11 and Harry L. A. Janssen1, (1)Toronto Centre for
Liver Disease, Toronto General Hospital, University Health
Network, (2)Institute of Medical Science, University of
Toronto, (3)Lair Centre, (4)Division of Infectious Diseases,
University of Alberta, (5)Department of Medicine, University
of Saskatchewan, (6)Medicine, University of British Columbia,
(7)Vancouver Infectious Diseases Centre, (8)University of
Ottawa, (9)Department of Medicine, Mcmaster University,
(10)Medicine, University of Calgary, (11)Institute of Health
Policy, Management and Evaluation, University of Toronto
Background: Tenofovir alafenamide fumarate (TAF), a new
prodrug of tenofovir has high plasma stability and results in
fewer renal adverse events compared to tenofovir disoproxil
fumarate (TDF) for chronic hepatitis B (CHB) treatment. We
aimed to study the effectiveness and renal safety of TAF
therapy in a real-world setting among CHB patients in Canada
Methods: CHB patients from 9 academic institutions across
Canadawho received TAF(either Nucleot(s)ide Analogue
(NA) naïve or experienced) were studied as part of the
Canadian Hepatitis (CanHepB) B Network. Kidney function
was measured by serum creatinine, estimated glomerular
filtration rate (eGFR) as per Cockcroft-Gault.Patients were
categorized according to theirchronic kidney disease (CKD)
stages using eGFR before switching to TAF and were followed
for 104 weeks after initiation of TAF Serum phosphate and
other biochemical and virologic markers were also serially
assessed Results: Of 103 patients receiving TAF, 81 (79%)
switched from TDF, 3 (3%) switched from another NA and 14
(14%) were NA naïve. At start of TAF treatment (baseline), the
mean (SD) age was 52 (13) years, 71 (69%) patients were
male and 81% of patients were Asian. Majority had HBV DNA
< 20 IU/mL (70%), 28 (33%) were HBeAg positive and mean
eGFR was 72.6 (0.28). CKD stages at baseline were Stage
1: 25(24%), Stage 2: 37(38%), Stage 3a: 20 (20%), Stage 3b
or higher: 17 (16%). Among the NA switch group, HBV-DNA
and HBsAg significantly declined after starting TAF (HBVDNA
log10 IU/ml during TAF:-0.07 [-0.09 - -0.06] per month;
P<0.001 vs. pre-TAF: (+0.01 [ -0.04 – 0.05]; P=0.8) (HBsAg
log10IU/ml during TAF -0.01 [-0.01 - -0.002]; P=0.009 vs. pre-
TAF: +0.11 [0.02 – 0.2]; P=0.02). eGFR increased significantly
after switching to TAF (during TAF: +0.11 [0.01- 0.22] per
month; P=0.04 vs. pre-TAF: -0.19 [95 CI% -0.35 – 0.02] per
month; P=0.02; Figure). This trend continued after the first
year of follow-up (eGFR week 0: 74.2, Week 52: 75.7, Week
104: 77.1; P<0.001). Serum phosphate decreased before
switching (-0.008 [-0.02 – -0.0004]mmol/Lper week; P=0.03)
and increased following TAF (+0.004 [0.01 – 0.12] mmol/Lper
week; P=0.03). Among patients with stage 2 CKD (eGFR 89-
60), eGFR significantly increased after switching compared
to pre-TAF (+0.20 [0.01- 0.41] per month; P=0.05 vs.-0.51
[-0.89 - -0.14] per month, P=0.01, respectively). Patients
with abnormal ALT before TAF showed a significant decline
after switching (-1.02 [-1.03 – -1.01] ULN per month; P<0.01).
Conclusion: In CHB patients on NA treatment, switching
to TAF led to improvement in kidney function, particularly in
those with stage 2 CKD. TAF was safe, well tolerated and
effective in this real-world cohort.
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发表于 2019-10-29 19:36