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Share your thoughts on this presentation with #IAS2019

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Presentation on theme: "Share your thoughts on this presentation with #IAS2019"— Presentation transcript:

1 Share your thoughts on this presentation with #IAS2019
Renal function trajectories after switching from TDF to TAF A nationwide cohort study Bernard Surial, Bruno Ledergerber, Alexandra Calmy, Matthias Cavassini, Huldrych Günthard, Helen Kovari, Marcel Stöckle, Enos Bernasconi, Pietro Vernazza, Christoph Fux, Hansjakob Furrer, Andri Rauch, Gilles Wandeler, and the Swiss HIV Cohort Study (SHCS) @b_surial Share your thoughts on this presentation with #IAS2019

2 Disclosures Received travel grant from Gilead sciences, paid to my home institution

3 Rationale and aims of the study
Background Improved renal safety of tenofovir alafenamide (TAF) vs tenofovir disoproxil fumarate (TDF) were shown in registration trials Real world data in patients with impaired renal function and co-morbidities at initiation of TAF are lacking Aims To evaluate the impact of switching from TDF to TAF on eGFR and proteinuria To identify subgroups who benefit most from switching from TDF to TAF

4 Methods Swiss HIV Cohort Study (SHCS): ~80% of HIV-infected adults on ART in Switzerland Inclusion criteria for the present study: Patients were either on TDF until the end of the observation period* (TDF Group) OR switched from TDF to TAF and remained on it (TAF Group) Had ≥ 2 creatinine measurements before and after baseline date** (≥ 1 month apart) Statistics: linear mixed-effect regression and multivariable logistic regression, adjusted for potential confounders, including co-morbidities, co-infections, co-medications * March 2019 **Baseline date defined as date of switch (TAF group) or 01. Oct (TDF group)

5 Patient Flow

6 Patient Characteristics

7 Co-Morbidities

8 eGFR at baseline Normal ≥ 90mL/min Mild 60-89 mL/min
Moderate to Severe below 60 mL/min

9 Change in eGFR over time
Adjusted for age, sex, ethnicity, diabetes, arterial hypertension, cardiovascular disease, HCV and HBV infection, use of ritonavir, cobicistat, dolutegravir and cotrimoxazole

10 Change in eGFR over time
Adjusted for age, sex, ethnicity, diabetes, arterial hypertension, cardiovascular disease, HCV and HBV infection, use of ritonavir, cobicistat, dolutegravir and cotrimoxazole

11 Change in eGFR over time
Adjusted for age, sex, ethnicity, diabetes, arterial hypertension, cardiovascular disease, HCV and HBV infection, use of ritonavir, cobicistat, dolutegravir and cotrimoxazole

12 Change in eGFR over time
Adjusted for age, sex, ethnicity, diabetes, arterial hypertension, cardiovascular disease, HCV and HBV infection, use of ritonavir, cobicistat, dolutegravir and cotrimoxazole

13 Factors associated with eGFR increase ≥ 10% at 12 months

14 Factors associated with eGFR increase ≥ 10% at 12 months

15 Change in protein-to-creatinine ratio over time

16 Change in protein-to-creatinine ratio over time

17 Conclusion 18 months after switch from TDF to TAF, eGFR improved in patients with established renal dysfunction, and remained similar among those with a normal renal function eGFR improvement may be less likely in the presence of a boosted PI Protein-to-creatinine ratio decreased after switching from TDF to TAF Longer term follow-up data are needed to confirm these results

18 All participants of the Swiss HIV Cohort Study as well as its members
Acknowledgements Gilles Wandeler Andri Rauch Bruno Ledergerber Alexandra Calmy Matthias Cavassini Huldrych Günthard Helen Kovari Marcel Stöckle Enos Bernasconi Pietro Vernazza Christoph Fux Hansjakob Furrer All participants of the Swiss HIV Cohort Study as well as its members

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