Intracellular 007-TP Concentrations are Associated with...
Transcript of Intracellular 007-TP Concentrations are Associated with...
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Intracellular 007-TP Concentrations are Associated with Gradients of
Adherence to Ledipasvir/SofosbuvirLeah C. J immerson 1, Mary M. Morrow 2, Samantha Mawhinney 2, Jose Cast i l lo-Manci l la 3, Ryan T. Huntley 1, Josh Blum 4, David Wyles 4, Sarah E. Rowan4, Steven Johnson 3, Sara Scherrer 3, Kr ist ina M. Brooks 1, Christ ine E. Macbrayne 1, Lane R. Bushman 1, Peter L . Anderson 1, Jennifer J. K iser 1
1. University of Colorado Skaggs School of Pharmacy and Pharmaceutical Sciences, Aurora, CO2. University of Colorado Department of Public Health, Aurora, CO3. University of Colorado Hospital Department of Infectious Diseases, Aurora, CO4. Denver Health, Denver, CO
MAY 23, 2018INTERNATIONAL WORKSHOP ON CLINICAL PHARMACOLOGY OF ANTIVIRAL THERAPY 2018, BALTIMORE, MD
Abstract #2
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Financial Disclosures
o I have no conflicts of interest to report
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Background: Significanceo HIV/HCV infected persons who use drugs are an under-treated and under-represented population
oConcern of low adherence
oRe-infection potential especially for injection drug users
oRestrictions on treatment eligibility
o Co-infected HIV/HCV patients are at a higher risk for liver failure, cirrhosis and death but are underrepresented in clinical trials with DAAs
o Knowledge gaps in the pharmacology of DAAs in this population
o Unknown relationship between adherence and PK
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Sofosbuvir metabolism• Sofosbuvir (SOF) is transported into cells and metabolized to a uridine-monophosphate analog and
an active triphosphate analog inside cells (007-TP, originally GS-461203)
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Aims of the study
1. Define 007-TP PK in a HIV/HCV co-infected, drug using population.
2. Determine the association between [007-TP] in DBS and PBMCs and adherence to LDV/SOF.
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Study Design
N=60 HIV/HCV infected
persons who use drugs
Day 1 Wk 2 Wk 4 Wk 6 Wk 8 Wk 10 Wk 12 Off-drug (pre, 1-18h, 24h)Sample=Blood tube + DBS card
vDOTN=19
WOTN=20
LDV/SOF
Adherence (ADH)=#doses taken/#prescribed between visits
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Methodso*Quantification of 007-TP:oLC-MS/MS in 50-50,000 fmol/sample range
oSample=7mm punch or 1-2million PBMCs
oStats:oMixed models used to allow for repeated measures
oFinal ADH results modeled as both as continuous and categorical (≤50%, >50-75%, and >75%)
oOne-phase decay for t ½ calculation
* Rower, J.E., et al., Antimicrob Agents Chemother, 2015
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Data N=39 % Median (IQR)
Sex M 85%F 15%
Race non black 73%black 27%
Ethnicity Hispanic 77%Not 23%
Weight (Kg) 71 (63, 78)Age (years) 51 (46, 55)
HCV GT 1a 62%1b 26%4 5%1 8%
eGFR(mL/min/1.73^2)
84 (43, 162)
Therapy DOT 49%WOT 51%
Cirrhosis 21%
Demographics
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Demographics: ADH
N=39 subjects #ADH obs=227
N #ADH Obs
≤50% ADH 7 14>50-75% ADH 14 22
>75% ADH 38 191
Overall ADH over 12 weeks: Median (range) 94% (7%, 100%)
ADH=#doses taken/#prescribed between each visit
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007-TP PKDBS GM (95%CI): 616 (447, 783) fmol/punch
PBMCs GM (95%CI):1820 (1212, 2596) fmol/10^6 cells
o DBS t ½ = 104 (59-182) hours o PBMCs t ½ = 26 (15, 110) hours
3 2
6 4
1 2 8
2 5 6
5 1 2
1 0 2 4
2 0 4 8
4 0 9 6
8 1 9 2
1 6 3 8 4
fmo
l/1
0^
6 c
ell
s
Wk
2
Wk
4
Wk
6
Wk
8
Wk
10
Wk
123 2
6 4
1 2 8
2 5 6
5 1 2
1 0 2 4
2 0 4 8
fmo
l/p
un
ch
Wk
2
Wk
4
Wk
6
Wk
8
Wk
10
Wk
12
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0 .0 0 .1 0 .2 0 .3 0 .4 0 .5 0 .6 0 .7 0 .8 0 .9 1 .0
0
5 0 0
1 0 0 0
1 5 0 0
2 0 0 0
A D H F ra c tio n
fmo
l/p
un
ch
Results: Adherence and DBS • For every 10% increase in ADH, DBS 007-
TP increased 7.0% (95% CI 3.8%, 10%) P<0.0001
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50%
>50-7
5%
>75%
1 6
3 2
6 4
1 2 8
2 5 6
5 1 2
1 0 2 4
2 0 4 8
% A D H
fmo
l/p
un
ch
Results: 007-TP/punch by ADH category
424 (332, 540)547 (349, 859)
622 (397, 976)
P=0.0003
P=0.02
Overall P=0.002
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0 .0 0 .1 0 .2 0 .3 0 .4 0 .5 0 .6 0 .7 0 .8 0 .9 1 .0
0
2 0 0 0
4 0 0 0
5 0 0 0
1 0 0 0 0
1 5 0 0 0
2 0 0 0 0
A D H F ra c tio n
fmo
l/1
0^
6 c
ell
s
Results: Adherence and PBMCs• For every 10% increase in ADH, PBMC 007-
TP increased 23% (95% CI 15%, 31%) P<0.0001
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50%
>50-7
5%
>75%
1 6
3 2
6 4
1 2 8
2 5 6
5 1 2
1 0 2 4
2 0 4 8
4 0 9 6
8 1 9 2
1 6 3 8 4
% A D H
fmo
l/1
0^
6 c
ell
s
Results: 007-TP PBMCs by ADH category
615 (387, 978)
867 (333, 2254)
1853 (739, 4646)
P<0.0001
P=0.17
Overall p<0.0001
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Covariate Analysis DBS
ref group (0)=non-black, female, WOT*ADH is per 10% increase, not winsorized
Effect variable
Univariate Multivariate%Change
007-TPP Val
%Change 007-TP
P Val
*ADH 8.67% <.0001 8.66% <.0001
Weight -1.45% 0.014 -1.30% 0.019eGFR -0.68% 0.037 -0.29% 0.396
Race 69.9% 0.002 24.9% 0.149
Sex -20.3% 0.313Age 1.03% 0.270
DOT vs WOT -14.0% 0.382
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Covariate Analysis PBMCs
ref group (0)=non-black, female, WOT*ADH is per 10% increase, not winsorized
Effect variable
Univariate Multivariate
%Change 007-TP
P Val%Change
007-TPP Val
*ADH 27.0% <.0001 23.8% <.0001
Weight -0.62% 0.463 -0.68% 0.265
eGFR -0.83% 0.057 -0.54% 0.155
Race 93.7% 0.006 9.67% 0.683
Sex -57.8% 0.002 -44.9% 0.008
Age 0.22% 0.862
DOT vs WOT -5.42% 0.810
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Conclusionso Half-life estimations support cumulative dosing of SOF (104 h in DBS, 26 h PBMC)
o ADH was the most significant predictor of 007-TP levels, remained after controlling for other covariates
o 007-TP levels were significantly lower in <50-75% ADH categories
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Future directions
o Develop a PK model that can predict ADH based on 007-TP levels in both DBS and PBMCs
o Further exploration of univariate and multivariate predictors after study completion
o Determine relationship between cure and ADH o3/36 subjects with SVR 12 visit were virologic failures
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Acknowledgmentso CAVP laboratoryo Jennifer Kiser, PharmDo Peter Anderson, PharmDo Ryan Huntley, BSo Ryan Coyle, BAo Kristina Brooks, PharmDo Cricket McHugh, BAo Lane Bushman, BSo Teisan Zheng, PhDo Becky Kerr, BSo Lucas Ellison, BAo Laura Roon, BA/BSo David Nerguzian, BSo Martin Williams, BSo Bethany Johnson, BAo Joe Gomez, BS
o Denver Healtho David Wyles, MD
o Josh Blum, MD
o Sarah Rowan, MD
o University of Colorado Hospital and CCTSI o Jose Castillo-Mancilla,
MD
o Steven Johnson, MD
o Sara Scherrer, MD
oFundingo National Institute on Drug
Abuse - 1R01DA040499-01o NIH/NCATS Colorado CTSA
Grant Number UL1 TR002535
o Gilead Sciences
o Department of Public HealthoMary Marrow, MS
o Samantha MaWhinney, PhD