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Kevin39beave

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Ine for drug testing. Plasma was stored at a central repository for resistance testing. We monitored adherence with electronic pill bottle monitors (MEMS 6 TrackCap, AARDEX Group, Ltd., Sion, Switzerland) for the first 2 months after subjects started antiretroviral therapy (ART). We selected a single medication for monitoring according to the following hierarchy: dosed most frequently, combination
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Ine for drug testing. Plasma was stored at a central repository for resistance testing. We monitored adherence with electronic pill bottle monitors (MEMS 6 TrackCap, AARDEX Group, Ltd., Sion, Switzerland) for the first 2 months after subjects started antiretroviral therapy (ART). We selected a single medication for monitoring according to the following hierarchy: dosed most frequently, combination
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Es would most likely not have been affected. The measures of immune activation were not assessed at enrollment into the study cohort, and we therefore cannot make temporal inferences of a causal nature nor could we control for them in the multivariable Cox models. We used prevalence rate ratios (PRRs) to estimate the associations of interest as risk was our parameter of interest. We chose PRRs as
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D a randomized trial to evaluate the efficacy of DAART in OTPs.for this trial and supporting CONSORT checklist are available as supporting information; see Checklist S1 and Protocol S1.Methods Design and Follow-upWe conducted a randomized controlled trial comparing 12 months of DAART to self-administered therapy (SAT) in five Baltimore OTPs - 3 hospital associated (1 Veterans Administration) and 2
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D a randomized trial to evaluate the efficacy of DAART in OTPs.for this trial and supporting CONSORT checklist are available as supporting information; see Checklist S1 and Protocol S1.Methods Design and Follow-upWe conducted a randomized controlled trial comparing 12 months of DAART to self-administered therapy (SAT) in five Baltimore OTPs - 3 hospital associated (1 Veterans Administration) and 2
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Ow-up will be needed to determine whether HCV cure through the use of direct-acting antivirals among HIV/ HCV coinfected elite controllers will make the risk for complications among these patients similar to their HIV monoinfected counterparts. Further studies will also be needed to determine the effects of antiretroviral therapy in this group of patients coupled to its risk/benefit ratio. Whereas