Project

Metabolism of antiretroviral drugs in HIV infected patients with toxicity – a pilot study

Automatically Closed · 2020 until 2020

Type
Clinical Studies
Range
Monocentric project at KSSG
Units
Status
Automatically Closed
Start Date
2020
End Date
2020
Financing
KSSG
Partner
EMBL, Heidelberg, Germany, https://www.embl.de/
Brief description/objective

Antiretroviral drugs can be responsible for a wide range of toxic side effects ranging from acute events to long-term toxicity. We hypothesize that the microbiome-mediated metabolism plays a substantial role in antiretroviral drug toxicity through several mechanisms.

This pilot study will compare the plasma metabolome of antiretroviral drugs from four major drug classes between patients experiencing adverse drug effects and controls. The aim is:

(1) Identification of key metabolites involved in HIV drug toxicities for the described antiretroviral drugs and side effects;

(2) Generation of hypotheses regarding valid microbiota derived biomarkers and the underlying pathomechanism that will lead to toxicity and

(3) Development a study protocol based on the findings for a follow-up study to validate the generated findings/hypotheses.

We will evaluate prospectively collected plasma samples stored in the Swiss HIV Cohort Study (SHCS) biobank. Metabolomics analysis of plasma samples will be performed using liquid chromatography coupled mass spectrometry (LC-MS). Targeted integration of the signals for drug and known drug metabolites will be performed and will reveal patients’ plasma levels of drug and drug metabolites. Furthermore, we will conduct untargeted analysis of the metabolomics data and perform differential analysis (including correction for multi-hypothesis testing) between patient cohorts with and without drug-related side effects. This analysis will identify metabolites that are different between the different patient groups. Based on these results, we will design a prospective study aiming at identifying metabolic and microbiome biomarkers that are predictive for toxic side effects.