Chronic Pain Clinical Trial
Official title:
Effects of Amitriptyline on Central Pain Processing in Healthy Volunteers Depending on CYP Pharmacogenetics
Low dose tricyclic antidepressant drugs are routinely administered co-analgesics in pain medicine. Amitriptyline is largely considered as a gold standard. Amitriptyline underlies cytochrome CYP2D6 and CYP2D19 metabolism. CYP2D6 is highly polymorphic; numerous genetic variants result in 4 major classes characterizing enzymatic activity: poor metabolizers, intermediate metabolizers, extensive metabolizers and ultrarapid metabolizers. It is not known to which extent metabolizer classes determine pain outcomes or side-effects. As only one in three pain patients is considered to be a responder to amitriptyline's co-analgesic effect, prediction of treatment efficacy with a fast and easy to perform bedside test may contribute to the patients quality of life. The aim of this study is to determine the influence of cytochrome variants on experimental pain, drug related side-effects and finally identification of active metabolites.
Background
Pain is defined as an ongoing unpleasant sensory experience, which can be classified
according to three major, although overlapping, etiologies: nociceptive, inflammatory and
neuropathic pain.
Antidepressants are widely used as co-analgesics in the management of chronic pain. An
overview of different substances and their relation to their mechanism of action is presented
in the review of Dharmashaktu et al. Low-dose tricyclic antidepressants are well established
in the treatment of neuropathic pain. Amitriptyline and imipramine are two widely used
substances of this group. The hypoalgesic effect of amitriptyline is mainly mediated by
inhibiting serotoninergic and noradrenergic reuptake. When administered at night time,
amitriptyline's sedating effect enhances sleep quality, considered as an important
improvement in quality of life in chronic pain patients.
Tricyclic antidepressants undergo biotransformation in the liver with CYP2D6 catalyzing
hydroxylation, whereas CYP2C19 mediates demethylation of the parent drug. The demethylated
metabolites are partially tricyclic drugs by themselves, such as nortriptyline and
desipramine, which are demethyl-metabolites of amitriptyline and imipramine. It is unknown
whether the analgesic effect of amitriptyline is mediated through its precursor or the
metabolites.
The CYP2D6 gene is highly polymorphic and the numerous genetic variants result in 4 major
metabolizer classes characterizing enzyme activity: poor metabolizers (PM) with no enzyme
activity, intermediate metabolizers (IM) with reduced enzyme activity, (EM) extensive
metabolizers carrying two functionally active alleles and ultrarapid metabolizers (UM)
carrying a gene duplication or multi-duplication resulting in increased enzyme activity.
CYP2D6 PMs have higher plasma concentrations of the parent drug than EMs and are, therefore,
more likely to experience dose-dependent adverse drug reactions. In 50 psychiatric patients
receiving amitriptyline 150 mg/d, carriers of two functional CYP2D6 alleles (EMs) had a
significantly lower risk of side effects than IM (12.1% vs. 76.5%). The lowest risk was
observed for carriers of two functional CYP2D6 alleles combined with only one functional
CYP2C19 allele. The combination of normal (fast) CYP2C19 and slightly diminished CYP2D6
function leads to high concentrations of toxic intermediate metabolites and an increase of
adverse events. On the other hand, CYP2D6 UMs may be at risk for sub-therapeutic
concentrations resulting in poor therapeutic response. Thus, genetically determined
differences in blood concentrations of antidepressants make dose adjustments advisable.
However, these findings and dose recommendations have only been evaluated for psychiatric
patients and no investigation on antidepressants as low-dosed co-analgesics are available up
to now.
Quantitative sensory tests (QST) have been intensively used for more than three decades to
explore the central processing of painful stimuli in patients and healthy volunteers. QST
were developed to assess the responses to sensory stimuli, providing psychophysical methods
for the assessment of the nociceptive system. In addition, large cohorts of healthy
volunteers have been investigated using QST measures to produce reference values.
QST measures are based on a multimodal and multi-tissue approach, combining different pain
modalities applied to different tissues in order to gather sufficient and discriminative
information about the human nociceptive system. QST will be our tool to characterize
analgesic efficacy of amitriptyline. QST offers the unique opportunity of experimentally
induced pain being quantitatively measured by psychophysical, behavioural and
neurophysiological responses.
Objective
We test the hypothesis that the extensive and ultrarapid CYP2D6 metabolizers are associated
with a higher analgesic effect of amitriptyline, compared to the poor and intermediate
metabolizers, as assessed by quantitative sensory tests. Plasma concentrations of
amitriptyline and its metabolites will be analysed as co-variates for drug efficacy.
Two sub-studies, one peak-level, single-dose administration and one steady-state, repeated
dose administration, are needed to assess the pharmacokinetics of amitriptyline and its
active metabolites.
Statistics are provided by José A. Biurrun Manresa.
Methods
Two consecutive randomized placebo-controlled two-way crossover sub-studies on amitriptyline
will be conducted in consenting, healthy, male volunteers. Both sub-studies have the same
aim: to determine the association between CYP2D6 genotype, drug response measured by QST and
plasma concentrations of amitriptyline and its metabolites. The first sub-study will be
conducted with a single high dose of amitriptyline (100 mg). The second sub-study will be
conducted with repeated low doses of amitriptyline (25 mg) once a day for 10 days.
In both sub-studies the same experimental procedures and statistical analyses will be
performed. The only difference between the sub-studies is the dose of amitriptyline and the
duration of drug intake.
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