Opioid Use Clinical Trial
Official title:
Opioid-Redox Study
Side effects of opioids can from practical view be divided into short-term and long-term.
Nervous system disorders are manifested by psychological status changes of the patient and
may cause confusion, mental and somatic dependency, dizziness and so on. Influencing the
vegetative and cardiovascular system hypotension can occur what is manifestation of
vasodilation and decreased myocardial inotropic activity. Another clinical sign is
bradycardia and is characterized by general weakness, sweating, collapse can develop. Effects
of opioids may cause respiratory depression, bronchospasm and bronchoconstriction. Side
effects on the gastrointestinal tract are nausea, vomiting, constipation and less frequently
dry mouth. The constipation does not develop tolerance and has to be avoided (dietary
modification, laxatives prevention) respectively during long-term opioid treatment
obstipation should be affected by blocking peripheral opioid receptors in the
gastrointestinal tract by application of an opioid antagonist methylnaltrexone, which does
not cross the blood brain barrier, or using naloxone, which is metabolized by "first-pass"
metabolism in the liver for example combined preparation containing oxycodone and naloxone
(Kulichová, 2012). Known side effects on parenchymatous organ especially on liver is
restricted biliary excretion caused by spasm of the biliary tract. Skin manifestations caused
by the effects of opioids are urticaria, dermatitis, and pruritus. Renal and urinary
disorders may develop as urinary retention and ureteral spasm. Rarely can occur disorders of
the immune system, which through the development of hypersensitivity may lead to the
development of anaphylactic shock (Kulichová, 2012). Opioids have a negative effect and the
endocrine system. Various studies have demonstrated the influence of opioids on regulatory
mechanisms. Fundamental changes occur in hypothalamic-pituitary complex, which directs the
activities of all the endocrine system. Secretion of hormones of the pituitary gland
regulates the nervous system through the hypothalamus, which is the coordination center of
autonomic function. The pituitary gland has coordinating function in relation to other
endocrine glands, and by production of their hormones affects the peripheral endocrine organs
and the targeting tissues (Kulichová, 2012), (Colameco, 2009).
Opioids decrease the secretion of gonadotropin-stimulating hormone, resulting in reduced
levels of luteinizing hormone. The result of these changes is reduced secretion of
testosterone and estradiol what results in symptoms of hypogonadism. Chronic administration
of exogenous opioids decreases the levels of adrenocorticotropic hormone and cortisol, as
well as their circadian rhythms. The result is a reduction in the response to stress. Effect
on prolactin is not entirely clear. Opioids can stimulate the hypothalamus through the
thyroid stimulating hormone, which may cause prolonged and increased response to opioids in
patients with hypothyroidism. Chronic use of opioids is associated with weight gain,
hyperglycemia and diabetes can worsen (Kulichová, 2012). It may be related to central effects
through the sympathetic nervous system and impaired insulin secretion. New laboratory
measurements show the development of oxidative stress in patients receiving morphine and
related drugs (Merdin, 2016).
The consequences of these biochemical changes further negatively affect the clinical outcome
of the patients. They may become predisposed to excessive progression of previously latent
diseases whose manifestations in patients previously were not apparent and there is emergence
of new diseases. The present data are essential to create a clinical prospective
observational studies to clarify this issue and its conclusions would be essential for new
therapeutic options for adjuvant therapy in patients suffering from chronic pain.
The process of the study, the choice of the patients, the collection and the processing of
data A. Potential participants of study will be familiarized with the course of research in
every detail before entering the study and after signing of an informed consent they will be
examined by algesiologist. The patients will receive ID number generated by computer because
of preserving of anonymity for the purpose of statistical processing of the data. Monitored
clinical parameters: The current consumption of analgesics, examination of the type of pain
(nociceptive vs. neuropathic - completed questionnaire for PainDetect, DN4 and LANSS Pain
scales), demographic information (weight, height, age). Examination of biochemical parameters
(ALT, AST, GMT, bilirubin, urea, creatinine, creatinine clearance, antioxidant enzymes and
their substrates (glutathione peroxidase, glutathione reductase, catalase, superoxide
dismutase, glutathione). These data will be entered into an online database. The statistical
analysis of the activities of the enzymes will determine the confidence interval (CI) of 95%.
Patients whose entrance numbers will be in this range will keep on in the study, remaining
patients will be excluded. The patients who will keep on in study will be divided into four
groups.
Group A: patients with chronic pain taking morphine, hydromorphone, oxycodone Group B:
patients with chronic pain taking transdermal patch (Buprenorphine) Group C: patients with
chronic pain taking transdermal patch (Fentanyl) Group D: opioid rotation B. The first
inspection will be carried out 6 months after the beginning of taking of opioids for severe
pain. During the first inspection, clinical and biochemical parameters will be examined same
as during the input examination of the patient. The patient will fill out a questionnaire
PainDetect, DN4 and LANSS Pain scales. C. The second inspection will be carried out 12 months
after the beginning of taking of opioids for severe pain. During the second inspection,
clinical and biochemical parameters will be examined same as during the previous two patient
examinations. The patient will fill out a questionnaire PainDetect, DN4 and LANSS Pain
scales.
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