Postoperative Pain Clinical Trial
Official title:
Pre- vs. Post-incisional Pregabalin for Postoperative Pain Attenuation and Analgesics Spare in Orthopedic Oncologic Patients: A Comparative, Randomized, Double Blind Study Protocol
Hypothesis
No studies considered the comparison of preemptive vs. post-surgery Pregabalin (PGL) only
administration. The investigators believe that the administration of PGL preemptively would
diminish pain sensation and therefore the need for opioids administration in
orthopedic-oncologic patients more effectively than if administered starting
postoperatively.
Background
Proper pain relief is a major concern of patients worldwide. Pain concerns the surgical team
as well, because of its correlation with clinical outcomes and patients' satisfaction rate.
Studies have shown that negative clinical outcome with regard to pain control includes
decreases in vital capacity and alveolar ventilation, pneumonia, tachycardia, hypertension,
myocardial ischemia, transition into chronic pain, poor wound healing, and psychological
sequelae. Pain has been found to be one of the three most common medical causes of
delayed/aborted discharge after ambulatory surgery, the other two being drowsiness and
postoperative nausea/vomiting. Despite progress that has been made with regard to
postoperative pain control, and the development of new standards for pain control, many
patients continue to experience intense pain after surgery.
Recent advances in the understanding of the particularities of central sensitization
indicate that it plays an important role in post surgical and post traumatic pain and
therefore should be avoided. We now distinguish postoperative pain, which is mostly
nociceptive, and which perceives pain following surgical insult, from the exacerbation of
acute nociceptive pain that leads to neural sensitization, when sensations that are not
normally painful, are perceived as painful, as in hyperalgesia and allodynia. Thus, acute
pain may transform into subacute or chronic pain, conditions that are harder to control when
more persistent (chronic) they become. Better pain control, possibly using drugs that affect
both acute and chronic pains, seems therefore the current optimal choice.
Multimodal analgesia Advances in knowledge of the neuropharmacological molecular mechanisms
of pain have led to the development of "multimodal analgesia" practice.
The concept of multimodal analgesia is now a well established clinical practice. For
example, non-steroidal anti-inflammatory medications combined with intravenous
patient-controlled morphine administration, may decrease nausea and sedation in patients
when compared with that using patient-controlled morphine analgesia alone. Multimodal
analgesia also can produce opioid sparing effects. Our group has shown repeatedly, that
multimodal analgesia spares postoperative morphine consumption and increases level of
patients' satisfaction. However, they may not improve postoperative outcome in terms of
faster recovery, reduced hospital stay, and decreased length of convalescence.
Analgesic adjuvant Adjuvants are compounds, which by themselves may have undesirable side
effects or low potency but in combination with opioids allow a reduction of narcotic dosing
for postoperative pain control. They are needed due to side effects of opioid analgesics,
which hinder recovery, especially when increasingly utilizing ambulatory surgical
procedures. One of the newer groups of products that are non-analgesic substances, therefore
named "adjuvants", are anticonvulsants (e.g., pregabalin).
Pregabalin (PGL) Interest has been focused on the analgesic, sedative, anxiolytic, and
opioid-sparing effects of pregabalin (PGL) (S+ 3-isobutyl GABA), a structural analog of GABA
(Gamma-Aminobutyric Acid) and a derivative of gabapentin in various pain settings, including
postoperative pain. Of a similar mechanism of action, it is thought to possess a superior
pharmacokinetic profile than gabapentin. Pregabalin has a variable role in neuropathic pain
conditions, such as post-herpetic neuralgia, painful diabetic neuropathy, central
neuropathic pain, and fibromyalgia. Some studies had not demonstrated a significant
analgesic effect in the acute, postoperative pain; others propose PGL to have effective
sedative and opioid-sparing effects , both useful characteristics for the control of acute
pain. Opioid sparing effects and improved pain scores have been seen after abdominal and
pelvic surgery. Its many potential actions such as reducing opioid requirements, prevention
and reduction of opioid tolerance, improvement of the quality of opioid analgesia, decreased
respiratory depression, relief of anxiety, and gastric sparing, make it an attractive drug
to consider for control of pain in the post operative period.
Population characteristics The orthopedic oncological patients are a specific group of
individuals whose demand for antinociception starts rather before surgery because of the
bone tumor-generated pain that usually signals the first existence of pathology.
Subsequently, these patients would require postoperatively more analgesics than after
general surgery and for a longer period of time. We have demonstrated previously that acute
pain that is superimposed on an already aroused CNS (central nervous system), i.e., the
presence of central sensitization, would create a situation where complete antinociception
is hard to obtain, as in these patients, and therefore the efficacy of the antinociceptive
protocol is best tested, comprised the possible transformation of acute into chronic pain.
preemptive drug has been pointed out as a beneficial tool for reducing perioperative pain.
Various techniques have been employed for this purpose; different drugs were used as well.
The beneficial effects of preemptive PGL were documented in patients who had undergone
lumbar discectomy, both immediately and 1 and 3 months after surgery.
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Allocation: Randomized, Intervention Model: Parallel Assignment, Masking: Double Blind (Caregiver, Investigator, Outcomes Assessor), Primary Purpose: Supportive Care
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