Meloxicam: An Update On Its Use In The Perioperative Period
Carolyn Kloepping1*, Stephen Van Beek2, Alex Bekker3
1 Asst Professor Department of Anesthesiology Rutgers New Jersey Medical School Newark, NJ, 07103.
2 Rutgers New Jersey Medical School Newark, NJ, 07103.
3 Professor and Chair, Department of Anesthesiology Professor, Department of Physiology and Pharmacology Rutgers New Jersey Medical School
Newark, NJ, 07103.
*Corresponding Author
Carolyn Kloepping,
Carolyn Kloepping,
Asst Professor, Department of Anesthesiology Rutgers New Jersey Medical School Newark.
E-mail: kloeppch@njms.rutgers.edu
Received: January 15, 2021; Accepted: January 29, 2021; Published: February 27, 2021
Citation: Carolyn Kloepping, Stephen Van Beek, Alex Bekker. Meloxicam: An Update on its Use in the Perioperative Period. Int J Anesth Res. 2021;09(01):611-618. doi: dx.doi.org/10.19070/2332-2780-21000122
Copyright: Carolyn Kloepping© 2021. This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use,
distribution and reproduction in any medium, provided the original author and source are credited.
Abstract
Meloxicam, a preferential COX-2 inhibitor, has been used to treat osteoarthritis, rheumatoid arthritis, ankylosing spondylitis, as
well as various chronic skeletomuscular pain syndromes. Where as oral meloxicam preparations are rarely indicated for treatment
of acute pain due to a poor dissolution rate and slow on set of action, the introduction of an intravenous NanoCrystal
Colloidal Dispersion formulation of meloxicam provides the possibility of using this drug for acute pain during the perioperative
period. This review summarizes pharmacologic properties of meloxicam, including its pharmacokinetics, pharmacodynamics,
adverse effects, and tolerability. We examine and discuss recently completed clinical trials that evaluated the efficacy and
safety of intravenous meloxicam in the treatment of postoperative pain. Literature retrieval was performed through PubMed
(through June 2020) using combinations of the terms meloxicam, acute pain, and pharmacology. In addition, bibliographical
information, including contributory unpublished data, was requested from the company developing the drug. Based on the
summary of the current literature, we conclude that intravenous meloxicam is an effective and well-tolerated analgesic agent
for the management of moderate to severe acute postoperative pain.
2.Introduction
3.Pharmacokinetic Properties
4.Pharmacodynamic Properties
5.Perioperative Use Of Meloxicam
6.Meloxicam For Treatment Of Neuropathic Pain
7.Tolerability
8.Conclusion
9.References
Introduction
Postoperative pain is a natural and expected consequence of
surgery, and opioids have been relied upon as the main stay of
treatment for acute pain. However, significant side effects and
risks can be associated with opioids, which include respiratory depression,
nausea and vomiting, ileus, urinary retention, pruritus,
as well as potential dependence and addiction. [1] The “Practice
Guidelines for Acute Pain Management in the Perioperative Setting”,
adopted by the American Society of Anesthesiology, recommend
multimodal strategies for the management of postoperative
pain, stating that “unless contraindicated, patients should
receive an around-the-clock regimen of NSAIDs, COXIBs, or
acetaminophen.”[2]
Meloxicam, an enol-carboxamide NSAID related to piroxicam,
has long been used to treat pain and inflammation. Unlike other
NSAIDs, it has a greater inhibitory activity against the inducible
isoform of cyclo-oxygenase (COX-2) than against the constitutive
isoform (COX-1). [3] COX-1 induces synthesis of prostacyclin,
which is responsible for vascular homeostasis, platelet aggregation,
renal function, and gastric cyto-protection. The expression
of COX-2 isoform increases during inflammation. While meloxicam’s
anti-inflammatory and analgesic properties are similar to
non-selective NSAIDs, it has both gastric mucosal and renal protective
properties. [4]
Oral formulations of meloxicam are widely used to treat osteoarthritis,
rheumatoid arthritis, ankylosing spondylitis, as well as various
pain syndromes of skeletomuscular origin, such as low back
pain. The half-life of meloxicam is approximately 20 hours. Maximum
meloxicam plasma concentration following oral administration
(patient in fasted state) was achieved after approximately 10
hours for the most part due to its poor dissolution rate. [5] Therefore,
oral preparations of meloxicam are not frequently indicated
for the treatment of acute or postoperative pain.
A novel intravenous formulation of NanoCrystal Colloidal Dispersion
Meloxicam has been developed in the last decade for
the management of acute pain. [6] A number of phase 2 and
phase 3 studies have been recently completed to evaluate efficacy
and safety of IV meloxicam for treatment of postoperative pain
in a number of clinical settings [7-14]. This article provides an
overview of the pharmacological properties of various meloxicam
preparations (i.e. oral, parenteral, and transdermal) as well as
clinical efficacy and tolerability in the treatment of postoperative
pain. [15]
Pharmacokinetic Properties
Absorption: The absorption of meloxicam has been studied following its
administration via intramuscular, oral, and rectal routes. The absolute
bioavailability (F) was 89% for oral capsules after a single
30mg dose. [5] Maximum meloxicam plasma concentration
(Cmax) was achieved after 5-6 hours (tmax) when administered
after breakfast [16]. When administered in a fasting state, the
Cmax for meloxicam doubled. When used chronically, NSAIDs
are typically administered after a meal: thus, Cmax=5-6 hours is
more clinically relevant. The absorption of meloxicam is independent
of dose over the range 7.5-30 mg, leading to dose-linear
increases in meloxicam plasma concentrations. [17] This consideration
enables easy dose titration in those patients requiring
higher or lower doses than normal.
Distribution: Meloxicam, as most NSAIDS, is highly protein bound (>99%)
to albumin. [18] The binding is consistent over the concentration
range encountered in clinical practice. This high protein binding
results in a restricted volume of distribution (Vd) of 10-15 L [17],
similar to that reported for other NSAIDs. [19, 20] Animal experiments
suggest that meloxicam is predominantly distributed to
highly perfused (albumin rich) compartments such as the blood,
liver, kidney, etc., with the volume of distribution approximating
the extracellular space.[18] Meloxicam does penetrate local tissue
as well, for example, 40-45% of the accompanying steady-state
meloxicam plasma concentrations are found in synovial fluid,
slightly lower concentrations being observed in the adjacent tissues.
[21]
Metabolism: Meloxicam is primarily eliminated by metabolic degradation,
about equal parts renal and fecal elimination, with <0.25% eliminated
unchanged in the urine and 1.6% of the parent compound
present in feces. [8] Meloxicam undergoes extensive phase 1 eliminations,
and no conjugated derivatives have been identified. The
metabolism of meloxicam is primarily mediated by CYP450 2C,
on the isoenzyme CYP2C9. [22] The main metabolite is formed
by the oxidation of the methyl group of the thyiozyl moiety; the
metabolites do not change renal blood flow, and are not nephrotoxic.
[23]
Elimination: The total clearance of oral meloxicam is 0.42-0.48 L/h. The elimination
half-life (t 1/2) is approximately 20 hours, which is relatively
short compared to other NSAID of the same class [16]. Unlike
diclofenac, which has a short elimination half-life (1-2 hours) and
require a slow-release formulation for a once-daily regimen, the
longer elimination half-life of meloxicam allows for daily dosing
without a slow release formulation. The efficacy of slow-release
formulations can be influenced by food in take, as in with Diclofenac
where there are variations in concentration-profiles
based on food intake. [16] This effect is less likely in meloxicam
due to its longer elimination half-life.
Anti-inflammatory and Antioxidant: The anti-inflammatory effects of meloxicam is well demonstrated
in rat models, inhibiting effects such as carrageenan or kaolininduced
rat paw edema, granuloma formation following cotton
implantation in rats, kaolin-induced rat pleurisy, and rat adjuvantinduced
arthritis. [16, 17] In these models, a single dose of meloxicam
curbed inflammation for a prolonged period of time.
Additionally, the antioxidant effects of meloxicam have been a
topic of interest and research. Meloxicam protects from hepatotoxicity
by strengthening the antioxidant barrier, and has been
cited as being neuroprotective in mice by augmenting antioxidant
enzymes. [24, 25, 26] Pawlukianiec et al, found that meloxicam
inhibits protein glycation, reduces protein oxidation products
when exposed to glycating and pro-oxidant factors, and increases
antioxidant properties of albumin. [24] This lends to further investigative
work on utilization of meloxicam as an antioxidant
and antiglycating agent in management of processes such as rheumatic
diseases. [24]
Analgesic: Meloxicam has been demonstrated to exert a prolonged effect
against inflammatory pain in the rat, and has also been studied in
other animal models. [27] Following a single oral administration,
the analgesic effect of meloxicam is not reduced by 50% until
18 hours after administration. [3] Additionally, meloxicam has a
markedly longer duration of action than piroxicam, diclofenac,
and indomethacin.
Anti-pyretic: Meloxicam, like other NSAIDs, has no effect on body temperature
in normothermic mammals; however, NSAIDs are influential
on pyrogen-induced fever. Meloxicam shows lower potency
against yeast-induced pyrexia than diclofenac and piroxicam. At
a dose of 0.1mg/kg, meloxicam was found to reduce endotoxininduced
fever in a cat. [28, 29]
Perioperative Use Of Meloxicam
Meloxicam is used for the management of acute and chronic pain,
and a number of studies on use of meloxicam for the treatment
of osteo- and rheumatoid arthritis have been published. [30-35]
In the following discussion, we will focus on the studies which
compare pharmacokinetic and efficacy of various meloxicam
preparations in the perioperative setting as well as for treatment
of neuropathic pain.
Although oral administration of meloxicam as 7.5 mg and 15 mg
tablet are most common, other doses and methods of meloxicam
delivery are available, such as transdermal and intravenous forms. Product formulation may have a significant impact, not only on
absorption rates but also on penetration depth and length of effect.
Oral route: The use of oral meloxicam has been extensively studied for the treatment of postoperative pain from elective surgery and dental procedures. In a study involving patients undergoing inguinal hernia repair under local anesthesia, patients were randomized to receive or not receive preoperative oral meloxicam dosing. In the postoperative period, IV diclofenac was administered for pain control. Results showed significantly lower VAS scores for the group preoperatively treated with meloxicam, and less use of rescue IV diclofenac (36% vs. 88%). [36]
For patients undergoing a total abdominal hysterectomy (n=36), Thompson et al. conducted a double blind randomized control study to examine the analgesic effect of a meloxicam suppository versus placebo suppository, administered preoperatively. [37] Postoperatively, patients received a morphine PCA, and pain scores and morphine usage were evaluated. VAS scores were significantly lower in the meloxicam suppository group, but PCA morphine usage was not decreased significantly in the treatment group. [37]
Aghadavoudi et al. compared preoperative dosing of meloxicam (15 mg) and celecoxib (400 mg) for the treatment of pain in a double-blind randomized control study for lower extremity surgery. [38] Although pain severity was higher in the first two hours in the celecoxib group and six hours postoperatively in the meloxicam group, by 12 hours there was no significant difference in pain scores. [38]
An updated Cochrane review recently evaluated the analgesic efficacy of a single dose oral analgesics in acute postoperative pain, summarizing results from randomized double-blind placebo controlled clinical trials involving NSAIDs (including meloxicam), paracetamol, and opioids for acute postoperative pain relief, through 2011. [39] In regards to the studies involving meloxicam, none met inclusion criteria for analysis, thus no final determination could be made. [39]
In addition to postoperative surgical pain, oral meloxicam has also been assessed in the management of pain following dental cases. [40, 41] Orozco-Solis et al. administered single-dose preprocedural meloxicam (15mg) or diclofenac (100mg) for patients undergoing mandibular third molar removal. Statistically significant decreased postoperative pain and increased mouth opening 24 hours post-surgery was evident in the meloxicam group, as well as an observed, but non-significant, decrease in facial swelling in both groups. [40] Calvo et al. compared the effects of 7.5mg meloxicam vs. 15mg meloxicam, administered in the postoperative period for up to four days, for pain also following third molar removal. [41] Patients receiving 7.5mg meloxicam who required osteotomy reported higher pain scores than those who did not require osteotomies, and used more rescue analgesics than those without osteotomy.[41] However, in the group which received 15mg of meloxicam, there was no significant difference in rescue analgesic dosing between osteotomy and non-osteotomy groups. [41]
Nekoofar et al examined use of meloxicam for endodontic pain requiring root canal. Patients were administered 15 mg meloxicam, 20 mg piroxicam, or a placebo preoperatively, and evaluated for postoperative pain rating. [42] The mean change of VAS between pre-dental procedure and eight hours post procedure was highest in the meloxicam group; however, the overall reduction of pain between meloxicam, piroxicam, and placebo was not significant. [42] In a similar, but large prospective double-blind randomized clinical trial, preoperative meloxicam (7.5 mg), acetaminophen (650 mg), and ibuprofen (400mg) were compared for efficacy in reducing pain after separator placement for orthodontic surgery; results did not reveal a statistical statistically significant difference in pain perception scores between the three groups. [43]
Utilization of preoperative versus postoperative oral meloxicam dosing in patients for orthopedic procedures has also been an area of focus. [44, 45, 46] Ren et al randomized scheduled total hip replacement patients to receive meloxicam 15 mg at 24 hours preoperation, 7.5 mg at 4 h, 24 h, 48 h and 72 h post-operation; or meloxicam 15 mg at 4 hours post-operation, then 7.5 mg at 24 h, 48 h and 72 h post-operation. [44] Between the two groups, PCA consumption, VAS scores at rest 6h, 12h, 24 hrs after surgery, and VAS with activity, 6 and 12 hrs after surgery, were decreased in patients administered preoperative meloxicam. Satisfaction scores were also higher in the preoperative meloxicam group versus postoperative. [44] In patients receiving total knee replacement with the above protocol, a similar decrease in PCA consumption and VAS scores was noted in those patients who received meloxicam preoperatively. [45] Likewise, for patients undergoing knee arthroscopies, preoperative meloxicam ( 24 hours or 1 hour) prior to surgery resulted in decreased patient global assessment (PGA) score, and less consumption of rescue pethidine. [46]
Transdermal/Transmucosal formulations: Alternative delivery options of meloxicam, such as transmucosal and transdermal, have been implemented for post-procedure periodontal and dental impaction surgeries. Transmucosal mucoadhesive meloxicam films at doses of either 45 mg, 30 mg, 20 mg, or 10 mg meloxicam per film were applied to post-periodontal flap surgery over surgical sites for a duration of four days, in a study by Rajeswari et al.[47] There were no reported adverse effects, and all patients noted immediate pain relief with application of the film, with pain control best captured in the 45mg and 30 mg groups; this subset had adequate pain control for the first 24 hours.[47]
Transdermal formulations of meloxicam, resulting in less systemic side effects as first pass metabolism would be avoided, have also been examined. Chen et al. focused on features needed in the transdermal delivery of meloxicam that would enhance permeation of meloxicam through the stratum corneum and the skin. [48] Formulation types including gels, liposomes, patches, micro emulsions, and physical approaches including electroporation, iontophoresis, and sonophoresis were reviewed, and although the author concluded that patches would be a better choice given more accurate dosing and compliance, further research is needed to ensure safety and desired effect. [48]
Pharmacokinetic studies comparing drug levels of meloxicam in plasma and synovial fluid following oral meloxicam, as well as meloxicam gel administration to hind legs in beagles, revealed higher concentrations in synovial fluid underlying the applied target site (gel administration) compared to oral delivery. [49] Furthermore, in the untreated leg, synovial fluid concentrations of meloxicam were similar to plasma concentrations following oral administration of meloxicam. [49]
Zhang et al compared conventional liposome, deformable liposome (transfersome) and microemulsion formulations as potential carriers for the dermal delivery of meloxicam. [50] Both liposomes and microemulsions were subjected to structural studies and applied to human cadaver skin. Transfer somes revealed a greater ability to penetrate the skin compared to the classical nondeformable liposomes, likely due to presence of surfactants acting as edge activators and destabilizing lipid bilayers, suggesting better potential as a transdermal drug carrier for meloxicam. [50]
Continued research and development of transdermal formulations of meloxicam may yield an alternate therapy option for patients with the potential to cause fewer systemic side effects.
Intravenous Administration: The use of intravenous meloxicam was evaluated in the 2001 by Romsing et al., where in postoperative patients were randomized to receive 7.5 mg meloxicam intravenously or via local wound infiltration following inguinal hernia repair. [51] Subsequently, a fixed postoperative pain regimen (acetaminophen plus codeine every six hours prn) was administered, and if necessary, supplemented with intravenous fentanyl for break through pain. Results reflected significantly lower plasma concentrations of meloxicam in the local infiltration group compared to the IV group, but no significant difference in pain scores or use of supplemental analgesics between groups. [51]
More recently, there has been renewed interest in the use of intravenous meloxicam, with several published studies and on going clinical research trials for postoperative pain control for abdominoplasty, orthopedic surgery, podiatric surgery, dental procedures, and other major surgical procedures. These studies utilized a formulation of intravenous meloxicam designed with a NanoCrystal colloidal dispersion that would enhance the bioavailability of meloxicam. [8-22]
Treatment of post-procedure dental pain with the intravenous NanoCrystal meloxicam formulation for removal of impacted third molars was assessed by Christensen et al in 2018. [8] The randomized, double-blind controlled trial evaluated the postoperative pain intensity, safety, and tolerability of intravenous meloxicam compared to ibuprofen and placebo. [8] Patients in the study needed greater than 2, third-molar removals, one of which required bony extraction. Those with significant pain within five hours post procedure were randomized to receive either IV meloxicam (15, 30, or 60mg), IV placebo, or PO ibuprofen tablets. [8] Meloxicam IV 60 mg produced the greatest reduction in pain, followed by 30mg and 15mg dosing. Additionally, a more rapid on set of pain relief was seen with IV meloxicam than for ibuprofen, with duration of effect lasting 24 hours. Although there was less rescue analgesia needed in the IV meloxicam groups, this was not statistically significant when compared to placebo. [8]
Use of intravenous meloxicam for ERAS protocols in colorectal surgeries was evaluated in a clinical trial by Silinsky et al. [14] Patients were administered 30mg IV meloxicam or placebo approximately 30 minutes prior to the procedure, and every 24 hours until discharge or administration no longer clinically appropriate. [14] Statistically significant findings included a decreased length and cost of hospital stay, reduction in opioid use, reduced postoperative pain intensity, reduced time to first bowel sound, and first flatus and first bowel movement, when compared to placebo. [14]
In a trial involving patients with moderate to severe pain following bunionectomy, the use of postoperative intravenous meloxicam (30 mg or 60 mg) administered every 24 hours for up to three days resulted in rapid on set of analgesia and significant decrease in pain intensity compared to placebo; there was no measurable difference between the two doses. [22] Similarly, daily dosing of intravenous meloxicam for patients following abdominoplasty(n=219), led to a significant reduction in pain intensity, pain global assessment scores, and decrease rescue dosing of oxycodone when compared to the placebo group. [9]
Two recent phase three studies evaluated the effect of postoperative daily intravenous meloxicam (30mg) vs. placebo for postoperative pain control for orthopedic and major elective surgeries. [10, 11] A statistically significant reduction in total opioid use was seen through out the treatment period in the IV meloxicam group compared to the placebo group. [10] A subsequent phase 3 randomized placebo-controlled study evaluated the safety of intravenous meloxicam (30 mg, once daily) following major elective surgery led to similar findings-reduced opioid consumption (23.6%) in subjects with moderate to severe postoperative pain following major elective surgery. [13]
Lastly, a phase two randomized clinical trial examined the effect of daily intravenous meloxicam (5-60 mg) on providing analgesia to subjects with moderate to severe pain after open abdominal hysterectomy. [12] There was a statistically significant improvement in the summed pain intensity difference and total pain relief over the first 24 hours after dosing compared with placebo, with quick on set of pain relief (within 6-8 minutes after IV meloxicam administration), and reduced total rescue opioid consumption (42%–71%) with meloxicam IV compared to placebo. [12]
Meloxicam For Treatment Of Neuropathic Pain
There has been some literature and research completed in examining
the effect of meloxicam on neuropathic pain. Takeda et al.
evaluated the role of spinal COX-2 on the pathophysiology of
neuropathic pain by using an intrathecal infusion of meloxicam
vs. saline following L5/L6 spinal nerve ligation in rats. [52] Intrathecal
infusions were either introduced immediately after nerve
ligation, or 7 days after ligation. A third subset introduced systemic
meloxicam 7 days after ligation. [52] Intrathecal meloxicam
was shown to prevent development of neuropathic pain and spinal
glial activation, but it did not reverse mechanical allodynia or
thermal hyperalgesia. Systemic meloxicam partially reversed existing
allodynia and hyperalgesia. This suggests that spinal COX-2
plays a role in development of neuropathic pain, while peripheral
COX-2 may improve the maintenance of neuropathic pain. [52]
In a subset of chemotherapy-induced neuropathic pain, Yamamoto
et al. evaluated the administration of meloxicam for symptomatic
neuropathy in patients receiving doxorubicin and paclitaxel
for breast cancer. [53] Of the 43 patients in the clinical trial,
15 patients developed neuropathy during paclitaxel and received
10mg meloxicam daily. [53] There was a statically significant reduction
in sensory neuropathy in 5 of the 15 patients, but motor
neuropathy did not improve after 2 months of meloxicam
therapy. [53]
Tolerability
Gastric: Gastric ulcers are a concern with all NSAIDs, and can be doselimiting
side effect to their usage. The pathology behind gastric
ulcers with NSAIDs is related to the inhibition of the biosynthesis
of cytoprotective prostaglandins in the gastric mucosa [28];
specifically, PGE2 and PGI1 protect the mucosa and inhibit acid
secretion in the stomach. As meloxicam is a weak inhibitor of
PGE2 in the rat stomach, it is less of a stimulator of gastric acid
secretion.
Tolerability of meloxicam compared to other NSAIDs has been
extensively evaluated by Zeidler et al. [34] In an observational
cohort of more than 13,000 patients, patients received meloxicam
at doses of 7.5mg or 15mg meloxicam daily to treat osteoarthritis,
rheumatoid arthritis, ankylosing spondylitis, or other
painful inflammatory disorders of the musculoskeletal systemfor
4-12 weeks. General tolerability was rated as “very good” or
“good” for 94% of the patients, but of note, two serious adverse
events: surgery for perforated gastric ulceration in a patient using
meloxicam in conjunction with aspirin and diclofenac, and ileus
in a patient using 45 mg meloxicam daily and prednisolone. [34]
The most common gastrointestinal adverse events were dyspepsia
(0.3%), nausea (0.2%), abdominal pain (0.1%), and diarrhea
(0.1%); however, there was no dose effect seen between the 7.5mg
and 15mg doses. [34]
In the Meloxicam Large-scale International Study Safety Assessment
(MELISSA) trial, a double blind, randomized, controlled,
prospective trial, assessed thetolerability of meloxicam versus diclofenac
in 9323 patients with osteoarthritis. [35] Patients who met inclusion criteria received meloxicam (7.5mg) or diclofenac
(100mg) for 28 days. Overall, patients who received meloxicam
had less GI adverse events (13%) compared to diclofenac (19%),
including dyspepsia, nausea, vomiting, abdominal pain, and diarrhea.
[35] Furthermore, the GI events were not found to be as
severe in patients who were given meloxicam, compared to diclofenac.
[35] Of the patients examined, three patients who received
meloxicam spent a total of 5 days hospitalized due to GI
events, and ten patients who received diclofenac spent a total of
121 days hospitalized for adverse GI events. [35]
Renal: In patients with normal, mild, and moderate renal impairment,
daily dosing of 15mg meloxicam resulted in similar free meloxicam
concentrations in all three groups, suggesting that meloxicam
dose may not need to be adjusted in patients with mild to moderate
renal impairment. [54] A phase 3 multicenter trial involving intravenous
meloxicam administration in patients with renal impairment
for postoperative pain control showed a low incidence of
renal adverse events, and no significant difference in pharmacokinetics
between patients with renal impairment and those without
renal dysfunction. [11] Likewise, in a systemic review conducted
by Asghar et al., evaluating 19 studies for renal and cardiovascular
risk in meloxicam use, meloxicam did not result in an increase
in the odds ratio of renal adverse events, as was seen with most
NSAIDs (excluding ibuprofen). [55] Zeidler et al.’s research, noted
above, described renal adverse reactions in four patients but
did not detail the extent of reactions. [34]
Cardiovascular: In regards to the risk of cardiovascular events with use of
NSAIDs, there is concern as to whether COX selectivity affects
the occurrence of these adverse events. In the review by Asghar
et al., five studies that reported >90 days of meloxicam usage
and exposure did not show any increased risk of myocardial adverse
events, but NSAIDs such as rofecoxib and diclofenac were
found to show increased risk. [55] Meloxicam was found to have
an elevated odds ratio in regards to vascular events compared to
myocardial and renal events; however, of the NSAIDs evaluated,
naproxen had the highest odds ratio of vascular events. [55] In
composite risk of cardiovascular and renal outcomes, meloxicam
was found to have an elevated composite odds ratio, but this was
not related to meloxicam dose. [55] In the study by Zeidler et al.,
no cases of myocardial infarction, hypertension, or cerebrovascular
events were reported. [34]
Hepatobiliary: There are few studies that have directly examined hepatobiliary
adverse events specifically with meloxicam, with the focus rather
on other NSAIDs. In the MELISSA trial noted earlier, serious
adverse hepatobiliary events were seen in five patients in the diclofenac
group, but no such events were observed in the meloxicam
group. [35] Further, statistically significant abnormal ALT
and AST, as well as increases in creatinine and urea levels, were
only seen in the diclofenac group. [35]
Conclusion
Systemic administration of meloxicam is a safe and effective
therapy to treat postoperative pain, and has been shown to improve
postoperative VAS scores, and reduce opioid consumption
and use of rescue analgesia in many of the studies referenced in
this review. Various delivery formulations have been established,
including transdermal, transmucosal, oral, and intravenous. The
relative selectivity of meloxicam for COX-2 may contribute to an
improved tolerability profile, and given its safety profile, can be
considered in individuals with mild to moderate renal or hepatobiliary
impairment. These findings, combined with the faster on
set of analgesia and longer duration of action, make meloxicam
a suitable alternative to traditional NSAIDs during the perioperative
period.
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