Parecoxib sodium is a white or almost white crystalline powder with the chemical name sodium
N-[4-(5-methyl-3-phenyl-1,2-oxazol-4-yl)benzenesulfonyl]propanecarboximidate which is freely soluble in water,
methanol, N,N-dimethylformamide. Parecoxib sodium is an amide prodrug of the cyclooxygenase II (COX-2) selective,
non-steroidal anti-inflammatory drug (NSAID) valdecoxib, with anti-inflammatory, analgesic, and antipyretic
activities. The structure of parecoxib sodium is showed in figure 1.
Fig. 1 Structure of parecoxib sodium
Application in the treatment of postoperative pain
Mechanism of action
Parecoxib sodium is approved through much of Europe for short term postoperative pain control.
Upon intravenous or intramuscular administration, parecoxib is hydrolyzed by hepatic carboxyesterases to its active
form, valdecoxib. Valdecoxib selectively binds to and inhibits COX-2. This prevents the conversion of arachidonic
acid into prostaglandins, which are involved in the regulation of pain, inflammation, and fever. This NSAID does not
inhibit COX-1 at therapeutic concentrations and, therefore, does not interfere with blood coagulation. Figure 2
shows the schematic of NSAID mechanism of action.
Fig. 2 Schematic of NSAID mechanism of action
COX-1, a constitutive enzyme, plays a major role in the release of PG to regulate hemostasis. COX-2, an inducible
enzyme, releases PG that mediates pain, inflammation, and fever. Nonselective NSAIDs inhibit both forms of COX [1].
When given at the recommended doses for management of acute pain, the onset of analgesia was 7–14 minutes and
reached a peak effect within 2 hours. After a single dose, the duration of analgesia was dose and clinical pain
model dependent and ranged from 6 to greater than 24 hours.
Comparation of parecoxib sodium between morphine in analgesia
A total of 32 patients, including 26 males and 6 females, were enrolled. Eighteen patients received (intravenous) IV
parecoxib sodium as an analgesic whereas 14 patients received IV morphine. Patients with a bone fracture were equal
in number for both groups. Table 1 shows result [2].
Study drug
Time (minutes)
Mean (SD)
Estimated marginal mean (95% CI)
P value
Parecoxib sodium
0
7.8 (1.3)
7.09, 8.41
5
5.7 (2.2)
4.77, 6.71
15
4.7 (2.3)
3.66, 5.64
30
3.9 (2.3)
2.93, 4.77
Morphine
0
7.1 (1.3)
6.38, 7.88
0.095
5
4.5 (1.7)
3.44, 5.65
15
3.1 (1.6)
1.94, 4.19
30
2.0 (1.4)
0.99, 3.09
Table 1. Comparison of mean numeric rating scale (NRS) between patients treated with IV
parecoxib sodium or IV
morphine based on time (SD = standard deviation, CI = confidence interval, p value = repeated measure analysis of
variance)
The mean numeric rating scale (NRS) for patients that were treated with IV morphine were 7.1 at 0 minutes, 4.5 at 5
minutes, 3.1 at 15 minutes, and 2.0 at 30 minutes. Mean NRS for patients who received IV parecoxib were 7.8 at 0
minutes, 5.7 at 5 minutes, 4.7 at 15 minutes, and 3.9 at 30 minutes.
There was non-significant trend toward superiority of IV morphine over IV parecoxib. Looking at its effectiveness
and the lack of opioid-related side-effects, the usage of IV parecoxib sodium may be extended further to a variety
of cases in the emergency department.
Alfa Chemistry offers high quality of parecoxib sodium which meets the CP & EP standards. Please feel free to contact us for APIs or technical services.
References
Raymond Sinatra. Role of COX-2 Inhibitors in the Evolution of Acute Pain Management. The Journal of Pain and
Symptom Management, 2002,24(1): S18-S27.
Kamarul Aryffin Baharuddin, Nik Hisamuddin NA Rahman, et al. Intravenous parecoxib sodium as an analgesic
alternative to morphine in acute trauma pain in the emergency department. International Journal of Emergency
Medicine, 7, 2 (2014).
