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. 2005 Jan 17;144(4):538–550. doi: 10.1038/sj.bjp.0706078

Table 3.

Changes in intestinal permeability following treatment with lumiracoxib and diclofenac

Treatment 51Cr-EDTA excretion in urine (%)
  Single dose Four doses
  30 mg kg−1 3 mg kg−1 10 mg kg−1 30 mg kg−1 100 mg kg−1
Lumiracoxib 2.5±0.2* (n=18) nt 1.8±0.2* (n=12) 4.3±0.4** (n=15) 31.3±3.2** (n=9)
Diclofenac 12.7±1.4** (n=24) 5.0 ±1.1**> (n=12) 12.8±1.5** (n=29) nt nt

Rats were given test compound or vehicle – either in a single dose or once daily for 4 consecutive days. Immediately following the last dose, each rat was administered 5 μCi of 51Cr-EDTA. The level of 51Cr-EDTA was then measured in urine collected over a 24-h period.

*

Results shown are means±s.e.m. (n), where n=number of rats per dose. The % permeability for the vehicle-treated rats was 1.9±0.1 (24) in the single-dose study and 1.59±0.06 (51) in the four-dose group.

**

*P<0.05 vs diclofenac-treated rats; **P<0.05 vs vehicle-treated rats; nt=not tested.