Effects of flunixin meglumine, meloxicam, and firocoxib on the acute-phase proteins in horses following standing castration

Filippo, Paula A. Di; Gobbi, Francielli P.; Lemos, Gabriela B.; Quirino, Célia R.; Martins, Carla B.; Fonseca, Leandro A.

doi:10.1590/1678-5150-PVB-6533

ABSTRACT:

Excessive infection and inflammation are the most common complications associated with castration. The objective of this study was to compare the efficacy of flunixin meglumine (FM), meloxicam (MX), or firocoxib (FX) for inflammation control after castration in horses using acute-phase proteins (APP) as markers of inflammation. Thirty healthy, unbroken, mixed-breed horses (body weight 358.62±45.57kg and age 4.99±2.63 years) were randomly (n=10 animals/group) allocated to receive one of three different post-castration anti-inflammatory medicines: Group 1 (FM 1.1mg/kg bwt, IV, s.i.d for 5 days); Group 2 (MX 0.6mg/kg bwt, IV, s.i.d for 5 days); and Group 3 (FX 0.1mg/kg bwt, IV, s.i.d for 5 days). All horses were castrated in standing position, using the open technique. Serum and peritoneal APP concentrations were measured by sodium dodecyl sulfate (SDS) polyacrylamide gel electrophoresis (PAGE) and determined before castration (0), and 3, 5, 24, 48, 72, 120 and 168 hours after castration. The results were submitted to analysis of variance using the SAS statistical program, and means were compared by the Student-Newman-Keuls test (p<0.05). Three animals from the MX group developed hyperthermia (with rectal temperatures of 39.8, 39.3 and 38.9°C on day 4, 5 and 6, respectively) and showed local clinical signs of inflammation (inguinal and excessive scrotal edema) and reluctance to walk, as well as a rigid gait of the hind limbs. The same complications were observed in one FX horse. No complications were observed among the FM animals. The castration resulted in significant changes in serum and peritoneal values of total proteins, ceruloplasmin (Cp), transferrin (Tf), albumin (Alb), haptoglobin (Hp) and α1-acid glycoprotein (Gp) in animals of all experimental groups. However, the animals of the MX and FX groups presented more intense acute phase response compared to the animals of the FM group. Changes in the APP were associated with the surgical trauma of castration, but the differences between groups were associated with the ability of the nonsteroidal anti-inflammatory drug to control the inflammation. In conclusion, and based on the findings of acute phase proteins, flunixin is more efficient to control the magnitude of inflammation following castration as compared to meloxicam and firocoxib.

INDEX TERMS:
Flunixin meglumine; meloxicam; firocoxib; proteins; horses; castration; equine; orchiectomy; inflammation; nonsteroidal anti-inflammatory agents; NSAIDs; SDS-polyacrylamide gel electrophoresis

[1] *Corresponding author: pdf@uenf.br

Total protein (g/dL)
Hours	Serum			Peritoneal fluid
Hours	Flunixin	Meloxican	Firocoxib	Flunixin	Meloxican	Firocoxib
0	7.4±0.7^a	6.7±0.9^a	7.1±0.4^a	0.8±0.3^b	0.7±0.2^b	0.8±0.5^b
3	6.2±1.2^ab	6.0±0.3^ab	6.8±0.7^ab	0.9±0.4^b	0.7±20.4^b	1.6±1.1^b
5	7.4±0.6^Aa	6.1±0.4^Bab	7.0±0.4^Aa	2.0±1.0^Aa	1.6±1.4^Ba	2.1±1.8^Aa
24	7.1±1.6^Aa	5.7±1.9^Bab	6.5±2.3^Aab	3.1±1.5^Aa	1.7±0.7^Ba	2.5 ±1.6^Aa
48	5.7±0.7^Ab	5.4±1.1^Bb	6.1±0.7^Ab	2.5±0.9 ^Aa	2.0±0.7^Ba	3.0±1.5^Aa
72	5.7±1.9^Ab	5.0±1.2^Bb	6.1±1.5^Ab	2.4±1.0^Aa	1.9±0.5^Ba	2.4±1.2^Aa
120	6.5±1.7^Aab	5.2±1.3^Bb	6.1±0.6^Ab	2.2± 0.4^Aa	1.6±0.3^Ba	2.6±0.8 ^Aa
168	6.4±1.6^Aab	5.9±1.0^Bab	6.7±1.3^Aab	2.3±0.7^Aa	1.6±0.4^Ba	2.4±1.1^Aa
Ceruloplasmin (mg/dL)
0	33.2±26.1	27.7±11.1	25.7±21.2	2.5±1.2^b	3.7±3.1^b	2.5±1.5^b
3	24.7±15.2^B	43.5±25.1^A	20.7±9.1^B	2.0±0.8^Bb	4.1±2.7^Ab	2.2±0.3^Bb
5	31.3±21.4^B	52.7±20.2^A	21.9±7.1^B	2.5±1.3^Bb	3.9±1.7^Ab	2.4±1.2^Bb
24	23.3±17.9^B	56.9±28.6^A	33.0±8.7^B	3.0±1.9^Bab	5.2±3.8^Aab	4.0 ±3.7^Bab
48	27.0±14.9	28.3±13.2	27.5±19.1	3.2±1.6 ^Bab	7.6±2.9^Aab	3.9±2.6^Bab
72	31.1±21.5^B	45.4±11.9^A	29.8±21.8^B	4.4±3.2^Ba	7.7±1.7^Aa	4.2± 2.1^Ba
120	34.7±10.2^B	53.2±25.0^A	37.3±28.8^B	3.9± 1.8^Ba	7.0±2.5^Aa	4.5±2.8^Ba
168	33.6±13.2^B	45.2±25.3^A	26.2±17.3^B	3.6±2 ^Bab	6.2±3.1^Aab	2.7±0.7 ^Bab
Transferrin (mg/dL)
0	443.8±189.3	523.2±141.9	573.2±161.5	66.9±52.7^b	60.3±32.1^b	68.7±34.3^b
3	356.2±269.0	465.5±147.0	525.7±166.1	70.4±36.3^Ab	52.1±30.6^Bb	58.0±39.1^ABb
5	424.2±140.9	556.4±163.6	501.1±225.4	135.7±55.3^Aa	65.8±28.6 ^Bab	113.6±81.8^Aab
24	454.3±96.7	506.5±183.4	584.9±151.2	128.1±90.7^Aa	70.0±7.3^Ba	154.1±125.7^Aa
48	541.1±143.2	446.7±132.8	500.5±139.4	147.2±103.7^Aa	97.9±52.9 ^Ba	130.6± 63.4^Aa
72	384.7±150.6	458.3±169.7	505.1±135.7	140.4±60.5^Ba	140.9±91^Ba	215.3±130.9^Aa
120	489.4±147.7	511.8±198.7	529.2±132.4	96.9±52.3^Ba	102.1±53.7^Ba	206.8±125.8^Aa
168	531.7±115.9	382.6±148.3	532.2±144.0	136.5±70.1^Ba	115.1±39.7^Ba	174.6±114.4^Aa

Albumin (mg/dL)
Hours	Serum			Peritoneal fluid
Hours	Flunixin	Meloxican	Firocoxib	Flunixin	Meloxican	Firocoxib
0	2708.1±670.7	2620.1±253.2	3052.3±301.4	594.3±256.6^b	419.7±401.9^b	615.8±252.1^b
3	2625.4±1066	2477.8±445.2	2563.5±857.9	656.1±419.3^b	510.1±303.6^b	622.7±388.1^b
5	2748.0±1162.1	2459.3±451.7	2145.7±832.6	1009.2±423.1^a	963.6±628.3^a	1030.6±623±5^a
24	2978.3±782.1	2455.7±621.1	2484.8±583.1	853.7±401.4^ab	983.2±384.6^a	1207.9±582.9^a
48	2742.1±434.2	2173.9±762.5	2244.1±840.6	1237.3±804.3^a	1252.9±395.9^a	1274.1±380.8^a
72	2481.6±797.4	2314.6±723.3	2462.2±263.4	1025.2±148.6^a	1256.1±302.8^a	1392.9±429.2^a
120	2466.3±448.1	2394.4±258.3	2121.7±701.5	791.9±203.9^ab	998.9±350.9^a	1181.6±401.4^a
168	2513.4±428.9	2232.6±652.3	2874.7±429.7	1005.1±585.2^a	902.6±326.4^a	1329.4±481.0^a
α_1-Acid Glycoprotein (mg/dL)
0	57.2±23.7	40.2±45.3^b	38.7±16.7^b	9.5±8.2^b	12.5± 12.2^b	9.7±15.3^b
3	48.5±25.0	51.8±12.2^a	48.0±18.3^a	25.0±23.1^Aa	11.6±8.8^Bb	11.4±15.0^Bab
5	37.5±29.3	51.5±17.8^a	42.8±24.7^a	23.1±17.2^Aa	15.1±15.4^Ba	13.7±16.9^Bab
24	45.6±22.4	68.9±22.3^a	49.7±16.1^a	29.8±19.2^Aa	14.6±11.2^Ba	23.9±21.1^Ba
48	46.7±16.9	51.9±20.6^a	52.1±32.2^a	29.4±25.7^Aa	23.3±18.^5Ba	23.5±11.0^Ba
72	39.4±21.7^B	55.4±35.7^Aa	65.8±26.5^Aa	32.8±12.1^Aa	20.2± 11.7^Ba	23.6±7.4^Bab
120	50.6±26.4^B	68.4±12.6^Aa	61.0±11.6^Aa	37.7±9.4^Aa	22.0±18.9^Ba	31.1±23.1^Ba
168	38.8±12.6^B	54.9±30.0^Aa	62.6±21.1^Aa	18.9±11.2^a	14.4 ±8.2^ab	14.5±11.7^ab
Haptoglobin (mg/dl)
0	159.2±47.7^b	136.7±59.9^b	123.1±44.9^b	19.2± 12.6^b	23.9±19.5^b	15.7±13.5^b
3	186.3±91.9^ab	147.1±74.8^ab	116.9±45.4^ab	28.3±14.5^b	27.8±28.6^b	19.3±11.1^b
5	168.2±89.1^ab	173.2±121.1^ab	132.4±55.9^ab	42.3±12.2^b	37.1±23.2^b	33.4±28.6^b
24	216.7±88.9^a	181.2±52.6^a	170.7±81.2^a	65.2±74.1^b	60.1±46.3^b	66.9±57.5^ab
48	263.1±165.6^a	186.5±77.1^a	276.9 ±170.4^a	106.8±102.9^a	91.5±62.5^a	91.0±39.0^a
72	198.6±133.7^a	250.2±134.5^a	214.3±82.1^a	85.4±79.3^Ba	124.2±63.8^Aa	101.4±75.4^ABa
120	240.8±110.2^a	251.5±81.2^a	229.1± 99.3^a	57.7±43.1^Bb	75.7±36.1^Ab	70.2±48.9^ABb
168	199.8±56.7^a	194.1±75.3^a	192.7±90.6^a	51.2±38.1^b	51.2± 27.9^b	42.5±54.0^b

Brasil

Brasil

Effects of flunixin meglumine, meloxicam, and firocoxib on the acute-phase proteins in horses following standing castration

Efeitos do flunixin meglumine, meloxicam e firocoxib na concentração de proteínas da fase aguda após em equinos após castração

ABSTRACT: