二氟沙星对实验性感染猪支原体性肺炎及链球菌病的药效学研究

以试管两倍稀释法测得二氟沙星对猪肺炎支原体（ Ｆ１６ 株）和兰氏 Ｃ 群类马链球菌（ Ｃ５５ １ ２０ ）的最小抑菌浓度分别是０１６ｍ ｇ／ Ｌ及 １６ｍ ｇ／ Ｌ。肌注给药对猪支原体性肺炎及链球菌病的实验性治疗结果表明,低、中、高剂量二氟沙星组（２５、５、１０ｍ ｇ／ｋｇ）及蒽诺沙星组（２５ｍ ｇ／ｋｇ）用药 ５ 天（每隔 １２ 小时给药一次）对猪支原体性肺炎的治愈率分别是 ８０％ 、９０％ 、１００％ 及９０％ ;而支原体感染对照组的自愈率为１０％ 。低、中、高剂量二氟沙星组及蒽诺沙星组（２５ｍ ｇ／ｋｇ）用药 ４ 天（每隔 １２ 小时给药一次）对猪链球菌病的治愈率分别是 ５０％ 、８０％ 、８０％ 及 ８０％ ,而链球菌感染对照组的死亡率为 ５０％ 。     

沙拉沙星对实验性感染猪链球菌病及大肠杆菌病的药效学

为兽医临床合理应用沙拉星（Ｓarafloxacin）提供理论依据,就其对实验性感染猪链球菌 病及大肠杆菌病的药效学进行了研究。以试管２倍稀释法测得沙拉沙星对兰氏Ｃ群类马链球菌（Ｃ５５１２０）和猪大肠杆菌（Ｏ５５）的最小抑菌浓度（ＭＩＣ）分别是０．８mg/Ｌ及０．０５mg/Ｌ。肌注给药对猪链球菌病和大肠杆菌病的试验性治疗结果不明,低、中 高剂量沙拉沙星组２．５、５、１０mg/kg）及环丙沙星组（５mg/kg）用药５d（每隔１２     

普鲁卡因青霉素－硫酸双氢链霉素混悬剂对猪链球菌病的临床药效观察

本研究报道了普鲁卡因青霉素－硫酸双氢链霉素混悬剂对试验性感染猪链球菌病的临床药效学。以试管2倍稀释法测得兰氏C群类马链球菌对青霉素、恩诺沙星的最小抑菌浓度(MIC)分别是0.0313、0.5 mg/L。肌注给药对猪链球菌病的试验性治疗结果表明,低、中、高剂量普鲁卡因青霉素－硫酸双氢链霉素混悬剂组(0.05、0.1、0.2 mL/kg体重,每毫升混悬剂含普鲁卡因青霉素、硫酸双氢链霉素200000 IU和250000 IU)及恩诺沙星组(2.5 mg/kg体重)用药3 d,对猪链球菌病的治愈率分别是60%、80%、90%及60%,而链球菌感染对照的死亡率为70%。     

环丙沙星对实验性猪支原体性肺炎的药效学研究

测定环丙沙星及对照药物对猪肺炎支原体的最小抑菌浓度，其中环丙沙星的抗支原体活性最强，最小抑菌浓度为0．01μg/ml。通过给18头健康猪气管内接种含有猪肺炎支原体的病肺悬液，复制具有典型症状的猪支原体性肺炎疾病模型，并进行环丙沙星2．5、5．0mg/kg肌注给药对实验性猪支原体性肺炎的疗效实验及血浆药物浓度监测，两组治愈率分别为83．3％（5／6）和100％（6／6）。治疗组多剂量给药期间，第1、3、5、7、9次给药后0．5及6h的血浆药物浓度，在2．5mg/kg剂量组平均为0．41μg/ml和0．17μg/ml,5.0mg/kg剂量组平均为0．71μg/ml和0．28μg/ml。两剂量组环丙沙星均无蓄积作用。     

乙基环丙沙星对实验性感染猪链球菌病及水肿病的药效学研究

本文报道以国内新近研制的畜禽专用氟喹诺酮类抗菌药──乙基环丙沙星（Ｅｎｒｏｆ－ｌｏｘａｃｉｎ），进行对实验性感染猪链球菌病及水肿病的药效学研究（２３０头猪）。试管两倍稀释法测得乙基环丙沙星对兰氏Ｃ群类马链球菌（Ｃ＿（５５１２０））和猪大肠杆菌（Ｏ＿（５４））的最小抑菌浓度（ＭＩＣ）分别是０．８及０．０５μｇ／ｍｌ。肌注给药对猪链球菌病和水肿病的实验性治疗结果表明，乙基环丙沙星低、中、高剂量组（分别为１．２５、２．５、１０ｍｇ／ｋｇ）用药６０（每天２次）对猪链球病的治愈率分别是５０％、９５％及９５％，而链球菌感染对照组的死亡率为７０％；乙基环丙沙星低、中、高剂量组（分别为１．２５、２．５、１０ｍｇ／ｋｇ）用药３ｄ（每隔１２ｈ给药一次）对猪水肿病的治愈率分别是８５％、９０％及９０％；而大肠杆菌感染对照组的死亡率为９０％。     

氟甲喹可溶性粉对实验性鸡大肠杆菌病的药效学研究

以试管肉汤两倍稀释法测得氟甲喹、恩诺沙星、强力霉素对鸡大肠杆菌的MIC分别为0.5、0.025及32mg/l,按2.5、5和10mg/kg的氟甲喹及5mg/kg的恩诺沙星分别给实验性鸡大肠杆菌病患鸡给药,每12小时给药1次,共3天。氟甲喹低、中、高剂量组及恩诺沙星组对鸡大肠杆菌病的治愈率分别为76.7%、83.3%、86.7%及93.3%,而感染对照鸡的死亡率为43.3%。氟甲喹中、高剂量组及恩诺沙星组的增重效果极显著高于感染对照鸡(P<0.01)。     

乙基环丙沙星对实验性感染猪链球菌病及水肿病的药效学研究

本文报道以国内新近研制的畜禽专用氟喹诺酮类抗菌药－－乙基环丙沙星（Ｅｎｒｏｆ－ｌｏｘａｃｉｎ），进行对实验性感染猪链球菌病及水肿病的药效学研究（２３０头猪）。试管两倍稀释法测得乙基环丙沙星对兰氏Ｃ群类马链球菌（Ｃ５５１２０）和猪大肠杆菌（Ｏ５４）的最小抑菌浓度（ＭＩＣ）分别是０．８及０．０５ｕｇ／ｍｌ。肌注给药对猪链球菌病和水肿病的实验性治疗结果表明，乙基环丙沙星低、中、高剂量组（分别为１．２５、     

单诺沙星对鸡败血支原体与大肠杆菌合并感染的药效学研究

采用试管二倍稀释法测得单诺沙星及其对照药物恩诺沙星、泰乐菌素对鸡败血支原体（MG）的最低抑菌浓度分别为0．0625、0.125、0.5mg/L。试验鸡每只左右气囊分别接种MG S6株菌液0.75ml、滴鼻约0.3ml，同时腹腔注射大肠杆菌菌液0.3ml,人工诱发鸡败血支原体与大肠杆菌合并感染的疾病模型。25、50、100mg/L的单诺沙星、500mg／L的恩诺沙星和500mg/L的泰乐菌素连续饮水5d给药，对人工合并感染鸡败血支原体与大肠杆菌病的治愈率分别为93.3%、96.6%、96.6%、93.3%、86.6%，而感染对照组的死亡率为23.3％。单诺沙星及其对照药物组的增重率显著高于感染对照组，并能极显著的降低感染鸡的死亡率、抗体反应阳性率、气囊损伤率及病原再分离率。     

达氟沙星对鸡毒支原体的临床疗效试验

试管内抑菌试验测得达氟沙星，氧氟沙星对鸡毒支原体的最小抑菌浓度（MIC）分别为0．048μg/ml，0．098μg/ml。人式感染鸡毒支原体的鸡24小时后，100、50、25ppm的达氟沙星、50ppm的氧氟沙星连续饮水5天给药，死亡率分别为0、0、3．3％、6．7％，而阳性对照组的死亡率为33％。达氟沙星及对照药物能显著降低鸡的死亡率，气囊损伤率及体内抗体阳性率。     

头孢噻呋混悬剂对猪链球菌Ⅱ型小鼠模型的治疗试验

建立小鼠链球菌病的模型,评价头孢噻呋混悬剂的疗效。选用小白鼠人工感染猪链球菌Ⅱ型建立疾病模型,并应用不同剂量头孢噻呋混悬剂进行治疗试验。结果表明,链球菌Ⅱ型感染的小鼠模型能表现出典型的临床症状及病理变化,且具有较好的重复性。5和10mg/kg组治愈率均为100%,2mg/kg组治愈率为70%。因此,头孢噻呋混悬剂作为注射剂治疗小鼠猪链球菌Ⅱ型感染以剂量5mg/kg为佳。     

Evaluation of tiamulin for treatment of mycoplasmal pneumonia in swine

During 3 trials, using affected pigs of various ages, tiamulin was evaluated for treatment of experimentally induced mycoplasmal pneumonia. Pneumonia was induced in respiratory tract disease-free swine by intratracheal inoculation of a lung homogenate containing Mycoplasma hyopneumoniae. Eleven days after inoculation, when more than 20% of pigs were coughing, pigs were allotted to 3 or 4 groups (n = 8 pigs each) and were given regimens of no medication or 60 mg, 120 mg, or 180 mg of tiamulin/L of drinking water for 10 days. Twenty-one days after cessation of medication, pigs were euthanatized and then were necropsied. Results obtained from the 3 trials did not indicate significant difference among treatment groups in severity of macroscopic or microscopic lesions induced by M hyopneumoniae or in detection of M hyopneumoniae by use of immunofluorescent technique. Clinical evaluations, daily gain, and feed efficiency did not differ significantly among treatment groups. In this study, tiamulin administration did not have beneficial effects in swine with mycoplasmal pneumonia.     

壮观霉素治疗猪支原体肺炎试验

本试验用壮观霉素,通过控制试验和临床治疗对人工感染和自然感染猪支原体肺炎的病猪进行治疗试验。控制试验分三种不同剂组,治疗１个疗程。１０毫克／千克体重的治愈率为７５％,治疗有效率为１００％。２０毫克／千克体重和３０毫克／千克体重的治愈率均为９１．７％,治疗有效率为１００％。     

Evaluation of tulathromycin for the treatment of pneumonia following experimental infection of swine with Mycoplasma hyopneumoniae

Tulathromycin was evaluated in the treatment of pneumonia in weaned pigs inoculated intranasally with Mycoplasma hyopneumoniae. Five days postchallenge, the pigs were randomized to treatment with a single IM administration of saline, a single IM administration of tulathromycin (2.5 mg/kg; day 0), or three IM administrations of enrofloxacin (5.0 mg/kg; days 0, 1, 2). Pigs were necropsied on day 12 or 13. Unchallenged controls remained healthy with no lung pathology. Compared with saline, coughing, mean lung lesion score, and proportional lung weight were significantly reduced and weight gain was significantly greater for tulathromycin-treated pigs (P < .05). Compared with enrofloxacin, there were no significant differences in proportional lung weight or weight gains, but coughing and lung lesion scores were greater for tulathromycin-treated pigs (P < .05). Tulathromycin was effective in the treatment of pneumonia following experimental infection with M. hyopneumoniae.     

沙拉沙星对实验性猪链球菌病及猪水肿病的药效学

将兽医专用氟喹诺酮类药物沙拉沙星以不同治疗方案分别对实验性猪链球菌病和猪水肿病进行药效学研究。在每天总剂量相同的情况下 ,每天 1次与每天 2次给药取得了较好而相似的疗效 (P>0 .0 5 ) :对猪链球菌病 ,每天总剂量为 10 m g/ kg时 ,肌注给药的治愈率分别为 10 0 %和 90 %,但在迅速改善临床症状方面 ,每天 1次给药优于每天 2次(P<0 .0 5 ) ;对猪水肿病 ,每天总剂量为 5 mg/ kg时 ,肌注给药的治愈率均为 10 0 %。结果表明 ,在总剂量相同时 ,以大剂量、长间隔与以较小剂量、短间隔治疗实验性猪链球菌病与猪水肿病 ,均取得相当的疗效。     

Efficacy of difloxacin in calves experimentally infected with Mannheimia haemolytica

OBJECTIVE: To determine the efficacy of difloxacin, a novel fluoroquinolone antibiotic, in calves experimentally infected with Mannheimia haemolytica (formerly Pasteurella haemolytica). ANIMALS: Seventy-two 3-month-old Holstein calves. PROCEDURES: Calves were inoculated with M haemolytica intratracheally; after they developed clinical signs of pneumonic pasteurellosis, they were randomly assigned to 1 of 6 groups (n = 12/group). Calves in each group were treated with 10% difloxacin (2.5 or 5 mg/kg of body weight), 5% difloxacin (2.5 or 5 mg/kg), enrofloxacin (5 mg/kg), or saline (0.9% NaCl) solution (control group), once daily for 5 days, and clinical signs were scored daily. On day 15, calves were euthanatized, and the percentage of diseased lung tissue was calculated. Swab specimens of the lungs were submitted for bacterial culture. RESULTS: Mortality rate and percentage of diseased lung tissue were significantly higher and cure rate and average daily gain were significantly lower for control calves, compared with calves in the treatment groups; however, no significant differences were found among treatment groups. Mannheimia haemolytica was isolated from the lungs of 10 control calves and from at least 2 calves in each of the treatment groups. CONCLUSIONS AND CLINICAL RELEVANCE: Results suggest that difloxacin and enrofloxacin were equally effective for treatment of calves with experimentally induced pneumonic pasteurellosis. However, treatment of infected calves with difloxacin or enrofloxacin may not eliminate the organism.     

Efficacy of in-feed medication with tylosin for the treatment and control of Mycoplasma hyopneumoniae infections

The efficacy of in-feed medication with tylosin for the treatment of enzootic pneumonia was examined in an experimental Mycoplasma hyopneumoniae infection model. One group of 10 conventional M. hyopneumoniae-free pigs was inoculated intratracheally with a highly virulent field isolate of M. hyopneumoniae; a second group of 10 pigs was inoculated in the same way and after 12 days was given tylosin at 100 mg/kg feed for 21 days; a third group of 10 pigs was inoculated with sterile culture medium, and these pigs were not given tylosin. The pigs were examined daily for clinical signs and each pig was given a respiratory disease score. Thirty-three days after they had been infected the pigs were euthanased, the lung lesions were quantified and samples of lung were processed for immunofluorescence testing for M. hyopneumoniae. The mean (sd) respiratory disease and lung lesion scores were significantly higher (P<0.05) in both the infected groups than in the uninfected group. Between 23 and 33 days after infection the mean respiratory disease score of the pigs treated with tylosin was 0.54 (0.22), significantly (P<0.05) lower than that of the infected pigs which were left untreated, 1.54 (0.46); similarly, their average lung lesion score, 1.72 (1.20), was significantly lower than that of the untreated pigs, 5.27 (3.85).     

In vitro evaluation of various quinolone antibacterial agents against veterinary mycoplasmas and porcine respiratory bacterial pathogens

The in vitro activities of 12 quinolones and four antibiotics were determined against 15 veterinary mycoplasmal species and four species of bacteria commonly involved in respiratory infections in pigs. The newer quinolones were markedly more active in vitro against a wide range of mycoplasmas than nalidixic acid and the earlier quinolones. Against Mycoplasma hyopneumoniae ciprofloxacin was the most active quinolone with a geometric mean minimal inhibitory concentration (MIC) against 16 strains of 0.01 microgram ml-1 compared with 0.04 microgram ml-1 for tiamulin, 0.06 microgram ml-1 for tylosin, 0.17 microgram ml-1 for oxytetracycline and 0.23 microgram ml-1 for gentamicin. M hyosynoviae was less sensitive to the quinolones with mean MICs of 0.6 microgram ml-1 for ofloxacin and 0.7 microgram ml-1 for ciprofloxacin compared with 0.034 microgram ml-1, or less, for tiamulin. Norfloxacin and its 6-chloro analogue were both mycoplasmacidal in vitro at five or 10 times their MICs against M hyopneumoniae UCD4. Tiamulin was mycoplasmastatic. The quinolones were also active against porcine Bordetella bronchiseptica and Pasteurella multocida strains and Haemophilus species. Ciprofloxacin was the most active quinolone with mean MICs of 0.58 microgram ml-1 against B bronchiseptica (nine strains), 0.026 microgram ml-1 against P multocida (five strains) and 0.01 microgram ml-1, or less, against Haemophilus pleuropneumoniae (nine strains) and H parasuis (two strains) compared with mean MICs of from 0.5 microgram ml-1 to 64 micrograms ml-1, or more, for the antibiotics. This combination of excellent mycoplasmacidal activity against M hyopneumoniae and good antibacterial activity, suggests that the quinolones have great potential for treating respiratory infections in pigs, including enzootic pneumonia.     

Protective effects of an oral microencapsulated Mycoplasma hyopneumoniae vaccine against experimental infection in pigs.

Oral microencapsulated Mycoplasma hyopneumoniae vaccines were tested for their ability to prevent mycoplasmal pneumonia in pigs. Eighteen four-week-old specific pathogen free pigs were divided into six groups of three. Each pig of groups 1 to 4 was inoculated intramuscularly with formalin-inactivated M hyopneumoniae in adjuvant and boosted orally 14 days later with four different microencapsulated vaccine microspheres. Group 5 was used as a positive control. All 15 pigs of groups 1 to 5 were challenged at 28 days after the first vaccination by an intratracheal inoculation of pneumonic lung suspension. The three pigs of group 6 were used as a negative control. All four vaccinated groups showed some protection when challenged, but the protection was more solid in pigs boosted with vaccine D (group 4) which contained less porcine serum in the microsphere. The study indicates that oral vaccination with M hyopneumoniae could play a role in prevention and eradication of mycoplasmal pneumonia in the pig.