Sildenafil Citrate

枸橼酸西地那非
  • 文章类型: Journal Article
    本研究旨在开发一种基于微乳液(ME)的含有柠檬酸西地那非(SC)-ME的皮肤递送平台,并评估其体外皮肤渗透性。
    使用伪三元相图和具有两个水平的三个变量的全阶乘设计来制备精确的ME。在设计阶段之后,合适的油比例,水,选择表面活性剂(S)和助表面活性剂(CS)的混合物来制备各种SC-ME制剂。分析了这些SC-ME的稳定性,液滴大小,体外SC释放,皮肤渗透性,和粘度特性。
    ME样品的液滴尺寸范围为6.24至32.65nm,粘度在114到239cps之间。释放曲线表明26-60%的SC在24小时内从不同的SC-ME释放。所有ME制剂都显着提高了通过大鼠皮肤的渗透系数(P)。具体来说,SC-ME7中的通量(Jss)增加了约117倍(Jss=0.0235mg/cm2。h)与对照样品(0.0002mg/cm2。h).
    研究得出的结论是,ME中水或油相与S/CS混合物的比例显着影响了物理化学特性和渗透参数。选定的ME改善了渗透系数和通过大鼠皮肤的渗透速率。通过和进入深皮肤层的增强的药物递送是理想的真皮ME的关键属性。这些发现表明,MEs可以作为SC和类似药物的有效透皮给药系统。然而,需要体内试验和临床研究来确认MEs的治疗效果.
    UNASSIGNED: This study aimed to develop a microemulsion (ME)-based skin delivery platform containing sildenafil citrate (SC)-ME and evaluate its in vitro skin permeability.
    UNASSIGNED: Accurate MEs were prepared using pseudo-ternary phase diagrams and a full factorial design with three variables at two levels. After the design phase, suitable ratios of oil, water, and a mixture of surfactant (S) and cosurfactant (CS) were selected to prepare various SC-ME formulations. These SC-MEs were analyzed for stability, droplet size, in vitro SC release, skin permeability, and viscosity properties.
    UNASSIGNED: The droplet size of the ME samples ranged from 6.24 to 32.65 nm, with viscosities between 114 to 239 cps. Release profiles indicated that 26 to 60% of SC was released from the different SC-MEs within 24 hours. All ME formulations significantly enhanced the permeability coefficient (P) through rat skin. Specifically, the flux (Jss) in SC-ME7 increased by approximately 117 times (Jss = 0.0235 mg/cm2.h) compared to the control sample (0.0002 mg/cm2.h).
    UNASSIGNED: The study concluded that the proportions of the water or oil phase and the S/CS mixture in the MEs significantly influenced the physicochemical characteristics and permeation parameters. The selected MEs improved both the permeability coefficient and the rate of permeation through rat skin. The enhanced drug delivery through and into deep skin layers is a key attribute of an ideal dermal ME. These findings suggest that MEs could serve as effective transdermal delivery systems for SC and similar drugs. However, in vivo assays and clinical research are needed to confirm the therapeutic efficacy of MEs.
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  • 文章类型: Case Reports
    背景:阴茎异常勃起被定义为勃起持续4小时以上而没有性刺激。阴茎异常勃起的原因有很多,但目前还没有关于西地那非诱发犬阴茎异常勃起的报道。在人类医学中,没有西地那非引起阴茎异常勃起的上市前报告,但上市后的监测表明,这是罕见的。在狗的肺动脉高压的情况下,西地那非是缓解症状的首选一线药物。
    方法:一只11岁的男性马耳他犬,出现呼吸急促和咳嗽,被诊断为黏液性二尖瓣疾病,美国兽医内科学院(ACVIM)C阶段,并接受了医学治疗。确诊18个月后,左心疾病导致严重肺动脉高压。诊断后20个月,发生胸腔积液,和西地那非(每天2次2mg/kg)加入现有的治疗。两周后,呼吸困难复发,确认胸腔积液复发,西地那非每天三次增加到2mg/kg。一天后,患者出现持续性勃起和阴茎疼痛。建议进行阴茎截肢和尿道造口术,但遭到拒绝;因此,提供镇痛和姑息治疗.患者在首次就诊22个月后死于急性呼吸困难,在死亡时没有特定的阴茎异常勃起复发。
    结论:据我们所知,这是西地那非诱导肺动脉高压犬阴茎异常勃起的首次报道。
    BACKGROUND: Priapism is defined as erection that lasts for more than 4 h without sexual stimulation. There are various causes of priapism, but there are no reports of sildenafil-induced priapism in dogs. In human medicine, there were no pre-marketing reports of priapism caused by sildenafil, but post-marketing surveillance has shown that it is rare. In cases of pulmonary hypertension in dogs, sildenafil is the first-line drug of choice for symptomatic relief.
    METHODS: An 11-year-old neutered male Maltese dog that presented with tachypnea and cough was diagnosed with myxomatous mitral valve disease, American College of Veterinary Internal Medicine (ACVIM) stage C, and was treated medically. Eighteen months after the diagnosis, severe pulmonary hypertension occurred due to left heart disease. At 20 months postdiagnosis, pleural effusion occurred, and sildenafil (2 mg/kg twice daily) was added to the existing treatment. Two weeks later, the dyspnea recurred, confirming pleural fluid recurrence, and sildenafil was increased to 2 mg/kg thrice daily. One day later, the patient developed persistent erections and penile pain. Penile amputation and urethrostomy were recommended but were refused; therefore, analgesia and palliative care were provided. The patient died of acute dyspnea 22 months after the first presentation, with no specific priapism recurrence at the time of death.
    CONCLUSIONS: To the best of our knowledge, this is the first report of sildenafil-induced priapism in a dog with pulmonary hypertension.
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  • 文章类型: Case Reports
    具有嗜酸性粒细胞增多和全身症状(DRESS)综合征和史蒂文斯-约翰逊综合征毒性表皮坏死松解症(SJS-TEN)的药物反应是对外源性药物的异常细胞毒性免疫反应的反应性实体。虽然它们通常被认为是不同的,单独的条件,我们介绍了一例在阿莫西林-克拉维酸同时开始使用和长期使用西地那非的情况下,DRESS综合征罕见地演变为SJS-TEN的病例,一名66岁的南亚女性有DRESS综合征和肺动脉高压的既往病史.我们讨论了导致她独特临床表现的条件,并为将来的临床遇到提供了考虑因素。
    Drug reactions with eosinophilia and systemic symptoms (DRESS) syndrome and Stevens-Johnson syndrome-toxic epidermal necrolysis (SJS-TEN) are reactive entities of aberrant cytotoxic immunologic reactions to exogenous medications. While they are conventionally seen as distinct, separate conditions, we present a case of a rare evolution of DRESS syndrome into SJS-TEN in the setting of simultaneous amoxicillin-clavulanate initiation and long-term sildenafil use in a 66-year-old South Asian female with a known history of prior DRESS syndrome and pulmonary arterial hypertension. We discuss the conditions leading to her unique clinical presentation and provide considerations for future clinical encounters.
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  • 文章类型: Journal Article
    目的:在本研究中,在实验大鼠中研究了西地那非对二甲双胍药代动力学的影响,我们还通过进行分子对接研究推测了分子机制。
    方法:采用高效液相色谱法分析大鼠血浆中的二甲双胍和西地那非(SIL)。MET的最佳色谱分离和定量,SIL和西替利嗪在PhenomenexEVOC18色谱柱上获得,三乙胺(0.3%):甲醇:乙腈(70:05:25v/v)作为流动相,流速为1ml/min,检测器在224nm处调谐。使用Strata-X盒通过固相萃取从大鼠血浆中提取MET和西地那非。该方法按照ICH指南进行验证。对于对接研究,从PubChem数据库下载了有机阳离子转运蛋白1(OCT1)蛋白和多药和毒素挤出(MATE)蛋白(5XJJ)的晶体结构。对接研究通过PyRx虚拟筛选软件进行,结果由BIOVIADiscoveryStudio进行分析。
    结果:完成了HPLC方法的验证,高效液相色谱法的日内和日间精密度研究表明%RSD值小于5%,在低的情况下,MET和SIL的提取回收率接近80%,中等和高QC样品。MET和SIL的血浆稳定性显示%RSD值<10%,中等,和高QC样品。对大鼠血浆中MET和SIL的敏感性研究表明,定量值的下限为8和10ng/mL,分别。记录药代动力学参数,实验和对照大鼠的Cmax分别为611.2和913.2ng/mL;MET的t1/21.66和1.98,AUC(0-t)1637.5和2727.24,AUC(0-∞)1832.38和2995.24。结果表明,实验大鼠(METSIL)的METCmax比对照组(仅MET)低33.07%,t1/2也短0.32h。对接分析表明,与OCT1相比,西地那非与MATE蛋白(5XJJ)的结合亲和力更高,表明MATE家族蛋白可能参与MET的药代动力学改变。
    结论:建立了高效液相色谱和固相萃取方法,并成功应用于MET和SIL的药代动力学研究。SIL的摄入改变了MET在大鼠体内的药代动力学。分子对接研究表明,MATE家族蛋白参与了MET药代动力学的改变。
    OBJECTIVE: In the present study, the effect of sildenafil on the pharmacokinetics of metformin was studied in experimental rats, and we also postulated the molecular mechanism by performing molecular docking studies.
    METHODS: Analysis of metformin and sildenafil (SIL) from rat plasma was done by high performance liquid chromatography. Optimum chromatographic separation and quantification of MET, SIL and Cetirizine was achieved on Phenomenex EVO C18 column with triethyl amine (0.3%): Methanol: Acetonitrile (70:05:25 v/v) as mobile phase maintaining flow rate of 1 ml/min, the detector was tuned at 224 nm. The extraction of MET and sildenafil from rat plasma was achieved by solid-phase extraction using Strata-X cartridges. The method was validated as per the ICH guidelines. For docking studies, the crystal structure of organic cation transporter 1 (OCT1) protein and multidrug and toxin extrusion (MATE) protein (5XJJ) were downloaded from the PubChem database. The docking study was performed by PyRx virtual screening software, and the results were analyzed by BIOVIA Discovery Studio.
    RESULTS: The validation of HPLC method was done, intraday and interday precision study of HPLC method demonstrated %RSD values less than 5%, the extraction recovery for MET and SIL were near to 80 % for low, medium and high QC samples. The plasma stability of MET and SIL showed % RSD values <10% for low, medium, and high QC samples. A sensitivity study for MET and SIL in rat plasma suggested a lower limit of quantification values of 8 and 10 ng/mL, respectively. The pharmacokinetic parameters were recorded, Cmax of experimental and control rats was 611.2 and 913.2 ng/mL; t1/2 1.66 and 1.98, AUC (0-t) 1637.5 and 2727.24, AUC (0-∞) 1832.38 and 2995.24 for MET. The results suggested that the Cmax of MET in experimental rats (MET + SIL) was 33.07% lower than the control (MET only) and also the t1/2 was 0.32 h shorter. Docking analysis suggested a higher binding affinity of sildenafil with MATE protein (5XJJ) compared to OCT1, suggesting possible involvement of MATE family proteins for pharmacokinetic alterations of MET.
    CONCLUSIONS: The HPLC and solid-phase extraction method were developed and applied successfully for the pharmacokinetics of MET and SIL. Intake of SIL altered the pharmacokinetics of MET in rats. Molecular docking studies suggested the involvement of MATE family proteins for alterations of MET pharmacokinetics.
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  • 文章类型: Case Reports
    我们报告了一例70多岁的男子,他在开始使用西地那非3天后出现咯血。在假设西地那非使用与咯血之间存在潜在联系之前,重要的是排除潜在的其他致病因素和合并症。患者患有多种医疗状况并服用各种药物。在检查中,没有发现异常。他的血液工作最近没有重大变化。停止西地那非与自发症状缓解同时发生。做了胸部CT,没有异常报告。假性咯血或恶性肿瘤可能是合并多种疾病的老年患者咯血的主要鉴别诊断。患者的并发抗凝可能会导致咯血,并且可能引起更大的临床关注。
    We report a case of a man in his 70s who developed haemoptysis 3 days after commencing sildenafil. Before postulating a potential connection between sildenafil use and haemoptysis, it is important to rule out potential other causative factors and comorbidities. The patient suffers from multiple medical conditions and takes various medications. On examination, no abnormalities were discovered. There were no recent significant changes in his bloodwork. Cessation of sildenafil coincided with spontaneous symptom resolution. Chest CT was performed, and no abnormalities were reported. Pseudohaemoptysis or malignancy may be the main differential diagnoses of haemoptysis in elderly patients with multiple comorbidities. Concurrent anticoagulation of the patient may predispose to haemoptysis and is likely to be of greater clinical concern.
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  • 文章类型: Journal Article
    肝脏执行许多基本任务,比如合成胆固醇,控制体内糖原的储存,解毒代谢物,除了表演,调节体内平衡。肝纤维化是以包括胶原纤维的细胞外基质(ECM)过度积累为特征的病理状态。西地那非(5型磷酸二酯酶的选择性抑制剂)具有抗炎,抗氧化和抗凋亡特性。它通常用于治疗男性勃起功能障碍。当前研究的目的是评估西地那非对四氯化碳(CCl4)引起的大鼠肝纤维化的肝保护潜力。确定了肝酶和氧化标记以及促纤维化基因。结果表明,西地那非通过恢复正常ALT水平减轻CCl4引起的肝功能障碍,AST,和GGT以及通过恢复增加的谷胱甘肽(GSH)所证明的抗氧化剂状态,还有过氧化氢酶.此外,a显著下调促纤维化基因的mRNA表达[胶原蛋白-1α,IL-1β,骨桥蛋白(OPN),和转化生长因子-β(TGF-β)]。此外,西地那非减轻肝小叶之间的门静脉纤维化,中央静脉的充血和扩张,和炎症细胞浸润。因此,据推测,西地那非可能通过抑制OPN,有助于控制CCl4引起的肝毒性.
    The liver carries out many essential tasks, such as synthesising cholesterol, controlling the body\'s storage of glycogen, and detoxifying metabolites, in addition to performing, and regulating homeostasis. Hepatic fibrosis is a pathological state characterized by over accumulation of extracellular matrix (ECM) including collagen fibers. Sildenafil (a selective inhibitor of type 5 phosphodiesterase) has anti-inflammatory, antioxidant and anti-apoptotic properties. It is commonly used to treat erectile dysfunction in male. The purpose of the current investigation was to evaluate sildenafil\'s hepatoprotective potential against liver fibrosis in rats that was caused by carbon tetrachloride (CCl4). Liver enzymes and oxidative markers as well as profibrotic genes were determined. The findings showed that sildenafil alleviates the hepatic dysfunctions caused by CCl4 by restoring normal levels of ALT, AST, and GGT as well as by restoring the antioxidant status demonstrated by increased glutathione (GSH), and catalase. In addition, a significantly down-regulated the mRNA expressions of profibrotic genes [collagen-1α, IL-1β, osteopontin (OPN), and transforming growth factor-β (TGF-β)]. Additionally, sildenafil lessens the periportal fibrosis between hepatic lobules, congestion and dilatation in the central vein, and the inflammatory cell infiltrations. As a result, it is hypothesized that sildenafil may be helpful in the management of hepatotoxicity brought on by CCl4 through suppressing OPN.
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  • 文章类型: Journal Article
    背景:Schumanniophytonmagnicum是一种药用植物,用于治疗包括疟疾在内的许多疾病,皮肤病,寄生虫感染,男性性功能障碍,女性不孕和伤寒。然而,喀麦隆的“巴卡”俾格米人没有对其民俗用途进行科学调查。
    目的:研究雄鼠熊果根水提物的壮阳和雄性激素活性,并通过UHPLC/MS分析植物成分。
    方法:将25只16周龄雄性大鼠分为5组,用蒸馏水(10ml/kg)口服30天,或枸橼酸西地那非(5mg/kg),或舒曼尼坦的水提取物(43毫克/千克,86mg/kg和172mg/kg)。通过将雄性大鼠与接受性雌性配对,在第1天和第30天监测性行为参数。实验结束时,处死大鼠,收集血液和生殖器官进行组织学切片,精子分析和生化分析。UHPLC/MS揭示了植物成分及其结构的存在。
    结果:植物提取物显著增加了坐骑,与正常对照组相比,射精和射入频率;与正常对照组相比,血清睾酮水平显着提高了一倍(2.15±0.70ng/ml)。舒马尼磷的水提物的UHPLC/MS鉴定了7个主要化合物,例如舒马尼磷A,Noreugenin和Rohitukine,具有抗氧化和抗菌活性。植物提取物显着提高了阴茎一氧化氮水平(P=0.05)。这些结果与施用柠檬酸西地那非后获得的结果相似。
    结论:舒马尼霉素的水提物可能是治疗勃起功能障碍的一种替代方法。
    BACKGROUND: Schumanniophyton magnificum is a medicinal plant used to manage many ailments including malaria, skin diseases, parasitic infections, male sexual dysfunctions, female infertility and typhoid fever. However, no scientific investigation has been made for its folkloric use by the \"Baka\" Pygmies of Cameroon as an aphrodisiac.
    OBJECTIVE: To investigate the aphrodisiac and androgenic activities of the aqueous extract of the roots of Schumanniophyton magnificum in male rats and analyze the phytoconstituents by UHPLC/MS.
    METHODS: Twenty-five male rats of 16-weeks old were divided into 5 groups and orally treated for 30 days with distilled water (10 ml/kg), or sildenafil citrate (5 mg/kg), or the aqueous extract of Schumanniophyton magnificum (43 mg/kg, 86 mg/kg and 172 mg/kg). The sexual behaviour parameters were monitored on day 1 and 30 by pairing male rats to receptive females. At the end of the experiment, rats were killed and the blood and reproductive organs were collected for histological sectioning, sperm analysis and biochemical analysis. The presence of phytoconstituents and their structures were revealed by UHPLC/MS.
    RESULTS: The plant extract significantly increased the mount, ejaculation and intromission frequencies in comparison to those in the normal control group; and significantly doubled the serum testosterone levels (2.15 ± 0.70 ng/ml) compared to the normal control group. UHPLC/MS of the aqueous extract of Schumanniophyton magnificum identified 7 major compounds such as Schumanniofioside A, Noreugenin and Rohitukine, with antioxidant and antibacterial activities. The plant extracts significantly increased the penile nitric oxide levels (P <0.05). These results were similar to those obtained after administration of sildenafil citrate.
    CONCLUSIONS: The aqueous extract of Schumanniophyton magnificum could be an alternative for erectile dysfunction management.
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  • 文章类型: Journal Article
    胶囊相微萃取(CPME)是一种有效的生物分析技术,可通过将过滤和搅拌机构直接集成到设备中来简化样品制备。一种新型复合吸附剂,旨在对目标分析物具有选择性,该吸附剂由通过溶胶-凝胶技术合成的混合模式吸附剂化学组成,具有良好的前景,并且优于常规的C18吸附剂。在这里,我们描述了离子液体(IL)/Carbowax20M功能化的溶胶-凝胶吸附剂(溶胶-凝胶IL/Carbowax20M)在多孔聚丙烯管的内腔中的封装,用于三种磷酸二酯酶-5抑制剂的胶囊相微萃取,即avanafil,西地那非,人血清和尿液样本中的他达拉非。通过扫描电子显微镜(SEM)和傅立叶变换红外光谱(FT-IR)对CPME器件进行了表征。CPME程序的实验参数(例如样品pH和离子强度,提取时间,搅拌速率,仔细优化洗脱溶剂和体积),以实现分析物的最高提取效率。方法验证是在精度方面进行的,线性度准确度,基体效应,定量下限,和检测限(LOD)。在所有分析物的50-1000ngmL-1范围内研究了方法线性,而在所有情况下精密度均小于11.8%。对于所有分析物,LOD值为17ngmL-1.IL/CW20M功能化的微萃取胶囊可重复使用至少25次用于尿液和血清样品。使用ComplexGAPI和BAGI指标评估了所提出方法的绿色特性和适用性。优化的CPME方案显示出减少的有机溶剂消耗和废物的产生,成本效益,和简单。最后,该方法已成功应用于含药物制剂给药后人尿中西地那非的分析。
    Capsule phase microextraction (CPME) is an efficient bioanalytical technique that streamlines the sample preparation by integrating the filtration and stirring mechanism directly into the device. A novel composite sorbent designed to be selective towards the target analytes consisting of mixed-mode sorbent chemistry synthesized by sol-gel technology is found promising and superior to the conventional C18 sorbents. Herein we describe the encapsulation of an ionic liquid (IL)/Carbowax 20M-functionalized sol-gel sorbent (sol-gel IL/Carbowax 20 M) in the lumen of porous polypropylene tubes for the capsule phase microextraction of three phosphodiesterase-5 inhibitors namely avanafil, sildenafil, and tadalafil in human serum and urine samples. The CPME device was characterized by Scanning Electron Microscopy (SEM) and Fourier-Transform Infrared Spectroscopy (FT-IR). The experimental parameters of CPME procedure (e.g. sample pH and ionic strength, extraction time, stirring rate, elution solvent and volume) were carefully optimized to achieve the highest possible extraction efficiency for the analytes. Method validation was conducted in terms of precision, linearity, accuracy, matrix effect, lower limits of quantification, and limits of detection (LOD). The method linearity was investigated in the range of 50-1000 ng mL-1 for all analytes while the precision was less than 11.8 % in all cases. For all analytes, the LOD values were 17 ng mL-1. The IL/CW 20M-functionalized microextraction capsules could be reused at least 25 times both for urine and serum samples. The green character and the applicability of the proposed method were evaluated using the ComplexGAPI and BAGI indexes. The optimized CPME protocol exhibited reduced consumption of organic solvent and generation of waste, cost-effectiveness, and simplicity. Finally, the proposed method was successfully applied to the analysis of sildenafil in human urine after administration of drug-containing formulation.
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  • 文章类型: Journal Article
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  • 文章类型: Case Reports
    支原体的治疗。在家养雪貂(Mustelaputoriusfuro)中很少描述肺炎。一个10个月大的孩子,0.53kg,雌性家养雪貂被认为是氧气依赖性的,持续一个月的慢性呼吸困难。体格检查结果包括呼吸困难,呼吸急促,双侧支气管囊泡声音增加,和间歇性非生产性咳嗽。血液异常包括轻度白细胞增多(8.6×103/微升),轻度中性粒细胞增多症(4.0×103/微升),轻度低蛋白血症(2.7g/dL),轻度高球蛋白血症(3.3g/dL),轻度低钠血症(147mEq/L),和轻度低氯血症(111.4mEq/L)。射线照片显示明显的弥漫性支气管模式,支气管周围袖套,轻度的主肺动脉隆起,扩张的尾叶肺动脉,腹部浆膜细节减少。超声心动图显示有中度肺动脉高压和二尖瓣收缩期前运动的迹象。支原体属的聚合酶链反应检测。是积极的,治疗开始使用多西环素(10mg/kgPOq12小时,持续16周),泼尼松龙(0.4mg/kgPOq12小时,持续13周,逐渐减少至0.2mg/kgPOq12小时,持续两周,然后最终增加到0.7mg/kgPOq12小时,直至另行通知),西地那非(0.3mg/kgPOq24小时,共13周),通过氧笼补充氧气六周。在开始多西环素治疗后11周的重复超声心动图中,肺动脉高压已经解决。在六个月后的随访中,雪貂在之前的处方药下是稳定的,并且不需要补充氧气.支原体属。雪貂出现呼吸窘迫时,应考虑肺动脉高压。
    Treatment of Mycoplasma spp. pneumonia has rarely been described in domestic ferrets (Mustela putorius furo). A 10-month-old, 0.53 kg, female spayed domestic ferret was presented for oxygen-dependent, chronic dyspnea of one-month\'s duration. Physical examination findings included dyspnea, tachypnea, increased bronchovesicular sounds bilaterally, and an intermittent non-productive cough. Bloodwork abnormalities included a mild leukocytosis (8.6×103/µL), mild neutrophilia (4.0×103/µL), mild hypoalbuminemia (2.7 g/dL), mild hyperglobulinemia (3.3 g/dL), mild hyponatremia (147 mEq/L), and mild hypochloremia (111.4 mEq/L). Radiographs revealed a marked diffuse bronchial pattern with peribronchial cuffing, a mild main pulmonary artery bulge, distended caudal lobar pulmonary arteries, and decreased serosal detail within the abdomen. An echocardiogram revealed indications of moderate pulmonary hypertension and systolic anterior motion of the mitral valve. Polymerase chain reaction testing for Mycoplasma spp. was positive, and treatment was initiated with doxycycline (10 mg/kg PO q 12 h for 16 weeks), prednisolone (0.4 mg/kg PO q 12 h for 13 weeks, tapered to 0.2 mg/kg PO q 12 h for two weeks, then eventually increased to 0.7 mg/kg PO q 12 h until further notice), sildenafil (0.3 mg/kg PO q 24 h for 13 weeks), and oxygen supplementation via an oxygen cage for six weeks. On repeat echocardiogram eleven weeks after initiation of doxycycline therapy, the pulmonary hypertension had resolved. At follow up six months later, the ferret was stable on previously prescribed medications and did not require oxygen supplementation. Mycoplasma spp. and pulmonary hypertension should be considered in cases of respiratory distress in ferrets.
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