阿普利莫司特(otezla)对l -精氨酸诱导大鼠急性胰腺炎的潜在治疗作用

Rabab EL-shafy, Salwa A. Elgendy
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摘要

背景:急性胰腺炎症是世界范围内的急症。Aprimelast (Otezla)是一种抑制磷酸二酯酶-4 (PDE4)和调节炎症介质的口服活性药物。没有研究检测其在治疗急性胰腺炎(AP)中的作用。目的:研究Aprimelast对l -精氨酸产生AP的影响。材料与方法:采用l -精氨酸250 mg/kg体重腹腔注射2次,间隔1小时建立AP大鼠模型。治疗组在与对照组相同剂量的l -精氨酸IP注射后,给予Aprimelast单次口服剂量20mg/kg体重,连续5天。治疗末期取血测定大鼠氧化应激参数谷胱甘肽(GSH)、丙二醛(MDA),然后处死大鼠。所有治疗动物切除胰腺,准备组织中肿瘤坏死因子(TNFalpha)和白细胞介素-10 (IL-10)的测定和组织病理学检查。结果:AP大鼠的组织学改变与胰腺组织损伤一致,血糖、血清淀粉酶和脂肪酶活性升高。此外,AP大鼠胰腺炎症生物标志物TNFalpha水平升高,抗炎生物标志物IL-10水平降低。此外,与对照组相比,AP组氧化应激生物标志物MDA升高,而抗氧化剂GSH水平降低。同时给药Aprimelast导致预先存在的参数和组织学的实质性改善。结论:Aprimelast对精氨酸诱导的成年白化大鼠AP具有抗炎和抗氧化作用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
THE POTENTIAL THERAPEUTIC EFFECT OF APRIMELAST (OTEZLA) ON L-ARGININE INDUCED ACUTE PANCREATITIS IN RATS
Background: Acute pancreatic inflammation is an emergency worldwide. Aprimelast (Otezla) is an orally active drug inhibiting phosphodiesterase-4 (PDE4) &modulate the inflammatory mediators. NO research was done to detect its role in treatment of acute pancreatitis (AP). Aim: this research was designed to determine the role of Aprimelast on AP produced by L-arginine. Materials & methods: A rat model of AP was developed by two injections of L-arginine 250 mg/kg body weight, intraperitoneal (IP), separated by a one-hour period. The treatment group received Aprimelast at a single daily oral dosage of 20mg/kg body weight for five consecutive days after IP injections of L-arginine at the same dose as before.AT the last of treating period, blood samples were taken for the assessment of the parameters of oxidative stress glutathione [GSH], malondialdehyde [MDA], then rats were sacrificed. The pancreas of all treated animals was excised, prepared for estimation of tumor necrotic factor (TNFalpha) & interleukin-10 (IL-10) in tissues and histopathological examination. Results: Rats with AP had histological alterations consistent with pancreatic tissue impairment, and elevated blood glucose, serum amylase, and lipase enzyme activities. Additionally, AP rats had increased levels of the pancreatic inflammatory biomarker TNFalpha and decreased levels of the anti-inflammatory biomarker IL-10. Additionally, the oxidative stress biomarker MDA was elevated in AP, whereas the antioxidant GSH level was reduced as contrasted to control group. Co-administration of Aprimelast led to substantial improvements in both pre-existing parameters and histology. Conclusion: These results suggested that Aprimelast may have beneficial therapeutic effect on Larginine induced AP in adult albino rats owing to its anti-inflammatory and anti-oxidative stress effects.
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