首页> 外文期刊>Journal of drug targeting >Sulfate-conjugated methylprednisolone as a colon-targeted methylprednisolone prodrug with improved therapeutic properties against rat colitis.
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Sulfate-conjugated methylprednisolone as a colon-targeted methylprednisolone prodrug with improved therapeutic properties against rat colitis.

机译:硫酸盐缀合的甲基泼尼松龙作为结肠靶向的甲基泼尼松龙的前药,具有改善的大鼠结肠炎治疗性能。

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Methylprednisolone (MP) is one of the most widely used corticosteroids for the treatment of inflammatory bowel disease (IBD). However, systemic adverse effects of MP limit its availability for the disease. In present study, sulfate-conjugated methylprednisolone (MPS) was evaluated in vivo as a colon-targeted prodrug of MP and its therapeutic properties against 2,4,6-trinitrobenzenesulfonic acid-induced rat colitis were investigated. Upon oral administration, a large fraction of MPS reached the large intestine, where MPS was converted to MP implying that MPS would deliver MP effectively to the large intestine. The fecal recovery of MP (after MPS administration) was much greater than that after MP administration and the urinary recovery of MP (after MPS administration) was much less than that after MP administration, suggesting that MPS should exhibit enhanced therapeutic activity and reduced systemic adverse effects. Consistent with this notion, MPS was more effective than MP in ameliorating rat colitis. Moreover, the adverse effects of MPS on adrenal function and thymus were much lower than those of MP. Taken together, MPS may be therapeutically superior to MP in IBD treatment.
机译:甲基强的松龙(MP)是治疗炎症性肠病(IBD)用途最广泛的皮质类固醇之一。但是,MP的全身性不良反应限制了其对疾病的利用。在本研究中,硫酸盐共轭甲基强的松龙(MPS)在体内作为MP的结肠靶向前药进行了评估,并研究了其对2,4,6-三硝基苯磺酸诱导的大鼠结肠炎的治疗性能。口服后,大部分MPS到达大肠,MPS转化为MP,这意味着MPS将有效地将MP输送到大肠。 MP的粪便恢复(MPS给药后)要比MP给药后大得多,MP的尿液回收(MPS给药后)要比MP给药后的尿回收率要低得多,这表明MPS应该表现出增强的治疗活性和减少的全身不良反应效果。与此观点一致,MPS在改善大鼠结肠炎方面比MP更有效。此外,MPS对肾上腺功能和胸腺的不利影响远低于MP。综上所述,MPS在IBD治疗中可能在治疗上优于MP。

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