首页> 美国卫生研究院文献>British Journal of Pharmacology and Chemotherapy >Sirolimus/cyclosporine/tacrolimus interactions on bile flow and biliary excretion of immunosuppressants in a subchronic bile fistula rat model
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Sirolimus/cyclosporine/tacrolimus interactions on bile flow and biliary excretion of immunosuppressants in a subchronic bile fistula rat model

机译:西罗莫司/环孢素/他克莫司相互作用对慢性胆汁瘘大鼠模型胆汁流量和胆汁排泄免疫抑制剂的影响

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class="enumerated" style="list-style-type:decimal">The new immunosuppressive agent sirolimus generally is combined in transplant patients with cyclosporine and tacrolimus which both exhibit cholestatic effects. Nothing is known about possible cholestatic effects of these combinations which might be important for biliary excretion of endogenous compounds as well as of immunosuppressants.Rats were daily treated with sirolimus (1 mg kg−1 p.o.), cyclosporine (10 mg kg−1 i.p.), tacrolimus (1 mg kg−1 i.p.), or a combination of sirolimus with cyclosporine or tacrolimus. After 14 days a bile fistula was installed to investigate the effects of the immunosuppressants and their combinations on bile flow and on biliary excretion of bile salts, cholesterol, and immunosuppressants.Cyclosporine as well as tacrolimus reduced bile flow (−22%; −18%), biliary excretion of bile salts (−15%;−36%) and cholesterol (−15%; −47%). Sirolimus decreased bile flow by 10%, but had no effect on cholesterol or bile salt excretion.Combination of sirolimus/cyclosporine decreased bile flow and biliary bile salt excretion to the same extent as cyclosporine alone, but led to a 2 fold increase of biliary cholesterol excretion. Combination of sirolimus/tacrolimus reduced bile flow only by 7.5% and did not change biliary bile salt and cholesterol excretion.Sirolimus enhanced blood concentrations of cyclosporine (+40%) and tacrolimus (+57%). Sirolimus blood concentration was increased by cyclosporine (+400%), but was not affected by tacrolimus.We conclude that a combination of sirolimus/tacrolimus could be the better alternative to the cotreatment of sirolimus/cyclosporine in cholestatic patients and in those facing difficulties in reaching therapeutic ranges of sirolimus blood concentration.
机译:class =“ enumerated” style =“ list-style-type:decimal”> <!-list-behavior =枚举前缀-word = mark-type = decimal max-label-size = 0-> 新的免疫抑制剂西罗莫司通常与环孢霉素和他克莫司联合用于移植患者,两者均表现出胆汁抑制作用。这些组合可能对胆汁淤积的影响尚不清楚,这可能对内源性化合物和免疫抑制剂的胆汁排泄很重要。 小白鼠每天接受西罗莫司(1mgmgkgkg -1 po),环孢霉素(10 mg kg -1 ip),他克莫司(1 mg kg -1 ip)或西罗莫司与环孢霉素或他克莫司的组合。 14天后,安装了一个胆瘘,以研究免疫抑制剂及其组合对胆汁流量以及胆汁盐,胆固醇和免疫抑制剂的胆汁排泄的影响。 −22%; − 18%),胆汁盐(−15%; − 36%)和胆固醇(−15%; − 47%)的胆汁排泄。西罗莫司使胆汁流量减少了10%,但对胆固醇或胆汁盐的排泄没有影响。 西罗莫司/环孢霉素的联合使用可降低胆汁流量和胆汁胆汁盐排泄,其程度与单独使用环孢菌素相同胆汁胆固醇排泄量增加2倍。西罗莫司/他克莫司的组合仅使胆汁流量减少了7.5%,并且没有改变胆汁盐和胆固醇的排泄。 西罗莫司提高了环孢素(+ 40%)和他克莫司(+ 57%)的血药浓度。西罗莫司的血药浓度被环孢菌素(+ 400%)增加,但不受他克莫司的影响。 我们得出结论,西罗莫司/他克莫司的联合治疗胆汁淤积可以更好地替代西罗莫司/环孢霉素患者和西罗莫司血药浓度难以达到治疗范围的患者。

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