首页> 外文期刊>Transplantation: Official Journal of the Transplantation Society >Synergistic effects of malononitrilamides (FK778, FK779) with tacrolimus (FK506) in prevention of acute heart and kidney allograft rejection and reversal of ongoing heart allograft rejection in the rat.
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Synergistic effects of malononitrilamides (FK778, FK779) with tacrolimus (FK506) in prevention of acute heart and kidney allograft rejection and reversal of ongoing heart allograft rejection in the rat.

机译:丙二腈(FK778,FK779)与他克莫司(FK506)协同预防大鼠急性心肾移植排斥反应和逆转正在进行的心脏移植排斥反应。

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BACKGROUND The effects of tacrolimus (FK506) and malononitrilamides (MNA) (FK778 and FK779) monotherapy and combination therapy were examined in prevention of acute heart and kidney allograft rejection and reversal of ongoing acute heart allograft rejection in the rat.METHODS Brown Norway (RT1n)-to-Lewis (RT11) and ACI (RT1a)-to-Lewis (RT11) combinations were used, respectively, for heart and kidney transplantation models. Immunosuppressants were administered orally from day 1 to day 14 for preventing acute rejection and from day 4 to day 34 after transplantation for the reversal of ongoing acute rejection.RESULTS In the prevention of acute heart rejection model, recipient rats treated with monotherapy of tacrolimus or MNA (FK778, FK779) showed a dose-related prolongation of mean survival time (MST) compared with naive control rats (P<0.01). The mean survival time in combination therapy of tacrolimus (FK506) and FK778 indicated that an additive to synergistic interaction was produced when compared withthe respective monotherapies (combination index [CI]=0.631-1.022). These results were reproducible with tacrolimus and FK779 combination therapy (CI=0.572-0.846). Furthermore, similar results were also found in the prevention of acute kidney allograft rejection in the rat (CI=0.137-0.516). In the reversal of ongoing acute heart allograft rejection, combination therapy of tacrolimus and FK778 demonstrated a strong synergistic interaction (CI=0.166-0.970) compared with monotherapy of tacrolimus or FK778.CONCLUSIONS Combination therapy of tacrolimus and MNA (FK778, FK779) produces synergistic effects in prevention of acute heart and kidney rejection and reversal of ongoing heart allograft rejection in the rat.
机译:背景研究了他克莫司(FK506)和丙二腈(MNA)(FK778和FK779)单一疗法和联合疗法在预防大鼠急性心肾移植排斥反应和逆转正在进行的急性心脏移植排斥反应中的作用.METHODS Brown Norway(RT1n -刘易斯(RT11)和ACI(RT1a)-刘易斯(RT11)的组合分别用于心脏和肾脏移植模型。为预防急性排斥反应,从移植后第1天至第14天口服免疫抑制剂,从移植后第4天至第34天口服免疫抑制剂,以逆转进行中的急性排斥反应。结果在预防急性心脏排斥反应模型中,接受他克莫司或MNA单药治疗的受体大鼠(FK778,FK779)与单纯对照组相比,显示出剂量相关的平均生存时间延长(MST)(P <0.01)。他克莫司(FK506)和FK778联合治疗的平均生存时间表明,与各自的单一疗法相比,它产生了协同相互作用的加成剂(联合指数[CI] = 0.631-1.022)。他克莫司和FK779联合疗法可重现这些结果(CI = 0.572-0.846)。此外,在预防大鼠急性肾移植排斥中也发现了相似的结果(CI = 0.137-0.516)。在持续的急性心脏异体移植排斥反应的逆转中,他克莫司和FK778的联合治疗与他克莫司或FK778的单药治疗相比显示出强大的协同作用(CI = 0.166-0.970)。结论他克莫司和MNA(FK778,FK779)的联合治疗产生协同作用。在预防大鼠急性心肾排斥反应和逆转正在进行的心脏同种异体移植排斥中的作用。

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