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他克莫司预处理可减轻预先存在的异种特异性免疫反应,并消除致敏仓鼠至大鼠肝移植模型中的超急性排斥反应。

Tacrolimus pretreatment attenuates preexisting xenospecific immunity and abrogates hyperacute rejection in a presensitized hamster to rat liver transplant model.

作者信息

Tsugita M, Valdivia L A, Rao A S, Pan F, Celli S, Demetris A J, Fung J J, Starzl T E

机构信息

Pittsburgh Transplantation Institute, University of Pittsburgh, Pennsylvania 15213, USA.

出版信息

Transplantation. 1996 Jun 27;61(12):1730-5. doi: 10.1097/00007890-199606270-00012.

Abstract

In the hamster to rat liver transplant model, we determined the efficacy of tacrolimus in attenuating natural xenospecific humoral immunity and in abrogating the hyperacute liver rejection that is produced by presensitizing the Lewis rat recipient. Hamster livers, transplanted orthotopically into naive rats (controls), were rejected with animal death after 6.4.+/- 0.5 (SD) days. The infusion on (day -6) of 1.5 x 10(7) hamster hepatocytes, or of 1.5 x 10(8) nonparenchymal cells (NPC), resulted in hyperacute rejection and death in < or = 1.9 days. However, when the rats were pretreated with 1 mg/kg/day tacrolimus from days -6 to -1, survival of non-presensitized animals was prolonged to 25 +/- 20 days and that of recipients presensitized with hamster hepatocytes to 36 +/- l6 days or with NPC to 32 +/- 1.7 days. The tacrolimus pretreatment significantly reduced the hamster-specific complement-dependent cytotoxic antibodies response directed to liver NPC but not to lymph node cell targets. These observations suggest that the prolongation of survival by appropriately timed treatment with this T cell directed drug model is caused by the inhibition of humoral as well as cellular xenograft rejection.

摘要

在仓鼠到大鼠的肝移植模型中,我们确定了他克莫司在减弱天然异种特异性体液免疫以及消除通过预先致敏Lewis大鼠受体而产生的超急性肝排斥反应方面的疗效。原位移植到未致敏大鼠(对照组)体内的仓鼠肝脏,在6.4±0.5(标准差)天后因动物死亡而被排斥。在第-6天输注1.5×10⁷个仓鼠肝细胞或1.5×10⁸个非实质细胞(NPC),会导致在≤1.9天内发生超急性排斥反应和死亡。然而,当大鼠从第-6天至-1天用1毫克/千克/天的他克莫司进行预处理时,未预先致敏动物的存活时间延长至25±20天,用仓鼠肝细胞预先致敏的受体的存活时间延长至36±16天,用NPC预先致敏的受体的存活时间延长至32±1.7天。他克莫司预处理显著降低了针对肝脏NPC而非淋巴结细胞靶标的仓鼠特异性补体依赖性细胞毒性抗体反应。这些观察结果表明,通过用这种针对T细胞的药物模型进行适时治疗来延长存活时间,是由于抑制了体液以及细胞性异种移植排斥反应。

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Immunol Today. 1993 Feb;14(2):79-83; discussion 88-90. doi: 10.1016/0167-5699(93)90063-Q.

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