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1
Tacrolimus pretreatment attenuates preexisting xenospecific immunity and abrogates hyperacute rejection in a presensitized hamster to rat liver transplant model.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。
Transplantation. 1996 Jun 27;61(12):1730-5. doi: 10.1097/00007890-199606270-00012.
2
FK506 treatment in combination with leflunomide in hamster-to-rat heart and liver xenograft transplantation.在仓鼠到大鼠心脏和肝脏异种移植中,FK506与来氟米特联合治疗。
Transplantation. 1998 Oct 15;66(7):832-7. doi: 10.1097/00007890-199810150-00004.
3
Heart and liver xenotransplantation under low-dose tacrolimus: graft survival after withdrawal of immunosuppression.低剂量他克莫司下的心脏和肝脏异种移植:免疫抑制撤除后的移植物存活情况
Transplantation. 2001 Jan 27;71(2):217-23. doi: 10.1097/00007890-200101270-00008.
4
Modification of humoral responses by the combination of leflunomide and cyclosporine in Lewis rats transplanted with hamster hearts.来氟米特与环孢素联合用药对移植仓鼠心脏的Lewis大鼠体液免疫反应的影响
Transplantation. 1997 Dec 27;64(12):1650-7. doi: 10.1097/00007890-199712270-00004.
5
Humoral and cellular immunopathology of hepatic and cardiac hamster-into-rat xenograft rejection. Marked stimulation of IgM++bright/IgD+dull splenic B cells.肝和心脏仓鼠-大鼠异种移植排斥反应的体液和细胞免疫病理学。脾脏中IgM++明亮/IgD+暗淡的B细胞受到显著刺激。
Am J Pathol. 1993 Jul;143(1):85-98.
6
Hamster-to-rat heart and liver xenotransplantation with FK506 plus antiproliferative drugs.使用FK506加抗增殖药物进行仓鼠到大鼠的心脏和肝脏异种移植。
Transplantation. 1993 Apr;55(4):701-7; discussion 707-8. doi: 10.1097/00007890-199304000-00003.
7
Importance of natural killer cells in the rejection of hamster skin xenografts.自然杀伤细胞在仓鼠皮肤异种移植排斥反应中的重要性。
Transplantation. 1998 Mar 15;65(5):727-34. doi: 10.1097/00007890-199803150-00021.
8
FK778 in experimental xenotransplantation: a detailed analysis of drug efficacy.FK778在实验性异种移植中的应用:药物疗效的详细分析
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Late xenograft rejection: comparison between liver and heart xenografts under low-dose tacrolimus.晚期异种移植排斥反应:低剂量他克莫司作用下肝与心脏异种移植的比较
Transplant Proc. 2002 Feb;34(1):111-2. doi: 10.1016/s0041-1345(01)02693-8.
10
Long-term survival of hamster hearts in presensitized rats.仓鼠心脏在致敏大鼠体内的长期存活
J Immunol. 2000 May 1;164(9):4883-92. doi: 10.4049/jimmunol.164.9.4883.

本文引用的文献

1
THE ANTIBODY RESPONSE OF RATS DEPLETED OF LYMPHOCYTES BY CHRONIC DRAINAGE FROM THE THORACIC DUCT.经胸导管慢性引流耗尽淋巴细胞的大鼠的抗体反应。
J Exp Med. 1963 Jan 31;117(2):303-20. doi: 10.1084/jem.117.2.303.
2
Pretreatment of recipients (nude rat) with donor antigens leads to prolonged survival of hamster heart xenografts.用供体抗原对受体(裸鼠)进行预处理可延长仓鼠心脏异种移植物的存活时间。
Transplant Proc. 1996 Apr;28(2):696-7.
3
Genetic control of the humoral immune response to xenografts. II. Monoclonal antibodies that cause rejection of heart xenografts are encoded by germline immunoglobulin genes.对异种移植体液免疫反应的遗传控制。II. 引起心脏异种移植排斥的单克隆抗体由种系免疫球蛋白基因编码。
Transplantation. 1995 Dec 27;60(12):1504-10. doi: 10.1097/00007890-199560120-00023.
4
Genetic control of the humoral immune response to xenografts. I. Functional characterization of rat monoclonal antibodies to hamster heart xenografts.对异种移植的体液免疫反应的遗传控制。I. 针对仓鼠心脏异种移植的大鼠单克隆抗体的功能特性
Transplantation. 1995 Dec 27;60(12):1497-503. doi: 10.1097/00007890-199560120-00022.
5
B-cell lineages exist in the mouse.B细胞谱系存在于小鼠体内。
Immunol Today. 1993 Feb;14(2):79-83; discussion 88-90. doi: 10.1016/0167-5699(93)90063-Q.
6
Modulation of acute and hyperacute rejection of xenografts in concordant hamster-to-rat combination.在仓鼠到大鼠的协调性异种移植组合中对异种移植物急性和超急性排斥反应的调节。
Transplant Proc. 1993 Feb;25(1 Pt 1):432-4.
7
The effect of splenectomy on cardiac and liver xenografts in the nude rat.脾切除术对裸鼠心脏和肝脏异种移植的影响。
Transplant Proc. 1994 Jun;26(3):1210.
8
The biological basis of and strategies for clinical xenotransplantation.临床异种移植的生物学基础与策略
Immunol Rev. 1994 Oct;141:213-44. doi: 10.1111/j.1600-065x.1994.tb00879.x.
9
Humoral and cellular immunopathology of hepatic and cardiac hamster-into-rat xenograft rejection. Marked stimulation of IgM++bright/IgD+dull splenic B cells.肝和心脏仓鼠-大鼠异种移植排斥反应的体液和细胞免疫病理学。脾脏中IgM++明亮/IgD+暗淡的B细胞受到显著刺激。
Am J Pathol. 1993 Jul;143(1):85-98.
10
Hamster-to-rat heart and liver xenotransplantation with FK506 plus antiproliferative drugs.使用FK506加抗增殖药物进行仓鼠到大鼠的心脏和肝脏异种移植。
Transplantation. 1993 Apr;55(4):701-7; discussion 707-8. doi: 10.1097/00007890-199304000-00003.

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.

DOI:10.1097/00007890-199606270-00012
PMID:8685952
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3005620/
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。