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通过在胸腺切除的小鼠中移植新生猪胸腺诱导特异性猪皮肤移植耐受。

The induction of specific pig skin graft tolerance by grafting with neonatal pig thymus in thymectomized mice.

作者信息

Zhao Y, Rodriguez-Barbosa J I, Swenson K, Barth R N, Shimizu A, Arn J S, Sachs D H, Sykes M

机构信息

Transplantation Biology Research Center, Massachusetts General Hospital/Harvard Medical School, Boston 02129, USA.

出版信息

Transplantation. 2000 Apr 15;69(7):1447-51. doi: 10.1097/00007890-200004150-00040.

Abstract

BACKGROUND

Xenogeneic donor-specific tolerance can be induced by transplanting fetal pig thymus and liver tissue (FP THY/LIV) to thymectomized (ATX), T/NK cell-depleted mice. By using neonatal pig tissue, we hoped to overcome two obstacles that arise with the use of fetal pig tissue: (1) the inability to keep fetal pigs alive after harvesting their thymic tissue, resulting in unavailability of their skin or other organs for grafting; and (2) the limited fetal thymic tissue yield, making application to large animals and humans more difficult.

METHODS

Neonatal pig thymus tissue (NP THY) was grafted into ATX, T/NK cell-depleted, 3Gy whole body-irradiated, originally immunocompetent B6 mice to evaluate the ability of NP THY to reconstitute mouse CD4+ T cells and to induce xenogeneic tolerance to donor pig skin grafts.

RESULTS

Repopulation of mouse CD4+ T cells in the peripheral tissues was observed in T/NK cell-depleted, ATX B6 mice that received NP THY with or without neonatal pig spleen (NP SPL), but not in those receiving NP SPL alone, indicating that pig thymus grafting was necessary and sufficient for mouse T cell recovery. Seven of nine NP THY/SPL-grafted ATX mice and two of six NP THY-grafted ATX mice that reconstituted >5% CD4+ cells in PBL accepted donor pig skin long-term without lymphocyte infiltration, whereas they rejected allogeneic BALB/c skin and third party pig skin grafts as rapidly as euthymic mice.

CONCLUSIONS

NP THY can support the development of mouse CD4+ T cells that are functional and specifically tolerant to donor pig antigens in ATX, T/NK cell-depleted, 3 Gy whole body-irradiated, originally immunocompetent B6 mice. Additional grafting of NP SPL with NP THY improves the efficiency of tolerance induction in this model.

摘要

背景

通过将胎猪胸腺和肝脏组织(FP THY/LIV)移植到经胸腺切除(ATX)、T/NK细胞耗竭的小鼠体内,可诱导异种供体特异性耐受。通过使用新生猪组织,我们希望克服使用胎猪组织时出现的两个障碍:(1)收获胸腺组织后无法使胎猪存活,导致其皮肤或其他器官无法用于移植;(2)胎胸腺组织产量有限,使得应用于大型动物和人类更加困难。

方法

将新生猪胸腺组织(NP THY)移植到经ATX、T/NK细胞耗竭、3Gy全身照射、原本具有免疫活性的B6小鼠体内,以评估NP THY重建小鼠CD4+ T细胞以及诱导对供体猪皮肤移植的异种耐受的能力。

结果

在接受NP THY(无论有无新生猪脾脏(NP SPL))的T/NK细胞耗竭、ATX B6小鼠的外周组织中观察到小鼠CD4+ T细胞的重新填充,但在仅接受NP SPL的小鼠中未观察到,这表明猪胸腺移植对于小鼠T细胞恢复是必要且充分的。在PBL中重建>5% CD4+细胞的9只NP THY/SPL移植的ATX小鼠中有7只以及6只NP THY移植的ATX小鼠中有2只长期接受供体猪皮肤,无淋巴细胞浸润,而它们排斥同种异体BALB/c皮肤和第三方猪皮肤移植的速度与正常小鼠一样快。

结论

NP THY可以支持在经ATX、T/NK细胞耗竭、3 Gy全身照射、原本具有免疫活性的B6小鼠中发育出对供体猪抗原具有功能且特异性耐受的小鼠CD4+ T细胞。NP SPL与NP THY的额外移植可提高该模型中耐受诱导的效率。

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