睾丸内接种供体抗原通过诱导CD8 + CD122 +和CD4 + CD25 +调节性T细胞促进传统共刺激阻断诱导的皮肤同种异体移植接受。

Donor-antigen Inoculation in the Testis Promotes Skin Allograft Acceptance Induced by Conventional Costimulatory Blockade via Induction of CD8 + CD122+ and CD4 + CD25+ Regulatory T Cells.

作者信息

Cong Lin, Wang Shu-Feng, Zhao Zhi-Li, Yang Rong-Ya

机构信息

1 Department of Dermatology, General Hospital of Beijing Military Command, Beijing, China. 2 Graduate School, Third Military Medical University, Chongqing, China. 3 Institute of Immunology, Third Military Medical University, Chongqing, China.

出版信息

Transplantation. 2016 Apr;100(4):763-71. doi: 10.1097/TP.0000000000001011.

DOI:10.1097/TP.0000000000001011

PMID:26569069

Abstract

BACKGROUND

Immune responses are somewhat suppressed in immune privileged sites, including the testes, which provide a preexisting opportunity to prolong allograft survival. Previous studies have shown that intratesticular islet allografts enjoy extended survival even without any immunosuppression. However, it is unknown if testicular immune privilege can be exploited to prolong the survival of a solid allograft, including the skin, because it is impractical to implant a solid tissue in human testes.

METHODS

To immunize recipient mice, splenocytes from BALB/c mice were injected into the testis of C57BL/6 recipients 1 week before skin transplantation. CD8 + CD122+ and CD4 + FoxP3+ regulatory T [Treg] cells were quantified by fluorescence-activated cell sorting.

RESULTS

Although donor-antigen inoculation alone did not delay skin allograft rejection, it significantly extended the allograft survival when combined with CD40/CD40L or B7/CD28 costimulatory blockade and further induced long-term skin allograft acceptance when both costimulatory pathways were blocked. Similarly, donor-antigen inoculation suppressed alloreactive T cell proliferation in draining lymph nodes of skin recipients in the presence of the same costimulatory blockade. Interestingly, donor-antigen inoculation via intratesticular injection increased CD8 + CD122+, but not CD4 + FoxP3+, Treg numbers after transplantation. However, both CD8 + CD122+ and CD4 + CD25+ Treg cells induced by donor-antigen inoculation and the costimulatory blockade were more potent in suppression than that induced without the inoculation. Depletion of CD8+ or CD25+ T cells largely abrogated long-term skin allograft survival induced by donor-antigen inoculation and the costimulatory blockade.

CONCLUSIONS

Intratesticular inoculation with donor antigens promotes long-term skin allograft survival induced by conventional costimulatory blockade via the induction of both CD8 + CD122+ and CD4 + CD25+ Treg cells.

摘要

背景

免疫豁免部位（包括睾丸）的免疫反应会受到一定程度的抑制，这为延长同种异体移植物存活提供了一个现成的机会。先前的研究表明，即使没有任何免疫抑制，睾丸内胰岛同种异体移植的存活时间也会延长。然而，尚不清楚是否可以利用睾丸免疫豁免来延长包括皮肤在内的实体同种异体移植物的存活时间，因为将实体组织植入人类睾丸是不切实际的。

方法

为了使受体小鼠免疫，在皮肤移植前1周，将BALB/c小鼠的脾细胞注射到C57BL/6受体的睾丸中。通过荧光激活细胞分选对CD8 + CD122+和CD4 + FoxP3+调节性T（Treg）细胞进行定量分析。

结果

尽管单独接种供体抗原并未延迟皮肤同种异体移植排斥反应，但与CD40/CD40L或B7/CD28共刺激阻断联合使用时，可显著延长同种异体移植物的存活时间，并且当两条共刺激途径均被阻断时，可进一步诱导长期的皮肤同种异体移植接受。同样，在相同的共刺激阻断存在的情况下，供体抗原接种可抑制皮肤受体引流淋巴结中的同种异体反应性T细胞增殖。有趣的是，通过睾丸内注射接种供体抗原可增加移植后CD8 + CD122+ Treg细胞数量，但不会增加CD4 + FoxP3+ Treg细胞数量。然而，供体抗原接种和共刺激阻断诱导的CD8 + CD122+和CD4 + CD25+ Treg细胞在抑制作用方面比未接种时诱导的更有效。去除CD8+或CD25+ T细胞在很大程度上消除了供体抗原接种和共刺激阻断诱导的长期皮肤同种异体移植存活。