Inflammation and T Cell Memory: Inter-related Barriers to Allograft Tolerance

炎症和 T 细胞记忆：同种异体移植耐受的相互关联的障碍

• 批准号: 8117651
• 负责人: TERRY B. STROM
• 金额: $ 150万
• 依托单位: BETH ISRAEL DEACONESS MEDICAL CENTER
• 依托单位国家: 美国
• 财政年份: 2007
• 资助国家: 美国
• 起止时间: 2007-08-20 至 2012-12-31
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/8117651
• 关键词: Acute; Allograft Tolerance; Allografting; Anti-Inflammatory Agents; Anti-inflammatory; Chronic; Clinical; Development; Drug toxicity; Engraftment; Equilibrium; Failure; Fertilization; Goals; Grant; Human; Immune response; Immunity; Immunosuppression; Infection; Inflammation; Inflammatory; Inflammatory Response; Injury; Insulin; Ischemia; Islet Cell; Islets of Langerhans Transplantation; Kidney Transplantation; Lead; Link; Maintenance; Malignant Neoplasms; Measures; Memory; Metabolic; Outcome; Primates; Protocols documentation; Regimen; Regulation; Regulatory T-Lymphocyte; Reperfusion Therapy; Role; Survival Rate; T cell response; T memory cell; Testing; Tissue Donors; Transplantation; cytokine; exhaustion; graft function; improved; in vivo; islet; islet allograft; kidney allograft; novel; programs; response; tool

DESCRIPTION (provided by applicant): Despite improvements in early post-transplant survival rates over the last two decades, a relentless annual attrition rate of 3-5 % in recipients of previously successful renal allografts continues to limit longer term outcomes. Long term outcomes with islet transplantation are simply unacceptable with only 10% of recipients remaining insulin free at five years. In islets metabolic exhaustion due to an inadequate islet cell mass may be an important impediment to long term graft function. Late allograft failure, resulting from chronic rejection, infection, drug toxicity, and malignancies emphasizes the limitations of chronically administered immunosuppression in kidney and islet transplantations. Therefore the ultimate goal of transplantation is to achieve long-term engraftment without maintenance immunosuppression. Pilot clinical tolerance protocols are currently being tested in humans, but there remain substantial barriers to achieving true tolerance in humans. The major objective of this Multi-Project grant is to improve the outcome following kidney and islet transplantation by defining the essential conditions for induction of durable tolerance to kidney and islet allografts, and defining the roles of inflammation and memory T cells in being major barriers to tolerance. Our central hypothesis is that the early pro-inflammatory responses due in large measure to ischemia-reperfusion and anoxic injury to the donor tissues incites adverse forms of anti-donor immunity, thereby provoking acute clinical or subclinical rejection and exaggerating the subsequent expansion of pre-existing donor reactive memory, and post transplant development of newly acquired donor reactive memory T cells. Thus, we hypothesize that an adverse balance of pro- to anti-inflammatory cytokines and anti-donor memory responses represent major obstacles to the induction and maintenance of tolerance. We propose novel and inter-related strategies to alter the balance of the alloimmune response to favor regulation and long-term tolerance taking into consideration the inflammatory- and memory-related barriers to tolerance in the context of islet and kidney transplantation. The rationale linking the specific aims of the two interrelated in vivo projects and the mechanistic studies is that we now have the tools to test the relevance and inter-relationship of inflammatory responses to the balance of aggressive and memory responses, T cell regulatory and tolerance induction. It, therefore, should be possible to define and systematically apply the perturbations of the innate and adaptive immune response that lead to tolerance in primate allograft recipients. Moreover, the Program will lead to cross-fertilization and sharing of facets of the best tolerance inducing regimens developing from Project 1 with those of Project 2.

描述（由申请人提供）：尽管在过去二十年中移植后早期存活率有所提高，但既往成功的肾移植受者每年3- 5%的持续流失率继续限制长期结局。胰岛移植的长期结果是完全不可接受的，只有10%的接受者在五年内保持无胰岛素。在胰岛中，由于胰岛细胞质量不足而导致的代谢衰竭可能是长期移植功能的重要障碍。由于慢性排斥反应、感染、药物毒性和恶性肿瘤导致的晚期同种异体移植失败强调了肾和胰岛移植中长期施用免疫抑制剂的局限性。因此，移植的最终目标是在没有维持免疫抑制的情况下实现长期植入。试点临床耐受性方案目前正在人体中进行测试，但在人体中实现真正的耐受性仍然存在重大障碍。这项多项目资助的主要目标是通过定义诱导对肾脏和胰岛同种异体移植物持久耐受的基本条件，以及定义炎症和记忆T细胞在耐受的主要障碍中的作用，来改善肾脏和胰岛移植后的结果。我们的中心假设是，早期促炎反应在很大程度上归因于供体组织的缺血-再灌注和缺氧损伤，从而激发了不利形式的抗供体免疫，从而引起急性临床或亚临床排斥反应，并夸大了先前存在的供体反应性记忆的随后扩展，以及新获得的供体反应性记忆T细胞的移植后发育。因此，我们假设促-抗炎细胞因子和抗供体记忆反应的不利平衡是诱导和维持耐受的主要障碍。我们提出了新的和相互关联的策略来改变同种免疫反应的平衡，以有利于调节和长期耐受，同时考虑到胰岛和肾移植背景下的炎症和记忆相关的耐受障碍。将两个相互关联的体内项目的具体目标和机制研究联系起来的基本原理是，我们现在有工具来测试炎症反应与攻击性和记忆反应、T细胞调节和耐受诱导的平衡的相关性和相互关系。因此，它应该是可能的定义和系统地应用干扰的先天性和适应性免疫反应，导致耐受灵长类动物同种异体移植受体。此外，该计划将导致项目1与项目2开发的最佳耐受诱导方案的交叉和共享。

项目成果

Tim-1 signaling substitutes for conventional signal 1 and requires costimulation to induce T cell proliferation.

• DOI: 10.4049/jimmunol.182.3.1379
• 发表时间: 2009-02-01
• 期刊: Journal of immunology (Baltimore, Md. : 1950)
• 作者: Mariat C;Degauque N;Balasubramanian S;Kenny J;DeKruyff RH;Umetsu DT;Kuchroo V;Zheng XX;Strom TB
• 通讯作者: Strom TB