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Cd4+Cd25+ Immune Regulatory Cells Are Required for Induction of Tolerance to Alloantigen via Costimulatory Blockade

机译:Cd4 + Cd25 +免疫调节细胞是通过共刺激封锁诱导对同种抗原的耐受性所必需的

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摘要

Immune regulatory CD4+CD25+ cells play a vital role in the induction and maintenance of self-tolerance and are essential for T cell homeostasis and the prevention of autoimmunity. Induction of tolerance to allogeneic donor grafts is a clinically desirable goal in bone marrow and solid organ transplantation. To determine whether CD4+CD25+ cells regulate T cell responses to alloantigen and are critical for tolerance induction, murine CD4+ T cells were tolerized to alloantigen via ex vivo CD40 ligand (CD40L)/CD40 or CD28/cytotoxic T lymphocyte–associated antigen 4/B7 blockade resulting in secondary mixed leukocyte reaction hyporesponsiveness and tolerance to alloantigen in vivo. CD4+CD25+ T cells were found to be potent regulators of alloresponses. Depletion of CD4+CD25+ T cells from the CD4+ responder population completely abrogated ex vivo tolerance induction to alloantigen as measured by intact responses to alloantigen restimulation in vitro and in vivo. Addback of CD4+CD25+ T cells to CD4+CD25− cultures restored tolerance induction. These data are the first to indicate that CD4+CD25+ cells are essential for the induction of tolerance to alloantigen and have important implications for tolerance-inducing strategies targeted at T cell costimulatory pathways.
机译:免疫调节性CD4 + CD25 +细胞在诱导和维持自我耐受中起着至关重要的作用,对于T细胞稳态和预防自身免疫至关重要。诱导对同种异体供体移植的耐受性是骨髓和实体器官移植的临床上理想的目标。为了确定CD4 + CD25 +细胞是否调节T细胞对同种抗原的反应并且对于耐受诱导至关重要,通过离体CD40配体(CD40L)/ CD40或CD28 /细胞毒性T淋巴细胞相关抗原4 / B7耐受鼠CD4 + T细胞对同种抗原的耐受。阻断导致继发性混合白细胞反应低反应性和体内对同种抗原的耐受性。发现CD4 + CD25 + T细胞是同种异体反应的有效调节剂。通过体外和体内对同种抗原再刺激的完整反应来测量,从CD4 +应答者群体中耗尽CD4 + CD25 + T细胞完全废除了对同种抗原的离体耐受性诱导。将CD4 + CD25 + T细胞加回到CD4 + CD25-培养物中可恢复耐受性诱导。这些数据首次表明CD4 + CD25 +细胞对于诱导对同种抗原的耐受性至关重要,并且对针对T细胞共刺激途径的耐受性诱导策略具有重要意义。

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