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Transfer of the inflammatory disease of HLA-B27 transgenic rats by bone marrow engraftment

机译:骨髓移植转移HLA-B27转基因大鼠的炎症性疾病

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摘要

We have previously produced lines of rats transgenic for HLA-B27 and human beta 2-microglobulin (h beta 2m) that develop a progressive inflammatory disease sharing many clinical and histologic features with the B27-associated human spondyloarthropathies, including gut and male genital inflammation, arthritis, and psoriasiform skin lesions. Other transgenic lines that express lower levels of B27 and h beta 2m remain healthy. To investigate the cellular basis for the multisystem inflammatory disease in these rats, we transferred lymphoid cell populations from disease-prone transgenic lines to irradiated disease- resistant transgenic and nontransgenic recipients. In recipients of cells from two different disease-prone lines, successful transfer required engraftment of bone marrow cells. Transfer of disease with fetal liver cells suggested that neither mature effector cells nor active disease in the donors was necessary for induction of disease in the recipients. Remission of the spontaneous disease in irradiated transgenic rats was induced by engraftment of nontransgenic bone marrow. These results suggest that the expression of HLA-B27 in bone marrow-derived cells alone is sufficient for the development of B27- associated disease, and that disease transfer requires engraftment of a bone marrow precursor cell for which mature cells in spleen or in lymph node cannot substitute.
机译:我们先前已经生产了可转基因的HLA-B27和人beta 2微球蛋白(h beta 2m)大鼠,它们发展为一种进行性炎症,与B27相关的人类脊椎关节病具有许多临床和组织学特征,包括肠道和男性生殖器炎症,关节炎和牛皮癣样皮肤病变。表达较低水平的B27和h beta 2m的其他转基因品系仍​​然健康。为了研究这些大鼠中多系统炎性疾病的细胞基础,我们将易患疾病的转基因株系中的淋巴样细胞群体转移至受辐照的抗病转基因和非转基因受体。在来自两个易患疾病的不同细胞系的受体中,成功的转移需要植入骨髓细胞。用胎儿肝细胞转移疾病表明,供体中成熟的效应细胞或活动性疾病都不需要在受体中诱发疾病。通过植入非转基因骨髓可诱导辐照的转基因大鼠自发性疾病缓解。这些结果表明,仅HLA-B27在骨髓来源的细胞中的表达就足以发展与B27相关的疾病,并且疾病转移需要植入骨髓前体细胞,该细胞的成熟细胞在脾脏或淋巴结中不能替代。

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