Barth C, Stachowski J, von Menges A, Lammerding P, Baldamus C A
Klinik IV für Medizin, Universitätsklinik Köln.
Med Klin (Munich). 1998 Jan 15;93(1):1-5. doi: 10.1007/BF03045032.
The pathogenesis of chronic renal allograft rejection is still speculative. Amongst other factors immune-mediated graft injury is proposed. Since the allo-antigen is specifically recognized by the variable (V) alpha and beta chains of the T-cell receptor, a restricted T-cell repertoire might support the notion of allo-antigen involvement in chronic rejection.
By the means of semiquantitative polymerase chain reaction the V beta families 1-20 were assessed in allograft biopsies with histologically confirmed chronic and acute rejection. At the same time the V beta repertoire was analyzed in PBMC.
The intragraft V beta repertoire was limited to 1 to 3 dominant V beta families in chronic and acute rejection. The response was highly individual and did not correlate to the type or degree of HLA mismatches. The T-cell repertoire in PBMC was polyclonal and did not reflect the immune response in the graft.
The finding of a restricted V beta repertoire in both forms of rejection might indicate an immunological basis not only for acute, but also for ongoing chronic rejection. Tailor-made antibodies against the dominant V beta clones might provide a tool for selective immunosuppression in both entities of rejection targeting only those T cells which were activated by allo-antigens.
慢性肾移植排斥反应的发病机制仍具有推测性。除其他因素外,免疫介导的移植物损伤也被提及。由于同种异体抗原是由T细胞受体的可变(V)α和β链特异性识别的,有限的T细胞库可能支持同种异体抗原参与慢性排斥反应这一观点。
通过半定量聚合酶链反应对组织学确诊为慢性和急性排斥反应的移植肾活检组织中的Vβ1 - 20家族进行评估。同时,对外周血单个核细胞(PBMC)中的Vβ库进行分析。
在慢性和急性排斥反应中,移植肾内的Vβ库局限于1至3个优势Vβ家族。这种反应具有高度个体差异性,且与HLA错配的类型或程度无关。PBMC中的T细胞库是多克隆性的,并不反映移植肾中的免疫反应。
在两种排斥反应形式中均发现有限的Vβ库,这可能表明不仅急性排斥反应,而且持续性慢性排斥反应都具有免疫学基础。针对优势Vβ克隆定制的抗体可能为两种排斥反应实体中的选择性免疫抑制提供一种工具,仅针对那些被同种异体抗原激活的T细胞。
