抗原提呈细胞的能力在儿童癌症患者中得到充分保存。

Gan Pub Date : 1984-12-01
Y Koide, T Hongo, R Iseki, Y Mori, T O Yoshida
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引用次数: 0

摘要

25例儿童癌症患者中有19例的T细胞对纯化蛋白衍生物(PPD)-脉冲抗原呈递细胞(APC)的增殖反应受损,尽管所有患者都接种了卡介苗。为了检验T细胞的这种低反应性是由T细胞功能障碍还是APC功能障碍引起的,本实验旨在评估患者或其父母的T细胞对来自患者或父母的ppd脉冲APC的增殖反应。这些组合似乎适合于评估T细胞或APC的活性,因为T细胞-APC相互作用至少需要HLA-D/DR抗原的部分身份。尽管来自对PPD表现出低反应性的患者的T细胞甚至对来自父母的PPD脉冲APC也没有反应,但来自父母的T细胞能够对来自患者的PPD脉冲APC以及自身的APC产生反应。这些观察结果强烈表明,儿童癌症患者对PPD的低反应性是由于T细胞功能障碍造成的,而APC的能力得到了充分的保留。换句话说,APC的能力似乎不受化疗、肿瘤细胞或其他因素的损害。抑制性T细胞似乎没有参与这种T细胞功能障碍。
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The capacity of antigen-presenting cells is fully preserved in childhood cancer patients.

T cells from 19 out of 25 childhood cancer patients showed impaired proliferative responses to purified protein derivatives (PPD)-pulsed antigen-presenting cells (APC) although all of the patients had been immunized with BCG. To test whether such low responsiveness of T cells results from the dysfunction of T cells or from that of APC, the experiment was designed to assess the proliferative response of T cells from patients or their parents to PPD-pulsed APC from patients or parents. These combinations seem to be suitable to assess the activity of T cells or APC since at least partial identity of HLA-D/DR antigens is required for T cell-APC interactions. Although T cells from patients who showed low responsiveness to PPD failed to respond even to PPD-pulsed APC from parents, T cells from parents were able to respond to PPD-pulsed APC from patients as well as to autologous APC. These observations strongly suggest that the low responsiveness to PPD in childhood cancer patients results from the dysfunction of T cells, and the capacity of APC is fully preserved. In other words, it appears that the capacity of APC is not impaired by chemotherapy, neoplastic cells, or other factors. Suppressor T cells appeared not to be involved in such dysfunction of T cells.

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Gan
Gan
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