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慢性淋巴细胞白血病中T细胞抗原的表达缺陷:与T细胞功能障碍的关系。

Defective expression of T cell antigens in chronic lymphocytic leukaemia: relationship to T cell dysfunction.

作者信息

Kay N E, Kaplan M E

出版信息

Br J Haematol. 1984 May;57(1):105-11. doi: 10.1111/j.1365-2141.1984.tb02870.x.

Abstract

In chronic lymphocytic leukaemia (CLL) peripheral blood T cells have a variety of functional abnormalities. To explore more extensively the T cell status of B-CLL patients, surface immunoglobulin-negative cells were isolated by sheep erythrocyte rosetting (ER) and the membrane phenotypes of the ER + cells defined by immunofluorescence utilizing monoclonal antibodies (MAb). In 11 of 18 CLL patients (CLL group I) there was excellent correlation between ER + and T3 (mature T cell marker) positivity. In the remaining patients (CLL group II), only 5-45% of ER + cells were T3 positive, suggesting that many rosetting cells were non-T. However, the ER +, T3 negative cells were nonreactive with OKM -1 (MAb which detects monocytes and 'null' lymphocytes) or with OKT11, 9.6, and 35.1, MAb against the T cell E receptor. Moreover ER +, T3 negative cells were not stained with OKT4, OKT8, OKT6, OKT9 , or OKT10 . Treatment of group II ER + cells with neuraminidase increased (from 27% to 74%) the mean percentages of T3 positive cells detected, but not other membrane antigens. ER + cells from group II patients, compared with normal and group I patients, exhibited diminished proliferative responses to PHA and Con-A (P less than 0.01) and supported poorly pokeweed mitogen-induced proliferation of normal allogeneic B cells (P less than 0.01). Thus, in approximately one-third of the CLL patients studied, many ER + cells poorly express a number of membrane antigens characteristic of normal mature T cells, one of which (T3) is unmasked by neuraminidase treatment. This phenotypic abnormality appears to be associated with significant T cell dysfunction in vitro and may, at least in part, contribute to the commonly encountered immunological defects present in these patients.

摘要

在慢性淋巴细胞白血病(CLL)中,外周血T细胞存在多种功能异常。为了更广泛地探究B - CLL患者的T细胞状态,通过绵羊红细胞玫瑰花结形成法(ER)分离出表面免疫球蛋白阴性细胞,并利用单克隆抗体(MAb)通过免疫荧光法确定ER +细胞的膜表型。在18例CLL患者中的11例(CLL第一组),ER +与T3(成熟T细胞标志物)阳性之间存在良好的相关性。在其余患者(CLL第二组)中,仅5% - 45%的ER +细胞为T3阳性,这表明许多玫瑰花结形成细胞并非T细胞。然而,ER +、T3阴性细胞与OKM -1(检测单核细胞和“裸”淋巴细胞的MAb)或与针对T细胞E受体的MAb OKT11、9.6和35.1无反应。此外,ER +、T3阴性细胞不被OKT4、OKT8、OKT6、OKT9或OKT10染色。用神经氨酸酶处理第二组的ER +细胞后,检测到的T3阳性细胞的平均百分比增加(从27%增至74%),但其他膜抗原未增加。与正常人和第一组患者相比,第二组患者的ER +细胞对PHA和Con - A的增殖反应减弱(P小于0.01),对商陆有丝分裂原诱导的正常同种异体B细胞增殖的支持能力也较差(P小于0.01)。因此,在所研究的大约三分之一的CLL患者中,许多ER +细胞很少表达正常成熟T细胞特有的多种膜抗原,其中一种(T3)可被神经氨酸酶处理后暴露出来。这种表型异常似乎与体外明显的T细胞功能障碍有关,并且可能至少部分地导致了这些患者中常见的免疫缺陷。

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