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滤泡增生和滤泡中心细胞淋巴瘤中的T细胞:T细胞受体相关CD3抗原的免疫超微结构研究

T-cells in follicular hyperplasia and follicular center-cell lymphomas: an immunoultrastructural study of the T-cell receptor-associated CD3 antigen.

作者信息

Angermeier P A, Hartman A L, Swerdlow S H

机构信息

Department of Pathology and Laboratory Medicine, University of Cincinnati College of Medicine, Ohio 45267.

出版信息

J Histochem Cytochem. 1987 Dec;35(12):1433-8. doi: 10.1177/35.12.2960729.

DOI:10.1177/35.12.2960729
PMID:2960729
Abstract

T-cells are an integral part of normal follicular centers and many follicular center-cell (FCC) lymphomas. Because the functional role of these cells remains imprecisely determined and because ultrastructural localization of the T-cell antigen receptor-associated CD3 antigen has not been previously reported, an immunoultrastructural study of four tonsils and four FCC lymphomas was performed using an anti-CD3 antibody (UCHT-1). Normal interfollicular CD3-positive T-cells always demonstrated surface membrane positivity, as did 94% of normal and 88% of neoplastic FCC-associated CD3-positive cells. Conversely, whereas only 5% of normal interfollicular CD3-positive cells showed perinuclear positivity, 58% of normal and 38% of neoplastic FCC-associated CD3-positive cells did (p less than 0.001). Definite endoplasmic reticulum (ER) staining for CD3 was identified in 4% and 8% of cells associated with normal or neoplastic FCC, respectively, but in none of the T-zone lymphocytes. Because the perinuclear space is reported to be a site of protein synthesis in cells with little ER, and because of the occasional ER staining observed in cells with perinuclear staining, perinuclear CD3 positivity probably represents CD3 synthesis in mature tonsillar T-cells. The frequency of perinuclear positivity in the FCC-associated T-cells, together with the loss of surface positivity in some cells at this site, suggests that this could represent in vivo T-cell "activation" in follicular centers, with modulation and resynthesis of the CD3 antigen. Furthermore, the results demonstrate a similar phenomenon in the T-cells associated with neoplastic follicular center cells.

摘要

T细胞是正常滤泡中心和许多滤泡中心细胞(FCC)淋巴瘤的一个组成部分。由于这些细胞的功能作用仍未明确确定,且T细胞抗原受体相关CD3抗原的超微结构定位此前尚未见报道,因此使用抗CD3抗体(UCHT-1)对4个扁桃体和4例FCC淋巴瘤进行了免疫超微结构研究。正常滤泡间CD3阳性T细胞总是表现为表面膜阳性,正常FCC相关CD3阳性细胞的94%和肿瘤性FCC相关CD3阳性细胞的88%也是如此。相反,虽然正常滤泡间CD3阳性细胞仅有5%显示核周阳性,但正常FCC相关CD3阳性细胞的58%和肿瘤性FCC相关CD3阳性细胞的38%显示核周阳性(P<0.001)。在与正常或肿瘤性FCC相关的细胞中,分别有4%和8%的细胞确定有内质网(ER)CD3染色,但在T区淋巴细胞中均未发现。由于据报道核周间隙是内质网较少的细胞中蛋白质合成的部位,且在有核周染色的细胞中偶尔观察到内质网染色,因此核周CD3阳性可能代表成熟扁桃体T细胞中CD3的合成。FCC相关T细胞中核周阳性的频率,以及该部位一些细胞表面阳性的丧失,表明这可能代表滤泡中心的体内T细胞“激活”,伴有CD3抗原的调节和再合成。此外,结果显示在与肿瘤性滤泡中心细胞相关的T细胞中也有类似现象。

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