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慢性Tγ淋巴细胞增多症和慢性T细胞肿瘤患者T细胞的功能特性

Functional properties of T cells in patients with chronic T gamma lymphocytosis and chronic T cell neoplasia.

作者信息

Rümke H C, Miedema F, ten Berge I J, Terpstra F, van der Reijden H J, van de Griend R J, de Bruin H G, von dem Borne A E, Smit J W, Zeijlemaker W P, Melief C J

出版信息

J Immunol. 1982 Jul;129(1):419-26.

PMID:6211484
Abstract

The expanded T cell populations of 10 patients with either T gamma lymphocytosis (five patients) or proven chronic T cell malignancy (five patients) were analyzed with respect to functional activity in vitro, including proliferative responses to mitogens, cytotoxic activity (killer [K] and natural killer [NK] cell activity), and regulatory activity on pokeweed mitogen- (PWM) induced immunoglobulin (Ig) synthesis (help and suppression) in comparison with marker phenotypes. In each of the five patients with T gamma lymphocytosis, only one out of three functionally distinct cell types was found: T gamma-K cells, T gamma-S cells, or T gamma-NK/K cells, which mediated K-cell activity, suppressive activity, and both NK and K cell activity, respectively. An expanded T gamma-K cell population was demonstrated in three patients with neutropenia with or without recurrent infections. T gamma-S cells were found in a patient with severe hypogammaglobulinemia, and T gamma-NK/K cells in one patient with asymptomatic lymphocytosis. T gamma-K and T gamma-S cells had a similar surface-marker profile (E+ or E-, Fc gamma+, OKT1-3+4-8+I1-M1-), whereas that of T gamma-NK/K cells was different (E+, Fc gamma+, OKT1-3-4-8-I1+M1+). Longitudinal studies of three untreated patients with T gamma-K lymphocytosis showed that the abnormalities were persistent but not progressive. In contrast, five patients with chronic T cell malignancy (two with T-CLL, two with cutaneous T cell lymphoma [CTCL], and one with T-PLL) all had progressive disease. The neoplastic cells in these cases were E+, Fc gamma-OKT1+4+6- with variable expression of the OKT3 and OKT8 markers. The only functional activity observed in these cells was suppressive activity by OKT3-4+8- cells from a patient with CTCL.

摘要

对10例患有Tγ淋巴细胞增多症(5例)或确诊为慢性T细胞恶性肿瘤(5例)患者的扩增T细胞群体进行了体外功能活性分析,包括对有丝分裂原的增殖反应、细胞毒性活性(杀伤[K]细胞和自然杀伤[NK]细胞活性),以及与标记表型相比,对商陆有丝分裂原(PWM)诱导的免疫球蛋白(Ig)合成的调节活性(辅助和抑制)。在5例Tγ淋巴细胞增多症患者中,每例仅发现三种功能不同的细胞类型中的一种:Tγ-K细胞、Tγ-S细胞或Tγ-NK/K细胞,它们分别介导K细胞活性、抑制活性以及NK和K细胞活性。在3例有或无反复感染的中性粒细胞减少症患者中证实存在扩增的Tγ-K细胞群体。在1例严重低丙种球蛋白血症患者中发现了Tγ-S细胞,在1例无症状淋巴细胞增多症患者中发现了Tγ-NK/K细胞。Tγ-K细胞和Tγ-S细胞具有相似的表面标记谱(E+或E-,Fcγ+,OKT1-3+4-8+I1-M1-),而Tγ-NK/K细胞的表面标记谱不同(E+,Fcγ+,OKT1-3-4-8-I1+M1+)。对3例未经治疗的Tγ-K淋巴细胞增多症患者的纵向研究表明,异常情况持续存在但无进展。相比之下,5例慢性T细胞恶性肿瘤患者(2例T细胞慢性淋巴细胞白血病、2例皮肤T细胞淋巴瘤[CTCL]和1例T细胞幼淋巴细胞白血病)均患有进展性疾病。这些病例中的肿瘤细胞为E+,Fcγ-OKT1+4+6-,OKT3和OKT8标记物表达可变。在这些细胞中观察到的唯一功能活性是来自1例CTCL患者的OKT3-4+8-细胞的抑制活性。

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