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人类T细胞急性淋巴细胞白血病的亚群衍生

Subset derivation of T-cell acute lymphoblastic leukemia in man.

作者信息

Reinherz E L, Nadler L M, Sallan S E, Schlossman S F

出版信息

J Clin Invest. 1979 Aug;64(2):392-7. doi: 10.1172/JCI109474.

Abstract

Normal human peripheral blood T cells can be characterized as belonging to either the TH+2 or TH-2 T-cell subset. Approximately 20% of T cells are TH+2, whereas 80% are TH-2 utilizing specific heteroantisera. To determine shether human T-cell acute lymphoblastic leukemia (T-ALL) cells belong to one or another T-cell subset, cell surface phenotyping was performed on tumor populations from 25 patients with T-ALL. Tmuor cells from these 25 individuals were either TH+1 or TH-2, but not both. 5 of 25 patients had TH+2 T-ALL cells. These TH+2 tumor populations were found exclusively in children and often without an accompanying thymic mass. TH-2 T-ALL, in contrast, occurred in both children and adults and was almost always associated with thymic enlargement. Although children with TH+2 T-ALL had as high or higher peripheral blast counts on presentation than their TH-2 T-ALL counterparts, overall survival was greater for the TH+2 group (greater than 36 mo) than the TH-2 group (less than 12 mo). These studies demonstrate that T-cell leukemias in man arise from distinct T-cell subsets and that cell surface characterization of T-cell malignancies may provide useful clinical data related to prognosis.

摘要

正常人类外周血T细胞可被分为TH+2或TH-2 T细胞亚群。利用特异性异种抗血清,约20%的T细胞为TH+2,而80%为TH-2。为确定人类T细胞急性淋巴细胞白血病(T-ALL)细胞属于哪种T细胞亚群,对25例T-ALL患者的肿瘤细胞群进行了细胞表面表型分析。这25例患者的肿瘤细胞要么是TH+1,要么是TH-2,不会同时兼具两者。25例患者中有5例具有TH+2 T-ALL细胞。这些TH+2肿瘤细胞群仅在儿童中发现,且通常无胸腺肿块。相比之下,TH-2 T-ALL在儿童和成人中均有发生,且几乎总是与胸腺肿大相关。虽然TH+2 T-ALL患儿初诊时外周血原始细胞计数与TH-2 T-ALL患儿相同或更高,但TH+2组的总生存期(大于36个月)长于TH-2组(小于12个月)。这些研究表明,人类T细胞白血病起源于不同的T细胞亚群,T细胞恶性肿瘤的细胞表面特征可能提供与预后相关的有用临床数据。

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