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使用单克隆抗Tn抗体和免疫组织化学方法检测白血病中的Tn抗原。

Detection of the Tn antigen in leukaemia using monoclonal anti-Tn antibody and immunohistochemistry.

作者信息

Roxby D J, Morley A A, Burpee M

机构信息

Department of Haematology, Flinders Medical Centre, Bedford Park, South Australia.

出版信息

Br J Haematol. 1987 Oct;67(2):153-6. doi: 10.1111/j.1365-2141.1987.tb02319.x.

Abstract

Exposure of the normally cryptic Tn antigen on haemopoietic cells leading to erythrocyte polyagglutination has been reported in a few cases of malignant or premalignant haemopoietic disorders and has been attributed to a selective deficiency of the enzyme 3-beta-D-galactosyl-transferase. A male patient presented with acute myelomonocytic leukaemia with no evidence of Tn expression but, 16 months later, in the terminal stage of the disease, the majority of the erythrocytes were found to be polyagglutinable. Tn expression was confirmed by the use of lectins and by agglutination with a Tn-specific monoclonal antibody, FBT3. Retrospective studies of stored blood and bone marrow smears were performed by immunocytochemistry using FBT3. Tn positive cells were first detected in the marrow 8 months prior to death. They increased progressively in number and, in the terminal illness, over 90% of erythroid precursors in the marrow and erythrocytes in peripheral blood and 40% of granulocyte precursors of the marrow and 10% of granulocytes in the blood were Tn positive. These observations suggest that Tn expression was present in a subclone of cells which became dominant during the course of the disease and that there may be a relationship between Tn expression and leukaemic progression.

摘要

在少数恶性或癌前造血系统疾病病例中,已报道造血细胞上正常隐匿的Tn抗原暴露会导致红细胞多凝集现象,这归因于3-β-D-半乳糖基转移酶的选择性缺乏。一名男性患者初诊为急性粒单核细胞白血病,无Tn表达证据,但16个月后,在疾病终末期,发现大多数红细胞具有多凝集性。通过使用凝集素以及与Tn特异性单克隆抗体FBT3凝集反应,证实了Tn表达。使用FBT3通过免疫细胞化学对储存的血液和骨髓涂片进行回顾性研究。Tn阳性细胞在死亡前8个月首次在骨髓中被检测到。它们的数量逐渐增加,在终末期疾病中,骨髓中超过90%的红系前体细胞、外周血中的红细胞以及骨髓中40%的粒细胞前体细胞和血液中10%的粒细胞为Tn阳性。这些观察结果表明,Tn表达存在于疾病过程中占主导地位的细胞亚克隆中,并且Tn表达与白血病进展之间可能存在关联。

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