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免疫表型和免疫基因型分析在急性非淋巴细胞白血病中的临床相关性

Clinical relevance of immunophenotypic and immunogenotypic analysis in acute non-lymphoblastic leukaemia.

作者信息

Papadopoulos K P, Bagg A, Bezwoda W R, Mendelow B V

机构信息

Department of Haematology, School of Pathology, South African Institute for Medical Research, Johannesburg.

出版信息

S Afr Med J. 1989 Oct 7;76(7):335-8.

PMID:2552592
Abstract

Molecular biology is playing an increasing role in defining pathology today, and has clinical relevance in the routine work-up of patients with malignant diseases, especially those of the blood and lymphatic system. The majority of acute non-lymphoblastic leukaemias (ANLL) express specific myeloid differentiation markers and are terminal deoxynucleotidyl transferase (Tdt) negative. Rarely, some cases are Tdt+ and express the T-cell marker CD7. Although uncommon in Tdt-ANLL, there appears to be a significant incidence of T-cell receptor beta chain (TCR beta) and/or immunoglobulin heavy chain (IgH) gene rearrangements in Tdt+ ANLLs. We have investigated the immunogenotype of 39 patients with ANLL, including 28 from whom immunophenotypic data were available. Thirty-seven of 39 cases had germline IgH and TCR beta genes. Two cases, one with a myeloid/CD7+ CD2+ immunophenotype, had non-germline IgH gene arrangements detectable on Hind III digests only. The possibility of Hind III polymorphisms, or of true somatic gene rearrangement of the IgH gene in these patients, is discussed. Two additional cases had a Tdt+ CD7+ immunophenotype with germline IgH and TCR beta chain genes. Our results confirm the infrequent occurrence of IgH and TCR beta gene rearrangements in ANLL. Expression of Tdt and/or CD7, often in association with IgH gene rearrangements, would appear to identify a subgroup of ANLL patients that respond poorly to standard ANLL therapy and have a poorer prognosis. The diagnostic and prognostic importance of multiparametric analysis in ANLL is emphasised.

摘要

分子生物学在当今病理学的界定中发挥着越来越重要的作用,并且在恶性疾病患者,尤其是血液和淋巴系统疾病患者的常规检查中具有临床相关性。大多数急性非淋巴细胞白血病(ANLL)表达特定的髓系分化标志物,且末端脱氧核苷酸转移酶(Tdt)呈阴性。极少数情况下,一些病例Tdt呈阳性并表达T细胞标志物CD7。虽然在Tdt阴性的ANLL中不常见,但在Tdt阳性的ANLL中,T细胞受体β链(TCRβ)和/或免疫球蛋白重链(IgH)基因重排的发生率似乎较高。我们研究了39例ANLL患者的免疫基因型,其中28例有免疫表型数据。39例中有37例IgH和TCRβ基因为种系基因。2例患者,其中1例具有髓系/CD7+CD2+免疫表型,仅在Hind III酶切时可检测到非种系IgH基因重排。讨论了这些患者中Hind III多态性或IgH基因真正体细胞基因重排的可能性。另外2例患者具有Tdt+CD7+免疫表型,IgH和TCRβ链基因为种系基因。我们的结果证实了ANLL中IgH和TCRβ基因重排的发生率较低。Tdt和/或CD7的表达,通常与IgH基因重排相关,似乎可识别出一组对标准ANLL治疗反应不佳且预后较差的ANLL患者。强调了多参数分析在ANLL诊断和预后中的重要性。

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