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婴儿急性淋巴细胞白血病初诊和复发时的独特基因型特征。

Unique genotypic features of infant acute lymphoblastic leukaemia at presentation and at relapse.

作者信息

Biondi A, Rossi V, di Celle P F, Carbone A, Benvestito S, Busca A, Giudici G, Giachino C, Basso G, Foa R

机构信息

Clinica Pediatrica Università di Milano, Monza, Italy.

出版信息

Br J Haematol. 1992 Apr;80(4):472-9. doi: 10.1111/j.1365-2141.1992.tb04560.x.

DOI:10.1111/j.1365-2141.1992.tb04560.x
PMID:1316141
Abstract

Acute lymphoblastic leukaemia (ALL) of infants aged less than 1 year represents a group of patients with peculiar biological features, poor response to therapy and unfavourable prognosis. In order better to characterize this type of leukaemia, we have investigated the immunoglobulin (Ig) and T-cell receptor (TCR) genes configuration of 21 infants with ALL, and compared the genotypic features with the phenotypic and karyotypic data, as well as with the clinical outcome. All cases had a pre-B phenotype; 12 (57%) of them were pre-pre-B ALL (CD10-, CD19+). Six of the 16 cases evaluated (38%) displayed chromosomal abnormalities; five had the typical translocation t(4;11)(q21;23). Eleven cases presented with a white blood cell count greater than 100 x 10(9)/l. The clinical course was unfavourable in 14 patients. The genotype of this group of ALL revealed several peculiarities. (1) Of the 21 cases, six (29%) displayed a multiple rearrangement pattern at the IgH locus. (2) In three cases (15%), the light chain genes were rearranged. (3) The TCR beta and gamma genes were rearranged in only one case (one case at the TCR beta and one at the TCR gamma locus). (4) The TCR delta chain was rearranged in eight cases (40%) and rarely deleted; the rearrangements observed were those most frequently observed in B cell-precursor ALL. Two cases were evaluated both at presentation and at relapse. While the immunophenotype had remained unmodified, comparison of Ig heavy chain gene rearrangements revealed clonal variations in both cases. Taken together, these findings further underline the biological peculiarities of infant ALL compared to ALL which occurs in older children and in adults, and stress the need of differentiated and aggressive therapeutic approach for these patients.

摘要

1岁以下婴儿的急性淋巴细胞白血病(ALL)代表了一组具有特殊生物学特征、对治疗反应不佳且预后不良的患者。为了更好地描述这种类型的白血病,我们研究了21例ALL婴儿的免疫球蛋白(Ig)和T细胞受体(TCR)基因构型,并将基因型特征与表型和核型数据以及临床结果进行了比较。所有病例均为前B表型;其中12例(57%)为前前B ALL(CD10-,CD19+)。16例评估病例中有6例(38%)显示染色体异常;5例有典型的t(4;11)(q21;23)易位。11例患者的白细胞计数大于100×10⁹/L。14例患者的临床病程不佳。这组ALL的基因型显示出几个特点。(1)21例中有6例(29%)在IgH位点呈现多重重排模式。(2)3例(15%)轻链基因发生重排。(3)TCRβ和γ基因仅在1例中发生重排(1例在TCRβ位点,1例在TCRγ位点)。(4)TCRδ链在8例(40%)中发生重排且很少缺失;观察到的重排是B细胞前体ALL中最常见的那些。2例在初诊和复发时均进行了评估。虽然免疫表型未改变,但Ig重链基因重排的比较显示两例均有克隆变异。综上所述,这些发现进一步强调了婴儿ALL与大龄儿童及成人ALL相比的生物学特殊性,并强调了对这些患者采用差异化和积极治疗方法的必要性。

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