Lymphoblastic Leukaemia in Infants

Czech version

Authors: J. Starý ¹; P. Gajdoš ²; J. Trka ¹; V. Vávra ¹; J. Hak ³; V. Mihál ⁴; B. Blažek ⁵; H. Hrstková ⁶; O. Hrušák ⁷; K. Michalová ⁸; M. Jarošová ⁹; Y. Jabali ¹⁰
Authors‘ workplace: II. dětská klinika UK 2. LF a FN Motol, Praha, 2 Státní zdravotní ústav Praha, 3 Dětská klinika FN Hradec Králové, 4 Dětská klinika FN Olomouc, 5 Dětská klinika FN Ostrava, 6 I. dětská interní klinika FN Brno, 7 Ústav imunologie UK 2. LF a FN Motol, Praha ¹
Published in: Transfuze Hematol. dnes,, 2002, No. 2, p. 47-54.
Category:

Overview

The therapeutic results in children with acute lymphoblastic leukaemia (ALL)are improving continu-ously with modern treatment protocols of combined chemotherapy.Approximately 75 %children andadolescents can be cured from their leukaemia.Among infants younger than one year ALL is a raredisease.Typical infant ALL originates from very early precursors of B cells with a specific genotype,large leukaemic mass on diagnosis and high risk of early relapse.Between 1990 –2000,671 children andadolescents 0 –18 years old were diagnosed with ALL in the Czech Republic.Only 24 (3.6 %)of them wereinfants.Boys (n 16)predominated over girls (n 8)and 10 infants were younger than 6 months.ALLdeveloped from very early precursors of B cells (pro-B ALL)in 16 children,cALL was diagnosed in 7and T-ALL in one child,respectively.Cytogenetic and molecular genetic investigation revealed trans-location t(4;11)/fusion gene MLL-AF4 in 11 (45.8 %)patients.Fifteen children were treated according tothe protocol ALL-BFM 90,ALL-BFM 95 was used in one child and age-tailored schedules POG 9407 andInterfant 99 were used in 5 and 3 children,respectively.Therapeutic results were analyzed in 21 childrenbecause the follow-up of 3 children on the Interfant 99 protocol was too short.The 5-year event-free-survival (EFS)was 33 %(SE 10 %)with a median follow-up of 7.9 years.Children with ALL andt(4;11)/MLL-AF4 had a significantly inferior outcome (EFS 10 %)in comparison to children without thistranslocation (EFS 55 %;p 0,01).Boys achieved better therapeutic results (EFS 45 %)than girls (EFS12 %;p 0,007).The explanation of this difference is the higher incidence of t(4;11)in girls.Anotherimportant risk factor in our group was a slow early treatment response in 33 %infants.Poor responseto early therapy is found only in 10 %older children.Infant ALL is a rare disease with a worse prognosisthan ALL in older children due to the different biological properties of the leukaemic cells.

Key words:
acute lymphoblastic leukaemia,infants,t(4;11),fusion gene MLL-AF4

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Labels

Haematology Internal medicine Clinical oncology

Diagnosis and Treatment of Childhood Mature B-acute Lymphoblastic Leukaemia inthe Czech Republic in 1990 –2000

Laboratory Diagnosisof Heparin-induced Thrombocytopenia

Albumin – to be or not to be ((infused)?

International Consensus on the Definition of Invasive Mycotic InfectionsPatients with Malignant Mycotic Infections in Patients with Malignant Diseases andafter Transplantation of Haematopoietic Cells

Article was published in

Transfusion and Haematology Today

2002 Issue 2