Classification of pediatric acute lymphoblastic leukemia by gene expression profiling

Ross, Mary Elizabeth; Zhou, Xiaodong; Song, Guangchun; Shurtleff, Sheila; Girtman, Kevin; Williams, W. Kent; Liu, Hsi‐Che; Mahfouz, Rami; Raimondi, Susana C.; Lenny, Noel; Patel, Anami; Downing, James R.

doi:10.1182/blood-2003-01-0338

Cited by 510 publications

(523 citation statements)

References 35 publications

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“…For these analyses, we focused on the 52 patients with B-lineage ALL to avoid a distortion of results solely based on gene expression differences between ALL immunophenotypes. Pronounced differences in gene expression profiles between B-and T-lineage ALL have been described before and were confirmed by our data, supporting the notion that these ALL subtypes represent distinct biological and clinical entities (10,12).…”

Section: Resultssupporting

confidence: 77%

“…Therefore, we asked whether those gene expression signatures that predict genetic and immunologic subtypes in initial ALL (10,12) could also faithfully classify relapse samples based on the present analysis. To this end, published data from 104 initial ALL patients (10) were used as training set to recalculate the diagnostic signatures of the ALL subtypes shown in Table 1.…”

Section: Resultsmentioning

confidence: 99%

“…For classification of microarray expression profiles into discrete ALL subtypes, we used the nearest shrunken centroid methods by Tibshirani et al (24). The diagnostic signatures of initial ALL published by Ross et al (10) were recalculated on the jointly normalized data. For predicting the fraction of S and G 2 -M phase cells in samples based on gene expression profiles, we used least angle regression (25).…”

Section: Methodsmentioning

confidence: 99%

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Expression of Late Cell Cycle Genes and an Increased Proliferative Capacity Characterize Very Early Relapse of Childhood Acute Lymphoblastic Leukemia

Kirschner-Schwabe

Lottaz

Tödling

et al. 2006

Clinical Cancer Research

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Purpose: In childhood acute lymphoblastic leukemia (ALL), f25% of patients suffer from relapse. In recurrent disease, despite intensified therapy, overall cure rates of 40% remain unsatisfactory and survival rates are particularly poor in certain subgroups. The probability of long-term survival after relapse is predicted from well-established prognostic factors (i.e., time and site of relapse, immunophenotype, and minimal residual disease). However, the underlying biological determinants of these prognostic factors remain poorly understood. Experimental Design: Aiming at identifying molecular pathways associated with these clinically well-defined prognostic factors, we did gene expression profiling on 60 prospectively collected samples of first relapse patients enrolled on the relapse trial ALL-REZ BFM 2002 of the Berlin-Frankfurt-Mu« nster study group. Results: We show here that patients with very early relapse of ALL are characterized by a distinctive gene expression pattern.We identified a set of 83 genes differentially expressed in very early relapsed ALL compared with late relapsed disease. The vast majority of genes were up-regulated and many were late cell cycle genes with a function in mitosis. In addition, samples from patients with very early relapse showed a significant increase in the percentage of S and G 2 -M phase cells and this correlated well with the expression level of cell cycle genes. Conclusions: Very early relapse of ALL is characterized by an increased proliferative capacity of leukemic blasts and up-regulated mitotic genes.The latter suggests that novel drugs, targeting late cell cycle proteins, might be beneficial for these patients that typically face a dismal prognosis.Acute lymphoblastic leukemia (ALL) is the most common malignant disease in children (1). Although event-free survival rates range between 70% and 75%, relapse of ALL remains the fourth most frequent diagnosis in childhood cancer affecting 25% of ALL patients (2). At relapse, overall cure rates of f40% remain unsatisfactory and survival rates are particularly poor in certain subgroups (3). Treatment of relapse usually implies intensified polychemotherapy containing high-dose elements. Although in most children, second remissions can be induced high-risk patients require further treatment intensification by stem cell transplantation. Stem cell transplantation provides a better relapse-free survival rate than chemotherapy alone but is also associated with higher treatment-related morbidity and mortality rates (2). Thus, alternative treatment strategies are needed to improve the treatment and outcome of patients with relapsed ALL.In the treatment of ALL relapse, intensity of chemotherapy and stem cell transplantation are indicated by well-established prognostic factors (summarized in ref.2), with the most evident being the time to relapse. Early recurrence of disease with respect to frontline therapy affects f60% of patients and is associated with a high rate of nonresponse to treatment, shorter duration of second ...

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Section: Resultssupporting

confidence: 77%

Section: Resultsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

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Expression of Late Cell Cycle Genes and an Increased Proliferative Capacity Characterize Very Early Relapse of Childhood Acute Lymphoblastic Leukemia

Kirschner-Schwabe

Lottaz

Tödling

et al. 2006

Clinical Cancer Research

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“…61 In gene expression profiling (GEP) studies, MLL-rearranged cases clustered together as one group in AML as well as in ALL. 13,[62][63][64] However, our laboratory showed that within MLL-rearranged infant ALL each type of MLL translocation is associated with a translocation-specific gene expression signature. 65 We identified a specific gene expression signature for the total group of MLL-rearranged AML cases, 12 but were also able to identify a specific signature for t(9;11)(p22;q23).…”

Section: Epidemiology Of Mll Aberrations In Pediatric Amlmentioning

confidence: 90%

The heterogeneity of pediatric MLL-rearranged acute myeloid leukemia

et al. 2011

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Translocations involving the mixed-lineage leukemia (MLL) gene, localized at 11q23, comprise 15 to 20% of all pediatric acute myeloid leukemia (AML) cases. This review summarizes current knowledge about the etiology, biology, clinical characteristics and differences in outcome in MLL-rearranged pediatric AML. Furthermore, we discuss the role of cooperating events in MLL-rearranged pediatric AML, and future therapeutic strategies to improve outcome. We conclude that MLL-rearranged pediatric AML is a heterogeneous disease, and prognosis depends on various factors, for example, translocation partner, age, WBC and additional cytogenetic aberrations. The relationship of outcome with specific translocation partners requires that they be searched for in the diagnostic work-up of AML. To achieve further improvements in outcome, unraveling the biology of MLL-rearranged pediatric AML is warranted.

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“…Three (trisomy) or four (tetrasomy) copies of chromosome 21 is common in childhood acute lymphoblastic leukemia (ALL) [2][3][4]. Children with Down syndrome (DS) who carry trisomy 21 in all their cells have a 20-fold increased risk for childhood ALL and 600-fold risk for acute megakaryocytic leukemia (AMKL) [5].…”

Section: Aneuploidy Of Chromosome 21 and Acute Megakaryocytic Leukemiamentioning

confidence: 99%

Trisomy of chromosome 21 in leukemogenesis

Izraeli

Rainis

Hertzberg

et al. 2007

Blood Cells, Molecules, and Diseases

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Extra copies of chromosome 21 are often found in sporadic leukemias. Constitutional trisomy 21 of Down syndrome (DS) is associated with markedly increased risk for childhood leukemia. Thus the oncogenic role of trisomy 21 in the more common sporadic childhood leukemias may be revealed through the investigations of the relatively rare leukemias of DS. Recent studies of the megakaryoblastic leukemias of Down syndrome have uncovered a developmental leukemogenic mechanism characterized by a unique pre-natal collaboration between overexpressed genes from chromosome 21 and an acquired mutation in the transcription factor GATA1. The base of the markedly enhanced risk for acute lymphoblastic leukemia conferred by trisomy 21 is still unclear. Studies of the leukemias of DS are likely to contribute to the general understanding of the oncogenic mechanisms of chromosomal aneuploidies, the most common abnormalities in cancer.

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Classification of pediatric acute lymphoblastic leukemia by gene expression profiling

Cited by 510 publications

References 35 publications

Expression of Late Cell Cycle Genes and an Increased Proliferative Capacity Characterize Very Early Relapse of Childhood Acute Lymphoblastic Leukemia

Expression of Late Cell Cycle Genes and an Increased Proliferative Capacity Characterize Very Early Relapse of Childhood Acute Lymphoblastic Leukemia

The heterogeneity of pediatric MLL-rearranged acute myeloid leukemia

Trisomy of chromosome 21 in leukemogenesis

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