Relapse prediction in acute myeloid leukaemia patients in complete remission using <i>WT1</i> as a molecular marker: development of a mathematical model to predict time from molecular to clinical relapse and define optimal sampling intervals

Ommen, Hans Beier; Nyvold, Charlotte Guldborg; Brændstrup, Karin; Andersen, Bodil Lind; Ommen, Ingrid Beier; Hasle, Henrik; Hokland, Peter; Østergaard, Mette

doi:10.1111/j.1365-2141.2008.07132.x

Cited by 67 publications

(94 citation statements)

References 33 publications

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“…59 Furthermore, the significance of normalized WT-1 expression levels post induction therapy was less clear, as 21 of 48 these patients relapsed. These findings are supported by Ommen et al 60 The available studies indicate that WT-1 levels above normal levels, which may be seen in normal regenerating marrow, are associated with subsequent relapse. These data are supported by finding them to correlate with disease-specific fusion gene transcript numbers.…”

Section: © F E R R a T A S T O R T I F O U N D A T I O Nsupporting

confidence: 79%

How and why minimal residual disease studies are necessary in leukemia: a review from WP10 and WP12 of the European LeukaemiaNet

Béné

Kaeda²

2009

Haematologica

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Resistance to therapeutic agents is a major factor in the failure of cancer treatments. In leukemia, the resistant cells remaining in the bone marrow and/or peripheral blood constitute minimal residual disease and are detectable by highly sensitive assays when the patient appears to be in complete remission. Early detection of the expansion of residual cells permits clinical intervention with the aim of reversing the proliferation of resistant leukemic cells. Therefore, accurate and precise measurement of minimal residual disease can greatly enhance optimization of oncology patients' clinical management. This notion is supported by a large body of data among chronic myeloid leukemia patients, but minimal residual disease detection and monitoring is increasingly applied to other types of leukemia, and is starting to be a factor in decision-making for some therapeutic trials in childhood acute lymphoblastic leukemia. Here, from the solid ground of minimal residual disease detection in chronic myeloid leukemia, the current state of the art and development of molecular techniques in other leukemias and the growing field of multiparameter flow cytometry are reviewed in two separate parts reporting on the respective advances, advantages and pitfalls of these emerging methods.Key words: minimal residual disease, leukemia, flow cytometry, standardization, monitoring. LeukaemiaNet. Haematologica 2009;94:1135-1150. doi:10.3324/haematol.2008 Citation: Béné MC and Kaeda JS. How and why minimal residual disease studies are necessary in leukemia: a review from WP10 and WP12 of the European

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Section: © F E R R a T A S T O R T I F O U N D A T I O Nsupporting

confidence: 79%

How and why minimal residual disease studies are necessary in leukemia: a review from WP10 and WP12 of the European LeukaemiaNet

Béné

Kaeda²

2009

Haematologica

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“…WT1 mRNA from PB detected MRD more sharply than the morphological findings of bone marrow aspiration. It has been reported that WT1 mRNA expression is a general molecular marker in leukemia (Inoue et al 1996;Cilloni et al 2002Cilloni et al , 2004Cilloni et al , 2008Lapillonne et al 2006;Ommen et al 2008). It is important to measure WT1 mRNA at any time, at diagnosis or in CR.…”

Section: Discussionmentioning

confidence: 99%

WT1 mRNA Level in Peripheral Blood Is a Sensitive Biomarker for Monitoring Minimal Residual Disease in Acute Myeloid Leukemia

Sakamoto

Mariya

Sasaki

et al. 2009

Tohoku J. Exp. Med.

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“…This approach requires the selection of a specific peptide epitope. In general, to enhance antigen immunoreactivity, the peptide should have strong hydrophilicity and a stable conformation, and either end of the peptide should be linear to maximize its availability for antibody binding (5,7). Using this criterion, we selected a 14-amino acid sequence (CALWVSGIFVDEVI) at the N-terminus of the FAMLF protein that was predicted to have high hydrophilicity, be readily accessible to antibody, and be specific to FAMLF, thereby reducing the likelihood of non-specific binding.…”

Section: Discussionmentioning

confidence: 99%

Protein expression and subcellular localization of familial acute myelogenous leukemia-related factor

Huang

Chen

et al. 2013

Oncology Reports

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Abstract. The present study was designed to evaluate the expression and subcellular distribution of the familial acute myelogenous leukemia-related factor (FAMLF). A 14-amino acid epitope of the predicted open reading frame of the FAMLF gene was identified using bioinformatics. This polypeptide was synthesized, conjugated to keyhole limpet hemocyanin and was subsequently used to produce antibodies. The antibody titer and specificity were characterized using ELISA and western blot assays, respectively. The antibody detected FAMLF protein expression in several human leukemia cell lines, bone marrow cells derived from one acute myeloid leukemia patient and one chronic myeloid leukemia patient, but not in bone marrow cells of healthy subjects. The FAMLF/ GFP fusion protein was expressed in both the nucleus and the cytoplasm of transfected NIH3T3 cells. Our results demonstrate that the FAMLF gene is expressed in an AML patient but not in healthy controls, suggesting its association with AML. IntroductionAcute myeloid leukemia (AML) is the most common hematological malignancy in adults, with a worldwide incidence of ~3.6 cases in 100,000 individuals (National Cancer Institute. SEER Stat Fact Sheets: Acute Myeloid Leukemia; http://seer. cancer.gov/statfacts/html/amyl.html). A number of AMLrelated chromosomal abnormalities and gene mutations have been identified, and their involvement in the regulation of DNA methylation, signal transduction, energy synthesis, and cellular structure has been reported (1).The identification of new AML-related genes may provide insight into disease prognosis, treatment response, and new therapeutic regimens for patients with AML. Mutations in CCAAT enhancer binding factor α (CEBPA) have been associated with prolonged recurrence-free survival in AML patients (2). Mutations in nucleophosmin-1 (NPM1) and the internal tandem duplications in FLT3 predict positive AML prognosis (3), and mutations in several genes such as MLL-PTD, FLT3/ITD, WT1, and C-KIT predict negative AML prognosis (4-7). Thus, screening for mutations in CEBPA, NPM1, FLT3, and KIT is part of the routine workup for AML (8,9).A number of drugs targeting AML-related genes have been tested for their efficacy in treating AML, including TNF-related apoptosis inducing ligand (TRAIL) and tipifarnib, an inhibitor of farnesyltransferase (FTase), alone or in combination with other anti-leukemia drugs (10,11). Inhibitors of histone deacetylase, proteasome and Bcl-2 antisense oligonucleotides have also been used as targeted drugs in the clinical treatment of AML (12). Furthermore, inhibitors of Fms-like tyrosine kinase 2 (FLT-2), such as lestaurtinib (CEP701), tandutinib (MLN518) and PKC412 have shown benefit in treating FLT3-associated AML (13).Previously, we identified a large family with a high incidence of AML in Fujian China (14). A total of 11 family members in 4 generations were diagnosed with AML; two patients developed acute erythroleukemia (M6), one suffered from minimally differentiated acute myeloblastic leukemia (M1), one ha...

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Relapse prediction in acute myeloid leukaemia patients in complete remission using WT1 as a molecular marker: development of a mathematical model to predict time from molecular to clinical relapse and define optimal sampling intervals

Cited by 67 publications

References 33 publications

How and why minimal residual disease studies are necessary in leukemia: a review from WP10 and WP12 of the European LeukaemiaNet

How and why minimal residual disease studies are necessary in leukemia: a review from WP10 and WP12 of the European LeukaemiaNet

WT1 mRNA Level in Peripheral Blood Is a Sensitive Biomarker for Monitoring Minimal Residual Disease in Acute Myeloid Leukemia

Protein expression and subcellular localization of familial acute myelogenous leukemia-related factor

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