Your search keyword '"Diana J. Slater"' showing total 19 results

1. A novel <scp> MBTPS2 </scp> variant associated with <scp>BRESHECK</scp> syndrome impairs <scp>sterol‐regulated</scp> transcription and the endoplasmic reticulum stress response

Author

Alanna Strong, Christopher J. Cardinale, Deborah Watson, Hakon Hakonarson, Jamie Merves, Cuiping Hou, Sophia E. Kim, Lawrence Copelovitch, Jeffrey T. Billheimer, Leslie Raffini, Elaine H. Zackai, Hilary B. Whitworth, Diana J. Slater, Michael E. March, Courtney Vaccaro, and Christopher Larosa

Subjects

Photophobia, Ichthyosis, business.industry, Endoplasmic reticulum, medicine.disease, Phenotype, Immunology, Genetics, Unfolded protein response, medicine, Missense mutation, medicine.symptom, business, Transcription factor, Genetics (clinical), Exome sequencing

Abstract

Ichthyosis follicularis, atrichia, and photophobia syndrome (IFAP syndrome) is a rare, X-linked disorder caused by pathogenic variants in membrane-bound transcription factor protease, site 2 (MBTPS2). Pathogenic MBTPS2 variants also cause BRESHECK syndrome, characterized by the IFAP triad plus intellectual disability and multiple congenital anomalies. Here we present a patient with ichthyosis, sparse hair, pulmonic stenosis, kidney dysplasia, hypospadias, growth failure, thrombocytopenia, anemia, bone marrow fibrosis, and chronic diarrhea found by research-based exome sequencing to harbor a novel, maternally inherited MBTPS2 missense variant (c.766 G>A; (p.Val256Leu)). In vitro modeling supports variant pathogenicity, with impaired cell growth in cholesterol-depleted media, attenuated activation of the sterol regulatory element-binding protein pathway, and failure to activate the endoplasmic reticulum stress response pathway. Our case expands both the genetic and phenotypic spectrum of BRESHECK syndrome to include a novel MBTPS2 variant and cytopenias, bone marrow fibrosis, and chronic diarrhea.

Published

2021

2. A new syndrome of moyamoya disease, kidney dysplasia, aminotransferase elevation, and skin disease associated with de novo variants in <scp> RNF213 </scp>

Author

Cuiping Hou, Kathleen M. Loomes, Erum A. Hartung, Diana J. Slater, Tamir Diamond, Courtney Vaccaro, Sanmati Cuddapah, Alanna Strong, Evelyn K. Shih, Anne Marie Cahill, Gina O'Grady, Deborah Watson, Jonathan R Bishop, Hakon Hakonarson, Dong Li, and William Wong

Subjects

0301 basic medicine, Pathology, medicine.medical_specialty, Angiogenesis, Disease, 030105 genetics & heredity, elevated aminotransferases, Clinical Reports, 03 medical and health sciences, Genetics, medicine, Genetic predisposition, Missense mutation, Erythema multiforme, Moyamoya disease, Genetics (clinical), Exome sequencing, Clinical Report, RNF213, kidney dysplasia, business.industry, erythema multiforme, medicine.disease, 030104 developmental biology, moyamoya disease, business, Kidney disease

Abstract

Ring‐finger protein 213 (RNF213) encodes a protein of unknown function believed to play a role in cellular metabolism and angiogenesis. Gene variants are associated with susceptibility to moyamoya disease. Here, we describe two children with moyamoya disease who also demonstrated kidney disease, elevated aminotransferases, and recurrent skin lesions found by exome sequencing to have de novo missense variants in RNF213. These cases highlight the ability of RNF213 to cause Mendelian moyamoya disease in addition to acting as a genetic susceptibility locus. The cases also suggest a new, multi‐organ RNF213‐spectrum disease characterized by liver, skin, and kidney pathology in addition to severe moyamoya disease caused by heterozygous, de novo C‐terminal RNF213 missense variants.

Published

2021

3. Single Cell Transcriptome Analysis of Peripheral Blood Mononuclear Cells in Freshly Isolated versus Stored Blood Samples

Author

Hui-Qi Qu, Charlly Kao, James Garifallou, Fengxiang Wang, James Snyder, Diana J. Slater, Cuiping Hou, Michael March, John J. Connolly, Joseph T. Glessner, and Hakon Hakonarson

Subjects

AP-1, NF-kB, peripheral blood mononuclear cells, single cell RNA-seq, Genetics, Genetics (clinical)

Abstract

Background: Peripheral blood mononuclear cells (PBMCs) are widely used as a model in the study of different human diseases. There is often a time delay from blood collection to PBMC isolation during the sampling process, which can result in an experimental bias, particularly when performing single cell RNA-seq (scRNAseq) studies. Methods: This study examined the impact of different time periods from blood draw to PBMC isolation on the subsequent transcriptome profiling of different cell types in PBMCs by scRNAseq using the 10X Chromium Single Cell Gene Expression assay. Results: Examining the five major cell types constituting the PBMC cell population, i.e., CD4+ T cells, CD8+ T cells, NK cells, monocytes, and B cells, both common changes and cell-type-specific changes were observed in the single cell transcriptome profiling over time. In particular, the upregulation of genes regulated by NF-kB in response to TNF was observed in all five cell types. Significant changes in key genes involved in AP-1 signaling were also observed. RBC contamination was a major issue in stored blood, whereas RBC adherence had no direct impact on the cell transcriptome. Conclusions: Significant transcriptome changes were observed across different PBMC cell types as a factor of time from blood draw to PBMC isolation and as a consequence of blood storage. This should be kept in mind when interpreting experimental results.

Published

2023

4. KMT2A‐MAML2 rearrangement emerged and regressed during neuroblastoma therapy without leukemia after 12.8‐year follow‐up

Author

Carolyn A. Felix, Xiang Yu, Marilyn M. Li, James W Davenport, Eric F. Rappaport, Nai-Kong V. Cheung, Brian D. Gregory, and Diana J. Slater

Subjects

Oncology, medicine.medical_specialty, DNA damage, medicine.medical_treatment, Article, Neuroblastoma, Internal medicine, medicine, Humans, Etoposide, Gene Rearrangement, Chemotherapy, Leukemia, Therapy Related Leukemia, biology, business.industry, Histone-Lysine N-Methyltransferase, Hematology, medicine.disease, Regimen, KMT2A, Pediatrics, Perinatology and Child Health, Trans-Activators, biology.protein, business, Myeloid-Lymphoid Leukemia Protein, Follow-Up Studies, Transcription Factors

Abstract

Twelve patients without therapy-related leukemia were studied after completing TOP2 poison chemotherapy in a high-risk neuroblastoma regimen. One patient harbored an inv(11) that was a KMT2A rearrangement. The KMT2A-MAML2 transcript was expressed at low level. The patient was prospectively followed. The inv(11) was undetectable in ensuing samples. Leukemia never developed after a 12.8-year follow-up period. Enriched etoposide-induced TOP2A cleavage in the relevant MAML2 genomic region supports a TOP2A DNA damage mechanism. After completing TOP2 poison chemotherapies, covert KMT2A-R clones may occur in a small minority of patients; however, not all KMT2A rearrangements herald a therapy-related leukemia diagnosis.

Published

2021

5. BglII-based panhandle and reverse panhandle PCR approaches increase capability for cloning der(II) and der(other) genomic breakpoint junctions ofMLL translocations

Author

Carolyn A. Felix, Diana J. Slater, and Blaine W. Robinson

Subjects

endocrine system, Cancer Research, Adolescent, Molecular Sequence Data, Models, Biological, Polymerase Chain Reaction, Translocation, Genetic, Restriction fragment, Exon, chemistry.chemical_compound, Bacterial Proteins, hemic and lymphatic diseases, Genetics, Humans, Cloning, Molecular, Deoxyribonucleases, Type II Site-Specific, neoplasms, Gene, BglII, Base Sequence, Models, Genetic, biology, Oligonucleotide, Chromosomes, Human, Pair 11, Breakpoint, Chromosome Breakage, Precursor Cell Lymphoblastic Leukemia-Lymphoma, biochemical phenomena, metabolism, and nutrition, Molecular biology, Sense strand, chemistry, biology.protein, bacteria, Chromosomes, Human, Pair 6, Chromosomes, Human, Pair 4, Myeloid-Lymphoid Leukemia Protein, DNA

Abstract

Panhandle PCR techniques to amplify known sequence flanked by unknown sequence have been useful for MLL genomic breakpoint junctions and fusion transcripts because MLL has a large number of partner genes. However, genomic panhandle PCR approaches are impeded when the restriction fragment that contains the breakpoint junction is too large to amplify. We devised new panhandle PCR approaches for MLL genomic breakpoint junctions that create the template from BglII restriction fragments by attaching MLL sequence to a BglII site in the partner gene. This leads to the annealing of MLL and its complement in the handle and creates an intrastrand loop containing the breakpoint junction sequence for amplification with primers all from MLL. BglII panhandle PCR for der(11) breakpoint junctions was accomplished by ligating a phosphorylated oligonucleotide containing a BglII overhang and sequence complementary to MLL exon 7 to the 3′ ends of BglII digested DNA, and forming the template from the sense strand of DNA. In BglII reverse panhandle PCR for der(other) breakpoint junctions, a phosphorylated oligonucleotide containing a BglII overhang and the complement of antisense sequence in MLL exon 10 was ligated to the 3′ ends of BglII digested DNA, and the template was formed from the antisense strand of DNA. These approaches amplified 5′-MLL-MLLT4-3′ and 5′-AFF1-MLL-3′ breakpoint junctions. The former is significant because few t(6;11) genomic breakpoint junctions have been sequenced. BglII panhandle PCR approaches increase the possibilities for cloning MLL genomic breakpoint junctions where there is heterogeneity in partner genes and breakpoint locations. © 2006 Wiley-Liss, Inc.

Published

2006

6. Low NAD(P)H:quinone oxidoreductase activity is associated with increased risk of leukemia with MLL translocations in infants and children

Author

Luca Lo Nigro, Diana J. Slater, Yunxia Wang, Christine F. Skibola, Carolyn A. Felix, Peter C. Nowell, Beverly J. Lange, and Martyn T. Smith

Subjects

Male, Oncology, Chromosomal translocation, Biochemistry, Translocation, Genetic, Risk Factors, hemic and lymphatic diseases, Genotype, Ethnicity, NAD(P)H Dehydrogenase (Quinone), Odds Ratio, Genetics, education.field_of_study, Leukemia, Hematology, Precursor Cell Lymphoblastic Leukemia-Lymphoma, Neoplasm Proteins, DNA-Binding Proteins, Leukemia, Myeloid, Child, Preschool, Acute Disease, Neoplastic Stem Cells, Myeloid-Lymphoid Leukemia Protein, Female, medicine.medical_specialty, Immunology, Population, Mutation, Missense, Biology, Internal medicine, Proto-Oncogenes, medicine, Humans, Point Mutation, Genetic Predisposition to Disease, education, Chromosomes, Human, Pair 11, Infant, Newborn, Cytogenetics, Infant, Histone-Lysine N-Methyltransferase, Cell Biology, Odds ratio, medicine.disease, Infant Acute Lymphoblastic Leukemia, Amino Acid Substitution, Chromosomes, Human, Pair 18, Transcription Factors

Abstract

An inactivating polymorphism at position 609 in the NAD(P)H:quinone oxidoreductase 1 gene (NQO1 C609T) is associated with an increased risk of adult leukemia. A small British study suggested thatNQO1 C609T was associated with an increased risk of infant leukemias with MLL translocations, especially infant acute lymphoblastic leukemia (ALL) with t(4;11). We explored NQO1 C609Tas a genetic risk factor in 39 pediatric de novo and 18 pediatric treatment-related leukemias with MLL translocations in the United States. Children with de novo B-lineage ALL withoutMLL translocations and a calculation of the expected genotype distribution in an ethnically matched population of disease-free subjects served as the comparison groups. Patients with de novo leukemias with MLL translocations were significantly more likely to be heterozygous at NQO1 C609T (odds ratio [OR] = 2.77, 95% confidence intervals [CI] 1.17-6.57;P = .02), and significantly more likely to have low/null NQO1 activity than patients with de novo B-lineage ALL withoutMLL translocations (OR = 2.47, 95% CI 1.08-5.68;P = .033). They were also significantly more likely to have low/null NQO1 activity than expected in an ethnically matched population of disease-free subjects (OR = 2.50,P = .02). Infants younger than 12 months old at diagnosis of leukemia with t(4;11) were most likely to have low/null NQO1 activity (OR > 10.0). Conversely, the distribution ofNQO1 genotypes among patients with treatment-related leukemias with MLL translocations was not statistically different than in the comparison groups. The inactivating NQO1polymorphism is associated with an increased risk of de novo leukemia with MLL translocations in infants and children.

Published

2002

7. MLL-SEPTIN6 fusion recurs in novel translocation of chromosomes 3, X, and 11 in infant acute myelomonocytic leukaemia and in t(X;11) in infant acute myeloid leukaemia, and MLL genomic breakpoint in complex MLL-SEPTIN6 rearrangement is a DNA topoisomerase II cleavage site

Author

Narayan R. Shah, Rita G Meek, Reshma S Autar, Diana J. Slater, Eric F. Rappaport, Wendy Reed Williams, Carolyn A. Felix, Brian D. Lovett, Thomas Ried, Neil Osheroff, and Eva Hilgenfeld

Subjects

Cancer Research, X Chromosome, Molecular Sequence Data, Chromosomal translocation, Biology, Leukemia, Myelomonocytic, Acute, Translocation, Genetic, Exon, GTP-Binding Proteins, hemic and lymphatic diseases, Proto-Oncogenes, Genetics, Humans, neoplasms, Molecular Biology, In Situ Hybridization, Fluorescence, X chromosome, Southern blot, Base Sequence, Chromosomes, Human, Pair 11, Breakpoint, Chromosome Mapping, Infant, Chromosome Breakage, Histone-Lysine N-Methyltransferase, Molecular biology, DNA-Binding Proteins, Cytoskeletal Proteins, DNA Topoisomerases, Type II, Fusion transcript, Chromosome 3, Leukemia, Myeloid, Acute Disease, Chromosomes, Human, Pair 3, Chromosome breakage, Myeloid-Lymphoid Leukemia Protein, Septins, Transcription Factors

Abstract

We examined the MLL translocation in two cases of infant AML with X chromosome disruption. The G-banded karyotype in the first case suggested t(X;3)(q22;p21)ins(X;11)(q22;q13q25). Southern blot analysis showed one MLL rearrangement. Panhandle PCR approaches were used to identify the MLL fusion transcript and MLL genomic breakpoint junction. SEPTIN6 from chromosome band Xq24 was the partner gene of MLL. MLL exon 7 was joined in-frame to SEPTIN6 exon 2 in the fusion transcript. The MLL genomic breakpoint was in intron 7; the SEPTIN6 genomic breakpoint was in intron 1. Spectral karyotyping revealed a complex rearrangement disrupting band 11q23. FISH with a probe for MLL confirmed MLL involvement and showed that the MLL-SEPTIN6 junction was on the der(X). The MLL genomic breakpoint was a functional DNA topoisomerase II cleavage site in an in vitro assay. In the second case, the karyotype revealed t(X;11)(q22;q23). Southern blot analysis showed two MLL rearrangements. cDNA panhandle PCR detected a transcript fusing MLL exon 8 in-frame to SEPTIN6 exon 2. MLL and SEPTIN6 are vulnerable to damage to form recurrent translocations in infant AML. Identification of SEPTIN6 and the SEPTIN family members hCDCrel and MSF as partner genes of MLL suggests a common pathway to leukaemogenesis.

Published

2002

8. Panhandle and reverse-panhandle PCR enable cloning of der(11) and der(other) genomic breakpoint junctions ofMLLtranslocations and identify complex translocation ofMLL,AF-4, andCDK6

Author

Jaclyn A. Biegel, Peter C. Nowell, Carolyn A. Felix, Eric F. Rappaport, Beverly J. Lange, Luca Lo Nigro, Nai-Kong V. Cheung, Leslie Raffini, and Diana J. Slater

Subjects

Derivative chromosome, Molecular Sequence Data, Chromosomal translocation, Protein Serine-Threonine Kinases, Biology, Polymerase Chain Reaction, Translocation, Genetic, hemic and lymphatic diseases, Proto-Oncogenes, Humans, Cloning, Molecular, neoplasms, Gene, Gene Rearrangement, Genetics, Multidisciplinary, Base Sequence, Chromosomes, Human, Pair 11, Breakpoint, Intron, Nuclear Proteins, Cyclin-Dependent Kinase 6, Histone-Lysine N-Methyltransferase, Biological Sciences, Fusion protein, Molecular biology, Cyclin-Dependent Kinases, Infant Acute Lymphoblastic Leukemia, DNA-Binding Proteins, Non-homologous end joining, Female, Chromosomes, Human, Pair 4, Transcriptional Elongation Factors, Myeloid-Lymphoid Leukemia Protein, Transcription Factors

Abstract

We used panhandle PCR to clone the der(11) genomic breakpoint junction in three leukemias with t(4;11) and devised reverse-panhandle PCR to clone the breakpoint junction of the other derivative chromosome. This work contributes two elements to knowledge onMLLtranslocations. First is reverse-panhandle PCR for cloning breakpoint junctions of the other derivative chromosomes, sequences of which are germane to understanding theMLLtranslocation process. The technique revealed duplicated sequences in one case of infant acute lymphoblastic leukemia (ALL) and small deletions in a case of treatment-related ALL. The second element is discovery of a three-way rearrangement ofMLL,AF-4, andCDK6in another case of infant ALL. Cytogenetic analysis was unsuccessful at diagnosis, but suggested t(4;11) and del(7)(q21q31) at relapse. Panhandle PCR analysis of the diagnostic marrow identified a breakpoint junction ofMLLintron 8 andAF-4intron 3. Reverse-panhandle PCR identified a breakpoint junction ofCDK6from band 7q21-q22 andMLLintron 9.CDK6encodes a critical cell cycle regulator and is the first gene of this type disrupted byMLLtranslocation. Cdk6 is overexpressed or disrupted by translocation in many cancers. The in-frameCDK6-MLLtranscript is provocative with respect to a potential contribution of the predicted Cdk6-MLL fusion protein in the genesis of the ALL, which also contains an in-frameMLL-AF4transcript. The sequences in these three cases show additionalMLLgenomic breakpoint heterogeneity. Each breakpoint junction suggests nonhomologous end joining and is consistent with DNA damage and repair.CDK6-MLLis a new fusion of both genes.

Published

2002

9. MLL Genomic Breakpoint Distribution Within the Breakpoint Cluster Region in De Novo Leukemia in Children

Author

Diana J. Slater, Beverly J. Lange, Margaret Masterson, Matthew R. Hosler, Robert I. Parker, Timothy R. Rebbeck, Peter C. Nowell, James A. Whitlock, and Carolyn A. Felix

Subjects

Adult, Male, medicine.medical_specialty, Adolescent, Translocation Breakpoint, Chromosomal translocation, Biology, Translocation, Genetic, Immunophenotyping, hemic and lymphatic diseases, Acute lymphocytic leukemia, Proto-Oncogenes, Diseases in Twins, medicine, Humans, Child, Genetics, Leukemia, Chromosomes, Human, Pair 11, Breakpoint, Age Factors, Infant, Newborn, Cytogenetics, breakpoint cluster region, Infant, Myeloid leukemia, DNA, Neoplasm, Histone-Lysine N-Methyltransferase, Hematology, Precursor Cell Lymphoblastic Leukemia-Lymphoma, medicine.disease, DNA-Binding Proteins, Blotting, Southern, DNA Topoisomerases, Type II, Treatment Outcome, Oncology, Leukemia, Myeloid, Child, Preschool, Karyotyping, Acute Disease, Pediatrics, Perinatology and Child Health, Female, Myeloid-Lymphoid Leukemia Protein, Transcription Factors

Abstract

Purpose: To assess translocation breakpoint distribution within the MLL genomic breakpoint cluster region (bcr), 40 cases of de novo leukemia in children were examined by karyotype and Southern blot analysis. Patients and Methods: Criteria for inclusion were karyotypic or molecular rearrangement of chromosome band 1 1q23. Of the 40 cases, 31 occurred in infants. Twenty cases were acute lymphoblastic leukemia (ALL), 17 were acute myeloid leukemia (AML), and 3 were biphenotypic. Results: Karyotype identified 27 cases with translocation of chromosome band 11q23 and 2 with abnormalities of band 1 1q1 3 but not 11q23. Southern blot analysis showed rearrangement within the MLL genomic bcr in 38 of the 40 cases. In these 38, additional probe-restriction digest combinations localized MLL genomic breakpoints to the 5' portion of the bcr in 14 cases and to the 3' portion in 18; material was insufficient for further localization to 5' or 3' within the bcr in 6 cases. In the two remaining cases, both with t(4;11)(q21 ;q23), one breakpoint mapped 5' of the bcr between intron 3 and exon 5, whereas the other breakpoint was neither within nor 5' of the MLL genomic bcr. Conclusions: Suggested trends warranting investigation in more patients were breakpoint sites in the 3' bcr in AML and in patients older than 12 months. The distribution of MLL genomic breakpoints within the bcr in de novo leukemia in children is distinct from that in adults, where the breakpoints cluster in the 5' portion of the bcr.

Published

1998

10. Panhandle Polymerase Chain Reaction Amplifies MLL Genomic Translocation Breakpoint Involving Unknown Partner Gene

Author

Carolyn A. Felix, Caroline S. Kim, Maureen D. Megonigal, Diana J. Slater, Douglas H. Jones, Nancy B. Spinner, Tammy Stump, Matthew R. Hosler, Peter C. Nowell, Beverly J. Lange, and Eric F. Rappaport

Subjects

hemic and lymphatic diseases, Immunology, Cell Biology, Hematology, Biochemistry

Abstract

We used a new approach called panhandle polymerase chain reaction (PCR) to clone an MLL genomic translocation breakpoint in a case of acute lymphoblastic leukemia of infancy in which karyotype analysis was technically unsuccessful and did not show the translocation partner. Panhandle PCR amplified known MLL sequence 5′ of the breakpoint and 3′ sequence from the unknown partner gene from a DNA template with an intrastrand loop schematically shaped like a pan with a handle. The 7-kb panhandle PCR product contained the translocation breakpoint in MLL intron 8. The partner DNA included unique nonrepetitive sequences, Alu and mammalian apparent LTR-retrotransposon (MaLR) repetitive sequences, and a region of homology to expressed sequence tags. MaLR sequences have not been found before near leukemia-associated translocation breakpoints. The nonrepetitive sequences were not homologous to known partner genes of MLL. Screening of somatic cell hybrid and radiation hybrid lines by PCR and fluorescence in situ hybridization analysis of normal metaphase chromosomes mapped the partner DNA to chromosome band 4q21. Reverse transcriptase-PCR identified an MLL-AF-4 chimeric mRNA, indicating that panhandle PCR identified a fusion of MLL with a previously uncharacterized AF-4 intronic sequence. Panhandle PCR facilitates cloning translocation breakpoints and identifying unknown partner genes.

Published

1997

11. Panhandle Polymerase Chain Reaction Amplifies MLL Genomic Translocation Breakpoint Involving Unknown Partner Gene

Author

Maureen D. Megonigal, Douglas H. Jones, Eric F. Rappaport, Diana J. Slater, Tammy S. Stump, Peter C. Nowell, Matthew R. Hosler, Carolyn A. Felix, Nancy B. Spinner, Beverly J. Lange, and Caroline S Kim

Subjects

Genetics, medicine.diagnostic_test, Immunology, Breakpoint, Intron, Translocation Breakpoint, Chromosomal translocation, Cell Biology, Hematology, Biology, Molecular cloning, Biochemistry, Molecular biology, law.invention, law, hemic and lymphatic diseases, medicine, Gene, Polymerase chain reaction, Fluorescence in situ hybridization

Abstract

We used a new approach called panhandle polymerase chain reaction (PCR) to clone an MLL genomic translocation breakpoint in a case of acute lymphoblastic leukemia of infancy in which karyotype analysis was technically unsuccessful and did not show the translocation partner. Panhandle PCR amplified known MLL sequence 5′ of the breakpoint and 3′ sequence from the unknown partner gene from a DNA template with an intrastrand loop schematically shaped like a pan with a handle. The 7-kb panhandle PCR product contained the translocation breakpoint in MLL intron 8. The partner DNA included unique nonrepetitive sequences, Alu and mammalian apparent LTR-retrotransposon (MaLR) repetitive sequences, and a region of homology to expressed sequence tags. MaLR sequences have not been found before near leukemia-associated translocation breakpoints. The nonrepetitive sequences were not homologous to known partner genes of MLL. Screening of somatic cell hybrid and radiation hybrid lines by PCR and fluorescence in situ hybridization analysis of normal metaphase chromosomes mapped the partner DNA to chromosome band 4q21. Reverse transcriptase-PCR identified an MLL-AF-4 chimeric mRNA, indicating that panhandle PCR identified a fusion of MLL with a previously uncharacterized AF-4 intronic sequence. Panhandle PCR facilitates cloning translocation breakpoints and identifying unknown partner genes.

Published

1997

12. The p53 gene in pediatric therapy-related leukemia and myelodysplasia

Author

Deborah Provisor, Nai Kong V Cheung, Naomi J. Winick, Matthew R. Hosler, Carolyn A. Felix, David Malkin, Eric A. Strauss, Ruth M. Heyn, Diana J. Slater, Beverly J. Lange, Elizabeth Sexsmith, and Kevin Salhany

Subjects

Chemotherapy, Monosomy, medicine.medical_treatment, Immunology, Cancer, Myeloid leukemia, Cell Biology, Hematology, Biology, medicine.disease, Biochemistry, Chromosome 17 (human), Leukemia, hemic and lymphatic diseases, Acute lymphocytic leukemia, medicine, Cancer research, Embryonal rhabdomyosarcoma

Abstract

We investigated the frequency of p53 mutations in 19 pediatric cases of therapy-related leukemia or myelodysplastic syndrome. Eleven children presented with acute myeloid leukemia, one with mixed-lineage leukemia, two with acute lymphoblastic leukemia, and five with myelodysplasia at times ranging from 11 months to 9 years after a primary cancer diagnosis. The primary cancers, which included 11 solid tumors and eight leukemias, were treated with various combinations of DNA topoisomerase II inhibitors, alkylating agents, or irradiation. Leukemic or myelodysplastic marrows were screened for possible mutations by single-strand conformation polymorphism (SSCP) analysis of p53 exons 4 to 8. The only observed mutation was an inherited 2- basepair deletion at codon 209 in exon 6 that would shift the open reading frame, create a premature termination codon, and foreshorten the resultant protein. Prior therapy in this patient included DNA topoisomerase II inhibitors, alkylating agents, and irradiation. The secondary leukemia presented as myelodysplasia with monosomies of chromosomes 5 and 7 and abnormalities of chromosome 17. Although the primary cancer was an embryonal rhabdomyosarcoma and there was a family history of cancer, the case did not fulfill the clinical criteria for Li-Fraumeni syndrome. This study suggests that germline p53 mutations may predispose some children to therapy-related leukemia and myelodysplasia, but that p53 mutations otherwise are infrequent in this setting.

Published

1996

13. Therapy-related acute myeloid leukemia-like MLL rearrangements are induced by etoposide in primary human CD34+ cells and remain stable after clonal expansion

Author

Christine Richardson, Diana J. Slater, Jolanta Libura, and Carolyn A. Felix

Subjects

Immunology, Chromosomal translocation, Antigens, CD34, Therapy-Related Acute Myeloid Leukemia, Biology, medicine.disease_cause, Biochemistry, Translocation, Genetic, hemic and lymphatic diseases, Proto-Oncogenes, medicine, Humans, Etoposide, Cells, Cultured, Cell Proliferation, Gene Rearrangement, Neoplasms, Second Primary, Cell Biology, Hematology, Gene rearrangement, Histone-Lysine N-Methyltransferase, medicine.disease, Fetal Blood, Hematopoietic Stem Cells, Molecular biology, Clone Cells, DNA-Binding Proteins, Leukemia, Haematopoiesis, Leukemia, Myeloid, Acute Disease, Myeloid-Lymphoid Leukemia Protein, Carcinogenesis, medicine.drug, Transcription Factors

Abstract

Rearrangements involving the MLL gene on chromosome band 11q23 are a hallmark of therapy-related acute myeloid leukemias following treatment with topoisomerase II poisons including etoposide. Therapy-related and de novo genomic translocation breakpoints cluster within a well-characterized 8.3-kb fragment of MLL. Repair of etoposide-stabilized DNA topoisomerase II covalent complexes may initiate MLL rearrangements observed in patients. We used a culture system of primary human hematopoietic CD34+ cells and inverse polymerase chain reaction to characterize the spectrum of stable genomic rearrangements promoted by etoposide exposure originating within an MLL translocation hotspot in therapy-related leukemia. Alterations to the region were observed at a readily detectable frequency in etoposide-treated cells. Illegitimate repair events after minimal repair included MLL tandem duplications and translocations, with minor populations of deletions or insertions. In stably repaired cells that proliferated for 10 to 14 days, the significant majority of illegitimate events were MLL tandem duplications, and several deletions, inversions, insertions, and translocations. Thus, etoposide promotes specific rearrangements of MLL consistent with the full spectrum of oncogenic events identified in leukemic samples. Although etoposide-initiated rearrangements are frequent, only a small subset of translocations occurs in cells that proliferate significantly.

Published

2004

14. Reciprocal DNA topoisomerase II cleavage events at 5'-TATTA-3' sequences in MLL and AF-9 create homologous single-stranded overhangs that anneal to form der(11) and der(9) genomic breakpoint junctions in treatment-related AML without further processing

Author

Diana J. Slater, Charles Saginario, Ian A. Blair, Neil Osheroff, Eric F. Rappaport, Maureen D. Megonigal, Eva Hilgenfeld, Carolyn A. Felix, Ryan J. Whitmarsh, Mingli Liu, Thomas Ried, Turid Knutsen, Nai-Kong V. Cheung, Martin Carroll, and Ya Zhuo

Subjects

Male, Cancer Research, Adolescent, DNA damage, Molecular Sequence Data, Biology, medicine.disease_cause, Cleavage (embryo), Translocation, Genetic, hemic and lymphatic diseases, Proto-Oncogenes, Genetics, medicine, Humans, Molecular Biology, Transcription factor, Etoposide, In Situ Hybridization, Fluorescence, Recombination, Genetic, Topoisomerase, Breakpoint, Intron, Nuclear Proteins, Histone-Lysine N-Methyltransferase, Molecular biology, DNA-Binding Proteins, Leukemia, Myeloid, Acute, DNA Topoisomerases, Type II, biology.protein, Carcinogenesis, Protein Processing, Post-Translational, Myeloid-Lymphoid Leukemia Protein, medicine.drug, Transcription Factors

Abstract

Few t(9;11) translocations in DNA topoisomerase II inhibitor-related leukemias have been studied in detail and the DNA damage mechanism remains controversial. We characterized the der(11) and der(9) genomic breakpoint junctions in a case of AML following etoposide and doxorubicin. Etoposide-, etoposide metabolite- and doxorubicin-induced DNA topoisomerase II cleavage was examined in normal homologues of the MLL and AF-9 breakpoint sequences using an in vitro assay. Induction of DNA topoisomerase II cleavage complexes in CEM and K562 cell lines was investigated using an in vivo complex of enzyme assay. The translocation occurred between identical 5'-TATTA-3' sequences in MLL intron 8 and AF-9 intron 5 without the gain or loss of bases. The 5'-TATTA-3' sequences were reciprocally cleaved by DNA topoisomerase II in the presence of etoposide, etoposide catechol or etoposide quinone, creating homologous 4-base 5' overhangs that would anneal to form both breakpoint junctions without any processing. der(11) and der(4) translocation breakpoints in a treatment-related ALL at the same site in MLL are consistent with a damage hotspot. Etoposide and both etoposide metabolites induced DNA topoisomerase II cleavage complexes in the hematopoietic cell lines. These results favor the model in which the chromosomal breakage leading to MLL translocations in DNA topoisomerase II inhibitor-related leukemias is a consequence of DNA topoisomerase II cleavage.

Published

2003

15. p53 mutations in leukemia and myelodysplastic syndrome after ovarian cancer

Author

Debra G B, Leonard, Lois B, Travis, Kathakali, Addya, Graca M, Dores, Eric J, Holowaty, Kjell, Bergfeldt, David, Malkin, Betsy A, Kohler, Charles F, Lynch, Tom, Wiklund, Marilyn, Stovall, Per, Hall, Eero, Pukkala, Diana J, Slater, and Carolyn A, Felix

Subjects

Adult, Ovarian Neoplasms, Leukemia, Base Sequence, DNA Mutational Analysis, DNA, Neoplasm, Middle Aged, Combined Modality Therapy, Myelodysplastic Syndromes, Antineoplastic Combined Chemotherapy Protocols, Mutation, Humans, Female, Cisplatin, Tumor Suppressor Protein p53, Aged

Abstract

Although p53 mutations occur in alkylating agent-related leukemias, their frequency and spectrum in leukemias after ovarian cancer have not been addressed. The purpose of this study was to examine p53 mutations in leukemias after ovarian cancer, for which treatment with platinum analogues was widely used.Adequate leukemic or dysplastic cells were available in 17 of 82 cases of leukemia or myelodysplastic syndrome that occurred in a multicenter, population-based cohort of 23,170 women with ovarian cancer. Eleven of the 17 received platinum compounds and other alkylating agents with or without DNA topoisomerase II inhibitors and/or radiation. Six received other alkylating agents, in one case, with radiation. Genomic DNA was extracted and p53 exons 5, 6, 7, and 8 were amplified by PCR. Mutations and loss of heterozygosity were analyzed on the WAVE instrument (Transgenomic) followed by selected analysis by sequencing.Eleven p53 mutations involving all four exons studied and one polymorphism were identified. Genomic DNA analyses were consistent with loss of heterozygosity for four of the mutations. The 11 mutations occurred in 9 cases, such that 6 of 11 leukemias after platinum-based regimens (55%) and 3 of 6 leukemias after other treatments (50%) contained p53 mutations. Two leukemias that occurred after treatment with platinum analogues contained two mutations. Among eight mutations in leukemias after treatment with platinum analogues, there were four G-to-A transitions and one G-to-C transversion.p53 mutations are common in leukemia and myelodysplastic syndrome after multiagent therapy for ovarian cancer. The propensity for G-to-A transitions may reflect specific DNA damage in leukemias after treatment with platinum analogues.

Published

2002

16. Panhandle PCR for cDNA: a rapid method for isolation of MLL fusion transcripts involving unknown partner genes

Author

Robert B. Wilson, Diana J. Slater, Peter C. Nowell, James A. Whitlock, Jorge A. Ortega, Carolyn A. Felix, Eric F. Rappaport, Douglas H. Jones, and Maureen D. Megonigal

Subjects

Male, DNA, Complementary, Oncogene Proteins, Fusion, Molecular Sequence Data, Sarcoma, Ewing, Biology, Polymerase Chain Reaction, Translocation, Genetic, Exon, Complementary DNA, hemic and lymphatic diseases, Proto-Oncogenes, Tumor Cells, Cultured, Coding region, Humans, RNA, Messenger, Child, Gene, neoplasms, Alleles, Rhabdomyosarcoma, Alveolar, Genetics, Multidisciplinary, Alternative splicing, breakpoint cluster region, Infant, Reproducibility of Results, Exons, Histone-Lysine N-Methyltransferase, Templates, Genetic, Biological Sciences, Peptide Elongation Factors, Molecular biology, Neoplasm Proteins, DNA-Binding Proteins, Alternative Splicing, Fusion transcript, Karyotyping, Myeloid-Lymphoid Leukemia Protein, Nucleic Acid Conformation, Transcriptional Elongation Factors, Transcription Factors

Abstract

Identifying translocations of the MLL gene at chromosome band 11q23 is important for the characterization and treatment of leukemia. However, cytogenetic analysis does not always find the translocations and the many partner genes of MLL make molecular detection difficult. We developed cDNA panhandle PCR to identify der(11) transcripts regardless of the partner gene. By reverse transcribing first-strand cDNAs with oligonucleotides containing coding sequence from the 5′ MLL breakpoint cluster region at the 5′ ends and random hexamers at the 3′ ends, known MLL sequence was attached to the unknown partner sequence. This enabled the formation of stem-loop templates with the fusion point of the chimeric transcript in the loop and the use of MLL primers in two-sided PCR. The assay was validated by detection of the known fusion transcript and the transcript from the normal MLL allele in the cell line MV4–11. cDNA panhandle PCR then was used to identify the fusion transcripts in two cases of treatment-related acute myeloid leukemia where the karyotypes were normal and the partner genes unknown. cDNA panhandle PCR revealed a fusion of MLL with AF-10 in one case and a fusion of MLL with ELL in the other. Alternatively spliced transcripts and exon scrambling were detectable by the method. Leukemias with normal karyotypes may contain cryptic translocations of MLL with a variety of partner genes. cDNA panhandle PCR is useful for identifying MLL translocations and determining unknown partner sequences in the fusion transcripts.

Published

2000

17. Duplicated regions of AF-4 intron 4 at t(4;11) translocation breakpoints

Author

Brian D. Lovett, Nancy B. Spinner, Nancy L. Owens, Diana J. Slater, Terence M. Williams, Carlo M. Croce, Eric F. Rappaport, Carolyn A. Felix, James A. Hoxie, Matthew R. Hosler, Peter C. Nowell, Beverly J. Lange, and Maureen D. Megonigal

Subjects

Adult, Adolescent, Sequence analysis, Molecular Sequence Data, Alu element, Chromosomal translocation, Biology, Translocation, Genetic, Alu Elements, hemic and lymphatic diseases, Gene Duplication, Gene duplication, Tumor Cells, Cultured, Humans, Amino Acid Sequence, Child, Gene, In Situ Hybridization, Fluorescence, Aged, Genetics, Base Sequence, Reverse Transcriptase Polymerase Chain Reaction, Chromosomes, Human, Pair 11, Breakpoint, Intron, Infant, Newborn, Infant, Karyotype, General Medicine, Sequence Analysis, DNA, Precursor Cell Lymphoblastic Leukemia-Lymphoma, Molecular biology, Introns, Leukemia, Myeloid, Acute, Karyotyping, Chromosomes, Human, Pair 4, Sequence Alignment

Abstract

Background: AF-4 is a common partner gene of MLL. AF-4 breakpoints occur in introns, but most AF-4 introns are uncharacterized. Methods and Results: We cloned AF-4 intron 4 and examined the frequency of breakpoints in this intron. The 5.8-kb intron is rich in repeat sequences and was the site of translocation in 3 of 17 leukemias with t(4;11). We cloned the der (11) and der (4) breakpoints and isolated the fusion transcripts in the cell line MV4-11 and in a de novo acute lymphoblastic leukemia (ALL). Both translocations joined MLL intron 6 and AF-4 intron 4. In MV4-11, 249 bases from AF-4 were present in both derivative chromosomes, indicating duplication. In the de novo ALL, duplication of 446 bases from MLL and AF-4 occurred. Reciprocal fusion transcripts were expressed. Conclusions: Intronic sequence of AF-4 is useful for molecular diagnosis of t(4;11). Duplicated intronic regions suggest staggered chromosomal breakage.

Published

2000

18. DNA Topoisomerase II Poisons and the Etiology of Acute Leukemia in Infants

Author

Eric F. Rappaport, Anna Sechser Perl, Christos P. Kolaris, Carolyn A. Felix, Diana J. Slater, and Neil Osheroff

Subjects

education.field_of_study, biology, Topoisomerase, Immunology, Breakpoint, Population, breakpoint cluster region, Translocation Breakpoint, Chromosomal translocation, Cell Biology, Hematology, Biochemistry, Molecular biology, chemistry.chemical_compound, chemistry, hemic and lymphatic diseases, biology.protein, medicine, education, neoplasms, DNA, Etoposide, medicine.drug

Abstract

Background: Chromosomal translocations leading to MLL chimeric oncoproteins are the primary aberrations in infant acute leukemias, but how these translocations are created has not been established. A Children’s Oncology Group population epidemiology study recently validated that maternal consumption of dietary items containing topoisomerase II interacting compounds during pregnancy increases the risk of infant AML with MLL translocations. An inactivating polymorphism in the gene encoding NQO1, which detoxifies the topoisomerase II poison p-benzoquinone, also is associated with an increased risk of MLL-rearranged acute leukemias in infants, with the greatest risk for cases with t(4;11). Although there is heterogeneity, it has been suggested that infant leukemias share the same biased MLL translocation breakpoint distribution 3′ in the breakpoint cluster region (bcr) as secondary leukemias arising following chemotherapeutic topoisomerase II poisons. These observations led us to investigate the relationship between topoisomerase II cleavage complexes induced by dietary substances or p-benzoquinone and translocation breakpoints 3′ in the bcr. Methods: Southern blot analysis was used to identify the MLL rearrangement in the AML of an infant male harboring the inactivating NQO1 polymorphism, and the MLL-AF9 genomic breakpoint junction was characterized by panhandle variant PCR. DNA substrates containing the normal homologues of the breakpoint sequences were utilized in topoisomerase II in vitro cleavage assays in the presence of p-benzoquinone or dietary substances to determine whether topoisomerase II cleavage sites were stimulated by these agents at the observed translocation breakpoints. Results: There was a single MLL bcr rearrangement in the infant AML, and the cloning demonstrated a breakpoint junction fusing MLL bcr position 6774, 6775, 6776, 6777, 6778, 6779, 6780 or 6781 in intron 8 to position 35940, 35941, 35942, 35943, 35944, 35945, 35946 or 35947 relative to the start of AF9 intron 5. Identical 5′-GTTCTTA-3′ sequences suggesting the DNA double strand break repair mechanism of NHEJ were present at both breakpoints. The normal homologues of the breakpoints in MLL and AF9 were reciprocally cleaved by topoisomerase II in the presence of p-benzoquinone, and the cleavage sites were resolved to form the breakpoint junction. The MLL substrate contained another topoisomerase II cleavage site at position 6760 that not only was the strongest cleavage site in this substrate with the enzyme alone, but also was enhanced by p-benzoquinone, genistein, genistin, quercitin, and catechin at levels comparable to or greater than the anticancer drug etoposide. Further analysis of 3′ MLL bcr substrates revealed cleavage stimulation by natural topoisomerase II poisons near additional translocation breakpoints. Conclusions: These results establish the relationship between topoisomerase II mediated damage from p-benzoquinone and dietary exposures and MLL translocation breakpoints. MLL translocation breakpoints in infant leukemias can be explained by topoisomerase II cleavage. The combined evidence from population epidemiology studies on maternal-fetal exposures, the NQO1-leukemia association implicating p-benzoquinone, genomic breakpoint junction cloning and topoisomerase II cleavage assays corroborate that topoisomerase II poisons damage MLL in acute leukemia in infants.

Published

2005

19. BglII‐based panhandle and reverse panhandle PCR approaches increase capability for cloning der(II) and der(other) genomic breakpoint junctions of MLL translocationsAll new sequences described herein were deposited in GenBank (GenBank Nos. DQ387204, DQ387205, and DQ387206).

Author

Blaine W. Robinson, Diana J. Slater, and Carolyn A. Felix

Published

2006