Your search keyword '"Bowles, Karla R."' showing total 5 results

1. Classification of genetic variants in genes associated with Lynch syndrome using a clinical history weighting algorithm.

Author

Morris B, Hughes E, Rosenthal E, Gutin A, and Bowles KR

Subjects

Algorithms, Colorectal Neoplasms, Hereditary Nonpolyposis genetics, DNA Mismatch Repair, Female, Genetic Association Studies, Genetic Predisposition to Disease, Genetic Testing, Humans, Colorectal Neoplasms, Hereditary Nonpolyposis classification, DNA-Binding Proteins genetics, MutL Protein Homolog 1 genetics, MutS Homolog 2 Protein genetics, Mutation

Abstract

Background: Lynch syndrome is a hereditary cancer syndrome associated with high risks of colorectal and endometrial cancer that is caused by pathogenic variants in the mismatch repair genes (MLH1, MSH2, MSH6, PMS2, EPCAM). Accurate classification of variants identified in these genes as pathogenic or benign enables informed medical management decisions. Previously, we developed a clinical History Weighting Algorithm (HWA) for the classification of variants of uncertain significance (VUSs) in BRCA1 and BRCA2. The BRCA1/2 HWA is based on the premise that pathogenic variants in these genes will be identified more often in individuals with strong personal and/or family histories of breast and/or ovarian cancer, while the identification of benign variants should be independent of cancer history. Here we report the development of a similar HWA to allow for classification of VUSs in genes associated with Lynch syndrome using data collected through both syndrome-specific and pan-cancer panel testing., Methods: Upon completion of algorithm development, the HWA was tested using simulated variants constructed from 79,214 probands, as well as 379 true variants. Positive (PPV) and negative predictive values (NPV) were calculated on a per gene basis., Results: 25,500 pathogenic and 50,500 benign simulated variants were analyzed using the HWA and the PPVs and NPVs for each gene were greater than 0.997 and 0.999, respectively. The HWA was also evaluated using 100 trials for each of the 379 true variants. PPVs of >0.998 and NPVs of >0.999 were obtained for all genes., Conclusions: We have developed and implemented a HWA to aid in the classification of VUSs in genes associated with Lynch syndrome. The work presented here demonstrates that this HWA is able to classify MLH1, MSH2, and MSH6 VUSs as either benign or pathogenic with high accuracy.

Published

2016

2. Functional evaluation of BRCA2 variants mapping to the PALB2-binding and C-terminal DNA-binding domains using a mouse ES cell-based assay.

Author

Biswas K, Das R, Eggington JM, Qiao H, North SL, Stauffer S, Burkett SS, Martin BK, Southon E, Sizemore SC, Pruss D, Bowles KR, Roa BB, Hunter N, Tessarollo L, Wenstrup RJ, Byrd RA, and Sharan SK

Subjects

Amino Acid Sequence, Animals, BRCA2 Protein chemistry, Cell Cycle Proteins, Cell Survival, Cells, Cultured, Chromosome Mapping, Conserved Sequence, DNA Breaks, Double-Stranded, DNA Repair, DNA-Binding Proteins, Embryonic Stem Cells drug effects, Embryonic Stem Cells physiology, Fanconi Anemia Complementation Group N Protein, Female, Genetic Association Studies, Humans, Likelihood Functions, Male, Mice, Mice, Transgenic, Mitomycin pharmacology, Models, Molecular, Mutagens pharmacology, Protein Binding, Protein Interaction Domains and Motifs genetics, Protein Structure, Quaternary, Structural Homology, Protein, BRCA2 Protein genetics, Breast Neoplasms genetics, Embryonic Stem Cells metabolism, Mutation, Nuclear Proteins metabolism, Tumor Suppressor Proteins metabolism

Abstract

Single-nucleotide substitutions and small in-frame insertions or deletions identified in human breast cancer susceptibility genes BRCA1 and BRCA2 are frequently classified as variants of unknown clinical significance (VUS) due to the availability of very limited information about their functional consequences. Such variants can most reliably be classified as pathogenic or non-pathogenic based on the data of their co-segregation with breast cancer in affected families and/or their co-occurrence with a pathogenic mutation. Biological assays that examine the effect of variants on protein function can provide important information that can be used in conjunction with available familial data to determine the pathogenicity of VUS. In this report, we have used a previously described mouse embryonic stem (mES) cell-based functional assay to characterize eight BRCA2 VUS that affect highly conserved amino acid residues and map to the N-terminal PALB2-binding or the C-terminal DNA-binding domains. For several of these variants, very limited co-segregation information is available, making it difficult to determine their pathogenicity. Based on their ability to rescue the lethality of Brca2-deficient mES cells and their effect on sensitivity to DNA-damaging agents, homologous recombination and genomic integrity, we have classified these variants as pathogenic or non-pathogenic. In addition, we have used homology-based modeling as a predictive tool to assess the effect of some of these variants on the structural integrity of the C-terminal DNA-binding domain and also generated a knock-in mouse model to analyze the physiological significance of a residue reported to be essential for the interaction of BRCA2 with meiosis-specific recombinase, DMC1.

Published

2012

3. Isolated left ventricular noncompaction is rarely caused by mutations in G4.5, alpha-dystrobrevin and FK Binding Protein-12.

Author

Kenton AB, Sanchez X, Coveler KJ, Makar KA, Jimenez S, Ichida F, Murphy RT, Elliott PM, McKenna W, Bowles NE, Towbin JA, and Bowles KR

Subjects

Acyltransferases, Base Sequence, Humans, RNA Splice Sites genetics, RNA, Messenger genetics, RNA, Messenger metabolism, Dystrophin-Associated Proteins genetics, Hypertrophy, Left Ventricular genetics, Mutation genetics, Proteins genetics, Tacrolimus Binding Protein 1A genetics, Transcription Factors genetics

Abstract

Isolated left ventricular noncompaction (LVNC) is a form of cardiomyopathy that most commonly presents in infancy with a hypertrophic and dilated left ventricle characterized by deep trabeculations and intertrabecular recesses. Our goal was to determine the frequency of mutations in G4.5, alpha-dystrobrevin, and FK Binding protein-12 in isolated LVNC patients. No mutations were identified in 47 of the 48 patients studied, while a splice site acceptor site mutation of intron 10 of G4.5 was identified in one patient, resulting in the deletion of exon 10 from the mRNA.

Published

2004

4. Mutations in Cypher/ZASP in patients with dilated cardiomyopathy and left ventricular non-compaction.

Author

Vatta M, Mohapatra B, Jimenez S, Sanchez X, Faulkner G, Perles Z, Sinagra G, Lin JH, Vu TM, Zhou Q, Bowles KR, Di Lenarda A, Schimmenti L, Fox M, Chrisco MA, Murphy RT, McKenna W, Elliott P, Bowles NE, Chen J, Valle G, and Towbin JA

Subjects

Adaptor Proteins, Signal Transducing, Blotting, Northern, Blotting, Western, Cardiomyopathy, Dilated diagnosis, Chromatography, High Pressure Liquid, Echocardiography, Humans, Immunohistochemistry, LIM Domain Proteins, Mutagenesis, Transfection, Cardiomyopathy, Dilated genetics, Carrier Proteins genetics, Heart Ventricles pathology, Homeodomain Proteins genetics, Muscle Proteins genetics, Mutation, Ventricular Dysfunction, Left genetics

Abstract

Objectives: We evaluated the role of Cypher/ZASP in the pathogenesis of dilated cardiomyopathy (DCM) with or without isolated non-compaction of the left ventricular myocardium (INLVM)., Background: Dilated cardiomyopathy, characterized by left ventricular dilation and systolic dysfunction with signs of heart failure, is genetically transmitted in 30% to 40% of cases. Genetic heterogeneity has been identified with mutations in multiple cytoskeletal and sarcomeric genes causing the phenotype. In addition, INLVM with a hypertrophic dilated left ventricle, ventricular dysfunction, and deep trabeculations, is also inherited, and the genes identified to date differ from those causing DCM. Cypher/ZASP is a newly identified gene encoding a protein that is a component of the Z-line in both skeletal and cardiac muscle., Methods: Diagnosis of DCM was performed by echocardiogram, electrocardiogram, and physical examination. In addition, levels of the muscular isoform of creatine kinase were measured to evaluate for skeletal muscle involvement. Cypher/ZASP was screened by denaturing high performance liquid chromatography (DHPLC) and direct deoxyribonucleic acid sequencing., Results: We identified and screened 100 probands with left ventricular dysfunction. Five mutations in six probands (6% of cases) were identified in patients with familial or sporadic DCM or INLVM. In vitro studies showed cytoskeleton disarray in cells transfected with mutated Cypher/ZASP., Conclusions: These data suggest that mutated Cypher/ZASP can cause DCM and INLVM and identify a mechanistic basis.

Published

2003

5. Genetic analysis in patients with left ventricular noncompaction and evidence for genetic heterogeneity

Author

Xing, Yanlin, Ichida, Fukiko, Matsuoka, Taro, Isobe, Takeshi, Ikemoto, Yumiko, Higaki, Takashi, Tsuji, Tohru, Haneda, Noriyuki, Kuwabara, Atsushi, Chen, Rui, Futatani, Takeshi, Tsubata, Shinichi, Watanabe, Sayaka, Watanabe, Kazuhiro, Hirono, Keiichi, Uese, Keiichiro, Miyawaki, Toshio, Bowles, Karla R., Bowles, Neil E., and Towbin, Jeffrey A.

Subjects

*CARDIOMYOPATHIES, *DNA, *NUCLEIC acids, *HETEROGENEITY

Abstract

Abstract: Left ventricular noncompaction (LVNC) is a cardiomyopathy characterized by numerous excessively trabeculations and deep intertrabecular recesses. This study was performed to investigate Japanese LVNC patients for disease-causing mutations in a series of selected candidate genes. DNA was isolated from the peripheral blood of 79 cases including 20 familial cases and 59 sporadic cases. DNA samples were screened for mutations in the genes encoding G4.5 (TAZ), α-dystrobrevin (DTNA), α1-syntrophin (SNTA1), FK506 Binding protein 1A (FKBP1A or FKPB12: FKBP1A), and LIM Domain Binding protein 3 (Cypher/ZASP: LDB3), using single-strand conformational polymorphism analysis and DNA sequencing. DNA variants were identified in 6 of the 79 cases, including four familial cases and two sporadic cases. A splice acceptor mutation of intron 8 in TAZ (IVS8-1G>C) was identified in one family with isolated LVNC, resulting in deletion of exon 9 from mRNA. In a sporadic case of isolated LVNC and Barth syndrome (BTHS), a 158insC in exon 2 of TAZ resulting in a frame-shift mutation was identified. A 1876G>A substitution changing an aspartic acid to asparagine (D626N) was identified in LDB3 in four members of two families with LVNC. A 163G>A polymorphism was identified in LDB3, which changed a valine to isoleucine (V55I) in one patient with isolated LVNC. In addition, in a family with nonisolated LVNC, a 362C>T mutation was identified in DTNA. LVNC, like other forms of inherited cardiomyopathy, is a genetically heterogeneous disease, associated with variable clinical symptoms and can be inherited as an autosomal or X-linked recessive disorder. [Copyright &y& Elsevier]

Published

2006