Your search keyword '"McGrath SD"' showing total 57 results

1. Progressive metastatic infantile fibrosarcoma with multiple acquired mutations.

Author

Furtado, Larissa V., Kacar, Marija, Mostafavi, Roya, Zonggao Shi, Ruiz, Robert, Koo, Selene C., Santiago, Teresa, Segers, Blair, Krasin, Matthew J., Abramson, Zachary R., Shulkin, Barry, Talbot, Lindsay J., Pappo, Alberto, and Gartrell, Jessica

Subjects

FIBROSARCOMA, GENETIC mutation, TUMORS in children, CHIMERIC proteins, METASTASIS

Abstract

Infantile fibrosarcoma is the most common soft-tissue sarcoma in children under the age of 1 yr and is defined molecularly by NTRK fusion proteins. This tumor is known to be locally invasive; however, although rare, metastases can occur. The NTRK fusion acts as a driver for tumor formation, which can be targeted by first- and second-generation TRK inhibitors. Although NTRK gatekeeper mutations have been well-described as mechanisms of resistance to these agents, alternative pathway mutations are rare. Here, we report the case of a patient with infantile fibrosarcoma treated with chemotherapy and TRK inhibition that developed metastatic, progressive disease with multiple acquired mutations, including TP53, SUFU, and an NTRK F617L gatekeeper mutation. Alterations in pathways of SUFU and TP53 have been widely described in the literature in other tumors; however, not yet in infantile fibrosarcoma. Although most patients have a sustained response to TRK inhibitors, a subset will go on to develop mechanisms of resistance that have implications for clinical management, such as in our patient. We hypothesize this constellation of mutations contributed to the patient's aggressive clinical course. Taken together, we report the first case of infantile fibrosarcoma with ETV6::NTRK3 and acquired SUFU, TP53, and NTRK F617L gatekeeper mutation along with detailed clinical course and management. Our report highlights the importance of genomic profiling in recurrent infantile fibrosarcoma to reveal actionable mutations, such as gatekeeper mutations, that can improve patient outcomes. [ABSTRACT FROM AUTHOR]

Published

2023

2. Identification and characterisation of spontaneous mutations causing deafness from a targeted knockout programme.

Author

Lewis, Morag A., Ingham, Neil J., Chen, Jing, Pearson, Selina, Di Domenico, Francesca, Rekhi, Sohinder, Allen, Rochelle, Drake, Matthew, Willaert, Annelore, Rook, Victoria, Pass, Johanna, Keane, Thomas, Adams, David J., Tucker, Abigail S., White, Jacqueline K., and Steel, Karen P.

Subjects

EMBRYONIC stem cells, STEM cell culture, GENETIC mutation, HEARING aids

Abstract

Background: Mice carrying targeted mutations are important for investigating gene function and the role of genes in disease, but off-target mutagenic effects associated with the processes of generating targeted alleles, for instance using Crispr, and culturing embryonic stem cells, offer opportunities for spontaneous mutations to arise. Identifying spontaneous mutations relies on the detection of phenotypes segregating independently of targeted alleles, and having a broad estimate of the level of mutations generated by intensive breeding programmes is difficult given that many phenotypes are easy to miss if not specifically looked for. Here we present data from a large, targeted knockout programme in which mice were analysed through a phenotyping pipeline. Such spontaneous mutations segregating within mutant lines may confound phenotypic analyses, highlighting the importance of record-keeping and maintaining correct pedigrees. Results: Twenty-five lines out of 1311 displayed different deafness phenotypes that did not segregate with the targeted allele. We observed a variety of phenotypes by Auditory Brainstem Response (ABR) and behavioural assessment and isolated eight lines showing early-onset severe progressive hearing loss, later-onset progressive hearing loss, low frequency hearing loss, or complete deafness, with vestibular dysfunction. The causative mutations identified include deletions, insertions, and point mutations, some of which involve new genes not previously associated with deafness while others are new alleles of genes known to underlie hearing loss. Two of the latter show a phenotype much reduced in severity compared to other mutant alleles of the same gene. We investigated the ES cells from which these lines were derived and determined that only one of the 8 mutations could have arisen in the ES cell, and in that case, only after targeting. Instead, most of the non-segregating mutations appear to have occurred during breeding of mutant mice. In one case, the mutation arose within the wildtype colony used for expanding mutant lines. Conclusions: Our data show that spontaneous mutations with observable effects on phenotype are a common side effect of intensive breeding programmes, including those underlying targeted mutation programmes. Such spontaneous mutations segregating within mutant lines may confound phenotypic analyses, highlighting the importance of record-keeping and maintaining correct pedigrees. [ABSTRACT FROM AUTHOR]

Published

2022

3. Identification and characterisation of spontaneous mutations causing deafness from a targeted knockout programme.

Author

Lewis, Morag A., Ingham, Neil J., Chen, Jing, Pearson, Selina, Di Domenico, Francesca, Rekhi, Sohinder, Allen, Rochelle, Drake, Matthew, Willaert, Annelore, Rook, Victoria, Pass, Johanna, Keane, Thomas, Adams, David J., Tucker, Abigail S., White, Jacqueline K., and Steel, Karen P.

Subjects

EMBRYONIC stem cells, STEM cell culture, ALLELES, GENETIC mutation

Abstract

Background: Mice carrying targeted mutations are important for investigating gene function and the role of genes in disease, but off-target mutagenic effects associated with the processes of generating targeted alleles, for instance using Crispr, and culturing embryonic stem cells, offer opportunities for spontaneous mutations to arise. Identifying spontaneous mutations relies on the detection of phenotypes segregating independently of targeted alleles, and having a broad estimate of the level of mutations generated by intensive breeding programmes is difficult given that many phenotypes are easy to miss if not specifically looked for. Here we present data from a large, targeted knockout programme in which mice were analysed through a phenotyping pipeline. Such spontaneous mutations segregating within mutant lines may confound phenotypic analyses, highlighting the importance of record-keeping and maintaining correct pedigrees. Results: Twenty-five lines out of 1311 displayed different deafness phenotypes that did not segregate with the targeted allele. We observed a variety of phenotypes by Auditory Brainstem Response (ABR) and behavioural assessment and isolated eight lines showing early-onset severe progressive hearing loss, later-onset progressive hearing loss, low frequency hearing loss, or complete deafness, with vestibular dysfunction. The causative mutations identified include deletions, insertions, and point mutations, some of which involve new genes not previously associated with deafness while others are new alleles of genes known to underlie hearing loss. Two of the latter show a phenotype much reduced in severity compared to other mutant alleles of the same gene. We investigated the ES cells from which these lines were derived and determined that only one of the 8 mutations could have arisen in the ES cell, and in that case, only after targeting. Instead, most of the non-segregating mutations appear to have occurred during breeding of mutant mice. In one case, the mutation arose within the wildtype colony used for expanding mutant lines. Conclusions: Our data show that spontaneous mutations with observable effects on phenotype are a common side effect of intensive breeding programmes, including those underlying targeted mutation programmes. Such spontaneous mutations segregating within mutant lines may confound phenotypic analyses, highlighting the importance of record-keeping and maintaining correct pedigrees. [ABSTRACT FROM AUTHOR]

Published

2022

4. Origins and Long-Term Patterns of Copy-Number Variation in Rhesus Macaques.

Author

Thomas, Gregg W C, Wang, Richard J, Nguyen, Jelena, Harris, R Alan, Raveendran, Muthuswamy, Rogers, Jeffrey, and Hahn, Matthew W

Subjects

DNA copy number variations, GENETIC mutation, SPERMATOGENESIS, GENOMES, DELETION mutation

Abstract

Mutations play a key role in the development of disease in an individual and the evolution of traits within species. Recent work in humans and other primates has clarified the origins and patterns of single-nucleotide variants, showing that most arise in the father's germline during spermatogenesis. It remains unknown whether larger mutations, such as deletions and duplications of hundreds or thousands of nucleotides, follow similar patterns. Such mutations lead to copy-number variation (CNV) within and between species, and can have profound effects by deleting or duplicating genes. Here, we analyze patterns of CNV mutations in 32 rhesus macaque individuals from 14 parent–offspring trios. We find the rate of CNV mutations per generation is low (less than one per genome) and we observe no correlation between parental age and the number of CNVs that are passed on to offspring. We also examine segregating CNVs within the rhesus macaque sample and compare them to a similar data set from humans, finding that both species have far more segregating deletions than duplications. We contrast this with long-term patterns of gene copy-number evolution between 17 mammals, where the proportion of deletions that become fixed along the macaque lineage is much smaller than the proportion of segregating deletions. These results suggest purifying selection acting on deletions, such that the majority of them are removed from the population over time. Rhesus macaques are an important biomedical model organism, so these results will aid in our understanding of this species and the disease models it supports. [ABSTRACT FROM AUTHOR]

Published

2021

5. The oncometabolite R-2-hydroxyglutarate dysregulates the differentiation of human mesenchymal stromal cells via inducing DNA hypermethylation.

Author

Liu, Lizhen, Hu, Kaimin, Feng, Jingjing, Wang, Huafang, Fu, Shan, Wang, Binsheng, Wang, Limengmeng, Xu, Yulin, Yu, Xiaohong, and Huang, He

Subjects

STROMAL cells, DNA, ISOCITRATE dehydrogenase, DNA methylation, DNA methyltransferases, GENETIC mutation

Abstract

Background: Isocitrate dehydrogenase (IDH1/2) gene mutations are the most frequently observed mutations in cartilaginous tumors. The mutant IDH causes elevation in the levels of R-enantiomer of 2-hydroxylglutarate (R-2HG). Mesenchymal stromal cells (MSCs) are reasonable precursor cell candidates of cartilaginous tumors. This study aimed to investigate the effect of oncometabolite R-2HG on MSCs.Methods: Human bone marrow MSCs treated with or without R-2HG at concentrations 0.1 to 1.5 mM were used for experiments. Cell Counting Kit-8 was used to detect the proliferation of MSCs. To determine the effects of R-2HG on MSC differentiation, cells were cultured in osteogenic, chondrogenic and adipogenic medium. Specific staining approaches were performed and differentiation-related genes were quantified. Furthermore, DNA methylation status was explored by Illumina array-based arrays. Real-time PCR was applied to examine the signaling component mRNAs involved in.Results: R-2HG showed no influence on the proliferation of human MSCs. R-2HG blocked osteogenic differentiation, whereas promoted adipogenic differentiation of MSCs in a dose-dependent manner. R-2HG inhibited chondrogenic differentiation of MSCs, but increased the expression of genes related to chondrocyte hypertrophy in a lower concentration (1.0 mM). Moreover, R-2HG induced a pronounced DNA hypermethylation state of MSC. R-2HG also improved promotor methylation of lineage-specific genes during osteogenic and chondrogenic differentiation. In addition, R-2HG induced hypermethylation and decreased the mRNA levels of SHH, GLI1and GLI2, indicating Sonic Hedgehog (Shh) signaling inhibition.Conclusions: The oncometabolite R-2HG dysregulated the chondrogenic and osteogenic differentiation of MSCs possibly via induction of DNA hypermethylation, improving the role of R-2HG in cartilaginous tumor development. [ABSTRACT FROM AUTHOR]

Published

2021

6. The leukemia strikes back: a review of pathogenesis and treatment of secondary AML.

Author

Cheung, Edna, Perissinotti, Anthony J., Bixby, Dale L., Burke, Patrick W., Pettit, Kristen M., Benitez, Lydia L., Brown, Julia, Scappaticci, Gianni B., and Marini, Bernard L.

Subjects

ANTINEOPLASTIC agents, PROTEIN metabolism, ANIMALS, DAUNOMYCIN, GENETIC mutation, PROTEINS, ACUTE myeloid leukemia, CYTARABINE

Abstract

Secondary AML is associated with a disproportionately poor prognosis, consistently shown to exhibit inferior response rates, event-free survival, and overall survival in comparison with de novo AML. Secondary AML may arise from the evolution of an antecedent hematologic disorder, or it may arise as a complication of prior cytotoxic chemotherapy or radiation therapy in the case of therapy-related AML. Because of the high frequency of poor-risk cytogenetics and high-risk molecular features, such as alterations in TP53, leukemic clones are often inherently chemoresistant. Standard of care induction had long remained conventional 7 + 3 until its reformulation as CPX-351, recently FDA approved specifically for secondary AML. However, recent data also suggests relatively favorable outcomes with regimens based on high-dose cytarabine or hypomethylating agents. With several investigational agents being studied, the therapeutic landscape becomes even more complex, and the treatment approach involves patient-specific, disease-specific, and therapy-specific considerations. [ABSTRACT FROM AUTHOR]

Published

2019

7. A genome-wide view of mutations in respiration-deficient mutants of Saccharomyces cerevisiae selected following carbon ion beam irradiation.

Author

Guo, Xiaopeng, Zhang, Miaomiao, Gao, Yue, Cao, Guozhen, Yang, Yang, Lu, Dong, and Li, Wenjian

Subjects

SACCHAROMYCES cerevisiae, ION beams, GENETIC mutation, IRRADIATION, GENOMES

Abstract

Mitochondrial dysfunction in Saccharomyces cerevisiae was selected as a marker of ion penetration following carbon ion beam (CIB) irradiation. Respiration-deficient mutants were screened. Following confirmation of negligible spontaneous mutation, eight genetically stable S. cerevisiae respiration-deficient mutant strains and a control strain were resequenced with ~ 200-fold read depth. Strategies were established to identify and validate the particular mutations induced by CIB irradiation. In the nuclear genome, CIB irradiation mainly caused base substitutions and some small (< 100 bp) insertions/deletions (indels), which were widely distributed across the chromosomes. Although mitochondrial dysfunction was selected as a screening marker, variants in the nuclear genome were detected at a high frequency (10−7) relative to spontaneous mutations (10−9). The transition to transversion ratio for base substitutions was 0.746, which was less than that of spontaneous mutations. In the mitochondrial genome, there were very large deletions including substantial gene areas, resulting in extremely low read coverage. Meanwhile, every mutant possessed a distinctive mutation pattern, for both the nuclear and the mitochondrial genome. Nuclear genomes contained scanty mitochondrial respiration-related genes that were potentially affected by verified mutations, suggesting that variants in the mitochondrial genome may be the main drivers of respiratory deficiencies. Our study confirmed the previous finding that heavy ion beam (HIB) irradiation mainly induces substantial base substitutions and some small indels but also yielded some novel findings, in particular, novel structural variants in the mitochondrial genomes. These data will enhance the understanding of HIB-induced damage and mutations and aid in the HIB-based microbial mutation breeding. [ABSTRACT FROM AUTHOR]

Published

2019

8. Genetic analysis of fundic gland‑type gastric adenocarcinoma.

Author

Liu, Lei, Zhang, Xuedong, Fan, Xue, and Zhu, Xiaoyun

Subjects

NUCLEIC acids, GENETIC mutation, MISSENSE mutation, IN situ hybridization, CHINESE people

Abstract

This study aimed to analyze the molecular characteristics of gastric adenocarcinoma of the fundic-gland type (GAFG) and explore the possible mechanism of tumor development. Samples from 10 Chinese patients with GAFG were collected at the Peking University International Hospital and Liaocheng People's Hospital between January 2015 and March 2022. The nucleic acid sequence of Epstein Barr virus-encoded RNA (EBV-EBER) was detected by in situ hybridization. Genetic mutation information for GNAS, KRAS, NRAS, BRAF, PIK3CA, TP53, APC, CTNNB1, HER2, MLH1, MSH2, MSH6, and PMS2 was obtained by Next-Generation Sequencing, and the relevant literature was reviewed. A total of eight instances of missense mutations were detected, consisting of seven cases with GNAS mutations, two cases with KRAS mutations, and one case with a TP53 mutation. Additionally, two patients had simultaneous missense mutations in GNAS and KRAS. Nonsynonymous mutations in APC, CTNNB1, NRAS, BRAF, PIK3CA, HER2, MLH1, MSH2, MSH6, or PMS2 were not observed in any cases. In addition, all tumors were EBER-negative. GAFG exhibits diversity at the molecular level, and GNAS mutations are more common than KRAS mutations, TP53 mutations, and microsatellite instability. To date, no association between EBV/HER2 and GAFG has been found. [ABSTRACT FROM AUTHOR]

Published

2023

9. FLT3-ITD Compared with DNMT3A R882 Mutation Is a More Powerful Independent Inferior Prognostic Factor in Adult Acute Myeloid Leukemia Patients After Allogeneic Hematopoietic Stem Cell Transplantation: A Retrospective Cohort Study.

Author

Ardestani, Majid Teremmahi, Kazemi, Ahmad, Chahardouli, Bahram, Mohammadi, Saeed, Nikbakht, Mohsen, Rostami, Shahrbano, Jalili, Mahdi, Vaezi, Mohammad, Alimoghaddam, Kamran, and Ghavamzadeh, Ardeshir

Subjects

BLOOD testing, CANCER relapse, GENETIC techniques, HEMATOPOIETIC stem cell transplantation, HOMOGRAFTS, LONGITUDINAL method, GENETIC mutation, POSTOPERATIVE period, PROTEIN-tyrosine kinases, STATISTICS, SURVIVAL, STEM cell research, TREATMENT effectiveness, DISEASE prevalence, ACUTE myeloid leukemia, RETROSPECTIVE studies, KAPLAN-Meier estimator, SEQUENCE analysis, LOG-rank test, ADULTS, GENETICS, PROGNOSIS

Abstract

Copyright of Turkish Journal of Hematology is the property of Galenos Yayinevi Tic. LTD. STI and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2018

10. Full-length mutation search of the TP53 gene in acute myeloid leukemia has increased significance as a prognostic factor.

Author

Terada, Kazuki, Yamaguchi, Hiroki, Ueki, Toshimitsu, Usuki, Kensuke, Kobayashi, Yutaka, Tajika, Kenji, Gomi, Seiji, Kurosawa, Saiko, Miyadera, Keiki, Tokura, Taichiro, Omori, Ikuko, Marumo, Atushi, Fujiwara, Yusuke, Yui, Shunsuke, Ryotokuji, Takeshi, Osaki, Yoshiki, Arai, Kunihito, Kitano, Tomoaki, Kosaka, Fumiko, and Wakita, Satoshi

Subjects

ACUTE myeloid leukemia, GENETIC mutation, P53 protein, DNA-binding proteins, PATIENTS, PROGNOSIS

Abstract

TP53 gene abnormality has been reported to be an unfavorable prognostic factor in acute myeloid leukemia (AML). However, almost all studies of TP53 gene abnormality so far have been limited to mutation searches in the DNA binding domain. As there have been few reports examining both mutation and deletion over the full-length of the TP53 gene, the clinical characteristics of TP53 gene abnormality have not yet been clearly established. In this study, TP53 gene mutation was observed in 7.3% of the total 412 de novo AML cases (33 mutations in 30 cases), with mutation outside the DNA binding domain in eight cases (27%). TP53 gene deletion was observed in 3.1% of 358 cases. All cases had monoallelic deletion with TP53 gene mutation on the opposite allele. Multivariate analysis demonstrated that TP53 gene mutation in the DNA binding domain and outside the DNA binding domain was an independent poor prognostic factor for overall survival and relapse-free survival among the total cohort and it is also an unfavorable prognostic factor in FLT3-ITD-negative AML cases aged 70 years or below with intermediate cytogenetic prognosis. In stratified treatment, full-length search for TP53 gene mutation is therefore very important. [ABSTRACT FROM AUTHOR]

Published

2018

11. Identification of genome variations in patients with lung adenocarcinoma using whole genome re-sequencing.

Author

GUIYUAN LI, YUNQING MEI, FAN YANG, SHENGMING YI, and LEMIN WANG

Subjects

ADENOCARCINOMA, CANCER treatment, NUCLEOTIDE sequencing, EPIDERMAL growth factor receptors, GENETIC mutation

Abstract

Lung adenocarcinoma is one of the types of non-small cell lung carcinoma, which tends to be treated with surgical therapy rather than radiation therapy. It occurs in smokers and non-smokers, and is the most common form of lung cancer among non-smokers and women. Gene rearrangements, including ALK, ROS1 and RET, and gene mutations, including epidermal growth factor receptor (EGFR), HER2, Kristen rat sarcoma viral oncogene homolog, BRAF, phosphoinositide-3-kinase, catalytic, a polypeptide and MET, have been identified in lung adenocarcinoma, which enable targeted therapy in lung adenocarcinoma, for example erlotinib, gefitinib and afatinib, which are EGFR inhibitors. The aim of the present study was to further investigate genome variations in lung adenocarcinoma. Single nucleotide polymorphisms (SNPs), insertions and deletions (InDels), structural variations (SVs) and copy number variations (CNVs) were identified in the whole genome from four patients with adenocarcinoma using a whole genome re-sequencing method performed on the Illumina HiSeq Xten platform. In total, ~415 GB of clean reads were obtained, the average sequencing depth was 31.10-fold, and 99.29% of the reference genome was covered by the clean reads. An average of 3,364,270 SNPs was identified, 98.76% of which were matched to the SNP database (dbSNP), and an average of 453,547 InDels were identified, 28.28% of which were in the dbSNP. The present study also identified a total of 13,050 SVs and 886 CNVs. The majority of the SVs were deletions (74.25%) and the major CNVs were in intergenic regions and coding sequence regions. In conclusion, the results of the present study generated an output of the genome alterations in lung adenocarcinoma, and provided a foundation for further investigation of the pathogenesis of lung adenocarcinoma. [ABSTRACT FROM AUTHOR]

Published

2017

12. IDH1 Mutation Is an Independent Inferior Prognostic Indicator for Patients with Myelodysplastic Syndromes.

Author

Wang, Na, Wang, Fei, Shan, Ningning, Sui, Xiaohui, and Xu, Hongzhi

Subjects

MYELODYSPLASTIC syndromes, NUCLEOTIDE sequencing, ISOCITRATE dehydrogenase, ANEMIA, GENETIC mutation

Abstract

Background: Genomic sequencing technologies have identified isocitrate dehydrogenase ( IDH ) mutations in haematological malignancies. The prognostic implications of somatic IDH mutation ( mIDH ) in myelodysplastic syndromes (MDS) remain controversial. Methods: Mutations in IDH1 and IDH2 were detected using genomic sequencing technologies in 97 patients with MDS. Results: Seven (7.2%) mutations were identified: 3 in IDH1 (all R132C) and 4 in IDH2 (3 R140Q and 1 R140L). The frequency of mutation was 16.6% (2/12) in refractory anaemia with excess blasts (RAEB)-1 and 14.7% (5/34) in RAEB-2. IDH1 / 2 mutations were closely associated with higher bone marrow blast counts (median 10.0 vs. 2.3%; p = 0.019) and lower absolute neutrophil counts (median 0.44 x 10 9 /L vs. 1.21 x 10 9 /L; p = 0.027). All IDH mutations were mutually exclusive and heterozygous. IDH mutations were not significantly correlated with any specific karyotype. Patients with IDH1 mutations exhibited shorter overall and progression-free survival (OS and PFS; p = 0.039 and p = 0.042, respectively), whereas IDH2 mutations did not affect OS or PFS ( p = 0.560 and p = 0.218, respectively). Multivariate analysis indicated that IDH1 mutation ( p = 0.018; hazard ratio [HR] 4.735; 95% confidence interval [CI] 1.299-17.264), karyotype risk ( p = 0.036; HR 1.619; 95% CI 1.033-2.539) and the revised International Prognostic Scoring System risk category ( p < 0.0001; HR 2.122; 95% CI 1.401-3.213) were independent inferior prognostic factors. Conclusions: IDH1 mutation is associated with a poor prognosis. [ABSTRACT FROM AUTHOR]

Published

2017

13. Toward a consensus on SNP and STR mutation rates on the human Y-chromosome.

Author

Balanovsky, O.

Subjects

POPULATION genetics, Y chromosome, GENETIC mutation, GENETIC genealogy, DNA

Abstract

The mutation rate on the Y-chromosome matters for estimating the time-to-the-most-recent-common-ancestor (TMRCA, i.e. haplogroup age) in population genetics, as well as for forensic, medical, and genealogical studies. Large-scale sequencing efforts have produced several independent estimates of Y-SNP mutation rates. Genealogical, or pedigree, rates tend to be slightly faster than evolutionary rates obtained from ancient DNA or calibrations using dated (pre)historical events. It is, therefore, suggested to report TMRCAs using an envelope defined by the average aDNA-based rate and the average pedigree-based rate. The current estimate of the 'envelope rate' is 0.75-0.89 substitutions per billion base pairs per year. The available Y-SNP mutation rates can be applied to high-coverage data from the entire X-degenerate region, but other datasets may demand recalibrated rates. While a consensus on Y-SNP rates is approaching, the debate on Y-STR rates has continued for two decades, because multiple genealogical rates were consistent with each other but three times faster than the single evolutionary estimate. Applying Y-SNP and Y-STR rates to the same haplogroups recently helped to clarify the issue. Genealogical and evolutionary STR rates typically provide lower and upper bounds of the 'true' (SNP-based) age. The genealogical rate often-but not always-works well for haplogroups less than 7000 years old. The evolutionary rate, although calibrated using recent events, inflates ages of young haplogroups and deflates the age of the entire Y-chromosomal tree, but often provides reasonable estimates for intermediate ages (old haplogroups). Future rate estimates and accumulating case studies should further clarify the Y-SNP rates. [ABSTRACT FROM AUTHOR]

Published

2017

14. The Y chromosomes of the great apes.

Author

Hallast, Pille and Jobling, Mark

Subjects

HOMINIDS, Y chromosome, X chromosome, CHROMOSOME structure, GENETIC mutation

Abstract

The great apes (orangutans, gorillas, chimpanzees, bonobos and humans) descended from a common ancestor around 13 million years ago, and since then their sex chromosomes have followed very different evolutionary paths. While great-ape X chromosomes are highly conserved, their Y chromosomes, reflecting the general lability and degeneration of this male-specific part of the genome since its early mammalian origin, have evolved rapidly both between and within species. Understanding great-ape Y chromosome structure, gene content and diversity would provide a valuable evolutionary context for the human Y, and would also illuminate sex-biased behaviours, and the effects of the evolutionary pressures exerted by different mating strategies on this male-specific part of the genome. High-quality Y-chromosome sequences are available for human and chimpanzee (and low-quality for gorilla). The chromosomes differ in size, sequence organisation and content, and while retaining a relatively stable set of ancestral single-copy genes, show considerable variation in content and copy number of ampliconic multi-copy genes. Studies of Y-chromosome diversity in other great apes are relatively undeveloped compared to those in humans, but have nevertheless provided insights into speciation, dispersal, and mating patterns. Future studies, including data from larger sample sizes of wild-born and geographically well-defined individuals, and full Y-chromosome sequences from bonobos, gorillas and orangutans, promise to further our understanding of population histories, male-biased behaviours, mutation processes, and the functions of Y-chromosomal genes. [ABSTRACT FROM AUTHOR]

Published

2017

15. The repeatability of genome-wide mutation rate and spectrum estimates.

Author

Behringer, Megan and Hall, David

Subjects

NUCLEOTIDE sequencing, GENETIC mutation, SPECIES diversity, SPECTRUM analysis, DNA repair, SCHIZOSACCHAROMYCES pombe

Abstract

Over the last decade, mutation studies have grown in popularity due to the affordability and accessibility of whole genome sequencing. As the number of species in which spontaneous mutation has been directly estimated approaches 20 across two domains of life, questions arise over the repeatability of results in such experiments. Five species were identified in which duplicate mutation studies have been performed. Across these studies the difference in estimated spontaneous mutation rate is at most, weakly significant ( p < 0.01). However, a highly significant ( p < 10), threefold difference in the rate of insertions/deletions (indels) exists between two recent studies in Schizosaccharomyces pombe. Upon investigation of the ancestral genome sequence for both studies, a possible anti-mutator allele was identified. The observed variation in indel rate may imply that the use of indel markers, such as microsatellites, for the investigation of genetic diversity within and among populations may be inappropriate because of the assumption of uniform mutation rate within a species. [ABSTRACT FROM AUTHOR]

Published

2016

16. BCR-ABL-positive acute myeloid leukemia: a new entity? Analysis of clinical and molecular features.

Author

Neuendorff, Nina, Burmeister, Thomas, Dörken, Bernd, Westermann, Jörg, Neuendorff, Nina Rosa, Dörken, Bernd, and Westermann, Jörg

Subjects

CHRONIC myeloid leukemia, LEUKEMIA treatment, ACUTE myeloid leukemia, PROTEIN-tyrosine kinase inhibitors, MYELODYSPLASTIC syndromes, STEM cell transplantation, PROTEIN kinase inhibitors, ALGORITHMS, DIFFERENTIAL diagnosis, GENES, HOMOGRAFTS, GENETIC mutation, PROGNOSIS, PROTEINS, TRANSFERASES, MYELOID leukemia, TREATMENT effectiveness, NUCLEAR proteins, ACUTE diseases, THERAPEUTICS

Abstract

BCR-ABL-positive acute myeloid leukemia (AML) is a rare subtype of AML that is now included as a provisional entity in the 2016 revised WHO classification of myeloid malignancies. Since a clear distinction between de novo BCR-ABL+ AML and chronic myeloid leukemia (CML) blast crisis is challenging in many cases, the existence of de novo BCR-ABL+ AML has been a matter of debate for a long time. However, there is increasing evidence suggesting that BCR-ABL+ AML is in fact a distinct subgroup of AML. In this study, we analyzed all published cases since 1975 as well as cases from our institution in order to present common clinical and molecular features of this rare disease. Our analysis shows that BCR-ABL predominantly occurs in AML-NOS, CBF leukemia, and AML with myelodysplasia-related changes. The most common BCR-ABL transcripts (p190 and p210) are nearly equally distributed. Based on the analysis of published data, we provide a clinical algorithm for the initial differential diagnosis of BCR-ABL+ AML. The prognosis of BCR-ABL+ AML seems to depend on the cytogenetic and/or molecular background rather than on BCR-ABL itself. A therapy with tyrosine kinase inhibitors (TKIs) such as imatinib, dasatinib, or nilotinib is reasonable, but-due to a lack of systematic clinical data-their use cannot be routinely recommended in first-line therapy. Beyond first-line treatment of AML, the use of TKI remains an individual decision, both in combination with intensive chemotherapy and/or as a bridge to allogeneic stem cell transplantation. In each single case, potential benefits have to be weighed against potential risks. [ABSTRACT FROM AUTHOR]

Published

2016

17. Deciphering intratumor heterogeneity using cancer genome analysis.

Author

Ryu, Daeun, Joung, Je-Gun, Kim, Nayoung, Kim, Kyu-Tae, and Park, Woong-Yang

Subjects

GENOMICS, NUCLEOTIDE sequencing, GENETIC mutation, DNA analysis, HETEROGENEITY

Abstract

Intratumor heterogeneity within individual cancer tissues underlies the numerous phenotypes of cancer. Tumor subclones ultimately affect therapeutic outcomes due to their distinct molecular features. Drug-resistant subclones are present at a low frequency in tissues at the time of biopsy, but can also arise as a result of acquired somatic mutations. A number of different approaches have been utilized to understand the nature of intratumor heterogeneity. Clonal analysis using whole exome or genome sequencing data can help monitor subclones in the context of tumor progression. Multiregional biopsies permit the molecular characterization of subclones within tumors. Deep sequencing has also provided researchers with the ability to measure the low allele fraction variant within a small number of cells. Ultimately, single-cell sequencing will enable the identification of every minor population within a tumor microenvironment. In the clinical context, the ability to identify and monitor the subclonal architecture of a tumor is valuable for the development of precise cancer therapeutic methods. [ABSTRACT FROM AUTHOR]

Published

2016

18. Genomic Alteration During Metastasis of Lung Adenocarcinoma.

Author

Tan, Qiang, Cui, Jian, Huang, Jia, Ding, Zhengping, Lin, Hao, Niu, Xiaomin, Li, Zhiming, Wang, Guan, Luo, Qingquan, and Lu, Shun

Subjects

LUNG cancer treatment, ADENOCARCINOMA, DISEASE relapse, GENOMICS, GENETIC mutation, NATURAL selection

Abstract

Background/Aims: Recurrent gene mutation has been identified by the analysis of exonic DNA from lung adenocarcinoma, but its progression has not been extensively profiled. The investigation of the mutational landscape of tumors provides new insights into cancer genome evolution and further discovers the interplay of somatic mutation, adaptation of clones to their environment and natural selection. Cancer development involves cycles of genomic damage, epigenetic deregulation, and increased cellular proliferation that eventually culminate in the carcinoma phenotype. Methods: Comparative whole exome sequencing of both primary and metastatic tumor tissues from four patients of stage IV lung adenocarcinoma patients with chest wall metastasis was performed. Both primary and metastatic tumors were diagnosed through biopsy followed by surgical resection. All tumor specimens were cut into several pieces to assess potential heterogenic clones within the tumor tissue. Adjacent normal lung tissue was also obtained to provide germline mutation background. Results: By modeling and analyzing progression of the cancer metastasis based on non-synonymous variants, we defined the extent of heterogeneity of cancer genomes and identified similar cancer evolution pattern in the four patients: metastasis was an early event occurring right after the primary cancer formation and evolution in the metastatic tumor was continuously and simultaneously in progression with that in the primary tumor. By characterizing the clonal hierarchy of genetic lesions, we further charted a pathway of oncogenic events along which genes may drive lung adenocarcinoma metastasis, such as TAS2R31 and UMODL1, involving in G-protein coupled receptor protein signaling pathway. Conclusion: The candidate genes identified in this study may become targets for the treatment of lung adenocarcinoma metastasis. © 2016 S. Karger AG, Basel [ABSTRACT FROM AUTHOR]

Published

2016

19. No Mutation Left Behind: The Impact of Reporting Recurrent Genetic Abnormalities on Outcomes of Patients with Acute Myeloid Leukemia.

Author

Brunner, Andrew M.

Subjects

ACUTE myeloid leukemia, GENETIC mutation

Abstract

A review of the article "Incidence, survival, and risk factors for adults with acute myeloid leukemia (AML) not otherwise specified and AML with recurrent genetic abnormalities: analysis of the Surveillance, Epidemiology, and End Results (SEER) database" by X Song is presented.

Published

2018

20. Longitudinal analysis of 25 sequential sample-pairs using a custom multiple myeloma mutation sequencing panel (MP).

Author

Kortüm, K., Langer, C., Monge, J., Bruins, L., Zhu, Y., Shi, C., Jedlowski, P., Egan, J., Ojha, J., Bullinger, L., Kull, M., Ahmann, G., Rasche, L., Knop, S, Fonseca, R., Einsele, H., Stewart, A., and Braggio, Esteban

Subjects

MULTIPLE myeloma, NUCLEOTIDE sequencing, BORTEZOMIB, DRUG resistance in cancer cells, GENETIC mutation, RAS oncogenes

Abstract

Recent advances in genomic sequencing technologies now allow results from deep next-generation sequencing to be obtained within clinically meaningful timeframes, making this an attractive approach to better guide personalized treatment strategies. No multiple myeloma-specific gene panel has been established so far; we therefore designed a 47-gene-targeting gene panel, containing 39 genes known to be mutated in ≥3 % of multiple myeloma cases and eight genes in pathways therapeutically targeted in multiple myeloma (MM). We performed targeted sequencing on tumor/germline DNA of 25 MM patients in which we also had a sequential sample post treatment. Mutation analysis revealed KRAS as the most commonly mutated gene (36 % in each time point), followed by NRAS (20 and 16 %), TP53 (16 and 16 %), DIS3 (16 and 16 %), FAM46C (12 and 16 %), and SP140 (12 and 12 %). We successfully tracked clonal evolution and identified mutation acquisition and/or loss in FAM46C, FAT1, KRAS, NRAS, SPEN, PRDM1, NEB, and TP53 as well as two mutations in XBP1, a gene associated with bortezomib resistance. Thus, we present the first longitudinal analysis of a MM-specific targeted sequencing gene panel that can be used for individual tumor characterization and for tracking clonal evolution over time. [ABSTRACT FROM AUTHOR]

Published

2015

21. The utility of next-generation sequencing in diagnosis and monitoring of acute myeloid leukemia and myelodysplastic syndromes.

Author

Duncavage, E. J. and Tandon, B.

Subjects

ACUTE myeloid leukemia, ACUTE myeloid leukemia treatment, MYELODYSPLASTIC syndromes treatment, MYELODYSPLASTIC syndromes, ACUTE myeloid leukemia diagnosis, GENES, GENETIC mutation, SEQUENCE analysis, DIAGNOSIS, GENETICS

Abstract

Myeloid malignancies including acute myeloid leukemia ( AML) and myelodysplastic syndromes ( MDS) are a heterogeneous group of disorders that share a common biology and are a major source of morbidity and mortality. In the last several years, studies using next-generation sequencing ( NGS) have identified a core set of recurrently mutated myeloid malignancy genes in the majority of patients with AML and MDS, including those with normal cytogenetics. DNA-level mutations in several of these genes including NPM1, FLT3, and CEBPA in AML and ASXL1, ETV6, EZH2, RUNX1, and TP53 in MDS are associated with changes in patient outcomes and are now tested for in clinical laboratories. In addition to providing prognostic information, these gene mutations can be used to monitor patient disease burden through the use of ultrasensitive detection techniques. In this review, we will focus on the clinical utility of various NGS-based methods including whole-genome sequencing, exome sequencing, and targeted panel-based sequencing in the initial diagnosis and management of AML and MDS and cover recent methodological advances for the molecular monitoring of AML and MDS. [ABSTRACT FROM AUTHOR]

Published

2015

22. The diagnostic and clinical impact of genetics and epigenetics in acute myeloid leukemia.

Author

Ohgami, R. S. and Arber, D. A.

Subjects

ACUTE myeloid leukemia, ACUTE myeloid leukemia diagnosis, CHROMOSOME abnormalities, CYTODIAGNOSIS, GENES, GENETIC mutation, DNA methylation, EPIGENOMICS, GENETICS

Abstract

Acute myeloid leukemia ( AML) is a complex disease, for which our understanding of the role of genetic and epigenetic changes has undergone significant advancements. Newer diagnostic and prognostic classifications have increasingly incorporated such information, and novel therapies have been developed to target specific genes, processes, and pathways based on this growing understanding. Given the rapid evolution of this field, it is critical for physicians and translational researchers to have a more in-depth understanding of this evolving landscape. Here, we review both genetics and epigenetics in acute myeloid leukemia from a practical standpoint. [ABSTRACT FROM AUTHOR]

Published

2015

23. Multiple system atrophy: the application of genetics in understanding etiology.

Author

Federoff, Monica, Schottlaender, Lucia, Houlden, Henry, and Singleton, Andrew

Subjects

MULTIPLE system atrophy, ETIOLOGY of diseases, NEURODEGENERATION, COHORT analysis, SINGLE nucleotide polymorphisms, GENETIC mutation, GENETICS

Abstract

Classically defined phenotypically by a triad of cerebellar ataxia, parkinsonism, and autonomic dysfunction in conjunction with pyramidal signs, multiple system atrophy (MSA) is a rare and progressive neurodegenerative disease affecting an estimated 3-4 per every 100,000 individuals among adults 50-99 years of age. With a pathological hallmark of alpha-synuclein-immunoreactive glial cytoplasmic inclusions (GCIs; Papp-Lantos inclusions), MSA patients exhibit marked neurodegenerative changes in the striatonigral and/or olivopontocerebellar structures of the brain. As a member of the alpha-synucleinopathy family, which is defined by its well-demarcated alpha-synuclein-immunoreactive inclusions and aggregation, MSA's clinical presentation exhibits several overlapping features with other members including Parkinson's disease (PD) and dementia with Lewy bodies (DLB). Given the extensive fund of knowledge regarding the genetic etiology of PD revealed within the past several years, a genetic investigation of MSA is warranted. While a current genome-wide association study is underway for MSA to further clarify the role of associated genetic loci and single-nucleotide polymorphisms, several cases have presented solid preliminary evidence of a genetic etiology. Naturally, genes and variants manifesting known associations with PD (and other phenotypically similar neurodegenerative disorders), including SNCA and MAPT, have been comprehensively investigated in MSA patient cohorts. More recently variants in COQ2 have been linked to MSA in the Japanese population although this finding awaits replication. Nonetheless, significant positive associations with subsequent independent replication studies have been scarce. With very limited information regarding genetic mutations or alterations in gene dosage as a cause of MSA, the search for novel risk genes, which may be in the form of common variants or rare variants, is the logical nexus for MSA research. We believe that the application of next generation genetic methods to MSA will provide valuable insight into the underlying causes of this disease, and will be central to the identification of etiologic-based therapies. [ABSTRACT FROM AUTHOR]

Published

2015

24. Lower frequency of NPM1 and FLT3- ITD mutations in a South African adult de novo AML cohort.

Author

Marshall, R. C., Tlagadi, A., Bronze, M., Kana, V., Naidoo, S., Wiggill, T. M., and Carmona, S. C.

Subjects

ACUTE myeloid leukemia, AGE factors in disease, CYTOGENETICS, FISHER exact test, LONGITUDINAL method, GENETIC mutation, PROBABILITY theory, STATISTICS, DATA analysis software, MANN Whitney U Test, GENETICS

Abstract

Introduction Acute myeloid leukemia ( AML) is a heterogeneous clonal disorder of hemopoietic progenitor cells diagnosed in individuals of any age, but with a median age of 67 years at presentation in adults. Assessment of the mutation status of nucleophosmin protein-1 ( NPM1) and FMS-like tyrosine kinase 3 internal tandem duplication ( FLT3- ITD) is essential for the prognosis, and treatment of AML. Methods A total of 160 de novo AML cases, both cytogenetically normal and abnormal, were analyzed for the presence of NPM1 and FLT3- ITD mutations, and the results assessed in conjunction with epidemiological, clinical, and laboratory findings. Results Nucleophosmin protein-1 mutations were found in 7.5%, while FLT3- ITD was present in 12% of these cases. Both of these were lower than expected. The median age at diagnosis of AML was 41 years, and for the FLT3- ITD only cases, median age was 33 years; these ages were younger than expected. Conclusion The lower reported frequencies and younger median age at diagnosis of AML and these specific mutations may be contributed to by a number of factors including effects of race on age of presentation, inclusion of patients diagnosed with de novo AML only, and a generally younger median age of the South African population. [ABSTRACT FROM AUTHOR]

Published

2014

25. Cancer genomics identifies disrupted epigenetic genes.

Author

Simó-Riudalbas, Laia and Esteller, Manel

Subjects

EPIGENETICS, CANCER genetics, CANCER research, GENETIC regulation, GENETIC mutation, CELL lines

Abstract

Latest advances in genome technologies have greatly advanced the discovery of epigenetic genes altered in cancer. The initial single candidate gene approaches have been coupled with newly developed epigenomic platforms to hasten the convergence of scientific discoveries and translational applications. Here, we present an overview of the evolution of cancer epigenomics and an updated catalog of disruptions in epigenetic pathways, whose misregulation can culminate in cancer. The creation of these basic mutational catalogs in cell lines and primary tumors will provide us with enough knowledge to move diagnostics and therapy from the laboratory bench to the bedside. [ABSTRACT FROM AUTHOR]

Published

2014

26. Comparative examination of various PCR-based methods for DNMT3A and IDH1/2 mutations identification in acute myeloid leukemia.

Author

Berenstein, Rimma, Wolfgang Blau, Igor, Kar, Asiye, Cay, Ruhiye, Sindram, Annette, Seide, Claudia, and Blau, Olga

Subjects

GENETIC mutation, ACUTE myeloid leukemia, DNA methyltransferases, NUCLEOTIDE sequencing, ENDONUCLEASES

Abstract

Background Mutations in epigenetic modifiers were reported in patients with acute myeloid leukaemia (AML) including mutations in DNA methyltransferase 3A gene (DNMT3A) in 20%-30% patients and mutations in isocitrate dehydrogenase 1/2 gene (IDH1/2) in 5%-15% patients. Novel studies have shown that mutations in DNMT3A and IDH1/2 influence prognosis, indicating an increasing need to detect these mutations during routine laboratory analysis. DNA sequencing for the identification of these mutations is time-consuming and cost-intensive. This study aimed to establish rapid screening tests to identify mutations in DNMT3A and IDH1/2 that could be applied in routine laboratory procedures and that could influence initial patient management. Methods In this study we developed an endonuclease restriction method to identify the most common DNMT3A mutation (R882H) and an amplification-refractory mutation system (ARMS) to analyse IDH2 R140Q mutations. Furthermore, we compared these methods with HRM analysis and evaluated the latter for the detection of IDH1 mutations. Results Of 230 samples from patients with AML 30 (13%) samples had DNMT3A mutations, 16 (7%) samples had IDH2 R140Q mutations and 36 (16%) samples had IDH1 mutations. Sensitivity assays performed using serial dilutions of mutated DNA showed that ARMS analysis had a sensitivity of 4.5%, endonuclease restriction had a sensitivity of 0.05% and HRM analysis had a sensitivity of 5.9%-7.8% for detecting different mutations. HRM analysis was the best screening method to determine the heterogeneity of IDH1 mutations. Furthermore, for the identification of mutations in IDH2 and DNMT3A, endonuclease restriction and ARMS methods showed a perfect concordance (100%) with Sanger sequencing while HRM analysis showed a near-perfect concordance (approximately 98%). Conclusion Our study suggested that all the developed methods were rapid, specific and easy to use and interpret. HRM analysis is the most timesaving and cost-efficient method to rapidly screen all the 3 genes at diagnosis in samples obtained from patients with AML. Endonuclease restriction and ARMS assays can be used separately or in combination with HRM analysis to obtain more reliable results. We propose that early screening of mutations in patients with AML having normal karyotype could facilitate risk stratification and improve treatment options. [ABSTRACT FROM AUTHOR]

Published

2014

27. The translation of cancer genomics: time for a revolution in clinical cancer care.

Author

Mardis, Elaine R.

Subjects

CANCER genetics, CANCER treatment, GENETIC mutation, GENOMICS, LIFE sciences, CANCER invasiveness

Abstract

The introduction of next-generation sequencing technologies has dramatically impacted the life sciences, perhaps most profoundly in the area of cancer genomics. Clinical applications of next-generation sequencing and associated methods are emerging from ongoing large-scale discovery projects that have catalogued hundreds of genes as having a role in cancer susceptibility, onset and progression. For example, discovery cancer genomics has confirmed that many of the same genes are altered by mutation, copy number gain or loss, or structural variation across multiple tumor types, resulting in a gain or loss of function that likely contributes to cancer development in these tissues. Beyond these frequently mutated genes, we now know there is a 'long tail' of less frequently mutated, but probably important, genes that play roles in cancer onset or progression. Here, I discuss some of the remaining barriers to clinical translation, and look forward to new applications of these technologies in cancer care. [ABSTRACT FROM AUTHOR]

Published

2014

28. Regulatory variation: an emerging vantage point for cancer biology.

Author

Li, Luolan, Lorzadeh, Alireza, and Hirst, Martin

Subjects

HUMAN genetic variation, GENETICS, GENOMES, CANCER, GENETIC mutation

Abstract

Transcriptional regulation involves complex and interdependent interactions of noncoding and coding regions of the genome with proteins that interact and modify them. Genetic variation/mutation in coding and noncoding regions of the genome can drive aberrant transcription and disease. In spite of accounting for nearly 98% of the genome comparatively little is known about the contribution of noncoding DNA elements to disease. Genome-wide association studies of complex human diseases including cancer have revealed enrichment for variants in the noncoding genome. A striking finding of recent cancer genome re-sequencing efforts has been the previously underappreciated frequency of mutations in epigenetic modifiers across a wide range of cancer types. Taken together these results point to the importance of dysregulation in transcriptional regulatory control in genesis of cancer. Powered by recent technological advancements in functional genomic profiling, exploration of normal and transformed regulatory networks will provide novel insight into the initiation and progression of cancer and open new windows to future prognostic and diagnostic tools. WIREs Syst Biol Med 2014, 6:37-59. doi: 10.1002/wsbm.1250 For further resources related to this article, please visit the WIREs website. Conflict of interest: The author has declared no conflicts of interest for this article. [ABSTRACT FROM AUTHOR]

Published

2014

29. BCR-ABL1 kinase domain mutations may persist at very low levels for many years and lead to subsequent TKI resistance.

Author

Parker, W T, Yeoman, A L, Jamison, B A, Yeung, D T, Scott, H S, Hughes, T P, and Branford, S

Subjects

CHRONIC myeloid leukemia, GENETIC mutation, IMATINIB, DRUG resistance in cancer cells, LONGITUDINAL method, AMINO acid sequence

Abstract

Background:BCR-ABL1 mutation analysis is recommended for chronic myeloid leukaemia patients. However, mutations may become undetectable after changing therapy, and it is unknown whether they have been eradicated.Methods:We examined longitudinal data of patients with imatinib-resistant mutations, which became undetectable by Sanger sequencing to determine whether mutations could reappear, and the related circumstances.Results:Identical imatinib- and nilotinib-resistant mutations reappeared following further therapy changes in five patients, and was associated with subsequent nilotinib resistance in four.Conclusion:The data suggest that some BCR-ABL1 mutations may persist at undetectable levels for many years after changing therapy, and can be reselected and confer resistance to subsequent inhibitors. [ABSTRACT FROM AUTHOR]

Published

2013

30. Acute myeloid leukemia: advances in diagnosis and classification.

Author

Hasserjian, R. P.

Subjects

ACUTE myeloid leukemia diagnosis, CYTODIAGNOSIS, GENES, KARYOTYPES, GENETIC mutation, PROGNOSIS, TUMORS, ACUTE myeloid leukemia, GENETICS

Abstract

Acute myeloid leukemia is an aggressive myeloid neoplasm characterized by ≥20% myeloblasts in the blood or bone marrow. Current treatment strategies for acute myeloid leukemia are based on both patient-related parameters such as age and performance status as well as the intrinsic characteristics of particular disease subtypes. Subtyping of acute myeloid leukemia requires an integration of information from the patient's clinical history (such as any prior preleukemic myeloid neoplasm or cytotoxic potentially leukemogenic therapy), the leukemia morphology, cytogenetic findings, and the mutation status of particular genes ( NPM1, FLT3, and CEBPA). In recent years, a barrage of information has become available regarding gene mutations that occur in acute myeloid leukemia and their influence on prognosis. Future therapies for acute myeloid leukemia will increasingly rely on the genetic signatures of individual leukemias and will adjust therapy to the predicted disease aggressiveness as well as employ therapies targeted against particular deregulated genetic pathways. This article reviews current standards for diagnosing and classifying acute myeloid leukemia according to the 2008 WHO Classification. Data that have subsequently accumulated regarding newly characterized gene mutations are also presented. It is anticipated that future leukemia classifications will employ a combination of karyotypic features and the gene mutation pattern to stratify patients to increasingly tailored treatment plans. [ABSTRACT FROM AUTHOR]

Published

2013

31. Genome-wide analysis of macrosatellite repeat copy number variation in worldwide populations: evidence for differences and commonalities in size distributions and size restrictions.

Author

Schaap, Mireille, Lemmers, Richard J. L. F., Maassen, Roel, van der Vliet, Patrick J., Hoogerheide, Lennart F., van Dijk, Herman K., Baştürk, Nalan, de Knijff, Peter, and van der Maarel, Silvère M.

Subjects

MICROSATELLITE repeats, X chromosome, GENETIC polymorphisms, BIOLOGICAL variation, POPULATION genetics, GENETIC mutation, DNA, BAYES' theorem, TANDEM repeats

Abstract

Background: Macrosatellite repeats (MSRs), usually spanning hundreds of kilobases of genomic DNA, comprise a significant proportion of the human genome. Because of their highly polymorphic nature, MSRs represent an extreme example of copy number variation, but their structure and function is largely understudied. Here, we describe a detailed study of six autosomal and two X chromosomal MSRs among 270 HapMap individuals from Central Europe, Asia and Africa. Copy number variation, stability and genetic heterogeneity of the autosomal macrosatellite repeats RS447 (chromosome 4p), MSR5p (5p), FLJ40296 (13q), RNU2 (17q) and D4Z4 (4q and 10q) and X chromosomal DXZ4 and CT47 were investigated. Results: Repeat array size distribution analysis shows that all of these MSRs are highly polymorphic with the most genetic variation among Africans and the least among Asians. A mitotic mutation rate of 0.4-2.2% was observed, exceeding meiotic mutation rates and possibly explaining the large size variability found for these MSRs. By means of a novel Bayesian approach, statistical support for a distinct multimodal rather than a uniform allele size distribution was detected in seven out of eight MSRs, with evidence for equidistant intervals between the modes. Conclusions: The multimodal distributions with evidence for equidistant intervals, in combination with the observation of MSR-specific constraints on minimum array size, suggest that MSRs are limited in their configurations and that deviations thereof may cause disease, as is the case for facioscapulohumeral muscular dystrophy. However, at present we cannot exclude that there are mechanistic constraints for MSRs that are not directly disease-related. This study represents the first comprehensive study of MSRs in different human populations by applying novel statistical methods and identifies commonalities and differences in their organization and function in the human genome. [ABSTRACT FROM AUTHOR]

Published

2013

32. Hierarchical cluster analysis of immunophenotype classify AML patients with NPM1 gene mutation into two groups with distinct prognosis.

Author

Chen, Chien-Yuan, Chou, Wen-Chien, Tsay, Woei, Tang, Jih-Luh, Ming Yao, Huang, Sheng-Yi, and Tien, Hwei-Fang

Subjects

ACUTE myeloid leukemia treatment, CLUSTER analysis (Statistics), IMMUNOPHENOTYPING, GENETIC mutation, CANCER prognosis, HEALTH outcome assessment

Abstract

Background: The prognostic implication of immunophenotyping in acute myeloid leukemia (AML) patients with NPM1 mutation remains unclear. Methods: Ninety-four of 543 AML patients diagnosed with NPM1 mutation between 1987 and 2007 were studied. The expression of surface antigens on leukemic cells was evaluated with respect to clinical manifestations and outcomes. In order to validate the prognostic effect of the immunophenotypic cluster, another 36 patients with NPM1 mutation diagnosed between 2008 and 2010 were analyzed. Results: Ninety-four patients with NPM1 mutations and complete immunophenotyping data were enrolled for a hierarchical cluster analysis and the result was correlated with clinico-laboratory characteristics. Clustering analysis divided the patients with NPM1 mutations into the following two groups: group I, CD34(-)/CD7(-), but with variable expression of HLA-DR; and group II, HLA DR(+)/CD34(+)/CD7(+). With a median follow-up of 53 months, the group II patients had a significantly shorter relapse-free survival (RFS, median: 3 vs. 23 months, p = 0.006) and overall survival (OS, median: 11 vs. 40 months, p = 0.02) than group I patients. Multivariate analysis of variables, including clinico-laboratory data and other gene mutations revealed that the immunophenotypic cluster is an independent prognostic factor (RFS, p = 0.002; OS, p = 0.024). In order to confirm the prognostic effect of the immunophenotypic cluster, another 36 patients with NPM1 mutation diagnosed between 2008 and 2010 were validated. Hierarchical cluster analysis also showed two distinct clusters, group I patient showed significant better RFS (p = 0.021), and OS (p = 0.055). In total, we stratified 130 NPM1-mutant patients, by FLT3-ITD mutation and immunophenotypic cluster into distinct prognostic groups (RFS, p < 0.001 and OS, p = 0.017). Conclusions: Among NPM1-mutated AML, the antigen expression pattern of HLADR(+) CD34(+) CD7(+) is associated with a poor prognosis, independent to the FLT3-ITD mutation. [ABSTRACT FROM AUTHOR]

Published

2013

33. Advances in biotechnology and informatics to link variation in the genome to phenotypes in plants and animals.

Author

Appels, R., Barrero, R., and Bellgard, M.

Subjects

BIOINFORMATICS, PLANT genomes, PHENOTYPES, BIOLOGICAL variation, METHYLATION, BIOTECHNOLOGY, GENETIC mutation

Abstract

Advances in our understanding of genome structure provide consistent evidence for the existence of a core genome representing species classically defined by phenotype, as well as conditionally dispensable components of the genome that shows extensive variation between individuals of a given species. Generally, conservation of phenotypic features between species reflects conserved features of the genome; however, this is evidently not necessarily always the case as demonstrated by the analysis of the tunicate chordate Oikopleura dioica. In both plants and animals, the methylation activity of DNA and histones continues to present new variables for modifying (eventually) the phenotype of an organism and provides for structural variation that builds on the point mutations, rearrangements, indels, and amplification of retrotransposable elements traditionally considered. The translation of the advances in the structure/function analysis of the genome to industry is facilitated through the capture of research outputs in 'toolboxes' that remain accessible in the public domain. [ABSTRACT FROM AUTHOR]

Published

2013

34. Comment on "Genomic Hypomethylation in the Human Germline Associates with Selective Structural Mutability in the Human Genome.".

Author

Watson, Corey T., Garg, Paras, and Sharp, Andrew J.

Subjects

METHYLATION, GERM cells, GENOMICS, GENETIC mutation, HUMAN chromosomes

Abstract

The authors explores a study which examined the association of genomic hypomethylation in the human germline with structural mutability in the human genome. The authors investigated repeat content within methylation deserts identified in the study and observed a strong enrichment for common repeats in windows with the lowest 1% methylation, with 30% of windows defined as methylation deserts containing less than 99th percentile of total repeat content.

Published

2013

35. Enzymatic assay for quantitative analysis of ( d)-2-hydroxyglutarate.

Author

Balss, Jörg, Pusch, Stefan, Beck, Ann-Christin, Herold-Mende, Christel, Krämer, Alwin, Thiede, Christian, Buckel, Wolfgang, Langhans, Claus-Dieter, Okun, Jürgen, and Deimling, Andreas

Subjects

QUANTITATIVE research, METABOLIC disorders, TUMORS, GENETIC mutation, DEHYDROGENASES, LIQUID chromatography-mass spectrometry, GAS chromatography/Mass spectrometry (GC-MS)

Abstract

Levels of ( d)-2-hydroxyglutarate [D2HG, ( R)-2-hydroxyglutarate] are increased in some metabolic diseases and in neoplasms with mutations in the isocitrate dehydrogenase 1 ( IDH1) and isocitrate dehydrogenase 2 ( IDH2) genes. Determination of D2HG is of relevance to diagnosis and monitoring of disease. Standard detection methods of D2HG levels are liquid-chromatography-mass spectrometry or gas-chromatography-mass spectrometry. Here we present a rapid, inexpensive and sensitive enzymatic assay for the detection of D2HG levels. The assay is based on the conversion of D2HG to α-ketoglutarate (αKG) in the presence of the enzyme ( d)-2-hydroxyglutarate dehydrogenase (HGDH) and nicotinamide adenine dinucleotide (NAD). Determination of D2HG concentration is based on the detection of stoichiometrically generated NADH. The quantification limit of the enzymatic assay for D2HG in tumor tissue is 0.44 μM and in serum 2.77 μM. These limits enable detection of basal D2HG levels in human tumor tissues and serum without IDH mutations. Levels of D2HG in frozen and paraffin-embedded tumor tissues containing IDH mutations or in serum from acute myeloid leukemia patients with IDH mutations are significantly higher and can be easily identified with this assay. In conclusion, the assay presented is useful for differentiating basal from elevated D2HG levels in tumor tissue, serum, urine, cultured cells and culture supernatants. [ABSTRACT FROM AUTHOR]

Published

2012

36. Detection of 'oncometabolite' 2-hydroxyglutarate by magnetic resonance analysis as a biomarker of IDH1/2 mutations in glioma.

Author

Kalinina, Juliya, Carroll, Anne, Wang, Liya, Yu, Qiqi, Mancheno, Danny, Wu, Shaoxiong, Liu, Frank, Ahn, Jun, He, Miao, Mao, Hui, and Meir, Erwin

Subjects

MAGNETIC resonance imaging, GENETIC mutation, GLIOMAS, ISOCITRATE dehydrogenase, BRAIN tumors, DIAGNOSTIC specimens

Abstract

Somatic mutations in isocitrate dehydrogenase (IDH)1 and 2 have been identified in a subset of gliomas, rendering these tumors with elevated levels of 'oncometabolite,' D-2-hydroxyglutarate (2HG). Herein, we report that 2HG can be precisely detected by magnetic resonance (MR) in human glioma specimens and used as a reliable biomarker to identify this subset of tumors. Specifically, we developed a two-dimensional correlation spectroscopy resonance method to reveal the distinctive cross-peak pattern of 2HG in the complex metabolite nuclear MR spectra of brain tumor tissues. This study demonstrates the feasibility, specificity, and selectivity of using MR detection and quantification of 2HG for the diagnosis and classification of IDH1/2 mutation-positive brain tumors. It further opens up the possibility of developing analogous non-invasive MR-based imaging and spectroscopy studies directly in humans in the neuro-oncology clinic. [ABSTRACT FROM AUTHOR]

Published

2012

37. IDH2 mutations are frequent in Chinese patients with acute myeloid leukemia and associated with NPM1 mutations and FAB-M2 subtype.

Author

Chao, H.-y., Jia, Z.-x., Chen, T., Lu, X.-z., Cen, L., Xiao, R., Jiang, N.-k., Ying, J.-h., Zhou, M., and Zhang, R.

Subjects

MYELOID leukemia genetics, BONE marrow examination, CHI-squared test, CHROMOSOME abnormalities, FISHER exact test, KARYOTYPES, GENETIC mutation, POLYMERASE chain reaction, PROBABILITY theory, RESEARCH funding, T-test (Statistics), DATA analysis software, SEQUENCE analysis

Abstract

Introduction: Gene mutations play an important role in acute myeloid leukemia (AML) pathogenesis. Several genes have been identified in AML, such as FLT3, KIT, NPM1, and JAK2. This study investigated the frequency of novel mutations in IDH1 (amino acid R132) and IDH2 (R140 and R172) and analyzed their impact on disease biology and interaction with other mutations in Chinese patients with de novo AML. Methods: A total of 195 patients were screened for mutations in the IDH1, IDH2, JAK2 V617F , NPM1, FLT3, and KIT genes, using polymerase chain reaction (PCR)-based and direct sequencing assays. Results: IDH mutations occurred at a considerable frequency of 15.89% in Chinese AML cases; IDH2 R140Q was the most frequent genetic alteration and was associated with older age, normal karyotype, and French-American-British classification M2 at diagnosis. There was a strong association of IDH2 mutation with NPM1 mutations and a trend with FLT3-internal-tandem duplication. Conclusion: IDH mutations may be a novel genetic marker in cytogenetically normal AML and may cooperate in leukemogenesis. [ABSTRACT FROM AUTHOR]

Published

2012

38. High frequency of complex TP53 mutations in CNS metastases from breast cancer.

Author

Lo Nigro, C, Vivenza, D, Monteverde, M, Lattanzio, L, Gojis, O, Garrone, O, Comino, A, Merlano, M, Quinlan, P R, Syed, N, Purdie, C A, Thompson, A, Palmieri, C, and Crook, T

Subjects

CENTRAL nervous system cancer, BREAST cancer, GENETIC mutation, CANCER invasiveness, ONCOGENES, METASTASIS

Abstract

Background:Brain metastasis from breast cancer is usually associated with a poor prognosis and early death. Alteration of p53 may contribute to malignant progression by abrogation of apoptosis induced by oncogene activation and by acquisition of gain-of-function properties, which promote tumour aggression. Mutation in TP53 occurs at high frequency in carcinomas of the lung and gastro-intestinal tract, but is much less frequent, at 25%, in primary breast cancer. The frequency of TP53 alteration in the central nervous system (CNS) metastatic breast cancer is not known.Methods:In all, 23 cases of histologically confirmed CNS metastatic breast cancer were identified and the coding sequence of TP53 determined. TP53 was also sequenced in two control series of primary breast carcinomas from independent clinical centres.Results:We demonstrate a strikingly high frequency of TP53 mutation in the CNS metastatic lesions with an over-representation of complex mutations (non-sense/deletions/insertions). Complex mutations occur in metastatic lesions in both triple-negative breast cancer and hormone receptor/HER2-positive cases. Analysis of paired primary carcinomas and brain metastatic lesions revealed evidence for both clonal selection and generation of new mutations (missense and complex) in progression from a primary breast carcinoma to brain metastasis.Conclusion:Mutation in TP53 is the most common genetic alteration reported during metastasis to the brain in breast cancer. [ABSTRACT FROM AUTHOR]

Published

2012

39. Age-dependent frequencies of NPM1 mutations and FLT3-ITD in patients with normal karyotype AML (NK-AML).

Author

Schneider, Friederike, Hoster, Eva, Schneider, Stephanie, Dufour, Annika, Benthaus, Tobias, Kakadia, Purvi, Bohlander, Stefan, Braess, Jan, Heinecke, Achim, Sauerland, Maria, Berdel, Wolfgang, Buechner, Thomas, Woermann, Bernhard, Feuring-Buske, Michaela, Buske, Christian, Creutzig, Ursula, Thiede, Christian, Zwaan, Michel, Heuvel-Eibrink, Marry, and Reinhardt, Dirk

Subjects

GENETIC mutation, PROGNOSIS, KARYOTYPES, AGE groups, CHARACTERISTIC classes

Abstract

Prognosis of AML in elderly patients is poor due to adverse patient characteristics and comorbidities. In addition, disease-associated parameters reveal differences between older and younger patients with AML. Survival in normal karyotype AML (NK-AML) is influenced by different clinical and molecular markers. The aim of this work was to investigate the frequencies of molecular markers in patients with NK-AML with a focus on NPM1 mutations and FLT3-ITD in different age groups. In the present study, we analyzed the frequencies of mutations of NPM1 and FLT3-ITD in a cohort of 1,321 adult patients and 148 children with AML treated within the AMLCG99, the AML98, and AML04 trials and their distribution in different age groups. Additionally, the frequencies of mutations in CEBPA genes, FLT3-TKD, and MLL-PTD were analyzed in the cohort with NK-AML ( n = 729). Our data show that the presence of mutations of NPM1 (from 60% to 40%) and FLT3-ITD (from 50% to 20%) significantly decreased with age in adult AML. Consequently, the proportion of NPM1−/ FLT3-ITD− patients increased with age. The decreasing frequency of NPM1 mutations in elderly patients was paralleled by a reduced complete remission (CR) rate in the elderly of 55% compared to 80% in the younger patients. By contrast, the frequencies of other gene mutations, like FLT3-TKD and MLL-PTD, and mutations in CEBPA were not age-dependent. The decreasing frequency of the favorable NPM1 mutations with increasing age may partially explain the worse outcome in the elderly patients. Furthermore, the increasing amount of elderly patients without NPM1 mutations or FLT3-ITD suggests that other molecular and clinical risk factors may influence prognosis in this age group. [ABSTRACT FROM AUTHOR]

Published

2012

40. Exome-assistant: a rapid and easy detection of disease-related genes and genetic variations from exome sequencing.

Author

Qi Liu, Enjian Shen, Qingjie Min, Xueying Li, Xin Wang, Xianfeng Li, Zhong Sheng Sun, and Jinyu Wu

Subjects

GENETIC polymorphisms, GENETIC mutation, SINGLE nucleotide polymorphisms, GENOMES, PATHOLOGY

Abstract

Background: Protein-coding regions in human genes harbor 85% of the mutations that are associated with disease-related traits. Compared with whole-genome sequencing of complex samples, exome sequencing serves as an alternative option because of its dramatically reduced cost. In fact, exome sequencing has been successfully applied to identify the cause of several Mendelian disorders, such as Miller and Schinzel-Giedio syndrome. However, there remain great challenges in handling the huge data generated by exome sequencing and in identifying potential disease-related genetic variations. Results: In this study, Exome-assistant (http://122.228.158.106/exomeassistant), a convenient tool for submitting and annotating single nucleotide polymorphisms (SNPs) and insertion/deletion variations (InDels), was developed to rapidly detect candidate disease-related genetic variations from exome sequencing projects. Versatile filter criteria are provided by Exome-assistant to meet different users' requirements. Exome-assistant consists of four modules: the single case module, the two cases module, the multiple cases module, and the reanalysis module. The two cases and multiple cases modules allow users to identify sample-specific and common variations. The multiple cases module also supports family-based studies and Mendelian filtering. The identified candidate disease-related genetic variations can be annotated according to their sample features. Conclusions: In summary, by exploring exome sequencing data, Exome-assistant can provide researchers with detailed biological insights into genetic variation events and permits the identification of potential genetic causes of human diseases and related traits. [ABSTRACT FROM AUTHOR]

Published

2012

41. Molecular alterations of isocitrate dehydrogenase 1 and 2 (IDH1 and IDH2) metabolic genes and additional genetic mutations in newly diagnosed acute myeloid leukemia patients.

Subjects

ISOCITRATE dehydrogenase, GENETIC mutation, ACUTE myeloid leukemia, HIGH performance liquid chromatography, POLYMERASE chain reaction, CHROMOSOME abnormalities, ENZYMES, KARYOTYPES, CYTOGENETICS, PATIENTS

Abstract

The article discusses a study conducted to characterize isocitrate dehydrogenase 1 and 2 (IDH1 and IDH2) mutations in newly diagnosed Acute Myeloid Leukemia (AML) patients. The study also investigates correlations of IDH1 and IDH2 mutations with AML to other parameters like clinical and hematologic characteristics, cytogenetics and additional genetic mutations. It has been stated that the study found that 44 patients out of a total cohort of 230 consecutive AML patients showed IDH mutation. The study also found no patients concurrently carried both IDH1 and IDH2 mutations that suggest that these mutations Aare mutually exclusive.

Published

2012

42. Drosophila Duplication Hotspots Are Associated with Late-Replicating Regions of the Genome.

Author

Cardoso-Moreira, Margarida, Emerson, J. J., Clark, Andrew G., and Manyuan Long

Subjects

GENETIC mutation, PHENOTYPES, DROSOPHILA simulans, GENETIC polymorphism research, DROSOPHILA melanogaster, ANIMAL behavior

Abstract

Duplications play a significant role in both extremes of the phenotypic spectrum of newly arising mutations: they can have severe deleterious effects (e.g. duplications underlie a variety of diseases) but can also be highly advantageous. The phenotypic potential of newly arisen duplications has stimulated wide interest in both the mutational and selective processes shaping these variants in the genome. Here we take advantage of the Drosophila simulans-Drosophila melanogaster genetic system to further our understanding of both processes. Regarding mutational processes, the study of two closely related species allows investigation of the potential existence of shared duplication hotspots, and the similarities and differences between the two genomes can be used to dissect its underlying causes. Regarding selection, the difference in the effective population size between the two species can be leveraged to ask questions about the strength of selection acting on different classes of duplications. In this study, we conducted a survey of duplication polymorphisms in 14 different lines of D. simulans using tiling microarrays and combined it with an analogous survey for the D. melanogaster genome. By integrating the two datasets, we identified duplication hotspots conserved between the two species. However, unlike the duplication hotspots identified in mammalian genomes, Drosophila duplication hotspots are not associated with sequences of high sequence identity capable of mediating non-allelic homologous recombination. Instead, Drosophila duplication hotspots are associated with late-replicating regions of the genome, suggesting a link between DNA replication and duplication rates. We also found evidence supporting a higher effectiveness of selection on duplications in D. simulans than in D. melanogaster. This is also true for duplications segregating at high frequency, where we find evidence in D. simulans that a sizeable fraction of these mutations is being driven to fixation by positive selection. [ABSTRACT FROM AUTHOR]

Published

2011

43. Inborn and acquired metabolic defects in cancer.

Author

Frezza, Christian, Pollard, Patrick J., and Gottlieb, Eyal

Subjects

SUCCINATE dehydrogenase, ONCOGENES, TUMOR suppressor genes, CELL metabolism, GENETIC mutation, KREBS cycle, MITOCHONDRIAL pathology, CANCER cells

Abstract

The observation that altered metabolism is the fundamental cause of cancer was made by Otto Warburg nearly a century ago. However, the subsequent identification of oncogenes and tumor suppressor genes has displaced Warburg's theory pointing towards genetic aberrations as the underlining cause of cancer. Nevertheless, in the last decade, cancer-associated mutations have been identified in genes coding for tricarboxylic acid cycle (TCA cycle, also known as Krebs cycle) and closely related enzymes that have essential roles in cellular metabolism. These observations have revived interest in Warburg's hypothesis and prompted a flurry of functional studies in the hope of gaining mechanistic insight into the links between mitochondrial dysfunction, metabolic alterations, and cancer. In this review, we discuss the potential pro-oncogenic signaling role of some TCA cycle metabolites and their derivatives (oncometabolites). In particular, we focus on their effects on dioxygenases, a family of oxygen and α-ketoglutarate-dependent enzymes that control, among other things, the levels and activity of the hypoxia-inducible transcription factors and the activity of DNA and histone demethylases. [ABSTRACT FROM AUTHOR]

Published

2011

44. Somatic mutations in cancer development.

Author

Luzzatto, Lucio

Subjects

SOMATIC cells, CANCER, GENETIC mutation, CELL populations, GENOMES

Abstract

The transformation of a normal cell into a cancer cell takes place through a sequence of a small number of discrete genetic events, somatic mutations: thus, cancer can be regarded properly as a genetic disease of somatic cells. The analogy between evolution of organisms and evolution of cell populations is compelling: in both cases what drives change is mutation, but it is Darwinian selection that enables clones that have a growth advantage to expand, thus providing a larger target size for the next mutation to hit. The search for molecular lesions in tumors has taken on a new dimension thanks to two powerful technologies: the micro-arrays for quantitative analysis of global gene expresssion (the transcriptome); and 'deep' sequencing for the global analysis of the entire genome (or at least the exome). The former offers the most complete phenotypic characterization of a tumor we could ever hope for - we could call this the ultimate phenotype; the latter can identify all the somatic mutations in an individual tumor - we could call this the somatic genotype. However, there is definitely the risk that while we are 'drowned by data, we remain thirsty for knowledge'. If we want to heed the teachings of Lorenzo Tomatis, I think the message is clear: we ought to take advantage of the new powerful technologies - not by becoming their slaves, but remaining their masters. Identifying somatic mutations in a tumor is important not because it qualifies for 'oncogenomics', but because through a deeper understanding of the nature of that particular tumor it can help us to optimize therapy or to design new therapeutic approaches. [ABSTRACT FROM AUTHOR]

Published

2011

45. Current findings for recurring mutations in acute myeloid leukemia.

Subjects

ACUTE myeloid leukemia, CANCER, GENETICS, GENETIC mutation, BONE marrow diseases, DNA methylation, GENETIC regulation, GENES, BIOSYNTHESIS

Abstract

The article presents a study focusing on current findings for recurring mutations in acute myeloid leukemia (AML). The study shows that the development of novel technologies has led to the identification of several important genetic mutations in AML. The findings of the study suggest a link between recurrent genetic alterations and aberrant epigenetic regulation, which resulting in abnormal DNA methylation statuses in myeloid malignancies. It also presents a chart related to clinical features of gene mutations in AML.

Published

2011

46. Identification of several novel non-p.R132 IDH1 variants in thyroid carcinomas.

Author

Jefferson Pessoa Hemerly

Subjects

BIOCHEMICAL variation, DEHYDROGENASES, THYROID cancer, ANTIBODY diversity, GLIOMAS, LEUKEMIA, GENETIC mutation, GENETICS

Abstract

CONTEXT: Somatic mutations at residue R132 of isocitrate dehydrogenase 1 (IDH1) were recently discovered in gliomas and leukaemia at a high frequency. IDH1 is a metabolic gene, and the R132 mutations create a new enzymatic activity. OBJECTIVES: To determine whether IDH1 had somatically acquired mutations in thyroid carcinomas. DESIGN: Exons 4 and 6 of IDH1 were sequenced in a large panel of thyroid tumours (n=138) and compared with the patients normal DNA (n=26). We also correlated IDH1 mutations with clinical–pathological data and BRAF and RAS mutational status. RESULTS: We identified four novel and two previously described non-synonymous variants in thyroid carcinomas, which were absent in benign tumours and paired normal thyroid. Although IDH1 variants occurred at higher frequency in follicular thyroid carcinomas, follicular variant of papillary thyroid carcinoma (PTC) and undifferentiated thyroid carcinomas than the observed variants in classical PTC (15/72 vs 3/37), it was not significant (P=0.1). Sequence alignment across several species shows that all IDH1 genetic alterations occurred at evolutionarily conserved residues located within the active site, and therefore, are likely to affect protein function. Unlike other tumours, IDH1 and BRAF or RAS mutations are not mutually exclusive. There was no association between IDH1 mutational status and clinical characteristics. CONCLUSION: IDH1-acquired genetic alterations are highly prevalent in thyroid carcinomas (16%). Our findings not only extend our understanding of the molecular mechanism underlying pathogenesis of thyroid tumours, but also emphasize the biological differences between tumour types. Those tumours with IDH1 mutations might benefit from therapies that exploit this alteration. [ABSTRACT FROM AUTHOR]

Published

2010

47. Copy Number Variation and Missense Mutations of the Agouti Signaling Protein (ASIP) Gene in Goat Breeds with Different Coat Colors.

Author

Fontanesi, L., Beretti, F., Riggio, V., González, E. Gómez, Dall'Olio, S., Davoli, R., Russo, V., and Portolano, B.

Subjects

ANIMAL coloration, BIOLOGICAL variation, GENETIC mutation, GENES, GENETIC research

Abstract

In goats, classical genetic studies reported a large number of alleles at the Agouti locus with effects on coat color and pattern distribution. From these early studies, the dominant AWt (white/tan) allele was suggested to cause the white color of the Saanen breed. Here, we sequenced the coding region of the goat ASIP gene in 6 goat breeds (Girgentana, Maltese, Derivata di Siria, Murciano-Granadina, Camosciata delle Alpi, and Saanen), with different coat colors and patterns. Five single nucleotide polymorphisms (SNPs) were identified, 3 of which caused missense mutations in conserved positions of the cysteine-rich carboxy-terminal domain of the protein (p.Ala96Gly, p.Cys126Gly, and p.Val128Gly). Allele and genotype frequencies suggested that these mutations are not associated or not completely associated with coat color in the investigated goat breeds. Moreover, genotyping and sequencing results, deviation from Hardy-Weinberg equilibrium, as well as allele copy number evaluation from semiquantitative fluorescent multiplex PCR, indicated the presence of copy number variation (CNV) in all investigated breeds. To confirm the presence of CNV and evaluate its extension, we applied a bovine-goat cross-species array comparative genome hybridization (aCGH) experiment using a custom tiling array based on bovine chromosome 13. aCGH results obtained for 8 goat DNA samples confirmed the presence of CNV affecting a region of less that 100 kb including the ASIP and AHCY genes. In Girgentana and Saanen breeds, this CNV might cause the AWt allele, as already suggested for a similar structural mutation in sheep affecting the ASIP and AHCY genes, providing evidence for a recurrent interspecies CNV. However, other mechanisms may also be involved in determining coat color in these 2 breeds. Copyright © 2009 S. Karger AG, Basel [ABSTRACT FROM AUTHOR]

Published

2010

48. Homoeolog-specific transcriptional bias in allopolyploid wheat.

Author

Akhunova, Alina R., Matniyazov, Rustam T., Hanquan Liang, and Akhunov, Eduard D.

Subjects

WHEAT, GENOMES, HAPLOIDY, GENETIC mutation, GENETIC polymorphisms

Abstract

Background: Interaction between parental genomes is accompanied by global changes in gene expression which, eventually, contributes to growth vigor and the broader phenotypic diversity of allopolyploid species. In order to gain a better understanding of the effects of allopolyploidization on the regulation of diverged gene networks, we performed a genome-wide analysis of homoeolog-specific gene expression in re-synthesized allohexaploid wheat created by the hybridization of a tetraploid derivative of hexaploid wheat with the diploid ancestor of the wheat D genome Ae. tauschii. Results: Affymetrix wheat genome arrays were used for both the discovery of divergent homoeolog-specific mutations and analysis of homoeolog-specific gene expression in re-synthesized allohexaploid wheat. More than 34,000 detectable parent-specific features (PSF) distributed across the wheat genome were used to assess AB genome (could not differentiate A and B genome contributions) and D genome parental expression in the allopolyploid transcriptome. In re-synthesized polyploid 81% of PSFs detected mid-parent levels of gene expression, and only 19% of PSFs showed the evidence of non-additive expression. Non-additive expression in both AB and D genomes was strongly biased toward up-regulation of parental type of gene expression with only 6% and 11% of genes, respectively, being down-regulated. Of all the non-additive gene expression, 84% can be explained by differences in the parental genotypes used to make the allopolyploid. Homoeolog-specific co-regulation of several functional gene categories was found, particularly genes involved in photosynthesis and protein biosynthesis in wheat. Conclusions: Here, we have demonstrated that the establishment of interactions between the diverged regulatory networks in allopolyploids is accompanied by massive homoeolog-specific up- and down-regulation of gene expression. This study provides insights into interactions between homoeologous genomes and their role in growth vigor, development, and fertility of allopolyploid species. [ABSTRACT FROM AUTHOR]

Published

2010

49. Combined mutations of ASXL1, CBL, FLT3, IDH1,IDH2, JAK2, KRAS, NPM1, NRAS, RUNX1, TET2 andWT1 genes in myelodysplastic syndromes andacute myeloid leukemias.

Author

Rocquain, Julien, Carbuccia, Nadine, Trouplin, Virginie, Raynaud, Stéphane, Murati, Anne, Nezri, Meyer, Tadrist, Zoulika, Olschwang, Sylviane, Vey, Norbert, Birnbaum, Daniel, Gelsi-Boyer, Véronique, and Mozziconacci, Marie-Joelle

Subjects

MYELODYSPLASTIC syndromes, MYELOID leukemia, GENETIC mutation, GENES, KARYOTYPES

Abstract

Background: Gene mutation is an important mechanism of myeloid leukemogenesis. However, the number and combination of gene mutated in myeloid malignancies is still a matter of investigation. Methods: We searched for mutations in the ASXL1, CBL, FLT3, IDH1, IDH2, JAK2, KRAS, NPM1, NRAS, RUNX1, TET2 and WT1 genes in 65 myelodysplastic syndromes (MDSs) and 64 acute myeloid leukemias (AMLs) without balanced translocation or complex karyotype. Results: Mutations in ASXL1 and CBL were frequent in refractory anemia with excess of blasts. Mutations in TET2 occurred with similar frequency in MDSs and AMLs and associated equally with either ASXL1 or NPM1 mutations. Mutations of RUNX1 were mutually exclusive with TET2 and combined with ASXL1 but not with NPM1. Mutations in FLT3 (mutation and internal tandem duplication), IDH1, IDH2, NPM1 and WT1 occurred primarily in AMLs. Conclusion: Only 14% MDSs but half AMLs had at least two mutations in the genes studied. Based on the observed combinations and exclusions we classified the 12 genes into four classes and propose a highly speculative model that at least a mutation in one of each class is necessary for developing AML with simple or normal karyotype. [ABSTRACT FROM AUTHOR]

Published

2010

50. Copy number variation on the human Y chromosome.

Author

Jobling, M. A.

Subjects

Y chromosome, HAPLOIDY, POPULATION genetics, GENEALOGY, PHYLOGENY, GENETIC mutation, X chromosome, SPERMATOGENESIS

Abstract

The Y chromosome is unusual in being constitutively haploid and escaping recombination for most of its length. This has led to a correspondingly unusual genomic landscape, rich in segmental duplications, which provide a potent environment for the generation of copy number variation (CNV). Interest in the chromosome comes from diverse fields, including infertility research, population genetics, forensics, and genealogy. Together with inclusion in more systematic surveys, this has led to the ascertainment of a variety of CNVs. Assessment in the context of the well-resolved Y phylogeny allows their mutational history to be deciphered and an estimation of mutation rate. The functional consequences of variants are moderated by the specialization of the chromosome and the presence of functionally equivalent X-chromosomal homologues for some genes. However, deletions of the AZFa, b, and c regions cause impaired spermatogenesis, while partial deletions and duplications within these regions, and deletions and duplications elsewhere, may be selectively neutral or have subtle phenotypes. Copyright © 2009 S. Karger AG, Basel [ABSTRACT FROM AUTHOR]

Published

2009