Your search keyword '"Minoche, A"' showing total 28 results

1. ClinSV: clinical grade structural and copy number variant detection from whole genome sequencing data.

Author

Minoche, Andre E., Lundie, Ben, Peters, Greg B., Ohnesorg, Thomas, Pinese, Mark, Thomas, David M., Zankl, Andreas, Roscioli, Tony, Schonrock, Nicole, Kummerfeld, Sarah, Burnett, Leslie, Dinger, Marcel E., and Cowley, Mark J.

Subjects

*EXOMES, *DNA copy number variations, *VISUALIZATION, *RARE diseases

Abstract

Whole genome sequencing (WGS) has the potential to outperform clinical microarrays for the detection of structural variants (SV) including copy number variants (CNVs), but has been challenged by high false positive rates. Here we present ClinSV, a WGS based SV integration, annotation, prioritization, and visualization framework, which identified 99.8% of simulated pathogenic ClinVar CNVs > 10 kb and 11/11 pathogenic variants from matched microarrays. The false positive rate was low (1.5–4.5%) and reproducibility high (95–99%). In clinical practice, ClinSV identified reportable variants in 22 of 485 patients (4.7%) of which 35–63% were not detectable by current clinical microarray designs. ClinSV is available at https://github.com/KCCG/ClinSV. [ABSTRACT FROM AUTHOR]

Published

2021

2. Genomes of the wild beets Beta patula and Beta vulgaris ssp. maritima.

Author

Rodríguez del Río, Álvaro, Minoche, André E., Zwickl, Nikolaus F., Friedrich, Anja, Liedtke, Susan, Schmidt, Thomas, Himmelbauer, Heinz, and Dohm, Juliane C.

Subjects

*BEETS, *SUGAR beets, *GENOMES, *GERMPLASM

Abstract

Summary: We present draft genome assemblies of Beta patula, a critically endangered wild beet endemic to the Madeira archipelago, and of the closely related Beta vulgaris ssp. maritima (sea beet). Evidence‐based reference gene sets for B. patula and sea beet were generated, consisting of 25 127 and 27 662 genes, respectively. The genomes and gene sets of the two wild beets were compared with their cultivated sister taxon B. vulgaris ssp. vulgaris (sugar beet). Large syntenic regions were identified, and a display tool for automatic genome‐wide synteny image generation was developed. Phylogenetic analysis based on 9861 genes showing 1:1:1 orthology supported the close relationship of B. patula to sea beet and sugar beet. A comparative analysis of the Rz2 locus, responsible for rhizomania resistance, suggested that the sequenced B. patula accession was rhizomania susceptible. Reference karyotypes for the two wild beets were established, and genomic rearrangements were detected. We consider our data as highly valuable and comprehensive resources for wild beet studies, B. patula conservation management, and sugar beet breeding research. Significance Statement: Wild beets of the genus Beta are important genetic resources for the improvement of cultivated beet varieties. This work presents genome assemblies and gene sets of Beta vulgaris ssp. maritima (sea beet) and of the critically endangered Beta patula, identifies orthologs and syntenic regions between sugar beet and the two wild beets, and provides valuable genome‐wide molecular resources for wild beet studies and sugar beet breeding. [ABSTRACT FROM AUTHOR]

Published

2019

3. Density management diagram for teak plantations in Tabasco, Mexico.

Author

Minoche, Djhon, Risio-Allione, Lucia, De Aza, Celia Herrero, and Martínez-Zurimendi, Pablo

Subjects

*TEAK, *PLANTATIONS, *PREDICTION models, *STAKEHOLDERS

Abstract

Density management diagrams are valuable tools for managing specific forest species. The aim of this study was to obtain a density management diagram for teak (Tectona grandis L.) plantations in the State of Tabasco in Mexico. To achieve this objective, a set of 10 plantations were studied, in which 42 plots were established. Two equations were fitted simultaneously, including one related to the quadratic mean diameter, stand density and dominant height and the other which related the total stand volume to the quadratic mean diameter, stand density and dominant height. The results showed that the diagram had an acceptable predictability, thus indicating its usefulness and accuracy in planning silvicultural interventions. This diagram is a very powerful tool that can enable stakeholders to manage teak plantations in the State of Tabasco. [ABSTRACT FROM AUTHOR]

Published

2017

4. The genome of the recently domesticated crop plant sugar beet (Beta vulgaris).

Author

Dohm, Juliane C., Minoche, André E., Holtgräwe, Daniela, Capella-Gutiérrez, Salvador, Zakrzewski, Falk, Tafer, Hakim, Rupp, Oliver, Sörensen, Thomas Rosleff, Stracke, Ralf, Reinhardt, Richard, Goesmann, Alexander, Kraft, Thomas, Schulz, Britta, Stadler, Peter F., Schmidt, Thomas, Gabaldón, Toni, Lehrach, Hans, Weisshaar, Bernd, and Himmelbauer, Heinz

Subjects

*CROPS, *PLANT genetics, *SUGAR beets, *CLIMATE change, *ETHANOL as fuel, *ANIMAL feeds, *BASE pairs, *CHROMOSOMES, *DIPLOIDY

Abstract

Sugar beet (Beta vulgaris ssp. vulgaris) is an important crop of temperate climates which provides nearly 30% of the world's annual sugar production and is a source for bioethanol and animal feed. The species belongs to the order of Caryophylalles, is diploid with 2n = 18 chromosomes, has an estimated genome size of 714-758 megabases and shares an ancient genome triplication with other eudicot plants. Leafy beets have been cultivated since Roman times, but sugar beet is one of the most recently domesticated crops. It arose in the late eighteenth century when lines accumulating sugar in the storage root were selected from crosses made with chard and fodder beet. Here we present a reference genome sequence for sugar beet as the first non-rosid, non-asterid eudicot genome, advancing comparative genomics and phylogenetic reconstructions. The genome sequence comprises 567 megabases, of which 85% could be assigned to chromosomes. The assembly covers a large proportion of the repetitive sequence content that was estimated to be 63%. We predicted 27,421 protein-coding genes supported by transcript data and annotated them on the basis of sequence homology. Phylogenetic analyses provided evidence for the separation of Caryophyllales before the split of asterids and rosids, and revealed lineage-specific gene family expansions and losses. We sequenced spinach (Spinacia oleracea), another Caryophyllales species, and validated features that separate this clade from rosids and asterids. Intraspecific genomic variation was analysed based on the genome sequences of sea beet (Beta vulgaris ssp. maritima; progenitor of all beet crops) and four additional sugar beet accessions. We identified seven million variant positions in the reference genome, and also large regions of low variability, indicating artificial selection. The sugar beet genome sequence enables the identification of genes affecting agronomically relevant traits, supports molecular breeding and maximizes the plant's potential in energy biotechnology. [ABSTRACT FROM AUTHOR]

Published

2014

5. Assembly and characterization of the genome of chard (Beta vulgaris ssp. vulgaris var. cicla).

Author

Lehner, Reinhard, Blazek, Lisa, Minoche, André E., Dohm, Juliane C., and Himmelbauer, Heinz

Subjects

*BEETS, *SUGAR beets, *GENOMES, *VEGETABLE farming, *PHENOTYPES, *CHROMOSOMES

Abstract

• We present the first genome assembly of chard, a member of the species Beta vulgaris affiliated with a cultigroup other than sugar beet. • Despite pronounced phenotypical differences between chard and sugar beet, we find that the two genomes are very closely related. • Sugar beet and chard encode for a similar number of genes, and ca. 50 % of them were recognised as 1:1 orthologs. • Assessing the variation distribution along chard chromosomes, we found extensive haplotype sharing between the two cultivars. • Our work paves the way towards understanding the phenotypic breadth of beet cultigroups and their domestication history. Chard (Beta vulgaris ssp. vulgaris var. cicla) is a member of one of four different cultigroups of beets. While the genome of sugar beet, the most prominent beet crop, has been studied extensively, molecular data on other beet cultivars is scant. Here, we present a genome assembly of chard, a vegetable crop grown for its fleshy leaves. We report a de novo genome assembly of 604 Mbp, slightly larger than sugar beet assemblies presented so far. About 57 % of the assembly was annotated as repetitive sequence, of which LTR retrotransposons were the most abundant. Based on the presence of conserved genes, the chard assembly was estimated to be at least 96 % complete regarding its gene space. We predicted 34,521 genes of which 27,582 genes were supported by evidence from transcriptomic sequencing reads, and 5503 of the evidence-supported genes had multiple isoforms. We compared the chard gene set with gene sets from sugar beet and two wild beets (i.e. Beta vulgaris ssp. maritima and Beta patula) to find orthology relationships and identified genome-wide syntenic regions between chard and sugar beet. Lastly, we determined genomic variants that distinguish sugar beet and chard. Assessing the variation distribution along the chard chromosomes, we found extensive haplotype sharing between the two cultivars. In summary, our work provides a foundation for the molecular analysis of Beta vulgaris cultigroups as a basis for chard genomics and to unravel the domestication history of beet crops. [ABSTRACT FROM AUTHOR]

Published

2021

6. Quantitative ctDNA Detection in Hepatoblastoma: Implications for Precision Medicine.

Author

Kahana-Edwin, Smadar, Torpy, James, Cain, Lucy E., Mullins, Anna, McCowage, Geoffrey, Woodfield, Sarah E., Vasudevan, Sanjeev A., Shea, Dan P. T., Minoche, Andre E., Espinoza, Andres F., Kummerfeld, Sarah, Goldstein, Leonard D., and Karpelowsky, Jonathan

Subjects

*ALPHA fetoproteins, *DNA, *SCIENTIFIC observation, *HEPATOBLASTOMA, *INDIVIDUALIZED medicine, *QUANTITATIVE research, *CANCER patients, *COMPARATIVE studies, *RESEARCH funding, *TUMOR markers, *COMBINED modality therapy, *SENSITIVITY & specificity (Statistics), *DECISION making in clinical medicine, *LONGITUDINAL method, BODY fluid examination

Abstract

Simple Summary: Driver mutations in CTNNB1 are a hallmark of hepatoblastoma and offer a common biomarker for a liquid biopsy approach that is based on the presence of CTNNB1 circulating tumor DNA (ctDNA). We provide promising evidence for the utility of quantitative CTNNB1 ctDNA detection in hepatoblastoma for dynamic tumor burden and treatment response monitoring, compared with the current clinical indicators and biomarkers for this disease. Hepatoblastoma is characterized by driver mutations in CTNNB1, making it an attractive biomarker for a liquid biopsy approach utilizing circulating tumor DNA (ctDNA). This prospective observational study sought to ascertain the feasibility of ctDNA detection in patients with hepatoblastoma and explore its associations with established clinical indicators and biomarkers, including serum Alpha-fetoprotein (AFP). We obtained 38 plasma samples and 17 tumor samples from 20 patients with hepatoblastoma. These samples were collected at various stages: 10 at initial diagnosis, 17 during neoadjuvant chemotherapy, 6 post-operatively, and 5 at disease recurrence. Utilizing a bespoke sequencing assay we developed called QUENCH, we identified single nucleotide variants and deletions in CTNNB1 ctDNA. Our study demonstrated the capability to quantitate ctDNA down to a variant allele frequency of 0.3%, achieving a sensitivity of 90% for patients at initial diagnosis, and a specificity of 100% at the patient level. Notably, ctDNA positivity correlated with tumor burden, and ctDNA levels exhibited associations with macroscopic residual disease and treatment response. Our findings provide evidence for the utility of quantitative ctDNA detection in hepatoblastoma management. Given the distinct detection targets, ctDNA and AFP-based stratification and monitoring approaches could synergize to enhance clinical decision-making. Further research is needed to elucidate the interplay between ctDNA and AFP and determine the optimal clinical applications for both methods in risk stratification and residual disease detection. [ABSTRACT FROM AUTHOR]

Published

2024

7. Cytosine Methylation of an Ancient Satellite Family in the Wild Beet Beta procumbens.

Author

Schmidt, Martin, Hense, Sarah, Minoche, andré E., Dohm, Juliane C., Himmelbauer, Heinz, Schmidt, Thomas, and Zakrzewski, Falk

Subjects

*CYTOSINE, *METHYLATION, *BEETS, *SATELLITE DNA, *PLANT epigenetics

Abstract

DNA methylation is an essential epigenetic feature for the regulation and maintenance of heterochromatin. Satellite DNA is a repetitive sequence component that often occurs in large arrays in heterochromatin of subtelomeric, intercalary and centromeric regions. Knowledge about the methylation status of satellite DNA is important for understanding the role of repetitive DNA in heterochromatization. In this study, we investigated the cytosine methylation of the ancient satellite family pEV in the wild beet Beta procumbens. The pEV satellite is widespread in species-specific pEV subfamilies in the genus Beta and most likely originated before the radiation of the Betoideae and Chenopodioideae. In B. procumbens, the pEV subfamily occurs abundantly and spans intercalary and centromeric regions. To uncover its cytosine methylation, we performed chromosome-wide immunostaining and bisulfite sequencing of pEV satellite repeats. We found that CG and CHG sites are highly methylated while CHH sites show only low levels of methylation. As a consequence of the low frequency of CG and CHG sites and the preferential occurrence of most cytosines in the CHH motif in pEV monomers, this satellite family displays only low levels of total cytosine methylation. © 2014 S. Karger AG, Basel [ABSTRACT FROM AUTHOR]

Published

2014

8. Whole Genome Sequencing, Focused Assays and Functional Studies Increasing Understanding in Cryptic Inherited Retinal Dystrophies.

Author

Nash, Benjamin M., Ma, Alan, Ho, Gladys, Farnsworth, Elizabeth, Minoche, Andre E., Cowley, Mark J., Barnett, Christopher, Smith, Janine M., Loi, To Ha, Wong, Karen, St Heaps, Luke, Wright, Dale, Dinger, Marcel E., Bennetts, Bruce, Grigg, John R., and Jamieson, Robyn V.

Subjects

*WHOLE genome sequencing, *RETINAL degeneration, *NON-coding RNA, *MOLECULAR diagnosis, *FUNCTIONAL genomics, *GENE targeting

Abstract

The inherited retinal dystrophies (IRDs) are a clinically and genetically complex group of disorders primarily affecting the rod and cone photoreceptors or other retinal neuronal layers, with emerging therapies heralding the need for accurate molecular diagnosis. Targeted capture and panel-based strategies examining the partial or full exome deliver molecular diagnoses in many IRD families tested. However, approximately one in three families remain unsolved and unable to obtain personalised recurrence risk or access to new clinical trials or therapy. In this study, we investigated whole genome sequencing (WGS), focused assays and functional studies to assist with unsolved IRD cases and facilitate integration of these approaches to a broad molecular diagnostic clinical service. The WGS approach identified variants not covered or underinvestigated by targeted capture panel-based clinical testing strategies in six families. This included structural variants, with notable benefit of the WGS approach in repetitive regions demonstrated by a family with a hybrid gene and hemizygous missense variant involving the opsin genes, OPN1LW and OPN1MW. There was also benefit in investigation of the repetitive GC-rich ORF15 region of RPGR. Further molecular investigations were facilitated by focused assays in these regions. Deep intronic variants were identified in IQCB1 and ABCA4, with functional RNA based studies of the IQCB1 variant revealing activation of a cryptic splice acceptor site. While targeted capture panel-based methods are successful in achieving an efficient molecular diagnosis in a proportion of cases, this study highlights the additional benefit and clinical value that may be derived from WGS, focused assays and functional genomics in the highly heterogeneous IRDs. [ABSTRACT FROM AUTHOR]

Published

2022

9. RLIM Is a Candidate Dosage-Sensitive Gene for Individuals with Varying Duplications of Xq13, Intellectual Disability, and Distinct Facial Features.

Author

Palmer, Elizabeth E., Carroll, Renee, Shaw, Marie, Kumar, Raman, Minoche, Andre E., Leffler, Melanie, Murray, Lucinda, Macintosh, Rebecca, Wright, Dale, Troedson, Chris, McKenzie, Fiona, Townshend, Sharron, Ward, Michelle, Nawaz, Urwah, Ravine, Anja, Runke, Cassandra K., Thorland, Erik C., Hummel, Marybeth, Foulds, Nicola, and Pichon, Olivier

Subjects

*INTELLECTUAL disabilities, *NON-coding RNA, *MESSENGER RNA, *GENES, *X chromosome, *SEIZURES (Medicine), *FACE

Abstract

Interpretation of the significance of maternally inherited X chromosome variants in males with neurocognitive phenotypes continues to present a challenge to clinical geneticists and diagnostic laboratories. Here we report 14 males from 9 families with duplications at the Xq13.2-q13.3 locus with a common facial phenotype, intellectual disability (ID), distinctive behavioral features, and a seizure disorder in two cases. All tested carrier mothers had normal intelligence. The duplication arose de novo in three mothers where grandparental testing was possible. In one family the duplication segregated with ID across three generations. RLIM is the only gene common to our duplications. However, flanking genes duplicated in some but not all the affected individuals included the brain-expressed genes NEXMIF , SLC16A2 , and the long non-coding RNA gene FTX. The contribution of the RLIM -flanking genes to the phenotypes of individuals with different size duplications has not been fully resolved. Missense variants in RLIM have recently been identified to cause X-linked ID in males, with heterozygous females typically having normal intelligence and highly skewed X chromosome inactivation. We detected consistent and significant increase of RLIM mRNA and protein levels in cells derived from seven affected males from five families with the duplication. Subsequent analysis of MDM2, one of the targets of the RLIM E3 ligase activity, showed consistent downregulation in cells from the affected males. All the carrier mothers displayed normal RLIM mRNA levels and had highly skewed X chromosome inactivation. We propose that duplications at Xq13.2-13.3 including RLIM cause a recognizable but mild neurocognitive phenotype in hemizygous males. [ABSTRACT FROM AUTHOR]

Published

2020

10. Increased Diagnostic Yield of Spastic Paraplegia with or Without Cerebellar Ataxia Through Whole-Genome Sequencing.

Author

Kim, Aryun, Kumar, Kishore R., Davis, Ryan L., Mallawaarachchi, Amali C., Gayevskiy, Velimir, Minoche, Andre E., Walls, Zachary, Kim, Han-Joon, Jang, Mihee, Cowley, Mark J., Choi, Ji-Hyun, Shin, Chaewon, Sue, Carolyn M., and Jeon, Beomseok

Subjects

*CEREBELLAR ataxia, *FAMILIAL spastic paraplegia, *FRIEDREICH'S ataxia, *DNA copy number variations, *PARAPLEGIA, *ATAXIA

Abstract

Inherited disorders of spasticity or ataxia exist on a spectrum with overlapping causative genes and phenotypes. We investigated the use of whole-genome sequencing (WGS) to detect a genetic cause when considering this spectrum of disorders as a single group. We recruited 18 Korean individuals with spastic paraplegia with or without cerebellar ataxia in whom common causes of hereditary cerebellar ataxia and hereditary spastic paraplegia had been excluded. We performed WGS with analysis for single nucleotide variants, small insertions and deletions, copy number variants (CNVs), structural variants (SVs) and intronic variants. Disease-relevant variants were identified in ABCD1 (n = 3), CAPN1 (n = 2), NIPA1 (n = 1) and PLA2G6 (n = 1) for 7/18 patients (38.9%). A 'reverse phenotyping' approach was used to clarify the diagnosis in individuals with PLA2G6 and ABCD1 variants. One of the ABCD1 disease-relevant variants was detected on analysis for intronic variants. No CNV or SV causes were found. The two males with ABCD1 variants were initiated on monitoring for adrenal dysfunction. This is one of only a few studies to analyse spastic-ataxias as a continuous spectrum using a single approach. The outcome was improved diagnosis of unresolved cases for which common genetic causes had been excluded. This includes the detection of ABCD1 variants which had management implications. Therefore, WGS may be particularly relevant to diagnosing spastic ataxias given the large number of genes associated with this condition and the relatively high diagnostic yield. [ABSTRACT FROM AUTHOR]

Published

2019

11. De Novo Variants Disrupting the HX Repeat Motif of ATN1 Cause a Recognizable Non-Progressive Neurocognitive Syndrome.

Author

Palmer, Elizabeth E., Hong, Seungbeom, Al Zahrani, Fatema, Hashem, Mais O., Aleisa, Fajr A., Ahmed, Heba M. Jalal, Kandula, Tejaswi, Macintosh, Rebecca, Minoche, Andre E., Puttick, Clare, Gayevskiy, Velimir, Drew, Alexander P., Cowley, Mark J., Dinger, Marcel, Rosenfeld, Jill A., Xiao, Rui, Cho, Megan T., Yakubu, Suliat F., Henderson, Lindsay B., and Guillen Sacoto, Maria J.

Subjects

*POLYGLUTAMINE, *NEURODEGENERATION, *AMINO acids, *EPILEPSY, *HUMAN genes

Abstract

Polyglutamine expansions in the transcriptional co-repressor Atrophin-1, encoded by ATN1, cause the neurodegenerative condition dentatorubral-pallidoluysian atrophy (DRPLA) via a proposed novel toxic gain of function. We present detailed phenotypic information on eight unrelated individuals who have de novo missense and insertion variants within a conserved 16-amino-acid "HX repeat" motif of ATN1. Each of the affected individuals has severe cognitive impairment and hypotonia, a recognizable facial gestalt, and variable congenital anomalies. However, they lack the progressive symptoms typical of DRPLA neurodegeneration. To distinguish this subset of affected individuals from the DRPLA diagnosis, we suggest using the term CHEDDA (congenital hypotonia, epilepsy, developmental delay, digit abnormalities) to classify the condition. CHEDDA-related variants alter the particular structural features of the HX repeat motif, suggesting that CHEDDA results from perturbation of the structural and functional integrity of the HX repeat. We found several non-homologous human genes containing similar motifs of eight to 10 HX repeat sequences, including RERE , where disruptive variants in this motif have also been linked to a separate condition that causes neurocognitive and congenital anomalies. These findings suggest that perturbation of the HX motif might explain other Mendelian human conditions. [ABSTRACT FROM AUTHOR]

Published

2019

12. Whole Genome Sequencing Improves Outcomes of Genetic Testing in Patients With Hypertrophic Cardiomyopathy.

Author

Bagnall, Richard D, Ingles, Jodie, Dinger, Marcel E, Cowley, Mark J, Ross, Samantha Barratt, Minoche, André E, Lal, Sean, Turner, Christian, Colley, Alison, Rajagopalan, Sulekha, Berman, Yemima, Ronan, Anne, Fatkin, Diane, and Semsarian, Christopher

Abstract

Background: Whole genome sequencing (WGS) is a comprehensive genetic testing approach that reports most types of nucleotide variants.Objectives: This study sought to assess WGS for hypertrophic cardiomyopathy (HCM) in which prior genetic testing did not establish a molecular diagnosis, and as a first-line genetic test.Methods: WGS was performed on 58 unrelated patients with HCM, 14 affected family members, and 2 unaffected parents of a severely affected proband. The authors searched for nucleotide variants in coding regions of 184 candidate cardiac hypertrophy genes. They also searched for nucleotide variants in deep intronic regions that alter RNA splicing, large genomic rearrangements, and mitochondrial genome variants. RNA analysis was performed to validate splice-altering variants.Results: The authors found a pathogenic or likely pathogenic variant in 9 of 46 families (20%) for which prior genetic testing was inconclusive. Three families had variants in genes not included in prior genetic testing. One family had a pathogenic variant that was filtered out with prior exome sequencing. Five families had pathogenic variants in noncoding regions, including 4 with deep intronic variants that activate novel splicing, and 1 mitochondrial genome variant. As a first-line genetic test, WGS identified a pathogenic variant in 5 of 12 families (42%) that had never received prior genetic testing.Conclusions: WGS identified additional genetic causes of HCM over targeted gene sequencing approaches. Extending genetic screening to deep intronic regions identified pathogenic variants in 9% of gene-elusive HCM. These findings translate to more accurate diagnosis and management in HCM families. [ABSTRACT FROM AUTHOR]

Published

2018

13. Diversification, evolution and methylation of short interspersed nuclear element families in sugar beet and related Amaranthaceae species.

Author

Schwichtenberg, Katrin, Wenke, Torsten, Zakrzewski, Falk, Seibt, Kathrin M., Minoche, André, Dohm, Juliane C., Weisshaar, Bernd, Himmelbauer, Heinz, and Schmidt, Thomas

Subjects

*CROP yields, *SUGAR beets, *AMARANTHACEAE, *BIODIVERSITY, *METHYLATION, *BIOLOGICAL evolution, *RETROTRANSPOSONS

Abstract

Short interspersed nuclear elements ( SINEs) are non-autonomous non-long terminal repeat retrotransposons which are widely distributed in eukaryotic organisms. While SINEs have been intensively studied in animals, only limited information is available about plant SINEs. We analysed 22 SINE families from seven genomes of the Amaranthaceae family and identified 34 806 SINEs, including 19 549 full-length copies. With the focus on sugar beet ( Beta vulgaris), we performed a comparative analysis of the diversity, genomic and chromosomal organization and the methylation of SINEs to provide a detailed insight into the evolution and age of Amaranthaceae SINEs. The lengths of consensus sequences of SINEs range from 113 nucleotides (nt) up to 224 nt. The SINEs show dispersed distribution on all chromosomes but were found with higher incidence in subterminal euchromatic chromosome regions. The methylation of SINEs is increased compared with their flanking regions, and the strongest effect is visible for cytosines in the CHH context, indicating an involvement of asymmetric methylation in the silencing of SINEs. [ABSTRACT FROM AUTHOR]

Published

2016

14. Molecular signatures of plastic phenotypes in two eusocial insect species with simple societies.

Author

Patalano, Solenn, Vlasova, Anna, Wyatt, Chris, Ewels, Philip, Camara, Francisco, Ferreira, Pedro G., Asher, Claire L., Jurkowski, Tomasz P., Segonds-Pichon, Anne, Bachman, Martin, González-Navarrete, Irene, Minoche, André E., Krueger, Felix, Lowy, Ernesto, Marcet-Houben, Marina, Rodriguez-Ales, Jose Luis, Nascimento, Fabio S., Balasubramanian, Shankar, Gabaldon, Toni, and Tarver, James E.

Subjects

*PHENOTYPIC plasticity, *SOCIAL evolution, *NUCLEOTIDE sequencing, *DNA methylation, *EUSOCIALITY, *INSECTS

Abstract

Phenotypic plasticity is important in adaptation and shapes the evolution of organisms. However, we understand little about what aspects of the genome are important in facilitating plasticity. Eusocial insect societies produce plastic phenotypes from the same genome, as reproductives (queens) and nonreproductives (workers). The greatest plasticity is found in the simple eusocial insect societies in which individuals retain the ability to switch between reproductive and nonreproductive phenotypes as adults. We lack comprehensive data on the molecular basis of plastic phenotypes. Here, we sequenced genomes, microRNAs (miRNAs), and multiple transcriptomes and methylomes from individual brains in a wasp (Polistes canadensis) and an ant (Dinoponera quadriceps) that live in simple eusocial societies. In both species, we found few differences between phenotypes at the transcriptional level, with little functional specialization, and no evidence that phenotype-specific gene expression is driven by DNA methylation or miRNAs. Instead, phenotypic differentiation was defined more subtly by nonrandom transcriptional network organization, with roles in these networks for both conserved and taxon-restricted genes. The general lack of highly methylated regions or methylome patterning in both species may be an important mechanism for achieving plasticity among phenotypes during adulthood. These findings define previously unidentified hypotheses on the genomic processes that facilitate plasticity and suggest that the molecular hallmarks of social behavior are likely to differ with the level of social complexity. [ABSTRACT FROM AUTHOR]

Published

2015

15. Profiling of extensively diversified plant LINEs reveals distinct plant-specific subclades.

Author

Heitkam, Tony, Holtgräwe, Daniela, Dohm, Juliane C., Minoche, André E., Himmelbauer, Heinz, Weisshaar, Bernd, and Schmidt, Thomas

Subjects

*PLANT genomes, *EUKARYOTIC genomes, *REVERSE transcriptase, *RETROTRANSPOSONS, *BEETS, *HETEROGENEITY, *MARKOV processes

Abstract

A large fraction of eukaryotic genomes is made up of long interspersed nuclear elements ( LINEs). Due to their capability to create novel copies via error-prone reverse transcription, they generate multiple families and reach high copy numbers. Although mammalian LINEs have been well described, plant LINEs have been only poorly investigated. Here, we present a systematic cross-species survey of LINEs in higher plant genomes shedding light on plant LINE evolution as well as diversity, and facilitating their annotation in genome projects. Applying a Hidden Markov Model ( HMM)-based analysis, 59 390 intact LINE reverse transcriptases ( RTs) were extracted from 23 plant genomes. These fall in only two out of 28 LINE clades (L1 and RTE) known in eukaryotes. While plant RTE LINEs are highly homogenous and mostly constitute only a single family per genome, plant L1 LINEs are extremely diverse and form numerous families. Despite their heterogeneity, all members across the 23 species fall into only seven L1 subclades, some of them defined here. Exemplarily focusing on the L1 LINEs of a basal reference plant genome ( Beta vulgaris), we show that the subclade classification level does not only reflect RT sequence similarity, but also mirrors structural aspects of complete LINE retrotransposons, like element size, position and type of encoded enzymatic domains. Our comprehensive catalogue of plant LINE RTs serves the classification of highly diverse plant LINEs, while the provided subclade-specific HMMs facilitate their annotation. [ABSTRACT FROM AUTHOR]

Published

2014

16. Identification of ALK Gene Alterations in Urothelial Carcinoma.

Author

Bellmunt, Joaquim, Selvarajah, Shamini, Rodig, Scott, Salido, Marta, de Muga, Silvia, Costa, Irmgard, Bellosillo, Beatriz, Werner, Lillian, Mullane, Stephanie, Fay, André P., O'Brien, Robert, Barretina, Jordi, Minoche, André E., Signoretti, Sabina, Montagut, Clara, Himmelbauer, Heinz, Berman, David M., Kantoff, Philip, Choueiri, Toni K., and Rosenberg, Jonathan E.

Subjects

*TRANSITIONAL cell carcinoma, *ANAPLASTIC lymphoma kinase, *ENZYME inhibitors, *PREDICTION theory, *HEALTH outcome assessment, *IMMUNOHISTOCHEMISTRY, *IN situ hybridization, *THERAPEUTICS

Abstract

Background: Anaplastic lymphoma kinase (ALK) genomic alterations have emerged as a potent predictor of benefit from treatment with ALK inhibitors in several cancers. Currently, there is no information about ALK gene alterations in urothelial carcinoma (UC) and its correlation with clinical or pathologic features and outcome. Methods: Samples from patients with advanced UC and correlative clinical data were collected. Genomic imbalances were investigated by array comparative genomic hybridization (aCGH). ALK gene status was evaluated by fluorescence in situ hybridization (FISH). ALK expression was assessed by immunohistochemistry (IHC) and high-throughput mutation analysis with Oncomap 3 platform. Next generation sequencing was performed using Illumina Genome Analyzer IIx, and Illumina HiSeq 2000 in the FISH positive case. Results: 70 of 96 patients had tissue available for all the tests performed. Arm level copy number gains at chromosome 2 were identified in 17 (24%) patients. Minor copy number alterations (CNAs) in the proximity of ALK locus were found in 3 patients by aCGH. By FISH analysis, one of these samples had a deletion of the 5′ALK. Whole genome next generation sequencing was inconclusive to confirm the deletion at the level of the ALK gene at the coverage level used. We did not observe an association between ALK CNA and overall survival, ECOG PS, or development of visceral disease. Conclusions: ALK genomic alterations are rare and probably without prognostic implications in UC. The potential for testing ALK inhibitors in UC merits further investigation but might be restricted to the identification of an enriched population. [ABSTRACT FROM AUTHOR]

Published

2014

17. The CHH motif in sugar beet satellite DNA: a modulator for cytosine methylation.

Author

Zakrzewski, Falk, Schubert, Veit, Viehoever, Prisca, Minoche, André E., Dohm, Juliane C., Himmelbauer, Heinz, Weisshaar, Bernd, and Schmidt, Thomas

Subjects

*SATELLITE DNA, *SUGAR beets, *CYTOSINE, *METHYLATION, *PLANT chromosomes, *PLANT genomes

Abstract

Methylation of DNA is important for the epigenetic silencing of repetitive DNA in plant genomes. Knowledge about the cytosine methylation status of satellite DNAs, a major class of repetitive DNA, is scarce. One reason for this is that arrays of tandemly arranged sequences are usually collapsed in next-generation sequencing assemblies. We applied strategies to overcome this limitation and quantified the level of cytosine methylation and its pattern in three satellite families of sugar beet ( Beta vulgaris) which differ in their abundance, chromosomal localization and monomer size. We visualized methylation levels along pachytene chromosomes with respect to small satellite loci at maximum resolution using chromosome-wide fluorescent in situ hybridization complemented with immunostaining and super-resolution microscopy. Only reduced methylation of many satellite arrays was obtained. To investigate methylation at the nucleotide level we performed bisulfite sequencing of 1569 satellite sequences. We found that the level of methylation of cytosine strongly depends on the sequence context: cytosines in the CHH motif show lower methylation (44-52%), while CG and CHG motifs are more strongly methylated. This affects the overall methylation of satellite sequences because CHH occurs frequently while CG and CHG are rare or even absent in the satellite arrays investigated. Evidently, CHH is the major target for modulation of the cytosine methylation level of adjacent monomers within individual arrays and contributes to their epigenetic function. This strongly indicates that asymmetric cytosine methylation plays a role in the epigenetic modification of satellite repeats in plant genomes. [ABSTRACT FROM AUTHOR]

Published

2014

18. Differential Expression Patterns of Non-Symbiotic Hemoglobins in Sugar Beet (Beta vulgaris ssp. vulgaris).

Author

Leiva-Eriksson, Nélida, Pin, Pierre A., Kraft, Thomas, Dohm, Juliane C., Minoche, André E., Himmelbauer, Heinz, and Bülow, Leif

Subjects

*GENE expression in plants, *HEMOGLOBINS, *BEET sugar, *CARYOPHYLLIDAE, *TEMPERATURE effect, *NUCLEOTIDE sequence

Abstract

Biennial sugar beet (Beta vulgaris spp. vulgaris) is a Caryophyllidae that has adapted its growth cycle to the seasonal temperature and daylength variation of temperate regions. This is the first time a holistic study of the expression pattern of non-symbiotic hemoglobins (nsHbs) is being carried out in a member of this group and under two essential environmental conditions for flowering, namely vernalization and length of photoperiod. BvHb genes were identified by sequence homology searches against the latest draft of the sugar beet genome. Three nsHb genes (BvHb1.1, BvHb1.2 and BvHb2) and one truncated Hb gene (BvHb3) were found in the genome of sugar beet. Gene expression profiling of the nsHb genes was carried out by quantitative PCR in different organs and developmental stages, as well as during vernalization and under different photoperiods. BvHb1.1 and BvHb2 showed differential expression during vernalization as well as during long and short days. The high expression of BvHb2 indicates that it has an active role in the cell, maybe even taking over some BvHb1.2 functions, except during germination where BvHb1.2 together with BvHb1.1—both Class 1 nsHbs—are highly expressed. The unprecedented finding of a leader peptide at the N-terminus of BvHb1.1, for the first time in an nsHb from higher plants, together with its observed expression indicate that it may have a very specific role due to its suggested location in chloroplasts. Our findings open up new possibilities for research, breeding and engineering since Hbs could be more involved in plant development than previously was anticipated. [ABSTRACT FROM AUTHOR]

Published

2014

19. Architecture and evolution of a minute plant genome.

Author

Ibarra-Laclette, Enrique, Lyons, Eric, Hernández-Guzmán, Gustavo, Pérez-Torres, Claudia Anahí, Carretero-Paulet, Lorenzo, Chang, Tien-Hao, Lan, Tianying, Welch, Andreanna J., Juárez, María Jazmín Abraham, Simpson, June, Fernández-Cortés, Araceli, Arteaga-Vázquez, Mario, Góngora-Castillo, Elsa, Acevedo-Hernández, Gustavo, Schuster, Stephan C., Himmelbauer, Heinz, Minoche, André E., Xu, Sen, Lynch, Michael, and Oropeza-Aburto, Araceli

Subjects

*PLANT genomes, *PLANT evolution, *CHROMOSOME duplication, *MOBILE genetic elements, *GRAPE genetics, *ANGIOSPERMS

Abstract

It has been argued that the evolution of plant genome size is principally unidirectional and increasing owing to the varied action of whole-genome duplications (WGDs) and mobile element proliferation. However, extreme genome size reductions have been reported in the angiosperm family tree. Here we report the sequence of the 82-megabase genome of the carnivorous bladderwort plant Utricularia gibba. Despite its tiny size, the U. gibba genome accommodates a typical number of genes for a plant, with the main difference from other plant genomes arising from a drastic reduction in non-genic DNA. Unexpectedly, we identified at least three rounds of WGD in U. gibba since common ancestry with tomato (Solanum) and grape (Vitis). The compressed architecture of the U. gibba genome indicates that a small fraction of intergenic DNA, with few or no active retrotransposons, is sufficient to regulate and integrate all the processes required for the development and reproduction of a complex organism. [ABSTRACT FROM AUTHOR]

Published

2013

20. Highly diverse chromoviruses of Beta vulgaris are classified by chromodomains and chromosomal integration.

Author

Weber, Beatrice, Heitkam, Tony, Holtgräwe, Daniela, Weisshaar, Bernd, Minoche, André E., Dohm, Juliane C., Himmelbauer, Heinz, and Schmidt, Thomas

Subjects

*CHROMOSOMES, *BEETS, *RETROTRANSPOSONS, *NUCLEOTIDE sequence, *PLANT genomes, *HETEROCHROMATIN, *GENETIC transcription

Abstract

Background: Chromoviruses are one of the three genera of Ty3-gypsy long terminal repeat (LTR) retrotransposons, and are present in high copy numbers in plant genomes. They are widely distributed within the plant kingdom, with representatives even in lower plants such as green and red algae. Their hallmark is the presence of a chromodomain at the C-terminus of the integrase. The chromodomain exhibits structural characteristics similar to proteins of the heterochromatin protein 1 (HP1) family, which mediate the binding of each chromovirus type to specific histone variants. A specific integration via the chromodomain has been shown for only a few chromoviruses. However, a detailed study of different chromoviral clades populating a single plant genome has not yet been carried out. Results: We conducted a comprehensive survey of chromoviruses within the Beta vulgaris (sugar beet) genome, and found a highly diverse chromovirus population, with significant differences in element size, primarily caused by their flanking LTRs. In total, we identified and annotated full-length members of 16 families belonging to the four plant chromoviral clades: CRM, Tekay, Reina, and Galadriel. The families within each clade are structurally highly conserved; in particular, the position of the chromodomain coding region relative to the polypurine tract is cladespecific. Two distinct groups of chromodomains were identified. The group II chromodomain was present in three chromoviral clades, whereas families of the CRM clade contained a more divergent motif. Physical mapping using representatives of all four clades identified a clade-specific integration pattern. For some chromoviral families, we detected the presence of expressed sequence tags, indicating transcriptional activity. Conclusions: We present a detailed study of chromoviruses, belonging to the four major clades, which populate a single plant genome. Our results illustrate the diversity and family structure of B. vulgaris chromoviruses, and emphasize the role of chromodomains in the targeted integration of these viruses. We suggest that the diverse sets of plant chromoviruses with their different localization patterns might help to facilitate plant-genome organization in a structural and functional manner. [ABSTRACT FROM AUTHOR]

Published

2013

21. Evolutionary reshuffling in the Errantivirus lineage Elbe within the Beta vulgaris genome.

Author

Wollrab, Cora, Heitkam, Tony, Holtgräwe, Daniela, Weisshaar, Bernd, Minoche, André E., Dohm, Juliane C., Himmelbauer, Heinz, and Schmidt, Thomas

Subjects

*BEETS, *RETROTRANSPOSONS, *RETROVIRUSES, *OPEN reading frames (Genetics), *PLANT viruses, *VIRAL envelopes, *VIRUSES

Abstract

LTR retrotransposons and retroviruses are closely related. Although a viral envelope gene is found in some LTR retrotransposons and all retroviruses, only the latter show infectivity. The identification of Ty3- gypsy-like retrotransposons possessing putative envelope-like open reading frames blurred the taxonomical borders and led to the establishment of the Errantivirus, Metavirus and Chromovirus genera within the Metaviridae. Only a few plant Errantiviruses have been described, and their evolutionary history is not well understood. In this study, we investigated 27 retroelements of four abundant Elbe retrotransposon families belonging to the Errantiviruses in Beta vulgaris (sugar beet). Retroelements of the Elbe lineage integrated between 0.02 and 5.59 million years ago, and show family-specific variations in autonomy and degree of rearrangements: while Elbe3 members are highly fragmented, often truncated and present in a high number of solo LTRs, Elbe2 members are mainly autonomous. We observed extensive reshuffling of structural motifs across families, leading to the formation of new retrotransposon families. Elbe retrotransposons harbor a typical envelope-like gene, often encoding transmembrane domains. During the course of Elbe evolution, the additional open reading frames have been strongly modified or independently acquired. Taken together, the Elbe lineage serves as retrotransposon model reflecting the various stages in Errantivirus evolution, and allows a detailed analysis of retrotransposon family formation. [ABSTRACT FROM AUTHOR]

Published

2012

22. Epigenetic profiling of heterochromatic satellite DNA.

Author

Zakrzewski, Falk, Weisshaar, Bernd, Fuchs, Jörg, Bannack, Ekaterina, Minoche, André, Dohm, Juliane, Himmelbauer, Heinz, and Schmidt, Thomas

Subjects

*DNA, *SUGAR beets, *CHROMOSOMES, *METHYLATION, *NUCLEOTIDES, *HYPOTHESIS, *QUANTITATIVE research

Abstract

Sugar beet ( Beta vulgaris) chromosomes consist of large heterochromatic blocks in pericentromeric, centromeric, and intercalary regions comprised of two different highly abundant DNA satellite families. To investigate DNA methylation at single base resolution at heterochromatic regions, we applied a method for strand-specific bisulfite sequencing of more than 1,000 satellite monomers followed by statistical analyses. As a result, we uncovered diversity in the distribution of different methylation patterns in both satellite families. Heavily methylated CG and CHG (H=A, T, or C) sites occur more frequently in intercalary heterochromatin, while CHH sites, with the exception of CAA, are only sparsely methylated, in both intercalary and pericentromeric/centromeric heterochromatin. We show that the difference in DNA methylation intensity is correlated to unequal distribution of heterochromatic histone H3 methylation marks. While clusters of H3K9me2 were absent from pericentromeric heterochromatin and restricted only to intercalary heterochromatic regions, H3K9me1 and H3K27me1 were observed in all types of heterochromatin. By sequencing of a small RNA library consisting of 6.76 million small RNAs, we identified small interfering RNAs (siRNAs) of 24 nucleotides in size which originated from both strands of the satellite DNAs. We hypothesize an involvement of these siRNAs in the regulation of DNA and histone methylation for maintaining heterochromatin. [ABSTRACT FROM AUTHOR]

Published

2011

23. p53 Gene Repair with Zinc Finger Nucleases Optimised by Yeast 1-Hybrid and Validated by Solexa Sequencing.

Author

Herrmann, Frank, Garriga-Canut, Mireia, Baumstark, Rebecca, Fajardo-Sanchez, Emmanuel, Cotterell, James, Minoche, André, Himmelbauer, Heinz, and Isalan, Mark

Subjects

*P53 antioncogene, *ZINC-finger proteins, *NUCLEASES, *YEAST, *NUCLEOTIDE sequence, *RANDOMIZED controlled trials, *GENETIC mutation, *TUMOR growth

Abstract

The tumor suppressor gene p53 is mutated or deleted in over 50% of human tumors. As functional p53 plays a pivotal role in protecting against cancer development, several strategies for restoring wild-type (wt) p53 function have been investigated. In this study, we applied an approach using gene repair with zinc finger nucleases (ZFNs). We adapted a commercially-available yeast one-hybrid (Y1H) selection kit to allow rapid building and optimization of 4-finger constructs from randomized PCR libraries. We thus generated novel functional zinc finger nucleases against two DNA sites in the human p53 gene, near cancer mutation 'hotspots'. The ZFNs were first validated using in vitro cleavage assays and in vivo episomal gene repair assays in HEK293T cells. Subsequently, the ZFNs were used to restore wt-p53 status in the SF268 human cancer cell line, via ZFN-induced homologous recombination. The frequency of gene repair and mutation by nonhomologous end-joining was then ascertained in several cancer cell lines, using a deep sequencing strategy. Our Y1H system facilitates the generation and optimisation of novel, sequence-specific four- to six-finger peptides, and the p53- specific ZFN described here can be used to mutate or repair p53 in genomic loci. [ABSTRACT FROM AUTHOR]

Published

2011

24. Application of Genome Sequencing from Blood to Diagnose Mitochondrial Diseases.

Author

Rius, Rocio, Compton, Alison G., Baker, Naomi L., Welch, AnneMarie E., Coman, David, Kava, Maina P., Minoche, Andre E., Cowley, Mark J., Thorburn, David R., and Christodoulou, John

Subjects

*MITOCHONDRIAL DNA, *NUCLEOTIDE sequencing, *MITOCHONDRIA, *NUCLEAR DNA, *DELETION mutation, *COST control

Abstract

Mitochondrial diseases can be caused by pathogenic variants in nuclear or mitochondrial DNA-encoded genes that often lead to multisystemic symptoms and can have any mode of inheritance. Using a single test, Genome Sequencing (GS) can effectively identify variants in both genomes, but it has not yet been universally used as a first-line approach to diagnosing mitochondrial diseases due to related costs and challenges in data analysis. In this article, we report three patients with mitochondrial disease molecularly diagnosed through GS performed on DNA extracted from blood to demonstrate different diagnostic advantages of this technology, including the detection of a low-level heteroplasmic pathogenic variant, an intragenic nuclear DNA deletion, and a large mtDNA deletion. Current technical improvements and cost reductions are likely to lead to an expanded routine diagnostic usage of GS and of the complementary "Omic" technologies in mitochondrial diseases. [ABSTRACT FROM AUTHOR]

Published

2021

25. Identification of a mutation in the extracellular domain of the Epidermal Growth Factor Receptor conferring cetuximab resistance in colorectal cancer.

Author

Montagut, Clara, Dalmases, Alba, Bellosillo, Beatriz, Crespo, Marta, Pairet, Silvia, Iglesias, Mar, Salido, Marta, Gallen, Manuel, Marsters, Scot, Tsai, Siao Ping, Minoche, André, Somasekar, Seshagiri, Serrano, Sergi, Himmelbauer, Heinz, Bellmunt, Joaquim, Rovira, Ana, Settleman, Jeff, Bosch, Francesc, and Albanell, Joan

Subjects

*EPIDERMAL growth factor receptors, *EXTRACELLULAR space, *CETUXIMAB, *COLON cancer treatment, *CANCER cell growth

Abstract

Antibodies against epidermal growth factor receptor (EGFR)-cetuximab and panitumumab-are widely used to treat colorectal cancer. Unfortunately, patients eventually develop resistance to these agents. We describe an acquired EGFR ectodomain mutation (S492R) that prevents cetuximab binding and confers resistance to cetuximab. Cells with this mutation, however, retain binding to and are growth inhibited by panitumumab. Two of ten subjects studied here with disease progression after cetuximab treatment acquired this mutation. A subject with cetuximab resistance harboring the S492R mutation responded to treatment with panitumumab. [ABSTRACT FROM AUTHOR]

Published

2012

26. Canfam_GSD: De novo chromosome-length genome assembly of the German Shepherd Dog (Canis lupus familiaris) using a combination of long reads, optical mapping, and Hi-C.

Author

Field, Matt A, Rosen, Benjamin D, Dudchenko, Olga, Chan, Eva K F, Minoche, Andre E, Edwards, Richard J, Barton, Kirston, Lyons, Ruth J, Tuipulotu, Daniel Enosi, Hayes, Vanessa M, D. Omer, Arina, Colaric, Zane, Keilwagen, Jens, Skvortsova, Ksenia, Bogdanovic, Ozren, Smith, Martin A, Aiden, Erez Lieberman, Smith, Timothy P L, Zammit, Robert A, and Ballard, J William O

Subjects

*GERMAN shepherd dog

Abstract

Background The German Shepherd Dog (GSD) is one of the most common breeds on earth and has been bred for its utility and intelligence. It is often first choice for police and military work, as well as protection, disability assistance, and search-and-rescue. Yet, GSDs are well known to be susceptible to a range of genetic diseases that can interfere with their training. Such diseases are of particular concern when they occur later in life, and fully trained animals are not able to continue their duties. Findings Here, we provide the draft genome sequence of a healthy German Shepherd female as a reference for future disease and evolutionary studies. We generated this improved canid reference genome (CanFam_GSD) utilizing a combination of Pacific Bioscience, Oxford Nanopore, 10X Genomics, Bionano, and Hi-C technologies. The GSD assembly is ∼80 times as contiguous as the current canid reference genome (20.9 vs 0.267 Mb contig N50), containing far fewer gaps (306 vs 23,876) and fewer scaffolds (429 vs 3,310) than the current canid reference genome CanFamv3.1. Two chromosomes (4 and 35) are assembled into single scaffolds with no gaps. BUSCO analyses of the genome assembly results show that 93.0% of the conserved single-copy genes are complete in the GSD assembly compared with 92.2% for CanFam v3.1. Homology-based gene annotation increases this value to ∼99%. Detailed examination of the evolutionarily important pancreatic amylase region reveals that there are most likely 7 copies of the gene, indicative of a duplication of 4 ancestral copies and the disruption of 1 copy. Conclusions GSD genome assembly and annotation were produced with major improvement in completeness, continuity, and quality over the existing canid reference. This resource will enable further research related to canine diseases, the evolutionary relationships of canids, and other aspects of canid biology. [ABSTRACT FROM AUTHOR]

Published

2020

27. De Novo Variants Disrupting the HX Repeat Motif of ATN1 Cause a Recognizable Non-progressive Neurocognitive Syndrome.

Author

Palmer, Elizabeth E., Hong, Seungbeom, Al Zahrani, Fatema, Hashem, Mais O., Aleisa, Fajr A., Jalal Ahmed, Heba M., Kandula, Tejaswi, Macintosh, Rebecca, Minoche, Andre E., Puttick, Clare, Gayevskiy, Velimir, Drew, Alexander P., Cowley, Mark J., Dinger, Marcel, Rosenfeld, Jill A., Xiao, Rui, Cho, Megan T., Yakubu, Suliat F., Henderson, Lindsay B., and Guillen Sacoto, Maria J.

Subjects

*SYNDROMES, *HUMAN genetics

Published

2019

28. Identification of a mutation in the extracellular domain of the Epidermal Growth Factor Receptor conferring cetuximab resistance in colorectal cancer.

Author

Montagut, Clara, Dalmases, Alba, Bellosillo, Beatriz, Crespo, Marta, Pairet, Silvia, Iglesias, Mar, Salido, Marta, Gallen, Manuel, Marsters, Scot, Tsai, Siao Ping, Minoche, André, Somasekar, Seshagiri, Serrano, Sergi, Himmelbauer, Heinz, Bellmunt, Joaquim, Rovira, Ana, Settleman, Jeff, Bosch, Francesc, and Albanell, Joan

Subjects

*PUBLISHED errata, *EPIDERMAL growth factor receptors, *COLON cancer

Abstract

A correction to the article "Identification of a mutation in the extracellular domain of the Epidermal Growth Factor Receptor conferring cetuximab resistance in colorectal cancer" that was published in the July 6, 2012 issue is presented.

Published

2012