Quantitative Genomics of 30 Complex Phenotypes in Wagyu x Angus F1 Progeny

Lifan Zhang; Jennifer J. Michal; James V. O'Fallon; Zengxiang Pan; Charles T. Gaskins; Jerry J. Reeves; Jan R. Busboom; Xiang Zhou; Bo Ding; Michael V. Dodson; Zhihua Jiang

doi:10.7150/ijbs.4403

Assessment of the Growth and Reproductive Performance of Cloned Pietrain Boars

Animals ◽

10.3390/ani10112053 ◽

2020 ◽

Vol 10 (11) ◽

pp. 2053

Author(s):

Junsong Shi ◽

Baohua Tan ◽

Lvhua Luo ◽

Zicong Li ◽

Linjun Hong ◽

...

Keyword(s):

Growth Rate ◽

Body Size ◽

Growth Performance ◽

Reproductive Performance ◽

Semen Quality ◽

Small Body ◽

Economic Benefits ◽

Large Animal ◽

Significant Difference ◽

F1 Progeny

How to maximize the use of the genetic merits of the high-ranking boars (also called superior ones) is a considerable question in the pig breeding industry, considering the money and time spent on selection. Somatic cell nuclear transfer (SCNT) is one of the potential ways to answer the question, which can be applied to produce clones with genetic resources of superior boar for the production of commercial pigs. For practical application, it is essential to investigate whether the clones and their progeny keep behaving better than the “normal boars”, considering that in vitro culture and transfer manipulation would cause a series of harmful effects to the development of clones. In this study, 59,061 cloned embryos were transferred into 250 recipient sows to produce the clones of superior Pietrain boars. The growth performance of 12 clones and 36 non-clones and the semen quality of 19 clones and 28 non-clones were compared. The reproductive performance of 21 clones and 25 non-clones were also tested. Furthermore, we made a comparison in the growth performance between 466 progeny of the clones and 822 progeny of the non-clones. Our results showed that no significant difference in semen quality and reproductive performance was observed between the clones and the non-clones, although the clones grew slower and exhibited smaller body size than the non-clones. The F1 progeny of the clones showed a greater growth rate than the non-clones. Our results demonstrated through the large animal population showed that SCNT manipulation resulted in a low growth rate and small body size, but the clones could normally produce F1 progeny with excellent growth traits to bring more economic benefits. Therefore, SCNT could be effective in enlarging the merit genetics of the superior boars and increasing the economic benefits in pig reproduction and breeding.

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Four chromosome scale genomes and a pan-genome annotation to accelerate pecan tree breeding

Nature Communications ◽

10.1038/s41467-021-24328-w ◽

2021 ◽

Vol 12 (1) ◽

Author(s):

John T. Lovell ◽

Nolan B. Bentley ◽

Gaurab Bhattarai ◽

Jerry W. Jenkins ◽

Avinash Sreedasyam ◽

...

Keyword(s):

Tree Breeding ◽

Pathogen Resistance ◽

Perennial Crop ◽

Crop Species ◽

Annotation Database ◽

Pan Genome ◽

Genome Integration ◽

Transformative Potential ◽

Genome Assemblies ◽

Quantitative Genomics

AbstractGenome-enabled biotechnologies have the potential to accelerate breeding efforts in long-lived perennial crop species. Despite the transformative potential of molecular tools in pecan and other outcrossing tree species, highly heterozygous genomes, significant presence–absence gene content variation, and histories of interspecific hybridization have constrained breeding efforts. To overcome these challenges, here, we present diploid genome assemblies and annotations of four outbred pecan genotypes, including a PacBio HiFi chromosome-scale assembly of both haplotypes of the ‘Pawnee’ cultivar. Comparative analysis and pan-genome integration reveal substantial and likely adaptive interspecific genomic introgressions, including an over-retained haplotype introgressed from bitternut hickory into pecan breeding pedigrees. Further, by leveraging our pan-genome presence–absence and functional annotation database among genomes and within the two outbred haplotypes of the ‘Lakota’ genome, we identify candidate genes for pest and pathogen resistance. Combined, these analyses and resources highlight significant progress towards functional and quantitative genomics in highly diverse and outbred crops.

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Maternal-effect lethal mutations on linkage group II of Caenorhabditis elegans.

Genetics ◽

10.1093/genetics/120.4.977 ◽

1988 ◽

Vol 120 (4) ◽

pp. 977-986

Author(s):

K J Kemphues ◽

M Kusch ◽

N Wolf

Keyword(s):

Caenorhabditis Elegans ◽

Linkage Group ◽

Maternal Effect ◽

Essential Genes ◽

The Other ◽

C Elegans ◽

Lethal Mutations ◽

Embryonic Lethal ◽

Embryonic Lethal Mutations ◽

F1 Progeny

Abstract We have analyzed a set of linkage group (LG) II maternal-effect lethal mutations in Caenorhabditis elegans isolated by a new screening procedure. Screens of 12,455 F1 progeny from mutagenized adults resulted in the recovery of 54 maternal-effect lethal mutations identifying 29 genes. Of the 54 mutations, 39 are strict maternal-effect mutations defining 17 genes. These 17 genes fall into two classes distinguished by frequency of mutation to strict maternal-effect lethality. The smaller class, comprised of four genes, mutated to strict maternal-effect lethality at a frequency close to 5 X 10(-4), a rate typical of essential genes in C. elegans. Two of these genes are expressed during oogenesis and required exclusively for embryogenesis (pure maternal genes), one appears to be required specifically for meiosis, and the fourth has a more complex pattern of expression. The other 13 genes were represented by only one or two strict maternal alleles each. Two of these are identical genes previously identified by nonmaternal embryonic lethal mutations. We interpret our results to mean that although many C. elegans genes can mutate to strict maternal-effect lethality, most genes mutate to that phenotype rarely. Pure maternal genes, however, are among a smaller class of genes that mutate to maternal-effect lethality at typical rates. If our interpretation is correct, we are near saturation for pure maternal genes in the region of LG II balanced by mnC1. We conclude that the number of pure maternal genes in C. elegans is small, being probably not much higher than 12.

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High efficiency and clinical relevance of exome sequencing in the daily practice of neurogenetics

Journal of Medical Genetics ◽

10.1136/jmedgenet-2020-107369 ◽

2021 ◽

pp. jmedgenet-2020-107369

Author(s):

Quentin Thomas ◽

Antonio Vitobello ◽

Frederic Tran Mau-Them ◽

Yannis Duffourd ◽

Agnès Fromont ◽

...

Keyword(s):

Exome Sequencing ◽

Neurological Disorders ◽

High Efficiency ◽

Neuromuscular Disorders ◽

Daily Practice ◽

Pathogenic Variants ◽

Complex Phenotypes ◽

Cerebellar Ataxias ◽

Mitochondrial Origin ◽

Second Tier

ObjectiveTo assess the efficiency and relevance of clinical exome sequencing (cES) as a first-tier or second-tier test for the diagnosis of progressive neurological disorders in the daily practice of Neurology and Genetic Departments.MethodsSixty-seven probands with various progressive neurological disorders (cerebellar ataxias, neuromuscular disorders, spastic paraplegias, movement disorders and individuals with complex phenotypes labelled ‘other’) were recruited over a 4-year period regardless of their age, gender, familial history and clinical framework. Individuals could have had prior genetic tests as long as it was not cES. cES was performed in a proband-only (60/67) or trio (7/67) strategy depending on available samples and was analysed with an in-house pipeline including software for CNV and mitochondrial-DNA variant detection.ResultsIn 29/67 individuals, cES identified clearly pathogenic variants leading to a 43% positive yield. When performed as a first-tier test, cES identified pathogenic variants for 53% of individuals (10/19). Difficult cases were solved including double diagnoses within a kindred or identification of a neurodegeneration with brain iron accumulation in a patient with encephalopathy of suspected mitochondrial origin.ConclusionThis study shows that cES is a powerful tool for the daily practice of neurogenetics offering an efficient (43%) and appropriate approach for clinically and genetically complex and heterogeneous disorders.

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Phenotypic homogeneity in childhood epilepsies evolves in gene-specific patterns across 3251 patient-years of clinical data

European Journal of Human Genetics ◽

10.1038/s41431-021-00908-8 ◽

2021 ◽

Author(s):

David Lewis-Smith ◽

Shiva Ganesan ◽

Peter D. Galer ◽

Katherine L. Helbig ◽

Sarah E. McKeown ◽

...

Keyword(s):

Clinical Data ◽

Similarity Analysis ◽

Genetic Studies ◽

Human Phenotype ◽

Phenotypic Similarity ◽

Complex Phenotypes ◽

Cognitive Framework ◽

Novel Approach ◽

Genetic Epilepsies

AbstractWhile genetic studies of epilepsies can be performed in thousands of individuals, phenotyping remains a manual, non-scalable task. A particular challenge is capturing the evolution of complex phenotypes with age. Here, we present a novel approach, applying phenotypic similarity analysis to a total of 3251 patient-years of longitudinal electronic medical record data from a previously reported cohort of 658 individuals with genetic epilepsies. After mapping clinical data to the Human Phenotype Ontology, we determined the phenotypic similarity of individuals sharing each genetic etiology within each 3-month age interval from birth up to a maximum age of 25 years. 140 of 600 (23%) of all 27 genes and 3-month age intervals with sufficient data for calculation of phenotypic similarity were significantly higher than expect by chance. 11 of 27 genetic etiologies had significant overall phenotypic similarity trajectories. These do not simply reflect strong statistical associations with single phenotypic features but appear to emerge from complex clinical constellations of features that may not be strongly associated individually. As an attempt to reconstruct the cognitive framework of syndrome recognition in clinical practice, longitudinal phenotypic similarity analysis extends the traditional phenotyping approach by utilizing data from electronic medical records at a scale that is far beyond the capabilities of manual phenotyping. Delineation of how the phenotypic homogeneity of genetic epilepsies varies with age could improve the phenotypic classification of these disorders, the accuracy of prognostic counseling, and by providing historical control data, the design and interpretation of precision clinical trials in rare diseases.

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Pediatric Bipolar Disorder: Complex Phenotypes, Genotypes, and Environments

Psychosocial Interventions for Genetically Influenced Problems in Childhood and Adolescence ◽

10.1002/9781118948187.ch06 ◽

2014 ◽

pp. 127-152

Keyword(s):

Bipolar Disorder ◽

Pediatric Bipolar Disorder ◽

Complex Phenotypes

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Biogenetic Mechanisms Predisposing to Complex Phenotypes in Parents May Function Differently in Their Children

The Journals of Gerontology Series A ◽

10.1093/gerona/gls243 ◽

2012 ◽

Vol 68 (7) ◽

pp. 760-768 ◽

Cited By ~ 2

Author(s):

Alexander M. Kulminski ◽

Konstantin G. Arbeev ◽

Kaare Christensen ◽

Eric Stallard ◽

Iva Miljkovic ◽

...

Keyword(s):

Complex Phenotypes

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Ethylene dibromide: effects of paternal exposure on the neurotransmitter enzymes in the developing brain of F1 progeny

Mutation Research/Environmental Mutagenesis and Related Subjects ◽

10.1016/0165-1161(85)90058-5 ◽

1985 ◽

Vol 147 (4) ◽

pp. 197-203 ◽

Cited By ~ 10

Author(s):

Louise L. Hsu ◽

Perrie M. Adams ◽

Donatella Fanini ◽

Marvin S. Legator

Keyword(s):

Developing Brain ◽

Ethylene Dibromide ◽

Paternal Exposure ◽

F1 Progeny ◽

Neurotransmitter Enzymes

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Engineering Complex Phenotypes in Industrial Strains

10.1002/9781118433034 ◽

2012 ◽

Cited By ~ 1

Keyword(s):

Complex Phenotypes ◽

Industrial Strains

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Laterality phenotypes in patients with schizophrenia, their siblings and controls: Associations with clinical and cognitive variables

The British Journal of Psychiatry ◽

10.1192/bjp.187.3.221 ◽

2005 ◽

Vol 187 (3) ◽

pp. 221-228 ◽

Cited By ~ 10

Author(s):

Milan Dragovic ◽

Geoff Hammond ◽

Johanna C. Badcock ◽

Assen Jablensky

Keyword(s):

Clinical Severity ◽

Hand Dominance ◽

Cognitive Variables ◽

Neurocognitive Deficits ◽

Neurocognitive Performance ◽

Course Of Illness ◽

Complex Phenotypes ◽

Novel Approach ◽

Behavioural Asymmetries ◽

Grade Of Membership

BackgroundVarious behavioural indices of brain lateralisation significantly intercorrelate, but current research in this area still focuses on single behavioural asymmetries, such as handedness.AimsTo describe a novel approach, which simultaneously integrates various laterality indices and delineates complex phenotypes.MethodGrade of membership analysis was used to describe latent, complex lateralisation phenotypes in patients with schizophrenia (n=157), their siblings (n=74) and controls (n=77). The indices used were asymmetries of eye, foot and hand; hand motor proficiency; and handedness of patient's first-degree relatives.ResultsThree distinct pure types of lateralisation (‘right’, ‘left’ and ‘mixed’) were evident in patients compared with two (‘right’ and ‘left’) in siblings and controls. The ‘mixed’ type in patients featured absence of eye and foot lateralisation and presence of familial sinistrality, despite a right-hand dominance for writing. Patients with schizophrenia expressing the ‘left’ phenotype had a more severe course of illness, significantly increased scores on two schizotypy factors and poorer neurocognitive performance. The pure types in the siblings were similar to those in healthy controls.ConclusionsThe findings suggest that a leftward reversal, rather than a reduction in lateralisation, is associated with clinical severity and neurocognitive deficits in patients with schizophrenia.

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