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Genetic Recombination by David Leach
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1Genetic Recombination As A Chemical Reaction Network
By Stefan Müller and Josef Hofbauer
The process of genetic recombination can be seen as a chemical reaction network with mass-action kinetics. We review the known results on existence, uniqueness, and global stability of an equilibrium in every compatibility class and for all rate constants, from both the population genetics and the reaction networks point of view.
“Genetic Recombination As A Chemical Reaction Network” Metadata:
- Title: ➤ Genetic Recombination As A Chemical Reaction Network
- Authors: Stefan MüllerJosef Hofbauer
- Language: English
“Genetic Recombination As A Chemical Reaction Network” Subjects and Themes:
- Subjects: Molecular Networks - Quantitative Biology
Edition Identifiers:
- Internet Archive ID: arxiv-1503.01155
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2Invariant Measures Of Genetic Recombination Process
By Arseniy V. Akopyan, Sergey A. Pirogov and Aleksandr N. Rybko
We construct the non-linear Markov process connected with biological model of bacterial genome recombination. The description of invariant measures of this process gives us the solution of one problem in elementary probability theory.
“Invariant Measures Of Genetic Recombination Process” Metadata:
- Title: ➤ Invariant Measures Of Genetic Recombination Process
- Authors: Arseniy V. AkopyanSergey A. PirogovAleksandr N. Rybko
“Invariant Measures Of Genetic Recombination Process” Subjects and Themes:
- Subjects: Probability - Mathematics
Edition Identifiers:
- Internet Archive ID: arxiv-1406.5313
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3Genetic Recombination In Cancer
By Sherbet, G. V. (Gajanan V.)
We construct the non-linear Markov process connected with biological model of bacterial genome recombination. The description of invariant measures of this process gives us the solution of one problem in elementary probability theory.
“Genetic Recombination In Cancer” Metadata:
- Title: ➤ Genetic Recombination In Cancer
- Author: Sherbet, G. V. (Gajanan V.)
- Language: English
“Genetic Recombination In Cancer” Subjects and Themes:
- Subjects: ➤ Cancer -- Genetic aspects - Genetic recombination - Neoplasms -- genetics - Neoplasm Metastasis - Recombination, Genetic - humane ziekten - human diseases - neoplasms - recombinatie - recombination - genetische stoornissen - genetic disorders - dna repair - chromosomen - chromosomes - Human Pathology - Humane pathologie
Edition Identifiers:
- Internet Archive ID: geneticrecombina0000sher
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4Nonhomologous Recombination Between Defective Poliovirus And Coxsackievirus Genomes Suggests A New Model Of Genetic Plasticity For Picornaviruses.
By Holmblat, Barbara, Jegouic, Sophie, Muslin, Claire, Blondel, Bruno, Joffret, Marie-Line and Delpeyroux, Francis
This article is from mBio , volume 5 . Abstract Most of the circulating vaccine-derived polioviruses (cVDPVs) implicated in poliomyelitis outbreaks in Madagascar have been shown to be recombinants between the type 2 poliovirus (PV) strain of the oral polio vaccine (Sabin 2) and another species C human enterovirus (HEV-C), such as type 17 coxsackie A virus (CA17) in particular. We studied intertypic genetic exchanges between PV and non-PV HEV-C by developing a recombination model, making it possible to rescue defective type 2 PV RNA genomes with a short deletion at the 3′ end by the cotransfection of cells with defective or infectious CA17 RNAs. We isolated over 200 different PV/CA17 recombinants, using murine cells expressing the human PV receptor (PVR) and selecting viruses with PV capsids. We found some homologous (H) recombinants and, mostly, nonhomologous (NH) recombinants presenting duplications of parental sequences preferentially located in the regions encoding proteins 2A, 2B, and 3A. Short duplications appeared to be stable, whereas longer duplications were excised during passaging in cultured cells or after multiplication in PVR-transgenic mice, generating H recombinants with diverse sites of recombination. This suggests that NH recombination events may be a transient, intermediate step in the generation and selection of the fittest H recombinants. In addition to the classical copy-choice mechanism of recombination thought to generate mostly H recombinants, there may also be a modular mechanism of recombination, involving NH recombinant precursors, shaping the genomes of recombinant enteroviruses and other picornaviruses.
“Nonhomologous Recombination Between Defective Poliovirus And Coxsackievirus Genomes Suggests A New Model Of Genetic Plasticity For Picornaviruses.” Metadata:
- Title: ➤ Nonhomologous Recombination Between Defective Poliovirus And Coxsackievirus Genomes Suggests A New Model Of Genetic Plasticity For Picornaviruses.
- Authors: ➤ Holmblat, BarbaraJegouic, SophieMuslin, ClaireBlondel, BrunoJoffret, Marie-LineDelpeyroux, Francis
- Language: English
Edition Identifiers:
- Internet Archive ID: pubmed-PMC4128350
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5Modulation Of Base Specific Mutation And Recombination Rates Enables Functional Adaptation Within The Context Of The Genetic Code
By Taison Tan, Leonard D. Bogarad and Michael W. Deem
The persistence of life requires populations to adapt at a rate commensurate with the dynamics of their environment. Successful populations that inhabit highly variable environments have evolved mechanisms to increase the likelihood of successful adaptation. We introduce a $64 \times 64$ matrix to quantify base-specific mutation potential, analyzing four different replicative systems, error-prone PCR, mouse antibodies, a nematode, and Drosophila. Mutational tendencies are correlated with the structural evolution of proteins. In systems under strong selective pressure, mutational biases are shown to favor the adaptive search of space, either by base mutation or by recombination. Such adaptability is discussed within the context of the genetic code at the levels of replication and codon usage.
“Modulation Of Base Specific Mutation And Recombination Rates Enables Functional Adaptation Within The Context Of The Genetic Code” Metadata:
- Title: ➤ Modulation Of Base Specific Mutation And Recombination Rates Enables Functional Adaptation Within The Context Of The Genetic Code
- Authors: Taison TanLeonard D. BogaradMichael W. Deem
- Language: English
Edition Identifiers:
- Internet Archive ID: arxiv-q-bio0404022
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6The Recombination Of Genetic Material
The persistence of life requires populations to adapt at a rate commensurate with the dynamics of their environment. Successful populations that inhabit highly variable environments have evolved mechanisms to increase the likelihood of successful adaptation. We introduce a $64 \times 64$ matrix to quantify base-specific mutation potential, analyzing four different replicative systems, error-prone PCR, mouse antibodies, a nematode, and Drosophila. Mutational tendencies are correlated with the structural evolution of proteins. In systems under strong selective pressure, mutational biases are shown to favor the adaptive search of space, either by base mutation or by recombination. Such adaptability is discussed within the context of the genetic code at the levels of replication and codon usage.
“The Recombination Of Genetic Material” Metadata:
- Title: ➤ The Recombination Of Genetic Material
- Language: English
Edition Identifiers:
- Internet Archive ID: recombinationofg0000unse
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7Characterizing Scales Of Genetic Recombination And Antibiotic Resistance In Pathogenic Bacteria Using Topological Data Analysis
By Kevin J. Emmett and Raul Rabadan
Pathogenic bacteria present a large disease burden on human health. Control of these pathogens is hampered by rampant lateral gene transfer, whereby pathogenic strains may acquire genes conferring resistance to common antibiotics. Here we introduce tools from topological data analysis to characterize the frequency and scale of lateral gene transfer in bacteria, focusing on a set of pathogens of significant public health relevance. As a case study, we examine the spread of antibiotic resistance in Staphylococcus aureus. Finally, we consider the possible role of the human microbiome as a reservoir for antibiotic resistance genes.
“Characterizing Scales Of Genetic Recombination And Antibiotic Resistance In Pathogenic Bacteria Using Topological Data Analysis” Metadata:
- Title: ➤ Characterizing Scales Of Genetic Recombination And Antibiotic Resistance In Pathogenic Bacteria Using Topological Data Analysis
- Authors: Kevin J. EmmettRaul Rabadan
“Characterizing Scales Of Genetic Recombination And Antibiotic Resistance In Pathogenic Bacteria Using Topological Data Analysis” Subjects and Themes:
- Subjects: Populations and Evolution - Quantitative Biology - Genomics
Edition Identifiers:
- Internet Archive ID: arxiv-1406.1219
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8GENETIC RECOMBINATION BETWEEN THE RESISTANCE TRANSFER FACTOR AND THE CHROMOSOME OF ESCHERICHIA COLI
Pathogenic bacteria present a large disease burden on human health. Control of these pathogens is hampered by rampant lateral gene transfer, whereby pathogenic strains may acquire genes conferring resistance to common antibiotics. Here we introduce tools from topological data analysis to characterize the frequency and scale of lateral gene transfer in bacteria, focusing on a set of pathogens of significant public health relevance. As a case study, we examine the spread of antibiotic resistance in Staphylococcus aureus. Finally, we consider the possible role of the human microbiome as a reservoir for antibiotic resistance genes.
“GENETIC RECOMBINATION BETWEEN THE RESISTANCE TRANSFER FACTOR AND THE CHROMOSOME OF ESCHERICHIA COLI” Metadata:
- Title: ➤ GENETIC RECOMBINATION BETWEEN THE RESISTANCE TRANSFER FACTOR AND THE CHROMOSOME OF ESCHERICHIA COLI
- Language: English
Edition Identifiers:
- Internet Archive ID: ➤ nasa_open_access_october_codes_PMC277208
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9UV-mutability And Genetic Recombination Of UV-induced Gamma-ray Sensitive Mutants Of Neurospora Crassa
By Ram Deva Mehta
Pathogenic bacteria present a large disease burden on human health. Control of these pathogens is hampered by rampant lateral gene transfer, whereby pathogenic strains may acquire genes conferring resistance to common antibiotics. Here we introduce tools from topological data analysis to characterize the frequency and scale of lateral gene transfer in bacteria, focusing on a set of pathogens of significant public health relevance. As a case study, we examine the spread of antibiotic resistance in Staphylococcus aureus. Finally, we consider the possible role of the human microbiome as a reservoir for antibiotic resistance genes.
“UV-mutability And Genetic Recombination Of UV-induced Gamma-ray Sensitive Mutants Of Neurospora Crassa” Metadata:
- Title: ➤ UV-mutability And Genetic Recombination Of UV-induced Gamma-ray Sensitive Mutants Of Neurospora Crassa
- Author: Ram Deva Mehta
- Language: English
Edition Identifiers:
- Internet Archive ID: Mehta1972
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10The Effect Of Recombination On The Neutral Evolution Of Genetic Robustness
By Gergely J. Szollosi and Imre Derenyi
Conventional population genetics considers the evolution of a limited number of genotypes corresponding to phenotypes with different fitness. As model phenotypes, in particular RNA secondary structure, have become computationally tractable, however, it has become apparent that the context dependent effect of mutations and the many-to-one nature inherent in these genotype-phenotype maps can have fundamental evolutionary consequences. It has previously been demonstrated that populations of genotypes evolving on the neutral networks corresponding to all genotypes with the same secondary structure only through neutral mutations can evolve mutational robustness [Nimwegen {\it et al.} Neutral evolution of mutational robustness, 1999 PNAS], by concentrating the population on regions of high neutrality. Introducing recombination we demonstrate, through numerically calculating the stationary distribution of an infinite population on ensembles of random neutral networks that mutational robustness is significantly enhanced and further that the magnitude of this enhancement is sensitive to details of the neutral network topology. Through the simulation of finite populations of genotypes evolving on random neutral networks and a scaled down microRNA neutral network, we show that even in finite populations recombination will still act to focus the population on regions of locally high neutrality.
“The Effect Of Recombination On The Neutral Evolution Of Genetic Robustness” Metadata:
- Title: ➤ The Effect Of Recombination On The Neutral Evolution Of Genetic Robustness
- Authors: Gergely J. SzollosiImre Derenyi
- Language: English
Edition Identifiers:
- Internet Archive ID: arxiv-0804.3279
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11Genetic Diversity, Heteroplasmy, And Recombination In Mitochondrial Genomes Of Daphnia Pulex, Daphnia Pulicaria, And Daphnia Obtusa
By Zhiqiang Ye, Chaoxian Zhao, R. Taylor Raborn, Man Lin, Wen Wei, Yue Hao, Michael Lynch
Genetic variants of mitochondrial DNA at the individual (heteroplasmy) and population (polymorphism) levels provide insight into their roles in multiple cellular and evolutionary processes. However, owing to the paucity of genome-wide data at the within-individual and population levels, the broad patterns of these two forms of variation remain poorly understood. Here, we analyze 1,804 complete mitochondrial genome sequences from Daphnia pulex , Daphnia pulicaria , and Daphnia obtusa . Extensive heteroplasmy is observed in D. obtusa , where the high level of intraclonal divergence must have resulted from a biparental-inheritance event, and recombination in the mitochondrial genome is apparent, although perhaps not widespread. Global samples of D. pulex reveal remarkably low mitochondrial effective population sizes, <3% of those for the nuclear genome. In addition, levels of population diversity in mitochondrial and nuclear genomes are uncorrelated across populations, suggesting an idiosyncratic evolutionary history of mitochondria in D. pulex . These population-genetic features appear to be a consequence of background selection associated with highly deleterious mutations arising in the strongly linked mitochondrial genome, which is consistent with polymorphism and divergence data suggesting a predominance of strong purifying selection. Nonetheless, the fixation of mildly deleterious mutations in the mitochondrial genome also appears to be driving positive selection on genes encoded in the nuclear genome whose products are deployed in the mitochondrion.
“Genetic Diversity, Heteroplasmy, And Recombination In Mitochondrial Genomes Of Daphnia Pulex, Daphnia Pulicaria, And Daphnia Obtusa” Metadata:
- Title: ➤ Genetic Diversity, Heteroplasmy, And Recombination In Mitochondrial Genomes Of Daphnia Pulex, Daphnia Pulicaria, And Daphnia Obtusa
- Author: ➤ Zhiqiang Ye, Chaoxian Zhao, R. Taylor Raborn, Man Lin, Wen Wei, Yue Hao, Michael Lynch
- Language: English
“Genetic Diversity, Heteroplasmy, And Recombination In Mitochondrial Genomes Of Daphnia Pulex, Daphnia Pulicaria, And Daphnia Obtusa” Subjects and Themes:
- Subjects: ➤ Daphnia - heteroplasmy - hybridization - mitochondria - nucleotide diversity - purifying selection
Edition Identifiers:
- Internet Archive ID: msac059
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The book is available for download in "texts" format, the size of the file-s is: 37.95 Mbs, the file-s for this book were downloaded 37 times, the file-s went public at Sat Apr 23 2022.
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12Genetic Recombination
By Leach, David (David Reginald Francis)
Genetic variants of mitochondrial DNA at the individual (heteroplasmy) and population (polymorphism) levels provide insight into their roles in multiple cellular and evolutionary processes. However, owing to the paucity of genome-wide data at the within-individual and population levels, the broad patterns of these two forms of variation remain poorly understood. Here, we analyze 1,804 complete mitochondrial genome sequences from Daphnia pulex , Daphnia pulicaria , and Daphnia obtusa . Extensive heteroplasmy is observed in D. obtusa , where the high level of intraclonal divergence must have resulted from a biparental-inheritance event, and recombination in the mitochondrial genome is apparent, although perhaps not widespread. Global samples of D. pulex reveal remarkably low mitochondrial effective population sizes, <3% of those for the nuclear genome. In addition, levels of population diversity in mitochondrial and nuclear genomes are uncorrelated across populations, suggesting an idiosyncratic evolutionary history of mitochondria in D. pulex . These population-genetic features appear to be a consequence of background selection associated with highly deleterious mutations arising in the strongly linked mitochondrial genome, which is consistent with polymorphism and divergence data suggesting a predominance of strong purifying selection. Nonetheless, the fixation of mildly deleterious mutations in the mitochondrial genome also appears to be driving positive selection on genes encoded in the nuclear genome whose products are deployed in the mitochondrion.
“Genetic Recombination” Metadata:
- Title: Genetic Recombination
- Author: ➤ Leach, David (David Reginald Francis)
- Language: English
“Genetic Recombination” Subjects and Themes:
- Subjects: ➤ genetische modificatie - crossing over - moleculaire genetica - genetic engineering - recombinant dna - molecular genetics - recombination - recombinatie - textbooks - studieboeken - Moleculaire genetica - Genetica (algemeen) - Recombination, Genetic - Genetic recombination - Genetik - Recombinaison génétique - Rekombination - Génétique - Genetics - Molecular Genetics - Genetics (General) - Recombinaison genetique - Genetique
Edition Identifiers:
- Internet Archive ID: geneticrecombina0000leac
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13A High-Resolution Genetic Map Of Yellow Monkeyflower Identifies Chemical Defense QTLs And Recombination Rate Variation.
By Holeski, Liza M., Monnahan, Patrick, Koseva, Boryana, McCool, Nick, Lindroth, Richard L. and Kelly, John K.
This article is from G3: Genes|Genomes|Genetics , volume 4 . Abstract Genotyping-by-sequencing methods have vastly improved the resolution and accuracy of genetic linkage maps by increasing both the number of marker loci as well as the number of individuals genotyped at these loci. Using restriction-associated DNA sequencing, we construct a dense linkage map for a panel of recombinant inbred lines derived from a cross between divergent ecotypes of Mimulus guttatus. We used this map to estimate recombination rate across the genome and to identify quantitative trait loci for the production of several secondary compounds (PPGs) of the phenylpropanoid pathway implicated in defense against herbivores. Levels of different PPGs are correlated across recombinant inbred lines suggesting joint regulation of the phenylpropanoid pathway. However, the three quantitative trait loci identified in this study each act on a distinct PPG. Finally, we map three putative genomic inversions differentiating the two parental populations, including a previously characterized inversion that contributes to life-history differences between the annual/perennial ecotypes.
“A High-Resolution Genetic Map Of Yellow Monkeyflower Identifies Chemical Defense QTLs And Recombination Rate Variation.” Metadata:
- Title: ➤ A High-Resolution Genetic Map Of Yellow Monkeyflower Identifies Chemical Defense QTLs And Recombination Rate Variation.
- Authors: ➤ Holeski, Liza M.Monnahan, PatrickKoseva, BoryanaMcCool, NickLindroth, Richard L.Kelly, John K.
- Language: English
Edition Identifiers:
- Internet Archive ID: pubmed-PMC4025480
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14AKT1/BRCA1 In The Control Of Homologous Recombination And Genetic Stability: The Missing Link Between Hereditary And Sporadic Breast Cancers.
By Guirouilh-Barbat, Josee, Wilhelm, Therese and Lopez, Bernard S.
This article is from Oncotarget , volume 1 . Abstract Endogenous replicative stress could be one trigger leading to tumor initiation: indeed, activation of the DNA damage response (DDR), considered the result of replicative stress, is observed in pre-cancerous cells; moreover, in hereditary breast cancers, almost all of the genes affected relate to the DDR. The most frequently mutated gene in hereditary breast cancers, BRCA1, is essential for homologous recombination (HR), a fundamental process for maintaining genome stability that permits the reactivation of blocked replication forks. Recent studies have established links between DDR and the oncogenic kinase AKT1, which is upregulated in about 50% of sporadic breast cancers. More specifically, the activation of AKT1 shows a deficient phenotype in BRCA1 and HR, revealing molecular similarities between hereditary and sporadic breast cancers. However, these results reveal a paradox regarding the physiological role of AKT1: in non-tumor cells, AKT1 promotes cellular proliferation, but consequently endangers genome integrity during replication if HR is inhibited. Since HR could itself lead to genetic instability, we propose that, under physiological conditions, moderate activation of AKT1 does not inhibit but prevents an excess of HR. The regulation of AKT1 would represent a fine transitory system for controlling HR and maintaining genomic integrity.
“AKT1/BRCA1 In The Control Of Homologous Recombination And Genetic Stability: The Missing Link Between Hereditary And Sporadic Breast Cancers.” Metadata:
- Title: ➤ AKT1/BRCA1 In The Control Of Homologous Recombination And Genetic Stability: The Missing Link Between Hereditary And Sporadic Breast Cancers.
- Authors: Guirouilh-Barbat, JoseeWilhelm, ThereseLopez, Bernard S.
- Language: English
Edition Identifiers:
- Internet Archive ID: pubmed-PMC3157734
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15Genetic Recombination : Editedby Raju Kucherlapati, Gerald R. Smith
This article is from Oncotarget , volume 1 . Abstract Endogenous replicative stress could be one trigger leading to tumor initiation: indeed, activation of the DNA damage response (DDR), considered the result of replicative stress, is observed in pre-cancerous cells; moreover, in hereditary breast cancers, almost all of the genes affected relate to the DDR. The most frequently mutated gene in hereditary breast cancers, BRCA1, is essential for homologous recombination (HR), a fundamental process for maintaining genome stability that permits the reactivation of blocked replication forks. Recent studies have established links between DDR and the oncogenic kinase AKT1, which is upregulated in about 50% of sporadic breast cancers. More specifically, the activation of AKT1 shows a deficient phenotype in BRCA1 and HR, revealing molecular similarities between hereditary and sporadic breast cancers. However, these results reveal a paradox regarding the physiological role of AKT1: in non-tumor cells, AKT1 promotes cellular proliferation, but consequently endangers genome integrity during replication if HR is inhibited. Since HR could itself lead to genetic instability, we propose that, under physiological conditions, moderate activation of AKT1 does not inhibit but prevents an excess of HR. The regulation of AKT1 would represent a fine transitory system for controlling HR and maintaining genomic integrity.
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- Language: English
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16DTIC AD0618860: GENETIC RECOMBINATION IN INTESTINAL BACTERIA. 3. STUDY OF THE GENETIC STRUCTURE OF DYSENTERY BACILLUS HYBRIDS (SEROLOGICAL PROPERTIES)
By Defense Technical Information Center
This article is from Oncotarget , volume 1 . Abstract Endogenous replicative stress could be one trigger leading to tumor initiation: indeed, activation of the DNA damage response (DDR), considered the result of replicative stress, is observed in pre-cancerous cells; moreover, in hereditary breast cancers, almost all of the genes affected relate to the DDR. The most frequently mutated gene in hereditary breast cancers, BRCA1, is essential for homologous recombination (HR), a fundamental process for maintaining genome stability that permits the reactivation of blocked replication forks. Recent studies have established links between DDR and the oncogenic kinase AKT1, which is upregulated in about 50% of sporadic breast cancers. More specifically, the activation of AKT1 shows a deficient phenotype in BRCA1 and HR, revealing molecular similarities between hereditary and sporadic breast cancers. However, these results reveal a paradox regarding the physiological role of AKT1: in non-tumor cells, AKT1 promotes cellular proliferation, but consequently endangers genome integrity during replication if HR is inhibited. Since HR could itself lead to genetic instability, we propose that, under physiological conditions, moderate activation of AKT1 does not inhibit but prevents an excess of HR. The regulation of AKT1 would represent a fine transitory system for controlling HR and maintaining genomic integrity.
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- Title: ➤ DTIC AD0618860: GENETIC RECOMBINATION IN INTESTINAL BACTERIA. 3. STUDY OF THE GENETIC STRUCTURE OF DYSENTERY BACILLUS HYBRIDS (SEROLOGICAL PROPERTIES)
- Author: ➤ Defense Technical Information Center
- Language: English
“DTIC AD0618860: GENETIC RECOMBINATION IN INTESTINAL BACTERIA. 3. STUDY OF THE GENETIC STRUCTURE OF DYSENTERY BACILLUS HYBRIDS (SEROLOGICAL PROPERTIES)” Subjects and Themes:
- Subjects: ➤ DTIC Archive - ARMY BIOLOGICAL LABS FREDERICK MD - *ENTEROBACTERIACEAE - USSR - BIOCHEMISTRY - BACILLUS - ESCHERICHIA COLI - RUSSIAN LANGUAGE - ANTIBODIES - SHIGELLA FLEXNERI - DYSENTERY - TRANSLATIONS - IMMUNE SERUMS - IMMUNITY - GENETICS - ANTIGENS
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17Genetic Recombination : Thinking About It In Phage And Fungi
By Stahl, Franklin W
This article is from Oncotarget , volume 1 . Abstract Endogenous replicative stress could be one trigger leading to tumor initiation: indeed, activation of the DNA damage response (DDR), considered the result of replicative stress, is observed in pre-cancerous cells; moreover, in hereditary breast cancers, almost all of the genes affected relate to the DDR. The most frequently mutated gene in hereditary breast cancers, BRCA1, is essential for homologous recombination (HR), a fundamental process for maintaining genome stability that permits the reactivation of blocked replication forks. Recent studies have established links between DDR and the oncogenic kinase AKT1, which is upregulated in about 50% of sporadic breast cancers. More specifically, the activation of AKT1 shows a deficient phenotype in BRCA1 and HR, revealing molecular similarities between hereditary and sporadic breast cancers. However, these results reveal a paradox regarding the physiological role of AKT1: in non-tumor cells, AKT1 promotes cellular proliferation, but consequently endangers genome integrity during replication if HR is inhibited. Since HR could itself lead to genetic instability, we propose that, under physiological conditions, moderate activation of AKT1 does not inhibit but prevents an excess of HR. The regulation of AKT1 would represent a fine transitory system for controlling HR and maintaining genomic integrity.
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- Title: ➤ Genetic Recombination : Thinking About It In Phage And Fungi
- Author: Stahl, Franklin W
- Language: English
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18Analysis Of Optimal Recombination In Genetic Algorithm For A Scheduling Problem With Setups
By A. V. Eremeev and Ju. V. Kovalenko
In this paper, we perform an experimental study of optimal recombination operator for makespan minimization problem on single machine with sequence-dependent setup times ($1|s_{vu}|C_{\max}$). The computational experiment on benchmark problems from TSPLIB library indicates practical applicability of optimal recombination in crossover operator of genetic algorithm for $1|s_{vu}|C_{\max}$.
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- Authors: A. V. EremeevJu. V. Kovalenko
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19Genetic Recombination Research Progress
In this paper, we perform an experimental study of optimal recombination operator for makespan minimization problem on single machine with sequence-dependent setup times ($1|s_{vu}|C_{\max}$). The computational experiment on benchmark problems from TSPLIB library indicates practical applicability of optimal recombination in crossover operator of genetic algorithm for $1|s_{vu}|C_{\max}$.
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- Language: English
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- Subjects: Genetic recombination - Recombination, Genetic - Research
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201991 FASEB MEETING GENETIC RECOMBINATION AND GENOME REARRANGEMENTS
Council for Tobacco Research Records; agenda; summarizes session topics, poster sessions, and workshops
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- Language: English
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21MHF1-2/CENP-S-X Performs Distinct Roles In Centromere Metabolism And Genetic Recombination.
By Bhattacharjee, Sonali, Osman, Fekret, Feeney, Laura, Lorenz, Alexander, Bryer, Claire and Whitby, Matthew C.
This article is from Open Biology , volume 3 . Abstract The histone-fold proteins Mhf1/CENP-S and Mhf2/CENP-X perform two important functions in vertebrate cells. First, they are components of the constitutive centromere-associated network, aiding kinetochore assembly and function. Second, they work with the FANCM DNA translocase to promote DNA repair. However, it has been unclear whether there is crosstalk between these roles. We show that Mhf1 and Mhf2 in fission yeast, as in vertebrates, serve a dual function, aiding DNA repair/recombination and localizing to centromeres to promote chromosome segregation. Importantly, these functions are distinct, with the former being dependent on their interaction with the FANCM orthologue Fml1 and the latter not. Together with Fml1, they play a second role in aiding chromosome segregation by processing sister chromatid junctions. However, a failure of this activity does not manifest dramatically increased levels of chromosome missegregation due to the Mus81–Eme1 endonuclease, which acts as a failsafe to resolve DNA junctions before the end of mitosis.
“MHF1-2/CENP-S-X Performs Distinct Roles In Centromere Metabolism And Genetic Recombination.” Metadata:
- Title: ➤ MHF1-2/CENP-S-X Performs Distinct Roles In Centromere Metabolism And Genetic Recombination.
- Authors: ➤ Bhattacharjee, SonaliOsman, FekretFeeney, LauraLorenz, AlexanderBryer, ClaireWhitby, Matthew C.
- Language: English
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- Internet Archive ID: pubmed-PMC3787749
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22FASEB CONFERENCE GENETIC RECOMBINATION AND GENOME REARRANGEMENTS TENTATIVE SCHEDULE JULY 9-14, 1989
Council for Tobacco Research Records; list; names session leaders and topics
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- Language: English
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23#2446 FASEB GENETIC RECOMBINATION & GENOME REARRANGE- 7/89 COPPER MTN, CO
Council for Tobacco Research Records; file folder; faseb genetic recombination folder; mar
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- Language: English
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24Replicated High-density Genetic Maps Of Two Great Tit Populations Reveal Fine-scale Genomic Departures From Sex-equal Recombination Rates.
By van Oers, K, Santure, A W, De Cauwer, I, van Bers, N EM, Crooijmans, R PMA, Sheldon, B C, Visser, M E, Slate, J and Groenen, M AM
This article is from Heredity , volume 112 . Abstract Linking variation in quantitative traits to variation in the genome is an important, but challenging task in the study of life-history evolution. Linkage maps provide a valuable tool for the unravelling of such trait−gene associations. Moreover, they give insight into recombination landscapes and between-species karyotype evolution. Here we used genotype data, generated from a 10k single-nucleotide polymorphism (SNP) chip, of over 2000 individuals to produce high-density linkage maps of the great tit (Parus major), a passerine bird that serves as a model species for ecological and evolutionary questions. We created independent maps from two distinct populations: a captive F2-cross from The Netherlands (NL) and a wild population from the United Kingdom (UK). The two maps contained 6554 SNPs in 32 linkage groups, spanning 2010 cM and 1917 cM for the NL and UK populations, respectively, and were similar in size and marker order. Subtle levels of heterochiasmy within and between chromosomes were remarkably consistent between the populations, suggesting that the local departures from sex-equal recombination rates have evolved. This key and surprising result would have been impossible to detect if only one population was mapped. A comparison with zebra finch Taeniopygia guttata, chicken Gallus gallus and the green anole lizard Anolis carolinensis genomes provided further insight into the evolution of avian karyotypes.
“Replicated High-density Genetic Maps Of Two Great Tit Populations Reveal Fine-scale Genomic Departures From Sex-equal Recombination Rates.” Metadata:
- Title: ➤ Replicated High-density Genetic Maps Of Two Great Tit Populations Reveal Fine-scale Genomic Departures From Sex-equal Recombination Rates.
- Authors: ➤ van Oers, KSanture, A WDe Cauwer, Ivan Bers, N EMCrooijmans, R PMASheldon, B CVisser, M ESlate, JGroenen, M AM
- Language: English
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- Internet Archive ID: pubmed-PMC3931172
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25High Recombination Rates And Hotspots In A Plasmodium Falciparum Genetic Cross.
By Jiang, Hongying, Li, Na, Gopalan, Vivek, Zilversmit, Martine M, Varma, Sudhir, Nagarajan, Vijayaraj, Li, Jian, Mu, Jianbing, Hayton, Karen, Henschen, Bruce, Yi, Ming, Stephens, Robert, McVean, Gilean, Awadalla, Philip, Wellems, Thomas E and Su, Xin-zhuan
This article is from Genome Biology , volume 12 . Abstract Background: The human malaria parasite Plasmodium falciparum survives pressures from the host immune system and antimalarial drugs by modifying its genome. Genetic recombination and nucleotide substitution are the two major mechanisms that the parasite employs to generate genome diversity. A better understanding of these mechanisms may provide important information for studying parasite evolution, immune evasion and drug resistance. Results: Here, we used a high-density tiling array to estimate the genetic recombination rate among 32 progeny of a P. falciparum genetic cross (7G8 × GB4). We detected 638 recombination events and constructed a high-resolution genetic map. Comparing genetic and physical maps, we obtained an overall recombination rate of 9.6 kb per centimorgan and identified 54 candidate recombination hotspots. Similar to centromeres in other organisms, the sequences of P. falciparum centromeres are found in chromosome regions largely devoid of recombination activity. Motifs enriched in hotspots were also identified, including a 12-bp G/C-rich motif with 3-bp periodicity that may interact with a protein containing 11 predicted zinc finger arrays. Conclusions: These results show that the P. falciparum genome has a high recombination rate, although it also follows the overall rule of meiosis in eukaryotes with an average of approximately one crossover per chromosome per meiosis. GC-rich repetitive motifs identified in the hotspot sequences may play a role in the high recombination rate observed. The lack of recombination activity in centromeric regions is consistent with the observations of reduced recombination near the centromeres of other organisms.
“High Recombination Rates And Hotspots In A Plasmodium Falciparum Genetic Cross.” Metadata:
- Title: ➤ High Recombination Rates And Hotspots In A Plasmodium Falciparum Genetic Cross.
- Authors: ➤ Jiang, HongyingLi, NaGopalan, VivekZilversmit, Martine MVarma, SudhirNagarajan, VijayarajLi, JianMu, JianbingHayton, KarenHenschen, BruceYi, MingStephens, RobertMcVean, GileanAwadalla, PhilipWellems, Thomas ESu, Xin-zhuan
- Language: English
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- Internet Archive ID: pubmed-PMC3218859
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26Recombination Between Poliovirus And Coxsackie A Viruses Of Species C: A Model Of Viral Genetic Plasticity And Emergence.
By Combelas, Nicolas, Holmblat, Barbara, Joffret, Marie-Line, Colbere-Garapin, Florence and Delpeyroux, Francis
This article is from Viruses , volume 3 . Abstract Genetic recombination in RNA viruses was discovered many years ago for poliovirus (PV), an enterovirus of the Picornaviridae family, and studied using PV or other picornaviruses as models. Recently, recombination was shown to be a general phenomenon between different types of enteroviruses of the same species. In particular, the interest for this mechanism of genetic plasticity was renewed with the emergence of pathogenic recombinant circulating vaccine-derived polioviruses (cVDPVs), which were implicated in poliomyelitis outbreaks in several regions of the world with insufficient vaccination coverage. Most of these cVDPVs had mosaic genomes constituted of mutated poliovaccine capsid sequences and part or all of the non-structural sequences from other human enteroviruses of species C (HEV-C), in particular coxsackie A viruses. A study in Madagascar showed that recombinant cVDPVs had been co-circulating in a small population of children with many different HEV-C types. This viral ecosystem showed a surprising and extensive biodiversity associated to several types and recombinant genotypes, indicating that intertypic genetic recombination was not only a mechanism of evolution for HEV-C, but an usual mode of genetic plasticity shaping viral diversity. Results suggested that recombination may be, in conjunction with mutations, implicated in the phenotypic diversity of enterovirus strains and in the emergence of new pathogenic strains. Nevertheless, little is known about the rules and mechanisms which govern genetic exchanges between HEV-C types, as well as about the importance of intertypic recombination in generating phenotypic variation. This review summarizes our current knowledge of the mechanisms of evolution of PV, in particular recombination events leading to the emergence of recombinant cVDPVs.
“Recombination Between Poliovirus And Coxsackie A Viruses Of Species C: A Model Of Viral Genetic Plasticity And Emergence.” Metadata:
- Title: ➤ Recombination Between Poliovirus And Coxsackie A Viruses Of Species C: A Model Of Viral Genetic Plasticity And Emergence.
- Authors: Combelas, NicolasHolmblat, BarbaraJoffret, Marie-LineColbere-Garapin, FlorenceDelpeyroux, Francis
- Language: English
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- Internet Archive ID: pubmed-PMC3185806
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27Extinction In Genetic Bit-string Model With Sexual Recombination
By D. Stauffer and S. Cebrat
We have analyzed the relations between the mutational pressure, recombination and selection pressure in the bit-string model with sexual reproduction. For specific sets of these parameters we have found three phase transitions with one phase where populations can survive. In this phase, recombination enhances the survival probability. Even if recombination is associated, to some extent, with additional mutations it could be advantageous to reproduction, indicating that the frequencies of recombinations and recombination-associated mutations can self-organize in Nature. Partitioning the diploid genome into pairs of chromosomes independently assorted during gamete production enables recombinations between groups of genes without the risk of mutations and is also advantageous for the strategy of sexual reproduction.
“Extinction In Genetic Bit-string Model With Sexual Recombination” Metadata:
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- Authors: D. StaufferS. Cebrat
- Language: English
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28GENETIC CHARACTERIZATION OF DAMAGE-INDUCED RECOMBINATION BETWEEN DISPERSED REPETITIVE SEQUENCES IN SACCHAROMYCES CEREVISIAE
Council for Tobacco Research Records; abstract; st proposes experiment demonstrating defects in specific dna repair functions; mul
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29The Recombination Of Genetic Material
Council for Tobacco Research Records; abstract; st proposes experiment demonstrating defects in specific dna repair functions; mul
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30DTIC ADA094873: Specialized Genetic Recombination Systems In Bacteria: Their Involvement In Gene Expression And Evolution,
By Defense Technical Information Center
Intermolecular exchange of a DNA segment, that is, genetic exchange or crossing over between homologous parental chromosomes resulting in the formation of a hybrid molecule, has long been recognized. This marvelous process is important in providing the breadth of phenotypic diversity seen within a single plant or animal species. Classical genetics and recent studies in molecular genetics have revealed a variety of genetic exchange systems in bacteria. These recombination systems can be divided into two broad categories: (a) generalized, and (b) specialized. In short, general recombination systems mediate genetic interchange at random points between largely homologous deoxyribonucleotide segments, whereas specialized recombination processes act in the absence of general recombination or apparent sequence homology between the interacting DNA regions. Specialized recombination systems are responsible for promoting the integration, deletion, transposition, or inversion of discrete DNA segments and can also influence the expression of nearby genes. Bacterial evolution was thought until recently to occur by a slow process involving small chromosomal alterations (i.e., mutations), environmental selection for the desirable mutations, and the accumulation of beneficial mutations through intercellular genetic exchange and generalized recombination. Mutational events which involve the addition, deletion, or substitution of only one or a few nucleotides can be called micro-evolutionary. Since the 1960's, however, a catalog of macro-evolutionary events has been amassed.
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31HYBRIDIZATION AND GENETIC RECOMBINATION OF CIRSIUM CALIFORNICUM AND C. OCCIDENTALE (ASTERACEAE: CARDUCEAE)
By Harrington Wells
Intermolecular exchange of a DNA segment, that is, genetic exchange or crossing over between homologous parental chromosomes resulting in the formation of a hybrid molecule, has long been recognized. This marvelous process is important in providing the breadth of phenotypic diversity seen within a single plant or animal species. Classical genetics and recent studies in molecular genetics have revealed a variety of genetic exchange systems in bacteria. These recombination systems can be divided into two broad categories: (a) generalized, and (b) specialized. In short, general recombination systems mediate genetic interchange at random points between largely homologous deoxyribonucleotide segments, whereas specialized recombination processes act in the absence of general recombination or apparent sequence homology between the interacting DNA regions. Specialized recombination systems are responsible for promoting the integration, deletion, transposition, or inversion of discrete DNA segments and can also influence the expression of nearby genes. Bacterial evolution was thought until recently to occur by a slow process involving small chromosomal alterations (i.e., mutations), environmental selection for the desirable mutations, and the accumulation of beneficial mutations through intercellular genetic exchange and generalized recombination. Mutational events which involve the addition, deletion, or substitution of only one or a few nucleotides can be called micro-evolutionary. Since the 1960's, however, a catalog of macro-evolutionary events has been amassed.
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32A Framework Including Recombination For Analyzing The Dynamics Of Within-Host HIV Genetic Diversity.
By Sargsyan, Ori
This article is from PLoS ONE , volume 9 . Abstract This paper presents a novel population genetic model and a computationally and statistically tractable framework for analyzing within-host HIV diversity based on serial samples of HIV DNA sequences. This model considers within-host HIV evolution during the chronic phase of infection and assumes that the HIV population is homogeneous at the beginning, corresponding to the time of seroconversion, and evolves according to the Wright-Fisher reproduction model with recombination and variable mutation rate across nucleotide sites. In addition, the population size and generation time vary over time as piecewise constant functions of time. Under this model I approximate the genealogical and mutational processes for serial samples of DNA sequences by a continuous coalescent-recombination process and an inhomogeneous Poisson process, respectively. Based on these derivations, an efficient algorithm is described for generating polymorphisms in serial samples of DNA sequences under the model including various substitution models. Extensions of the algorithm are also described for other demographic scenarios that can be more suitable for analyzing the dynamics of genetic diversity of other pathogens in vitro and in vivo. For the case of the infinite-sites model, I derive analytical formulas for the expected number of polymorphic sites in sample of DNA sequences, and apply the developed simulation and analytical methods to explore the fit of the model to HIV genetic diversity based on serial samples of HIV DNA sequences from 9 HIV-infected individuals. The results particularly show that the estimates of the ratio of recombination rate over mutation rate can vary over time between very high and low values, which can be considered as a consequence of the impact of selection forces.
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33Replication And Recombination Of Genetic Material
This article is from PLoS ONE , volume 9 . Abstract This paper presents a novel population genetic model and a computationally and statistically tractable framework for analyzing within-host HIV diversity based on serial samples of HIV DNA sequences. This model considers within-host HIV evolution during the chronic phase of infection and assumes that the HIV population is homogeneous at the beginning, corresponding to the time of seroconversion, and evolves according to the Wright-Fisher reproduction model with recombination and variable mutation rate across nucleotide sites. In addition, the population size and generation time vary over time as piecewise constant functions of time. Under this model I approximate the genealogical and mutational processes for serial samples of DNA sequences by a continuous coalescent-recombination process and an inhomogeneous Poisson process, respectively. Based on these derivations, an efficient algorithm is described for generating polymorphisms in serial samples of DNA sequences under the model including various substitution models. Extensions of the algorithm are also described for other demographic scenarios that can be more suitable for analyzing the dynamics of genetic diversity of other pathogens in vitro and in vivo. For the case of the infinite-sites model, I derive analytical formulas for the expected number of polymorphic sites in sample of DNA sequences, and apply the developed simulation and analytical methods to explore the fit of the model to HIV genetic diversity based on serial samples of HIV DNA sequences from 9 HIV-infected individuals. The results particularly show that the estimates of the ratio of recombination rate over mutation rate can vary over time between very high and low values, which can be considered as a consequence of the impact of selection forces.
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34Genetic Recombination Is Targeted Towards Gene Promoter Regions In Dogs.
By Auton, Adam, Rui Li, Ying, Kidd, Jeffrey, Oliveira, Kyle, Nadel, Julie, Holloway, J. Kim, Hayward, Jessica J., Cohen, Paula E., Greally, John M., Wang, Jun, Bustamante, Carlos D. and Boyko, Adam R.
This article is from PLoS Genetics , volume 9 . Abstract The identification of the H3K4 trimethylase, PRDM9, as the gene responsible for recombination hotspot localization has provided considerable insight into the mechanisms by which recombination is initiated in mammals. However, uniquely amongst mammals, canids appear to lack a functional version of PRDM9 and may therefore provide a model for understanding recombination that occurs in the absence of PRDM9, and thus how PRDM9 functions to shape the recombination landscape. We have constructed a fine-scale genetic map from patterns of linkage disequilibrium assessed using high-throughput sequence data from 51 free-ranging dogs, Canis lupus familiaris. While broad-scale properties of recombination appear similar to other mammalian species, our fine-scale estimates indicate that canine highly elevated recombination rates are observed in the vicinity of CpG rich regions including gene promoter regions, but show little association with H3K4 trimethylation marks identified in spermatocytes. By comparison to genomic data from the Andean fox, Lycalopex culpaeus, we show that biased gene conversion is a plausible mechanism by which the high CpG content of the dog genome could have occurred.
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- Authors: ➤ Auton, AdamRui Li, YingKidd, JeffreyOliveira, KyleNadel, JulieHolloway, J. KimHayward, Jessica J.Cohen, Paula E.Greally, John M.Wang, JunBustamante, Carlos D.Boyko, Adam R.
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35DTIC AD0842473: Genetics - On The Mechanism Of Transfer Of Genetic Material In The Course Of Recombination With Escherichia Coli K 12
By Defense Technical Information Center
The segment of chromosome of bacteria Hfr on which bears the high frequency of recombination is a segment oriented O---R, the order of transmission of characteristics being a function of their distance from the unknown origin O. The probability, for a given characteristic, of appearing among the recombinants is much weaker, the farther removed it is from origin O. There can be genetic recombination when only a small fragment of chromosome of parent Hfr is transmitted to an F- bacteria, which corresponds to the conception of Hayes (1). As to the mechanism of integration of genetic material transmitted, recombination with E. coli K 12 seems therefore that it could be aligned with transduction.
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- Subjects: ➤ DTIC Archive - Wollman, Elie L - ARMY BIOLOGICAL LABS FREDERICK MD - *ESCHERICHIA COLI - *GENETICS - PROBABILITY - CHROMOSOMES - FRANCE - TRANSLATIONS - AMINO ACIDS - BIOSYNTHESIS - HISTOLOGICAL TECHNIQUES
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36Genetic Recombination
By Wilson, John H., 1944-
The segment of chromosome of bacteria Hfr on which bears the high frequency of recombination is a segment oriented O---R, the order of transmission of characteristics being a function of their distance from the unknown origin O. The probability, for a given characteristic, of appearing among the recombinants is much weaker, the farther removed it is from origin O. There can be genetic recombination when only a small fragment of chromosome of parent Hfr is transmitted to an F- bacteria, which corresponds to the conception of Hayes (1). As to the mechanism of integration of genetic material transmitted, recombination with E. coli K 12 seems therefore that it could be aligned with transduction.
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37#2999 FASEB GENETIC RECOMBINATION & GENOMIC REARRANGEMENT-7/28-8/2/91-VT.
Council for Tobacco Research Records; file folder; faseb file
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38Genetic Polymorphisms In Homologous Recombination Repair Genes In Healthy Slovenian Population And Their Influence On DNA Damage.
By Goricar, Katja, Erculj, Nina, Zadel, Maja and Dolzan, Vita
This article is from Radiology and Oncology , volume 46 . Abstract Background: Homologous recombination (HR) repair is an important mechanism involved in repairing double-strand breaks in DNA and for maintaining genomic stability. Polymorphisms in genes coding for enzymes involved in this pathway may influence the capacity for DNA repair. The aim of this study was to select tag single nucleotide polymorphisms (SNPs) in specific genes involved in HR repair, to determine their allele frequencies in a healthy Slovenian population and their influence on DNA damage detected with comet assay. Materials and methods: In total 373 individuals were genotyped for nine tag SNPs in three genes: XRCC3 722C>T, XRCC3 -316A>G, RAD51 -98G>C, RAD51 -61G>T, RAD51 1522T>G, NBS1 553G>C, NBS1 1197A>G, NBS1 37117C>T and NBS1 3474A>C using competitive allele-specific amplification (KASPar assay). Comet assay was performed in a subgroup of 26 individuals to determine the influence of selected SNPs on DNA damage. Results: We observed that age significantly affected genotype frequencies distribution of XRCC3 -316A>G (P = 0.039) in healthy male blood donors. XRCC3 722C>T (P = 0.005), RAD51 -61G>T (P = 0.023) and NBS1 553G>C (P = 0.008) had a statistically significant influence on DNA damage. Conclusions: XRCC3 722C>T, RAD51 -61G>T and NBS1 553G>C polymorphisms significantly affect the repair of damaged DNA and may be of clinical importance as they are common in Slovenian population.
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39Genetic Diversity And Recombination Analysis Of Sweepoviruses From Brazil.
By Albuquerque, Leonardo C, Inoue-Nagata, Alice K, Pinheiro, Bruna, Resende, Renato O, Moriones, Enrique and Navas-Castillo, Jesus
This article is from Virology Journal , volume 9 . Abstract Background: Monopartite begomoviruses (genus Begomovirus, family Geminiviridae) that infect sweet potato (Ipomoea batatas) around the world are known as sweepoviruses. Because sweet potato plants are vegetatively propagated, the accumulation of viruses can become a major constraint for root production. Mixed infections of sweepovirus species and strains can lead to recombination, which may contribute to the generation of new recombinant sweepoviruses. Results: This study reports the full genome sequence of 34 sweepoviruses sampled from a sweet potato germplasm bank and commercial fields in Brazil. These sequences were compared with others from public nucleotide sequence databases to provide a comprehensive overview of the genetic diversity and patterns of genetic exchange in sweepoviruses isolated from Brazil, as well as to review the classification and nomenclature of sweepoviruses in accordance with the current guidelines proposed by the Geminiviridae Study Group of the International Committee on Taxonomy of Viruses (ICTV). Co-infections and extensive recombination events were identified in Brazilian sweepoviruses. Analysis of the recombination breakpoints detected within the sweepovirus dataset revealed that most recombination events occurred in the intergenic region (IR) and in the middle of the C1 open reading frame (ORF). Conclusions: The genetic diversity of sweepoviruses was considerably greater than previously described in Brazil. Moreover, recombination analysis revealed that a genomic exchange is responsible for the emergence of sweepovirus species and strains and provided valuable new information for understanding the diversity and evolution of sweepoviruses.
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- Authors: ➤ Albuquerque, Leonardo CInoue-Nagata, Alice KPinheiro, BrunaResende, Renato OMoriones, EnriqueNavas-Castillo, Jesus
- Language: English
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40Origins Of Sex : Three Billion Years Of Genetic Recombination
By Margulis, Lynn, 1938-2011 and Sagan, Dorion, 1959-
This article is from Virology Journal , volume 9 . Abstract Background: Monopartite begomoviruses (genus Begomovirus, family Geminiviridae) that infect sweet potato (Ipomoea batatas) around the world are known as sweepoviruses. Because sweet potato plants are vegetatively propagated, the accumulation of viruses can become a major constraint for root production. Mixed infections of sweepovirus species and strains can lead to recombination, which may contribute to the generation of new recombinant sweepoviruses. Results: This study reports the full genome sequence of 34 sweepoviruses sampled from a sweet potato germplasm bank and commercial fields in Brazil. These sequences were compared with others from public nucleotide sequence databases to provide a comprehensive overview of the genetic diversity and patterns of genetic exchange in sweepoviruses isolated from Brazil, as well as to review the classification and nomenclature of sweepoviruses in accordance with the current guidelines proposed by the Geminiviridae Study Group of the International Committee on Taxonomy of Viruses (ICTV). Co-infections and extensive recombination events were identified in Brazilian sweepoviruses. Analysis of the recombination breakpoints detected within the sweepovirus dataset revealed that most recombination events occurred in the intergenic region (IR) and in the middle of the C1 open reading frame (ORF). Conclusions: The genetic diversity of sweepoviruses was considerably greater than previously described in Brazil. Moreover, recombination analysis revealed that a genomic exchange is responsible for the emergence of sweepovirus species and strains and provided valuable new information for understanding the diversity and evolution of sweepoviruses.
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- Title: ➤ Origins Of Sex : Three Billion Years Of Genetic Recombination
- Authors: Margulis, Lynn, 1938-2011Sagan, Dorion, 1959-
- Language: English
“Origins Of Sex : Three Billion Years Of Genetic Recombination” Subjects and Themes:
- Subjects: ➤ Sex (Biology) - Genetic recombination - Recombination, Genetic - Sex - Sexualité (Biologie) - Recombinaison génétique - Geslachtelijke voortplanting - Evolutie - Paleontologie - Sexe (biologie) - 21030 sex 21030 evolution
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41High Genome Heterozygosity And Endemic Genetic Recombination In The Wheat Stripe Rust Fungus.
By Zheng, Wenming, Huang, Lili, Huang, Jinqun, Wang, Xiaojie, Chen, Xianming, Zhao, Jie, Guo, Jun, Zhuang, Hua, Qiu, Chuangzhao, Liu, Jie, Liu, Huiquan, Huang, Xueling, Pei, Guoliang, Zhan, Gangming, Tang, Chunlei, Cheng, Yulin, Liu, Minjie, Zhang, Jinshan, Zhao, Zhongtao, Zhang, Shijie, Han, Qingmei, Han, Dejun, Zhang, Hongchang, Zhao, Jing, Gao, Xiaoning, Wang, Jianfeng, Ni, Peixiang, Dong, Wei, Yang, Linfeng, Yang, Huanming, Xu, Jin-Rong, Zhang, Gengyun and Kang, Zhensheng
This article is from Nature Communications , volume 4 . Abstract Stripe rust, caused by Puccinia striiformis f. sp. tritici (Pst), is one of the most destructive diseases of wheat. Here we report a 110-Mb draft sequence of Pst isolate CY32, obtained using a ‘fosmid-to-fosmid’ strategy, to better understand its race evolution and pathogenesis. The Pst genome is highly heterozygous and contains 25,288 protein-coding genes. Compared with non-obligate fungal pathogens, Pst has a more diverse gene composition and more genes encoding secreted proteins. Re-sequencing analysis indicates significant genetic variation among six isolates collected from different continents. Approximately 35% of SNPs are in the coding sequence regions, and half of them are non-synonymous. High genetic diversity in Pst suggests that sexual reproduction has an important role in the origin of different regional races. Our results show the effectiveness of the ‘fosmid-to-fosmid’ strategy for sequencing dikaryotic genomes and the feasibility of genome analysis to understand race evolution in Pst and other obligate pathogens.
“High Genome Heterozygosity And Endemic Genetic Recombination In The Wheat Stripe Rust Fungus.” Metadata:
- Title: ➤ High Genome Heterozygosity And Endemic Genetic Recombination In The Wheat Stripe Rust Fungus.
- Authors: ➤ Zheng, WenmingHuang, LiliHuang, JinqunWang, XiaojieChen, XianmingZhao, JieGuo, JunZhuang, HuaQiu, ChuangzhaoLiu, JieLiu, HuiquanHuang, XuelingPei, GuoliangZhan, GangmingTang, ChunleiCheng, YulinLiu, MinjieZhang, JinshanZhao, ZhongtaoZhang, ShijieHan, QingmeiHan, DejunZhang, HongchangZhao, JingGao, XiaoningWang, JianfengNi, PeixiangDong, WeiYang, LinfengYang, HuanmingXu, Jin-RongZhang, GengyunKang, Zhensheng
- Language: English
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- Internet Archive ID: pubmed-PMC3826619
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42Genetic Recombination Is Associated With Intrinsic Disorder In Plant Proteomes.
By Yruela, Inmaculada and Contreras-Moreira, Bruno
This article is from BMC Genomics , volume 14 . Abstract Background: Intrinsically disordered proteins, found in all living organisms, are essential for basic cellular functions and complement the function of ordered proteins. It has been shown that protein disorder is linked to the G + C content of the genome. Furthermore, recent investigations have suggested that the evolutionary dynamics of the plant nucleus adds disordered segments to open reading frames alike, and these segments are not necessarily conserved among orthologous genes. Results: In the present work the distribution of intrinsically disordered proteins along the chromosomes of several representative plants was analyzed. The reported results support a non-random distribution of disordered proteins along the chromosomes of Arabidopsis thaliana and Oryza sativa, two model eudicot and monocot plant species, respectively. In fact, for most chromosomes positive correlations between the frequency of disordered segments of 30+ amino acids and both recombination rates and G + C content were observed. Conclusions: These analyses demonstrate that the presence of disordered segments among plant proteins is associated with the rates of genetic recombination of their encoding genes. Altogether, these findings suggest that high recombination rates, as well as chromosomal rearrangements, could induce disordered segments in proteins during evolution.
“Genetic Recombination Is Associated With Intrinsic Disorder In Plant Proteomes.” Metadata:
- Title: ➤ Genetic Recombination Is Associated With Intrinsic Disorder In Plant Proteomes.
- Authors: Yruela, InmaculadaContreras-Moreira, Bruno
- Language: English
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- Internet Archive ID: pubmed-PMC3828576
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43#3695 GENETIC RECOMBINATION AND GENOME REARRANGEMENTS
Council for Tobacco Research Records; letter; notifies of contribution for conference
“#3695 GENETIC RECOMBINATION AND GENOME REARRANGEMENTS” Metadata:
- Title: ➤ #3695 GENETIC RECOMBINATION AND GENOME REARRANGEMENTS
- Language: English
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- Internet Archive ID: tobacco_mxmv0000
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44Genetic Diversity And Recombination In Natural Populations Of The Nematode-trapping Fungus Arthrobotrys Oligospora From China.
By Zhang, Ying, Qiao, Min, Xu, Jianping, Cao, Yang, Zhang, Ke-Qin and Yu, Ze-Fen
This article is from Ecology and Evolution , volume 3 . Abstract Nematophagous fungi can trap and capture nematodes and other small invertebrates. This unique ability has made them ideal organisms from which to develop biological control agents against plant- and animal-parasitic nematodes. However, effective application of biocontrol agents in the field requires a comprehensive understanding about the ecology and population genetics of the nematophagous fungi in natural environments. Here, we genotyped 228 strains of the nematode-trapping fungus Arthrobotrys oligospora using 12 single nucleotide polymorphic markers located on eight random DNA fragments. The strains were from different ecological niches and geographical regions from China. Our analyses identified that ecological niche separations contributed significantly, whereas geographic separation contributed relatively little to the overall genetic variation in our samples of A. oligospora. Interestingly, populations from stressful environments seemed to be more variable and showed more evidence for recombination than those from benign environments at the same geographic areas. We discussed the implications of our results to the conservation and biocontrol application of A. oligospora in agriculture and forestry.
“Genetic Diversity And Recombination In Natural Populations Of The Nematode-trapping Fungus Arthrobotrys Oligospora From China.” Metadata:
- Title: ➤ Genetic Diversity And Recombination In Natural Populations Of The Nematode-trapping Fungus Arthrobotrys Oligospora From China.
- Authors: ➤ Zhang, YingQiao, MinXu, JianpingCao, YangZhang, Ke-QinYu, Ze-Fen
- Language: English
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- Internet Archive ID: pubmed-PMC3586641
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