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1Chromosomal Aberrations And Aneuploidy In Oral Potentially Malignant Lesions: Distinctive Features For Tongue.
By Castagnola, Patrizio, Malacarne, Davide, Scaruffi, Paola, Maffei, Massimo, Donadini, Alessandra, Di Nallo, Emanuela, Coco, Simona, Tonini, Gian Paolo, Pentenero, Monica, Gandolfo, Sergio and Giaretti, Walter
This article is from BMC Cancer , volume 11 . Abstract Background: The mucosae of the oral cavity are different at the histological level but appear all equally exposed to common genotoxic agents. As a result of this exposure, changes in the mucosal epithelia may develop giving rise to Oral Potentially Malignant Lesions (OPMLs), which with time may in turn progress to Oral Squamous Cell Carcinomas (OSCCs). Therefore, much effort should be devoted to identify features able to predict the likeliness of progression associated with an OPML. Such features may be helpful in assisting the clinician to establish both appropriate therapies and follow-up schedules. Here, we report a pilot study that compared the occurrence of DNA aneuploidy and chromosomal copy number aberrations (CNAs) in the OPMLs from different oral anatomical subsites. Methods: Samples from histologically diagnosed OPMLs were processed for high resolution DNA flow cytometry (hr DNA-FCM) in order to determine the relative DNA content expressed by the DNA index (DI). Additionally, array-Comparative Genomic Hybridization (a-CGH) analysis was performed on DNA obtained from diploid nuclei suspensions directly. When aneuploid nuclei were detected, these were physically separated from diploid nuclei on the base of their DI values by means of a DNA-FCM-Sorter in order to improve the a-CGH analysis. Results: Tongue OPMLs were more frequently associated with DNA aneuploidy and CNAs than OPMLs arising from all the other mucosal subsites. Conclusions: We suggest that the follow-up and the management of the patients with tongue OPMLs should receive a distinctive special attention. Clearly, this hypothesis should be validated in a prospective clinical study.
“Chromosomal Aberrations And Aneuploidy In Oral Potentially Malignant Lesions: Distinctive Features For Tongue.” Metadata:
- Title: ➤ Chromosomal Aberrations And Aneuploidy In Oral Potentially Malignant Lesions: Distinctive Features For Tongue.
- Authors: ➤ Castagnola, PatrizioMalacarne, DavideScaruffi, PaolaMaffei, MassimoDonadini, AlessandraDi Nallo, EmanuelaCoco, SimonaTonini, Gian PaoloPentenero, MonicaGandolfo, SergioGiaretti, Walter
- Language: English
Edition Identifiers:
- Internet Archive ID: pubmed-PMC3229618
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2Human Afflictions And Chromosomal Aberrations
By Turpin, Raymond, 1895-
This article is from BMC Cancer , volume 11 . Abstract Background: The mucosae of the oral cavity are different at the histological level but appear all equally exposed to common genotoxic agents. As a result of this exposure, changes in the mucosal epithelia may develop giving rise to Oral Potentially Malignant Lesions (OPMLs), which with time may in turn progress to Oral Squamous Cell Carcinomas (OSCCs). Therefore, much effort should be devoted to identify features able to predict the likeliness of progression associated with an OPML. Such features may be helpful in assisting the clinician to establish both appropriate therapies and follow-up schedules. Here, we report a pilot study that compared the occurrence of DNA aneuploidy and chromosomal copy number aberrations (CNAs) in the OPMLs from different oral anatomical subsites. Methods: Samples from histologically diagnosed OPMLs were processed for high resolution DNA flow cytometry (hr DNA-FCM) in order to determine the relative DNA content expressed by the DNA index (DI). Additionally, array-Comparative Genomic Hybridization (a-CGH) analysis was performed on DNA obtained from diploid nuclei suspensions directly. When aneuploid nuclei were detected, these were physically separated from diploid nuclei on the base of their DI values by means of a DNA-FCM-Sorter in order to improve the a-CGH analysis. Results: Tongue OPMLs were more frequently associated with DNA aneuploidy and CNAs than OPMLs arising from all the other mucosal subsites. Conclusions: We suggest that the follow-up and the management of the patients with tongue OPMLs should receive a distinctive special attention. Clearly, this hypothesis should be validated in a prospective clinical study.
“Human Afflictions And Chromosomal Aberrations” Metadata:
- Title: ➤ Human Afflictions And Chromosomal Aberrations
- Author: Turpin, Raymond, 1895-
- Language: English
“Human Afflictions And Chromosomal Aberrations” Subjects and Themes:
- Subjects: ➤ Human chromosome abnormalities - Karyotypes - Chromosome abnormalities - Chromosome Aberrations - Karyotyping - Chromosomes humains -- Anomalies - Caryotypes - Aberrations chromosomiques - Chromosom - Mensch
Edition Identifiers:
- Internet Archive ID: humanafflictions0000turp_v9y7
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3NASA Technical Reports Server (NTRS) 20110012712: The Distribution Of Chromosomal Aberrations In Human Cells Predicted By A Generalized Time-Dependent Model Of Radiation-Induced Formation Of Aberrations
By NASA Technical Reports Server (NTRS)
New experimental data show how chromosomal aberrations for low- and high-LET radiation are dependent on DSB repair deficiencies in wild-type, AT and NBS cells. We simulated the development of chromosomal aberrations in these cells lines in a stochastic track-structure-dependent model, in which different cells have different kinetics of DSB repair. We updated a previously formulated model of chromosomal aberrations, which was based on a stochastic Monte Carlo approach, to consider the time-dependence of DSB rejoining. The previous version of the model had an assumption that all DSBs would rejoin, and therefore we called it a time-independent model. The chromosomal-aberrations model takes into account the DNA and track structure for low- and high-LET radiations, and provides an explanation and prediction of the statistics of rare and more complex aberrations. We compared the program-simulated kinetics of DSB rejoining to the experimentally-derived bimodal exponential curves of the DSB kinetics. We scored the formation of translocations, dicentrics, acentric and centric rings, deletions, and inversions. The fraction of DSBs participating in aberrations was studied in relation to the rejoining time. Comparisons of simulated dose dependence for simple aberrations to the experimental dose-dependence for HF19, AT and NBS cells will be made.
“NASA Technical Reports Server (NTRS) 20110012712: The Distribution Of Chromosomal Aberrations In Human Cells Predicted By A Generalized Time-Dependent Model Of Radiation-Induced Formation Of Aberrations” Metadata:
- Title: ➤ NASA Technical Reports Server (NTRS) 20110012712: The Distribution Of Chromosomal Aberrations In Human Cells Predicted By A Generalized Time-Dependent Model Of Radiation-Induced Formation Of Aberrations
- Author: ➤ NASA Technical Reports Server (NTRS)
- Language: English
“NASA Technical Reports Server (NTRS) 20110012712: The Distribution Of Chromosomal Aberrations In Human Cells Predicted By A Generalized Time-Dependent Model Of Radiation-Induced Formation Of Aberrations” Subjects and Themes:
- Subjects: ➤ NASA Technical Reports Server (NTRS) - CHROMOSOME ABERRATIONS - DEOXYRIBONUCLEIC ACID - CELLS (BIOLOGY) - RADIATION EFFECTS - RADIATION DOSAGE - INVERSIONS - MUTATIONS - CHROMOSOMES - TIME DEPENDENCE - STOCHASTIC PROCESSES - Ponomarev, Artem L. - George, K. - Cucinotta, F. A.
Edition Identifiers:
- Internet Archive ID: NASA_NTRS_Archive_20110012712
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4A Study Of Chromosomal Aberrations And Sisterchromatid Exchanges Induced By Agricul Tural Germicide Dimieling
By Wei-Shun, He, Al., Liu Ai-Hua Et, Hui-Xiang, Zhu and Gui-Qing, Wang
New experimental data show how chromosomal aberrations for low- and high-LET radiation are dependent on DSB repair deficiencies in wild-type, AT and NBS cells. We simulated the development of chromosomal aberrations in these cells lines in a stochastic track-structure-dependent model, in which different cells have different kinetics of DSB repair. We updated a previously formulated model of chromosomal aberrations, which was based on a stochastic Monte Carlo approach, to consider the time-dependence of DSB rejoining. The previous version of the model had an assumption that all DSBs would rejoin, and therefore we called it a time-independent model. The chromosomal-aberrations model takes into account the DNA and track structure for low- and high-LET radiations, and provides an explanation and prediction of the statistics of rare and more complex aberrations. We compared the program-simulated kinetics of DSB rejoining to the experimentally-derived bimodal exponential curves of the DSB kinetics. We scored the formation of translocations, dicentrics, acentric and centric rings, deletions, and inversions. The fraction of DSBs participating in aberrations was studied in relation to the rejoining time. Comparisons of simulated dose dependence for simple aberrations to the experimental dose-dependence for HF19, AT and NBS cells will be made.
“A Study Of Chromosomal Aberrations And Sisterchromatid Exchanges Induced By Agricul Tural Germicide Dimieling” Metadata:
- Title: ➤ A Study Of Chromosomal Aberrations And Sisterchromatid Exchanges Induced By Agricul Tural Germicide Dimieling
- Authors: Wei-Shun, HeAl., Liu Ai-Hua EtHui-Xiang, ZhuGui-Qing, Wang
Edition Identifiers:
- Internet Archive ID: ➤ zoological-research-2095-8137-1538
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5NASA Technical Reports Server (NTRS) 20110014117: Analysis Of Terminal Deletions Using A Generalized Time-Dependent Model Of Radiation-Induced Formation Of Chromosomal Aberrations
By NASA Technical Reports Server (NTRS)
We have developed a model that can simulate different types of radiation induced chromosomal aberrations (CA's) and can provide predictions on the frequency and size of chromosomes with terminal deletions. Chromosomes with terminal deletions lack telomeres and this can elicit sister chromatid unions and the prolonged breakage/fusion/bridge (B/F/B) cycles that have been observed in mammalian tumors. The loss of a single telomere has been shown to cause extensive genomic instability through the B/F/B cycle process. Our model uses a stochastic process of DNA broken end joining, in which a realistic spectrum of CA's is created from improperly joined DNA free ends formed by DNA double strand breaks (DSBs). The distribution of the DNA free ends is given by a mechanistic model that takes into account the chromatin structure and track structure for high-LET radiation. The model allows for DSB clustering from high-LET radiation and simulates the formation of CA's in stages that correspond to the actual time after radiation exposure. The time scale for CA formation is derived from experimental data on DSB repair kinetics. At any given time a nucleus may have intact chromosomes, CA's, and/or unrepaired fragments, some of which are defined as terminal deletions, if they are capped by one telomere. The model produces a spectrum of terminal deletions with their corresponding probabilities and size distributions for different heavy ions exposures for the first division after exposure. This data provides valuable information because there is limited experimental data available in the literature on the on the actual size of terminal deletions. We compare our model output to the available experimental data and make a reasonable extrapolation on the number of chromosomes lacking telomeres in human lymphocytes exposed to heavy ions. This model generates data which may lead to predictions on the rate of genomic instability in cells after exposure to high charge and energy nuclei affecting astronauts during space missions.
“NASA Technical Reports Server (NTRS) 20110014117: Analysis Of Terminal Deletions Using A Generalized Time-Dependent Model Of Radiation-Induced Formation Of Chromosomal Aberrations” Metadata:
- Title: ➤ NASA Technical Reports Server (NTRS) 20110014117: Analysis Of Terminal Deletions Using A Generalized Time-Dependent Model Of Radiation-Induced Formation Of Chromosomal Aberrations
- Author: ➤ NASA Technical Reports Server (NTRS)
- Language: English
“NASA Technical Reports Server (NTRS) 20110014117: Analysis Of Terminal Deletions Using A Generalized Time-Dependent Model Of Radiation-Induced Formation Of Chromosomal Aberrations” Subjects and Themes:
- Subjects: ➤ NASA Technical Reports Server (NTRS) - CHROMOSOME ABERRATIONS - TIME DEPENDENCE - DEOXYRIBONUCLEIC ACID - GENOME - RADIATION DOSAGE - MATHEMATICAL MODELS - TELOMERES - MAMMALS - TUMORS - STOCHASTIC PROCESSES - EXTRAPOLATION - HEAVY IONS - LYMPHOCYTES - PROBABILITY THEORY - Ponomarev, Artem L. - George, K. - Cucinotta, Francis A.
Edition Identifiers:
- Internet Archive ID: NASA_NTRS_Archive_20110014117
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6Chromosomal Aberrations In Human Lymphocytes And Fibroblasts After Exposure To Very Low Doses Of High-LET Radiation.
By Hada, Megumi, George, Kerry, Chappell, Lori and Cucinotta, Francis A.
This article is from Journal of Radiation Research , volume 55 . Abstract Purpose: The relationship between biological effects and low doses of radiation is still uncertain, especially for high-LET radiation exposures. Estimates of risk from exposure to low doses and low dose rates are often extrapolated from the Japanese atomic bomb survivor data using either linear or linear-quadratic models fitted to dose–response data. In this study, we determined the dose–response for chromosome damage after exposure to very low doses of high-LET radiation and assessed the radiation qualities of Fe, Si and Oxygen ions.Materials and methods: Chromosomal aberrations (CA) were measured in human peripheral blood lymphocytes and normal skin fibroblasts after exposure to very low doses (0.01–0.20 Gy) of 77-MeV/u oxygen (LET = 55 keV/µm), 170-MeV/u 28Si (LET = 99 keV/µm), or 56Fe ions with energies of 600- or 450-MeV/u (LET = 180 or 195 keV/µm). These exposures included doses that, on average, produce fewer than one in five direct ion traversals per cell nucleus. Chromosomes were analyzed using the whole-chromosome fluorescence in situ hybridization (FISH) technique during the first cell division after irradiation, and CA were identified as either simple exchanges (translocations and dicentrics) or complex exchanges (involving more than two breaks in two or more chromosomes). The frequencies of CA in the painted chromosome(s) were evaluated as the ratio between aberrations scored and total cells analyzed. The dose–response for simple exchanges was assessed using a generalized linear model assuming binomial errors per number of chromosomes scored. The model coefficients were extrapolated to whole-genome equivalents. The linear dose–response denoted as the targete effects (TE) model considered the mean number of radiation tracks per cell. Two different non-targeted effect (NTE) models, P = P0 + αT + κ × I (NTE1), and P = P0 + αT (1 − e−T) + κe−T × I (NTE2), were compared with the simple linear model, P = P0 + αT. Akaike information criteria (AIC) and Bayes information criteria (BIC) were used to compare TE and NTE models for fitting chromosome aberrations in low dose range.Results: Doses that on average produce more than one ion traversal per cell nucleus showed a linear dose–response for CA in both lymphocytes and fibroblasts. However, for doses that produce fewer than one tracks per cell in fibroblasts, O, Si and Fe particles showed a dose-independent response for CA that was significantly elevated relative to background frequencies. For fibroblasts the NTE model 2, P = P0 + αT (1 − e−T) + κe−T × I, showed improved fit to CA in low dose range compared with TE model or NTE1 model. For lymphocytes, tests of the various models were less clear with TE model optimal for Si and Fe while the NTE2 model optimal for O particles. When low-dose exposures were fractionated with 2-h intervals, increased frequencies of both simple and complex exchanges were observed. Nitric oxide scavenger reduced CA induced by low doses of high-LET irradiation. Inhibition of transforming growth factor-β receptor-1 reduced the frequency of simple exchanges.Conclusions: The results show a non-linear dose–response for CA in fibroblasts after very low doses of high-LET exposure. Possible explanations for this could involve non-targeted effects due to aberrant cell signaling [ 1], perhaps involving nitric oxide and TGF-β, or could be due to delta-ray dose fluctuations [ 2] where CA are induced in cells that receive a significant dose from delta-rays emanating from the multiple ion tracks that do not directly traverse cell nuclei.
“Chromosomal Aberrations In Human Lymphocytes And Fibroblasts After Exposure To Very Low Doses Of High-LET Radiation.” Metadata:
- Title: ➤ Chromosomal Aberrations In Human Lymphocytes And Fibroblasts After Exposure To Very Low Doses Of High-LET Radiation.
- Authors: Hada, MegumiGeorge, KerryChappell, LoriCucinotta, Francis A.
- Language: English
Edition Identifiers:
- Internet Archive ID: pubmed-PMC3941494
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7Preliminary Observation On Chromosomal Aberrations Of Bone Marrow Cells Of Rats Induced By Yunnan Tin Ore Powder
By Wei-Shun, He, Al., Liu Ai-Hua Et, Cui-Fen, Zhao and Al., Sun La-Hua Et
This article is from Journal of Radiation Research , volume 55 . Abstract Purpose: The relationship between biological effects and low doses of radiation is still uncertain, especially for high-LET radiation exposures. Estimates of risk from exposure to low doses and low dose rates are often extrapolated from the Japanese atomic bomb survivor data using either linear or linear-quadratic models fitted to dose–response data. In this study, we determined the dose–response for chromosome damage after exposure to very low doses of high-LET radiation and assessed the radiation qualities of Fe, Si and Oxygen ions.Materials and methods: Chromosomal aberrations (CA) were measured in human peripheral blood lymphocytes and normal skin fibroblasts after exposure to very low doses (0.01–0.20 Gy) of 77-MeV/u oxygen (LET = 55 keV/µm), 170-MeV/u 28Si (LET = 99 keV/µm), or 56Fe ions with energies of 600- or 450-MeV/u (LET = 180 or 195 keV/µm). These exposures included doses that, on average, produce fewer than one in five direct ion traversals per cell nucleus. Chromosomes were analyzed using the whole-chromosome fluorescence in situ hybridization (FISH) technique during the first cell division after irradiation, and CA were identified as either simple exchanges (translocations and dicentrics) or complex exchanges (involving more than two breaks in two or more chromosomes). The frequencies of CA in the painted chromosome(s) were evaluated as the ratio between aberrations scored and total cells analyzed. The dose–response for simple exchanges was assessed using a generalized linear model assuming binomial errors per number of chromosomes scored. The model coefficients were extrapolated to whole-genome equivalents. The linear dose–response denoted as the targete effects (TE) model considered the mean number of radiation tracks per cell. Two different non-targeted effect (NTE) models, P = P0 + αT + κ × I (NTE1), and P = P0 + αT (1 − e−T) + κe−T × I (NTE2), were compared with the simple linear model, P = P0 + αT. Akaike information criteria (AIC) and Bayes information criteria (BIC) were used to compare TE and NTE models for fitting chromosome aberrations in low dose range.Results: Doses that on average produce more than one ion traversal per cell nucleus showed a linear dose–response for CA in both lymphocytes and fibroblasts. However, for doses that produce fewer than one tracks per cell in fibroblasts, O, Si and Fe particles showed a dose-independent response for CA that was significantly elevated relative to background frequencies. For fibroblasts the NTE model 2, P = P0 + αT (1 − e−T) + κe−T × I, showed improved fit to CA in low dose range compared with TE model or NTE1 model. For lymphocytes, tests of the various models were less clear with TE model optimal for Si and Fe while the NTE2 model optimal for O particles. When low-dose exposures were fractionated with 2-h intervals, increased frequencies of both simple and complex exchanges were observed. Nitric oxide scavenger reduced CA induced by low doses of high-LET irradiation. Inhibition of transforming growth factor-β receptor-1 reduced the frequency of simple exchanges.Conclusions: The results show a non-linear dose–response for CA in fibroblasts after very low doses of high-LET exposure. Possible explanations for this could involve non-targeted effects due to aberrant cell signaling [ 1], perhaps involving nitric oxide and TGF-β, or could be due to delta-ray dose fluctuations [ 2] where CA are induced in cells that receive a significant dose from delta-rays emanating from the multiple ion tracks that do not directly traverse cell nuclei.
“Preliminary Observation On Chromosomal Aberrations Of Bone Marrow Cells Of Rats Induced By Yunnan Tin Ore Powder” Metadata:
- Title: ➤ Preliminary Observation On Chromosomal Aberrations Of Bone Marrow Cells Of Rats Induced By Yunnan Tin Ore Powder
- Authors: Wei-Shun, HeAl., Liu Ai-Hua EtCui-Fen, ZhaoAl., Sun La-Hua Et
Edition Identifiers:
- Internet Archive ID: ➤ zoological-research-2095-8137-1206
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8The Human Genetic Mutant Cell Repository : List Of Genetic Variants, Chromosomal Aberrations And Normal Cell Cultures Submitted To The Repository
By Institute for Medical Research (Camden, N.J.) and United States. National Institute for General Medical Sciences
Includes bibliographical references and index
“The Human Genetic Mutant Cell Repository : List Of Genetic Variants, Chromosomal Aberrations And Normal Cell Cultures Submitted To The Repository” Metadata:
- Title: ➤ The Human Genetic Mutant Cell Repository : List Of Genetic Variants, Chromosomal Aberrations And Normal Cell Cultures Submitted To The Repository
- Authors: ➤ Institute for Medical Research (Camden, N.J.)United States. National Institute for General Medical Sciences
- Language: English
Edition Identifiers:
- Internet Archive ID: humangeneticmuta04inst
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9NASA Technical Reports Server (NTRS) 20140004421: Simulations Of DSB Yields And Radiation-induced Chromosomal Aberrations In Human Cells Based On The Stochastic Track Structure IIduced By HZE Particles
By NASA Technical Reports Server (NTRS)
The formation of double-strand breaks (DSBs) and chromosomal aberrations (CAs) is of great importance in radiation research and, specifically, in space applications. We are presenting a new particle track and DNA damage model, in which the particle stochastic track structure is combined with the random walk (RW) structure of chromosomes in a cell nucleus. The motivation for this effort stems from the fact that the model with the RW chromosomes, NASARTI (NASA radiation track image) previously relied on amorphous track structure, while the stochastic track structure model RITRACKS (Relativistic Ion Tracks) was focused on more microscopic targets than the entire genome. We have combined chromosomes simulated by RWs with stochastic track structure, which uses nanoscopic dose calculations performed with the Monte-Carlo simulation by RITRACKS in a voxelized space. The new simulations produce the number of DSBs as function of dose and particle fluence for high-energy particles, including iron, carbon and protons, using voxels of 20 nm dimension. The combined model also calculates yields of radiation-induced CAs and unrejoined chromosome breaks in normal and repair deficient cells. The joined computational model is calibrated using the relative frequencies and distributions of chromosomal aberrations reported in the literature. The model considers fractionated deposition of energy to approximate dose rates of the space flight environment. The joined model also predicts of the yields and sizes of translocations, dicentrics, rings, and more complex-type aberrations formed in the G0/G1 cell cycle phase during the first cell division after irradiation. We found that the main advantage of the joined model is our ability to simulate small doses: 0.05-0.5 Gy. At such low doses, the stochastic track structure proved to be indispensable, as the action of individual delta-rays becomes more important.
“NASA Technical Reports Server (NTRS) 20140004421: Simulations Of DSB Yields And Radiation-induced Chromosomal Aberrations In Human Cells Based On The Stochastic Track Structure IIduced By HZE Particles” Metadata:
- Title: ➤ NASA Technical Reports Server (NTRS) 20140004421: Simulations Of DSB Yields And Radiation-induced Chromosomal Aberrations In Human Cells Based On The Stochastic Track Structure IIduced By HZE Particles
- Author: ➤ NASA Technical Reports Server (NTRS)
- Language: English
“NASA Technical Reports Server (NTRS) 20140004421: Simulations Of DSB Yields And Radiation-induced Chromosomal Aberrations In Human Cells Based On The Stochastic Track Structure IIduced By HZE Particles” Subjects and Themes:
- Subjects: ➤ NASA Technical Reports Server (NTRS) - CHROMOSOME ABERRATIONS - DEOXYRIBONUCLEIC ACID - DAMAGE - RADIATION DOSAGE - STOCHASTIC PROCESSES - RANDOM WALK - IRON - CARBON - PROTONS - MATHEMATICAL MODELS - TARGETS - Ponomarev, Artem - Plante, Ianik - George, Kerry - Wu, Honglu
Edition Identifiers:
- Internet Archive ID: NASA_NTRS_Archive_20140004421
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The book is available for download in "texts" format, the size of the file-s is: 0.62 Mbs, the file-s for this book were downloaded 57 times, the file-s went public at Wed Nov 16 2016.
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10NASA Technical Reports Server (NTRS) 20110012711: Space Radiation Effects On Human Cells: Modeling DNA Breakage, DNA Damage Foci Distribution, Chromosomal Aberrations And Tissue Effects
By NASA Technical Reports Server (NTRS)
Future long-tem space travel will face challenges from radiation concerns as the space environment poses health risk to humans in space from radiations with high biological efficiency and adverse post-flight long-term effects. Solar particles events may dramatically affect the crew performance, while Galactic Cosmic Rays will induce a chronic exposure to high-linear-energy-transfer (LET) particles. These types of radiation, not present on the ground level, can increase the probability of a fatal cancer later in astronaut life. No feasible shielding is possible from radiation in space, especially for the heavy ion component, as suggested solutions will require a dramatic increase in the mass of the mission. Our research group focuses on fundamental research and strategic analysis leading to better shielding design and to better understanding of the biological mechanisms of radiation damage. We present our recent effort to model DNA damage and tissue damage using computational models based on the physics of heavy ion radiation, DNA structure and DNA damage and repair in human cells. Our particular area of expertise include the clustered DNA damage from high-LET radiation, the visualization of DSBs (DNA double strand breaks) via DNA damage foci, image analysis and the statistics of the foci for different experimental situations, chromosomal aberration formation through DSB misrepair, the kinetics of DSB repair leading to a model-derived spectrum of chromosomal aberrations, and, finally, the simulation of human tissue and the pattern of apoptotic cell damage. This compendium of theoretical and experimental data sheds light on the complex nature of radiation interacting with human DNA, cells and tissues, which can lead to mutagenesis and carcinogenesis later in human life after the space mission.
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- Title: ➤ NASA Technical Reports Server (NTRS) 20110012711: Space Radiation Effects On Human Cells: Modeling DNA Breakage, DNA Damage Foci Distribution, Chromosomal Aberrations And Tissue Effects
- Author: ➤ NASA Technical Reports Server (NTRS)
- Language: English
“NASA Technical Reports Server (NTRS) 20110012711: Space Radiation Effects On Human Cells: Modeling DNA Breakage, DNA Damage Foci Distribution, Chromosomal Aberrations And Tissue Effects” Subjects and Themes:
- Subjects: ➤ NASA Technical Reports Server (NTRS) - RADIATION EFFECTS - GALACTIC COSMIC RAYS - ASTRONAUTS - CHROMOSOME ABERRATIONS - DEOXYRIBONUCLEIC ACID - HUMAN PERFORMANCE - MUTAGENESIS - PROBABILITY THEORY - RADIATION DOSAGE - RADIATION DAMAGE - SPACE MISSIONS - SPACECREWS - SHIELDING - RISK - Ponomarev, A. L. - Huff, J. L. - Cucinotta, F. A.
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- Internet Archive ID: NASA_NTRS_Archive_20110012711
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11RESEARCH ABSTRACT TREATMENT OF OVERDISPERSED, AGGREGATED DATA ON HUMAN CHROMOSOMAL ABERRATIONS
Philip Morris Records; abstract; conf, confidential; extr, extra
“RESEARCH ABSTRACT TREATMENT OF OVERDISPERSED, AGGREGATED DATA ON HUMAN CHROMOSOMAL ABERRATIONS” Metadata:
- Title: ➤ RESEARCH ABSTRACT TREATMENT OF OVERDISPERSED, AGGREGATED DATA ON HUMAN CHROMOSOMAL ABERRATIONS
- Language: English
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12NASA Technical Reports Server (NTRS) 20140003799: Simulations Of DSB Yields And Radiation-induced Chromosomal Aberrations In Human Cells Based On The Stochastic Track Structure Induced By HZE Particles
By NASA Technical Reports Server (NTRS)
The formation of double-strand breaks (DSBs) and chromosomal aberrations (CAs) is of great importance in radiation research and, specifically, in space applications. We are presenting a new particle track and DNA damage model, in which the particle stochastic track structure is combined with the random walk (RW) structure of chromosomes in a cell nucleus. The motivation for this effort stems from the fact that the model with the RW chromosomes, NASARTI (NASA radiation track image) previously relied on amorphous track structure, while the stochastic track structure model RITRACKS (Relativistic Ion Tracks) was focused on more microscopic targets than the entire genome. We have combined chromosomes simulated by RWs with stochastic track structure, which uses nanoscopic dose calculations performed with the Monte-Carlo simulation by RITRACKS in a voxelized space. The new simulations produce the number of DSBs as function of dose and particle fluence for high-energy particles, including iron, carbon and protons, using voxels of 20 nm dimension. The combined model also calculates yields of radiation-induced CAs and unrejoined chromosome breaks in normal and repair deficient cells. The joined computational model is calibrated using the relative frequencies and distributions of chromosomal aberrations reported in the literature. The model considers fractionated deposition of energy to approximate dose rates of the space flight environment. The joined model also predicts of the yields and sizes of translocations, dicentrics, rings, and more complex-type aberrations formed in the G0/G1 cell cycle phase during the first cell division after irradiation. We found that the main advantage of the joined model is our ability to simulate small doses: 0.05-0.5 Gy. At such low doses, the stochastic track structure proved to be indispensable, as the action of individual delta-rays becomes more important.
“NASA Technical Reports Server (NTRS) 20140003799: Simulations Of DSB Yields And Radiation-induced Chromosomal Aberrations In Human Cells Based On The Stochastic Track Structure Induced By HZE Particles” Metadata:
- Title: ➤ NASA Technical Reports Server (NTRS) 20140003799: Simulations Of DSB Yields And Radiation-induced Chromosomal Aberrations In Human Cells Based On The Stochastic Track Structure Induced By HZE Particles
- Author: ➤ NASA Technical Reports Server (NTRS)
- Language: English
“NASA Technical Reports Server (NTRS) 20140003799: Simulations Of DSB Yields And Radiation-induced Chromosomal Aberrations In Human Cells Based On The Stochastic Track Structure Induced By HZE Particles” Subjects and Themes:
- Subjects: ➤ NASA Technical Reports Server (NTRS) - COMPUTERIZED SIMULATION - ELECTROMAGNETIC RADIATION - CHROMOSOME ABERRATIONS - CHROMOSOMES - RADIATION DAMAGE - CELL DIVISION - RADIATION DOSAGE - PARTICLE TRACKS - STOCHASTIC PROCESSES - Ponomarev, Artem - Plante, Ianik - George, Kerry - Wu, Honglu
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13NASA Technical Reports Server (NTRS) 20110014175: Chromosomal Aberrations In Normal And AT Cells Exposed To High Dose Of Low Dose Rate Irradiation
By NASA Technical Reports Server (NTRS)
Ataxia telangiectasia (A-T) is a human autosomally recessive syndrome characterized by cerebellar ataxia, telangiectases, immune dysfunction, and genomic instability, and high rate of cancer incidence. A-T cell lines are abnormally sensitive to agents that induce DNA double strand breaks, including ionizing radiation. The diverse clinical features in individuals affected by A-T and the complex cellular phenotypes are all linked to the functional inactivation of a single gene (AT mutated). It is well known that cells deficient in ATM show increased yields of both simple and complex chromosomal aberrations after high-dose-rate irradiation, but, less is known on how cells respond to low-dose-rate irradiation. It has been shown that AT cells contain a large number of unrejoined breaks after both low-dose-rate irradiation and high-dose-rate irradiation, however sensitivity for chromosomal aberrations at low-dose-rate are less often studied. To study how AT cells respond to low-dose-rate irradiation, we exposed confluent normal and AT fibroblast cells to up to 3 Gy of gamma-irradiation at a dose rate of 0.5 Gy/day and analyzed chromosomal aberrations in G0 using fusion PCC (Premature Chromosomal Condensation) technique. Giemsa staining showed that 1 Gy induces around 0.36 unrejoined fragments per cell in normal cells and around 1.35 fragments in AT cells, whereas 3Gy induces around 0.65 fragments in normal cells and around 3.3 fragments in AT cells. This result indicates that AT cells can rejoin breaks less effectively in G0 phase of the cell cycle? compared to normal cells. We also analyzed chromosomal exchanges in normal and AT cells after exposure to 3 Gy of low-dose-rate rays using a combination of G0 PCC and FISH techniques. Misrejoining was detected in the AT cells only? When cells irradiated with 3 Gy were subcultured and G2 chromosomal aberrations were analyzed using calyculin-A induced PCC technique, the yield of unrejoined breaks decreased in both normal and AT cells and misrejoined breaks increased in both cell lines. The present study suggests that AT cells begin to rejoin breaks when a certain number of breaks are accumulated and an increased number of exchanges were observed in G0 AT cells, which is similar situation after high-dose-rate irradiation.
“NASA Technical Reports Server (NTRS) 20110014175: Chromosomal Aberrations In Normal And AT Cells Exposed To High Dose Of Low Dose Rate Irradiation” Metadata:
- Title: ➤ NASA Technical Reports Server (NTRS) 20110014175: Chromosomal Aberrations In Normal And AT Cells Exposed To High Dose Of Low Dose Rate Irradiation
- Author: ➤ NASA Technical Reports Server (NTRS)
- Language: English
“NASA Technical Reports Server (NTRS) 20110014175: Chromosomal Aberrations In Normal And AT Cells Exposed To High Dose Of Low Dose Rate Irradiation” Subjects and Themes:
- Subjects: ➤ NASA Technical Reports Server (NTRS) - ATAXIA - CHROMOSOME ABERRATIONS - CELLS (BIOLOGY) - GENETICS - IMMUNE SYSTEMS - DOSAGE - IRRADIATION - FIBROBLASTS - MUTATIONS - EXPOSURE - CANCER - DEOXYRIBONUCLEIC ACID - Kawata, T. - Shigematsu, N. - Kawaguchi, O. - Liu, C. - Furusawa, Y. - Hirayama, R. - George, K. - Cucinotta, F.
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- Internet Archive ID: NASA_NTRS_Archive_20110014175
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14Role Of P53 Codon 72 Polymorphism In Chromosomal Aberrations And Mitotic Index In Patients With Chronic Hepatitis B.
By Akbas, H., Yalcin, K., Isi, H., Tekes, S., Atay, A.E., Akkus, Z. and Budak, T.
This article is from Brazilian Journal of Medical and Biological Research , volume 45 . Abstract Polymorphisms of the p53 gene, which participates in DNA repair, can affect the functioning of the p53 protein. The Arg and Pro variants in p53 codon 72 were shown to have different regulation properties of p53-dependent DNA repair target genes that can affect various levels of cytogenetic aberrations in chronic hepatitis B patients. The present study aimed to examine the frequency of chromosomal aberrations and the mitotic index in patients with chronic hepatitis B and their possible association with p53 gene exon 4 codon 72 Arg72Pro (Ex4+119 G>C; rs1042522) polymorphism. Fifty-eight patients with chronic hepatitis B and 30 healthy individuals were genotyped in terms of the p53 gene codon 72 Arg72Pro polymorphism by PCR-RFLP. A 72-h cell culture was performed on the same individuals and evaluated in terms of chromosomal aberrations and mitotic index. A high frequency of chromosomal aberrations and low mitotic index were detected in the patient group compared to the control group. A higher frequency of chromosomal aberrations was detected in both the patient and the control groups with a homozygous proline genotype (13 patients, 3 control subjects) compared to patients and controls with other genotypes [Arg/Pro (38 patients, 20 control subjects) and Arg/Arg (7 patients, 7 control subjects)]. We observed an increased frequency of cytogenetic aberrations in patients with chronic hepatitis B. In addition, a higher frequency of cytogenetic aberrations was observed in p53 variants having the homozygous proline genotype compared to variants having other genotypes both in patients and healthy individuals.
“Role Of P53 Codon 72 Polymorphism In Chromosomal Aberrations And Mitotic Index In Patients With Chronic Hepatitis B.” Metadata:
- Title: ➤ Role Of P53 Codon 72 Polymorphism In Chromosomal Aberrations And Mitotic Index In Patients With Chronic Hepatitis B.
- Authors: ➤ Akbas, H.Yalcin, K.Isi, H.Tekes, S.Atay, A.E.Akkus, Z.Budak, T.
- Language: English
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- Internet Archive ID: pubmed-PMC3854153
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15Complex Chromosomal Aberrations In CLL Patients - Case Report
By Milanowski, Janusz. Redaktor naukowy
artykuł w: Annales Universitatis Mariae Curie-Skłodowska. Sectio D, Medicina, Supplementum. Supl. 9 (2002), s. 193-198 ; tytuł równoległy w języku polskim: Złożone zaburzenia chromosomowe u chorych z PBL-B - opis przypadku ; streszczenie w języku polskim
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- Title: ➤ Complex Chromosomal Aberrations In CLL Patients - Case Report
- Author: ➤ Milanowski, Janusz. Redaktor naukowy
- Language: eng ; pol
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- Internet Archive ID: ➤ dlibra.umcs.lublin.pl.czas4054_57_2002_supl_9_24_44663
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16APPLICATION FOR RESEARCH CONTRACT TREATMENT OF OVERDISPERSED, AGGREGATED DATA ON HUMAN CHROMOSOMAL ABERRATIONS.
Philip Morris Records; bibliography; budget; budget review; form; research proposal, scientific; resume; conf, confidential; pare, parent
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- Language: English
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17NASA Technical Reports Server (NTRS) 20170001349: Dependence Of Early And Late Chromosomal Aberrations On Radiation Quality And Cell Types
By NASA Technical Reports Server (NTRS)
Exposure to radiation induces different types of DNA damage, increases mutation and chromosome aberration rates, and increases cellular transformation in vitro and in vivo. The susceptibility of cells to radiation depends on genetic background and growth condition of cells, as well as types of radiation. Mammalian cells of different tissue types and with different genetic background are known to have different survival rate and different mutation rate after cytogenetic insults. Genomic instability, induced by various genetic, metabolic, and environmental factors including radiation, is the driving force of tumorigenesis. Accurate measurements of the relative biological effectiveness (RBE) is important for estimating radiation-related risks. To further understand genomic instability induced by charged particles and their RBE, we exposed human lymphocytes ex vivo, human fibroblast AG1522, human mammary epithelial cells (CH184B5F5/M10), and bone marrow cells isolated from CBA/CaH(CBA) and C57BL/6 (C57) mice to high energy protons and Fe ions. Normal human fibroblasts AG1522 have apparently normal DNA damage response and repair mechanisms, while mammary epithelial cells (M10) are deficient in the repair of DNA DSBs. Mouse strain CBA is radio-sensitive while C57 is radio-resistant. Metaphase chromosomes at different cell divisions after radiation exposure were collected and chromosome aberrations were analyzed as RBE for different cell lines exposed to different radiations at various time points up to one month post irradiation.
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- Title: ➤ NASA Technical Reports Server (NTRS) 20170001349: Dependence Of Early And Late Chromosomal Aberrations On Radiation Quality And Cell Types
- Author: ➤ NASA Technical Reports Server (NTRS)
- Language: English
“NASA Technical Reports Server (NTRS) 20170001349: Dependence Of Early And Late Chromosomal Aberrations On Radiation Quality And Cell Types” Subjects and Themes:
- Subjects: ➤ NASA Technical Reports Server (NTRS) - 03cf0a55a6da484fa6e03d958c1539ec - 316dbf9ef8174348aff0f3b247543f4b - 33513aa1bf6446d3bbd3703df1568611 - 420008cb67df49088372f0f8a02a8218 - 7e398a23162244b98a096bffa8b3af6a - 9f92a7b0c8bf45d7bd41a0b73285a720 - a2f389f15d9b44aeb107bf856618db9d - Bowler, Deborah - Cocoa Beach, FL, United States - d758da71c8424f26b8d6eb7f04eab1ea - fddb57b3b71d4e7fa4127d7f68ad361f - Goss, Rosalin - Headington, United Kingdom - Houston, TX, United States - Houston Univ.-Clear Lake - Kadhim, Munira - KBRwyle Science, Technology and Engineering - Krieger, Stephanie - Lu, Tao - NASA Johnson Space Center - NASA Kennedy Space Center - Oxford Brookes Univ. - Rohde, Larry - Texas Southern Univ. - Universities Space Research Association - Wilson, Bobby - Wu, Honglu - Yeshitla, Samrawit - Zhang, Ye
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- Internet Archive ID: NASA_NTRS_Archive_20170001349
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18Functional Genomic Analysis Of Chromosomal Aberrations In A Compendium Of 8000 Cancer Genomes.
By Kim, Tae-Min, Xi, Ruibin, Luquette, Lovelace J., Park, Richard W., Johnson, Mark D. and Park, Peter J.
This article is from Genome Research , volume 23 . Abstract A large database of copy number profiles from cancer genomes can facilitate the identification of recurrent chromosomal alterations that often contain key cancer-related genes. It can also be used to explore low-prevalence genomic events such as chromothripsis. In this study, we report an analysis of 8227 human cancer copy number profiles obtained from 107 array comparative genomic hybridization (CGH) studies. Our analysis reveals similarity of chromosomal arm-level alterations among developmentally related tumor types as well as a number of co-occurring pairs of arm-level alterations. Recurrent (“pan-lineage”) focal alterations identified across diverse tumor types show an enrichment of known cancer-related genes and genes with relevant functions in cancer-associated phenotypes (e.g., kinase and cell cycle). Tumor type-specific (“lineage-restricted”) alterations and their enriched functional categories were also identified. Furthermore, we developed an algorithm for detecting regions in which the copy number oscillates rapidly between fixed levels, indicative of chromothripsis. We observed these massive genomic rearrangements in 1%–2% of the samples with variable tumor type-specific incidence rates. Taken together, our comprehensive view of copy number alterations provides a framework for understanding the functional significance of various genomic alterations in cancer genomes.
“Functional Genomic Analysis Of Chromosomal Aberrations In A Compendium Of 8000 Cancer Genomes.” Metadata:
- Title: ➤ Functional Genomic Analysis Of Chromosomal Aberrations In A Compendium Of 8000 Cancer Genomes.
- Authors: ➤ Kim, Tae-MinXi, RuibinLuquette, Lovelace J.Park, Richard W.Johnson, Mark D.Park, Peter J.
- Language: English
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- Internet Archive ID: pubmed-PMC3561863
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19Chromosomal Aberrations In Human Lymphocytes And Fibroblasts After Exposure To Very Low Doses Of High-LET Radiation
This article is from Genome Research , volume 23 . Abstract A large database of copy number profiles from cancer genomes can facilitate the identification of recurrent chromosomal alterations that often contain key cancer-related genes. It can also be used to explore low-prevalence genomic events such as chromothripsis. In this study, we report an analysis of 8227 human cancer copy number profiles obtained from 107 array comparative genomic hybridization (CGH) studies. Our analysis reveals similarity of chromosomal arm-level alterations among developmentally related tumor types as well as a number of co-occurring pairs of arm-level alterations. Recurrent (“pan-lineage”) focal alterations identified across diverse tumor types show an enrichment of known cancer-related genes and genes with relevant functions in cancer-associated phenotypes (e.g., kinase and cell cycle). Tumor type-specific (“lineage-restricted”) alterations and their enriched functional categories were also identified. Furthermore, we developed an algorithm for detecting regions in which the copy number oscillates rapidly between fixed levels, indicative of chromothripsis. We observed these massive genomic rearrangements in 1%–2% of the samples with variable tumor type-specific incidence rates. Taken together, our comprehensive view of copy number alterations provides a framework for understanding the functional significance of various genomic alterations in cancer genomes.
“Chromosomal Aberrations In Human Lymphocytes And Fibroblasts After Exposure To Very Low Doses Of High-LET Radiation” Metadata:
- Title: ➤ Chromosomal Aberrations In Human Lymphocytes And Fibroblasts After Exposure To Very Low Doses Of High-LET Radiation
- Language: English
Edition Identifiers:
- Internet Archive ID: ➤ nasa_open_access_october_codes_PMC3941494
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20NASA Technical Reports Server (NTRS) 20140013114: Induction Of Chromosomal Aberrations At Fluences Of Less Than One HZE Particle Per Cell Nucleus
By NASA Technical Reports Server (NTRS)
The assumption of a linear dose response used to describe the biological effects of high LET radiation is fundamental in radiation protection methodologies. We investigated the dose response for chromosomal aberrations for exposures corresponding to less than one particle traversal per cell nucleus by high energy and charge (HZE) nuclei. Human fibroblast and lymphocyte cells where irradiated with several low doses of <0.1 Gy, and several higher doses of up to 1 Gy with O (77 keV/ (long-s)m), Si (99 keV/ (long-s)m), Fe (175 keV/ (long-s)m), Fe (195 keV/ (long-s)m) or Fe (240 keV/ (long-s)m) particles. Chromosomal aberrations at first mitosis were scored using fluorescence in situ hybridization (FISH) with chromosome specific paints for chromosomes 1, 2 and 4 and DAPI staining of background chromosomes. Non-linear regression models were used to evaluate possible linear and non-linear dose response models based on these data. Dose responses for simple exchanges for human fibroblast irradiated under confluent culture conditions were best fit by non-linear models motivated by a non-targeted effect (NTE). Best fits for the dose response data for human lymphocytes irradiated in blood tubes were a NTE model for O and a linear response model fit best for Si and Fe particles. Additional evidence for NTE were found in low dose experiments measuring gamma-H2AX foci, a marker of double strand breaks (DSB), and split-dose experiments with human fibroblasts. Our results suggest that simple exchanges in normal human fibroblasts have an important NTE contribution at low particle fluence. The current and prior experimental studies provide important evidence against the linear dose response assumption used in radiation protection for HZE particles and other high LET radiation at the relevant range of low doses.
“NASA Technical Reports Server (NTRS) 20140013114: Induction Of Chromosomal Aberrations At Fluences Of Less Than One HZE Particle Per Cell Nucleus” Metadata:
- Title: ➤ NASA Technical Reports Server (NTRS) 20140013114: Induction Of Chromosomal Aberrations At Fluences Of Less Than One HZE Particle Per Cell Nucleus
- Author: ➤ NASA Technical Reports Server (NTRS)
- Language: English
“NASA Technical Reports Server (NTRS) 20140013114: Induction Of Chromosomal Aberrations At Fluences Of Less Than One HZE Particle Per Cell Nucleus” Subjects and Themes:
- Subjects: ➤ NASA Technical Reports Server (NTRS) - CHROMOSOME ABERRATIONS - CHROMOSOMES - RADIATION DOSAGE - LINEAR ENERGY TRANSFER (LET) - MUTATIONS - IRRADIATION - BIOLOGICAL EFFECTS - MATHEMATICAL MODELS - FLUORESCENCE - MITOSIS - REGRESSION ANALYSIS - Hada, Megumi - Chappell, Lori J. - Wang, Minli - George, Kerry A. - Cucinotta, Francis A.
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- Internet Archive ID: NASA_NTRS_Archive_20140013114
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21Brahmarasayana Protects Against Ethyl Methanesulfonate Or Methyl Methanesulfonate Induced Chromosomal Aberrations In Mouse Bone Marrow Cells.
By Guruprasad, Kanive Parashiva, Subramanian, Advait, Singh, Vikram Jeet, Sharma, Raghavendra Sudheer Kumar, Gopinath, Puthiya Mundyat, Sewram, Vikash, Varier, Panniyampilly Madhavankutty and Satyamoorthy, Kapaettu
This article is from BMC Complementary and Alternative Medicine , volume 12 . Abstract Background: Ayurveda, the traditional Indian system of medicine has given great emphasis to the promotion of health. Rasayana is one of the eight branches of Ayurveda which refers to rejuvenant therapy. It has been reported that rasayanas have immuno-modulatory, antioxidant and antitumor functions, however, the genotoxic potential and modulation of DNA repair of many rasayanas have not been evaluated. Methods: The present study assessed the role of Brahmarasayana (BR) on Ethyl methanesulfonate (EMS)-and Methyl methanesulfonate (MMS)-induced genotoxicity and DNA repair in in vivo mouse test system. The mice were orally fed with BR (5 g or 8 mg / day) for two months and 24 h later EMS or MMS was given intraperitoneally. The genotoxicity was analyzed by chromosomal aberrations, sperm count, and sperm abnormalities. Results: The results have revealed that BR did not induce significant chromosomal aberrations when compared to that of the control animals (p >0.05). On the other hand, the frequencies of chromosomal aberrations induced by EMS (240 mg / kg body weight) or MMS (125 mg / kg body weight) were significantly higher (p
“Brahmarasayana Protects Against Ethyl Methanesulfonate Or Methyl Methanesulfonate Induced Chromosomal Aberrations In Mouse Bone Marrow Cells.” Metadata:
- Title: ➤ Brahmarasayana Protects Against Ethyl Methanesulfonate Or Methyl Methanesulfonate Induced Chromosomal Aberrations In Mouse Bone Marrow Cells.
- Authors: ➤ Guruprasad, Kanive ParashivaSubramanian, AdvaitSingh, Vikram JeetSharma, Raghavendra Sudheer KumarGopinath, Puthiya MundyatSewram, VikashVarier, Panniyampilly MadhavankuttySatyamoorthy, Kapaettu
- Language: English
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22Analysis Of Chromosomal Aberrations And FLT3 Gene Mutations In Childhood Acute Myelogenous Leukemia Patients.
By Coskunp?nar, Ender, Anak, Sema, Agaoglu, Leyla, Unuvar, Aysegul, Devecioglu, Omer, Aydogan, Gonul, Timur, Cetin, Oner, Ahmet Faik, Y?ld?rmak, Y?ld?z, Celkan, Tiraje, Y?ld?z, Inci, Sarper, Nazan and Ozbek, Ugur
This article is from Turkish Journal of Hematology , volume 29 . Abstract Objective: To identify the well-known common translocations and FLT3 mutations in childhood acute myelogenousleukemia (AML) patients in Turkey.Material and Methods: The study included 50 newly diagnosed patients in which t(15;17), t(8;21), and inv(16)chromosomal translocations were identified using real-time PCR and FLT3 gene mutations were identified via direct PCR amplification PCR-RE analysis.Results: In all, t(15;17) chromosomal aberrations were observed in 4 patients (8.0%), t(8;21) chromosomal aberrationswere observed in 12 patients (24.0%), inv(16) chromosomal aberrations were observed in 3 patients (6.0%), and FLT3-ITD mutations were observed in 2 patients (4.0%); FLT3-D835 point mutation heterozygosity was observed in only 1patient (2.0%) patient.Conclusion: Despite of the known literature, a patient with FLT3-ITD and FLT3-D835 double mutation shows a bettersurvival and this might be due to the complementation effect of the t(15;17) translocation. The reportedmutation ratein this article (4%) of FLT3 gene seems to be one of the first results for Turkish population.
“Analysis Of Chromosomal Aberrations And FLT3 Gene Mutations In Childhood Acute Myelogenous Leukemia Patients.” Metadata:
- Title: ➤ Analysis Of Chromosomal Aberrations And FLT3 Gene Mutations In Childhood Acute Myelogenous Leukemia Patients.
- Authors: ➤ Coskunp?nar, EnderAnak, SemaAgaoglu, LeylaUnuvar, AysegulDevecioglu, OmerAydogan, GonulTimur, CetinOner, Ahmet FaikY?ld?rmak, Y?ld?zCelkan, TirajeY?ld?z, InciSarper, NazanOzbek, Ugur
- Language: English
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23Chromosomal Aberrations : Basic And Applied Aspects
This article is from Turkish Journal of Hematology , volume 29 . Abstract Objective: To identify the well-known common translocations and FLT3 mutations in childhood acute myelogenousleukemia (AML) patients in Turkey.Material and Methods: The study included 50 newly diagnosed patients in which t(15;17), t(8;21), and inv(16)chromosomal translocations were identified using real-time PCR and FLT3 gene mutations were identified via direct PCR amplification PCR-RE analysis.Results: In all, t(15;17) chromosomal aberrations were observed in 4 patients (8.0%), t(8;21) chromosomal aberrationswere observed in 12 patients (24.0%), inv(16) chromosomal aberrations were observed in 3 patients (6.0%), and FLT3-ITD mutations were observed in 2 patients (4.0%); FLT3-D835 point mutation heterozygosity was observed in only 1patient (2.0%) patient.Conclusion: Despite of the known literature, a patient with FLT3-ITD and FLT3-D835 double mutation shows a bettersurvival and this might be due to the complementation effect of the t(15;17) translocation. The reportedmutation ratein this article (4%) of FLT3 gene seems to be one of the first results for Turkish population.
“Chromosomal Aberrations : Basic And Applied Aspects” Metadata:
- Title: ➤ Chromosomal Aberrations : Basic And Applied Aspects
- Language: English
“Chromosomal Aberrations : Basic And Applied Aspects” Subjects and Themes:
- Subjects: ➤ Medical genetics - Human chromosome abnormalities - Aberrations chromosomiques - Chromosome Aberrations - Chromosomes humains -- Anomalies - Chromosomenaberration - Humans Genetic disorders - Génétique médicale - Genetique medicale
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- Internet Archive ID: chromosomalaberr0000unse
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24Chromosomal Aberrations In In-Vitro Matured Oocytes Influence Implantation And Ongoing Pregnancy Rates In A Mouse Model Undergoing Intracytoplasmic Sperm Injection.
By Li, Min, Zhao, Hong-Cui, Li, Rong, Yu, Yang and Qiao, Jie
This article is from PLoS ONE , volume 9 . Abstract Implantation failure and early pregnancy loss have been reported to be closely related to the quality of mammalian oocytes; however, the pregnant outcome of embryos from in-vitro matured (IVM) oocytes remains unknown. In this study we examined spindle assembly and chromosome segregation during differentiation, and the duration of IVM of mouse oocytes. The resulting implantation and pregnancy outcomes were analyzed to clarify the relationship between the spindle and chromosomes of IVM oocytes and implantation and early pregnancy. Cumulus-enclosed germinal vesicle oocytes were collected and randomly cultured in IVM medium with different IVM durations. One part of IVM oocytes were analyzed the spindle and chromosome morphology by immunofluorescence method, and the other part of them were fertilized by intracytoplasmic sperm injection. The resulting embryos were transferred into pseudo-pregnant female mice, and the post-implantation and full term development was observed. The chromosome aberrations and incorrect spindle assembly seems not affect the early development and blastocyst cell number derived from IVM oocytes, however the development potential of the resulting embryos after implantation were significant decreased with the ratio increasing of chromosome aberrations and incorrect spindle assembly. Accordingly, the full-term development was also decreased. In conclusion, the present study showed the spindle assembly of in vitro-matured oocytes was one of the most important factors that affected the implantation and ongoing pregnancy rates of IVM oocytes, and the improvement by an appropriate duration of maturation in vitro will enhance the post-implantation development potential of the resulting embryos, and decrease implantation failure and early pregnancy loss.
“Chromosomal Aberrations In In-Vitro Matured Oocytes Influence Implantation And Ongoing Pregnancy Rates In A Mouse Model Undergoing Intracytoplasmic Sperm Injection.” Metadata:
- Title: ➤ Chromosomal Aberrations In In-Vitro Matured Oocytes Influence Implantation And Ongoing Pregnancy Rates In A Mouse Model Undergoing Intracytoplasmic Sperm Injection.
- Authors: Li, MinZhao, Hong-CuiLi, RongYu, YangQiao, Jie
- Language: English
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- Internet Archive ID: pubmed-PMC4110001
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25Lecture 5.chromosomal Aberrations
By Share and Care
Powerpoint of Chromosomal abberations Dr. Reem Mubjer
“Lecture 5.chromosomal Aberrations” Metadata:
- Title: ➤ Lecture 5.chromosomal Aberrations
- Author: Share and Care
- Language: English
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- Internet Archive ID: ➤ Lecture5.chromosomalAberrations
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26Human Afflictions And Chromosomal Aberrations
By Turpin, Raymond, 1895-
Powerpoint of Chromosomal abberations Dr. Reem Mubjer
“Human Afflictions And Chromosomal Aberrations” Metadata:
- Title: ➤ Human Afflictions And Chromosomal Aberrations
- Author: Turpin, Raymond, 1895-
- Language: eng,fre
“Human Afflictions And Chromosomal Aberrations” Subjects and Themes:
- Subjects: Human chromosome abnormalities - Karyotypes
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- Internet Archive ID: humanafflictions0000turp
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27Studies On Brahma Rasayana In Male Swiss Albino Mice: Chromosomal Aberrations And Sperm Abnormalities.
By Guruprasad, K. P., Mascarenhas, Roshan, Gopinath, P. M. and Satyamoorthy, K.
This article is from Journal of Ayurveda and Integrative Medicine , volume 1 . Abstract Ayurveda, the Indian holistic healthcare system encompasses traditional medicines with a principle of creating harmony and maintaining balance within the natural rhythms of the body. Rasayana is one of the branches of Ayurveda frequently used as rejuvenant therapy to overcome many discomforts and prevent diseases. It has been reported that rasayanas have immunomodulatory, antioxidant and antitumor functions. However, the genotoxic potential of many rasayanas remains to be evaluated. The present study was undertaken to assess the role of Brahma rasayana(BR) on genotoxicity in vivo in a mouse test system. The older mice (9 months) were orally fed with rasayana for 8 weeks. The treated groups showed no signs of dose-dependent toxicity at the dosage levels tested. The body weight loss/gain and feed consumption were unaffected at tested doses. Furthermore, sperm abnormalities and chromosomal aberrations were insignificant in the treatment group when compared to controls. However, there was a marginal increase in sperm count in the BR treated animals. These findings clearly indicate that there are no observed adverse genotoxic effects elicited by BR in experimental animals such as mice.
“Studies On Brahma Rasayana In Male Swiss Albino Mice: Chromosomal Aberrations And Sperm Abnormalities.” Metadata:
- Title: ➤ Studies On Brahma Rasayana In Male Swiss Albino Mice: Chromosomal Aberrations And Sperm Abnormalities.
- Authors: Guruprasad, K. P.Mascarenhas, RoshanGopinath, P. M.Satyamoorthy, K.
- Language: English
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- Internet Archive ID: pubmed-PMC3149391
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28Spectra Of Chromosomal Aberrations In 325 Leukemia Patients And Implications For The Development Of New Molecular Detection Systems.
By Choi, Hyun-Jung, Kim, Hye-Ran, Shin, Myung-Geun, Kook, Hoon, Kim, Hyeoung-Joon, Shin, Jong-Hee, Suh, Soon-Pal and Ryang, Dong-Wook
This article is from Journal of Korean Medical Science , volume 26 . Abstract This study investigated the spectrum of chromosomal abnormalities in 325 leukemia patients and developed optimal profiles of leukemic fusion genes for multiplex RT-PCR. We prospectively analyzed blood and bone marrow specimens of patients with acute leukemia. Twenty types of chromosomal abnormalities were detected in 42% from all patients by commercially available multiplex RT-PCR for detecting 28 fusion genes and in 35% by cytogenetic analysis including FISH analysis. The most common cytogenetic aberrations in acute myeloid leukemia patients was PML/PARA, followed by AML1/MGT8 and MLL1, and in acute lymphoid leukemia patients was BCR/ABL, followed by TEL/AML1 and MLL1 gene rearrangement. Among the negative results for multiplex RT-PCR, clinically significant t(3;3)(q21;q26.2), t(8;14)(q24;q32) and i(17)(q10) were detected by conventional cytogenetics. The spectrum and frequency of chromosomal abnormalities in our leukemia patients are differed from previous studies, and may offer optimal profiles of leukemic fusion genes for the development of new molecular detection systems.
“Spectra Of Chromosomal Aberrations In 325 Leukemia Patients And Implications For The Development Of New Molecular Detection Systems.” Metadata:
- Title: ➤ Spectra Of Chromosomal Aberrations In 325 Leukemia Patients And Implications For The Development Of New Molecular Detection Systems.
- Authors: ➤ Choi, Hyun-JungKim, Hye-RanShin, Myung-GeunKook, HoonKim, Hyeoung-JoonShin, Jong-HeeSuh, Soon-PalRyang, Dong-Wook
- Language: English
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- Internet Archive ID: pubmed-PMC3124718
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29Chromosomal Copy Number Aberrations In Colorectal Metastases Resemble Their Primary Counterparts And Differences Are Typically Non-Recurrent.
By Mekenkamp, Leonie J. M., Haan, Josien C., Israeli, Danielle, van Essen, Hendrik F. B., Dijkstra, Jeroen R., van Cleef, Patricia, Punt, Cornelis J. A., Meijer, Gerrit A., Nagtegaal, Iris D. and Ylstra, Bauke
This article is from PLoS ONE , volume 9 . Abstract The metastatic process is complex and remains a major obstacle in the management of colorectal cancer. To gain a better insight into the pathology of metastasis, we investigated genomic aberrations in a large cohort of matched colorectal cancer primaries and distant metastases from various sites by high resolution array comparative genomic hybridization. In total, 62 primary colorectal cancers, and 68 matched metastases (22 liver, 11 lung, 12 ovary, 12 omentum, and 11 distant lymph nodes) were analyzed. Public datasets were used for validation purposes. Metastases resemble their matched primary tumors in the majority of the patients. This validates the significant overlap in chromosomal aberrations between primary tumors and corresponding metastases observed previously. We observed 15 statistically significant different regions between the primary tumors and their matched metastases, of which only one recurrent event in metastases was observed. We conclude, based on detailed analysis and large independent datasets, that chromosomal copy number aberrations in colorectal metastases resemble their primary counterparts, and differences are typically non-recurrent.
“Chromosomal Copy Number Aberrations In Colorectal Metastases Resemble Their Primary Counterparts And Differences Are Typically Non-Recurrent.” Metadata:
- Title: ➤ Chromosomal Copy Number Aberrations In Colorectal Metastases Resemble Their Primary Counterparts And Differences Are Typically Non-Recurrent.
- Authors: ➤ Mekenkamp, Leonie J. M.Haan, Josien C.Israeli, Daniellevan Essen, Hendrik F. B.Dijkstra, Jeroen R.van Cleef, PatriciaPunt, Cornelis J. A.Meijer, Gerrit A.Nagtegaal, Iris D.Ylstra, Bauke
- Language: English
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- Internet Archive ID: pubmed-PMC3914793
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30APPLICATION FOR RESEARCH CONTRACT TREATMENT OF OVERDISPERSED, AGGREGATED DATA ON HUMAN CHROMOSOMAL ABERRATIONS
Philip Morris Records; bibliography; budget; budget review; form; research proposal, scientific; resume; conf, confidential; pare, parent
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- Title: ➤ APPLICATION FOR RESEARCH CONTRACT TREATMENT OF OVERDISPERSED, AGGREGATED DATA ON HUMAN CHROMOSOMAL ABERRATIONS
- Language: English
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- Internet Archive ID: tobacco_nnlm0000
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31RESEARCH ABSTRACT TREATMENT OF OVERDISPERSED, AGGREGATED DATA ON HUMAN CHROMOSOMAL ABERRATIONS
Philip Morris Records; abstract; conf, confidential; extr, extra
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- Title: ➤ RESEARCH ABSTRACT TREATMENT OF OVERDISPERSED, AGGREGATED DATA ON HUMAN CHROMOSOMAL ABERRATIONS
- Language: English
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- Internet Archive ID: tobacco_ynlm0000
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32Giant Invasive Sacral Schwannoma Showing Chromosomal Numerical Aberrations [-14,+18,+22].
By Kanamori, Masahiko, Yasuda, Taketoshi, Hori, Takeshi and Suzuki, Kayo
This article is from Asian Spine Journal , volume 7 . Abstract Here, we report on a rare case of a giant invasive sacral schwannoma. The patient was a 58-year-old woman who had a 6-year history of non-specific buttock pain. Histological investigation confirmed the diagnosis of cellular schwannoma. The following numerical aberration was detected using the GTG-banding method for karyotypes: 47,XX,-14,+18,+22. Cytogenetic studies of schwannomas have indicated a complete or partial loss of chromosome 22 as the most common abnormality, but this case is cytogenetically rare because of the recurrence of trisomy 22.
“Giant Invasive Sacral Schwannoma Showing Chromosomal Numerical Aberrations [-14,+18,+22].” Metadata:
- Title: ➤ Giant Invasive Sacral Schwannoma Showing Chromosomal Numerical Aberrations [-14,+18,+22].
- Authors: Kanamori, MasahikoYasuda, TaketoshiHori, TakeshiSuzuki, Kayo
- Language: English
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- Internet Archive ID: pubmed-PMC3779776
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The book is available for download in "texts" format, the size of the file-s is: 6.24 Mbs, the file-s for this book were downloaded 65 times, the file-s went public at Fri Oct 24 2014.
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33Genetic Mechanisms In Human Disease: Chromosomal Aberrations
By Montagu, Ashley, 1905- ed
Includes bibliography
“Genetic Mechanisms In Human Disease: Chromosomal Aberrations” Metadata:
- Title: ➤ Genetic Mechanisms In Human Disease: Chromosomal Aberrations
- Author: Montagu, Ashley, 1905- ed
- Language: English
“Genetic Mechanisms In Human Disease: Chromosomal Aberrations” Subjects and Themes:
- Subjects: Medical genetics - Genetics
Edition Identifiers:
- Internet Archive ID: geneticmechanism00mont
Downloads Information:
The book is available for download in "texts" format, the size of the file-s is: 1189.55 Mbs, the file-s for this book were downloaded 96 times, the file-s went public at Wed Aug 03 2011.
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Source: The Open Library
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Available books for downloads and borrow from The Open Library
1Chromosomal aberrations
By G. Obe and A. T. Natarajan

“Chromosomal aberrations” Metadata:
- Title: Chromosomal aberrations
- Authors: G. ObeA. T. Natarajan
- Language: English
- Number of Pages: Median: 332
- Publisher: ➤ Island Press - Springer-Verlag Berlin and Heidelberg GmbH & Co. K
- Publish Date: 1990
“Chromosomal aberrations” Subjects and Themes:
- Subjects: ➤ Genetique medicale - Chromosomenaberration - Medical genetics - Chromosome Aberrations - Chromosomes humains - Anomalies - Human chromosome abnormalities - Aberrations chromosomiques
Edition Identifiers:
- The Open Library ID: OL12776021M - OL50687349M
- Online Computer Library Center (OCLC) ID: 21482093
- Library of Congress Control Number (LCCN): 90009804
- All ISBNs: 3540525408 - 9783642756832 - 3642756832 - 9783540525400
Author's Alternative Names:
"G OBE"Access and General Info:
- First Year Published: 1990
- Is Full Text Available: Yes
- Is The Book Public: No
- Access Status: Borrowable
Online Access
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