Literatura académica sobre el tema "Y-STR HAPLOTYPES"
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Artículos de revistas sobre el tema "Y-STR HAPLOTYPES"
Pardo-Seco, Jacobo, Alberto Gómez-Carballa, Xabier Bello, Federico Martinón-Torres y Antonio Salas. "Biogeographical informativeness of Y-STR haplotypes". Science Bulletin 64, n.º 19 (octubre de 2019): 1381–84. http://dx.doi.org/10.1016/j.scib.2019.07.025.
Texto completoHallenberg, Charlotte, Karsten Nielsen, Bo Simonsen, Juan Sanchez y Niels Morling. "Y-chromosome STR haplotypes in Danes". Forensic Science International 155, n.º 2-3 (diciembre de 2005): 205–10. http://dx.doi.org/10.1016/j.forsciint.2004.12.019.
Texto completoHallenberg, Charlotte, Bo Simonsen, Juan Sanchez y Niels Morling. "Y-chromosome STR haplotypes in Somalis". Forensic Science International 151, n.º 2-3 (julio de 2005): 317–21. http://dx.doi.org/10.1016/j.forsciint.2005.01.011.
Texto completoHolmlund, Gunilla, Helena Nilsson, Andreas Karlsson y Bertil Lindblom. "Y-chromosome STR haplotypes in Sweden". Forensic Science International 160, n.º 1 (junio de 2006): 66–79. http://dx.doi.org/10.1016/j.forsciint.2005.05.008.
Texto completoRobino, C., S. Inturri, S. Gino, C. Torre, C. Di Gaetano, F. Crobu, V. Romano, G. Matullo y A. Piazza. "Y-chromosomal STR haplotypes in Sicily". Forensic Science International 159, n.º 2-3 (junio de 2006): 235–40. http://dx.doi.org/10.1016/j.forsciint.2005.05.015.
Texto completoKido, Akira, Yuji Dobashi, Rie Susukida, Noboru Fujitani, Masaaki Hara y Masakazu Oya. "Y-Chromosomal STR Haplotypes in Indonesians". Journal of Forensic Sciences 50, n.º 4 (2005): 1–3. http://dx.doi.org/10.1520/jfs2005044.
Texto completoMohyuddin, Aisha, Qasim Ayub, Raheel Qamar, Tatiana Zerjal, Agnar Helgason, S. Qasim Mehdi y Chris Tyler-Smith. "Y-chromosomal STR haplotypes in Pakistani populations". Forensic Science International 118, n.º 2-3 (mayo de 2001): 141–46. http://dx.doi.org/10.1016/s0379-0738(01)00382-6.
Texto completoBeleza, S., C. Alves, A. González-Neira, M. Lareu, A. Amorim, A. Carracedo y L. Gusmão. "Extending STR markers in Y chromosome haplotypes". International Journal of Legal Medicine 117, n.º 1 (febrero de 2003): 27–33. http://dx.doi.org/10.1007/s00414-002-0317-8.
Texto completoFondevila, Manuel, Juan Carlos Jaime, Antonio Salas, Marı́a Victoria Lareu y Ángel Carracedo. "Y-chromosome STR haplotypes in Córdoba (Argentina)". Forensic Science International 137, n.º 2-3 (noviembre de 2003): 217–20. http://dx.doi.org/10.1016/j.forsciint.2003.07.006.
Texto completoHashiyada, Masaki, Toshio Nagashima, Yukio Itakura, Jun Sakai, Yoshimasa Kanawaku, Jun Kanetake, Masayuki Nata y Masato Funayama. "12 Y-chromosomal STR haplotypes in Japanese". Forensic Science International 158, n.º 2-3 (mayo de 2006): 204–12. http://dx.doi.org/10.1016/j.forsciint.2005.04.035.
Texto completoTesis sobre el tema "Y-STR HAPLOTYPES"
Berdos, Paulina Niki. "THE DESIGN AND DEVELOPMENT OF A COMPREHENSIVE 49 LOCUS Y-STR DATABASE FOR MAJOR U.S. POPULATIONS". Master's thesis, University of Central Florida, 2004. http://digital.library.ucf.edu/cdm/ref/collection/ETD/id/4472.
Texto completoM.S.
Department of Chemistry
Arts and Sciences
Chemistry
Cloete, Kevin Wesley. "Development of Y-STR genotyping systems suitable for sexual assault cases in South Africa". Thesis, University of the Western Cape, 2010. http://etd.uwc.ac.za/usrfiles/modules/etd/docs/etd_gen8Srv25Nme4_4315_1274816776.pdf.
Texto completoMwema, Hadija Saidi. "Forensic identification of six of Tanzanian populations using the extended haplotype markers". Thesis, University of the Western Cape, 2011. http://etd.uwc.ac.za/index.php?module=etd&action=viewtitle&id=gen8Srv25Nme4_2349_1325671867.
Texto completoNiger Congo (Kuria and Sukuma), Nilo Saharan (Luo and Maasai) and Afro Asiatic (Iraqw and Alagwa).
Fernandes, Isabella Lacerda. "Estimativa da taxa de mutação de marcadores STRs do cromossomo Y em uma amostra da população brasileira e sua importância no processo de identificação humana". Pontifícia Universidade Católica de Goiás, 2015. http://localhost:8080/tede/handle/tede/2394.
Texto completoMicrosatellite markers are short sequences, repetitive, highly polymorphic and hereditary present in the DNA, which follow the Mendelian pattern of segregation. Due to its haplotype heritage has been used to trace the paternal line to be passed from generation to generation without any changes, except in cases of mutation. The stepwise mutation model is more acceptable to mutation in microsatellite markers, assuming that each mutational event the length of a microsatellite changes by one or a few repeating units due to slippage process, which occurs during replication DNA. This study aimed to estimate the rates of change of microsatellite markers of the Y chromosome in a sample of the population and its implications in human identification process. It is a molecular study, which was conducted at Biocroma Laboratory in partnership with LaGene and Replicon in Goiânia-Goiás. Samples of study were selected from 80 cases of investigation of paternity by DNA analysis, undergo mutation analysis in the Y chromosome haplotypes with molecular amplification system PowerPlex® Y23 System - Promega Corporation. Were identified 15 records of germline mutations in the Y chromosome between alleged parents and children related to suspected samples. The results have identified 9 mutations gain and 6 mutations loss of repetitions numbers. The DYS576 marker had the highest number of reported mutations (20%), followed by DYS570, which identified two mutations (13.33%). The markers DYS389 II, DYS391, DYS481, DYS549, DYS438, DYS439, DYS393, DYS458, DYS385 a - b DYS456 showed only 1 (6.66%) mutation record each. In the other markers, DYS389 I, DYS448, DYS19, DYS533, DYS437, DYS635, DYS390, DYS392, DYS643 and Y-GATA-H4 mutations were not identified in the samples analyzed in this study. Thus the identification of mutations increases the tools that are used in genetic analysis link laboratories and can deliver a more reliable result minimizing potential errors in the analyzes.
Os marcadores microssatélites são sequências curtas, repetitivas, altamente polimórficas e hereditárias presentes no DNA, que seguem o padrão mendeliano de segregação. Devido a sua herança haplotípica tem sido utilizado para rastrear a linhagem paterna por ser passado de geração em geração sem nenhuma alteração, exceto em casos de mutação. O modelo step-wise mutation é o mais aceito para mutação nos marcadores microssatélites, admitindo-se que, a cada evento mutacional o comprimento de um microssatélite altera por uma ou poucas unidades de repetição devido ao processo de slippage, que ocorre durante a replicação do DNA. Este trabalho teve como objetivo estimar as taxas de mutações dos marcadores microssatélites do cromossomo Y em uma amostra da população brasileira e suas implicações no processo de identificação humana. Trata-se de um estudo molecular, que foi conduzido no Laboratório Biocroma em parceria com o LaGene e Replicon em Goiânia-Goiás. As amostras de estudo foram selecionadas de 80 casos de investigação de paternidade pela análise do DNA, submetidos a análise de mutações nos haplótipos do cromossomo Y com o sistema de amplificação molecular PowerPlex® Y23 System Promega Corporation. Foram identificados 15 registros de mutações germinativas no cromossomo Y entre supostos pais e supostos filhos referentes às amostras analisadas. Os resultados obtidos permitiram identificar 9 mutações de ganho e 6 mutações de perda de números de repetições. O marcador DYS576 apresentou o maior número de mutações registrados (20%), seguido pelo DYS570, que permitiu identificar 2 mutações (13,33%). Os marcadores DYS389 II, DYS391, DYS481, DYS549, DYS438, DYS439, DYS393, DYS458, DYS385 a-b e DYS456 apresentaram apenas 1 (6,66%) registro de mutação cada. Nos demais marcadores, DYS389 I, DYS448, DYS19, DYS533, DYS437, DYS635, DYS390, DYS392, DYS643 e Y-GATA-H4 não foram identificadas mutações nas amostras analisadas neste estudo. Desta forma a identificação das mutações aumenta as ferramentas que são utilizadas nos laboratórios de análise de vínculo genético e que podem garantir um resultado mais confiável minimizando possíveis erros nas análises.
Lin, Bao-Shun y 林寶順. "Analysis of the association between surnames and Y-chromosomal STR haplotypes in the Taiwanese Han population". Thesis, 2012. http://ndltd.ncl.edu.tw/handle/44266291517315853303.
Texto completo國立臺灣大學
法醫學研究所
100
Background and purpose It is a biological necessity that a son inherit the Y chromosome of his father. Since Han population follow the paternal surname system, the surname can be thought of as traits ‘linked’ to the Y chromosome. Therefore, Han males with same surname may have same or similar Y haplotypes. The aim of our study was to analyze the Y chromosomal short tandem repeats (STR) haplotypes of groups of men with same surname and to assess the actual extent of correlation between surnames and Y-STR haplotypes in Taiwanese Han. Materials and Methods We genotyped 17 Y-STR markers (DYS456, DYS389I, DYS390, DYS389II, DYS458, DYS19, DYS385a, DYS385b, DYS393, DYS391, DYS439, DYS635, DYS392, Y-GATA-H4, DYS437, DYS438, DYS448) in 735 unrelated male Taiwanese Han. The individuals were subdivided into 10 groups according to their surname, including most common surnames: Chen(102), Lin(107), Li(107), less common surnames: Zhou(42), Jian(29), Tang(8), Cao(8), and rare surnames: Hua(21), Yin(5), and Ruan(6). The Y-STR data of another group of unrelated male Taiwanese Han(200) sampled from general population and 367 male Taiwanese Han from FORDDAS were served as a control population. Haplotype frequencies and haplotype diversity of each group were calculated. Possible descent cluster was identified. The correlation between surname and haplotypes of each group was analyzed. Results: Among these 10 surname groups, the haplotype diversity values were from 0.9143 (Hua) to 1 (Cao, Yin and Ruan). The common surname Chen, Lin and Li have high haplotype diversity and the haplotypes of these surname groups are well distribution as the general population. The haplotype distributions of less common surnames are similar to that of the common surnames except the surname Jian. Jian group has a haplotype shared by seven persons with two one-step neighbors near this core haplotype. This Jian’s cluster include 31.03% of its group. The rare surname Hua group has relatively lower haplotype diversity and a cluster with 42.86% of its group. A particular haplotype was shared by 6 persons with three one-step neighbors, whereas this haplotype has not been identified in other surname groups. This Y-STR haplotype may be specific to men with surname Hua. The Principal Coordinate Analysis showed similar distribution of 17 Y-STR loci of 10 different surname groups and Taiwanese Han. Conclusions: Our results suggest that the origins of the common surnames in Taiwanese are heterogeneous. Many interference factors have obscured the Y-STR linkage within common surname groups. The less common and rare surname groups may have the chance to find a bigger descent cluster which has potential to be used in forensic human identification.
Cereda, G. "Current challenges in statistical DNA evidence evaluation". Doctoral thesis, 2017. http://hdl.handle.net/2158/1272989.
Texto completoSeidenberg, Verena. "Ein bronzezeitlicher Familienclan als genetisches Archiv – Morphologisch-paläogenetische Bearbeitung des Skelettkollektivs aus der Lichtensteinhöhle". Doctoral thesis, 2016. http://hdl.handle.net/11858/00-1735-0000-002B-7D55-C.
Texto completoCainé, Laura Sofia Ramos Mendes. "Y-STR markers, haplotype discrimination and sensibility in sexual assault cases. The impact of different technologies". Master's thesis, 2016. https://repositorio-aberto.up.pt/handle/10216/83549.
Texto completoCainé, Laura Sofia Ramos Mendes. "Y-STR markers, haplotype discrimination and sensibility in sexual assault cases. The impact of different technologies". Dissertação, 2016. https://repositorio-aberto.up.pt/handle/10216/83549.
Texto completoSaidi, Mwema Hadija. "Forensic identification of six of Tanzanian populations using the extended haplotype markers". Thesis, 2011. http://hdl.handle.net/11394/3571.
Texto completoMagister Scientiae - MSc
Capítulos de libros sobre el tema "Y-STR HAPLOTYPES"
Mahasneh, Ihsane Ali, Berjas Abumsimir, Moulay Mustapha Ennaji y Yassine Kasmi. "The global genomic allelic heterogeneity of the HOXB 13 variants of prostate cancer and gene therapy application for different genealogical lineages of the Y-chromosome haplogroups and haplotypes of STR microsatellites". En Immunological Implications and Molecular Diagnostics of Genitourinary Cancer, 411–33. Elsevier, 2023. http://dx.doi.org/10.1016/b978-0-323-85496-2.00011-7.
Texto completoRoewer, Lutz. "The Y-Chromosome Haplotype Reference Database (YHRD) — Publicly Available Reference and Research Datasets for the Forensic Interpretation of Y-Chromosome STR Profiles". En Security Science and Technology, 231–48. WORLD SCIENTIFIC (EUROPE), 2016. http://dx.doi.org/10.1142/9781786340788_0012.
Texto completoActas de conferencias sobre el tema "Y-STR HAPLOTYPES"
Udina, I. G., A. S. Gracheva, Yu А. Vasiliev, E. Yu Pobedonosteva y O. L. Kurbatova. "PECULIARITIES OF DISTRIBUTION OF Y-CHROMOSOME HAPLOGROUPS IN GENERATIONS OF MEGAPOLIS POPULATION UNDER ACTION OF MIGRATION". En NOVEL TECHNOLOGIES IN MEDICINE, BIOLOGY, PHARMACOLOGY AND ECOLOGY. Institute of information technology, 2022. http://dx.doi.org/10.47501/978-5-6044060-2-1.110-113.
Texto completoChen, Meng-Yi, Chang-En Pu, Fang-Chin Wu, Huei-Yu Lai y Chin-Wen Ho. "Rapidly mutating Y-STRs population data in Taiwan and haplotype probability estimation for forensic purposes". En 2015 International Carnahan Conference on Security Technology (ICCST). IEEE, 2015. http://dx.doi.org/10.1109/ccst.2015.7389717.
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