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  • About
  • The Global ETD Search service is a free service for researchers to find electronic theses and dissertations. This service is provided by the Networked Digital Library of Theses and Dissertations.
    Our metadata is collected from universities around the world. If you manage a university/consortium/country archive and want to be added, details can be found on the NDLTD website.
1

Sister chromatid exchange rates in human twins

Zukowski, Mark M. January 1978 (has links)
No description available.
2

Studies on human chromosome satellite association

Hemel, Jan Oscar van, January 1971 (has links)
Proefschrift: Rijksuniversiteit te Utrecht. / "Stellingen" (2 p.) and vita inserted. Summary and afterword in Dutch. Bibliography: p. 64-69.
3

Human chromosome structure DNA content, base ratio and quinacrine fluorescence ; Giemsa technique for the detection of sister chromatid exchanges /

Korenberg, Julie Ruth, January 1976 (has links)
Thesis - Wisconsin. / Vita. Includes reprint. Bibliography: leaves 257-272.
4

Studies on human chromosome satellite association

Hemel, Jan Oscar van, January 1971 (has links)
Proefschrift: Rijksuniversiteit te Utrecht. / "Stellingen" (2 p.) and vita inserted. Summary and afterword in Dutch. Bibliography: p. 64-69.
5

THE IN VITRO EFFECTS OF ETHYL METHANESULFONATE ON HUMAN LYMPHOCYTE CHROMOSOMES

Young, Veronica Marie Ladensack, 1948- January 1976 (has links)
No description available.
6

Comparative and functional genomic analysis of a gene dense region at chromosome 7q22

Wilson, Michael Davies. 10 April 2008 (has links)
Genomic sequencing, comparative genomic analysis and mouse transgenics were used to investigate two regions of human chromosome 7 that are associated with chromosomal loss, duplication and disease. Williams-Beuren syndrome (WBS) is a complex neuro-developmental disorder arising from a microdeletion at chromosome band 7q11.23 that results in a hemizygous condition for a number of genes. Within this region we completely characterized 200 kilobases (kb) of genomic DNA sequence containing the genes LIMKI, WBSCRl and RFC2. The orthologous region on mouse chromosome 5 was sequenced and compared to 7q11.23. A previously unidentified gene, ( WBSCRS), was found in the region commonly deleted in WBS patients. Expression patterns and alternative splice variants of WBSCRS and WBSCRl were determined. Chromosome 7q22 has been the focus of many cytogenetic and molecular studies aimed at delineating regions commonly deleted in myeloid leukemias and myelodysplastic syndromes. We have compared a gene dense, G-C rich sub-region of 7q22 to the orthologous region on mouse chromosome 5. A physical map of 640 kb of genomic DNA from mouse chromosome 5 was derived from a series of overlapping bacterial artificial chromosomes (BAC). A 296 kb segment from the physical map, spanning from acetylcholine esterase (Ache) to transferrin receptor 2 (Tfr2), was compared to 267 kb of human sequence. A conserved linkage of twelve genes including arsenite resistance 2 (Ars2) and zonadhesin (Zan) was identified. The paired immunoglobulin-like receptor locus (PILR) at 7q22 shares homology with 7q11.23 and contains the inhibiting PILRA and activating PILRB receptors. These receptors are expressed in myeloid cells and have been established as novel regulators of innate immunity. Expression analysis of the human PILRB gene revealed it has been dramatically affected by the insertion of a segmental duplication that is paralogous to the sequence flanking the WBS critical region. Sequencing and analysis of the orthologous region in the mouse genome revealed a previously unreported paired immunoglobulin like receptor gene (Pilrb2). An evolutionary analysis of the PILR locus in six mammalian genomes revealed that this locus is dynamically evolving by means of gene duplication, insertion, mutation and conversion. Ars2 is a novel gene that is present in a diverse number of eukaryotic organisms and is essential for development in Danio rerio and Arabidopsis thaliana. To address the role of Ars2 in mammals, we characterized its expression in mouse and human tissues and implemented a gene targeting strategy to create a null allele in the mouse genome. Ars2 was found to be transcribed throughout development and was expressed ubiquitously in mouse and human tissues. The Ars2 protein localized to the nucleus. Ars2 null mice have an early embryonic lethal phenotype establishing that Ars2 is necessary for the development of diverse multi-cellular organisms. Zonadhesin (ZAN) is the only mammalian sperm protein that has been demonstrated to bind to intact zona pellucida of the egg in a species-specific manner. We investigated the in vivo role of zonadhesin by creating a mutant mouse line that lacks zonadhesin. Zonadhesin null mice show no obvious phenotype and were determined, through natural mating, to be equally as fertile as their wildtype littermates. A web-based software tool called Laj (Local alignments with java) was developed to display comparative genomic sequence data in an intuitive and informative way. All of our genomic sequence comparisons can be viewed at http:Nweb.uvic.cal-bioweb/laj.html. Laj is available at http://bio.cse.psu.edu/.
7

Investigation of candidate tumor suppressor genes on chromosomes 3 and 14 in nasopharyngeal carcinoma /

Cheung, Kwok Leung. January 2009 (has links)
Thesis (Ph.D.)--Hong Kong University of Science and Technology, 2009. / Includes bibliographical references (p. 141-157).
8

Statistical study of human constitutional chromosome rearrangement breakpoint distributions

Vásárhelyi, Krisztina January 1990 (has links)
In this study the question of nonrandomness in the distribution of human constitutional rearrangements was evaluated. The distribution of breakpoints were analysed in three groups of reciprocal translocations and three groups of inversions, subdivided according to method of ascertainment of cases for study. In addition, one data set of structural aberrations obtained from sperm chromosomes was also analysed. The method of statistical analysis, based on the binomial distribution, was developed specifically to allow testing distributions in chromosome segments as small as chromosome bands. The distribution of breakpoints was analysed in all data sets using this method, in addition to testing for overall nonrandomness using goodness of fit statistics. Nonrandomness in breakpoint distributions was found in reciprocal translocations (rcp) and inversions ascertained through abnormalities and through incidental events. However, random distribution was observed in incidentally ascertained de novo rearrangements as well as in sperm chromosome aberrations. The nonrandomness in the distribution of rcp breakpoints can be largely attributed to a bias in ascertainment of cases based on the phenotypic manifestations of chromosomal imbalance resulting from a rearrangement. A dependence of the probability of producing specific types of balanced or unbalanced progeny on the position of breakpoints is a likely explanation for the nonrandomness produced in breakpoint distributions. However, some bands including, 5q35, 7p22, 9p22, 13ql4, and 17q25, were observed in different ascertainment groups, excluding selection bias as a likely explanation for this observation. These bands may represent true sites of nonrandom rearrangement due to some factor associated with an underlying DNA sequence or structural characteristic of chromatin that predisposes to rearrangement at specific sites. The nonrandomness observed in the distribution of inversion breakpoints is most likely the product of a founder effect. Many identical inversions in apparently unrelated individuals have been found suggesting that a few ancestral mutations have become widespread in the population. A large data set of incidentally ascertained de novo inversions is required to distinguish between sites of frequent breakage and nonrandomness produced by the ascertainment of related cases. All evidence considered together, indisputable predisposition to rearrangement at specific sites was not found in this study. Furthermore, an overall random association of constitutional rearrangement breakpoints in bands with known oncogenes and fragile sites was observed. However, the possibility of oncogenes and fragile sites as factors involved in constitutional rearrangements in a few isolated cases cannot be excluded. Nonrandomness was found when distribution of breakpoints in light and dark G bands was compared. An excess of breakpoints in some light G bands was observed even after a conservative correction for a possible pattern recognition bias which may lead to the overascertainment of breakpoints in light G bands. / Medicine, Faculty of / Medical Genetics, Department of / Graduate
9

A sequential decision procedure for computer identification of human chromosomes

Sherwood, Everett Morris, 1945- January 1976 (has links)
No description available.
10

Chromosomal DNA synthesis in cultured diploid human fibroblasts

Brody, Shirley, January 1969 (has links)
Thesis (Ph. D.)--University of Wisconsin--Madison, 1969. / Typescript. Vita. eContent provider-neutral record in process. Description based on print version record. Includes bibliography.

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