The effects of age on sister-chromatid-exchange

Trent, Jeffrey M.

January 1976

No description available.

Chromosome replication.

Molecular study of the deleted in liver cancer 2 (DLC2)h[electronic resource] : solution structure of the SAM domain and interaction with MCM7 /

Fung, King-leung.

January 2005

Thesis (Ph. D.)--University of Hong Kong, 2006. / Title proper from title frame. Also available in printed format.

Mathematical modelling of chromosome replication and replicative stress

Karschau, Jens

January 2013

Previous theoretical work on DNA replication neglected how the starting points (origins) take their place and how replication time is a ected when origins fail to activate. It is however crucial that origin loci are chosen so that too large gaps between them are avoided; otherwise the time until completion of chromosome replication becomes much longer than is allowed by the cell cycle. We investigate what the optimal origin location should be depending on the likelihood of origins failing. We show analytically and numerically that there exist regimes for origins, either to be positioned together in groups spaced far away from the next, or as equally scattered single origins depending on the uncertainty when activation occurs. The model reproduces origin distributions of frog embryos which are thought to be random, and shows contrarily that grouping must occur in order to swiftly complete replication; known as the random completion problem. The model also holds when considering a circular DNA topology for archaeal genomes, as well as if applied to the whole replication pro ling data of yeast. We study how an optimal origin distribution can arise and propose a mechanism to solve the random completion problem. We show that regular spacing emerges as an inherent property of the car parking model. We introduce a spatial requirement for origins to bind to DNA; origins occupy space on the DNA and can only bind stably if there is su cient space for them. Such a model leads to a well ordered origin distribution with minimal gaps as required for on time DNA replication in frog embryos. The optimal origin distribution emerges directly from our model because origins have a higher chance to bind to large empty regions instead of small once, therefore destroying large inter origin gaps. We also introduce a model to account for the interaction of replication forks with each other which leads to their assembly into replication factories. We show using Boltzmann statistics that their assembly is stochastic. A rst model only considers two pairs of forks which we then extend to describe properties of measured experimental distributions such as fork numbers per factory during on a whole yeast genome approach. Our in silico distribution of forks per factory matches in vivo data well; which suggests that active forks encounter each other randomly for an association into replication factories.

530

Chromosome replication

PURIFICATION AND CHARACTERIZATION OF BACTERIAL PHAGE PHI29 GENE 6 PROTEIN.

HODGES-GARCIA, YVONNE KATHLEEN.

January 1986

A DNA fragment containing the coding region for gene 6 of Bacterial phage ϕ29 was placed into an expression vector. The ϕ29 gene 6 protein was isolated in large amounts by chromatography on double-stranded DNA cellulose and DE52 cellulose. The ϕ29 gene 6 protein was determined to be greater 95% pure and has a molecular weight of approximately 16,000. The ϕ29 gene 6 protein is thought to be a dimer in its native form. The partial N-terminal amino acid sequence of the purified protein is identically to the inferred amino acid sequence from the nucleotide sequence of ϕ29 gene 6. Gene 6 protein of ϕ29 aggregates in a more purified state which suggest protein to protein interactions. Purified gene 6 protein did not stimulate the ϕ29 in vitro DNA replication system and may require binding with other replication proteins to enable it to function. Gene 6 protein binds weakly to double-stranded and single-strand DNA cellulose. There is segmental amino acid sequence and secondary structure homology with adenovirus DNA binding protein Antibody to gene 6 protein inhibits it from binding to ϕ29 DNA. The results presented in this dissertation suggest that ϕ29 gene 6 protein is a weak DNA bind protein and may not be required for the in vitro ϕ29 DNA replication system.

DNA.

Molecular genetics.

Chromosome replication.

TRISOMICS IN THE PROGENY OF DESYNAPTIC MUTANTS OF HORDEUM VULGARE.

Eckhoff, Joyce Lynne Alwine.

January 1982

No description available.

Barley -- Genetics.

Trisomy.

Chromosome replication.

Selfishness in moderation for self-propagation the yeast plasmid purloins the host mitotic apparatus for its segregation /

Mehta, Shwetal Vatsal, Jayaram, Makkuni,

January 2003

Thesis (Ph. D.)--University of Texas at Austin, 2003. / Supervisor: Makkuni Jayaram. Vita. Includes bibliographical references. Also available from UMI.

Selfishness in moderation for self-propagation : the yeast plasmid purloins the host mitotic apparatus for its segregation

Mehta, Shwetal Vatsal, 1973-

13 July 2011

Not available / text

Saccharomyces cerevisiae

Plasmids

Chromosome replication

Temporal and morphologic sequence of DNA replication in the mammalian chromosome complements.

Sinha, Anil K.

January 1965

Almost a decade ago, Breuer and Pavan (1955) reported for the first time that during larval growth DNA synthesis proceeds disproportionately along polytene chromosomes of Rhynochosciara (R. angelae). In such chromosomes, treated by Feulgen reaction, the intensity of stain appeared heavier at the points where the bulbs were formed, thus indicating localized accumulation of DNA molecules. [...]

Genetics.

Genetics.

Chromosome replication.

DNA.

Temporal and morphologic sequence of DNA replication in the mammalian chromosome complements.

Sinha, Anil K.

January 1965

No description available.

Chromosome replication.

DNA.

Genetics.

Genetics.

ANALYSIS OF THE X-Y SYNAPTONEMAL COMPLEX IN PEROMYSCUS.

Hicken, Suzanne.

January 1983

No description available.

Sex chromosomes.

Meiosis.

Peromyscus.

Chromosome replication.