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Complete genome sequence of Shewanella putrefaciens. Final report

Description: Seventy percent of the costs for genome sequencing Shewanella putrefaciens (oneidensis) were requested. These funds were expected to allow completion of the low-pass (5-fold) random sequencing and complete closure and annotation of the 200 kbp plasmid. Because of cost reduction that occurred during the period of this grant, these goals have been far exceeded. Currently, the S. putrefaciens genome is very nearly completely closed, even though the genome was significantly larger than expected and extremely repetitive. The entire genome sequence has been made BLAST searchable on the TIGR web page, and an extensive effort has been made to make data and analyses available to all researchers working on S. putrefaciens (oneidensis).
Date: April 1, 2001
Creator: Heidelberg, John F.
Partner: UNT Libraries Government Documents Department

Towards a Library of Standard Operating Procedures (SOPs) for (meta)genomic annotation

Description: Genome annotations describe the features of genomes and accompany sequences in genome databases. The methodologies used to generate genome annotation are diverse and typically vary amongst groups. Descriptions of the annotation procedure are helpful in interpreting genome annotation data. Standard Operating Procedures (SOPs) for genome annotation describe the processes that generate genome annotations. Some groups are currently documenting procedures but standards are lacking for structure and content of annotation SOPs. In addition, there is no central repository to store and disseminate procedures and protocols for genome annotation. We highlight the importance of SOPs for genome annotation and endorse a central online repository of SOPs.
Date: April 1, 2008
Creator: Kyrpides, Nikos; Angiuoli, Samuel V.; Cochrane, Guy; Field, Dawn; Garrity, George; Gussman, Aaron et al.
Partner: UNT Libraries Government Documents Department

Origins of the Human Genome Project

Description: The human genome project was borne of technology, grew into a science bureaucracy in the US and throughout the world, and is now being transformed into a hybrid academic and commercial enterprise. The next phase of the project promises to veer more sharply toward commercial application, harnessing both the technical prowess of molecular biology and the rapidly growing body of knowledge about DNA structure to the pursuit of practical benefits. Faith that the systematic analysis of DNA structure will prove to be a powerful research tool underlies the rationale behind the genome project. The notion that most genetic information is embedded in the sequence of CNA base pairs comprising chromosomes is a central tenet. A rough analogy is to liken an organism's genetic code to computer code. The coal of the genome project, in this parlance, is to identify and catalog 75,000 or more files (genes) in the software that directs construction of a self-modifying and self-replicating system -- a living organism.
Date: July 1, 1993
Creator: Cook-Deegan, Robert
Partner: UNT Libraries Government Documents Department

Third International E. coli genome meeting

Description: Proceedings of the Third E. Coli Genome Meeting are provided. Presentations were divided into sessions entitled (1) Large Scale Sequencing, Sequence Analysis; (2) Databases; (3) Sequence Analysis; (4) Sequence Divergence in E. coli Strains; (5) Repeated Sequences and Regulatory Motifs; (6) Mutations, Rearrangements and Stress Responses; and (7) Origins of New Genes. The document provides a collection of abstracts of oral and poster presentations.
Date: December 31, 1994
Partner: UNT Libraries Government Documents Department

An overview of the human genome project

Description: The human genome project is one of the most ambitious scientific projects to date, with the ultimate goal being a nucleotide sequence for all four billion bases of human DNA. In the process of determining the nucleotide sequence for each base, the location, function, and regulatory regions from the estimated 100,000 human genes will be identified. The genome project itself relies upon maps of the human genetic code derived from several different levels of resolution. Genetic linkage analysis provides a low resolution genome map. The information for genetic linkage maps is derived from the analysis of chromosome specific markers such as Sequence Tagged Sites (STSs), Variable Number of Tandem Repeats (VNTRs) or other polymorphic (highly informative) loci in a number of different-families. Using this information the location of an unknown disease gene can be limited to a region comprised of one million base pairs of DNA or less. After this point, one must construct or have access to a physical map of the region of interest. Physical mapping involves the construction of an ordered overlapping (contiguous) set of recombinant DNA clones. These clones may be derived from a number of different vectors including cosmids, Bacterial Artificial Chromosomes (BACs), P1 derived Artificial Chromosomes (PACs), somatic cell hybrids, or Yeast Artificial Chromosomes (YACs). The ultimate goal for physical mapping is to establish a completely overlapping (contiguous) set of clones for the entire genome. After a gene or region of interest has been localized using physical mapping the nucleotide sequence is determined. The overlap between genetic mapping, physical mapping and DNA sequencing has proven to be a powerful tool for the isolation of disease genes through positional cloning.
Date: January 1, 1994
Creator: Batzer, M. A.
Partner: UNT Libraries Government Documents Department

The genome of black cottonwood, Populus trichocarpa (Torr.&Gray)

Description: We report the draft genome of the black cottonwood tree, Populus trichocarpa. Integration of shotgun sequence assembly with genetic mapping enabled chromosome-scale reconstruction of the genome. Over 45,000 putative protein-coding genes were identified. Analysis of the assembled genome revealed a whole-genome duplication event, with approximately 8,000 pairs of duplicated genes from that event surviving in the Populus genome. A second, older duplication event is indistinguishably coincident with the divergence of the Populus and Arabidopsis lineages. Nucleotide substitution, tandem gene duplication and gross chromosomal rearrangement appear to proceed substantially slower in Populus relative to Arabidopsis. Populus has more protein-coding genes than Arabidopsis, ranging on average between 1.4-1.6 putative Populus homologs for each Arabidopsis gene. However, the relative frequency of protein domains in the two genomes is similar. Overrepresented exceptions in Populus include genes associated with disease resistance, meristem development, metabolite transport and lignocellulosic wall biosynthesis.
Date: September 1, 2006
Creator: Tuskan, G. A.; DiFazio, S.; Jansson, S.; Bohlmann, J.; Grigoriev,I.; Hellsten, U. et al.
Partner: UNT Libraries Government Documents Department

Algorithm for genome contig assembly. Final report

Description: An algorithm was developed for genome contig assembly which extended the range of data types that could be included in assembly and which ran on the order of a hundred times faster than the algorithm it replaced. Maps of all existing cosmid clone and YAC data at the Human Genome Information Resource were assembled using ICA. The resulting maps are summarized.
Date: September 1, 1995
Partner: UNT Libraries Government Documents Department

Controlling our destinies: Historical, philosophical, social and ethical perspectives on the Human Genome Project: Final report, July 1, 1995-June 30, 1996

Description: This report briefly describes the efforts by the organizing committee in preparation for the conference entitled Controlling Our Destinies: Historical, Philosophical, Social, and Ethical Perspectives on the Human Genome Project. The conference was held October 5-8, 1995.
Date: September 25, 1996
Creator: Sloan, P.R.
Partner: UNT Libraries Government Documents Department

Human genome education model project. Ethical, legal, and social implications of the human genome project: Education of interdisciplinary professionals

Description: This meeting was held June 10, 1996 at Georgetown University. The purpose of this meeting was to provide a multidisciplinary forum for exchange of state-of-the-art information on the human genome education model. Topics of discussion include the following: psychosocial issues; ethical issues for professionals; legislative issues and update; and education issues.
Date: December 31, 1996
Creator: Weiss, J.O. & Lapham, E.V.
Partner: UNT Libraries Government Documents Department

5. international workshop on the identification of transcribed sequences

Description: This workshop was held November 5--8, 1995 in Les Embiez, France. The purpose of this conference was to provide a multidisciplinary forum for exchange of state-of-the-art information on mapping the human genome. Attention is focused on the following topics: transcriptional maps; functional analysis; techniques; model organisms; and tissue specific libraries and genes. Abstracts are included of the papers that were presented.
Date: December 31, 1995
Partner: UNT Libraries Government Documents Department

Report of the fifth international workshop on human X chromosome mapping

Description: A high-quality integrated genetic and physical map of the X chromosome from telomere to telomere, based primarily on YACs formatted with probes and STSs, is increasingly close to reality. At the Fifth International X Chromosome Workshop, organized by A.M. Poustka and D. Schlessinger in Heidelberg, Germany, April 24--27, 1994, substantial progress was recorded on extension and refinement of the physical map, on the integration of genetic and cytogenetic data, on attempts to use the map to direct gene searches, and on nascent large-scale sequencing efforts. This report summarizes physical and genetic mapping information presented at the workshop and/or published since the reports of the fourth International X Chromosome Workshop. The principle aim of the workshop was to derive a consensus map of the chromosome, in terms of physical contigs emphasizing the location of genes and microsatellite markers. The resulting map is presented and updates previous versions. This report also updates the list of highly informative microsatellites. The text highlights the working state of the map, the genes known to reside on the X, and the progress toward integration of various types of data.
Date: December 31, 1994
Creator: Willard, H. F.; Cremers, F.; Mandel, J. L.; Monaco, A. P.; Nelson, D. L. & Schlessinger, D.
Partner: UNT Libraries Government Documents Department

Small genomes: New initiatives in mapping and sequencing. Workshop summary report

Description: The workshop was held 5--7 July 1993 at the Center for Advanced Research in Biotechnology (CARB) and hosted by the University of Maryland Biotechnology Institute (UMBI) and the National Institute of Standards and Technology (NIST). The objective of this workshop was to bring together individuals interested in DNA technologies and to determine the impact of these current and potential improvements of the speed and cost-effectiveness of mapping and sequencing on the planning of future small genome projects. A major goal of the workshop was to spur the collaboration of more diverse groups of scientists working on this topic, and to minimize competitiveness as an inhibitory factor to progress.
Date: December 31, 1993
Creator: McKenney, K. & Robb, F.
Partner: UNT Libraries Government Documents Department

The Genetic Privacy Act and commentary

Description: The Genetic Privacy Act is a proposal for federal legislation. The Act is based on the premise that genetic information is different from other types of personal information in ways that require special protection. The DNA molecule holds an extensive amount of currently indecipherable information. The major goal of the Human Genome Project is to decipher this code so that the information it contains is accessible. The privacy question is, accessible to whom? The highly personal nature of the information contained in DNA can be illustrated by thinking of DNA as containing an individual`s {open_quotes}future diary.{close_quotes} A diary is perhaps the most personal and private document a person can create. It contains a person`s innermost thoughts and perceptions, and is usually hidden and locked to assure its secrecy. Diaries describe the past. The information in one`s genetic code can be thought of as a coded probabilistic future diary because it describes an important part of a unique and personal future. This document presents an introduction to the proposal for federal legislation `the Genetic Privacy Act`; a copy of the proposed act; and comment.
Date: February 28, 1995
Creator: Annas, G.J.; Glantz, L.H. & Roche, P.A.
Partner: UNT Libraries Government Documents Department

The Human Genome Diversity (HGD) Project. Summary document

Description: In 1991 a group of human geneticists and molecular biologists proposed to the scientific community that a world wide survey be undertaken of variation in the human genome. To aid their considerations, the committee therefore decided to hold a small series of international workshops to explore the major scientific issues involved. The intention was to define a framework for the project which could provide a basis for much wider and more detailed discussion and planning--it was recognized that the successful implementation of the proposed project, which has come to be known as the Human Genome Diversity (HGD) Project, would not only involve scientists but also various national and international non-scientific groups all of which should contribute to the project`s development. The international HGD workshop held in Sardinia in September 1993 was the last in the initial series of planning workshops. As such it not only explored new ground but also pulled together into a more coherent form much of the formal and informal discussion that had taken place in the preceding two years. This report presents the deliberations of the Sardinia workshop within a consideration of the overall development of the HGD Project to date.
Date: December 31, 1993
Partner: UNT Libraries Government Documents Department

Human Genome Diversity Project. Summary of planning workshop 3(B): Ethical and human-rights implications

Description: The third planning workshop of the Human Genome Diversity Project was held on the campus of the US National Institutes of Health in Bethesda, Maryland, from February 16 through February 18, 1993. The second day of the workshop was devoted to an exploration of the ethical and human-rights implications of the Project. This open meeting centered on three roundtables, involving 12 invited participants, and the resulting discussions among all those present. Attendees and their affiliations are listed in the attached Appendix A. The discussion was guided by a schedule and list of possible issues, distributed to all present and attached as Appendix B. This is a relatively complete, and thus lengthy, summary of the comments at the meeting. The beginning of the summary sets out as conclusions some issues on which there appeared to be widespread agreement, but those conclusions are not intended to serve as a set of detailed recommendations. The meeting organizer is distributing his recommendations in a separate memorandum; recommendations from others who attended the meeting are welcome and will be distributed by the meeting organizer to the participants and to the Project committee.
Date: December 31, 1993
Partner: UNT Libraries Government Documents Department

[Genome plasticity and catabolic potential of pseudomonas cepacia]. Progress report

Description: This progress report describes efforts directed at understanding the genomic structure of Pseudomonas cepacia. Variously reported are descriptions of the replicons in the genome, organization of macrorestriction fragments comprising the genome, use of a Tn-5- 751S to insertionally inactivate and map selected genes, construction of IS407 derivatives containing a trimethoprim resistance marker and SwaI site, and analysis of nucleotide sequences of IS401 and IS408.
Date: December 31, 1993
Partner: UNT Libraries Government Documents Department

Final report: 'Rhodopseudomonas palustris' genome workshop to be held in Spring of 2001

Description: The ''Rhodopseudomonas palustris'' genome workshop took place in Iowa City on April 6-8, 2001. The purpose of the meeting was to instruct members of the annotation working group in approaches to accomplishing the 'human' phase of the 'R. palustris' genome annotation. A partial draft of a paper describing the 'Rhodopseudomonas palustris' genome has been written and a full version of the paper should be ready for submission by the end of the summer 2002.
Date: June 5, 2002
Creator: Harwood, Caroline S.
Partner: UNT Libraries Government Documents Department