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Start Over Author "Ben F. Koop" Journal molecular phylogenetics and evolution
5 results on '"Ben F. Koop"'

1. Analysis and Comparison of the Mouse and Human Immunoglobulin Heavy Chain JH–Cμ–Cδ Locus

Author

T.D. Durfee, Frederick R. Blattner, J. Bansberg, A. Clausell, H.-L. Chen, A C Gilliam, Julia E. Richards, Ben F. Koop, J. Wells, and Philip W. Tucker

Subjects
Immunoglobulin delta-Chains, Inverted repeat, Molecular Sequence Data, Locus (genetics), Biology, Mice, Intergenic region, Sequence Homology, Nucleic Acid, Genetics, Animals, Humans, Coding region, Molecular Biology, Gene, Ecology, Evolution, Behavior and Systematics, Base Sequence, Genes, Immunoglobulin, Immunoglobulin mu-Chains, Chromosome Mapping, DNA, Molecular biology, Immunoglobulin J-Chains, Immunoglobulin heavy chain, Immunoglobulin Heavy Chains, Immunoglobulin J Chain
Abstract

We report here 23,686 bases of contiguous DNA sequences from the mouse germline immunoglobulin heavy chain (H) constant (C) mu delta region. The sequence spans the joining (JH) regions, the mu constant region (C mu), the delta constant region (C delta) coding regions, a domain relic, the mu switch region (S mu), seven blocks of simple sequence repeats, a large unique sequence inverted repeat, a large unique sequence forward repeat, and all of the intervening material. A comparison of this 23.7-kb region with the corresponding human C mu/C delta region reveals clear homology in the coding and introns of C mu but not in the 5' flanking J gene segments nor in the intergenic and C delta regions. This mixed pattern of similarity between the human and the mouse sequences contrasts with high levels of similarity found in the T-cell receptor C alpha/C delta region and alpha and beta myosin genes and the very low levels found in the gamma-crystallin, XRCC1, and beta-globin gene clusters. The human and mouse comparison further suggests the incorporation of novel sequences into expressed genes of IgD.

Published
1996
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2. Partial 28S rDNA sequences and the antiquity of hydrothermal vent endemic gastropods

Author

Ben F. Koop and Andrew G. McArthur

Subjects
Molecular Sequence Data, DNA, Ribosomal, Evolution, Molecular, Patellogastropoda, 28S ribosomal RNA, Sequence Homology, Nucleic Acid, RNA, Ribosomal, 28S, Genetics, Animals, Heterobranchia, Molecular Biology, Ecology, Evolution, Behavior and Systematics, Phylogeny, biology, Phylogenetic tree, Vetigastropoda, Base Sequence, Ecology, Euthyneura, Sequence Analysis, DNA, biology.organism_classification, Evolutionary biology, Mollusca, Valvata, Architaenioglossa, Sequence Alignment
Abstract

A molecular phylogenetic investigation of the hypothesized antiquity of the hydrothermal vent endemic Neomphalina (Mollusca; Gastropoda) is reported. Sequences of two domains of the gene encoding for 28S ribosomal RNA were acquired for 3 outgroup and 32 gastropod genera. Use of the likelihood ratio test indicated complex substitution patterns for these domains and taxa, corresponding to a general time-reversible model with among-site rate variation. Phylogenetic analyses were performed using this model under maximum likelihood criteria. The data lacked resolution of gastropod radiations of the Paleozoic and all three of the outgroup sequences were randomized relative to the ingroup. Acceleration of evolutionary rates had additionally randomized the sequences of the Patellogastropoda relative to the other Gastropoda. The data resolved radiations of the Mesozoic and supported monophyly of the sampled Neritopsina, Vetigastropoda, Neomphalina, Caenogastropoda (including Campanile and the Architaenioglossa), and Heterobranchia (Valvata + Euthyneura), although several results were not significantly different from nonmonophyletic alternatives. Mesozoic origins of the hydrothermal vent endemic Neomphalina are preliminarily supported and implications for the hydrothermal vent refugia hypothesis discussed. Issues related to phylogenetic resolution of the Gastropoda are additionally discussed.

Published
1999

3. The structure and evolution of the ribosomal proteins encoded in the spc operon of the archaeon (Crenarchaeota) Sulfolobus acidocaldarius

Author

Alastair T. Matheson, Isolde Kusser, Decheng Yang, Andreas K.E. Köpke, and Ben F. Koop

Subjects
Sulfolobus acidocaldarius, Ribosomal Proteins, Operon, Archaeal Proteins, Molecular Sequence Data, Regulatory Sequences, Nucleic Acid, Genes, Archaeal, Sulfolobus, Evolution, Molecular, Start codon, Crenarchaeota, Ribosomal protein, Genetics, Animals, Amino Acid Sequence, Cloning, Molecular, Codon, Molecular Biology, Ecology, Evolution, Behavior and Systematics, Phylogeny, Base Composition, biology, Sequence Analysis, DNA, biology.organism_classification, Eukaryotic Cells, Genes, Bacterial, Euryarchaeota, Archaea
Abstract

The genes for nine ribosomal proteins, L24, L5, S14, S8, L6, L18, S5, L30, and L15, have been isolated and sequenced from the spc operon in the archaeon (Crenarchaeota) Sulfolobus acidocaldarius, and the putative amino acid sequence of the proteins coded by these genes has been determined. In addition, three other genes in the spc operon, coding for ribosomal proteins S4E, L32E, and L19E (equivalent to rat ribosomal proteins S4, L32, and L19), were sequenced and the structure of the putative proteins was determined. The order of the ribosomal protein genes in the spc operon of the Crenarchaeota kingdom of Archaea is identical to that present in the Euryarchaeota kingdom of Archaea and also identical to that found in bacteria, except for the genes for r-proteins S4E, L32E, and L19E, which are absent in bacteria. Although AUG is the initiation codon in most of the spc genes, GUG (val) and UUG (leu) are also used as initiation codons in S. acidocaldarius. Over 70% of the codons in the Sulfolobus spc operon have A or U in the third position, reflecting the low GC content of Sulfolobus DNA. Phylogenetic analysis indicated that the archaeal r-proteins are a sister group of their eucaryotic counterparts but did not resolve the question of whether the Archaea is monophyletic, as suggested by the L6P, L15P, and L18P trees, or the question of whether the Crenarchaeota is separate from the Euryarchaeota and closer to the Eucarya, as suggested by the S8P, S5P, and L24P trees. In the case of the three Sulfolobus r-proteins that do not have a counterpart in the bacterial ribosome (S4E, L32E, and L19E), the archaeal r-proteins showed substantial identity to their eucaryotic equivalents, but in all cases the archaeal proteins formed a separate group from the eucaryotic proteins.

Published
1999

4. Evolution and selection of primate T cell antigen receptor BV8 gene subfamily

Author

Leroy Hood, Patrick Charmley, Duane Martindale, Jerry L. Slightom, William K. Funkhouser, and Ben F. Koop

Subjects
Nonsynonymous substitution, Adult, Primates, Receptors, Antigen, T-Cell, alpha-beta, Molecular Sequence Data, Restriction Mapping, Biology, Evolution, Molecular, Negative selection, Gene duplication, Gene cluster, Genetics, Animals, Humans, Gene conversion, Selection, Genetic, Molecular Biology, Gene, Ecology, Evolution, Behavior and Systematics, Phylogeny, Gene Rearrangement, Polymorphism, Genetic, Base Sequence, T-cell receptor, Genetic Variation, FOSL1, Germ Cells, Multigene Family, Sequence Alignment
Abstract

The set of potential T cell receptor specificities is highly diverse. The relative contributions of T cell receptor (TCR) Vβ gene segment polymorphisms, duplications, deletions, and gene conversions to this final T cell receptor protein diversity are unknown. To study these mechanisms, we sequenced and compared closely related primate TCR gene segments from BV8S1, S2, and S5. Interspecies comparisons show that these gene segments have sustained multiple duplication, gene conversion, and deletion events during the last 35 million years of anthropoid primate evolution. BV8 coding sequences are generally conserved with respect to their flanking noncoding sequences, but we find no evidence for positive or negative selection in sequences coding for the first two putative complementarity-determining (ligand-binding) regions. Sequences of TCRBV8 gene segments from unrelated humans demonstrate no nonsynonymous substitutions in nonleader regions of either the BV8S1 or S2 gene segments. We conclude that gene duplication, deletion, and conversion mechanisms contribute in a substantial way to the overall diversity of the TCRBV8 gene segment repertoire in primate evolution and that germline substitutions and consequent polymorphisms in CDRs 1 and 2 of these gene segments probably do not play an active role in generating TCR β chain protein variation.

Published
1997

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