Your search keyword '"Cline RT"' showing total 8 results

1. The structure of the presenilin 1 (S182) gene and identification of six novel mutations in early onset AD families

Author

Harry Houlden, Janet A. Johnston, Mike Hutton, Bengt Winblad, Jordi Pérez-Tur, Alonso Martínez, N Mehta, Ken Kosik, Karin Axelman, Lena Lilius, M. Arcos, C Humphreys, C Zehr, Alison Goate, Mark Raymond Adams, Julie S. Snowden, Corinne Lendon, Chad G. Pearson, Cline Rt, Venter Jc, Lotta Forsell, David G. Mann, Matti Viitanen, S Sarner, R Harvey, Lars Lannfelt, John Collinge, Lucia Madrigal, T Ashworth, Maria I. Behrens, Karen Duff, Robert Clark, John Hardy, George Roberts, Nick C. Fox, Dennis W. Dickson, Kevin M. Korenblat, John C. Morris, Sue Froelich, Amanda J. Myers, Martin N. Rossor, Richard Crook, Minna Pöyhönen, Francisco Lopera, Christopher Talbot, Phillips Ca, Michelle Wragg, M Baker, P Roques, C He, Jorge Ossa, Adriana Ruiz, D Neary, F. Busfield, Joanne Norton, Rebecca A. Fuldner, Eric Karran, A Kennedy, Matti Haltia, Guy Prihar, R Cowburn, Peter L. Lantos, and Sarah Lincoln

Subjects

Genetic Linkage, Molecular Sequence Data, Pedigree chart, Biology, Polymerase Chain Reaction, Presenilin, 03 medical and health sciences, 0302 clinical medicine, Genetic linkage, Alzheimer Disease, Genetics, Presenilin-1, Humans, Point Mutation, Family, Amino Acid Sequence, Age of Onset, Gene, 030304 developmental biology, Early onset, DNA Primers, Chromosomes, Human, Pair 14, 0303 health sciences, Genomic Library, Base Sequence, Alternative splicing, Age Factors, Chromosome, Chromosome Mapping, Membrane Proteins, Exons, Introns, Pedigree, Alternative Splicing, Human genome, 030217 neurology & neurosurgery

Abstract

Genetic linkage studies place a gene causing early onset familial Alzheimer's disease (FAD) on chromosome 14q24.3 (refs 1–4). Five mutations within the S182 (Presenilin 1: PS–1) gene, which maps to this region, have recently been reported in several early onset FAD kindreds5. We have localized the PS-1 gene to a 75 kb region and present the structure of this gene, evidence for alternative splicing and describe six novel mutations in early onset FAD pedigrees all of which alter residues conserved in the STM26 (Presenilin 2: PS-2) gene.

Published

1995

2. Involvement of Streptococcus mutans regulator RR11 in oxidative stress response during biofilm growth and in the development of genetic competence.

Author

Perry JA, Lévesque CM, Suntharaligam P, Mair RW, Bu M, Cline RT, Peterson SN, and Cvitkovitch DG

Subjects

Bacterial Proteins genetics, Gene Expression Profiling, Gene Knockout Techniques, Oligonucleotide Array Sequence Analysis, Signal Transduction, Bacterial Proteins physiology, Biofilms growth & development, Gene Expression Regulation, Bacterial, Oxidative Stress, Streptococcus mutans physiology, Transformation, Bacterial

Abstract

Aims: To identify the genes regulated by RR11, the regulator of the Streptococcus mutans HK/RR11 two-component system., Methods and Results: The S. mutans RR11-encoding gene was inactivated, and the effects of gene disruption on the cell's ability to form biofilms under stresses and acquire extracellular DNA were tested. Biofilm was reduced in cells lacking RR11 following exposure to oxidative stress. RR11-defective cells showed approx. 20-fold reduction in transformation efficiency. Microarray used to decipher the RR11-regulated genes in biofilm showed that approx. 5% of the UA159 genome underwent a significant change in expression. RR11 was found to regulate 174 genes, including genes involved in competence, stress-response and cell division., Conclusions: Target genes controlled by RR11during biofilm growth have been identified by a comparison of transcriptional profiles between an RR11 defective mutant and the parental strain. The results demonstrated that RR11 is involved in the control of diverse cellular processes, including the formation of biofilm under oxidative stress and development of genetic competence., Significance and Impact of the Study: The regulator of HK/RR11 system controls a large regulon and is an important regulator involved in stress response during S. mutans biofilm growth enabling the survival and persistence of its progeny in the microbial community.

Published

2008

3. Phase variable desialylation of host proteins that bind to Streptococcus pneumoniae in vivo and protect the airway.

Author

King SJ, Hippe KR, Gould JM, Bae D, Peterson S, Cline RT, Fasching C, Janoff EN, and Weiser JN

Subjects

Animals, Bacterial Proteins metabolism, Blood microbiology, Humans, Nasopharynx microbiology, Oligonucleotide Array Sequence Analysis methods, Pneumonia, Pneumococcal microbiology, Rats, Streptococcus pneumoniae genetics, Immunoglobulin A metabolism, Lactoferrin metabolism, N-Acetylneuraminic Acid metabolism, Neuraminidase metabolism, Secretory Component metabolism, Streptococcus pneumoniae growth & development, Streptococcus pneumoniae pathogenicity

Abstract

Most clinical isolates of Streptococcus pneumoniae consist of heterogeneous populations of at least two colony phenotypes, opaque and transparent, selected for in the bloodstream and nasopharynx, respectively. Microarray analysis revealed 24 orfs that demonstrated differences in expression greater than twofold between variants of independent strains. Twenty-one of these showed increased expression in the transparent variants, including 11 predicted to be involved in sugar metabolism. A single genomic region contains seven of these loci including the gene that encodes the neuraminidase, NanA. In contrast to previous studies, there was no contribution of NanA to adherence of S. pneumoniae to epithelial cells or colonization in an animal model. However, we observed NanA-dependent desialylation of human airway components that bind to the organism and may mediate bacterial clearance. Targets of desialylation included human lactoferrin, secretory component, and IgA2 that were shown to be present on the surface of the pneumococcus in vivo during pneumococcal pneumonia. The efficiency of desialylation was increased in the transparent variants and enhanced for host proteins binding to the surface of S. pneumoniae. Because deglycosylation affects the function of many host proteins, NanA may contribute to a protease-independent mechanism to modify bound targets and facilitate enhanced survival of the bacterium.

Published

2004

4. Complete genome sequence and comparative genomic analysis of an emerging human pathogen, serotype V Streptococcus agalactiae.

Author

Tettelin H, Masignani V, Cieslewicz MJ, Eisen JA, Peterson S, Wessels MR, Paulsen IT, Nelson KE, Margarit I, Read TD, Madoff LC, Wolf AM, Beanan MJ, Brinkac LM, Daugherty SC, DeBoy RT, Durkin AS, Kolonay JF, Madupu R, Lewis MR, Radune D, Fedorova NB, Scanlan D, Khouri H, Mulligan S, Carty HA, Cline RT, Van Aken SE, Gill J, Scarselli M, Mora M, Iacobini ET, Brettoni C, Galli G, Mariani M, Vegni F, Maione D, Rinaudo D, Rappuoli R, Telford JL, Kasper DL, Grandi G, and Fraser CM

Subjects

Amino Acid Sequence, Biological Evolution, Humans, Molecular Sequence Data, Oligonucleotide Array Sequence Analysis, Phylogeny, Serotyping, Species Specificity, Streptococcal Infections microbiology, Streptococcus agalactiae classification, Streptococcus pneumoniae genetics, Streptococcus pyogenes genetics, Virulence genetics, Genome, Bacterial, Streptococcus agalactiae genetics, Streptococcus agalactiae pathogenicity

Abstract

The 2,160,267 bp genome sequence of Streptococcus agalactiae, the leading cause of bacterial sepsis, pneumonia, and meningitis in neonates in the U.S. and Europe, is predicted to encode 2,175 genes. Genome comparisons among S. agalactiae, Streptococcus pneumoniae, Streptococcus pyogenes, and the other completely sequenced genomes identified genes specific to the streptococci and to S. agalactiae. These in silico analyses, combined with comparative genome hybridization experiments between the sequenced serotype V strain 2603 V/R and 19 S. agalactiae strains from several serotypes using whole-genome microarrays, revealed the genetic heterogeneity among S. agalactiae strains, even of the same serotype, and provided insights into the evolution of virulence mechanisms.

Published

2002

5. Gene expression analysis of the Streptococcus pneumoniae competence regulons by use of DNA microarrays.

Author

Peterson S, Cline RT, Tettelin H, Sharov V, and Morrison DA

Subjects

Bacterial Proteins metabolism, Gene Expression Profiling, Genes, Bacterial, Mutation, RNA, Bacterial genetics, RNA, Messenger analysis, Transformation, Genetic, Bacterial Proteins genetics, Oligonucleotide Array Sequence Analysis, Regulon genetics, Streptococcus pneumoniae genetics

Abstract

Competence for genetic transformation in Streptococcus pneumoniae is coordinated by the competence-stimulating peptide (CSP), which induces a sudden and transient appearance of competence during exponential growth in vitro. Models of this quorum-sensing mechanism have proposed sequential expression of several regulatory genes followed by induction of target genes encoding DNA-processing-pathway proteins. Although many genes required for transformation are known to be expressed only in response to CSP, the relative timing of their expression has not been established. Overlapping expression patterns for the genes cinA and comD (G. Alloing, B. Martin, C. Granadel, and J. P. Claverys, Mol. Microbiol. 29:75-83, 1998) suggest that at least two distinct regulatory mechanisms may underlie the competence cycle. DNA microarrays were used to estimate mRNA levels for all known competence operons during induction of competence by CSP. The known competence regulatory operons, comAB, comCDE, and comX, exhibited a low or zero initial (uninduced) signal, strongly increased expression during the period between 5 and 12 min after CSP addition, and a decrease nearly to original values by 15 min after initiation of exposure to CSP. The remaining competence genes displayed a similar expression pattern, but with an additional delay of approximately 5 min. In a mutant defective in ComX, which may act as an alternate sigma factor to allow expression of the target competence genes, the same regulatory genes were induced, but the other competence genes were not. Finally, examination of the expression of 60 candidate sites not previously associated with competence identified eight additional loci that could be induced by CSP.

Published

2000

6. Global transposon mutagenesis and a minimal Mycoplasma genome.

Author

Hutchison CA, Peterson SN, Gill SR, Cline RT, White O, Fraser CM, Smith HO, and Venter JC

Subjects

ATP-Binding Cassette Transporters genetics, ATP-Binding Cassette Transporters metabolism, Amino Acyl-tRNA Synthetases genetics, Bacterial Proteins genetics, Chromosome Mapping, DNA Polymerase III genetics, DNA Polymerase III metabolism, DNA Replication genetics, Glycolysis genetics, Lipoproteins genetics, Mycoplasma metabolism, Mycoplasma pneumoniae genetics, Mycoplasma pneumoniae metabolism, Ribosomal Proteins genetics, Transcription, Genetic, DNA Transposable Elements, Genes, Essential, Genome, Bacterial, Mutagenesis, Insertional, Mycoplasma genetics

Abstract

Mycoplasma genitalium with 517 genes has the smallest gene complement of any independently replicating cell so far identified. Global transposon mutagenesis was used to identify nonessential genes in an effort to learn whether the naturally occurring gene complement is a true minimal genome under laboratory growth conditions. The positions of 2209 transposon insertions in the completely sequenced genomes of M. genitalium and its close relative M. pneumoniae were determined by sequencing across the junction of the transposon and the genomic DNA. These junctions defined 1354 distinct sites of insertion that were not lethal. The analysis suggests that 265 to 350 of the 480 protein-coding genes of M. genitalium are essential under laboratory growth conditions, including about 100 genes of unknown function.

Published

1999

7. Alanine scanning mutagenesis of conserved arginine/lysine-arginine/lysine-X-X-arginine/lysine G protein-activating motifs on m1 muscarinic acetylcholine receptors.

Author

Lee NH, Geoghagen NS, Cheng E, Cline RT, and Fraser CM

Subjects

Amino Acid Sequence, Animals, Base Sequence, Binding Sites, Binding, Competitive, CHO Cells, Carbachol pharmacology, Cell Membrane metabolism, Conserved Sequence, Cricetinae, DNA Primers, Guanosine Triphosphate pharmacology, Kinetics, Molecular Sequence Data, Mutagenesis, Site-Directed, N-Methylscopolamine, Oxotremorine pharmacology, Protein Structure, Secondary, Quinuclidinyl Benzilate metabolism, Receptor, Muscarinic M2, Receptors, Muscarinic biosynthesis, Receptors, Muscarinic chemistry, Recombinant Proteins chemistry, Recombinant Proteins metabolism, Scopolamine Derivatives metabolism, Second Messenger Systems, Transfection, Alanine, GTP-Binding Proteins metabolism, Receptors, Muscarinic physiology

Abstract

Alanine scanning mutagenesis of B-B-X-X-B motifis (where B is a basic residue and X is any nonbasic residue) in m1 muscarinic acetylcholine receptors was performed to determine the relative roles of basic amino acids in receptor coupling. This conserved motif is found in many G protein-coupled receptors and has been implicated in G protein activation. The KKAAR365 motif, located at the carboxyl-terminal third intracellular loop of m1 receptors, was mutated to AAAAA365, thereby generating a triple-substitution mutant devoid of ability to stimulate either phosphoinositide (PI) hydrolysis or cAMP accumulation. In contrast, a triple-alanine substitution of the KRTPR140 motif in the carboxyl-terminal second intracellular loop, yielding mutant AATPA140, had no effect on receptor coupling to the two independent second messenger pathways. Analysis of a series of single- and double-substitution mutants demonstrate that all three basic residues of the KKAAR365 motif participate in efficient m1 receptor coupling. The presence of second and third basic residues in this motif was absolutely critical for full agonist recognition of a high and low affinity state of the receptor. Mutation of either Lys362 or Lys365, but not-Lys361, abolished guanine nucleotide-dependent conversion of agonist affinity states and correlated with an inability of full agonists to fully activate PI hydrolysis. The different combinatorial double-substitution mutants also revealed that Lys365 was necessary but not sufficient, in the context of the KKAAR365 motif, for efficient receptor coupling. This residue cannot facilitate full agonist-stimulated Pl hydrolysis in the absence of both Lys361 and Lys362. In comparison, the critical residue Lys362 was both necessary and sufficient. Substitution of nearby basic residues Lys361 and Lys365 with alanine yielded mutant AKAAA365, which exhibited partial ability to couple PI hydrolysis after full agonist stimulation. Therefore, Lys365 seems to function in a hierarchal (interdependent) manner with nearby basic residues, whereas Lys361 and Lys362 can act independent of surrounding basic residues to facilitate partial m1 receptor coupling after full agonist stimulation. In contrast, all three residues must be present for stimulation of PI hydrolysis by a partial agonist.

Published

1996

8. Complete analysis of the presenilin 1 gene in early onset Alzheimer's disease.

Author

Hutton M, Busfield F, Wragg M, Crook R, Perez-Tur J, Clark RF, Prihar G, Talbot C, Phillips H, Wright K, Baker M, Lendon C, Duff K, Martinez A, Houlden H, Nichols A, Karran E, Roberts G, Roques P, Rossor M, Venter JC, Adams MD, Cline RT, Phillips CA, and Goate A

Subjects

Alzheimer Disease metabolism, Base Sequence, Cluster Analysis, DNA Primers, Exons physiology, Genetic Linkage, Genome, Humans, Ireland, Membrane Proteins metabolism, Molecular Sequence Data, Mutation, Open Reading Frames, Presenilin-1, United Kingdom, Alzheimer Disease genetics, Membrane Proteins genetics

Abstract

The presenilin 1 gene has recently been identified as the locus on chromosome 14 which is responsible for a large proportion of early onset, autosomal dominantly inherited Alzheimer's disease (AD). We have elucidated the intron/exon structure of the gene and designed intronic primers to enable direct sequencing of the entire coding region (10 exons) of the presenilin gene in a large number of families. This strategy has enabled us to find a further two novel mutations in the gene. We discuss the distribution of mutations and the proportions of autosomal dominant AD with a mean age of onset below 60 years caused by mutations in this gene.

Published

1996