Your search keyword '"Tibor A. Rauch"' showing total 2 results

1. Disease-promoting and -protective genomic loci on mouse chromosomes 3 and 19 control the incidence and severity of autoimmune arthritis

Author

Timea Besenyei, Anna Laszlo, Tibor A. Rauch, Katalin Mikecz, V A Adarichev, Ferenc Boldizsár, and Tibor T. Glant

Subjects

Genetic Markers, Male, Quantitative Trait Loci, Immunology, Congenic, Arthritis, Locus (genetics), Biology, Quantitative trait locus, medicine.disease_cause, Article, Autoimmune Diseases, Autoimmunity, Mice, Mice, Congenic, Genetics, medicine, Animals, Humans, Genetics (clinical), Autoantibodies, Immunity, Cellular, Mice, Inbred BALB C, Chromosome Mapping, medicine.disease, Arthritis, Experimental, Chromosomes, Mammalian, genomic DNA, Cartilage, Phenotype, Chromosome 3, Genetic Loci, Genetic marker, Cytokines, Female, Proteoglycans, Disease Susceptibility

Abstract

Proteoglycan (PG)-induced arthritis (PGIA) is a murine model of rheumatoid arthritis. Arthritis-prone BALB/c mice are 100% susceptible, whereas the major histocompatibility complex-matched DBA/2 strain is completely resistant to PGIA. To reduce the size of the disease-suppressive loci for sequencing and to find causative genes of arthritis, we created a set of BALB/c.DBA/ 2-congenic/subcongenic strains carrying DBA/2 genomic intervals overlapping the entire Pgia26 locus on chromosome 3 (chr3) and Pgia23/Pgia12 loci on chr19 in the arthritis-susceptible BALB/c background. Upon immunization of these subcongenic strains and their wild-type (BALB/c) littermates, we identified a major Pgia26a sublocus on chr3 that suppressed disease onset, incidence and severity via controlling the complex trait of T-cell responses. The region was reduced to 3 Mbp (11.8 Mbp with flanking regions) in size and contained gene(s) influencing the production of a number of proinflammatory cytokines. Additionally, two independent loci (Pgia26b and Pgia26c) suppressed the clinical scores of arthritis. The Pgia23 locus (~3 Mbp in size) on chr19 reduced arthritis susceptibility and onset, and the Pgia12 locus (6 Mbp) associated with low arthritis severity. Thus, we have reached the critical sizes of arthritis-associated genomic loci on mouse chr3 and chr19, which are ready for high-throughput sequencing of genomic DNA.

Published

2012

2. How to find the real one

Author

Tibor A. Rauch and Ibolya Kiss

Subjects

Genetics, Spliceosome, Splice site mutation, Mature messenger RNA, Intron, Computational biology, Biology, General Biochemistry, Genetics and Molecular Biology, Neurology, RNA splicing, Human genome, Precursor mRNA, Gene, General Environmental Science

Abstract

The mature mRNA always carries nucleotide sequences that faithfully mirror the protein product according to the rules of the genetic code. However, in the chromosome, the nucleotide sequence that represents a certain protein is interrupted by additional sequences. Therefore, most eukaryotic genes are longer than their final mRNA products. The human genome project revealed that only a tiny portion of sequences serves as protein-coding region and almost one quarter of the genome is occupied by non-coding intervening sequences. The elimination of these non-coding regions from the precursor RNA in a process termed splicing must be extremely precise, because even a single nucleotide mistake may cause a fatal error. At present, two types of intervening sequences have been identified in protein-coding genes. One of them, the U2-dependent or major-class is prevalent and represents 99% of known sequences. The other one, the so-called U12-dependent or minor-class of introns, occurs in much lesser amounts in the genome. The basic problem of nuclear splicing concerns i/ the molecular mechanisms, which ensure that the coding regions are correctly recognized and spliced together; ii/ the principles and mechanisms that guarantee the high fidelity of the splicing system; iii/ the differences in the excision mechanisms of the two classes of introns. We are going to present models explaining how intervening sequences are accurately removed and the coding regions correctly juxtaposed. The two splicing mechanisms will also be compared.

Published

2003