Your search keyword '"Kivirikko, S."' showing total 3 results

1. Genetic linkage of familial granulomatous inflammatory arthritis, skin rash, and uveitis to chromosome 16

Author

Gerard Tromp, Kuivaniemi H, Raphael S, Ala-Kokko L, Christiano A, Considine E, Dhulipala R, Hyland J, Jokinen A, Kivirikko S, Korn R, Madhatheri S, McCarron S, Pulkkinen L, Punnett H, Shimoya K, Spotila L, Tate A, and Cj, Williams

Subjects

Adult, Male, Granuloma, Adolescent, Genetic Linkage, Arthritis, Infant, Newborn, Chromosome Mapping, Infant, Syndrome, Skin Diseases, Pedigree, Uveitis, Humans, Female, Child, Chromosomes, Human, Pair 16, Research Article

Abstract

Blau syndrome (MIM 186580), first described in a large, three-generation kindred, is an autosomal, dominantly inherited disease characterized by multiorgan, tissue-specific inflammation. Its clinical phenotype includes granulomatous arthritis, skin rash, and uveitis and probably represents a subtype of a group of clinical entities referred to as "familial granulomatosis." It is the sole human model with recognizably Mendelian inheritance for a variety of multisystem inflammatory diseases affecting a significant percentage of the population. A genomewide search for the Blau susceptibility locus was undertaken after karyotypic analysis revealed no abnormalities. Sixty-two of the 74-member pedigree were genotyped with dinucleotide-repeat markers. Linkage analysis was performed under a dominant model of inheritance with reduced penetrance. The marker D16S298 gave a maximum LOD score of 3.75 at theta = .04, with two-point analysis. LOD scores for flanking markers were consistent and placed the Blau susceptibility locus within the 16p12-q21 interval.

Published

1996

2. Distribution of type XV collagen transcripts in human tissue and their production by muscle cells and fibroblasts

Author

Kivirikko S, Janna Saarela, Jc, Myers, Autio-Harmainen H, and Pihlajaniemi T

Subjects

Adult, Transcription, Genetic, Muscles, Placenta, RNA Probes, Fibroblasts, Blotting, Northern, Umbilical Cord, Fetus, Organ Specificity, Humans, Collagen, RNA, Messenger, Cells, Cultured, In Situ Hybridization, Research Article

Abstract

Type XV collagen is a recently identified member of the diverse family of collagens, its structure being characterized by extensive interruptions in the collagenous sequences. A combination of Northern blot hybridization of fetal and adult human tissues and in situ hybridization analyses of a fetus with Down's syndrome, several placentas, and adult skin were used to localize expression of its mRNAs. Northern blot analysis revealed marked expression in heart, skeletal muscle, and placenta tissues and moderate levels in the kidney and pancreas. Clear in situ hybridization signals were detected in fibroblasts and endothelial cells in all tissues studied. Examination of fetal heart, skeletal muscle, and smooth muscle tissues showed that the high type XV collagen mRNA level in the muscle RNA was localized not only to fibroblasts residing in the endomysium but also to myoblasts. Interestingly, type XV collagen mRNAs were also synthesized by certain epithelial cells in kidney, lung, pancreas, and placenta. It was the morphologically immature glomeruli in the kidney and the lower parts of the nephron, especially the collecting ducts, that contained these mRNAs but not the mature glomeruli or proximal tubules, suggesting differences in expression during development. These findings indicate a wide distribution of type XV collagen transcripts, the main producers being mesenchymally derived cells, particularly muscle cells and fibroblasts.

3. Genetic linkage of familial granulomatous inflammatory arthritis, skin rash, and uveitis to chromosome 16

Author

Tromp, G., Helena Kuivaniemi, Raphael, S., Ala-Kokko, L., Christiano, A., Considine, E., Dhulipala, R., Hyland, J., Jokinen, A., Kivirikko, S., Korn, R., Madhatheri, S., Mccarron, S., Pulkkinen, L., Punnett, H., Shimoya, K., Spotila, L., Tate, A., and Williams, C. J.