Your search keyword '"Assum G"' showing total 5 results

1. Analysis of human extrachromosomal DNA elements originating from different beta-satellite subfamilies.

Author

Assum G, Fink T, Steinbeisser T, and Fisel KJ

Subjects

Base Sequence, Blotting, Southern, Consensus Sequence, Female, Heterochromatin, Humans, Male, Molecular Sequence Data, Repetitive Sequences, Nucleic Acid, Sequence Analysis, DNA, DNA, Circular analysis, DNA, Satellite analysis, Extrachromosomal Inheritance

Abstract

By screening total human DNA with probes derived from the small polydisperse circular (spc) DNA fraction of cultured human cells, we identified three clones that carry long stretches of beta-satellite DNA. Further experiments have shown that the three sequences belong to at least two different beta-satellite subfamilies, which are characterized by different higher order subunits. Members of one of these subfamilies are located in the cytological satellites of all acrocentric chromosomes, whereas members of another are located on the short arms of the acrocentrics on both sides of the stalk regions and also in the centromeric regions of chromosomes 1 and 9. This is the first time that beta-satellite sequences obtained from the spcDNA of human cells have been assigned to beta-satellite subfamilies that are organized as long arrays of tandemly arranged higher order monomers. This indicates that beta-satellite sequences can be excised from their chromosomal loci via intrastrand-recombination processes.

Published

1993

2. Increased amount and contour length distribution of small polydisperse circular DNA (spcDNA) in Fanconi anemia.

Author

Motejlek K, Schindler D, Assum G, and Krone W

Subjects

Adolescent, Adult, Cells, Cultured, Child, Child, Preschool, DNA, Circular ultrastructure, Female, Fibroblasts, Humans, Male, DNA, Circular metabolism, Fanconi Anemia genetics

Abstract

Small polydisperse circular DNA (spcDNA) in Fanconi anemia (FA) was analyzed from cultured fibroblast-like cells by electron microscopy. Application of the mica-press adsorption technique for the semi-quantitative determination of spcDNA amounts to three FA and three normal control skin-derived fibroblast strains revealed 85-fold increased levels of spcDNA in the FA cells. An even higher excess over controls was suggested when the FA fibroblasts were propagated for up to 11 serial in vitro passages, consistent with the short replicative life-span of primary FA cells and their rapid transition into a poorly dividing state, in which spcDNA reportedly further increases. In addition, contour length distributions of gradient-purified spcDNA preparations from five FA fibroblast strains were compared with those from five normal control strains. Mean spcDNA contour lengths were significantly greater in the FA than in the control cells. The reported findings of increased spcDNA amounts and sizes in FA coincide with a similar association of chromosome instability and abnormal spcDNA formation previously observed in cultured cells derived from angiofibromas in tuberous sclerosis. Circumstantial evidence from the present study in the paradigmatic chromosome breakage syndrome FA further supports the suggestion that a common mechanism underlies chromosome instability and the surplus generation of spcDNA. Notably, this apparent mechanism is functional in homonuclear primary cell strains with a distinct inherited basis of their chromosome instability, and is not restricted to heteroploid and neoplastoid cell lines.

Published

1993

3. The size of small polydisperse circular DNA (spcDNA) in angiofibroma-derived cell cultures from patients with tuberous sclerosis (TSC) differs from that in fibroblasts.

Author

Motejlek K, Assum G, Krone W, and Kleinschmidt AK

Subjects

Adult, Fibroblasts chemistry, Humans, Male, Tumor Cells, Cultured, DNA, Circular chemistry, DNA, Neoplasm chemistry, Histiocytoma, Benign Fibrous chemistry, Skin chemistry, Tuberous Sclerosis genetics

Abstract

Cell cultures were derived from angiofibromas of three patients with tuberous sclerosis (TSC), from the unaffected skin of these patients, and from the skin of five healthy donors. The length distributions of the small polydisperse circular DNA (spcDNA) fraction of these cell cultures were then analyzed. Nearly half the spcDNA molecules from the angiofibroma cultures were longer than 0.4 micron, whereas only about 7% exceeded this threshold in the spcDNA preparations from the skin fibroblast cultures. The percentage of the larger size class of spcDNA showed an increase at higher numbers of in vitro passages in all three types of cultures, but this effect was much more conspicuous in the angiofibroma-derived cultures than in those from the skin fibroblasts. An age-dependent increase in the overall amount of spcDNA was only seen in the angiofibroma-derived cultures. Our earlier finding of elevated amounts of spcDNA in angiofibroma cultures was confirmed in cultures from an additional TSC patient.

Published

1991

4. Increased amounts of small polydisperse circular DNA (spcDNA) in angiofibroma-derived cell cultures from patients with tuberous sclerosis (TS)

Author

Neidlinger C, Assum G, Krone W, Dietrich C, Hochsattel R, and Klotz G

Subjects

Adult, Cells, Cultured, DNA, Circular isolation & purification, DNA, Neoplasm genetics, DNA, Neoplasm isolation & purification, Female, Histiocytoma, Benign Fibrous complications, Humans, Male, Middle Aged, Reference Values, Skin cytology, Tuberous Sclerosis complications, Tumor Cells, Cultured, DNA, Circular genetics, Histiocytoma, Benign Fibrous genetics, Tuberous Sclerosis genetics

Abstract

Much greater amounts of small polydisperse circular DNA (spcDNA) have been detected, in cell cultures derived from angiofibromas of six patients with tuberous sclerosis (TS) than in those from the skin of these patients or from the skin of 11 healthy donors. This observation could be confirmed by spreading the DNA of appropriate fractions from CsCl density gradients. The findings suggest the existence of a relationship between the chromosomal instability observed in angiofibroma cultures and the mobilization of spcDNA.

Published

1988

5. Restriction analysis of chromosomal sequences homologous to single-copy fragments cloned from small polydisperse circular DNA (spcDNA).

Author

Assum G, Böckle B, Fink T, Dmochewitz U, and Krone W

Subjects

Humans, Nucleic Acid Hybridization, Restriction Mapping, Base Sequence, DNA, Circular genetics, Polymorphism, Genetic, Polymorphism, Restriction Fragment Length, Sequence Homology, Nucleic Acid

Abstract

Restriction fragments from the fraction of small polydisperse circular DNA (spcDNA) were cloned in pBR322. The spcDNA was prepared from cell cultures derived from an angiofibroma of a patient with tuberous sclerosis (TS). Such cultures have been shown previously to contain increased amounts of spcDNA. Four cloned spcDNA fragments containing single-copy sequences were chosen to characterize the homologous chromosomal DNA segments by restriction analysis. When used as hybridization probes, these four fragments generate well-defined nonvariable patterns in the chromosomal DNA from healthy donors. The restriction patterns obtained with one of the fragments (D-C4) can best be interpreted by assuming the presence of two copies of the homologous sequences in chromosomal DNA. A second sequence, A-B4, occurs at least 30-50 times in the haploid human genome. In both cases the duplicated regions span relatively large segments of DNA.

Published

1989