Heterogeneity analysis in 40 X-linked retinitis pigmentosa families

Heterogeneity analysis in 40 X-linked retinitis pigmentosa families

Analysis of genetic heterogeneity in 40 kindreds with X-linked retinitis pigmentosa (XLRP), with 20 polymorphic markers, showed that significant heterogeneity is present (P = .001) and that 56% of kindreds are of RP3 type and that 26% are of RP2 type. The location of the RP3 locus was found to be 0....

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Veröffentlicht in:American journal of human genetics 1994-07, Vol.55 (1), p.105-111
Hauptverfasser: TEAGUE, P. W, ALDRED, M. A, BUNDEY, S, JAY, B, BIRD, A. C, BHATTACHARYA, S. S, WRIGHT, A. F, JAY, M, DEMPSTER, M, HARRISON, C, CAROTHERS, A. D, HARDWICK, L. J, EVANS, H. J, STRAIN, L, BROCK, D. J. H
Format: Artikel
Sprache:eng
Schlagworte:
BASIC BIOLOGICAL SCIENCES
Bayes Theorem
Biological and medical sciences
BIOLOGICAL VARIABILITY
BODY
BODY AREAS
Chi-Square Distribution
CHROMOSOMES
DISEASES
EYES
FACE
Female
Genetic Linkage
GENETIC MAPPING
GENETIC VARIABILITY
Genotype
HEAD
HEREDITARY DISEASES
HETEROCHROMOSOMES
Heterozygote
HUMAN CHROMOSOMES
HUMAN POPULATIONS
HUMAN X CHROMOSOME
Humans
Lod Score
Male
MAPPING
Medical sciences
Odds Ratio
Ophthalmology
ORGANS
Original
Phenotype
Polymorphism, Genetic
POPULATIONS
RETINA
Retinitis Pigmentosa - genetics
Retinopathies
SENSE ORGANS
Sex Chromosome Aberrations - genetics
X Chromosome
X CHROMOSOME 550400 > Genetics
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Zusammenfassung:Analysis of genetic heterogeneity in 40 kindreds with X-linked retinitis pigmentosa (XLRP), with 20 polymorphic markers, showed that significant heterogeneity is present (P = .001) and that 56% of kindreds are of RP3 type and that 26% are of RP2 type. The location of the RP3 locus was found to be 0.4 cM distal to OTC in the Xp21.1 region, and that of the RP2 locus was 6.5 cM proximal to DXS7 in Xp11.2-p11.3. Bayesian probabilities of linkage to RP2, RP3, or to neither locus were calculated. This showed that 20 of 40 kindreds could be assigned to one or the other locus, with a probability > .70 (14 kindreds with RP3 and 6 kindreds with RP2 disease). A further three kindreds were found to be unlinked to either locus, with a probability > .8. The remaining 17 kindreds could not be classified unambiguously. This highlights the difficulty of classifying families in the presence of genetic heterogeneity, where the two loci are separated by an estimated 16 cM.
ISSN:0002-9297
1537-6605