Abstract
DNA at the end point of the gene deletion associated with one form of hereditary persistence of fetal hemoglobin (HPFH) was cloned and used as a probe in gene mapping experiments to analyze the extent and approximate 3' end points of various deletions associated with HPFH and delta beta-thalassemia. The deletions in the two known forms of deletion-type HPFH were shown to be considerably more extensive than in the two cases of delta beta-thalassemia studied. The overall extents of the deletions in the two types of HPFH were quite similar in both cases and the 3' end points were located at a minimum distance of approximately equal to 52 and 57 kilobases from the 3' extremity of the beta-globin gene. In contrast, the 3' end points of the deletions in the two forms of delta beta-thalassemia were located approximately equal to 5 and 10 kilobases to the 3' side of the beta-globin gene. The extent of these deletions and the nature of the DNA brought into the vicinity of the gamma-globin genes by the deletions may therefore be a more important influence on the phenotype of the deletions than the specific nature of the DNA sequences that are deleted within the non-alpha-globin gene cluster as a result of the mutations.
Keywords
Fetal hemoglobinGeneticsBiologyGeneThalassemiaGlobinGene clusterMolecular biologyPoint mutationMutationFetus
MeSH Terms
Base SequenceChromosome DeletionCloningMolecularDNA Restriction EnzymesFetal HemoglobinGenesHumansNucleic Acid HybridizationThalassemiagamma-Globulins
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Publication Info
- Year
- 1983
- Type
- article
- Volume
- 80
- Issue
- 22
- Pages
- 6937-6941
- Citations
- 126
- Access
- Closed
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Cite This
Dorothy Tuan,
Eleanor Feingold,
Morgan Newman
et al.
(1983).
Different 3' end points of deletions causing delta beta-thalassemia and hereditary persistence of fetal hemoglobin: implications for the control of gamma-globin gene expression in man..
Proceedings of the National Academy of Sciences
, 80
(22)
, 6937-6941.
https://doi.org/10.1073/pnas.80.22.6937
Identifiers
- DOI
- 10.1073/pnas.80.22.6937
- PMID
- 6196781
- PMCID
- PMC390101