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Inheritance of human plasma dopamine-β-hydroxylase thermal stability

✍ Scribed by John P. Vuchetich; Joel Dunnette; Kathryn L. Lunetta; Richard M. Weinshilboum; Dr. R. Arlen Price; G. P. Vogler


Publisher
John Wiley and Sons
Year
1991
Tongue
English
Weight
840 KB
Volume
8
Category
Article
ISSN
0741-0395

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✦ Synopsis


Although the structural gene for human dopamine-P-hydroxylase (DBH) has been cloned, the mechanism by which DBH physical properties and activity are regulated is not well understood. Previous reports have suggested that three-allele or twolocus models may account for the genetic regulation of these traits in human blood. It is an interesting challenge to determine the extent to which quantitative analyses will complement or guide molecular genetic studies. In this study we analyzed data on the physical property of DBH thermal stability and DBH activity in 230 individuals in 53 families in an attempt to clarify genetic mechanisms for the inheritance of these traits. Commingling and segregation analyses of the thermal stability data provided the first clear evidence of a major gene polymorphism for DBH thermal stability analyzed as a quantitative trait. Major gene transmission was supported within a mixed model (& = 13.39, P < .004). In keeping with earlier findings, similar analyses of DBH activity provided strong evidence of genetic transmission. However, in our data support for a major gene polymorphism was equivocal = 2.99, P = .22).


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## Abstract The __DBH__ locus controls plasma dopamine β‐hydroxylase activity (pDβH). A 5′‐upstream single nucleotide polymorphism (SNP) at __DBH__ (−1021C → T) explains ∼45% of the variance in pDβH, and a non‐synonymous SNP in exon 11 (+ 1603C → T) an additional 2%. However, that regression result