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KMID : 0981820100300030307
Korean Journal of Laboratory Medicine
2010 Volume.30 No. 3 p.307 ~ p.311
Clinical Characteristics and ALB Gene Mutation Analysis of Korean Patients with Bisalbuminemia
Kim Yong-Hyun

Lee Yong-Wha
Jeon Byung-Ryul
Lee You-Kyoung
Shin Hee-Bong
Park Sung-Kyu
Lee Seung-Tae
Kim Jong-Won
Ki Chang-Seok
Jeon Byung-Ryul
Kang Dong-Hee
Park Sung-Kyu
Hong Dae-Sik
Lee Seung-Tae
Ki Chang-Seok
Abstract
Background: Bisalbuminemia is a hereditary or an acquired condition characterized by the presence of 2 albumin variants with different mobilities on serum protein electrophoresis (SPE). The clinical significance of bisalbuminemia has not been clearly established. However, some regions of the albumin variant may affect the biochemical analysis of biomolecules such as steroid or thyroid hormones by altering their albumin-binding affinities. In this study, we analyzed the clinical manifestations, genetic variations, and the albumin-binding characteristics in Korean patients with bisalbuminemia.

Methods: We performed SPE for samples from 580 Korean subjects and identified bisalbuminemia on the basis of the results of SPE. The clinical and biochemical characteristics, ALB gene mutations, and the structures of the albumin variants of patients with bisalbuminemia were analyzed.

Results: SPE showed bisalbuminemia in 2 patients. One patient showed a genetic variation known as Nagasaki-1 (Asp293Gly) and the other showed a hitherto unreported missense mutation (c.593A>T; Lys198Ile). In both cases, the serum concentrations of the substances with binding affinity for albumin were not affected, and the mutation sites of the albumin were not located with the protein-binding loci.

Conclusions: The 2 Korean patients with bisalbuminemia showed genetic variations, including a novel missense mutation. The ALB gene analysis with 3D modeling is useful for determining the nature of bisalbuminemia and for predicting the effects on the albumin-binding affinity of other biochemical compounds.
KEYWORD
Bisalbuminemia, Albumin, ALB, Mutation
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