Your search keyword '"ALBUMIN GENE"' showing total 4 results

1. A novel splicing mutation in the albumin gene (c.270+1G>T) causes analbuminaemia in a German infant.

Author

Caridi, Gianluca, Thomas, Wolfgang, Campagnoli, Monica, Lugani, Francesca, Galliano, Monica, and Minchiotti, Lorenzo

Subjects

*METABOLIC disorders, *GENETIC mutation, *GENETIC engineering, *PUBLIC health, *NUCLEOTIDE sequencing

Abstract

Congenital analbuminaemia is a rare autosomal recessive disorder manifested by the presence of a very low amount of circulating serum albumin. The clinical diagnosis may be challenging because of the absence of unambiguous symptoms and because hypoalbuminemia may have many causes different from a genetic lack of the protein. We describe the clinical and molecular characterization of a new case of congenital analbuminaemia in an infant of apparently non-consanguineous parents from Treves, Germany. For molecular diagnosis, we used our strategy, based on the screening of the albumin gene by single-strand conformation polymorphism, heteroduplex analysis and direct DNA sequencing, which revealed that the proband is homozygous and both parents are heterozygous, for a novel G > T transversion at nucleotide c.270+ 1, the first base of intron 3. The mutation inactivates the strongly conserved GT dinucleotide at the 5' splice site consensus sequence of this intron. In conclusion, we report the clinical findings and the molecular defect of this case, which contributes to a better understanding of the biological mechanism of congenital analbuminaemia. [ABSTRACT FROM AUTHOR]

Published

2016

2. Congenital analbuminemia caused by a novel aberrant splicing in the albumin gene.

Author

Caridi, Gianluca, Dagnino, Monica, Erdeve, Omer, Di Duca, Marco, Yildiz, Duran, Alan, Serdar, Atasay, Begum, Arsan, Saadet, Campagnoli, Monica, Galliano, Monica, and Minchiotti, Lorenzo

Subjects

*ALBUMINS, *ECTOPIC tissue, *GENES, *NUCLEOTIDE sequence, *GENETIC mutation

Abstract

Introduction: Congenital analbuminemia is a rare autosomal recessive disorder manifested by the presence of a very low amount of circulating serum albumin. It is an allelic heterogeneous defect, caused by variety of mutations within the albumin gene in homozygous or compound heterozygous state. Herein we report the clinical and molecular characterization of a new case of congenital analbuminemia diagnosed in a female newborn of consanguineous (first degree cousins) parents from Ankara, Turkey, who presented with a low albumin concentration (< 8 g/L) and severe clinical symptoms. Materials and methods: The albumin gene of the index case was screened by single-strand conformation polymorphism, heteroduplex analysis, and direct DNA sequencing. The effect of the splicing mutation was evaluated by examining the cDNA obtained by reverse transcriptase - polymerase chain reaction (RT-PCR) from the albumin mRNA extracted from proband's leukocytes. Results: DNA sequencing revealed that the proband is homozygous, and both parents are heterozygous, for a novel G>A transition at position c.1652+1, the first base of intron 12, which inactivates the strongly conserved GT dinucleotide at the 5' splice site consensus sequence of this intron. The splicing defect results in the complete skipping of the preceding exon (exon 12) and in a frame-shift within exon 13 with a premature stop codon after the translation of three mutant amino acid residues. Conclusions: Our results confirm the clinical diagnosis of congenital analbuminemia in the proband and the inheritance of the trait and contribute to shed light on the molecular genetics of analbuminemia. [ABSTRACT FROM AUTHOR]

Published

2014

3. Congenital analbuminaemia: Molecular defects and biochemical and clinical aspects.

Author

Minchiotti, Lorenzo, Galliano, Monica, Caridi, Gianluca, Kragh-Hansen, Ulrich, and Peters,, Theodore

Subjects

*CONGENITAL disorders, *MOLECULAR biology, *MESSENGER RNA, *NUCLEOTIDE sequence, *GENETIC mutation, *ATHEROSCLEROSIS

Abstract

Abstract: Background: DNA and mRNA sequencing of the coding regions of the human albumin gene (ALB) and of its intron/exon junctions has revealed twenty-one different molecular defects causing congenital analbuminaemia (CAA). Scope of review: To describe the mutations in molecular terms and to present the current knowledge about the most important biochemical and clinical effects of CAA. Major conclusions: CAA is rare, but its frequency seems to be significantly higher in restricted and minimally admixed populations. The condition affects especially the lipid metabolism but apart from a possible increased risk for atherosclerotic complications, it is generally associated with mild clinical symptoms in adults. By contrast, several reports indicate that analbuminaemic individuals may be at risk during the perinatal and childhood periods, in which they seem to show increased morbidity and mortality. The twenty-one causative defects include seven nonsense mutations, seven changes affecting splicing, five frame-shift/deletions, one frame-shift/insertion and one mutation in the start codon. These results indicate that the trait is an allelic heterogeneous disorder caused by homozygous (nineteen cases) or compound heterozygous (single case) inheritance of defects. Most mutations are unique, but one, named Kayseri, is responsible for about half of the known cases. General significance: Study of the defects in the ALB resulting in CAA allows the identification of “hot spot” regions and contributes to understanding the molecular mechanism underlying the trait. Such studies could also give molecular information about different aspects of ALB regulation and shed light on the regulatory mechanisms involved in the synthesis of the protein. This article is part of a Special Issue entitled Serum Albumin. [Copyright &y& Elsevier]

Published

2013

4. A novel splicing mutation causes analbuminemia in a Portuguese boy

Author

Caridi, Gianluca, Dagnino, Monica, Di Duca, Marco, Pinto, Helena, Espinheira, Maria do Céu, Guerra, António, Fernandes, Susana, Campagnoli, Monica, Galliano, Monica, and Minchiotti, Lorenzo

Subjects

*SERUM albumin, *BLOOD diseases, *GENETIC disorders, *GENETIC mutation, *NUCLEOTIDE sequence, *GENETIC polymorphisms, *PORTUGUESE people, *BOYS, *GENETICS, *DISEASES

Abstract

Abstract: Analbuminemia is a rare autosomal recessive disorder manifested by the absence or severe reduction of circulating serum albumin in homozygous or compound heterozygous subjects. It is an allelic heterogeneous defect, caused by a variety of mutations within the albumin gene. The analbuminemic condition was suspected in a Portuguese boy who presented with low albumin level (about 3.8g/L) and a significant hypercholesterolemia, but with no clinical findings. The albumin gene was screened by single strand conformational polymorphism and heteroduplex analysis and submitted to direct DNA sequencing. The proband was found to be homozygous for a previously unreported G>A change at position c.1289+1, the first base of intron 10, which inactivates the strongly conserved GT dinucleotide at the 5′ splice site consensus sequence of the intron. The effect of this mutation was evaluated by examining the cDNA obtained by RT-PCR from the albumin mRNA extracted from proband''s leukocytes. The splicing defect results in the skipping of the preceding exon. The subsequent reading frame-shift in exon 11 produces a premature stop codon located 33 codons downstream the 5′ end of the exon. This extensive cDNA alteration is responsible for the analbuminemic trait. Both parents were found to be heterozygous for the same mutation. DNA and cDNA sequence analysis established the diagnosis of congenital analbuminemia in the proband. The effects of the so far identified splice-site mutations in the albumin gene are discussed. [Copyright &y& Elsevier]

Published

2012