Multiple splice defects in ABCA1 cause low HDL-C in a family with Hypoalphalipoproteinemia and premature coronary disease

AN Ladd; AT Remaley; David F Gardner; E Kim; E Wagner; F Del Gatto; G Franceschini; HH Hobbs; JC Cohen; Jeffrey Rhyne; LK Curtiss; LR Brunham; M Bodzioch; M Fagnani; M Huizing; M Krawczak; M Mantaring; M Miller; M Miller; M Miller; M Miller; Michael Miller; ML Alfaro Leon; MW Hentze; Myrna M Mantaring; N Lopez-Bigas; N Lopez-Bigas; R Frikke-Schmidt; S Ho Hong; S Rust; S Santamarina-Fojo; SH Hong; SH Hong; SH Korman; TD Schneider; VK Nalla; WT Friedewald

Multiple splice defects in ABCA1 cause low HDL-C in a family with Hypoalphalipoproteinemia and premature coronary disease

Authors: AN Ladd
AT Remaley
David F Gardner
E Kim
E Wagner
F Del Gatto
G Franceschini
HH Hobbs
JC Cohen
Jeffrey Rhyne
LK Curtiss
LR Brunham
M Bodzioch
M Fagnani
M Huizing
M Krawczak
M Mantaring
M Miller
M Miller
M Miller
M Miller
Michael Miller
ML Alfaro Leon
MW Hentze
Myrna M Mantaring
N Lopez-Bigas
N Lopez-Bigas
R Frikke-Schmidt
S Ho Hong
S Rust
S Santamarina-Fojo
SH Hong
SH Hong
SH Korman
TD Schneider
VK Nalla
WT Friedewald
Publication date: 1 January 2009
Publisher: BioMed Central
Doi

Abstract

Abstract Background Mutations at splice junctions causing exon skipping are uncommon compared to exonic mutations, and two intronic mutations causing an aberrant phenotype have rarely been reported. Despite the high number of functional <it>ABCA1 </it>mutations reported to date, splice variants have been reported infrequently. We screened DNA from a 41 year-old male with low HDL-C (12 mg/dL [0.31 mmol/L]) and a family history of premature coronary heart disease (CHD) using polymerase chain reaction single-strand conformation polymorphism (SSCP) analysis. Methods Family members with low levels of HDL-C (n = 6) were screened by SSCP for mutations in <it>ABCA1</it>. Samples with altered SSCP patterns were sequenced directly using either an ABI 3700 or ABI3730Xl DNA Analyzer. To screen for splicing defects, cDNA was isolated from the proband's RNA and was sequenced as above. A series of minigenes were constructed to determine the contribution of normal and defective alleles. Results Two novel splice variants in <it>ABCA1 </it>were identified. The first mutation was a single base pair change (T->C) in IVS 7, 6 bps downstream from the exon7/intron7 junction. Amplification of cDNA and allelic subcloning identified skipping of Exon 7 that results in the elimination of 59 amino acids from the first extracellular loop of the ABCA1 protein. The second mutation was a single base pair change (G->C) at IVS 31 -1, at the intron/exon junction of exon 32. This mutation causes skipping of exon 32, resulting in 8 novel amino acids followed by a stop codon and a predicted protein size of 1496 AA, compared to normal (2261 AA). Bioinformatic studies predicted an impact on splicing as confirmed by <it>in vitro </it>assays of constitutive splicing. Conclusion In addition to carnitine-acylcarnitine translocase (CACT) deficiency and Hermansky-Pudlak syndrome type 3, this represents only the third reported case in which 2 different splice mutations has resulted in an aberrant clinical phenotype.</p