In 8 carriers across 3 kindreds, short and medium-size truncated apoB mutations invariably caused fatty liver, while short variants caused intestinal lipid malabsorption.
Case Report (n=8)
The study demonstrates that the clinical phenotype of familial heterozygous hypobetalipoproteinemia, including fatty liver and malabsorption, varies depending on the size of the truncated apolipoprotein B.
We report the clinical phenotype in three kindreds with familial heterozygous hypobetalipoproteinemia (FHBL) carrying novel truncated apolipoprotein Bs (apoBs) of different sizes (apoB-8.15, apoB-33.4 and apoB-75.7). In D.A. kindred, we found three carriers of a C-deletion in exon 10 leading to the synthesis of apoB-8.15 not detectable in plasma. They showed steatorrhea and fatty liver. In N.L. kindred, the proband is heterozygous for a nonsense mutation in exon 26, leading to the formation of apoB-33.4. He had premature cerebrovascular disease and fatty liver; two apoB-33.4 carriers in this kindred showed only fatty liver. In B.E. kindred, the proband is heterozygous for a T-deletion in exon 26, which converts tyrosine at codon 3435 into a stop codon, resulting in apoB-75.7. The proband, a heavy alcohol drinker, had steatohepatitis, whereas his teetotaller daughter, an apoB-75.7 carrier, had no detectable fatty liver. This study suggests that: i ) fatty liver invariably develops in FHBL carriers of short and medium-size truncated apoBs ( apoB-48), but its occurrence needs additional environmental factors in carriers of longer apoB forms; ii ) intestinal lipid malabsorption develops only in carriers of short truncated apoBs, which are not secreted into the plasma; and iii ) cerebrovascular disease due to premature atherosclerosis may occur even in FHBL subjects. -Tarugi, P.,
Tarugi et al. (Mon,) conducted a case report in Familial heterozygous hypobetalipoproteinemia (FHBL) (n=8). Truncated apolipoprotein B mutations was evaluated on Clinical phenotype (fatty liver, steatorrhea, cerebrovascular disease). In 8 carriers across 3 kindreds, short and medium-size truncated apoB mutations invariably caused fatty liver, while short variants caused intestinal lipid malabsorption.
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