The E32K variant of PCSK9 exacerbates the phenotype of familial hypercholesterolaemia by increasing PCSK9 function and concentration in the circulation

Tohru Noguchi; Shoji Katsuda; Masa-Aki Kawashiri; Hayato Tada; Atsushi Nohara; Akihiro Inazu; Masakazu Yamagishi; Junji Kobayashi; Hiroshi Mabuchi

doi:10.1016/j.atherosclerosis.2009.11.018

The E32K variant of PCSK9 exacerbates the phenotype of familial hypercholesterolaemia by increasing PCSK9 function and concentration in the circulation

Atherosclerosis. 2010 May;210(1):166-72. doi: 10.1016/j.atherosclerosis.2009.11.018. Epub 2009 Nov 20.

Authors

Tohru Noguchi¹, Shoji Katsuda, Masa-Aki Kawashiri, Hayato Tada, Atsushi Nohara, Akihiro Inazu, Masakazu Yamagishi, Junji Kobayashi, Hiroshi Mabuchi

Affiliation

¹ Department of Lipidology, Graduate School of Medical Science, Kanazawa University, Takara-machi 13-1, Kanazawa 920-8640, Japan. [email protected]

PMID: 20006333
DOI: 10.1016/j.atherosclerosis.2009.11.018

Abstract

Objective: Proprotein convertase subtilisin/kexin type 9 (PCSK9) regulates cholesterol trafficking by mediating degradation of cell-surface LDL receptors (LDLR). Gain-of-function PCSK9 mutations are known to increase plasma LDL-C levels. We attempted to find gain-of-function PCSK9 mutations in Japanese subjects and determine the frequency and impacts of these mutations, especially on circulating PCSK9 and LDL-C levels.

Methods: PCR-SSCP followed by direct sequence analysis was performed for all 12 exons and intronic junctions of the PCSK9 in 55 subjects with clinically diagnosed familial hypercholesterolaemia (clinical-FH), who were confirmed to have no LDLR mutations. Among the mutations detected, PCSK9 E32K was likely to be a gain-of-function mutation, and screening was performed by PCR-RFLP in clinical-FH and general Japanese controls. The levels of PCSK9 in plasma from subjects and in media of HepG2 cells transfected with PCSK9 constructs were measured by ELISA.

Results: We detected 7 PCSK9 variants, including E32K. The frequency of PCSK9 E32K in clinical-FH (6.42%) was significantly higher than that in controls (1.71%). Three cases representing homozygous FH phenotypes were double heterozygous for PCSK9 E32K and LDLR C183S, C292X or K790X. Two cases were true homozygous for PCSK9 E32K; to our knowledge, these are the first true homozygotes for gain-of-function PCSK9 mutations reported to date. The PCSK9 E32K mutant had over 30% increased levels of PCSK9 in plasma from the subjects and in media of transiently transfected HepG2 cells as compared with those in controls. Furthermore, LDL-C levels in the PCSK9 E32K true homozygotes and heterozygotes were 2.10- and 1.47-fold higher than those in controls with comparable circulating PCSK9 levels, respectively, suggesting enhanced function of PCSK9 E32K.

Conclusions: We found 2 true homozygotes for PCSK9 E32K and 3 double heterozygotes for PCSK9 E32K and LDLR mutations associated with autosomal dominant hypercholesterolaemia. This study provided evidence that PCSK9 E32K significantly affects LDL-C levels via increased mass and function of PCSK9, and could exacerbate the clinical phenotypes of patients carrying LDLR mutations.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Adult
Asian People / genetics
Cholesterol, LDL / blood
Enzyme-Linked Immunosorbent Assay
Exons
Heterozygote
Homozygote
Humans
Hyperlipoproteinemia Type II / genetics*
Introns
Middle Aged
Mutation
Polymerase Chain Reaction
Polymorphism, Restriction Fragment Length
Proprotein Convertase 9
Proprotein Convertases
Serine Endopeptidases / blood
Serine Endopeptidases / genetics*
Serine Endopeptidases / physiology

Substances

Cholesterol, LDL
PCSK9 protein, human
Proprotein Convertase 9
Proprotein Convertases
Serine Endopeptidases