New insights of altered lipid profile in Fragile X Syndrome

Artuela Çaku; Nabil G Seidah; Audrey Lortie; Nancy Gagné; Patrice Perron; Jean Dubé; Francois Corbin

doi:10.1371/journal.pone.0174301

New insights of altered lipid profile in Fragile X Syndrome

PLoS One. 2017 Mar 23;12(3):e0174301. doi: 10.1371/journal.pone.0174301. eCollection 2017.

Authors

Artuela Çaku¹, Nabil G Seidah², Audrey Lortie¹, Nancy Gagné³, Patrice Perron⁴, Jean Dubé¹, Francois Corbin¹

Affiliations

¹ Department of Biochemistry, Université de Sherbrooke, Sherbrooke, Québec, Canada.
² Nabil G. Seidah, Laboratory of Biochemical Neuroendocrinology, Clinical Research Institute, affiliated to the Université de Montréal, Montréal, Québec, Canada.
³ Department of Paediatrics, Université de Sherbrooke, Sherbrooke, Québec, Canada.
⁴ Department of Medicine, Université de Sherbrooke, Sherbrooke, Québec, Canada.

Abstract

Background: Fragile X Syndrome (FXS) is the main genetic cause of autism and intellectual deficiency resulting the absence of the Fragile X Mental Retardation Protein (FMRP). Clinical picture is characterized by cognitive impairment associated with a broad spectrum of psychiatric comorbidities including autism spectrum disorders and attention-deficit/hyperactivity disorders. Some of these disorders have been associated with lipid abnormalities and lower cholesterol levels. Since lipids are important for neuronal development, we aim to investigate the lipid profile of French Canadian-FXS individuals and to identify the altered components of cholesterol metabolism as well as their association with clinical profile.

Methods: Anthropometric data were collected from 25 FXS individuals and 26 controls. Lipid assessment included: total cholesterol (TC), triglycerides, LDL, HDL, ApoB, ApoA1, PCSK9, Lp(a) and lipoprotein electrophoresis. Aberrant and adaptive behaviour of affected individuals was respectively assessed by the ABC-C and ABAS questionnaires.

Results: FXS participants had a higher body mass index as compared to controls while 38% of them had TC<10th percentile. Lower levels of LDL, HDL and apoA1 were observed in FXS group as compared to controls. However, PCSK9 levels did not differ between the two groups. As expected, PCSK9 levels correlated with total cholesterol (rs = 0.61, p = 0.001) and LDL (rs = 0.46, p = 0.014) in the control group, while no association was present in the FXS group. An inverse relationship was observed between total cholesterol and aberrant behaviour as determined by ABC-C total score.

Conclusion: Our results showed the presence of hypocholesterolemia in French Canadian-FXS population, a condition that seems to influence their clinical phenotype. We identified for the first time a potential underlying alteration of PCSK9 function in FXS that could result from the absence of FMRP. Further investigations are warranted to better understand the association between cholesterol metabolism, PCSK9, FMRP and clinical profile.

MeSH terms

Apolipoprotein A-I / blood
Apolipoproteins B / blood
Body Mass Index
Case-Control Studies
Cholesterol / blood
Cholesterol, HDL / blood
Cholesterol, LDL / blood
Female
Fragile X Syndrome / blood*
Fragile X Syndrome / metabolism
Humans
Lipid Metabolism
Lipids / blood*
Male
Proprotein Convertase 9 / blood
Triglycerides / blood
Young Adult

Substances

APOA1 protein, human
Apolipoprotein A-I
Apolipoproteins B
Cholesterol, HDL
Cholesterol, LDL
Lipids
Triglycerides
Cholesterol
PCSK9 protein, human
Proprotein Convertase 9

Grants and funding

FC received funding from Foundation of Stars. JD received funding from "Diabetes, Obesity, and Cardiovascular Complications" axis of Research Center of Centre Hospitalier de l'Université de Sherbrooke. The funders had no role in study design, data collection and analysis, decision to publish, or preparation of the manuscript.