APP, PSEN1, and PSEN2 mutations in early-onset Alzheimer disease: A genetic screening study of familial and sporadic cases

Hélène-Marie Lanoiselée; Gaël Nicolas; David Wallon; Anne Rovelet-Lecrux; Morgane Lacour; Stéphane Rousseau; Anne-Claire Richard; Florence Pasquier; Adeline Rollin-Sillaire; Olivier Martinaud; Muriel Quillard-Muraine; Vincent de la Sayette; Claire Boutoleau-Bretonniere; Frédérique Etcharry-Bouyx; Valérie Chauviré; Marie Sarazin; Isabelle le Ber; Stéphane Epelbaum; Thérèse Jonveaux; Olivier Rouaud; Mathieu Ceccaldi; Olivier Félician; Olivier Godefroy; Maite Formaglio; Bernard Croisile; Sophie Auriacombe; Ludivine Chamard; Jean-Louis Vincent; Mathilde Sauvée; Cecilia Marelli-Tosi; Audrey Gabelle; Canan Ozsancak; Jérémie Pariente; Claire Paquet; Didier Hannequin; Dominique Campion; collaborators of the CNR-MAJ project

doi:10.1371/journal.pmed.1002270

APP, PSEN1, and PSEN2 mutations in early-onset Alzheimer disease: A genetic screening study of familial and sporadic cases

PLoS Med. 2017 Mar 28;14(3):e1002270. doi: 10.1371/journal.pmed.1002270. eCollection 2017 Mar.

Authors

Hélène-Marie Lanoiselée^{1

2}, Gaël Nicolas³, David Wallon¹, Anne Rovelet-Lecrux³, Morgane Lacour¹, Stéphane Rousseau³, Anne-Claire Richard³, Florence Pasquier^{4

5}, Adeline Rollin-Sillaire^{4

5}, Olivier Martinaud¹, Muriel Quillard-Muraine⁶, Vincent de la Sayette⁷, Claire Boutoleau-Bretonniere⁸, Frédérique Etcharry-Bouyx⁹, Valérie Chauviré⁹, Marie Sarazin¹⁰, Isabelle le Ber¹¹, Stéphane Epelbaum¹¹, Thérèse Jonveaux¹², Olivier Rouaud¹³, Mathieu Ceccaldi¹⁴, Olivier Félician¹⁴, Olivier Godefroy¹⁵, Maite Formaglio¹⁶, Bernard Croisile¹⁶, Sophie Auriacombe¹⁷, Ludivine Chamard¹⁸, Jean-Louis Vincent¹⁹, Mathilde Sauvée²⁰, Cecilia Marelli-Tosi²¹, Audrey Gabelle²¹, Canan Ozsancak², Jérémie Pariente²², Claire Paquet²³, Didier Hannequin¹, Dominique Campion^{3

24}; collaborators of the CNR-MAJ project

Affiliations

¹ Normandie Univ, UNIROUEN, Inserm U1245 and Rouen University Hospital, Department of Neurology and CNR-MAJ, Normandy Center for Genomic and Personalized Medicine, Rouen, France.
² Department of Neurology, Orleans Regional Hospital, Orleans, France.
³ Normandie Univ, UNIROUEN, Inserm U1245 and Rouen University Hospital, Department of Genetics and CNR-MAJ, Normandy Center for Genomic and Personalized Medicine, Rouen, France.
⁴ Department of Neurology and CNR-MAJ, Lille University Hospital, Lille, France.
⁵ Inserm UMR-S 1171, Université Lille Nord de France, Lille, France.
⁶ Biochemistry Laboratory, Rouen University Hospital, Rouen, France.
⁷ Department of Neurology, Caen University Hospital, Caen, France.
⁸ Department of Neurology, Nantes University Hospital, Nantes, France.
⁹ Department of Neurology, Angers University Hospital, Angers, France.
¹⁰ Department of Neurology, Saint Anne University Hospital, Paris, France.
¹¹ CNR-MAJ, AP-HP, Hôpital de la Pitié-Salpêtrière, Paris, France; and ICM, Inserm U1127, CNRS UMR 7225, Sorbonne Universités, UPMC-P6 UMR S 1127 - Hôpital Pitié-Salpêtrière, Paris, France.
¹² Department of Neurology, Nancy University Hospital, Nancy, France.
¹³ Department of Neurology, Dijon University Hospital, Dijon, France.
¹⁴ Aix Marseille University, Inserm, INS, Institut de Neurosciences des Systèmes, Marseille, France; AP-HM, Service de Neurologie et Neuropsychologie, CHU Timone, Marseille, France.
¹⁵ Department of Neurology, Amiens University Hospital Center, Amiens, France.
¹⁶ Department of Neurology and CMRR Lyon University Hospital, Lyon, France.
¹⁷ Department of Neurology, Bordeaux University Hospital, Bordeaux, France.
¹⁸ Department of Neurology, Besançon University Hospital, Besançon, France.
¹⁹ Biochemistry Laboratory, Lille University Hospital, Lille, France.
²⁰ Department of Neurology, Grenoble University Hospital, Grenoble, France.
²¹ Department of Neurology, Montpellier University Hospital, Montpellier, France.
²² Department of Neurology, Toulouse University Hospital, Toulouse, France.
²³ CMRR Paris Nord AP-HP, Hôpital Lariboisière, INSERM, U942, Université Paris Diderot, Sorbonne Paris Cité, UMRS 942, Paris, France.
²⁴ Department of Research, Centre Hospitalier du Rouvray, Sotteville-lès-Rouen, France.

Abstract

Background: Amyloid protein precursor (APP), presenilin-1 (PSEN1), and presenilin-2 (PSEN2) mutations cause autosomal dominant forms of early-onset Alzheimer disease (AD-EOAD). Although these genes were identified in the 1990s, variant classification remains a challenge, highlighting the need to colligate mutations from large series.

Methods and findings: We report here a novel update (2012-2016) of the genetic screening of the large AD-EOAD series ascertained across 28 French hospitals from 1993 onwards, bringing the total number of families with identified mutations to n = 170. Families were included when at least two first-degree relatives suffered from early-onset Alzheimer disease (EOAD) with an age of onset (AOO) ≤65 y in two generations. Furthermore, we also screened 129 sporadic cases of Alzheimer disease with an AOO below age 51 (44% males, mean AOO = 45 ± 2 y). APP, PSEN1, or PSEN2 mutations were identified in 53 novel AD-EOAD families. Of the 129 sporadic cases screened, 17 carried a PSEN1 mutation and 1 carried an APP duplication (13%). Parental DNA was available for 10 sporadic mutation carriers, allowing us to show that the mutation had occurred de novo in each case. Thirteen mutations (12 in PSEN1 and 1 in PSEN2) identified either in familial or in sporadic cases were previously unreported. Of the 53 mutation carriers with available cerebrospinal fluid (CSF) biomarkers, 46 (87%) had all three CSF biomarkers-total tau protein (Tau), phospho-tau protein (P-Tau), and amyloid β (Aβ)42-in abnormal ranges. No mutation carrier had the three biomarkers in normal ranges. One limitation of this study is the absence of functional assessment of the possibly and probably pathogenic variants, which should help their classification.

Conclusions: Our findings suggest that a nonnegligible fraction of PSEN1 mutations occurs de novo, which is of high importance for genetic counseling, as PSEN1 mutational screening is currently performed in familial cases only. Among the 90 distinct mutations found in the whole sample of families and isolated cases, definite pathogenicity is currently established for only 77%, emphasizing the need to pursue the effort to classify variants.

MeSH terms

Adult
Age of Onset
Alzheimer Disease / diagnosis*
Alzheimer Disease / genetics*
Amyloid beta-Protein Precursor / genetics*
Female
France
Genetic Testing
Humans
Male
Middle Aged
Mutation
Presenilin-1 / genetics*
Presenilin-2 / genetics*

Substances

APP protein, human
Amyloid beta-Protein Precursor
PSEN1 protein, human
PSEN2 protein, human
Presenilin-1
Presenilin-2

Grants and funding

This study was funded by the following grants: Clinical Research Hospital Program from the French Ministry of Health (PHRC, GMAJ 2008/067) to DC; Funding from the French Ministry of Health to the National Reference Centre for Young Alzheimer Disease (CNR-MAJ) to DH; Joint Program for Neurodegenerative Disease Research from the European Union (JPND PERADES, ANR-13-JPRF-0001-04) to DC. The funders had no role in study design, data collection and analysis, decision to publish, or preparation of the manuscript.