ADAM30 Downregulates APP-Linked Defects Through Cathepsin D Activation in Alzheimer's Disease

Florent Letronne; Geoffroy Laumet; Anne-Marie Ayral; Julien Chapuis; Florie Demiautte; Mathias Laga; Michel E Vandenberghe; Nicolas Malmanche; Florence Leroux; Fanny Eysert; Yoann Sottejeau; Linda Chami; Amandine Flaig; Charlotte Bauer; Pierre Dourlen; Marie Lesaffre; Charlotte Delay; Ludovic Huot; Julie Dumont; Elisabeth Werkmeister; Franck Lafont; Tiago Mendes; Franck Hansmannel; Bart Dermaut; Benoit Deprez; Anne-Sophie Hérard; Marc Dhenain; Nicolas Souedet; Florence Pasquier; David Tulasne; Claudine Berr; Jean-Jacques Hauw; Yves Lemoine; Philippe Amouyel; David Mann; Rebecca Déprez; Frédéric Checler; David Hot; Thierry Delzescaux; Kris Gevaert; Jean-Charles Lambert

doi:10.1016/j.ebiom.2016.06.002

ADAM30 Downregulates APP-Linked Defects Through Cathepsin D Activation in Alzheimer's Disease

EBioMedicine. 2016 Jul:9:278-292. doi: 10.1016/j.ebiom.2016.06.002. Epub 2016 Jun 2.

Authors

Florent Letronne¹, Geoffroy Laumet¹, Anne-Marie Ayral¹, Julien Chapuis¹, Florie Demiautte¹, Mathias Laga², Michel E Vandenberghe³, Nicolas Malmanche¹, Florence Leroux⁴, Fanny Eysert¹, Yoann Sottejeau¹, Linda Chami⁵, Amandine Flaig¹, Charlotte Bauer⁵, Pierre Dourlen¹, Marie Lesaffre⁶, Charlotte Delay¹, Ludovic Huot⁷, Julie Dumont⁴, Elisabeth Werkmeister⁸, Franck Lafont⁸, Tiago Mendes¹, Franck Hansmannel⁹, Bart Dermaut¹, Benoit Deprez⁴, Anne-Sophie Hérard³, Marc Dhenain³, Nicolas Souedet³, Florence Pasquier¹⁰, David Tulasne⁶, Claudine Berr¹¹, Jean-Jacques Hauw¹², Yves Lemoine⁷, Philippe Amouyel¹³, David Mann¹⁴, Rebecca Déprez⁴, Frédéric Checler⁵, David Hot⁷, Thierry Delzescaux³, Kris Gevaert², Jean-Charles Lambert¹⁵

Affiliations

¹ INSERM, U1167, Laboratoire d'Excellence Distalz, F59000 Lille, France; Institut Pasteur de Lille, F59000 Lille, France; Univ. Lille, F59000 Lille, France.
² Department of Medical Protein Research, VIB, Ghent, Belgium; Department of Biochemistry, Ghent University, Ghent, Belgium.
³ CEA, DSV, I2BM, MIRCen, Fontenay aux Roses, France; CNRS, UMR 9199, Fontenay aux Roses, France.
⁴ Institut Pasteur de Lille, F59000 Lille, France; Univ. Lille, F59000 Lille, France; INSERM U1177, Drugs and Molecules for Living Systems, F5900 Lille, France.
⁵ Institut de Pharmacologie Moléculaire et Cellulaire, UMR 7275 CNRS, Laboratoire d'Excellence Distalz, Nice, France; Université de Nice-Sophia-Antipolis, Valbonne, France.
⁶ Univ. Lille, CNRS, Institut Pasteur de Lille, UMR 8161 - M3T - Mechanisms of Tumorigenesis and Targeted Therapies, F-59000 Lille, France.
⁷ Institut Pasteur de Lille, F59000 Lille, France; Univ. Lille, F59000 Lille, France; Center for Infection and Immunity of Lille, CNRS UMR 8204, INSERM 1019, Lille, France.
⁸ Institut Pasteur de Lille, F59000 Lille, France.
⁹ INSERM, U954, Vandoeuvre-lès-Nancy, France; Department of Hepato-Gastroenterology, University Hospital of Nancy, Université Henri Poincaré 1, Vandoeuvre-lès-Nancy, France.
¹⁰ Univ. Lille, Inserm, U1171, - Degenerative & Vascular Cognitive Disorders, Laboratoire d'Excellence Distalz, F-59000 Lille, France; CHR&U, Lille, France.
¹¹ INSERM, U1061, Université de Montpellier I, Hôpital La Colombière, Montpellier, France.
¹² APHP-Raymond Escourolle Neuropathology Laboratory, la salpétrière Hospital, Paris, France.
¹³ INSERM, U1167, Laboratoire d'Excellence Distalz, F59000 Lille, France; Institut Pasteur de Lille, F59000 Lille, France; Univ. Lille, F59000 Lille, France; CHR&U, Lille, France.
¹⁴ Institute of Brain, Behaviour and Mental Health, University of Manchester, Salford Royal Hospital, Salford, UK.
¹⁵ INSERM, U1167, Laboratoire d'Excellence Distalz, F59000 Lille, France; Institut Pasteur de Lille, F59000 Lille, France; Univ. Lille, F59000 Lille, France. Electronic address: jean-charles.lambert@pasteur-lille.fr.

Abstract

Although several ADAMs (A disintegrin-like and metalloproteases) have been shown to contribute to the amyloid precursor protein (APP) metabolism, the full spectrum of metalloproteases involved in this metabolism remains to be established. Transcriptomic analyses centred on metalloprotease genes unraveled a 50% decrease in ADAM30 expression that inversely correlates with amyloid load in Alzheimer's disease brains. Accordingly, in vitro down- or up-regulation of ADAM30 expression triggered an increase/decrease in Aβ peptides levels whereas expression of a biologically inactive ADAM30 (ADAM30(mut)) did not affect Aβ secretion. Proteomics/cell-based experiments showed that ADAM30-dependent regulation of APP metabolism required both cathepsin D (CTSD) activation and APP sorting to lysosomes. Accordingly, in Alzheimer-like transgenic mice, neuronal ADAM30 over-expression lowered Aβ42 secretion in neuron primary cultures, soluble Aβ42 and amyloid plaque load levels in the brain and concomitantly enhanced CTSD activity and finally rescued long term potentiation alterations. Our data thus indicate that lowering ADAM30 expression may favor Aβ production, thereby contributing to Alzheimer's disease development.

Keywords: ADAM30; APP; Alzheimer; Amyloid; LTP; Metabolism.

MeSH terms

ADAM Proteins / antagonists & inhibitors
ADAM Proteins / genetics
ADAM Proteins / metabolism*
Alzheimer Disease / metabolism
Alzheimer Disease / pathology
Amino Acid Sequence
Amyloid beta-Peptides / metabolism*
Animals
Brain / metabolism
Brain / pathology
Cathepsin D / chemistry
Cathepsin D / metabolism*
Cell Line, Tumor
Down-Regulation / drug effects
HEK293 Cells
Humans
Lysosomes / metabolism
Macrolides / pharmacology
Mice
Mice, Inbred C57BL
Mice, Transgenic
Microscopy, Fluorescence
Patch-Clamp Techniques
Pepstatins / pharmacology
RNA Interference
RNA, Small Interfering / metabolism

Substances

Amyloid beta-Peptides
Macrolides
Pepstatins
RNA, Small Interfering
bafilomycin A
Cathepsin D
ADAM Proteins
ADAM30 protein, human
pepstatin