Aberrant upregulation of the glycolytic enzyme PFKFB3 in CLN7 neuronal ceroid lipofuscinosis

Irene Lopez-Fabuel; Marina Garcia-Macia; Costantina Buondelmonte; Olga Burmistrova; Nicolo Bonora; Paula Alonso-Batan; Brenda Morant-Ferrando; Carlos Vicente-Gutierrez; Daniel Jimenez-Blasco; Ruben Quintana-Cabrera; Emilio Fernandez; Jordi Llop; Pedro Ramos-Cabrer; Aseel Sharaireh; Marta Guevara-Ferrer; Lorna Fitzpatrick; Christopher D Thompton; Tristan R McKay; Stephan Storch; Diego L Medina; Sara E Mole; Peter O Fedichev; Angeles Almeida; Juan P Bolaños

doi:10.1038/s41467-022-28191-1

Aberrant upregulation of the glycolytic enzyme PFKFB3 in CLN7 neuronal ceroid lipofuscinosis

Nat Commun. 2022 Jan 27;13(1):536. doi: 10.1038/s41467-022-28191-1.

Authors

Irene Lopez-Fabuel^#^{1

2}, Marina Garcia-Macia^#^{3

4

5}, Costantina Buondelmonte^{3

4}, Olga Burmistrova⁶, Nicolo Bonora^{3

4}, Paula Alonso-Batan^{3

4}, Brenda Morant-Ferrando^{3

4}, Carlos Vicente-Gutierrez^{3

4

5}, Daniel Jimenez-Blasco^{3

4

5}, Ruben Quintana-Cabrera^{3

4

5}, Emilio Fernandez^{3

4

5}, Jordi Llop⁷, Pedro Ramos-Cabrer^{7

8}, Aseel Sharaireh⁹, Marta Guevara-Ferrer⁹, Lorna Fitzpatrick⁹, Christopher D Thompton⁹, Tristan R McKay⁹, Stephan Storch¹⁰, Diego L Medina^{11

12}, Sara E Mole¹³, Peter O Fedichev⁶, Angeles Almeida^{3

4}, Juan P Bolaños^{14

15

16}

Affiliations

¹ Institute of Functional Biology and Genomics (IBFG), Universidad de Salamanca, CSIC, Salamanca, Spain. ilofa@usal.es.
² Institute of Biomedical Research of Salamanca (IBSAL), Hospital Universitario de Salamanca, Salamanca, Spain. ilofa@usal.es.
³ Institute of Functional Biology and Genomics (IBFG), Universidad de Salamanca, CSIC, Salamanca, Spain.
⁴ Institute of Biomedical Research of Salamanca (IBSAL), Hospital Universitario de Salamanca, Salamanca, Spain.
⁵ Centro de Investigación Biomédica en Red de Fragilidad y Envejecimiento Saludable (CIBERFES), Madrid, Spain.
⁶ Gero Discovery LLC, Moscow, Russia.
⁷ CIC biomaGUNE, Basque Research and Technology Alliance (BRTA), Donostia-San Sebastián, Spain.
⁸ Ikerbasque, Basque Foundation for Science, Bilbao, Spain.
⁹ Centre for Bioscience, Manchester Metropolitan University, Manchester, M1 5GD, UK.
¹⁰ University Children's Research@Kinder-UKE, University Medical Center Hamburg-Eppendorf, Hamburg, Germany.
¹¹ Telethon Institute of Genetics and Medicine (TIGEM), High Content Screening Facility, Via Campi Flegrei 34, 80078, Pozzuoli, Italy.
¹² Medical Genetics Unit, Department of Medical and Translational Science, Federico II University, 80138, Naples, Italy.
¹³ MRC Laboratory for Molecular Biology and GOS Institute of Child Health, University College London, London, UK.
¹⁴ Institute of Functional Biology and Genomics (IBFG), Universidad de Salamanca, CSIC, Salamanca, Spain. jbolanos@usal.es.
¹⁵ Institute of Biomedical Research of Salamanca (IBSAL), Hospital Universitario de Salamanca, Salamanca, Spain. jbolanos@usal.es.
¹⁶ Centro de Investigación Biomédica en Red de Fragilidad y Envejecimiento Saludable (CIBERFES), Madrid, Spain. jbolanos@usal.es.

^# Contributed equally.

Abstract

CLN7 neuronal ceroid lipofuscinosis is an inherited lysosomal storage neurodegenerative disease highly prevalent in children. CLN7/MFSD8 gene encodes a lysosomal membrane glycoprotein, but the biochemical processes affected by CLN7-loss of function are unexplored thus preventing development of potential treatments. Here, we found, in the Cln7^∆ex2 mouse model of CLN7 disease, that failure in autophagy causes accumulation of structurally and bioenergetically impaired neuronal mitochondria. In vivo genetic approach reveals elevated mitochondrial reactive oxygen species (mROS) in Cln7^∆ex2 neurons that mediates glycolytic enzyme PFKFB3 activation and contributes to CLN7 pathogenesis. Mechanistically, mROS sustains a signaling cascade leading to protein stabilization of PFKFB3, normally unstable in healthy neurons. Administration of the highly selective PFKFB3 inhibitor AZ67 in Cln7^∆ex2 mouse brain in vivo and in CLN7 patients-derived cells rectifies key disease hallmarks. Thus, aberrant upregulation of the glycolytic enzyme PFKFB3 in neurons may contribute to CLN7 pathogenesis and targeting PFKFB3 could alleviate this and other lysosomal storage diseases.

Publication types

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

MeSH terms

Animals
Autophagy
Child, Preschool
Disease Models, Animal
Female
Humans
Lysosomal Membrane Proteins / metabolism
Lysosomal Storage Diseases / metabolism
Lysosomes / metabolism
Male
Membrane Transport Proteins / genetics
Membrane Transport Proteins / metabolism*
Mice
Mice, Inbred C57BL
Mitochondria / metabolism*
Neuronal Ceroid-Lipofuscinoses / genetics
Neuronal Ceroid-Lipofuscinoses / metabolism*
Neurons / metabolism
Phosphofructokinase-2 / genetics
Phosphofructokinase-2 / metabolism*
Up-Regulation

Substances

Lysosomal Membrane Proteins
MFSD8 protein, human
Membrane Transport Proteins
PFKFB3 protein, human
PFKFB3 protein, mouse
Phosphofructokinase-2

Supplementary concepts

Ceroid Lipofuscinosis, Neuronal, 7