Multimodal investigation of melanopsin retinal ganglion cells in Alzheimer's disease

Author:

La Morgia Chiara123ORCID,Mitolo Micaela45,Romagnoli Martina3ORCID,Stanzani Maserati Michelangelo1,Evangelisti Stefania2ORCID,De Matteis Maddalena1,Capellari Sabina12,Bianchini Claudio2,Testa Claudia46,Vandewalle Gilles7ORCID,Santoro Aurelia89,Carbonelli Michele2,D'Agati Pietro1,Filardi Marco1011,Avanzini Pietro12,Barboni Piero13,Zenesini Corrado14,Baccari Flavia14,Liguori Rocco12ORCID,Tonon Caterina24,Lodi Raffaele24,Carelli Valerio23

Affiliation:

1. IRCCS Istituto delle Scienze Neurologiche di Bologna UOC Clinica Neurologica Bologna Italy

2. Dipartimento di Scienze Biomediche e Neuromotorie Università di Bologna Bologna Italy

3. IRCCS Istituto delle Scienze Neurologiche di Bologna Programma di Neurogenetica Bologna Italy

4. IRCCS Istituto delle Scienze Neurologiche di Bologna Programma Neuroimmagini Funzionali e Molecolari Bologna Italy

5. Dipartimento di Medicina e Chirurgia Università di Parma Parma Italy

6. Dipartimento di Fisica ed Astronomia Università di Bologna Bologna Italy

7. Sleep and Chronobiology Lab, GIGA‐Cyclotron Research Centre‐In Vivo Imaging University of Liège Liège Belgium

8. Dipartimento di Medicina Specialistica Diagnostica e Sperimentale Università di Bologna Bologna Italy

9. Alma Mater Research Institute on Global Challenges and Climate Change (Alma Climate) Università di Bologna Bologna Italy

10. Dipartimento di Medicina di Base, Neuroscienze e degli Organi di Senso Università di Bari Aldo Moro Bari Italy

11. Centro per le Malattie Neurodegenerative e l'Invecchiamento Cerebrale Università di Bari Aldo Moro‐ A.O. Pia Fondazione Cardinale G. Panico Tricase Italy

12. CNR Istituto di Neuroscienze Parma Italy

13. IRCCS San Raffaele Milan Italy

14. IRCCS Istituto delle Scienze Neurologiche di Bologna Unità di Epidemiologia e Statistica Bologna Italy

Abstract

AbstractObjectiveIn Alzheimer's disease (AD), the presence of circadian dysfunction is well‐known and may occur early in the disease course. The melanopsin retinal ganglion cell (mRGC) system may play a relevant role in contributing to circadian dysfunction. In this study, we aimed at evaluating, through a multimodal approach, the mRGC system in AD at an early stage of disease.MethodsWe included 29 mild–moderate AD (70.9 ± 11 years) and 26 (70.5 ± 8 years) control subjects. We performed an extensive neurophtalmological evaluation including optical coherence tomography with ganglion cell layer segmentation, actigraphic evaluation of the rest‐activity rhythm, chromatic pupillometry analyzed with a new data‐fitting approach, and brain functional MRI combined with light stimuli assessing the mRGC system.ResultsWe demonstrated a significant thinning of the infero‐temporal sector of the ganglion cell layer in AD compared to controls. Moreover, we documented by actigraphy the presence of a circadian‐impaired AD subgroup. Overall, circadian measurements worsened by age. Chromatic pupillometry evaluation highlighted the presence of a pupil‐light response reduction in the rod condition pointing to mRGC dendropathy. Finally, brain fMRI showed a reduced occipital cortex activation with blue light particularly for the sustained responses.InterpretationOverall, the results of this multimodal innovative approach clearly document a dysfunctional mRGC system at early stages of disease as a relevant contributing factor for circadian impairment in AD providing also support to the use of light therapy in AD.

Publisher

Wiley

Subject

Neurology (clinical),General Neuroscience

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