Location of pathogenic variants in <i>PSEN1</i> impacts progression of cognitive, clinical, and neurodegenerative measures in autosomal‐dominant Alzheimer's disease-Reference-Cited by-同舟云学术

Location of pathogenic variants in PSEN1 impacts progression of cognitive, clinical, and neurodegenerative measures in autosomal‐dominant Alzheimer's disease

Published:2023-06-08 Issue:8 Volume:22 Page:
ISSN:1474-9718
Container-title:Aging Cell
language:en
Short-container-title:Aging Cell

Author:

Schultz Stephanie A.¹^ORCID,Shirzadi Zahra¹,Schultz Aaron P.¹,Liu Lei²³^ORCID,Fitzpatrick Colleen D.¹,McDade Eric⁴,Barthelemy Nicolas R.⁴,Renton Alan⁵,Esposito Bianca⁵,Joseph‐Mathurin Nelly⁴,Cruchaga Carlos⁴,Chen Charles D.⁴,Goate Alison⁵,Allegri Ricardo Francisco⁶,Benzinger Tammie L. S.⁴,Berman Sarah⁷,Chui Helena C.⁸,Fagan Anne M.⁴,Farlow Martin R.⁹,Fox Nick C.¹⁰,Gordon Brian A.⁴,Day Gregory S.¹¹,Graff‐Radford Neill R.¹¹,Hassenstab Jason J.⁴,Hanseeuw Bernard J.¹²¹³,Hofmann Anna¹⁴,Jack Clifford R.¹⁵,Jucker Mathias¹⁴,Karch Celeste M.⁴,Koeppe Robert A.¹⁶,Lee Jae‐Hong¹⁷,Levey Allan I.¹⁸,Levin Johannes¹⁹²⁰²¹,Martins Ralph N.²²,Mori Hiroshi²³,Morris John C.⁴,Noble James²⁴,Perrin Richard J.⁴,Rosa‐Neto Pedro²⁵,Salloway Stephen P.²⁶,Sanchez‐Valle Raquel²⁷,Schofield Peter R.²⁸²⁹,Xiong Chengjie⁴,Johnson Keith A.¹²,Bateman Randall J.⁴,Sperling Reisa A.¹²,Chhatwal Jasmeer P.¹²,

Affiliation:

1. Massachusetts General Hospital, Harvard Medical School Boston Massachusetts USA

2. Brigham and Women's Hospital Boston Massachusetts USA

3. Ann Romney Center for Neurologic Diseases Boston Massachusetts USA

4. Washington University in St. Louis School of Medicine St. Louis Missouri USA

5. Department of Genetics and Genomic Sciences Icahn School of Medicine at Mount Sinai New York New York USA

6. INEBA Buenos Aires Argentina

7. University of Pittsburgh Pittsburgh Pennsylvania USA

8. Department of Neurology, Keck School of Medicine University of Southern California Los Angeles California USA

9. Indiana Alzheimer's Disease Research Center Indianapolis Indiana USA

10. Dementia Research Centre & UK Dementia Research Institute UCL Institute of Neurology London UK

11. Mayo Clinic Jacksonville Florida USA

12. Institute of Neuroscience, UCLouvain Brussels Belgium

13. Gordon Center for Medical Imaging in the Radiology Department of MGH Boston Massachusetts USA

14. German Center for Neurodegenerative Diseases (DZNE) Tuebingen Germany

15. Mayo Clinic Rochester Minnesota USA

16. University of Michigan Ann Arbor Michigan USA

17. Asan Medical Center University of Ulsan College of Medicine Seoul South Korea

18. Emory Goizueta Alzheimer's Disease Research Center Atlanta Georgia USA

19. German Center for Neurodegenerative Diseases (DZNE) Munich Germany

20. Department of Neurology Ludwig‐Maximilians‐Universität München Munich Germany

21. Munich Cluster for Systems Neurology (SyNergy) Munich Germany

22. Edith Cowan University Joondalup Western Australia Australia

23. Osaka City University Medical School Osaka Japan

24. Columbia University New York New York USA

25. Translational Neuroimaging Laboratory, Le Centre intégré universitaire de santé et de services sociaux (CIUSSS) de l'Ouest‐de‐l'Île‐de‐Montréal; Department of Neurology and Neurosurgery McGill University Montreal Canada

26. Butler Hospital Providence Rhode Island USA

27. Alzheimer's disease and other cognitive disorders Unit, Neurology Department, Hospital Clínic de Barcelona Institut d'Investigacions Biomediques Barcelona Spain

28. Neuroscience Research Australia Randwick New South Wales Australia

29. School of Medical Sciences University of New South Wales Sydney New South Wales Australia

Abstract

AbstractAlthough pathogenic variants in PSEN1 leading to autosomal‐dominant Alzheimer disease (ADAD) are highly penetrant, substantial interindividual variability in the rates of cognitive decline and biomarker change are observed in ADAD. We hypothesized that this interindividual variability may be associated with the location of the pathogenic variant within PSEN1. PSEN1 pathogenic variant carriers participating in the Dominantly Inherited Alzheimer Network (DIAN) observational study were grouped based on whether the underlying variant affects a transmembrane (TM) or cytoplasmic (CY) protein domain within PSEN1. CY and TM carriers and variant non‐carriers (NC) who completed clinical evaluation, multimodal neuroimaging, and lumbar puncture for collection of cerebrospinal fluid (CSF) as part of their participation in DIAN were included in this study. Linear mixed effects models were used to determine differences in clinical, cognitive, and biomarker measures between the NC, TM, and CY groups. While both the CY and TM groups were found to have similarly elevated Aβ compared to NC, TM carriers had greater cognitive impairment, smaller hippocampal volume, and elevated phosphorylated tau levels across the spectrum of pre‐symptomatic and symptomatic phases of disease as compared to CY, using both cross‐sectional and longitudinal data. As distinct portions of PSEN1 are differentially involved in APP processing by γ‐secretase and the generation of toxic β‐amyloid species, these results have important implications for understanding the pathobiology of ADAD and accounting for a substantial portion of the interindividual heterogeneity in ongoing ADAD clinical trials.

Funder

Alzheimer's Association

National Institute on Aging

Publisher

Wiley

Subject

Cell Biology,Aging

Link

https://onlinelibrary.wiley.com/doi/pdf/10.1111/acel.13871

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