TY - JOUR
T1 - Discovery and validation of dominantly inherited Alzheimer’s disease mutations in populations from Latin America
AU - for the Dominantly Inherited Alzheimer Network
AU - Takada, Leonel Tadao
AU - Aláez-Verson, Carmen
AU - Burgute, Bhagyashri D.
AU - Nitrini, Ricardo
AU - Sosa, Ana Luisa
AU - Castilhos, Raphael Machado
AU - Chaves, Marcia Fagundes
AU - Longoria, Erika Mariana
AU - Carrillo-Sánchez, Karol
AU - Brucki, Sonia Maria Dozzi
AU - Flores-Lagunes, Luis Leonardo
AU - Molina, Carolina
AU - Olivares, Marcos Jimenez
AU - Ziegemeier, Ellen
AU - Petranek, Jennifer
AU - Goate, Alison M.
AU - Cruchaga, Carlos
AU - Renton, Alan E.
AU - Fernández, Maria Victoria
AU - Day, Gregory S.
AU - McDade, Eric
AU - Bateman, Randall J.
AU - Karch, Celeste M.
AU - Llibre-Guerra, Jorge J.
N1 - Funding Information:
The Dominantly Inherited Alzheimer Network (DIAN, U19AG032438) is funded by the National Institute on Aging (NIA), Alzheimer’s Association (SG-20-690363), the German Center for Neurodegenerative Diseases (DZNE), The Institute for Neurological Research (FLENI), and CONICET (PICT 2015/2110), partial support by the Research and Development Grants for Dementia from Japan Agency for Medical Research and Development, AMED, and the Korea Health Technology R&D Project through the Korea Health Industry Development Institute (KHIDI). This manuscript has been reviewed by DIAN Study investigators for scientific content and consistency of data interpretation with previous DIAN Study publications. We acknowledge the altruism of the participants and their families and the DIAN research and support staff at each of the participating sites for their contributions to this study.
Funding Information:
Data collection and sharing for this project was supported by The Dominantly Inherited Alzheimer Network (DIAN, UF1 AG032438), funded by the National Institute on Aging (NIA), Alzheimer’s Association (SG-20-690363), the Foundation for Barnes-Jewish Hospital, and the McDonnell Academy. This manuscript has been reviewed by DIAN Study investigators for scientific content and consistency of data interpretation with previous DIAN Study publications. The funding source had no role in the design and conduct of the study, collection, management, analysis, and interpretation of the data, preparation, review, or approval of the manuscript, or decision to submit the manuscript for publication. The corresponding author had full access to the data in the study and had final responsibility for the decision to submit for publication.
Publisher Copyright:
© 2022, The Author(s).
PY - 2022/12
Y1 - 2022/12
N2 - Background: In fewer than 1% of patients, AD is caused by autosomal dominant mutations in either the presenilin 1 (PSEN1), presenilin 2 (PSEN2), or amyloid precursor protein (APP) genes. The full extent of familial AD and frequency of these variants remains understudied in Latin American (LatAm) countries. Due to the rare nature of these variants, determining the pathogenicity of a novel variant in these genes can be challenging. Here, we use a systematic approach to assign the likelihood of pathogenicity in variants from densely affected families in Latin American populations. Methods: Clinical data was collected from LatAm families at risk for DIAD. Symptomatic family members were identified and assessed by local clinicians and referred for genetic counseling and testing. To determine the likelihood of pathogenicity among variants of unknown significance from LatAm populations, we report pedigree information, frequency in control populations, in silico predictions, and cell-based models of amyloid-beta ratios. Results: We identified five novel variants in the presenilin1 (PSEN1) gene from Brazilian and Mexican families. The mean age at onset in newly identified families was 43.5 years (range 36–54). PSEN1 p.Val103_Ser104delinsGly, p.Lys395Ile, p.Pro264Se, p.Ala275Thr, and p.Ile414Thr variants have not been reported in PubMed, ClinVar, and have not been reported in dominantly inherited AD (DIAD) families. We found that PSEN1 p.Val103_Ser104delinsGly, p.Lys395Ile, p.Pro264Se, and p.Ala275Thr produce Aβ profiles consistent with known AD pathogenic mutations. PSEN1 p.Ile414Thr did not alter Aβ in a manner consistent with a known pathogenic mutation. Conclusions: Our study provides further insights into the genetics of AD in LatAm. Based on our findings, including clinical presentation, imaging, genetic, segregations studies, and cell-based analysis, we propose that PSEN1 p.Val103_Ser104delinsGly, p.Lys395Ile, p.Pro264Se, and p.Ala275Thr are likely pathogenic variants resulting in DIAD, whereas PSEN1 p.Ile414Thr is likely a risk factor. This report is a step forward to improving the inclusion/engagement of LatAm families in research. Family discovery is of great relevance for the region, as new initiatives are underway to extend clinical trials and observational studies to families living with DIAD.
AB - Background: In fewer than 1% of patients, AD is caused by autosomal dominant mutations in either the presenilin 1 (PSEN1), presenilin 2 (PSEN2), or amyloid precursor protein (APP) genes. The full extent of familial AD and frequency of these variants remains understudied in Latin American (LatAm) countries. Due to the rare nature of these variants, determining the pathogenicity of a novel variant in these genes can be challenging. Here, we use a systematic approach to assign the likelihood of pathogenicity in variants from densely affected families in Latin American populations. Methods: Clinical data was collected from LatAm families at risk for DIAD. Symptomatic family members were identified and assessed by local clinicians and referred for genetic counseling and testing. To determine the likelihood of pathogenicity among variants of unknown significance from LatAm populations, we report pedigree information, frequency in control populations, in silico predictions, and cell-based models of amyloid-beta ratios. Results: We identified five novel variants in the presenilin1 (PSEN1) gene from Brazilian and Mexican families. The mean age at onset in newly identified families was 43.5 years (range 36–54). PSEN1 p.Val103_Ser104delinsGly, p.Lys395Ile, p.Pro264Se, p.Ala275Thr, and p.Ile414Thr variants have not been reported in PubMed, ClinVar, and have not been reported in dominantly inherited AD (DIAD) families. We found that PSEN1 p.Val103_Ser104delinsGly, p.Lys395Ile, p.Pro264Se, and p.Ala275Thr produce Aβ profiles consistent with known AD pathogenic mutations. PSEN1 p.Ile414Thr did not alter Aβ in a manner consistent with a known pathogenic mutation. Conclusions: Our study provides further insights into the genetics of AD in LatAm. Based on our findings, including clinical presentation, imaging, genetic, segregations studies, and cell-based analysis, we propose that PSEN1 p.Val103_Ser104delinsGly, p.Lys395Ile, p.Pro264Se, and p.Ala275Thr are likely pathogenic variants resulting in DIAD, whereas PSEN1 p.Ile414Thr is likely a risk factor. This report is a step forward to improving the inclusion/engagement of LatAm families in research. Family discovery is of great relevance for the region, as new initiatives are underway to extend clinical trials and observational studies to families living with DIAD.
KW - Dominantly inherited Alzheimer disease
KW - Early-onset Alzheimer disease
KW - Latin America
KW - Presenilin 1
UR - http://www.scopus.com/inward/record.url?scp=85135523924&partnerID=8YFLogxK
U2 - 10.1186/s13195-022-01052-1
DO - 10.1186/s13195-022-01052-1
M3 - Article
C2 - 35932032
AN - SCOPUS:85135523924
SN - 1758-9193
VL - 14
JO - Alzheimer's Research and Therapy
JF - Alzheimer's Research and Therapy
IS - 1
M1 - 108
ER -