Your search keyword '"Whitehead Patrice L"' showing total 4 results

1. Increased APOE ε4 expression is associated with the difference in Alzheimer's disease risk from diverse ancestral backgrounds.

Author

Griswold AJ, Celis K, Bussies PL, Rajabli F, Whitehead PL, Hamilton-Nelson KL, Beecham GW, Dykxhoorn DM, Nuytemans K, Wang L, Gardner OK, Dorfsman DA, Bigio EH, Mesulam MM, Weintraub S, Geula C, Gearing M, McGrath-Martinez E, Dalgard CL, Scott WK, Haines JL, Pericak-Vance MA, Young JI, and Vance JM

Subjects

Aged, Aged, 80 and over, Alleles, Female, Heterozygote, Humans, Male, Alzheimer Disease ethnology, Alzheimer Disease genetics, Apolipoprotein E4 genetics, Black People genetics, Sequence Analysis, RNA, White People genetics

Abstract

Introduction: Apolipoprotein E (APOE) ε4 confers less risk for Alzheimer's disease (AD) in carriers with African local genomic ancestry (ALA) than APOE ε4 carriers with European local ancestry (ELA). Cell type specific transcriptional variation between the two local ancestries (LAs) could contribute to this disease risk differences., Methods: Single-nucleus RNA sequencing was performed on frozen frontal cortex of homozygous APOE ε4/ε4 AD patients: seven with ELA, four with ALA., Results: A total of 60,908 nuclei were sequenced. Within the LA region (chr19:44-46Mb), APOE was the gene most differentially expressed, with ELA carriers having significantly more expression (overall P < 1.8E -317 ) in 24 of 32 cell clusters. The transcriptome of one astrocyte cluster, with high APOE ε4 expression and specific to ELA, is suggestive of A1 reactive astrocytes., Discussion: AD patients with ELA expressed significantly greater levels of APOE than ALA APOE ε4 carriers. These differences in APOE expression could contribute to the reduced risk for AD seen in African APOE ε4 carriers., (© 2021 the Alzheimer's Association.)

Published

2021

2. Ancestral origin of ApoE ε4 Alzheimer disease risk in Puerto Rican and African American populations.

Author

Rajabli F, Feliciano BE, Celis K, Hamilton-Nelson KL, Whitehead PL, Adams LD, Bussies PL, Manrique CP, Rodriguez A, Rodriguez V, Starks T, Byfield GE, Sierra Lopez CB, McCauley JL, Acosta H, Chinea A, Kunkle BW, Reitz C, Farrer LA, Schellenberg GD, Vardarajan BN, Vance JM, Cuccaro ML, Martin ER, Haines JL, Byrd GS, Beecham GW, and Pericak-Vance MA

Subjects

Aged, Aged, 80 and over, Case-Control Studies, Female, Gene Frequency, Genetic Variation, Genetics, Population, Genome-Wide Association Study, Humans, Male, Puerto Rico ethnology, Risk Factors, Black or African American genetics, Alzheimer Disease genetics, Apolipoprotein E4 genetics, Hispanic or Latino genetics

Abstract

The ApoE ε4 allele is the most significant genetic risk factor for late-onset Alzheimer disease. The risk conferred by ε4, however, differs across populations, with populations of African ancestry showing lower ε4 risk compared to those of European or Asian ancestry. The cause of this heterogeneity in risk effect is currently unknown; it may be due to environmental or cultural factors correlated with ancestry, or it may be due to genetic variation local to the ApoE region that differs among populations. Exploring these hypotheses may lead to novel, population-specific therapeutics and risk predictions. To test these hypotheses, we analyzed ApoE genotypes and genome-wide array data in individuals from African American and Puerto Rican populations. A total of 1,766 African American and 220 Puerto Rican individuals with late-onset Alzheimer disease, and 3,730 African American and 169 Puerto Rican cognitively healthy individuals (> 65 years) participated in the study. We first assessed average ancestry across the genome ("global" ancestry) and then tested it for interaction with ApoE genotypes. Next, we assessed the ancestral background of ApoE alleles ("local" ancestry) and tested if ancestry local to ApoE influenced Alzheimer disease risk while controlling for global ancestry. Measures of global ancestry showed no interaction with ApoE risk (Puerto Rican: p-value = 0.49; African American: p-value = 0.65). Conversely, ancestry local to the ApoE region showed an interaction with the ApoE ε4 allele in both populations (Puerto Rican: p-value = 0.019; African American: p-value = 0.005). ApoE ε4 alleles on an African background conferred a lower risk than those with a European ancestral background, regardless of population (Puerto Rican: OR = 1.26 on African background, OR = 4.49 on European; African American: OR = 2.34 on African background, OR = 3.05 on European background). Factors contributing to the lower risk effect in the ApoE gene ε4 allele are likely due to ancestry-specific genetic factors near ApoE rather than non-genetic ethnic, cultural, and environmental factors., Competing Interests: The authors have declared that no competing interests exist.

Published

2018

3. Immune and Inflammatory Pathways Implicated by Whole Blood Transcriptomic Analysis in a Diverse Ancestry Alzheimer's Disease Cohort.

Author

Griswold, Anthony J., Sivasankaran, Sathesh K., Van Booven, Derek, Gardner, Olivia K., Rajabli, Farid, Whitehead, Patrice L., Hamilton-Nelson, Kara L., Adams, Larry D., Scott, Aja M., Hofmann, Natalia K., Vance, Jeffery M., Cuccaro, Michael L., Bush, William S., Martin, Eden R., Byrd, Goldie S., Haines, Jonathan L., Pericak-Vance, Margaret A., and Beecham, Gary W.

Subjects

BLOOD testing, ALZHEIMER'S disease, APOLIPOPROTEIN E4, NUCLEOTIDE sequence, GENEALOGY, GENE expression profiling, BRAIN metabolism, BIOCHEMISTRY, SEQUENCE analysis, CASE-control method, PHENOMENOLOGY, CELLULAR signal transduction, RESEARCH funding

Abstract

Background: Significant work has identified genetic variants conferring risk and protection for Alzheimer's disease (AD), but functional effects of these variants is lacking, particularly in under-represented ancestral populations. Expression studies performed in easily accessible tissue, such as whole blood, can recapitulate some transcriptional changes occurring in brain and help to identify mechanisms underlying neurodegenerative processes.Objective: We aimed to identify transcriptional differences between AD cases and controls in a cohort of diverse ancestry.Methods: We analyzed the protein coding transcriptome using RNA sequencing from peripheral blood collected from 234 African American (AA) (115 AD, 119 controls) and 240 non-Hispanic Whites (NHW) (121 AD, 119 controls). To identify case-control differentially expressed genes and pathways, we performed stratified, joint, and interaction analyses using linear regression models within and across ancestral groups followed by pathway and gene set enrichment analyses.Results: Overall, we identified 418 (291 upregulated, 127 downregulated) and 488 genes (352 upregulated, 136 downregulated) differentially expressed in the AA and NHW datasets, respectively, with only 16 genes commonly differentially expressed in both ancestral groups. Joint analyses provided greater power to detect case-control differences and identified 1,102 differentially expressed genes between cases and controls (812 upregulated, 290 downregulated). Interaction analysis identified only 27 genes with different effects in AA compared to NHW. Pathway and gene-set enrichment analyses revealed differences in immune response-related pathways that were enriched across the analyses despite different underlying gene sets.Conclusion: These results support the hypothesis of converging underlying pathophysiological processes in AD across ancestral groups. [ABSTRACT FROM AUTHOR]

Published

2020

4. Genetic analyses in multiplex families confirms chromosome 5q35 as a risk locus for Alzheimer's Disease in individuals of African Ancestry.

Author

Nuytemans, Karen, Rajabli, Farid, Jean-Francois, Melissa, Kurup, Jiji Thulaseedhara, Adams, Larry D., Starks, Takiyah D., Whitehead, Patrice L., Kunkle, Brian W., Caban-Holt, Allison, Haines, Jonathan L., Cuccaro, Michael L., Vance, Jeffery M., Byrd, Goldie S., Beecham, Gary W., Reitz, Christiane, and Pericak-Vance, Margaret A.

Subjects

*DISEASE risk factors, *APOLIPOPROTEIN E4, *GENE enhancers, *CHROMOSOMES, *GENEALOGY, *ALZHEIMER'S disease, *NUCLEOTIDE sequencing

Abstract

There is a paucity of genetic studies of Alzheimer Disease (AD) in individuals of African Ancestry, despite evidence suggesting increased risk of AD in the African American (AA) population. We performed whole-genome sequencing (WGS) and multipoint linkage analyses in 51 multi-generational AA AD families ascertained through the Research in African American Alzheimer Disease Initiative (REAAADI) and the National Institute on Aging Late Onset Alzheimer's disease (NIA-LOAD) Family Based Study. Variants were prioritized on minor allele frequency (<0.01), functional potential of coding and noncoding variants, co-segregation with AD and presence in multi-ancestry ADSP release 3 WGS data. We identified a significant linkage signal on chromosome 5q35 (HLOD=3.3) driven by nine families. Haplotype segregation analysis in the family with highest LOD score identified a 3'UTR variant in INSYN2B with the most functional evidence. Four other linked AA families harbor within-family shared variants located in INSYN2B 's promoter or enhancer regions. This AA family-based finding shows the importance of diversifying population-level genetic data to better understand the genetic determinants of AD on a global scale. • Genome-wide significant linkage (HLOD=3.3) on chr5q35 found in 9 AA AD families. • Rare regulatory variants for INSYN2B identified to segregate with AD in AA families. • Diversifying family-based design and WGS analyses crucial to understand AD globally. [ABSTRACT FROM AUTHOR]

Published

2024