Exploring Alzheimer's Disease Molecular Variability via Calculation of Personalized Transcriptional Signatures

Hila Dagan; Efrat Flashner-Abramson; Swetha Vasudevan; Maria R Jubran; Ehud Cohen; Nataly Kravchenko-Balasha

doi:10.3390/biom10040503

Exploring Alzheimer's Disease Molecular Variability via Calculation of Personalized Transcriptional Signatures

Biomolecules. 2020 Mar 26;10(4):503. doi: 10.3390/biom10040503.

Authors

Hila Dagan¹, Efrat Flashner-Abramson², Swetha Vasudevan², Maria R Jubran², Ehud Cohen³, Nataly Kravchenko-Balasha²

Affiliations

¹ The Rachel and Selim Benin School of Computer Science and Engineering, Hebrew University, Jerusalem 9190416, Israel.
² Department for Bio-medical Research, Faculty of Dental Medicine, Hebrew University of Jerusalem, Jerusalem 91120, Israel.
³ Department of Biochemistry and Molecular Biology, The Institute for Medical Research Israel - Canada, The Hebrew University School of Medicine, Jerusalem 9112102, Israel.

Abstract

Despite huge investments and major efforts to develop remedies for Alzheimer's disease (AD) in the past decades, AD remains incurable. While evidence for molecular and phenotypic variability in AD have been accumulating, AD research still heavily relies on the search for AD-specific genetic/protein biomarkers that are expected to exhibit repetitive patterns throughout all patients. Thus, the classification of AD patients to different categories is expected to set the basis for the development of therapies that will be beneficial for subpopulations of patients. Here we explore the molecular heterogeneity among a large cohort of AD and non-demented brain samples, aiming to address the question whether AD-specific molecular biomarkers can progress our understanding of the disease and advance the development of anti-AD therapeutics. We studied 951 brain samples, obtained from up to 17 brain regions of 85 AD patients and 22 non-demented subjects. Utilizing an information-theoretic approach, we deciphered the brain sample-specific structures of altered transcriptional networks. Our in-depth analysis revealed that 7 subnetworks were repetitive in the 737 diseased and 214 non-demented brain samples. Each sample was characterized by a subset consisting of ~1-3 subnetworks out of 7, generating 52 distinct altered transcriptional signatures that characterized the 951 samples. We show that 30 different altered transcriptional signatures characterized solely AD samples and were not found in any of the non-demented samples. In contrast, the rest of the signatures characterized different subsets of sample types, demonstrating the high molecular variability and complexity of gene expression in AD. Importantly, different AD patients exhibiting similar expression levels of AD biomarkers harbored distinct altered transcriptional networks. Our results emphasize the need to expand the biomarker-based stratification to patient-specific transcriptional signature identification for improved AD diagnosis and for the development of subclass-specific future treatment.

Keywords: Alzheimer’s disease; altered transcriptional network structure; information theory; patient-specific transcriptional signatures; surprisal analysis.

Publication types

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

MeSH terms

Aged
Aged, 80 and over
Alzheimer Disease / genetics*
Alzheimer Disease / physiopathology
Apolipoproteins E / genetics
Brain / physiopathology*
Calcium Signaling / genetics
Case-Control Studies
Databases, Genetic
Humans
Middle Aged
Precision Medicine / methods
Reproducibility of Results
Transcriptome / genetics*

Substances

ApoE protein, human
Apolipoproteins E