Principal Investigator: Julie Anne Saugstad

Contributors: Joseph F. Quinn

DESCRIPTION (provided by applicant): Alzheimer’s disease (AD) is the most common form of dementia and is the sixth leading cause of death in the United States. The greatest known risk factor for AD is increasing age; the majority of people with AD are age 65 and older. AD is a progressive disease, with dementia symptoms gradually worsening over several years. Current AD treatments cannot stop disease progression, but they can temporarily slow the progression of dementia symptoms and improve quality of life for those with AD and their caregivers. There is no diagnostic biomarker that can be used to predict the onset of AD, nor is there a biomarker which can distinguish early AD from age-related dementia. Such a discriminatory tool would be invaluable in guiding clinicians towards early interventional efforts. The existence of extracellular RNAs in biofluids represents a fertile molecular landscape from which diagnostic and prognostic biomarkers may be isolated, characterized, and exploited. Accordingly, the identification of extracellular RNAs in the cerebrospinal fluid (CSF) provides an opportunity to define important biomarkers for clinical use in characterizing dementias such as AD. MicroRNAs are members of the non-protein-coding family of RNAs that serve as regulators of post-transcriptional gene expression. MicroRNAs are increasingly being identified in circulating fluids such as CSF, plasma, serum, and placental tissue, where their expression is correlated with several diseases including brain injury, degenerative diseases, and mental health disorders. We propose to identify microRNAs in CSF to examine their utility as diagnostic biomarkers for AD. To achieve this goal, we have established a highly qualified, multidisciplinary investigative team with expertise AD, dementia, and CSF biomarkers, advanced genomic methodologies, biostatistics, and clinical studies to examine the clinical utility of microRNAs in CSF as diagnostic biomarkers for AD.

Related Projects

exRNA Biomarkers for Human Glioma

Bob S. Carter
University of California, San Diego

Plasma miRNA Predictors of Adverse Mechanical and Electrical Remodeling After Myocardial Infarction

Bob S. Carter
Beth Israel Deaconess Medical Center

Extracellular RNAs: Biomarkers for Cardiovascular Risk and Disease

Jane E. Freedman
University of Massachusetts Medical School, Worcester

ExRNA Signatures Predict Outcomes After Brain Injury

Matthew Huentelman
Translational Genomics Research Institute

ExRNAs for Early Identification of Pregnancies at Risk for Placental Dysfunction

Louise C. Laurent
University Of California, San Diego

Extracellular Non-coding RNA Biomarkers of Hepatocellular Cancer

Tushar Patel
Mayo Clinic, Jacksonville

Clinical Utility of Extracellular RNA as Marker of Kidney Disease Progression

Thomas Tuschl
Rockefeller University

Circulating MicroRNAs as Disease Biomarkers in Multiple Sclerosis

Howard L. Weiner
Brigham And Women's Hospital

Clinical Utility of Salivary exRNA Biomarkers for Gastric Cancer Detection

David T. Wong
University Of California, Los Angeles