Cerebrospinal fluid mitochondrial DNA in the Alzheimer's disease continuum
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Date
2017-05-01Author
Cervera Carles, Laura
Alcolea, Daniel
Estanga Alustiza, Ainara
Ecay Torres, Mirian
Izagirre Otaegi, Andrea
Clerigué, Montserrat
García Sebastián, Maite
Villanua Bernues, Jorge Alberto
Escalas, Claudia
Blesa, Rafael
Martínez Lage, Pablo
Lleó, Alberto
Fortea, Juan
Clarimón, Jordi
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Neurobiology of Aging 53 : 192.e1-192.e4 (2017)
Abstract
Low levels of cell-free mitochondrial DNA (mtDNA) in the cerebrospinal fluid (CSF) of Alzheimer’s disease
(AD) patients have been identified and proposed as a novel biomarker for the disease. The lack of
validation studies of previous results prompted us to replicate this finding in a comprehensive series of
patients and controls. We applied droplet digital polymerase chain reaction in CSF specimens from 124
patients representing the AD spectrum and 140 neurologically healthy controls. The following pre-
analytical and analytical parameters were evaluated: the effect of freeze-thaw cycles on mtDNA, the
linearity of mtDNA load across serial dilutions, and the mtDNA levels in the diagnostic groups. We found
a wide range of mtDNA copies, which resulted in a high degree of overlap between groups. Although the
AD group presented significantly higher mtDNA counts, the receiver-operating characteristic analysis
disclosed an area under the curve of 0.715 to distinguish AD patients from controls. MtDNA was highly
stable with low analytical variability. In conclusion, mtDNA levels in CSF show a high interindividual
variability, with great overlap within phenotypes and presents low sensitivity for AD