CSF proteome profiling reveals biomarkers to discriminate dementia with Lewy bodies from Alzheimer´s disease.
Marta Del Campo MilanLisa VermuntCarel F W PeetersAnne SiebenYanaika S Hok-A-HinAlberto LleóDaniel AlcoleaMirrelijn van NeeSebastiaan EngelborghsJuliette L van AlphenSanaz ArezoumandanAlice Chen-PlotkinDavid J IrwinWiesje Maria van der FlierAfina W LemstraCharlotte E TeunissenPublished in: Nature communications (2023)
Diagnosis of dementia with Lewy bodies (DLB) is challenging and specific biofluid biomarkers are highly needed. We employed proximity extension-based assays to measure 665 proteins in the cerebrospinal fluid (CSF) from patients with DLB (n = 109), Alzheimer´s disease (AD, n = 235) and cognitively unimpaired controls (n = 190). We identified over 50 CSF proteins dysregulated in DLB, enriched in myelination processes among others. The dopamine biosynthesis enzyme DDC was the strongest dysregulated protein, and could efficiently discriminate DLB from controls and AD (AUC:0.91 and 0.81 respectively). Classification modeling unveiled a 7-CSF biomarker panel that better discriminate DLB from AD (AUC:0.93). A custom multiplex panel for six of these markers (DDC, CRH, MMP-3, ABL1, MMP-10, THOP1) was developed and validated in independent cohorts, including an AD and DLB autopsy cohort. This DLB CSF proteome study identifies DLB-specific protein changes and translates these findings to a practicable biomarker panel that accurately identifies DLB patients, providing promising diagnostic and clinical trial testing opportunities.
Keyphrases
- cerebrospinal fluid
- clinical trial
- mild cognitive impairment
- cognitive decline
- end stage renal disease
- cognitive impairment
- genome wide
- chronic kidney disease
- metabolic syndrome
- ejection fraction
- high throughput
- machine learning
- prognostic factors
- randomized controlled trial
- dna methylation
- single cell
- peritoneal dialysis
- small molecule
- parkinson disease
- study protocol