CSF proteomic profiling with amyloid/tau positivity identifies distinctive sex-different alteration of multiple proteins involved in Alzheimer's disease.
Anh N DoMuhammad AliJigyasha TimsinaLihua WangDaniel WesternMenghan LiuJessie SanfordMatitee Rosende-RocaMerce BoadaRaquel PuertaEdward N WilsonAgustin RuizPau Pastornull nullTony Wyss-CorayCruchaga CarlosYun Ju SungPublished in: medRxiv : the preprint server for health sciences (2024)
In Alzheimer's disease (AD), the most common cause of dementia, females have higher prevalence and faster progression, but sex-specific molecular findings in AD are limited. Here, we comprehensively examined and validated 7,006 aptamers targeting 6,162 proteins in cerebral spinal fluid (CSF) from 2,077 amyloid/tau positive cases and controls to identify sex-specific proteomic signatures of AD. In discovery (N=1,766), we identified 330 male-specific and 121 female-specific proteomic alternations in CSF (FDR <0.05). These sex-specific proteins strongly predicted amyloid/tau positivity (AUC=0.98 in males; 0.99 in females), significantly higher than those with age, sex, and APOE-ε4 (AUC=0.85). The identified sex-specific proteins were well validated (r≥0.5) in the Stanford study (N=108) and Emory study (N=148). Biological follow-up of these proteins led to sex differences in cell-type specificity, pathways, interaction networks, and drug targets. Male-specific proteins, enriched in astrocytes and oligodendrocytes, were involved in postsynaptic and axon-genesis. The male network exhibited direct connections among 152 proteins and highlighted PTEN, NOTCH1, FYN, and MAPK8 as hubs. Drug target suggested melatonin (used for sleep-wake cycle regulation), nabumetone (used for pain), daunorubicin, and verteporfin for treating AD males. In contrast, female-specific proteins, enriched in neurons, were involved in phosphoserine residue binding including cytokine activities. The female network exhibits strong connections among 51 proteins and highlighted JUN and 14-3-3 proteins (YWHAG and YWHAZ) as hubs. Drug target suggested biperiden (for muscle control of Parkinson's disease), nimodipine (for cerebral vasospasm), quinostatin and ethaverine for treating AD females. Together, our findings provide mechanistic understanding of sex differences for AD risk and insights into clinically translatable interventions.
Keyphrases
- subarachnoid hemorrhage
- cell proliferation
- physical activity
- spinal cord
- cognitive decline
- cerebrospinal fluid
- computed tomography
- magnetic resonance
- gene expression
- emergency department
- mild cognitive impairment
- skeletal muscle
- metabolic syndrome
- oxidative stress
- magnetic resonance imaging
- neuropathic pain
- pain management
- drug delivery
- high fat diet
- single cell
- drug induced
- amino acid
- binding protein
- nucleic acid