Thus, these select differentially expressed proteins provide a molecular signature distinguishing control, AsymAD and AD brains. Gene ontology (GO) enrichment analysis of classifier proteins Sitagliptin phosphate monohydrate that are significantly decreased (n=67) in AD indicated overrepresentation of protein folding capacity and microtubule cytoskeleton proteins, whereas those related to response to protein stimulus and response to biotic stimulus, were over-represented among proteins increased in AD (n=55) (Fig. proteomics, we define changes in the proteome of human brain linked to preclinical and clinical stages of Alzheimers Disease (AD). These data uncover modules of co-expressed proteins that correlate with AD phenotypes, are distinct from modules recognized from gene co-expression data, and highlight non-neuronal drivers of disease. == Intro == The neuropathological changes of Alzheimers disease (AD) begin two decades or more before signs of cognitive impairment (Sperling et al., 2011). Currently, our understanding of the pathological events and the molecular transition from the asymptomatic phase (AsymAD) (Driscoll et al., 2006) to clinically evident dementia is limited. Although amyloid-beta (A) deposition in the brain is hypothesized to be a central force driving AD pathogenesis (Selkoe and Hardy, 2016), individuals remain cognitively normal for many years despite accumulating aggregates of A plaques and tau neurofibrillary tangles (Sperling et al., 2011). Large-scale analysis of molecular alterations in human brain provides an unbiased, data-driven approach to identify the many complicated processes involved in AD pathogenesis and to prioritize their links to relevant clinical and neuropathological traits, including changes in the asymptomatic phase of disease. Systems-level analyses of large data sets have emerged because essential tools for determining key molecular pathways and potential new drug focuses on. Algorithms such as weighted gene co-expression network analysis (WGCNA) classify the transcriptome into biologically meaningful modules of co-expressed genes linked to specific cell types, organelles, and biological pathways (Miller et al., 2008; Oldham, 2014). Co-expression modules also link to disease processes in which the most centrally connected genes are highly enriched intended for key drivers that play prominent Sitagliptin phosphate monohydrate roles in disease pathogenesis RIEG (Cerami et al., 2010; Huan et al., 2013; Tran et al., 2011). However , there are noticeable spatial, temporal, and quantitative differences between mRNA and protein expression (Abreu et al., 2009). In human being tissues only about one-third of mRNA-protein pairs show significant correlation in expression levels, with noticeable variation depending on their functions (Zhang et al., 2014a). This relationship is not well comprehended in complex tissues such as brain; mRNA-protein correlation coefficients reach no higher than 0. 47 even in terribly isolated brain cell types (Sharma et al., 2015). While transcriptome networks in AD brain have been examined (Miller et al., 2008; Miller et al., 2013; Zhang et al., 2013), network changes in the AD brain proteome, including those associated with early asymptomatic stages of disease, have not been explored. In this study, we coupled label-free mass Sitagliptin phosphate monohydrate spectrometry centered proteomics and systems biology to define networks of highly correlated proteins associated with neuropathology and cognitive decline in the brains of healthy controls, AsymAD, and AD. Similar to RNA-based networks, the brain proteome is organized in biologically meaningful networks related to distinct functions and cell types (i. e., neurons, oligodendrocyte, astrocyte, and microglia). Downregulation of modules associated with neurons and synapses and up-regulation of astroglial modules were strongly associated with amyloid plaque and neurofibrillary tangle pathologies, consistent with RNA-based networks previously reported for late stage AD. However , comparison of RNA and protein networks shows that more than half of the protein co-expression modules are not well represented at the RNA level. These include modules associated with microtubule function, RNA/DNA binding, post-translational modification, and inflammation that were also strongly associated with AD phenotypes. Moreover, several of these were linked to AsymAD, progressively changing with cognitive status, and disease specific (i. e., not altered in other neurodegenerative diseases). Finally, common AD risk loci, identified by the IGAP consortium genome wide association study (GWAS) were concentrated in glial-related modules in both the proteome and transcriptome consistent with their causal role in AD. Our findings highlight the use of large-scale proteomics and integrated systems Sitagliptin phosphate monohydrate biology to unravel the molecular etiology promoting initiation and progression of AD. == Results == == Proteomic analysis of human brain tissues == We collected post-mortem brain tissue from 50 individuals representing 15 controls, 15 AsymAD and 20 AD cases Sitagliptin phosphate monohydrate from the Baltimore Longitudinal Study of Aging (BLSA) (OBrien et al., 2009). For 47 cases, we analyzed tissue from both the dorsolateral prefrontal cortex (FC, Brodmann Area.