摘要:SummaryAge is the major risk factor in most carcinomas, yet little is known about how proteomes change with age in any human epithelium. We present comprehensive proteomes comprised of >9,000 total proteins and >15,000 phosphopeptides from normal primary human mammary epithelia at lineage resolution from ten women ranging in age from 19 to 68 years. Data were quality controlled and results were biologically validated with cell-based assays. Age-dependent protein signatures were identified using differential expression analyses and weighted protein co-expression network analyses. Upregulation of basal markers in luminal cells, including KRT14 and AXL, were a prominent consequence of aging. PEAK1 was identified as an age-dependent signaling kinase in luminal cells, which revealed a potential age-dependent vulnerability for targeted ablation. Correlation analyses between transcriptome and proteome revealed age-associated loss of proteostasis regulation. Age-dependent proteome changes in the breast epithelium identified heretofore unknown potential therapeutic targets for reducing breast cancer susceptibility.Graphical abstractDisplay OmittedHighlights•Age-dependent proteomic profiling of HMECs at lineage resolution•Loss of proteostasis is unique to the luminal epithelial lineage with age•Identification of co-regulated proteins with age in luminal cells including PEAK1•PEAK1 inhibition selectively ablates older luminal cells – cancer cell of originDevelopmental biology; Complex system biology; Proteomics