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<metadata xmlns:xsi="http://www.w3.org/2001/XMLSchema-instance" xmlns:dc="http://purl.org/dc/elements/1.1/"><dc:title>Population and single-cell analyses reveal immune cell-specific expression profiles associated with Alzheimer's disease risk</dc:title><dc:creator>Lindbohm,	Joni V.	(Avtor)
	</dc:creator><dc:creator>Stražar,	Martin	(Avtor)
	</dc:creator><dc:creator>Lee,	Hang-Mao	(Avtor)
	</dc:creator><dc:creator>Ashenberg,	Orr	(Avtor)
	</dc:creator><dc:creator>Mars,	Nina	(Avtor)
	</dc:creator><dc:description>INTRODUCTION Dysregulation of the peripheral immune system may increase Alzheimer's disease (AD) risk, but the underlying cell type-specific mechanisms remain unclear. METHODS We conducted Mendelian randomization and colocalization analyses of 4489 genes using single-cell expression quantitative trait locus data from unstimulated and stimulated peripheral immune cells, integrated with an AD genome-wide association study (N = 455,258). Spatial transcriptomics of brain tissue samples was used to identify brain-infiltrating immune cells. RESULTS Thirteen genes were associated with AD risk. Expression of BIN1, CTSW, CTSH, HLA-DRB1, TSTD1, PLEKHA1, and SCIMP increased AD risk, while EPHA1-AS1, FCER1G, FIBP, KAT8, STX4, and HLA-DQA1 reduced it. These associations were peripheral immune cell type and state specific. PLEKHA1 and TSTD1 were upregulated and FIBP downregulated in natural killer and T cells in AD brain tissue. DISCUSSION These findings link immune cell-specific gene expression to AD risk across activation states and within brain-infiltrating immune cells, highlighting potential targets for immune-based AD prevention and treatment.</dc:description><dc:date>2026</dc:date><dc:date>2026-03-25 11:02:43</dc:date><dc:type>Neznano</dc:type><dc:identifier>28598</dc:identifier><dc:identifier>UDK: 616.8</dc:identifier><dc:identifier>ISSN pri članku: 1552-5279</dc:identifier><dc:identifier>DOI: 10.1002/alz.71282</dc:identifier><dc:identifier>COBISS_ID: 272963843</dc:identifier><dc:language>sl</dc:language></metadata>
