Abstract
Adult hippocampal neurogenesis, the process of generating new neurons, relies on a rare population of neural stem and progenitor cells (NPCs) within the dentate gyrus complex microenvironment. Discovering the specific genes that define these cells is vital yet challenging due to overlapping expression patterns, limiting detection of rare cell populations using traditional approaches. By employing the computational digital sorting algorithm (DSA) that deconvolves complex gene expression data based on pattern recognition, we identified 129 genes enriched in murine NPCs. We validated these genes against published single-cell RNA sequencing (scRNA-seq) data and discovered that 25 human orthologs were known to cause Mendelian neurological conditions. In addition, leveraging a variety of computational tools and clinical and population databases, we identified 15 genes bearing novel damaging variants linked to neurological phenotypes, suggesting their potential role in contributing to human phenotypes. These discoveries illuminate NPC molecular underpinnings and underscore their relevance to both brain development and disease.