Project description:Agrotis clavis (heart and club)

Project description:Agrotis clavis (heart and club) genome assembly, ilAgrClav1

Project description:Agrotis clavis (heart and club) genome assembly, ilAgrClav1, alternate haplotype

Project description:Agrotis clavis overview

Project description:Agrotis exclamationis (heart and dart moth), genomic and transcriptomic data

Project description:Schoenoplectus triqueter (club-rush), genomic and transcriptomic data

Project description:Clavariadelphus pistillaris (giant club), genomic and transcriptomic data

Project description:Agrotis puta (shuttle-shaped dart), genomic and transcriptomic data

Project description:Trypoxylon clavicerum (club horned wood borer wasp), genomic and transcriptomic data

Project description:Prostate cancer treatment resistance is a significant challenge facing the field. Genomic and transcriptomic profiling have partially elucidated the mechanisms through which cancer cells escape treatment, but their relation toward the tumor microenvironment (TME) remains elusive. Here we present a comprehensive transcriptomic landscape of the prostate TME at multiple points in the standard treatment timeline employing single-cell RNA-sequencing and spatial transcriptomics data from 120 patients. We identify club-like cells as a key epithelial cell subtype that acts as an interface between the prostate and the immune system. Tissue areas enriched with club-like cells have depleted androgen signaling and upregulated expression of luminal progenitor cell markers. Club-like cells display a senescence-associated secretory phenotype and their presence is linked to increased polymorphonuclear myeloid-derived suppressor cell (PMN-MDSC) activity. Our results indicate that club-like cells are associated with myeloid inflammation previously linked to androgen deprivation therapy resistance, providing a rationale for their therapeutic targeting.