Patient-derived ovarian cancer models demonstrate the influence of tumor-associated macrophages on therapeutic response.

While most ovarian cancer (OC) patients respond to front-line platinum/taxane chemotherapy and surgical debulking, the majority will develop platinum-resistance and recur. Our study investigated how tumor-associated macrophages (TAMs) within the tumor microenvironment (TME) affect chemotherapy outcomes using OC patient-derived organoids and humanized patient-derived xenografts (huPDX). macrophage migration assays demonstrated the selective recruitment of M2 macrophages to organoids. M2 macrophages, but not M1, increase organoid viability and reduce their sensitivity to paclitaxel in co-culture assays. Furthermore, BMS777607, a receptor tyrosine kinase inhibitor capable of repolarizing M2 macrophages , reduced organoid viability via a macrophage-dependent mechanism. In a platinum-sensitive huPDX model, the presence of human immune cells increased between-mouse variability in response to paclitaxel with two of four mice demonstrating tumor regrowth after two weeks. A TAM-targeted CSF-1 R inhibitor, BLZ945, combined with paclitaxel reduced tumor burden with no regrowth, suggesting that TAMs promote paclitaxel resistance in this model. Our study demonstrates that TAMs influence response to paclitaxel in both patient-derived OC organoids and huPDX. These models are useful for evaluating immunomodulatory therapy effects and could serve as a robust platform for preclinical testing of novel anti-cancer treatments, providing insights into the complex interplay between immune cells and cancer therapeutics.