Litcius/Paper detail

Notch signaling suppresses neuroendocrine differentiation and alters the immune microenvironment in advanced prostate cancer

Sheng‐Yu Ku, Yanqing Wang, Maria Mica Garcia, Yasutaka Yamada, Kei Mizuno, Mark D. Long, Spencer R. Rosario, Meenalakshmi Chinnam, Majd Al Assaad, Loredana Puca, Min Jin Kim, Martin Bakht, Varadha Balaji Venkadakrishnan, Brian D. Robinson, Andrés Acosta, Kristine M. Wadosky, Juan Miguel Mosquera, David W. Goodrich, Himisha Beltran

2024Journal of Clinical Investigation38 citationsDOIOpen Access PDF

Abstract

Notch signaling can have either an oncogenic or tumor-suppressive function in cancer depending on the cancer type and cellular context. While Notch can be oncogenic in early prostate cancer, we identified significant downregulation of the Notch pathway during prostate cancer progression from adenocarcinoma to neuroendocrine (NE) prostate cancer, where it functions as a tumor suppressor. Activation of Notch in NE and Rb1/Trp53-deficient prostate cancer models led to phenotypic conversion toward a more indolent, non-NE state with glandular features and expression of luminal lineage markers. This was accompanied by upregulation of MHC and type I IFN and immune cell infiltration. Overall, these data support Notch signaling as a suppressor of NE differentiation in advanced prostate cancer and provide insights into how Notch signaling influences lineage plasticity and the tumor microenvironment (TME).

Topics & Concepts

Immune systemProstate cancerNotch signaling pathwayCancer researchNeuroendocrine differentiationTumor microenvironmentProstateSignal transductionCancerCell signalingBiologyMedicineCell biologyImmunologyInternal medicineProstate Cancer Treatment and ResearchEpigenetics and DNA MethylationLung Cancer Research Studies