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Data from Supraphysiologic Testosterone Induces Ferroptosis and Activates Immune Pathways through Nucleophagy in Prostate Cancer

Posted on 2023-03-31 - 04:45
Abstract

The discovery that androgens play an important role in the progression of prostate cancer led to the development of androgen deprivation therapy (ADT) as a first line of treatment. However, paradoxical growth inhibition has been observed in a subset of prostate cancer upon administration of supraphysiologic levels of testosterone (SupraT), both experimentally and clinically. Here we report that SupraT activates cytoplasmic nucleic acid sensors and induces growth inhibition of SupraT-sensitive prostate cancer cells. This was initiated by the induction of two parallel autophagy-mediated processes, namely, ferritinophagy and nucleophagy. Consequently, autophagosomal DNA activated nucleic acid sensors converge on NFκB to drive immune signaling pathways. Chemokines and cytokines secreted by the tumor cells in response to SupraT resulted in increased migration of cytotoxic immune cells to tumor beds in xenograft models and patient tumors. Collectively, these findings indicate that SupraT may inhibit a subset of prostate cancer by activating nucleic acid sensors and downstream immune signaling.

Significance:

This study demonstrates that supraphysiologic testosterone induces two parallel autophagy-mediated processes, ferritinophagy and nucleophagy, which then activate nucleic acid sensors to drive immune signaling pathways in prostate cancer.

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FUNDING

DOD grants

Allegheny Health Network-Johns Hopkins Cancer Research Fund

Shared Instrumentation grant

NCI

Office of the Director of the National Institutes of Health

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Cancer Research

AUTHORS (25)

  • Rajendra Kumar
    Janet Mendonca
    Olutosin Owoyemi
    Kavya Boyapati
    Naiju Thomas
    Suthicha Kanacharoen
    Max Coffey
    Deven Topiwala
    Carolina Gomes
    Busra Ozbek
    Tracy Jones
    Marc Rosen
    Liang Dong
    Sadie Wiens
    W. Nathaniel Brennen
    John T. Isaacs
    Angelo M. De Marzo
    Mark C. Markowski
    Emmanuel S. Antonarakis
    David Z. Qian
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