Clinical and Genomic Features of Androgen Indifferent Prostate Cancer

Jack Masur; Aakrosh Ratan; Krzysztof Wierbilowicz; Adanma Ayanambakkam; Michelle L. Churchman; Laura S. Graham; George Daniel Grass; Sumati Gupta; Sean Q. Kern; Jennifer King; Zin Myint; Robert J. Rounbehler; Bodour Salhia; Eric A. Singer; Yousef Zakharia; Bryce M. Paschal; Paul V. Viscuse

doi:10.3390/ijms26020679

Clinical and Genomic Features of Androgen Indifferent Prostate Cancer

Jack Masur^*, Aakrosh Ratan, Krzysztof Wierbilowicz, Adanma Ayanambakkam, Michelle L. Churchman, Laura S. Graham, George Daniel Grass, Sumati Gupta, Sean Q. Kern, Jennifer King, Zin Myint, Robert J. Rounbehler, Bodour Salhia, Eric A. Singer, Yousef Zakharia, Bryce M. Paschal, Paul V. Viscuse

^*Corresponding author for this work

Research output: Contribution to journal › Article › peer-review

Abstract

Androgen-indifferent prostate cancer (AIPC) is increasingly common and particularly lethal. Data describing these tumors are sparse, and AIPC remains a poorly understood malignancy. Utilizing the Oncology Research Information Exchange Network (ORIEN) database, we enriched for tumors with features of AIPC using previously described characteristics. Our AIPC cohort included three subgroups: aggressive variant prostate cancer (AVPC), neuroendocrine PC (NEPC), and double-negative PC (DNPC). Of 1496 total PC patients available for analysis, we identified 323 (22%) as MCRPC. Of those, 39 (12%) met AIPC criteria (17 AVPC, 13 NEPC, 9 DNPC) and 284 (88%) were non-AIPC. Forty-three percent of AIPC patients had de novo metastatic disease vs. 15% for non-AIPC (p = 0.003). Homologous recombination deficiency (HRD) and tumor mutational burden (TMB) did not differ between cohorts, but microsatellite instability scores (MSI) were significantly higher in AIPC (p = 0.019). Using Gene Set Enrichment Analysis (GSEA), we found that genes defining response to androgens and genes involved in oxidative phosphorylation were the most downregulated, whereas genes involved in epithelial–mesenchymal transition (EMT) and immune signaling were significantly upregulated in AIPC vs. non-AIPC. Our study demonstrates the potential for predefined criteria that aim to enrich for AIPC and suggests opportunities for therapeutic investigation.

Original language	English
Article number	679
Journal	International Journal of Molecular Sciences
Volume	26
Issue number	2
DOIs	https://doi.org/10.3390/ijms26020679
State	Published - Jan 2025

Keywords

androgen-indifferent prostate cancer
biomarkers
genomics
molecular biology
prostate cancer
therapeutic targets

Access to Document

10.3390/ijms26020679

Cite this

Masur, J., Ratan, A., Wierbilowicz, K., Ayanambakkam, A., Churchman, M. L., Graham, L. S., Grass, G. D., Gupta, S., Kern, S. Q., King, J., Myint, Z., Rounbehler, R. J., Salhia, B., Singer, E. A., Zakharia, Y., Paschal, B. M., & Viscuse, P. V. (2025). Clinical and Genomic Features of Androgen Indifferent Prostate Cancer. International Journal of Molecular Sciences, 26(2), Article 679. https://doi.org/10.3390/ijms26020679

@article{78cce16bb55b4674b60d9cbe6dc89196,

title = "Clinical and Genomic Features of Androgen Indifferent Prostate Cancer",

abstract = "Androgen-indifferent prostate cancer (AIPC) is increasingly common and particularly lethal. Data describing these tumors are sparse, and AIPC remains a poorly understood malignancy. Utilizing the Oncology Research Information Exchange Network (ORIEN) database, we enriched for tumors with features of AIPC using previously described characteristics. Our AIPC cohort included three subgroups: aggressive variant prostate cancer (AVPC), neuroendocrine PC (NEPC), and double-negative PC (DNPC). Of 1496 total PC patients available for analysis, we identified 323 (22%) as MCRPC. Of those, 39 (12%) met AIPC criteria (17 AVPC, 13 NEPC, 9 DNPC) and 284 (88%) were non-AIPC. Forty-three percent of AIPC patients had de novo metastatic disease vs. 15% for non-AIPC (p = 0.003). Homologous recombination deficiency (HRD) and tumor mutational burden (TMB) did not differ between cohorts, but microsatellite instability scores (MSI) were significantly higher in AIPC (p = 0.019). Using Gene Set Enrichment Analysis (GSEA), we found that genes defining response to androgens and genes involved in oxidative phosphorylation were the most downregulated, whereas genes involved in epithelial–mesenchymal transition (EMT) and immune signaling were significantly upregulated in AIPC vs. non-AIPC. Our study demonstrates the potential for predefined criteria that aim to enrich for AIPC and suggests opportunities for therapeutic investigation.",

keywords = "androgen-indifferent prostate cancer, biomarkers, genomics, molecular biology, prostate cancer, therapeutic targets",

author = "Jack Masur and Aakrosh Ratan and Krzysztof Wierbilowicz and Adanma Ayanambakkam and Churchman, {Michelle L.} and Graham, {Laura S.} and Grass, {George Daniel} and Sumati Gupta and Kern, {Sean Q.} and Jennifer King and Zin Myint and Rounbehler, {Robert J.} and Bodour Salhia and Singer, {Eric A.} and Yousef Zakharia and Paschal, {Bryce M.} and Viscuse, {Paul V.}",

note = "Publisher Copyright: {\textcopyright} 2025 by the authors.",

year = "2025",

month = jan,

doi = "10.3390/ijms26020679",

language = "English",

volume = "26",

journal = "International Journal of Molecular Sciences",

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Masur, J, Ratan, A, Wierbilowicz, K, Ayanambakkam, A, Churchman, ML, Graham, LS, Grass, GD, Gupta, S, Kern, SQ, King, J, Myint, Z, Rounbehler, RJ, Salhia, B, Singer, EA, Zakharia, Y, Paschal, BM & Viscuse, PV 2025, 'Clinical and Genomic Features of Androgen Indifferent Prostate Cancer', International Journal of Molecular Sciences, vol. 26, no. 2, 679. https://doi.org/10.3390/ijms26020679

TY - JOUR

T1 - Clinical and Genomic Features of Androgen Indifferent Prostate Cancer

AU - Masur, Jack

AU - Ratan, Aakrosh

AU - Wierbilowicz, Krzysztof

AU - Ayanambakkam, Adanma

AU - Churchman, Michelle L.

AU - Graham, Laura S.

AU - Grass, George Daniel

AU - Gupta, Sumati

AU - Kern, Sean Q.

AU - King, Jennifer

AU - Myint, Zin

AU - Rounbehler, Robert J.

AU - Salhia, Bodour

AU - Singer, Eric A.

AU - Zakharia, Yousef

AU - Paschal, Bryce M.

AU - Viscuse, Paul V.

PY - 2025/1

Y1 - 2025/1

N2 - Androgen-indifferent prostate cancer (AIPC) is increasingly common and particularly lethal. Data describing these tumors are sparse, and AIPC remains a poorly understood malignancy. Utilizing the Oncology Research Information Exchange Network (ORIEN) database, we enriched for tumors with features of AIPC using previously described characteristics. Our AIPC cohort included three subgroups: aggressive variant prostate cancer (AVPC), neuroendocrine PC (NEPC), and double-negative PC (DNPC). Of 1496 total PC patients available for analysis, we identified 323 (22%) as MCRPC. Of those, 39 (12%) met AIPC criteria (17 AVPC, 13 NEPC, 9 DNPC) and 284 (88%) were non-AIPC. Forty-three percent of AIPC patients had de novo metastatic disease vs. 15% for non-AIPC (p = 0.003). Homologous recombination deficiency (HRD) and tumor mutational burden (TMB) did not differ between cohorts, but microsatellite instability scores (MSI) were significantly higher in AIPC (p = 0.019). Using Gene Set Enrichment Analysis (GSEA), we found that genes defining response to androgens and genes involved in oxidative phosphorylation were the most downregulated, whereas genes involved in epithelial–mesenchymal transition (EMT) and immune signaling were significantly upregulated in AIPC vs. non-AIPC. Our study demonstrates the potential for predefined criteria that aim to enrich for AIPC and suggests opportunities for therapeutic investigation.

AB - Androgen-indifferent prostate cancer (AIPC) is increasingly common and particularly lethal. Data describing these tumors are sparse, and AIPC remains a poorly understood malignancy. Utilizing the Oncology Research Information Exchange Network (ORIEN) database, we enriched for tumors with features of AIPC using previously described characteristics. Our AIPC cohort included three subgroups: aggressive variant prostate cancer (AVPC), neuroendocrine PC (NEPC), and double-negative PC (DNPC). Of 1496 total PC patients available for analysis, we identified 323 (22%) as MCRPC. Of those, 39 (12%) met AIPC criteria (17 AVPC, 13 NEPC, 9 DNPC) and 284 (88%) were non-AIPC. Forty-three percent of AIPC patients had de novo metastatic disease vs. 15% for non-AIPC (p = 0.003). Homologous recombination deficiency (HRD) and tumor mutational burden (TMB) did not differ between cohorts, but microsatellite instability scores (MSI) were significantly higher in AIPC (p = 0.019). Using Gene Set Enrichment Analysis (GSEA), we found that genes defining response to androgens and genes involved in oxidative phosphorylation were the most downregulated, whereas genes involved in epithelial–mesenchymal transition (EMT) and immune signaling were significantly upregulated in AIPC vs. non-AIPC. Our study demonstrates the potential for predefined criteria that aim to enrich for AIPC and suggests opportunities for therapeutic investigation.

KW - androgen-indifferent prostate cancer

KW - biomarkers

KW - genomics

KW - molecular biology

KW - prostate cancer

KW - therapeutic targets

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