Clinical, pathologic, and molecular features of amphicrine prostate cancer

Author:

Graham Laura S.1ORCID,Haffner Michael C.2ORCID,Sayar Erolcan2ORCID,Gawne Agnes2,Schweizer Michael T.34ORCID,Pritchard Colin C.5,Coleman Ilsa2,Nelson Peter S.23,Yu Evan Y.34

Affiliation:

1. Department of Internal Medicine, Division of Medical Oncology  University of Colorado Aurora Colorado USA

2. Divisions of Human Biology and Clinical Research Division Fred Hutchinson Cancer Center Seattle Washington USA

3. Department of Internal Medicine, Division of Medical Oncology University of Washington Seattle Washington USA

4. Clinical Research Division Fred Hutchinson Cancer Center Seattle Washington USA

5. Department of Lab Medicine University of Washington Seattle Washington USA

Abstract

AbstractBackgroundAmphicrine prostate carcinoma (AMPC) is a poorly defined subset of prostate cancer in which cells co‐express luminal prostate epithelial and neuroendocrine markers. The optimal treatment strategy is unknown. We sought to further characterize the clinical, histomorphologic, and molecular characteristics of AMPC and to identify areas of potential future treatment investigations.MethodsWe retrospectively identified 17 cases of AMPC at a single institution, defined as synaptophysin expression in >70% of cells and co‐expression of androgen receptor (AR) signaling markers (either AR, PSA, or NKX3.1) in >50% of cells. Clinical and histologic features of AMPC cases as well as response to treatment and clinical outcomes were described.ResultsFive AMPC cases arose de novo in the absence of prior systemic treatment and behaved distinctly from cases that were treatment‐emergent. In these de novo cases, despite expression of neuroendocrine markers, prognosis appeared more favorable than high‐grade neuroendocrine carcinoma, with two (40%) patients with de novo metastatic disease, universal response to androgen deprivation therapy, and no deaths at a median follow‐up of 12.3 months. Treatment‐emergent AMPC arose a median of 41.1 months after androgen deprivation therapy initiation and was associated with poor response to therapy.ConclusionsWe show that amphicrine prostate cancer is a unique entity and differs in clinical and molecular features from high‐grade neuroendocrine carcinomas of the prostate. Our study highlights the need to recognize AMPC as a unique molecularly defined subgroup of prostate cancer.

Funder

U.S. Department of Defense

Doris Duke Charitable Foundation

National Institutes of Health

Publisher

Wiley

Subject

Urology,Oncology

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