Characterization of ERG, AR and PTEN Gene Status in Circulating Tumor Cells from Patients with Castration-resistant Prostate Cancer

Overview

Journal Cancer Res

Specialty Oncology

Date 2009 Apr 3

PMID 19339269

Citations 247

Authors

Gerhardt Attard

Joost F Swennenhuis

David Olmos

Alison H M Reid

Elaine Vickers

Roger AHern

Rianne Levink

Frank Coumans

Joana Moreira

Ruth Riisnaes

Nikhil Babu Oommen

George Hawche

Charles Jameson

Emilda Thompson

Ronald Sipkema

Craig P Carden

Christopher Parker

David Dearnaley

Stan B Kaye

Colin S Cooper

Arturo Molina

Michael E Cox

Leon W M M Terstappen

Johann S de Bono

Affiliations

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Abstract

Hormone-driven expression of the ERG oncogene after fusion with TMPRSS2 occurs in 30% to 70% of therapy-naive prostate cancers. Its relevance in castration-resistant prostate cancer (CRPC) remains controversial as ERG is not expressed in some TMPRSS2-ERG androgen-independent xenograft models. However, unlike these models, CRPC patients have an increasing prostate-specific antigen, indicating active androgen receptor signaling. Here, we collected blood every month from 89 patients (54 chemotherapy-naive patients and 35 docetaxel-treated patients) treated in phase I/phase II clinical trials of an orally available, highly specific CYP17 inhibitor, abiraterone acetate, that ablates the synthesis of androgens and estrogens that drive TMPRSS2-ERG fusions. We isolated circulating tumor cells (CTC) by anti-epithelial cell adhesion molecule immunomagnetic selection followed by cytokeratin and CD45 immunofluorescence and 4',6-diamidino-2-phenylindole staining. We used multicolor fluorescence in situ hybridization to show that CRPC CTCs, metastases, and prostate tissue invariably had the same ERG gene status as therapy-naive tumors (n=31). We then used quantitative reverse transcription-PCR to show that ERG expression was maintained in CRPC. We also observed homogeneity in ERG gene rearrangement status in CTCs (n=48) in contrast to significant heterogeneity of AR copy number gain and PTEN loss, suggesting that rearrangement of ERG may be an earlier event in prostate carcinogenesis. We finally report a significant association between ERG rearrangements in therapy-naive tumors, CRPCs, and CTCs and magnitude of prostate-specific antigen decline (P=0.007) in CRPC patients treated with abiraterone acetate. These data confirm that CTCs are malignant in origin and indicate that hormone-regulated expression of ERG persists in CRPC.

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