Recent Discoveries in the Androgen Receptor Pathway in Castration-Resistant Prostate Cancer

Obinata, Daisuke; Lawrence, Mitchell G.; Takayama, Ken‐ichi; Choo, Nicholas; Risbridger, Gail P.; Takahashi, Satoru; Inoue, Satoshi

doi:10.3389/fonc.2020.581515

Cited by 30 publications

(42 citation statements)

References 132 publications

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“…Here, we describe two novel cell lines which represent castration resistant sublines of the commonly used, androgen dependent prostate cancer cells lines LAPC4 and VCaP. It is worth noting that other groups have described similar models previously [34][35][36][37][38][39]61 . However, for many of these lines there is limited profiling data publicly available.…”

Section: Discussionmentioning

confidence: 99%

“…To help fill this need, we developed two novel CRPC cell line models which were derived from the commonly used prostate cancer cell lines, LAPC4 and VCaP 20,32,33 . Although castration resistant sublines of VCaP and LAPC4 have been used in prior studies, [34][35][36][37][38][39] . We therefore present a comprehensive characterization of LAPC4-CR and VCaP-CR models and delineate transcriptional and proteomic differences between castration resistant and parental, androgen dependent lines.…”

Section: Introductionmentioning

confidence: 99%

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Phenotypic Characterization of Two Novel Cell Line Models of Castration Resistant Prostate Cancer

Haffner

Bhamidipati

Tsai

et al. 2021

Preprint

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BACKGROUND: Resistance to androgen deprivation therapies is a major driver of mortality in advanced prostate cancer. Therefore, there is a need to develop new pre-clinical models that allow the investigation of resistance mechanisms and the assessment of drugs for the treatment of castration resistant prostate cancer. METHODS: We generated two novel cell line models (LAPC4-CR and VCaP-CR) which were derived by passaging LAPC4 and VCaP cells in vivo and in vitro under castrate conditions. We performed detailed transcriptomic (RNA-seq) and proteomic analyses (SWATH-MS) to delineate expression differences between castration-sensitive and castration-resistant cell lines. Furthermore, we characterized the in vivo and in vitro growth characteristics of the novel cell line models. RESULTS: The two cell line derivatives LAPC4-CR and VCaP-CR showed castration resistant growth in vitro and in vivo which was only minimally inhibited by AR antagonists, enzalutamide and bicalutamide. High-dose androgen treatment resulted in significant growth arrest of VCaP-CR but not in LAPC4-CR cells. Both cell lines maintained AR expression, but exhibited distinct expression changes on the mRNA and protein level. Integrated analyses including data from LNCaP and the previously described castration resistant LNCaP-abl cells revealed an expression signature of castration resistance. CONCLUSIONS: The two novel cell line models LAPC4-CR and VCaP-CR and their comprehensive characterization on the RNA and protein level represent important resources to study the molecular mechanisms of castration resistance.

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Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Phenotypic Characterization of Two Novel Cell Line Models of Castration Resistant Prostate Cancer

Haffner

Bhamidipati

Tsai

et al. 2021

Preprint

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“…Other mutations, including T878A and F876L, show agonistic effects with treatment with AR antagonists flutamide and bicalutamide, respectively, as well as with new-generation AR antagonists such as enzalutamide [ 18 , 19 ]. Prominent AR mutations and their effects on AR activity are summarized well in another review [ 20 ].…”

Section: The Role Of Androgen Receptor (Ar) In Ar-dependent Castration-resistant Prostate Cancer (Crpc)mentioning

confidence: 99%

Undesirable Status of Prostate Cancer Cells after Intensive Inhibition of AR Signaling: Post-AR Era of CRPC Treatment

2021

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Recent advances in prostate cancer (PC) research unveiled real androgen receptor (AR) functions in castration-resistant PC (CRPC). Moreover, AR still accelerates PC cell proliferation via the activation of several mechanisms (e.g., mutation, variants, and amplifications in CRPC). New-generation AR signaling-targeted agents, inhibiting extremely the activity of AR, were developed based on these incontrovertible mechanisms of AR-induced CRPC progression. However, long-term administration of AR signaling-targeted agents subsequently induces the major problem that AR (complete)-independent CRPC cells present neither AR nor prostate-specific antigen, including neuroendocrine differentiation as a subtype of AR-independent CRPC. Moreover, there are few treatments effective for AR-independent CRPC with solid evidence. This study focuses on the transformation mechanisms of AR-independent from AR-dependent CRPC cells and potential treatment strategy for AR-independent CRPC and discusses them based on a review of basic and clinical literature.

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“…8,9 New therapies are required for these diverse forms of CRPC; however, preclinical development is often hampered by a shortage of patient-derived models and the limited ability to deploy them in drug screening. 10 Two of the most common ways in which human prostate cancer tissue is used in preclinical research is as patientderived xenografts (PDXs) and organoids. Serially transplantable PDXs are tumors that are continually transplanted in immunocompromised mice.…”

Section: Introductionmentioning

confidence: 99%

High-Throughput Imaging Assay for Drug Screening of 3D Prostate Cancer Organoids

et al. 2021

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New treatments are required for advanced prostate cancer; however, there are fewer preclinical models of prostate cancer than other common tumor types to test candidate therapeutics. One opportunity to increase the scope of preclinical studies is to grow tissue from patient-derived xenografts (PDXs) as organoid cultures. Here we report a scalable pipeline for automated seeding, treatment and an analysis of the drug responses of prostate cancer organoids. We established organoid cultures from 5 PDXs with diverse phenotypes of prostate cancer, including castrate-sensitive and castrate-resistant disease, as well as adenocarcinoma and neuroendocrine pathology. We robotically embedded organoids in Matrigel in 384-well plates and monitored growth via brightfield microscopy before treatment with poly ADP-ribose polymerase inhibitors or a compound library. Independent readouts including metabolic activity and live-cell imaging–based features provided robust measures of organoid growth and complementary ways of assessing drug efficacy. Single organoid analyses enabled in-depth assessment of morphological differences between patients and within organoid populations and revealed that larger organoids had more striking changes in morphology and composition after drug treatment. By increasing the scale and scope of organoid experiments, this automated assay complements other patient-derived models and will expedite preclinical testing of new treatments for prostate cancer.

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Recent Discoveries in the Androgen Receptor Pathway in Castration-Resistant Prostate Cancer

Cited by 30 publications

References 132 publications

Phenotypic Characterization of Two Novel Cell Line Models of Castration Resistant Prostate Cancer

Phenotypic Characterization of Two Novel Cell Line Models of Castration Resistant Prostate Cancer

Undesirable Status of Prostate Cancer Cells after Intensive Inhibition of AR Signaling: Post-AR Era of CRPC Treatment

High-Throughput Imaging Assay for Drug Screening of 3D Prostate Cancer Organoids

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