Platinum-Based Chemotherapy for Variant Castrate-Resistant Prostate Cancer

Aparicio, Ana; Harzstark, Andrea L.; Corn, Paul G.; Wen, Sijin; Araujo, John C.; Tu, Shi‐Ming; Pagliaro, Lance C.; Kim, Jeri; Millikan, Randall E.; Ryan, Charles J.; Tannir, Nizar M.; Zurita, Amado J.; Mathew, Paul; Arap, Wadih; Troncoso, Patricia; Thall, Peter F.; Logothetis, Christopher J.

doi:10.1158/1078-0432.ccr-12-3791

Cited by 353 publications

(377 citation statements)

References 43 publications

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“…Thus, prostate cancer cells with mutant p53 not only can evade apoptosis but likely will have more effective homologous recombination repair due to lack of suppression of RAD51 transcription by wild-type p53. Although none of the DNA-damaging chemotherapy agents has been approved for the treatment of prostate cancer, a platinum-based chemotherapy regimen demonstrated a 16-month median overall survival in a phase 2 study of 120 patients who met the predefined criteria of anaplastic prostate cancers (Aparicio et al, 2013). Anaplastic prostate cancer shares several features of small-cell prostate cancer and is likely enriched with cell cycle checkpoint alterations, based on its rapid proliferation.…”

Section: Discussionmentioning

confidence: 99%

Dynamic Regulation of Rad51 by E2F1 and p53 in Prostate Cancer Cells upon Drug-Induced DNA Damage under Hypoxia

Wang

McGregor

et al. 2014

Mol Pharmacol

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Intratumoral hypoxia has been proposed to create a "mutator" phenotype through downregulation of DNA repair, leading to increased genomic instability and drug resistance. Such downregulation of DNA repair has been proposed to sensitize hypoxic cancer cells to DNA-damaging agents and inhibitors of DNA repair. Here, we showed that prostate cancer cells with mutant p53 were resistant to the poly(ADP-ribose) polymerase inhibitor, veliparib (2-[(2R)-2-methylpyrrolidin-2-yl]-1H-benzimidazole-4-carboxamide, dihydrochloride; Abbott Laboratories, Abbott Park, IL), and the DNA-damaging topoisomerase I inhibitor camptothecin-11 (CPT-11) or SN38 (7-ethyl-10-hydroxycamptothecin) under hypoxia. Upregulation of Rad51 by E2F1 upon DNA damage under hypoxia contributed to such resistance, which was reversed by either inhibiting RAD51 transcription with small interfering RNA or by expressing wild-type p53 in the p53 null prostate cancer line. Accumulation of endogenous p53 but not E2F1 and suppressed RAD51 transcription was observed in prostate cancer line with wild-type p53 after DNA damage under hypoxia. Combining veliparib with CPT-11 significantly enhanced DNA damage and apoptosis under both hypoxic and normoxic culture conditions. Such enhanced DNA damage and antitumor activities were seen in the presence of Rad51 upregulation and confirmed in vivo with PC3 mouse xenografts. These data illustrate a dynamic regulation of Rad51 by E2F1 and p53 in prostate cancer cells' response to hypoxia and DNA damage. The veliparib and CPT-11 combination can be further explored as a treatment of metastatic castrationresistant prostate cancers that have frequent p53 mutations and enriched genomic instability.

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Section: Discussionmentioning

confidence: 99%

Dynamic Regulation of Rad51 by E2F1 and p53 in Prostate Cancer Cells upon Drug-Induced DNA Damage under Hypoxia

Wang

McGregor

et al. 2014

Mol Pharmacol

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“…2,3 In a subset of patients, therapeutic resistance to AR-targeting therapy is accompanied by the emergence of a histologic subtype that morphologically resembles de novo small-cell prostate cancer, a highly aggressive histologic variant present in , 1% of untreated prostate cancers at the time of diagnosis. 4 It is not clear if the treatment-emergent variant, variously labeled neuroendocrine prostate cancer and aggressive variant, 5,6 is the same disease entity as de novo small-cell prostate cancer. We have termed this histology treatment-emergent smallcell neuroendocrine prostate cancer or t-SCNC.…”

Section: Introductionmentioning

confidence: 99%

Clinical and Genomic Characterization of Treatment-Emergent Small-Cell Neuroendocrine Prostate Cancer: A Multi-institutional Prospective Study

Aggarwal

Huang

Alumkal

et al. 2018

JCO

497

618

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The prevalence and features of treatment-emergent small-cell neuroendocrine prostate cancer (t-SCNC) are not well characterized in the era of modern androgen receptor (AR)-targeting therapy. We sought to characterize the clinical and genomic features of t-SCNC in a multi-institutional prospective study. MethodsPatients with progressive, metastatic castration-resistant prostate cancer (mCRPC) underwent metastatic tumor biopsy and were followed for survival. Metastatic biopsy specimens underwent independent, blinded pathology review along with RNA/DNA sequencing. ResultsA total of 202 consecutive patients were enrolled. One hundred forty-eight (73%) had prior disease progression on abiraterone and/or enzalutamide. The biopsy evaluable rate was 79%. The overall incidence of t-SCNC detection was 17%. AR amplification and protein expression were present in 67% and 75%, respectively, of t-SCNC biopsy specimens. t-SCNC was detected at similar proportions in bone, node, and visceral organ biopsy specimens. Genomic alterations in the DNA repair pathway were nearly mutually exclusive with t-SCNC differentiation (P = .035). Detection of t-SCNC was associated with shortened overall survival among patients with prior AR-targeting therapy for mCRPC (hazard ratio, 2.02; 95% CI, 1.07 to 3.82). Unsupervised hierarchical clustering of the transcriptome identified a small-cell-like cluster that further enriched for adverse survival outcomes (hazard ratio, 3.00; 95% CI, 1.25 to 7.19). A t-SCNC transcriptional signature was developed and validated in multiple external data sets with . 90% accuracy. Multiple transcriptional regulators of t-SCNC were identified, including the pancreatic neuroendocrine marker PDX1.Conclusion t-SCNC is present in nearly one fifth of patients with mCRPC and is associated with shortened survival. The near-mutual exclusivity with DNA repair alterations suggests t-SCNC may be a distinct subset of mCRPC. Transcriptional profiling facilitates the identification of t-SCNC and novel therapeutic targets.J Clin Oncol 36.

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“…2). Evolving or secondary neuroendocrine transformation is increasingly recognized in advanced PC [20,21] and may represent one form of EP similar to what has recently been described in lung cancer [22]. It is well documented from autopsy and pathology studies of human PC that many histological phenotypes emerge during hormonal therapy for PC, including squamous differentiation, neuroendocrine differentiation, and a general loss of markers of prostate differentiation [6,23], as shown in Fig.…”

Section: Introductionmentioning

confidence: 88%

Development of a Novel Method to Detect Prostate Cancer Circulating Tumor Cells (CTCs) Based on Epithelial-Mesenchymal Transition Biology

Armstrong¹

2014

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Public reporting burden for this collection of information is estimated to average 1 hour per response, including the time for reviewing instructions, searching existing data sources, gathering and maintaining the data needed, and completing and reviewing this collection of information. Send comments regarding this burden estimate or any other aspect of this collection of information, including suggestions for reducing this burden to Department of Defense, Washington Headquarters Services, Directorate for Information Operations and Reports (0704-0188), 1215 Jefferson Davis Highway, Suite 1204, Arlington, VA 22202-4302. Respondents should be aware that notwithstanding any other provision of law, no person shall be subject to any penalty for failing to comply with a collection of information if it does not display a currently valid OMB control number. PLEASE DO NOT RETURN YOUR FORM TO THE ABOVE ADDRESS. REPORT DATE December 2014 REPORT TYPE PERFORMING ORGANIZATION NAME(S) AND ADDRESS(ES)Duke University Medical Durham, NC 27705 AND ADDRESS(ES) PERFORMING ORGANIZATION REPORT NUMBER SPONSORING / MONITORING AGENCY NAME(S) AND ADDRESS(ES) 10. SPONSOR/MONITOR'S ACRONYM(S) U.S. Army Medical Research and Materiel CommandFort Detrick, Maryland 21702-5012 SPONSOR/MONITOR'S REPORT NUMBER(S) DISTRIBUTION / AVAILABILITY STATEMENTApproved for Public Release; Distribution Unlimited SUPPLEMENTARY NOTES ABSTRACTThe purpose of this DOD NIA is to develop a novel method to detect circulating tumor cells (CTCs) from men with metastatic castration resistant prostate cancer (CRPC) based on a range of CTC phenotypes. The novel method employs a nanoparticle polymersome that contains near-infrared emissive porphyrins and permits antibody conjugation for target engagement and flow sorting in the infrared spectrum for specificity. We are developing near infrared emissive polymersomes (NIR-EPs) that contain antibodies to EpCAM, N-cadherin, OB-cadherin, and PSMA which permit the isolation and enumeration ev vivo of CTCs bearing these antigens in the circulation of men with CRPC. These specialized CTC detection nanoparticles permit the isolation of specific CTC phenotypes including epithelial, mesenchymal, and prostate cancer specific targets. In year 2 we have continued to optimize the methodology and chemistry for the creation of these NIR-EPs, including chemical synthesis, antibody conjugation, optimal reagents and processing, positive and negative control cell applications, and methods for red cell lysis, leukocyte depletion, and flow sorting of CTCs in the infrared spectrum. Challenges have included specificity due to antibody affinity during conjugation. This work is ongoing in the Therien laboratory to provide a clinical reagent for the ex vivo capture and identification of CTCs without binding to leukocytes nonspecifically. A 6 month no cost extension was requested to continue this optimization process. 2 Many patients with metastatic PC, however, have undetectable CTCs, limiting clinical utility. We have identified epithelial-mesench...

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Platinum-Based Chemotherapy for Variant Castrate-Resistant Prostate Cancer

Cited by 353 publications

References 43 publications

Dynamic Regulation of Rad51 by E2F1 and p53 in Prostate Cancer Cells upon Drug-Induced DNA Damage under Hypoxia

Dynamic Regulation of Rad51 by E2F1 and p53 in Prostate Cancer Cells upon Drug-Induced DNA Damage under Hypoxia

Clinical and Genomic Characterization of Treatment-Emergent Small-Cell Neuroendocrine Prostate Cancer: A Multi-institutional Prospective Study

Development of a Novel Method to Detect Prostate Cancer Circulating Tumor Cells (CTCs) Based on Epithelial-Mesenchymal Transition Biology

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