Phenotypic characterization of two novel cell line models of castration‐resistant prostate cancer

Haffner, Michael C.; Bhamidipati, Akshay; Tsai, Harrison; Esopi, David; Vaghasia, Ajay; Low, Jin-Yih; Patel, Radhika A.; Güner, Güneş; Pham, Minh-Tam; Castagna, Nicole; Hicks, Jessica L.; Wyhs, Nicolas; Aebersold, Ruedi; Marzo, Angelo M. De; Nelson, William G.; Guo, Tiannan; Yegnasubramanian, Srinivasan

doi:10.1002/pros.24210

Cited by 9 publications

(12 citation statements)

References 73 publications

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“…Both hormone sensitive cell lines, LNCaP and VCaP, demonstrate altered ORR responses to metabolic inhibitors after ADT compared to control conditions (Figure 4B,C). Responses demonstrate some variation between lines which is unsurprising due to their different genetic phenotypes 48 . LNCaP cells in FBS control conditions show altered ORR (normalized to the media control) for all metabolic inhibitors (Figure 4B).…”

Section: Resultsmentioning

confidence: 99%

“…Previous work has investigated AR antagonists after ADT and observed similar signaling responses, 6,33 here, we focus on targeted metabolic inhibitors. Differences in responses to metabolic inhibitors was noted between hormone‐sensitive cell lines, reflecting the genetic and perhaps epigenetic heterogeneity of PC 48,54 . Importantly, OMI of two hormone sensitive lines showed that ADT‐treated cells were resistant to several targeted metabolic inhibitors, most notably inhibition of FA metabolism.…”

Section: Discussionmentioning

confidence: 99%

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Prostate cancer cells demonstrate unique metabolism and substrate adaptability acutely after androgen deprivation therapy

et al. 2022

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Background Androgen deprivation therapy (ADT) has been the standard of care for advanced hormone‐sensitive prostate cancer (PC), yet tumors invariably develop resistance resulting in castrate‐resistant PC. The acute response of cancer cells to ADT includes apoptosis and cell death, but a large fraction remains arrested but viable. In this study, we focused on intensively characterizing the early metabolic changes that result after ADT to define potential metabolic targets for treatment. Methods A combination of mass spectrometry, optical metabolic imaging which noninvasively measures drug responses in cells, oxygen consumption rate, and protein expression analysis was used to characterize and block metabolic pathways over several days in multiple PC cell lines with variable hormone response status including ADT sensitive lines LNCaP and VCaP, and resistant C4‐2 and DU145. Results Mass spectrometry analysis of LNCaP pre‐ and postexposure to ADT revealed an abundance of glycolytic intermediates after ADT. In LNCaP and VCaP, a reduction in the optical redox ratio [NAD(P)H/FAD], extracellular acidification rate, and a downregulation of key regulatory enzymes for fatty acid and glutamine utilization was acutely observed after ADT. Screening several metabolic inhibitors revealed that blocking fatty acid oxidation and synthesis reversed this stress response in the optical redox ratio seen with ADT alone in LNCaP and VCaP. In contrast, both cell lines demonstrated increased sensitivity to the glycolytic inhibitor 2‐Deoxy‐ d‐glucose(2‐DG) and maintained sensitivity to electron transport chain inhibitor Malonate after ADT exposure. ADT followed by 2‐DG results in synergistic cell death, a result not seen with simultaneous administration. Conclusions Hormone‐sensitive PC cells displayed altered metabolic profiles early after ADT including an overall depression in energy metabolism, induction of a quiescent/senescent phenotype, and sensitivity to selected metabolic inhibitors. Glycolytic blocking agents (e.g., 2‐DG) as a sequential treatment after ADT may be promising.

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Section: Resultsmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Prostate cancer cells demonstrate unique metabolism and substrate adaptability acutely after androgen deprivation therapy

et al. 2022

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“…Androgen treatment rapidly stimulates the transcription of hundreds to thousands of protein-encoding genes, but moreover, represses a number of genes, with a considerable overlap between different hormone-dependent prostate cancer cell lines [ 85 , 167 , 168 , 169 ]. A number of non-coding transcripts are also directly regulated by the AR [ 149 ].…”

Section: Transcriptomementioning

confidence: 99%

From Omics to Multi-Omics Approaches for In-Depth Analysis of the Molecular Mechanisms of Prostate Cancer

Nevedomskaya

Haendler

2022

IJMS

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Cancer arises following alterations at different cellular levels, including genetic and epigenetic modifications, transcription and translation dysregulation, as well as metabolic variations. High-throughput omics technologies that allow one to identify and quantify processes involved in these changes are now available and have been instrumental in generating a wealth of steadily increasing data from patient tumors, liquid biopsies, and from tumor models. Extensive investigation and integration of these data have led to new biological insights into the origin and development of multiple cancer types and helped to unravel the molecular networks underlying this complex pathology. The comprehensive and quantitative analysis of a molecule class in a biological sample is named omics and large-scale omics studies addressing different prostate cancer stages have been performed in recent years. Prostate tumors represent the second leading cancer type and a prevalent cause of cancer death in men worldwide. It is a very heterogenous disease so that evaluating inter- and intra-tumor differences will be essential for a precise insight into disease development and plasticity, but also for the development of personalized therapies. There is ample evidence for the key role of the androgen receptor, a steroid hormone-activated transcription factor, in driving early and late stages of the disease, and this led to the development and approval of drugs addressing diverse targets along this pathway. Early genomic and transcriptomic studies have allowed one to determine the genes involved in prostate cancer and regulated by androgen signaling or other tumor-relevant signaling pathways. More recently, they have been supplemented by epigenomic, cistromic, proteomic and metabolomic analyses, thus, increasing our knowledge on the intricate mechanisms involved, the various levels of regulation and their interplay. The comprehensive investigation of these omics approaches and their integration into multi-omics analyses have led to a much deeper understanding of the molecular pathways involved in prostate cancer progression, and in response and resistance to therapies. This brings the hope that novel vulnerabilities will be identified, that existing therapies will be more beneficial by targeting the patient population likely to respond best, and that bespoke treatments with increased efficacy will be available soon.

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“…Chromogranin A (CgA) is an acidic glycoprotein commonly expressed in all neuroendocrine cells and serum levels are increased in patients with neuroendocrine tumors 7 . Neuroendocrine activity can also be detected in prostate cancer as a marker of its neuroendocrine differentiation; more specifically, CgA levels are elevated in castration‐resistant PCa patients 8–11 …”

Section: Introductionmentioning

confidence: 99%

“…7 Neuroendocrine activity can also be detected in prostate cancer as a marker of its neuroendocrine differentiation; more specifically, CgA levels are elevated in castrationresistant PCa patients. [8][9][10][11] In recent years, the prognostic capacity of CgA as a biomarker for PCa has been extensively evaluated. Hong et al in their recent meta-analysis indicated that having high CgA levels represents an independent predictor of worse overall survival (OS) and progression-free survival (PFS) in castration-resistant prostate cancer (CRPC) patients.…”

Section: Introductionmentioning

confidence: 99%

Serum levels of chromogranin are not predictive of poorly differentiated prostate cancer: Results from a multicenter radical prostatectomy cohort

et al. 2022

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Background Recently a possible link between elevated Chromogranin A (CgA) levels and poorly differentiated prostate cancer has been proposed. The aim of our study was to explore the association of CgA levels and the risk of poorly differentiated prostate cancer (PCa) in men undergoing radical retropubic prostatectomy (RRP). Materials and Methods From 2012 onwards, 335 consecutive men undergoing RRP for PCa at three centers in Italy were enrolled into a prospective database. Body mass index (BMI) was calculated before RRP. Blood samples were collected and tested for total prostate‐specific antigen (PSA) levels and chromogranin A (CgA). We evaluated the association between serum levels of CgA and upstaging and upgrading using logistic regression analyses. Results Median age and preoperative PSA levels were 65 years (interquartile range [IQR]: 60–69) and 7.2 ng/ml (IQR: 5.3–10.4), respectively. Median BMI was 26.1 kg/m2 (IQR: 24–29) with 56 (16%) obese (BMI ≥ 30 kg/m2). Median CgA levels were 51 (39/71). Overall, 129/335 (38,5%) presented an upstaging, and 99/335 (30%) presented an upgrading. CgA was not a predictor of upstaging or upgrading on RP. Conclusions In our multicenter cohort of patients, CgA is not a predictor of poorly differentiated PCa on radical prostatectomy. According to our experience, CgA should not be considered a reliable marker to predict poorly differentiated or advanced prostate cancer.

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Phenotypic characterization of two novel cell line models of castration‐resistant prostate cancer

Cited by 9 publications

References 73 publications

Prostate cancer cells demonstrate unique metabolism and substrate adaptability acutely after androgen deprivation therapy

Prostate cancer cells demonstrate unique metabolism and substrate adaptability acutely after androgen deprivation therapy

From Omics to Multi-Omics Approaches for In-Depth Analysis of the Molecular Mechanisms of Prostate Cancer

Serum levels of chromogranin are not predictive of poorly differentiated prostate cancer: Results from a multicenter radical prostatectomy cohort

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