Understanding Failure and Improving Treatment Using HDAC Inhibitors for Prostate Cancer

Rana, Zohaib; Diermeier, Sarah D.; Hanif, Muhammad; Rosengren, Rhonda J.

doi:10.3390/biomedicines8020022

Cited by 59 publications

(47 citation statements)

References 130 publications

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“…Metastatic PCs (mPCs) are commonly managed with androgen deprivation therapy (ADT); resistance nonetheless commonly develops in the form of castration-resistant PC (CRPC) [ 11 , 12 ]. Although multiple therapeutic options are available for CRPCs, including taxane-based chemotherapy [ 13 ], AR-targeting therapy involving either abiraterone or enzalutamide [ 12 , 14 , 15 , 16 ], and immunotherapy [ 17 , 18 ], effective control of CRPC remains the major challenge [ 12 , 19 , 20 ]. This reflects the complex mechanisms underlying PC progression.…”

Section: Introductionmentioning

confidence: 99%

Differential Expression of a Panel of Ten CNTN1-Associated Genes during Prostate Cancer Progression and the Predictive Properties of the Panel towards Prostate Cancer Relapse

Chow

Kapoor

et al. 2021

Genes

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Contactin 1 (CNTN1) is a new oncogenic protein of prostate cancer (PC); its impact on PC remains incompletely understood. We observed CNTN1 upregulation in LNCaP cell-derived castration-resistant PCs (CRPC) and CNTN1-mediated enhancement of LNCaP cell proliferation. CNTN1 overexpression in LNCaP cells resulted in enrichment of the CREIGHTON_ENDOCRINE_THERAPY_RESISTANCE_3 gene set that facilitates endocrine resistance in breast cancer. The leading-edge (LE) genes (n = 10) of this enrichment consist of four genes with limited knowledge on PC and six genes novel to PC. These LE genes display differential expression during PC initiation, metastatic progression, and CRPC development, and they predict PC relapse following curative therapies at hazard ratio (HR) 2.72, 95% confidence interval (CI) 1.96–3.77, and p = 1.77 × 10-9 in The Cancer Genome Atlas (TCGA) PanCancer cohort (n = 492) and HR 2.72, 95% CI 1.84–4.01, and p = 4.99 × 10−7 in Memorial Sloan Kettering Cancer Center (MSKCC) cohort (n = 140). The LE gene panel classifies high-, moderate-, and low-risk of PC relapse in both cohorts. Additionally, the gene panel robustly predicts poor overall survival in clear cell renal cell carcinoma (ccRCC, p = 1.13 × 10−11), consistent with ccRCC and PC both being urogenital cancers. Collectively, we report multiple CNTN1-related genes relevant to PC and their biomarker values in predicting PC relapse.

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Section: Introductionmentioning

confidence: 99%

Differential Expression of a Panel of Ten CNTN1-Associated Genes during Prostate Cancer Progression and the Predictive Properties of the Panel towards Prostate Cancer Relapse

Chow

Kapoor

et al. 2021

Genes

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“…HDAC inhibitors attenuate acetylation events and block several cancer-related signaling pathways [ 59 ]. Small molecules containing zinc-binding groups, such as hydroxamic acids, have been among the most effective inhibitors of HDACs [ 60 , 61 ]. The 3-hydroxypyridin-2-thiones have shown potent and selective inhibitory activity for HDAC6 and HDAC8 with IC 50 values in the nM range [ 36 , 37 ] and are structurally similar to 1d and 1e .…”

Section: Resultsmentioning

confidence: 99%

High Antiproliferative Activity of Hydroxythiopyridones over Hydroxypyridones and Their Organoruthenium Complexes

et al. 2021

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Hydroxypyr(id)ones are a pharmaceutically important class of compounds that have shown potential in diverse areas of drug discovery. We investigated the 3-hydroxy-4-pyridones 1a–1c and 3-hydroxy-4-thiopyridones 1d–1f as well as their Ru(η6-p-cymene)Cl complexes 2a–2f, and report here the molecular structures of 1b and 1d as determined by X-ray diffraction analysis. Detailed cell biological investigations revealed potent cytotoxic activity, in particular of the 3-hydroxy-4-thiopyridones 1d–1f, while the Ru complexes of both compound types were less potent, despite still showing antiproliferative activity in the low μM range. The compounds did not modulate the cell cycle distribution of cancer cells but were cytostatic in A549 and cytotoxic in NCI-H522 non-small lung cancer cells, among other effects on cancer cells.

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“…While this strategy in prostate cancer still awaits to be further exploited, the (de-)acetylation inhibitors are already used in clinical trials. HDAC inhibitors vorinostat, pracinostat, panobinostat, and romidepsin underwent phase II clinical trials for prostate cancers but results were not satisfying to recommend phase III trials as majority of patients exhibited either toxicity or disease progression [ 435 ]. The CBP/p300 bromodomain inhibitor CCS1477, the only CBP/p300 inhibitor currently in clinical trials, is under clinical evaluation for the treatment of prostate cancer [ 436 ].…”

Section: Therapeutic Potential Of Post-translational Modificationsmentioning

confidence: 99%

Post-Translational Modifications That Drive Prostate Cancer Progression

Samaržija

2021

Biomolecules

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While a protein primary structure is determined by genetic code, its specific functional form is mostly achieved in a dynamic interplay that includes actions of many enzymes involved in post-translational modifications. This versatile repertoire is widely used by cells to direct their response to external stimuli, regulate transcription and protein localization and to keep proteostasis. Herein, post-translational modifications with evident potency to drive prostate cancer are explored. A comprehensive list of proteome-wide and single protein post-translational modifications and their involvement in phenotypic outcomes is presented. Specifically, the data on phosphorylation, glycosylation, ubiquitination, SUMOylation, acetylation, and lipidation in prostate cancer and the enzymes involved are collected. This type of knowledge is especially valuable in cases when cancer cells do not differ in the expression or mutational status of a protein, but its differential activity is regulated on the level of post-translational modifications. Since their driving roles in prostate cancer, post-translational modifications are widely studied in attempts to advance prostate cancer treatment. Current strategies that exploit the potential of post-translational modifications in prostate cancer therapy are presented.

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Understanding Failure and Improving Treatment Using HDAC Inhibitors for Prostate Cancer

Cited by 59 publications

References 130 publications

Differential Expression of a Panel of Ten CNTN1-Associated Genes during Prostate Cancer Progression and the Predictive Properties of the Panel towards Prostate Cancer Relapse

Differential Expression of a Panel of Ten CNTN1-Associated Genes during Prostate Cancer Progression and the Predictive Properties of the Panel towards Prostate Cancer Relapse

High Antiproliferative Activity of Hydroxythiopyridones over Hydroxypyridones and Their Organoruthenium Complexes

Post-Translational Modifications That Drive Prostate Cancer Progression

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