Your search keyword '"HISTONE DEACETYLASE"' showing total 232 results

1. Recent Advances in the Clinical Translation of Small-Cell Lung Cancer Therapeutics.

Author

Das, Subhadeep and Samaddar, Shayak

Subjects

*THERAPEUTIC use of antineoplastic agents, *PROTEIN kinase inhibitors, *DRUG resistance in cancer cells, *ENZYME inhibitors, *CANCER chemotherapy, *LUNG tumors, *SMALL cell carcinoma, *HISTONE deacetylase, *DISEASE progression, *CHEMICAL inhibitors

Abstract

Simple Summary: Small-cell lung cancer (SCLC) is an aggressive type of lung cancer, often linked to a poor prognosis for the majority of patients. Platinum–etoposide-based chemotherapy, combined with immunotherapy, constitutes the standard treatment for patients with small-cell lung cancer (SCLC). Nonetheless, SCLC often recurs and develops resistance to treatment. The development of targeted treatment options for patients with SCLC has presented challenges; however, several emerging therapies demonstrate potential efficacy. Recent progress in SCLC research has uncovered essential insights into the biological traits of the disease, which could facilitate the discovery of biomarkers. Additionally, evaluating novel therapies will be crucial for enhancing treatment outcomes for patients with SCLC. Small-cell lung cancer (SCLC) is a recalcitrant form of cancer, representing 15% of lung cancer cases globally. SCLC is classified within the range of neuroendocrine pulmonary neoplasms, exhibiting shared morphologic, ultrastructural, immunohistochemical, and molecular genomic features. It is marked by rapid proliferation, a propensity for early metastasis, and an overall poor prognosis. The current conventional therapies involve platinum–etoposide-based chemotherapy in combination with immunotherapy. Nonetheless, the rapid emergence of therapeutic resistance continues to pose substantial difficulties. The genomic profiling of SCLC uncovers significant chromosomal rearrangements along with a considerable mutation burden, typically involving the functional inactivation of the tumor suppressor genes TP53 and RB1. Identifying biomarkers and evaluating new treatments is crucial for enhancing outcomes in patients with SCLC. Targeted therapies such as topoisomerase inhibitors, DLL3 inhibitors, HDAC inhibitors, PARP inhibitors, Chk1 inhibitors, etc., have introduced new therapeutic options for future applications. In this current review, we will attempt to outline the key molecular pathways that play a role in the development and progression of SCLC, together with a comprehensive overview of the most recent advancements in the development of novel targeted treatment strategies, as well as some ongoing clinical trials against SCLC, with the goal of improving patient outcomes. [ABSTRACT FROM AUTHOR]

Published

2025

2. HDAC Inhibitors Can Enhance Radiosensitivity of Head and Neck Cancer Cells Through Suppressing DNA Repair.

Author

Antrobus, Jennifer, Mackinnon, Bethany, Melia, Emma, Hughes, Jonathan R., and Parsons, Jason L.

Subjects

*SURVIVAL, *DIAGNOSTIC imaging, *RESEARCH funding, *HEAD & neck cancer, *RADIATION, *ENZYMES, *CELLULAR signal transduction, *TREATMENT effectiveness, *FLUORESCENT antibody technique, *CELL lines, *RADIATION-sensitizing agents, *DNA repair, *DNA damage, *MICROSCOPY, *HISTONE deacetylase, *EPIDERMAL growth factor receptors, *CHEMICAL inhibitors

Abstract

Simple Summary: Head and neck cancers are the seventh-most common cancers worldwide, with reported incidence of ~800,000 cases per year worldwide. Radiotherapy remains an important treatment for the disease, although cancer resistance remains a common problem. We performed a drug screen to identify those that can enhance the sensitivity of head and neck cancer models to radiotherapy. We identified that specific drugs (mocetinostat, CUDC-101, and pracinostat) can cause more effective cell killing of head and neck cancer cells grown in both 2D and 3D, and hold promise as more effective treatments for patients in the clinic. Background/Objectives: The incidence of head and neck squamous cell carcinoma (HNSCC), currently ~800,000 cases per year worldwide, is rising. Radiotherapy remains a mainstay for the treatment of HNSCC, although inherent radioresistance, particularly in human papillomavirus (HPV)-negative disease subtypes, remains a significant barrier to effective treatment. Therefore, combinatorial strategies using drugs or inhibitors against specific cellular targets are necessary to enhance HNSCC radiosensitivity to lead to an improvement in patient outcomes. Given that radiotherapy acts through targeting and damaging DNA, a common strategy is to focus on enzymes within DNA-dependent cellular pathways, such as DNA damage repair. Methods: Here, we have employed a 3D spheroid model of HNSCC (FaDu) in combination with a targeted drug screen to identify novel radiosensitisers that suppress tumour growth. Results: We identified that histone deacetylases (HDACs) were prominent candidates, and subsequently identified that the HDAC inhibitors mocetinostat and pracinostat, as well as the combined HDAC–epidermal growth factor receptor inhibitor CUDC-101, were effective at radiosensitising cell models of HNSCC (FaDu, A253, UMSCC11b) through their impact on both spheroid growth and clonogenic survival assays. We also demonstrated that this combinatorial strategy leads to inhibition of the repair of DNA double-strand breaks through the neutral comet assay and γH2AX foci analysis using immunofluorescence microscopy, providing a mechanism of action through which HDAC inhibition functions in HNSCC radiosensitisation. Conclusions: We believe that this approach should be further investigated in preclinical models, in order to realise the full therapeutic potential of HDAC inhibition for the radiosensitisation of HNSCC, eventually leading to improved patient treatment efficacy and outcomes. [ABSTRACT FROM AUTHOR]

Published

2024

3. HDAC6 as a Prognostic Factor and Druggable Target in HER2-Positive Breast Cancer.

Author

Cortesi, Michela, Bravaccini, Sara, Ravaioli, Sara, Petracci, Elisabetta, Angeli, Davide, Tumedei, Maria Maddalena, Balzi, William, Pirini, Francesca, Zanoni, Michele, Possanzini, Paola, Rocca, Andrea, Palleschi, Michela, Ulivi, Paola, Martinelli, Giovanni, and Maltoni, Roberta

Subjects

*BREAST cancer prognosis, *TRASTUZUMAB, *CANCER relapse, *DRUG resistance in cancer cells, *RESEARCH funding, *BREAST tumors, *PHARMACEUTICAL chemistry, *LOGISTIC regression analysis, *POLYMERASE chain reaction, *DESCRIPTIVE statistics, *GENE expression, *ODDS ratio, *CELL lines, *IMMUNOHISTOCHEMISTRY, *ONCOGENES, *DRUG efficacy, *CASE-control method, *CONFIDENCE intervals, *HISTONE deacetylase, *BIOMARKERS, *CHEMICAL inhibitors

Abstract

Simple Summary: Adjuvant trastuzumab is the standard of care for HER2+ breast cancer (BC) patients. However, >50% of patients become resistant. This study aimed at identifying the molecular factors associated with disease relapse and investigating them as therapeutically exploitable targets. Our findings encourage the exploration of the role of HDAC6 as a prognostic factor and the combinatorial use of HDAC6 selective inhibitors combined with trastuzumab in HER2+ BC, in particular for those patients experiencing drug resistance. Background: Adjuvant trastuzumab is the standard of care for HER2+ breast cancer (BC) patients. However, >50% of patients become resistant. This study aimed at the identification of the molecular factors associated with disease relapse and their further investigation as therapeutically exploitable targets. Methods: Analyses were conducted on formalin-fixed paraffin-embedded tissues of the primary tumors of relapsed (cases) and not relapsed (controls) HER2+ BC patients treated with adjuvant trastuzumab. The nCounter Human Breast Cancer Panel 360 was used. Logistic regression and partitioning around medoids were employed to identify the genes associated with disease recurrence. Cytotoxicity experiments using trastuzumab-resistant cell lines and a network pharmacology approach were carried out to investigate drug efficacy. Results: A total of 52 patients (26 relapsed and 26 not relapsed) were analyzed. We found that a higher expression of HDAC6 was significantly associated with an increased risk of recurrence, with an adjusted OR of 3.20 (95% CI 1.38–9.91, p = 0.016). Then, we investigated the cytotoxic activity of the selective HDAC6 inhibitor Nexturastat A (NextA) on HER2+ cell lines, which were both sensitive and trastuzumab-resistant. A sub-cytotoxic concentration of NextA, combined with trastuzumab, showed a synergistic effect on BC cell lines. Finally, using a network pharmacology approach, we identified HSP90AA1 as the putative molecular candidate responsible for the synergism observed in vitro. Conclusions: Our findings encourage the exploration of the role of HDAC6 as a prognostic factor and the combinatorial use of HDAC6 selective inhibitors combined with trastuzumab in HER2+ BC, in particular for those patients experiencing drug resistance. [ABSTRACT FROM AUTHOR]

Published

2024

4. Panobinostat Synergizes with Chemotherapeutic Agents and Improves Efficacy of Standard-of-Care Chemotherapy Combinations in Ewing Sarcoma Cells.

Author

Smith, Kaitlyn H., Trovillion, Erin M., Sholler, Chloe, Gandra, Divya, McKinney, Kimberly Q., Mulama, David, Dykema, Karl J., Nagulapally, Abhinav B., Oesterheld, Javier, and Saulnier Sholler, Giselle L.

Subjects

*THERAPEUTIC use of antineoplastic agents, *RESEARCH funding, *TUMORS in children, *ANTINEOPLASTIC agents, *CELL cycle, *CANCER cell culture, *CANCER chemotherapy, *RNA, *BIOINFORMATICS, *GENE expression, *CELL lines, *ETOPOSIDE, *DRUG efficacy, *DOXORUBICIN, *DNA damage, *EWING'S sarcoma, *CELL survival, *DRUG synergism, *HISTONE deacetylase, *PHARMACODYNAMICS

Abstract

Simple Summary: There has been little improvement in Ewing sarcoma survival rates over the past several decades and new therapeutic options are desperately needed. Histone deacetylases (HDACs) are known to play a role in cancer development and progression. We show that HDAC2 is overexpressed in Ewing sarcoma cells and that an HDAC inhibitor, Panobinostat, is cytotoxic to Ewing sarcoma cells both alone and when combined with standard of care. Mechanistically, we show that Panobinostat increases the DNA damage caused by standard of care leading to the death of the Ewing sarcoma cells. We believe that HDAC inhibition combined with standard-of-care chemotherapeutics may be an effective treatment option for Ewing sarcoma patients. Background: The survival rate of patients with Ewing sarcoma (EWS) has seen very little improvement over the past several decades and remains dismal for those with recurrent or metastatic disease. HDAC2, ALK, JAK1, and CDK4 were identified as potential targets using RNA sequencing performed on EWS patient tumors with the bioinformatic analysis of gene expression. Methods/Results: The pan-HDAC inhibitor Panobinostat was cytotoxic to all the Ewing sarcoma cell lines tested. Mechanistically, Panobinostat decreases the expression of proteins involved in the cell cycle, including Cyclin D1 and phospho-Rb, and DNA damage repair, including CHK1. Further, Panobinostat induces a G1 cell cycle arrest. The combination of Panobinostat with Doxorubicin or Etoposide, both of which are used as standard of care in upfront treatment, leads to a synergistic effect in EWS cells. The combination of Panobinostat and Doxorubicin induces an accumulation of DNA damage, a decrease in the expression of DNA damage repair proteins CHK1 and CHK2, and an increase in caspase 3 cleavage. The addition of Panobinostat to standard-of-care chemotherapy combinations significantly reduces cell viability compared to that of chemotherapy alone. Conclusions: Overall, our data indicate that HDAC2 is overexpressed in many EWS tumor samples and HDAC inhibition is effective in targeting EWS cells, alone and in combination with standard-of-care chemotherapy agents. This work suggests that the addition of an HDAC inhibitor to upfront treatment may improve response. [ABSTRACT FROM AUTHOR]

Published

2024

5. Histone Deacetylase Inhibitors for Peripheral T-Cell Lymphomas.

Author

Irimia, Ruxandra and Piccaluga, Pier Paolo

Subjects

*T-cell lymphoma, *ANTINEOPLASTIC agents, *APOPTOSIS, *CELL cycle, *TREATMENT effectiveness, *CANCER chemotherapy, *GENE expression, *HISTONE deacetylase, *CHEMICAL inhibitors

Abstract

Simple Summary: Nodal peripheral T-cell lymphomas (PTCLs) are among the most aggressive lymphomas and in the majority of cases are considered incurable. Therefore, there is a cogent need for novel therapies. In this review, the authors analyzed the biological rationale, the experimental experience, and the real-world data concerning the use of histone deacetylase inhibitors (HDACis) to treat PTCLs. Histone deacetylase inhibitors (HDACis) are being recognized as a potentially effective treatment approach for peripheral T-cell lymphomas (PTCLs), a heterogeneous group of aggressive malignancies with an unfavorable prognosis. Recent evidence has shown that HDACis are effective in treating PTCL, especially in cases where the disease has relapsed or is resistant to conventional treatments. Several clinical trials have demonstrated that HDACis, such as romidepsin and belinostat, can elicit long-lasting positive outcomes in individuals with PTCLs, either when used alone or in conjunction with conventional chemotherapy. They exert their anti-tumor effects by regulating gene expression through the inhibition of histone deacetylases, which leads to cell cycle arrest, induction of programmed cell death, and,the transformation of cancerous T cells, as demonstrated by gene expression profile studies. Importantly, besides clinical trials, real-world evidence indicated that the utilization of HDACis presents a significant and beneficial treatment choice for PTCLs. However, although HDACis showed potential effectiveness, they could not cure most patients. Therefore, new combinations with conventional drugs as well as new targeted agents are under investigation. [ABSTRACT FROM AUTHOR]

Published

2024

6. Epigenetics and Control of Tumor Angiogenesis in Melanoma: An Update with Therapeutic Implications.

Author

Cazzato, Gerardo, Sgarro, Nicoletta, Casatta, Nadia, Lupo, Carmelo, Ingravallo, Giuseppe, and Ribatti, Domenico

Subjects

*MELANOMA treatment, *THERAPEUTIC use of antineoplastic agents, *VASCULAR endothelial growth factors, *DNA methyltransferases, *CANCER invasiveness, *EPIGENOMICS, *MICRORNA, *GLYCOPROTEINS, *NEOVASCULARIZATION inhibitors, *DNA methylation, *HISTONES, *METASTASIS, *GENE expression, *NEOVASCULARIZATION, *HISTONE deacetylase, *CHEMICAL inhibitors

Abstract

Simple Summary: Angiogenesis is a crucial process in the progression and metastasis of melanoma. Recent research has highlighted the significant role of epigenetic modifications in regulating angiogenesis. This review comprehensively examines the current understanding of how epigenetic mechanisms, including DNA methylation, histone modifications, and non-coding RNAs, influence angiogenic pathways in melanoma, with some important therapeutic approaches. Angiogenesis, the formation of new blood vessels from pre-existing ones, is a crucial process in the progression and metastasis of melanoma. Recent research has highlighted the significant role of epigenetic modifications in regulating angiogenesis. This review comprehensively examines the current understanding of how epigenetic mechanisms, including DNA methylation, histone modifications, and non-coding RNAs, influence angiogenic pathways in melanoma. DNA methylation, a key epigenetic modification, can silence angiogenesis inhibitors such as thrombospondin-1 and TIMP3 while promoting pro-angiogenic factors like vascular endothelial growth factor (VEGF). Histone modifications, including methylation and acetylation, also play a pivotal role in regulating the expression of angiogenesis-related genes. For instance, the acetylation of histones H3 and H4 is associated with the upregulation of pro-angiogenic genes, whereas histone methylation patterns can either enhance or repress angiogenic signals, depending on the specific histone mark and context. Non-coding RNAs, particularly microRNAs (miRNAs) further modulate angiogenesis. miRNAs, such as miR-210, have been identified as key regulators, with miR-9 promoting angiogenesis by targeting E-cadherin and enhancing the expression of VEGF. This review also discusses the therapeutic potential of targeting epigenetic modifications to inhibit angiogenesis in melanoma. Epigenetic drugs, such as DNA methyltransferase inhibitors (e.g., 5-azacytidine) and histone deacetylase inhibitors (e.g., Vorinostat), have shown promise in preclinical models by reactivating angiogenesis inhibitors and downregulating pro-angiogenic factors. Moreover, the modulation of miRNAs and lncRNAs presents a novel approach for anti-angiogenic therapy. [ABSTRACT FROM AUTHOR]

Published

2024

7. Inhibition of Histone Deacetylase Activity Increases Cisplatin Efficacy to Eliminate Metastatic Cells in Pediatric Liver Cancers.

Author

Gulati, Ruhi, Fleifil, Yasmeen, Jennings, Katherine, Bondoc, Alex, Tiao, Greg, Geller, James, Timchenko, Lubov, and Timchenko, Nikolai

Subjects

*RISK assessment, *CISPLATIN, *CANCER relapse, *CANCER, *ENZYME inhibitors, *ANTINEOPLASTIC agents, *NEURONS, *CELL proliferation, *DISEASE eradication, *HEPATOBLASTOMA, *TRANSCRIPTION factors, *METASTASIS, *CELL lines, *FIBROBLASTS, *DRUG efficacy, *HEPATOCELLULAR carcinoma, *HISTONE deacetylase, *PHARMACODYNAMICS, *DISEASE risk factors, *CHILDREN

Abstract

Simple Summary: Patients with pediatric liver cancers hepatoblastoma and hepatocellular carcinoma very often develop lung metastases. These cancers can present with lung metastases and are at higher risk of relapse. Although cisplatin is very effective at clearing lung metastases, they can still relapse. Therefore, there is an urgent need to develop therapeutic approaches to prevent the development of lung metastases in patients with pediatric liver cancers. In this paper, we show that the metastatic microenvironment of HBL and HCC patients contains a heterogeneous cell population that formed tumor clusters. We found that both fresh primary tumors and generated primary cell cultures had increased the expression of HDAC1, a histone deacetylase, and the transcription factor Sp5. Sp5 and HDAC1 work in tandem by transporting HDAC1 to the promoters of genes and changing their expression. We analyzed the effects of the HDAC inhibitor, SAHA, on the metastasis-initiating cells in combination with cisplatin. We found that HDAC inhibition increases the efficacy of cisplatin to eliminate these metastasis-initiating cells. The pediatric liver cancers, hepatoblastoma and hepatocellular carcinoma, are dangerous cancers which often spread to the lungs. Although treatments with cisplatin significantly improve outcomes, cisplatin may not eliminate metastasis-initiating cells. Our group has recently shown that the metastatic microenvironments of hepatoblastoma contain Cancer Associated Fibroblasts (CAFs) and neuron-like cells, which initiate cancer spread from liver to lungs. In this study, we found that these cells express high levels of HDAC1; therefore, we examined if histone deacetylase inhibition improves cisplatin anti-proliferative effects and reduces the formation of tumor clusters in pediatric liver cancer metastatic microenvironments. Methods: New cell lines were generated from primary hepatoblastoma liver tumors (hbl) and lung metastases (LM) of HBL patients. In addition, cell lines were generated from hepatocellular neoplasm, not otherwise specified (HCN-NOS) tumor samples, and hcc cell lines. Hbl, LM and hcc cells were treated with cisplatin, SAHA or in combination. The effect of these drugs on the number of cells, formation of tumor clusters and HDAC1-Sp5-p21 axis were examined. Results: Both HBL and HCC tissue specimens have increased HDAC1-Sp5 pathway activation, recapitulated in cell lines generated from the tumors. HDAC inhibition with vorinostat (SAHA) increases cisplatin efficacy to eliminate CAFs in hbl and in hcc cell lines. Although the neuron-like cells survive the combined treatments, proliferation was inhibited. Notably, combining SAHA with cisplatin overcame cisplatin resistance in an LM cell line from an aggressive case with multiple metastases. Underlying mechanisms of this enhanced inhibition include suppression of the HDAC1-Sp5 pathway and elevation of an inhibitor of proliferation p21. Similar findings were found with gemcitabine treatments suggesting that elimination of proliferative CAFs cells is a key event in the inhibition of mitotic microenvironment. Conclusions: Our studies demonstrate the synergistic benefits of HDAC inhibition and cisplatin to eliminate metastasis-initiating cells in pediatric liver cancers. [ABSTRACT FROM AUTHOR]

Published

2024

8. G9a in Cancer: Mechanisms, Therapeutic Advancements, and Clinical Implications.

Author

Ni, Yuchao, Shi, Mingchen, Liu, Liangliang, Lin, Dong, Zeng, Hao, Ong, Christopher, and Wang, Yuzhuo

Subjects

*PROTEIN metabolism, *EPIGENOMICS, *IMMUNOTHERAPY, *CELL proliferation, *PROSTATE tumors, *HISTONES, *METHYLTRANSFERASES, *GENE expression, *TUMOR suppressor genes, *MOLECULAR structure, *MOLECULAR biology, *DISEASE progression, *HISTONE deacetylase

Abstract

Simple Summary: In this review, we have summarized the crucial role of G9a in cellular biology and disease. By synthesizing recent research discoveries, we delve into the functions of G9a in gene expression regulation, cell proliferation, and biological development. Additionally, we explore its potential involvement in cancer and discuss its prospects as a therapeutic target specifically in prostate cancer. In summary, this review provides a comprehensive perspective on G9a, enhances understanding of the significance of G9a in biology and cancer, and offers insights into future research and drug development. G9a, also named EHMT2, is a histone 3 lysine 9 (H3K9) methyltransferase responsible for catalyzing H3K9 mono- and dimethylation (H3K9me1 and H3K9me2). G9a contributes to various aspects of embryonic development and tissue differentiation through epigenetic regulation. Furthermore, the aberrant expression of G9a is frequently observed in various tumors, particularly in prostate cancer, where it contributes to cancer pathogenesis and progression. This review highlights the critical role of G9a in multiple cancer-related processes, such as epigenetic dysregulation, tumor suppressor gene silencing, cancer lineage plasticity, hypoxia adaption, and cancer progression. Despite the increased research on G9a in prostate cancer, there are still significant gaps, particularly in understanding its interactions within the tumor microenvironment and its broader epigenetic effects. Furthermore, this review discusses the recent advancements in G9a inhibitors, including the development of dual-target inhibitors that target G9a along with other epigenetic factors such as EZH2 and HDAC. It aims to bring together the existing knowledge, identify gaps in the current research, and suggest future directions for research and treatment strategies. [ABSTRACT FROM AUTHOR]

Published

2024

9. A Comprehensive Understanding of Post-Translational Modification of Sox2 via Acetylation and O -GlcNAcylation in Colorectal Cancer.

Author

Seo, Yoojeong, Kim, Dong Keon, Park, Jihye, Park, Soo Jung, Park, Jae Jun, Cheon, Jae Hee, and Kim, Tae Il

Subjects

*CARRIER proteins, *RESEARCH funding, *COLORECTAL cancer, *TRANSCRIPTION factors, *METABOLISM, *LIQUID chromatography, *PROTEOMICS, *ACETYLTRANSFERASES, *MASS spectrometry, *TRANSFERASES, *HISTONE deacetylase, *SEX determination

Abstract

Simple Summary: This study provides insights into the regulation of Sox2, specifically focusing on the acetylation of Sox2 K75 residue and O-GlcNAcylation of S246 residue. These post-translational modifications (PTM) are orchestrated through interactions with ACSS2/p300 for acetylation and miR29a/HDAC4 for deacetylation, respectively. These findings shed light on the significance of these PTMs in the development and progression of colorectal cancer. Aberrant expression of the pluripotency-associated transcription factor Sox2 is associated with poor prognosis in colorectal cancer (CRC). We investigated the regulatory roles of major post-translational modifications in Sox2 using two CRC cell lines, SW480 and SW620, derived from the same patient but with low and high Sox2 expression, respectively. Acetylation of K75 in the Sox2 nuclear export signal was relatively increased in SW480 cells and promotes Sox2 nucleocytoplasmic shuttling and proteasomal degradation of Sox2. LC-MS-based proteomics analysis identified HDAC4 and p300 as binding partners involved in the acetylation-mediated control of Sox2 expression in the nucleus. Sox2 K75 acetylation is mediated by the acetyltransferase activity of CBP/p300 and ACSS3. In SW620 cells, HDAC4 deacetylates K75 and is regulated by miR29a. O-GlcNAcylation on S246, in addition to K75 acetylation, also regulates Sox2 stability. These findings provide insights into the regulation of Sox2 through multiple post-translational modifications and pathways in CRC. [ABSTRACT FROM AUTHOR]

Published

2024

10. Gα i 2 Protein Inhibition Blocks Chemotherapy- and Anti-Androgen-Induced Prostate Cancer Cell Migration.

Author

Caggia, Silvia, Johnston, Alexis, Walunj, Dipak T., Moore, Aanya R., Peer, Benjamin H., Everett, Ravyn W., Oyelere, Adegboyega K., and Khan, Shafiq A.

Subjects

*THERAPEUTIC use of antineoplastic agents, *ANTIANDROGENS, *CANCER chemotherapy, *METASTASIS, *ANTINEOPLASTIC agents, *CELL motility, *RESEARCH funding, *DOCETAXEL, *MEMBRANE proteins, *CELL lines, *MOLECULAR structure, *HISTONE deacetylase, *CARRIER proteins, *PROSTATE tumors, *CHEMICAL inhibitors

Abstract

Simple Summary: Chemotherapy is the first line of treatment for malignant tumors. However, recent discoveries have shown that a relapse and the formation of metastatic disease could be facilitated by these treatments. In this study, we show how several chemotherapeutic drugs induced prostate cancer cells migration. Additionally we propose that combination therapy with newly synthesized inhibitors could block the chemotherapy-driven metastatic behavior of prostate cancer cells. We have previously shown that heterotrimeric G-protein subunit alphai2 (Gαi2) is essential for cell migration and invasion in prostate, ovarian and breast cancer cells, and novel small molecule inhibitors targeting Gαi2 block its effects on migratory and invasive behavior. In this study, we have identified potent, metabolically stable, second generation Gαi2 inhibitors which inhibit cell migration in prostate cancer cells. Recent studies have shown that chemotherapy can induce the cancer cells to migrate to distant sites to form metastases. In the present study, we determined the effects of taxanes (docetaxel), anti-androgens (enzalutamide and bicalutamide) and histone deacetylase (HDAC) inhibitors (SAHA and SBI-I-19) on cell migration in prostate cancer cells. All treatments induced cell migration, and simultaneous treatments with new Gαi2 inhibitors blocked their effects on cell migration. We concluded that a combination treatment of Gαi2 inhibitors and chemotherapy could blunt the capability of cancer cells to migrate and form metastases. [ABSTRACT FROM AUTHOR]

Published

2024

11. Evaluation of the Histone Deacetylase 2 (HDAC-2) Expression in Human Breast Cancer.

Author

Damaskos, Christos, Psilopatis, Iason, Garmpi, Anna, Dimitroulis, Dimitrios, Nikolettos, Konstantinos, Vrettou, Kleio, Sarantis, Panagiotis, Koustas, Evangelos, Kouraklis, Gregory, Antoniou, Efstathios A., Karamouzis, Michail V., Nikolettos, Nikolaos, Tsikouras, Panagiotis, Marinos, Georgios, Kontomanolis, Emmanouil, Kontzoglou, Konstantinos, and Garmpis, Nikolaos

Subjects

*BREAST cancer prognosis, *STAINS & staining (Microscopy), *CANCER invasiveness, *IMMUNOHISTOCHEMISTRY, *GENE expression, *DESCRIPTIVE statistics, *SYMPTOMS, *HISTONE deacetylase, *PROGRESSION-free survival, *BREAST tumors

Abstract

Simple Summary: Histone deacetylase inhibitors (HDACIs) represent a relatively new drug class with potent regulatory effects on the epigenetics in cancer, ranging from apoptosis induction and cancer cell death to cell cycle arrest. In spite of the fact that HDACIs have, so far, received approval for the treatment of mainly hematologic malignancies, there are numerous preclinical, as well as, clinical trials in the setting of (triple negative) breast cancer with very promising results. In this study, we aimed at assessing the clinical importance of HDAC-2 in triple negative breast cancer. A total of 138 breast cancer specimens were examined immunohistochemically. This current study demonstrated that increased HDAC-2 expression correlates with significant clinicopathological parameters of triple negative breast cancer patients, such as survival, recurrence, and disease stage. Background/Aim: Triple negative breast cancer belongs to the most aggressive breast cancer forms. Histone deacetylases (HDACs) constitute a class of enzymes that exhibit a significant role in breast cancer genesis and progression. In this study, we aimed at assessing the clinical importance of HDAC-2 in triple negative breast cancer. Materials and Methods: A total of 138 breast cancer specimens were examined on an immunohistochemical basis. A statistical analysis was performed in order to examine the association between HDAC-2 and the survival and clinicopathological features of the patients. Results: Increased HDAC-2 expression was observed in every fourth case of triple negative breast cancer with positive HDAC-2 staining, whereas only 12 out of 98 non-triple negative breast cancer samples showed high HDAC-2 expression. HDAC-2 overexpression correlated with prolonged overall survival (OS) and disease-free survival (DFS) in triple negative breast cancer. Conclusions: High HDAC-2 levels in triple negative breast cancer seem to positively influence patient survival, disease stage and recurrence. [ABSTRACT FROM AUTHOR]

Published

2024

12. First-in-Human Dose-Escalation Study of the Novel Oral Depsipeptide Class I-Targeting HDAC Inhibitor Bocodepsin (OKI-179) in Patients with Advanced Solid Tumors.

Author

Schreiber, Anna R., Kagihara, Jodi A., Corr, Bradley R., Davis, S. Lindsey, Lieu, Christopher, Kim, Sunnie S., Jimeno, Antonio, Camidge, D. Ross, Williams, Jud, Heim, Amy M., Martin, Anne, DeMattei, John A., Holay, Nisha, Triplett, Todd A., Eckhardt, S. Gail, Litwiler, Kevin, Winkler, James, Piscopio, Anthony D., and Diamond, Jennifer R.

Subjects

*THERAPEUTIC use of antineoplastic agents, *DRUG dosage, *DRUG tolerance, *CLINICAL trials, *NAUSEA, *TIME, *PROTEIN kinase inhibitors, *TREATMENT duration, *CANCER patients, *DESCRIPTIVE statistics, *RESEARCH funding, *TUMORS, *HISTONE deacetylase, *FATIGUE (Physiology), *THROMBOCYTOPENIA, *DRUG toxicity, *PATIENT safety, *CHEMICAL inhibitors

Abstract

Simple Summary: Histone deacetylase (HDAC) inhibitors are anti-cancer agents that have demonstrated efficacy in hematologic malignancies; however, the utility of available agents is limited, owing to narrow therapeutic indices and suboptimal isoform selectivity. Bocodepsin (OKI-179) is a novel, orally bioavailable, Class I-targeting depsipeptide HDAC inhibitor with promising anti-cancer activity in preclinical solid tumor models. In this first-in-human phase I clinical study, we report the safety and tolerability of OKI-179 administered orally daily with intermittent and continuous dosing schedules. OKI-179 was well tolerated with low rates of high-grade adverse events, supporting the potential for the successful combination of OKI-179 with other targeted anti-cancer agents. OKI-179 is currently being investigated in combination with the MEK inhibitor binimetinib in patients with NRAS-mutated melanoma. (1) Background: Histone deacetylases (HDACs) play a critical role in epigenetic signaling in cancer; however, available HDAC inhibitors have limited therapeutic windows and suboptimal pharmacokinetics (PK). This first-in-human phase I dose escalation study evaluated the safety, PK, pharmacodynamics (PDx), and efficacy of the oral Class I-targeting HDAC inhibitor bocodepsin (OKI-179). (2) Patients and Methods: Patients (n = 34) with advanced solid tumors were treated with OKI-179 orally once daily in three schedules: 4 days on 3 days off (4:3), 5 days on 2 days off (5:2), or continuous in 21-day cycles until disease progression or unacceptable toxicity. Single-patient escalation cohorts followed a standard 3 + 3 design. (3) Results: The mean duration of treatment was 81.2 (range 11–447) days. The most frequent adverse events in all patients were nausea (70.6%), fatigue (47.1%), and thrombocytopenia (41.2%). The maximum tolerated dose (MTD) of OKI-179 was 450 mg with 4:3 and 200 mg with continuous dosing. Dose-limiting toxicities included decreased platelet count and nausea. Prolonged disease control was observed, including two patients with platinum-resistant ovarian cancer. Systemic exposure to the active metabolite exceeded the preclinical efficacy threshold at doses lower than the MTD and was temporally associated with increased histone acetylation in circulating T cells. (4) Conclusions: OKI-179 has a manageable safety profile at the recommended phase 2 dose (RP2D) of 300 mg daily on a 4:3 schedule with prophylactic oral antiemetics. OKI-179 is currently being investigated with the MEK inhibitor binimetinib in patients with NRAS-mutated melanoma in the phase 2 Nautilus trial. [ABSTRACT FROM AUTHOR]

Published

2024

13. ZFP64 Promotes Gallbladder Cancer Progression through Recruiting HDAC1 to Activate NOTCH1 Signaling Pathway.

Author

He, Zhiqiang, Zhong, Yuhan, Hu, Haijie, and Li, Fuyu

Subjects

*DISEASE progression, *IN vitro studies, *GALLBLADDER tumors, *IN vivo studies, *ANIMAL experimentation, *ONE-way analysis of variance, *CANCER invasiveness, *APOPTOSIS, *CELL receptors, *CELL motility, *EPITHELIAL-mesenchymal transition, *CELLULAR signal transduction, *CELL proliferation, *RESEARCH funding, *TRANSCRIPTION factors, *HISTONE deacetylase, *MICE

Abstract

Simple Summary: Gallbladder cancer (GBC) is one of the solid tumors with the worst prognosis, and existing treatments for GBC are not effective. Understanding the disease process of GBC from the perspective of molecular mechanisms is helpful in developing new therapies. In this study, we aimed at exploring a meaningful regulator in GBC. Through a series of in vitro and in vivo assays, we confirmed that zinc finger protein 64 (ZFP64) is a potential promoter and ZFP64-Notch1-HDAC1 is an essential oncogenic axis in GBC progression. Targeting ZFP64 may pave the way for the development of effective therapy for this disease. The lack of meaningful and effective early-stage markers remains the major challenge in the diagnosis of gallbladder cancer (GBC) and a huge barrier to timely treatment. Zinc finger protein 64 (ZFP64), a member of the zinc finger protein family, is considered to be a promising predictor in multiple tumors, but its potential effect in GBC still remains unclear. Here, we identified that ZFP64 was a vital regulatory protein in GBC. We found that ZFP64 expressed higher in GBC gallbladder carcinoma tissues than in normal tissues and was positively correlated with poor prognosis. Furthermore, ZFP64 was responsible for the migration, invasion, proliferation, anti-apoptosis, and epithelial mesenchymal transition (EMT) of GBC cells in vitro and in vivo. Mechanistically, through Co-IP assay, we confirmed that ZFP64 recruits HDAC1 localized to the promoter region of NUMB for deacetylation and therefore inhibits NUMB expression. The downregulation of NUMB enhanced the activation of the Notch1 signaling pathway, which is indispensable for the GBC-promotion effect of ZFP64 on GBC. In conclusion, ZFP64 regulated GBC progression and metastasis through upregulating the Notch1 signaling pathway, and thus ZFP64 is expected to become a new focus for a GBC prognostic marker and targeted therapy. [ABSTRACT FROM AUTHOR]

Published

2023

14. Active Autophagy Is Associated with Favorable Outcome in Patients with Surgically Resected Cholangiocarcinoma.

Author

Bankov, Katrin, Schulze, Falko, Gretser, Steffen, Reis, Henning, Abedin, Nada, Finkelmeier, Fabian, Trojan, Jörg, Zeuzem, Stefan, Schnitzbauer, Andreas A., Walter, Dirk, Wild, Peter J., and Kinzler, Maximilian N.

Subjects

*CONFIDENCE intervals, *CHOLANGIOCARCINOMA, *AUTOPHAGY, *IMMUNOHISTOCHEMISTRY, *MULTIVARIATE analysis, *TREATMENT effectiveness, *DESCRIPTIVE statistics, *RESEARCH funding, *HISTONE deacetylase, *LONGITUDINAL method, *DISEASE complications

Abstract

Simple Summary: Autophagy can exert a dual role in the context of cancer progression. However, data on the prevalence and impact of autophagy in primary cholangiocarcinoma (CCA) tissue are very limited. Active autophagy was present in a minority of the CCA patients (23.3%). We found a significantly impaired overall survival rate for patients with non-active autophagy (32.7 months) compared to CCA patients with active autophagy (68.4 months). In line with this, absence of active autophagy was an independent risk factor for overall survival. Moreover, in patients with active autophagy, pan-acetylation was significantly more prominent compared to those with non-active autophagy. Our data strengthen the role of active autophagy as a prognostically relevant marker and a potential therapeutic target in CCA patients. Data on the impact of autophagy in primary cholangiocarcinoma (CCA) remain scarce. Here, we therefore investigated the role of active autophagy and its impact on survival in CCA patients. All CCA patients who underwent surgical resection with curative intent between 08/2005 and 12/2021 at University Hospital Frankfurt were evaluated. Autophagic key proteins were studied by immunohistochemistry. iCCA processed for gene expression profiling of immune-exhaustion gene sets was used for an autophagy approach in silico. Active autophagy was present in 23.3% of the 172 CCA patients. Kaplan–Meier curves revealed median OS of 68.4 months (95% CI = 46.9–89.9 months) and 32.7 months (95% CI = 23.6–41.8 months) for active and non-active autophagy, respectively (p ≤ 0.001). In multivariate analysis, absence of active autophagy (HR = 2, 95% CI = 1.1–3.5, p = 0.015) was an independent risk factor for OS. Differential-expression profiling revealed significantly upregulated histone deacetylases (HDAC) mRNA in patients showing non-active autophagy. In line with this, pan-acetylated lysine was significantly more prominent in CCA patients with ongoing autophagy (p = 0.005). Our findings strengthen the role of active autophagy as a prognostically relevant marker and a potential therapeutic target. [ABSTRACT FROM AUTHOR]

Published

2023

15. Potential of Synthetic and Natural Compounds as Novel Histone Deacetylase Inhibitors for the Treatment of Hematological Malignancies.

Author

Pal, Dilipkumar, Raj, Khushboo, Nandi, Shyam Sundar, Sinha, Surajit, Mishra, Abhishek, Mondal, Arijit, Lagoa, Ricardo, Burcher, Jack T., and Bishayee, Anupam

Subjects

*GENETIC mutation, *APOPTOSIS, *GENE expression, *HEMATOLOGIC malignancies, *HISTONE deacetylase, *MOLECULAR structure, *TRANSCRIPTION factors, *CELL death, *CHEMICAL inhibitors

Abstract

Simple Summary: Histone deacetylases (HDACs) are epigenetic regulators that influence chromatin structure and gene transcription, but also the function of non-histone targets like chaperones and proteins participating in the DNA damage response. Histone modifications are implicated in cancer and HDAC inhibitors (HDACis) can be useful to treat hematological malignancies, including leukemia, B-cell lymphoma, virus-associated tumors, and multiple myeloma. Several HDACis were approved for clinical use and others are showing promising results, especially as adjuvants to conventional treatments. In addition to synthetic inhibitors, this work discusses the potential of phytocompounds, such as chrysin and oleacein as well as marine-derived agents, such as halenaquinone and xestoquinone, as therapeutic agents against hematological cancers. Histone deacetylases (HDACs) and histone acetyltransferases (HATs) are enzymes that remove or add acetyl groups to lysine residues of histones, respectively. Histone deacetylation causes DNA to more snugly encircle histones and decreases gene expression, whereas acetylation has the opposite effect. Through these small alterations in chemical structure, HATs and HDACs regulate DNA expression. Recent research indicates histone deacetylase inhibitors (HDACis) may be used to treat malignancies, including leukemia, B-cell lymphoma, virus-associated tumors, and multiple myeloma. These data suggest that HDACis may boost the production of immune-related molecules, resulting in the growth of CD8-positive T-cells and the recognition of nonreactive tumor cells by the immune system, thereby diminishing tumor immunity. The argument for employing epigenetic drugs in the treatment of acute myeloid leukemia (AML) patients is supported by evidence that both epigenetic changes and mutations in the epigenetic machinery contribute to AML etiology. Although hypomethylating drugs have been licensed for use in AML, additional epigenetic inhibitors, such as HDACis, are now being tested in humans. Preclinical studies evaluating the efficacy of HDACis against AML have shown the ability of specific agents, such as anobinostat, vorinostat, and tricostatin A, to induce growth arrest, apoptosis, autophagy and cell death. However, these inhibitors do not seem to be successful as monotherapies, but instead achieve results when used in conjunction with other medications. In this article, we discuss the mounting evidence that HDACis promote extensive histone acetylation, as well as substantial increases in reactive oxygen species and DNA damage in hematological malignant cells. We also evaluate the potential of various natural product-based HDACis as therapeutic agents to combat hematological malignancies. [ABSTRACT FROM AUTHOR]

Published

2023

16. Targeting and Sensitization of Breast Cancer Cells to Killing with a Novel Interleukin-13 Receptor α2-Specific Hybrid Cytolytic Peptide.

Author

Jannoo, Riaz, Walker, William, and Kanamarlapudi, Venkateswarlu

Subjects

*THERAPEUTIC use of antineoplastic agents, *METHYLTRANSFERASES, *CELL receptors, *RESEARCH funding, *CELL lines, *HISTONE deacetylase, *BREAST tumors, *PEPTIDES, *NECROSIS, *EPIGENOMICS

Abstract

Simple Summary: Breast cancer is the most commonly diagnosed cancer and the second leading cause of cancer deaths among women globally. Due to its biological heterogeneity, breast cancer treatment and prognosis are highly variable among patients. In particular, the triple-negative subtype (TNBC) has a poorer prognosis with a lack of targeted therapies. With this in mind, we sought to develop a potentially more effective, novel receptor-targeting strategy. This study describes measuring the expression of the putative biomarker, interleukin-13 receptor (IL-13R)α2, in breast cancer (including TNBC) and its therapeutic targeting using a novel hybrid cytolytic peptide (Pep-1-Phor21) approach. We have shown in this manuscript that IL-13Rα2 exhibits potential as a therapeutic target, particularly for TNBC types of breast cancer. Importantly, drug-induced breast cancer cell lysis could be enhanced by treatment with epigenetically active anti-cancer compounds, suggesting that a combination adjuvant therapy of Pep-1-Phor21 with such compounds may be a particularly productive strategy for TNBC. Highly metastatic breast cancers, such as triple-negative subtypes (TNBC), require the most effective treatments. Since interleukin-13 receptor (IL-13R)α2 is reportedly over-expressed in some cancers, we investigated here its expression and the feasibility of therapeutically targeting this receptor in breast cancer using a novel hybrid cytolytic peptide (Pep-1-Phor21) consisting of IL-13Rα2-binding (Pep-1) and cytolytic (Phor21) domains. This study demonstrates that particularly TNBC tissues and cells display the prominent expression of IL-13Rα2. Furthermore, Pep-1-Phor21 induced the rapid necrosis of tumor cells expressing cell-surface IL-13Rα2. Notably, IL-13Rα2 expression was found to be epigenetically regulated in breast cancer cells in that the inhibition of histone deacetylase (HDAC) or DNA methyltransferase (DNMT) upregulated IL-13Rα2 expression, thereby sensitizing them to Pep-1-Phor21. IL-13Rα2-negative non-malignant cells were refractory to these epigenetic effects. Consistent with its cytolytic activity, Pep-1-Phor21 readily destroyed IL-13Rα2-expressing breast cancer spheroids with HDAC or DNMT inhibition, further enhancing cytolytic activity. Therefore, the Pep-1-Phor21-mediated targeting of IL-13Rα2 is a potentially novel therapeutic strategy for TNBC. Given that tumor cells can be selectively sensitized to Pep-1-Phor21 via the epigenetic up-regulation of IL-13Rα2, a combined adjuvant approach involving Pep-1-Phor21 and epigenetic inhibitors may be an effective strategy. [ABSTRACT FROM AUTHOR]

Published

2023

17. The Emerging Role of Histone Deacetylase Inhibitors in Cervical Cancer Therapy.

Author

Psilopatis, Iason, Garmpis, Nikolaos, Garmpi, Anna, Vrettou, Kleio, Sarantis, Panagiotis, Koustas, Evangelos, Antoniou, Efstathios A., Dimitroulis, Dimitrios, Kouraklis, Gregory, Karamouzis, Michail V., Marinos, Georgios, Kontzoglou, Konstantinos, Nonni, Afroditi, Nikolettos, Konstantinos, Fleckenstein, Florian N., Zoumpouli, Christina, and Damaskos, Christos

Subjects

*IN vitro studies, *SYSTEMATIC reviews, *ANTINEOPLASTIC agents, *APOPTOSIS, *GENE expression, *CELL cycle, *MESSENGER RNA, *HISTONE deacetylase, *MEDLINE, *PHARMACODYNAMICS, *CHEMICAL inhibitors, CERVIX uteri tumors

Abstract

Simple Summary: Histone deacetylase inhibitors (HDACIs) are a relatively new drug class with important effects on the epigenetic regulation in cancer, inducing cancer cell death, apoptosis induction, and cell cycle arrest. Even though HDACIs have, to date, received approval for mainly hematologic malignancies, there are plentiful studies in cervical cancer setting with encouraging results. The present review summarizes all studies with HDACIs in cervical cancer from the emerging data in labor research to the possible applicability in clinical practice. Cervical carcinoma is one of the most common cancers among women globally. Histone deacetylase inhibitors (HDACIs) constitute anticancer drugs that, by increasing the histone acetylation level in various cell types, induce differentiation, cell cycle arrest, and apoptosis. The aim of the current review is to study the role of HDACIs in the treatment of cervical cancer. A literature review was conducted using the MEDLINE and LIVIVO databases with a view to identifying relevant studies. By employing the search terms "histone deacetylase" and "cervical cancer", we managed to identify 95 studies published between 2001 and 2023. The present work embodies the most up-to-date, comprehensive review of the literature centering on the particular role of HDACIs as treatment agents for cervical cancer. Both well-established and novel HDACIs seem to represent modern, efficacious anticancer drugs, which, alone or in combination with other treatments, may successfully inhibit cervical cancer cell growth, induce cell cycle arrest, and provoke apoptosis. In summary, histone deacetylases seem to represent promising future treatment targets in cervical cancer. [ABSTRACT FROM AUTHOR]

Published

2023

18. Targeting HDAC2-Mediated Immune Regulation to Overcome Therapeutic Resistance in Mutant Colorectal Cancer.

Author

Conte, Mariarosaria, Di Mauro, Annabella, Capasso, Lucia, Montella, Liliana, De Simone, Mariacarla, Nebbioso, Angela, and Altucci, Lucia

Subjects

*TISSUE arrays, *GENETIC mutation, *IMMUNOHISTOCHEMISTRY, *IMMUNE system, *MICROARRAY technology, *APOPTOSIS, *COLORECTAL cancer, *GENE expression, *RESEARCH funding, *GENE expression profiling, *CELL proliferation, *HISTONE deacetylase, *TUMOR markers, *CELL lines, *DRUG resistance in cancer cells, *CHEMICAL inhibitors

Abstract

Simple Summary: Epigenetic processes contribute to the regulation of the immune system by activating multiple transcriptional changes, which in turn, are the product of immune cell reprogramming. Given that the deregulation of these mechanisms promotes cancer progression by altering the balance of genes controlling cell proliferation and death, the objective of this study was to identify a genetic/epigenetic/immunological colorectal cancer signature through a preliminary in silico analysis aimed at identifying the pathogenic causes of colorectal cancer associated with expression levels of histone deacetylase 2 (HDAC2) and two immune system regulators, class II major histocompatibility complex transactivator (CIITA) and beta-2 microglobulin (B2M), in a cohort of patients harboring a common dysregulation of these genes. We next extended the study by investigating a tissue microarray cohort of colorectal cancer patients from a diagnostic/prognostic perspective. A large body of clinical and experimental evidence indicates that colorectal cancer is one of the most common multifactorial diseases. Although some useful prognostic biomarkers for clinical therapy have already been identified, it is still difficult to characterize a therapeutic signature that is able to define the most appropriate treatment. Gene expression levels of the epigenetic regulator histone deacetylase 2 (HDAC2) are deregulated in colorectal cancer, and this deregulation is tightly associated with immune dysfunction. By interrogating bioinformatic databases, we identified patients who presented simultaneous alterations in HDAC2, class II major histocompatibility complex transactivator (CIITA), and beta-2 microglobulin (B2M) genes based on mutation levels, structural variants, and RNA expression levels. We found that B2M plays an important role in these alterations and that mutations in this gene are potentially oncogenic. The dysregulated mRNA expression levels of HDAC2 were reported in about 5% of the profiled patients, while other specific alterations were described for CIITA. By analyzing immune infiltrates, we then identified correlations among these three genes in colorectal cancer patients and differential infiltration levels of genetic variants, suggesting that HDAC2 may have an indirect immune-related role in specific subgroups of immune infiltrates. Using this approach to carry out extensive immunological signature studies could provide further clinical information that is relevant to more resistant forms of colorectal cancer. [ABSTRACT FROM AUTHOR]

Published

2023

19. New Approaches to Targeting Epigenetic Regulation in Bladder Cancer.

Author

Thompson, Daryl, Lawrentschuk, Nathan, and Bolton, Damien

Subjects

*COMBINATION drug therapy, *GENETIC mutation, *METASTASIS, *TRANSFERASES, *HISTONE deacetylase, *EPIGENOMICS, BLADDER tumors

Abstract

Simple Summary: Epigenetic changes occur in parts of the genome other than in nucleotides. They are considered reversible and are therefore important targets for cancer therapy. Epigenetic changes have been observed in urological cancers, including urothelial carcinoma, and in recent years have been a topic of investigation for the treatment of metastatic bladder cancer that has failed traditional therapy. We performed a review of the current literature to assess the evidence and role for targeted epigenetic therapy in bladder cancer. While we found 25 clinical trials investigating this topic, there have been no phase 3 human clinical trials to date. This is an emerging topic in urology, and future directions involve further research into bladder cancer-specific epigenetic changes, as well as the development of novel agents to target these mutations. Epigenetics is a growing field and in bladder cancer, it is of particular interest in advanced or metastatic disease. As opposed to genetic mutations in which the nucleotide sequence itself is altered, epigenetic alterations refer to changes to the genome that do not involve nucleotides. This is of great interest in cancer research because epigenetic alterations are reversible, making them a promising target for pharmacological agents. While chemoimmunotherapy is the mainstay for metastatic disease, there are few alternatives for patients who have progressed on first- or second-line treatment. By targeting reversible epigenetic alterations, novel epigenetic therapies are important potential treatment options for these patients. A search of clinical registries was performed in order to identify and collate epigenetic therapies currently in human trials. A literature search was also performed to identify therapies that are currently in preclinical stages, whether this be in vivo or in vitro models. Twenty-five clinical trials were identified that investigated the use of epigenetic inhibitors in patients with bladder cancer, often in combination with another agent, such as platinum-based chemotherapy or pembrolizumab. The main classes of epigenetic inhibitors studied include DNA-methyltransferase (DNMT) inhibitors, histone deacetylase (HDAC) inhibitors, and histone methyltransferase (HMT) inhibitors. At present, no phase 3 clinical trials have been registered. Few trials have published results, though DNMT inhibitors have shown the most promise thus far. Many patients with advanced or metastatic bladder cancer have limited treatment options, particularly when first- or second-line chemoimmunotherapy fails. Epigenetic alterations, which are common in bladder cancer, are potential targets for drug therapies, and these epigenetic agents are already in use for many cancers. While they have shown promise in pre-clinical trials for bladder cancer, more research is needed to assess their benefit in clinical settings. [ABSTRACT FROM AUTHOR]

Published

2023

20. Antiandrogen-Equipped Histone Deacetylase Inhibitors Selectively Inhibit Androgen Receptor (AR) and AR-Splice Variant (AR-SV) in Castration-Resistant Prostate Cancer (CRPC).

Author

Chandrasekaran, Balaji, Tapadar, Subhasish, Wu, Bocheng, Saran, Uttara, Tyagi, Ashish, Johnston, Alexis, Gaul, David A., Oyelere, Adegboyega K., and Damodaran, Chendil

Subjects

*IN vitro studies, *DRUG efficacy, *ANTIANDROGENS, *IN vivo studies, *ANIMAL experimentation, *IMMUNOHISTOCHEMISTRY, *CASTRATION-resistant prostate cancer, *GENE expression, *CELLULAR signal transduction, *CELL proliferation, *RESEARCH funding, *HISTONE deacetylase, *ANDROGEN receptors, *MICE, *CHEMICAL inhibitors

Abstract

Simple Summary: SBI-46, an antiandrogen-equipped histone deacetylase inhibitor, is the lead compound developed for targeting castration-resistant prostate cancer (CRPC). We determined the anticancer effect of SBI-46 on in vitro and in vivo models of CRPC. In our results, SBI-46 downregulates AR and AR-splice variant (SV) expression and its downstream target genes in CRPC cells. Additionally, SBI-46 inhibits AR expression and nuclear localization in the presence of DHT. We further demonstrated that SBI-46 induces apoptosis by activating the pro-apoptotic genes Bax, cleaved PARP, and cleaved caspase-9, as well as downregulating the expression of the antiapoptotic genes Bcl2 and BCl-xL. Additionally, the oral administration of SBI-46 abrogates the growth of C4-2B and 22Rv1 CRPC xenograft tumors that express AR or both AR and AR-SV. Finally, our results demonstrate that SBI-46 exerts an anticancer effect by inhibiting AR and AR-SV in preclinical models of CRPC. Background: Epigenetic modification influences androgen receptor (AR) activation, often resulting in prostate cancer (PCa) development and progression. Silencing histone-modifying enzymes (histone deacetylases-HDACs) either genetically or pharmacologically suppresses PCa proliferation in preclinical models of PCa; however, results from clinical studies were not encouraging. Similarly, PCa patients eventually become resistant to androgen ablation therapy (ADT). Our goal is to develop dual-acting small molecules comprising antiandrogen and HDAC-inhibiting moieties that may overcome the resistance of ADT and effectively suppress the growth of castration-resistant prostate cancer (CRPC). Methods: Several rationally designed antiandrogen-equipped HDAC inhibitors (HDACi) were synthesized, and their efficacy on CRPC growth was examined both in vitro and in vivo. Results: While screening our newly developed small molecules, we observed that SBI-46 significantly inhibited the proliferation of AR+ CRPC cells but not AR- CRPC and normal immortalized prostate epithelial cells (RWPE1) or normal kidney cells (HEK-293 and VERO). Molecular analysis confirmed that SBI-46 downregulated the expressions of both AR+ and AR-splice variants (AR-SVs) in CRPC cells. Further studies revealed the downregulation of AR downstream (PSA) events in CRPC cells. The oral administration of SBI-46 abrogated the growth of C4-2B and 22Rv1 CRPC xenograft tumors that express AR or both AR and AR-SV in xenotransplanted nude mice models. Further, immunohistochemical analysis confirmed that SBI-46 inhibits AR signaling in xenografted tumor tissues. Conclusion: These results demonstrate that SBI-46 is a potent agent that inhibits preclinical models of CRPC by downregulating the expressions of both AR and AR-SV. Furthermore, these results suggest that SBI-46 may be a potent compound for treating CRPC. [ABSTRACT FROM AUTHOR]

Published

2023

21. Implications of Transglutaminase-Mediated Protein Serotonylation in the Epigenetic Landscape, Small Cell Lung Cancer, and Beyond.

Author

Lin, Jason and Wu, Shang-Chuen

Subjects

*LUNG cancer prevention, *THERAPEUTIC use of antineoplastic agents, *POLYSACCHARIDES, *TRANSGLUTAMINASES, *GENE expression, *HISTONES, *HISTONE deacetylase, *MOLECULAR structure, *EPIGENOMICS, *ENZYME inhibitors

Abstract

Simple Summary: From the landmark report of protein serotonylation on small GTPases in 2003 to the most recent discovery of serotonin-modified histone H3 leading to epigenetic changes, over the course of the past 20 years, there is still a cloud of mystery surrounding this rare post-translational modification, other than the fact that tissue transglutaminase, perhaps most famously known for its role in celiac disease, is the enzyme responsible for catalyzing this transamidation reaction. This review seeks to interpret the role of protein serotonylation in transcriptional regulation through some of the mechanistic and intertwining details of the modification, its potential modulation of the epigenetic landscape, as well as potential implications in lung and other types of cancer. In the case of small-cell lung carcinoma, the highly metastatic nature of the disease and the propensity for several chromatin modifiers to harbor mutations suggest that epigenetic manipulation may also be a promising route for oncotherapy, but histone deacetylase inhibitors on their own do not appear to be particularly effective, suggesting that there may be other regulatory parameters that dictate the effectiveness of vorinostat's reversal of histone deacetylation. Recent discoveries that serotonylation of histone H3 alters the permissibility of gene expression have led to renewed attention to this rare modification, as facilitated by transglutaminase 2, and at the same time introduce new questions about whether this modification belongs to a part of the concerted cohort of regulator events for modulating the epigenetic landscape. This review explores the mechanistic details behind protein serotonylation and its possible connections to the epigenome via histone modifications and glycan interactions and attempts to elucidate the role of transglutaminase 2, such that optimizations to existing histone deacetylase inhibitor designs or combination therapies may be devised for lung and other types of cancer. [ABSTRACT FROM AUTHOR]

Published

2023

22. SMAC Mimetics Synergistically Cooperate with HDAC Inhibitors Enhancing TNF-α Autocrine Signaling.

Author

Shibuya, Yusuke, Kudo, Kei, Zeligs, Kristen P., Anderson, David, Hernandez, Lidia, Ning, Franklin, Cole, Christopher B., Fergusson, Maria, Kedei, Noemi, Lyons, John, Taylor, Jason, Korrapati, Soumya, and Annunziata, Christina M.

Subjects

*IN vitro studies, *OVARIAN tumors, *INDOLE compounds, *IN vivo studies, *OLIGOPEPTIDES, *CELL physiology, *CANCER relapse, *APOPTOSIS, *SIGNAL peptides, *EARLY detection of cancer, *NF-kappa B, *CELLULAR signal transduction, *GENE expression, *DRUG synergism, *TUMOR necrosis factors, *RESEARCH funding, *HISTONE deacetylase, *CASPASES, *CHEMICAL inhibitors

Abstract

Simple Summary: The combination of a SMAC mimetic with an HDAC inhibitor is a novel and promising strategy for cancer treatment. The HDAC inhibitor mechanistically synergizes with SMAC mimetics by stimulating autocrine TNF-α production. The overexpression of inhibitor of apoptosis (IAP) proteins is strongly related to poor survival of women with ovarian cancer. Recurrent ovarian cancers resist apoptosis due to the dysregulation of IAP proteins. Mechanistically, Second Mitochondrial Activator of Caspases (SMAC) mimetics suppress the functions of IAP proteins to restore apoptotic pathways resulting in tumor death. We previously conducted a phase 2 clinical trial of the single-agent SMAC mimetic birinapant and observed minimal drug response in women with recurrent ovarian cancer despite demonstrating on-target activity. Accordingly, we performed a high-throughput screening matrix to identify synergistic drug combinations with birinapant. SMAC mimetics in combination with an HDAC inhibitor showed remarkable synergy and was, therefore, selected for further evaluation. We show here that this synergy observed both in vitro and in vivo results from multiple convergent pathways to include increased caspase activation, HDAC inhibitor-mediated TNF-α upregulation, and alternative NF-kB signaling. These findings provide a rationale for the integration of SMAC mimetics and HDAC inhibitors in clinical trials for recurrent ovarian cancer where treatment options are still limited. [ABSTRACT FROM AUTHOR]

Published

2023

23. The Class IIA Histone Deacetylase (HDAC) Inhibitor TMP269 Downregulates Ribosomal Proteins and Has Anti-Proliferative and Pro-Apoptotic Effects on AML Cells.

Author

Urwanisch, Laura, Unger, Michael Stefan, Sieberer, Helene, Dang, Hieu-Hoa, Neuper, Theresa, Regl, Christof, Vetter, Julia, Schaller, Susanne, Winkler, Stephan M., Kerschbamer, Emanuela, Weichenberger, Christian X., Krenn, Peter W., Luciano, Michela, Pleyer, Lisa, Greil, Richard, Huber, Christian G., Aberger, Fritz, and Horejs-Hoeck, Jutta

Subjects

*FLOW cytometry, *IN vitro studies, *ANTINEOPLASTIC agents, *APOPTOSIS, *GENE expression, *COMPARATIVE studies, *PROTEOMICS, *BIOINFORMATICS, *AZACITIDINE, *RESEARCH funding, *CELL proliferation, *HISTONE deacetylase, *CELL lines, *RIBOSOMAL proteins, *CELL death, *SULFONAMIDES, *PHENOTYPES, *PHARMACODYNAMICS, *CHEMICAL inhibitors

Abstract

Simple Summary: Epigenetic alterations strongly contribute to the development of various types of cancer, including blood cancers such as acute myeloid leukemia (AML). Unlike genetic mutations, epigenetic changes in cancer are reversible. Therefore, targeted modification of epigenetic regulators, such as histone deacetylases (HDACs), is under intense investigation. Here, we analyzed gene expression for all four classes of HDACs in AML patients compared to healthy controls. We observed significant overexpression of various HDACs, including the relatively unexplored HDAC class IIA members. To investigate the cellular consequences of HDAC inhibition, we treated AML cell lines with the class IIA HDAC inhibitor TMP269 and observed significant effects on the cellular proteome and the growth of AML cells. We further demonstrate that the combination of TMP269 and venetoclax results in enhanced cell apoptosis. Our work provides new data for the HDAC inhibitor TMP269 and suggests that TMP269 might be an alternative compound for polytherapy in AML. Acute myeloid leukemia (AML) is a hematopoietic malignancy characterized by altered myeloid progenitor cell proliferation and differentiation. As in many other cancers, epigenetic transcriptional repressors such as histone deacetylases (HDACs) are dysregulated in AML. Here, we investigated (1) HDAC gene expression in AML patients and in different AML cell lines and (2) the effect of treating AML cells with the specific class IIA HDAC inhibitor TMP269, by applying proteomic and comparative bioinformatic analyses. We also analyzed cell proliferation, apoptosis, and the cell-killing capacities of TMP269 in combination with venetoclax compared to azacitidine plus venetoclax, by flow cytometry. Our results demonstrate significantly overexpressed class I and class II HDAC genes in AML patients, a phenotype which is conserved in AML cell lines. In AML MOLM-13 cells, TMP269 treatment downregulated a set of ribosomal proteins which are overexpressed in AML patients at the transcriptional level. TMP269 showed anti-proliferative effects and induced additive apoptotic effects in combination with venetoclax. We conclude that TMP269 exerts anti-leukemic activity when combined with venetoclax and has potential as a therapeutic drug in AML. [ABSTRACT FROM AUTHOR]

Published

2023

24. TRIM10 Is Downregulated in Acute Myeloid Leukemia and Plays a Tumor Suppressive Role via Regulating NF-κB Pathway.

Author

Li, Lin, Li, Qi, Zou, Zhengrong, Huang, Zoufang, and Chen, Yijian

Subjects

*PROTEIN metabolism, *IN vitro studies, *IN vivo studies, *DNA, *WESTERN immunoblotting, *ANIMAL experimentation, *METHYLTRANSFERASES, *ANTINEOPLASTIC agents, *NF-kappa B, *APOPTOSIS, *CELLULAR signal transduction, *CELL proliferation, *RESEARCH funding, *CELL lines, *POLYMERASE chain reaction, *HISTONE deacetylase, *EPIGENOMICS, *MICE

Abstract

Simple Summary: Acute myeloid leukemia (AML) remains an incurable hematological malignancy and patients have short survival due to AML relapse. In this study, we identified that TRIM10 was most downregulated in AML cell lines and AML patients. We further found that TRIM10 inhibits the growth of AML cells in vitro and in vivo. More importantly, our results indicated that TRIM10 plays a tumor suppressor role in AML cells by affecting the NF-κB signal pathway, which can be targeted with epigenetic therapy. Background: Accumulating evidence suggests that members of the tripartite motif (TRIMs) family play a crucial role in the development and progression of hematological malignancy. Here, we explored the expression and potential role of TRIM10 in acute myeloid leukemia (AML). Methods: The expression levels of TRIM10 were investigated in AML patients and cell lines by RNA-seq, qRT-PCR and Western blotting analysis. Lentiviral infection was used to regulate the level of TRIM10 in AML cells. The effects of TRIM10 on apoptosis, drug sensitivity and proliferation of AML cells were evaluated by flow cytometry and cell-counting kit-8 (CCK-8) assay, as well as being assessed in a murine model. Results: TRIM10 mRNA and protein expression was reduced in primary AML samples and AML cell lines in comparison to the normal controls and a human normal hematopoietic cell line, respectively. Moreover, overexpression of TRIM10 in HL60 and K562 cells inhibited AML cell proliferation and induced cell apoptosis. The nude mice study further confirmed that overexpression of TRIM10 blocked tumor growth and inhibited cell proliferation. In contrast, knockdown of TRIM10 in AML cells showed contrary results. Subsequent mechanistic studies demonstrated that knockdown of TRIM10 enhanced the expression of nuclear protein P65, which implied the activation of the NF-κB signal pathway. Consistently, overexpression of TRIM10 in AML cells showed a contrary result. These data indicated that inactivation of the NF-κB pathway is involved in TRIM10-mediated regulation in AML. TRIM10 expression can be de-repressed by a combination that targets both DNA methyltransferase and histone deacetylase. Conclusions: Our results strongly suggested that TRIM10 plays a tumor suppressive role in AML development associated with the NF-κB signal pathway and may be a potential target of epigenetic therapy against leukemia. [ABSTRACT FROM AUTHOR]

Published

2023

25. Cell-of-Origin Targeted Drug Repurposing for Triple-Negative and Inflammatory Breast Carcinoma with HDAC and HSP90 Inhibitors Combined with Niclosamide.

Author

Bhattacharya, Udayan, Kamran, Mohammad, Manai, Maroua, Cristofanilli, Massimo, and Ince, Tan A.

Subjects

*DRUG repositioning, *EVALUATION of medical care, *HEAT shock proteins, *RESEARCH funding, *MESSENGER RNA, *HISTONE deacetylase, *CELL lines, *BREAST tumors, *AMIDES, *CHEMICAL inhibitors

Abstract

Simple Summary: The human body is composed of hundreds of different normal cell types. Some of the important and unique features of these normal cell types are inherited by the cancer cells that arise from them. Indeed, the activities of the tumor gene mutations are constrained by this normal cell inheritance. For example, we previously found that the same oncogenes produce highly malignant tumors in some cell types but not in others. In this study, we demonstrate that this cell-of-origin difference can be used to develop cell-targeted therapies, a novel concept that differs from gene-targeted therapies. This cell-based approach guided us to a surprising discovery that a drug approved for treating tapeworm infestation in combination with an antibiotic derivative can significantly enhance the killing of breast cancer cells. Since these drugs are already approved for clinical use, it may be possible to repurpose them to treat breast cancer. We recently identified a cell-of-origin-specific mRNA signature associated with metastasis and poor outcome in triple-negative carcinoma (TNBC). This TNBC cell-of-origin signature is associated with the over-expression of histone deacetylases and zinc finger protein HDAC1, HDAC7, and ZNF92, respectively. Based on this signature, we discovered that the combination of three drugs (an HDAC inhibitor, an anti-helminthic Niclosamide, and an antibiotic Tanespimycin that inhibits HSP90) synergistically reduces the proliferation of the twelve tested TNBC cell lines. Additionally, we discovered that four out of five inflammatory breast carcinoma cell lines are sensitive to this combination. Significantly, the concentration of the drugs that are used in these experiments are within or below clinically achievable dose, and the synergistic activity only emerged when all three drugs were combined. Our results suggest that HDAC and HSP90 inhibitors combined with the tapeworm drug Niclosamide can achieve remarkably synergistic inhibition of TNBC and IBC. Since Niclosamide, HDAC, and HSP90 inhibitors were approved for clinical use for other cancer types, it may be possible to repurpose their combination for TNBC and IBC. [ABSTRACT FROM AUTHOR]

Published

2023

26. Dual LSD1 and HDAC6 Inhibition Induces Doxorubicin Sensitivity in Acute Myeloid Leukemia Cells.

Author

Bulut, Ipek, Lee, Adam, Cevatemre, Buse, Ruzic, Dusan, Belle, Roman, Kawamura, Akane, Gul, Sheraz, Nikolic, Katarina, Ganesan, A., and Acilan, Ceyda

Subjects

*LSD (Drug), *COMBINATION drug therapy, *DOXORUBICIN, *APOPTOSIS, *HYDROLASES, *CELLULAR signal transduction, *CELL proliferation, *GENE expression profiling, *HISTONE deacetylase, *MOLECULAR structure, *ENZYME inhibitors, *PHARMACODYNAMICS

Abstract

Simple Summary: GSK2879552 is a LSD1 inhibitor in clinical development. By structural modification, we obtained an analogue that is a potent and selective dual inhibitor of HDAC6 and LSD1 (IC50 110 and 540 nM, respectively). The dual targeting agent was superior to GSK2879552 in the growth inhibition of two acute myeloid leukemia (AML) cell lines. In combination experiments, the dual inhibitor primed AML cells to apoptosis with a sublethal concentration of doxorubicin. Our data suggest that doxorubicin toxicity can be reduced by parallel inhibition of HDAC6 and LSD1. Defects in epigenetic pathways are key drivers of oncogenic cell proliferation. We developed a LSD1/HDAC6 multitargeting inhibitor (iDual), a hydroxamic acid analogue of the clinical candidate LSD1 inhibitor GSK2879552. iDual inhibits both targets with IC50 values of 540, 110, and 290 nM, respectively, against LSD1, HDAC6, and HDAC8. We compared its activity to structurally similar control probes that act by HDAC or LSD1 inhibition alone, as well as an inactive null compound. iDual inhibited the growth of leukemia cell lines at a higher level than GSK2879552 with micromolar IC50 values. Dual engagement with LSD1 and HDAC6 was supported by dose dependent increases in substrate levels, biomarkers, and cellular thermal shift assay. Both histone methylation and acetylation of tubulin were increased, while acetylated histone levels were only mildly affected, indicating selectivity for HDAC6. Downstream gene expression (CD11b, CD86, p21) was also elevated in response to iDual treatment. Remarkably, iDual synergized with doxorubicin, triggering significant levels of apoptosis with a sublethal concentration of the drug. While mechanistic studies did not reveal changes in DNA repair or drug efflux pathways, the expression of AGPAT9, ALOX5, BTG1, HIPK2, IFI44L, and LRP1, previously implicated in doxorubicin sensitivity, was significantly elevated. [ABSTRACT FROM AUTHOR]

Published

2022

27. Histone Deacetylase Functions in Gastric Cancer: Therapeutic Target?

Author

Badie, Amandine, Gaiddon, Christian, and Mellitzer, Georg

Subjects

*THERAPEUTIC use of antineoplastic agents, *STOMACH tumors, *DRUG approval, *EARLY detection of cancer, *HISTONE deacetylase, *TUMOR markers, *CHEMICAL inhibitors

Abstract

Simple Summary: Our knowledge about the identity of many cancers has increased greatly during the last years and progress in their early identification as well as treatment options led to a net increase in the survival of many cancer patients. Unfortunately, gastric cancer does not belong to these cancers as it is still very badly treated and the chances to survive it are very low, less than 25%. This is mainly due to the fact that currently there are no possibilities to detect it at early stages and that tumors of gastric cancer patients seem all to be more or less different. In this respect, our knowledge about the differences between the gastric cancer from one patient to another is very limited. However, one family of proteins called "Histone Deacetylases" or HDACs, in contrast, seem to be present or their function altered in gastric cancers. This review summarizes our current knowledge about their role in gastric cancer development and their potential as an early detection marker and target to develop new treatment options. Gastric cancer (GC) is one of the most aggressive cancers. Therapeutic treatments are based on surgery combined with chemotherapy using a combination of platinum-based agents. However, at metastatic stages of the disease, survival is extremely low due to late diagnosis and resistance mechanisms to chemotherapies. The development of new classifications has not yet identified new prognostic markers for clinical use. The studies of epigenetic processes highlighted the implication of histone acetylation status, regulated by histone acetyltransferases (HATs) and by histone deacetylases (HDACs), in cancer development. In this way, inhibitors of HDACs (HDACis) have been developed and some of them have already been clinically approved to treat T-cell lymphoma and multiple myeloma. In this review, we summarize the regulations and functions of eighteen HDACs in GC, describing their known targets, involved cellular processes, associated clinicopathological features, and impact on survival of patients. Additionally, we resume the in vitro, pre-clinical, and clinical trials of four HDACis approved by Food and Drug Administration (FDA) in cancers in the context of GC. [ABSTRACT FROM AUTHOR]

Published

2022

28. HDACi: The Columbus' Egg in Improving Cancer Treatment and Reducing Neurotoxicity?

Author

Squarzoni, Angelica, Scuteri, Arianna, and Cavaletti, Guido

Subjects

*TREATMENT of peripheral neuropathy, *TUMOR treatment, *NEUROTOXICOLOGY, *SYNDROMES, *CARCINOGENESIS, *ANTINEOPLASTIC agents, *GENE expression, *HISTONE deacetylase, *T-cell lymphoma

Abstract

Simple Summary: The inhibitors of histone deacetylases (HDACs) enzymes are an emerging class of drugs proposed for the treatment of several tumors. Despite a general antineoplastic effectiveness, HDACs inhibitors showed conflicting results concerning their effects on the nervous system. Such a discrepancy could be ascribable to the different actions of the HDACs and to drug selectivity. In this review, we analyzed the role of the main HDACs within the nervous system to better understand the effect of their inhibition, with the aim of identifying the most promising candidate to become an effective antineoplastic drug with a limited neurotoxic profile. Histone deacetylases (HDACs) are a group of enzymes that modify gene expression through the lysine acetylation of both histone and non-histone proteins, leading to a broad range of effects on various biological pathways. New insights on this topic broadened the knowledge on their biological activity and even more questions arose from those discoveries. The action of HDACs is versatile in biological pathways and, for this reason, inhibitors of HDACs (HDACis) have been proposed as a way to interfere with HDACs' involvement in tumorigenesis. In 2006, the first HDACi was approved by FDA for the treatment of cutaneous T-cell lymphoma; however, more selective HDACis were recently approved. In this review, we will consider new information on HDACs' expression and their regulation for the treatment of central and peripheral nervous system diseases. [ABSTRACT FROM AUTHOR]

Published

2022

29. Dialysis as a Novel Adjuvant Treatment for Malignant Cancers.

Author

Hobro, Sture, Nilsson, Anders, Sternby, Jan, Öberg, Carl, Pietras, Kristian, Axelson, Håkan, Carneiro, Ana, Kinhult, Sara, Christensson, Anders, Fors, Jonas, Maciejewski, Steven, Knox, Jason, Forsal, Innas, Källquist, Linda, and Roos, Viktoria

Subjects

*GLUCOSE metabolism, *GLUTAMINE metabolism, *METABOLISM, *TREATMENT effectiveness, *CELLULAR signal transduction, *TUMORS, *HEMODIALYSIS, *HISTONE deacetylase, *OXIDATION-reduction reaction, *EPIGENOMICS, *KETONES, *PATIENT safety

Abstract

Simple Summary: There is a clear need for new cancer therapies as many cancers have a very short long-term survival rate. For most advanced cancers, therapy resistance limits the benefit of any single-agent chemotherapy, radiotherapy, or immunotherapy. Cancer cells show a greater dependence on glucose and glutamine as fuel than healthy cells do. In this article, we propose using 4- to 8-h dialysis treatments to change the blood composition, i.e., lowering glucose and glutamine levels, and elevating ketone levels—thereby disrupting major metabolic pathways important for cancer cell survival. The dialysis' impact on cancer cells include not only metabolic effects, but also redox balance, immunological, and epigenetic effects. These pleiotropic effects could potentially enhance the effectiveness of traditional cancer treatments, such as radiotherapies, chemotherapies, and immunotherapies—resulting in improved outcomes and longer survival rates for cancer patients. Cancer metabolism is characterized by an increased utilization of fermentable fuels, such as glucose and glutamine, which support cancer cell survival by increasing resistance to both oxidative stress and the inherent immune system in humans. Dialysis has the power to shift the patient from a state dependent on glucose and glutamine to a ketogenic condition (KC) combined with low glutamine levels—thereby forcing ATP production through the Krebs cycle. By the force of dialysis, the cancer cells will be deprived of their preferred fermentable fuels, disrupting major metabolic pathways important for the ability of the cancer cells to survive. Dialysis has the potential to reduce glucose levels below physiological levels, concurrently increase blood ketone body levels and reduce glutamine levels, which may further reinforce the impact of the KC. Importantly, ketones also induce epigenetic changes imposed by histone deacetylates (HDAC) activity (Class I and Class IIa) known to play an important role in cancer metabolism. Thus, dialysis could be an impactful and safe adjuvant treatment, sensitizing cancer cells to traditional cancer treatments (TCTs), potentially making these significantly more efficient. [ABSTRACT FROM AUTHOR]

Published

2022

30. CREPT Disarms the Inhibitory Activity of HDAC1 on Oncogene Expression to Promote Tumorigenesis.

Author

Cao, Yajun, Ning, Bobin, Tian, Ye, Lan, Tingwei, Chu, Yunxiang, Ren, Fangli, Wang, Yinyin, Meng, Qingyu, Li, Jun, Jia, Baoqing, and Chang, Zhijie

Subjects

*ONCOGENES, *CARCINOGENESIS, *CELL cycle proteins, *GENE expression, *TUMOR suppressor genes, *HISTONE deacetylase, *CELL lines, *POLYMERASE chain reaction

Abstract

Simple Summary: It has been proposed that highly expressed HDAC1 (histone deacetylases 1) removes the acetyl group from the histones at the promoter regions of tumor suppressor genes to block their expression in tumors. We here revealed the underlying mechanism that HDAC1 differentially regulates the expression of oncogenes and tumor suppressors. In detail, we found that HDAC1 is unable to occupy the promoters of oncogenes but maintains its occupancy with the tumor suppressors due to its interaction with an oncoprotein, CREPT (cell cycle-related and expression-elevated protein in tumor). Histone deacetylases 1 (HDAC1), an enzyme that functions to remove acetyl molecules from ε-NH3 groups of lysine in histones, eliminates the histone acetylation at the promoter regions of tumor suppressor genes to block their expression during tumorigenesis. However, it remains unclear why HDAC1 fails to impair oncogene expression. Here we report that HDAC1 is unable to occupy at the promoters of oncogenes but maintains its occupancy with the tumor suppressors due to its interaction with CREPT (cell cycle-related and expression-elevated protein in tumor, also named RPRD1B), an oncoprotein highly expressed in tumors. We observed that CREPT competed with HDAC1 for binding to oncogene (such as CCND1, CLDN1, VEGFA, PPARD and BMP4) promoters but not the tumor suppressor gene (such as p21 and p27) promoters by a chromatin immunoprecipitation (ChIP) qPCR experiment. Using immunoprecipitation experiments, we deciphered that CREPT specifically occupied at the oncogene promoter via TCF4, a transcription factor activated by Wnt signaling. In addition, we performed a real-time quantitative PCR (qRT-PCR) analysis on cells that stably over-expressed CREPT and/or HDAC1, and we propose that HDAC1 inhibits CREPT to activate oncogene expression under Wnt signaling activation. Our findings revealed that HDAC1 functions differentially on tumor suppressors and oncogenes due to its interaction with the oncoprotein CREPT. [ABSTRACT FROM AUTHOR]

Published

2022

31. Histone Deacetylase 3 Governs β-Estradiol-ERα-Involved Endometrial Tumorigenesis via Inhibition of STING Transcription.

Author

Chen, Guofang, Yan, Qiang, Liu, Lin, Wen, Xinyue, Zeng, Hongliang, and Yin, Shasha

Subjects

*REVERSE transcriptase polymerase chain reaction, *FLOW cytometry, *XENOGRAFTS, *ESTRADIOL, *ANIMAL experimentation, *ANTINEOPLASTIC agents, *CELLULAR signal transduction, *INTERFERONS, *GENE expression, *TREATMENT effectiveness, *ENDOMETRIAL tumors, *MESSENGER RNA, *CELL proliferation, *HISTONE deacetylase, *TRANSCRIPTION factors, *CELL lines, *MICE, *EPIGENOMICS

Abstract

Simple Summary: Endometrial carcinoma is one of the most threatening gynecological malignancies to women's health, with mortality linked to it increasing, and finding novel and effective methods to combat endometrial carcinoma is becoming a clinical challenge. The stimulator of interferon genes (STING) pathway plays a crucial role in antitumor immunity, and it is strictly regulated by many types of post-translational modifications. The aim of our study was to uncover the expression and the contribution of acetylation involved in the regulation of STING to endometrial cancer. We confirmed that STING expression was deregulated by both β-estradiol and HDAC3, and worked as an important regulator of proliferation and apoptosis. Inhibition of HDAC3 increased STING expression, thereby inhibiting tumorigenesis. Therefore, this study uncovers a novel molecular mechanism by which HDAC3 inhibits STING transcription via β-estradiol-ERα, and provides a promising therapy with a combination of HDAC and STING for combating endometrial cancer. Purpose: The stimulator of interferon genes (STING) pathway plays a crucial role in antitumor immunity, and it is strictly regulated by many types of post-translational modifications. However, the contribution of acetylation involved in the regulation of STING to endometrial tumorigenesis remains unclear. Methods: We attempted to identify the key role of STING in endometrial carcinoma (EC) tissue and cell lines and explore its epigenetic regulation mechanism by HDACs that are critically involved in EC. We used IHC and qRT-PCR to detect the protein level and mRNA level of STING expression in endometrial carcinoma tissues, then explored the potential role of STING in tumor proliferation and apoptosis by CCK8 and flow cytometry, and identified the STING effect in the tumorigenicity by a mouse xenograft assay. We explored the possible relationship of acetylation alteration in STING regulation by ChIP analysis and Co-IP, and we knocked out STING in ECC1 and Ishikawa cells using CRISPR-Cas9 to further confirm the critical role of STING restoration induced by HDAC3 inhibitor RGFP-966 in the proliferation and apoptosis. Results: We found that STING expression was largely decreased and worked as an important regulator of cell proliferation and apoptosis; either activated or overexpressed STING, with both pharmacological and genetic approaches, largely blocked cell proliferation and induced apoptosis in EC. Moreover, STING expression was deregulated by both β-estradiol and HDAC3. Mechanically, we determined that HDAC3 can interact with β-estradiol-ERα and induce deacetylation of histone 3 lysine 4 at the STING promoter, thereby decreasing STING expression. Inhibition of HDAC3 increased STING expression, thereby inhibiting tumorigenesis. Conclusion: This study reveals a novel molecular mechanism by which HDAC3 inhibits STING transcription via β-estradiol-ERα and provides a promising therapy (a combination of HDAC and STING) for combating endometrial cancer. [ABSTRACT FROM AUTHOR]

Published

2022

32. Histone Deacetylase Inhibitors as a Therapeutic Strategy to Eliminate Neoplastic "Stromal" Cells from Giant Cell Tumors of Bone.

Author

Venneker, Sanne, van Eenige, Robin, Kruisselbrink, Alwine B., Palubeckaitė, Ieva, Taliento, Alice E., Briaire-de Bruijn, Inge H., Hogendoorn, Pancras C. W., van de Sande, Michiel A. J., Gelderblom, Hans, Mei, Hailiang, Bovée, Judith V. M. G., and Szuhai, Karoly

Subjects

*IN vitro studies, *GENETIC mutation, *CARCINOGENESIS, *GIANT cell tumors, *APOPTOSIS, *STROMAL cells, *BONE tumors, *GENE expression profiling, *HISTONE deacetylase, *CELL lines, *EPIGENOMICS, *CHEMICAL inhibitors

Abstract

Simple Summary: Giant cell tumor of bone (GCTB) is an intermediate bone neoplasm which consists of several cell populations, including the neoplastic "stromal" cells. These cells harbor a mutation in one of the histone H3.3 genes (H3F3A), and are therefore considered as the driving component of GCTB. This mutation causes changes in the epigenetic landscape, leading to aberrant gene expression patterns that may drive tumor growth. Surgery is currently the only curative treatment option because contemporary systemic therapies cannot remove the neoplastic cells from GCTB lesions, leading to re-outgrowth of the tumor when the treatment is discontinued. Therefore, the aim of this study was to explore whether therapeutic targeting of the epigenome can eliminate the neoplastic cells from GCTB lesions. The findings from this study indicate that histone deacetylase (HDAC) inhibitors may represent such a treatment strategy, which could improve the quality of life of GCTB patients who currently require life-long treatment. The neoplastic "stromal" cells in giant cell tumor of bone (GCTB) harbor a mutation in the H3F3A gene, which causes alterations in the epigenome. Current systemic targeted therapies, such as denosumab, do not affect the neoplastic cells, resulting in relapse upon treatment discontinuation. Therefore, this study examined whether targeting the epigenome could eliminate the neoplastic cells from GCTB. We established four novel cell lines of neoplastic "stromal" cells that expressed the H3F3A p.G34W mutation. These cell lines were used to perform an epigenetics compound screen (n = 128), which identified histone deacetylase (HDAC) inhibitors as key epigenetic regulators in the neoplastic cells. Transcriptome analysis revealed that the neoplastic cells expressed all HDAC isoforms, except for HDAC4. Therefore, five HDAC inhibitors targeting different HDAC subtypes were selected for further studies. All GCTB cell lines were very sensitive to HDAC inhibition in both 2D and 3D in vitro models, and inductions in histone acetylation, as well as apoptosis, were observed. Thus, HDAC inhibition may represent a promising therapeutic strategy to eliminate the neoplastic cells from GCTB lesions, which remains the paramount objective for GCTB patients who require life-long treatment with denosumab. [ABSTRACT FROM AUTHOR]

Published

2022

33. A Selective Histone Deacetylase Inhibitor Induces Autophagy and Cell Death via SCNN1A Downregulation in Glioblastoma Cells.

Author

Chang, Hui Hua, Chang, Yao-Yuan, Tsai, Bing-Chen, Chen, Li-Jyun, Chang, An-Chi, Chuang, Jian-Ying, Gean, Po-Wu, and Hsueh, Yuan-Shuo

Subjects

*BIOCHEMISTRY, *AUTOPHAGY, *PHENOMENOLOGICAL biology, *GLIOMAS, *RNA, *CELL survival, *GENE expression, *BIOINFORMATICS, *COMPARATIVE studies, *TEMOZOLOMIDE, *HISTONE deacetylase, *CELL death, *ENZYME inhibitors, *PHARMACODYNAMICS, *CHEMICAL inhibitors

Published

2022

34. From HDAC to Voltage-Gated Ion Channels: What's Next? The Long Road of Antiepileptic Drugs Repositioning in Cancer.

Author

Pellegrino, Michele, Ricci, Elena, Ceraldi, Rosangela, Nigro, Alessandra, Bonofiglio, Daniela, Lanzino, Marilena, and Morelli, Catia

Subjects

*ANTICONVULSANTS, *DRUG repositioning, *CALCIUM channels, *BIOAVAILABILITY, *ANTINEOPLASTIC agents, *DRUG labeling, *HISTONE deacetylase, *TUMORS, *PHARMACODYNAMICS

Published

2022

35. White Paper: Mimetics of Class 2 Tumor Suppressor Proteins as Novel Drug Candidates for Personalized Cancer Therapy.

Author

Dahl, Edgar, Villwock, Sophia, Habenberger, Peter, Choidas, Axel, Rose, Michael, and Klebl, Bert M.

Subjects

*INDIVIDUALIZED medicine, *TUMOR suppressor genes, *GENOMES, *TUMORS, *HISTONE deacetylase, *MEDICAL needs assessment, *PHENOTYPES

Published

2022

36. Can We Efficiently Target HDAC in Cancer?

Author

Kiesslich, Tobias and Neureiter, Daniel

Subjects

*THERAPEUTIC use of antineoplastic agents, *SERIAL publications, *TUMORS, *HISTONE deacetylase, *ENZYME inhibitors, *CHEMICAL inhibitors

Published

2022

37. Histone Deacetylase Inhibitors Restore Cancer Cell Sensitivity towards T Lymphocytes Mediated Cytotoxicity in Pancreatic Cancer.

Author

Looi, Chin-King, Gan, Li-Lian, Sim, Wynne, Hii, Ling-Wei, Chung, Felicia Fei-Lei, Leong, Chee-Onn, Lim, Wei-Meng, and Mai, Chun-Wai

Subjects

*PANCREATIC tumors, *ADENOCARCINOMA, *CONFIDENCE intervals, *WESTERN immunoblotting, *CELLULAR signal transduction, *GENE expression, *RESEARCH funding, *SURVIVAL analysis (Biometry), *T cells, *HISTONE deacetylase, *CELL lines, *CHEMICAL inhibitors

Abstract

Simple Summary: Pancreatic ductal adenocarcinoma (PDAC) is an aggressive pancreatic cancer that is resistant to most treatments due to its tumour microenvironment. In search of an effective therapeutic agents that can overcome the tumour microenvironment, we analysed the PDAC patients genomic profilings and identified that patients with high cytotoxic T lymphocytes (CTL) killing activity were associated with better clinical outcomes. Through genomic and proteomic approaches, we identified potential small molecules that may restore CTL activity in PDAC. We validated the findings using two CTL-resistant PDAC cells and concluded that histone deacetylase inhibitors (givinostat and dacinostat) can reverse CTL sensitivity in CTL-resistant PDAC cells. Despite medical advancements, the prognosis of pancreatic ductal adenocarcinoma (PDAC) has not improved significantly over the past 50 years. By utilising the large-scale genomic datasets available from the Australia Pancreatic Cancer Project (PACA-AU) and The Cancer Genomic Atlas Project (TCGA-PAAD), we studied the immunophenotype of PDAC in silico and identified that tumours with high cytotoxic T lymphocytes (CTL) killing activity were associated with favourable clinical outcomes. Using the STRING protein–protein interaction network analysis, the identified differentially expressed genes with low CTL killing activity were associated with TWIST/IL-6R, HDAC5, and EOMES signalling. Following Connectivity Map analysis, we identified 44 small molecules that could restore CTL sensitivity in the PDAC cells. Further high-throughput chemical library screening identified 133 inhibitors that effectively target both parental and CTL-resistant PDAC cells in vitro. Since CTL-resistant PDAC had a higher expression of histone proteins and its acetylated proteins compared to its parental cells, we further investigated the impact of histone deacetylase inhibitors (HDACi) on CTL-mediated cytotoxicity in PDAC cells in vitro, namely SW1990 and BxPC3. Further analyses revealed that givinostat and dacinostat were the two most potent HDAC inhibitors that restored CTL sensitivity in SW1990 and BxPC3 CTL-resistant cells. Through our in silico and in vitro studies, we demonstrate the novel role of HDAC inhibition in restoring CTL resistance and that combinations of HDACi with CTL may represent a promising therapeutic strategy, warranting its further detailed molecular mechanistic studies and animal studies before embarking on the clinical evaluation of these novel combined PDAC treatments. [ABSTRACT FROM AUTHOR]

Published

2022

38. Histone Demethylase JMJD2D: A Novel Player in Colorectal and Hepatocellular Cancers.

Author

Chen, Qiang, Peng, Kesong, Mo, Pingli, and Yu, Chundong

Subjects

*COLORECTAL cancer, *HISTONE deacetylase, *HEPATOCELLULAR carcinoma

Abstract

Simple Summary: Histone demethylase JMJD2D is a multifunctional epigenetic factor coordinating androgen receptor activation, DNA damage repair, DNA replication, cell cycle regulation, and inflammation modulation. JMJD2D is also a well-established epigenetic facilitator in the progression of multiple malignant tumors, especially in colorectal cancer (CRC) and hepatocellular cancer (HCC). This review aims to summarize the mechanisms of JMJD2D in promoting CRC and HCC progression, which provides novel ideas for targeting JMJD2D in oncotherapy. JMJD2D promotes gene transcription by reducing H3K9 methylation and serves as a coactivator to enhance the activities of multiple carcinogenic pathways, including Wnt/β-catenin, Hedgehog, HIF1, JAK-STAT3, and Notch signaling; or acts as an antagonist of the tumor suppressor p53. Posttranslational modifications (PTMs) of histones are well-established contributors in a variety of biological functions, especially tumorigenesis. Histone demethylase JMJD2D (also known as KDM4D), a member of the JMJD2 subfamily, promotes gene transcription by antagonizing H3K9 methylation. JMJD2D is an epigenetic factor coordinating androgen receptor activation, DNA damage repair, DNA replication, and cell cycle regulation. Recently, the oncogenic role of JMJD2D in colorectal cancer (CRC) and hepatocellular cancer (HCC) has been recognized. JMJD2D serves as a coactivator of β-catenin, Gli1/2, HIF1α, STAT3, IRF1, TCF4, and NICD or an antagonist of p53 to promote the progression of CRC and HCC. In this review, we summarize the molecular mechanisms of JMJD2D in promoting the progression of CRC and HCC as well as the constructive role of its targeting inhibitors in suppressing tumorigenesis and synergistically enhancing the efficacy of anti-PD-1/PD-L1 immunotherapy. [ABSTRACT FROM AUTHOR]

Published

2022

39. Potential Prognostic Markers for Relapsed/Refractory vs. Responsive Acute Myeloid Leukemia.

Author

Vitkevičienė, Aida, Skliutė, Giedrė, Žučenka, Andrius, Borutinskaitė, Veronika, and Navakauskienė, Rūta

Subjects

*CANCER relapse, *GENE expression, *LYSINE, *TUMOR markers, *HISTONE deacetylase, *EPIGENOMICS, *ACETYLTRANSFERASES

Abstract

Simple Summary: Acute myeloid leukemia (AML) is the most common blood cancer in the elderly, which progresses rapidly and is often fatal. The prognosis for AML remains poor in most older patients: only about 15% of patients over 60 years of age can recover. Our aim is to determine new potential AML clinical treatment prognosis markers. We analyzed certain genes, proteins and the epigenome profile in therapy-resistant and responsive AML patients at diagnosis stage and after clinical treatment. We determined that MYC, WT1, IDH1, CDKN1A, HDAC2, TET1, KAT6A and GATAD2A gene expression changes might characterize refractory AML. Therefore, these genes could have an impact for AML prognosis. Acute myeloid leukemia (AML) is a heterogeneous disease. A significant proportion of AML patients is refractory to clinical treatment or relapses. Our aim is to determine new potential AML clinical treatment prognosis markers. We investigated various cell fate and epigenetic regulation important gene level differences between refractory and responsive AML patient groups at diagnosis stage and after clinical treatment using RT-qPCR. We demonstrated that oncogenic MYC and WT1 and metabolic IDH1 gene expression was significantly higher and cell cycle inhibitor CDKN1A (p21) gene expression was significantly lower in refractory patients' bone marrow cells compared to treatment responsive patients both at diagnosis and after clinical treatment. Moreover, we determined that, compared to clinical treatment responsive patients, refractory patients possess a significantly higher gene expression of histone deacetylase 2 (HDAC2) and epigenetic DNA modulator TET1 and a significantly lower gene expression of lysine acetyltransferase 6A (KAT6A) and nucleosome remodeling and deacetylase (NuRD) complex component GATAD2A. We suggest that MYC, WT1, IDH1, CDKN1A, HDAC2, TET1, KAT6A and GATAD2A gene expression changes might characterize refractory AML. Thus, they might be useful for AML prognosis. Additionally, we suggest that epigenetic modulation might be beneficial in combination with standard treatment. [ABSTRACT FROM AUTHOR]

Published

2022

40. A Histone Deacetylase Inhibitor Induces Acetyl-CoA Depletion Leading to Lethal Metabolic Stress in RAS-Pathway Activated Cells.

Author

Basseville, Agnes, Violet, Pierre-Christian, Safari, Maryam, Sourbier, Carole, Linehan, W. Marston, Robey, Robert W., Levine, Mark, Sackett, Dan L., and Bates, Susan E.

Subjects

*PROTEIN metabolism, *FLOW cytometry, *CELLULAR signal transduction, *METABOLIC syndrome, *GENE expression profiling, *HISTONE deacetylase, *CELL lines, *SENSITIVITY & specificity (Statistics), *CHEMICAL inhibitors

Abstract

Simple Summary: Epigenetic therapies have been difficult to translate to solid tumors, in part because a lack of a full mechanistic understanding has not allowed the selection of tumors most likely to benefit from the therapies. Here we identified a RAS-phenotype that can be targeted by the histone deacetylase inhibitor (HDACi) romidepsin. We showed that the hyperacetylation induced by romidepsin depletes acetyl-CoA, the cell donor substrate for acetylation, and it leads to metabolic stress and death in KRAS-activated cells. Transcriptomic analysis confirmed that perturbation of two acetyl-CoA generation pathways (fatty acid metabolism and branched-chain amino acid (BCAA) metabolism) were correlated with HDACi sensitivity in a 608-cell line panel and in patients treated with belinostat. Our analysis highlights the potential utility of an acetyl-CoA phenotype to sharpen treatment choices for RAS-activated tumors, and it suggests that acetyl-CoA depletion could be a key effect underlying the myriad cellular responses that follow HDAC inhibition. Background: The mechanism of action of romidepsin and other histone deacetylase inhibitors is still not fully explained. Our goal was to gain a mechanistic understanding of the RAS-linked phenotype associated with romidepsin sensitivity. Methods: The NCI60 dataset was screened for molecular clues to romidepsin sensitivity. Histone acetylation, DNA damage, ROS production, metabolic state (real-time measurement and metabolomics), and gene expression alterations (transcriptomics) were determined in KRAS-WT versus KRAS-mutant cell groups. The search for biomarkers in response to HDACi was implemented by supervised machine learning analysis on a 608-cell transcriptomic dataset and validated in a clinical dataset. Results: Romidepsin treatment induced depletion in acetyl-CoA in all tested cell lines, which led to oxidative stress, metabolic stress, and increased death—particularly in KRAS-mutant cell lines. Romidepsin-induced stresses and death were rescued by acetyl-CoA replenishment. Two acetyl-CoA gene expression signatures associated with HDACi sensitivity were derived from machine learning analysis in the CCLE (Cancer Cell Line Encyclopedia) cell panel. Signatures were then validated in the training cohort for seven HDACi, and in an independent 13-patient cohort treated with belinostat. Conclusions: Our study reveals the importance of acetyl-CoA metabolism in HDAC sensitivity, and it highlights acetyl-CoA generation pathways as potential targets to combine with HDACi. [ABSTRACT FROM AUTHOR]

Published

2022

41. Inhibition of HDAC and Signal Transduction Pathways Induces Tight Junctions and Promotes Differentiation in p63-Positive Salivary Duct Adenocarcinoma.

Author

Nakano, Masaya, Ohwada, Kizuku, Shindo, Yuma, Konno, Takumi, Kohno, Takayuki, Kikuchi, Shin, Tsujiwaki, Mitsuhiro, Ishii, Daichi, Nishida, Soshi, Kakuki, Takuya, Obata, Kazufumi, Miyata, Ryo, Kurose, Makoto, Kondoh, Atsushi, Takano, Kenichi, and Kojima, Takashi

Subjects

*THERAPEUTIC use of antineoplastic agents, *CELL differentiation, *SALIVARY gland tumors, *ADENOCARCINOMA, *CARCINOGENESIS, *ANTINEOPLASTIC agents, *RNA, *CELLULAR signal transduction, *GENE expression, *CELL proliferation, *HISTONE deacetylase, *PAROTID glands, *CELL lines, *ANTIBIOTICS, *PHARMACODYNAMICS, *CHEMICAL inhibitors

Abstract

Simple Summary: The p53 family p63 gene is essential for the proliferation and differentiation of various epithelial cells, and it is overexpressed in some salivary gland neoplasia. Histone deacetylases (HDACs) are thought to play a crucial role in carcinogenesis, and HDAC inhibitors downregulate p63 expression in cancers. p63 is not only a diagnostic marker of salivary gland neoplasia, but it also promotes the malignancy. Inhibition of HDAC and signal transduction pathways inhibited cell proliferation and migration, induced tight junctions, and promoted differentiation in p63-positive salivary duct adenocarcinoma (SDC). It is, therefore, useful in therapy for p63-positive SDC cells. Background: The p53 family p63 is essential for the proliferation and differentiation of various epithelial basal cells. It is overexpressed in several cancers, including salivary gland neoplasia. Histone deacetylases (HDACs) are thought to play a crucial role in carcinogenesis, and HDAC inhibitors downregulate p63 expression in cancers. Methods: In the present study, to investigate the roles and regulation of p63 in salivary duct adenocarcinoma (SDC), human SDC cell line A253 was transfected with siRNA-p63 or treated with the HDAC inhibitors trichostatin A (TSA) and quisinostat (JNJ-26481585). Results: In a DNA array, the knockdown of p63 markedly induced mRNAs of the tight junction (TJ) proteins cingulin (CGN) and zonula occuludin-3 (ZO-3). The knockdown of p63 resulted in the recruitment of the TJ proteins, the angulin-1/lipolysis-stimulated lipoprotein receptor (LSR), occludin (OCLN), CGN, and ZO-3 at the membranes, preventing cell proliferation, and leading to increased cell metabolism. Treatment with HDAC inhibitors downregulated the expression of p63, induced TJ structures, recruited the TJ proteins, increased the epithelial barrier function, and prevented cell proliferation and migration. Conclusions: p63 is not only a diagnostic marker of salivary gland neoplasia, but it also promotes the malignancy. Inhibition of HDAC and signal transduction pathways is, therefore, useful in therapy for p63-positive SDC cells. [ABSTRACT FROM AUTHOR]

Published

2022

42. Epigenetic-Like Stimulation of Receptor Expression in SSTR2 Transfected HEK293 Cells as a New Therapeutic Strategy.

Author

Kotzerke, Joerg, Buesser, Dorothee, Naumann, Anne, Runge, Roswitha, Huebinger, Lisa, Kliewer, Andrea, Freudenberg, Robert, and Brogsitter, Claudia

Subjects

*METHYLTRANSFERASES, *COLONY-forming units assay, *CELL receptors, *RADIOISOTOPES, *GENE expression, *CELL survival, *NEUROENDOCRINE tumors, *DESCRIPTIVE statistics, *HISTONE deacetylase, *EPIGENOMICS, *VALPROIC acid, *CHEMICAL inhibitors

Abstract

Simple Summary: Neuroendocrine tumors (NETs) expressing the somatostatin receptor subtype 2 (SSTR2) are promising targets for peptide receptor radionuclide therapy (PRRT) using the somatostatin analogue Lu-177-DOTATATE. Patients expressing low levels of SSTR2 do not benefit from PRRT. Therefore, an approach to increase the efficacy of PRRT utilizing the effects of 5-aza-2′-deoxycytidine (5-aza-dC) and valproic acid (VPA) on the SSTR2 expression levels is investigated. The cell lines HEKsst2 and PC3 are incubated with 5-aza-dC and VPA in different combinations. The drug pretreatment of HEKsst2 cells leads to increased Lu-177-DOTATATE uptake values (factor 28) and lower cell survival (factor 4) in comparison to unstimulated cells; in PC3 cells, the effects are negligible. Further, for the stimulated cell types, the maintenance of the intrinsic radiosensitivity in each cell type is confirmed by X-ray irradiation. The increased SSTR2 expression induced by VPA and 5-aza-dC stimulation in HEKsst2 cells might improve treatment strategies for patients with NETs. The aim of the study was to increase the uptake of the SSTR2-targeted radioligand Lu-177-DOTATATE using the DNA methyltransferase inhibitor (DNMTi) 5-aza-2′-deoxycytidine (5-aza-dC) and the histone deacetylase inhibitor (HDACi) valproic acid (VPA). The HEKsst2 and PC3 cells were incubated with variable concentrations of 5-aza-dC and VPA to investigate the uptake of Lu-177-DOTATATE. Cell survival, subsequent to external X-rays (0.6 or 1.2 Gy) and a 24 h incubation with 57.5 or 136 kBq/mL Lu-177-DOTATATE, was investigated via colony formation assay to examine the effect of the epidrugs. In the case of stimulated HEKsst2 cells, the uptake of Lu-177-DOTATATE increased by a factor of 28 in comparison to the unstimulated cells. Further, stimulated HEKsst2 cells demonstrated lower survival fractions (factor 4). The survival fractions of the PC3 cells remained almost unchanged. VPA and 5-aza-dC did not induce changes to the intrinsic radiosensitivity of the cells after X-ray irradiation. Clear stimulatory effects on HEKsst2 cells were demonstrated by increased cell uptake of the radioligand and enhanced SST2 receptor quantity. In conclusion, the investigated approach is suitable to stimulate the somatostatin receptor expression and thus the uptake of Lu-177-DOTATATE, enabling a more efficient treatment for patients with poor response to peptide radionuclide therapy (PRRT). [ABSTRACT FROM AUTHOR]

Published

2022

43. HDAC Inhibition with Valproate Improves Direct Cytotoxicity of Monocytes against Mesothelioma Tumor Cells.

Author

Hoyos, Clotilde, Fontaine, Alexis, Jacques, Jean-Rock, Heinen, Vincent, Louis, Renaud, Duysinx, Bernard, Scherpereel, Arnaud, Wasielewski, Eric, Jamakhani, Majeed, Hamaidia, Malik, and Willems, Luc

Subjects

*MESOTHELIOMA, *CYTOKINES, *PHAGOCYTOSIS, *MACROPHAGES, *IMMUNOSUPPRESSION, *IMMUNE system, *HISTONE deacetylase, *CELL lines, *VALPROIC acid, *MONOCYTES, *PHENOTYPES, *CHEMICAL inhibitors

Abstract

Simple Summary: Tumor-associated macrophages and monocyte myeloid-derived immunosuppressive cells are associated with bad prognosis in malignant pleural mesothelioma (MPM). This study shows that peripheral blood monocytes can, nevertheless, be cytotoxic for MPM tumor cells. This cytotoxic activity that involves direct cell-to-cell contact can be improved with a lysine deacetylase inhibitor (VPA), opening new prospects for further improvement of still unsatisfactory MPM therapies. The composition of the tumor microenvironment (TME) mediates the outcome of chemo- and immunotherapies in malignant pleural mesothelioma (MPM). Tumor-associated macrophages (TAMs) and monocyte myeloid-derived immunosuppressive cells (M-MDSCs) constitute a major fraction of the TME. As central cells of the innate immune system, monocytes exert well-characterized functions of phagocytosis, cytokine production, and antibody-dependent cell-mediated cytotoxicity (ADCC). The objective of this study was to evaluate the ability of monocytes to exert a direct cytotoxicity by cell-to-cell contact with MPM cells. The experimental model is based on cocultures between human blood-derived monocytes sorted by negative selection and mesothelioma cell lines. Data show (i) that blood-derived human monocytes induce tumor cell death by direct cell-to-cell contact, (ii) that VPA is a pharmacological enhancer of this cytotoxic activity, (iii) that VPA increases monocyte migration and their aggregation with MPM cells, and (iv) that the molecular mechanisms behind VPA modulation of monocytes involve a downregulation of the membrane receptors associated with the M2 phenotype, i.e., CD163, CD206, and CD209. These conclusions, thus, broaden our understanding about the molecular mechanisms involved in immunosurveillance of the tumor microenvironment and open new prospects for further improvement of still unsatisfactory MPM therapies [ABSTRACT FROM AUTHOR]

Published

2022

44. Histone Deacetylase Inhibitors Impair Glioblastoma Cell Motility and Proliferation.

Author

Rampazzo, Elena, Manfreda, Lorenzo, Bresolin, Silvia, Cani, Alice, Mariotto, Elena, Bortolozzi, Roberta, Della Puppa, Alessandro, Viola, Giampietro, and Persano, Luca

Subjects

*GLIOMAS, *WNT proteins, *CELL motility, *CELL survival, *CELLULAR signal transduction, *INTERFERONS, *CELL proliferation, *HISTONE deacetylase, *TRANSCRIPTION factors, *CHEMICAL inhibitors

Abstract

Simple Summary: Glioblastoma (GBM) is considered the deadliest brain tumor; with patients displaying a high incidence of relapse and a 3-year survival of only 3–5%. For these reasons, investigation of the molecular basis of the disease could provide novel targets for therapy and improve patient prognoses. Based on our previous data, demonstrating that high levels of the transcription factor TCF4 (TCF7L2) sustain the aggressiveness and the stem cell features of these tumors, in this study we tested the ability of the histone deacetylase inhibitors (HDI) Trichostatin-A and Vorinostat to suppress TCF4 levels. We demonstrated that HDI treatment impairs proliferation and viability of GBM cells. Moreover, molecular analysis of HDI effects disclosed their ability to counteract tumor cell motility by affecting the RhoA-GTPase and the interferon pathways, supporting their further characterization as potential anti-GBM agents. Despite being subjected to high-dose chemo and radiotherapy, glioblastoma (GBM) patients still encounter almost inevitable relapse, due to the capability of tumor cells to disseminate and invade normal brain tissues. Moreover, the presence of a cancer stem cell (CSC) subpopulation, already demonstrated to better resist and evade treatments, further frustrates potential therapeutic approaches. In this context, we previously demonstrated that GBM is characterized by a tightly-regulated balance between the β-catenin cofactors TCF1 and TCF4, with high levels of TCF4 responsible for sustaining CSC in these tumors; thus, supporting their aggressive features. Since histone deacetylase inhibitors (HDI) have been reported to strongly reduce TCF4 levels in colon cancer cells, we hypothesized that they could also exert a similar therapeutic action in GBM. Here, we treated primary GBM cultures with Trichostatin-A and Vorinostat, demonstrating their ability to strongly suppress the Wnt-dependent pathways; thus, promoting CSC differentiation and concomitantly impairing GBM cell viability and proliferation. More interestingly, analysis of their molecular effects suggested a prominent HDI action against GBM cell motility/migration, which we demonstrated to rely on the inhibition of the RhoA-GTPase and interferon intracellular cascades. Our results suggest HDI as potential therapeutic agents in GBM, through their action on multiple cancer hallmarks. [ABSTRACT FROM AUTHOR]

Published

2022

45. Quantitative Analysis of Cell Aggregation Dynamics Identifies HDAC Inhibitors as Potential Regulators of Cancer Cell Clustering

Author

Fabien Gava, Sébastien Déjean, Joseph Agossa, Bernard Ducommun, Odile Mondesert, Julie Pignolet, Valérie Lobjois, and Renaud Morin

Subjects

Cancer Research, Chemistry, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, anchorage-independent aggregation, Computational biology, medicine.disease, In vitro, Cell aggregation, Article, Metastasis, transcriptional expression, Oncology, cancer cell clustering, Connectivity Map, HDAC inhibitors, Cell culture, Cancer cell, Gene expression, medicine, Histone deacetylase, Gene, RC254-282

Abstract

Simple Summary Metastases formation involves the formation, circulation and seeding of cohesive group of tumor cells called circulating tumors cells clusters at distant organs from the primary tumor. These clusters have a much higher metastatic potential than individual circulating tumor cell, it is therefore important to understand the molecular mechanisms involved in their formation. To this aim, in this study, from the analysis of the relationship between in vitro aggregation quantitative characterization of 25 cancer cell lines and their expression data, we identified genes significantly associated with aggregation. Interestingly, we found that these genes were strongly correlated with the transcriptional signature induced by HDAC inhibitors treatment and we finally showed experimentally that two HDAC inhibitors inhibits tumor cells cluster formation in vitro. These results open new therapeutic perspectives to prevent metastasis formation. Abstract Characterization of the molecular mechanisms involved in tumor cell clustering could open the way to new therapeutic strategies. Towards this aim, we used an in vitro quantitative procedure to monitor the anchorage-independent cell aggregation kinetics in a panel of 25 cancer cell lines. The analysis of the relationship between selected aggregation dynamic parameters and the gene expression data for these cell lines from the CCLE database allowed identifying genes with expression significantly associated with aggregation parameter variations. Comparison of these transcripts with the perturbagen signatures from the Connectivity Map resource highlighted that they were strongly correlated with the transcriptional signature of most histone deacetylase (HDAC) inhibitors. Experimental evaluation of two HDAC inhibitors (SAHA and ISOX) showed that they inhibited the initial step of in vitro tumor cell aggregation. This validates our findings and reinforces the potential interest of HDCA inhibitors to prevent metastasis spreading.

Published

2021

46. Comparing the Effect of Multiple Histone Deacetylase Inhibitors on SSTR2 Expression and [111In]In-DOTATATE Uptake in NET Cells

Author

Leo J. Hofland, Maria J. Klomp, Peter M. van Koetsveld, Simone U. Dalm, Marion de Jong, Fadime Dogan, Internal Medicine, and Radiology & Nuclear Medicine

Subjects

peptide receptor radionuclide therapy, Cancer Research, Mocetinostat, Entinostat, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, epigenetic drugs, histone deacetylase inhibitors, [111In]In-DOTATATE, SSTR2, chemistry.chemical_compound, somatostatin type-2 receptors, Oncology, chemistry, SDG 3 - Good Health and Well-being, Panobinostat, Radionuclide therapy, Cancer research, Somatostatin receptor 2, Histone deacetylase, Radiosensitivity, neuroendocrine tumors, Receptor, upregulation, RC254-282

Abstract

The aim of this study was to increase somatostatin type-2 receptor (SSTR2) expression on neuroendocrine tumor (NET) cells using histone deacetylase inhibitors (HDACis), potentially increasing the uptake of SSTR2-targeted radiopharmaceuticals and subsequently improving treatment efficacy of peptide receptor radionuclide therapy (PRRT). Human NET cell lines BON-1, NCI-H727, and GOT1 were treated with HDACis (i.e., CI-994, entinostat, LMK-235, mocetinostat, panobinostat, or valproic acid (VPA), entinostat and VPA were the HDACis tested in GOT1 cells) to examine SSTR2 mRNA expression levels and uptake of SSTR2-targeting radiotracer [111In]In-DOTATATE. Reversibility of the induced effects was examined after drug-withdrawal. Finally, the effect of VPA on radiosensitivity was investigated. A strong stimulatory effect in BON-1, NCI-H727, and GOT1 cells was observed after HDACi treatment, both on SSTR2 mRNA expression levels and [111In]In-DOTATATE uptake. The effects of the HDACis were largely reversible over a period of seven days, demonstrating largest reductions within the first day. The reversibility profile of the induced effects suggests that proper timing of HDACi treatment is most likely essential for a beneficial outcome. In addition to increasing SSTR2 expression levels, VPA enhanced the radiosensitivity of all cell lines. In conclusion, HDACi treatment increased SSTR2 expression, and radiosensitivity was also enhanced upon VPA treatment.

Published

2021

47. Histone Deacetylase (HDAC)-1, -2, -4, and -6 in Uveal Melanomas: Associations with Clinicopathological Parameters and Patients’ Survival

Author

Pawel Gajdzis, Nathalie Cassoux, Sophie Gardrat, Christos Masaoutis, Georgia Levidou, Jerzy Klijanienko, Stamatios Theocharis, Eougken Danas, Piotr Donizy, Malgorzata Gajdzis, and Alexandros Pergaris

Subjects

Cancer Research, Monosomy, Mitotic index, biology, business.industry, Melanoma, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, medicine.disease_cause, medicine.disease, Article, Histone, Oncology, HDAC, immunohistochemistry, biology.protein, Cancer research, Medicine, Immunohistochemistry, Clinical significance, Histone deacetylase, prognosis, uveal melanoma, business, Carcinogenesis, RC254-282

Abstract

Simple Summary Histone Deacetylases (HDACs) have been reportedly associated with tumor development and progression in several types of human malignancy, being currently investigated as potential targets of anti-cancer therapy. The aim of this study is to assess the clinical significance and prognostic role of the of HDAC-1, -2, -4, and -6 immunohistochemical expression, in 75 uveal melanoma (UM) cases. HDACs are differentially expressed in UMs, HDAC-2 being the most frequently expressed isoform, whereas cytoplasmic expression of class I HDAC isoforms is also observed. Additionally, HDAC-1 was associated with increased tumor size, HDAC-6 with mitotic index, and HDAC-2 with epithelioid cell morphology and presence of tumor-infiltrating lymphocytes, both parameters of adverse prognosis. Moreover, our data support a significant association of HDAC-2 with patients’ improved OS. These findings suggest that HDACs, and especially HDAC-2, may be implicated in the formation and progression of UM. Abstract Background: Uveal melanoma (UM) represents the most common primary intraocular malignancy in adults, exerting high metastatic potential and poor prognosis. Histone deacetylases (HDACs) play a key role in carcinogenesis, and HDAC inhibitors (HDACIs) are currently being explored as anti-cancer agents in clinical settings. The aim of this study was to evaluate the clinical significance of HDAC-1, -2, -4, and -6 expression in UM. Methods: HDAC-1, -2, -4, and -6 expression was examined immunohistochemically in 75 UM tissue specimens and was correlated with tumors’ clinicopathological characteristics, the presence of tumor-infiltrating lymphocytes (TILS), as well as with our patients’ overall survival (OS). Results: HDAC-2 was the most frequently expressed isoform (66%), whereas we confirmed in addition to the expected nuclear expression the presence of cytoplasmic expression of class I HDAC isoforms, namely HDAC-1 (33%) and HDAC-2 (9.5%). HDAC-4 and -6 expression was cytoplasmic. HDAC-1 nuclear expression was associated with increased tumor size (p = 0.03), HDAC-6 with higher mitotic index (p = 0.03), and nuclear HDAC-2 with epithelioid cell morphology (p = 0.03) and presence of tumor-infiltrating lymphocytes (p = 0.04). The association with the remaining parameters including Monosomy 3 was not significant. Moreover, the presence as well as the nuclear expression pattern of HDAC-2 were correlated with patients’ improved OS and remained significant in multivariate survival analysis. Conclusions: These findings provide evidence for a potential role of HDACs and especially HDAC-2 in the biological mechanisms governing UM evolution and progression.

Published

2021

48. The Synergistic Anti-Tumor Activity of EZH2 Inhibitor SHR2554 and HDAC Inhibitor Chidamide through ORC1 Reduction of DNA Replication Process in Diffuse Large B Cell Lymphoma

Author

Zhitao Ying, Lijuan Deng, Hui Yu, Feier Feng, Jun Zhu, Luni Hu, Jiao Li, Lan Mi, Dedao Wang, Wei Fang, Chao Zhong, Meng Wu, Xing Wang, Yime Zhang, Yunfei Shi, Yuqin Song, Yingying Ye, and Ning Ding

Subjects

Cancer Research, Cell growth, EZH2 inhibitor, diffuse large B-cell lymphoma, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, macromolecular substances, Cell cycle, medicine.disease, Article, chemistry.chemical_compound, Oncology, chemistry, In vivo, Apoptosis, Chidamide, Cancer research, medicine, Viability assay, Histone deacetylase, synergistic effects, DNA replication process, Diffuse large B-cell lymphoma, RC254-282

Abstract

Simple Summary The EZH2-targeted drugs have demonstrated notable therapeutic effects in EZH2 mutant B-cell lymphoma patients. In this study, we demonstrated that the combination of EZH2 inhibitor SHR2554 and HDAC inhibitor HBI8000 exert synergistic anti-proliferative activity in both EZH2 wide-type and mutation B-cell lymphoma. More importantly, gene expression profile analysis revealed simultaneous treatment with these agents led to dramatic inhibition of DNA replication initiator protein ORC1, which might contribute to great efficacy of combination strategy. The combination of EZH2 inhibitor and HDAC inhibitor could provide a potential therapeutic treatment for both EZH2 wide-type and mutation B-cell lymphoma patients. Abstract Background: Upregulation of H3K27me3 induced by EZH2 overexpression or somatic heterozygous mutations were implicated in lymphomagenesis. It has been demonstrated that several EZH2-target agents have notable therapeutic effects in EZH2-mutant B-cell lymphoma patients. Here we present a novel highly selective EZH2 inhibitor SHR2554 and possible combination strategy in diffuse large B-cell lymphoma (DLBCL). Methods: Cell proliferation, cell cycle and apoptosis were analyzed by CellTiter-Glo Luminescent Cell Viability Assay and flow cytometry. Western Blot was used to detect the expression of related proteins. The gene expression profiling post combination treatment was analyzed by RNA-Seq. Finally, CDX and PDX models were used to evaluate the synergistic anti-tumor effects of the combination treatment in vivo. Results: The novel EZH2 inhibitor SHR2554 inhibited proliferation and induced G1 phase arrest in EZH2-mutant DLBCL cell lines. The combination of EZH2 inhibitor SHR2554 with histone deacetylase (HDAC) inhibitor chidamide (hereafter referred to as HBI8000) exerted synergistic anti-proliferative activity in vitro and in vivo. Gene expression profile analysis revealed dramatic inhibition of the DNA replication process in combined treatment. Conclusions: SHR2554, a potent, highly selective small molecule inhibitor of EZH2, inhibited EZH2-mutant DLBCL more significantly in vitro and in vivo. The combination of HDAC inhibitor HBI8000 with EZH2 inhibitor SHR2554 exhibited dramatic anti-tumor activity in both mutant and wild-type DLBCL, which may become a potential therapeutic modality for the treatment of DLBCL patients.

Published

2021

49. Valproic Acid and Breast Cancer: State of the Art in 2021

Author

Andrzej Stepulak, Marta Halasa, Wirginia Kukula-Koch, Estera Okon, and Anna Wawruszak

Subjects

0301 basic medicine, Cancer Research, medicine.medical_treatment, Review, Targeted therapy, 03 medical and health sciences, 0302 clinical medicine, Breast cancer, breast cancer, In vivo, medicine, Adverse effect, RC254-282, Valproic Acid, epigenetics, business.industry, valproic acid (VPA), histone acetylation, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, targeted therapy, medicine.disease, 030104 developmental biology, Anticonvulsant, Oncology, histone deacetylases (HDACs), 030220 oncology & carcinogenesis, Toxicity, Cancer research, Histone deacetylase, business, medicine.drug, histone deacetylase inhibitor (HDI)

Abstract

Simple Summary Breast cancer (BC) is the most common cancer diagnosed among women worldwide. Despite numerous studies, the pathogenesis of BC is still poorly understood, and effective therapy of this disease remains a challenge for medicine. This article provides the current state of knowledge of the impact of valproic acid (VPA) on different histological subtypes of BC, used in monotherapy or in combination with other active agents in experimental studies in vitro and in vivo. The comprehensive review highlights the progress that has been made on this topic recently. Abstract Valproic acid (2-propylpentanoic acid, VPA) is a short-chain fatty acid, a member of the group of histone deacetylase inhibitors (HDIs). VPA has been successfully used in the treatment of epilepsy, bipolar disorders, and schizophrenia for over 50 years. Numerous in vitro and in vivo pre-clinical studies suggest that this well-known anticonvulsant drug significantly inhibits cancer cell proliferation by modulating multiple signaling pathways. Breast cancer (BC) is the most common malignancy affecting women worldwide. Despite significant progress in the treatment of BC, serious adverse effects, high toxicity to normal cells, and the occurrence of multi-drug resistance (MDR) still limit the effective therapy of BC patients. Thus, new agents which improve the effectiveness of currently used methods, decrease the emergence of MDR, and increase disease-free survival are highly needed. This review focuses on in vitro and in vivo experimental data on VPA, applied individually or in combination with other anti-cancer agents, in the treatment of different histological subtypes of BC.

Published

2021

50. A Novel ZIP4-HDAC4-VEGFA Axis in High-Grade Serous Ovarian Cancer

Author

Tian Li Wang, Robert E. Emerson, Qipeng Fan, Lihong Li, and Yan Xu

Subjects

0301 basic medicine, Cancer Research, medicine.medical_treatment, medicine.disease_cause, Article, cancer stem cell (CSC), 03 medical and health sciences, 0302 clinical medicine, Cancer stem cell, medicine, endothelial growth factor A (VEGFA), RC254-282, Cisplatin, ZIP4, Gene knockdown, Chemistry, Growth factor, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, HDAC4, Vascular endothelial growth factor A, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, high-grade serous ovarian cancer (HGSOC), Cancer research, histone deacetylase 4 (HDAC4), Histone deacetylase, Carcinogenesis, medicine.drug

Abstract

Simple Summary Despite tremendous research efforts, epithelial ovarian cancer (EOC) remains one of the most difficult cancers to detect early and treat successfully for >5-year survival. We have recently shown that ZIP4, a zinc transporter, is a novel cancer stem cell (CSC) marker and a therapeutic target for EOC. The current work focuses on developing new strategies to target ZIP4 and inhibit its CSC activities in EOC. We found that cells expressing high levels of ZIP4 were supersensitive to a group of inhibitors called HDACis. One of the major targets of these inhibitors is a protein called HDAC4. We revealed the new molecular bases for the ZIP4-HDAC4 axis and tested the efficacies of targeting this axis in the lab and in mouse models. Our study provides a new mechanistic-based targeting strategy for EOC. Abstract We have recently identified ZIP4 as a novel cancer stem cell (CSC) marker in high-grade serous ovarian cancer (HGSOC). While it converts drug-resistance to cisplatin (CDDP), we unexpectedly found that ZIP4 induced sensitization of HGSOC cells to histone deacetylase inhibitors (HDACis). Mechanistically, ZIP4 selectively upregulated HDAC IIa HDACs, with little or no effect on HDACs in other classes. HDAC4 knockdown (KD) and LMK-235 inhibited spheroid formation in vitro and tumorigenesis in vivo, with hypoxia inducible factor-1 alpha (HIF1α) and endothelial growth factor A (VEGFA) as functional downstream mediators of HDAC4. Moreover, we found that ZIP4, HDAC4, and HIF1α were involved in regulating secreted VEGFA in HGSOC cells. Furthermore, we tested our hypothesis that co-targeting CSC via the ZIP4-HDAC4 axis and non-CSC using CDDP is necessary and highly effective by comparing the effects of ZIP4-knockout/KD, HDAC4-KD, and HDACis, in the presence or absence of CDDP on tumorigenesis in mouse models. Our results showed that the co-targeting strategy was highly effective. Finally, data from human HGSOC tissues showed that ZIP4 and HDAC4 were upregulated in a subset of recurrent tumors, justifying the clinical relevance of the study. In summary, our study provides a new mechanistic-based targeting strategy for HGSOC.

Published

2021