Your search keyword '"Baniahmad, A"' showing total 27 results

1. LncRNA/miRNA/mRNA Network Introduces Novel Biomarkers in Prostate Cancer

Author

Mohammad Taheri, Arash Safarzadeh, Bashdar Mahmud Hussen, Soudeh Ghafouri-Fard, and Aria Baniahmad

Subjects

prostate cancer, ceRNA, lncRNA, miRNA, regulatory network, Cytology, QH573-671

Abstract

The construction of a competing endogenous RNA (ceRNA) network is an important step in the identification of the role of differentially expressed genes in cancers. In the current research, we used a number of bioinformatics tools to construct the ceRNA network in prostate cancer and identify the importance of these modules in predicting the survival of patients with this type of cancer. An assessment of microarray data of prostate cancer and normal samples using the Limma package led to the identification of differential expressed (DE) RNAs that we stratified into mRNA, lncRNA, and miRNAs, resulting in 684 DEmRNAs, including 437 downregulated DEmRNAs (such as TGM4 and SCGB1A1) and 241 upregulated DEmRNAs (such as TDRD1 and CRISP3); 6 DElncRNAs, including 1 downregulated DElncRNA (H19) and 5 upregulated DElncRNAs (such as PCA3 and PCGEM1); and 59 DEmiRNAs, including 30 downregulated DEmiRNAs (such as hsa-miR-1274a and hsa-miR-1274b) and 29 upregulated DEmiRNAs (such as hsa-miR-1268 and hsa-miR-1207-5p). The ceRNA network contained a total of 5 miRNAs, 5 lncRNAs, and 17 mRNAs. We identified hsa-miR-17, hsa-miR-93, hsa-miR-150, hsa-miR-25, PART1, hsa-miR-125b, PCA3, H19, RND3, and ITGB8 as the 10 hub genes in the ceRNA network. According to the ROC analysis, the expression levels of 19 hub genes showed a high diagnostic value. Taken together, we introduce a number of novel promising diagnostic biomarkers for prostate cancer.

Published

2022

2. A Concise Review on Dysregulation of LINC00665 in Cancers

Author

Soudeh Ghafouri-Fard, Tayyebeh Khoshbakht, Bashdar Mahmud Hussen, Aria Baniahmad, Mohammad Taheri, and Mohammadreza Hajiesmaeili

Subjects

LINC00665, cancer, biomarker, Cytology, QH573-671

Abstract

Long Intergenic Non-Protein Coding RNA 665 (LINC00665) is an RNA gene located on the minus strand of chromosome 19. This lncRNA acts as a competing endogenous RNA for miR-4458, miR-379-5p, miR-551b-5p, miR-3619-5p, miR-424-5p, miR-9-5p, miR-214-3p, miR-126-5p, miR-149-3p, miR-379-5p, miR-665, miR-34a-5p, miR-186-5p, miR-138-5p, miR-181c-5p, miR-98, miR-195-5p, miR-224-5p, miR-3619, miR-708, miR-101, miR-1224-5p, miR-34a-5p, and miR-142-5p. Via influencing expression of these miRNAs, it can enhance expression of a number of oncogenes. Moreover, LINC00665 can influence activity of Wnt/β-Catenin, TGF-β, MAPK1, NF-κB, ERK, and PI3K/AKT signaling. Function of this lncRNA has been assessed through gain-of-function tests and/or loss-of-function studies. Furthermore, diverse research groups have evaluated its expression levels in tissue samples using microarray and RT-qPCR techniques. In this manuscript, we have summarized the results of these studies and categorized them in three sections, i.e., cell line studies, animal studies, and investigations in clinical samples.

Published

2022

3. Androgen-Induced MIG6 Regulates Phosphorylation of Retinoblastoma Protein and AKT to Counteract Non-Genomic AR Signaling in Prostate Cancer Cells

Author

Tim Schomann, Kimia Mirzakhani, Julia Kallenbach, Jing Lu, Seyed Mohammad Mahdi Rasa, Francesco Neri, and Aria Baniahmad

Subjects

prostate cancer, cellular senescence, bipolar androgen therapy, AKT signaling, Microbiology, QR1-502

Abstract

The bipolar androgen therapy (BAT) includes the treatment of prostate cancer (PCa) patients with supraphysiological androgen level (SAL). Interestingly, SAL induces cell senescence in PCa cell lines as well as ex vivo in tumor samples of patients. The SAL-mediated cell senescence was shown to be androgen receptor (AR)-dependent and mediated in part by non-genomic AKT signaling. RNA-seq analyses compared with and without SAL treatment as well as by AKT inhibition (AKTi) revealed a specific transcriptome landscape. Comparing the top 100 genes similarly regulated by SAL in two human PCa cell lines that undergo cell senescence and being counteracted by AKTi revealed 33 commonly regulated genes. One gene, ERBB receptor feedback inhibitor 1 (ERRFI1), encodes the mitogen-inducible gene 6 (MIG6) that is potently upregulated by SAL, whereas the combinatory treatment of SAL with AKTi reverses the SAL-mediated upregulation. Functionally, knockdown of ERRFI1 enhances the pro-survival AKT pathway by enhancing phosphorylation of AKT and the downstream AKT target S6, whereas the phospho-retinoblastoma (pRb) protein levels were decreased. Further, the expression of the cell cycle inhibitor p15INK4b is enhanced by SAL and ERRFI1 knockdown. In line with this, cell senescence is induced by ERRFI1 knockdown and is enhanced slightly further by SAL. Treatment of SAL in the ERRFI1 knockdown background enhances phosphorylation of both AKT and S6 whereas pRb becomes hypophosphorylated. Interestingly, the ERRFI1 knockdown does not reduce AR protein levels or AR target gene expression, suggesting that MIG6 does not interfere with genomic signaling of AR but represses androgen-induced cell senescence and might therefore counteract SAL-induced signaling. The findings indicate that SAL treatment, used in BAT, upregulates MIG6, which inactivates both pRb and the pro-survival AKT signaling. This indicates a novel negative feedback loop integrating genomic and non-genomic AR signaling.

Published

2022

4. Interaction between Non-Coding RNAs and Androgen Receptor with an Especial Focus on Prostate Cancer

Author

Mohammad Taheri, Tayyebeh Khoshbakht, Elena Jamali, Julia Kallenbach, Soudeh Ghafouri-Fard, and Aria Baniahmad

Subjects

androgen receptor, miRNA, lncRNA, circular RNAs, prostate cancer, Cytology, QH573-671

Abstract

The androgen receptor (AR) is a member of the nuclear receptor superfamily and has three functional domains, namely the N-terminal, DNA binding, and C-terminal domain. The N-terminal domain harbors potent transactivation functions, whereas the C-terminal domain binds to androgens and antiandrogens used to treat prostate cancer. AR has genomic activity being DNA binding-dependent or through interaction with other DNA-bound transcription factors, as well as a number of non-genomic, non-canonical functions, such as the activation of the ERK, AKT, and MAPK pathways. A bulk of evidence indicates that non-coding RNAs have functional interactions with AR. This type of interaction is implicated in the pathogenesis of human malignancies, particularly prostate cancer. In the current review, we summarize the available data on the role of microRNAs, long non-coding RNAs, and circular RNAs on the expression of AR and modulation of AR signaling, as well as the effects of AR on their expression. Recognition of the complicated interaction between non-coding RNAs and AR has practical importance in the design of novel treatment options, as well as modulation of response to conventional therapeutics.

Published

2021

5. ING Tumour Suppressors and ING Splice Variants as Coregulators of the Androgen Receptor Signalling in Prostate Cancer

Author

Anna Melekhova and Aria Baniahmad

Subjects

inhibitor of growth family, tumour suppressor type 2, androgen receptor, prostate cancer, corepressor, coactivator, Cytology, QH573-671

Abstract

Prevention and overcoming castration resistance of prostate cancer (PC) remains one of the main unsolved problems in modern oncology. Hence, many studies are focused on the investigation of novel androgen receptor (AR) regulators that could serve as potential drug targets in disease therapy. Among such factors, inhibitor of growth (ING) proteins were identified. Some ING proteins act as AR transcriptional coregulators, indicating their relevance for PC research. The ING family consists of five protein-coding genes from ING1 to ING5 and pseudogene INGX. The ING genes were revealed through their sequence homology to the first identified ING1 from an in vivo screen. ING factors are a part of histone modification complexes. With the help of the conserved plant homeodomain (PHD) motif, ING factors bind to Histone 3 Lysine 4 (H3K4) methylation mark with a stronger affinity to the highest methylation grade H3K4me3 and recruit histone acetyltransferases (HAT) and histone deacetylases (HDAC) to chromatin. ING1 and ING2 are core subunits of mSIN3a-HDAC corepressor complexes, whereas ING3–5 interact with different HAT complexes that serve as coactivators. ING members belong to type II tumour suppressors and are frequently downregulated in many types of malignancies, including PC. As the family name indicates, ING proteins are able to inhibit cell growth and tumour development via regulation of cell cycle and cancer-relevant pathways such as apoptosis, cellular senescence, DNA repair, cell migration, invasion, and angiogenesis. Many ING splice variants that enhance the diversity of ING activity were discovered. However, it seems that the existence of multiple ING splice variants is underestimated, since alternative splice variants, such as the AR coregulators ING1 and ING3, counteract full-length ING and thus play an opposite functional role. These results open a novel prospective investigation direction in understanding ING factors biology in PC and other malignancies.

Published

2021

6. A Novel Splice Variant of the Inhibitor of Growth 3 Lacks the Plant Homeodomain and Regulates Epithelial–Mesenchymal Transition in Prostate Cancer Cells

Author

Anna Melekhova, Mirjam Leeder, Thanakorn Pungsrinont, Tim Schmäche, Julia Kallenbach, Marzieh Ehsani, Kimia Mirzakhani, Seyed Mohammad Mahdi Rasa, Francesco Neri, and Aria Baniahmad

Subjects

prostate cancer, plant homeodomain, inhibitor of growth 3, Microbiology, QR1-502

Abstract

Inhibitor of growth 3 (ING3) is one of five members of the ING tumour suppressor family, characterized by a highly conserved plant homeodomain (PHD) as a reader of the histone mark H3K4me3. ING3 was reported to act as a tumour suppressor in many different cancer types to regulate apoptosis. On the other hand, ING3 levels positively correlate with poor survival prognosis of prostate cancer (PCa) patients. In PCa cells, ING3 acts rather as an androgen receptor (AR) co-activator and harbours oncogenic properties in PCa. Here, we show the identification of a novel ING3 splice variant in both the human PCa cell line LNCaP and in human PCa patient specimen. The novel ING3 splice variant lacks exon 11, ING3∆ex11, which results in deletion of the PHD, providing a unique opportunity to analyse functionally the PHD of ING3 by a natural splice variant. Functionally, overexpression of ING3Δex11 induced morphological changes of LNCaP-derived 3D spheroids with generation of lumen and pore-like structures within spheroids. Since these structures are an indicator of epithelial–mesenchymal transition (EMT), key regulatory factors and markers for EMT were analysed. The data suggest that in contrast to ING3, ING3Δex11 specifically modulates the expression of key EMT-regulating upstream transcription factors and induces the expression of EMT markers, indicating that the PHD of ING3 inhibits EMT. In line with this, ING3 knockdown also induced the expression of EMT markers, confirming the impact of ING3 on EMT regulation. Further, ING3 knockdown induced cellular senescence via a pathway leading to cell cycle arrest, indicating an oncogenic role for ING3 in PCa. Thus, the data suggest that the ING3Δex11 splice variant lacking functional PHD exhibits oncogenic characteristics through triggering EMT in PCa cells.

Published

2021

7. Sex Differences in Diabetes- and TGF-β1-Induced Renal Damage

Author

Nadja Ziller, Roland Kotolloshi, Mohsen Esmaeili, Marita Liebisch, Ralf Mrowka, Aria Baniahmad, Thomas Liehr, Gunter Wolf, and Ivonne Loeffler

Subjects

diabetic nephropathy, diabetes mellitus, kidney, tubulointerstitial fibrosis, sex differences, transforming growth factor beta 1, Cytology, QH573-671

Abstract

While females are less affected by non-diabetic kidney diseases compared to males, available data on sex differences in diabetic nephropathy (DN) are controversial. Although there is evidence for an imbalance of sex hormones in diabetes and hormone-dependent mechanisms in transforming growth factor β1 (TGF-β1) signaling, causes and consequences are still incompletely understood. Here we investigated the influence of sex hormones and sex-specific gene signatures in diabetes- and TGF-β1-induced renal damage using various complementary approaches (a db/db diabetes mouse model, ex vivo experiments on murine renal tissue, and experiments with a proximal tubular cell line TKPTS). Our results show that: (i) diabetes affects sex hormone concentrations and renal expression of their receptors in a sex-specific manner; (ii) sex, sex hormones and diabetic conditions influence differences in expression of TGF-β1, its receptor and bone morphogenetic protein 7 (BMP7); (iii) the sex and sex hormones, in combination with variable TGF-β1 doses, determine the net outcome in TGF-β1-induced expression of connective tissue growth factor (CTGF), a profibrotic cytokine. Altogether, these results suggest complex crosstalk between sex hormones, sex-dependent expression pattern and profibrotic signals for the precise course of DN development. Our data may help to better understand previous contradictory findings regarding sex differences in DN.

Published

2020

8. Kaonic Atoms to Investigate Global Symmetry Breaking

Author

Catalina Curceanu, Carlo Guaraldo, Diana Sirghi, Aidin Amirkhani, Ata Baniahmad, Massimiliano Bazzi, Giovanni Bellotti, Damir Bosnar, Mario Bragadireanu, Michael Cargnelli, Marco Carminati, Alberto Clozza, Luca De Paolis, Raffaele Del Grande, Carlo Fiorini, Mihail Iliescu, Masahiko Iwasaki, Pietro King, Paolo Levi Sandri, Johann Marton, Marco Miliucci, Paweł Moskal, Szymon Niedźwiecki, Shinji Okada, Kristian Piscicchia, Alessandro Scordo, Michał Silarski, Florin Sirghi, Magdalena Skurzok, Antonio Spallone, Marlene Tüchler, Gianlorenzo Utica, Oton Vazquez Doce, and Johann Zmeskal

Subjects

kaonic atoms, sigma terms, low-energy QCD, Mathematics, QA1-939

Abstract

Kaonic atoms measure the antikaon-nucleus interaction at almost zero relative energy, allowing one to determine basic low-energy quantum chromodynamics (QCD) quantities, namely, the antikaon-nucleon ( K ¯ N) scattering lengths. The latter are important for extracting the sigma terms which are built on the symmetry breaking part of the Hamiltonian, thereby providing a measure of chiral and SU(3) symmetries breaking. After discussing the sigma terms and their relations to the kaonic atoms, we describe the most precise measurement in the literature of kaonic hydrogen, performed at LNF-INFN by the SIDDHARTA experiment. Kaonic deuterium is still to be measured, and two experiments are planned. The first, SIDDHARTA-2 at LNF-INFN was installed on DA Φ NE in spring 2019 and will collect data in 2020. The second, E57 at J-PARC, will become operative in 2021.

Published

2020

9. LncRNA/miRNA/mRNA Network Introduces Novel Biomarkers in Prostate Cancer

Author

Taheri, Mohammad, primary, Safarzadeh, Arash, additional, Hussen, Bashdar Mahmud, additional, Ghafouri-Fard, Soudeh, additional, and Baniahmad, Aria, additional

Published

2022

10. A Concise Review on Dysregulation of LINC00665 in Cancers

Author

Ghafouri-Fard, Soudeh, primary, Khoshbakht, Tayyebeh, additional, Hussen, Bashdar Mahmud, additional, Baniahmad, Aria, additional, Taheri, Mohammad, additional, and Hajiesmaeili, Mohammadreza, additional

Published

2022

11. X-ray Detectors for Kaonic Atoms Research at DAΦNE

Author

Catalina Curceanu, Aidin Amirkhani, Ata Baniahmad, Massimiliano Bazzi, Giovanni Bellotti, Carolina Berucci, Damir Bosnar, Mario Bragadireanu, Michael Cargnelli, Alberto Clozza, Raffaele Del Grande, Carlo Fiorini, Francesco Ghio, Carlo Guaraldo, Mihail Iliescu, Masaiko Iwasaki, Paolo Levi Sandri, Johann Marton, Marco Miliucci, Pavel Moskal, Szymon Niedźwiecki, Shinji Okada, Dorel Pietreanu, Kristian Piscicchia, Alessandro Scordo, Hexi Shi, Michal Silarski, Diana Sirghi, Florin Sirghi, Magdalena Skurzok, Antonio Spallone, Hideyuki Tatsuno, Oton Vazquez Doce, Eberhard Widmann, and Johann Zmeskal

Subjects

kaonic atoms, strong interaction, X-ray detectors, Physics, QC1-999

Abstract

This article presents the kaonic atom studies performed at the INFN National Laboratory of Frascati (Laboratori Nazionali di Frascati dell’INFN, LNF-INFN) since the opening of this field of research at the DA Φ NE collider in early 2000. Significant achievements have been obtained by the DA Φ NE Exotic Atom Research (DEAR) and Silicon Drift Detector for Hadronic Atom Research by Timing Applications (SIDDHARTA) experiments on kaonic hydrogen, which have required the development of novel X-ray detectors. The 2019 installation of the new SIDDHARTA-2 experiment to measure kaonic deuterium for the first time has been made possible by further technological advances in X-ray detection.

Published

2019

12. Androgen-Induced MIG6 Regulates Phosphorylation of Retinoblastoma Protein and AKT to Counteract Non-Genomic AR Signaling in Prostate Cancer Cells

Author

Schomann, Tim, primary, Mirzakhani, Kimia, additional, Kallenbach, Julia, additional, Lu, Jing, additional, Rasa, Seyed Mohammad Mahdi, additional, Neri, Francesco, additional, and Baniahmad, Aria, additional

Published

2022

13. Inhibitor of Growth Factors Regulate Cellular Senescence

Author

Ghafouri-Fard, Soudeh, primary, Taheri, Mohammad, additional, and Baniahmad, Aria, additional

Published

2022

14. PITX1 Is a Regulator of TERT Expression in Prostate Cancer with Prognostic Power

Author

Poos, Alexandra M., primary, Schroeder, Cornelia, additional, Jaishankar, Neeraja, additional, Röll, Daniela, additional, Oswald, Marcus, additional, Meiners, Jan, additional, Braun, Delia M., additional, Knotz, Caroline, additional, Frank, Lukas, additional, Gunkel, Manuel, additional, Spilger, Roman, additional, Wollmann, Thomas, additional, Polonski, Adam, additional, Makrypidi-Fraune, Georgia, additional, Fraune, Christoph, additional, Graefen, Markus, additional, Chung, Inn, additional, Stenzel, Alexander, additional, Erfle, Holger, additional, Rohr, Karl, additional, Baniahmad, Aria, additional, Sauter, Guido, additional, Rippe, Karsten, additional, Simon, Ronald, additional, and Koenig, Rainer, additional

Published

2022

15. Role of PI3K-AKT-mTOR Pathway as a Pro-Survival Signaling and Resistance-Mediating Mechanism to Therapy of Prostate Cancer

Author

Pungsrinont, Thanakorn, Kallenbach, Julia, and Baniahmad, Aria

Subjects

Male, PKB/AKT, QH301-705.5, TOR Serine-Threonine Kinases, PTEN Phosphohydrolase, Prostatic Neoplasms, AR antagonist resistance, Antineoplastic Agents, Review, prostate cancer, PI3K, Phosphatidylinositol 3-Kinases, Chemistry, Drug Resistance, Neoplasm, Receptors, Androgen, androgen receptor, mTOR, Humans, Molecular Targeted Therapy, castration-resistance, Biology (General), Proto-Oncogene Proteins c-akt, QD1-999, Phosphoinositide-3 Kinase Inhibitors, Signal Transduction

Abstract

Androgen deprivation therapy (ADT) and androgen receptor (AR)-targeted therapy are the gold standard options for treating prostate cancer (PCa). These are initially effective, as localized and the early stage of metastatic disease are androgen- and castration-sensitive. The tumor strongly relies on systemic/circulating androgens for activating AR signaling to stimulate growth and progression. However, after a certain point, the tumor will eventually develop a resistant stage, where ADT and AR antagonists are no longer effective. Mechanistically, it seems that the tumor becomes more aggressive through adaptive responses, relies more on alternative activated pathways, and is less dependent on AR signaling. This includes hyperactivation of PI3K-AKT-mTOR pathway, which is a central signal that regulates cell pro-survival/anti-apoptotic pathways, thus, compensating the blockade of AR signaling. The PI3K-AKT-mTOR pathway is well-documented for its crosstalk between genomic and non-genomic AR signaling, as well as other signaling cascades. Such a reciprocal feedback loop makes it more complicated to target individual factor/signaling for treating PCa. Here, we highlight the role of PI3K-AKT-mTOR signaling as a resistance mechanism for PCa therapy and illustrate the transition of prostate tumor from AR signaling-dependent to PI3K-AKT-mTOR pathway-dependent. Moreover, therapeutic strategies with inhibitors targeting the PI3K-AKT-mTOR signal used in clinic and ongoing clinical trials are discussed.

Published

2021

16. A Novel Splice Variant of the Inhibitor of Growth 3 Lacks the Plant Homeodomain and Regulates Epithelial–Mesenchymal Transition in Prostate Cancer Cells

Author

Melekhova, A., Leeder, M., Pungsrinont, T., Schmache, T., Kallenbach, J., Ehsani, M., Mirzakhani, K., Rasa, S. M. M., Neri, F., and Baniahmad, A.

Subjects

Cyclin-Dependent Kinase Inhibitor p21, Male, Epithelial-Mesenchymal Transition, inhibitor of growth 3, RNA Splicing, Small Interfering, Microbiology, Article, Cell Line, Histones, Cell Line, Tumor, Spheroids, Cellular, Humans, plant homeodomain, RNA, Small Interfering, Cyclin-Dependent Kinase Inhibitor p16, Cell Proliferation, Homeodomain Proteins, Neoplastic, Tumor, Tumor Suppressor Proteins, Twist-Related Protein 1, Prostatic Neoplasms, Zinc Finger E-box-Binding Homeobox 1, Inhibitor of growth 3, Plant homeodomain, Prostate cancer, Signal Transduction, Snail Family Transcription Factors, TATA-Box Binding Protein, Gene Expression Regulation, Neoplastic, prostate cancer, QR1-502, Gene Expression Regulation, embryonic structures, RNA, Cellular, Spheroids

Abstract

Inhibitor of growth 3 (ING3) is one of five members of the ING tumour suppressor family, characterized by a highly conserved plant homeodomain (PHD) as a reader of the histone mark H3K4me3. ING3 was reported to act as a tumour suppressor in many different cancer types to regulate apoptosis. On the other hand, ING3 levels positively correlate with poor survival prognosis of prostate cancer (PCa) patients. In PCa cells, ING3 acts rather as an androgen receptor (AR) co-activator and harbours oncogenic properties in PCa. Here, we show the identification of a novel ING3 splice variant in both the human PCa cell line LNCaP and in human PCa patient specimen. The novel ING3 splice variant lacks exon 11, ING3∆ex11, which results in deletion of the PHD, providing a unique opportunity to analyse functionally the PHD of ING3 by a natural splice variant. Functionally, overexpression of ING3Δex11 induced morphological changes of LNCaP-derived 3D spheroids with generation of lumen and pore-like structures within spheroids. Since these structures are an indicator of epithelial-mesenchymal transition (EMT), key regulatory factors and markers for EMT were analysed. The data suggest that in contrast to ING3, ING3Δex11 specifically modulates the expression of key EMT-regulating upstream transcription factors and induces the expression of EMT markers, indicating that the PHD of ING3 inhibits EMT. In line with this, ING3 knockdown also induced the expression of EMT markers, confirming the impact of ING3 on EMT regulation. Further, ING3 knockdown induced cellular senescence via a pathway leading to cell cycle arrest, indicating an oncogenic role for ING3 in PCa. Thus, the data suggest that the ING3Δex11 splice variant lacking functional PHD exhibits oncogenic characteristics through triggering EMT in PCa cells.

Published

2021

17. Interaction between Non-Coding RNAs and Androgen Receptor with an Especial Focus on Prostate Cancer

Author

Taheri, Mohammad, primary, Khoshbakht, Tayyebeh, additional, Jamali, Elena, additional, Kallenbach, Julia, additional, Ghafouri-Fard, Soudeh, additional, and Baniahmad, Aria, additional

Published

2021

18. ING Tumour Suppressors and ING Splice Variants as Coregulators of the Androgen Receptor Signalling in Prostate Cancer

Author

Melekhova, Anna, primary and Baniahmad, Aria, additional

Published

2021

19. Androgen Receptor-Dependent Mechanisms Mediating Drug Resistance in Prostate Cancer

Author

Marzieh, Ehsani, Faith Oluwakemi, David, and Aria, Baniahmad

Subjects

castration resistant PCa, androgen receptor, Review, androgen deprivation therapy, AR antagonists, urologic and male genital diseases, prostate cancer, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, lcsh:RC254-282

Abstract

Simple Summary Prostate cancer can develop under hormone treatment and chemotherapy from a castration-sensitive towards a castration-resistant into a drug resistant-tumor. The main hormonal drug target is the androgen receptor (AR). Androgen deprivation therapy reduces body-own androgen production and AR antagonists inhibit androgen-mediated activation of AR. Here, molecular mechanisms are described that review knowledge about tumor cells escape therapy by developing bypass mechanisms of AR-signaling. This includes genomic and non-genomic signaling. Deciphering the involved molecules that mediate castration and drug resistance will provide the basis of potential novel drug targets that may be used in addition to AR inhibition as combinatory treatment. Abstract Androgen receptor (AR) is a main driver of prostate cancer (PCa) growth and progression as well as the key drug target. Appropriate PCa treatments differ depending on the stage of cancer at diagnosis. Although androgen deprivation therapy (ADT) of PCa is initially effective, eventually tumors develop resistance to the drug within 2–3 years of treatment onset leading to castration resistant PCa (CRPC). Castration resistance is usually mediated by reactivation of AR signaling. Eventually, PCa develops additional resistance towards treatment with AR antagonists that occur regularly, also mostly due to bypass mechanisms that activate AR signaling. This tumor evolution with selection upon therapy is presumably based on a high degree of tumor heterogenicity and plasticity that allows PCa cells to proliferate and develop adaptive signaling to the treatment and evolve pathways in therapy resistance, including resistance to chemotherapy. The therapy-resistant PCa phenotype is associated with more aggressiveness and increased metastatic ability. By far, drug resistance remains a major cause of PCa treatment failure and lethality. In this review, various acquired and intrinsic mechanisms that are AR‑dependent and contribute to PCa drug resistance will be discussed.

Published

2021

20. Antithetic hTERT Regulation by Androgens in Prostate Cancer Cells: hTERT Inhibition Is Mediated by the ING1 and ING2 Tumor Suppressors

Author

Bartsch, Sophie, primary, Mirzakhani, Kimia, additional, Neubert, Laura, additional, Stenzel, Alexander, additional, Ehsani, Marzieh, additional, Esmaeili, Mohsen, additional, Pungsrinont, Thanakorn, additional, Kacal, Merve, additional, Rasa, Seyed Mohammad Mahdi, additional, Kallenbach, Julia, additional, Damodaran, Divya, additional, Ribaudo, Federico, additional, Grimm, Marc-Oliver, additional, Neri, Francesco, additional, and Baniahmad, Aria, additional

Published

2021

21. Androgen Receptor-Dependent Mechanisms Mediating Drug Resistance in Prostate Cancer

Author

Ehsani, Marzieh, primary, David, Faith Oluwakemi, additional, and Baniahmad, Aria, additional

Published

2021

22. Sex Differences in Diabetes- and TGF-β1-Induced Renal Damage

Author

Ziller, Nadja, primary, Kotolloshi, Roland, additional, Esmaeili, Mohsen, additional, Liebisch, Marita, additional, Mrowka, Ralf, additional, Baniahmad, Aria, additional, Liehr, Thomas, additional, Wolf, Gunter, additional, and Loeffler, Ivonne, additional

Published

2020

23. Mechanisms of Androgen Receptor Agonist- and Antagonist-Mediated Cellular Senescence in Prostate Cancer

Author

Kokal, Miriam, primary, Mirzakhani, Kimia, additional, Pungsrinont, Thanakorn, additional, and Baniahmad, Aria, additional

Published

2020

24. Kaonic Atoms to Investigate Global Symmetry Breaking

Author

Curceanu, Catalina, primary, Guaraldo, Carlo, additional, Sirghi, Diana, additional, Amirkhani, Aidin, additional, Baniahmad, Ata, additional, Bazzi, Massimiliano, additional, Bellotti, Giovanni, additional, Bosnar, Damir, additional, Bragadireanu, Mario, additional, Cargnelli, Michael, additional, Carminati, Marco, additional, Clozza, Alberto, additional, De Paolis, Luca, additional, Del Grande, Raffaele, additional, Fiorini, Carlo, additional, Iliescu, Mihail, additional, Iwasaki, Masahiko, additional, King, Pietro, additional, Levi Sandri, Paolo, additional, Marton, Johann, additional, Miliucci, Marco, additional, Moskal, Paweł, additional, Niedźwiecki, Szymon, additional, Okada, Shinji, additional, Piscicchia, Kristian, additional, Scordo, Alessandro, additional, Silarski, Michał, additional, Sirghi, Florin, additional, Skurzok, Magdalena, additional, Spallone, Antonio, additional, Tüchler, Marlene, additional, Utica, Gianlorenzo, additional, Vazquez Doce, Oton, additional, and Zmeskal, Johann, additional

Published

2020

25. Mechanisms of Androgen Receptor Agonist- and Antagonist-Mediated Cellular Senescence in Prostate Cancer

Author

Aria Baniahmad, Kimia Mirzakhani, Miriam Kokal, and Thanakorn Pungsrinont

Subjects

0301 basic medicine, Agonist, Senescence, Cancer Research, medicine.drug_class, Review, urologic and male genital diseases, bipolar androgen therapy, lcsh:RC254-282, 03 medical and health sciences, Prostate cancer, 0302 clinical medicine, androgen receptor antagonist, medicine, cellular senescence, PKB/Akt, Chemistry, prostate cancer, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Androgen, medicine.disease, supraphysiological androgen levels, Androgen receptor, 030104 developmental biology, Oncology, Androgen Therapy, 030220 oncology & carcinogenesis, Cancer cell, Cancer research, antiandrogen, Tyrosine kinase, Src

Abstract

The androgen receptor (AR) plays a leading role in the control of prostate cancer (PCa) growth. Interestingly, structurally different AR antagonists with distinct mechanisms of antagonism induce cell senescence, a mechanism that inhibits cell cycle progression, and thus seems to be a key cellular response for the treatment of PCa. Surprisingly, while physiological levels of androgens promote growth, supraphysiological androgen levels (SAL) inhibit PCa growth in an AR-dependent manner by inducing cell senescence in cancer cells. Thus, oppositional acting ligands, AR antagonists, and agonists are able to induce cellular senescence in PCa cells, as shown in cell culture model as well as ex vivo in patient tumor samples. This suggests a dual AR-signaling dependent on androgen levels that leads to the paradox of the rational to keep the AR constantly inactivated in order to treat PCa. These observations however opened the option to treat PCa patients with AR antagonists and/or with androgens at supraphysiological levels. The latter is currently used in clinical trials in so-called bipolar androgen therapy (BAT). Notably, cellular senescence is induced by AR antagonists or agonist in both androgen-dependent and castration-resistant PCa (CRPC). Pathway analysis suggests a crosstalk between AR and the non-receptor tyrosine kinase Src-Akt/PKB and the PI3K-mTOR-autophagy signaling in mediating AR-induced cellular senescence in PCa. In this review, we summarize the current knowledge of therapeutic induction and intracellular pathways of AR-mediated cellular senescence.

Published

2020

26. X-ray Detectors for Kaonic Atoms Research at DAΦNE

Author

Curceanu, Catalina, primary, Amirkhani, Aidin, additional, Baniahmad, Ata, additional, Bazzi, Massimiliano, additional, Bellotti, Giovanni, additional, Berucci, Carolina, additional, Bosnar, Damir, additional, Bragadireanu, Mario, additional, Cargnelli, Michael, additional, Clozza, Alberto, additional, Del Grande, Raffaele, additional, Fiorini, Carlo, additional, Ghio, Francesco, additional, Guaraldo, Carlo, additional, Iliescu, Mihail, additional, Iwasaki, Masaiko, additional, Levi Sandri, Paolo, additional, Marton, Johann, additional, Miliucci, Marco, additional, Moskal, Pavel, additional, Niedźwiecki, Szymon, additional, Okada, Shinji, additional, Pietreanu, Dorel, additional, Piscicchia, Kristian, additional, Scordo, Alessandro, additional, Shi, Hexi, additional, Silarski, Michal, additional, Sirghi, Diana, additional, Sirghi, Florin, additional, Skurzok, Magdalena, additional, Spallone, Antonio, additional, Tatsuno, Hideyuki, additional, Vazquez Doce, Oton, additional, Widmann, Eberhard, additional, and Zmeskal, Johann, additional

Published

2019

27. X-ray Detectors for Kaonic Atoms Research at DAΦNE

Author

Shinji Okada, Hexi Shi, A. Baniahmad, Florin Sirghi, Catalina Curceanu, G. Bellotti, Carolina Berucci, Paolo Levi Sandri, Szymon Niedźwiecki, Raffaele Del Grande, Johann Zmeskal, M. Iliescu, Dorel Pietreanu, Alberto Clozza, M. Iwasaki, Marco Miliucci, A. Spallone, Johann Marton, C. Guaraldo, Pavel Moskal, A. Amirkhani, H. Tatsuno, Carlo Fiorini, Oton Vazquez Doce, Mario Bragadireanu, Kristian Piscicchia, Eberhard Widmann, Michał Silarski, Magdalena Skurzok, Massimiliano Bazzi, F. Ghio, Alessandro Scordo, Michael Cargnelli, Damir Bosnar, and Diana Sirghi

Subjects

Silicon drift detector, Kaonic hydrogen, Hadron, X-ray detector, kaonic atoms, strong interaction, X-ray detectors, 01 natural sciences, law.invention, Nuclear physics, law, 0103 physical sciences, Atom, 010306 general physics, Collider, Exotic atom, Physics, 010308 nuclear & particles physics, Condensed Matter Physics, lcsh:QC1-999, NATURAL SCIENCES. Physics, Electronic, Optical and Magnetic Materials, PRIRODNE ZNANOSTI. Fizika, Deuterium, lcsh:Physics

Abstract

This article presents the kaonic atom studies performed at the INFN National Laboratory of Frascati (Laboratori Nazionali di Frascati dell&rsquo, INFN, LNF-INFN) since the opening of this field of research at the DA &Phi, NE collider in early 2000. Significant achievements have been obtained by the DA &Phi, NE Exotic Atom Research (DEAR) and Silicon Drift Detector for Hadronic Atom Research by Timing Applications (SIDDHARTA) experiments on kaonic hydrogen, which have required the development of novel X-ray detectors. The 2019 installation of the new SIDDHARTA-2 experiment to measure kaonic deuterium for the first time has been made possible by further technological advances in X-ray detection.

Published

2019