Your search keyword '"Evangelia A. Papakonstanti"' showing total 39 results

1. A combined opposite targeting of p110δ PI3K and RhoA abrogates skin cancer

Author

Niki Tzenaki, Lydia Xenou, Evangelia Goulielmaki, Anna Tsapara, Irene Voudouri, Angelika Antoniou, George Valianatos, Maria Tzardi, Eelco De Bree, Aikaterini Berdiaki, Antonios Makrigiannakis, and Evangelia A. Papakonstanti

Subjects

Biology (General), QH301-705.5

Abstract

Abstract Malignant melanoma is the most aggressive and deadly skin cancer with an increasing incidence worldwide whereas SCC is the second most common non-melanoma human skin cancer with limited treatment options. Here we show that the development and metastasis of melanoma and SCC cancers can be blocked by a combined opposite targeting of RhoA and p110δ PI3K. We found that a targeted induction of RhoA activity into tumours by deletion of p190RhoGAP-a potent inhibitor of RhoA GTPase-in tumour cells together with adoptive macrophages transfer from δD910A/D910A mice in mice bearing tumours with active RhoA abrogated growth progression of melanoma and SCC tumours. Τhe efficacy of this combined treatment is the same in tumours lacking activating mutations in BRAF and in tumours harbouring the most frequent BRAF(V600E) mutation. Furthermore, the efficiency of this combined treatment is associated with decreased ATX expression in tumour cells and tumour stroma bypassing a positive feedback expression of ATX induced by direct ATX pharmacological inactivation. Together, our findings highlight the importance of targeting cancer cells and macrophages for skin cancer therapy, emerge a reverse link between ATX and RhoA and illustrate the benefit of p110δ PI3K inhibition as a combinatorial regimen for the treatment of skin cancers.

Published

2024

2. Focus on PTEN regulation

Author

Miriam eBermudez-Brito, Evangelia eGoulielmaki, and Evangelia A Papakonstanti

Subjects

localization, transcription, Pten, protein interactions, translation, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

The role of PTEN as a tumour suppressor has been for a long time attributed to its lipid phosphatase activity against PI(3,4,5)P3, the phospholipid product of the class I PI3Ks. Besides its traditional role as a lipid phosphatase at the plasma membrane, a wealth of data has shown that PTEN can function independently of its phosphatase activity and that PTEN also exists and plays a role in the nucleus, in cytoplasmic organelles and extracellularly. Accumulating evidence has shed light on diverse physiological functions of PTEN which are accompanied by a complex regulation of its expression and activity. PTEN levels and function are regulated transcriptionally, post-transcriptionally and post-translationally. PTEN is also sensitive to regulation by its interacting proteins and its localization. Herein, we summarize the current knowledge on mechanisms that regulate the expression and enzymatic activity of PTEN and its role in human diseases.

Published

2015

3. Galectin-1 overexpression in endometriosis and its regulation by neuropeptides (CRH, UCN) indicating its important role in reproduction and inflammation.

Author

Aikaterini Vergetaki, Udo Jeschke, Thomas Vrekoussis, Eirini Taliouri, Luca Sabatini, Evangelia A Papakonstanti, and Antonis Makrigiannakis

Subjects

Medicine, Science

Abstract

Endometriosis is an inflammatory disease of women of reproductive age featured by the presence of ectopic endometrium and is strongly related to infertility. Galectins, carbonhydrate-binding proteins, have been found to have pro- or anti-inflammatory roles in the reproductive tract and in pathological conditions concerning infertility. Galectin-1, which is expressed at endometrium and decidua, plays a major role in implantation and trophoblast invasion. Also, the neuropeptides, corticotropin releasing hormone (CRH) and urocortin (UCN) and their receptors are expressed in eutopic and ectopic endometrium showing a differential expression pattern in endometriotic women compared to healthy ones. The aim of this study was to examine the galectin-1 expression in endometriotic lesions and compare its expression in eutopic endometrium of endometriotic and healthy women. Furthermore, we examined the effect of CRH and UCN in galectin-1 expression in Ishikawa cell line and macrophages and investigated the implication of CRHR1 in these responses. Eutopic and ectopic endometrium specimens, Ishikawa cell line and mice macrophages were used. Immunohistochemistry and western blot analysis were performed in order to identify galectin-1 expression in ectopic and eutopic endometrium of women with and without endometriosis and the regulatory effect of CRH and UCN on galectin-1 expression. This study presents for the first time that galectin-1 is overexpressed in endometriotic lesions compared to eutopic endometrium of endometriotic women and is more abundantly expressed in eutopic endometrium of disease women compared to healthy ones. Furthermore, it is shown that CRH and UCN upregulate galectin-1 expression in Ishikawa cell line and macrophages and this effect is mediated through CRHR1. These results suggest that galectin-1 might play an important role in endometriosis pathology and infertility profile of women suffering from endometriosis by being at the same time regulated by CRH and UCN interfering in the immune disequilibrium which characterizes this pathological condition.

Published

2014

4. p110d PI3 kinase pathway: emerging roles in cancer

Author

Niki eTzenaki and Evangelia A Papakonstanti

Subjects

Cancer, Pten, solid tumors, p110d PI3K, hematologic malignancies, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Class IA PI3Ks consists of three isoforms of the p110 catalytic subunit designated p110a, p110b and p110d which are encoded by three separate genes. Gain-of-function mutations on PIK3CA gene encoding for p110a isoform have been detected in a wide variety of human cancers whereas no somatic mutations of genes encoding for p110b or p110d have been reported. Unlike p110a and p110b which are ubiquitously expressed, p110d is highly enriched in leukocytes and thus the p110d PI3K pathway has attracted more attention for its involvement in immune disorders. However, findings have been accumulated showing that the p110d PI3K plays a seminal role in the development and progression of some hematologic malignancies. A wealth of knowledge has come from studies showing the central role of p110d PI3K in B-cell functions and B-cell malignancies. Further data have documented that wild-type p110d becomes oncogenic when overexpressed in cell culture models and that p110d is the predominant isoform expressed in some human solid tumor cells playing a prominent role in these cells. Genetic inactivation of p110d in mice models and highly-selective inhibitors of p110d have demonstrated an important role of this isoform in differentiation, growth, survival, motility and morphology with the inositol phosphatase PTEN to play a critical role in p110d signaling. In this review, we summarize our understanding of the p110d PI3K signaling pathway in hematopoietic cells and malignancies, we highlight the evidence showing the oncogenic potential of p110d in cells of non-hematopoietic origin and we discuss perspectives for potential novel roles of p110d PI3K in cancer.

Published

2013

5. Differential expression of CRH, UCN, CRHR1 and CRHR2 in eutopic and ectopic endometrium of women with endometriosis.

Author

Aikaterini Vergetaki, Udo Jeschke, Thomas Vrekoussis, Eirini Taliouri, Luca Sabatini, Evangelia A Papakonstanti, and Antonis Makrigiannakis

Subjects

Medicine, Science

Abstract

Endometriosis is considered as a benign aseptic inflammatory disease, characterised by the presence of ectopic endometrium-like tissue. Its symptoms (mostly pain and infertility) are reported as constant stressors. Corticotropin releasing hormone (CRH) and urocortin (UCN) are neuropeptides, strongly related to stress and inflammation. The effects of CRH and UCN are mediated through CRHR1 and CRHR2 receptors which are implicated in several reproductive functions acting as inflammatory components. However, the involvement of these molecules to endometriosis remains unknown. The aim of this study was to examine the expression of CRHR1 and CRHR2 in endometriotic sites and to compare the expression of CRHR1 and CRHR2 in eutopic endometrium of endometriotic women to that of healthy women. We further compared the expression of CRH, UCN, CRHR1 and CRHR2 in ectopic endometrium to that in eutopic endometrium of women with endometriosis. Endometrial biopsy specimens were taken from healthy women (10 patients) and endometrial and endometriotic biopsy specimens were taken from women with endometriosis (16 patients). Τhe expression of CRH, UCN, CRHR1, and CRHR2 was tested via RT-PCR, immunohistochemistry and Western blotting. This study shows for the first time that CRH and UCN receptor subtypes CRHR1β and CRHR2α are expressed in endometriotic sites and that they are more strongly expressed (p

Published

2013

6. p110δ PI3K as a therapeutic target of solid tumours

Author

Evangelia A. Papakonstanti and Lydia Xenou

Subjects

0301 basic medicine, medicine.medical_treatment, P110α, 03 medical and health sciences, 0302 clinical medicine, Cancer immunotherapy, Neoplasms, medicine, Carcinoma, Tumor Microenvironment, Animals, Humans, Molecular Targeted Therapy, business.industry, Cancer, General Medicine, medicine.disease, Class Ia Phosphatidylinositol 3-Kinase, 030104 developmental biology, Drug development, P110δ, 030220 oncology & carcinogenesis, Cancer cell, Cancer research, Liver cancer, business, Signal Transduction

Abstract

From the time of first characterization of PI3K as a heterodimer made up of a p110 catalytic subunit and a regulatory subunit, a wealth of evidence have placed the class IA PI3Ks at the forefront of drug development for the treatment of various diseases including cancer. The p110α isoform was quickly brought at the centre of attention in the field of cancer research by the discovery of cancer-specific gain-of-function mutations in PIK3CA gene in a range of human solid tumours. In contrast, p110δ PI3K was placed into the spotlight of immunity, inflammation and haematologic malignancies because of the preferential expression of this isoform in leucocytes and the rare mutations in PIK3CD gene. The last decade, however, several studies have provided evidence showing that the correlation between the PIK3CA mutations and the response to PI3K inhibition is less clear than originally considered, whereas concurrently an unexpected role of p110δ PI3K in solid tumours has being emerging. While PIK3CD is mostly non-mutated in cancer, the expression levels of p110δ protein seem to act as an intrinsic cancer-causing driver in various solid tumours including breast, prostate, colorectal and liver cancer, Merkel-Cell carcinoma, glioblastoma and neurobalstoma. Furthermore, p110δ selective inhibitors are being studied as potential single agent treatments or as combination partners in attempt to improve cancer immunotherapy, with both strategies to shown great promise for the treatment of several solid tumours. In this review, we discuss the evidence implicating the p110δ PI3K in human solid tumours, their impact on the current state of the field and the potential of using p110δ-selective inhibitors as monotherapy or combined therapy in different cancer contexts.

Published

2019

7. Control of axonal growth and regeneration of sensory neurons by the p110delta PI 3-kinase.

Author

Britta J Eickholt, Aminul I Ahmed, Meirion Davies, Evangelia A Papakonstanti, Wayne Pearce, Michelle L Starkey, Antonio Bilancio, Anna C Need, Andrew J H Smith, Susan M Hall, Frank P Hamers, Karl P Giese, Elizabeth J Bradbury, and Bart Vanhaesebroeck

Subjects

Medicine, Science

Abstract

The expression and function of the 8 distinct catalytic isoforms of PI 3-kinase (PI3K) in the nervous system are unknown. Whereas most PI3Ks have a broad tissue distribution, the tyrosine kinase-linked p110delta isoform has previously been shown to be enriched in leukocytes. Here we report that p110delta is also highly expressed in the nervous system. Inactivation of p110delta in mice did not affect gross neuronal development but led to an increased vulnerability of dorsal root ganglia neurons to exhibit growth cone collapse and decreases in axonal extension. Loss of p110delta activity also dampened axonal regeneration following peripheral nerve injury in adult mice and impaired functional recovery of locomotion. p110delta inactivation resulted in reduced neuronal signaling through the Akt protein kinase, and increased activity of the small GTPase RhoA. Pharmacological inhibition of ROCK, a downstream effector of RhoA, restored axonal extension defects in neurons with inactive p110delta, suggesting a key role of RhoA in p110delta signaling in neurons. Our data identify p110delta as an important signaling component for efficient axonal elongation in the developing and regenerating nervous system.

Published

2007

8. Pharmacological inactivation of the PI3K p110δ prevents breast tumour progression by targeting cancer cells and macrophages

Author

Niki Tzenaki, Margarita Andreou, Eelco de Bree, Antonis Makrigiannakis, Miriam Bermudez-Brito, Evangelia Goulielmaki, Maria Tzardi, Evangelia A. Papakonstanti, and Eleftheria Tsentelierou

Subjects

0301 basic medicine, Cancer Research, Adoptive cell transfer, Cell Survival, Immunology, Apoptosis, Breast Neoplasms, Article, Metastasis, 03 medical and health sciences, Cellular and Molecular Neuroscience, Breast cancer, Cell Line, Tumor, Animals, Humans, Medicine, Macrophage, lcsh:QH573-671, Neoplasm Metastasis, PI3K/AKT/mTOR pathway, Cell Proliferation, Neoplasm Staging, Mice, Inbred BALB C, lcsh:Cytology, business.industry, Adenine, Macrophages, PTEN Phosphohydrolase, Cancer, Cell Biology, medicine.disease, Class Ia Phosphatidylinositol 3-Kinase, Enzyme Activation, 030104 developmental biology, Cancer cell, Disease Progression, Quinazolines, Cancer research, Female, business

Abstract

Patient selection for PI3K-targeted solid cancer treatment was based on the PIK3CA/PTEN mutational status. However, it is increasingly clear that this is not a good predictor of the response of breast cancer cells to the anti-proliferative effect of PI3K inhibitors, indicating that isoform(s) other than p110α may modulate cancer cells sensitivity to PI3K inhibition. Surprisingly, we found that although no mutations in the p110δ subunit have been detected thus far in breast cancer, the expression of p110δ becomes gradually elevated during human breast cancer progression from grade I to grade III. Moreover, pharmacological inactivation of p110δ in mice abrogated the formation of tumours and the recruitment of macrophages to tumour sites and strongly affected the survival, proliferation and apoptosis of grafted tumour cells. Pharmacological inactivation of p110δ in mice with defective macrophages or in mice with normal macrophages but grafted with p110δ-lacking tumours suppressed only partly tumour growth, indicating a requisite role of p110δ in both macrophages and cancer cells in tumour progression. Adoptive transfer of δD910A/D910A macrophages into mice with defected macrophages suppressed tumour growth, eliminated the recruitment of macrophages to tumour sites and prevented metastasis compared with mice that received WT macrophages further establishing that inactivation of p110δ in macrophage prevents tumour progression. Our work provides the first in vivo evidence for a critical role of p110δ in cancer cells and macrophages during solid tumour growth and may pave the way for the use of p110δ inhibitors in breast cancer treatment.

Published

2018

9. Preclinical development of a novel, highly selective PI3Kδ inhibitor, IOA-244, for the treatment of solid malignancies

Author

Amy R. MacQueen, Michael Lahn, Anna Tsapara, L. Van der Veen, Pritom Shah, Evangelia A. Papakonstanti, and Zoë Johnson

Subjects

business.industry, Melanoma, T cell, Cancer, Hematology, medicine.disease, Immune tolerance, Immune system, medicine.anatomical_structure, Oncology, In vivo, Cancer research, medicine, Myeloid-derived Suppressor Cell, business, CD8

Abstract

Background Inhibiting PI3Kδ preferentially targets regulatory T cells and myeloid derived suppressor cells, breaking tumour-induced immune tolerance and restoring anti-tumour immunity. Bioinformatics and protein expression studies have shown that PIK3CD / PI3Kδ is highly expressed in certain solid malignancies, and therefore inhibition of PI3Kδ may modulate tumour growth and development via intrinsic as well as immune driven effects. Methods In vitro proliferation of primary human T cells demonstrated the selective effects of PI3Kδ inhibition on Treg cells. In vivo immune mediated effects of IOA-244 were tested using the CT26 mouse model. High PI3Kδ expressing MDA-MB-231 breast cancer cells, as well as a patient derived melanoma model with high PIK3CD profile were tested in T cell deficient hosts. Results IOA-244 is a novel, highly selective PI3Kδ inhibitor, with the unique property of being ATP non-competitive. IOA-244 showed a selective and concentration-dependent suppression of human Treg cell proliferation whilst leaving CD8+ T cell proliferation intact. In mouse models with a full immune system, IOA-244 inhibited tumour growth when combined with either anti-PD-1 or anti-PD-L1. Furthermore, the composition of the tumour infiltrating lymphocytes showed a marked decrease in the suppressor cell populations, i.e. Tregs and MDSCs. In nude mice we demonstrated that IOA-244 can effectively inhibit the growth of PI3Kδ-expressing breast cancer cells as a monotherapy. To support the clinical development of IOA-244 we demonstrate that patient derived melanoma cells with a high expression of PIK3CD are susceptible to treatment with IOA-244 in a mouse patient-derived xenograft model. Conclusions Solid tumours with a high Treg:CD8 ratio and / or a high protein expression of PI3Kδ may be amenable to treatment with IOA-244. Based on these and other supporting data, IOA-244 has received clinical trial approval in two European countries and phase I clinical testing is expected to start by the end of 2020. Legal entity responsible for the study iOnctura SA. Funding iOnctura SA. Disclosure Z. Johnson: Leadership role: iOnctura SA. L. Van der Veen: Leadership role: iOnctura SA. M. Lahn: Leadership role: iOnctura SA. All other authors have declared no conflicts of interest.

Published

2019

10. Abstract 2692: Preclinical development of a novel, highly selective PI3Kδ inhibitor, IOA-244, for the treatment of solid malignancies

Author

Michael Lahn, Lars van der Veen, Katherine Ewings, Pritom Shah, Anna Tsapara, Zoë Johnson, Evangelia A. Papakonstanti, and Amy R. MacQueen

Subjects

0301 basic medicine, Cancer Research, Chemistry, T cell, Immune tolerance, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, medicine.anatomical_structure, Immune system, Oncology, In vivo, 030220 oncology & carcinogenesis, medicine, Myeloid-derived Suppressor Cell, Cancer research, Cytotoxic T cell, CD8, B cell

Abstract

The Class I Phosphatidylinositol-4,5-bisphosphate 3-kinase (PI3K) family is an attractive target class for the treatment of hematological and solid malignancies. In addition to the direct effects of PI3Kδ inhibition on B cell malignancies, inhibiting PI3Kδ preferentially targets regulatory T cells and myeloid derived suppressor cells, thus breaking tumor-induced immune tolerance and restoring anti-tumor immunity. To date, the development of selective inhibitors of the Class I PI3K family has been hampered by the lack of isoform specificity as well as safety issues. IOA-244 is a novel, highly selective, orally bioavailable PI3Kδ inhibitor, with the unique property of being ATP non-competitive; these characteristics make IOA-244 the ideal drug to explore the hypothesis that PI3Kδ inhibition can modulate anti-tumor immunity as a monotherapy and in combination in clinical trials. In mouse models, IOA-244 inhibited tumor growth when combined with either anti-PD-1 or anti-PD-L1. In the CT26 model the composition of the tumour infiltrating lymphocytes showed a marked decrease in the suppressor cell populations, i.e. Tregs and MDSCs, as well as tumor associated macrophages (TAMs). Conversely a concomitant increase in natural killer cells as well as the ratio of cytotoxic CD8+ T cells: Treg cells was observed. Furthermore, in vitro studies using primary human T cells demonstrated a selective and concentration-dependent suppression of Treg cells by IOA-244 whilst leaving CD8+ T cell proliferation intact. In addition to effects on the immune system, we are exploring the potential of IOA-244 to mediate direct anti-cancer effects on solid tumors with a high expression of PIK3CD. IOA-244 induced a concentration-dependent inhibition of p-AKT in MDA-MB-231 cells. Furthermore, we demonstrate strong anti-proliferative activity by IOA-244 on hepatocellular tumor lines in vitro. Activity in these and other cell and patient derived lines is being studied, both in xenograft in vivo studies and in vitro models. Based on GLP toxicology studies, IOA-244 has the potential to be a best-in-class PI3Kδ inhibitor with a safety and pharmacokinetic profile that is amenable for use alone and in combination with immunotherapies for the treatment of solid malignancies. IOA-244 is poised to enter phase I clinical testing in selected cancer indications in the first half of 2019. Citation Format: Katherine Ewings, Amy MacQueen, Pritom Shah, Anna Tsapara, Evangelia Papakonstanti, Lars van der Veen, Michael Lahn, Zoe Johnson. Preclinical development of a novel, highly selective PI3Kδ inhibitor, IOA-244, for the treatment of solid malignancies [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2019; 2019 Mar 29-Apr 3; Atlanta, GA. Philadelphia (PA): AACR; Cancer Res 2019;79(13 Suppl):Abstract nr 2692.

Published

2019

11. High levels of p110δ PI3K expression in solid tumor cells suppress PTEN activity, generating cellular sensitivity to p110δ inhibitors through PTEN activation

Author

Aikaterini Vergetaki, Niki Tzenaki, Bart Vanhaesebroeck, Antonis Makrigiannakis, Kalliopi Stratigi, Evangelia A. Papakonstanti, and Margarita Andreou

Subjects

Male, medicine.medical_specialty, Cell, Breast Neoplasms, P110α, Biochemistry, Mice, Cell Line, Tumor, Internal medicine, Genetics, medicine, Animals, Protein Isoforms, PTEN, Molecular Biology, PI3K/AKT/mTOR pathway, Cell Proliferation, Phosphoinositide-3 Kinase Inhibitors, biology, Cell growth, Adenine, PTEN Phosphohydrolase, Prostatic Neoplasms, Cancer, medicine.disease, Class Ia Phosphatidylinositol 3-Kinase, Endocrinology, medicine.anatomical_structure, P110δ, Cell culture, NIH 3T3 Cells, Quinazolines, biology.protein, Cancer research, Female, Proto-Oncogene Proteins c-akt, Biotechnology

Abstract

Class IA PI3K isoforms have divergent, nonredundant cell biological roles. In untransformed cells and tissues, p110α and p110β are ubiquitously expressed, whereas p110δ expression is highly enriched in leukocytes. High levels of p110δ expression have been documented in some solid tumor cell lines, but the functional role is unknown. This study aimed to elucidate the link between elevated expression of p110δ PI3K and cancer. We report that in breast and prostate cancer cells that contain leukocyte levels of p110δ, p110δ activity dampens the activity of the PTEN tumor suppressor. Indeed, inactivation of p110δ in these cells led to PTEN activation, suppression of Akt phosphorylation, and inhibition of cell proliferation, with inhibition of PTEN activity being able to counterbalance p110δ inactivation. Likewise, forced overexpression of p110δ in cells with low p110δ expression reduced PTEN activity, resulting in increased Akt phosphorylation. Our data indicate that the oncogenic potential of p110δ PI3K overexpression might at least partially act through PTEN inactivation, and that p110δ-selective PI3K inhibitors can have a dual antitumor mechanism, namely by directly inhibiting p110δ signaling and by a broader inhibition of class I PI3K activity through PTEN activation. These data may have important implications in the intervention of breast cancer.

Published

2012

12. Functional CSF‐1 receptors are located at the nuclear envelope and activatedviathe p110δ isoform of PI 3‐kinase

Author

Olivier Zwaenepoel, Aikaterini Vergetaki, Bart Vanhaesebroeck, Evangelia A. Papakonstanti, Antonis Makrigiannakis, and Niki Tzenaki

Subjects

Macrophage colony-stimulating factor, Class I Phosphatidylinositol 3-Kinases, Nuclear Envelope, Endocytic cycle, Breast Neoplasms, Receptor, Macrophage Colony-Stimulating Factor, Biology, Biochemistry, Cell Line, Mice, Phosphatidylinositol 3-Kinases, Cell Line, Tumor, Genetics, Animals, Humans, Phosphorylation, RNA, Small Interfering, Receptor, Molecular Biology, Protein kinase B, PI3K/AKT/mTOR pathway, Phosphoinositide-3 Kinase Inhibitors, rab5 GTP-Binding Proteins, Mice, Knockout, Macrophage Colony-Stimulating Factor, Macrophages, Molecular biology, Cell biology, P110δ, Cancer cell, Female, Signal transduction, Proto-Oncogene Proteins c-akt, Cyclin-Dependent Kinase Inhibitor p27, Signal Transduction, Biotechnology

Abstract

Colony stimulating factor-1 (CSF-1) and its receptor (CSF-1R) are key regulators of macrophage biology, and their elevated expression in cancer cells has been linked to poor prognosis. CSF-1Rs are thought to function at the plasma membrane. We show here that functional CSF-1Rs are present at the nuclear envelope of various cell types, including primary macrophages, human cancer cell lines, and primary human carcinomas. In response to CSF-1, added to intact cells or isolated nuclei, nucleus-associated CSF-1R became phosphorylated and triggered the phosphorylation of Akt and p27 inside the nucleus. Extracellularly added CSF-1 was also found to colocalize with nucleus-associated CSF-1Rs. All these activities were found to depend selectively on the activity of the p110δ isoform of phosphoinositide 3-kinase (PI3K). This finding was related to the p110δ-dependent translocation of exogenous CSF-1 to the nucleus-associated CSF-1Rs, correlating with a prominent role of p110δ in activation of the Rab5 GTPase, a key regulator of the endocytic trafficking. siRNA-silencing of Rab5a phenocopied p110δ inactivation and nuclear CSF-1 signaling. Our work demonstrates for the first time the presence of functional nucleus-associated CSF-1Rs, which are activated by extracellular CSF-1 by a mechanism that involves p110δ and Rab5 activity. These findings may have important implications in cancer development.

Published

2011

13. The p110δ isoform of PI 3-kinase negatively controls RhoA and PTEN

Author

Bart Vanhaesebroeck, Evangelia A. Papakonstanti, and Anne J. Ridley

Subjects

RHOA, RAC1, Article, General Biochemistry, Genetics and Molecular Biology, Mice, Phosphatidylinositol 3-Kinases, Cytosol, Animals, Humans, PTEN, Molecular Biology, Protein kinase B, Cells, Cultured, PI3K/AKT/mTOR pathway, General Immunology and Microbiology, biology, Effector, Cell growth, Kinase, Chemotaxis, Macrophage Colony-Stimulating Factor, Macrophages, General Neuroscience, PTEN Phosphohydrolase, DNA, Cell biology, Enzyme Activation, Isoenzymes, biology.protein, Cancer research, rhoA GTP-Binding Protein, Cyclin-Dependent Kinase Inhibitor p27, Protein Binding

Abstract

Inactivation of PI 3-kinase (PI3K) signalling is critical for tumour suppression by PTEN. This is thought to be a unidirectional relationship in which PTEN degrades the lipids produced by PI3K, thus controlling cell proliferation, survival and migration. We now show that this relationship is in fact bidirectional, whereby PI3K reciprocally controls PTEN. We report that the p110delta PI3K negatively regulates PTEN, through a pathway involving inhibition of RhoA. Inactivation of p110delta in macrophages led to reduced Akt and Rac1 activation, but paradoxically to increased RhoA and PTEN activity. Partial inactivation of p190RhoGAP and a reduced binding of cytoplasmic RhoA to the cyclin-dependent kinase inhibitor p27 both contributed to the increased RhoA-GTP levels upon p110delta inactivation. Pharmacological inhibition of ROCK, a downstream effector kinase of RhoA, restored all signalling and functional defects of p110delta inactivation, including Akt phosphorylation, chemotaxis and proliferation. This work identifies the RhoA/ROCK pathway as a major target of p110delta-mediated PI3K signalling, and establishes for the first time that PI3K controls itself, via a feedback loop involving PTEN.

Published

2007

14. Focus on PTEN Regulation

Author

Evangelia A. Papakonstanti, Evangelia Goulielmaki, and Miriam Bermúdez Brito

Subjects

Genetics, PTEN, Cancer Research, Phosphatase, translation, Review, Biology, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, lcsh:RC254-282, protein interactions, localization, Cell biology, law.invention, Protein–protein interaction, Oncology, Cytoplasm, law, Lipid phosphatase activity, Organelle, biology.protein, Suppressor, Tensin, transcription

Abstract

The role of phosphatase and tensin homolog on chromosome 10 (PTEN) as a tumor suppressor has been for a long time attributed to its lipid phosphatase activity against PI(3,4,5)P3, the phospholipid product of the class I PI3Ks. Besides its traditional role as a lipid phosphatase at the plasma membrane, a wealth of data has shown that PTEN can function independently of its phosphatase activity and that PTEN also exists and plays a role in the nucleus, in cytoplasmic organelles, and extracellularly. Accumulating evidence has shed light on diverse physiological functions of PTEN, which are accompanied by a complex regulation of its expression and activity. PTEN levels and function are regulated transcriptionally, post-transcriptionally, and post-translationally. PTEN is also sensitive to regulation by its interacting proteins and its localization. Herein, we summarize the current knowledge on mechanisms that regulate the expression and enzymatic activity of PTEN and its role in human diseases.

Published

2015

15. Focal adhesion kinase phosphorylates the phosphatase and tensin homolog deleted on chromosome 10 under the control of p110δ phosphoinositide-3 kinase

Author

Michalis Aivaliotis, Evangelia A. Papakonstanti, and Niki Tzenaki

Subjects

RHOA, Class I Phosphatidylinositol 3-Kinases, Molecular Sequence Data, Biochemistry, Focal adhesion, chemistry.chemical_compound, Cell Line, Tumor, Genetics, Tensin, PTEN, Humans, Amino Acid Sequence, Phosphorylation, Molecular Biology, PI3K/AKT/mTOR pathway, Phosphoinositide 3-kinase, biology, Chromosomes, Human, Pair 10, PTEN Phosphohydrolase, Tyrosine phosphorylation, Molecular biology, chemistry, Focal Adhesion Protein-Tyrosine Kinases, biology.protein, Gene Deletion, Biotechnology

Abstract

The phosphatase and tensin homolog deleted on chromosome 10 (PTEN) tumor suppressor protein is regulated by various mechanisms that are not fully understood. This includes regulation by Tyr phosphorylation by a mechanism that remains elusive. Here, we show that focal adhesion kinase (FAK) phosphorylates PTEN in vitro, in cell-free systems and in cells. Furthermore, by mass spectrometry, we identified Tyr336 on PTEN as being phosphorylated by FAK. Tyr336 phosphorylation increased phosphatase activity, protein-lipid interaction, and protein stability of PTEN. In cells, including primary mouse macrophages and human cancer cell lines, FAK was found to be negatively regulated by p110δ phosphoinositide-3 kinase (PI3K), whereas the activation of FAK was positively regulated by RhoA-associated kinase (ROCK). Indeed, the phosphorylation of FAK was unexpectedly increased in macrophages derived from mice expressing kinase-dead p110δ. Pharmacologic inactivation of RhoA/ROCK reduced the phosphorylation of FAK to normal levels in cells with genetically inactivated p110δ. Likewise, pharmacologic inactivation of FAK reduced the phosphorylation of PTEN in cells expressing kinase-dead p110δ and restored the functional defects of p110δ inactivation, including Akt phosphorylation and cell proliferation. This work identifies FAK as a target of p110δ PI3K that links RhoA with PTEN and establishes for the first time that PTEN is a substrate of FAK-mediated Tyr phosphorylation.

Published

2015

16. The opioid agonist ethylketocyclazocine reverts the rapid, non-genomic effects of membrane testosterone receptors in the human prostate LNCaP cell line

Author

Marilena Kampa, Elias Castanas, Anastassia Hatzoglou, Christos Stournaras, Evangelia A. Papakonstanti, and Vassilia-Ismini Alexaki

Subjects

Male, Cell signaling, Ethylketocyclazocine, Pharmacology, Biology, Binding, Competitive, LNCaP, Reaction Time, Tumor Cells, Cultured, Humans, Testosterone, Opioid peptide, Receptor, Binding Sites, Cell growth, Carcinoma, Cell Membrane, Prostatic Neoplasms, Serum Albumin, Bovine, Cell Biology, Prostate-Specific Antigen, Protein-Tyrosine Kinases, Actin cytoskeleton, Cell biology, Analgesics, Opioid, Actin Cytoskeleton, Opioid Peptides, Receptors, Androgen, Focal Adhesion Kinase 1, Focal Adhesion Protein-Tyrosine Kinases, Cell Division, Signal Transduction

Abstract

Neuropeptides influence cancer cell replication and growth. Opioid peptides, and opiergic neurons are found in the prostate gland, and they are proposed to exert a role in tumor regulation, influencing cancer cell growth, as opioid agonists inhibit cell growth in several systems, including the human prostate cancer cell line LNCaP. In the same cell line, the existence of membrane testosterone receptors was recently reported, which increase, in a non-genomic manner, the secretion of PSA, and modify actin cytoskeleton dynamics, through the signaling cascade FAK→PI-3 kinase→Cdc42/Rac1. In the present work, we present data supporting that the general opioid agonist Ethylketocyclazocine (EKC) decreases testosterone-BSA (a non-internalizable testosterone analog) induced PSA secretion. Furthermore, we report that this opioid affects this non-genomic testosterone action, by modifying the distribution of the actin cytoskeleton in the cells, disrupting the above signaling cascade. In addition, after long (>24 h) incubation, opioids decrease the number of membrane testosterone receptors, and reverse their effect on the signaling molecules. In conclusion, our results provide some new insights of a possible action of opioids in prostate cancer control by interfering with the action and the expression of membrane testosterone receptors and signaling.

Published

2004

17. Tumor Necrosis Factor-α Promotes Survival of Opossum Kidney Cells via Cdc42-induced Phospholipase C-γ1 Activation and Actin Filament Redistribution

Author

Evangelia A. Papakonstanti and Christos Stournaras

Subjects

Cell Survival, Apoptosis, macromolecular substances, CDC42, Biology, Kidney, medicine, Animals, Enzyme Inhibitors, cdc42 GTP-Binding Protein, Cytoskeleton, Molecular Biology, Cells, Cultured, Phospholipase C, Caspase 3, Phospholipase C gamma, Tumor Necrosis Factor-alpha, Opossums, Articles, Cell Biology, Actin cytoskeleton, Cell biology, Actin Cytoskeleton, medicine.anatomical_structure, Cdc42 GTP-Binding Protein, Caspases, Type C Phospholipases, Mutation, Tumor necrosis factor alpha

Abstract

Although the renal proximal tubular epithelial cells are targeted in a variety of inflammatory diseases of the kidney, the signaling mechanism by which tumor necrosis factor (TNF)-alpha exerts its effects in these cells remains unclear. Here, we report that TNF-alpha elicits antiapoptotic effects in opossum kidney cells and that this response is mediated via actin redistribution through a novel signaling mechanism. More specifically, we show that TNF-alpha prevents apoptosis by inhibiting the activity of caspase-3 and this effect depends on actin polymerization state and nuclear factor-kappaB activity. We also demonstrate that the signaling cascade triggered by TNF-alpha is governed by the phosphatidylinositol-3 kinase, Cdc42/Rac1, and phospholipase (PLC)-gamma1. In this signaling cascade, Cdc42 was found to be selectively essential for PLC-gamma1 activation, whereas phosphatidylinositol-3,4,5-triphosphate alone is not sufficient to activate the phospholipase. Moreover, PLC-gamma1 was found to associate in vivo with the small GTPase(s). Interestingly, PLC-gamma1 was observed to associate with constitutively active (CA) Cdc42V12, but not with CA Rac1V12, whereas no interaction was detected with Cdc42(T17N). The inactive Cdc42(T17N) and the PLC-gamma1 inhibitor U73122 prevented actin redistribution and depolymerization, confirming that both signaling molecules are responsible for the reorganization of actin. Additionally, the actin filament stabilizer phallacidin potently blocked the nuclear translocation of nuclear factor-kappaB and its binding activity, resulting in abrogation of the TNF-alpha-induced inhibition of caspase-3. To conclude, our findings suggest that actin may play a pivotal role in the response of opossum kidney cells to TNF-alpha and implicate Cdc42 in directly regulating PLC-gamma1 activity.

Published

2004

18. Association of PI-3 Kinase with PAK1 Leads to Actin Phosphorylation and Cytoskeletal Reorganization

Author

Evangelia A. Papakonstanti and Christos Stournaras

Subjects

Narcotics, rac1 GTP-Binding Protein, Actin phosphorylation, Recombinant Fusion Proteins, Arp2/3 complex, Ethylketocyclazocine, macromolecular substances, Protein Serine-Threonine Kinases, Mitogen-activated protein kinase kinase, Cell Fractionation, Kidney, Article, Cell Line, Phosphatidylinositol 3-Kinases, Animals, cdc42 GTP-Binding Protein, Molecular Biology, Cytoskeleton, Phosphoinositide-3 Kinase Inhibitors, biology, MAP kinase kinase kinase, Tumor Necrosis Factor-alpha, Cyclin-dependent kinase 5, Caseins, Actin remodeling, Opossums, Cell Biology, Actin cytoskeleton, Immunohistochemistry, Actins, Peptide Fragments, Cell biology, Androstadienes, Enzyme Activation, p21-Activated Kinases, Guanosine 5'-O-(3-Thiotriphosphate), biology.protein, Cyclin-dependent kinase 9, Wortmannin

Abstract

The family of p21-activated kinases (PAKs) have been implicated in the rearrangement of actin cytoskeleton by acting downstream of the small GTPases Rac and Cdc42. Here we report that even though Cdc42/Rac1 or Akt are not activated, phosphatidylinositol-3 (PI-3) kinase activation induces PAK1 kinase activity. Indeed, we demonstrate that PI-3 kinase associates with the N-terminal regulatory domain of PAK1 (amino acids 67–150) leading to PAK1 activation. The association of the PI-3 kinase with the Cdc42/Rac1 binding-deficient PAK1(H83,86L) confirms that the small GTPases are not involved in the PI-3 kinase-PAK1 interaction. Furthermore, PAK1 was activated in cells expressing the dominant-negative forms of Cdc42 or Rac1. Additionally, we show that PAK1 phosphorylates actin, resulting in the dissolution of stress fibers and redistribution of microfilaments. The phosphorylation of actin was inhibited by the kinase-dead PAK1(K299R) or the PAK1 autoinhibitory domain (PAK1(83–149)), indicating that PAK1 was responsible for actin phosphorylation. We conclude that the association of PI-3 kinase with PAK1 regulates PAK1 kinase activity through a Cdc42/Rac1-independent mechanism leading to actin phosphorylation and cytoskeletal reorganization.

Published

2002

19. Galectin-1 overexpression in endometriosis and its regulation by neuropeptides (CRH, UCN) indicating its important role in reproduction and inflammation

Author

Eirini Taliouri, Thomas Vrekoussis, Antonis Makrigiannakis, Evangelia A. Papakonstanti, Aikaterini Vergetaki, Luca Sabatini, and Udo Jeschke

Subjects

Infertility, medicine.medical_specialty, endocrine system, Galectin 1, Corticotropin-Releasing Hormone, Urology, Endometriosis, lcsh:Medicine, Endometrium, Receptors, Corticotropin-Releasing Hormone, Mice, Internal medicine, medicine, otorhinolaryngologic diseases, Medicine and Health Sciences, Animals, Humans, Receptor, lcsh:Science, Urocortins, Urocortin, Inflammation, Multidisciplinary, business.industry, Reproduction, Decidua, Female infertility, lcsh:R, Trophoblast, Subfertility, Obstetrics and Gynecology, medicine.disease, Female Subfertility, female genital diseases and pregnancy complications, medicine.anatomical_structure, Endocrinology, Gene Expression Regulation, Women's Health, lcsh:Q, Female, business, Research Article

Abstract

Endometriosis is an inflammatory disease of women of reproductive age featured by the presence of ectopic endometrium and is strongly related to infertility. Galectins, carbonhydrate-binding proteins, have been found to have pro- or anti-inflammatory roles in the reproductive tract and in pathological conditions concerning infertility. Galectin-1, which is expressed at endometrium and decidua, plays a major role in implantation and trophoblast invasion. Also, the neuropeptides, corticotropin releasing hormone (CRH) and urocortin (UCN) and their receptors are expressed in eutopic and ectopic endometrium showing a differential expression pattern in endometriotic women compared to healthy ones. The aim of this study was to examine the galectin-1 expression in endometriotic lesions and compare its expression in eutopic endometrium of endometriotic and healthy women. Furthermore, we examined the effect of CRH and UCN in galectin-1 expression in Ishikawa cell line and macrophages and investigated the implication of CRHR1 in these responses. Eutopic and ectopic endometrium specimens, Ishikawa cell line and mice macrophages were used. Immunohistochemistry and western blot analysis were performed in order to identify galectin-1 expression in ectopic and eutopic endometrium of women with and without endometriosis and the regulatory effect of CRH and UCN on galectin-1 expression. This study presents for the first time that galectin-1 is overexpressed in endometriotic lesions compared to eutopic endometrium of endometriotic women and is more abundantly expressed in eutopic endometrium of disease women compared to healthy ones. Furthermore, it is shown that CRH and UCN upregulate galectin-1 expression in Ishikawa cell line and macrophages and this effect is mediated through CRHR1. These results suggest that galectin-1 might play an important role in endometriosis pathology and infertility profile of women suffering from endometriosis by being at the same time regulated by CRH and UCN interfering in the immune disequilibrium which characterizes this pathological condition.

Published

2014

20. PLC-γ1 Signaling Pathway and Villin Activation Are Involved In Actin Cytoskeleton Reorganization Induced by Na+/Pi Cotransport Up-regulation

Author

Achille Gravanis, Evangelia A. Papakonstanti, Christos Stournaras, and Dimitrios S. Emmanouel

Subjects

biology, Actin cytoskeleton reorganization, Tyrosine phosphorylation, macromolecular substances, Microfilament, Actin cytoskeleton, digestive system, Cell biology, chemistry.chemical_compound, chemistry, Genetics, biology.protein, Molecular Medicine, Phosphorylation, Cytoskeleton, Villin, Molecular Biology, Genetics (clinical), Actin

Abstract

The brief incubation of opossum kidney (OK) cells with low Pi results in Na+/Pi co-transport up-regulation and in substantial, but transient, cytoskeletal reorganization. In this study, we examined signaling events involved in the depolymerization of microfilaments. Confocal laser scanning microscopy, immunoblot and immunoprecipitation experiments revealed villin co-localization with mainly actin short filaments and monomers, indicating that under the conditions used, villin acted as an actin-severing protein. Further analysis revealed that low concentrations of extracellular phosphate resulted in phospholipase Cγ1 (PLC-γ1) translocation to the actin cytoskeleton, without increases in its tyrosine phosphorylation. Additionally, tyrosine phosphorylation of a portion of insoluble villin was increased; whereas, only tyrosine phosphorylated villin associated with PLC-γ1. Although, tyrosine phosphorylation of PLC-γ1 was not observed during Na+/Pi cotransport up-regulation, genistein treatment abolished the enzyme’s translocation to the actin cytoskeleton, as well as its association with villin. In addition, villin was found to associate with the 85-KDa subunit (p85) of phosphatidylinositol (PI)-3 kinase, concomitant with PLC-γ1, in the cytoskeletal fraction of Na+/Pi cotransport up-regulated cells. Our observations suggest a signaling mechanism linking low ambient Pi levels to the acute up-regulation of its cotransport with sodium and the depolymerization of the subcortical actin cytoskeleton.

Published

2000

21. Actin Cytoskeleton: A Signaling Sensor in Cell Volume Regulation

Author

Evangelia A. Papakonstanti, Christos Stournaras, and Eleftheria A. Vardaki

Subjects

biology, Physiology, Arp2/3 complex, Actin remodeling, Actin cytoskeleton, Microfilament, Actins, Cell biology, Actin remodeling of neurons, Profilin, biology.protein, MDia1, Cytoskeleton, Cell Size, Signal Transduction

Abstract

The actin microfilaments are well known dynamic structures that support and organize the cell membrane and functions associated with the membrane such as ion channels and transporters. In addition, many aspects of cellular physiology seem to be actively modulated by changes in actin cytoskeleton dynamics, which involve reorganization and restructuring of the filaments. For both of these reasons, the actin cytoskeleton has attracted special attention since the early days of cell volume regulation research. Mechanisms controlling the actin equilibrium in response to external stimuli were studied and the signaling cascades leading to the regulation of actin cytoskeleton dynamics have been partially elucidated. They include: a) activation of specific actin binding proteins that regulate actin polymerization dynamics, b) activation of protein kinases or phosphatases regulating phosphorylation of specific cytoskeletal proteins and c) activation of signal transduction pathways leading from membrane receptor activation to actin reorganization involving small GTPases of the Rho and Rac families. These intracellular signal transducers are activated by extracellular stimuli that include hormones, growth factors, cytokines, or ions, many of them in turn are partially known to participate in cell volume regulation. These findings provide strong evidence that the actin cytoskeleton is involved in cell volume regulation by sensing and mediating extracellular signals.

Published

2000

22. TNF-α Induces Actin Cytoskeleton Reorganization in Glomerular Epithelial Cells Involving Tyrosine Phosphorylation of Paxillin and Focal Adhesion Kinase

Author

Christos Stournaras, Evangelia A. Papakonstanti, Dimitrios S. Emmanouel, Sevasti B. Koukouritaki, E. A. Vardaki, and E. Lianos

Subjects

biology, PTK2, Actin cytoskeleton reorganization, Actin remodeling, Arp2/3 complex, macromolecular substances, Vinculin, Actin cytoskeleton, Cell biology, Genetics, biology.protein, Molecular Medicine, MDia1, Molecular Biology, Genetics (clinical), Paxillin

Abstract

Glomerular permeability for macromolecules depends partially on proper attachment of the glomerular epithelial cells (GEC) to the glomerular basement membrane (GBM). The latter requires integrity of the actin cytoskeleton, which in turn is regulated by specific actin-associated proteins. Since several glomerulopathies characterized by heavy proteinuria are associated with increased glomerular tumor necrosis factor α (TNF-α) expression, we studied the interaction of TNF-α with the actin cytoskeleton of cultured rat GEC. Incubation of GEC with 10 ng/ml TNF-α for variable time periods ranging from 15 min to 24 hr demonstrated a marked accentuation and redistribution of actin microfilaments, as shown by direct fluorescence analysis and confocal laser scanning microscopy. Quantitative biochemical determination of the G/total-actin ratio confirmed the above observations. Indeed, this ratio was significantly reduced, indicating substantial polymerization of G-actin and formation of F-actin. Concurrently, TNF-α rapidly induced tyrosine phosphorylation of both paxillin and focal adhesion kinase, without affecting the expression levels of these two proteins. In addition, tyrosine phosphorylation of vinculin became evident, indicating involvement of this focal adhesion marker in the observed actin reorganization. Inhibition of tyrosine phosphorylation by genistein prevented the reorganization of the actin cytoskeleton by TNF-α. We conclude that TNF-α induces substantial reorganization of actin cytoskeleton and focal adhesions. These effects occur simultaneously, with a prompt TNF-α-induced tyrosine phosphorylation of paxillin and focal adhesion kinase, indicating that these proteins, known to regulate actin polymerization and formation of focal adhesions, may be directly involved in the mechanism controlling the observed actin redistribution. These findings suggest that the observed TNF-α-actin cytoskeleton interactions may relate to the pathogenesis of glomerulopathies with heavy proteinuria, in which increased glomerular expression of TNF-α is associated with disturbances in the attachment of podocytes to the GBM.

Published

1999

23. Early alterations of actin cytoskeleton in OK cells by opioids

Author

Dimitrios S. Emmanouel, Evangelia A. Papakonstanti, Efstathia Bakogeorgou, Christos Stournaras, Roland Hartig, and Elias Castanas

Subjects

biology, Chemistry, Actin remodeling, Arp2/3 complex, macromolecular substances, Cell Biology, Microfilament, Actin cytoskeleton, Biochemistry, Cell biology, Actin remodeling of neurons, Profilin, biology.protein, MDia1, Cytoskeleton, Molecular Biology

Abstract

Recently we identified and characterized opioid binding sites in OK (opossum kidney) cells and observed decreased proliferation of these cells in response to opioids. In the present study we investigated the effects of opioids on the actin cytoskeleton and explored whether their antiproliferative action may relate to alterations in the distribution or the dynamics of actin microfilaments. Exposure of OK cells to the opioids alphaS1 casomorphin and ethylketocyclazocine resulted in a rapid and substantial actin microfilament reorganization. This was documented by a significant dose-dependent decrease in the amounts of F-actin, determined by measurements of quantitative fluorescence, by immunoblot analysis and by a concomitant increase of the G/total-actin ratio measured by the DNase I inhibition assay. These changes were verified by confocal laser scanning microscopy, which showed marked redistribution of the microfilamentous structures in the presence of the opioids without affecting the organization of microtubules or vimentin intermediate filaments. The effect of opioids on actin polymerization dynamics occurred within 15 min and persisted for at least 2 h, while their restoration to control levels was accomplished 6 h later, indicating a reversible phenomenon. Northern blot analysis showed that the concentration of the actin transcript was unaffected. The addition of diprenorphine, a general opioid antagonist, prevented the effects of opioids on the actin cytoskeleton. The inhibition of OK cell proliferation, induced by ethylketocyclazocine and alphaS1 casomorphin was partially prevented in the presence of phallacidin, which stabilizes microfilaments. Our findings demonstrate that opioids, acting via kappa 1 binding sites, induce rapidly modifications in the dynamics of actin polymerization, and in the organization of microfilaments in OK cells, which may relate to their antiproliferative effect on these cells.

Published

1998

24. Differential Expression of CRH, UCN, CRHR1 and CRHR2 in Eutopic and Ectopic Endometrium of Women with Endometriosis

Author

Thomas Vrekoussis, Antonis Makrigiannakis, Aikaterini Vergetaki, Luca Sabatini, Evangelia A. Papakonstanti, Eirini Taliouri, and Udo Jeschke

Subjects

Infertility, medicine.medical_specialty, endocrine system, Anatomy and Physiology, Corticotropin-Releasing Hormone, Endometriosis, lcsh:Medicine, Endometrium, Receptors, Corticotropin-Releasing Hormone, Corticotropin-releasing hormone, Diagnostic Medicine, Internal medicine, medicine, otorhinolaryngologic diseases, Pathology, Humans, lcsh:Science, Receptor, Biology, Urocortins, Urocortin, Multidisciplinary, medicine.diagnostic_test, business.industry, lcsh:R, Reproductive System, Decidualization, Obstetrics and Gynecology, medicine.disease, medicine.anatomical_structure, Endocrinology, Gene Expression Regulation, Case-Control Studies, Medicine, Women's Health, lcsh:Q, Female, business, hormones, hormone substitutes, and hormone antagonists, Biomarkers, Menstrual Abnormalities, Endometrial biopsy, Research Article, General Pathology

Abstract

Endometriosis is considered as a benign aseptic inflammatory disease, characterised by the presence of ectopic endometrium-like tissue. Its symptoms (mostly pain and infertility) are reported as constant stressors. Corticotropin releasing hormone (CRH) and urocortin (UCN) are neuropeptides, strongly related to stress and inflammation. The effects of CRH and UCN are mediated through CRHR1 and CRHR2 receptors which are implicated in several reproductive functions acting as inflammatory components. However, the involvement of these molecules to endometriosis remains unknown. The aim of this study was to examine the expression of CRHR1 and CRHR2 in endometriotic sites and to compare the expression of CRHR1 and CRHR2 in eutopic endometrium of endometriotic women to that of healthy women. We further compared the expression of CRH, UCN, CRHR1 and CRHR2 in ectopic endometrium to that in eutopic endometrium of women with endometriosis. Endometrial biopsy specimens were taken from healthy women (10 patients) and endometrial and endometriotic biopsy specimens were taken from women with endometriosis (16 patients). Τhe expression of CRH, UCN, CRHR1, and CRHR2 was tested via RT-PCR, immunohistochemistry and Western blotting. This study shows for the first time that CRH and UCN receptor subtypes CRHR1β and CRHR2α are expressed in endometriotic sites and that they are more strongly expressed (p

Published

2013

25. p110δ PI3 kinase pathway: emerging roles in cancer

Author

Evangelia A. Papakonstanti and Niki Tzenaki

Subjects

Genetics, Gene isoform, PTEN, Cancer Research, biology, Somatic cell, Kinase, Review Article, hematologic malignancies, solid tumors, P110α, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, lcsh:RC254-282, p110δ PI3K, Oncology, P110δ, Cancer research, biology.protein, cancer, Gene, p110d PI3K, PI3K/AKT/mTOR pathway

Abstract

Class IA PI3Ks consists of three isoforms of the p110 catalytic subunit designated p110α, p110β, and p110δ which are encoded by three separate genes. Gain-of-function mutations on PIK3CA gene encoding for p110α isoform have been detected in a wide variety of human cancers whereas no somatic mutations of genes encoding for p110β or p110δ have been reported. Unlike p110α and p110β which are ubiquitously expressed, p110δ is highly enriched in leukocytes and thus the p110δ PI3K pathway has attracted more attention for its involvement in immune disorders. However, findings have been accumulated showing that the p110δ PI3K plays a seminal role in the development and progression of some hematologic malignancies. A wealth of knowledge has come from studies showing the central role of p110δ PI3K in B-cell functions and B-cell malignancies. Further data have documented that wild-type p110δ becomes oncogenic when overexpressed in cell culture models and that p110δ is the predominant isoform expressed in some human solid tumor cells playing a prominent role in these cells. Genetic inactivation of p110δ in mice models and highly-selective inhibitors of p110δ have demonstrated an important role of this isoform in differentiation, growth, survival, motility, and morphology with the inositol phosphatase PTEN to play a critical role in p110δ signaling. In this review, we summarize our understanding of the p110δ PI3K signaling pathway in hematopoietic cells and malignancies, we highlight the evidence showing the oncogenic potential of p110δ in cells of non-hematopoietic origin and we discuss perspectives for potential novel roles of p110δ PI3K in cancer.

Published

2013

26. Identification and characterization of opioid and somatostatin binding sites in the opossum kidney (OK) cell line and their effect on growth

Author

Elias Castanas, Efstathia Bakogeorgou, Anastassia Hatzoglou, Evangelia A. Papakonstanti, Christos Stournaras, and Dimitrios S. Emmanouel

Subjects

Delta cell, medicine.medical_specialty, Chemistry, Somatostatin receptor, Cell Biology, Biochemistry, Endocrinology, Somatostatin, Internal medicine, medicine, Somatostatin receptor 3, Somatostatin receptor 2, Somatostatin binding, Somatostatin receptor 1, Diprenorphine, Molecular Biology, hormones, hormone substitutes, and hormone antagonists, medicine.drug

Abstract

Opioids and somatostatin analogs have been implicated in the modulation of renal water handling, but whether their action is accomplished through central and/or peripheral mechanisms remains controversial. In different cell systems, on the other hand, opioids and somatostatin inhibit cell proliferation. In the present study, we have used an established cell line, derived from opossum kidney (OK) proximal tubules, in order to characterize opioid and somatostatin receptors and to investigate the action of opioids and somatostatin on tubular epithelial tissue. Our results show the presence of one class of opioid binding sites with kappa, selectivity (KD 4.6 +/- 0.9 nM, 57,250 sites/cell), whereas delta, mu, or other subtypes of the kappa site were absent. Somatostatin presents also a high affinity site on these cells (KD 24.5 nM, 330,000 sites/cell). No effect of either opioids or somatostatin on the activity of the NA+/Pi cotransporter was observed, indicating that these agents do not affect ion transport mechanisms. However, opioid agonists and somatostatin analogs decrease OK cell proliferation in a dose-dependent manner; in the same nanomolar concentration range, they displayed reversible specific binding for these agents. The addition of diprenorphine, a general opioid antagonist, reversed the effects of opioids, with the exception of morphine. Furthermore, morphine interacts with the somatostatin receptor in this cell line too, as was the case in the breast cancer T47D cell line. Our results indicate that in the proximal tubule opioids and somatostatin do not affect transport, but they might have a role in the modulation of renal cell proliferation either during ontogenesis or in kidney repair.

Published

1996

27. Na+/Pi co-transport alters rapidly cytoskeletal protein polymerization dynamics in opossum kidney cells

Author

Evangelia A. Papakonstanti, Achille Gravanis, Dimitrios S. Emmanouel, and Christos Stournaras

Subjects

macromolecular substances, Kidney, Microfilament, Microtubules, Biochemistry, Phosphates, chemistry.chemical_compound, Drug Stability, Tubulin, Microtubule, Extracellular, Animals, Cytoskeleton, Molecular Biology, Cytochalasin B, Cells, Cultured, Actin, Symporters, biology, Kidney metabolism, Sodium-Phosphate Cotransporter Proteins, Opossums, Cell Biology, Actins, Up-Regulation, Cell biology, Actin Cytoskeleton, Kinetics, Microscopy, Fluorescence, chemistry, biology.protein, Carrier Proteins, Research Article

Abstract

We studied with biochemical and immunofluorescent techniques the interactions between the actin microfilament and tubulin microtubule cytoskeleton and Na+/Pi co-transport in opossum kidney cells, a line with proximal tubular characteristics. On brief (5 min) incubation of the cells with a low (0.1 mM) concentration of Pi, a rapid F-actin depolymerization takes place, which fails to occur in cells incubated under similar conditions with 1 mM Pi. The disassembly of actin microfilaments could be quantitatively expressed as a 33% increase in the ratio of monomeric G-actin to polymerized F-actin (G/F-actin ratio from 0.80±0.03 to 1.06±0.06, n = 28, P < 0.01), owing to a significant decrease in the latter. Under these conditions microfilaments were also markedly destabilized, as shown by their diminished resistance to graded cytochalasin B concentrations. In addition, incubation of opossum kidney cells with low Pi concentrations (0.1 mM) resulted within 5 min in a substantial depolymerization of microtubules, shown by immunofluorescence microscopy and measured as a 70.9±6.9% (n = 11, P < 0.01) decrement by immunoblot analysis. These changes, which occur only when extracellular Pi concentrations are kept low, seem to be related to a significant increase within 5 min in the rate of cellular Pi uptake by 25.5% under these conditions. The shifts in the dynamic equilibria between monomeric and polymerized actin and tubulin in response to cellular Pi uptake were transient, being fully reversible within 30 min. Moreover, the effect of Pi seemed to be specific because inhibition of its uptake by phosphonoformic acid blunted microtubular disassembly markedly. In contrast, measurement of Pi uptake in the presence of agents known to stabilize cytoskeletal structures showed a substantial decrease with phallacidin, which stabilizes microfilaments, whereas the microtubule stabilizer taxol had no apparent effect. These results indicate that acute alterations in the polymerization dynamics and stability of both microfilaments and microtubules are involved in the modulation of Na+/Pi co-transport and suggest important cytoskeletal participation in proximal tubular transport functions.

Published

1996

28. Membrane androgen receptor activation in prostate and breast tumor cells: molecular signaling and clinical impact

Author

Evangelia A. Papakonstanti, Konstantinos Alevizopoulos, Galatea Kallergi, Christos Stournaras, and Natalia Papadopoulou

Subjects

Male, Clinical Biochemistry, Cell, Apoptosis, Breast Neoplasms, Biology, Biochemistry, Models, Biological, Actin cytoskeleton organization, Prostate cancer, Cell Line, Tumor, Genetics, medicine, Humans, Molecular Biology, Cytoskeleton, Cell growth, Membrane Proteins, Prostatic Neoplasms, Cell Biology, Actin cytoskeleton, medicine.disease, Actins, Cell biology, Androgen receptor, medicine.anatomical_structure, Receptors, Androgen, Female, Membrane androgen receptor, Intracellular, Signal Transduction

Abstract

In recent years, membrane androgen receptors (mARs) have been identified in prostate and breast tumor cells, and their activation by specific mAR ligands was linked to the regulation of crucial cell responses, such as cell growth, motility, and apoptosis. Analysis of the molecular signals triggered by mAR in the presence of anti-androgens has clearly differentiated mAR-dependent biological actions from those induced by the activation of the classical intracellular androgen receptors (iARs). In this review, we summarize the specific cellular events attributed to mAR activation and the experimental results on distinct non-genomic signaling cascades operating in various tumor cells independently of the iAR. Furthermore, we discuss the crucial role of actin cytoskeleton organization and signaling in mediating mAR responses. Finally, we assess the clinical impact of the reported mAR-induced apoptotic regression of prostate cancer cells both in vitro and in vivo and discuss the potential role of mAR as a novel therapeutic target. © 2008 IUBMB IUBMB Life, 61(1): 56–61, 2009

Published

2008

29. Distinct roles of class IA PI3K isoforms in primary and immortalised macrophages

Author

Olivier Zwaenepoel, Gemma Nock, Antonio Bilancio, Anne J. Ridley, Benjamin T. Houseman, Emily Burns, Kevan M. Shokat, Bart Vanhaesebroeck, Evangelia A. Papakonstanti, Papakonstanti, Ea, Zwaenepoel, O, Bilancio, Antonio, Burns, E, Nock, Ge, Houseman, B, Shokat, K, Ridley, Aj, and Vanhaesebroeck, B.

Subjects

Gene isoform, rac1 GTP-Binding Protein, rho GTP-Binding Proteins, Cell type, RHOA, Class I Phosphatidylinositol 3-Kinases, Receptor, Macrophage Colony-Stimulating Factor, Biology, Cell Line, Mice, Phosphatidylinositol 3-Kinases, Cell Movement, PTEN, Animals, Protein Isoforms, Protein kinase B, Protein Kinase Inhibitors, PI3K/AKT/mTOR pathway, Cells, Cultured, Phosphoinositide-3 Kinase Inhibitors, Chemotaxis, Macrophage Colony-Stimulating Factor, Macrophages, Neuropeptides, PTEN Phosphohydrolase, Cell migration, Cell Biology, Cell biology, rac GTP-Binding Proteins, biology.protein, rhoA GTP-Binding Protein, Tyrosine kinase, Proto-Oncogene Proteins c-akt

Abstract

The class IA isoforms of phosphoinositide 3-kinase (p110alpha, p110beta and p110delta) often have non-redundant functions in a given cell type. However, for reasons that are unclear, the role of a specific PI3K isoform can vary between cell types. Here, we compare the relative contributions of PI3K isoforms in primary and immortalised macrophages. In primary macrophages stimulated with the tyrosine kinase ligand colony-stimulating factor 1 (CSF1), all class IA PI3K isoforms participate in the regulation of Rac1, whereas p110delta selectively controls the activities of Akt, RhoA and PTEN, in addition to controlling proliferation and chemotaxis. The prominent role of p110delta in these cells correlates with it being the main PI3K isoform that is recruited to the activated CSF1 receptor (CSF1R). In immortalised BAC1.2F5 macrophages, however, the CSF1R also engages p110alpha, which takes up a more prominent role in CSF1R signalling, in processes including Akt phosphorylation and regulation of DNA synthesis. Cell migration, however, remains dependent mainly on p110delta. In other immortalised macrophage cell lines, such as IC-21 and J774.2, p110alpha also becomes more prominently involved in CSF1-induced Akt phosphorylation, at the expense of p110delta.These data show that PI3K isoforms can be differentially regulated in distinct cellular contexts, with the dominant role of the p110delta isoform in Akt phosphorylation and proliferation being lost upon cell immortalisation. These findings suggest that p110delta-selective PI3K inhibitors may be more effective in inflammation than in cancer.

Published

2008

30. Cell responses regulated by early reorganization of actin cytoskeleton

Author

Christos Stournaras and Evangelia A. Papakonstanti

Subjects

Receptors, Steroid, Biophysics, Arp2/3 complex, Apoptosis, macromolecular substances, Ligands, Biochemistry, GPCRs, Ion Channels, Receptors, G-Protein-Coupled, Actin remodeling of neurons, Structural Biology, Cell Movement, TNFα, Genetics, Humans, Neoplasm Invasiveness, Actin-binding protein, Cytoskeleton, Molecular Biology, biology, Tumor Necrosis Factor-alpha, Actin remodeling, Cell Biology, Actin cytoskeleton, Cell response, Actins, Cell biology, Actin Cytoskeleton, Profilin, biology.protein, MDia1, Ion channel, Membrane-androgen receptor, Signal Transduction

Abstract

Microfilaments exist in a dynamic equilibrium between monomeric and polymerized actin and the ratio of monomers to polymeric forms is influenced by a variety of extracellular stimuli. The polymerization, depolymerization and redistribution of actin filaments are modulated by several actin-binding proteins, which are regulated by upstream signalling molecules. Actin cytoskeleton is involved in diverse cellular functions including migration, ion channels activity, secretion, apoptosis and cell survival. In this review we have outlined the role of actin dynamics in representative cell functions induced by the early response to extracellular stimuli.

Published

2008

31. Actin cytoskeleton architecture and signaling in osmosensing

Author

Evangelia A, Papakonstanti and Christos, Stournaras

Subjects

Octoxynol, Phalloidine, Rhodamines, Immunoblotting, Actins, Phenylmethylsulfonyl Fluoride, Solubility, Osmotic Pressure, Animals, Deoxyribonuclease I, Humans, Cytoskeleton, Cell Size, Signal Transduction

Abstract

Since the early days of cell volume regulation research, the role of actin cytoskeleton organization and rearrangement has attracted specific interest. Rapid modifications in actin dynamics and architecture have been described. They were shown to regulate cell volume changes, as well as regulatory volume decrease in a large variety of cell types, including hepatocytes, lymphocytes, fibroblasts, myocytes, and various tumor cells. Using microscopic and biochemical analyses, modifications of actin organization and polymerization dynamics were studied. This chapter summarizes the molecular approaches applied so far for the quantitative assessment of actin cytoskeleton dynamics in the various cell types. It demonstrates that rapid modifications of actin cytoskeleton dynamics regulated by specific signaling pathways play a functional role in cell volume regulation. It is concluded that studying actin polymerization dynamics and signaling represents a challenging tool for the understanding of osmosensing and osmosignaling regulation in cellular physiology.

Published

2007

32. Actin Cytoskeleton Architecture and Signaling in Osmosensing

Author

Evangelia A. Papakonstanti and Christos Stournaras

Subjects

Actin remodeling of neurons, Profilin, biology.protein, Actin remodeling, Arp2/3 complex, macromolecular substances, Biology, Actin cytoskeleton, Cytoskeleton, Actin cytoskeleton organization, Actin, Cell biology

Abstract

Since the early days of cell volume regulation research, the role of actin cytoskeleton organization and rearrangement has attracted specific interest. Rapid modifications in actin dynamics and architecture have been described. They were shown to regulate cell volume changes, as well as regulatory volume decrease in a large variety of cell types, including hepatocytes, lymphocytes, fibroblasts, myocytes, and various tumor cells. Using microscopic and biochemical analyses, modifications of actin organization and polymerization dynamics were studied. This chapter summarizes the molecular approaches applied so far for the quantitative assessment of actin cytoskeleton dynamics in the various cell types. It demonstrates that rapid modifications of actin cytoskeleton dynamics regulated by specific signaling pathways play a functional role in cell volume regulation. It is concluded that studying actin polymerization dynamics and signaling represents a challenging tool for the understanding of osmosensing and osmosignaling regulation in cellular physiology.

Published

2007

33. Control of axonal growth and regeneration of sensory neurons by the p110delta PI 3-kinase

Author

Meirion Davies, Wayne Pearce, Aminul I. Ahmed, Frank P. T. Hamers, Karl Peter Giese, Bart Vanhaesebroeck, Evangelia A. Papakonstanti, Andrew J.H. Smith, Anna C. Need, Elizabeth J. Bradbury, Susan M. Hall, Britta J. Eickholt, Antonio Bilancio, Michelle L. Starkey, Eickholt, Bj, Ahmed, Ai, Davies, M, Papakonstanti, Ea, Pearce, W, Starkey, Ml, Bilancio, Antonio, Need, Ac, Smith, Aj, Hall, Sm, Hamers, Fp, Giese, Kp, Bradbury, Ej, and Vanhaesebroeck, B.

Subjects

Nervous system, Male, Pathology, RHOA, lcsh:Medicine, Biochemistry, Cell Biology/Cell Signaling, Mice, Phosphatidylinositol 3-Kinases, 0302 clinical medicine, Small GTPase, lcsh:Science, Cells, Cultured, Phosphoinositide-3 Kinase Inhibitors, Mice, Knockout, 0303 health sciences, Multidisciplinary, biology, Kinase, Neuroscience/Neurodevelopment, Immunohistochemistry, Sciatic Nerve, Cell biology, medicine.anatomical_structure, Peripheral nerve injury, Science & Technology - Other Topics, Electrophoresis, Polyacrylamide Gel, Neuroscience/Neurobiology of Disease and Regeneration, Research Article, Gene isoform, medicine.medical_specialty, Class I Phosphatidylinositol 3-Kinases, General Science & Technology, Cell Biology/Neuronal Signaling Mechanisms, Morpholines, Cell Biology/Developmental Molecular Mechanisms, Blotting, Western, 03 medical and health sciences, MD Multidisciplinary, medicine, Animals, Neurons, Afferent, Protein kinase B, PI3K/AKT/mTOR pathway, 030304 developmental biology, Science & Technology, MULTIDISCIPLINARY SCIENCES, lcsh:R, PTEN Phosphohydrolase, Axons, Nerve Regeneration, Developmental Biology/Neurodevelopment, nervous system, Chromones, Cell Biology/Neuronal and Glial Cell Biology, biology.protein, lcsh:Q, rhoA GTP-Binding Protein, Proto-Oncogene Proteins c-akt, 030217 neurology & neurosurgery

Abstract

The expression and function of the 8 distinct catalytic isoforms of PI 3-kinase (PI3K) in the nervous system are unknown. Whereas most PI3Ks have a broad tissue distribution, the tyrosine kinase-linked p110delta isoform has previously been shown to be enriched in leukocytes. Here we report that p110delta is also highly expressed in the nervous system. Inactivation of p110delta in mice did not affect gross neuronal development but led to an increased vulnerability of dorsal root ganglia neurons to exhibit growth cone collapse and decreases in axonal extension. Loss of p110delta activity also dampened axonal regeneration following peripheral nerve injury in adult mice and impaired functional recovery of locomotion. p110delta inactivation resulted in reduced neuronal signaling through the Akt protein kinase, and increased activity of the small GTPase RhoA. Pharmacological inhibition of ROCK, a downstream effector of RhoA, restored axonal extension defects in neurons with inactive p110delta, suggesting a key role of RhoA in p110delta signaling in neurons. Our data identify p110delta as an important signaling component for efficient axonal elongation in the developing and regenerating nervous system.

Published

2007

34. Activation of membrane androgen receptors potentiates the antiproliferative effects of paclitaxel on human prostate cancer cells

Author

Panayiotis A. Theodoropoulos, Elias Castanas, Achille Gravanis, Christos Stournaras, Marilena Kampa, Efstathios N. Stathopoulos, Ploutarchos Anezinis, Christina Kogia, Evangelia A. Papakonstanti, Ioannis Charalampopoulos, Anastassia Hatzoglou, Laboratory of Experimental Endocrinology, University of Crete [Heraklion] (UOC), Dept of Biochemistry, Urology Clinic, Venizelion Hospital, Dept of Pharmacology, Department of Pathology, University of Crete [Heraklion] (UOC)-School of Medicine, Transduction du signal et oncogénèse, and Institut Curie [Paris]-Institut National de la Santé et de la Recherche Médicale (INSERM)

Subjects

Male, Cancer Research, Cell Membrane Permeability, Apoptosis, Pharmacology, MESH: Dose-Response Relationship, Drug, chemistry.chemical_compound, Mice, 0302 clinical medicine, Antineoplastic Combined Chemotherapy Protocols, Tumor Cells, Cultured, MESH: Animals, Testosterone, MESH: Cell Membrane Permeability, Receptor, Cytoskeleton, 0303 health sciences, Mice, Inbred BALB C, Serum Albumin, Bovine, 3. Good health, MESH: Antineoplastic Combined Chemotherapy Protocols, Oncology, Paclitaxel, Receptors, Androgen, 030220 oncology & carcinogenesis, MESH: Receptors, Androgen, medicine.drug_class, MESH: Mice, Inbred BALB C, MESH: Testosterone, Mice, Nude, [SDV.BC]Life Sciences [q-bio]/Cellular Biology, Biology, 03 medical and health sciences, MESH: Cell Proliferation, LNCaP, medicine, MESH: Mice, Nude, MESH: Cytoskeleton, Animals, Humans, MESH: Paclitaxel, MESH: Tumor Cells, Cultured, MESH: Mice, 030304 developmental biology, Cell Proliferation, MESH: Humans, Dose-Response Relationship, Drug, Cell growth, MESH: Apoptosis, Cell Membrane, Prostatic Neoplasms, Androgen, MESH: Male, Androgen receptor, chemistry, MESH: Prostatic Neoplasms, Cancer cell, Cancer research, MESH: Serum Albumin, Bovine, MESH: Cell Membrane

Abstract

Genomic signaling mechanisms require a relatively long time to get into action and represent the main way through which steroid hormones affect target cells. In addition, steroids may rapidly activate cellular functions by non-genomic signaling mechanisms involving membrane sites. Understanding in depth the molecular mechanisms of the non-genomic action represents an important frontier for developing new and more selective pharmacologic tools for endocrine therapies. In the present study, we report that membrane-impermeable testosterone-bovine serum albumin (BSA) acts synergistically with paclitaxel in modifying actin and tubulin cytoskeleton dynamics in LNCaP (androgen sensitive) and DU-145 (androgen insensitive) human prostate cancer cell lines. In addition, coincubation of either cell line with testosterone-BSA and paclitaxel induced inhibition of cell proliferation and apoptosis. Finally, in vivo experiments in LNCaP and DU-145 tumor xenografts in nude mice showed that both agents decrease tumor mass, whereas testosterone-BSA enhances the effect of paclitaxel. Our findings suggest that chronic activation of membrane androgen receptors in vitro and in vivo facilitates and sustains for a longer time the antitumoral action of cytoskeletal acting agents. [Mol Cancer Ther 2006;5(5):1342–51]

Published

2006

35. Membrane androgen receptor activation induces apoptotic regression of human prostate cancer cells in vitro and in vivo

Author

Achille Gravanis, Christina Kogia, Marilena Kampa, Ploutarchos Anezinis, Christos Stournaras, Constantina Dambaki, Anastassia Hatzoglou, Elias Castanas, Efstathios N. Stathopoulos, Evangelia A. Papakonstanti, Ioannis Charalampopoulos, and Panayiotis A. Theodoropoulos

Subjects

Male, medicine.medical_specialty, medicine.drug_class, Endocrinology, Diabetes and Metabolism, Clinical Biochemistry, Transplantation, Heterologous, Mice, Nude, Apoptosis, Biology, urologic and male genital diseases, Biochemistry, Flutamide, Oligodeoxyribonucleotides, Antisense, Prostate cancer, chemistry.chemical_compound, Mice, Endocrinology, DU145, Cell Movement, Internal medicine, Cell Line, Tumor, LNCaP, medicine, Cell Adhesion, Animals, Humans, Testosterone, Mice, Inbred BALB C, Biochemistry (medical), Cell Membrane, Prostatic Neoplasms, Serum Albumin, Bovine, medicine.disease, Androgen, Flow Cytometry, Androgen receptor, chemistry, Receptors, Androgen, Membrane androgen receptor

Abstract

Nongenomic androgen actions imply mechanisms different from the classical intracellular androgen receptor (iAR) activation. We have recently reported the identification of a membrane androgen receptor (mAR) on LNCaP human prostate cancer cells, mediating testosterone signal transduction within minutes. In the present study we provide evidence that activation of mAR by nonpermeable, BSA-coupled testosterone results in 1) inhibition of LNCaP cell growth (with a 50% inhibitory concentration of 5.08 nM, similar to the affinity of testosterone for membrane sites); 2) induction in LNCaP cells of both apoptosis and the proapoptotic Fas protein; and 3) a significant decrease in migration, adhesion, and invasion of iAR-negative DU145 human prostate cancer cells. These actions persisted in the presence of antiandrogen flutamide or after decreasing the content of iAR in LNCaP cells by iAR antisense oligonucleotides. Testosterone-BSA was also effective in inducing apoptosis of DU145 human prostate cancer cells, negative for iAR, but expressing mAR sites. In LNCaP cell-inoculated nude mice, treatment with testosterone-BSA (4.8 mg/kg body weight) for 1 month resulted in a 60% reduction of tumor size compared with that in control animals receiving only BSA, an effect that was not affected by the antiandrogen flutamide. Our findings suggest that activators of mAR may represent a new class of antitumoral agents of prostate cancer.

Published

2004

36. Distinct signaling pathways regulate differential opioid effects on actin cytoskeleton in malignant MCF7 and nonmalignant MCF12A human breast epithelial cells

Author

Marilena Kampa, Elias Castanas, Kostas Krasagakis, Anna Tsapara, Evangelia A. Papakonstanti, Galatea Kallergi, and Christos Stournaras

Subjects

Narcotics, Antineoplastic Agents, Breast Neoplasms, macromolecular substances, Phosphatidylinositol 3-Kinases, Tumor Cells, Cultured, Humans, Phosphorylation, Cytoskeleton, Epithelial polarity, Microscopy, Confocal, biology, Actin cytoskeleton reorganization, Actin remodeling, Caseins, Cell Biology, Vinculin, Protein-Tyrosine Kinases, Actin cytoskeleton, Actins, Peptide Fragments, Cell biology, rac GTP-Binding Proteins, Focal Adhesion Kinase 1, Focal Adhesion Protein-Tyrosine Kinases, biology.protein, Cancer research, Female, Lamellipodium, Villin, Filopodia, Cell Division, Signal Transduction

Abstract

The mechanisms through which opioids regulate the activity of malignant breast epithelial cells are currently unknown. In the present study we report the differential actin cytoskeleton reorganization induced by opioids in malignant (MCF7) and nonmalignant (MCF12A) breast epithelial cells expressing functional opioid receptors. Exposure of MCF7 cells to the opioid agonist alpha(s1) casomorphin induced important actin assembly and reorganization, including the formation of filopodia and lamellipodia. In contrast, incubation of MCF12A cells with alpha(s1) casomorphin revealed a partial but transient disassembly of actin microfilaments. Immunoprecipitation and immunoblot analyses showed rapid phosphorylation of focal adhesion kinase (FAK) and vinculin in opioid-treated MCF7 cells. Moreover, FAK associates with phosphatidylinositol-3 (PI-3 kinase), the latter being subsequently phosphorylated and activated. In addition, a substantial activation of the small GTPase Rac1 was observed. Pretreatment of MCF7 cells with the specific PI-3 kinase inhibitor wortmannin abolished both the activation of Rac1 and actin reorganization, while the opioid-induced phosphorylation of FAK and vinculin remained unaffected. Interestingly, in opioid-treated MCF12A cells this signaling cascade remained inactive, while we identified rapid phosphorylation of actin regulating the protein villin. Finally, opioids differentially inhibited cell motility in each cell line. Our data suggest a distinct, opioid-induced, signaling pathway activated in malignant breast epithelial cells, leading to important actin reorganization. These findings may indicate a potential antineoplastic role of opiates, based on the activation of differential signaling mechanisms.

Published

2003

37. A rapid, nongenomic, signaling pathway regulates the actin reorganization induced by activation of membrane testosterone receptors

Author

Christos Stournaras, Marilena Kampa, Evangelia A. Papakonstanti, and Elias Castanas

Subjects

Male, rac1 GTP-Binding Protein, macromolecular substances, Biology, Wortmannin, chemistry.chemical_compound, Phosphatidylinositol 3-Kinases, Endocrinology, Cell surface receptor, Tumor Cells, Cultured, Humans, Testosterone, Enzyme Inhibitors, Phosphorylation, Cytoskeleton, Receptor, cdc42 GTP-Binding Protein, Molecular Biology, Phosphoinositide-3 Kinase Inhibitors, Actin cytoskeleton reorganization, Cell Membrane, Neuropeptides, Prostatic Neoplasms, Dihydrotestosterone, Serum Albumin, Bovine, General Medicine, Prostate-Specific Antigen, Protein-Tyrosine Kinases, Actin cytoskeleton, Actins, Cell biology, rac GTP-Binding Proteins, Androstadienes, chemistry, Receptors, Androgen, Focal Adhesion Kinase 1, Focal Adhesion Protein-Tyrosine Kinases, Membrane androgen receptor, Signal transduction, Signal Transduction

Abstract

The human prostate cancer cell line LNCaP bears functional membrane testosterone receptors, which modify the actin cytoskeleton and increase the secretion of prostate-specific antigen (PSA) within minutes. Membrane steroid receptors are, indeed, a newly identified element of steroid action that is different from the classical intracellular sites. In the present work, using a nonpermeable analog of testosterone (testosterone-BSA), we investigated the signaling pathway that is triggered by the membrane testosterone receptors' activation and leads to actin cytoskeleton reorganization. We report that exposure of cells to testosterone-BSA resulted in phosphorylation of focal adhesion kinase (FAK), the association of FAK with the phosphatidylinositol-3 (PI-3) kinase, and the subsequent activation of the latter as well as the activation of the small guanosine triphosphatases Cdc42/Rac1. Pretreatment of cells with the specific PI-3 kinase inhibitor wortmannin abolished both the activation of the small guanosine triphosphatases and the alterations of actin cytoskeleton, whereas it did not affect the phosphorylation of FAK. These findings indicate that PI-3 kinase is activated downstream of FAK and upstream of Cdc42/Rac1, which subsequently regulate the actin organization. Moreover, wortmannin diminished the secretion of PSA, implying that the signaling events described above are responsible for the testosterone-BSA-induced PSA secretion. Our results are discussed under the prism of a possible implication of these membrane receptors in prostate cancer chemotherapy.

Published

2003

38. The human prostate cancer cell line LNCaP bears functional membrane testosterone receptors that increase PSA secretion and modify actin cytoskeleton

Author

Elias Castanas, Marilena Kampa, Anastassia Hatzoglou, Christos Stournaras, Efstathios N. Stathopoulos, and Evangelia A. Papakonstanti

Subjects

Male, Receptors, Cell Surface, Biology, Biochemistry, Filamentous actin, Models, Biological, Actin cytoskeleton organization, chemistry.chemical_compound, Cell surface receptor, LNCaP, Genetics, medicine, Tumor Cells, Cultured, Humans, Cytochalasin, Testosterone, Molecular Biology, Binding Sites, Cell Membrane, Prostatic Neoplasms, Biological Transport, Dihydrotestosterone, Prostate-Specific Antigen, Actin cytoskeleton, Molecular biology, Actin Cytoskeleton, chemistry, Receptors, Androgen, Membrane androgen receptor, Biotechnology, medicine.drug

Abstract

Recent findings have shown that, in addition to the genomic action of steroids, through intracellular receptors, short-time effects could be mediated through binding to membrane sites. In the present study of prostate cancer LNCaP cells, we report that dihydrotestosterone and the non-internalizable analog testosterone-BSA increase rapidly the release of prostate-specific antigen (PSA) in the culture medium. Membrane testosterone binding sites were identified through ligand binding on membrane preparations, flow cytometry, and confocal laser microscopy of the non-internalizable fluorescent analog testosterone-BSA-FITC, on whole cells. Binding on these sites is time- and concentration-dependent and specific for testosterone, presenting a KD of 10.9 nM and a number of 144 sites/mg protein (approximately 13000 sites/cell). Membrane sites differ immunologically for intracellular androgen receptors. The secretion of PSA after membrane testosterone receptor stimulation was inhibited after pretreatment with the actin cytoskeleton disrupting agent cytochalasin B. In addition, membrane testosterone binding modifies the intracellular dynamic equilibrium of monomeric to filamentous actin and remodels profoundly the actin cytoskeleton organization. These results are discussed in the context of a possible involvement of these sites in cancer chemotherapy.

Published

2002

39. Opioid agonists modify breast cancer cell proliferation by blocking cells to the G2/M phase of the cycle: involvement of cytoskeletal elements

Author

Christos Stournaras, Elias Castanas, Pierre-Marie Martin, Christophe Dussert, Evangelia A. Papakonstanti, Efstathia Bakogeorgou, Anastassia Hatzoglou, and Simone Panagiotou

Subjects

G2 Phase, medicine.drug_class, Mitosis, Breast Neoplasms, Ethylketocyclazocine, Pharmacology, Biology, Microfilament, Biochemistry, medicine, Tumor Cells, Cultured, Humans, Cytoskeleton, Molecular Biology, Cell growth, Etorphine, Cell Biology, Cell cycle, Actin cytoskeleton, Actins, Analgesics, Opioid, Opioid, Diprenorphine, Opioid antagonist, medicine.drug

Abstract

Opioids decrease cell proliferation in different systems including breast, prostate, lung, kidney, and intestine, through an interaction with opioid as well as other membrane-receptor systems (somatostatin, cholinergic), through an unidentified mechanism. Recently, we have reported an interaction of taxol with opioid membrane sites (BBRC 235, 201-204, 1997), and an involvement of opioids to the modification of actin cytoskeleton in renal OK cells (J Cell Biochem. [19981 70:60-69), indicating a possible action of the opioid effect. In the present work, we have examined the effect of two general opioid agonists (ethylketocyclazocine and etorphine) on the cell cycle, in human breast cancer T47D cells, as well as a possible modification of the cellular cytoskeleton under their action, in order to explain the antiproliferative effect of these agents. These two opioids produce a dose-dependent and reversible decrease of the proliferation of T47D cells, with a maximum attained at 10(-8) M. The addition of 10(-8) M of either opioid produced a significant increase of the number of cells arrested in the G2/M phase. Confocal laser microscopy revealed a modification of the actin and tubulin microfilaments, with a clear redistribution at the periphery of the cell, reversed by the addition of the general opioid antagonist diprenorphine. Furthermore, differences between the two opioids were obvious, attributed to the different receptor affinity of each agent. The observed redistribution of actin and tubulin cytoskeletal elements gives therefore a possible answer of the antiproliferative action of opioids. The modification of the cytoskeleton, directly involved to cell division, might provoke a "mechanical" obstacle, which could be the reason of the antiproliferative effect of these agonists. Furthermore, the observed tubulin-opioid interaction by opioids provides a possible explanation of the arrest at the G2/M phase of T47D cells under opioid treatment. Nevertheless, although the observed interaction of opioids with cytoskeletal elements gives a plausible answer of the antiproliferative effects of the agents, this might not be the only action of these agents in cell proliferation. Other, direct or indirect, genomic actions, which which remains to be elucidated, might be taken into consideration.

Published

1999