Search

Your search keyword '"Pompili, Simona"' showing total 28 results
Start Over Author "Pompili, Simona" Search Limiters Peer Reviewed
28 results on '"Pompili, Simona"'

7. PPAR-Gamma Orchestrates EMT, AGE, and Cellular Senescence Pathways in Colonic Epithelium and Restrains the Progression of IBDs.

Author

Pompili, Simona, Vetuschi, Antonella, Latella, Giovanni, Smakaj, Amarildo, Sferra, Roberta, and Cappariello, Alfredo

Subjects
*RECEPTOR for advanced glycation end products (RAGE), *CELLULAR aging, *ADVANCED glycation end-products, *EXTRACELLULAR matrix proteins, *INFLAMMATORY bowel diseases, *TRANSFORMING growth factors
Abstract

Intestinal fibrosis, the most common complication of inflammatory bowel disease (IBD), is characterized by an uncontrolled deposition of extracellular matrix proteins leading to complications resolvable only with surgery. Transforming growth factor is the key player in the epithelial-mesenchymal transition (EMT) and fibrogenesis process, and some molecules modulating its activity, including peroxisome proliferator-activated receptor (PPAR)-γ and its agonists, exert a promising antifibrotic action. The purpose of this study is to evaluate the contribution of signaling other than EMT, such as the AGE/RAGE (advanced glycation end products/receptor of AGEs) and the senescence pathways, in the etiopathogenesis of IBD. We used human biopsies from control and IBD patients, and we used a mouse model of colitis induced by dextran-sodium-sulfate (DSS), without/with treatments with GED (PPAR-gamma-agonist), or 5-aminosalicylic acid (5-ASA), a reference drug for IBD treatment. In patients, we found an increase in EMT markers, AGE/RAGE, and senescence signaling activation compared to controls. Consistently, we found the overexpression of the same pathways in DSS-treated mice. Surprisingly, the GED reduced all the pro-fibrotic pathways, in some circumstances more efficiently than 5-ASA. Results suggest that IBD patients could benefit from a combined pharmacological treatment targeting simultaneously different pathways involved in pro-fibrotic signals. In this scenario, PPAR-gamma activation could be a suitable strategy to alleviate the signs and symptoms of IBD and also its progression. [ABSTRACT FROM AUTHOR]

Published
2023
Full Text
View/download PDF

11. Extracellular Vesicles and Resistance to Anticancer Drugs: A Tumor Skeleton Key for Unhinging Chemotherapies.

Author

Pompili, Simona, Vetuschi, Antonella, Sferra, Roberta, and Cappariello, Alfredo

Subjects
DRUG resistance, EXTRACELLULAR vesicles, ANTINEOPLASTIC agents, CLINICAL medicine, CARRIER proteins, LEBER'S hereditary optic atrophy
Abstract

Although surgical procedures and clinical care allow reaching high success in fighting most tumors, cancer is still a formidable foe. Recurrence and metastatization dampen the patients' overall survival after the first diagnosis; nevertheless, the large knowledge of the molecular bases drives these aspects. Chemoresistance is tightly linked to these features and is mainly responsible for the failure of cancer eradication, leaving patients without a crucial medical strategy. Many pathways have been elucidated to trigger insensitiveness to drugs, generally associated with the promotion of tumor growth, aggressiveness, and metastatisation. The main mechanisms reported are the expression of transporter proteins, the induction or mutations of oncogenes and transcription factors, the alteration in genomic or mitochondrial DNA, the triggering of autophagy or epithelial-to-mesenchymal transition, the acquisition of a stem phenotype, and the activation of tumor microenvironment cells. Extracellular v esicles (EVs) can directly transfer or epigenetically induce to a target cell the molecular machinery responsible for the acquisition of resistance to drugs. In this review, we resume the main body of knowledge supporting the crucial role of EVs in the context of chemoresistance, with a particular emphasis on the mechanisms related to some of the main drugs used to fight cancer. [ABSTRACT FROM AUTHOR]

Published
2022
Full Text
View/download PDF

13. Article Dual CXCR4 and E-Selectin Inhibitor, GMI-1359, Shows Anti-Bone Metastatic Effects and Synergizes with Docetaxel in Prostate Cancer Cell Intraosseous Growth.

Author

Festuccia, Claudio, Mancini, Andrea, Gravina, Giovanni Luca, Colapietro, Alessandro, Vetuschi, Antonella, Pompili, Simona, Ventura, Luca, Monache, Simona Delle, Iorio, Roberto, Del Fattore, Andrea, Fogler, William, and Magnani, John

Subjects
CANCER cell growth, CASTRATION-resistant prostate cancer, CXCR4 receptors, PROSTATE cancer, DOCETAXEL
Abstract

Metastatic castration resistant prostate cancer (mCRPC) relapses due to acquired resistance to docetaxel-based chemotherapy and remains a major threat to patient survival. In this report, we tested the effectiveness of a dual CXCR4/E-selectin antagonist, GM-I1359, in vitro and in vivo, as a single agent or in combination with docetaxel (DTX). This agent was compared to the single CXCR4 antagonist, CTCE-9908, and E-selectin antagonist, GMI-1271. Here we demonstrate that CXCR4 antagonism reduced growth and enhanced DTX treatment in PCa cell lines as well as restored DTX effectiveness in DTX-resistant cell models. The efficacy of dual antagonist was higher respect to those observed for single CXCR4 antagonism. GM1359 impacted bone marrow colonization and growth in intraventricular and intratibial cell injection models. The anti-proliferative effects of GMI-1359 and DTX correlated with decreased size, osteolysis and serum levels of both mTRAP and type I collagen fragment (CTX) in intra-osseous tumours suggesting that the dual CXCR4/E-selectin antagonist was a docetaxel-sensitizing agent for bone metastatic growth. Single agent CXCR4 (CTCE-9908) and E-selectin (GMI-1271) antagonists resulted in lower sensitizing effects compared to GMI-1359. These data provide a biologic rationale for the use of a dual E-selectin/CXCR4 inhibitor as an adjuvant to taxane-based chemotherapy in men with mCRPC to prevent and reduce bone metastases. [ABSTRACT FROM AUTHOR]

Published
2020
Full Text
View/download PDF

14. Role of the Angiogenic Factors in Cholangiocarcinoma.

Author

Mancinelli, Romina, Mammola, Caterina Loredana, Sferra, Roberta, Pompili, Simona, Vetuschi, Antonella, and Pannarale, Luigi

Subjects
VASCULAR endothelial growth factors, PLACENTAL growth factor, CHOLANGIOCARCINOMA, TUMOR markers, GROWTH factors, BILE ducts
Abstract

Angiogenesis plays a fundamental role in tumor growth and progression. It is regulated by several growth factors, including vascular endothelial growth factor protein family (VEGF) and its receptors, which are probably the most important factors responsible for the development of new vessels. The VEGF family includes several members: VEGF-A, VEGF-B, VEGF-C, VEGF-D, VEGF-E, placental growth factor (PlGF), and their receptors VEGFR-1, VEGFR-2 and VEGFR-3. Other relevant factors are represented by angiopoietins, thrombospondin-1, and endothelins. However, since the therapeutic benefit associated with VEGF-targeted therapy is really complex, a better understanding of these pathways will lead to future advances in the use of these agents for clinic management of tumors. Here we present a review regarding the role of angiogenic factors in cholangiocarcinoma, which arise from cholangiocytes, the epithelial cells of bile ducts. They are rare and aggressive neoplasms with a poor prognosis and limited treatment options, classified as intrahepatic, perihilar, and distal cholangiocarcinoma based on their anatomical location. Therefore, the identification of specific signaling pathways or new tumor biomarkers is crucial in order to develop more effective anti-angiogenic therapies. [ABSTRACT FROM AUTHOR]

Published
2019
Full Text
View/download PDF

15. Immunolocalization of Advanced Glycation End Products, Mitogen Activated Protein Kinases, and Transforming Growth Factor-β/Smads in Pelvic Organ Prolapse.

Author

Vetuschi, Antonella, Pompili, Simona, Gallone, Anna, D'Alfonso, Angela, Carbone, Maria Gabriella, Carta, Gaspare, Festuccia, Claudio, Gaudio, Eugenio, Colapietro, Alessandro, and Sferra, Roberta

Subjects
ADVANCED glycation end-products, TRANSFORMING growth factors, PELVIC organ prolapse, PROTEIN kinases, MATRIX metalloproteinases
Abstract

Collagen and matrix metalloproteinases (MMP) play a pivotal role in the pathophysiology of Pelvic Organ Prolapse (POP) as a switch between type I and III collagen together with a simultaneous activation of MMPs have been observed in the vaginal wall. The aim of this study was to evaluate the Advanced Glycation End (AGE) products, ERK1/2 and transforming growth factor (TGF)-β/Smad pathway expression in muscularis propria in women with POP compared with control patients. We examined 20 patients with POP and 10 control patients treated for uterine fibromatosis. Immunohistochemical analysis using AGE, RAGE, ERK1/2, Smads-2/3, Smad-7, MMP-3, and collagen I-III, TIMP, and α-SMA were performed. Smad-2/3, Smad-7, AGE, ERK1/2, p-ERK, and p-Smad3 were also evaluated using Western-blot analysis. POP samples from the anterior vaginal wall showed disorganization of the normal muscularis architecture. In POP samples, AGE, ERK1/2, Smad-2/3, MMP-3, and collagen III were upregulated in muscularis whereas in controls, Smad-7 and collagen I were increased. The receptor for AGEs (RAGE) was mild or absent both in controls and prolapse. We demonstrated the involvement of these markers in women with POP but further studies are required to elucidate if the overexpression of these molecules could play a crucial role in the pathophysiology of POP disease. [ABSTRACT FROM AUTHOR]

Published
2018
Full Text
View/download PDF

17. The novel CXCR4 antagonist, PRX177561, reduces tumor cell proliferation and accelerates cancer stem cell differentiation in glioblastoma preclinical models.

Author

Gravina, Giovanni Luca, Mancini, Andrea, Colapietro, Alessandro, Vitale, Flora, Vetuschi, Antonella, Pompili, Simona, Rossi, Giulia, Marampon, Francesco, Richardson, Peter J., Patient, Lee, Burbidge, Stephen, and Festuccia, Claudio

Subjects
BRAIN tumors, CANCER cell proliferation, GLIOBLASTOMA multiforme, CELL proliferation, GLIOMAS
Abstract

Glioblastoma is the most frequent and the most lethal primary brain tumor among adults. Standard of care is the association of radiotherapy with concomitant or adjuvant temozolomide. However, to date, recurrence is inevitable. The CXCL12/CXCR4 pathway is upregulated in the glioblastoma tumor microenvironment regulating tumor cell proliferation, local invasion, angiogenesis, and the efficacy of radio-chemotherapy. In this study, we evaluated the effects of the novel CXCR4 antagonist, PRX177561, in preclinical models of glioblastoma. CXCR4 expression and PRX177561 effects were assessed on a panel of 12 human glioblastoma cells lines and 5 patient-derived glioblastoma stem cell cultures. Next, the effect of PRX177561 was tested in vivo, using subcutaneous injection of U87MG, U251, and T98G cells as well as orthotopic intrabrain inoculation of luciferase-transfected U87MG cells. Here we found that PRX177561 impairs the proliferation of human glioblastoma cell lines, increases apoptosis, and reduces CXCR4 expression and cell migration in response to stromal cell-derived factor 1alpha in vitro. PRX177561 reduced the expression of stem cell markers and increased that of E-cadherin and glial fibrillary acidic protein in U87MG cells consistent with a reduction in cancer stem cells. In vivo, PRX177561 reduced the weight and increased the time to progression of glioblastoma subcutaneous tumors while increasing disease-free survival and overall survival of mice bearing orthotopic tumors. Our findings suggest that targeting stromal cell-derived factor 1 alpha/CXCR4 axis by PRX177561 might represent a novel therapeutic approach against glioblastoma and support further investigation of this compound in more complex preclinical settings in order to determine its therapeutic potential. [ABSTRACT FROM AUTHOR]

Published
2017
Full Text
View/download PDF

19. Role of glycogen synthase kinase-3β and PPAR-γ on epithelial-to-mesenchymal transition in DSS-induced colorectal fibrosis.

Author

Di Gregorio, Jacopo, Sferra, Roberta, Speca, Silvia, Vetuschi, Antonella, Dubuquoy, Caroline, Desreumaux, Pierre, Pompili, Simona, Cristiano, Loredana, Gaudio, Eugenio, Flati, Vincenzo, and Latella, Giovanni

Subjects
GLYCOGEN synthases, PEROXISOME proliferator-activated receptors, CELL transformation, EXTRACELLULAR matrix, MESENCHYMAL stem cells, MYOFIBROBLASTS
Abstract

Background: Intestinal fibrosis is characterized by abnormal production and deposition of extracellular matrix (ECM) proteins by activated myofibroblasts. The main progenitor cells of activated myofibroblasts are the fibroblasts and the epithelial cells, the latter through the epithelial-mesenchymal transition (EMT). Aim: To evaluate the action of the new PPAR-γ modulator, GED-0507-34 Levo (GED) on the expression of EMT associated and regulatory proteins such as TGF-β, Smad3, E-cadherin, Snail, ZEB1, β-catenin, and GSK-3β, in a mouse model of DSS-induced intestinal fibrosis. Methods: Chronic colitis and fibrosis were induced by oral administration of 2.5% DSS (w/v) for 6 weeks. GW9662 (GW), a selective PPAR-γ inhibitor, was also administered by intraperitoneal injection at the dose of 1 mg/kg/day combined with GED treatment. All drugs were administered at the beginning of the second cycle of DSS (day 12). 65 mice were randomly divided into five groups (H2O as controls n = 10, H2O+GED n = 10, DSS n = 15, DSS+GED n = 15, DSS+GED+GW n = 15). The colon was excised for macroscopic examination and histological and morphometric analyses. The level of expression of molecules involved in EMT and fibrosis, like TGF-β, Smad3, E-cadherin, Snail, ZEB1, β-catenin, GSK-3β and PPAR-γ, was assessed by immunohistochemistry, immunofluorescence, western blot and Real Time PCR. Results: GED improved the DSS-induced chronic colitis and fibrosis. GED was able to reduce the expression of the main fibrosis markers (α-SMA, collagen I-III and fibronectin) as well as the pivotal pro-fibrotic molecules IL-13, TGF-β and Smad3, while it increased the anti-fibrotic PPAR-γ. All these GED effects were nullified by co-administration of GW with GED. Furthermore, GED was able to normalize the expression levels of E-cadherin and β-catenin and upregulated GSK-3β, that are all known to be involved both in EMT and fibrosis. Conclusions: The DSS-induced intestinal fibrosis was improved by the new PPAR-γ modulator GED-0507-34 Levo through the modulation of EMT mediators and pro-fibrotic molecules and through GSK-3β induction. [ABSTRACT FROM AUTHOR]

Published
2017
Full Text
View/download PDF

20. PPAR-Gamma coordinates EMT, AGE, and senescence signaling and mitigates the intestinal fibrosis in IBDs.

Author

Pompili, Simona, Cappariello, Alfredo, Latella, Giovanni, Sferra, Roberta, and Vetuschi, Antonella

Abstract

The article focuses on investigating the contribution of AGE/RAGE (advanced glycation end products/receptor of AGEs) and senescence pathways in the context of inflammatory bowel disease (IBD) and highlights the potential of PPAR-γ activation, particularly with GED (PPAR-gamma-agonist).

Published
2023

22. Ferroptosis-resistance supports cellular senescence in the development of liver injury in an experimental mouse model of Nonalcoholic fatty liver disease/Nonalcoholic steatohepatitis (NAFLD/NASH) induced by "Wester-style" diet assumption.

Author

Pompili, Simona, Cappariello, Alfredo, Gaudio, Eugenio, Onori, Paolo, Latella, Giovanni, Sferra, Roberta, and Vetuschi, Antonella

Subjects
*NON-alcoholic fatty liver disease, *CELLULAR aging, *LABORATORY mice, *ANIMAL disease models, *WESTERN diet, *FAT
Abstract

NAFLD/NASH is a worldwide and unresolved health problem. Several factors concur to its onset and among them, a crucial cause is represented by unbalanced alimentary habits (1). One of the worst regimens for the liver fitness is the so called "Western-style diet" (WSD), characterized by an excessive assumption of fats and sugars. This dietary regimen induces severe alterations in liver parenchyma ranging from simple steatosis to fibrosis and hepatocarcinoma (2,3). Many different mechanisms have been considered as key players of the liver damage, including most recently senescence and ferroptosis. Indeed, several studies revealed that an alteration of these processes is involved in the exacerbation of many diseases, among which nonalcoholic livers alterations. However, despite senescence and ferroptosis share several molecular players and are triggered by the reactive oxygen species (ROS), limited studies focused their attention in the possible direct connection between senescence and ferroptosis in the progression of NAFLD/NASH. On these bases, we analyzed the molecular pathways of the senescence and ferroptosis in livers of a mouse model of WSD. In particular, we used an Amylin-modified liver NASH mouse model fed for 23 weeks with an unbalanced diet (fat 40%, sucrose 20%, cholesterol 2% Kcal). The main features of liver injury such as hepatomegaly, hepatic lipidic accumulation, elevated plasmatic ALT, inflammatory infiltration was confirmed, as well as an increase of apoptosis rate, Ki67 and p53 expression. On the senescence side, the number of β -galactosidase (β-gal) positive cells increased, as well as expression of secretory associated senescent phenotype (SASP) members interleukin-(Il)-6 and matrix metalloprotease (MMP)-1. On the ferroptosis side, iron overload and increase of DNA damage revealed by positiveness for phospo-histone H2 (p-H2AX) were confirmed. The expression of glutathione peroxidase-4, gpx-4, counteracting iron-mediated ferroptotic cell dead, was also increased. Notably, a high number of gpx-4 and β-gal positive cells were noted in WSD fed mice compared to control. In conclusion, our data suggest that a mechanism of ferroptosis resistance mediated by gpx4 occurs in senescent cells, fostering the deterioration of the liver fitness. [ABSTRACT FROM AUTHOR]

Published
2021

23. Deep characterization of pro-fibrotic, pro-inflammatory and senescent signaling in the intestinal inflammatory bowel diseases (IBD).

Author

Pompili, Simona, Vetuschi, Antonella, Latella, Giovanni, Sferra, Roberta, and Cappariello, Alfredo

Subjects
*INFLAMMATORY bowel diseases, *INTESTINES, *EXTRACELLULAR matrix proteins, *ADVANCED glycation end-products
Abstract

The article offers information on the deep characterization of pro-fibrotic, proinflammatory and senescent signaling in the intestinal inflammatory bowel diseases (IBD) . It mentions that inflammatory bowel disease (IBD), including Chron's disease (CD) and ulcerative colitis (UC), constitute a broad spectrum of chronic inflammatory disorders affecting the gastrointestinal tract.

Published
2022

24. Prolonged Chronic Consumption of a High Fat with Sucrose Diet Alters the Morphology of the Small Intestine.

Author

Sferra, Roberta, Pompili, Simona, Cappariello, Alfredo, Gaudio, Eugenio, Latella, Giovanni, and Vetuschi, Antonella

Subjects
*HIGH-carbohydrate diet, *HIGH-fat diet, *SMALL intestine, *LIPID metabolism, *LEPTIN receptors, *FAT
Abstract

(1) The high-fat diet (HFD) of western countries has dramatic effect on the health of several organs, including the digestive tract, leading to the accumulation of fats that can also trigger a chronic inflammatory process, such as that which occurs in non-alcohol steatohepatitis. The effects of a HFD on the small intestine, the organ involved in the absorption of this class of nutrients, are still poorly investigated. (2) To address this aspect, we administered a combined HFD with sucrose (HFD w/Suc, fat: 58% Kcal) regimen (18 months) to mice and investigated the morphological and molecular changes that occurred in the wall of proximal tract of the small intestine compared to the intestine of mice fed with a standard diet (SD) (fat: 18% Kcal). (3) We found an accumulation of lipid droplets in the mucosa of HFD w/Suc-fed mice that led to a disarrangement of mucosa architecture. Furthermore, we assessed the expression of several key players involved in lipid metabolism and inflammation, such as perilipin, leptin, leptin receptor, PI3K, p-mTOR, p-Akt, and TNF-α. All these molecules were increased in HFD mice compared to the SD group. We also evaluated anti-inflammatory molecules like adiponectin, adiponectin receptor, and PPAR-γ, and observed their significant reduction in the HFD w/Suc group compared to the control. Our data are in line with the knowledge that improper eating habits present a primary harmful assault on the bowel and the entire body's health. (4) These results represent a promising starting point for future studies, helping to better understand the complex and not fully elucidated spectrum of intestinal alterations induced by the overconsumption of fat. [ABSTRACT FROM AUTHOR]

Published
2021
Full Text
View/download PDF

25. The Brain Penetrating and Dual TORC1/TORC2 Inhibitor, RES529, Elicits Anti-Glioma Activity and Enhances the Therapeutic Effects of Anti-Angiogenetic Compounds in Preclinical Murine Models.

Author

Gravina, Giovanni Luca, Mancini, Andrea, Colapietro, Alessandro, Delle Monache, Simona, Sferra, Roberta, Pompili, Simona, Vitale, Flora, Martellucci, Stefano, Marampon, Francesco, Mattei, Vincenzo, Biordi, Leda, Sherris, David, and Festuccia, Claudio

Subjects
NEOVASCULARIZATION inhibitors, ANIMAL experimentation, CELL lines, GLIOMAS, MICE, PHOSPHOTRANSFERASES, VASCULAR endothelial growth factors, BEVACIZUMAB, SIGNAL peptides, THERAPEUTICS
Abstract

Background. Glioblastoma multiforme (GBM) is a devastating disease showing a very poor prognosis. New therapeutic approaches are needed to improve survival and quality of life. GBM is a highly vascularized tumor and as such, chemotherapy and anti-angiogenic drugs have been combined for treatment. However, as treatment-induced resistance often develops, our goal was to identify and treat pathways involved in resistance to treatment to optimize the treatment strategies. Anti-angiogenetic compounds tested in preclinical and clinical settings demonstrated recurrence associated to secondary activation of the phosphatidylinositol 3-kinase (PI3K)/AKT/mTOR pathway. Aims. Here, we determined the sensitizing effects of the small molecule and oral available dual TORC1/TORC2 dissociative inhibitor, RES529, alone or in combination with the anti-VEGF blocking antibody, bevacizumab, or the tyrosine kinase inhibitor, sunitinib, in human GBM models. Results. We observed that RES529 effectively inhibited dose-dependently the growth of GBM cells in vitro counteracting the insurgence of recurrence after bevacizumab or sunitinib administration in vivo. Combination strategies were associated with reduced tumor progression as indicated by the analysis of Time to Tumor Progression (TTP) and disease-free survival (DSF) as well as increased overall survival (OS) of tumor bearing mice. RES529 was able to reduce the in vitro migration of tumor cells and tubule formation from both brain-derived endothelial cells (angiogenesis) and tumor cells (vasculogenic mimicry). Conclusions. In summary, RES529, the first dual TORC1/TORC2 dissociative inhibitor, lacking affinity for ABCB1/ABCG2 and having good brain penetration, was active in GBM preclinical/murine models giving credence to its use in clinical trial for patients with GBM treated in association with anti-angiogenetic compounds. [ABSTRACT FROM AUTHOR]

Published
2019
Full Text
View/download PDF

26. Can Nrf2 Modulate the Development of Intestinal Fibrosis and Cancer in Inflammatory Bowel Disease?

Author

Pompili, Simona, Sferra, Roberta, Gaudio, Eugenio, Viscido, Angelo, Frieri, Giuseppe, Vetuschi, Antonella, and Latella, Giovanni

Subjects
*INFLAMMATORY bowel diseases, *FIBROSIS, *CANCER, *MORPHOGENESIS, *NEURODEGENERATION
Abstract

One of the main mechanisms carried out by the cells to counteract several forms of stress is the activation of the nuclear factor erythroid 2-related factor (Nrf2) signaling. Nrf2 signaling controls the expression of many genes through the binding of a specific cis-acting element known as the antioxidant response element (ARE). Activation of Nrf2/ARE signaling can mitigate several pathologic mechanisms associated with an autoimmune response, digestive and metabolic disorders, as well as respiratory, cardiovascular, and neurodegenerative diseases. Indeed, several studies have demonstrated that Nrf2 pathway plays a key role in inflammation and in cancer development in many organs, including the intestine. Nrf2 appears to be involved in inflammatory bowel disease (IBD), an immune-mediated chronic and disabling disease, with a high risk of developing intestinal fibrotic strictures and cancer. Currently, drugs able to increase cytoprotective Nrf2 function are in clinical trials or already being used in clinical practice to reduce the progression of some degenerative conditions. The role of Nrf2 in cancer development and progression is controversial, and drugs able to inhibit abnormal levels of Nrf2 are also under investigation. The goal of this review is to analyze and discuss Nrf2-dependent signals in the initiation and progression of intestinal fibrosis and cancers occurring in IBD. [ABSTRACT FROM AUTHOR]

Published
2019
Full Text
View/download PDF

27. Dual PI3 K/mTOR inhibition reduces prostate cancer bone engraftment altering tumor-induced bone remodeling.

Author

Mancini, Andrea, Colapietro, Alessandro, Pompili, Simona, Del Fattore, Andrea, Delle Monache, Simona, Biordi, Leda Assunta, Angelucci, Adriano, Mattei, Vincenzo, Liang, Chris, Gravina, Giovanni Luca, and Festuccia, Claudio

Subjects
PROSTATE cancer, MTOR inhibitors, BONE remodeling, BONE metastasis, OSTEOBLASTS
Abstract

Morbidity in advanced prostate cancer patients is largely associated with bone metastatic events. The development of novel therapeutic strategies is imperative in order to effectively treat this incurable stage of the malignancy. In this context, Akt signaling pathway represents a promising therapeutic target able to counteract biochemical recurrence and metastatic progression in prostate cancer. We explored the therapeutic potential of a novel dual PI3 K/mTOR inhibitor, X480, to inhibit tumor growth and bone colonization using different in vivo prostate cancer models including the subcutaneous injection of aggressive and bone metastatic (PC3) and non-bone metastatic (22rv1) cell lines and preclinical models known to generate bone lesions. We observed that X480 both inhibited the primary growth of subcutaneous tumors generated by PC3 and 22rv1 cells and reduced bone spreading of PCb2, a high osteotropic PC3 cell derivative. In metastatic bone, X480 inhibited significantly the growth and osteolytic activity of PC3 cells as observed by intratibial injection model. X480 also increased the bone disease-free survival compared to untreated animals. In vitro experiments demonstrated that X480 was effective in counteracting osteoclastogenesis whereas it stimulated osteoblast activity. Our report provides novel information on the potential activity of PI3 K/Akt inhibitors on the formation and progression of prostate cancer bone metastases and supports a biological rationale for the use of these inhibitors in castrate-resistant prostate cancer patients at high risk of developing clinically evident bone lesions. [ABSTRACT FROM AUTHOR]

Published
2018
Full Text
View/download PDF

28. Expression of pro-fibrotic and anti-fibrotic molecules in dimethylnitrosamine-induced hepatic fibrosis.

Author

Sferra, Roberta, Vetuschi, Antonella, Pompili, Simona, Gaudio, Eugenio, Speca, Silvia, and Latella, Giovanni

Subjects
*GENE expression, *DIMETHYLNITROSAMINE, *HEPATIC fibrosis, *EXTRACELLULAR matrix, *GROWTH factors
Abstract

Background Hepatic fibrosis is characterized by a progressive accumulation of fibrillar extracellular matrix (ECM) proteins, produced by activated myofibroblasts which are modulated by both profibrotic and antifibrotic factors. Objective To evaluate in vivo the expression of pro-fibrotic molecules like avβ6 integrin, transforming growth factor-β (TGF-β), Smad3, connective tissue growth factor (CTGF) and mammalian target of Rapamycin (mTOR), as well as anti-fibrotic peroxisome proliferator-activated receptor-γ (PPARγ) in an experimental model of chronic hepatitis-associated fibrosis induced by intraperitoneal administration of dimethylnitrosamine (DMN) in mice. Methods Chronic hepatitis was induced in 12 Smad3 wild-type (WT) and 12 knock-out (KO) mice by intraperitoneal DMN administration. Histological, morphometric and immunohistochemical analyses using α-smooth muscle actin (α-SMA), collagen types I–III, TGF-β1, Smad3, avβ6 integrin, CTGF, mTOR and PPARγ antibodies were performed. Results The liver of DMN-treated Smad3 WT mice showed a higher degree of hepatic accumulation of connective tissue compared to KO mice. The expression of α-SMA, collagen I–III and CTGF was increased in Smad3 WT compared to KO mice treated with DMN, associated with a concomitant up-regulation of avβ6, TGFβ, Smad3, and mTOR and a reduction in PPARγ expression. Conclusions These results suggest a possible interaction between pro-fibrotic and anti-fibrotic molecules in the development of hepatic fibrosis. [ABSTRACT FROM AUTHOR]

Published
2017
Full Text
View/download PDF

Catalog

Books, media, physical & digital resources
See catalog results