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2. p63 orchestrates serine and one carbon metabolism enzymes expression in head and neck cancer.

Author

Cappello, Angela, Tosetti, Giulia, Smirnov, Artem, Ganini, Carlo, Yang, Xue, Shi, Yufang, Wang, Ying, Melino, Gerry, Bernassola, Francesca, and Candi, Eleonora

Subjects
CARBON metabolism, GENE expression, HEAD & neck cancer, ENZYME metabolism, SERINE, HOMEOSTASIS, METABOLISM
Abstract

Background: Head and neck squamous cell carcinoma (HNSCC) is characterized by high proliferation and limited differentiation. The altered expression of the p53 family members, and specifically of p63, represents a pivotal event in the pathogenesis of HNSCC. Physiologically, p63 affects metabolism through the direct transactivation of the enzyme hexokinase 2, and subsequently controls the proliferation of epithelial cells; nonetheless, its role in cancer metabolism is still largely unclear. The high energetic demand of cancer and the consequent needs of a metabolic reshape, also involve the serine and glycine catabolic and anabolic pathways, including the one carbon metabolism (OCM), to produce energetic compounds (purines) and to maintain cellular homeostasis (glutathione and S-adenosylmethionine). Results: The involvement in serine/glycine starvation by other p53 family members has been reported, including HNSCC. Here, we show that in HNSCC p63 controls the expression of the enzymes regulating the serine biosynthesis and one carbon metabolism. p63 binds the promoter region of genes involved in the serine biosynthesis as well as in the one carbon metabolism. p63 silencing in a HNSCC cell line affects the mRNA and protein levels of these selected enzymes. Moreover, the higher expression of TP63 and its target enzymes, negatively impacts on the overall survival of HNSCC patients. Conclusion: These data indicate a direct role of p63 in the metabolic regulation of HNSCC with significant clinical effects. [ABSTRACT FROM AUTHOR]

Published
2023
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3. ZNF750: A Novel Prognostic Biomarker in Metastatic Prostate Cancer.

Author

Montanaro, Manuela, Agostini, Massimiliano, Anemona, Lucia, Bonanno, Elena, Servadei, Francesca, Finazzi Agrò, Enrico, Asimakopoulos, Anastasios D., Ganini, Carlo, Cipriani, Chiara, Signoretti, Marta, Bove, Pierluigi, Rugolo, Francesco, Imperiali, Benedetta, Melino, Gerry, Mauriello, Alessandro, and Scimeca, Manuel

Subjects
PROSTATE cancer, METASTASIS, PROSTATE cancer patients, BIOMARKERS, PROSTATE-specific antigen, GLEASON grading system, PROGRESSION-free survival
Abstract

Prostate cancer is the most frequently diagnosed cancer and the fifth leading cause of cancer death among men in 2020. The clinical decision making for prostate cancer patients is based on the stratification of the patients according to both clinical and pathological parameters such as Gleason score and prostate-specific antigen levels. However, these tools still do not adequately predict patient outcome. The aim of this study was to investigate whether ZNF750 could have a role in better stratifying patients, identifying those with a higher risk of metastasis and with the poorest prognosis. The data reported here revealed that ZNF750 protein levels are reduced in human prostate cancer samples, and this reduction is even higher in metastatic samples. Interestingly, nuclear positivity is significantly reduced in patients with metastatic prostate cancer, regardless of both Gleason score and grade group. More importantly, the bioinformatics analysis indicates that ZNF750 expression is positively correlated with better prognosis. Overall, our findings suggest that nuclear expression of ZNF750 may be a reliable prognostic biomarker for metastatic prostate cancer, which lays the foundation for the development of new biological therapies. [ABSTRACT FROM AUTHOR]

Published
2023
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4. No Time to Die: How Kidney Cancer Evades Cell Death.

Author

Ganini, Carlo, Montanaro, Manuela, Scimeca, Manuel, Palmieri, Giampiero, Anemona, Lucia, Concetti, Livia, Melino, Gerry, Bove, Pierluigi, Amelio, Ivano, Candi, Eleonora, and Mauriello, Alessandro

Subjects
RENAL cancer, APOPTOSIS, RENAL cell carcinoma, CANCER cell growth, CANCER cells, CELL death, PYROPTOSIS
Abstract

The understanding of the pathogenesis of renal cell carcinoma led to the development of targeted therapies, which dramatically changed the overall survival rate. Nonetheless, despite innovative lines of therapy accessible to patients, the prognosis remains severe in most cases. Kidney cancer rarely shows mutations in the genes coding for proteins involved in programmed cell death, including p53. In this paper, we show that the molecular machinery responsible for different forms of cell death, such as apoptosis, ferroptosis, pyroptosis, and necroptosis, which are somehow impaired in kidney cancer to allow cancer cell growth and development, was reactivated by targeted pharmacological intervention. The aim of the present review was to summarize the modality of programmed cell death in the pathogenesis of renal cell carcinoma, showing in vitro and in vivo evidence of their potential role in controlling kidney cancer growth, and highlighting their possible therapeutic value. [ABSTRACT FROM AUTHOR]

Published
2022
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5. The efficacy of a suppository based on Phenolmicin P3 and Bosexil (Mictalase®) in control of irritative symptoms in patients undergoing thulium laser enucleation of prostate: a single-center, randomized, controlled, open label, phase III study.

Author

Bertolo, Riccardo, Cipriani, Chiara, Vittori, Matteo, Carilli, Marco, Maiorino, Francesco, Iacovelli, Valerio, Ganini, Carlo, Antonucci, Michele, Signoretti, Marta, Petta, Filomena, Panei, Massimo, and Bove, Pierluigi

Subjects
SURGICAL enucleation, ENUCLEATION of the eye, URINARY tract infections, THULIUM, TREATMENT effectiveness, PROSTATE
Abstract

Background: Several studies described post-operative irritative symptoms after laser enucleation of prostate, sometimes associated with urge incontinence, probably linked to laser-induced prostatic capsule irritation, and potential for lower urinary tract infections We aimed to evaluate the efficacy of a suppository based on Phenolmicin P3 and Bosexil (Mictalase®) in control of irritative symptoms in patients undergoing thulium laser enucleation of prostate (ThuLEP).Methods: In this single-center, prospective, randomized, open label, phase-III study, patients with indication to ThuLEP were enrolled (Dec2019-Feb2021-Institutional ethics committee STS CE Lazio approval no.1/N-726-ClinicalTrials.gov NCT05130918). The report conformed to CONSORT 2010 guidelines. Eligible patients were 1:1 randomized. Randomization defined Group A: patients who were administered Mictalase® suppositories twice a day for 5 days, then once a day for other 10 days; Group B: patients who did not receive Mictalase® ("controls"). Study endpoints were evaluated at 15 and 30 days postoperation. Primary endpoint included evaluation of effects of the suppository on irritative symptoms by administering IPSS + QoL questionnaire. Secondary endpoint included evaluation of effects on urinary tract infections by performance of urinalysis with urine culture.Results: 111 patients were randomized: 56 in Group A received Mictalase®. Baseline and perioperative data were comparable. At 15-days, no significant differences were found in terms of IPSS + QoL scores and urinalysis parameters. A significant difference in the rate of positive urine cultures favored Group A (p = 0.04). At 30-days follow-up, significant differences were found in median IPSS score (6 [IQR 3-11] versus 10 [5-13], Group A vs B, respectively, p = 0.02). Urinalysis parameters and rate of positive urine cultures were not significantly different.Conclusions: The present randomized trial investigated the efficacy of Mictalase® in control of irritative symptoms and prevention of lower urinary tract infections in patients undergoing ThuLEP. IPSS improvement 30-days postoperation was more pronounced in patients who received Mictalase®. Lower rate of positive urine culture favored Mictalase® group 15-days postoperatively.Trial Registration: The clinical trial has been registered on ClinicalTrials.gov on November 23rd, 2021-Registration number NCT05130918. [ABSTRACT FROM AUTHOR]

Published
2022
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6. The p53 family member p73 in the regulation of cell stress response.

Author

Rozenberg, Julian M., Zvereva, Svetlana, Dalina, Aleksandra, Blatov, Igor, Zubarev, Ilya, Luppov, Daniil, Bessmertnyi, Alexander, Romanishin, Alexander, Alsoulaiman, Lamak, Kumeiko, Vadim, Kagansky, Alexander, Melino, Gerry, Ganini, Carlo, and Barlev, Nikolai A.

Subjects
CELLULAR control mechanisms, CELL death, DNA sequencing, TUMOR growth, DNA repair, P53 protein
Abstract

During oncogenesis, cells become unrestrictedly proliferative thereby altering the tissue homeostasis and resulting in subsequent hyperplasia. This process is paralleled by resumption of cell cycle, aberrant DNA repair and blunting the apoptotic program in response to DNA damage. In most human cancers these processes are associated with malfunctioning of tumor suppressor p53. Intriguingly, in some cases two other members of the p53 family of proteins, transcription factors p63 and p73, can compensate for loss of p53. Although both p63 and p73 can bind the same DNA sequences as p53 and their transcriptionally active isoforms are able to regulate the expression of p53-dependent genes, the strongest overlap with p53 functions was detected for p73. Surprisingly, unlike p53, the p73 is rarely lost or mutated in cancers. On the contrary, its inactive isoforms are often overexpressed in cancer. In this review, we discuss several lines of evidence that cancer cells develop various mechanisms to repress p73-mediated cell death. Moreover, p73 isoforms may promote cancer growth by enhancing an anti-oxidative response, the Warburg effect and by repressing senescence. Thus, we speculate that the role of p73 in tumorigenesis can be ambivalent and hence, requires new therapeutic strategies that would specifically repress the oncogenic functions of p73, while keeping its tumor suppressive properties intact. [ABSTRACT FROM AUTHOR]

Published
2021
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7. Global mapping of cancers: The Cancer Genome Atlas and beyond.

Author

Ganini, Carlo, Amelio, Ivano, Bertolo, Riccardo, Bove, Pierluigi, Buonomo, Oreste Claudio, Candi, Eleonora, Cipriani, Chiara, Di Daniele, Nicola, Juhl, Hartmut, Mauriello, Alessandro, Marani, Carla, Marshall, John, Melino, Sonia, Marchetti, Paolo, Montanaro, Manuela, Natale, Maria Emanuela, Novelli, Flavia, Palmieri, Giampiero, Piacentini, Mauro, and Rendina, Erino Angelo

Published
2021
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8. Cancer predictive studies.

Author

Amelio, Ivano, Bertolo, Riccardo, Bove, Pierluigi, Candi, Eleonora, Chiocchi, Marcello, Cipriani, Chiara, Di Daniele, Nicola, Ganini, Carlo, Juhl, Hartmut, Mauriello, Alessandro, Marani, Carla, Marshall, John, Montanaro, Manuela, Palmieri, Giampiero, Piacentini, Mauro, Sica, Giuseppe, Tesauro, Manfredi, Rovella, Valentina, Tisone, Giuseppe, and Shi, Yufang

Subjects
MOLECULAR biologists, CANCER, CANCER patients, NEUROBLASTOMA, TREATMENT effectiveness
Abstract

The identification of individual or clusters of predictive genetic alterations might help in defining the outcome of cancer treatment, allowing for the stratification of patients into distinct cohorts for selective therapeutic protocols. Neuroblastoma (NB) is the most common extracranial childhood tumour, clinically defined in five distinct stages (1–4 & 4S), where stages 3–4 define chemotherapy-resistant, highly aggressive disease phases. NB is a model for geneticists and molecular biologists to classify genetic abnormalities and identify causative disease genes. Despite highly intensive basic research, improvements on clinical outcome have been predominantly observed for less aggressive cancers, that is stages 1,2 and 4S. Therefore, stages 3–4 NB are still complicated at the therapeutic level and require more intense fundamental research. Using neuroblastoma as a model system, here we herein outline how cancer prediction studies can help at steering preclinical and clinical research toward the identification and exploitation of specific genetic landscape. This might result in maximising the therapeutic success and minimizing harmful effects in cancer patients. [ABSTRACT FROM AUTHOR]

Published
2020
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10. Tivantinib (ARQ197) in hepatocellular carcinoma.

Author

Porta, Camillo, Giglione, Palma, Ferrari, Alessandra, Reversi, Francesca, Liguigli, Wanda, Imarisio, Ilaria, and Ganini, Carlo

Abstract

Here we review the development of tivantinib, a selective oral inhibitor of c-MET. The initially identified dose and schedule for clinical use was 360 mg twice daily. Biological considerations and early results suggested its activity against hepatocellular carcinoma after progression on sorafenib. The results of randomized Phase II study in this setting have already been reported; while in the overall population, the risk of progression was reduced by 36% (HR: 0.64; 90% CI: 0.43-0.94; p = 0.04), in the pre-defined MET-high population median overall survival (7.2 vs 3.8 months; p = 0.01), median time to progression (2.7 vs 1.4 months; p = 0.03) as well as disease control rate (50 vs 20%), were increased by tivantinib. During study conduction, tivantinib dose was amended to 240 mg twice daily, due to a high incidence of neutropenia, without losing clinical efficacy. Presently, a global Phase III trial is being conducted. [ABSTRACT FROM AUTHOR]

Published
2015
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11. Sunitinib in advanced metastatic non-clear cell renal cell carcinoma: a single institution retrospective study.

Author

Paglino C, Imarisio I, Ganini C, Morbini P, Vercelli A, Bregant C, Porta C, Paglino, Chiara, Imarisio, Ilaria, Ganini, Carlo, Morbini, Patrizia, Vercelli, Alessandro, Bregant, Cristina, and Porta, Camillo

Abstract

Aim: Sunitinib is an orally active multi-targeted tyrosine kinase inhibitor that exerts its antitumor effects primarily through the selective inhibition of VEGF. Novel targeted therapies such as sunitinib have transformed the treatment of advanced metastatic renal cell carcinomas, particularly those with clear cell histology. Here, our experience in patients with non-clear cell kidney cancer treated as part of the sunitinib Expanded Access Program is reported.Materials& Methods: This was a retrospective assessment of 21 patients with non-clear cell renal cell carcinoma who were treated with oral sunitinib 50 mg/day in repeated 6 weekly cycles (4 weeks on and 2 weeks off). Disease assessment and physical examination were recorded at baseline and tumor assessments were performed every 3 months, according to Response Evaluation Criteria In Solid Tumors. The primary outcome measure was progression-free survival.Results: Patients received an average of 6.38 cycles of sunitinib; one patient was classified as a complete responder and two as partial responders. The overall response rate was 14.3% and clinical benefit was attained by 52.4%. The median progression-free survival was 4.1 months while median overall survival was 14.6 months. In general, sunitinib was well tolerated and only three patients experienced a grade 3 toxicity, which resolved with dosage reduction.Conclusion: As expected, sunitinib exerted lower antitumor activity in patients with non-clear cell renal cell carcinoma than was achieved in the general population with metastatic kidney cancer. However, responses (one complete and two partial) were documented and clinical benefit was observed in more than half of all patients. [ABSTRACT FROM AUTHOR]

Published
2012
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13. Changes in Circulating Pro-Angiogenic Cytokines, other than VEGF, before Progression to Sunitinib Therapy in Advanced Renal Cell Carcinoma Patients.

Author

Porta, Camillo, Paglino, Chiara, Imarisio, Ilaria, Ganini, Carlo, Sacchi, Lucia, Quaglini, Silvana, Giunta, Vania, and De amici, Mara

Subjects
RENAL cancer, FIBROBLAST growth factors, HEPATOCYTE growth factor, INTERLEUKIN-6, DISEASE progression, RENAL cell carcinoma, PATIENTS
Abstract

Objectives: This study included a cohort of advanced renal cell carcinoma patients treated with sunitinib. Since resistance to sunitinib may be mediated through angiogenic cytokines other than VEGF, we measured the circulating levels of three pro-angiogenic cytokines: basic fibroblast growth factor (bFGF), hepatocyte growth factor (HGF), and interleukin (IL)-6. Methods: Cytokines were measured at baseline and on the first day of each treatment cycle until progression in 85 advanced kidney cancer patients treated with sunitinib using a quantitative sandwich enzyme immunoassay (ELISA) technique. Results: Even though no statistically significant differences in the titers of the three cytokines were observed between baseline and the time of progression in the whole patient cohort, in 45.3, 46.6, and 37.3% of the patients a more than 50% increase between baseline and the time of progression was shown in circulating IL-6, bFGF, and HGF, respectively. Furthermore, this increase was more than 100% in 37.3, 44, and 30.6% of the patients, respectively. We also demonstrated that, in these patients, cytokines tended to increase and to remain high immediately before progression. Conclusions: In a large percentage of kidney cancer patients, progression is preceded by a significant increase in pro-angiogenic cytokines other than VEGF. Copyright © 2012 S. Karger AG, Basel [ABSTRACT FROM AUTHOR]

Published
2012
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14. Store-Operated Ca2+ Entry Is Remodelled and Controls In VitroAngiogenesis in Endothelial Progenitor Cells Isolated from Tumoral Patients.

Author

Lodola, Francesco, Laforenza, Umberto, Bonetti, Elisa, Lim, Dmitry, Dragoni, Silvia, Bottino, Cinzia, Hwei Ling Ong, Guerra, Germano, Ganini, Carlo, Massa, Margherita, Manzoni, Mariangela, Ambudkar, Indu S., Genazzani, Armando A., Rosti, Vittorio, Pedrazzoli, Paolo, Tanzi, Franco, Moccia, Francesco, Porta, Camillo, and Boulton, Michael E.

Subjects
ENDOTHELIAL cells, BONE marrow, TUMORS, METASTASIS, CANCER cells, CATIONS
Abstract

Background:Endothelial progenitor cells (EPCs) may be recruited from bone marrow to sustain tumor vascularisation and promote the metastatic switch. Understanding the molecular mechanisms driving EPC proliferation and tubulogenesis could outline novel targets for alternative anti-angiogenic treatments. Store-operated Ca2+ entry (SOCE), which is activated by a depletion of the intracellular Ca2+ pool, regulates the growth of human EPCs, where is mediated by the interaction between the endoplasmic reticulum Ca2+-sensor, Stim1, and the plasmalemmal Ca2+ channel, Orai1. As oncogenesis may be associated to the capability of tumor cells to grow independently on Ca2+ influx, it is important to assess whether SOCE regulates EPC-dependent angiogenesis also in tumor patients. Methodology/Principal Findings: The present study employed Ca2+ imaging, recombinant sub-membranal and mitochondrial aequorin, real-time polymerase chain reaction, gene silencing techniques and western blot analysis to investigate the expression and the role of SOCE in EPCs isolated from peripheral blood of patients affected by renal cellular carcinoma (RCC; RCC-EPCs) as compared to control EPCs (N-EPCs). SOCE, activated by either pharmacological (i.e. cyclopiazonic acid) or physiological (i.e. ATP) stimulation, was significantly higher in RCC-EPCs and was selectively sensitive to BTP-2, and to the trivalent cations, La3+ and Gd3+. Furthermore, 2-APB enhanced thapsigargin-evoked SOCE at low concentrations, whereas higher doses caused SOCE inhibition. Conversely, the anti-angiogenic drug, carboxyamidotriazole (CAI), blocked both SOCE and the intracellular Ca2+ release. SOCE was associated to the over-expression of Orai1, Stim1, and transient receptor potential channel 1 (TRPC1) at both mRNA and protein level The intracellular Ca2+ buffer, BAPTA, BTP-2, and CAI inhibited RCC-EPC proliferation and tubulogenesis. The genetic suppression of Stim1, Orai1, and TRPC1 blocked CPA-evoked SOCE in RCC-EPCs. Conclusions:SOCE is remodelled in EPCs from RCC patients and stands out as a novel molecular target to interfere with RCC vascularisation due to its ability to control proliferation and tubulogenesis. [ABSTRACT FROM AUTHOR]

Published
2012
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16. Lingual metastasis from renal cell carcinoma: a case report and literature review.

Author

Ganini, Carlo, Lasagna, Angioletta, Ferraris, Elisa, Gatti, Patrizia, Paglino, Chiara, Imarisio, Ilaria, Morbini, Patrizia, Benazzo, Marco, and Porta, Camillo

Subjects
LITERATURE reviews, KIDNEY injuries, MICROSPHERES
Abstract

Renal cell carcinoma (RCC) accounts for the 3% of all solid tumors. Despite continuous improvement in the therapy regimen, less has been achieved in terms of enabling an earlier diagnosis: the neoplasia usually reveals its presence at an advanced stage, obviously affecting prognosis. The most frequent sites of secondary disease are shown to be lungs (50-60%), bone (30-40%), liver (30-40%) and brain (5%); while the head and neck district seems to account for less than 1% of patients with primary kidney lesion. We report here the case of a 70-year old man who presented with acute renal failure due to abdominal recurrence of RCC 18 years post nephrectomy. After a few months of follow up without any systemic therapy due to the renal impairment, the patient presented a vascularized tongue lesion that was demonstrated to be a secondary localization of the RCC. This lesion has, therefore, been treated with microsphere embolization to stop the frequent bleeding and to lessen the unbearable concomitant symptoms it caused, such as dysphagia and pain. A tongue lesion that appears in a RCC patient should always be considered suspect and a multidisciplinary study should be conducted both to assess whether it is a metastasis or a primary new lesion and to understand which method should be selected, if necessary, to treat it (surgery, radiation or embolization). Lingual metastasis should be examined accurately not only because they seem to implicate a poor prognosis, but also because they carry a burden of symptoms that not only threatens patients' lives but also has a strong impact on their quality of life. [ABSTRACT FROM AUTHOR]

Published
2012
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17. Surgery and Target Agents for Renal Cell Carcinoma Treatment: The Path between Proper Interaction.

Author

Ganini, Carlo, Rovereto, Bruno, and Porta, Camillo

Subjects
RENAL cell carcinoma, THERAPEUTICS, RARE diseases, SURGERY, COMBINED modality therapy
Abstract

Background: Renal cell carcinoma accounts for 3% of all solid tumors and currently causes about 3,500 deaths/year in the UK. Once an orphan disease, it has undergone an impressive change in its natural history with an improvement in overall survival, thanks to the development of new target agents. Introduction: In its management, renal cell carcinoma has been treated with both surgical and medical approaches. Nowadays, many more drugs are available, especially in the metastatic setting, so that we should reconsider the peculiar role of surgery and its interaction with target agents. Conclusions: Cytoreductive nephrectomy still plays a major role in the management of the disease, though no really solid data have been still obtained. Adjuvant and neoadjuvant settings, instead, are still under evaluation, especially new adjuvant therapies involving the numerous target agents we have. Finally, metastasectomy has a controversial role, with some evidence of more efficacy than the medical treatment, though it shows too many biases to be considered certain. The picture that comes out suggests a complex frame, in which we have great power to act, but in which we need to better comprehend the interactions that could be created between surgery and medical therapies, to achieve an optimal multimodal treatment for renal cell carcinoma. [ABSTRACT FROM AUTHOR]

Published
2011
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18. Liquid biopsies and cancer omics.

Author

Amelio, Ivano, Bertolo, Riccardo, Bove, Pierluigi, Buonomo, Oreste Claudio, Candi, Eleonora, Chiocchi, Marcello, Cipriani, Chiara, Di Daniele, Nicola, Ganini, Carlo, Juhl, Hartmut, Mauriello, Alessandro, Marani, Carla, Marshall, John, Montanaro, Manuela, Palmieri, Giampiero, Piacentini, Mauro, Sica, Giuseppe, Tesauro, Manfredi, Rovella, Valentina, and Tisone, Giuseppe

Published
2020
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19. Store-operated ca(2+) entry does not control proliferation in primary cultures of human metastatic renal cellular carcinoma.

Author

Dragoni, Silvia, Turin, Ilaria, Laforenza, Umberto, Potenza, Duilio Michele, Bottino, Cinzia, Glasnov, Toma N, Prestia, Martina, Ferulli, Federica, Saitta, Anna, Mosca, Alessandra, Guerra, Germano, Rosti, Vittorio, Luinetti, Ombretta, Ganini, Carlo, Porta, Camillo, Pedrazzoli, Paolo, Tanzi, Franco, Montagna, Daniela, and Moccia, Francesco

Published
2014
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