198 results on '"Iacopo Sardi"'
Search Results
2. Vascular complications in craniopharyngioma-resected paediatric patients: a single-center experience
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Barbara Castelli, Mirko Scagnet, Federico Mussa, Lorenzo Genitori, Iacopo Sardi, and Stefano Stagi
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paediatric neuro-oncology ,craniopharyngioma ,deep venous thrombosis ,vascular complications ,neurosurgery ,Diseases of the endocrine glands. Clinical endocrinology ,RC648-665 - Abstract
BackgroundCraniopharyngioma (CP), although slow growing and histologically benign, has high morbidity, mostly related to hypothalamus-pituitary dysfunction and electrolyte imbalance. Increased risk of vascular complications has been described. However, data are still poor, especially in the paediatric population. The aim of our study was to evaluate the occurrence, timing, and predisposing factors of deep venous thrombosis (DVT) and other vascular alterations in neurosurgical paediatric CP patients.Materials and MethodsIn a single-centre, retrospective study, we investigated 19 CP patients (11 males, 8 females, mean age 10.5 ± 4.3 years), who underwent neurosurgery between December 2016 and August 2022, referred to Meyer Children’s Hospital IRCCS in Florence.ResultsFive patients (26.3%) presented vascular events, which all occurred in connection with sodium imbalances. Three DVT (two with associated pulmonary embolism, in one case leading to death) developed in the post-operative period, most frequently at 7-10 days. Elevated D-dimers, a reduced partial activated thrombin time and a prolonged C-reactive protein increase were highly related to thrombotic vascular events. One case of posterior cerebral artery pseudoaneurysm was described soon after neurosurgery, requiring vascular stenting. Superficial vein thrombophlebitis was a late complication in one patient with other predisposing factors.ConclusionCP patients undergoing neurosurgery are at risk of developing DVT and vascular alterations, thus careful follow-up is mandatory. In our study, we found that the phase of transition from central diabetes insipidus to a syndrome of inappropriate antidiuretic hormone secretion may be a period of significant risk for DVT occurrence. Careful vascular follow-up is mandatory in CP-operated patients.
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- 2024
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3. Corrigendum: Bevacizumab-Irinotecan combination therapy in recurrent low-grade glioma, previously treated with chemo-radiotherapy: a case report
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Barbara Castelli, Carla Fonte, Milena Guidi, Marco Tellini, Marco Di Nicola, Alessandro Iacono, Anna Maria Buccoliero, Daniela Greto, Lorenzo Genitori, and Iacopo Sardi
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low-grade gliomas ,bevacizumab ,irinotecan ,pilocytic astrocytoma ,case report ,Neoplasms. Tumors. Oncology. Including cancer and carcinogens ,RC254-282 - Published
- 2024
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4. Bevacizumab-Irinotecan combination therapy in recurrent low-grade glioma, previously treated with chemo-radiotherapy: a case report
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Barbara Castelli, Carla Fonte, Milena Guidi, Marco Tellini, Marco Di Nicola, Alessandro Iacono, Anna Maria Buccoliero, Daniela Greto, Lorenzo Genitori, and Iacopo Sardi
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low-grade gliomas ,bevacizumab ,irinotecan ,pilocytic astrocytoma ,case report ,Neoplasms. Tumors. Oncology. Including cancer and carcinogens ,RC254-282 - Abstract
Low grade gliomas (LGGs) of pineal region are usually difficult to remove and they frequently relapse or progress after front line chemotherapy. Bevacizumab-Irinotecan (BEVIRI) combination has been successfully attempted in children with recurrent LGGs, in most cases not previously irradiated. The efficacy of bevacizumab has also been described in radiation necrosis. Considering the possible overlapping of radiation treatment effect and disease progression and difficulty in differentiating, we report on the use of BEVIRI in a case of a recurrent relapsing low-grade glioma of the pineal region, subjected to multiple neurosurgical interventions, also treated with a carboplatin-etoposide regimen and a radiation course, at present at one-year follow-up showing a stable response, with no adverse events.
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- 2023
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5. Diencephalic syndrome in childhood, a challenging cause of failure to thrive: miniseries and literature review
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Sandra Trapani, Barbara Bortone, Martina Bianconi, Chiara Rubino, Iacopo Sardi, Paolo Lionetti, and Giuseppe Indolfi
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Diencephalic syndrome ,Failure to thrive ,Nystagmus ,Children ,Brain tumors ,Pediatrics ,RJ1-570 - Abstract
Abstract The aim of our study was to better define the clinical pattern of diencephalic syndrome, a rare but potentially lethal cause of failure to thrive in infancy. Poor weight gain or weight loss, the characteristic presenting feature, often firstly attributed to gastrointestinal or endocrinological or genetic diseases, is secondary to a malfunctioning hypothalamus, caused by a diencephalic tumor. Due to its unexpected clinical onset, diagnostic delay and misdiagnosis are common. We described a case series of 3 children with diencephalic syndrome admitted at our Hospital, over a 5-year period. Furthermore, a narrative review on all pediatric cases published in the last seventy years was performed. Clinical pattern, timing to diagnosis, neuroimaging, management, and outcome were analyzed. Our three cases are singularly described in all clinical and diagnostic findings. Overall, 100 children were selected; all these cases as well as our children presented with failure to thrive: 96% had body mass index or weight-length/height ratio lower than 5th percentile. Vomiting and hyperactivity are reported in 35 and 26% of cases, respectively. The neurological features, mainly nystagmus reported in 43%, may occur late in the disease course. In conclusion, the diagnostic delay is the hallmark of diencephalic syndrome, confirming the lack of knowledge by clinicians. The poor weight gain/loss despite adequate length growth and food intake, especially in children with hyperactivity and good psychomotor development, should alert pediatricians towards this condition, before neurological signs/symptoms occurrence.
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- 2022
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6. Unforeseen cytomegalovirus retinopathy following high dose thiotepa and proton irradiation in a pediatric patient with high-risk medulloblastoma: A case report
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Elisabetta Bigagli, Sara Agostiniani, Alessandra Pugi, Barbara Rombi, Elena Eve Tornaboni, Maria Luigia Censullo, Carlotta Gemma Gori, Rossana Pavone, and Iacopo Sardi
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retinopathy ,leukoencephalopathy ,cytomegalovirus ,thiotepa ,proton irradiation ,medulloblastoma ,Pediatrics ,RJ1-570 - Abstract
In immunocompetent individuals, cytomegalovirus (CMV) infection is usually mild but may cause severe complications such as retinitis, pneumonitis, and encephalitis in immunocompromised individuals. So far, cases of CMV retinitis in patients with medulloblastoma undergoing chemotherapy and radiotherapy, have not been reported. We herein report the case of a pediatric patient with high-risk medulloblastoma who experienced an unexpected CMV retinopathy and leukoencephalopathy following high dose thiotepa and proton irradiation. The patient underwent a four-course induction therapy (1st cycle: methotrexate and vinorelbine; 2nd cycle: etoposide and hematopoietic stem cells apheresis; 3rd cycle: cyclophosphamide and vinorelbine; 4th cycle: carboplatin and vinorelbine) and then a consolidation phase consisting in high dose thiotepa followed by autologous HSC transplant and proton cranio-spinal irradiation plus boost to the primary tumor site and pituitary site with concomitant vinorelbine. After two months of maintenance treatment with lomustine and vinorelbine, the patient showed complete blindness and leukoencephalopathy. A diagnosis of CMV retinopathy was made and oral valganciclovir was administered. CMV retinopathy was judged to be possibly related to the use of high dose thiotepa worsened by radiotherapy. This case report suggests that in pediatric patients undergoing immunosuppressive chemo-radiotherapy, CMV reactivation should be carefully monitored to prevent serious complications such as retinopathy and visual loss.
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- 2023
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7. Expert Opinion on the Management of Growth Hormone Deficiency in Brain Tumor Survivors: Results From an Italian Survey
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Natascia Di Iorgi, Giovanni Morana, Marco Cappa, Ludovico D’Incerti, Maria Luisa Garrè, Armando Grossi, Lorenzo Iughetti, Patrizia Matarazzo, Maria Parpagnoli, Gabriella Pozzobon, Mariacarolina Salerno, Iacopo Sardi, Malgorzata Gabriela Wasniewska, Stefano Zucchini, Andrea Rossi, and Mohamad Maghnie
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growth hormone deficiency ,pediatric brain tumor survivors ,brain MRI ,radiotherapy ,recombinant human growth hormone (rhGH) ,Diseases of the endocrine glands. Clinical endocrinology ,RC648-665 - Abstract
BackgroundGrowth hormone deficiency (GHD) is the first and most common endocrine complication in pediatric brain tumor survivors (BTS). GHD can occur due to the presence of the tumor itself, surgery, or cranial radiotherapy (CRT).AimsThis study aimed to evaluate management and adherence to current guidelines of the Italian centers engaged in the diagnosis and follow-up of GHD patients with BTS.MethodsA multidisciplinary scientific board of pediatric endocrinologists, oncologists and radiologists with neuroimaging expertise discussed and reviewed the main issues relating to the management of GHD in pediatric BTS and developed a survey. The survey included questions relating to organizational aspects, risk factors, diagnosis, definition of stable disease, and treatment. The online survey was sent to an expanded panel of specialists dedicated to the care of pediatric BTS, distributed among the three specialty areas and throughout the country (23 Italian cities and 37 Centers).ResultsThe online questionnaire was completed by 86.5% (32 out of 37) of the Centers involved. Most had experience in treating these patients, reporting that they follow more than 50 BTS patients per year. Responses were analyzed descriptively and aggregated by physician specialty. Overall, the results of the survey showed some important controversies in real life adherence to the current guidelines, with discrepancies between endocrinologists and oncologists in the definition of risk factors, diagnostic work-up, decision-making processes and safety. Furthermore, there was no agreement on the neuroimaging definition of stable oncological disease and how to manage growth hormone therapy in patients with residual tumor and GHD.ConclusionsThe results of the first Italian national survey on the management of GHD in BTS highlighted the difference in management on some important issues. The time to start and stop rhGH treatment represent areas of major uncertainty. The definition of stable disease remains critical and represents a gap in knowledge that must be addressed within the international guidelines in order to increase height and to improve metabolic and quality of life outcomes in cancer survivors with GHD.
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- 2022
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8. Optical Coherence Tomography Significance in Managing Early Onset of Optic Pathway Gliomas in Children Younger than 5 Years of Age—A Retrospective Study
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Rossana Pavone, Carla Fonte, Iacopo Sardi, Roberto Caputo, Elisa Marziali, Fabio Mazzeo, Jacopo Secci, Alessia Bergamini, Salvatore De Masi, Maria Carmela Leo, Maria Luigia Censullo, and Giacomo Maria Bacci
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optic pathway glioma ,neurofibromatosis ,optical coherence tomography ,pRNFL ,SD-OCT ,OPG ,Pediatrics ,RJ1-570 - Abstract
We aimed to investigate the significance of optical coherence tomography (SD-OCT) in managing pediatric optic pathway gliomas (OPGs) in children younger than 5 years of age. A retrospective monocentric study was conducted. SD-OCT scans were obtained using the handheld iVue system to assess peripapillary retinal nerve fibre layer (pRNFL) thickness at three time points: baseline (OCT1), end of treatment (OCT2), and at last follow-up (OCT3). We compared the median value of pRNFL (and interquartile range—IQR) at different follow-up times and in different sub-groups (stable disease—SD, partial response—PR, and progression disease—PD). Thirteen children younger than 5 years of age were included. The Median follow-up time was 3.9 years (IQR 1.2). Six patients showed a pRNFL change of more than 10% during follow-up. Seven patients showed PD during follow-up. Median pRNFL at baseline was 81.5 µm (IQR 31.5); median pRNFL at the end of treatment was 73 µm (IQR 33); median pRNFL at last follow-up was 72 µm (IQR 38.5). The mean pRNFL at baseline was significantly lower than the mean normative values. Only subjects with PD showed pRNFL change close to statistical significance. This study confirms the role of SD-OCT in managing OPGs for therapeutic decisions and strategy planning of visual rehabilitation.
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- 2022
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9. Case Report: A Case of Glioblastoma in a Patient With Haberland Syndrome
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Silvia Ferranti, Iacopo Sardi, Milena Guidi, Chiara Lembo, and Salvatore Grosso
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Haberland syndrome ,encephalocraniocutaneous lipomatosis ,glioblastoma ,tumor ,epilepsy ,Pediatrics ,RJ1-570 - Abstract
Haberland syndrome or encephalocraniocutaneous lipomatosis is a rare ectomesodermal dysgenesis defined by the triad including ocular, skin, and central nervous system involvement, which is commonly unilateral. This disorder is attributed to a post-zygotic mutation responsible for a neural tube and neural crest dysgenesis. We report the case of a 15-year-old female with Haberland syndrome with pharmacoresistant epilepsy who developed a World Health Organization-grade IV glioblastoma. This is the first case of pediatric glioblastoma associated with Haberland syndrome. The previously reported pediatric cases included benign brain tumors. To our knowledge, this is the fifth case of brain tumor associated with encephalocraniocutaneous lipomatosis and the second case of glioblastoma associated with this syndrome. The hypothesis that Haberland syndrome is associated with an increased risk of tumor development is intriguing, although the rarity of the condition is nowadays preventing us from drawing definitive conclusions about this potential link between the two entities. Further studies are needed to establish the real relationship between encephalocraniocutaneous lipomatosis and the risk of brain tumors.
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- 2021
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10. Use of High-Dose Chemotherapy in Front-Line Therapy of Infants Aged Less Than 12 Months Treated for Aggressive Brain Tumors
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Milena Guidi, Laura Giunti, Anna Maria Buccoliero, Mariarita Santi, Barbara Spacca, Salvatore De Masi, Lorenzo Genitori, and Iacopo Sardi
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congenital tumor ,chemotherapy ,glioblastoma ,brain tumor ,newborn ,Pediatrics ,RJ1-570 - Abstract
Introduction: Malignant brain tumors in infants less than 12 months of age are extremely rare, and they have poor prognosis. We evaluated genetic characteristics and response rates of infants with congenital brain tumors subjected to high-dose chemotherapy and autologous stem cell transplant after gross total tumor resection.Materials and Methods: In total, 10 infants, aged less than 12 months, were enrolled in this study. The median age was 56 days (range: 1–279 days). Pathological examination demonstrated the following: four anaplastic astrocytomas, two glioblastomas, two central nervous system (CNS) embryonal tumors, not otherwise specified (NOS), and two atypical teratoid/rhabdoid tumors.Results: All patients were exposed to induction chemotherapy regimen, two high-dose chemotherapy courses, and autologous stem cell transplant after maximal surgery. At 1–3–5 years, the global overall survival (OS) was 90, 70, and 70% and the progression-free survival (PFS) was 80–60 and 60%. In all the patients, the copy number variants (CNVs) profile was analyzed using the SNP/CGH array approach. To investigate the clinical relevance of germline SMARCB1 mutation in AT/RT patients, we performed sequence analysis of the coding regions. The two patients with AT/RT were found to have germline SMARCB1 mutations. No BRAF mutations were found, and only NTRK gene fusion was present in one patient. We also have examined the association with OS and PFS and different histological subtypes of infant CNS proving that high-grade astrocytoma has better overall survival than other tumor types (p: 0.007 and p: 0.0590).Conclusion: High-dose chemotherapy regimen represents a valid therapeutic approach for congenital brain tumors with a high rate of response. The molecular analysis has to be analyzed in all infants' brain tumor types. High-grade gliomas are characterized by a better prognosis than other histologies of infant CNS.
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- 2020
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11. Sirolimus in Infants with Multiple Cardiac Rhabdomyomas Associated with Tuberous Sclerosis Complex
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Maurizio Lucchesi, Enrico Chiappa, Flavio Giordano, Francesco Mari, Lorenzo Genitori, and Iacopo Sardi
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mTOR inhibitors ,Sirolimus ,Tuberous sclerosis complex ,Cardiac rhabdomyomas ,Subpendymal giant cell astrocytomas ,Neoplasms. Tumors. Oncology. Including cancer and carcinogens ,RC254-282 - Abstract
Introduction: Cardiac rhabdomyomas represent a frequent manifestation of tuberous sclerosis. Tumor growth, mainly prenatally, can result in intrauterine fetal or neonatal deaths in almost 10% of patients. Case Report: We treated 3 consecutive infants aged less than 12 months with sirolimus, an oral mTOR inhibitor. All patients achieved significant reductions in cardiac rhabdomyomas. A complete response was documented in 2 patients, while a partial response with tumor debulking greater than 50% was seen in the other one. The median time to best cardiac response was 1.9 months in all patients, and 3.3 months in those with complete response. The side effects profile was acceptable. Conclusion: Sirolimus may have a significant role in promoting natural regression of cardiac rhabdomyomas. Prospective clinical trials are needed.
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- 2018
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12. Role of eculizumab in a pediatric refractory gemcitabine-induced thrombotic microangiopathy: a case report
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Ludovica Facchini, Maurizio Lucchesi, Alessia Stival, Rosa Maria Roperto, Francesca Melosi, Marco Materassi, Silvia Farina, Veronica Tintori, Maurizio de Martino, and Iacopo Sardi
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Microangiopathy ,Eculizumab ,Gemcitabine ,Medulloblastoma ,Radiotherapy ,Brain tumors ,Medicine - Abstract
Abstract Background The incidence of gemcitabine-induced hemolytic uremic syndrome has already been described in adults. Several approaches have been employed in the treatment of gemcitabine-induced hemolytic uremic syndrome with different outcomes. One of the most promising agents is eculizumab, which is a monoclonal antibody directed against C5 complement protein. Case presentation We reported the case of a 3-year-old white boy with medulloblastoma who underwent high-dose chemotherapy and craniospinal irradiation. Afterwards he started maintenance chemotherapy with gemcitabine and oxaliplatin. After five courses he presented a progressive clinical worsening, which resulted in a systemic thrombotic microangiopathy. Initially he was treated with rituximab without clinical improvement. Therefore he started therapy with repeated cycles of eculizumab. After seven infusions he showed a gradual improvement and finally a complete remission of gemcitabine-induced hemolytic uremic syndrome. Conclusions Eculizumab prevents serious complement-mediated vascular damage for chemotherapy-induced thrombotic microangiopathy in pediatric cases.
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- 2017
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13. A New Treatment Opportunity for DIPG and Diffuse Midline Gliomas: 5-ALA Augmented Irradiation, the 5aai Regimen
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Richard E. Kast, Alex P. Michael, Iacopo Sardi, Terry C. Burns, Tim Heiland, Georg Karpel-Massler, Francois G. Kamar, and Marc-Eric Halatsch
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5-aminolevulinic acid ,diffuse intrinsic pontine glioma ,diffuse midline gliomas ,fluorescence ,glioblastoma ,irradiation ,photodynamic ,prognosis ,protoporphyrin ix ,reactive oxygen species ,Neurosciences. Biological psychiatry. Neuropsychiatry ,RC321-571 - Abstract
Prognosis for diffuse intrinsic pontine glioma (DIPG) and generally for diffuse midline gliomas (DMG) has only marginally improved over the last ~40 years despite dozens of chemotherapy and other therapeutic trials. The prognosis remains invariably fatal. We present here the rationale for a planned study of adding 5-aminolevulinic acid (5-ALA) to the current irradiation of DIPG or DMG: the 5aai regimen. In a series of recent papers, oral 5-ALA was shown to enhance standard therapeutic ionizing irradiation. 5-ALA is currently used in glioblastoma surgery to enable demarcation of overt tumor margins by virtue of selective uptake of 5-ALA by neoplastic cells and selective conversion to protoporphyrin IX (PpIX), which fluoresces after excitation by 410 nm (blue) light. 5-ALA is also useful in treating glioblastomas by virtue of PpIX’s transfer of energy to O2 molecules, producing a singlet oxygen that in turn oxidizes intracellular DNA, lipids, and proteins, resulting in selective malignant cell cytotoxicity. This is called photodynamic treatment (PDT). Shallow penetration of light required for PpIX excitation and resultant energy transfer to O2 and cytotoxicity results in the inaccessibility of central structures like the pons or thalamus to sufficient light. The recent demonstration that keV and MeV photons can also excite PpIX and generate singlet O2 allows for reconsideration of 5-ALA PDT for treating DMG and DIPG. 5-ALA has an eminently benign side effect profile in adults and children. A pilot study in DIPG/DMG of slow uptitration of 5-ALA prior to each standard irradiation session—the 5aai regimen—is warranted.
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- 2020
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14. Augmentation of 5-Aminolevulinic Acid Treatment of Glioblastoma by Adding Ciprofloxacin, Deferiprone, 5-Fluorouracil and Febuxostat: The CAALA Regimen
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Richard E. Kast, Nicolas Skuli, Iacopo Sardi, Felix Capanni, Martin Hessling, Guido Frosina, Anton P. Kast, Georg Karpel-Massler, and Marc-Eric Halatsch
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5-aminolevulinic acid ,ciprofloxacin ,deferiprone ,fluorescence ,5-fluorouracil ,febuxostat ,glioblastoma ,photodynamic treatment ,temozolomide ,Neurosciences. Biological psychiatry. Neuropsychiatry ,RC321-571 - Abstract
The CAALA (Complex Augmentation of ALA) regimen was developed with the goal of redressing some of the weaknesses of 5-aminolevulinic acid (5-ALA) use in glioblastoma treatment as it now stands. 5-ALA is approved for use prior to glioblastoma surgery to better demarcate tumor from brain tissue. 5-ALA is also used in intraoperative photodynamic treatment of glioblastoma by virtue of uptake of 5-ALA and its preferential conversion to protoporphyrin IX in glioblastoma cells. Protoporphyrin IX becomes cytotoxic after exposure to 410 nm or 635 nm light. CAALA uses four currently-marketed drugs—the antibiotic ciprofloxacin, the iron chelator deferiprone, the antimetabolite 5-FU, and the xanthine oxidase inhibitor febuxostat—that all have evidence of ability to both increase 5-ALA mediated intraoperative glioblastoma demarcation and photodynamic cytotoxicity of in situ glioblastoma cells. Data from testing the full CAALA on living minipigs xenotransplanted with human glioblastoma cells will determine safety and potential for benefit in advancing CAALA to a clinical trial.
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- 2018
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15. Cyclooxygenase-2 Pathway Correlates with VEGF Expression in Head and Neck Cancer. Implications for Tumor Angiogenesis and Metastasis
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Oreste Gallo, Alessandro Franchi, Lucia Magnelli, Iacopo Sardi, Alfredo Vannacci, Vieri Boddit, Vincenzo Chiarugi, and Emanuela Masini
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head and neck cancer ,COX-2 ,VEGF ,angiogenesis ,Neoplasms. Tumors. Oncology. Including cancer and carcinogens ,RC254-282 - Abstract
We evaluated the role of COX-2 pathway in 35 head and neck cancers (HNCs) by analyzing COX-2 expression and prostaglandin E2 (PGE2) production in relation to tumor angiogenesis and lymph node metastasis. COX-2 activity was also correlated to vascular endothelial growth factor (VEGF) mRNA and protein expression. COX-2 mRNA and protein expression was higher in tumor samples than in normal mucosa. PGE2 levels were higher in the tumor front zone in comparison with tumor core and normal mucosa (P
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- 2001
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16. Pleomorphic Xanthoastrocytoma: a single institution retrospective analysis and a review of the literature
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Beatrice Detti, Silvia Scoccianti, Virginia Maragna, Sara Lucidi, Michele Ganovelli, Maria Ausilia Teriaca, Saverio Caini, Isacco Desideri, Benedetta Agresti, Daniela Greto, Anna Maria Buccoliero, Alessandro Della Puppa, Iacopo Sardi, and Lorenzo Livi
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Adult ,Proto-Oncogene Proteins B-raf ,Brain Neoplasms ,Humans ,Radiology, Nuclear Medicine and imaging ,General Medicine ,Astrocytoma ,Child ,Follow-Up Studies ,Retrospective Studies - Abstract
Background Pleomorphic xanthoastrocytoma (PXA) is a rare low-grade brain tumor. To date, limited studies have analyzed factors affecting survival outcomes and defined the therapeutic strategy. The aim of this retrospective analysis was to investigate the clinicopathologic characteristics of PXA and identify factors associated with outcomes. Methods We retrospectively analyzed a cohort of 16 adult and children patients with PXA who underwent primary resection from 1997 to 2019, referred to our Radiation Oncology Unit and to Meyer’s Paediatric Hospital. We also reviewed the relevant literature. Results All patients underwent primary surgical resection; 10 patients received adjuvant radiation treatment course, ranging from DTF 54 to 64 Gy; 8 of them received, in addition, concurrent adjuvant chemotherapy; 6 patients underwent only radiological follow-up. After a median follow up was 60 months: median OS was 34.9 months (95% CI 30–218), 1-year OS 87%, 5-years OS 50%, 10-years OS 50%; median PFS 24.4 months (95% CI 13–156), 1-year PFS 80%, 5-years PFS 33%, 10-years PFS 33%. A chi-square test showed a significant association between OS and recurrent disease (p = 0.002) and with chemotherapy adjuvant treatment (p = 0.049). A borderline statistical significant association was instead recognized with BRAF mutation (p = 0.058). Conclusions Despite our analysis did not reveal a strong prognostic or predictive factor able to address pleomorphic xanthoastrocytoma management; however, in selected patients could be considered the addition of adjuvant radiation chemotherapy treatment after adequate neurosurgical primary resection. Furthermore, recurrent disease evidenced a detrimental impact on survival.
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- 2022
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17. MDACT: A New Principle of Adjunctive Cancer Treatment Using Combinations of Multiple Repurposed Drugs, with an Example Regimen
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Richard E. Kast, Alex Alfieri, Hazem I. Assi, Terry C. Burns, Ashraf M. Elyamany, Maria Gonzalez-Cao, Georg Karpel-Massler, Christine Marosi, Michael E. Salacz, Iacopo Sardi, Pieter Van Vlierberghe, Mohamed S. Zaghloul, and Marc-Eric Halatsch
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Cancer Research ,multidrug regimen ,CELL LUNG-CANCER ,TUMOR-GROWTH ,COLON-CANCER ,glioblastoma ,repurposing ,Biology and Life Sciences ,CUSP9v3 ,IN-VITRO ,COLORECTAL-CANCER ,lung cancer ,TO-LYMPHOCYTE RATIO ,ALDEHYDE DEHYDROGENASE ,colon cancer ,Oncology ,II TYPE-1 RECEPTOR ,CARBONIC-ANHYDRASE IX ,cholangiocarcinoma ,RENIN-ANGIOTENSIN-SYSTEM - Abstract
Simple Summary We present eight core attributes of cancer growth that we must address for a more effective treatment than we currently have. To do this we outline why a regimen simultaneously using many different drugs will be needed. At our current state of knowledge, even adding two or three drugs will not counter all the growth attributes of a currently incurable cancer. We show in this paper, the details of how an example six drug regimen, when added alongside of current traditional treatments, might inhibit enough of the eight core growth driving elements to allow those standard treatments to be more effective. We further show how medicines from general medical practice used to treat pain, fungal infections, psychosis, leprosy and other non-cancer related illnesses can be repurposed to block cancer cells' survival pathways and growth drives. In part one of this two-part paper, we present eight principles that we believe must be considered for more effective treatment of the currently incurable cancers. These are addressed by multidrug adjunctive cancer treatment (MDACT), which uses multiple repurposed non-oncology drugs, not primarily to kill malignant cells, but rather to reduce the malignant cells' growth drives. Previous multidrug regimens have used MDACT principles, e.g., the CUSP9v3 glioblastoma treatment. MDACT is an amalgam of (1) the principle that to be effective in stopping a chain of events leading to an undesired outcome, one must break more than one link; (2) the principle of Palmer et al. of achieving fractional cancer cell killing via multiple drugs with independent mechanisms of action; (3) the principle of shaping versus decisive operations, both being required for successful cancer treatment; (4) an idea adapted from Chow et al., of using multiple cytotoxic medicines at low doses; (5) the idea behind CUSP9v3, using many non-oncology CNS-penetrant drugs from general medical practice, repurposed to block tumor survival paths; (6) the concept from chess that every move creates weaknesses and strengths; (7) the principle of mass-by adding force to a given effort, the chances of achieving the goal increase; and (8) the principle of blocking parallel signaling pathways. Part two gives an example MDACT regimen, gMDACT, which uses six repurposed drugs-celecoxib, dapsone, disulfiram, itraconazole, pyrimethamine, and telmisartan-to interfere with growth-driving elements common to cholangiocarcinoma, colon adenocarcinoma, glioblastoma, and non-small-cell lung cancer. gMDACT is another example of-not a replacement for-previous multidrug regimens already in clinical use, such as CUSP9v3. MDACT regimens are designed as adjuvants to be used with cytotoxic drugs.
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- 2022
18. Second series by the Italian Association of Pediatric Hematology and Oncology of children and adolescents with intracranial ependymoma: an integrated molecular and clinical characterization with a long-term follow-up
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Annamaria Buccoliero, Luisa Chiapparini, Felice Giangaspero, Elisabetta Viscardi, Hendrik Witt, Piergiorgio Modena, Pascal Johann, Angela Mastronuzzi, Simone Minasi, Bianca Pollo, Kristian W. Pajtler, Maurizio Mascarin, Francesca R. Buttarelli, Lucia Quaglietta, Maura Massimino, Manila Antonelli, Antonio Ruggiero, Francesco Barretta, Daniele Bertin, Lorenza Gandola, Carlo Patriarca, Alessandra Erbetta, Marco Gessi, Iacopo Sardi, Stefan M. Pfister, Vittoria Donofrio, Luna Boschetti, Isabella Morra, Elisabetta Schiavello, and Maria Luisa Garrè
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Oncology ,Ependymoma ,Cancer Research ,medicine.medical_specialty ,Long term follow up ,medicine.medical_treatment ,Copy number analysis ,children ,CDKN2A ,Internal medicine ,follow-up ,medicine ,molecular events ,Series (stratigraphy) ,business.industry ,Intracranial ependymoma ,prognosis ,medicine.disease ,Radiation therapy ,Settore MED/38 - PEDIATRIA GENERALE E SPECIALISTICA ,Neurology (clinical) ,Pediatric hematology ,business - Abstract
Background A prospective 2002–2014 study stratified 160 patients by resection extent and histological grade, reporting results in 2016. We re-analyzed the series after a median of 119 months, adding retrospectively patients’ molecular features. Methods Follow-up of all patients was updated. DNA copy number analysis and gene-fusion detection could be completed for 94/160 patients, methylation classification for 68. Results Progression-free survival (PFS) and overall survival (OS) at 5/10 years were 66/58%, and 80/73%. Ten patients had late relapses (range 66–126 mo), surviving after relapse no longer than those relapsing earlier (0–5 y). On multivariable analysis a better PFS was associated with grade II tumor and complete surgery at diagnosis and/or at radiotherapy; female sex and complete resection showed a positive association with OS. Posterior fossa (PF) tumors scoring ≥0.80 on DNA methylation analysis were classified as PFA (n = 41) and PFB (n = 9). PFB patients had better PFS and OS. Eighteen/32 supratentorial tumors were classified as RELA, and 3 as other molecular entities (anaplastic PXA, LGG MYB, HGNET). RELA had no prognostic impact. Patients with 1q gain or cyclin-dependent kinase inhibitor 2A (CDKN2A) loss had worse outcomes, included significantly more patients >3 years old (P = 0.050) and cases of dissemination at relapse (P = 0.007). Conclusions Previously described prognostic factors were confirmed at 10-year follow-up. Late relapses occurred in 6.2% of patients. Specific molecular features may affect outcome: PFB patients had a very good prognosis; 1q gain and CDKN2A loss were associated with dissemination. To draw reliable conclusions, modern ependymoma trials need to combine diagnostics with molecular risk stratification and long-term follow-up.
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- 2020
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19. An alternative procedure to leukapheresis for peripheral hematopoietic progenitor cell collection in very‐low‐weight children: A single pediatric center experience
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Silvia Galli, S. Bisin, Daniela Calzolari, V. Cunial, L. Piccini, Erika Maccarelli, R. Ceccantini, Stefano Ermini, Franco Bambi, Veronica Tintori, Paola Pavan, Francesca Brugnolo, Francesca Gentile, Iacopo Sardi, Sonia Muricci, Valentina Gori, Marco Berchielli, Valentina Becherucci, Daniela Maggio, B. Bindi, Elisa Allegro, and Elena De Rienzo
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Male ,medicine.medical_specialty ,CD34 ,030204 cardiovascular system & hematology ,Pallor ,Blood cell ,03 medical and health sciences ,0302 clinical medicine ,Humans ,Medicine ,Autologous transplantation ,Leukapheresis ,Adverse effect ,business.industry ,Body Weight ,Infant ,Hematology ,General Medicine ,Hematopoietic Stem Cells ,Hematopoietic Stem Cell Mobilization ,Surgery ,Peripheral ,medicine.anatomical_structure ,Hematopoietic progenitor ,Female ,medicine.symptom ,business ,030215 immunology - Abstract
Background PBSC collection using a blood cell separator in very low weight patients can be frequently complicated by severe adverse effects and technical difficulties. Material and methods From March 2013 to January 2017, 14 PBSC collections were performed in 12 children weighing less than 10 kg, affected by different solid tumours. PBSC collection was performed with a "homemade" aseptically assembled circuit. The circuit is composed by a 150 mL collection bag connected with a 4 stopcock ramp, perfused with ACD. This circuit allows collection of a specific total blood amount from CVC, depending on CD34+ /kg target. Results Mean CD34+ cell performance per collection was 9.3 × 106 /kg. Tolerance to the procedure was very good as none of the patients experienced complications, with the exception of a patient who showed mild cyanosis and pallor after collection. Moreover, no bleeding or thrombotic complications have been observed. To date, 16 PBSC reinfusions have been performed in 7 children with a mean CD34+ cells viability of 98.1% ± 2.7 and mean WBC viability of 57% ± 10. Cell recovery after thawing was 87% ± 10.8. A rapid graft intake for both neutrophils and platelets, between day 7 and 20 after reinfusion was observed. Discussion The procedure of total blood collection without the use of a cell separator is feasible and allows a good PBSC collection without significant side effects in very low-weight children. Moreover, this method could represent a valid and safe alternative to leukapheresis in patients where classic procedure could be difficult to apply.
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- 2020
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20. Pediatric High Grade Glioma Classification Criteria and Molecular Features of a Case Series
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Anna Maria Buccoliero, Laura Giunti, Selene Moscardi, Francesca Castiglione, Aldesia Provenzano, Iacopo Sardi, Mirko Scagnet, Lorenzo Genitori, and Chiara Caporalini
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Genetics ,Humans ,Glioma ,Child ,Genetics (clinical) ,pediatric ,high-grade glioma ,astrocytoma ,thalamic glioma ,gene panel ,IDH2 mutation ,EZHIP ,TP53 ,H3F3A ,case report - Abstract
Pediatric high-grade gliomas (pHGGs) encompass a heterogeneous group of tumors. Three main molecular types (H3.3 mutant, IDH mutant, and H3.3/IDH wild-type) and a number of subtypes have been identified. We provide an overview of pHGGs and present a mono-institutional series. We studied eleven non-related pHGG samples through a combined approach of routine diagnostic tools and a gene panel. TP53 and H3F3A were the most mutated genes (six patients each, 54%). The third most mutated gene was EGFR (three patients, 27%), followed by PDGFRA and PTEN (two patients each, 18%). Variants in the EZHIP, MSH2, IDH1, IDH2, TERT, HRAS, NF1, BRAF, ATRX, and PIK3CA genes were relatively infrequent (one patient each, 9%). In one case, gene panel analysis documented the presence of a pathogenic IDH2 variant (c.419G>A, p.Arg140Gln) never described in gliomas. More than one-third of patients carry a variant in a gene associated with tumor-predisposing syndromes. The absence of constitutional DNA did not allow us to identify their constitutional origin.
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- 2022
21. Toxicity and Clinical Results after Proton Therapy for Pediatric Medulloblastoma: A Multi-Centric Retrospective Study
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Alessandro Ruggi, Fraia Melchionda, Iacopo Sardi, Rossana Pavone, Linda Meneghello, Lidija Kitanovski, Lorna Zadravec Zaletel, Paolo Farace, Mino Zucchelli, Mirko Scagnet, Francesco Toni, Roberto Righetto, Marco Cianchetti, Arcangelo Prete, Daniela Greto, Silvia Cammelli, Alessio Giuseppe Morganti, Barbara Rombi, Ruggi A., Melchionda F., Sardi I., Pavone R., Meneghello L., Kitanovski L., Zaletel L.Z., Farace P., Zucchelli M., Scagnet M., Toni F., Righetto R., Cianchetti M., Prete A., Greto D., Cammelli S., Morganti A.G., and Rombi B.
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radiation ,Cancer Research ,Oncology ,pediatric brain tumors ,proton therapy ,medulloblastoma ,toxicity ,pediatric brain tumor - Abstract
Medulloblastoma is the most common malignant brain tumor in children. Even if current treatment dramatically improves the prognosis, survivors often develop long-term treatment-related sequelae. The current radiotherapy standard for medulloblastoma is craniospinal irradiation with a boost to the primary tumor site and to any metastatic sites. Proton therapy (PT) has similar efficacy compared to traditional photon-based radiotherapy but might achieve lower toxicity rates. We report on our multi-centric experience with 43 children with medulloblastoma (median age at diagnosis 8.7 years, IQR 6.6, M/F 23/20; 26 high-risk, 14 standard-risk, 3 ex-infant), who received active scanning PT between 2015 and 2021, with a focus on PT-related acute-subacute toxicity, as well as some preliminary data on late toxicity. Most acute toxicities were mild and manageable with supportive therapy. Hematological toxicity was limited, even among HR patients who underwent hematopoietic stem-cell transplantation before PT. Preliminary data on late sequelae were also encouraging, although a longer follow-up is needed.
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- 2022
22. Treatment and outcome of intracranial ependymoma after first relapse in the 2nd AIEOP protocol
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Francesca R. Buttarelli, Maria Luisa Garrè, Francesco Barretta, Lucia Quaglietta, Felice Giangaspero, Maura Massimino, Manila Antonelli, Iacopo Sardi, Giuseppe Scimone, Piergiorgio Modena, Veronica Biassoni, Pascal Johann, Antonio Ruggiero, Maurizio Mascarin, Angela Mastronuzzi, Luna Boschetti, Rosa Maria Mura, Luisa Chiapparini, Giovanni Scarzello, Carlo Giussani, Elisabetta Schiavello, Alessandra Erbetta, Marzia Giagnacovo, Elisabetta Viscardi, Andrea Carai, Paolo Ferroli, Daniele Bertin, Lorenza Gandola, Anna Mussano, and Salvina Barra
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Cancer Research ,medicine.medical_specialty ,Chemotherapy ,business.industry ,Standard treatment ,medicine.medical_treatment ,Salvage treatment ,ependymoma relapse ,Female sex ,dissemination ,complete surgery ,re-irradiation ,First relapse ,Oncology ,Settore MED/38 - PEDIATRIA GENERALE E SPECIALISTICA ,Homogeneous ,Internal medicine ,medicine ,Cumulative incidence ,Intracranial ependymoma ,Neurology (clinical) ,business ,1q gain - Abstract
Background More than 40% of patients with intracranial ependymoma need a salvage treatment within 5 years after diagnosis, and no standard treatment is available as yet. We report the outcome after first relapse of 64 patients treated within the 2nd AIEOP protocol. Methods We considered relapse sites and treatments, that is, various combinations of complete/incomplete surgery, if followed by standard or hypofractionated radiotherapy (RT) ± chemotherapy (CT). Molecular analyses were available for 38/64 samples obtained at first diagnosis. Of the 64 cases, 55 were suitable for subsequent analyses. Results The median follow-up was 147 months after diagnosis, 84 months after first relapse, 5-year EFS/OS were 26.2%/30.8% (median EFS/OS 13/32 months) after relapse. For patients with a local relapse (LR), the 5-year cumulative incidence of second LRs was 51.6%, with a 5-year event-specific probability of being LR-free of 40.0%. Tumor site/grade, need for shunting, age above/below 3 years, molecular subgroup at diagnosis, had no influence on outcomes. Due to variation in the RT dose/fractionation used and the subgroup sizes, it was not possible to assess the impact of the different RT modalities. Multivariable analyses identified completion of surgery, the absence of symptoms at relapse, and female sex as prognostically favorable. Tumors with a 1q gain carried a higher cumulative incidence of dissemination after first relapse. Conclusions Survival after recurrence was significantly influenced by symptoms and completeness of surgery. Only a homogeneous protocol with well-posed, randomized questions could clarify the numerous issues, orient salvage treatment, and ameliorate prognosis for this group of patients.
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- 2022
23. Clinical-pathological study of 28 glial and mixed neuronal-glial tumors diagnosed within the first year of life
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Mirko Scagnet, Selene Moscardi, Chiara Caporalini, Iacopo Sardi, Lorenzo Genitori, Anna Maria Buccoliero, Francesca Castiglione, Barbara Spacca, and Laura Giunti
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Pathology ,medicine.medical_specialty ,Adolescent ,Astrocytoma ,Pathology and Forensic Medicine ,medicine ,Subependymal zone ,Humans ,Gangliocytoma ,Child ,neoplasms ,Ganglioglioma ,Pilocytic astrocytoma ,business.industry ,Brain Neoplasms ,Not Otherwise Specified ,General Medicine ,Glioma ,medicine.disease ,nervous system diseases ,nervous system ,Neurology ,Giant cell ,Immunohistochemistry ,Neurology (clinical) ,business ,Glioblastoma ,Anaplastic astrocytoma - Abstract
Our purpose was to investigate the incidence of gliomas and neuronal-glial tumors, their outcome, and H3.3K27M, BRAFV600E, and IDH status in children within 1 year of age affected by CNS tumor. We collected 28 consecutive gliomas and mixed tumors. Immunohistochemistry and/or molecular analyses were performed on formalin-fixed/paraffin-embedded specimens. 24 (86%) tumors were supratentorial. 15 (54%) tumors were astrocytomas (5 glioblastomas, 1 anaplastic astrocytoma, 1 pilocytic astrocytoma, 3 pilomixoid astrocytomas, 2 subependymal giant cell astrocytomas, 3 astrocytomas not otherwise specified (NOS)), 4 (14%) were anaplastic ependymomas, and 9 (32%) were mixed tumors (5 gangliogliomas, 2 gangliocytomas, 2 desmoplastic infantile gangliogliomas (DIGs)). Alive patients were: 4 (67%) affected by high-grade astrocytoma (mean follow-up 64 months), 4 (67%) affected by low-grade astrocytoma (mean follow-up 83 months), 2 (67%) affected by astrocytoma NOS (mean follow-up 60 months), 1 (25%) affected by anaplastic ependymoma (follow-up 12 months), and 9 (100%) affected by mixed tumors (mean follow-up 74 months). H3.3K27M and IDH were not-mutated in any tumor (100%). BRAFV600E mutation was documented in 6 (21%) tumors (4 gangliogliomas, 1 gangliocytoma, and 1 astrocytoma NOS resulted as anaplastic pleomorphic xanthoastrocytoma 8 years later). Gliomas and mixed tumors diagnosed within 1 year of age are morphologically heterogeneous. Moreover, analogously to those affecting older children, they are IDH1-2 and H3.3K27M (when located outside midline) not-mutated while BRAFV600E mutation is typical of gangliogliomas/gangliocytomas and pleomorphic xanthoastrocytomas. High-grade astrocytomas have a more favorable prognosis compared with the same lesions occurring later in life while ependymomas have a poorer outcome.
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- 2021
24. Hippo Pathway in Regulating Drug Resistance of Glioblastoma
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Giacomo Casati, Laura Giunti, Anna Lisa Iorio, Arianna Marturano, Luisa Galli, and Iacopo Sardi
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QH301-705.5 ,Hippo pathway ,Organic Chemistry ,chemoresistance ,General Medicine ,Review ,Catalysis ,signaling pathways ,Computer Science Applications ,Neoplasm Proteins ,Inorganic Chemistry ,Chemistry ,Drug Resistance, Neoplasm ,tumor heterogeneity ,Humans ,glioblastoma (GBM) ,Hippo Signaling Pathway ,tumor microenvironment (TME) ,immunotherapy ,Physical and Theoretical Chemistry ,Biology (General) ,Glioblastoma ,Molecular Biology ,QD1-999 ,Spectroscopy - Abstract
Glioblastoma (GBM) represents the most common and malignant tumor of the Central Nervous System (CNS), affecting both children and adults. GBM is one of the deadliest tumor types and it shows a strong multidrug resistance (MDR) and an immunosuppressive microenvironment which remain a great challenge to therapy. Due to the high recurrence of GBM after treatment, the understanding of the chemoresistance phenomenon and how to stimulate the antitumor immune response in this pathology is crucial. The deregulation of the Hippo pathway is involved in tumor genesis, chemoresistance and immunosuppressive nature of GBM. This pathway is an evolutionarily conserved signaling pathway with a kinase cascade core, which controls the translocation of YAP (Yes-Associated Protein)/TAZ (Transcriptional Co-activator with PDZ-binding Motif) into the nucleus, leading to regulation of organ size and growth. With this review, we want to highlight how chemoresistance and tumor immunosuppression work in GBM and how the Hippo pathway has a key role in them. We linger on the role of the Hippo pathway evaluating the effect of its de-regulation among different human cancers. Moreover, we consider how different pathways are cross-linked with the Hippo signaling in GBM genesis and the hypothetical mechanisms responsible for the Hippo pathway activation in GBM. Furthermore, we describe various drugs targeting the Hippo pathway. In conclusion, all the evidence described largely support a strong involvement of the Hippo pathway in gliomas progression, in the activation of chemoresistance mechanisms and in the development of an immunosuppressive microenvironment. Therefore, this pathway is a promising target for the treatment of high grade gliomas and in particular of GBM.
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- 2021
25. Proton therapy: A therapeutic opportunity for aggressive pediatric meningioma
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Francesco Toni, Maurizio Amichetti, Andrea Pession, Fraia Melchionda, Barbara Rombi, Alessandro Ruggi, Mirko Scagnet, Torunn I. Yock, Giulia Giulietti, Mino Zucchelli, Iacopo Sardi, Viscardo Paolo Fabbri, Francesca Gianno, Silvia Cammelli, Alessio G. Morganti, and Barbara Rombi, Alessandro Ruggi, Iacopo Sardi, Mino Zucchelli, Mirko Scagnet, Francesco Toni, Silvia Cammelli, Giulia Giulietti, Viscardo Paolo Fabbri, Francesca Gianno, Maurizio Amichetti, Torunn Ingrid Yock, Alessio Giuseppe Morganti, Andrea Pession, Fraia Melchionda
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Male ,medicine.medical_specialty ,medicine.medical_treatment ,Economic shortage ,pediatric brain tumors, pediatric meningioma, proton therapy, radiotherapy ,03 medical and health sciences ,0302 clinical medicine ,medicine ,otorhinolaryngologic diseases ,Meningeal Neoplasms ,Proton Therapy ,Humans ,Pediatric meningioma ,Child ,Proton therapy ,business.industry ,Cancer ,Infant ,Hematology ,medicine.disease ,Radiation therapy ,Oncology ,Pediatric brain ,030220 oncology & carcinogenesis ,Pediatrics, Perinatology and Child Health ,Radiology ,business ,Meningioma ,030215 immunology - Abstract
Meningiomas are an extremely rare histology among pediatric brain tumors, and there is a shortage of literature on their management. Proton therapy is currently used safely and effectively for many types of both pediatric and adult cancer, and its main advantage is the sparing of healthy tissues from radiation, which could translate in the reduction of late side effects. We review the literature on radiotherapy and proton therapy for pediatric meningiomas and report clinical outcomes for two aggressive pediatric meningiomas we treated with protons. Proton therapy might be a safe and effective therapeutic option for this rare subgroup of tumors.
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- 2020
26. Primary Intracerebral Alveolar Soft Part Sarcoma: Report of a Case and Review of the Literature
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Anna Maria Buccoliero, Chiara Caporalini, Giampiero Di Giacomo, Selene Moscardi, Rita Alaggio, Regina Mura, Gioia Di Stefano, Iacopo Sardi, Matteo Lenge, Mirko Scagnet, Lorenzo Genitori, Massimo Basile, Angelica Zin, and Flavio Giordano
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Pathology ,medicine.medical_specialty ,Adolescent ,Central nervous system ,Soft Tissue Neoplasms ,Pathology and Forensic Medicine ,Diagnosis, Differential ,03 medical and health sciences ,0302 clinical medicine ,Female patient ,Alveolar soft part sarcoma ,Medicine ,Humans ,Pathological ,business.industry ,Soft tissue ,medicine.disease ,Primary Alveolar Soft Part Sarcoma ,Molecular analysis ,medicine.anatomical_structure ,Sarcoma, Alveolar Soft Part ,030220 oncology & carcinogenesis ,Surgery ,Female ,Anatomy ,Differential diagnosis ,business ,030217 neurology & neurosurgery - Abstract
Alveolar soft part sarcomas (ASPSs) are rare malignant tumors representing ∼1% of all soft tissue sarcomas. Most ASPS occurring in the central nervous system are metastases. In contrast, primary intracranial ASPSs are extremely rare and only 8 cases have been previously reported in English literature. Here, we report a case of primary alveolar soft part sarcoma in a 16-year-old female patient with no evidence of primary extracranial tumors. Histologically this case fulfilled the criteria of ASPS, and a molecular confirmation has been archived. To date, only 9 primary intracranial ASPS cases, including ours, have been reported in the literature. This report highlights the clinical and pathological characteristics, differential diagnosis, and molecular analysis of primary ASPS of the central nervous system.
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- 2021
27. Angiocentric glioma-associated seizures: The possible role of EATT2, pyruvate carboxylase and glutamine synthetase
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Sabrina Rossi, Felice Giangaspero, Anna Maria Buccoliero, Marco Gessi, Lorenzo Genitori, Mariarita Santi, Flavio Giordano, Luca Bertero, Eleonora Aronica, Mirko Scagnet, Selene Moscardi, Vittoria Donofrio, Federico Mussa, Carmen Barba, Valerio Conti, Irene Migliastro, Chiara Caporalini, Francesca Gianno, Francesca Diomedi-Camassei, Renzo Guerrini, Iacopo Sardi, Manila Antonelli, Pathology, APH - Aging & Later Life, APH - Mental Health, and Amsterdam Neuroscience - Cellular & Molecular Mechanisms
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LEAT ,Angiocentric Glioma ,Glutamic Acid ,Pathogenesis ,03 medical and health sciences ,Epilepsy ,Brain ,Central nervous system ,Tumor ,Glutamate-Ammonia Ligase ,Humans ,Pyruvate Carboxylase ,Glioma ,Seizures ,0302 clinical medicine ,Glutamine synthetase ,medicine ,Chemistry ,Glutamate receptor ,General Medicine ,Glutamic acid ,medicine.disease ,Pyruvate carboxylase ,Neurology ,Cancer research ,Neurology (clinical) ,030217 neurology & neurosurgery - Abstract
Purpose Our purpose was to better understand the pathogenesis of seizures associated with angiocentric glioma. Angiocentric glioma is an indolent and rare low-grade glioma. Its typical clinical presentation is with epileptic seizures. The pathogenesis of tumor-associated seizures is poorly understood. Among the possible pathomechanisms, the increased neurotoxic concentrations of the glutamate has been proposed. Glutamate transporters, pyruvate carboxylase and glutamine synthetase are involved in maintaining the physiological concentration of glutamate in the inter synaptic spaces. Methods We evaluated the immunohistochemical expression of EAAT2 (the most important glutamate transporter), pyruvate carboxylase and glutamine synthetase in 17 angiocentric gliomas. Results EAAT2 was never expressed (0%) in the neoplastic cells in none of the cases studied. Pyruvate carboxylase was expressed in the cytoplasm of the neoplastic cells in 16/17 cases (94 %). Glutamine synthetase was expressed in the cytoplasm of the neoplastic cells in 15/17 cases (88 %). Conclusion The net result of this enzymatic expression, in particular considering the loss of EAAT2, could be an increased glutamate concentration in the synaptic clef, which might increase local network excitability initially involving intratumoral neurons. The observation that the angiocentric glioma-associated epilepsy might be at least in part related to EAAT2 deficiency opens up interesting therapeutic perspectives.
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- 2021
28. Case Report: A Case of Glioblastoma in a Patient With Haberland Syndrome
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Chiara Lembo, Iacopo Sardi, Silvia Ferranti, Salvatore Grosso, and Milena Guidi
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medicine.medical_specialty ,tumor ,Brain tumor ,encephalocraniocutaneous lipomatosis ,Case Report ,Pediatrics ,World health ,03 medical and health sciences ,Epilepsy ,Dysgenesis ,0302 clinical medicine ,medicine ,business.industry ,lcsh:RJ1-570 ,Neural tube ,glioblastoma ,Neural crest ,lcsh:Pediatrics ,medicine.disease ,Dermatology ,Haberland syndrome ,medicine.anatomical_structure ,030220 oncology & carcinogenesis ,Pediatrics, Perinatology and Child Health ,Encephalocraniocutaneous Lipomatosis ,epilepsy ,business ,030217 neurology & neurosurgery ,Glioblastoma - Abstract
Haberland syndrome or encephalocraniocutaneous lipomatosis is a rare ectomesodermal dysgenesis defined by the triad including ocular, skin, and central nervous system involvement, which is commonly unilateral. This disorder is attributed to a post-zygotic mutation responsible for a neural tube and neural crest dysgenesis. We report the case of a 15-year-old female with Haberland syndrome with pharmacoresistant epilepsy who developed a World Health Organization-grade IV glioblastoma. This is the first case of pediatric glioblastoma associated with Haberland syndrome. The previously reported pediatric cases included benign brain tumors. To our knowledge, this is the fifth case of brain tumor associated with encephalocraniocutaneous lipomatosis and the second case of glioblastoma associated with this syndrome. The hypothesis that Haberland syndrome is associated with an increased risk of tumor development is intriguing, although the rarity of the condition is nowadays preventing us from drawing definitive conclusions about this potential link between the two entities. Further studies are needed to establish the real relationship between encephalocraniocutaneous lipomatosis and the risk of brain tumors.
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- 2021
29. Genetic signature and treatment of pediatric high-grade glioma
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Luisa Galli, Anna Maria Buccoliero, Laura Giunti, Milena Guidi, Lorenzo Genitori, M Censullo, Iacopo Sardi, and Chiara Caporalini
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Oncology ,Cancer Research ,medicine.medical_specialty ,business.industry ,Cancer ,Articles ,medicine.disease ,Malignancy ,Genetic analysis ,Molecular medicine ,03 medical and health sciences ,Histone H3 ,0302 clinical medicine ,030220 oncology & carcinogenesis ,Glioma ,Internal medicine ,Mutation (genetic algorithm) ,medicine ,030211 gastroenterology & hepatology ,business ,Anaplastic astrocytoma - Abstract
Pediatric high-grade glioma (HGG) is a type of malignancy that carries a poor prognosis. The genetic analysis of HGGs has previously identified useful mutations, the targeting of which has improved prognosis. Thus, further research into the more common mutations, such as H3 histone variants (HIST1H3B and H3F3A) and BRAF V600E, may be useful in identifying tumors with different prognoses, as the mutations are considered to drive two distinct oncogenic programs. The present study performed a retrospective analysis of pediatric HGGs. In total, 42 cases of HGG, including 32 cases (76.1%) of anaplastic astrocytoma and 10 cases (23.8%) of glioblastoma multiforme (GBM), were assessed. The median age of the patients was 7 years (range, 0-32 years). Mutations on histone H3, in particular the K27M and G34R mutations in the distinct variants HIST1H3B and H3F3A, in addition to the presence of the BRAF V600E mutation, were analyzed in 24 patients. The H3F3A K27M mutation was identified in 7 patients (29.1%), while the HIST1H3B K27M mutation was only observed in 1 patient with GBM. In addition, 5 patients harbored a BRAF V600E mutation (21%), while the H3F3A G34R mutation was not recorded in any of the patients. The overall survival of the wild-type patients at 20 months was 68% [confidence interval (CI): 38-85%] compared with 28% (CI: 0.4-60%) in patients with the H3F3A K27M mutation. These results suggested that patients with the H3F3A K27M mutation had a worse prognosis compared with wild-type patients (P=0.0045). Moreover, 3/5 patients with the BRAF V600E mutation had HGGs that were derived from a previous low-grade glioma (LGG; P=0.001). In conclusion, these results suggested that histone H3 mutations may help predict the outcome in patients with HGG. In addition, the BRAF V600E mutation was found to be associated with an increased risk of anaplastic progression. The novel data of the present study may help better define the clinical and radiological characteristics of glioma.
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- 2021
30. Contributors
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Manmeet S. Ahluwalia, Mohammed Ahmed, Mohsen Akbari, Alvaro G. Alvarado, Meitham Amereh, Kartik Angara, Ali S. Arbab, David M. Ashley, Ryan J. Atkins, Husam A. Babikir, Stephen J. Bagley, Kristen A. Batich, Sabrina Battista, Giacomo Casati, Maria Luigia Censullo, Laura Cerchia, Niall M. Corcoran, Alex Cordero, Sunit Das, Sanaz Dastghaib, Xavier Declèves, Cecilia Diceglie, Nicholas J. Dunne, Adam Eljarrah, Jawad Fares, Monica Fedele, Henry S. Friedman, Marina Gergues, Saeid Ghavami, Laura Giunti, Milena Guidi, Kshama Gupta, Sima Hajiahmadi, Akira Hara, Christopher M. Hovens, Ahmed Idbaih, Anna Lisa Iorio, Toru Iwama, Mohammed Jaloudi, M. Janaki Ramaiah, Lynn Jena, David Olayinka Kamson, Deepak Kanojia, Mustafa Khasraw, Harmon Singh Khela, Takamasa Kinoshita, Gaspar J. Kitange, Harley I. Kornblum, Vijay Kumar Kutala, John Laterra, Hakho Lee, Sang Y. Lee, Maciej S. Lesniak, James K. Liu, Alessia Lo Dico, Kirsten Ludwig, William T. Maich, Theo Mantamadiotis, Cristina Martelli, Tarik F. Massoud, Helen O. McCarthy, Masafumi Miyai, Shaik Mohammad Naushad, Pooneh Mokarram, Ahmed Musah-Eroje, Sree Deepthi Muthukrishnan, Arutselvan Natarajan, Marina Nikolopoulos, Luisa Ottobrini, Ramasamy Paulmurugan, David Prado, Pranela Rameshwar, Yasmeen Rauf, Rajasekhar Reddy Manyam, Barbara Rombi, Sabra K. Salim, Daniela Salvatore, John H. Sampson, Iacopo Sardi, Neil Savage, Vibha Harindra Savanur, Amir Seyfoori, Zahra Shahsavari, Huilin Shao, Shahla Shojaei, Sheila K. Singh, Georgios Solomou, Laura A. Sordillo, Peter P. Sordillo, Stanley S. Stylli, Uday Kumar Sukumar, Hiroyuki Tomita, Arata Tomiyama, Ilya Ulasov, Chitra Venugopal, Maite Verreault, Colin Watts, Chi Yan Wong, and Mozhdeh Zamani
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- 2021
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31. Drug penetration through the blood–brain barrier after radiotherapy: New approaches to bypass glioblastoma chemoresistance
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M Censullo, Barbara Rombi, Laura Giunti, Anna Lisa Iorio, Milena Guidi, Iacopo Sardi, and Giacomo Casati
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Chemotherapy ,Microglia ,business.industry ,medicine.medical_treatment ,Blood–brain barrier ,medicine.disease ,Radiation therapy ,medicine.anatomical_structure ,In vivo ,Glioma ,medicine ,Cancer research ,Doxorubicin ,Stem cell ,business ,medicine.drug - Abstract
Glioblastoma (GBM) is one of the most aggressive tumors known. For many years, the most varied therapeutic strategies have been adopted without obtaining significant prognostic results. Intrinsic resistance of GBM is due to the interaction between tumor and microglia cells, especially in a hypoxic microenvironment. Instead, the blood–brain barrier (BBB) plays an essential role of extrinsic resistance to certain drugs preventing their release into the brain. Although in vitro and in vivo studies show that doxorubicin is a highly toxic chemotherapy agent for glioma cells, its effectiveness in the treatment of GBM is limited by efflux pumps that actively expel this agent at the BBB level. Realistically, mechanical damage induced by radiation therapy temporarily modifies the BBB making it more permeable to anthracyclines. Whole brain radiotherapy (WBRT) could be a novel approach to alter the whole BBB allowing effective drugs, such as doxorubicin, to reach diffuse GBM stem cells at therapeutic doses.
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- 2021
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32. GCT-01. Pediatric intracranial germ cell tumors and primary polyuria-polydipsia syndrome: a 13-year single institutional experience
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Rossana Pavone, Carla Fonte, Franco Ricci, Gaia Varriale, Giorgia Enrico, Maria Luigia Censullo, Carlotta Gemma Gori, Milena Guidi, Anna Maria Buccoliero, Chiara Caporalini, Lorenzo Genitori, and Iacopo Sardi
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Cancer Research ,Oncology ,Neurology (clinical) - Abstract
Intracranial germ cell tumors (IGCTs) represent about 4% of all childhood brain tumors. They are common in both the pineal and pituitary regions and sometimes they can be bifocal. Suprasellar and bifocal IGCTs usually present stereotypical symptoms, including primary polyuria-polydipsia syndrome (PPS). Consolidated IGCTs’ therapy is based on the International Society of Pediatric Oncologic (SIOP) CNS GCT II protocol consisting of primary pre-radiation chemotherapy combining etoposide, carboplatin and/or cisplatin and ifosfamide. PPS management in these patients requires monitoring of electrolytes and fluids during chemotherapy, especially for cisplatin and/or ifosfamide-based cycles, for which hyperhydratation is required. We report the results of our single-center cohort of patients with IGCTs treated between 2008 and 2021, focusing on the clinical presentation, treatment and long-term follow-up. Thirty-one patients were analyzed (median age=13 years, 87% male). Twelve children (39%) presented a PPS and needed desmopressin treatment, maintained at long-term follow-up data update in all. Over these PPS patients, 6 had bifocal germinomas, 4 suprasellar germinomas, 1 metastatic germinoma and 1 non-germinomatous IGCT. Eleven PPS children (92%) received cisplatin and/or ifosfamide-based chemotherapy: all of them had optimal biochemical urine and blood investigations before, during and after chemotherapy. None of them presented serious complications during treatment. After a median follow-up of 5 years, two patients (6.5%) died (1 IGCT-related, 1 non-cancer related) and one had a second malignancy (parotid gland mucoepidermoid carcinoma, 6 years after IGCT diagnosis). Childhood IGCTs have an excellent prognosis, but present a significant risk of long-lasting severe endocrine sequelae which may be worsened by the primary oncological strategy, requiring careful management of complications related to fluid and electrolytes disturbances. In order to avoid post-treatment pituitary insufficiency, guidelines for diabetes insipidus management when cisplatin and/or ifosfamide-based protocols are used should be established and all patients should receive meticulous endocrine follow-up.
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- 2022
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33. QOL-25. Neurocognitive assessment of pediatric medulloblastoma treated by MBMET_MEYER trial. Censullo M.L1, Bertoluzzo G2, Fonte C1, Pavone R1, Guidi M1, Enrico G1, Gori C.G1, Martin R2, Teodori C2, Sardi I1 1Neuro-Oncology Unit, Department of Pediatric Oncology, Meyer Children’s University Hospital, Florence, Italy2Psychology Unit, Meyer Children’s University Hospital, Florence, Italy
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Maria Luigia Censullo, Giulia Bertoluzzo, Carla Fonte, Rossana Pavone, Milena Guidi, Enrico Giorgia, Carlotta Gemma Gori, Rosanna Martin, Caterina Teodori, and Iacopo Sardi
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Cancer Research ,Oncology ,Neurology (clinical) - Abstract
The MBMET_MEYER is an interventistic monocentric trial of Meyer Children’s Hospital. The goal of this protocol is to reduce toxicity by use of protontherapy and reducing chemo-induced neurotoxicity by limited use of high dose chemotherapy. To date, a neurocognitive assessment is the standard in medulloblastomas but it is very difficult an assessment at baseline for clinical problems such as age, intracranial hypertension and immediate intervention. 10 neurocognitive assessments were reviewed in patients with medulloblastoma treated by MBMET_MEYER protocol: 3 anaplastic medulloblastoma M0 and 7 classic (2 M0, 1 M1, 1 M2, 3 M3). The median age was 10 years (range 5-18). All the patients were treated with surgery (gross total removal), 2 received chemotherapy and conventional radiotherapy, 8 chemotherapy and protontherapy and only 1 received autologos-hemotopoietic stem cell transplant for progression disease after induction chemotherapy. As for protocol, the neurocognitive assessment was defined by Weschler Intelligence Scales, fonemic and semantic fluency, immediate and deferred memory, tests for working memory, attention and visuo-spatial tests at baseline, after treatment and at the end of follow-up. For 3 patients it was not possible a baseline assessment for bad clinic conditions, 8 are still in treatment. From interviews and assessments emerged that 80% of patients had neurocognitive deficits: at baseline 5 had speed elaboration difficulties, 1 of these also presented verbal deficit, 1 showed problems in recalling verbal material and 1 in working memory; after two years from chemotherapy and radiotherapy 2 presented speed processig and working memory deficit. In conclusion, an assessment at baseline is very difficult for post-surgical problems but necessary to perform as soon. In this way, it is possible to evaluate the impact of the treatment on neurocognitive impairment. Further investigations are necessary to well understand the appropriate schedule of neurocognitive assessment of pediatric medulloblastoma.
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- 2022
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34. P04.20 The role of YAP in Glioblastoma cell lines
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A Marturano, Iacopo Sardi, Laura Giunti, G Casati, and Anna Lisa Iorio
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Cancer Research ,Cell growth ,Autophagy ,Cancer ,Biology ,medicine.disease ,Cell nucleus ,medicine.anatomical_structure ,Oncology ,Cell culture ,Apoptosis ,Cancer research ,medicine ,Neurology (clinical) ,Signal transduction ,Transcription factor - Abstract
BACKGROUND Glioblastoma (GBM) is a primary human malignant brain tumor, the most common in adults. Several studies have highlighted the Hippo-pathway as a cancer signalling network. The Hippo pathway is an evolutionarily conserved signal cascade, which is involved in the control of organ growth. Dysregulations among this pathway have been found in lung, ovarian, liver and colorectal cancer. The key downstream effector of the Hippo-pathway is the Yes-associated protein (YAP); in the nucleus, its function as transcription co-activator is to interact with transcription factors, resulting in the expression of target genes involved in pro-proliferating and anti-apoptotic programs. MATERIAL AND METHODS Using western blotting analysis, we determined the nuclear expression of YAP on three GBM cell lines (U87MG, T98G and A172). To investigate which inhibitors against the Hippo-pathway were the most efficient, we performed a cytotoxic assay: we treated all the three cell lines with different inhibitors such as Verteporfin (VP), Cytochalasin D (CIT), Latrunculin A (LAT), Dobutamine (DOB) and Y27632. Afterwards, we performed a treatment using Doxorubicin (DOX) combined with the inhibitors, evaluating its cytotoxic effect on our cell lines, through cell viability experiments. More western blotting experiments were performed to investigate the oncogenic role of YAP at nucleus level. Furthermore, preliminary experiments have been conducted in order to investigate the apoptosis, senescence and autophagy modulation due to the Hippo-pathway. RESULTS We showed our cell lines express nuclear YAP. We assessed the efficiency of the main inhibitors against Hippo-pathway, proving that VP, LAT A and CIT show a strong cytostatic effect, linked to time increase; plus we saw a cytotoxic effect on T98G. The association of DOX with selected inhibitors is able to reduce cell viability and nuclear YAP expression rate in all three GBM lines. Finally, preliminary experiments were set up to assess how and if the mechanisms of apoptosis, autophagy and senescence were affected by the Hippo-pathway. The combination of DOX with inhibitors promotes resistance to apoptosis. CONCLUSION Our results show that nuclear YAP is present in all tumor lines, thus confirming that this molecular pathway is functioning in GBM lines. Nuclear YAP is more highly expressed after DOX administration. Moreover, the combined treatment (DOX with Hippo-pathway inhibitors) reduces both cell proliferation and viability, and increases the rate of apoptosis. Preliminary experiments on senescence and autophagy were used to determine the best Hippo-pathway inhibitor. These data demonstrate that the Hippo-pathway plays a crucial role in GBM proliferation and resistance to apoptosis. Inhibiting this pathway and in particular the transcription factor YAP, in association with DOX, might be an excellent therapeutic target.
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- 2021
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35. Neurosurgical treatment of subependymal giant cell astrocytomas in tuberous sclerosis complex: a series of 44 surgical procedures in 31 patients
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Flavio Giordano, Renzo Guerrini, Matteo Lenge, Francesco Mari, Lorenzo Mongardi, Anna Maria Buccoliero, Eleonora Aronica, Carla Moscheo, Iacopo Sardi, Roberto Biagiotti, Lorenzo Genitori, Pathology, ANS - Cellular & Molecular Mechanisms, APH - Aging & Later Life, and APH - Mental Health
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medicine.medical_specialty ,mTOR inhibitors ,Astrocytoma ,03 medical and health sciences ,Tuberous sclerosis ,0302 clinical medicine ,Tuberous Sclerosis ,Subependymal zone ,medicine ,Humans ,030212 general & internal medicine ,Child ,Retrospective Studies ,Tuberous sclerosis complex (TSC) ,Tumor size ,business.industry ,Brain Neoplasms ,General Medicine ,Surgical procedures ,Discovery and development of mTOR inhibitors ,medicine.disease ,Hydrocephalus ,Surgery ,Subependymal giant cell astrocytoma (SEGA) ,Giant cell ,Pediatrics, Perinatology and Child Health ,Neurology (clinical) ,Neurosurgery ,Neoplasm Recurrence, Local ,business ,030217 neurology & neurosurgery - Abstract
Background: Subependymal giant cell astrocytomas (SEGA) are benign tumors characteristic of tuberous sclerosis complex (TSC) that may cause hydrocephalus. Various treatments are nowadays available as mTOR inhibitors or surgery. Surgery is still a valid option especially for symptomatic and larger tumors. Methods: From January 1994 to December 2015, 31 TSC patients harboring SEGA underwent surgery at the Department of Neurosurgery of the Meyer Pediatric Hospital, Florence. Indications for surgery were tumor size and location, growth and cystization/hemorrhage, and hydrocephalus. Clinical data, preoperative and postoperative MRI, recurrence rate, further surgical procedures, and related complications were analyzed. Results: A total of 44 surgeries were performed in 31 TSC patients affected by SEGA, achieving gross total removal (GTR) and subtotal removal (STR), respectively, in 36 and 8 patients. Recurrences occurred in 11 patients; 9 of them underwent further surgical procedures and 2 were treated with mTOR pathway inhibitors. Surgical morbidity and mortality were, respectively, 22.7% and 2.3%. After a mean follow-up of 4.9 years, 90% of patients were tumor-free with good neurological status in 93.3%; twelve (40%) had a ventriculo-peritoneal shunt (VPS) for hydrocephalus. Conclusions: The present series confirms that the surgical approach, combined with mTOR inhibitors, is still a valid option for the treatment of SEGAs.
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- 2020
36. Use of High-Dose Chemotherapy in Front-Line Therapy of Infants Aged Less Than 12 Months Treated for Aggressive Brain Tumors
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Mariarita Santi, Salvatore De Masi, Lorenzo Genitori, Barbara Spacca, Iacopo Sardi, Anna Maria Buccoliero, Milena Guidi, and Laura Giunti
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Oncology ,medicine.medical_specialty ,medicine.medical_treatment ,Brain tumor ,030204 cardiovascular system & hematology ,chemotherapy ,Pediatrics ,03 medical and health sciences ,0302 clinical medicine ,newborn ,030225 pediatrics ,Internal medicine ,medicine ,Original Research ,Chemotherapy ,business.industry ,Not Otherwise Specified ,glioblastoma ,lcsh:RJ1-570 ,Induction chemotherapy ,Astrocytoma ,lcsh:Pediatrics ,medicine.disease ,Chemotherapy regimen ,Regimen ,congenital tumor ,Pediatrics, Perinatology and Child Health ,business ,brain tumor ,Anaplastic astrocytoma - Abstract
Introduction: Malignant brain tumors in infants less than 12 months of age are extremely rare, and they have poor prognosis. We evaluated genetic characteristics and response rates of infants with congenital brain tumors subjected to high-dose chemotherapy and autologous stem cell transplant after gross total tumor resection. Materials and Methods: In total, 10 infants, aged less than 12 months, were enrolled in this study. The median age was 56 days (range: 1-279 days). Pathological examination demonstrated the following: four anaplastic astrocytomas, two glioblastomas, two central nervous system (CNS) embryonal tumors, not otherwise specified (NOS), and two atypical teratoid/rhabdoid tumors. Results: All patients were exposed to induction chemotherapy regimen, two high-dose chemotherapy courses, and autologous stem cell transplant after maximal surgery. At 1-3-5 years, the global overall survival (OS) was 90, 70, and 70% and the progression-free survival (PFS) was 80-60 and 60%. In all the patients, the copy number variants (CNVs) profile was analyzed using the SNP/CGH array approach. To investigate the clinical relevance of germline SMARCB1 mutation in AT/RT patients, we performed sequence analysis of the coding regions. The two patients with AT/RT were found to have germline SMARCB1 mutations. No BRAF mutations were found, and only NTRK gene fusion was present in one patient. We also have examined the association with OS and PFS and different histological subtypes of infant CNS proving that high-grade astrocytoma has better overall survival than other tumor types (p: 0.007 and p: 0.0590). Conclusion: High-dose chemotherapy regimen represents a valid therapeutic approach for congenital brain tumors with a high rate of response. The molecular analysis has to be analyzed in all infants' brain tumor types. High-grade gliomas are characterized by a better prognosis than other histologies of infant CNS.
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- 2020
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37. EPEN-03. LONG-TERM FOLLOW-UP OF AIEOP 2ND SERIES OF CHILDREN AND ADOLESCENT WITH PRIMARY INTRACRANIAL (ST:SUPRATENTORIAL; PF: POSTERIOR FOSSA) EPENDYMOMA AND METHYLATION GROUPS RE-ANALYSES
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Luisa Chiapparini, Francesco Barretta, Simone Minasi, Elisabetta Schiavello, Piergiorgio Modena, Lucia Quaglietta, Maria Luisa Garrè, Maura Massimino, Alessandra Erbetta, Stefan M. Pfister, Luna Boschetti, Felice Giangaspero, Antonio Ruggiero, Pascal Johann, Angela Mastronuzzi, Iacopo Sardi, Manila Antonelli, Veronica Biassoni, Francesca R. Buttarelli, Bianca Pollo, Annamaria Buccoliero, Kristian W. Pajtler, Lorenza Gandola, Hendrik Witt, Maurizio Mascarin, Daniele Bertin, and Elisabetta Viscardi
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Ependymoma ,Pleomorphic xanthoastrocytoma ,Cancer Research ,Series (stratigraphy) ,Pediatrics ,medicine.medical_specialty ,business.industry ,Long term follow up ,Posterior fossa ,medicine.disease ,Pharmaceutical Adjuvants ,Oncology ,Second Look Surgery ,medicine ,AcademicSubjects/MED00300 ,AcademicSubjects/MED00310 ,Neurology (clinical) ,business - Abstract
BACKGROUND This 2002–2014 Italian prospective study stratified 160 patients by surgical resection (complete=NED/incomplete=ED) and centrally-reviewed grade. Grade2/NED patients received focal radiotherapy (RT) up to 59.4Gy, Grade3/NED received 4 courses of VEC(vincristine,etoposide,cyclophosphamide) after RT.ED patients received 1–4 VEC courses, second-look surgery, 59.4 Gy+8Gy boost on measurable residue. METHODS We re-analyzed data at 115 months follow-up including methylation profile on available samples. RESULTS Global PFS/OS at 5/10 years were 66/59% and 80/74%, respectively. Of the 64 relapsers at median 20 months, 53 died at median 37/18 months after diagnosis/relapse, respectively.10/64 relapsed after 5 years (66–126 months); 4 died, relapse was local in 8/10, metastatic 1, combined 1;5/10 patients were below age 3, 5 females, 8 PF tumors. Their survival post-relapse was not longer than earlier relapsers’. At univariable analysis, age over 3 years, female sex, complete surgery, grade 2, no shunt confirmed better PFS/OS. 66/95 analyzed tumors received a score >0.80 through the DNA methylation-based central nervous system tumor classifier: 41/8 as PFA/PFB, respectively,14/17 ST as RELA-positive (3 scored for other molecular entities i.e. anaplastic PXA, LGG MYB, HGNET). Prognostic factors were equally distributed among PFA/PFB groups,1 only group B patient relapsed locally at 96 months. CONCLUSIONS Already published prognostic factors remained at long-term follow-up;6.2% patients had late relapses. OS after relapse was not better in late relapsers. Group B confirmed better prognosis but all patients had received «at least» adjuvant RT. Modern ependymoma trials need long follow-up to draw firm conclusions.
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- 2020
38. Targeting GD2-positive glioblastoma by chimeric antigen receptor empowered mesenchymal progenitors
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Malvina Prapa, Giacomo Pavesi, Marco Bestagno, Iacopo Sardi, Edwin M. Horwitz, Massimo Dominici, Alberto Feletti, Giulia Grisendi, Franco Bambi, Filippo Rossignoli, Giulia Golinelli, Carlotta Spano, and Monica Cellini
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0301 basic medicine ,Cancer Research ,Stromal cell ,Cell ,Drug development ,Biology ,Immunotherapy, Adoptive ,Article ,03 medical and health sciences ,Targeted therapies ,0302 clinical medicine ,Antigen ,Antigens, Neoplasm ,Cell Line, Tumor ,Gangliosides ,Neuroblastoma ,medicine ,Humans ,Progenitor cell ,Molecular Biology ,Receptors, Chimeric Antigen ,Brain Neoplasms ,Mesenchymal stem cell ,Mesenchymal Stem Cells ,medicine.disease ,Chimeric antigen receptor ,CNS cancer ,Molecular Medicine ,030104 developmental biology ,medicine.anatomical_structure ,030220 oncology & carcinogenesis ,Cancer research ,Female ,Stem cell ,Glioblastoma - Abstract
Tumor targeting by genetically modified mesenchymal stromal/stem cells (MSCs) carrying anti-cancer molecules represents a promising cell-based strategy. We previously showed that the pro-apoptotic agent tumor necrosis factor-related apoptosis-inducing ligand (TRAIL) can be successfully delivered by MSCs to cancer sites. While the interaction between TRAIL and its receptors is clear, more obscure is the way in which MSCs can selectively target tumors and their antigens. Several neuroectoderm-derived neoplasms, including glioblastoma (GBM), sarcomas, and neuroblastoma, express high levels of the tumor-associated antigen GD2. We have already challenged this cell surface disialoganglioside by a chimeric antigen receptor (CAR)-T cell approach against neuroblastoma. With the intent to maximize the therapeutic profile of MSCs delivering TRAIL, we here originally developed a bi-functional strategy where TRAIL is delivered by MSCs that are also gene modified with the truncated form of the anti-GD2 CAR (GD2 tCAR) to mediate an immunoselective recognition of GD2-positive tumors. These bi-functional MSCs expressed high levels of TRAIL and GD2 tCAR associated with a robust anti-tumor activity against GD2-positive GBM cells. Most importantly, the anti-cancer action was reinforced by the enhanced targeting potential of such bi-functional cells. Collectively, our results suggest that a truncated anti-GD2 CAR might be a powerful new tool to redirect MSCs carrying TRAIL against GD2-expressing tumors. This affinity-based dual targeting holds the promise to combine site-specific and prolonged retention of MSCs in GD2-expressing tumors, thereby providing a more effective delivery of TRAIL for still incurable cancers.
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- 2018
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39. Dysembryoplastic neuroepithelial tumors: A single-institutional series with special reference to glutamine synthetase expression
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Carmen Barba, Anna Maria Buccoliero, Federico Mussa, Gianna Baroni, Chiara Caporalini, Selene Moscardi, Iacopo Sardi, Mirko Scagnet, Gioia Di Stefano, Lorenzo Genitori, and Flavio Giordano
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Male ,0301 basic medicine ,Pathology ,medicine.medical_specialty ,Adolescent ,Central nervous system ,Biology ,Pathology and Forensic Medicine ,Young Adult ,03 medical and health sciences ,0302 clinical medicine ,Glutamate-Ammonia Ligase ,Glutamine synthetase ,medicine ,Humans ,Neoplasm ,Premovement neuronal activity ,Child ,Neurons ,Brain Neoplasms ,Glutamate receptor ,Glioma ,General Medicine ,medicine.disease ,Immunohistochemistry ,Neoplasms, Neuroepithelial ,Glutamine ,030104 developmental biology ,medicine.anatomical_structure ,Cerebral cortex ,Astrocytes ,Child, Preschool ,030220 oncology & carcinogenesis ,Cancer research ,Female - Abstract
Dysembryoplastic neuroepithelial tumors (DNT) is a benign (World Health Organisation, WHO, grade I) glioneuronal tumor and it represent one of the most frequent neoplasm in patient affected by seizures. The epileptic neuronal activity can be determined by abnormal synchronization, excessive glutamate excitation and\or inadequate GABA inhibition. Increasing evidence suggests that the astrocytes might be involved in this process even if neurons play a relevant role. In particular astrocytes promote the clearance of glutamate, a potent excitatory neurotransmitter of the central nervous system. Indeed, elevated concentrations of extracellular glutamate may determine iper-excitability and seizures as well as other neurological disorders. So, astrocytes, converting glutamate into glutamine via the enzyme glutamine synthetase (GS), could play a protective anti-seizures role. In the present study, we analyzed the immunohistochemical expression of GS in 20 DNTs specimens documenting a constant immunoistochemical expression of GS in astrocytes of the lesional tissue and of the cerebral cortex.
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- 2021
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40. Corrigendum to ‘Angiocentric glioma-associated seizures: The possible role of EATT2, pyruvate carboxylase and glutamine synthetase [Seizure: European Journal of Epilepsy 86 (2021) 152-154]
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Sabrina Rossi, Valerio Conti, Francesca Diomedi-Camassei, Manila Antonelli, Flavio Giordano, Carmen Barba, Luca Bertero, Anna Maria Buccoliero, Lorenzo Genitori, Federico Mussa, Vittoria Donofrio, Iacopo Sardi, Eleonora Aronica, Felice Giangaspero, Irene Migliastro, Selene Moscardi, Mariarita Santi, Marco Gessi, Renzo Guerrini, Chiara Caporalini, Francesca Gianno, and Mirko Scagnet
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Epilepsy ,Neurology ,Angiocentric Glioma ,Glutamine synthetase ,Cancer research ,medicine ,Neurology (clinical) ,General Medicine ,Biology ,medicine.disease ,Pyruvate carboxylase - Published
- 2021
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41. P06.07 Germline mutation of SMARCE1 gene in a family with spinal meningiomas
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Laura Giunti, Lorenzo Genitori, Anna Lisa Iorio, V Serio, G Casati, E Fiorentini, Annamaria Buccoliero, A Marturano, B Rinaldi, and Iacopo Sardi
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Cancer Research ,Germline mutation ,Oncology ,Spinal Meningiomas ,Cancer research ,Neurology (clinical) ,Biology ,SMARCE1 Gene - Abstract
BACKGROUND Meningioma is the most common benign primary intracranial tumor, arising from arachnoid cells of the meninges, but in 20% of cases displays aggressive behavior. Meningiomas are mainly sporadic and the familial forms are very rare. Meningioma account for a small subset (1–4%) of all pediatric brain tumors and may be associated with hereditary tumor predisposition syndrome caused by germline mutations of NF2, SMARCB1, SUFU, and SMARCE1 genes. MATERIAL AND METHODS We present a case of a 16-year-old girl with spinal clear cell meningiomas (CCMs) WHO II with a second spinal lesion identified during the follow-up. Considering the multiple lesions, we performed Whole Exome Sequencing (WES) on DNA from peripheral blood to search for an underlying CCMs tumor predisposition syndrome (#607174). RESULTS We identified a heterozygous frameshift variant c.439delA (p.Ser147fs) in SMARCE1, chromatin remodelling factor that acts as a tumor suppressor gene. Meningioma analysis by Sanger sequencing showed a loss of heterozygosity (LOH) of the wild-type allele. We identified the c.439delA in the constitutional DNA of the father and the sister but not in the mother. At the moment, the father is asymptomatic and the 14 years old sister showed two spinal lesions (meningiomas likely) at the first MRI. CONCLUSION We report a family study of hereditary tumor predisposition syndrome to CCMs with SMARCE1 mutation in which are present two asymptomatic carriers with different ages and gender. The asymptomatic carriers will undergo neurological examination and MRI of the brain and spine, according to a screening protocol. The incomplete penetrance phenomenon is known in SMARCE1-related families with CCMs and it is probably due to the interaction of SMARCE1 with yet unidentified genes.
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- 2021
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42. Tumor response of temozolomide in combination with morphine in a xenograft model of human glioblastoma
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Anna Lisa Iorio, Giacomo Laffi, Maurizio de Martino, Francesco Cardile, Lorenzo Genitori, Claudio Pisano, Martina Da Ros, Maurizio Lucchesi, Fabiana Colelli, Iacopo Sardi, and Giacomo Signorino
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0301 basic medicine ,Oncology ,medicine.medical_specialty ,medicine.medical_treatment ,Animal model ,Blood-brain barrier ,Glioblastoma ,Morphine ,Temozolomide ,temozolomide ,Pharmacology ,Blood–brain barrier ,03 medical and health sciences ,0302 clinical medicine ,In vivo ,Internal medicine ,medicine ,Chemotherapy ,business.industry ,animal model ,glioblastoma ,morphine ,blood-brain barrier ,medicine.disease ,Radiation therapy ,030104 developmental biology ,medicine.anatomical_structure ,030220 oncology & carcinogenesis ,Toxicity ,business ,Research Paper ,medicine.drug - Abstract
// Anna Lisa Iorio 1 , Martina da Ros 1 , Lorenzo Genitori 1 , Maurizio Lucchesi 1 , Fabiana Colelli 2 , Giacomo Signorino 2 , Francesco Cardile 2 , Giacomo Laffi 3 , Maurizio de Martino 1 , Claudio Pisano 2 and Iacopo Sardi 1 1 Neuro-Oncology Unit, Department of Pediatric Oncology, Meyer Children’s Hospital, Florence, Italy 2 BIOGEM Research Institute, Ariano Irpino, Italy 3 Department of Experimental and Clinical Medicine, University of Florence, Florence, Italy Correspondence to: Iacopo Sardi, email: iacopo.sardi@meyer.it Keywords: temozolomide, glioblastoma, morphine, blood-brain barrier, animal model Received: November 15, 2016 Accepted: July 13, 2017 Published: August 03, 2017 ABSTRACT Despite multimodal treatments comprising, radiation therapy (RT) and chemotherapy with temozolomide (TMZ), the prognosis of glioblastoma multiforme (GBM) remains dismal and consolidated therapy yields a median survival of 14.6 months. Blood Brain Barrier (BBB) mediated chemoresistance and high dose related toxicity make necessary the development of new therapeutic approach to sensitize GBM to TMZ. The aim of the present study was to investigate the potential of the treatment morphine plus TMZ metronmic doses (1,77 and 0,9 mg/kg) in GBM therapy. The effect of morphine, on tumor cell growth and P-glycoprothein (P-gp) activity, was investigate in in vitro models. The results demonstrated that GBM cells growth is not influenced by morphine treatment and, for the first time, we show that morphine is an inhibitor of the activity of P-gp efflux transporter who is markedly expressed on BBB. In vivo , response to the treatments TMZ plus morphine was investigated in an orthotopic nude mice model of GBM. Animals treated with TMZ metronomic doses showed a significant tumor growth inhibition compared to untreated mice and association with morphine appears to improve TMZ efficacy. Moreover, the combination of morphine with lower dose of TMZ result in a cytostatic effect on tumor growth over the period of the pharmacological treatments. In conclusion this novel approach could be a successful strategy to overcome chemoresistance and side effects TMZ mediated, reducing drug dosage and improving long term response, in GBM therapy.
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- 2017
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43. Role of eculizumab in a pediatric refractory gemcitabine-induced thrombotic microangiopathy: a case report
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Alessia Stival, Veronica Tintori, Maurizio de Martino, Marco Materassi, Maurizio Lucchesi, Iacopo Sardi, L. Facchini, S. Farina, Rosa Maria Roperto, and Francesca Melosi
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Male ,Antimetabolites, Antineoplastic ,medicine.medical_specialty ,Thrombotic microangiopathy ,medicine.medical_treatment ,030232 urology & nephrology ,lcsh:Medicine ,Case Report ,Antibodies, Monoclonal, Humanized ,Deoxycytidine ,Gastroenterology ,Brain tumors ,03 medical and health sciences ,Fatal Outcome ,0302 clinical medicine ,Internal medicine ,medicine ,Humans ,Cerebellar Neoplasms ,Medulloblastoma ,Chemotherapy ,Radiotherapy ,business.industry ,Microangiopathy ,lcsh:R ,General Medicine ,Eculizumab ,medicine.disease ,Gemcitabine ,Oxaliplatin ,Complement Inactivating Agents ,Child, Preschool ,030220 oncology & carcinogenesis ,Hemolytic-Uremic Syndrome ,Immunology ,Rituximab ,business ,medicine.drug - Abstract
Background The incidence of gemcitabine-induced hemolytic uremic syndrome has already been described in adults. Several approaches have been employed in the treatment of gemcitabine-induced hemolytic uremic syndrome with different outcomes. One of the most promising agents is eculizumab, which is a monoclonal antibody directed against C5 complement protein. Case presentation We reported the case of a 3-year-old white boy with medulloblastoma who underwent high-dose chemotherapy and craniospinal irradiation. Afterwards he started maintenance chemotherapy with gemcitabine and oxaliplatin. After five courses he presented a progressive clinical worsening, which resulted in a systemic thrombotic microangiopathy. Initially he was treated with rituximab without clinical improvement. Therefore he started therapy with repeated cycles of eculizumab. After seven infusions he showed a gradual improvement and finally a complete remission of gemcitabine-induced hemolytic uremic syndrome. Conclusions Eculizumab prevents serious complement-mediated vascular damage for chemotherapy-induced thrombotic microangiopathy in pediatric cases.
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- 2017
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44. P14.46 SUBEPENDYMAL GIANT CELLS ASTROCYTOMA (SEGA) IN TUBEROUS SCLEROSIS COMPLEX (TSC): A SERIES OF 31 PATIENTS
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Lorenzo Genitori, M Grandoni, Milena Guidi, C Moscheo, Annamaria Buccoliero, Flavio Giordano, Iacopo Sardi, Francesco Mari, and Matteo Lenge
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Cancer Research ,Pathology ,medicine.medical_specialty ,Tumor size ,business.industry ,Astrocytoma ,medicine.disease ,Hydrocephalus ,nervous system diseases ,Poster Presentations ,Tuberous sclerosis ,Oncology ,Giant cell ,Subependymal zone ,Medicine ,Neurology (clinical) ,business ,Benign neoplasms ,Intracranial pressure - Abstract
Background Subependymal Giant Cells Astrocytomas (SEGAs) are characteristic of Tuberous Sclerosis Complex (TSC). They are usually benign tumors but may rapidly grow and cause hydrocephalus and raised intracranial pressure. Surgery is mandatory for large and symptomatic SEGAs METHODS 31 patients harboring SEGAs in TSC were admitted for surgery. The main indications for surgery were tumor size and location, tumoral growth and cystization/hemorrhage, and hydrocephalus. In presence of symptomatic hydrocephalus firts surgery aimed to reduce intracranial pressure RESULTS Forty-four surgeries were performed in 31 patients achieving Gross Total and Subtotal Removal in 36 and 8 patients respectively. Recurrences occurred in 11 patients; nine of them were reoperated while two were administered therapy with m-TOR pathway inhibitors. Surgical morbidity and mortality accounted for 22.7% and 2.3% respectively; hydrocephalus was the main complication. After an average follow-up of 5 years, 90% of patients had no evidence of the disease and most (93,3%) had a good clinical status after surgery; 12 out of 30 patients (40%) had a VP-shunt for hydrocephalus Conclusions GTR is feasible and represents the treatment of choice of SEGAs in TSC. Therapy with m-TOR pathway inhibitors is to be considered in selected patients and especially in recurrences of SEGAs
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- 2019
45. P04.08 The role of SCN1A in glioblastomas and mixed neuronal glial tumors of pediatric age
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Carmen Barba, Annamaria Buccoliero, Davide Mei, Milena Guidi, R Guerrini, Sabrina Giglio, Iacopo Sardi, Cetica, Laura Giunti, De Gregorio, Lorenzo Genitori, and M Censullo
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Mixed Glioma ,Cancer Research ,Pathology ,medicine.medical_specialty ,business.industry ,Central nervous system ,Tissue membrane ,Cancer ,Pediatric age ,medicine.disease ,Poster Presentations ,Epilepsy ,medicine.anatomical_structure ,Oncology ,Glioma ,medicine ,Neurology (clinical) ,business ,Glioblastoma - Abstract
BACKGROUND Low and high grade gliomas, are the most common pediatric central nervous system (CNS) tumors and they show an extremely broad range of clinical behavior. Pediatric glioma is distinct from its adult counterpart with different genetic/epigenetic profile and biological features. Recently, several studies have shown the involvement of voltage-gated Na+ channels (VGSC) in different types of cancer, including gliomas. VGSC are multimeric transmembrane complexes, responsible for membrane depolarization in excitable cells playing an important role also in cell proliferation, migration, apoptosis and differentiation. VGSC are therapeutic targets in cardiovascular and neurological disorders and, in cancers, they could be a novel target for the development of promising anticancer therapy MATERIAL AND METHODS Firstly, we explored the genetic background of 9 pediatric glioblastomas (1–9 pGBMs), through whole-exome sequencing (WES) using HiSeq1000 platform (Illumina) with paired-end approach. On the basis of our results, we extended our study in another group of 16 epileptogenic mixed neuronal-glial tumors of pediatric age, (WHO grade I and II), through an amplicon approach (TSCA) using MiniSeq System platform (Illumina) RESULTS We identified variants in SCN1A gene in 3/9 pGBMs: case 3 had c.5782C>G in tumor and blood; case 5 showed c.2278G>T and two mosaic variants (c.5933C>T, 22% and c.4942C>T, 14%); case 6 showed c.667G>T variant only in tumor, and not in other non tumoral tissues (blood, urine and buccal swab). No variants in SCN1A were identified in a group of 16 pediatric mixed gliomas CONCLUSION In this study, we explore the genetic background of two groups of pediatric neuroepithelial brain tumors, through Next generation sequencing approach. We identified only in pGBMs variants in SCN1A gene that encoded for VGSCs and is involved in a spectrum of early-onset epileptic encephalopathies. None of our mutated patients showed history of epilepsy. Now, it is not clear the significance of these variants in pGBMs but interestingly, these variants are present in pGBM and not in mixed gliomas. Further studies on a big cohort of patients are needed to establish if they could play a role in pGBMs aggressiveness, migration and progression. Moreover, VGSCs could be a pharmacological target in pGBMs treatment
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- 2019
46. HGG-17. NEW PHARMACOLOGICAL APPROACHES IN GLIOBLASTOMA THERAPY: BIOLOGICAL EFFECTS AND MOLECULAR ALTERATIONS
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Martina Da Ros, Iacopo Sardi, Laura Giunti, Veronica De Gregorio, Anna Lisa Iorio, and Lorenzo Genitori
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Cancer Research ,business.industry ,Cell growth ,medicine.disease ,Oncology ,Cell culture ,Apoptosis ,In Situ Nick-End Labeling ,Cancer research ,polycyclic compounds ,Medicine ,Doxorubicin ,Neurology (clinical) ,business ,Cytotoxicity ,High Grade Glioma ,Survival rate ,medicine.drug ,Glioblastoma - Abstract
INTRODUCTION: Although decades of research have been trialed, the prognosis for patients with glioblastoma (GBM) has not significantly changed, highlighting the urgency of innovative strategies. Therefore, we investigated on GBM preclinical models the potential of a new pharmacological approach, combining doxorubicin (Dox), a historical anticancer agent with a high toxicity in vitro, and rapamycin (Rapa), a potent inhibitor of cell proliferation. METHODOLOGIES: We analyzed the synergistic effect obtained using Dox combined to Rapa on A172, U87MG and T98G GBM cell lines. MTT and TUNEL analysis were used to assess cytotoxicity and apoptosis. We also evaluated the effectiveness of the treatment in an orthotopic xenograft mice model of GBM with U87MG-luc cells by treatment with Dox, Rapa and their combination. At the end of experiments, brain tissues were collected for histological analysis. RESULTS: In vitro results showed that T98G was resistant to Dox but sensible to Rapa. Prolonging treatments, we observed a significant difference comparing Rapa vs Dox plus Rapa groups (p
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- 2019
47. Combined Treatment with Doxorubicin and Rapamycin Is Effective against In Vitro and In Vivo Models of Human Glioblastoma
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Martina Da Ros, Iacopo Sardi, Maurizio de Martino, Claudio Pisano, Lorenzo Genitori, and Anna Lisa Iorio
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0301 basic medicine ,mTOR inhibitor ,medicine.medical_treatment ,lcsh:Medicine ,Pharmacology ,chemotherapy ,doxorubicin ,Article ,03 medical and health sciences ,0302 clinical medicine ,In vivo ,medicine ,polycyclic compounds ,Cytotoxic T cell ,Doxorubicin ,Chemotherapy ,business.industry ,rapamycin ,lcsh:R ,glioblastoma ,General Medicine ,medicine.disease ,In vitro ,nervous system diseases ,030104 developmental biology ,Cell culture ,030220 oncology & carcinogenesis ,Toxicity ,business ,medicine.drug ,Glioblastoma - Abstract
Despite numerous clinical trials, glioblastoma (GBM) remains a tumor that is difficult to treat. The aim of this study was to investigate the potential of a new pharmacological approach, combining doxorubicin (Dox) and rapamycin (Rapa), in in vitro and in vivo GBM models. Cytotoxic and anti-proliferative effects of Rapa plus Dox treatments were analyzed in GBM cell lines. The in vivo effectiveness of these treatments was investigated in an orthotopic xenograft mice model of GBM. In vitro results demonstrated that prolonged exposure to Rapa sensitize GBM cells to Dox treatments. In vivo results demonstrated that Rapa (5 mg/kg) plus Dox (5 mg/kg) determined the major tumor growth inhibition (&minus, 97.29% vs. control) but results in greater toxicity. The combination Rapa plus Dox (2.5 mg/kg) showed a tumor inhibition like Rapa plus Dox (5 mg/kg) with a toxicity comparable to Rapa alone. Thus, this study demonstrated the efficacy of this pharmacological approach, providing the rationale for a clinical application of this combinational therapy in &ldquo, poor-responder&rdquo, GBM patients.
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- 2019
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48. A microRNA profile of pediatric glioblastoma: The role of NUCKS1 upregulation
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Sabrina Giglio, Iacopo Sardi, Anna Maria Buccoliero, Veronica De Gregorio, Samuela Landini, Benedetta Mazzinghi, Laura Giunti, Martina Da Ros, Lorenzo Genitori, and Alberto Magi
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Cancer Research ,Oncogene ,Microarray analysis techniques ,pediatric brain tumor ,Articles ,Biology ,Cell cycle ,microRNAs ,glioblastoma multiforme ,03 medical and health sciences ,0302 clinical medicine ,Oncology ,Downregulation and upregulation ,030220 oncology & carcinogenesis ,microRNA ,Gene expression ,Cancer research ,030211 gastroenterology & hepatology ,Casein kinase 1 ,gene ,Gene ,high-grade glioma - Abstract
MicroRNAs (miRNAs/miRs) are a novel class of gene regulators that may be involved in tumor chemoresistance. Recently, specific miRNA expression profiles have been identified in adult glioblastoma (aGBM), but there are only limited data available on the role of miRNAs in pediatric GBM (pGBM). In the present study, the expression profile of miRNAs was examined in seven pGBMs and three human GBM cell lines (U87MG, A172 and T98G), compared with a non-tumoral pool of pediatric cerebral cortex samples by microarray analysis. A set of differentially expressed miRNAs was identified, including miR-490, miR-876-3p, miR-876-5p, miR-448 and miR-137 (downregulated), as well as miR-501-3p (upregulated). Through bioinformatics analysis, a series of target genes was predicted. In addition, similar gene expression patterns in pGBMs and cell lines was confirmed. Of note, drug resistant T98G cells had upregulated nuclear casein kinase and cyclin-dependent kinase substrate 1 (NUCKS1) expression, a protein overexpressed in many tumors that serves an important role in cell proliferation and progression. On the basis of the present preliminary report, it could be intriguing to further investigate the relationship between each of the identified differentially expressed miRNAs and NUCKS1, in order to clarify their involvement in the multi-drug resistance mechanism of pGBMs.
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- 2019
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49. Central Nervous System Congenital Tumors
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Massimiliano Sanzo, Annamaria Buccoliero, Iacopo Sardi, Leonardo Bussolin, Chiara Caporalini, Lorenzo Genitori, Milena Guidi, Flavio Giordano, Regina Mura, and Barbara Spacca
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medicine.medical_specialty ,Pediatrics ,Medical treatment ,business.industry ,Incidence (epidemiology) ,Central nervous system ,Disease ,medicine.anatomical_structure ,Epidemiology ,medicine ,In patient ,Neurosurgery ,Presentation (obstetrics) ,business - Abstract
Central nervous system (CNS) tumors are the most common solid tumors in childhood. Those tumors are a heterogeneous entity because of their different histologies, behavior, incidence, and therapies that can even be different in different ages of life and, within the childhood, can be different at different stages. A peculiar group are tumors developed before 3 year of age, because of the complex interaction of the disease with the developing brain and because of severe limitation on the treatment with implications both on the side of the surgery and on the medical treatment. Such kind of observation is even more evident if we consider patients younger than 12 months of age. Within this group are included the so-called congenital tumors, considered as the tumors diagnosed in patients younger than 2 months of age, but this definition is commonly extended up to 2 years of age. We will expose a review of the literature and the experience of our Center of Neurosurgery and Neuro-oncology about CNS tumors diagnosed in children younger than 12 months of age, with particular interest in epidemiology and risk factors, clinical presentation, histology, surgical and medical treatment, and outcome. Particular attention is given to neurosurgical difficulties in this age group.
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- 2019
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50. Optical coherence tomography significance in managing complex neurofibromatosis 2-related papilledema: Report of a case
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Flavio Giordano, Gareth Evans, Regina Mura, Giacomo Bacci, Roberto Caputo, Iacopo Sardi, Franco Trabalzini, Sergio Nappini, Omar N. Pathmanaban, and Carla Fonte
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Shunt placement ,medicine.medical_specialty ,optical coherence tomography ,neurofibromatosis ,medicine.diagnostic_test ,business.industry ,vision loss ,Case Report ,medicine.disease ,03 medical and health sciences ,0302 clinical medicine ,Optical coherence tomography ,Multidisciplinary approach ,multidisciplinary approach ,030221 ophthalmology & optometry ,medicine ,General Earth and Planetary Sciences ,Radiology ,medicine.symptom ,Neurofibromatosis ,Papilledema ,business ,shunt placement ,030217 neurology & neurosurgery ,General Environmental Science - Abstract
This case describes the strong utility of optical coherence tomography in multidisciplinary management of a complex case of type 2 neurofibromatosis.
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- 2021
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