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2. Intrapartum Ultrasonography for Detecting Fetal Macrosomia

Author

Arena B, Zanchi Sm, Croce P, Perotti D, Croce G, and Panzeri L

Subjects
medicine.medical_specialty, Anesthesiology and Pain Medicine, Obstetrics, business.industry, medicine, Fetal macrosomia, Ultrasonography, business, medicine.disease
Abstract

Objective: To compare the accuracy of three ultrasound methods to estimate fetal weight within 48 hours before delivery, in order to recognize macrosomia, defined as birth weight greater than 4000 g.Methods: A prospective and ultrasonic study was performed on a sample of singleton pregnancies between 37 weeks and 41 weeks plus 6 days of gestation. Fetal weight was evaluated with Estimated Fetal Weight (EFW) formula, with the measurement of the Abdominal Circumference (AC) and with the assessment of the Abdominal Circumference corrected with the constant “c” (ACc).Results: 1030 patients with single pregnancy were included, 67.28% of them were primiparous, average Body Mass Index (BMI) at birth was 27.37 and macrosomia was found in 77 (8,08%) fetuses. EFW showed a sensitivity of 61.53%, a specificity of 90.72%, a positive predictive value (PPV) of 27.58% and negative predictive value (NPV) of 97.46%, to recognize birth weight of more than 4000 g. AC greater than 375 mm presented a sensitivity of 53.24%, a specificity of 93.21%, a PPV of 41.41% and a NPV of 95.67%, to detect macrosomic fetuses. ACc greater than 375 mm showed a sensitivity of 66.23%, a specificity of 88.65%, a PPV of 34.35% and a NPV of 96.68%, to predict macrosomia. The mean absolute error when the neonatal weight was greater than 4000 g, with EFW was 9,23%, with AC were 11,02% and with ACc was 9,32%.Conclusions: In this study was shown that either EFW, or AC-only, or ACc are useful tools to detect fetal macrosomia. The measurement of AC and Acc seem to be the easiest methods to learn and to be used every time. During the first stage of labor, ultrasound scan associated to clinic evaluation, provides further elements to physician, to allow a better management of delivery. The finding of a NPV greater than 95% with the three methods, leads to exclude macrosomia with a good approximation, even in case of clinic hypothesis.

Published
2019
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6. Loss of Heterozygosity Analysis at Different Chromosome Regions in Wilms Tumor Confirms 1p Allelic Loss as a Marker of Worse Prognosis: A Study from the Italian Association of Pediatric Hematology and Oncology

Author

Spreafico F, Gamba B, Mariani L, Collini P, D'Angelo P, Di Cataldo A, Indolfi P, Nantron M, Terenziani M, Morosi C, Radice P, Perotti D, AIEOP Wilms Tumor Working Group, PESSION, ANDREA, Spreafico F, Gamba B, Mariani L, Collini P, D'Angelo P, Pession A, Di Cataldo A, Indolfi P, Nantron M, Terenziani M, Morosi C, Radice P, Perotti D, and AIEOP Wilms Tumor Working Group

Subjects
Genetic Markers, Male, Oncology, medicine.medical_specialty, Vincristine, Multivariate analysis, Adolescent, pediatrics, kidney neoplasms, loss of heterozygosity, pediatrics, Wilms tumor, Urology, STAGE-I, CHILDRENS-CANCER, RENAL TUMORS, SHORT ARM, 16Q, ANAPLASIA, RELAPSE, GENE, 11Q, AGE, Loss of heterozygosity, Chromosome regions, Internal medicine, medicine, Overall survival, Humans, kidney neoplasms, Prospective Studies, Child, loss of heterozygosity, Wilms tumor, business.industry, Infant, Wilms' tumor, Prognosis, medicine.disease, Child, Preschool, Microsatellite, Female, business, Allelic loss, medicine.drug
Abstract

PURPOSE: The specific aims of the AIEOP-TW-2003 protocol included prospectively investigating a possible association of tumor loss of heterozygosity with outcomes in children treated for Wilms tumor. MATERIALS AND METHODS: We analyzed 125 unilateral favorable histology Wilms tumors registered between 2003 and 2008 in the Italian cooperative protocol for microsatellite markers mapped to chromosomes 1p, 7p, 11q, 16q and 22q. RESULTS: The 3-year disease-free survival and overall survival probabilities were 0.87 (95% CI 0.81-0.93) and 0.98 (95% CI 0.96-1.0), respectively. Loss of heterozygosity at 1p was significantly associated with a worse disease-free survival (probability 0.67 for patients with and 0.92 for those without 1p loss of heterozygosity, p = 0.0009), as confirmed also by multivariate analysis adjusting for tumor stage and patient age at diagnosis. There was no difference in disease-free survival probability among children with loss of heterozygosity in the other chromosomal regions tested. The worse outlook for children older than 2 years at diagnosis did not seem to be influenced by the loss of heterozygosity patterns considered. CONCLUSIONS: Chromosome 1p loss of heterozygosity seems to be a risk factor for nonanaplastic Wilms tumor, possibly regardless of other clinical factors. Our findings were uninformative regarding loss of heterozygosity in the other chromosomal regions tested.

Published
2013
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7. Possible role of pandemic AH1N1 swine flu virus in a childhood leukemia cluster

Author

Cazzaniga, G, Bisanti, L, Randi, G, Deandrea, S, Bungaro, S, Pregliasco, F, Perotti, D, Spreafico, F, Masera, G, Valsecchi, M, Biondi, A, Greaves, M, Valsecchi, MG, Cazzaniga, G, Bisanti, L, Randi, G, Deandrea, S, Bungaro, S, Pregliasco, F, Perotti, D, Spreafico, F, Masera, G, Valsecchi, M, Biondi, A, Greaves, M, and Valsecchi, MG

Published
2017

10. A novel WT1 mutation in familial wilms tumor

Author

MELCHIONDA, FRAIA, LIMA, MARIO, PESSION, ANDREA, Spreafico F, Ciceri S, Collini P, Massimino M, Radice P, Perotti D., Melchionda F, Spreafico F, Ciceri S, Lima M, Collini P, Pession A, Massimino M, Radice P, and Perotti D

Subjects
wilms tumor, case report, child, cryptorchism, gene mutation, hematuria, histopathology, human, hypospadias, immunohistochemistry, immunoreactivity, kidney tumor, letter, male, nephrectomy, nephroblastoma, preschool child, priority journal, WT1 protein
Abstract

To the Editor: Wilms tumor (WT), the most frequent pediatric renal tumor, primarily occurs as a sporadic disease, but approximately 2% of cases have an affected relative [1]. While the underlying cause of most familial WTs is currently unknown, few reports described pedigrees associated with anomalies of the WT1 gene [2–5]. We report on a WT pedigree resulting from a novel WT1 mutation. The index patient, a 23-month-old (46, XY karyotype) presented with bilateral cryptorchidism and proximal severe penile hypospadia. Serial abdomino-pelvic ultrasounds did not reveal signs of renal pathology, and normal renal function was assessed by blood and urine tests. Apart from the presence of genitourinary (GU) anomalies, the child did not present any clinical evidence of known syndromes predisposing to WT development. At 23 months of age, following the onset of macroscopic hematuria, abdominal ultrasound revealed a left renal mass. The patient underwent radical nephrectomy, and histological examination revealed a unicentric, triphasic WT without anaplasia. Perilobar nephrogenic rests were present, as well as dysplastic medullary rays. The patient received treatment according to the Associazione Italiana Ematologia Oncologia Pediatrica (AIEOP) TW-2003 protocol for stage IV disease, because of the presence of pulmonary metastases. At present, the child is in complete remission, 3 months after completing therapy. His mother had been successfully treated for stage II WT in 1978, when she was 22 months old. She showed a normal growth and development, without any GU abnormalities or syndromic signs. While she was considering the possibility of an assisted conception treatment due to her difficulty in conceiving, she got spontaneously pregnant at 32 years of age. No nephropathies or renal cancers were reported in other members of her family and no GU abnormalities were referred in her parents and her two brothers. Two novelWT1 germline variants, the silent variation c.981C>T and the frameshift mutation c.983delC (p.P328QfsX53) causing the loss of the C-terminal of the WT1 protein, were detected in the peripheral blood leukocytes (PBL) DNAs of both affected subjects (Fig. 1Aand B). TumorDNAwas available only fromthe child. WT1 sequencing revealed no further anomaly and loss of entire wild-type WT1 allele could be excluded based on the maintenance of heterozygosity for both the novel identified variants (Fig. 1C). Immunohistochemistry forWT1 on tumor cells disclosed a focal and weak immunoreactivity with WT clone WT49 (against amino acids 1–181 of theN-terminal ofWT1), but not withWT1 (C-19) antibody (against the last 19 amino acids of the C-terminal ofWT1) (Fig. 1E and F). This is consistent with the expression in the tumor of the mutated, but not of the constitutionally wild-type allele, and indicates a likely etiologic role of the mutated allele in tumorigenesis. The analysis of the CTNNB1 gene disclosed the c.133_135delTCT (p.S45del) in-frame deletion in tumor DNA (Fig. 1G), in agreement with the described co-occurrence of WT1 and b-cateninmutations in WTs [6].ThisWTpedigreeadds tothe fewalreadyreportedinwhicha role of WT1 mutation has been established.

Published
2013

13. Protocollo AIEOP Tumore di Wilms ( TW) 2003 : osservazioni preliminari

Author

Spreafico F., Collini P., Piva L., Gandola L., Nantron M., Bianchi M., D'Angelo P., Indolfi P., Di Cataldo A., Terenziani M., Tamaro P., Provenzi M., Gambini C., Pucci A., Rizzo A., Santoro N., Martone A., Favre C., Federici S., Tettoni K., Miglionico L., Melchionda F., Barone A., Perotti D., Radice P., Fossati Bellani F., PESSION, ANDREA, Spreafico F., Collini P., Piva L., Gandola L., Nantron M., Pession A., Bianchi M., D'Angelo P., Indolfi P., Di Cataldo A., Terenziani M., Tamaro P., Provenzi M., Gambini C., Pucci A., Rizzo A., Santoro N., Martone A., Favre C., Federici S., Tettoni K., Miglionico L., Melchionda F., Barone A., Perotti D., Radice P., and Fossati - Bellani F.

Published
2007

14. Constitutional de novo deletion of the FBXW7 gene in a patient with focal segmental glomerulosclerosis and multiple primitive tumors

Author

Roversi, G, Picinelli, C, Bestetti, I, Crippa, M, Perotti, D, Ciceri, S, Saccheri, F, Collini, P, Poliani, P, Catania, S, Peissel, B, Pagni, F, Russo, S, Peterlongo, P, Manoukian, S, Finelli, P, ROVERSI, GAIA, PAGNI, FABIO, Finelli, P., Roversi, G, Picinelli, C, Bestetti, I, Crippa, M, Perotti, D, Ciceri, S, Saccheri, F, Collini, P, Poliani, P, Catania, S, Peissel, B, Pagni, F, Russo, S, Peterlongo, P, Manoukian, S, Finelli, P, ROVERSI, GAIA, PAGNI, FABIO, and Finelli, P.

Abstract

Multiple primary malignant neoplasms are rare entities in the clinical setting, but represent an important issue in the clinical management of patients since they could be expression of a genetic predisposition to malignancy. A high resolution genome wide array CGH led us to identify the first case of a de novo constitutional deletion confined to the FBXW7 gene, a well known tumor suppressor, in a patient with a syndromic phenotype characterized by focal segmental glomerulosclerosis and multiple primary early/atypical onset tumors, including Hodgkin's lymphoma, Wilms tumor and breast cancer. Other genetic defects may be associated with patient's phenotype. In this light, constitutional mutations at BRCA1, BRCA2, TP53, PALB2 and WT1 genes were excluded by performing sequencing and MLPA analysis; similarly, we ruled out constitutional abnormalities at the imprinted 11p15 region by methylation specific -MLPA assay. Our observations sustain the role of FBXW7 as cancer predisposition gene and expand the spectrum of its possible associated diseases.

Published
2015

17. Why Wilms tumour diagnosed in children

Author

Dangelo, P, DI CATALDO, Andrea, Bianchi, M, Bisogno, G, Catania, S, Collini, P, Indolfi, P, Marchianò, A, Melchionda, F, Mosa, C, Nantron, M, Perotti, D, Pession, A, Piva, L, Provenzi, M, Terenziani, M, and Spreafico, F.

Published
2010

20. Protocollo AIEOP tumore di Wilms 2003: osservazioni preliminari

Author

Spreafico, F, Collini, P, Piva, L, Gandola, L, Nantron, M, Pession, A, Bianchi, M, Dangelo, P, Indolfi, P, DI CATALDO, Andrea, Terenziani, M, Tamaro, P, Provenzi, M, Gambini, C, Pucci, A, Rizzo, A, Santoro, N, Martone, A, Favre, C, Federici, S, Tettoni, K, Miglionico, L, Melchionda, F, Barone, A, Perotti, D, Radice, P, and FOSSATI BELLANI, F.

Published
2007

21. Cytogenetic and molecular characterization of T-cell acute lymphoblastic leukemia as a second tumor after anaplastic large-cell lymphoma in a boy

Author

Perotti, D., Sozzi, G., Ferrari, A., Casanova, M., Gambirasio, F., Mondini, P., Mezzelani, A., Giardini, R., Pettenella, F., Papini, D., Andrea Biondi, Fossati-Bellani, F., and Massimino, M.

Subjects
secondary T-cell lymphoblastic leukemia, hemic and lymphatic diseases, childhood cancer, DNA analysis, cytogenetics
Abstract

We report a case of acute T-cell lymphoblastic leukemia which developed in a hoy 8.5 years after successful treatment for anaplastic large-cell lymphoma. Cytogenetic and molecular characterizations of the second tumor were performed. The cytogenetic investigation revealed a complex pattern of karyotypic alterations, including double minutes, ring chromosomes, and a duplication of the p21-32 region of chromosome 1. The microsatellite DNA analysis excluded rearrangement or deletion of the TALI gene in the tumor cells; rearrangements of the MLL gene were excluded by Southern blot analysis. To the best of our knowledge, this is the first report of T-cell lymphoblastic leukemia arising after treatment of CD 30(+) anaplastic large-cell lymphoma. The different T-cell receptor rearrangement evidenced in the two tumors indicates that this second malignancy most likely emerged de novo, but was plausibly related to the previous radiation and chemotherapy. (C) 1999, Ferrata Storti Foundation.

Published
1999

22. Different mechanisms cause imprinting defects at the IGF2/H19 locus in Beckwith-Wiedemann syndrome and Wilms' tumour.

Author

Sparago, A, Verde, G, De Crescenzo, A, Citro, V, Cubellis, Mv, Rinaldi, Mm, Boccuto, Luigi, Neri, Giovanni, Magnani, C, D'Angelo, P, Collini, P, Perotti, D, Sebastio, G, Maher, R, Riccio, A., Sparago, A, Verde, G, De Crescenzo, A, Citro, V, Cubellis, Mv, Rinaldi, Mm, Boccuto, Luigi, Neri, Giovanni, Magnani, C, D'Angelo, P, Collini, P, Perotti, D, Sebastio, G, Maher, R, and Riccio, A.

Published
2008

24. Different mechanisms cause imprinting defects at the IGF2/H19 locus in Beckwith-Wiedemann syndrome and Wilms' tumour

Author

Cerrato, F., primary, Sparago, A., additional, Verde, G., additional, De Crescenzo, A., additional, Citro, V., additional, Cubellis, M. V., additional, Rinaldi, M. M., additional, Boccuto, L., additional, Neri, G., additional, Magnani, C., additional, D'Angelo, P., additional, Collini, P., additional, Perotti, D., additional, Sebastio, G., additional, Maher, E. R., additional, and Riccio, A., additional

Published
2008
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29. WTX R353X mutation in a family with osteopathia striata and cranial sclerosis (OS-CS): case report and literature review of the disease clinical, genetic and radiological features

Author

Zicari Anna, Tarani Luigi, Perotti Daniela, Papetti Laura, Nicita Francesco, Liberati Natascia, Spalice Alberto, Salvatori Guglielmo, Guaraldi Federica, and Duse Marzia

Subjects
Osteopathia striata, Cranial sclerosis, Horan-Beighton syndrome, WTX, Bone dysplasia, Pediatrics, RJ1-570
Abstract

Abstract Osteopathia striata with cranial sclerosis (OS-CS) or Horan-Beighton syndrome is a rare X-linked dominant inherited bone dysplasia, characterized by longitudinal striations of long bones and cranial sclerosis. Patients can be asymptomatic or present with typical facial dysmorphism, sensory defects, internal organs anomalies, growth and mental retardation, depending on the severity of the disease. WTX gene (Xq11) has been recently identified as the disease causing gene. Aim of this article is to present the case of a 6 year old girl initially evaluated for bilateral hearing loss. Patient’s head CT scan pointed out sclerosis of skull base and mastoid cells, and abnormal middle-ear ossification. Clinical examination of the patient and her mother were suspicious for OS-CS. The diagnosis was confirmed by X-rays examination showing typical longitudinal striation. Genetic analysis allowed the identification of maternally transmitted heterozygous nonsense c.1057C>T (p.R353X) WTX gene mutation. We also provide a systematic review of currently available knowledge about clinical, radiologic and genetic features typical of the OS-CS.

Published
2012
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30. Possible role of pandemic AH1N1 swine flu virus in a childhood leukemia cluster

Author

Cazzaniga, Giovanni, Bisanti, Luigi, Randi, Giorgia, Deandrea, Silvia, Bungaro, Silvia, Pregliasco, Fabrizio, Perotti, Daniela, Spreafico, Filippo, Masera, Giuseppe, Valsecchi, Maria Grazia, Biondi, Andrea, Greaves, Mel, Cazzaniga, G, Bisanti, L, Randi, G, Deandrea, S, Bungaro, S, Pregliasco, F, Perotti, D, Spreafico, F, Masera, G, Valsecchi, M, Biondi, A, and Greaves, M

Subjects
Cancer Research, Space-Time Cluster, Childhood Leukemia, AH1N1, Hematology, delayed infection hypothesis, Precursor Cell Lymphoblastic Leukemia-Lymphoma, Article, Influenza A Virus, H1N1 Subtype, Anesthesiology and Pain Medicine, Italy, Child, Preschool, Influenza, Human, Humans, Child, Pandemics
Published
2017

31. Constitutional de novo deletion of the FBXW7 gene in a patient with focal segmental glomerulosclerosis and multiple primitive tumors

Author

Silvia Russo, Paolo Peterlongo, Fabio Pagni, Paola Collini, Chiara Picinelli, Siranoush Manoukian, Gaia Roversi, Sara Ciceri, Bernard Peissel, Milena Crippa, Ilaria Bestetti, Daniela Perotti, Fabiana Saccheri, Pietro Luigi Poliani, Serena Catania, Palma Finelli, Roversi, G, Picinelli, C, Bestetti, I, Crippa, M, Perotti, D, Ciceri, S, Saccheri, F, Collini, P, Poliani, P, Catania, S, Peissel, B, Pagni, F, Russo, S, Peterlongo, P, Manoukian, S, and Finelli, P

Subjects
Adult, Male, F-Box-WD Repeat-Containing Protein 7, PALB2, Ubiquitin-Protein Ligases, DNA Mutational Analysis, Karyotype, Cell Cycle Proteins, Biology, Multidisciplinary, cancer, genetic, multiple primitive tumours, Malignancy, Article, Neoplasms, Multiple Primary, Focal segmental glomerulosclerosis, FBXW7, medicine, Genetic predisposition, cancer, multiple primitive tumours, Humans, Genetic Predisposition to Disease, Multiplex ligation-dependent probe amplification, Genetic Association Studies, In Situ Hybridization, Fluorescence, Comparative Genomic Hybridization, Multidisciplinary, Basic Helix-Loop-Helix Leucine Zipper Transcription Factors, Glomerulosclerosis, Focal Segmental, F-Box Proteins, Wilms' tumor, Middle Aged, medicine.disease, Lymphoma, Cancer research, Female, genetic, Gene Deletion, Comparative genomic hybridization
Abstract

Multiple primary malignant neoplasms are rare entities in the clinical setting, but represent an important issue in the clinical management of patients since they could be expression of a genetic predisposition to malignancy. A high resolution genome wide array CGH led us to identify the first case of a de novo constitutional deletion confined to the FBXW7 gene, a well known tumor suppressor, in a patient with a syndromic phenotype characterized by focal segmental glomerulosclerosis and multiple primary early/atypical onset tumors, including Hodgkin’s lymphoma, Wilms tumor and breast cancer. Other genetic defects may be associated with patient’s phenotype. In this light, constitutional mutations at BRCA1, BRCA2, TP53, PALB2 and WT1 genes were excluded by performing sequencing and MLPA analysis; similarly, we ruled out constitutional abnormalities at the imprinted 11p15 region by methylation specific -MLPA assay. Our observations sustain the role of FBXW7 as cancer predisposition gene and expand the spectrum of its possible associated diseases.

Published
2015

32. Genomic profiling by whole-genome single nucleotide polymorphism arrays in Wilms tumor and association with relapse

Author

Paolo Radice, Serena Catania, Marilina Nantron, Paolo Verderio, Andrea Pession, Pio D'Adamo, Fabio Macciardi, Filippo Spreafico, Paolo Indolfi, Franca Fossati-Bellani, Maurizio Bianchi, Paola Collini, Federica Torri, Beatrice Gamba, Daniela Perotti, Monica Terenziani, Sara Pizzamiglio, Paolo D'Angelo, Perotti D, Spreafico F, Torri F, Gamba B, D'Adamo P, Pizzamiglio S, Terenziani M, Catania S, Collini P, Nantron M, Pession A, Bianchi M, Indolfi P, D'Angelo P, Fossati-Bellani F, Verderio P, Macciardi F, Radice P, Daniela, Perotti, Filippo, Spreafico, Federica, Torri, Beatrice, Gamba, D'Adamo, ADAMO PIO, Sara, Pizzamiglio, Monica, Terenziani, Serena, Catania, Paola, Collini, Marilina, Nantron, Andrea, Pession, Maurizio, Bianchi, Paolo, Indolfi, Paolo, D'Angelo, Franca Fossati, Bellani, Paolo, Verderio, Fabio, Macciardi, and Paolo, Radice

Subjects
Oncology, Genetic Markers, Male, Cancer Research, medicine.medical_specialty, Adolescent, DNA Copy Number Variations, Single-nucleotide polymorphism, Kaplan-Meier Estimate, Biology, Allelic Imbalance, Bioinformatics, Polymorphism, Single Nucleotide, Wilms Tumor, 03 medical and health sciences, 0302 clinical medicine, genetic [DNA Copy Number Variations], Recurrence, Internal medicine, Genetics, medicine, SNP, Humans, Genetic Predisposition to Disease, DNA Copy Number Variations: genetics, Prospective Studies, Allele, Child, Survival rate, Genotyping, 030304 developmental biology, Chromosome Aberrations, 0303 health sciences, Genome, Human, Chromosome, Infant, Wilms' tumor, medicine.disease, ADVERSE PROGNOSTIC-FACTOR, CANCER-STUDY-GROUP, CHILDRENS-CANCER, INTERNATIONAL-SOCIETY, EXPRESSION PATTERNS, RENAL TUMORS, ALLELE LOSS, STAGE-I, HETEROZYGOSITY, 16Q, 3. Good health, Genetic marker, 030220 oncology & carcinogenesis, Child, Preschool, Female, Genome-Wide Association Study
Abstract

Despite the excellent survival rate of Wilms tumor (WT) patients, only approximately one-half of children who suffer tumor recurrence reach second durable remission. This underlines the need for novel markers to optimize initial treatment. We investigated 77 tumors using Illumina 370CNV-QUAD genotyping BeadChip arrays and compared their genomic profiles to detect copy number (CN) abnormalities and allelic ratio anomalies associated with the following clinicopathological variables: relapse (yes vs. no), age at diagnosis (≤24 months vs. >24 months), and disease stage (low stage, I and II, vs. high stage, III and IV). We found that CN gains at chromosome region 1q21.1-q31.3 were significantly associated with relapse. Additional genetic events, including allelic imbalances at chromosome arms 1p, 1q, 3p, 3q, and 14q were also found to occur at higher frequency in relapsing tumors. Interestingly, allelic imbalances at 1p and 14q also showed a borderline association with higher tumor stages. No genetic events were found to be associated with age at diagnosis. This is the first genome wide analysis with single nucleotide polymorphism (SNP) arrays specifically investigating the role of genetic anomalies in predicting WT relapse on cases prospectively enrolled in the same clinical trial. Our study, besides confirming the role of 1q gains, identified a number of additional candidate genetic markers, warranting further molecular investigations. © 2012 Wiley Periodicals, Inc.

Published
2012

33. Functional inactivation of the WTX gene is not a frequent event in Wilms' tumors

Author

Andrea Pession, Monica Terenziani, Franca Fossati-Bellani, Paolo Radice, Michele Sardella, Filippo Spreafico, Beatrice Gamba, Daniela Perotti, Paola Collini, Marilina Nantron, Perotti D, Gamba B, Sardella M, Spreafico F, Terenziani M, Collini P, Pession A, Nantron M, Fossati-Bellani F, and Radice P.

Subjects
Male, Cancer Research, DNA Mutational Analysis, Loss of Heterozygosity, Biology, medicine.disease_cause, Wilms Tumor, Loss of heterozygosity, Germline mutation, Genetics, medicine, Humans, Allele, Molecular Biology, X chromosome, Alleles, Adaptor Proteins, Signal Transducing, Mutation, Chromosomes, Human, X, Tumor Suppressor Proteins, Chromosome, Wilms' tumor, medicine.disease, Female, Carcinogenesis, Gene Deletion, Microsatellite Repeats
Abstract

For many years the precise genetic etiology of the majority of Wilms' tumors has remained unexplained. Recently, the WTX gene, mapped to chromosome Xq11.1, has been reported to be lost or mutated in approximately one-third of Wilms' tumors. Moreover, in female cases, the somatically inactivated alleles were found to invariantly derive from the active chromosome X. Consequently, WTX has been proposed as a 'one-hit' tumor suppressor gene. To provide further insights on the contribution of WTX to the development of the disease, we have examined 102 Wilms' tumors, obtained from 43 male and 57 female patients. Quantitative PCR analyses detected WTX deletions in 5 of 45 (11%) tumors from males, whereas loss of heterozygosity at WTX-linked microsatellites was observed in 9 tumors from 50 informative females (19%). However, in the latter group, using a combination of HUMARA assay and bisulfite-modified DNA sequencing, we found that the deletion affected the active chromosome X only in two cases (4%). Sequence analyses detected an inactivating somatic mutation of WTX in a single tumor, in which a strongly reduced expression of the mutant allele respect to the wild-type allele was observed, a finding not consistent with its localization on the active chromosome X. Overall, a functional somatic nullizygosity of the WTX gene was ascertained only in seven of the Wilms' tumors included in the study (approximately 7%). Our findings indicate that previously reported estimates on the proportion of Wilms' tumors due to WTX alterations should be reconsidered.

Published
2008

34. Different mechanisms cause imprinting defects at the IGF2/H19 locus in Beckwith-Wiedemann syndrome and Wilms' tumour

Author

Gianfranco Sebastio, Paola Collini, Gaetano Verde, Maria Vittoria Cubellis, Maria Michela Rinaldi, Valentina Citro, Andrea Riccio, Cinzia Magnani, Agostina De Crescenzo, Angela Sparago, Luigi Boccuto, Daniela Perotti, Flavia Cerrato, Paolo D'Angelo, Eamonn R. Maher, Giovanni Neri, Cerrato, Flavia, Sparago, A., Verde, G., DE CRESCENZO, A., Citro, V., Cubellis, M., Rinaldi, M., Boccuto, L., Neri, G., Magnani, C., D'Angelo, P., Collini, P., Perrotti, D., Sebastio, G., Maher, E., Riccio, Andrea, Cerrato, F, Sparago, A, Verde, G, DE CRESCENZO, A, Citro, V, Cubellis, MARIA VITTORIA, Rinaldi, Mm, Boccuto, L, Neri, G, Magnani, C, Dangelo, P, Collini, P, Perotti, D, Sebastio, G, and Maher, E. AND RICCIO A.

Subjects
Male, CCCTC-Binding Factor, Beckwith-Wiedemann Syndrome, RNA, Untranslated, Beckwith–Wiedemann syndrome, Locus (genetics), Biology, Settore MED/03 - GENETICA MEDICA, Wilms Tumor, Insulin-Like Growth Factor II, Chromosome Segregation, Genetics, medicine, Humans, Epigenetics, Allele, Imprinting (psychology), Molecular Biology, Alleles, Genetics (clinical), Chromosomes, Human, Pair 11, human cancer, BWS syndrome, Wilms' tumor, General Medicine, DNA Methylation, medicine.disease, Pedigree, genomic imprinting, DNA-Binding Proteins, Repressor Proteins, Haplotypes, Italy, Mutation, DNA methylation, Female, RNA, Long Noncoding, imprinting, Genomic imprinting, Gene Deletion, epigenetic
Abstract

The parent of origin-dependent expression of the IGF2 and H19 genes is controlled by the imprinting centre 1 (IC1) consisting in a methylation-sensitive chromatin insulator. Deletions removing part of IC1 have been found in patients affected by the overgrowth- and tumour-associated Beckwith - Wiedemann syndrome (BWS). These mutations result in the hypermethylation of the remaining IC1 region, loss of IGF2/H19 imprinting and fully penetrant BWS phenotype when maternally transmitted. We now report that 12 additional cases with IC1 hypermethylation have a similar clinical phenotype but showed neither a detectable deletion nor other mutation in the local vicinity. Likewise, no IC1 deletion was detected in 40 sporadic non-syndromic Wilms' tumours. A detailed analysis of the BWS patients showed that the hypermethylation variably affected the IC1 region and was generally mosaic. We observed that all these cases were sporadic and in at least two families affected and unaffected members shared the same maternal IC1 allele but not the abnormal maternal chromosome epigenotype. Furthermore, the chromosome with the imprinting defect derived from either the maternal grandfather or maternal grandmother. Overall, these results indicate that methylation-imprinting defects at the IGF2-H19 locus can result from inherited mutations of the IC and have high recurrence risk or arise independently from the sequence context and generally not transmitted to the progeny. Despite these differences, the epigenetic abnormalities are usually present in the patients in the mosaic form and probably acquired by post-zygotic de novo methylation. Distinguishing between these two groups of cases is important for genetic counselling. © The Author 2008. Published by Oxford University Press. All rights reserved.

Published
2008
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35. Treatment of high-risk relapsed Wilms tumor with dose-intensive chemotherapy, marrow-ablative chemotherapy, and autologous hematopoietic stem cell support: Experience by the Italian Association of Pediatric Hematology and Oncology

Author

Luigi Piva, Filippo Spreafico, Alessandro Jenkner, Gabriella Casazza, Roberto Luksch, Andrea Pession, Lorenza Gandola, Paola Collini, Daniela Perotti, Sandro Dallorso, Franca Fagioli, Gianni Bisogno, Paolo D'Angelo, Spreafico F, Bisogno G, Collini P, Jenkner A, Gandola L, D'Angelo P, Casazza G, Piva L, Luksch R, Perotti D, Pession A, Fagioli F, and Dallorso S.

Subjects
Oncology, Male, Transplantation Conditioning, medicine.medical_treatment, Hematopoietic stem cell transplantation, Nephrectomy, Pediatrics, chemistry.chemical_compound, High-dose chemotherapy, Relapse, Child, Ifosfamide, Graft Survival, Remission Induction, Hematopoietic Stem Cell Transplantation, Hematology, Perinatology and Child Health, Survival Rate, Treatment Outcome, Italy, Child, Preschool, Absolute neutrophil count, Female, Autologous, medicine.drug, medicine.medical_specialty, Antineoplastic Agents, Transplantation, Autologous, Wilms Tumor, Internal medicine, medicine, Humans, Preschool, Survival rate, Salvage Therapy, Chemotherapy, Transplantation, business.industry, Infant, Wilms' tumor, medicine.disease, Carboplatin, Surgery, Radiation therapy, chemistry, Pediatrics, Perinatology and Child Health, Autologous hematopoietic stem cell transplantation, Wilms tumor, business
Abstract

Background We evaluated an intensified chemotherapy strategy in children with Wilms tumor who relapsed with high-risk features. Procedures From January 2001 to June 2006, we treated 20 consecutive children with reinduction chemotherapy (using ifosfamide/carboplatin/etoposide in 15/20 cases), with (n = 15) or without (n = 5) subsequent high-dose chemotherapy and hematopoietic stem cell support, surgery where feasible, and radiation therapy. The median time to relapse was 10 months after nephrectomy. All but two children initially received doxorubicin as first-line therapy. Results All patients were assessed for outcome: 13 are currently alive, 12 of them in remission a median 25 months since their relapse, one with progressing tumor. The treatment was unsuccessful in eight children: the disease progressed during reinduction in three, and relapsed in five. There was one toxic death. All transplanted patients engrafted to a neutrophil count >0.5 × 103/µl after a median 11 days, and to an unsustained platelet count >25,000/µl after a median of 13 days. Three-year disease-free and overall survival rates were 56 ± 12% and 55 ± 13%, respectively. Neither recurrence within 12 months of nephrectomy nor extra-lung recurrence negatively affected outcome. A survival advantage was demonstrated in patients without disease evidence prior to transplant. Conclusion A disease-free survival rate nearing 50% is a realistic target in children with high-risk recurrent Wilms tumor. The benefit of autologous hematopoietic stem cell transplantation for consolidation deserves to be investigated in a randomized, controlled study. Pediatr Blood Cancer 2008;51:23–28. © 2008 Wiley-Liss, Inc.

Published
2008

36. Bevacizumab-containing treatment for relapsed or refractory Wilms tumor.

Author

Al-Jilaihawi S, Spreafico F, Mavinkurve-Groothuis A, Drost J, Perotti D, Koenig C, and Brok J

Subjects
Humans, Child, Prognosis, Neovascularization, Pathologic drug therapy, Neovascularization, Pathologic pathology, Bevacizumab administration & dosage, Bevacizumab adverse effects, Bevacizumab pharmacology, Wilms Tumor drug therapy, Wilms Tumor pathology, Kidney Neoplasms drug therapy, Kidney Neoplasms pathology, Angiogenesis Inhibitors administration & dosage, Angiogenesis Inhibitors adverse effects, Angiogenesis Inhibitors pharmacology, Antineoplastic Combined Chemotherapy Protocols administration & dosage, Antineoplastic Combined Chemotherapy Protocols adverse effects, Antineoplastic Combined Chemotherapy Protocols pharmacology, Neoplasm Recurrence, Local drug therapy
Abstract

Introduction: Angiogenesis is critical for tumor growth and metastasis. Bevacizumab is an antiangiogenic drug used to treat various adult and childhood solid tumors. Its potential efficacy in Wilms tumor (WT) with poor prognosis is not established., Areas Covered: The response to bevacizumab-containing regimens in relapsed or refractory WT was reviewed in available literature. Searches were conducted using PubMed, Scopus, and ClinicalTrials.gov databases. Eight papers were identified, published between 2007 and 2020, including six treatment regimens, predominantly vincristine, irinotecan, and bevacizumab (VIB) ± temozolomide (VITB). Among 16 evaluable patients, there were two complete responses, seven partial responses, five patients achieved stable disease (SD), and two patients had progressive disease. Objective responses (OR) were observed in 56% of all cases. OR or SD was observed in 89% (8/9) patients who received VIB/VITB. Bevacizumab was generally well tolerated. Related toxicities included hypertension, proteinuria, and delayed wound healing., Expert Opinion: This review suggests potential effectiveness and good tolerability of bevacizumab in the setting of relapsed/refractory WT when used in combination with other drugs. Such combination therapies may serve as a bridging treatment option to other interventions and more personalized treatment options in the future; however, focused trials are needed to obtain additional evidence.

Published
2024
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37. Widening the spectrum of players affected by genetic changes in Wilms tumor relapse.

Author

Ciceri S, Bertolotti A, Serra A, Gattuso G, Boschetti L, Capasso M, Cecchi C, Sorrentino S, Quarello P, Ciniselli CM, Verderio P, De Cecco L, Manenti G, Diomedi Camassei F, Collini P, Spreafico F, and Perotti D

Abstract

Few studies investigated the genetics of relapsed Wilms tumor (WT), suggesting the SIX1 gene, the microRNA processing genes, and the MYCN network as possibly involved in a relevant percentage of relapses. We investigated 28 relapsing WT patients (10 new cases and 18 cases in which the involvement of SIX and miRNAPG had been excluded) with a panel of ∼5000 genes. We identified variants affecting genes involved in DNA damage prevention and repair in 12/28 relapsing patients (42.9%), and affecting genes involved in chromatin modification and regulation in 6/28 relapsing patients (21.4%), widening the spectrum of anomalies detected in relapsed tumors. The disclosure of molecular pathways possibly underlying tumor progression might allow to use molecularly targeted therapies at relapse. Surprisingly, germline anomalies, mostly affecting DNA damage prevention and repair genes, were identified in 13/28 patients (46.4%), raising the issue of performing a genetic testing to all children presenting with a WT., Competing Interests: The authors declare no competing interest., (© 2024 The Author(s).)

Published
2024
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38. Hallmark discoveries in the biology of Wilms tumour.

Author

Perotti D, Williams RD, Wegert J, Brzezinski J, Maschietto M, Ciceri S, Gisselsson D, Gadd S, Walz AL, Furtwaengler R, Drost J, Al-Saadi R, Evageliou N, Gooskens SL, Hong AL, Murphy AJ, Ortiz MV, O'Sullivan MJ, Mullen EA, van den Heuvel-Eibrink MM, Fernandez CV, Graf N, Grundy PE, Geller JI, Dome JS, Perlman EJ, Gessler M, Huff V, and Pritchard-Jones K

Subjects
Humans, Neoplasm Recurrence, Local, Biomarkers, Biology, Kidney Neoplasms therapy, Wilms Tumor therapy
Abstract

The modern study of Wilms tumour was prompted nearly 50 years ago, when Alfred Knudson proposed the 'two-hit' model of tumour development. Since then, the efforts of researchers worldwide have substantially expanded our knowledge of Wilms tumour biology, including major advances in genetics - from cloning the first Wilms tumour gene to high-throughput studies that have revealed the genetic landscape of this tumour. These discoveries improve understanding of the embryonal origin of Wilms tumour, familial occurrences and associated syndromic conditions. Many efforts have been made to find and clinically apply prognostic biomarkers to Wilms tumour, for which outcomes are generally favourable, but treatment of some affected individuals remains challenging. Challenges are also posed by the intratumoural heterogeneity of biomarkers. Furthermore, preclinical models of Wilms tumour, from cell lines to organoid cultures, have evolved. Despite these many achievements, much still remains to be discovered: further molecular understanding of relapse in Wilms tumour and of the multiple origins of bilateral Wilms tumour are two examples of areas under active investigation. International collaboration, especially when large tumour series are required to obtain robust data, will help to answer some of the remaining unresolved questions., (© 2023. Springer Nature Limited.)

Published
2024
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39. A Gradual Transition Toward Anaplasia in Wilms Tumor Through Tolerance to Genetic Damage.

Author

Uno K, Rastegar B, Jansson C, Durand G, Valind A, Chattopadhyay S, Bertolotti A, Ciceri S, Spreafico F, Collini P, Perotti D, Mengelbier LH, and Gisselsson D

Subjects
Humans, Anaplasia genetics, Mutation, Prognosis, DNA, Kidney Neoplasms genetics, Kidney Neoplasms pathology, Wilms Tumor genetics, Wilms Tumor drug therapy, Wilms Tumor pathology
Abstract

Patients with Wilms tumor (WT) in general have excellent survival, but the prognosis of patients belonging to the subgroup of WT with diffuse anaplasia (DA) is poor due to frequent resistance to chemotherapy. We hypothesized that DA WT cells might undergo changes, such as acquiring a persistent tolerance to DNA damage and copy number aberrations (CNAs), which could eventually lead to their resistance to chemotherapy treatment. Tissue sections from chemotherapy-treated DA WTs (n = 12) were compared with chemotherapy-treated nonanaplastic WTs (n = 15) in a tissue microarray system, enabling analysis of 769 tumor regions. All regions were scored for anaplastic features and immunohistochemistry was used to quantify p53 expression, proliferation index (Ki67), and DNA double-strand breaks (γH2AX). CNAs were assessed by array-based genotyping and TP53 mutations using targeted sequencing. Proliferation index and the frequency of DNA double-strand breaks (γH2AX dot expression) increased with higher anaplasia scores. Almost all (95.6%) areas with full-scale anaplasia had TP53 mutations or loss of heterozygosity, along with an increased amount of CNAs. Interestingly, areas with wild-type TP53 with loss of heterozygosity and only one feature of anaplasia (anaplasia score 1) also had significantly higher proliferation indices, more DNA double-strand breaks, and more CNAs than regions without any anaplastic features (score 0); such areas may be preanaplastic cell populations under selective pressure for TP53 mutations. In conclusion, we suggest that chemoresistance of DA WTs may be partly explained by a high proliferative capability of anaplastic cells, which also have a high burden of double-stranded DNA breaks and CNAs, and that there is a gradual emergence of anaplasia in WT., (Copyright © 2023 The Authors. Published by Elsevier Inc. All rights reserved.)

Published
2024
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40. The pathophysiology of bilateral and multifocal Wilms tumors: What we can learn from the study of predisposition syndromes.

Author

Welter N, Brzezinski J, Treece A, Chintagumpala M, Young MD, Perotti D, Kieran K, Jongmans MCJ, and Murphy AJ

Subjects
Child, Humans, Genes, Wilms Tumor, Syndrome, Genotype, Disease Susceptibility, Wilms Tumor pathology, Kidney Neoplasms pathology
Abstract

Approximately 5% of patients with Wilms tumor present with synchronous bilateral disease. The development of synchronous bilateral Wilms tumor (BWT) is highly suggestive of a genetic or epigenetic predisposition. Patients with known germline predisposition to Wilms tumor (WT1 variants, Beckwith Wiedemann spectrum, TRIM28 variants) have a higher incidence of BWT. This Children's Oncology Group (COG)-International Society for Pediatric Oncology (SIOP-) HARMONICA initiative review for pediatric renal tumors details germline genetic and epigenetic predisposition to BWT development, with an emphasis on alterations in 11p15.5 (ICR1 gain of methylation, paternal uniparental disomy, and postzygotic somatic mosaicism), WT1, TRIM28, and REST. Molecular mechanisms that result in BWT are often also present in multifocal Wilms tumor (multiple separate tumors in one or both kidneys). We identify priority areas for international collaborative research to better understand how predisposing genetic or epigenetic factors associate with response to neoadjuvant chemotherapy, oncologic outcomes, and long-term renal function outcomes., (© 2022 Wiley Periodicals LLC.)

Published
2023
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41. Molecular Signature of Biological Aggressiveness in Clear Cell Sarcoma of the Kidney (CCSK).

Author

Fiore M, Taddia A, Indio V, Bertuccio SN, Messelodi D, Serravalle S, Bandini J, Spreafico F, Perotti D, Collini P, Di Cataldo A, Pasquinelli G, Chiarini F, Fois M, Melchionda F, Pession A, and Astolfi A

Subjects
Humans, HEK293 Cells, Repressor Proteins genetics, Kidney metabolism, Sarcoma, Clear Cell genetics, Sarcoma, Clear Cell pathology, Kidney Neoplasms pathology, Wilms Tumor
Abstract

Clear cell sarcoma of the kidney (CCSK) is a rare pediatric renal tumor with a worse prognosis than Wilms' tumor. Although recently, BCOR internal tandem duplication (ITD) has been found as a driver mutation in more than 80% of cases, a deep molecular characterization of this tumor is still lacking, as well as its correlation with the clinical course. The aim of this study was to investigate the differential molecular signature between metastatic and localized BCOR-ITD-positive CCSK at diagnosis. Whole-exome sequencing (WES) and whole-transcriptome sequencing (WTS) were performed on six localized and three metastatic BCOR-ITD-positive CCSKs, confirming that this tumor carries a low mutational burden. No significant recurrences of somatic or germline mutations other than BCOR-ITD were identified among the evaluated samples. Supervised analysis of gene expression data showed enrichment of hundreds of genes, with a significant overrepresentation of the MAPK signaling pathway in metastatic cases ( p < 0.0001). Within the molecular signature of metastatic CCSK, five genes were highly and significantly over-expressed: FGF3, VEGFA, SPP1, ADM, and JUND. The role of FGF3 in the acquisition of a more aggressive phenotype was investigated in a cell model system obtained by introducing the ITD into the last exon of BCOR by Crispr/Cas9 gene editing of the HEK-293 cell line. Treatment with FGF3 of BCOR-ITD HEK-293 cell line induced a significant increase in cell migration versus both untreated and scramble cell clone. The identification of over-expressed genes in metastatic CCSKs, with a particular focus on FGF3, could offer new prognostic and therapeutic targets in more aggressive cases.

Published
2023
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42. Gene expression-based dissection of inter-histotypes, intra-histotype and intra-tumor heterogeneity in pediatric tumors.

Author

Ciceri S, Carenzo A, Iannó MF, Bertolotti A, Morosi C, Luksch R, Spreafico F, Collini P, Radice P, Massimino M, De Cecco L, and Perotti D

Subjects
Child, Humans, Mutation, Epigenomics, Gene Expression, Tumor Microenvironment, Genetic Heterogeneity, Neoplasm Recurrence, Local genetics
Abstract

Intra-tumor heterogeneity (ITH) fosters tumor evolution, resistance to therapy, and relapse. Recently, many evidence have been accumulated on the occurrence of genetic ITH in pediatric cancers. With this study we aimed to address the downstream effects that genetic and epigenetic ITH, and tumor-microenvironment interactions may produce within a tumor mass. To this aim, we investigated by high-throughput gene expression multiple samples of 5 hepatoblastomas, 5 neuroblastomas, 5 rhabdomyosarcomas, and 5 Wilms tumors. Principal component analysis, single sample hallmark gene sets analysis, and weighted gene co-expression network analysis were performed on gene expression data. We observed that the different tumors clustered by histotype, and then by case, and in addition, a variable degree of ITH was visible in all the investigated cases. The ITH highlighted in this study can represent a challenge in tumor treatment since we demonstrated that different druggable hallmarks and targets may be heterogeneously present within the same tumor mass, and this can potentially lead to therapeutic failure. Despite this heterogeneity, we could highlight some commonalities among the different histotypes investigated, supporting the feasibility to move in the clinic from a histotype-driven to a target-driven, sometimes agnostic, approach at least in some cases., (© 2022. The Author(s).)

Published
2022
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43. Finding the way to Wilms tumor by comparing the primary and relapse tumor samples.

Author

Spreafico F, Ciceri S, and Perotti D

Subjects
Child, Humans, Recurrence, Kidney Neoplasms genetics, Wilms Tumor genetics
Abstract

In this issue of Cell Reports Medicine, Gadd and colleagues presented on behalf of the Children's Oncology Group their comprehensive analysis of genetic changes associated with relapse in children with favorable histology Wilms tumor., Competing Interests: Declaration of interests The authors declare no competing interests., (Copyright © 2022 The Authors. Published by Elsevier Inc. All rights reserved.)

Published
2022
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44. Outcome of SIOP patients with low- or intermediate-risk Wilms tumour relapsing after initial vincristine and actinomycin-D therapy only - the SIOP 93-01 and 2001 protocols.

Author

Groenendijk A, van Tinteren H, Jiang Y, de Krijger RR, Vujanic GM, Godzinski J, Rübe C, Schenk JP, Morosi C, Pritchard-Jones K, Al-Saadi R, Vaidya SJ, Verschuur AC, Ramírez-Villar GL, Graf N, de Camargo B, Drost J, Perotti D, van den Heuvel-Eibrink MM, Brok J, Spreafico F, and Mavinkurve-Groothuis AMC

Subjects
Antineoplastic Combined Chemotherapy Protocols adverse effects, Carboplatin, Child, Dactinomycin, Disease-Free Survival, Doxorubicin, Etoposide, Female, Humans, Ifosfamide therapeutic use, Male, Neoplasm Recurrence, Local pathology, Neoplasm Staging, Retrospective Studies, Vincristine, Kidney Neoplasms pathology, Wilms Tumor therapy
Abstract

Purpose: Society of International Pediatric Oncology - Renal Tumor Study Group (SIOP-RTSG) treatment recommendations for relapsed Wilms tumour (WT) are stratified by the intensity of first-line treatment. To explore the evidence for the treatment of patients relapsing after vincristine and actinomycin-D (VA) treatment for primary WT, we retrospectively evaluated rescue treatment and survival of this patient group., Patients and Methods: We included 109 patients with relapse after VA therapy (no radiotherapy) for stage I-II primary low- or intermediate-risk WT from the SIOP 93-01 and SIOP 2001 studies. Univariate Cox regression analysis was performed to study the effect of relapse treatment intensity on event-free survival (EFS) and overall survival (OS). Relapse treatment intensity was classified into vincristine, actinomycin-D, and either doxorubicin or epirubicin (VAD), and more intensive therapies (ifosfamide/carboplatin/etoposide [ICE]/≥ 4 drugs/high-dose chemotherapy with haematopoietic stem cell transplantation [HD HSCT])., Results: Relapse treatment regimens included either VAD, or cyclophosphamide/carboplatin/etoposide/doxorubicin (CyCED), or ICE backbones. Radiotherapy was administered in 62 patients and HD HSCT in 15 patients. Overall, 5-year EFS and OS after relapse were 72.3% (95% confidence interval [CI]: 64.0-81.6%) and 79.3% (95% CI: 71.5-88.0%), respectively. Patients treated with VAD did not fare worse when compared with patients treated with more intensive therapies (hazard ratio EFS: 0.611 [95% CI: 0.228-1.638] [p-value = 0.327] and hazard ratio OS: 0.438 [95% CI: 0.126-1.700] [p-value = 0.193])., Conclusion: Patients with relapsed WT after initial VA-only treatment showed no inferior EFS and OS when treated with VAD regimens compared with more intensive rescue regimens. A subset of patients relapsing after VA may benefit from less intensive rescue treatment than ICE/CyCED-based regimens and deserve to be pinpointed by identifying additional (molecular) prognostic factors in future studies., Competing Interests: Conflict of interest statement The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2021 The Authors. Published by Elsevier Ltd.. All rights reserved.)

Published
2022
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45. Analysis of the mutational status of SIX1/2 and microRNA processing genes in paired primary and relapsed Wilms tumors and association with relapse.

Author

Ciceri S, Montalvão-de-Azevedo R, Tajbakhsh A, Bertolotti A, Spagnuolo RD, Boschetti L, Capasso M, D'Angelo P, Serra A, Diomedi-Camassei F, Meli M, Nantron M, Quarello P, Buccoliero AM, Tamburini A, Ciniselli CM, Verderio P, Collini P, Radice P, Spreafico F, and Perotti D

Subjects
Humans, Mutation, Survival Analysis, Wilms Tumor mortality, Homeodomain Proteins genetics, Homeodomain Proteins metabolism, MicroRNAs genetics, Nerve Tissue Proteins genetics, Wilms Tumor genetics
Abstract

Whereas 90% of patients with Wilms tumor (WT) reach cure, approximately half of patients developing a recurrent tumor die of the disease. Therefore, to disclose events leading to recurrence represents a clinical need. To study paired primary/recurrent tumor samples, being aware of the intra-tumoral heterogeneity, might help finding these answers. We previously suggested that mutations in SIX1 and DROSHA underlie WT recurrence. With the aim to better investigate this scenario, we collected 19 paired primary/recurrent tumors and 10 primary tumors from relapsing patients and searched for mutations in the SIX1/2 genes and microRNA processing genes (miRNAPGs). We found SIX1 mutation in one case, miRNAPGs mutations in seven cases, and the co-occurrence of SIX1 and miRNAPG mutations in one case. We could observe that, whereas in primary tumors the mutations could be heterogeneously present, in all cases they were positively selected and homogeneously present in the recurrent disease, as also indicated by a "moderate" and "almost perfect" agreement (according to the Landis and Koch classification criteria) between paired samples. Analysis of SIX1/2 genes and miRNAPGs in 50 non-relapsing WTs disclosed SIX2 mutation in one case and miRNAPGs mutations in seven. A borderline statistically significant association was observed between miRNAPGs mutations and the occurrence of relapse (p value: 0.05). These data suggest that SIX1 and miRNAPGs mutations may provide an advantage during tumor progression to recurrence and can represent oncogenic drivers in WT development., (© 2020. The Author(s), under exclusive licence to Springer Nature America, Inc. part of Springer Nature.)

Published
2021
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47. Prognostic Factors for Wilms Tumor Recurrence: A Review of the Literature.

Author

Groenendijk A, Spreafico F, de Krijger RR, Drost J, Brok J, Perotti D, van Tinteren H, Venkatramani R, Godziński J, Rübe C, Geller JI, Graf N, van den Heuvel-Eibrink MM, and Mavinkurve-Groothuis AMC

Abstract

In high-income countries, the overall survival of children with Wilms tumors (WT) is ~90%. However, overall, 15% of patients experience tumor recurrence. The adverse prognostic factors currently used for risk stratification (advanced stage, high risk histology, and combined loss of heterozygosity at 1p and 16q in chemotherapy-naïve WTs) are present in only one third of these cases, and the significance of these factors is prone to change with advancing knowledge and improved treatment regimens. Therefore, we present a comprehensive, updated overview of the published prognostic variables for WT recurrence, ranging from patient-, tumor- and treatment-related characteristics to geographic and socioeconomic factors. Improved first-line treatment regimens based on clinicopathological characteristics and advancing knowledge on copy number variations unveil the importance of further investigating the significance of biological markers for WT recurrence in international collaborations.

Published
2021
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48. Unmet needs for relapsed or refractory Wilms tumour: Mapping the molecular features, exploring organoids and designing early phase trials - A collaborative SIOP-RTSG, COG and ITCC session at the first SIOPE meeting.

Author

Brok J, Mavinkurve-Groothuis AMC, Drost J, Perotti D, Geller JI, Walz AL, Geoerger B, Pasqualini C, Verschuur A, Polanco A, Jones KP, van den Heuvel-Eibrink M, Graf N, and Spreafico F

Subjects
Biomarkers, Tumor antagonists & inhibitors, Clinical Trials as Topic, Combined Modality Therapy, Humans, Kidney Neoplasms drug therapy, Kidney Neoplasms genetics, Neoplasm Recurrence, Local drug therapy, Neoplasm Recurrence, Local pathology, Organoids drug effects, Organoids metabolism, Prognosis, Survival Rate, Wilms Tumor drug therapy, Wilms Tumor genetics, Biomarkers, Tumor genetics, Drug Resistance, Neoplasm, Kidney Neoplasms pathology, Needs Assessment standards, Organoids pathology, Wilms Tumor pathology
Abstract

Wilms tumour (WT) accounts for about 6% of all childhood cancers and overall survival of WT is about 90% in international protocols. However, for WT subgroups with much poorer prognoses, i.e. typically high-risk (unfavorable) histology and/or relapse, there is an unmet need to better understand the biology of WT and to translate biological findings into clinics through early phase clinical trials that evaluate innovative therapies. The main challenges are the small numbers of children suitable for early phase trials, the genetic heterogeneity of WT and the low number of somatic mutations that are currently considered 'druggable'. Accordingly, a joint meeting between clinical and biology experts from the international cooperative groups of the Renal Tumour Study Group of the International Society of Paediatric Oncology, the Renal Tumour Committee of the Children's Oncology Group and the European Innovative Therapies for Children with Cancer consortium and parents representatives was organised during the first SIOPE meeting in Prague, 2019. We reviewed WT molecular features, ongoing/planned early phase trials and explored available knowledge on organoid technology. The key messages were: (1) relapsed WT should undergo whenever possible thorough molecular characterization and be enrolled in protocols or trials with systematic data collecting and reporting; (2) WT displays few known 'actionable' targets and currently no novel agent has appeared promising; (3) we need to improve the enrolment rate of WT candidates in early phase trials especially for the relatively small subgroup of relapses with an adverse prognostic signature; (4) despite some agnostic early phase trials existing, development of WT-focused trials are warranted; (5) growing organoids with parallel testing of drug panels seems feasible and may direct individual treatment and encourage clinical researchers to incorporate the most promising agents into early phase trials., Competing Interests: Declaration of interest statement None declared., (Copyright © 2020 Elsevier Ltd. All rights reserved.)

Published
2021
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