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1. Base-Excision Repair Mutational Signature in Two Sebaceous Carcinomas of the Eyelid

Author: Sangiorgi, Eugenio, Giannuzzi, Federico, Molinario, Clelia, Rapari, Giulia, Riccio, Melania, Cuffaro, Giovanni, Castri, Federica, Benvenuto, Roberta, Genuardi, Maurizio, Massi, Daniela, Savino, Gustavo, Sangiorgi, Eugenio (ORCID:0000-0001-9079-9175), Genuardi, Maurizio (ORCID:0000-0002-7410-8351), Savino, Gustavo (ORCID:0000-0002-9993-5986), Sangiorgi, Eugenio, Giannuzzi, Federico, Molinario, Clelia, Rapari, Giulia, Riccio, Melania, Cuffaro, Giovanni, Castri, Federica, Benvenuto, Roberta, Genuardi, Maurizio, Massi, Daniela, Savino, Gustavo, Sangiorgi, Eugenio (ORCID:0000-0001-9079-9175), Genuardi, Maurizio (ORCID:0000-0002-7410-8351), and Savino, Gustavo (ORCID:0000-0002-9993-5986)
Abstract: Personalized medicine aims to develop tailored treatments for individual patients based on specific mutations present in the affected organ. This approach has proven paramount in cancer treatment, as each tumor carries distinct driver mutations that respond to targeted drugs and, in some cases, may confer resistance to other therapies. Particularly for rare conditions, personalized medicine has the potential to revolutionize treatment strategies. Rare cancers often lack extensive datasets of molecular and pathological information, large-scale trials for novel therapies, and established treatment guidelines. Consequently, surgery is frequently the only viable option for many rare tumors, when feasible, as traditional multimodal approaches employed for more common cancers often play a limited role. Sebaceous carcinoma of the eyelid is an exceptionally rare cancer affecting the eye's adnexal tissues, most frequently reported in Asia, but whose prevalence is significantly increasing even in Europe and the US. The sole established curative treatment is surgical excision, which can lead to significant disfigurement. In cases of metastatic sebaceous carcinoma, validated drug options are currently lacking. In this project, we set out to characterize the mutational landscape of two sebaceous carcinomas of the eyelid following surgical excision. Utilizing available bioinformatics tools, we demonstrated our ability to identify common features promptly and accurately in both tumors. These features included a Base-Excision Repair mutational signature, a notably high tumor mutational burden, and key driver mutations in somatic tissues. These findings had not been previously reported in similar studies. This report underscores how, in the case of rare tumors, it is possible to comprehensively characterize the mutational landscape of each individual case, potentially opening doors to targeted therapeutic options.
Published: 2023

2. Variation in the risk of colorectal cancer in families with Lynch syndrome: a retrospective cohort study

Author: Genuardi, Maurizio, International Mismatch Repair, Consortium, Genuardi Maurizio (ORCID:0000-0002-7410-8351), International Mismatch Repair Consortium, Genuardi, Maurizio, International Mismatch Repair, Consortium, Genuardi Maurizio (ORCID:0000-0002-7410-8351), and International Mismatch Repair Consortium
Abstract: Background: Existing clinical practice guidelines for carriers of pathogenic variants of DNA mismatch repair genes (Lynch syndrome) are based on the mean age-specific cumulative risk (penetrance) of colorectal cancer for all carriers of pathogenic variants in the same gene. We aimed to estimate the variation in the penetrance of colorectal cancer between carriers of pathogenic variants in the same gene by sex and continent of residence. Methods: In this retrospective cohort study, we sourced data from the International Mismatch Repair Consortium, which comprises 273 members from 122 research centres or clinics in 32 countries from six continents who are involved in Lynch syndrome research. Families with at least three members and at least one confirmed carrier of a pathogenic or likely pathogenic variant in a DNA mismatch repair gene (MLH1, MSH2, MSH6, or PMS2) were included. The families of probands with known de-novo pathogenic variants were excluded. Data were collected on the method of ascertainment of the family, sex, carrier status, cancer diagnoses, and ages at the time of pedigree collection and at last contact or death. We used a segregation analysis conditioned on ascertainment to estimate the mean penetrance of colorectal cancer and modelled unmeasured polygenic factors to estimate the variation in penetrance. The existence of unknown familial risk factors modifying colorectal cancer risk for Lynch syndrome carriers was tested by use of a Wald p value for the null hypothesis that the polygenic SD is zero. Findings: 5585 families with Lynch syndrome from 22 countries were eligible for the analysis. Of these, there were insufficient numbers to estimate penetrance for Asia and South America, and for those with EPCAM variants. Therefore, we used data (collected between July 11, 2014, and Dec 31, 2018) from 5255 families (1829 MLH1, 2179 MSH2, 798 MSH6, and 449 PMS2), comprising 79 809 relatives, recruited in 15 countries in North America, Europe, and Australa
Published: 2021

3. Overview of hereditary breast and ovarian cancer (HBOC) guidelines across Europe

Author: Genuardi, Maurizio, David Humberto Marmolejo, 1, Mark Yu Zheng Wong, 2, Svetlana Bajalica-Lagercrantz, 3, Marc Tischkowitz, 2, Judith Balmaña, 4, extended ERN-GENTURIS Thematic Group, 3, Genuardi Maurizio (ORCID:0000-0002-7410-8351), David Humberto Marmolejo 1, Mark Yu Zheng Wong 2, Svetlana Bajalica-Lagercrantz 3, Marc Tischkowitz 2, Judith Balmaña 4, extended ERN-GENTURIS Thematic Group 3, Genuardi, Maurizio, David Humberto Marmolejo, 1, Mark Yu Zheng Wong, 2, Svetlana Bajalica-Lagercrantz, 3, Marc Tischkowitz, 2, Judith Balmaña, 4, extended ERN-GENTURIS Thematic Group, 3, Genuardi Maurizio (ORCID:0000-0002-7410-8351), David Humberto Marmolejo 1, Mark Yu Zheng Wong 2, Svetlana Bajalica-Lagercrantz 3, Marc Tischkowitz 2, Judith Balmaña 4, and extended ERN-GENTURIS Thematic Group 3
Abstract: Hereditary breast and ovarian cancer (HBOC) is a syndrome defined by an increased risk of developing breast and/or ovarian cancer most commonly due to germline disease-causing variants in the BRCA1 and BRCA2 genes, but also other causative genes such as PALB2, ATM and CHEK2. As genetic testing becomes more prevalent and new clinical data emerge, updates of national guidelines are required to incorporate these advances in our knowledge. The aim of this work is to review the guidelines for HBOC genetic testing and clinical surveillance across European countries, mostly affiliated to the European Reference Network (ERN) for Genetic Tumor Risk Syndroms (GENTURIS). Young onset breast cancer (BC), triple negative phenotype, or bilateral BC are considered as criteria for genetic testing in all, with differences in age limits. Testing of invasive epithelial non-mucinous ovarian cancer is also universally accepted. While breast magnetic resonance imaging (MRI) is consistently recommended in high-risk individuals, age of onset for mammograms differ between 30 and 40 years. Risk-reducing mastectomy is commonly offered as an option, while risk-reducing salpingo-oophorectomy is universally recommended. The largest differences are observed with respect to ovarian surveillance prior to risk-reducing salpingo-oophorectomy and in breast surveillance for carriers of non-BRCA1/2 genes. These differences in national guidelines reflect the variations in clinical consensus that may be reached in the absence of consistent evidence for some recommendations.
Published: 2021

4. Deregulated expression of the imprinted DLK1-DIO3 region in Glioblastoma Stem-like Cells: tumor suppressor role of lncRNA MEG3

Author: Buccarelli, Mariachiara, Lulli, Valentina, Giuliani, Alessandro, Signore, Michele, Martini, Maurizio, D'Alessandris, Quintino Giorgio, Giannetti, Stefano, Novelli, Agnese, Ilari, Ramona, Giurato, Giorgio, Boe, Alessandra, Castellani, Giorgia, Spartano, Serena, Marangi, Giuseppe, Biffoni, Mauro, Genuardi, Maurizio, Pallini, Roberto, Marziali, Giovanna, Ricci-Vitiani, Lucia, Martini, Maurizio (ORCID:0000-0002-6260-6310), D'Alessandris, Quintino G (ORCID:0000-0002-2953-9291), Giannetti, Stefano (ORCID:0000-0002-9456-8865), Marangi, Giuseppe (ORCID:0000-0002-6898-8882), Genuardi, Maurizio (ORCID:0000-0002-7410-8351), Pallini, Roberto (ORCID:0000-0002-4611-8827), Buccarelli, Mariachiara, Lulli, Valentina, Giuliani, Alessandro, Signore, Michele, Martini, Maurizio, D'Alessandris, Quintino Giorgio, Giannetti, Stefano, Novelli, Agnese, Ilari, Ramona, Giurato, Giorgio, Boe, Alessandra, Castellani, Giorgia, Spartano, Serena, Marangi, Giuseppe, Biffoni, Mauro, Genuardi, Maurizio, Pallini, Roberto, Marziali, Giovanna, Ricci-Vitiani, Lucia, Martini, Maurizio (ORCID:0000-0002-6260-6310), D'Alessandris, Quintino G (ORCID:0000-0002-2953-9291), Giannetti, Stefano (ORCID:0000-0002-9456-8865), Marangi, Giuseppe (ORCID:0000-0002-6898-8882), Genuardi, Maurizio (ORCID:0000-0002-7410-8351), and Pallini, Roberto (ORCID:0000-0002-4611-8827)
Abstract: Background: Glioblastoma (GBM) stem-like cells (GSCs) are thought to be responsible for the maintenance and aggressiveness of GBM, the most common primary brain tumor in adults. This study aims at elucidating the involvement of deregulations within the imprinted DLK-DIO3 region on chromosome 14q32 in GBM pathogenesis. Methods: RT-PCR analyses were performed on GSCs and GBM tissues. Methylation analyses, gene expression and Reverse-Phase protein Array profiles were used to investigate the tumor suppressor function of MEG3. Results: Loss of expression of genes and non-coding RNAs within the DLK1-DIO3 region was observed in GSCs and GBM tissues compared to normal brain. This down-regulation is mainly mediated by epigenetic silencing. Kaplan-Meier analysis indicated that low expression of MEG3 and MEG8 lncRNAs significantly correlated with short survival in GBM patients. MEG3 restoration impairs tumorigenic abilities of GSCs in vitro by inhibiting cell growth, migration and colony formation and decreases in vivo tumor growth reducing infiltrative growth. These effects were associated with modulation of genes involved in cell adhesion and Epithelial to Mesenchymal Transition (EMT). Conclusions: In GBM, MEG3 acts as a tumor-suppressor mainly regulating cell adhesion, EMT and cell proliferation, thus providing a potential candidate for novel GBM therapies.
Published: 2020

5. Reversion to Normal of FMR1 Expanded Alleles: A Rare Event in Two Independent Fragile X Syndrome Families

Author: Tabolacci, Elisabetta, Pietrobono, Roberta, Maneri, Giulia, Remondini, Laura, Nobile, Veronica, Della Monica, Matteo, Pomponi, Maria Grazia, Genuardi, Maurizio, Neri, Giovanni, Chiurazzi, Pietro, Tabolacci, Elisabetta (ORCID:0000-0002-4707-2242), Genuardi, Maurizio (ORCID:0000-0002-7410-8351), Chiurazzi, Pietro (ORCID:0000-0001-5104-1521), Tabolacci, Elisabetta, Pietrobono, Roberta, Maneri, Giulia, Remondini, Laura, Nobile, Veronica, Della Monica, Matteo, Pomponi, Maria Grazia, Genuardi, Maurizio, Neri, Giovanni, Chiurazzi, Pietro, Tabolacci, Elisabetta (ORCID:0000-0002-4707-2242), Genuardi, Maurizio (ORCID:0000-0002-7410-8351), and Chiurazzi, Pietro (ORCID:0000-0001-5104-1521)
Abstract: Fragile X syndrome (FXS) is mostly due to the expansion and subsequent methylation of a polymorphic CGG repeat in the 5' UTR of the FMR1 gene. Full mutation alleles (FM) have more than 200 repeats and result in FMR1 gene silencing and FXS. FMs arise from maternal premutations (PM) that have 56-200 CGGs; contractions of a maternal PM or FM are rare. Here, we describe two unaffected boys in two independent FXS families who inherited a non-mosaic allele in the normal and intermediate range, respectively, from their mothers who are carriers of an expanded CGG allele. The first boy inherited a 51 CGG allele (without AGG interruptions) from his mother, who carries a PM allele with 72 CGGs. The other boy inherited from his FM mother an unusual allele with 19 CGGs resulting from a deletion, removing 85 bp upstream of the CGG repeat. Given that transcription of the deleted allele was found to be preserved, we assume that the binding sites for FMR1 transcription factors are excluded from the deletion. Such unusual cases resulting in non-mosaic reduction of maternal CGG expansions may help to clarify the molecular mechanisms underlying the instability of the FMR1 gene.
Published: 2020

6. Gastrointestinal juvenile-like (inflammatory/hyperplastic) mucosal polyps in neurofibromatosis type 1 with no concurrent genetic or clinical evidence of other syndromes

Author: Ravegnini, Gloria, Quero, Giuseppe, Sammarini, Giulia, Giustiniani, Maria Cristina, Castri, Federica, Pomponi, Maria Grazia, Angelini, Sabrina, Alfieri, Sergio, Genuardi, Maurizio, Zamboni, Giuseppe, Ricci, Riccardo, Quero, Giuseppe (ORCID:0000-0002-0001-9479), Alfieri, Sergio (ORCID:0000-0002-0404-724X), Genuardi, Maurizio (ORCID:0000-0002-7410-8351), Ricci, Riccardo (ORCID:0000-0002-9089-5084), Ravegnini, Gloria, Quero, Giuseppe, Sammarini, Giulia, Giustiniani, Maria Cristina, Castri, Federica, Pomponi, Maria Grazia, Angelini, Sabrina, Alfieri, Sergio, Genuardi, Maurizio, Zamboni, Giuseppe, Ricci, Riccardo, Quero, Giuseppe (ORCID:0000-0002-0001-9479), Alfieri, Sergio (ORCID:0000-0002-0404-724X), Genuardi, Maurizio (ORCID:0000-0002-7410-8351), and Ricci, Riccardo (ORCID:0000-0002-9089-5084)
Abstract: Gastrointestinal “juvenile-like (inflammatory/hyperplastic) mucosal polyps” (JLIHMPs) have been proposed as a neurofibromatosis type 1 (NF1)-specific gastrointestinal manifestation. Juvenile polyposis syndrome (JPS) has also been reported in a NF1 patient, harboring concurrent NF1 and SMAD4 germline mutations. Additionally, NF1-like cafe-au-lait spots have been described in biallelic mismatch repair deficiency, another condition featuring gastrointestinal polyps. The SMAD4 and BMPR1A genes that are involved in 50–60% of JPS cases have not been investigated in the ~ 20 published cases of NF1-associated JLIHMPs with the exception of the abovementioned patient with concomitant JPS and NF1. NF1 defects have been found in the only two cases exhaustively tested. Therefore, JLIHMP has been questioned as an independent, NF1-specific entity. Incidental associations between NF1 and gastrointestinal polyposes at risk for gastrointestinal carcinoma should not be overlooked, given their implications in terms of clinical surveillance. We describe two patients featuring JLIHMPs in clinically/genetically proven NF1, in the absence of SMAD4 and BMPR1A mutations. In one case, the intervening mucosa was markedly inflamed, unlike JPS. We suggest that JLIHMP probably represents a gastrointestinal lesion specific to NF1.
Published: 2019

7. The chromosome analysis of the miscarriage tissue. Miscarried embryo/fetal crown rump length (CRL) measurement: A practical use

Author: D'Ippolito, Silvia, Di Simone, Nicoletta, Orteschi, Daniela, Pomponi, Maria Grazia, Genuardi, Maurizio, Sisti, Leuconoe Grazia, Castellani, Roberta, Rossi, Esther, Scambia, Giovanni, Zollino, Marcella, D'Ippolito, Silvia (ORCID:0000-0002-6160-0558), Di Simone, Nicoletta (ORCID:0000-0003-1273-3335), Genuardi, Maurizio (ORCID:0000-0002-7410-8351), Rossi, Esther (ORCID:0000-0003-3819-4229), Scambia, Giovanni (ORCID:0000-0003-2758-1063), Zollino, Marcella (ORCID:0000-0003-4871-9519), D'Ippolito, Silvia, Di Simone, Nicoletta, Orteschi, Daniela, Pomponi, Maria Grazia, Genuardi, Maurizio, Sisti, Leuconoe Grazia, Castellani, Roberta, Rossi, Esther, Scambia, Giovanni, Zollino, Marcella, D'Ippolito, Silvia (ORCID:0000-0002-6160-0558), Di Simone, Nicoletta (ORCID:0000-0003-1273-3335), Genuardi, Maurizio (ORCID:0000-0002-7410-8351), Rossi, Esther (ORCID:0000-0003-3819-4229), Scambia, Giovanni (ORCID:0000-0003-2758-1063), and Zollino, Marcella (ORCID:0000-0003-4871-9519)
Abstract: Objective To investigate whether miscarried embryo/fetal crown rump length (CRL) measurement may yield a practical application for predicting a conclusive result at the cytogenetic analysis of miscarriage tissue. Our study might help in improving the cytogenetic method, the results of which may be affected by maternal cell contamination (MCC). In particular, we aimed at establishing whether the miscarried embryo/fetal CRL measurement shows accuracy in predicting the possibility of MCC and the scan cut-off value useful to this purpose and, as a result, suggest a multi-step procedure for the genetic ascertainment. Methods Women experiencing at least two miscarriages of less than 20 weeks size at the Pregnancy Loss Unit at Fondazione Policlinico A. Gemelli underwent a scan before surgery. The CRL value was recorded. After the dilatation and courettage (D&C) procedure, miscarriage tissue was processed through the proposed multi-step procedure before performing oligo-nucleotide- based and SNP (single nucleotide polymorphisms)-based comparative genomic hybridization (CGH+SNP) microarray analysis. Results 63 women and 63 miscarriages met the criteria. By using the Receiving Operator Characteristic (ROC) curves, CRL showed an AUC of 0.816 (95%CI:0.703±0.928,p<0.001). A CRL24.5 mm cut-off value showed a higher positive likelihood ratio (5.27) but, conversely, a higher negative likelihood ratio (0.64) in predicting the possibility of MCC. Microarray analysis was successful in the totality of cases in which the embryo/fetal origin of miscarriage tissues was proven.
Published: 2017

8. Assessment of the InSiGHT Interpretation Criteria for the Clinical Classification of 24 MLH1 and MSH2 Gene Variants.

Author: Tricarico, R, Kasela, M, Mareni, C, Thompson, Ba, Drouet, A, Staderini, L, Gorelli, G, Crucianelli, F, Ingrosso, V, Kantelinen, J, Papi, L, De Angioletti, M, Berardi, M, Gaildrat, P, Soukarieh, O, Turchetti, D, Martins, A, Spurdle, Ab, Nyström, M, Genuardi, Maurizio, Genuardi, Maurizio (ORCID:0000-0002-7410-8351), Tricarico, R, Kasela, M, Mareni, C, Thompson, Ba, Drouet, A, Staderini, L, Gorelli, G, Crucianelli, F, Ingrosso, V, Kantelinen, J, Papi, L, De Angioletti, M, Berardi, M, Gaildrat, P, Soukarieh, O, Turchetti, D, Martins, A, Spurdle, Ab, Nyström, M, Genuardi, Maurizio, and Genuardi, Maurizio (ORCID:0000-0002-7410-8351)
Abstract: Pathogenicity assessment of DNA variants in disease genes to explain their clinical consequences is an integral component of diagnostic molecular testing. The International Society for Gastrointestinal Hereditary Tumors (InSiGHT) has developed specific criteria for the interpretation of mismatch repair (MMR) gene variants. Here, we performed a systematic investigation of 24 MLH1 and MSH2 variants. The assessments were done by analyzing population frequency, segregation, tumor molecular characteristics, RNA effects, protein expression levels, and in vitro MMR activity. Classifications were confirmed for 15 variants and changed for three, and for the first time determined for six novel variants. Overall, based on our results, we propose the introduction of some refinements to the InSiGHT classification rules. The proposed changes have the advantage of homogenizing the InSIGHT interpretation criteria with those set out by the Evidence-based Network for the Interpretation of Germline Mutant Alleles (ENIGMA) consortium for the BRCA1/BRCA2 genes. We also observed that the addition of only few clinical data was sufficient to obtain a more stable classification for variants considered as "likely pathogenic" or "likely nonpathogenic." This shows the importance of obtaining as many as possible points of evidence for variant interpretation, especially from the clinical setting.
Published: 2017

9. Incidence of and survival after subsequent cancers in carriers of pathogenic MMR variants with previous cancer: a report from the prospective Lynch syndrome database

Author: Møller, P, Seppälä, I, Bernstein, I, Holinski Feder, E, Sala, P, Evans, Dg, Lindblom, A, Macrae, F, Blanco, I, Sijmons, R, Jeffries, J, Vasen, H, Burn, J, Nakken, S, Hovig, E, Rødland, Ea, Tharmaratnam, K, de Vos Tot Nederveen Cappel, Wh, Hill, J, Wijnen, J, Jenkins, M, Green, K, Lalloo, F, Sunde, L, Mints, M, Bertario, L, Pineda, M, Navarro, M, Morak, M, Renkonen Sinisalo, L, Frayling, Im, Plazzer, Jp, Pylvanainen, K, Genuardi, Maurizio, Mecklin, Jp, Möslein, G, Sampson, Jr, Capella, G, Mallorca, Group, Genuardi, Maurizio (ORCID:0000-0002-7410-8351), Møller, P, Seppälä, I, Bernstein, I, Holinski Feder, E, Sala, P, Evans, Dg, Lindblom, A, Macrae, F, Blanco, I, Sijmons, R, Jeffries, J, Vasen, H, Burn, J, Nakken, S, Hovig, E, Rødland, Ea, Tharmaratnam, K, de Vos Tot Nederveen Cappel, Wh, Hill, J, Wijnen, J, Jenkins, M, Green, K, Lalloo, F, Sunde, L, Mints, M, Bertario, L, Pineda, M, Navarro, M, Morak, M, Renkonen Sinisalo, L, Frayling, Im, Plazzer, Jp, Pylvanainen, K, Genuardi, Maurizio, Mecklin, Jp, Möslein, G, Sampson, Jr, Capella, G, Mallorca, Group, and Genuardi, Maurizio (ORCID:0000-0002-7410-8351)
Abstract: BJECTIVE: Today most patients with Lynch syndrome (LS) survive their first cancer. There is limited information on the incidences and outcome of subsequent cancers. The present study addresses three questions: (i) what is the cumulative incidence of a subsequent cancer; (ii) in which organs do subsequent cancers occur; and (iii) what is the survival following these cancers? DESIGN: Information was collated on prospectively organised surveillance and prospectively observed outcomes in patients with LS who had cancer prior to inclusion and analysed by age, gender and genetic variants. RESULTS: 1273 patients with LS from 10 countries were followed up for 7753 observation years. 318 patients (25.7%) developed 341 first subsequent cancers, including colorectal (n=147, 43%), upper GI, pancreas or bile duct (n=37, 11%) and urinary tract (n=32, 10%). The cumulative incidences for any subsequent cancer from age 40 to age 70 years were 73% for pathogenic MLH1 (path_MLH1), 76% for path_MSH2 carriers and 52% for path_MSH6 carriers, and for colorectal cancer (CRC) the cumulative incidences were 46%, 48% and 23%, respectively. Crude survival after any subsequent cancer was 82% (95% CI 76% to 87%) and 10-year crude survival after CRC was 91% (95% CI 83% to 95%). CONCLUSIONS: Relative incidence of subsequent cancer compared with incidence of first cancer was slightly but insignificantly higher than cancer incidence in patients with LS without previous cancer (range 0.94-1.49). The favourable survival after subsequent cancers validated continued follow-up to prevent death from cancer. The interactive website http://lscarisk.org was expanded to calculate the risks by gender, genetic variant and age for subsequent cancer for any patient with LS with previous cancer.
Published: 2017

10. Assessment of the InSiGHT Interpretation Criteria for the Clinical Classification of 24 MLH1 and MSH2 Gene Variants

Author: Tricarico, Rossella, Kasela, Mariann, Mareni, Cristina, Thompson, Bryony A., Drouet, Aurélie, Staderini, Lucia, Gorelli, Greta, Crucianelli, Francesca, Ingrosso, Valentina, Kantelinen, Jukka, Papi, Laura, De Angioletti, Maria, Berardi, Margherita, Gaildrat, Pascaline, Soukarieh, Omar, Turchetti, Daniela, Martins, Alexandra, Spurdle, Amanda B., Nyström, Minna, Genuardi, Maurizio, Genuardi, Maurizio (ORCID:0000-0002-7410-8351), Tricarico, Rossella, Kasela, Mariann, Mareni, Cristina, Thompson, Bryony A., Drouet, Aurélie, Staderini, Lucia, Gorelli, Greta, Crucianelli, Francesca, Ingrosso, Valentina, Kantelinen, Jukka, Papi, Laura, De Angioletti, Maria, Berardi, Margherita, Gaildrat, Pascaline, Soukarieh, Omar, Turchetti, Daniela, Martins, Alexandra, Spurdle, Amanda B., Nyström, Minna, Genuardi, Maurizio, and Genuardi, Maurizio (ORCID:0000-0002-7410-8351)
Abstract: Pathogenicity assessment of DNA variants in disease genes to explain their clinical consequences is an integral component of diagnostic molecular testing. The International Society for Gastrointestinal Hereditary Tumors (InSiGHT) has developed specific criteria for the interpretation of mismatch repair (MMR) gene variants. Here, we performed a systematic investigation of 24 MLH1 and MSH2 variants. The assessments were done by analyzing population frequency, segregation, tumor molecular characteristics, RNA effects, protein expression levels, and in vitro MMR activity. Classifications were confirmed for 15 variants and changed for three, and for the first time determined for six novel variants. Overall, based on our results, we propose the introduction of some refinements to the InSiGHT classification rules. The proposed changes have the advantage of homogenizing the InSIGHT interpretation criteria with those set out by the Evidence-based Network for the Interpretation of Germline Mutant Alleles (ENIGMA) consortium for the BRCA1/BRCA2 genes. We also observed that the addition of only few clinical data was sufficient to obtain a more stable classification for variants considered as “likely pathogenic” or “likely nonpathogenic.” This shows the importance of obtaining as many as possible points of evidence for variant interpretation, especially from the clinical setting.
Published: 2017

11. The Role of Genetic Testing in the Identification of Young Athletes with Inherited Primitive Cardiac Disorders at Risk of Exercise Sudden Death

Author: Tiziano, Francesco Danilo, Palmieri, Vincenzo, Genuardi, Maurizio, Zeppilli, Paolo, Tiziano, Francesco Danilo (ORCID:0000-0002-5545-6158), Palmieri, Vincenzo (ORCID:0000-0002-4478-4033), Genuardi, Maurizio (ORCID:0000-0002-7410-8351), Zeppilli, Paolo (ORCID:0000-0002-5228-3634), Tiziano, Francesco Danilo, Palmieri, Vincenzo, Genuardi, Maurizio, Zeppilli, Paolo, Tiziano, Francesco Danilo (ORCID:0000-0002-5545-6158), Palmieri, Vincenzo (ORCID:0000-0002-4478-4033), Genuardi, Maurizio (ORCID:0000-0002-7410-8351), and Zeppilli, Paolo (ORCID:0000-0002-5228-3634)
Abstract: Although relatively rare, inherited primitive cardiac disorders (IPCDs) in athletes have a deep social impact since they often present as sudden cardiac death (SCD) of young and otherwise healthy persons. The diagnosis of these conditions is likely underestimated due to the lack of shared clinical criteria and to the existence of several borderline clinical pictures. We will focus on the clinical and molecular diagnosis of the most common IPCDs, namely hypertrophic cardiomyopathies, long QT syndrome, arrhythmogenic right ventricular cardiomyopathy, and left ventricular non-compaction. Collectively, these conditions account for the majority of SCD episodes and/or cardiologic clinical problems in athletes. In addition to the clinical and instrumental tools for the diagnosis of IPCD, the viral technological advances in genetic testing have facilitated the molecular confirmation of these conditions. However, genetic testing presents several issues: the limited sensitivity (globally, around 50%), the low prognostic predictive value, the probability to find pathogenic variants in different genes in the same patient, and the risk of non-interpretable results. In this review, we will analyze the pros and cons of the different clinical approaches for the presymptomatic identification, the diagnosis and management of IPCD athletes, and we will discuss the indications to the genetic testing for patients and their relatives, particularly focusing on the most complex scenarios, such as presymptomatic tests, uncertain results, and unexpected findings.
Published: 2016

12. Recommendations for the implementation of BRCA testing in the care and treatment pathways of ovarian cancer patients

Author: Pinto, Carmine, Bella, Maria Angela, Capoluongo, Ettore Domenico, Carrera, Paola, Clemente, Claudio, Colombo, Nicoletta, Cortesi, Laura, De Rosa, Gaetano, Fenizia, Francesca, Genuardi, Maurizio, Gori, Stefania, Guarneri, Valentina, Marchetti, Antonio, Marchetti, Paolo, Normanno, Nicola, Pasini, Barbara, Pignata, Sandro, Radice, Paolo, Ricevuto, Enrico, Dello Russo, Antonio, Tagliaferri, Pierosandro, Tassone, Pierfrancesco, Truini, Mauro, Varesco, Liliana, Capoluongo, Ettore Domenico (ORCID:0000-0001-9872-0572), Genuardi, Maurizio (ORCID:0000-0002-7410-8351), Pinto, Carmine, Bella, Maria Angela, Capoluongo, Ettore Domenico, Carrera, Paola, Clemente, Claudio, Colombo, Nicoletta, Cortesi, Laura, De Rosa, Gaetano, Fenizia, Francesca, Genuardi, Maurizio, Gori, Stefania, Guarneri, Valentina, Marchetti, Antonio, Marchetti, Paolo, Normanno, Nicola, Pasini, Barbara, Pignata, Sandro, Radice, Paolo, Ricevuto, Enrico, Dello Russo, Antonio, Tagliaferri, Pierosandro, Tassone, Pierfrancesco, Truini, Mauro, Varesco, Liliana, Capoluongo, Ettore Domenico (ORCID:0000-0001-9872-0572), and Genuardi, Maurizio (ORCID:0000-0002-7410-8351)
Abstract: In the last 20 years, following the identification of the BRCA1 and BRCA2 genes (hereinafter referred to as the BRCA genes), preventive pathways have been developed for the identification and clinical management of individuals at high risk of developing breast and ovarian cancer due to the presence of a pathogenic variant in either of these genes. These pathways are aimed at educating high-risk subjects on programs targeted toward early diagnosis and cancer risk reduction. The approval of a novel class of drugs, the PARP enzyme inhibitors, for the treatment of ovarian cancer patients carrying high-risk BRCA pathogenic variants has changed this scenario. BRCA testing, in addition to providing information on the risk of disease, has become also a predictive marker of drug response in ovarian carcinoma patients. These recommendations prepared by Associazione Italiana di Oncologia Medica (AIOM), Società Italiana Genetica Umana (SIGU), Società Italiana di Biochimica Clinica e Biologia Molecolare Clinica (SIBIOC) and Società Italiana di Anatomia Patologica e Citologia Diagnostica – Italian Division of the International Academy of Pathology (SIAPEC-IAP) are focused on the implementation of BRCA testing in the care and treatment pathways of ovarian cancer patients.
Published: 2016

13. Recurrent candidiasis and early-onset gastric cancer in a patient with a genetically defined partial MYD88 defect

Author: Vogelaar, Ingrid P., Ligtenberg, Marjolijn J. L., van der Post, Rachel S., de Voer, Richarda M., Kets, C. Marleen, Jansen, Trees J. G., Jacobs, Liesbeth, Schreibelt, Gerty, de Vries, I. Jolanda M., Netea, Mihai G., Hoogerbrugge, Nicoline, Lubinski, Jan, Jakubowska, Anna, Teodorczyk, Urszula, Schackert, Hans K., Aalfs, Cora M., Gómez García, Encarna B., Ranzani, Guglielmina N., Molinaro, Valeria, van Hest, Liselotte P., Hes, Frederik J., Holinski Feder, Elke, Genuardi, Maurizio, Ausems, Margreet G. E. M., Sijmons, Rolf H., Wagner, Anja, van der Kolk, Lizet E., Pinheiro, Hugo, Oliveira, Carla, Bjørnevoll, Inga, Høberg Vetti, Hildegunn, Han, J., van Krieken, J. M., Genuardi, Maurizio (ORCID:0000-0002-7410-8351), Vogelaar, Ingrid P., Ligtenberg, Marjolijn J. L., van der Post, Rachel S., de Voer, Richarda M., Kets, C. Marleen, Jansen, Trees J. G., Jacobs, Liesbeth, Schreibelt, Gerty, de Vries, I. Jolanda M., Netea, Mihai G., Hoogerbrugge, Nicoline, Lubinski, Jan, Jakubowska, Anna, Teodorczyk, Urszula, Schackert, Hans K., Aalfs, Cora M., Gómez García, Encarna B., Ranzani, Guglielmina N., Molinaro, Valeria, van Hest, Liselotte P., Hes, Frederik J., Holinski Feder, Elke, Genuardi, Maurizio, Ausems, Margreet G. E. M., Sijmons, Rolf H., Wagner, Anja, van der Kolk, Lizet E., Pinheiro, Hugo, Oliveira, Carla, Bjørnevoll, Inga, Høberg Vetti, Hildegunn, Han, J., van Krieken, J. M., and Genuardi, Maurizio (ORCID:0000-0002-7410-8351)
Abstract: Gastric cancer is caused by both genetic and environmental factors. A woman who suffered from recurrent candidiasis throughout her life developed diffuse-type gastric cancer at the age of 23 years. Using whole-exome sequencing we identified a germline homozygous missense variant in MYD88. Immunological assays on peripheral blood mononuclear cells revealed an impaired immune response upon stimulation with Candida albicans, characterized by a defective production of the cytokine interleukin-17. Our data suggest that a genetic defect in MYD88 results in an impaired immune response and may increase gastric cancer risk.
Published: 2016

14. Correlation between mutations and mRNA expression of APC and MUTYH genes: new insight into hereditary colorectal polyposis predisposition.

Author: Aceto, Gitana Maria, Fantini, Fabiana, De Iure, Sabrina, Di Nicola, Marta, Palka, Giandomenico, Valenzano, Rosa, Di Gregorio, Patrizia, Stigliano, Vincenza, Genuardi, Maurizio, Battista, Pasquale, Cama, Alessandro, Curia, Maria Cristina, Genuardi, Maurizio (ORCID:0000-0002-7410-8351), Aceto, Gitana Maria, Fantini, Fabiana, De Iure, Sabrina, Di Nicola, Marta, Palka, Giandomenico, Valenzano, Rosa, Di Gregorio, Patrizia, Stigliano, Vincenza, Genuardi, Maurizio, Battista, Pasquale, Cama, Alessandro, Curia, Maria Cristina, and Genuardi, Maurizio (ORCID:0000-0002-7410-8351)
Abstract: BACKGROUND: Transcript dosage imbalance may influence the transcriptome. To gain insight into the role of altered gene expression in hereditary colorectal polyposis predisposition, in the present study we analyzed absolute and allele-specific expression (ASE) of adenomatous polyposis coli (APC) and mutY Homolog (MUTYH) genes. METHODS: We analyzed DNA and RNA extracted from peripheral blood mononuclear cells (PBMC) of 49 familial polyposis patients and 42 healthy blood donors selected according similar gender and age. Patients were studied for germline alterations in both genes using dHPLC, MLPA and automated sequencing. APC and MUTYH mRNA expression levels were investigated by quantitative Real-Time PCR (qRT-PCR) analysis using TaqMan assay and by ASE assays using dHPLC-based primer extension. RESULTS: Twenty out of 49 patients showed germline mutations: 14 in APC gene and six in MUTYH gene. Twenty-nine patients did not show mutations in both genes. Results from qRT-PCR indicated that gene expression of both APC and MUTYH was reduced in patients analyzed. In particular, a significant reduction in APC expression was observed in patients without APC germline mutation vs control group (P < 0.05) while APC expression in the mutation carrier patients, although lower compared to control individuals, did not show statistical significance. On the other hand a significant reduced MUTYH expression was detected in patients with MUTYH mutations vs control group (P < 0.05). Altered ASE of APC was detected in four out of eight APC mutation carriers. In particular one case showed a complete loss of one allele. Among APC mutation negative cases, 4 out of 13 showed a moderate ASE. ASE of MUTYH did not show any altered expression in the cases analyzed. Spearman's Rho Test analysis showed a positive and significant correlation between APC and MUTYH genes both in cases and in controls (P = 0.020 and P < 0.001). CONCLUSIONS: APC and MUTYH showed a reduced germline expression, not always
Published: 2015

15. Variable expressivity of a familial 1.9 Mb microdeletion in 3q28 leading to haploinsufficiency of TP63: Refinement of the critical region for a new microdeletion phenotype

Author: Gurrieri, Fiorella, Ponzi, Emanuela, Asaro, Alessia, Orteschi, Daniela, Genuardi, Maurizio, Zollino, Marcella, Gurrieri, Fiorella (ORCID:0000-0002-6775-5972), Genuardi, Maurizio (ORCID:0000-0002-7410-8351), Zollino, Marcella (ORCID:0000-0003-4871-9519), Gurrieri, Fiorella, Ponzi, Emanuela, Asaro, Alessia, Orteschi, Daniela, Genuardi, Maurizio, Zollino, Marcella, Gurrieri, Fiorella (ORCID:0000-0002-6775-5972), Genuardi, Maurizio (ORCID:0000-0002-7410-8351), and Zollino, Marcella (ORCID:0000-0003-4871-9519)
Abstract: We report on a 3-year-old male with intellectual disability (ID), characteristic facial features, polydactyly and epilepsy carrying a paternally inherited 3q28 deletion of 1.9 Mb. The father, carrying the same deletion, presents with cleft palate, nail dystrophy and learning difficulties. The deleted region in this family is one of the smallest so far reported among genomic deletions affecting 3q27-3q28 for which some phenotypic descriptions are available. In particular, since the phenotype of our proband is strikingly similar to that previously described in a patient with a 9.3 Mb deletion, the deletion identified in this report contributes to the definition of the molecular boundaries of a genomic region responsible for a distinct clinical phenotype. Within the deleted interval there are 9 annotated genes, including TP63. Gain of function mutations of TP63 are known to be responsible for a group of conditions with distal limb and ectodermal involvement, such as ADULT, EEC, LMS, and SHFM4 syndromes. Interestingly, our cases demonstrate a milder phenotypic effect for loss of function of this gene
Published: 2015

16. Variable expressivity of a familial 1.9 Mb microdeletion in 3q28 leading to haploinsufficiency of TP63: Refinement of the critical region for a new microdeletion phenotype.

Author: Ponzi, Emanuela, Asaro, Alessia, Orteschi, Daniela, Genuardi, Maurizio, Zollino, Marcella, Guerrieri, Fiorella, Genuardi, Maurizio (ORCID:0000-0002-7410-8351), Zollino, Marcella (ORCID:0000-0003-4871-9519), Ponzi, Emanuela, Asaro, Alessia, Orteschi, Daniela, Genuardi, Maurizio, Zollino, Marcella, Guerrieri, Fiorella, Genuardi, Maurizio (ORCID:0000-0002-7410-8351), and Zollino, Marcella (ORCID:0000-0003-4871-9519)
Abstract: We report on a 3-year-old male with intellectual disability (ID), characteristic facial features, polydactyly and epilepsy carrying a paternally inherited 3q28 deletion of 1.9 Mb. The father, carrying the same deletion, presents with cleft palate, nail dystrophy and learning difficulties. The deleted region in this family is one of the smallest so far reported among genomic deletions affecting 3q27-3q28 for which some phenotypic descriptions are available. In particular, since the phenotype of our proband is strikingly similar to that previously described in a patient with a 9.3 Mb deletion, the deletion identified in this report contributes to the definition of the molecular boundaries of a genomic region responsible for a distinct clinical phenotype. Within the deleted interval there are 9 annotated genes, including TP63. Gain of function mutations of TP63 are known to be responsible for a group of conditions with distal limb and ectodermal involvement, such as ADULT, EEC, LMS, and SHFM4 syndromes. Interestingly, our cases demonstrate a milder phenotypic effect for loss of function of this gene.
Published: 2015

17. FANCM c.5791C>T nonsense mutation (rs144567652) induces exon skipping, affects DNA repair activity and is a familial breast cancer risk factor.

Author: Peterlongo, P, Catucci, I, Colombo, M, Caleca, L, Mucaki, E, Bogliolo, M, Marin, M, Damiola, F, Bernard, L, Pensotti, V, Volorio, S, Dall'Olio, V, Meindl, A, Bartram, C, Sutter, C, Surowy, H, Sornin, V, Dondon, Mg, Eon Marchais, S, Stoppa Lyonnett, D, Andrieu, N, Sinilnikova, Om, Genesis, Mitchell G, James, Pa, Thompson, E, Kconfab, Swe, Brca, Marchetti, M, Verzeroli, C, Tartari, C, Capone, G, Putignano, Al, Genuardi, Maurizio, Medici, V, Marchi, I, Federico, M, Tognazzo, S, Matricardi, L, Agata, S, Dolcetti, R, Della Puppa, L, Cini, G, Gismondi, V, Viassolo, V, Perfumo, C, Mencarelli, Ma, Baldassarri, M, Peissel, B, Roversi, G, Silvestri, V, Rizzolo, P, Spina, F, Vivanet, C, Tibiletti, Mg, Caligo, Ma, Gambino, G, Tommasi, S, Pilato, B, Tondini, C, Corna, C, Bonanni, B, Barile, M, Osorio, A, Benitez, J, Balestrino, L, Ottini, L, Manoukian, S, Pierotti, Ma, Renieri, A, Varesco, L, Couch, Fj, Wang, X, Delivee, P, Hilbers, F, Van Asperen, Cj, Viel, A, Montagna, M, Cortesi, L, Diez, O, Balmana, J, Hauke, J, Scmutzler, Rk, Papi, L, Pujana, Ma, Lazaro, S, Falanga, A, Offit, K, Vijai, J, Campbell, I, Burwinkel, B, Kvist, A, Enrencrona, H, Mazoyer, S, Pizzamiglio, S, Verderio, P, Surralles, J, Rogan, Pk, Radice, P., Genuardi, Maurizio (ORCID:0000-0002-7410-8351), Peterlongo, P, Catucci, I, Colombo, M, Caleca, L, Mucaki, E, Bogliolo, M, Marin, M, Damiola, F, Bernard, L, Pensotti, V, Volorio, S, Dall'Olio, V, Meindl, A, Bartram, C, Sutter, C, Surowy, H, Sornin, V, Dondon, Mg, Eon Marchais, S, Stoppa Lyonnett, D, Andrieu, N, Sinilnikova, Om, Genesis, Mitchell G, James, Pa, Thompson, E, Kconfab, Swe, Brca, Marchetti, M, Verzeroli, C, Tartari, C, Capone, G, Putignano, Al, Genuardi, Maurizio, Medici, V, Marchi, I, Federico, M, Tognazzo, S, Matricardi, L, Agata, S, Dolcetti, R, Della Puppa, L, Cini, G, Gismondi, V, Viassolo, V, Perfumo, C, Mencarelli, Ma, Baldassarri, M, Peissel, B, Roversi, G, Silvestri, V, Rizzolo, P, Spina, F, Vivanet, C, Tibiletti, Mg, Caligo, Ma, Gambino, G, Tommasi, S, Pilato, B, Tondini, C, Corna, C, Bonanni, B, Barile, M, Osorio, A, Benitez, J, Balestrino, L, Ottini, L, Manoukian, S, Pierotti, Ma, Renieri, A, Varesco, L, Couch, Fj, Wang, X, Delivee, P, Hilbers, F, Van Asperen, Cj, Viel, A, Montagna, M, Cortesi, L, Diez, O, Balmana, J, Hauke, J, Scmutzler, Rk, Papi, L, Pujana, Ma, Lazaro, S, Falanga, A, Offit, K, Vijai, J, Campbell, I, Burwinkel, B, Kvist, A, Enrencrona, H, Mazoyer, S, Pizzamiglio, S, Verderio, P, Surralles, J, Rogan, Pk, Radice, P., and Genuardi, Maurizio (ORCID:0000-0002-7410-8351)
Abstract: Numerous genetic factors that influence breast cancer risk are known. However, approximately two-thirds of the overall familial risk remain unexplained. To determine whether some of the missing heritability is due to rare variants conferring high to moderate risk, we tested for an association between the c.5791C>T nonsense mutation (p.Arg1931*; rs144567652) in exon 22 of FANCM gene and breast cancer. An analysis of genotyping data from 8635 familial breast cancer cases and 6625 controls from different countries yielded an association between the c.5791C>T mutation and breast cancer risk [odds ratio (OR) = 3.93 (95% confidence interval (CI) = 1.28-12.11; P = 0.017)]. Moreover, we performed two meta-analyses of studies from countries with carriers in both cases and controls and of all available data. These analyses showed breast cancer associations with OR = 3.67 (95% CI = 1.04-12.87; P = 0.043) and OR = 3.33 (95% CI = 1.09-13.62; P = 0.032), respectively. Based on information theory-based prediction, we established that the mutation caused an out-of-frame deletion of exon 22, due to the creation of a binding site for the pre-mRNA processing protein hnRNP A1. Furthermore, genetic complementation analyses showed that the mutation influenced the DNA repair activity of the FANCM protein. In summary, we provide evidence for the first time showing that the common p.Arg1931* loss-of-function variant in FANCM is a risk factor for familial breast cancer.
Published: 2015

18. Towards a European consensus for reporting incidental findings during clinical NGS testing

Author: Hehir Kwa, Jy, Claustres, M, Hastings, Rj, Van Ravenswaaij Arts, C, Christenhusz, G, Genuardi, Maurizio, Melegh, B, Cambon Thomsen, A, Patsalis, P, Vermeesch, J, Cornel, Mc, Serle, B, Palotie, A, Capoluongo, Ettore Domenico, Peterlin, B, Estivill, X, Robinson, Pn, Genuardi, Maurizio (ORCID:0000-0002-7410-8351), Capoluongo, Ettore Domenico (ORCID:0000-0001-9872-0572), Hehir Kwa, Jy, Claustres, M, Hastings, Rj, Van Ravenswaaij Arts, C, Christenhusz, G, Genuardi, Maurizio, Melegh, B, Cambon Thomsen, A, Patsalis, P, Vermeesch, J, Cornel, Mc, Serle, B, Palotie, A, Capoluongo, Ettore Domenico, Peterlin, B, Estivill, X, Robinson, Pn, Genuardi, Maurizio (ORCID:0000-0002-7410-8351), and Capoluongo, Ettore Domenico (ORCID:0000-0001-9872-0572)
Abstract: In 2013, the American College of Medical Genetics (ACMG) examined the issue of incidental findings in whole exome and whole genome sequencing, and introduced recommendations to search for, evaluate and report medically actionable variants in a set of 56 genes. At a debate held during the 2014 European Society for Human Genetics Conference (ESHG) in Milan, Italy, the first author of that paper presented this view in a debate session that did not end with a conclusive vote from the mainly European audience for or against reporting back actionable incidental findings. In this meeting report, we elaborate on the discussions held during a special meeting hosted at the ESHG in 2013 from posing the question 'How to reach a (European) consensus on reporting incidental findings and unclassified variants in diagnostic next generation sequencing'. We ask whether an European consensus exists on the reporting of incidental findings in genome diagnostics, and present a series of key issues that require discussion at both a national and European level in order to develop recommendations for handling incidental findings and unclassified variants in line with the legal and cultural particularities of individual European member states.
Published: 2015

19. Involvement of MBD4 inactivation in mismatch repair-deficient tumorigenesis.

Author: Tricarico, Rossella, Cortellino, Salvatore, Riccio, Antonio, Jagmohan Changur, Shantie, Van Der Klift, Helen, Wijnen, Juul, Turner, David, Ventura, Andrea, Rovella, Valentina, Percesepe, Antonio, Lucci Cordisco, Emanuela, Radice, Paolo, Bertario, Lucio, Pedroni, Monica, Ponz De Leon, Maurizio, Mancuso, Pietro, Devarajan, Karthik, Cai, Kathy, Klein Szanto, Andrea, Neri, Giovanni, Moller, Pal, Viel, Alessandra, Genuardi, Maurizio, Fodde, Riccardo, Bellacosa, Alfonso, Lucci Cordisco, Emanuela (ORCID:0000-0002-6279-7604), Genuardi, Maurizio (ORCID:0000-0002-7410-8351), Tricarico, Rossella, Cortellino, Salvatore, Riccio, Antonio, Jagmohan Changur, Shantie, Van Der Klift, Helen, Wijnen, Juul, Turner, David, Ventura, Andrea, Rovella, Valentina, Percesepe, Antonio, Lucci Cordisco, Emanuela, Radice, Paolo, Bertario, Lucio, Pedroni, Monica, Ponz De Leon, Maurizio, Mancuso, Pietro, Devarajan, Karthik, Cai, Kathy, Klein Szanto, Andrea, Neri, Giovanni, Moller, Pal, Viel, Alessandra, Genuardi, Maurizio, Fodde, Riccardo, Bellacosa, Alfonso, Lucci Cordisco, Emanuela (ORCID:0000-0002-6279-7604), and Genuardi, Maurizio (ORCID:0000-0002-7410-8351)
Abstract: The DNA glycosylase gene MBD4 safeguards genomic stability at CpG sites and is frequently mutated at coding poly-A tracks in mismatch repair (MMR)-defective colorectal tumors (CRC). Mbd4 biallelic inactivation in mice provided conflicting results as to its role in tumorigenesis. Thus, it is unclear whether MBD4 alterations are only secondary to MMR defects without functional consequences or can contribute to the mutator phenotype. We investigated MBD4 variants in a large series of hereditary/familial and sporadic CRC cases. Whereas MBD4 frameshifts were only detected in tumors, missense variants were found in both normal and tumor DNA. In CRC with double-MBD4/MMR and single-MBD4 variants, transition mutation frequency was increased, indicating that MBD4 defects may affect the mutational landscape independently of MMR defect. Mbd4-deficient mice showed reduced survival when combined with Mlh1-/- genotype. Taken together, these data suggest that MBD4 inactivation may contribute to tumorigenesis, acting as a modifier of MMR-deficient cancer phenotype.
Published: 2015

20. Association of type and location of BRCA1 and BRCA2 mutations with risk of breast and ovarian cancer.

Author: Rebbeck Tr, Mitra N, Cimba, Consortium, Wan, F, Genuardi, Maurizio, Healey, S, Mcguffog, L, Mazoyer, S, Chenevix Trench, G, Laitman, Y, Easton, Df, Antoniou, Ac, Nathanson, Kl, Genuardi, Maurizio (ORCID:0000-0002-7410-8351), Rebbeck Tr, Mitra N, Cimba, Consortium, Wan, F, Genuardi, Maurizio, Healey, S, Mcguffog, L, Mazoyer, S, Chenevix Trench, G, Laitman, Y, Easton, Df, Antoniou, Ac, Nathanson, Kl, and Genuardi, Maurizio (ORCID:0000-0002-7410-8351)
Abstract: IMPORTANCE: Limited information about the relationship between specific mutations in BRCA1 or BRCA2 (BRCA1/2) and cancer risk exists. OBJECTIVE: To identify mutation-specific cancer risks for carriers of BRCA1/2. DESIGN, SETTING, AND PARTICIPANTS: Observational study of women who were ascertained between 1937 and 2011 (median, 1999) and found to carry disease-associated BRCA1 or BRCA2 mutations. The international sample comprised 19,581 carriers of BRCA1 mutations and 11,900 carriers of BRCA2 mutations from 55 centers in 33 countries on 6 continents. We estimated hazard ratios for breast and ovarian cancer based on mutation type, function, and nucleotide position. We also estimated RHR, the ratio of breast vs ovarian cancer hazard ratios. A value of RHR greater than 1 indicated elevated breast cancer risk; a value of RHR less than 1 indicated elevated ovarian cancer risk. EXPOSURES: Mutations of BRCA1 or BRCA2. MAIN OUTCOMES AND MEASURES: Breast and ovarian cancer risks. RESULTS: Among BRCA1 mutation carriers, 9052 women (46%) were diagnosed with breast cancer, 2317 (12%) with ovarian cancer, 1041 (5%) with breast and ovarian cancer, and 7171 (37%) without cancer. Among BRCA2 mutation carriers, 6180 women (52%) were diagnosed with breast cancer, 682 (6%) with ovarian cancer, 272 (2%) with breast and ovarian cancer, and 4766 (40%) without cancer. In BRCA1, we identified 3 breast cancer cluster regions (BCCRs) located at c.179 to c.505 (BCCR1; RHR = 1.46; 95% CI, 1.22-1.74; P = 2 × 10(-6)), c.4328 to c.4945 (BCCR2; RHR = 1.34; 95% CI, 1.01-1.78; P = .04), and c. 5261 to c.5563 (BCCR2', RHR = 1.38; 95% CI, 1.22-1.55; P = 6 × 10(-9)). We also identified an ovarian cancer cluster region (OCCR) from c.1380 to c.4062 (approximately exon 11) with RHR = 0.62 (95% CI, 0.56-0.70; P = 9 × 10(-17)). In BRCA2, we observed multiple BCCRs spanning c.1 to c.596 (BCCR1; RHR = 1.71; 95% CI, 1.06-2.78; P = .03), c.772 to c.1806 (BCCR1'; RHR = 1.63; 95% CI, 1.10-2.40; P = .01), and c.73
Published: 2015

21. Anti-miR21 oligonucleotide enhances chemosensitivity of T98G cell line to doxorubicin by inducing apoptosis

Author: Genuardi, Maurizio, Laura, Giunti, Martina Da, Ro, Serena, Vinci, Stefania, Gelmini, Anna Lisa, Iorio, Anna Maria, Buccoliero, Stefania, Cardellicchio, Francesca, Castiglione, Lorenzo, Genitori, Maurizio De, Martino, Sabrina, Giglio, Iacopo, Sardi, Genuardi, Maurizio (ORCID:0000-0002-7410-8351), Genuardi, Maurizio, Laura, Giunti, Martina Da, Ro, Serena, Vinci, Stefania, Gelmini, Anna Lisa, Iorio, Anna Maria, Buccoliero, Stefania, Cardellicchio, Francesca, Castiglione, Lorenzo, Genitori, Maurizio De, Martino, Sabrina, Giglio, Iacopo, Sardi, and Genuardi, Maurizio (ORCID:0000-0002-7410-8351)
Abstract: Various signal transduction pathways seem to be involved in chemoresistance mechanism of glioblastomas (GBMs). miR-21 is an important oncogenic miRNA which modulates drug resistance of tumor cells. We analyzed the expression of 5 miRNAs, previously found to be dysregulated in high grade gliomas, in 9 pediatric (pGBM) and in 5 adult (aGBM) GBMs. miR-21 was over-expressed, with a significant difference between pGBMs and aGBMs represented by a 4 times lower degree of expression in the pediatric compared to the adult series (p = 0.001). Doxorubicin (Dox) seems to be an effective anti-glioma agent with high antitumor activity also against glioblastoma stem cells. We therefore evaluated the chemosensitivity to Dox in 3 GBM cell lines (A172, U87MG and T98G). Dox had a cytotoxic effect after 48 h of treatment in A172 and U87MG, while T98G cells were resistant. TUNEL assay verified that Dox induced apoptosis in A172 and U87MG but not in T98G. miR-21 showed a low basal expression in treated cells and was over-expressed in untreated cells. To validate the possible association of miR-21 with drug resistance of T98G cells, we transfected anti-miR-21 inhibitor into the cells. The expression level of miR-21 was significantly lower in T98G transfected cells (than in the parental control cells). Transfected cells showed a high apoptotic rate compared to control after Dox treatment by TUNEL assay, suggesting that combined Dox and miR-21 inhibitor therapy can sensitize GBM resistant cells to anthracyclines by enhancing apoptosis.
Published: 2014

22. Characterization of the rs2802292 SNP identifies FOXO3A as a modifier locus predicting cancer risk in patients with PJS and PHTS hamartomatous polyposis syndromes.

Author: Forte, Giovanna, Grossi, Valentina, Celestini, Valentina, Lucisano, Giuseppe, Scardapane, Marco, Varvara, Dora, Patruno, Margherita, Bagnulo, Rosanna, Loconte, Daria, Giunti, Laura, Petracca, Antonio, Giglio, Sabrina, Genuardi, Maurizio, Pellegrini, Fabio, Resta, Nicoletta, Simone, Cristiano, Genuardi, Maurizio (ORCID:0000-0002-7410-8351), Forte, Giovanna, Grossi, Valentina, Celestini, Valentina, Lucisano, Giuseppe, Scardapane, Marco, Varvara, Dora, Patruno, Margherita, Bagnulo, Rosanna, Loconte, Daria, Giunti, Laura, Petracca, Antonio, Giglio, Sabrina, Genuardi, Maurizio, Pellegrini, Fabio, Resta, Nicoletta, Simone, Cristiano, and Genuardi, Maurizio (ORCID:0000-0002-7410-8351)
Abstract: BACKGROUND: Hamartomatous polyposis syndromes (HPS) are inherited conditions associated with high cancer risk. They include the Peutz-Jeghers and the PTEN hamartoma tumor syndromes, which are caused by mutations in the LKB1 and PTEN genes, respectively. Estimation of cancer risk is crucial in order to optimize surveillance, but no prognostic markers are currently available for these conditions. Our study relies on a 'signal transduction' hypothesis based on the crosstalk between LKB1/AMPK and PI3K/PTEN/Akt signaling at the level of the tumor suppressor protein FoxO3A. Interestingly, the FOXO3A rs2802292 G-allele was shown to be associated with longevity, reduced risk of aging-related diseases and increased expression of FoxO3A mRNA. METHODS: We typed rs2802292 in 150 HPS unrelated patients and characterized the expression of FoxO3A by quantitative PCR and immunoblot analysis in human intestinal cell lines. RESULTS: We found a significantly higher risk for malignancies in females and TT genotype carriers compared to patients having at least one G-allele. Subgroup analysis for each HPS syndrome revealed a G-allele-associated beneficial effect on cancer risk occurring mainly in males. Molecular characterization of human intestinal cell lines showed that the G-allele significantly correlated with increased basal expression of FoxO3A mRNA and protein. CONCLUSION: Our results suggest an inverse correlation between the protective allele (G) copy number and cancer risk, and might be useful to optimize surveillance in HPS patients. Further investigations are needed to confirm our hypothesis and to ascertain whether differences in therapeutic response exist across genotypes.
Published: 2014

23. MLH1 constitutional and somatic methylation in patients with MLH1 negative tumors fulfilling the revised Bethesda criteria.

Author: Genuardi, Maurizio, Crucianelli, Francesca, Tricarico, Rossella, Turchetti, Daniela, Gorelli, Greta, Gensini, Francesca, Sestini, Roberta, Giunti, Laura, Pedroni, Monica, Ponz De Leon, Maurizio, Civitelli, Serenella, Genuardi, Maurizio (ORCID:0000-0002-7410-8351), Genuardi, Maurizio, Crucianelli, Francesca, Tricarico, Rossella, Turchetti, Daniela, Gorelli, Greta, Gensini, Francesca, Sestini, Roberta, Giunti, Laura, Pedroni, Monica, Ponz De Leon, Maurizio, Civitelli, Serenella, and Genuardi, Maurizio (ORCID:0000-0002-7410-8351)
Abstract: Lynch syndrome (LS) is a tumor predisposing condition caused by constitutional defects in genes coding for components of the mismatch repair (MMR) apparatus. While hypermethylation of the promoter of the MMR gene MLH1 occurs in about 15% of colorectal cancer samples, it has also been observed as a constitutional alteration, in the absence of DNA sequence mutations, in a small number of LS patients. In order to obtain further insights on the phenotypic characteristics of MLH1 epimutation carriers, we investigated the somatic and constitutional MLH1 methylation status of 14 unrelated subjects with a suspicion of LS who were negative for MMR gene constitutional mutations and whose tumors did not express the MLH1 protein. A novel case of constitutional MLH1 epimutation was identified. This patient was affected with multiple primary tumors, including breast cancer, diagnosed starting from the age of 55 y. Investigation of her offspring by allele specific expression revealed that the epimutation was not stable across generations. We also found MLH1 hypermethylation in cancer samples from 4 additional patients who did not have evidence of constitutional defects. These patients had some characteristics of LS, namely early age at onset and/or positive family history, raising the possibility of genetic influences in the establishment of somatic MLH1 methylation.
Published: 2014

24. Application of a 5-tiered scheme for standardized classification of 2,360 unique mismatch repair gene variants in the InSiGHT locus-specific database.

Author: Genuardi, Maurizio, Spurdle, Ab, Plazzer, Jp, Greenblatt, M, Akagi, K, Al Mulla, F, Bapat, B, Bernstein, I, Capellá, G, Den Dunnen, Jt, Du Sart, D, Fabre, A, Farrell, Mp, Farrington, Sm, Frayling, Im, Frebourg, T, Goldgar, De, Heinen, Cd, Holinski Feder, E, Kohonen Corish, M, Robinson, Kl, Leung, Sy, Martins, A, Moller, P, Morak, M, Nystrom, M, Peltomaki, P, Pineda, M, Qi, M, Ramesar, R, Rasmussen, Lj, Royer Pokora, B, Scott, Rj, Sijmons, R, Tavtigian, Sv, Tops, Cm, Weber, T, Wijnen, J, Woods, Mo, Macrae, F, Thompson, Ba, Genuardi, Maurizio (ORCID:0000-0002-7410-8351), Genuardi, Maurizio, Spurdle, Ab, Plazzer, Jp, Greenblatt, M, Akagi, K, Al Mulla, F, Bapat, B, Bernstein, I, Capellá, G, Den Dunnen, Jt, Du Sart, D, Fabre, A, Farrell, Mp, Farrington, Sm, Frayling, Im, Frebourg, T, Goldgar, De, Heinen, Cd, Holinski Feder, E, Kohonen Corish, M, Robinson, Kl, Leung, Sy, Martins, A, Moller, P, Morak, M, Nystrom, M, Peltomaki, P, Pineda, M, Qi, M, Ramesar, R, Rasmussen, Lj, Royer Pokora, B, Scott, Rj, Sijmons, R, Tavtigian, Sv, Tops, Cm, Weber, T, Wijnen, J, Woods, Mo, Macrae, F, Thompson, Ba, and Genuardi, Maurizio (ORCID:0000-0002-7410-8351)
Abstract: The clinical classification of hereditary sequence variants identified in disease-related genes directly affects clinical management of patients and their relatives. The International Society for Gastrointestinal Hereditary Tumours (InSiGHT) undertook a collaborative effort to develop, test and apply a standardized classification scheme to constitutional variants in the Lynch syndrome-associated genes MLH1, MSH2, MSH6 and PMS2. Unpublished data submission was encouraged to assist in variant classification and was recognized through microattribution. The scheme was refined by multidisciplinary expert committee review of the clinical and functional data available for variants, applied to 2,360 sequence alterations, and disseminated online. Assessment using validated criteria altered classifications for 66% of 12,006 database entries. Clinical recommendations based on transparent evaluation are now possible for 1,370 variants that were not obviously protein truncating from nomenclature. This large-scale endeavor will facilitate the consistent management of families suspected to have Lynch syndrome and demonstrates the value of multidisciplinary collaboration in the curation and classification of variants in public locus-specific databases.
Published: 2014

25. Revised guidelines for the clinical management of Lynch syndrome (HNPCC): recommendations by a group of European experts

Author: Vasen, Hf, Blanco, I, Aktan Collan, K, Gopie, Jp, Alonso, A, Aretz, S, Bernstein, I, Bertario, L, Burn, J, Capella, G, Colas, C, Engel, C, Frayling, Im, Genuardi, Maurizio, Heinimann, K, Hes, Fj, Hodgson, Sv, Karagiannis, Ja, Lalloo, F, Lindblom, A, Mecklin, Jp, Møller, P, Myrhoj, T, Nagengast, Fm, Parc, Y, Ponz De Leon, M, Renkonen Sinisalo, L, Sampson, Jr, Stormorken, A, Sijmons, Rh, Tejpar, S, Thomas, Herbert, Rahner, Wijnen, Jt, Järvinen, Hj, Möslein, G., Genuardi, Maurizio (ORCID:0000-0002-7410-8351), Vasen, Hf, Blanco, I, Aktan Collan, K, Gopie, Jp, Alonso, A, Aretz, S, Bernstein, I, Bertario, L, Burn, J, Capella, G, Colas, C, Engel, C, Frayling, Im, Genuardi, Maurizio, Heinimann, K, Hes, Fj, Hodgson, Sv, Karagiannis, Ja, Lalloo, F, Lindblom, A, Mecklin, Jp, Møller, P, Myrhoj, T, Nagengast, Fm, Parc, Y, Ponz De Leon, M, Renkonen Sinisalo, L, Sampson, Jr, Stormorken, A, Sijmons, Rh, Tejpar, S, Thomas, Herbert, Rahner, Wijnen, Jt, Järvinen, Hj, Möslein, G., and Genuardi, Maurizio (ORCID:0000-0002-7410-8351)
Abstract: Lynch syndrome (LS) is characterised by the development of colorectal cancer, endometrial cancer and various other cancers, and is caused by a mutation in one of the mismatch repair genes: MLH1, MSH2, MSH6 or PMS2. In 2007, a group of European experts (the Mallorca group) published guidelines for the clinical management of LS. Since then substantial new information has become available necessitating an update of the guidelines. In 2011 and 2012 workshops were organised in Palma de Mallorca. A total of 35 specialists from 13 countries participated in the meetings. The first step was to formulate important clinical questions. Then a systematic literature search was performed using the Pubmed database and manual searches of relevant articles. During the workshops the outcome of the literature search was discussed in detail. The guidelines described in this paper may be helpful for the appropriate management of families with LS. Prospective controlled studies should be undertaken to improve further the care of these families.
Published: 2013

26. MUTYH-associated polyposis (MAP): evidence for the origin of the common European mutations p.Tyr179Cys and p.Gly396Asp by founder events.

Author: Genuardi, Maurizio, Aretz, S, Tricarico, R, Papi, L, Spier, L, Pin, E, Horpaopan, S, Lucci Cordisco, L, Pedroni, M, Stienen, D, Gentile, A, Panza, A, Piepoli, A, De Leon, Mp, Friedl, W, Viel, A., Genuardi, Maurizio (ORCID:0000-0002-7410-8351), Genuardi, Maurizio, Aretz, S, Tricarico, R, Papi, L, Spier, L, Pin, E, Horpaopan, S, Lucci Cordisco, L, Pedroni, M, Stienen, D, Gentile, A, Panza, A, Piepoli, A, De Leon, Mp, Friedl, W, Viel, A., and Genuardi, Maurizio (ORCID:0000-0002-7410-8351)
Abstract: MUTYH-associated polyposis (MAP) is an autosomal recessive adenomatous polyposis caused by biallelic germline mutations of the base-excision-repair gene MUTYH. In MAP patients of European origin, the combined allele frequency of the mutations p.Tyr179Cys and p.Gly396Asp ranges between 50 and 82%, while these mutations have not been identified in Far Eastern Asian populations, supporting the hypothesis that a founder effect has occurred at some point in European history. To investigate the natural history of the two common European MUTYH alleles, we genotyped six gene-flanking microsatellite markers in 80 unrelated Italian and German MAP patients segregating one or both mutations and calculated their age in generations (g) by using DMLE+2.2 software. Three distinct common haplotypes, one for p.Tyr179Cys and two for p.Gly396Asp, were identified. Estimated mutation ages were 305 g (95% CS: 271-418) for p.Tyr179Cys and 350 g (95% CS: 313-435) for p.Gly396Asp. These results provide evidence for strong founder effects and suggest that the p.Tyr179Cys and p.Gly396Asp mutations derive from ancestors who lived between 5-8 thousand years and 6-9 thousand years B.C., respectively
Published: 2013

27. Encomium: Giovanni Neri--polyhedral and down-to-earth mentor.

Author: Genuardi, Maurizio, Gurrieri, Fiorella, Zollino, M., Genuardi, Maurizio (ORCID:0000-0002-7410-8351), Gurrieri, Fiorella (ORCID:0000-0002-6775-5972), Genuardi, Maurizio, Gurrieri, Fiorella, Zollino, M., Genuardi, Maurizio (ORCID:0000-0002-7410-8351), and Gurrieri, Fiorella (ORCID:0000-0002-6775-5972)
Abstract: I've never been certain whether the moral of the Icarus story should only be, as is generally accepted, "don't try to fly too high" or whether is might also be thougt of as "forget the was and feathers, and do a bette job on the wings".
Published: 2013

28. The growing complexity of the intestinal polyposis syndromes.

Author: Lucci Cordisco, Emanuela, Risio, M, Venesio, T, Genuardi, Maurizio, Lucci Cordisco, Emanuela (ORCID:0000-0002-6279-7604), Genuardi, Maurizio (ORCID:0000-0002-7410-8351), Lucci Cordisco, Emanuela, Risio, M, Venesio, T, Genuardi, Maurizio, Lucci Cordisco, Emanuela (ORCID:0000-0002-6279-7604), and Genuardi, Maurizio (ORCID:0000-0002-7410-8351)
Abstract: Familial adenomatous polyposis has been the first form of inherited intestinal polyposis to be recognized. For a long time it has been considered the main polyposis syndrome, associated with an easily recognizable phenotype, with a marginal role attributed to a few very rare hamartomatous conditions. More recently, it has been gradually demonstrated that the intestinal polyposes encompass a range of conditions within a wide spectrum of disease severity, polyp histology, and extraintestinal manifestations. A growing number of genes and phenotypes has been identified, and heterogeneity of somatic molecular pathways underlying epithelial transformation in different syndromes and associated tumors has been documented. Increasing knowledge on the molecular bases and more widespread use of genetic tests has shown phenotypic overlaps between conditions that were previously considered distinct, highlighting diagnostic difficulties. With the advent of next generation sequencing, the diagnosis and the classification of these syndromes will be progressively based more on genetic testing results. However, the phenotypic variability documented among patients with mutations in the same genes cannot be fully explained by different expressivity, indicating a role for as yet unknown modifying factors. Until the latter will be identified, the management of patients with polyposis syndromes should be guided by both clinical and genetic findings.
Published: 2013

29. Clinical and genetic study of a family with a paternally inherited 15q11-q13 duplication.

Author: Genuardi, Maurizio, Marini, C, Cecconi, A, Contini, E, Pantaleo, M, Metitieri, T, Guarducci, S, Giglio, S, Guerrini, R., Genuardi, Maurizio (ORCID:0000-0002-7410-8351), Genuardi, Maurizio, Marini, C, Cecconi, A, Contini, E, Pantaleo, M, Metitieri, T, Guarducci, S, Giglio, S, Guerrini, R., and Genuardi, Maurizio (ORCID:0000-0002-7410-8351)
Abstract: Interstitial chromosome 15q11-q13 duplications are associated with developmental delay, behavioral problems and additional manifestations, including epilepsy. In most affected individuals the duplicated chromosome is maternally derived, whereas paternal inheritance is more often associated with a normal phenotype. Seizures have not been described in patients with paternal dup 15q11-q13. We describe a family with five individuals in three generations with a paternally-inherited 15q11-q13 duplication, four of whom exhibited abnormal phenotypic characteristics, including seizures. The 18-year-old female proband presented with moderate intellectual disability, obesity, and epilepsy. Her brother manifested learning disability and behavioral problems. They both inherited the 15q11-q13 dup from their father who had a normal phenotype. Their paternal uncle and grandfather also had the duplication and were reported to have had seizures. Array-CGH and MLPA analyses showed that the duplication included the TUBGCP5, CYFIP1, MKRN3, MAGEL2, NDN, SNRPN, UBE3A, ATP10A, GABRB3, GABRA5, GABRG3, and OCA2 genes. This report provides evidence for intrafamilial phenotypic variability of paternal dup 15q11-q13, ranging from normal to intellectual disability and seizures, and potentially expanding the phenotype of paternal 15q11-q13 interstitial duplications.
Published: 2013

30. Clinical and Genetic Study of a Family With a Paternally Inherited 15q11-q13 Duplication

Author: Marini, C, Cecconi, A, Contini, E, Pantaleo, M, Metitieri, T, Guarducci, S, Giglio, S, Guerrini, R, Genuardi, Maurizio, Genuardi, Maurizio (ORCID:0000-0002-7410-8351), Marini, C, Cecconi, A, Contini, E, Pantaleo, M, Metitieri, T, Guarducci, S, Giglio, S, Guerrini, R, Genuardi, Maurizio, and Genuardi, Maurizio (ORCID:0000-0002-7410-8351)
Abstract: Interstitial chromosome 15q11-q13 duplications are associated with developmental delay, behavioral problems and additional manifestations, including epilepsy. In most affected individuals the duplicated chromosome is maternally derived, whereas paternal inheritance is more often associated with a normal phenotype. Seizures have not been described in patients with paternal dup 15q11-q13. We describe a family with five individuals in three generations with a paternally-inherited 15q11-q13 duplication, four of whom exhibited abnormal phenotypic characteristics, including seizures. The 18-year-old female proband presented with moderate intellectual disability, obesity, and epilepsy. Her brother manifested learning disability and behavioral problems. They both inherited the 15q11-q13 dup from their father who had a normal phenotype. Their paternal uncle and grandfather also had the duplication and were reported to have had seizures. Array-CGH and MLPA analyses showed that the duplication included the TUBGCP5, CYFIP1, MKRN3, MAGEL2, NDN, SNRPN, UBE3A, ATP10A, GABRB3, GABRA5, GABRG3, and OCA2 genes. This report provides evidence for intrafamilial phenotypic variability of paternal dup 15q11-q13, ranging from normal to intellectual disability and seizures, and potentially expanding the phenotype of paternal 15q11-q13 interstitial duplications. (C) 2013 Wiley Periodicals, Inc.
Published: 2013

31. The policy of public health genomics in Italy

Author: Simone, B, Mazzucco, W, Gualano, M, Agodi, A, Coviello, D, Bricarelli, F, Dallapiccola, B, Di Maria, E, Federici, A, Genuardi, Maurizio, Varesco, L, Ricciardi, W, Boccia, Stefania, Genuardi, Maurizio (ORCID:0000-0002-7410-8351), Boccia, S. (ORCID:0000-0002-1864-749X), Simone, B, Mazzucco, W, Gualano, M, Agodi, A, Coviello, D, Bricarelli, F, Dallapiccola, B, Di Maria, E, Federici, A, Genuardi, Maurizio, Varesco, L, Ricciardi, W, Boccia, Stefania, Genuardi, Maurizio (ORCID:0000-0002-7410-8351), and Boccia, S. (ORCID:0000-0002-1864-749X)
Abstract: Italy has a monitoring system for genetic testing, consisting in a periodic census of clinical and laboratory activities performed in the country. The experience is limited, however, concerning the translation of genomic testing for complex diseases into clinical practice. For the first time the Italian Ministry of Health has introduced a policy strategic plan on genomics and predictive medicine within the 2010-2012 National Prevention Plan. This achievement was supported by the Italian Network for Public Health Genomics (GENISAP) and will likely contribute to the integration of public health genomics into health care in the country. Our experience might be of interest not only in Italy, but in other high-income countries, struggling to keep a healthy economy and healthy citizens. (C) 2013 Elsevier Ireland Ltd. All rights reserved.
Published: 2013

32. Duodenal carcinoma in a 37-year-old man with Cowden/Bannayan syndrome

Author: De Leon, M, Di Gregorio, C, Giunti, L, Roncucci, L, Pedroni, M, Tinca, A, Crucianelli, F, Tricarico, R, Genuardi, Maurizio, Genuardi, Maurizio (ORCID:0000-0002-7410-8351), De Leon, M, Di Gregorio, C, Giunti, L, Roncucci, L, Pedroni, M, Tinca, A, Crucianelli, F, Tricarico, R, Genuardi, Maurizio, and Genuardi, Maurizio (ORCID:0000-0002-7410-8351)
Abstract: A 37-year-old man was hospitalised because of anaemia and fatigue due to an infiltrating adenocarcinoma of the Treitz angle (duodenum), together with gastric, duodenal and colorectal polyps. After the operation, removal of colorectal lesions revealed the presence of ganglioneuromatosis of the large bowel. Further investigations showed lack of MLH1 protein expression and microsatellite instability in the duodenal neoplasm, while the gene was normally expressed in the polyps. MLH1 sequence and Multiple Ligation-dependent Probes Amplification analysis (from constitutional DNA) were normal. Analysis of the PTEN gene revealed the presence of a constitutional mutation (c.510 T>A; p.Ser170Arg) which had been associated with the Cowden phenotype. Further detailed clinical investigations revealed macrocephaly (63 cm), melanotic spots of the penis, small angiomas, millimetric trichilemmomas in the nose and multiple lipomas, which led to the diagnosis of Cowden/Bannayan disease. The unusual appearance of a duodenal carcinoma as the first symptom rendered the identification of the syndrome extremely difficult. (C) 2012 Editrice Gastroenterologica Italiana S.r.l. Published by Elsevier Ltd. All rights reserved.
Published: 2013

33. Gene variants of unknown clinical significance in Lynch syndrome. An introduction for clinicians

Author: Sijmons, R, Greenblatt, M, Genuardi, Maurizio, Genuardi, Maurizio (ORCID:0000-0002-7410-8351), Sijmons, R, Greenblatt, M, Genuardi, Maurizio, and Genuardi, Maurizio (ORCID:0000-0002-7410-8351)
Abstract: Clinicians referring patients for genetic testing for Lynch syndrome will sooner or later receive results for DNA Mismatch Repair (MMR) genes reporting DNA changes that are unclear from a clinical point of view. These changes are referred to as variants of unknown, or unclear, clinical significance (VUS). In contrast to clearly pathogenic mutations, VUS do not firmly diagnose Lynch syndrome at the molecular level and cannot be used to identify with certainty any of the patients' asymptomatic relatives as Lynch syndrome mutation carriers. The International database that collects MMR gene variants (www.insight-group.org/mutations) already lists more than 1,000 different VUSs and these variants are likely the tip of the iceberg. This paper aims at introducing non-geneticist clinicians to the topic of clinical MMR gene variant interpretation. Many lines of evidence are being used to classify VUS. Some are already familiar to clinicians and others may be less familiar but are expected to become important in clinical genetics in the coming years. Clinicians can play an important role in collecting the data needed to interpret the MMR variants detected in their patients.
Published: 2013

34. Clinical utility gene card for: MUTYH-associated polyposis (MAP), Autosomal recessive colorectal adenomatous polyposis, Multiple colorectal adenomas, Multiple adenomatous polyps (MAP) - update 2012

Author: Aretz, S, Genuardi, Maurizio, Hes, F., Genuardi, Maurizio (ORCID:0000-0002-7410-8351), Aretz, S, Genuardi, Maurizio, Hes, F., and Genuardi, Maurizio (ORCID:0000-0002-7410-8351)
Abstract: MUTYH-associated polyposis (MAP), Autosomal recessive colorectal adenomatous polyposis, Multiple colorectal adenomas, Multiple adenomatous polyps (MAP).
Published: 2013

35. MUTYH c.933+3A > C, associated with a severely impaired gene expression, is the first Italian founder mutation in MUTYH-Associated Polyposis

Author: Pin, E, Pastrello, C, Tricarico, R, Papi, L, Quaia, M, Fornasarig, M, Carnevali, I, Oliani, C, Fornasin, A, Agostini, M, Maestro, R, Barana, D, Aretz, S, Genuardi, Maurizio, Viel, A., Genuardi, Maurizio (ORCID:0000-0002-7410-8351), Pin, E, Pastrello, C, Tricarico, R, Papi, L, Quaia, M, Fornasarig, M, Carnevali, I, Oliani, C, Fornasin, A, Agostini, M, Maestro, R, Barana, D, Aretz, S, Genuardi, Maurizio, Viel, A., and Genuardi, Maurizio (ORCID:0000-0002-7410-8351)
Abstract: MUTYH variants are differently distributed in geographical areas of the world. In MUTYH-associated polyposis (MAP) patients from North-Eastern Italy, c.933+3A>C (IVS10+3A>C), a transversion causing an aberrant splicing process, accounts for nearly 1/5 of all mutations. The aim of this study was to verify whether its high frequency in North-Eastern Italy is due to a founder effect and to clarify its impact on MUTYH transcripts and protein. Haplotype analysis and age estimate performed on members of eleven Italian MAP families and cancer-free controls provided evidence that c.933+3A>C is a founder mutation originated about 83 generations ago. In addition, the Italian haplotype associated with the c.933+3A>C was also found in German families segregating the same mutation, indicating it had a common origin in Western Europe. Altogether c.933+3A>C and the two common Caucasian mutations p. Tyr179Cys and p.Gly396Asp represent about 60% of MUTYH alterations in MAP patients from North-Eastern Italy, suggesting the opportunity to perform targeted molecular screening for these variants in the diagnostic setting. Expression analyses performed on lymphoblastoid cell lines supported the notion that MUTYH c.933+3A>C alters splicing causing the synthesis of a non functional protein. However, some primary transcripts escape aberrant splicing, producing traces of full-length transcript and wild-type protein in a homozygote; this is in agreement with clinical findings that suggest a relatively mild phenotypic effect for this mutation. Overall, these data, that demonstrate a founder effect and further elucidate the splicing alterations caused by the MUTYH c.933+3A>C mutation, have important implications for genetic counseling and molecular diagnosis of MAP.
Published: 2013

36. Identification of a BRCA2-specific modifier locus at 6p24 related to breast cancer risk

Author: Genuardi, Maurizio, Vijai, J, Dicks, E, Soucy, P, Sinilnikova, Om, Pankratz, V, Wang, X, Eldridge, Rc, Tessier, Dc, Vincent, D, Bacot, F, Hogervorst, Fb, Peock, S, Stoppa Lyonnet, D, Barile, M, Alonso, Mr, Kirchhoff, T, Mcguffog, L, Barrowdale, D, Dunning, Am, Lee, A, Klein, Rj, Gaudet, Mm, Kuchenbaecker, Kb, Dennis, J, Healey, S., Genuardi, Maurizio (ORCID:0000-0002-7410-8351), Genuardi, Maurizio, Vijai, J, Dicks, E, Soucy, P, Sinilnikova, Om, Pankratz, V, Wang, X, Eldridge, Rc, Tessier, Dc, Vincent, D, Bacot, F, Hogervorst, Fb, Peock, S, Stoppa Lyonnet, D, Barile, M, Alonso, Mr, Kirchhoff, T, Mcguffog, L, Barrowdale, D, Dunning, Am, Lee, A, Klein, Rj, Gaudet, Mm, Kuchenbaecker, Kb, Dennis, J, Healey, S., and Genuardi, Maurizio (ORCID:0000-0002-7410-8351)
Abstract: Common genetic variants contribute to the observed variation in breast cancer risk for BRCA2 mutation carriers; those known to date have all been found through population-based genome-wide association studies (GWAS). To comprehensively identify breast cancer risk modifying loci for BRCA2 mutation carriers, we conducted a deep replication of an ongoing GWAS discovery study. Using the ranked P-values of the breast cancer associations with the imputed genotype of 1.4 M SNPs, 19,029 SNPs were selected and designed for inclusion on a custom Illumina array that included a total of 211,155 SNPs as part of a multi-consortial project. DNA samples from 3,881 breast cancer affected and 4,330 unaffected BRCA2 mutation carriers from 47 studies belonging to the Consortium of Investigators of Modifiers of BRCA1/2 were genotyped and available for analysis. We replicated previously reported breast cancer susceptibility alleles in these BRCA2 mutation carriers and for several regions (including FGFR2, MAP3K1, CDKN2A/B, and PTHLH) identified SNPs that have stronger evidence of association than those previously published. We also identified a novel susceptibility allele at 6p24 that was inversely associated with risk in BRCA2 mutation carriers (rs9348512; per allele HR = 0.85, 95% CI 0.80-0.90, P = 3.9 × 10(-8)). This SNP was not associated with breast cancer risk either in the general population or in BRCA1 mutation carriers. The locus lies within a region containing TFAP2A, which encodes a transcriptional activation protein that interacts with several tumor suppressor genes. This report identifies the first breast cancer risk locus specific to a BRCA2 mutation background. This comprehensive update of novel and previously reported breast cancer susceptibility loci contributes to the establishment of a panel of SNPs that modify breast cancer risk in BRCA2 mutation carriers. This panel may have clinical utility for women with BRCA2 mutations weighing options for medical prevention of br
Published: 2013

37. Gene variants of unknown clinical significance in Lynch syndrome. An introduction for clinicians.

Author: Genuardi, Maurizio, Sijmons, Rh, Greenblatt, Ms, Genuardi, Maurizio (ORCID:0000-0002-7410-8351), Genuardi, Maurizio, Sijmons, Rh, Greenblatt, Ms, and Genuardi, Maurizio (ORCID:0000-0002-7410-8351)
Abstract: Clinicians referring patients for genetic testing for Lynch syndrome will sooner or later receive results for DNA Mismatch Repair (MMR) genes reporting DNA changes that are unclear from a clinical point of view. These changes are referred to as variants of unknown, or unclear, clinical significance (VUS). In contrast to clearly pathogenic mutations, VUS do not firmly diagnose Lynch syndrome at the molecular level and cannot be used to identify with certainty any of the patients' asymptomatic relatives as Lynch syndrome mutation carriers. The International database that collects MMR gene variants ( www.insight-group.org/mutations ) already lists more than 1,000 different VUSs and these variants are likely the tip of the iceberg. This paper aims at introducing non-geneticist clinicians to the topic of clinical MMR gene variant interpretation. Many lines of evidence are being used to classify VUS. Some are already familiar to clinicians and others may be less familiar but are expected to become important in clinical genetics in the coming years. Clinicians can play an important role in collecting the data needed to interpret the MMR variants detected in their patients.
Published: 2013

38. The growing complexity of the intestinal polyposis syndromes

Author: Lucci Cordisco, Emanuela, Risio, M, Venesio, T, Genuardi, Maurizio, Lucci Cordisco, Emanuela (ORCID:0000-0002-6279-7604), Genuardi, Maurizio (ORCID:0000-0002-7410-8351), Lucci Cordisco, Emanuela, Risio, M, Venesio, T, Genuardi, Maurizio, Lucci Cordisco, Emanuela (ORCID:0000-0002-6279-7604), and Genuardi, Maurizio (ORCID:0000-0002-7410-8351)
Abstract: Familial adenomatous polyposis has been the first form of inherited intestinal polyposis to be recognized. For a long time it has been considered the main polyposis syndrome, associated with an easily recognizable phenotype, with a marginal role attributed to a few very rare hamartomatous conditions. More recently, it has been gradually demonstrated that the intestinal polyposes encompass a range of conditions within a wide spectrum of disease severity, polyp histology, and extraintestinal manifestations. A growing number of genes and phenotypes has been identified, and heterogeneity of somatic molecular pathways underlying epithelial transformation in different syndromes and associated tumors has been documented. Increasing knowledge on the molecular bases and more widespread use of genetic tests has shown phenotypic overlaps between conditions that were previously considered distinct, highlighting diagnostic difficulties. With the advent of next generation sequencing, the diagnosis and the classification of these syndromes will be progressively based more on genetic testing results. However, the phenotypic variability documented among patients with mutations in the same genes cannot be fully explained by different expressivity, indicating a role for as yet unknown modifying factors. Until the latter will be identified, the management of patients with polyposis syndromes should be guided by both clinical and genetic findings.
Published: 2013

39. Encomium: Giovanni Neri--polyhedral and down-to-earth mentor

Author: Genuardi, Maurizio, Gurrieri, Fiorella, Zollino, Marcella, Genuardi, Maurizio (ORCID:0000-0002-7410-8351), Gurrieri, Fiorella (ORCID:0000-0002-6775-5972), Zollino, Marcella (ORCID:0000-0003-4871-9519), Genuardi, Maurizio, Gurrieri, Fiorella, Zollino, Marcella, Genuardi, Maurizio (ORCID:0000-0002-7410-8351), Gurrieri, Fiorella (ORCID:0000-0002-6775-5972), and Zollino, Marcella (ORCID:0000-0003-4871-9519)
Abstract: N/A
Published: 2013

40. The policy of public health genomics in Italy

Author: Simone, Benedetto, Mazzucco, Walter, Gualano, Mr, Agodi, A, Coviello, Domenico, Dagna Bricarelli, F, Dallapiccola, B, Di Maria, E, Federici, A, Genuardi, Maurizio, Varesco, L, Ricciardi, Walter, Boccia, Stefania, Genuardi, Maurizio (ORCID:0000-0002-7410-8351), Ricciardi, Gualtiero (ORCID:0000-0002-5655-688X), Boccia, Stefania (ORCID:0000-0002-1864-749X), Simone, Benedetto, Mazzucco, Walter, Gualano, Mr, Agodi, A, Coviello, Domenico, Dagna Bricarelli, F, Dallapiccola, B, Di Maria, E, Federici, A, Genuardi, Maurizio, Varesco, L, Ricciardi, Walter, Boccia, Stefania, Genuardi, Maurizio (ORCID:0000-0002-7410-8351), Ricciardi, Gualtiero (ORCID:0000-0002-5655-688X), and Boccia, Stefania (ORCID:0000-0002-1864-749X)
Abstract: Italy has a monitoring system for genetic testing, consisting in a periodic census of clinical and laboratory activities performed in the country. The experience is limited, however, concerning the translation of genomic testing for complex diseases into clinical practice. For the first time the Italian Ministry of Health has introduced a policy strategic plan on genomics and predictive medicine within the 2010-2012 National Prevention Plan. This achievement was supported by the Italian Network for Public Health Genomics (GENISAP) and will likely contribute to the integration of public health genomics into health care in the country. Our experience might be of interest not only in Italy, but in other high-income countries, struggling to keep a healthy economy and healthy citizens.
Published: 2013

41. MUTYH-associated polyposis (MAP): evidence for the origin of the common European mutations p.Tyr179Cys and p.Gly396Asp by founder events

Author: Aretz, S, Tricarico, R, Papi, L, Spier, I, Pin, E, Horpaopan, S, Lucci Cordisco, Emanuela, Pedroni, M, Stienen, D, Gentile, A, Panza, A, Piepoli, A, De Leon, Mp, Friedl, W, Viel, A, Genuardi, Maurizio, Lucci Cordisco, Emanuela (ORCID:0000-0002-6279-7604), Genuardi, Maurizio (ORCID:0000-0002-7410-8351), Aretz, S, Tricarico, R, Papi, L, Spier, I, Pin, E, Horpaopan, S, Lucci Cordisco, Emanuela, Pedroni, M, Stienen, D, Gentile, A, Panza, A, Piepoli, A, De Leon, Mp, Friedl, W, Viel, A, Genuardi, Maurizio, Lucci Cordisco, Emanuela (ORCID:0000-0002-6279-7604), and Genuardi, Maurizio (ORCID:0000-0002-7410-8351)
Abstract: MUTYH-associated polyposis (MAP) is an autosomal recessive adenomatous polyposis caused by biallelic germline mutations of the base-excision-repair gene MUTYH. In MAP patients of European origin, the combined allele frequency of the mutations p.Tyr179Cys and p.Gly396Asp ranges between 50 and 82%, while these mutations have not been identified in Far Eastern Asian populations, supporting the hypothesis that a founder effect has occurred at some point in European history. To investigate the natural history of the two common European MUTYH alleles, we genotyped six gene-flanking microsatellite markers in 80 unrelated Italian and German MAP patients segregating one or both mutations and calculated their age in generations (g) by using DMLE+2.2 software. Three distinct common haplotypes, one for p.Tyr179Cys and two for p.Gly396Asp, were identified. Estimated mutation ages were 305 g (95% CS: 271-418) for p.Tyr179Cys and 350 g (95% CS: 313-435) for p.Gly396Asp. These results provide evidence for strong founder effects and suggest that the p.Tyr179Cys and p.Gly396Asp mutations derive from ancestors who lived between 5-8 thousand years and 6-9 thousand years B.C., respectively.European Journal of Human Genetics advance online publication, 30 January 2013; doi:10.1038/ejhg.2012.309.
Published: 2013

42. Cancer risk associated with STK11/LKB1 germline mutations in Peutz-Jeghers syndrome patients: Results of an Italian multicenter study

Author: Resta, N, Pierannunzio, D, Lenato, Gm, Stella, A, Capocaccia, R, Bagnulo, R, Lastella, P, Susca, Fc, Bozzao, C, Loconte, Dc, Sabbà, C, Urso, E, Sala, P, Fornasarig, M, Grammatico, P, Piepoli, A, Host, C, Turchetti, D, Viel, A, Memo, L, Giunti, L, Stigliano, V, Varesco, L, Bertario, L, Genuardi, Maurizio, Lucci Cordisco, Emanuela, Tibiletti, Mg, Di Gregorio, C, Andriulli, A, Ponz De Leon, M., Genuardi, Maurizio (ORCID:0000-0002-7410-8351), Lucci Cordisco, Emanuela (ORCID:0000-0002-6279-7604), Resta, N, Pierannunzio, D, Lenato, Gm, Stella, A, Capocaccia, R, Bagnulo, R, Lastella, P, Susca, Fc, Bozzao, C, Loconte, Dc, Sabbà, C, Urso, E, Sala, P, Fornasarig, M, Grammatico, P, Piepoli, A, Host, C, Turchetti, D, Viel, A, Memo, L, Giunti, L, Stigliano, V, Varesco, L, Bertario, L, Genuardi, Maurizio, Lucci Cordisco, Emanuela, Tibiletti, Mg, Di Gregorio, C, Andriulli, A, Ponz De Leon, M., Genuardi, Maurizio (ORCID:0000-0002-7410-8351), and Lucci Cordisco, Emanuela (ORCID:0000-0002-6279-7604)
Abstract: BACKGROUND: Germline mutations in the STK11/LKB1 gene cause Peutz-Jeghers syndrome, an autosomal-dominantly inherited condition characterized by mucocutaneous pigmentation, hamartomatous gastrointestinal polyposis, and an increased risk for various malignancies. We here report the results of the first Italian collaborative study on Peutz-Jeghers syndrome. AIMS: To assess cancer risks in a large homogenous cohort of patients with Peutz-Jeghers syndrome, carrying, in large majority, an identified STK11/LKB1 mutation. METHODS: One-hundred and nineteen patients with Peutz-Jeghers syndrome, ascertained in sixteen different Italian centres, were enrolled in a retrospective cohort study. Relative and cumulative cancer risks and genotype-phenotype correlations were evaluated. RESULTS: 36 malignant tumours were found in 31/119 (29 STK11/LKB1 mutation carriers) patients. The mean age at first cancer diagnosis was 41 years. The relative overall cancer risk was 15.1 with a significantly higher risk (p<0.001) in females (22.0) than in males (8.6). Highly increased relative risks were present for gastrointestinal (126.2) and gynaecological cancers (27.7), in particular for pancreatic (139.7) and cervical cancer (55.6). The Kaplan-Meier estimates for overall cumulative cancer risks were 20%, 43%, 71%, and 89%, at age 40, 50, 60 and 65 years, respectively. CONCLUSION: Peutz-Jeghers syndrome entails markedly elevated cancer risks, mainly for pancreatic and cervical cancers. This study provides a helpful reference for improving current surveillance protocols.
Published: 2013

43. La Genomica in Sanità Pubblica. Sintesi delle evidenze e delle conoscenze disponibili sull’utilizzo della genomica ai fini della prevenzione.

Author: Boccia, Stefania, Simone, B, Gualano, Maria Rosaria, Agodi, A, Coviello, Domenico, Dagna Bricarelli, F, Dallapiccola, B, Di Maria, E, Genuardi, Maurizio, Ricciardi, Walter, Boccia, Stefania (ORCID:0000-0002-1864-749X), Genuardi, Maurizio (ORCID:0000-0002-7410-8351), Ricciardi, Gualtiero (ORCID:0000-0002-5655-688X), Boccia, Stefania, Simone, B, Gualano, Maria Rosaria, Agodi, A, Coviello, Domenico, Dagna Bricarelli, F, Dallapiccola, B, Di Maria, E, Genuardi, Maurizio, Ricciardi, Walter, Boccia, Stefania (ORCID:0000-0002-1864-749X), Genuardi, Maurizio (ORCID:0000-0002-7410-8351), and Ricciardi, Gualtiero (ORCID:0000-0002-5655-688X)
Abstract: Public Health Genomics (PHG) has been defined as the responsible and effective translation of genome-based knowledge for the benefit of population health (Bellagio workshop, April 2005). The Italian Network of Public Health Genomics (GENISAP, http://istituti.unicatt.it/igiene_1830.html) was founded in 2006 as a follow-up of the PHG European Network (PHGEN) research activities. It is coordinated by Walter Ricciardi and Stefania Boccia from the Institute of Hygiene of the Faculty of Medicine of the Università Cattolica del Sacro Cuore, Rome. The aim of GENISAP is to integrate genomics into public health policy and practice in Italy in a responsible and effective manner. As such, GENISAP members elaborated the present document to describe the state of the art of PHG in Italy, in order to encourage the generation of evidence-based knowledge on genetic testing especially for common complex disorders. In Italy, about 560,000 genetic tests, including 311,069 cytogenetic and 248,691 molecular analyses, were recorded in 2007, but there is limited experience of translation of genomic testing for complex diseases into clinical practice (mostly on hereditary breast/ovarian and colorectal cancer syndromes). The collaboration between the Italian Health Ministry - that has introduced an action plan on genomics and predictive medicine in the 2010-2012 National Prevention Plan - and the GENISAP network will result in a fast advancement of Public Health Genomics in Italy.
Published: 2012

44. Fabry disease: polymorphic haplotypes and a novel missense mutation in the GLA gene

Author: Ferri, L, Guido, C, La Marca, G, Malvagia, S, Cavicchi, C, Fiumara, A, Barone, R, Parini, R, Antuzzi, D, Feliciani, C, Zampetti, A, Manna, Raffaele, Giglio, S, Della Valle, C, Wu, X, Valenzano, K, Benjamin, E, Donati, M, Guerrini, R, Genuardi, Maurizio, Morrone, A., Manna, Raffaele (ORCID:0000-0003-1560-3907), Genuardi, Maurizio (ORCID:0000-0002-7410-8351), Ferri, L, Guido, C, La Marca, G, Malvagia, S, Cavicchi, C, Fiumara, A, Barone, R, Parini, R, Antuzzi, D, Feliciani, C, Zampetti, A, Manna, Raffaele, Giglio, S, Della Valle, C, Wu, X, Valenzano, K, Benjamin, E, Donati, M, Guerrini, R, Genuardi, Maurizio, Morrone, A., Manna, Raffaele (ORCID:0000-0003-1560-3907), and Genuardi, Maurizio (ORCID:0000-0002-7410-8351)
Abstract: Fabry disease (FD) is an X-linked lysosomal storage disorder with a heterogeneous spectrum of clinical manifestations that are caused by the deficiency of a-galactosidase A (alpha-Gal-A) activity. Although useful for diagnosis in males, enzyme activity is not a reliable biochemical marker in heterozygous females due to random X-chromosome inactivation, thus rendering DNA sequencing of the alpha-Gal-A gene, alpha-galactosidase gene (GLA), the most reliable test for the confirmation of diagnosis in females. The spectrum of GLA mutations is highly heterogeneous. Many polymorphic GLA variants have been described, but it is unclear if haplotypes formed by combinations of such variants correlate with FD, thus complicating molecular diagnosis in females with normal alpha-Gal-A activity. We tested 67 female probands with clinical manifestations that may be associated with FD and 110 control males with normal alpha-Gal-A activity. Five different combinations of GLA polymorphic variants were identified in 14 of the 67 females, whereas clearcut pathogenetic alterations, p. Met51Ile and p. Met290Leu, were identified in two cases. The latter has not been reported so far, and both mutant forms were found to be responsive to the pharmacological chaperone deoxygalactonojirimycin (DGJ; migalastat hydrochloride). Analysis of the male control population, as well as male relatives of a suspected FD female proband, permitted the identification of seven different GLA gene haplotypes in strong linkage disequilibrium. The identification of haplotypes in control males provides evidence against their involvement in the development of FD phenotypic manifestations.
Published: 2012

45. Morquio A syndrome due to Maternal Uniparental Isodisomy of the telomeric end of chromosome 16

Author: Catarzi, S, Giunti, L, Papadia, F, Gabrielli, O, Guerrini, R, Donati, M, Genuardi, Maurizio, Morrone, A., Genuardi, Maurizio (ORCID:0000-0002-7410-8351), Catarzi, S, Giunti, L, Papadia, F, Gabrielli, O, Guerrini, R, Donati, M, Genuardi, Maurizio, Morrone, A., and Genuardi, Maurizio (ORCID:0000-0002-7410-8351)
Abstract: Morquio A syndrome (MPS IVA) is a recessive lysosomal storage disorder (LSD) caused by mutations in the GALNS gene leading to the deficiency of lysosomal enzyme N-acetylgalactosamine-6-sulfate sulfatase (GALNS). Patients show a broad spectrum of phenotypes ranging from classical severe type to mild forms. Classical forms are characterized by severe bone dysplasia and usually normal intelligence. So far, more than 170 unique mutations have been identified in the GALNS gene of MPS IVA patients. We report on a Morquio A patient with a classical phenotype who was found to be homozygous for a missense mutation (c.236 G > A: p.Cys79Tyr) in the GALNS gene. This alteration affects the highly conserved p.Cys79 that is transformed into formylglycine, the catalytic residue of the active site. The mutation was present in the proband's mother, but not in the father, whose paternity was confirmed by microsatellite analysis. In order to test the hypothesis of maternal uniparental disomy (UPD), we investigated the segregation of sixteen microsatellite markers from chromosome 16. The results showed a condition of maternal UPD due to an error in meiosis I. Maternal isodisomy of the 16q24 region led to homozygosity for the GALNS mutant allele, causing the patient's disease. These findings allow to add for the first time the LSD Morquio A syndrome to the list of conditions that can be caused by UPD. The possibility of UPD is relevant when giving genetic counseling to couples since the recurrent risk in future pregnancies is dramatically reduced. (C) 2011 Elsevier Inc. All rights reserved.
Published: 2012

46. Stepwise functional assessment of unclassified DNA variants

Author: Genuardi, Maurizio, Genuardi, Maurizio (ORCID:0000-0002-7410-8351), Genuardi, Maurizio, and Genuardi, Maurizio (ORCID:0000-0002-7410-8351)
Abstract: Verification of the three-step model in assessing the pathogenicity of mismatch repair gene variants.
Published: 2011

47. High resolution melting analysis for a rapid identification of heterozygous and homozygous sequence changes in the MUTYH gene

Author: Tricarico, R, Crucianelli, F, Alvau, A, Orlando, C, Sestini, R, Tonelli, F, Valanzano, R, Genuardi, Maurizio, Genuardi, Maurizio (ORCID:0000-0002-7410-8351), Tricarico, R, Crucianelli, F, Alvau, A, Orlando, C, Sestini, R, Tonelli, F, Valanzano, R, Genuardi, Maurizio, and Genuardi, Maurizio (ORCID:0000-0002-7410-8351)
Abstract: Background: MUTYH-associated polyposis (MAP) is an autosomal recessive form of intestinal polyposis predisposing to colorectal carcinoma. High resolution melting analysis (HRMA) is a mutation scanning method that allows detection of heterozygous sequence changes with high sensitivity, whereas homozygosity for a nucleotide change may not lead to significant curve shape or melting temperature changes compared to homozygous wildtype samples. Therefore, HRMA has been mainly applied to the detection of mutations associated with autosomal dominant or X-linked disorders, while applications to autosomal recessive conditions are less common. Methods: MUTYH coding sequence and UTRs were analyzed by both HRMA and sequencing on 88 leukocyte genomic DNA samples. Twenty-six samples were also examined by SSCP. Experiments were performed both with and without mixing the test samples with wild-type DNA. Results: The results show that all MUTYH sequence variations, including G > C and A > T homozygous changes, can be reliably identified by HRMA when a condition of artificial heterozygosity is created by mixing test and reference DNA. HRMA had a sensitivity comparable to sequencing and higher than SSCP. Conclusions: The availability of a rapid and inexpensive method for the identification of MUTYH sequence variants is relevant for the diagnosis of colorectal cancer susceptibility, since the MAP phenotype is highly variable.
Published: 2011

48. Deciphering the Colon Cancer Genes-Report of the InSiGHT-Human Variome Project Workshop, UNESCO, Paris 2010

Author: Kohonen Corish, M, Macrae, F, Genuardi, Maurizio, Aretz, S, Bapat, B, Bernstein, I, Burn, J, Cotton, R, Den Dunnen, J, Frebourg, T, Greenblatt, M, Hofstra, R, Holinski Feder, E, Lappalainen, I, Lindblom, A, Maglott, D, Moller, P, Morreau, H, Moslein, G, Sijmons, R, Spurdle, A, Tavtigian, S, Tops, C, Weber, T, De Wind, N, Woods, M., Genuardi, Maurizio (ORCID:0000-0002-7410-8351), Kohonen Corish, M, Macrae, F, Genuardi, Maurizio, Aretz, S, Bapat, B, Bernstein, I, Burn, J, Cotton, R, Den Dunnen, J, Frebourg, T, Greenblatt, M, Hofstra, R, Holinski Feder, E, Lappalainen, I, Lindblom, A, Maglott, D, Moller, P, Morreau, H, Moslein, G, Sijmons, R, Spurdle, A, Tavtigian, S, Tops, C, Weber, T, De Wind, N, Woods, M., and Genuardi, Maurizio (ORCID:0000-0002-7410-8351)
Abstract: The Human Variome Project (HVP) has established a pilot program with the International Society for Gastrointestinal Hereditary Tumours (InSiGHT) to compile all inherited variation affecting colon cancer susceptibility genes. An HVP-InSiGHT Workshop was held on May 10, 2010, prior to the HVP Integration and Implementation Meeting at UNESCO in Paris, to review the progress of this pilot program. A wide range of topics were covered, including issues relating to genotype-phenotype data submission to the InSiGHT Colon Cancer Gene Variant Databases (chromium.liacs.nl/LOVD2/colon_cancer/home.php). The meeting also canvassed the recent exciting developments in models to evaluate the pathogenicity of unclassified variants using in silico data, tumor pathology information, and functional assays, and made further plans for the future progress and sustainability of the pilot program.
Published: 2011

49. Thymidylate synthase expression and genotype have no major impact on the clinical outcome of colorectal cancer patients treated with 5-fluorouracil

Author: Vignoli, M, Nobili, S, Napoli, C, Putignano, A, Morganti, M, Papi, L, Valanzano, R, Cianchi, F, Tonelli, F, Mazzei, T, Mini, E, Genuardi, Maurizio, Genuardi, Maurizio (ORCID:0000-0002-7410-8351), Vignoli, M, Nobili, S, Napoli, C, Putignano, A, Morganti, M, Papi, L, Valanzano, R, Cianchi, F, Tonelli, F, Mazzei, T, Mini, E, Genuardi, Maurizio, and Genuardi, Maurizio (ORCID:0000-0002-7410-8351)
Abstract: BACKGROUND AND OBJECTIVES: Thymidylate synthase (TS) expression levels appear to be related to response to 5-fluorouracil-(5-FU)-based chemotherapy in colorectal cancer (CRC) patients. Three polymorphisms have been proposed as modulators of TS expression: a tandemly repeated sequence (2R/3R) in the 5' UTR, a SNP (G>C) within the 3R allele and a 6bp deletion in the 3' UTR. To evaluate the influence of TS expression and polymorphisms on clinical outcome of 5-FU-treated patients we performed a comprehensive genetic analysis on 63 CRC patients. METHODS: TS expression levels were analyzed in normal and tumor tissues. TS coding sequence and UTR polymorphisms were investigated on DNA from normal tissue. LOH analysis was performed to determine tumor genotype. RESULTS: A difference in disease-free survival (DFS), although not statistically significant, was observed between high and low mRNA expression levels: patients with low levels showed longer DFS. The 2R2R genotype showed significantly lower expression than the 3R3R and 2R3R genotypes in normal tissue. No other TS polymorphism was associated with mRNA expression or clinical outcome. CONCLUSIONS: The results obtained in this pilot study indicate that the number of 5' UTR repeats is the major genetic determinant of TS expression. The lack of association with other polymorphisms might be partially explained by the existence of linkage disequilibrium in the TS gene. Our data support the growing evidence that TS control may require multiple mechanisms acting in close coordination with one another and suggest that TS genotyping alone in tumor samples is not sufficient to accurately predict response to 5-FU.
Published: 2011

50. Constitutional FLCN mutations in patients with suspected Birt-Hogg-Dube syndrome ascertained for non-cutaneous manifestations

Author: Maffe, A, Toschi, B, Circo, G, Giachino, D, Giglio, S, Rizzo, A, Carloni, A, Poletti, V, Tomassetti, S, Ginardi, C, Ungari, S, Genuardi, Maurizio, Genuardi, Maurizio (ORCID:0000-0002-7410-8351), Maffe, A, Toschi, B, Circo, G, Giachino, D, Giglio, S, Rizzo, A, Carloni, A, Poletti, V, Tomassetti, S, Ginardi, C, Ungari, S, Genuardi, Maurizio, and Genuardi, Maurizio (ORCID:0000-0002-7410-8351)
Abstract: Birt-Hogg-Dube syndrome (BHDS) is characterized by a clinical triad including cutaneous hamartomas originating from hair follicles, lung cysts/pneumothorax, and kidney tumors. Inactivating mutations of the tumor suppressor gene FLCN are identified in most families with BHDS. Usually, patients are referred for genetic examination by dermatologists because of the presence of typical multiple skin tumors with or without additional symptoms. However, because of phenotypic variability and incomplete penetrance, the clinical presentation of BHDS is not yet fully defined. Criteria for genetic testing and diagnosis that take into account variable manifestations have recently been proposed by the European BHD Consortium. We sequenced the FLCN gene coding region in a series of 19 patients selected for kidney and/or lung manifestations. Overall, FLCN mutations were found in 9 of 19 (47%) families and were detected only in probands who had either > 2 components of the clinical triad or a single component (renal or pulmonary) along with a family history of another main BHDS manifestation. Typical cutaneous lesions were present only in 8 of 21 FLCN mutation carriers aged > 20 years identified in the mutation-positive families. In addition, we provide clinical and molecular evidence that parotid oncocytoma, so far reported in six BHDS cases, is associated with this condition, based on the observation of a patient with bilateral parotid involvement and marked reduction of the wild-type FLCN allele signal in tumor DNA. Overall, the results obtained in this study contribute to the definition of the phenotypic characteristics that should be considered for BHDS diagnosis and FLCN mutation testing.
Published: 2011

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