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1. Liquid biopsy: a right tool in a right context?

Author

La Mantia, M., primary, Cutaia, S., additional, Gristina, V., additional, Galvano, A., additional, Capoluongo, E., additional, Rolfo, C., additional, Malapelle, U., additional, Incorvaia, L., additional, Badalamenti, G., additional, Russo, A., additional, and Bazan, V., additional

Published
2023
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2. List of contributors

Author

Arbitrio, M., primary, Badalamenti, G., additional, Barraco, N., additional, Bazan, V., additional, Bono, M., additional, Brando, C., additional, Busuito, G., additional, Buttitta, F., additional, Calcara, K., additional, Cancelliere, D., additional, Capoluongo, E., additional, Caracciolo, D., additional, Castiglia, M., additional, Cordua, A., additional, Cuomo, O., additional, Cusenza, S., additional, Cutaia, S., additional, Del Re, M., additional, Di Martino, M.T., additional, D’Apolito, M., additional, Fanale, D., additional, Felicioni, L., additional, Fiorillo, L., additional, Fiorino, A., additional, Galvano, A., additional, Giordano, A., additional, Giurintano, A., additional, Greco, M., additional, Gristina, V., additional, Iacono, F., additional, Incorvaia, L., additional, La Mantia, M., additional, Lianidou, E., additional, Malapelle, U., additional, Marchetti, A., additional, Navicella, A., additional, Pedone, E., additional, Perez, A., additional, Pisapia, P., additional, Pivetti, A., additional, Rolfo, C., additional, Rossetti, R., additional, Russo, A., additional, Scalia, R., additional, Spinnato, V., additional, Staropoli, N., additional, Tagliaferri, P., additional, Tassone, P., additional, Taverna, S., additional, Troncone, G., additional, and Uppolo, V., additional

Published
2023
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3. Current clinically validated applications of liquid biopsy

Author

Capoluongo, E., primary, Rolfo, C., additional, Galvano, A., additional, Gristina, V., additional, Perez, A., additional, Barraco, N., additional, La Mantia, M., additional, Incorvaia, L., additional, Badalamenti, G., additional, Russo, A., additional, and Bazan, V., additional

Published
2023
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5. Implementation of preventive and predictive BRCA testing in patients with breast, ovarian, pancreatic, and prostate cancer: a position paper of Italian Scientific Societies

Author

Beretta, Giordano, Bella, Maria Angela, Bracarda, Sergio, Colombo, Nicoletta, Conteduca, Vincenza, Del Mastro, Lucia, Galvano, Antonio, Gristina, Valerio, Guarneri, Valentina, La Verde, Nicla, Lorusso, Domenica, Marchetti, Paolo, Normanno, Nicola, Ottini, Laura, Pensabene, Matilde, Pignata, Sandro, Procopio, Giuseppe, Ricevuto, Enrico, Silvestris, Nicola, Tassone, Pierfrancesco, Tucci, Marcello, Donato, Vittorio, Carrara, Silvia, Paiella, Salvatore, Gentilini, Oreste, Gunelli, Roberta, Nicolis, Fabrizio, Buttitta, Fiamma, Colecchia, Maurizio, Fassan, Matteo, Malapelle, Umberto, Marchetti, Antonio, Marchiò, Caterina, Scarpa, Aldo, Truini, Mauro, Zamboni, Giuseppe, Gion, Massimo, Trevisiol, Chiara, Gronchi, Alessandro, Danesi, Romano, Di Marco, Vito, Carrera, Paola, Ghiorzo, Paola, Pasini, Barbara, Varesco, Liliana, Artibani, Walter, Ludovico, Giuseppe, Campanella, Ornella, Vatrano, Simona, Tagliafico, Enrico, Russo, A., Incorvaia, L., Capoluongo, E., Tagliaferri, P., Gori, S., Cortesi, L., Genuardi, M., Turchetti, D., De Giorgi, U., Di Maio, M., Barberis, M., Dessena, M., Del Re, M., Lapini, A., Luchini, C., Jereczek-Fossa, B.A., Sapino, A., and Cinieri, S.

Published
2022
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6. The molecular profiling of solid tumors by liquid biopsy: a position paper of the AIOM–SIAPEC-IAP–SIBioC–SIC–SIF Italian Scientific Societies

Author

Russo, A., Incorvaia, L., Del Re, M., Malapelle, U., Capoluongo, E., Gristina, V., Castiglia, M., Danesi, R., Fassan, M., Giuffrè, G., Gori, S., Marchetti, A., Normanno, N., Pinto, C., Rossi, G., Santini, D., Sartore-Bianchi, A., Silvestris, N., Tagliaferri, P., Troncone, G., Cinieri, S., and Beretta, G.D.

Published
2021
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7. The Pathogenic RET Val804Met Variant in Acromegaly: A New Clinical Phenotype?

Author

Chiloiro, Sabrina, Capoluongo, Ettore Domenico, Costanza, Flavia, Minucci, Angelo, Giampietro, Antonella, Infante, A., Milardi, Domenico, Ricciardi Tenore, C., De Bonis, Maria Valeria, Gaudino, Simona, Rindi, Guido, Olivi, Alessandro, De Marinis, L., Pontecorvi, Alfredo, Doglietto, Francesco, Bianchi, Antonio, Chiloiro S. (ORCID:0000-0001-9241-2392), Capoluongo E. D. (ORCID:0000-0001-9872-0572), Costanza F., Minucci A., Giampietro A., Milardi D., De Bonis M., Gaudino S. (ORCID:0000-0003-1681-4343), Rindi G. (ORCID:0000-0003-2996-4404), Olivi A. (ORCID:0000-0002-4489-7564), Pontecorvi A. (ORCID:0000-0003-0570-6865), Doglietto F. (ORCID:0000-0002-7438-0734), Bianchi A., Chiloiro, Sabrina, Capoluongo, Ettore Domenico, Costanza, Flavia, Minucci, Angelo, Giampietro, Antonella, Infante, A., Milardi, Domenico, Ricciardi Tenore, C., De Bonis, Maria Valeria, Gaudino, Simona, Rindi, Guido, Olivi, Alessandro, De Marinis, L., Pontecorvi, Alfredo, Doglietto, Francesco, Bianchi, Antonio, Chiloiro S. (ORCID:0000-0001-9241-2392), Capoluongo E. D. (ORCID:0000-0001-9872-0572), Costanza F., Minucci A., Giampietro A., Milardi D., De Bonis M., Gaudino S. (ORCID:0000-0003-1681-4343), Rindi G. (ORCID:0000-0003-2996-4404), Olivi A. (ORCID:0000-0002-4489-7564), Pontecorvi A. (ORCID:0000-0003-0570-6865), Doglietto F. (ORCID:0000-0002-7438-0734), and Bianchi A.

Abstract

Several genetic investigations were conducted to identify germline and somatic mutations in somatotropinomas, a subtype of pituitary tumors. To our knowledge, we report the first acromegaly patient carrying a RET pathogenic variant: c.2410G>A (rs79658334), p.Val804Met. Alongside the fact that the patient’s father and daughter carried the same variant, we investigated the clinical significance of this variant in the context of somatotropinomas and other endocrine tumors, reviewing the RET mutations’ oncogenic mechanisms. The aim was to search for new targets to precisely manage and treat acromegaly. Our case describes a new phenotype associated with the RET pathogenic variant, represented by aggressive acromegaly, and suggests consideration for RET mutation screening if NGS for well-established PitNET-associated gene mutations renders negative.

Published
2024

9. Implementation of preventive and predictive BRCA testing in patients with breast, ovarian, pancreatic, and prostate cancer: a position paper of Italian Scientific Societies

Author

Russo, A, Incorvaia, L, Capoluongo, E, Tagliaferri, P, Gori, S, Cortesi, L, Genuardi, M, Turchetti, D, De Giorgi, U, Di Maio, M, Barberis, M, Dessena, M, Del Re, M, Lapini, A, Luchini, C, Jereczek-Fossa, B, Sapino, A, Cinieri, S, Beretta, G, Bella, M, Bracarda, S, Colombo, N, Conteduca, V, Del Mastro, L, Galvano, A, Gristina, V, Guarneri, V, La Verde, N, Lorusso, D, Marchetti, P, Normanno, N, Ottini, L, Pensabene, M, Pignata, S, Procopio, G, Ricevuto, E, Silvestris, N, Tassone, P, Tucci, M, Donato, V, Carrara, S, Paiella, S, Gentilini, O, Gunelli, R, Nicolis, F, Buttitta, F, Colecchia, M, Fassan, M, Malapelle, U, Marchetti, A, Marchio, C, Scarpa, A, Truini, M, Zamboni, G, Gion, M, Trevisiol, C, Gronchi, A, Danesi, R, Di Marco, V, Carrera, P, Ghiorzo, P, Pasini, B, Varesco, L, Artibani, W, Ludovico, G, Campanella, O, Vatrano, S, Tagliafico, E, Russo A., Incorvaia L., Capoluongo E., Tagliaferri P., Gori S., Cortesi L., Genuardi M., Turchetti D., De Giorgi U., Di Maio M., Barberis M., Dessena M., Del Re M., Lapini A., Luchini C., Jereczek-Fossa B. A., Sapino A., Cinieri S., Beretta G., Bella M. A., Bracarda S., Colombo N., Conteduca V., Del Mastro L., Galvano A., Gristina V., Guarneri V., La Verde N., Lorusso D., Marchetti P., Normanno N., Ottini L., Pensabene M., Pignata S., Procopio G., Ricevuto E., Silvestris N., Tassone P., Tucci M., Donato V., Carrara S., Paiella S., Gentilini O., Gunelli R., Nicolis F., Buttitta F., Colecchia M., Fassan M., Malapelle U., Marchetti A., Marchio C., Scarpa A., Truini M., Zamboni G., Gion M., Trevisiol C., Gronchi A., Danesi R., Di Marco V., Carrera P., Ghiorzo P., Pasini B., Varesco L., Artibani W., Ludovico G., Campanella O., Vatrano S., Tagliafico E., Russo, A, Incorvaia, L, Capoluongo, E, Tagliaferri, P, Gori, S, Cortesi, L, Genuardi, M, Turchetti, D, De Giorgi, U, Di Maio, M, Barberis, M, Dessena, M, Del Re, M, Lapini, A, Luchini, C, Jereczek-Fossa, B, Sapino, A, Cinieri, S, Beretta, G, Bella, M, Bracarda, S, Colombo, N, Conteduca, V, Del Mastro, L, Galvano, A, Gristina, V, Guarneri, V, La Verde, N, Lorusso, D, Marchetti, P, Normanno, N, Ottini, L, Pensabene, M, Pignata, S, Procopio, G, Ricevuto, E, Silvestris, N, Tassone, P, Tucci, M, Donato, V, Carrara, S, Paiella, S, Gentilini, O, Gunelli, R, Nicolis, F, Buttitta, F, Colecchia, M, Fassan, M, Malapelle, U, Marchetti, A, Marchio, C, Scarpa, A, Truini, M, Zamboni, G, Gion, M, Trevisiol, C, Gronchi, A, Danesi, R, Di Marco, V, Carrera, P, Ghiorzo, P, Pasini, B, Varesco, L, Artibani, W, Ludovico, G, Campanella, O, Vatrano, S, Tagliafico, E, Russo A., Incorvaia L., Capoluongo E., Tagliaferri P., Gori S., Cortesi L., Genuardi M., Turchetti D., De Giorgi U., Di Maio M., Barberis M., Dessena M., Del Re M., Lapini A., Luchini C., Jereczek-Fossa B. A., Sapino A., Cinieri S., Beretta G., Bella M. A., Bracarda S., Colombo N., Conteduca V., Del Mastro L., Galvano A., Gristina V., Guarneri V., La Verde N., Lorusso D., Marchetti P., Normanno N., Ottini L., Pensabene M., Pignata S., Procopio G., Ricevuto E., Silvestris N., Tassone P., Tucci M., Donato V., Carrara S., Paiella S., Gentilini O., Gunelli R., Nicolis F., Buttitta F., Colecchia M., Fassan M., Malapelle U., Marchetti A., Marchio C., Scarpa A., Truini M., Zamboni G., Gion M., Trevisiol C., Gronchi A., Danesi R., Di Marco V., Carrera P., Ghiorzo P., Pasini B., Varesco L., Artibani W., Ludovico G., Campanella O., Vatrano S., and Tagliafico E.

Abstract

Constitutional BRCA1/BRCA2 pathogenic or likely pathogenic variants (PVs) are associated with an increased risk for developing breast and ovarian cancers. Current evidence indicates that BRCA1/2 PVs are also associated with pancreatic cancer, and that BRCA2 PVs are associated with prostate cancer risk. The identification of carriers of constitutional PVs in the BRCA1/2 genes allows the implementation of individual and family prevention pathways, through validated screening programs and risk-reducing strategies. According to the relevant and increasing therapeutic predictive implications, the inclusion of BRCA testing in the routine management of patients with breast, ovarian, pancreatic and prostate cancers represent a key requirement to optimize medical or surgical therapeutic and prevention decision-making, and access to specific anticancer therapies. Therefore, accurate patient selection, the use of standardized and harmonized procedures, and adherence to homogeneous testing criteria, are essential elements to implement BRCA testing in clinical practice. This consensus position paper has been developed and approved by a multidisciplinary Expert Panel of 64 professionals on behalf of the AIOM–AIRO–AISP–ANISC–AURO–Fondazione AIOM–SIAPEC/IAP–SIBioC–SICO–SIF–SIGE–SIGU–SIU–SIURO–UROP Italian Scientific Societies, and a patient association (aBRCAdaBRA Onlus). The working group included medical, surgical and radiation oncologists, medical and molecular geneticists, clinical molecular biologists, surgical and molecular pathologists, organ specialists such as gynecologists, gastroenterologists and urologists, and pharmacologists. The manuscript is based on the expert consensus and reports the best available evidence, according to the current eligibility criteria for BRCA testing and counseling, it also harmonizes with current Italian National Guidelines and Clinical Recommendations.

Published
2022

10. 70MO Genomic profiling to expand precision cancer medicine in the real world: The ROME trial

Author

Botticelli, A., primary, Scagnoli, S., additional, Conte, P.F., additional, Cremolini, C., additional, Ascierto, P.A., additional, Aglietta, M., additional, Mazzuca, F., additional, Capoluongo, E., additional, Malapelle, U., additional, Nuti, M., additional, D'Amati, G., additional, Cerbelli, B., additional, Pruneri, G., additional, Giannini, G., additional, Cappuzzo, F., additional, Biffoni, M., additional, Blandino, G., additional, Cognetti, F., additional, Curigliano, G., additional, and Marchetti, P., additional

Published
2023
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11. The dynamics of circulating tumour DNA (ctDNA) during treatment reflects tumour response in advanced melanoma patients

Author

Dinardo, L., Delregno, L., Distefani, A., Mannino, Maria, Fossati, Barbara, Catapano, S., Quattrini, Laura, Pellegrini, C., Cortellini, A., Parisi, Carmelo Maria Antonio, Capoluongo, Ettore Domenico, Autilio, C., Fargnoli, Maria Concetta, Peris, Ketty, Mannino M., Fossati B., Quattrini L., Parisi A., Capoluongo E. (ORCID:0000-0001-9872-0572), Fargnoli M. C., Peris K. (ORCID:0000-0002-5237-0463), Dinardo, L., Delregno, L., Distefani, A., Mannino, Maria, Fossati, Barbara, Catapano, S., Quattrini, Laura, Pellegrini, C., Cortellini, A., Parisi, Carmelo Maria Antonio, Capoluongo, Ettore Domenico, Autilio, C., Fargnoli, Maria Concetta, Peris, Ketty, Mannino M., Fossati B., Quattrini L., Parisi A., Capoluongo E. (ORCID:0000-0001-9872-0572), Fargnoli M. C., and Peris K. (ORCID:0000-0002-5237-0463)

Abstract

Despite the introduction of targeted (BRAFi/MEKi) and immune checkpoint inhibitors (ICIs) has significantly reduced the recurrence rate and improved the overall survival (OS) of patients with Stage III and IV melanoma, only a percentage will benefit of durable disease control. The aim of this study was to examine whether the levels of circulating tumour DNA (ctDNA) in plasma of advanced melanoma patients undergoing BRAFi/MEKi or ICIs vary according to the patients' survival outcomes (i.e. progression-free survival (PFS) and OS) and disease progression. Plasma samples of Stage III-IV melanoma patients were collected at baseline (treatment initiation) and thereafter every 3 months. Circulating BRAFV600E/K and NRASQ61R/K mutations were analysed through droplet digital PCR (ddPCR, Bio-Rad) in a total of 177 plasma samples from 48 melanoma patients (19 Stage III, 29 Stage IV). Baseline ctDNA concentration was significantly associated with OS (HR = 1.003, 95% CI = 1.000–1.006, p = 0.043) and PFS (HR = 1.004, 95% CI = 1.000–1.007, p = 0.029) independent of clinical-prognostic confounders. For each unit increase in the ∆ctDNA (concentration difference between the last follow-up and baseline) there was a 24% increased risk of disease progression, irrespective of treatment type and stage at diagnosis (OR = 1.24, 95% CI = 1.03–1.49, p = 0.020, AUC = 0.93). Patients with reduction of ctDNA level from baseline to the last follow-up had longer OS (HR = 0.14; 95% CI = 0.05–0.44, p = 0.001) and PFS (HR = 0.08; 95% CI = 0.03–0.27, p < 0.0001) compared to patients with increased ctDNA, including adjustment for confounding factors. Our findings suggest that variation of ctDNA over time during melanoma treatment reflects the clinical outcome and tumour response to therapy and might be helpful in clinical monitoring.

Published
2023

15. 1665P Genomic mutational landscape of solid tumors: Preliminary results from ROME trial

Author

Botticelli, A., primary, Scagnoli, S., additional, Conte, P.F., additional, Cremolini, C., additional, Ascierto, P.A., additional, Cappuzzo, F., additional, Aglietta, M., additional, Mazzuca, F., additional, Capoluongo, E., additional, Blandino, G., additional, Malapelle, U., additional, Nuti, M., additional, D'Amati, G., additional, Cerbelli, B., additional, Pruneri, G., additional, Biffoni, M., additional, Giannini, G., additional, Cognetti, F., additional, Curigliano, G., additional, and Marchetti, P., additional

Published
2022
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18. Implementation of preventive and predictive BRCA testing in patients with breast, ovarian, pancreatic, and prostate cancer: a position paper of Italian Scientific Societies

Author

Russo, A., primary, Incorvaia, L., additional, Capoluongo, E., additional, Tagliaferri, P., additional, Gori, S., additional, Cortesi, L., additional, Genuardi, M., additional, Turchetti, D., additional, De Giorgi, U., additional, Di Maio, M., additional, Barberis, M., additional, Dessena, M., additional, Del Re, M., additional, Lapini, A., additional, Luchini, C., additional, Jereczek-Fossa, B.A., additional, Sapino, A., additional, Cinieri, S., additional, Beretta, Giordano, additional, Bella, Maria Angela, additional, Bracarda, Sergio, additional, Colombo, Nicoletta, additional, Conteduca, Vincenza, additional, Del Mastro, Lucia, additional, Galvano, Antonio, additional, Gristina, Valerio, additional, Guarneri, Valentina, additional, La Verde, Nicla, additional, Lorusso, Domenica, additional, Marchetti, Paolo, additional, Normanno, Nicola, additional, Ottini, Laura, additional, Pensabene, Matilde, additional, Pignata, Sandro, additional, Procopio, Giuseppe, additional, Ricevuto, Enrico, additional, Silvestris, Nicola, additional, Tassone, Pierfrancesco, additional, Tucci, Marcello, additional, Donato, Vittorio, additional, Carrara, Silvia, additional, Paiella, Salvatore, additional, Gentilini, Oreste, additional, Gunelli, Roberta, additional, Nicolis, Fabrizio, additional, Buttitta, Fiamma, additional, Colecchia, Maurizio, additional, Fassan, Matteo, additional, Malapelle, Umberto, additional, Marchetti, Antonio, additional, Marchiò, Caterina, additional, Scarpa, Aldo, additional, Truini, Mauro, additional, Zamboni, Giuseppe, additional, Gion, Massimo, additional, Trevisiol, Chiara, additional, Gronchi, Alessandro, additional, Danesi, Romano, additional, Di Marco, Vito, additional, Carrera, Paola, additional, Ghiorzo, Paola, additional, Pasini, Barbara, additional, Varesco, Liliana, additional, Artibani, Walter, additional, Ludovico, Giuseppe, additional, Campanella, Ornella, additional, Vatrano, Simona, additional, and Tagliafico, Enrico, additional

Published
2022
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19. Spliceogenic analysis of BRCA1 c.439T>C (rs794727800) variant by High Resolution Melting Analysis

Author

Minucci, A., Mazzuccato, G., D'Indinosante, M., Di Nardo, L., Concolino, P., De Bonis, M., Urbani, A., Scambia, G., Fagotti, A., Capoluongo, E., Minucci A., D'Indinosante M., Di Nardo L., Concolino P., Urbani A. (ORCID:0000-0001-9168-3174), Scambia G. (ORCID:0000-0003-2758-1063), Fagotti A. (ORCID:0000-0001-5579-335X), Capoluongo E. (ORCID:0000-0001-9872-0572), Minucci, A., Mazzuccato, G., D'Indinosante, M., Di Nardo, L., Concolino, P., De Bonis, M., Urbani, A., Scambia, G., Fagotti, A., Capoluongo, E., Minucci A., D'Indinosante M., Di Nardo L., Concolino P., Urbani A. (ORCID:0000-0001-9168-3174), Scambia G. (ORCID:0000-0003-2758-1063), Fagotti A. (ORCID:0000-0001-5579-335X), and Capoluongo E. (ORCID:0000-0001-9872-0572)

Abstract

Correct classification of genomic variants causing potentially aberrant splicing is of utmost importance for patient management, especially in clinically actionable genes such as BRCA1/2. In this article, we report molecular evaluation of the BRCA1 c.439T>C (rs794727800, p.Leu147=) variant based on RNA of a patient suffering with high-grade serous ovarian cancer syndrome, to add new evidence to the only in silico data available for this variant. High Resolution Melting Analysis (HRMA) was used for the first time to investigate the spliceogenicity of a BRCA1 variant. HRMA with Sanger sequencing provided evidence that the c.439C allele does not cause aberrant splicing of the BRCA1 exon 7. In addition, HRMA with Sanger highlighted a different expression of the naturally occurring BRCA1 r.442_444del (c.442_444delCAG, p.Gln148del, at DNA level) isoform between blood and tumor, in this patient. HRMA is an alternative molecular approach to analyze spliceogenic properties of the c.439T>C variant and potentially for all those BRCA1/2 variants affecting splicing sites. These new evidences allowed to classify definitively the c.439T>C variant as benign. Furthermore, the different BRCA1 r.442_444del expression opens the discussion to consider a wider classification criteria for the splicing variants, including molecular evaluation at tissue level, which is an aspect currently scarcely considered in BRCA1/2 variant classification recommendations.

Published
2020

20. The friendly use of chloroquine in the COVID-19 disease: a warning for the G6PD -deficient males and for the unaware carriers of pathogenic alterations of the G6PD gene

Author

Capoluongo E. D., Amato F., Castaldo G., Capoluongo, E. D., Amato, F., and Castaldo, G.

Subjects
Male, Drug, Heterozygote, 030213 general clinical medicine, media_common.quotation_subject, Pneumonia, Viral, Clinical Biochemistry, Disease, Glucosephosphate Dehydrogenase, 030204 cardiovascular system & hematology, Betacoronavirus, 03 medical and health sciences, 0302 clinical medicine, Chloroquine, Humans, Medicine, Pandemics, media_common, Betacoronaviru, Pandemic, SARS-CoV-2, Coronavirus Infection, Genetic heterogeneity, business.industry, Incidence (epidemiology), Biochemistry (medical), COVID-19, Hydroxychloroquine, General Medicine, Hepatitis C, medicine.disease, Glucosephosphate Dehydrogenase Deficiency, Immunology, Female, Coronavirus Infections, business, G6PD, Human, medicine.drug
Abstract

There is a great debate regarding the usefulness and efficacy of this medication in anti-viral treatment: chloroquine is not included in the panel recommended for HIV treatment, while its modest effect in the therapy of human virus infection is reported for chronic hepatitis C These findings did not allow for its inclusion in the standardised therapeutic protocols for hepatitis C patients The benefits of chloroquine therapy strongly depend on: (i) the age of the patient;(ii) the clinical presentation and (iii) the stage of the COVID-19 disease Noteworthy, the use of this drug is contraindicated in some conditions, particularly the glucose-6-phosphate dehydrogenase (G6PD) deficiency The latter is a condition that has not been deeply taken into account particularly when, on the web, there has been a "viral" spread of news emphasizing the safe use and the free availability of chloroquine Therefore, before establishing that the use of chloroquine in the treatment of SARS-CoV-2 could represent a good option in light of such announcements, we should not miss the following important information that limit the friendly access to the drug: (a) G6PD is a housekeeping enzyme that, in the red blood cell (RBC), guarantees the production of NADPH, which is required to preserve glutathione in the reduced state (GSH), (b) G6PD deficiency shows marked genetic heterogeneity In this regard, we have reported more than 186 mutations, (c) G6PD deficiency is a necessary but not sufficient condition for the occurrence of clinical manifestations: the incidence of clinically evident favism in a group of randomly selected enzymopenic individuals resulted to be less than 30%, (d) the estimated number of G6PD-deficient individuals is close to 400 million people worldwide, while the number of pathogenic gene variants is generally concentrated in a small group of variations that can be easily detected in reference laboratories, and (e) as the rate of deficient RBCs in heterozygote carriers is not predictable a priori, potential individual clinical complications can strongly be proportional to the fraction of the number of G6PD-imbalanced RBCs Moreover, the majority of G6PD-deficient subjects do not show clinical manifestations in the steady state and the condition remains undetected until they are exposed to an exogenous haemolytic trigger such as bacterial or viral infections, ingestion of fava beans (favism) or drugs, mainly the hydroxychloroquine

Published
2020

22. Recommendations for the implementation of BRCA1/2 testing in ovarian cancer patients: From tumor to germline analysis. Joint document from SIBioC, AIOM, SIGU, SIAPEC-IAP

Author

Barberis, M, Bella, M, Buttitta, F, Capoluongo, E, Carrera, P, Colombo, N, Cortesi, L, Genuardi, M, Gion, M, Gori, S, Guarneri, V, Verde, N, Lorusso, D, Marchetti, A, Marchetti, P, Normanno, N, Pasini, B, Pensabene, M, Pignata, S, Radice, P, Ricevuto, E, Russo, A, Sapino, A, Tagliaferri, P, Tassone, P, Trevisiol, C, Truini, M, Varesco, L, Barberis M., Bella M. A., Buttitta F., Capoluongo E., Carrera P., Colombo N., Cortesi L., Genuardi M., Gion M., Gori S., Guarneri V., Verde N. L., Lorusso D., Marchetti A., Marchetti P., Normanno N., Pasini B., Pensabene M., Pignata S., Radice P., Ricevuto E., Russo A., Sapino A., Tagliaferri P., Tassone P., Trevisiol C., Truini M., Varesco L., Barberis, M, Bella, M, Buttitta, F, Capoluongo, E, Carrera, P, Colombo, N, Cortesi, L, Genuardi, M, Gion, M, Gori, S, Guarneri, V, Verde, N, Lorusso, D, Marchetti, A, Marchetti, P, Normanno, N, Pasini, B, Pensabene, M, Pignata, S, Radice, P, Ricevuto, E, Russo, A, Sapino, A, Tagliaferri, P, Tassone, P, Trevisiol, C, Truini, M, Varesco, L, Barberis M., Bella M. A., Buttitta F., Capoluongo E., Carrera P., Colombo N., Cortesi L., Genuardi M., Gion M., Gori S., Guarneri V., Verde N. L., Lorusso D., Marchetti A., Marchetti P., Normanno N., Pasini B., Pensabene M., Pignata S., Radice P., Ricevuto E., Russo A., Sapino A., Tagliaferri P., Tassone P., Trevisiol C., Truini M., and Varesco L.

Abstract

Since the approval of the first poly adenosine diphosphate (ADP) ribose polymerase inhibitor (PARPi), olaparib for platinum-sensitive relapsed high grade ovarian cancer, with either germline or somatic BRCA1/2 deleterious variants, the strategies for BRCA1/2 testing are dynamically changing. In fact, along with germline assay, patients are now tested for tumor BRCA1/2 also above all for treatment decisions. In fact, it is reported as by tumor BRCA analysis we can identify 3–9% more mutated women which can therefore benefit from PARPi therapy. Although this new type of approach looks like challenging, in particular due to the technical and analytical difficulties regarding low quality DNA deriving from formalin-fixed paraffin-embedded specimens, the new CE-IVD on NGS-based pipelines, can overcome these issues, allowing specialized molecular laboratories to ensure high quality results and perform the best test settings. Nevertheless, each new NGS pipeline (CE-IVD or in house) should be validated using peculiar samples along with commercially available reference and certified materials, before being introduced in routine settings. The validation set should be appropriately chosen in order to provide unequivocal data regarding robustness of each NGS tBRCA pipeline. Therefore, in order to harmonize the patient and laboratory path, a group of Italian Scientific Societies [Italian Society of Clinical Chemistry (SIBioC), Italian Association of Medical Oncology (AIOM), Italian Association of Clinical Pathology (SIAPEC), Italian Society of Human Genetics (SIGU)] provided the present recommendations which are aimed to guide all professionals (oncologists, gynaecologists, clinical and laboratory geneticists, clinical molecular biologists and pathologists). The intersociety group is confident that the present paper can offer all ovarian cancer women a well-organized pathway of diagnosis and treatment.

Published
2019

23. The Changing Clinical Spectrum of Hypophysitis

Author

Chiloiro, S., Capoluongo, E. D., Tartaglione, T., Giampietro, A., Bianchi, A., Giustina, A., Pontecorvi, A., De Marinis, L., Chiloiro S. (ORCID:0000-0001-9241-2392), Capoluongo E. D. (ORCID:0000-0001-9872-0572), Tartaglione T. (ORCID:0000-0003-3896-4078), Giampietro A., Giustina A., Pontecorvi A. (ORCID:0000-0003-0570-6865), Chiloiro, S., Capoluongo, E. D., Tartaglione, T., Giampietro, A., Bianchi, A., Giustina, A., Pontecorvi, A., De Marinis, L., Chiloiro S. (ORCID:0000-0001-9241-2392), Capoluongo E. D. (ORCID:0000-0001-9872-0572), Tartaglione T. (ORCID:0000-0003-3896-4078), Giampietro A., Giustina A., and Pontecorvi A. (ORCID:0000-0003-0570-6865)

Abstract

Hypophysitis is a rare and potentially life-threatening disease, characterized by an elevated risk of complications, such as occurrence of acute central hypoadrenalism, persistent hypopituitarism, or extension of the inflammatory process to the neighboring neurological structures. In recent years, a large number of patients have been described as being affected by hypophysitis, due to the increased administration of immuno-chemotherapies. At the present time, the heterogeneous nature of hypophysitis diagnostic criteria and of the treatment protocols makes the management of affected patients difficult. We review the current data and evidence on primary and secondary hypophysitis, in order to suggest a diagnostic and therapeutic protocol that should be focused on a multidisciplinary approach, for reaching a prompt diagnosis and an appropriate and safe treatment.

Published
2019

24. Novel BRCA1 Large Genomic Rearrangements in Italian Breast/Ovarian Cancer Patients

Author

Rizza, R, Hackmann, K, Paris, I, Minucci, A, De Leo, R, Schrock, E, Urbani, A, Capoluongo, E, Gelli, G, Concolino, P, Urbani, A (ORCID:0000-0001-9168-3174), Capoluongo, E (ORCID:0000-0001-9872-0572), Rizza, R, Hackmann, K, Paris, I, Minucci, A, De Leo, R, Schrock, E, Urbani, A, Capoluongo, E, Gelli, G, Concolino, P, Urbani, A (ORCID:0000-0001-9168-3174), and Capoluongo, E (ORCID:0000-0001-9872-0572)

Abstract

Background In recent years, the number of patients being offered BRCA1/2 testing has changed dramatically. Advances in high-throughput sequencing technology have led many diagnostic laboratories to test next-generation sequencing (NGS)-based platforms as the main technology for clinical testing. As a consequence, the proportion of novel BRCA1/2 variants detected has greatly increased. Here, we describe two novel BRCA1 large deletions detected in Italian patients affected by hereditary breast and ovarian cancer syndrome (HBOC). Methods We applied an NGS pipeline with a reliable copy number variation (CNV) prediction algorithm. Successively, samples were investigated using the Multiplex Amplicon Quantification (MAQ) assay and array comparative genomic hybridization (CGH). In a single case, long-range polymerase chain reaction (PCR) was employed for careful detection of the breakpoint region, while the RepeatMasker program was used to identify Alu sequences at the junction point. Results A 137.8 kb deletion, involving the first six exons of BRCA1 and the full NBR2, BRCA1P1, NBR1, and TMEM106a genes, was detected in an Italian woman diagnosed with high-grade serous ovarian carcinoma. A second rearrangement, involving the deletion of BRCA1 11-14 exons, was detected in a breast cancer patient and was fully characterized and reported according to recommended Human Genome Variation Society (HGVS) nomenclature: NG_005905.2: g.125038_143266del; NM_007294.3: c.2817_4716del; NP_009225: p.Lys862Metfs? Conclusion Although it was not possible to perform a familial segregation analysis and more direct evidence of the relationship between genotype and phenotype is necessary, both of the novel reported rearrangements cause the loss of crucial functional domains of the BRCA1 protein and this event supports their pathogenicity.

Published
2019

25. Identification of two novel LDLR variants by next generation sequencing

Author

Moffa S., Mazzuccato G., de Bonis M., de Paolis E., Onori M. E., Pontecorvi A., Urbani A., Giaccari A., Capoluongo E., Minucci A., Moffa, S., Mazzuccato, G., de Bonis, M., de Paolis, E., Onori, M. E., Pontecorvi, A., Urbani, A., Giaccari, A., Capoluongo, E., and Minucci, A.

Subjects
SmartSeq, Next generation sequencing, LDL-cholesterol, FH-Devyser Kit, Novel LDLR variant
Abstract

Introduction. Familial hypercholesterolemia (FH) is an autosomal dominant inherited disease characterized by elevated plasma low-density lipoprotein cholesterol (LDL-C). Targeted Next Generation Sequencing (NGS) is a new opportunity to expand the existing pathogenic variants (PVs) spectrum associated to FH. Our aim was to report a diagnostic NGS-based approach to detect variants associated to FH. Methods. We report two patients: a 48-year-old Asian woman, without known history of hypercholesterolemia and a 46-year-old Caucasian man, with childhood hypercholesterolemia. Results. An effective NGS-based pipeline, FH-Devyser kit/Amplicon Suite, beginning from sequencing to data analysis, did not identify known PVs in the LDLR, APOB, APOE, LDLRAP1, STAP1 and PCSK9 genes, but revealed two novel LDLR variants (c.1564A>T, p.Ile522Phe and c.1688C>T, p.Pro563Leu). Discussion and conclusions. This study showed that an effective NGS-based pipeline led to a definitive diagnosis in two FH families, allowing to plan their therapeutic treatment. Although the functional consequence of the two LDLR variants needs to be assessed in vitro, the in silico analysis and high preservation of the two amino acid positions observed in the LDLR protein, across different animal species, suggest that both variants are deleterious.

Published
2020

27. Bringing onco‐innovation to Europe’s healthcare systems: The potential of biomarker testing, real world evidence, tumour agnostic therapies to empower personalised medicine

Author

Horgan, J.H., Ciliberto, G. (Gennaro), Conte, P. (Pierfranco), Curigliano, G. (Giuseppe), Seijo, L. (Luis), Montuenga, L.M. (Luis M.), Garassino, M. (Marina), Penault-Llorca, F. (Frederique), Galli, F. (Fabrizia), Ray-Coquard, I. (Isabelle), Querleu, D. (Denis), Riegman, P.H.J. (Peter), Kerr, K. (Keith), Poppel, H. (Hein) van, Bjartell, A. (Anders), Codacci-Pisanelli, G. (G.), Koeva‐balabanova, J. (Jasmina), Paradiso, A. (Angelo), Maravic, Z. (Zorana), Fotaki, V. (Vassiliki), Malats, N. (Núria), Bernini, C. (Chiara), Buglioni, S. (Simonetta), Kent, A. (Alastair), Munzone, E. (Elisabetta), Belina, I. (Ivica), Meerbeeck, J.P. (Jan) van, Duffy, M.J. (Michael), Jagielska, B. (Beata), Capoluongo, E. (Ettore), Horgan, J.H., Ciliberto, G. (Gennaro), Conte, P. (Pierfranco), Curigliano, G. (Giuseppe), Seijo, L. (Luis), Montuenga, L.M. (Luis M.), Garassino, M. (Marina), Penault-Llorca, F. (Frederique), Galli, F. (Fabrizia), Ray-Coquard, I. (Isabelle), Querleu, D. (Denis), Riegman, P.H.J. (Peter), Kerr, K. (Keith), Poppel, H. (Hein) van, Bjartell, A. (Anders), Codacci-Pisanelli, G. (G.), Koeva‐balabanova, J. (Jasmina), Paradiso, A. (Angelo), Maravic, Z. (Zorana), Fotaki, V. (Vassiliki), Malats, N. (Núria), Bernini, C. (Chiara), Buglioni, S. (Simonetta), Kent, A. (Alastair), Munzone, E. (Elisabetta), Belina, I. (Ivica), Meerbeeck, J.P. (Jan) van, Duffy, M.J. (Michael), Jagielska, B. (Beata), and Capoluongo, E. (Ettore)

Abstract

Rapid and continuing advances in biomarker testing are not being matched by uptake in health systems, and this is hampering both patient care and innovation. It also risks costing health systems the opportunity to make their services more efficient and, over time, more economical. The potential that genomics has brought to biomarker testing in diagnosis, prediction and research is being realised, pre‐eminently in many cancers, but also in an ever‐wider range of conditions— notably BRCA1/2 testing in ovarian, breast, pancreatic and prostate cancers. Nevertheless, the implementation of genetic testing in clinical routine setting is still challenging. Development is impeded by country‐related heterogeneity, data deficiencies, and lack of policy alignment on standards, approval—and the role of real‐world evidence in the process—and reimbursement. The acute nature of the problem is compellingly illustrated by the particular challenges facing the development and use of tumour agnostic therapies, where the gaps in preparedness for taking advantage of this innovative approach to cancer therapy are sharply exposed. Europe should already have in place a guarantee of universal access to a minimum suite of biomarker tests and should be planning for an optimum testing scenario with a wider range of biomarker tests integrated into a more sophisticated health system articulated around personalised medicine. Improving healthcare and winning advantages for Europe’s industrial competitiveness and innovation require an appropriate policy framework—starting with an update to outdated recommendations. We show herein the main issues and proposals that emerged during the previous advisory boards organised by the European Alliance for Personalized Medicine which mainly focus on possible scenarios of harmonisation of both oncogenetic testing and management of cancer patients.

Published
2021
Full Text
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28. Let‐7a‐5p, mir‐100‐5p, mir‐101‐3p, and mir‐199a‐3p hyperexpression as potential predictive biomarkers in early breast cancer patients

Author

Fuso, Paola, Di Salvatore, Mariantonietta, Santonocito, Concetta, Guarino, Donatella, Autilio, C., Mule, A., Arciuolo, Damiano, Rinninella, A., Mignone, Flavio, Ramundo, M., Di Stefano, B., Orlandi, Armando, Capoluongo, Ettore Domenico, Nicolotti, Nicola, Franceschini, Gianluca, Sanchez, A. M., Tortora, Giampaolo, Scambia, Giovanni, Barone, C., Cassano, Alessandra, Fuso P., Di Salvatore M., Santonocito C. (ORCID:0000-0003-3624-1386), Guarino D., Arciuolo D., Mignone F., Orlandi A. (ORCID:0000-0001-5253-4678), Capoluongo E. (ORCID:0000-0001-9872-0572), Nicolotti N., Franceschini G. (ORCID:0000-0002-2950-3395), Tortora G. (ORCID:0000-0002-1378-4962), Scambia G. (ORCID:0000-0003-2758-1063), Cassano A. (ORCID:0000-0002-3311-7163), Fuso, Paola, Di Salvatore, Mariantonietta, Santonocito, Concetta, Guarino, Donatella, Autilio, C., Mule, A., Arciuolo, Damiano, Rinninella, A., Mignone, Flavio, Ramundo, M., Di Stefano, B., Orlandi, Armando, Capoluongo, Ettore Domenico, Nicolotti, Nicola, Franceschini, Gianluca, Sanchez, A. M., Tortora, Giampaolo, Scambia, Giovanni, Barone, C., Cassano, Alessandra, Fuso P., Di Salvatore M., Santonocito C. (ORCID:0000-0003-3624-1386), Guarino D., Arciuolo D., Mignone F., Orlandi A. (ORCID:0000-0001-5253-4678), Capoluongo E. (ORCID:0000-0001-9872-0572), Nicolotti N., Franceschini G. (ORCID:0000-0002-2950-3395), Tortora G. (ORCID:0000-0002-1378-4962), Scambia G. (ORCID:0000-0003-2758-1063), and Cassano A. (ORCID:0000-0002-3311-7163)

Abstract

Background: The aim of this study is to identify miRNAs able to predict the outcomes in breast cancer patients after neoadjuvant chemotherapy (NAC). Patients and methods: We retrospec-tively analyzed 24 patients receiving NAC and not reaching pathologic complete response (pCR). miRNAs were analyzed using an Illumina Next‐Generation‐Sequencing (NGS) system. Results: Event‐free survival (EFS) and overall survival (OS) were significantly higher in patients with up-regulation of let‐7a‐5p (EFS p = 0.006; OS p = 0.0001), mirR‐100‐5p (EFS s p = 0.01; OS p = 0.03), miR‐ 101‐3p (EFS p = 0.05; OS p = 0.01), and miR‐199a‐3p (EFS p = 0.02; OS p = 0.01) in post‐NAC samples, independently from breast cancer subtypes. At multivariate analysis, only let‐7a‐5p was significantly associated with EFS (p = 0.009) and OS (p = 0.0008). Conclusion: Up‐regulation of the above miRNAs could represent biomarkers in breast cancer.

Published
2021

29. A new founder BRCA1 haplotype identified in the Puglia region is associated with a specific age-related cancer onset in three unrelated families

Author

Capoluongo, Ettore Domenico, De Matteis, Elisabetta, Cucinotto, I, Ronzino, G, Santonocito, Concetta, Tornesello, Assunta, De Giorgio, Mr, Lucci Cordisco, Emanuela, Minucci, Angelo, Genuardi, Maurizio, Capoluongo E (ORCID:0000-0001-9872-0572), De Matteis E, Santonocito C (ORCID:0000-0003-3624-1386), Tornesello A (ORCID:0000-0002-7485-7440), Lucci Cordisco E (ORCID:0000-0002-6279-7604), Minucci A, Genuardi M. (ORCID:0000-0002-7410-8351), Capoluongo, Ettore Domenico, De Matteis, Elisabetta, Cucinotto, I, Ronzino, G, Santonocito, Concetta, Tornesello, Assunta, De Giorgio, Mr, Lucci Cordisco, Emanuela, Minucci, Angelo, Genuardi, Maurizio, Capoluongo E (ORCID:0000-0001-9872-0572), De Matteis E, Santonocito C (ORCID:0000-0003-3624-1386), Tornesello A (ORCID:0000-0002-7485-7440), Lucci Cordisco E (ORCID:0000-0002-6279-7604), Minucci A, and Genuardi M. (ORCID:0000-0002-7410-8351)

Abstract

No abstract available

Published
2021

30. Bringing onco?innovation to Europe’s healthcare systems: The potential of biomarker testing, real world evidence, tumour agnostic therapies to empower personalised medicine

Author

Horgan, D, Ciliberto, G, Conte, P, Curigliano, G, Seijo, L, Montuenga, LM, Garassino, M, Penault?llorca, F, Galli, F, Ray?coquard, I, Querleu, D, Riegman, Peter, Kerr, K, van Poppel, H, Bjartell, A, Codacci?pisanelli, G, Koeva?balabanova, J, Paradiso, A, Maravic, Z, Fotaki, V, Malats, N, Bernini, C, Buglioni, S, Kent, A, Munzone, E, Belina, I, Van Meerbeeck, J, Duffy, M, Jagielska, B, Capoluongo, E, Horgan, D, Ciliberto, G, Conte, P, Curigliano, G, Seijo, L, Montuenga, LM, Garassino, M, Penault?llorca, F, Galli, F, Ray?coquard, I, Querleu, D, Riegman, Peter, Kerr, K, van Poppel, H, Bjartell, A, Codacci?pisanelli, G, Koeva?balabanova, J, Paradiso, A, Maravic, Z, Fotaki, V, Malats, N, Bernini, C, Buglioni, S, Kent, A, Munzone, E, Belina, I, Van Meerbeeck, J, Duffy, M, Jagielska, B, and Capoluongo, E

Abstract

Rapid and continuing advances in biomarker testing are not being matched by uptake in health systems, and this is hampering both patient care and innovation. It also risks costing health systems the opportunity to make their services more efficient and, over time, more economical. The potential that genomics has brought to biomarker testing in diagnosis, prediction and research is being realised, pre‐eminently in many cancers, but also in an ever‐wider range of conditions— notably BRCA1/2 testing in ovarian, breast, pancreatic and prostate cancers. Nevertheless, the implementation of genetic testing in clinical routine setting is still challenging. Development is impeded by country‐related heterogeneity, data deficiencies, and lack of policy alignment on standards, approval—and the role of real‐world evidence in the process—and reimbursement. The acute nature of the problem is compellingly illustrated by the particular challenges facing the development and use of tumour agnostic therapies, where the gaps in preparedness for taking advantage of this innovative approach to cancer therapy are sharply exposed. Europe should already have in place a guarantee of universal access to a minimum suite of biomarker tests and should be planning for an optimum testing scenario with a wider range of biomarker tests integrated into a more sophisticated health system articulated around personalised medicine. Improving healthcare and winning advantages for Europe’s industrial competitiveness and innovation require an appropriate policy framework—starting with an update to outdated recommendations. We show herein the main issues and proposals that emerged during the previous advisory boards organised by the European Alliance for Personalized Medicine which mainly focus on possible scenarios of harmonisation of both oncogenetic testing and management of cancer patients.

Published
2021

31. Droplet digital PCR for large genomic rearrangements detection: A promising strategy in tissue BRCA1 testing

Author

De Paolis, E., De Bonis, M., Concolino, Paola, Piermattei, Angelo, Fagotti, Anna, Urbani, Andrea, Scambia, Giovanni, Minucci, Angelo, Capoluongo, Ettore Domenico, Concolino P., Piermattei A. (ORCID:0000-0002-6835-1179), Fagotti A. (ORCID:0000-0001-5579-335X), Urbani A. (ORCID:0000-0001-9168-3174), Scambia G. (ORCID:0000-0003-2758-1063), Minucci A., Capoluongo E. (ORCID:0000-0001-9872-0572), De Paolis, E., De Bonis, M., Concolino, Paola, Piermattei, Angelo, Fagotti, Anna, Urbani, Andrea, Scambia, Giovanni, Minucci, Angelo, Capoluongo, Ettore Domenico, Concolino P., Piermattei A. (ORCID:0000-0002-6835-1179), Fagotti A. (ORCID:0000-0001-5579-335X), Urbani A. (ORCID:0000-0001-9168-3174), Scambia G. (ORCID:0000-0003-2758-1063), Minucci A., and Capoluongo E. (ORCID:0000-0001-9872-0572)

Abstract

Background and aims: With the introduction of Olaparib as target therapy for High Grade Serous Ovarian Cancer (HGSOC) patients with germline and somatic BRCA1/2 mutations, the genetic test performed on tumor tissue has become important like the germline test. In somatic testing the evaluation of Large Genomic Rearrangements (LGRs) represents the main challenge. We describe a droplet digital PCR (ddPCR) assay for the evaluation of target BRCA1 LGRs on blood and formalin-fixed paraffin-embedded (FFPE)/Fresh Frozen Tissue (FFT) samples. Materials and methods: We analyzed blood, FFPE and FFT samples in a validation setting of n = 78 HGSOC patients. We applied the ddPCR to BRCA1 exons 2, 20 and 21 as some of the most common BRCA1 exons involved in LGRs in our cohort of patients. Results: The ddPCR custom assays allowed the identification of LGRs in all sample types, including FFPE specimens. Moreover, we were able to clearly detect LGRs accounted as somatic event. Conclusion: The introduction of ddPCR in a comprehensive workflow, encompassing both germline and somatic tests, represents an improvement in BRCA1/2 testing. ddPCR can overcome challenges related to BRCA testing, especially on FFPE analysis. Finally, ddPCR represents a promising alternative strategy to the established standard methods currently used in clinical setting.

Published
2021

34. Recommendations for the implementation of BRCA1/2 testing in ovarian cancer patients: From tumor to germline analysis. Joint document from SIBioC, AIOM, SIGU, SIAPEC-IAP

Author

Barberis M., Bella M. A., Buttitta F., Capoluongo E., Carrera P., Colombo N., Cortesi L., Genuardi M., Gion M., Gori S., Guarneri V., Verde N. L., Lorusso D., Marchetti A., Marchetti P., Normanno N., Pasini B., Pensabene M., Pignata S., Radice P., Ricevuto E., Russo A., Sapino A., Tagliaferri P., Tassone P., Trevisiol C., Truini M., Varesco L., Barberis, M, Bella, M, Buttitta, F, Capoluongo, E, Carrera, P, Colombo, N, Cortesi, L, Genuardi, M, Gion, M, Gori, S, Guarneri, V, Verde, N, Lorusso, D, Marchetti, A, Marchetti, P, Normanno, N, Pasini, B, Pensabene, M, Pignata, S, Radice, P, Ricevuto, E, Russo, A, Sapino, A, Tagliaferri, P, Tassone, P, Trevisiol, C, Truini, M, and Varesco, L

Subjects
BRCA2 protein, BRCA1 protein
Abstract

Since the approval of the first poly adenosine diphosphate (ADP) ribose polymerase inhibitor (PARPi), olaparib for platinum-sensitive relapsed high grade ovarian cancer, with either germline or somatic BRCA1/2 deleterious variants, the strategies for BRCA1/2 testing are dynamically changing. In fact, along with germline assay, patients are now tested for tumor BRCA1/2 also above all for treatment decisions. In fact, it is reported as by tumor BRCA analysis we can identify 3–9% more mutated women which can therefore benefit from PARPi therapy. Although this new type of approach looks like challenging, in particular due to the technical and analytical difficulties regarding low quality DNA deriving from formalin-fixed paraffin-embedded specimens, the new CE-IVD on NGS-based pipelines, can overcome these issues, allowing specialized molecular laboratories to ensure high quality results and perform the best test settings. Nevertheless, each new NGS pipeline (CE-IVD or in house) should be validated using peculiar samples along with commercially available reference and certified materials, before being introduced in routine settings. The validation set should be appropriately chosen in order to provide unequivocal data regarding robustness of each NGS tBRCA pipeline. Therefore, in order to harmonize the patient and laboratory path, a group of Italian Scientific Societies [Italian Society of Clinical Chemistry (SIBioC), Italian Association of Medical Oncology (AIOM), Italian Association of Clinical Pathology (SIAPEC), Italian Society of Human Genetics (SIGU)] provided the present recommendations which are aimed to guide all professionals (oncologists, gynaecologists, clinical and laboratory geneticists, clinical molecular biologists and pathologists). The intersociety group is confident that the present paper can offer all ovarian cancer women a well-organized pathway of diagnosis and treatment.

Published
2019

35. Reccomendations for using of molecular assays on liquid biopsy: The first document provided by intersociety Group AIOM, SIF, SIAPEC-IAP, SIBioC

Author

Capoluongo E., Barberis M., Crino L., Danesi R., Re M. D., Gori S., Marchetti A., Marchio C., Normanno N., Pinto C., Russo A., Sapino A., Bianchi A. S., Truini M., Venesio T., Capoluongo E., Barberis M., Crino L., Danesi R., Re M.D., Gori S., Marchetti A., Marchio C., Normanno N., Pinto C., Russo A., Sapino A., Bianchi A.S., Truini M., and Venesio T.

Subjects
Liquid biopsy, Settore MED/06 - Oncologia Medica
Abstract

Liquid biopsy in cancer patients is mainly based on the analysis of circulating tumor DNA (ctDNA) enriched from biological fluids. This approach has more recently been proposed for the detection of oncogenic alterations in blood, cerebrospinal fluid (CSF), or urine through the use of sensitive technologies, mainly digital PCR (ddPCR) and massive parallel sequencing (MPS). Liquid biopsies have the advantage of overcoming some of the drawbacks associated with tumor biopsies, being blood samples easy to obtain from patients. Plasma ctDNA may better represent the total landscape of oncogenic alterations found across all tumor sites. Several commercially available liquid biopsy platforms based on MPS technology are currently analytically validated, with sensitivities, specificities, false negative rates, false positive rates, positive predictive values, and negative predictive values evaluated in comparison with tissue. The specificity of ctDNA is generally high while the sensitivity varies between different platforms. However, these data have not yet led to the incorporation of ctDNA into routine clinical practice. The present Reccomandation represents a synthesis of the main evidences supporting use of liquid biopsy based assays in clinical setting. This inter-society approved document was prepared by a panel of expert belonging to four scientific societies who tried to provide the main useful information for the implementation of liquid biopsy-based test in clinical and laboratory practice.

Published
2019

36. In silico investigation of the molecular effects caused by R123H variant in secretory phospholipase A2-IIA associated with ARDS

Author

Righino, B, Minucci, A, Pirolli, D, Capoluongo, E, Conti, G, De Luca, D, De Rosa, Mc, Pirolli, D (ORCID:0000-0003-2303-2577), Capoluongo, E (ORCID:0000-0001-9872-0572), Conti, G (ORCID:0000-0002-8566-9365), De Rosa, MC, Righino, B, Minucci, A, Pirolli, D, Capoluongo, E, Conti, G, De Luca, D, De Rosa, Mc, Pirolli, D (ORCID:0000-0003-2303-2577), Capoluongo, E (ORCID:0000-0001-9872-0572), Conti, G (ORCID:0000-0002-8566-9365), and De Rosa, MC

Abstract

Phospholipase A2-IIA catalyzes the hydrolysis of the sn-2 ester of glycerophospholipids. A rare c.428G > A (p.Arg143His) variant in PLA2G2A gene was found in two infants affected by acute respiratory distress syndrome (ARDS) by whole coding region and exon/intron boundaries sequencing. To obtain insights into the possible molecular effects of the rare R123H mutation in secretory PLA2-IIA (sPLA2-IIA), molecular modelling, molecular dynamics (MD) using principal component analysis (PCA) and continuum electrostatic calculations were conducted on the crystal structure of the wild type protein and on a generated model structure of the R123H mutant. Analysis of MD trajectories indicate that the overall stability of the protein is not affected by this mutation but nevertheless the catalytically crucial H -bond between Tyr51 and Asp91 as well as main electrostatic interactions in the region close to the mutation site are altered. PCA results indicate that the R123H replacement alter the internal molecular motions of the enzyme and that collective motions are increased. Electrostatic surface potential studies suggest that after mutation the interfacial binding to anionic phospholipid membranes and anionic proteins may be changed. The strengthening of electrostatic interactions may be propagated into the active site region thus potentially affecting the substrate recognition and enzymatic activity. Our findings provide the basis for further investigation and advances our understanding of the effects of mutations on sPLA2 structure and function.

Published
2018

37. Spectrum of germline BRCA1 and BRCA2 variants identified in 2351 ovarian and breast cancer patients referring to a reference cancer hospital of Rome

Author

Santonocito, Concetta, Rizza, Roberta, Paris, Ida, De Marchis, L., Paolillo, C., Tiberi, G., Scambia, Giovanni, Capoluongo, Ettore Domenico, Santonocito C. (ORCID:0000-0003-3624-1386), Rizza R., Paris I., Scambia G. (ORCID:0000-0003-2758-1063), Capoluongo E. (ORCID:0000-0001-9872-0572), Santonocito, Concetta, Rizza, Roberta, Paris, Ida, De Marchis, L., Paolillo, C., Tiberi, G., Scambia, Giovanni, Capoluongo, Ettore Domenico, Santonocito C. (ORCID:0000-0003-3624-1386), Rizza R., Paris I., Scambia G. (ORCID:0000-0003-2758-1063), and Capoluongo E. (ORCID:0000-0001-9872-0572)

Abstract

Pathogenic variants (PVs) carriers in BRCA1 or BRCA2 are associated with an elevated lifetime risk of developing breast cancer (BC) and/or ovarian cancer (OC). The prevalence of BRCA1 and BRCA2 germline alterations is extremely variable among different ethnic groups. Particularly, the rate of variants in Italian BC and/or OC families is rather controversial and ranges from 8% to 37%, according to different reports. By In Vitro Diagnostic (IVD) next generation sequencing (NGS)‐based pipelines, we routinely screened thousands of patients with either sporadic or cancer family history. By NGS, we identified new PVs and some variants of uncertain significance (VUS) which were also evaluated in silico using dedicated tools. We report in detail data regarding BRCA1/2 variants identified in 517 out of 2351 BC and OC patients. The aim of this study was to report the incidence and spectrum of BRCA1/2 variants observed in BC and/or OC patients, tested in at Policlinico Gemelli Foundation Hospital, the origin of which is mainly from Central and Southern Italy. This study provides an overview of the variant frequency in these geographic areas of Italy and provides data that could be used in the clinical management of patients.

Published
2020

38. BRCA testing delay during the COVID-19 pandemic: How to act?

Author

Minucci, Angelo, Scambia, Giovanni, De Bonis, M., De Paolis, E., Santonocito, Concetta, Fagotti, Anna, Capoluongo, Ettore Domenico, Concolino, Paola, Urbani, A., Minucci A., Scambia G. (ORCID:0000-0003-2758-1063), Santonocito C. (ORCID:0000-0003-3624-1386), Fagotti A. (ORCID:0000-0001-5579-335X), Capoluongo E. (ORCID:0000-0001-9872-0572), Concolino P., Minucci, Angelo, Scambia, Giovanni, De Bonis, M., De Paolis, E., Santonocito, Concetta, Fagotti, Anna, Capoluongo, Ettore Domenico, Concolino, Paola, Urbani, A., Minucci A., Scambia G. (ORCID:0000-0003-2758-1063), Santonocito C. (ORCID:0000-0003-3624-1386), Fagotti A. (ORCID:0000-0001-5579-335X), Capoluongo E. (ORCID:0000-0001-9872-0572), and Concolino P.

Abstract

Recently, our lab, part of a referral center in Italy, reported its experience regarding the execution of germline BRCA1/2 (gBRCA) testing during the first months of the coronavirus disease-2019 (COVID-19) pandemic, which highlights a substantial reduction (about 60%) compared with the first 2 months of the current year. This evidence appeared to be a lockdown effect due to extraordinary restriction measures to slow down the spread of SARS-CoV-2. In this study, we aimed to evaluate the overall effects of the ongoing pandemic on gBRCA testing in our institution and to understand how COVID-19 has influenced testing after the complete lockdown (March 8–May 5, 2020). Additionally, we compared this year’s trend with trends of the last 3 years to better monitor gBRCA testing progress. This detailed analysis highlights two important findings: (1) gBRCA testing did not increase significantly after the lockdown period (May–October 2020) compared with the lockdown period (March–April 2020), emphasizing that even after the lockdown period testing remained low. (2) Comparing the total tests per year (January–October 2017, 2018, 2019, with 2020), the impact of COVID-19 on gBRCA testing is apparent, with similarities of trends registered in 2017. These evidences reveal a gBRCA testing delay for cancer patients and healthy patients at this moment, and the new era of gBRCA testing in the management of ovarian, breast, pancreas and prostate cancer patients has been seriously questioned due to the COVID-19 pandemic. As consequence, we underline that measures to guarantee oncogenetic testing (e.g., gBRCA testing) along with new diagnostic/clinic strategies are mandatory. For these reasons, several proposals are presented in this study.

Published
2020

39. High resolution melting profiles (HRMPs) obtained by magnetic induction cycler (MIC) have been used to monitor the BRCA2 status highlighted by next generation tumor sequencing (NGTS): a combined approach in a diagnostic environment

Author

Mazzuccato, G., De Bonis, M., Carboni, V., Marchetti, Claudia, Urbani, Andrea, Scambia, Giovanni, Capoluongo, Ettore Domenico, Fagotti, Anna, Minucci, Angelo, Marchetti C. (ORCID:0000-0001-7098-8956), Urbani A. (ORCID:0000-0001-9168-3174), Scambia G. (ORCID:0000-0003-2758-1063), Capoluongo E. (ORCID:0000-0001-9872-0572), Fagotti A. (ORCID:0000-0001-5579-335X), Minucci A., Mazzuccato, G., De Bonis, M., Carboni, V., Marchetti, Claudia, Urbani, Andrea, Scambia, Giovanni, Capoluongo, Ettore Domenico, Fagotti, Anna, Minucci, Angelo, Marchetti C. (ORCID:0000-0001-7098-8956), Urbani A. (ORCID:0000-0001-9168-3174), Scambia G. (ORCID:0000-0003-2758-1063), Capoluongo E. (ORCID:0000-0001-9872-0572), Fagotti A. (ORCID:0000-0001-5579-335X), and Minucci A.

Abstract

Resistance can be the result of secondary tissue variants (STVs), which restore the open reading frame of the germline BRCA allele, producing functional BRCA protein in germline BRCA1/2 (BRCA) pathogenic variant (PV) carriers, treated with platinum-based chemotherapy or poly-(ADP-ribose) polymerase inhibitors (PARP-1). We reported recently a BRCA2 mutant high grade serous ovarian cancer (HGSOC) patient with acquired resistance to the PARP-1 olaparib due to a STV detected by next generation tumor sequencing (NGTS). The aim of this study was to evaluate the versatility of the high-resolution melting analysis (HRMA) obtained by magnetic induction cycler (MIC) to monitor the BRCA2 status in formalin-fixed paraffin-embedded (FFPE) tissue samples of this patient and to compare the results obtained by NGTS. HRMA highlighted the BRCA2 STV previously detected in the IIIrd HGSOC recurrence following the tissue BRCA2 tissue status comparing the high resolution melting profiles (HRMPs). HRMPs differentiate not only BRCA2 alleles, but also their different allele abundance. We underline that (1) the MIC uses a latest generation technology guaranteeing temperature uniformity and maintenance in each well allowing high and accurate performance to obtain reported results and (2) the HRMA maintains a high sensitivity and specificity when it is performed on FFPE samples. Finally, this study represents an additional use of the HRMA, confirming its extreme versatility in the diagnostic environment.

Published
2020

40. Feasibility of tumor testing for BRCA status in high-grade serous ovarian cancer using fresh-frozen tissue based approach

Author

Marchetti, Claudia, Minucci, Angelo, D'Indinosante, Marco, Ergasti, Raffaella, Arcieri, M., Capoluongo, Ettore Domenico, Pietragalla, A., Caricato, C., Scambia, Giovanni, Fagotti, Anna, Marchetti C. (ORCID:0000-0001-7098-8956), Minucci A., D'Indinosante M., Ergasti R., Capoluongo E. D. (ORCID:0000-0001-9872-0572), Scambia G. (ORCID:0000-0003-2758-1063), Fagotti A. (ORCID:0000-0001-5579-335X), Marchetti, Claudia, Minucci, Angelo, D'Indinosante, Marco, Ergasti, Raffaella, Arcieri, M., Capoluongo, Ettore Domenico, Pietragalla, A., Caricato, C., Scambia, Giovanni, Fagotti, Anna, Marchetti C. (ORCID:0000-0001-7098-8956), Minucci A., D'Indinosante M., Ergasti R., Capoluongo E. D. (ORCID:0000-0001-9872-0572), Scambia G. (ORCID:0000-0003-2758-1063), and Fagotti A. (ORCID:0000-0001-5579-335X)

Abstract

Objective: For many years, BRCA mutational status has only been considered as a predictor of ovarian cancer susceptibility and as a prognostic factor. Nonetheless, in the era of precision medicine, it has also become a predictive biomarker of response to platinum-based-chemotherapy and, more recently, to PARP-inhibitors, also in the frontline setting. We assessed the feasibility of a fresh frozen tissue-based-BRCA-screening workflow in a tertiary referral center. Methods: We consecutively enrolled a series of 456 newly diagnosed FIGO-Stage IIIC-IV, high grade serous-ovarian cancer patients. All patients receiving tumor-biopsy underwent tBRCA-testing. Results: Clinically relevant tissue-BRCA (tBRCA) variants were observed in 145 women (31.8%), particularly we recognized 89 (61.4%) patients with BRCA1-pathogenetic variants (PVs) and 56 women (38.6%) with BRCA2-PVs. Among 292 tBRCA wild-type (wt) patients, 88 cases were germline BRCA tested (gBRCA) and 86 (97.8%) were confirmed as gBRCAwt, while 1 (1.1%) had gBRCA variant of uncertain significance and 1 had gBRCA mutation (1.1%). The concordance of tumor test versus germline BRCA test was 86.3% (209/242). Large genomic rearrangements (LGRs) were suspected in 13/292 tBRCAwt patients (4.5%) by using bioinformatic algorithm and multiplex ligation-dependent probe amplification (MLPA) was performed, with evidence of PVs in only 1 case. Conclusions: Fresh-frozen tissue-based BRCA screening workflow is feasible and reliable. It allows to enlarge the BRCA mutated population that might receive PARPi with the greatest benefit, without missing cascade testing for family members and therefore, maintaining its preventive role.

Published
2020

41. A new founder BRCA1 haplotype identified in the Puglia region is associated with a specific age-related cancer onset in three unrelated families

Author

Capoluongo, E., De Matteis, E., Cucinotto, I., Ronzino, G., Santonocito, C., Tornesello, A., De Giorgio, M. R., Lucci Cordisco, E., Minucci, A., Genuardi, M., Santonocito C. (ORCID:0000-0003-3624-1386), Tornesello A. (ORCID:0000-0002-7485-7440), Lucci Cordisco E. (ORCID:0000-0002-6279-7604), Minucci A., Genuardi M. (ORCID:0000-0002-7410-8351), Capoluongo, E., De Matteis, E., Cucinotto, I., Ronzino, G., Santonocito, C., Tornesello, A., De Giorgio, M. R., Lucci Cordisco, E., Minucci, A., Genuardi, M., Santonocito C. (ORCID:0000-0003-3624-1386), Tornesello A. (ORCID:0000-0002-7485-7440), Lucci Cordisco E. (ORCID:0000-0002-6279-7604), Minucci A., and Genuardi M. (ORCID:0000-0002-7410-8351)

Abstract

No abstract available

Published
2020

42. Salvage lymphadenectomy in recurrent ovarian cancer patients: Analysis of clinical outcome and BRCA1/2 gene mutational status

Author

Gallotta, Valerio, Bruno, M, Conte, C, Giudice, Maria Teresa, Davià, F, Moro, F, Zannoni, Gian Franco, Fagotti, Anna, De Bonis, M, Capoluongo, E, Scambia, Giovanni, Ferrandina, Maria Gabriella, Gallotta, V, Giudice, M T, Zannoni, G F (ORCID:0000-0003-1809-129X), Fagotti, A (ORCID:0000-0001-5579-335X), Scambia, G (ORCID:0000-0003-2758-1063), Ferrandina, G (ORCID:0000-0003-4672-4197), Gallotta, Valerio, Bruno, M, Conte, C, Giudice, Maria Teresa, Davià, F, Moro, F, Zannoni, Gian Franco, Fagotti, Anna, De Bonis, M, Capoluongo, E, Scambia, Giovanni, Ferrandina, Maria Gabriella, Gallotta, V, Giudice, M T, Zannoni, G F (ORCID:0000-0003-1809-129X), Fagotti, A (ORCID:0000-0001-5579-335X), Scambia, G (ORCID:0000-0003-2758-1063), and Ferrandina, G (ORCID:0000-0003-4672-4197)

Abstract

BJECTIVE: This study is aimed to analyze the clinical outcome of recurrent ovarian cancer patients bearing isolated lymph-node recurrence (ILNR) who underwent salvage lymphadenectomy (SL). The prognostic role of clinicopathological variables and the mutational status of BRCA1/2 have also been investigated. METHODS: This retrospective, single-institutional study included women with platinum-sensitive lymph node recurrence underwent to SL between June 2008 and June 2018. Univariate and multivariate analysis was performed to evaluate the impact of clinical parameters, and BRCA1/2 mutational status on post salvage lymphadenectomy progression-free survival (PSL-PFS). RESULTS: As of June 2019, the median follow-up after SL was 30 months, and the relapse has been documented in 48 (56.5%) patients. In the whole series, the median PSL-PFS was 21 months, and the 3-year PSL-PFS was 36.7%. The median PSL-PFS, according to patients with ILNR (N = 71) versus patients with lymph-nodes and other sites of disease (N = 14), was 27 months versus 12 months, respectively. Univariate analysis of variables conditioning PSL-PFS showed that platinum-free interval (PFI) ≥12 months, normal Ca125 serum levels, and number of metastatic lymph-nodes ≤3 played a statistically significant favorable role. In multivariate analysis, PFI duration ≥12 months and the number of metastatic lymph nodes ≤3 were shown to keep their favorable, independent prognostic value on PSL-PFS. CONCLUSIONS: In the context of SL, the patients with long PFI and low metastatic lymph node numbers at ILNR diagnosis have the best outcome. The BRCA mutational status seems not associated with clinical variables and PSL-PFS, differently from other sites of disease in ROC patients.

Published
2020

46. BRCA screening among Jewish community of Rome

Author

De Marchis, L., primary, Minucci, A., additional, Gelibter, A., additional, Mazzuccato, G., additional, Magri, V., additional, Moscati, G., additional, Madaio, R., additional, Marchetti, P., additional, Urbani, A., additional, Cortesi, E., additional, and Capoluongo, E., additional

Published
2020
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49. A novel CYP24A1 genotype associated to a clinical picture of hypercalcemia, nephrolithiasis and low bone mass (vol 45, pg 291, 2016)

Author

Ferraro, Pm, Minucci, A, Primiano, A, De Paolis, E, Gervasoni, J, Persichilli, S, Naticchia, A, Capoluongo, E, Gambaro, G, Ferraro, PM (ORCID:0000-0002-1379-022X), Persichilli, S (ORCID:0000-0002-7955-8810), Capoluongo, E (ORCID:0000-0001-9872-0572), Gambaro, G (ORCID:0000-0001-5733-2370), Ferraro, Pm, Minucci, A, Primiano, A, De Paolis, E, Gervasoni, J, Persichilli, S, Naticchia, A, Capoluongo, E, Gambaro, G, Ferraro, PM (ORCID:0000-0002-1379-022X), Persichilli, S (ORCID:0000-0002-7955-8810), Capoluongo, E (ORCID:0000-0001-9872-0572), and Gambaro, G (ORCID:0000-0001-5733-2370)

Abstract

Mutations of the CYP24A1 gene, encoding for the enzyme 25(OH)D-24-hydroxylase, can cause hypercalcemia, hypercalciuria, nephrolithiasis and nephrocalcinosis. We report the case of a 22-year-old male patient with recurrent nephrolithiasis, nephrocalcinosis, hypercalcemia with low parathyroid hormone levels, hypercalciuria and low bone mass. Gene sequencing showed that the patient had compound heterozygous mutations including a novel genotype of the CYP24A1 gene. Genetic CYP24A1 testing and biochemical analyses were offered to other family members; the father was heterozygous for the same novel genotype and was also affected with recurrent nephrolithiasis.

Published
2017

50. Identification of twenty-nine novel germline unclassified variants of BRCA1 and BRCA2 genes in 1400 Italian individuals

Author

Santonocito, C, Scapaticci, M, Guarino, D, Bartolini, A, Minucci, A, Concolino, P, Scambia, G, Paris, I, Capoluongo, E., Santonocito, C (ORCID:0000-0003-3624-1386), Scambia, G (ORCID:0000-0003-2758-1063), Capoluongo, E. (ORCID:0000-0001-9872-0572), Santonocito, C, Scapaticci, M, Guarino, D, Bartolini, A, Minucci, A, Concolino, P, Scambia, G, Paris, I, Capoluongo, E., Santonocito, C (ORCID:0000-0003-3624-1386), Scambia, G (ORCID:0000-0003-2758-1063), and Capoluongo, E. (ORCID:0000-0001-9872-0572)

Abstract

Objectives: Breast and/or ovarian cancers are complex multifactorial diseases caused by interaction of both genetic and non-genetic factors and characterized by predisposition to inheritance. BRCA1 and BRCA2 genes are the most clinically involved with these kinds of cancer and the spectrum of variants affecting these genes is very wide. In fact, point variants, large or small insertions/deletions, genomic rearrangements can be found in these patients, although a large number of variants with uncertain biological and clinical significance continues to be identified. Next-generation sequencing (NGS) technology is actually the most powerful tool for the discovering of causative mutations and novel disease genes, moreover it allows to make a rapid diagnosis of genetic variants giving fast, inexpensive and detailed genetic information. Material and methods: In this study, we report the screening of BRCA1 and BRCA2 genes on 1400 consecutive Caucasian patients with breast and/or ovarian cancer history or family risk, attending the oncogenetic ambulatory at the Foundation Policlinico Agostino Gemelli in Rome. Results: We describe twenty-nine novel BRCA1 and BRCA2 variants detected in Italian individuals suffering from hereditary breast and ovarian cancer syndrome (HBOC). Conclusion: Data regarding novel variants can provide useful information not only at epidemiological but also at clinical level, allowing for the better managing of breast and ovarian cancer patients and their family members. (C) 2017 Elsevier Ltd. All rights reserved.

Published
2017

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