Your search keyword '"Fossati C."' showing total 23 results

1. Una coppia di codici: un Lucano del sec. XII e il poema di anonimo genovese sulla presa di Almeria del 1147

Author

Fossati, C., Losappio, D., Ferrari, Mirella, Ferrari, Mirella (ORCID:0000-0003-0195-9398), Fossati, C., Losappio, D., Ferrari, Mirella, and Ferrari, Mirella (ORCID:0000-0003-0195-9398)

Abstract

A MS of Lucan of the 12. century and the autograph copy of a poem on the capture of Almeria by Genoa in 1147, both in the Fondo Trotti of the Biblioteca Ambrosiana, show evidence to have been written in the same place, to be located in Spain, and then to have been kept adjacent until today.

Published

2024

2. I figli di Gian Galeazzo annunciano a Venceslao re dei Romani la morte del padre

Author

FOSSATI C, LOSAPPIO D, Monti, Carla Maria, MONTI CM (ORCID:0000-0001-8351-2471), FOSSATI C, LOSAPPIO D, Monti, Carla Maria, and MONTI CM (ORCID:0000-0001-8351-2471)

Abstract

La sera stessa della morte di Gian Galeazzo Visconti (3 sett. 1402), i figli Giovanni Maria e Filippo Maria, di quattordici e dieci anni, scrivono a Venceslao re dei Romani per assicurargli la fedeltà del ducato e porsi sotto la sua protezione in un momento politico che si preannuncia gravido di difficoltà. La lettera, stesa presumibilmente da un segretario, è un vero panegirico del duca, ritratto quale padre premuroso, cristiano devoto, fe- dele suddito di Venceslao, da cui nel 1395 aveva ricevuto il titolo ducale. È trasmessa da un unico testimone, Milano, Bibl. Ambrosiana, H 211 inf., che appartiene a un gruppo di codici definiti miscellanee cancelle- resche viscontee, realizzate attorno al terzo decennio del Quattrocento sotto la signoria di Filippo Maria Visconti. Ciò che caratterizza l’Ambro- siano è la forte presenza di testi legati all’affermazione del potere di Gian Galeazzo, alcuni dei quali trasmessi in attestazione unica. L’articolo offre edizione critica, traduzione e commento della lettera.

Published

2024

3. Endocrine, auxological and metabolic profile in children and adolescents with Down syndrome: from infancy to the first steps into adult life

Author

Molinari, S, Fossati, C, Nicolosi, M, Di Marco, S, Faraguna, M, Limido, F, Ocello, L, Pellegrinelli, C, Lattuada, M, Gazzarri, A, Lazzerotti, A, Sala, D, Vimercati, C, Capitoli, G, Daolio, C, Biondi, A, Balduzzi, A, Cattoni, A, Molinari, Silvia, Fossati, Chiara, Nicolosi, Maria Laura, Di Marco, Santo, Faraguna, Martha Caterina, Limido, Francesca, Ocello, Laura, Pellegrinelli, Claudia, Lattuada, Martina, Gazzarri, Alessandra, Lazzerotti, Alessandra, Sala, Debora, Vimercati, Chiara, Capitoli, Giulia, Daolio, Cecilia, Biondi, Andrea, Balduzzi, Adriana, Cattoni, Alessandro, Molinari, S, Fossati, C, Nicolosi, M, Di Marco, S, Faraguna, M, Limido, F, Ocello, L, Pellegrinelli, C, Lattuada, M, Gazzarri, A, Lazzerotti, A, Sala, D, Vimercati, C, Capitoli, G, Daolio, C, Biondi, A, Balduzzi, A, Cattoni, A, Molinari, Silvia, Fossati, Chiara, Nicolosi, Maria Laura, Di Marco, Santo, Faraguna, Martha Caterina, Limido, Francesca, Ocello, Laura, Pellegrinelli, Claudia, Lattuada, Martina, Gazzarri, Alessandra, Lazzerotti, Alessandra, Sala, Debora, Vimercati, Chiara, Capitoli, Giulia, Daolio, Cecilia, Biondi, Andrea, Balduzzi, Adriana, and Cattoni, Alessandro

Abstract

Down syndrome (DS) is the most common chromosomal disorder worldwide. Along with intellectual disability, endocrine disorders represent a remarkable share of the morbidities experienced by children, adolescents and young adults with DS. Auxological parameters are plotted on syndrome-specific charts, as growth rates are reduced compared to healthy age- and gender-matched peers. Furthermore, children with DS are at increased risk for thyroid dysfunctions, diabetes mellitus, osteopenia and obesity compared to general population. Additionally, male individuals with DS often show infertility, while women tend to experience menopause at an overall younger age than healthy controls. Given the recent outstanding improvements in the care of severe DS-related comorbidities, infant mortality has dramatically decreased, with a current average life expectancy exceeding 60 years. Accordingly, the awareness of the specificities of DS in this field is pivotal to timely detect endocrine dysfunctions and to undertake a prompt dedicated treatment. Notably, best practices for the screening and monitoring of pediatric endocrine disorders in DS are still controversial. In addition, specific guidelines for the management of metabolic issues along the challenging period of transitioning from pediatric to adult health care are lacking. By performing a review of published literature, we highlighted the issues specifically involving children and adolescent with DS, aiming at providing clinicians with a detailed up-to-date overview of the endocrine, metabolic and auxological disorders in this selected population, with an additional focus on the management of patients in the critical phase of the transitioning from childhood to adult care.

Published

2024

4. THYROID FUNCTION DISORDERS IN THE CHILD AND ADOLESCENT WITH TRISOMY 21

Author

Molinari, S, Fossati, C, Gazzarri, A, Lazzerotti, A, Barzaghi, S, Ocello, L, Grimaldi, C, Nicolosi, M, Biondi, A, Cattoni, A, Molinari S., Fossati C., Gazzarri A., Lazzerotti A., Barzaghi S., Ocello L., Grimaldi C., Nicolosi M. L., Biondi A., Cattoni A., Molinari, S, Fossati, C, Gazzarri, A, Lazzerotti, A, Barzaghi, S, Ocello, L, Grimaldi, C, Nicolosi, M, Biondi, A, Cattoni, A, Molinari S., Fossati C., Gazzarri A., Lazzerotti A., Barzaghi S., Ocello L., Grimaldi C., Nicolosi M. L., Biondi A., and Cattoni A.

Abstract

Thyroid function disorders are the most frequently detected medical complication among patients with trisomy 21, with a reported prevalence ranging from 4-8% in childhood to 50% or more in adulthood. Over 1% of newborns with Down syndrome show clinical and/or biochemical signs consistent with congenital hypothyroidism, which is generally promptly identified by means of the neonatal screening. 30% of patients are diagnosed with transient congenital hypothyroidism, while 70% show a lifelong need for hormonal replacement therapy with levothyroxine. Moreover, non-autoimmune subclinical hypothyroidism is the most frequent finding, with reported prevalence ranging from 23 to 60%. It is still controversial whether subclinical hypothyroidism can be labelled as a pathological condition or the expression of a mere asymptomatic upwards shift of TSH, with no clinical impact. In addition, syndrome-related abnormalities in the mechanisms underlying immune tolerance result in a greater occurrence of autoimmune disorders. Graves’ disease and autoimmune hypothyroidism in Hashimoto thyroiditis are experienced by almost 30% of patients with trisomy 21. Finally, it is frequent that the latter clinical picture switches into hyperthyroidism and vice versa in an unpredictable clinical continuum. Given the increased lifelong risk of experiencing thyroid function disorders in children and adolescents with trisomy 21, a systematic periodic clinical and biochemical assessment is recommended to promptly detect and possibly treat pathological conditions.

Published

2023

5. Thyroid Function Tests in Children and Adolescents with Trisomy 21: Definition of Syndrome-Specific Reference Ranges

Author

Cattoni, A, Molinari, S, Capitoli, G, Masera, N, Nicolosi, M, Barzaghi, S, Marziali, G, Lazzerotti, A, Gazzarri, A, Vimercati, C, Sala, D, Biondi, A, Galimberti, S, Fossati, C, Cattoni, Alessandro, Molinari, Silvia, Capitoli, Giulia, Masera, Nicoletta, Nicolosi, Maria Laura, Barzaghi, Silvia, Marziali, Giulia, Lazzerotti, Alessandra, Gazzarri, Alessandra, Vimercati, Chiara, Sala, Debora, Biondi, Andrea, Galimberti, Stefania, Fossati, Chiara, Cattoni, A, Molinari, S, Capitoli, G, Masera, N, Nicolosi, M, Barzaghi, S, Marziali, G, Lazzerotti, A, Gazzarri, A, Vimercati, C, Sala, D, Biondi, A, Galimberti, S, Fossati, C, Cattoni, Alessandro, Molinari, Silvia, Capitoli, Giulia, Masera, Nicoletta, Nicolosi, Maria Laura, Barzaghi, Silvia, Marziali, Giulia, Lazzerotti, Alessandra, Gazzarri, Alessandra, Vimercati, Chiara, Sala, Debora, Biondi, Andrea, Galimberti, Stefania, and Fossati, Chiara

Abstract

CONTEXT: The lack of syndrome-specific reference ranges for thyroid function tests (TFT) among pediatric patients with Down syndrome (DS) results in an overestimation of the occurrence of hypothyroidism in this population. OBJECTIVE: To (a) outline the age-dependent distribution of TFT among pediatric patients with DS; (b) describe the intraindividual variability of TFT over time; and (c) assess the role of elevated thyrotropin (TSH) in predicting the future onset of overt hypothyroidism. METHODS: In this retrospective, monocentric, observational analysis, we included 548 patients with DS (0-18 years) longitudinally assessed between 1992 and 2022. Exclusion criteria were abnormal thyroid anatomy, treatments affecting TFT, and positive thyroid autoantibodies. RESULTS: We determined the age-dependent distribution of TSH, FT3, and FT4 and outlined the relative nomograms for children with DS. Compared with non-syndromic patients, median TSH levels were statistically greater at any age (P < .001). Median FT3 and FT4 levels were statistically lower than controls (P < .001) only in specific age classes (0-11 for FT3, 11-18 years for FT4). TSH levels showed a remarkable fluctuation over time, with a poor (23%-53%) agreement between the TSH centile classes at 2 sequential assessments. Finally, the 75th centile was the threshold above which TSH values predicted future evolution into overt hypothyroidism with the best statistical accuracy, with a satisfactory negative predictive value (0.91), but poor positive predictive value (0.15). CONCLUSION: By longitudinally assessing TFT in a wide pediatric DS population, we outlined the syndrome-specific reference nomograms for TSH, FT3, and FT4 and demonstrated a persistent upward shift of TSH compared to non-syndromic children.

Published

2023

6. Children with special health care needs attending emergency department in Italy: analysis of 3479 cases

Author

Cianci, P, D'Apolito, V, Moretti, A, Barbagallo, M, Paci, S, Carbone, M, Lubrano, R, Urbino, A, Dionisi Vici, C, Memo, L, Zampino, G, La Marca, G, Villani, A, Corsello, G, Selicorni, A, Campania, A, Geremia, C, Castagno, E, Masi, S, Poggi, G, Vestri, M, Fossali, E, Rocchi, A, Dadalt, L, Arrighini, A, Chiappa, S, Renna, S, Piccotti, E, Borgna, C, Govoni, M, Biondi, A, Fossati, C, Iughetti, L, Bertolani, P, Salvatoni, A, Agosti, M, Fuca, F, Ilardi, A, Giuffrida, S, Diguardo, V, Boni, S, D'Antiga, L, Ruggeri, M, Chiaretti, A, Amarri, S, Peduto, A, Bernardi, F, Corsini, I, Deangelis, G, Ruberto, C, Zuccotti, G, Stringhi, C, Lombardi, G, Salladini, C, Dimichele, S, Parola, L, Porta, A, Biasucci, G, Bellini, M, Ortisi, M, Apuril, E, Midulla, F, Tarani, L, Parlapiano, G, Lietti, D, Sforzini, C, Marseglia, G, Savasta, S, Falsaperla, R, Vitaliti, M, Chiarelli, F, Rossi, N, Banderali, G, Giacchero, R, Bernardo, L, Pinto, F, Fabiani, E, Ficcadenti, A, Pellegrini, G, Giacoma, S, Biban, P, Spada, S, Tipo, V, Ghitti, C, Bolognini, S, Mariani, G, Russo, A, Colella, M, Verrico, A, Bruni, P, Poddighe, D, Cagnoli, G, Morandi, F, Gadaleta, A, Barbi, E, Bruno, I, Graziano, R, Sgaramella, P, Catalani, M, Baldoni, I, Colarusso, G, Galvagno, G, Barone, A, Longo, A, Nardella, G, Portale, G, Garigali, G, Bona, G, Erbela, M, Agostiniani, R, Nanni, L, Schieven, E, Dona, M, Varisco, T, Russo, F, Distefano, V, Dipietro, F, Tarallo, L, Imperato, L, Parisi, G, Salzano, R, Raiola, G, Talarico, V, Bellu, R, Cannone, A, Ferrante, P, Cianci P., D'Apolito V., Moretti A., Barbagallo M., Paci S., Carbone M. T., Lubrano R., Urbino A., Dionisi Vici C., Memo L., Zampino G., La Marca G., Villani A., Corsello G., Selicorni A., Campania A., Geremia C., Castagno E., Masi S., Poggi G., Vestri M., Fossali E., Rocchi A., DaDalt L., Arrighini A., Chiappa S., Renna S., Piccotti E., Borgna C., Govoni M. R., Biondi A., Fossati C., Iughetti L., Bertolani P., Salvatoni A., Agosti M., Fuca F., Ilardi A., Giuffrida S., DiGuardo V., Boni S., D'Antiga L., Ruggeri M., Chiaretti A., Amarri S., Peduto A., Bernardi F., Corsini I., DeAngelis G. L., Ruberto C., Zuccotti G. V., Stringhi C., Lombardi G., Salladini C., DiMichele S., Parola L., Porta A., Biasucci G., Bellini M., Ortisi M. T., Apuril E., Midulla F., Tarani L., Parlapiano G., Lietti D., Sforzini C., Marseglia G. L., Savasta S., Falsaperla R., Vitaliti M. C., Chiarelli F., Rossi N., Banderali G., Giacchero R., Bernardo L., Pinto F., Fabiani E., Ficcadenti A., Pellegrini G., Giacoma S., Biban P., Spada S., Tipo V., Ghitti C., Bolognini S., Mariani G., Russo A., Colella M. G., Verrico A., Bruni P., Poddighe D., Cagnoli G., Morandi F., Gadaleta A., Barbi E., Bruno I. I., Graziano R., Sgaramella P., Catalani M. P., Baldoni I., Colarusso G., Galvagno G., Barone A. P., Longo A., Nardella G., Portale G., Garigali G., Bona G., Erbela M., Agostiniani R., Nanni L., Schieven E., Dona M., Varisco T., Russo F., DiStefano V. A., DiPietro F., Tarallo L., Imperato L., Parisi G., Salzano R., Raiola G., Talarico V., Bellu R., Cannone A., Ferrante P., Cianci, P, D'Apolito, V, Moretti, A, Barbagallo, M, Paci, S, Carbone, M, Lubrano, R, Urbino, A, Dionisi Vici, C, Memo, L, Zampino, G, La Marca, G, Villani, A, Corsello, G, Selicorni, A, Campania, A, Geremia, C, Castagno, E, Masi, S, Poggi, G, Vestri, M, Fossali, E, Rocchi, A, Dadalt, L, Arrighini, A, Chiappa, S, Renna, S, Piccotti, E, Borgna, C, Govoni, M, Biondi, A, Fossati, C, Iughetti, L, Bertolani, P, Salvatoni, A, Agosti, M, Fuca, F, Ilardi, A, Giuffrida, S, Diguardo, V, Boni, S, D'Antiga, L, Ruggeri, M, Chiaretti, A, Amarri, S, Peduto, A, Bernardi, F, Corsini, I, Deangelis, G, Ruberto, C, Zuccotti, G, Stringhi, C, Lombardi, G, Salladini, C, Dimichele, S, Parola, L, Porta, A, Biasucci, G, Bellini, M, Ortisi, M, Apuril, E, Midulla, F, Tarani, L, Parlapiano, G, Lietti, D, Sforzini, C, Marseglia, G, Savasta, S, Falsaperla, R, Vitaliti, M, Chiarelli, F, Rossi, N, Banderali, G, Giacchero, R, Bernardo, L, Pinto, F, Fabiani, E, Ficcadenti, A, Pellegrini, G, Giacoma, S, Biban, P, Spada, S, Tipo, V, Ghitti, C, Bolognini, S, Mariani, G, Russo, A, Colella, M, Verrico, A, Bruni, P, Poddighe, D, Cagnoli, G, Morandi, F, Gadaleta, A, Barbi, E, Bruno, I, Graziano, R, Sgaramella, P, Catalani, M, Baldoni, I, Colarusso, G, Galvagno, G, Barone, A, Longo, A, Nardella, G, Portale, G, Garigali, G, Bona, G, Erbela, M, Agostiniani, R, Nanni, L, Schieven, E, Dona, M, Varisco, T, Russo, F, Distefano, V, Dipietro, F, Tarallo, L, Imperato, L, Parisi, G, Salzano, R, Raiola, G, Talarico, V, Bellu, R, Cannone, A, Ferrante, P, Cianci P., D'Apolito V., Moretti A., Barbagallo M., Paci S., Carbone M. T., Lubrano R., Urbino A., Dionisi Vici C., Memo L., Zampino G., La Marca G., Villani A., Corsello G., Selicorni A., Campania A., Geremia C., Castagno E., Masi S., Poggi G., Vestri M., Fossali E., Rocchi A., DaDalt L., Arrighini A., Chiappa S., Renna S., Piccotti E., Borgna C., Govoni M. R., Biondi A., Fossati C., Iughetti L., Bertolani P., Salvatoni A., Agosti M., Fuca F., Ilardi A., Giuffrida S., DiGuardo V., Boni S., D'Antiga L., Ruggeri M., Chiaretti A., Amarri S., Peduto A., Bernardi F., Corsini I., DeAngelis G. L., Ruberto C., Zuccotti G. V., Stringhi C., Lombardi G., Salladini C., DiMichele S., Parola L., Porta A., Biasucci G., Bellini M., Ortisi M. T., Apuril E., Midulla F., Tarani L., Parlapiano G., Lietti D., Sforzini C., Marseglia G. L., Savasta S., Falsaperla R., Vitaliti M. C., Chiarelli F., Rossi N., Banderali G., Giacchero R., Bernardo L., Pinto F., Fabiani E., Ficcadenti A., Pellegrini G., Giacoma S., Biban P., Spada S., Tipo V., Ghitti C., Bolognini S., Mariani G., Russo A., Colella M. G., Verrico A., Bruni P., Poddighe D., Cagnoli G., Morandi F., Gadaleta A., Barbi E., Bruno I. I., Graziano R., Sgaramella P., Catalani M. P., Baldoni I., Colarusso G., Galvagno G., Barone A. P., Longo A., Nardella G., Portale G., Garigali G., Bona G., Erbela M., Agostiniani R., Nanni L., Schieven E., Dona M., Varisco T., Russo F., DiStefano V. A., DiPietro F., Tarallo L., Imperato L., Parisi G., Salzano R., Raiola G., Talarico V., Bellu R., Cannone A., and Ferrante P.

Abstract

Background: Although children with special health care needs (CSHCN) represent a minority of the population, they go through more hospitalizations, more admissions to the Emergency Department (ED), and receive a major number of medical prescriptions, in comparison to general pediatric population. Objectives of the study were to determine the reasons for admission to the ED in Italian CSHCN, and to describe the association between patient’s demographic data, clinical history, and health services requirements. Methods: Ad hoc web site was created to collect retrospective data of 3479 visits of CSHCN to the ED in 58 Italian Hospitals. Results: Seventy-two percent of patients admitted to ED were affected by a previously defined medical condition. Most of the ED admissions were children with syndromic conditions (54%). 44.2% of the ED admissions were registered during the night-time and/or at the weekends. The hospitalization rate was of 45.6% among patients admitted to the ED. The most common reason for admission to the ED was the presence of respiratory symptoms (26.6%), followed by gastrointestinal problems (21.3%) and neurological disorders (18.2%). 51.4% of the access were classified as ‘urgent’, with a red/yellow triage code. Considering the type of ED, 61.9% of the visits were conducted at the Pediatric EDs (PedEDs), 33.5% at the Functional EDs (FunEDs) and 4.6% at the Dedicated EDs (DedEDs). Patients with more complex clinical presentation were more likely to be evaluated at the PedEDs. CSHCN underwent to a higher number of medical procedures at the PedEDs, more in comparison to other EDs. Children with medical devices were directed to a PedED quite exclusively when in need for medical attention. Subjects under multiple anti-epileptic drug therapy attended to PedEDs or FunEDs generally. Patients affected by metabolic diseases were more likely to look for medical attention at FunEDs. Syndromic patients mostly required medical attention at the DedEDs. Conclusions

Published

2020

7. Response to the United Nations Human Rights Council's Report on Race and Gender Discrimination in Sport: An Expression of Concern and a Call to Prioritise Research

Author

Hamilton, BR, Martinez-Patino, MJ, Barrett, J, Seal, L, Tucker, R, Papadopoulou, T, Bigard, X, Kolliari-Turner, A, Lollgen, H, Zupet, P, Ionescu, A, Debruyne, A, Jones, N, Steinacker, JM, Vonbank, K, Lima, G, Fagnani, F, Fossati, C, Di Luigi, L, Pigozzi, F, Casasco, M, Geistlinger, M, Wolfarth, B, Seto, JT, Bachl, N, Twycross-Lewis, R, Niederseer, D, Bosch, A, Swart, J, Constantinou, D, Muniz-Pardos, B, Casajus, JA, Badtieva, V, Zelenkova, I, Bilzon, JLJ, Dohi, M, Schneider, C, Loland, S, Verroken, M, Marqueta, PM, Arroyo, F, Pedrinelli, A, Natsis, K, Verhagen, E, Roberts, WO, Lazzoli, JK, Friedman, R, Erdogan, A, Cintron, AV, Yung, S-HP, van Rensburg, DCJ, Ramagole, DA, Rozenstoka, S, Drummond, F, Webborn, N, Guppy, FM, Pitsiladis, YP, Hamilton, BR, Martinez-Patino, MJ, Barrett, J, Seal, L, Tucker, R, Papadopoulou, T, Bigard, X, Kolliari-Turner, A, Lollgen, H, Zupet, P, Ionescu, A, Debruyne, A, Jones, N, Steinacker, JM, Vonbank, K, Lima, G, Fagnani, F, Fossati, C, Di Luigi, L, Pigozzi, F, Casasco, M, Geistlinger, M, Wolfarth, B, Seto, JT, Bachl, N, Twycross-Lewis, R, Niederseer, D, Bosch, A, Swart, J, Constantinou, D, Muniz-Pardos, B, Casajus, JA, Badtieva, V, Zelenkova, I, Bilzon, JLJ, Dohi, M, Schneider, C, Loland, S, Verroken, M, Marqueta, PM, Arroyo, F, Pedrinelli, A, Natsis, K, Verhagen, E, Roberts, WO, Lazzoli, JK, Friedman, R, Erdogan, A, Cintron, AV, Yung, S-HP, van Rensburg, DCJ, Ramagole, DA, Rozenstoka, S, Drummond, F, Webborn, N, Guppy, FM, and Pitsiladis, YP

Published

2021

8. Children with special health care needs attending emergency department in Italy: analysis of 3479 cases

Author

Cianci, P., D'Apolito, V., Moretti, A., Barbagallo, M., Paci, S., Carbone, M. T., Lubrano, R., Urbino, A., Dionisi Vici, Carlo, Memo, L., Zampino, Giuseppe, La Marca, G., Villani, Andrea, Corsello, G., Selicorni, A., Campania, A., Geremia, C., Castagno, Emanuele, Masi, S., Poggi, G., Vestri, M., Fossali, E., Rocchi, A., Dadalt, L., Arrighini, A., Chiappa, S., Renna, S., Piccotti, E., Borgna, C., Govoni, M. R., Biondi, Alberto, Fossati, C., Iughetti, L., Bertolani, P., Salvatoni, A., Agosti, M., Fuca, F., Ilardi, A., Giuffrida, S., Diguardo, V., Boni, S., D'Antiga, L., Ruggeri, M., Chiaretti, Antonio, Amarri, S., Peduto, A., Bernardi, F., Corsini, I., Deangelis, G. L., Ruberto, C., Zuccotti, G. V., Stringhi, C., Lombardi, Gianmarco, Salladini, C., Dimichele, S., Parola, L., Porta, Anita Maria, Biasucci, G., Bellini, M., Ortisi, M. T., Apuril, E., Midulla, F., Tarani, L., Parlapiano, G., Lietti, D., Sforzini, C., Marseglia, G. L., Savasta, S., Falsaperla, R., Vitaliti, M. C., Chiarelli, F., Rossi, N., Banderali, G., Giacchero, R., Bernardo, Letizia, Pinto, Francesco, Fabiani, Emiliano, Ficcadenti, A., Pellegrini, Maria Grazia, Giacoma, S., Biban, P., Spada, S., Tipo, V., Ghitti, Carla, Bolognini, Silvia, Mariani, G., Russo, A., Colella, M. G., Verrico, A., Bruni, P., Poddighe, D., Cagnoli, G., Morandi, Federica, Gadaleta, A., Barbi, E., Bruno, I. I., Graziano, R., Sgaramella, P., Catalani, M. P., Baldoni, I., Colarusso, G., Galvagno, G., Barone, A. P., Longo, A., Nardella, G., Portale, G., Garigali, G., Bona, G., Erbela, M., Agostiniani, R., Nanni, Lorenzo, Schieven, E., Dona, M., Varisco, T., Russo, F., Distefano, V. A., Dipietro, F., Tarallo, L., Imperato, L., Parisi, G., Salzano, R., Raiola, G., Talarico, V., Bellu, R., Cannone, A., Ferrante, P., Dionisi Vici C., Zampino G. (ORCID:0000-0003-3865-3253), Villani A., Castagno E., Biondi A. (ORCID:0000-0002-2470-7858), Chiaretti A. (ORCID:0000-0002-9971-1640), Lombardi G., Porta A., Bernardo L., Pinto F., Fabiani E. (ORCID:0000-0002-6209-8934), Pellegrini G., Ghitti C., Bolognini S., Morandi F. (ORCID:0000-0002-8218-4602), Nanni L. (ORCID:0000-0003-2569-8583), Cianci, P., D'Apolito, V., Moretti, A., Barbagallo, M., Paci, S., Carbone, M. T., Lubrano, R., Urbino, A., Dionisi Vici, Carlo, Memo, L., Zampino, Giuseppe, La Marca, G., Villani, Andrea, Corsello, G., Selicorni, A., Campania, A., Geremia, C., Castagno, Emanuele, Masi, S., Poggi, G., Vestri, M., Fossali, E., Rocchi, A., Dadalt, L., Arrighini, A., Chiappa, S., Renna, S., Piccotti, E., Borgna, C., Govoni, M. R., Biondi, Alberto, Fossati, C., Iughetti, L., Bertolani, P., Salvatoni, A., Agosti, M., Fuca, F., Ilardi, A., Giuffrida, S., Diguardo, V., Boni, S., D'Antiga, L., Ruggeri, M., Chiaretti, Antonio, Amarri, S., Peduto, A., Bernardi, F., Corsini, I., Deangelis, G. L., Ruberto, C., Zuccotti, G. V., Stringhi, C., Lombardi, Gianmarco, Salladini, C., Dimichele, S., Parola, L., Porta, Anita Maria, Biasucci, G., Bellini, M., Ortisi, M. T., Apuril, E., Midulla, F., Tarani, L., Parlapiano, G., Lietti, D., Sforzini, C., Marseglia, G. L., Savasta, S., Falsaperla, R., Vitaliti, M. C., Chiarelli, F., Rossi, N., Banderali, G., Giacchero, R., Bernardo, Letizia, Pinto, Francesco, Fabiani, Emiliano, Ficcadenti, A., Pellegrini, Maria Grazia, Giacoma, S., Biban, P., Spada, S., Tipo, V., Ghitti, Carla, Bolognini, Silvia, Mariani, G., Russo, A., Colella, M. G., Verrico, A., Bruni, P., Poddighe, D., Cagnoli, G., Morandi, Federica, Gadaleta, A., Barbi, E., Bruno, I. I., Graziano, R., Sgaramella, P., Catalani, M. P., Baldoni, I., Colarusso, G., Galvagno, G., Barone, A. P., Longo, A., Nardella, G., Portale, G., Garigali, G., Bona, G., Erbela, M., Agostiniani, R., Nanni, Lorenzo, Schieven, E., Dona, M., Varisco, T., Russo, F., Distefano, V. A., Dipietro, F., Tarallo, L., Imperato, L., Parisi, G., Salzano, R., Raiola, G., Talarico, V., Bellu, R., Cannone, A., Ferrante, P., Dionisi Vici C., Zampino G. (ORCID:0000-0003-3865-3253), Villani A., Castagno E., Biondi A. (ORCID:0000-0002-2470-7858), Chiaretti A. (ORCID:0000-0002-9971-1640), Lombardi G., Porta A., Bernardo L., Pinto F., Fabiani E. (ORCID:0000-0002-6209-8934), Pellegrini G., Ghitti C., Bolognini S., Morandi F. (ORCID:0000-0002-8218-4602), and Nanni L. (ORCID:0000-0003-2569-8583)

Abstract

Background: Although children with special health care needs (CSHCN) represent a minority of the population, they go through more hospitalizations, more admissions to the Emergency Department (ED), and receive a major number of medical prescriptions, in comparison to general pediatric population. Objectives of the study were to determine the reasons for admission to the ED in Italian CSHCN, and to describe the association between patient’s demographic data, clinical history, and health services requirements. Methods: Ad hoc web site was created to collect retrospective data of 3479 visits of CSHCN to the ED in 58 Italian Hospitals. Results: Seventy-two percent of patients admitted to ED were affected by a previously defined medical condition. Most of the ED admissions were children with syndromic conditions (54%). 44.2% of the ED admissions were registered during the night-time and/or at the weekends. The hospitalization rate was of 45.6% among patients admitted to the ED. The most common reason for admission to the ED was the presence of respiratory symptoms (26.6%), followed by gastrointestinal problems (21.3%) and neurological disorders (18.2%). 51.4% of the access were classified as ‘urgent’, with a red/yellow triage code. Considering the type of ED, 61.9% of the visits were conducted at the Pediatric EDs (PedEDs), 33.5% at the Functional EDs (FunEDs) and 4.6% at the Dedicated EDs (DedEDs). Patients with more complex clinical presentation were more likely to be evaluated at the PedEDs. CSHCN underwent to a higher number of medical procedures at the PedEDs, more in comparison to other EDs. Children with medical devices were directed to a PedED quite exclusively when in need for medical attention. Subjects under multiple anti-epileptic drug therapy attended to PedEDs or FunEDs generally. Patients affected by metabolic diseases were more likely to look for medical attention at FunEDs. Syndromic patients mostly required medical attention at the DedEDs. Conclusions

Published

2020

9. Nissen fundoplication in Cornelia de Lange syndrome spectrum: Who are the potential candidates?

Author

Parma, B., Cianci, P., Mariani, M., Cereda, Ambrogia, Panceri, R., Fossati, C., Maestri, L., Macchini, F., Onesimo, Roberta, Zampino, Giuseppe, Betalli, P., Cheli, M., Selicorni, A., Cereda A., Onesimo R., Zampino G. (ORCID:0000-0003-3865-3253), Parma, B., Cianci, P., Mariani, M., Cereda, Ambrogia, Panceri, R., Fossati, C., Maestri, L., Macchini, F., Onesimo, Roberta, Zampino, Giuseppe, Betalli, P., Cheli, M., Selicorni, A., Cereda A., Onesimo R., and Zampino G. (ORCID:0000-0003-3865-3253)

Abstract

Cornelia de Lange spectrum (CdLSp) is a rare genetic condition characterized by intellectual disability, facial dysmorphisms, major malformations, growth impairment, and development delay. Approximately 80% of CdLSp patients have gastroesophageal reflux disease (GERD) with a varied clinical presentation. The aim of this study is to define potential clinical/genetic risk factors based on the clinical phenotype description of CdLSp patients with severe GERD who underwent surgical treatment. We retrospectively collected data from 23 CdLSp patients, 13 females and 10 males. Mean age of the patients undergoing surgical treatment was of 4 years. 21/23 (91%) had a molecular characterization, of which 21/21 (100%) had a NIPBL gene mutation, while 2/23 (9%) did not have a genetical characterization, only a clinical diagnosis. Most of our patients presented a moderate–severe severity score (21/23, 91%) with limb malformations evidenced in 10/23 (44%) of our patients and a moderate–severe intellectual disability in 20/23 (87%). Therefore, CdLSp patients harboring NIPBL variants, upper limb malformations and severe psychomotor delay are more likely to suffer from severe GERD, not responsive to proton pump inhibitors treatment. These features should be considered as clinical markers for potentially severe GERD that might require surgical treatment.

Published

2020

10. Lentiviral haemopoietic stem/progenitor cell gene therapy for treatment of Wiskott-Aldrich syndrome: interim results of a non-randomised, open-label, phase 1/2 clinical study

Author

Ferrua, F, Cicalese, M, Galimberti, S, Giannelli, S, Dionisio, F, Barzaghi, F, Migliavacca, M, Bernardo, M, Calbi, V, Assanelli, A, Facchini, M, Fossati, C, Albertazzi, E, Scaramuzza, S, Brigida, I, Scala, S, Basso-Ricci, L, Pajno, R, Casiraghi, M, Canarutto, D, Salerio, F, Albert, M, Bartoli, A, Wolf, H, Fiori, R, Silvani, P, Gattillo, S, Villa, A, Biasco, L, Dott, C, Culme-Seymour, E, van Rossem, K, Atkinson, G, Valsecchi, M, Roncarolo, M, Ciceri, F, Naldini, L, Aiuti, A, Cicalese, MP, Bernardo, ME, Assanelli, AA, Albert, MH, Wolf, HM, Fiori, Rossan, Culme-Seymour, EJ, Valsecchi, MG, Roncarolo, MG, Ferrua, F, Cicalese, M, Galimberti, S, Giannelli, S, Dionisio, F, Barzaghi, F, Migliavacca, M, Bernardo, M, Calbi, V, Assanelli, A, Facchini, M, Fossati, C, Albertazzi, E, Scaramuzza, S, Brigida, I, Scala, S, Basso-Ricci, L, Pajno, R, Casiraghi, M, Canarutto, D, Salerio, F, Albert, M, Bartoli, A, Wolf, H, Fiori, R, Silvani, P, Gattillo, S, Villa, A, Biasco, L, Dott, C, Culme-Seymour, E, van Rossem, K, Atkinson, G, Valsecchi, M, Roncarolo, M, Ciceri, F, Naldini, L, Aiuti, A, Cicalese, MP, Bernardo, ME, Assanelli, AA, Albert, MH, Wolf, HM, Fiori, Rossan, Culme-Seymour, EJ, Valsecchi, MG, and Roncarolo, MG

Abstract

Background: Wiskott-Aldrich syndrome is a rare, life-threatening, X-linked primary immunodeficiency characterised by microthrombocytopenia, infections, eczema, autoimmunity, and malignant disease. Lentiviral vector-mediated haemopoietic stem/progenitor cell (HSPC)gene therapy is a potentially curative treatment that represents an alternative to allogeneic HSPC transplantation. Here, we report safety and efficacy data from an interim analysis of patients with severe Wiskott-Aldrich syndrome who received lentiviral vector-derived gene therapy. Methods: We did a non-randomised, open-label, phase 1/2 clinical study in paediatric patients with severe Wiskott-Aldrich syndrome, defined by either WAS gene mutation or absent Wiskott-Aldrich syndrome protein (WASP)expression or a Zhu clinical score of 3 or higher. We included patients who had no HLA-identical sibling donor available or, for children younger than 5 years of age, no suitable 10/10 matched unrelated donor or 6/6 unrelated cord blood donor. After treatment with rituximab and a reduced-intensity conditioning regimen of busulfan and fludarabine, patients received one intravenous infusion of autologous CD34+ cells genetically modified with a lentiviral vector encoding for human WAS cDNA. The primary safety endpoints were safety of the conditioning regimen and safety of lentiviral gene transfer into HSPCs. The primary efficacy endpoints were overall survival, sustained engraftment of genetically corrected HSPCs, expression of vector-derived WASP, improved T-cell function, antigen-specific responses to vaccinations, and improved platelet count and mean platelet volume normalisation. This interim analysis was done when the first six patients treated had completed at least 3 years of follow-up. The planned analyses are presented for the intention-to-treat population. This trial is registered with ClinicalTrials.gov (number NCT01515462)and EudraCT (number 2009-017346-32). Findings: Between April 20, 2010, and Feb 26, 201

Published

2019

11. Lentiviral haemopoietic stem/progenitor cell gene therapy for treatment of Wiskott-Aldrich syndrome: interim results of a non-randomised, open-label, phase 1/2 clinical study

Author

Ferrua, F, Cicalese, M, Galimberti, S, Giannelli, S, Dionisio, F, Barzaghi, F, Migliavacca, M, Bernardo, M, Calbi, V, Assanelli, A, Facchini, M, Fossati, C, Albertazzi, E, Scaramuzza, S, Brigida, I, Scala, S, Basso-Ricci, L, Pajno, R, Casiraghi, M, Canarutto, D, Salerio, F, Albert, M, Bartoli, A, Wolf, H, Fiori, R, Silvani, P, Gattillo, S, Villa, A, Biasco, L, Dott, C, Culme-Seymour, E, van Rossem, K, Atkinson, G, Valsecchi, M, Roncarolo, M, Ciceri, F, Naldini, L, Aiuti, A, Cicalese, MP, Bernardo, ME, Assanelli, AA, Albert, MH, Wolf, HM, Fiori, Rossan, Culme-Seymour, EJ, Valsecchi, MG, Roncarolo, MG, Ferrua, F, Cicalese, M, Galimberti, S, Giannelli, S, Dionisio, F, Barzaghi, F, Migliavacca, M, Bernardo, M, Calbi, V, Assanelli, A, Facchini, M, Fossati, C, Albertazzi, E, Scaramuzza, S, Brigida, I, Scala, S, Basso-Ricci, L, Pajno, R, Casiraghi, M, Canarutto, D, Salerio, F, Albert, M, Bartoli, A, Wolf, H, Fiori, R, Silvani, P, Gattillo, S, Villa, A, Biasco, L, Dott, C, Culme-Seymour, E, van Rossem, K, Atkinson, G, Valsecchi, M, Roncarolo, M, Ciceri, F, Naldini, L, Aiuti, A, Cicalese, MP, Bernardo, ME, Assanelli, AA, Albert, MH, Wolf, HM, Fiori, Rossan, Culme-Seymour, EJ, Valsecchi, MG, and Roncarolo, MG

Abstract

Background: Wiskott-Aldrich syndrome is a rare, life-threatening, X-linked primary immunodeficiency characterised by microthrombocytopenia, infections, eczema, autoimmunity, and malignant disease. Lentiviral vector-mediated haemopoietic stem/progenitor cell (HSPC)gene therapy is a potentially curative treatment that represents an alternative to allogeneic HSPC transplantation. Here, we report safety and efficacy data from an interim analysis of patients with severe Wiskott-Aldrich syndrome who received lentiviral vector-derived gene therapy. Methods: We did a non-randomised, open-label, phase 1/2 clinical study in paediatric patients with severe Wiskott-Aldrich syndrome, defined by either WAS gene mutation or absent Wiskott-Aldrich syndrome protein (WASP)expression or a Zhu clinical score of 3 or higher. We included patients who had no HLA-identical sibling donor available or, for children younger than 5 years of age, no suitable 10/10 matched unrelated donor or 6/6 unrelated cord blood donor. After treatment with rituximab and a reduced-intensity conditioning regimen of busulfan and fludarabine, patients received one intravenous infusion of autologous CD34+ cells genetically modified with a lentiviral vector encoding for human WAS cDNA. The primary safety endpoints were safety of the conditioning regimen and safety of lentiviral gene transfer into HSPCs. The primary efficacy endpoints were overall survival, sustained engraftment of genetically corrected HSPCs, expression of vector-derived WASP, improved T-cell function, antigen-specific responses to vaccinations, and improved platelet count and mean platelet volume normalisation. This interim analysis was done when the first six patients treated had completed at least 3 years of follow-up. The planned analyses are presented for the intention-to-treat population. This trial is registered with ClinicalTrials.gov (number NCT01515462)and EudraCT (number 2009-017346-32). Findings: Between April 20, 2010, and Feb 26, 201

Published

2019

12. Understanding the relevance of comprehensive facial injury (CFI) score: Statistical analysis of overall surgical time and length of stay outcomes

Author

Canzi, G, De Ponti, E, Fossati, C, Novelli, G, Cimbanassi, S, Bozzetti, A, Sozzi, D, Canzi, G, De Ponti, E, Fossati, C, Novelli, G, Cimbanassi, S, Bozzetti, A, and Sozzi, D

Abstract

Comprehensive facial injury (CFI) score is a powerful and extremely simple scale used to grade the clinical severity of all facial injuries, and is expressed in terms of the overall surgical time needed for definitive treatment. Its statistical validation was previously reported in 2019. The aim of this study was to investigate further the link with duration of surgery, applying the score to a larger sample of patients, and to evaluate the relationship between CFI score and other extremely relevant dependent variables: length of stay (LOS) in high care units (HCU) and in intensive care units (ICU). 1406 patients with diagnosis of at least one facial bone fracture, and treated by the same team in two highly specialized trauma centers, were studied. For each patient a specific CFI score is assigned and overall surgical time, length of stay, and presence of associated injuries were recorded. Data were divided into six clusters according to CFI score: (1) 0–5, (2) 6–10, (3) 11–15, (4) 16–20, (5) 21–25, and (6) >25. Regressions between CFI clusters and duration of surgery (minutes), LOS in ICU (days), and in HCU (days) were established. In addition, the presence of associated head and/or somatovisceral injuries was analyzed and related to CFI score. Statistical analysis confirmed linear regression existing between each CFI cluster and overall surgical time (p < 0.00001), with improved significance of the results using median values of surgical duration for each cluster (p = 0.0001). It also demonstrated the existence of linear regression between all CFI clusters and LOS in HCU (p = 0.0001) and between CFI clusters 3–6 and median values of LOS in ICU (p = 0.0001). Finally, associated injuries were observed to be more frequent in high CFI score clusters, occurring in around 90% of patients with a CFI score >25 (p < 0.00001). Association of head and facial injuries play a major role in high LOS in ICU values, whereas coexistence of facial, head and somatoviscera

Published

2019

13. Il dialogo tra la morte e il custode delle porte di Bartolomeo di Piacenza, poeta di fine Trecento

Author

Cocco, C, Fossati C, Grisafi A, Mosetti Casaretto F, Boiani G, Petoletti, Marco, Petoletti (ORCID:0000-0002-9632-0302), Cocco, C, Fossati C, Grisafi A, Mosetti Casaretto F, Boiani G, Petoletti, Marco, and Petoletti (ORCID:0000-0002-9632-0302)

Abstract

This essay analyses the writings of a teacher of Piacenza, Bartholomew de Ripa, who lived and worked between the XIV and the XV century in Northern Italy (Cremona, Mantua, Milan, Pavia and Piacenza). He is the author of many short poems which were copied, among other texts, in a manuscript now Milan, Bibl. Trivulziana, Triv. 760, fol. 43-87, written by his own hand. Among Bartholomew’s poems, a dialogue between the Death and the keeper of the gates of Piacenza, which was written during the plague of 1399, is noteworthy. This text is published here for the first time.

Published

2018

14. 14q32.3-qter trisomic segment: A case report and literature review

Author

Villa, N, Scatigno, A, Redaelli, S, Conconi, D, Cianci, P, Farina, C, Fossati, C, Dalpra', L, Maitz, S, Selicorni, A, VILLA, NICOLETTA, REDAELLI, SERENA, CONCONI, DONATELLA, FOSSATI, CHIARA, DALPRA', LEDA, Selicorni, A., Villa, N, Scatigno, A, Redaelli, S, Conconi, D, Cianci, P, Farina, C, Fossati, C, Dalpra', L, Maitz, S, Selicorni, A, VILLA, NICOLETTA, REDAELLI, SERENA, CONCONI, DONATELLA, FOSSATI, CHIARA, DALPRA', LEDA, and Selicorni, A.

Abstract

Background: Segmental duplication of the long arm of chromosome 14 (14q) has commonly been reported to affect the proximal segment of 14q, while distal duplication is a rare condition and often associated with segmental monosomy of other chromosomes. Case presentation: We report the clinical and genetic characterization of a 4-year-old male patient with 14q32.3-qter trisomy resulting from an adjacent segregation of a paternal reciprocal translocation (14;21)(q32.1;p12). The child shows minor facial anomalies, severe developmental delay, growth retardation, and a history of congenital hypothyroidism and neonatal transitory hyperglycemic crises. Conclusions: To the best of our knowledge, only 15 other cases of segmental 14q trisomy were documented. We compared molecularly defined cases to identify a minimal common duplicated region and to find genes with a hypothetical role in the phenotype. The presented case supports the previous suggestion of a pure "distal 14q partial duplication" and underlines the clinical variability.

Published

2016

15. 14q32.3-qter trisomic segment: A case report and literature review

Author

Villa, N, Scatigno, A, Redaelli, S, Conconi, D, Cianci, P, Farina, C, Fossati, C, Dalpra', L, Maitz, S, Selicorni, A, VILLA, NICOLETTA, REDAELLI, SERENA, CONCONI, DONATELLA, FOSSATI, CHIARA, DALPRA', LEDA, Selicorni, A., Villa, N, Scatigno, A, Redaelli, S, Conconi, D, Cianci, P, Farina, C, Fossati, C, Dalpra', L, Maitz, S, Selicorni, A, VILLA, NICOLETTA, REDAELLI, SERENA, CONCONI, DONATELLA, FOSSATI, CHIARA, DALPRA', LEDA, and Selicorni, A.

Abstract

Background: Segmental duplication of the long arm of chromosome 14 (14q) has commonly been reported to affect the proximal segment of 14q, while distal duplication is a rare condition and often associated with segmental monosomy of other chromosomes. Case presentation: We report the clinical and genetic characterization of a 4-year-old male patient with 14q32.3-qter trisomy resulting from an adjacent segregation of a paternal reciprocal translocation (14;21)(q32.1;p12). The child shows minor facial anomalies, severe developmental delay, growth retardation, and a history of congenital hypothyroidism and neonatal transitory hyperglycemic crises. Conclusions: To the best of our knowledge, only 15 other cases of segmental 14q trisomy were documented. We compared molecularly defined cases to identify a minimal common duplicated region and to find genes with a hypothetical role in the phenotype. The presented case supports the previous suggestion of a pure "distal 14q partial duplication" and underlines the clinical variability.

Published

2016

16. Behavioral profile in RASopathies

Author

Alfieri, P, Piccini, G, Caciolo, C, Perrino, F, Gambardella, Ml, Mallardi, M, Cesarini, L, Leoni, C, Leone, D, Fossati, C, Selicorni, A, Digilio, Mc, Tartaglia, M, Mercuri, Eugenio Maria, Zampino, Giuseppe, Vicari, Stefano, Mercuri, Eugenio Maria (ORCID:0000-0002-9851-5365), Zampino, G (ORCID:0000-0003-3865-3253), Vicari, S. (ORCID:0000-0002-5395-2262), Alfieri, P, Piccini, G, Caciolo, C, Perrino, F, Gambardella, Ml, Mallardi, M, Cesarini, L, Leoni, C, Leone, D, Fossati, C, Selicorni, A, Digilio, Mc, Tartaglia, M, Mercuri, Eugenio Maria, Zampino, Giuseppe, Vicari, Stefano, Mercuri, Eugenio Maria (ORCID:0000-0002-9851-5365), Zampino, G (ORCID:0000-0003-3865-3253), and Vicari, S. (ORCID:0000-0002-5395-2262)

Abstract

Here, we describe neurobehavioral features in patients with RASopathies (i.e., Noonan syndrome, LEOPARD syndrome, Costello syndrome, and cardiofaciocutaneous syndrome), developmental disorders caused by mutations in genes coding transducers participating in the RAS-MAPK signaling cascade. Parents of 70 individuals with a RASopathy were asked to fill out the following questionnaires: Child Behavior Checklist (CBCL), Social Communication Questionnaire version lifetime (SCQ-L), and Modified Checklist for Autism in toddlers (M-CHAT). Data analysis indicated high rates of internalizing (37%) and externalizing problems (31%) on CBCL. Scores over the cut-off were documented in 64% of patients with cardiofaciocutaneous syndrome, 44% with Costello syndrome, and 12% with Noonan syndrome on SCQ-L/M-CHAT. Our findings indicate that mutations promoting dysregulation of the RAS-MAPK cascade mark an increased psychopathological risk and highlight that autistic-like behavior could be underdiagnosed in patients with RASopathies.

Published

2014

17. A systems medicine clinical platform for understanding and managing non- communicable diseases

Author

Cesario, A, Auffray, C, Agusti, A, Apolone, G, Balling, R, Barbanti, P, Bellia, A, Boccia, Stefania, Bousquet, J, Cardaci, V, Cazzola, M, Dall'Armi, V, Daraselia, N, Ros, Ld, Bufalo, Ad, Ducci, G, Ferri, L, Fini, M, Fossati, C, Gensini, G, Granone, Pm, Kinross, J, Lauro, D, Cascio, Gl, Lococo, Filippo, Lococo, A, Maier, D, Marcus, F, Margaritora, Stefano, Marra, Camillo, Minati, G, Neri, M, Pasqua, F, Pison, C, Pristipino, C, Roca, J, Rosano, G, Rossini, Paolo Maria, Russo, P, Salinaro, G, Shenhar, S, Soreq, H, Sterk, Pj, Stocchi, F, Torti, M, Volterrani, M, Wouters, Efm, Frustaci, A, Bonassi, S., Boccia, S (ORCID:0000-0002-1864-749X), Lococo, F (ORCID:0000-0002-9383-5554), Margaritora, S (ORCID:0000-0002-9796-760X), Marra, Camillo (ORCID:0000-0003-3994-4044), Rossini, Paolo Maria (ORCID:0000-0003-2665-534X), Cesario, A, Auffray, C, Agusti, A, Apolone, G, Balling, R, Barbanti, P, Bellia, A, Boccia, Stefania, Bousquet, J, Cardaci, V, Cazzola, M, Dall'Armi, V, Daraselia, N, Ros, Ld, Bufalo, Ad, Ducci, G, Ferri, L, Fini, M, Fossati, C, Gensini, G, Granone, Pm, Kinross, J, Lauro, D, Cascio, Gl, Lococo, Filippo, Lococo, A, Maier, D, Marcus, F, Margaritora, Stefano, Marra, Camillo, Minati, G, Neri, M, Pasqua, F, Pison, C, Pristipino, C, Roca, J, Rosano, G, Rossini, Paolo Maria, Russo, P, Salinaro, G, Shenhar, S, Soreq, H, Sterk, Pj, Stocchi, F, Torti, M, Volterrani, M, Wouters, Efm, Frustaci, A, Bonassi, S., Boccia, S (ORCID:0000-0002-1864-749X), Lococo, F (ORCID:0000-0002-9383-5554), Margaritora, S (ORCID:0000-0002-9796-760X), Marra, Camillo (ORCID:0000-0003-3994-4044), and Rossini, Paolo Maria (ORCID:0000-0003-2665-534X)

Abstract

Non-Communicable Diseases (NCDs) are among the most pressing global health problems of the twenty-first century. Their rising incidence and prevalence is linked to severe morbidity and mortality, and they are putting economic and managerial pressure on healthcare systems around the world. Moreover, NCDs are impeding healthy aging by negatively affecting the quality of life of a growing number of the global population. NCDs result from the interaction of various genetic, environmental and habitual factors, and cluster in complex ways, making the complex identification of resulting phenotypes not only difficult, but also a top research priority. The degree of complexity required to interpret large patient datasets generated by advanced high-throughput functional genomics assays has now increased to the point that novel computational biology approaches are essential to extract information that is relevant to the clinical decision-making process. Consequently, system-level models that interpret the interactions between extensive tissues, cellular and molecular measurements and clinical features are also being created to identify new disease phenotypes, so that disease definition and treatment are optimized, and novel therapeutic targets discovered. Likewise, Systems Medicine (SM) platforms applied to extensively-characterized patients provide a basis for more targeted clinical trials, and represent a promising tool to achieve better prevention and patient care, thereby promoting healthy aging globally. The present paper: (1) reviews the novel systems approaches to NCDs; (2) discusses how to move efficiently from Systems Biology to Systems Medicine; and (3) presents the scientific and clinical background of the San Raffaele Systems Medicine Platform.

Published

2014

18. A systems medicine clinical platform for understanding and managing non- communicable diseases

Author

Cesario, Alfredo, Auffray, C, Agusti, A, Apolone, G, Balling, R, Barbanti, P, Bellia, A, Boccia, Stefania, Bousquet, J, Cardaci, V, Cazzola, M, Dall'Armi, V, Daraselia, N, Ros, Ld, Bufalo, Ad, Ducci, G, Ferri, L, Fini, M, Fossati, C, Gensini, G, Granone, Pm, Kinross, J, Lauro, D, Cascio, Gl, Lococo, Filippo, Lococo, A, Maier, D, Marcus, F, Margaritora, Stefano, Marra, Camillo, Minati, G, Neri, M, Pasqua, F, Pison, C, Pristipino, C, Roca, J, Rosano, G, Rossini, Paolo Maria, Russo, P, Salinaro, G, Shenhar, S, Soreq, H, Sterk, Pj, Stocchi, F, Torti, M, Volterrani, M, Wouters, Efm, Frustaci, Alessandra, Bonassi, S., Cesario, Alfredo (ORCID:0000-0003-4687-0709), Boccia, Stefania (ORCID:0000-0002-1864-749X), Lococo, F (ORCID:0000-0002-9383-5554), Margaritora, Stefano (ORCID:0000-0002-9796-760X), Marra, Camillo (ORCID:0000-0003-3994-4044), Rossini, Paolo Maria (ORCID:0000-0003-2665-534X), Cesario, Alfredo, Auffray, C, Agusti, A, Apolone, G, Balling, R, Barbanti, P, Bellia, A, Boccia, Stefania, Bousquet, J, Cardaci, V, Cazzola, M, Dall'Armi, V, Daraselia, N, Ros, Ld, Bufalo, Ad, Ducci, G, Ferri, L, Fini, M, Fossati, C, Gensini, G, Granone, Pm, Kinross, J, Lauro, D, Cascio, Gl, Lococo, Filippo, Lococo, A, Maier, D, Marcus, F, Margaritora, Stefano, Marra, Camillo, Minati, G, Neri, M, Pasqua, F, Pison, C, Pristipino, C, Roca, J, Rosano, G, Rossini, Paolo Maria, Russo, P, Salinaro, G, Shenhar, S, Soreq, H, Sterk, Pj, Stocchi, F, Torti, M, Volterrani, M, Wouters, Efm, Frustaci, Alessandra, Bonassi, S., Cesario, Alfredo (ORCID:0000-0003-4687-0709), Boccia, Stefania (ORCID:0000-0002-1864-749X), Lococo, F (ORCID:0000-0002-9383-5554), Margaritora, Stefano (ORCID:0000-0002-9796-760X), Marra, Camillo (ORCID:0000-0003-3994-4044), and Rossini, Paolo Maria (ORCID:0000-0003-2665-534X)

Abstract

Non-Communicable Diseases (NCDs) are among the most pressing global health problems of the twenty-first century. Their rising incidence and prevalence is linked to severe morbidity and mortality, and they are putting economic and managerial pressure on healthcare systems around the world. Moreover, NCDs are impeding healthy aging by negatively affecting the quality of life of a growing number of the global population. NCDs result from the interaction of various genetic, environmental and habitual factors, and cluster in complex ways, making the complex identification of resulting phenotypes not only difficult, but also a top research priority. The degree of complexity required to interpret large patient datasets generated by advanced high-throughput functional genomics assays has now increased to the point that novel computational biology approaches are essential to extract information that is relevant to the clinical decision-making process. Consequently, system-level models that interpret the interactions between extensive tissues, cellular and molecular measurements and clinical features are also being created to identify new disease phenotypes, so that disease definition and treatment are optimized, and novel therapeutic targets discovered. Likewise, Systems Medicine (SM) platforms applied to extensively-characterized patients provide a basis for more targeted clinical trials, and represent a promising tool to achieve better prevention and patient care, thereby promoting healthy aging globally. The present paper: (1) reviews the novel systems approaches to NCDs; (2) discusses how to move efficiently from Systems Biology to Systems Medicine; and (3) presents the scientific and clinical background of the San Raffaele Systems Medicine Platform.

Published

2014

19. Two cases of hepatic adenomas in patients with Wolf-Hirschhorn syndrome: a new rare complication?

Author

Prunotto, G, Cianci, P, Cereda, A, Scatigno, A, Fossati, C, Maitz, S, Biondi, A, Selicorni, A, BIONDI, ANDREA, Selicorni, A., Prunotto, G, Cianci, P, Cereda, A, Scatigno, A, Fossati, C, Maitz, S, Biondi, A, Selicorni, A, BIONDI, ANDREA, and Selicorni, A.

Abstract

Wolf-Hirschhorn syndrome (WHS) is a rare microdeletion syndrome associated with a characteristic facial appearance, failure to thrive, psychomotor delays, and various major malformations of internal organs; many medical complications have been described (feeding difficulties, epilepsy, hearing problems). Benign or malignant oncologic problems are not a typical feature of the natural history of these patients. We report on two patients with WHS patients in whom hepatic adenoma (HA) were diagnosed during adolescence. The clinical evolution of liver involvement was different between the two. We discuss the possibility of considering HA as a rare medical problem in the follow-up of WHS patients

Published

2013

20. Partial duplication of the PARK2 gene in a child with developmental delay and her normal mother: a second report

Author

Mariani, M, Crosti, F, Redaelli, S, Fossati, C, Piras, R, Biondi, A, Dalpra', L, Selicorni, A, BIONDI, ANDREA, DALPRA', LEDA, Selicorni, A., Mariani, M, Crosti, F, Redaelli, S, Fossati, C, Piras, R, Biondi, A, Dalpra', L, Selicorni, A, BIONDI, ANDREA, DALPRA', LEDA, and Selicorni, A.

Published

2013

21. The association of neural axis and craniovertebral junction anomalies with scoliosis in Rubinstein-Taybi syndrome

Author

Giussani, C, Selicorni, A, Fossati, C, Ingelmo, P, Canonico, F, Landi, A, Trezza, A, Riva, M, Sganzerla, E, GIUSSANI, CARLO GIORGIO, SGANZERLA, ERIK PIETRO, Giussani, C, Selicorni, A, Fossati, C, Ingelmo, P, Canonico, F, Landi, A, Trezza, A, Riva, M, Sganzerla, E, GIUSSANI, CARLO GIORGIO, and SGANZERLA, ERIK PIETRO

Abstract

Object Rubinstein-Taybi syndrome (RSTS) is a rare condition with characteristic genetic and clinical features. The presence of variable vertebral and neural axis abnormalities has been reported in the literature. We describe the possible association of multiple different spinal anomalies in these patients. Results The radiological exams of two RSTS patients (a female and male of 11 and 13 years) have been reviewed. Both patients presented the simultaneous association of craniovertebral junction bony abnormalities (occipito-C1 condyle subluxation and posterior C2-C3 arches fusion), Chiari I malformation, spinal cord syrinx, low-lying conus medullaris, and scoliosis. Conclusion An association of different spinal cord anomalies is possible in RSTS patients and has to be investigated with a comprehensive neuroimaging study in order to address the proper treatment and prevent the development of neurologic deficits. © Springer-Verlag 2012.

Published

2012

22. A GIS and Associated Database for the Italian Stranding Network. A Cooperative Project Based on GIS Technologies

Author

PAVIA UNIV (ITALY), Pavan, G., Podesta, M., D'Amico, A., Portunato, N., Fossati, C., Manghi, M., Quero, M., Teloni, V., PAVIA UNIV (ITALY), Pavan, G., Podesta, M., D'Amico, A., Portunato, N., Fossati, C., Manghi, M., Quero, M., and Teloni, V.

Abstract

The "Centro Studi Cetacei" (CSC) is a research group established in 1985 at the Natural History Museum of Milan as part of the Italian Society for Natural Sciences. One of the most important projects of CSC was to create a national network (Italian Stranding Network) to collect data about stranded Cetaceans along the Italian coasts, or entangled in fishing nets, or found dead in open waters. The Centro Studi Cetacei is recognized by the Italian Ministry of Agricultural, Food and Forest Resources, by the C.I.T.E.S. Office and by the Ministry of Environment (Nature Conservation Service). Since 1986 the Italian Stranding Network has been collecting data on more than 2600 strandings (>2700 animals), concerning 12 cetacean species, and has published regular annual reports. The dataset also includes 164 events recorded in the former project "Progetto Cetacei" as well as historical data found on literature and newspapers. As it represents one the most comprehensive dataset available for the Mediterranean Sea, the Italian Stranding Network archive has been chosen as a case study of a Cetacean GIS application.

Published

2001

23. Software and Hardware Sound Analysis Tools for Field Work

Author

UNIVERSITA DEGLI STUDI DI PAVIA (ITALY)CENTRO INTERDISCIPLINARE DI BIOACUSTICA E RICERCHE AMBIENTALI, Pavan, G., Manghi, M., Fossati, C., UNIVERSITA DEGLI STUDI DI PAVIA (ITALY)CENTRO INTERDISCIPLINARE DI BIOACUSTICA E RICERCHE AMBIENTALI, Pavan, G., Manghi, M., and Fossati, C.

Abstract

The latest version of the real-time Digital Signal Processing Workstation developed at CIBRA runs in a standard Windows environment and can use a wide range of sound acquisition devices. It can be based on a notebook to allow on-field use. Depending on the acquisition devices, recording, analysis and display can be performed in real-time up to 500 k samples/sec to provide useful bandwidth to more than 200 kHz. The software was primarily developed for continuous real-time monitoring in bioacoustical studies.

Published

1999