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Dive into the research topics where Massimiliano Scalvenzi is active.

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Featured researches published by Massimiliano Scalvenzi.


British Journal of Dermatology | 1999

Dermatoscopic pitfalls in differentiating pigmented Spitz naevi from cutaneous melanomas

Giuseppe Argenziano; Massimiliano Scalvenzi; Stefania Staibano; B. Brunetti; Domenico Piccolo; Mario Delfino; G. De Rosa; Hp Soyer

Epiluminescence microscopy (ELM, skin surface microscopy, dermoscopy, dermatoscopy) is a valuable method for improving the diagnostic accuracy in pigmented skin lesions. Specific ELM criteria are already recognized for differentiating pigmented Spitz naevi (PSN) from cutaneous melanomas (CM). Our purpose was to describe the ELM appearance of a series of PSN with emphasis on PSN and CM with overlapping features. Thirty‐six consecutive patients with PSN, and three cases of CM (selected from a larger database) exhibiting ELM ‘spitzoid’ features, were evaluated clinically, dermatoscopically and histopathologically. Most PSN (27 of 36; 75%) displayed two typical ELM patterns, namely, the starburst (19 of 36; 53%) or the globular pattern (eight of 36; 22%), which were correlated to different histopathological findings. In nine of 36 (25%) PSN, atypical ELM features which are more commonly seen in CM were observed. These PSN with an atypical pattern were characterized by an uneven distribution of colours and structures, and an irregular diffuse pigmentation resembling blue–white veil or irregular extensions (black blotches). These atypical lesions mostly occurred in children and showed no history of growth. In contrast, in three examples of CM, the typical ELM criteria of malignancy were less recognizable and either the characteristic starburst or globular pattern usually seen in PSN was present. These three lesions occurred in adults and had a recent history of change in colour, shape or size. The overlap in ELM features of some PSN and CM represents a major diagnostic pitfall when ELM examination is considered alone. In these atypical cases, clinical history including the age of the patient may be the only clue to enable a correct diagnosis.


British Journal of Dermatology | 2004

Clinically equivocal melanocytic skin lesions with features of regression: a dermoscopic-pathological study.

Iris Zalaudek; Giuseppe Argenziano; G. Ferrara; Hp Soyer; Rosamaria Corona; Francesco Sera; Lorenzo Cerroni; Andreina Carbone; A. Chiominto; Lorenza Cicale; G. De Rosa; A. Ferrari; R. Hofmann-Wellenhof; Josep Malvehy; Ketty Peris; Maria A. Pizzichetta; Susana Puig; Massimiliano Scalvenzi; Stefania Staibano; Vincenzo Ruocco

Background  Benign melanocytic skin lesions may be difficult to differentiate from melanoma both clinically and dermoscopically. One of the most confounding dermoscopic features, commonly seen in melanoma but in our experience also in melanocytic naevi, is represented by the so‐called blue–white structures (BWS).


Archives of Dermatology | 2008

Time Required for a Complete Skin Examination With and Without Dermoscopy: A Prospective, Randomized Multicenter Study

Iris Zalaudek; Harald Kittler; Ashfaq A. Marghoob; Anna Balato; Andreas Blum; Stéphane Dalle; Gerardo Ferrara; Regina Fink-Puches; Caterina M. Giorgio; Rainer Hofmann-Wellenhof; Josep Malvehy; Elvira Moscarella; Susana Puig; Massimiliano Scalvenzi; Luc Thomas; Giuseppe Argenziano

OBJECTIVE To determine the time required to perform a complete skin examination (CSE) as a means of opportunistic screening for skin cancer both without and with dermoscopy. DESIGN Randomized, prospective multicenter study. SETTING Eight referral pigmented lesion clinics. Patients From June 2006 to January 2007, 1359 patients with at least 1 melanocytic or nonmelanocytic skin lesion were randomly selected to receive a CSE without dermoscopy or CSE with dermoscopy. For each patient, the total number of lesions and the duration of the CSE were recorded. A total of 1328 patients were eligible for analysis (31 were excluded because of missing data). MAIN OUTCOME MEASURES The median time (measured in seconds) needed for CSE with and without dermoscopy and according to total cutaneous lesion count. RESULTS The median time needed for CSE without dermoscopy was 70 seconds and with dermoscopy was 142 seconds, a significant difference of 72 seconds (P < .001). The use of dermoscopy increased the duration of CSE, and this increase was in direct proportion to the patients total lesion count. In contrast, the time required to perform a CSE without dermoscopy remained the same irrespective of whether the patients had few or many lesions. CONCLUSIONS A CSE aided by dermoscopy takes significantly longer than a CSE without dermoscopy. However, a thorough CSE, with or without dermoscopy, requires less than 3 minutes, which is a reasonable amount of added time to potentially prevent the morbidity and mortality associated with skin cancer.


Cancer | 2002

Dermoscopic and histopathologic diagnosis of equivocal melanocytic skin lesions: an interdisciplinary study on 107 cases

Gerardo Ferrara; Giuseppe Argenziano; H. Peter Soyer; Rosamaria Corona; Francesco Sera; Bruno Brunetti; Lorenzo Cerroni; Sergio Chimenti; Laila El Shabrawi-Caelen; Angela Ferrari; Rainer Hofmann-Wellenhof; Steven Kaddu; Domenico Piccolo; Massimiliano Scalvenzi; Stefania Staibano; Ingrid H. Wolf; Gaetano De Rosa

Dermoscopy (dermatoscopy, epiluminescence microscopy) is increasingly employed for the preoperative detection of cutaneous melanoma; dermoscopic features of pigmented skin lesions have been previously defined using histopathology as the key to the code. In a preliminary study on 10 cases evaluated by nine dermoscopists and nine histopathologists, the authors experienced that when at least two dermoscopists disagree in evaluating a melanocytic lesion, even histopathologic consultations may give equivocal results.


International Journal of Dermatology | 2008

Dermoscopic patterns of superficial basal cell carcinoma

Massimiliano Scalvenzi; Serena Lembo; Maria Grazia Francia; Anna Balato

Background  Superficial basal cell carcinoma (BCC) presents as a scaly, pink to red–brown patch and is predominantly located on the trunk. Clinical diagnosis may not be always easy and implicates a variety of differential diagnoses; in this situation dermoscopy has been reported improving the diagnostic accuracy. This study investigated dermoscopic patterns of superficial BCC focalizing the most specific and frequent structures in order to improve the diagnostic accuracy.


Dermatology | 2007

Dermoscopy Key Points: Recommendations from the International Dermoscopy Society

Jonathan Bowling; Giuseppe Argenziano; A Azenha; J Bandic; R Bergman; Andreas Blum; Horacio Cabo; A Di Stephani; James M. Grichnik; Allan C. Halpern; R Hofman-Wellenhof; Robert H. Johr; Harald Kittler; Alfred W. Kopf; Jürgen Kreusch; David Langford; J. Malvehy; Ashfaq A. Marghoob; Scott W. Menzies; Fezal Ozdemir; Ketty Peris; D Piccolo; Maria A. Pizzichetta; D Polsky; Susana Puig; Harold S. Rabinovitz; Pietro Rubegni; Toshiaki Saida; Massimiliano Scalvenzi; Stefania Seidenari

J. Bowling G. Argenziano A. Azenha J. Bandic R. Bergman A. Blum H. Cabo A. Di Stephani J. Grichnik A. Halpern R. Hofman-Wellenhof R. Johr H. Kittler A. Kopf J. Kreusch D. Langford J. Malvehy A. Marghoob S. Menzies F. Ozdemir K. Peris D. Piccolo M.A. Pizzichetta D. Polsky S. Puig H. Rabinovitz P. Rubegni T. Saida M. Scalvenzi S. Seidenari H.P. Soyer M. Tanaka I. Zalaudek R.P. Braun


Journal of The American Academy of Dermatology | 2012

Total body skin examination for skin cancer screening in patients with focused symptoms

Giuseppe Argenziano; Iris Zalaudek; Rainer Hofmann-Wellenhof; Renato Marchiori Bakos; Wilma Bergman; Andreas Blum; Paolo Broganelli; Horacio Cabo; Filomena Caltagirone; Caterina Catricalà; Maurizio Coppini; Lucas Dewes; Maria Grazia Francia; Alessandro Garrone; Bengü Gerçeker Türk; Giovanni Ghigliotti; Jason Giacomel; Jean-Yves Gourhant; Gerald Hlavin; Nicole A. Kukutsch; Dario Lipari; Gennaro Melchionda; Fezal Ozdemir; Giovanni Pellacani; Riccardo Pellicano; Susana Puig; Massimiliano Scalvenzi; Ana Maria Sortino-Rachou; Anna Virgili; Harald Kittler

BACKGROUND The value of total body skin examination (TBSE) for skin cancer screening is controversial. OBJECTIVE We sought to determine whether TBSE could be helpful in patients with focused skin symptoms who would not otherwise have undergone TBSE. METHODS In a prospective, multicenter, cross-sectional study consecutive adult patients were recruited during a period of 18 months. Physicians first inspected problem areas and uncovered areas and then performed TBSE. Equivocal lesions detected in both steps were excised or biopsied. Primary outcomes were the absolute and relative risks of missing skin cancer and the number of patients needed to examine to detect melanoma or another malignancy. A secondary outcome was the proportion of false-positive results obtained by TBSE. RESULTS We examined 14,381 patients and detected 40 (0.3%) patients with melanoma and 299 (2.1%) with at least one nonmelanoma skin cancer by TBSE. In 195 (1.3%) patients equivocal lesions found by TBSE turned out to be benign. We calculated that 47 patients need to be examined by TBSE to find one skin malignancy and 400 patients to detect one melanoma. The risk of missing one malignancy if not performing TBSE was 2.17% (95% confidence interval 1.25-3.74). Factors significantly increasing the chance to find a skin cancer were age, male gender, previous nonmelanoma skin cancer, fair skin type, skin tumor as the reason for consultation, and presence of an equivocal lesion on problem/uncovered areas. LIMITATIONS The impact of TBSE on skin cancer mortality was not evaluated. CONCLUSIONS TBSE improves skin cancer detection in patients with focused skin symptoms and shows a low rate of false-positive results.


Journal of The European Academy of Dermatology and Venereology | 2007

Telediagnosis and face-to-face diagnosis reliability for melanocytic and non-melanocytic ‘pink’ lesions

Gabriella Fabbrocini; Anna Balato; O Rescigno; M Mariano; Massimiliano Scalvenzi; B Brunetti

Background  Telemedicine is a worldwide healthcare practice that, during the last years, has dramatically reduced the time of consultation for patients. Teledermoscopy aids in the current management of skin cancers in general and particularly of melanoma; telemedicine and teledermoscopy give the chance to provide consultations with experts also by long distance.


Clinical and translational medicine | 2014

FKBP51 increases the tumour-promoter potential of TGF-beta

Simona Romano; Anna D’Angelillo; Paolo D’Arrigo; Stefania Staibano; Adelaide Greco; Arturo Brunetti; Massimiliano Scalvenzi; Rita Bisogni; Iris Scala; Maria Fiammetta Romano

BackgroundFKBP51 (FKBP5 Official Symbol) is a large molecular weight component of the family of FK506 binding proteins (FKBP). In recent years, research studies from our laboratory highlighted functions for FKBP51 in the control of apoptosis and melanoma progression. FKBP51 expression correlated with the invasiveness and aggressiveness of melanoma. Since a role for TGF-β in the enhanced tumorigenic potential of melanoma cells is widely described, we hypothesized a cooperative effect between FKBP51 and TGF-β in melanoma progression.MethodsSAN and A375 melanoma cell lines were utilized for this study. Balb/c IL2γ NOD SCID served to assess the ability to colonize organs and metastasize of different cell lines, which was evaluated by in vivo imaging. Realtime PCR and western blot served for measurement of mRNA and protein expression, respectively.ResultsBy comparing the metastatic potential of two melanoma cell lines, namely A375 and SAN, we confirmed that an increased capability to colonize murine organs was associated with increased levels of FKBP51. A375 melanoma cell line expressed FKBP51 mRNA levels 30-fold higher in comparison to the SAN mRNA level and appeared more aggressive than SAN melanoma cell line in an experimental metastasis model. In addition, A375 expressed, more abundantly than SAN, the TGF-β and the pro angiogenic TGF-β receptor type III (TβRIII) factors. FKBP51 silencing produced a reduction of TGF-β and TβRIII gene expression in A375 cell line, in accordance with previous studies. We found that the inducing effect of TGF-β on Sparc and Vimentin expression was impaired in condition of FKBP51 depletion, suggesting that FKBP51 is an important cofactor in the TGF-β signal. Such a hypothesis was supported by co immunoprecipitation assays, showing that FKBP51 interacted with either Smad2,3 and p300. In normal melanocytes, FKBP51 potentiated the effect of TGF-β on N-cadherin expression and conferred a mesenchymal-like morphology to such round-shaped cells.ConclusionsOverall, our findings show that FKBP51 enhances some pro oncogenic functions of TGF-β, suggesting that FKBP51-overexpression may help melanoma to take advantage of the tumor promoting activities of the cytokine.


Journal of The European Academy of Dermatology and Venereology | 1998

Hereditary multiple fibrofolliculomas, trichodiscomas and acrochordons: syndrome of Birt-Hogg-Dubè

Massimiliano Scalvenzi; Giuseppe Argenziano; Elena Sammarco; Mario Delfino

The syndrome of Birt-Hogg-Dubè (BHD) is an autosomal dominant syndrome, characterized by a triad of cutaneous lesions including multiple fibrofolliculomas, trichodiscomas, and acrochordons. There are many clinical expressions, solitary and multiple forms, with or without other skin tumors. In the literature BHD syndrome has been associated with internal malignancy. We describe a patient with multiple firm, skin-colored papules in which the three types of lesion are documented. No signs of systemic disease were present.

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Claudia Costa

University of Naples Federico II

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Giuseppe Argenziano

Seconda Università degli Studi di Napoli

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Stefania Staibano

University of Naples Federico II

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Anna Balato

University of Naples Federico II

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Maria Grazia Francia

University of Naples Federico II

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Massimo Mascolo

University of Naples Federico II

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Gerardo Ferrara

Seconda Università degli Studi di Napoli

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Nicola Balato

University of Naples Federico II

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Susana Puig

University of Barcelona

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Iris Zalaudek

Medical University of Graz

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