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Automated melanoma detection with a novel multispectral imaging system: results of a prospective study

Stefano Tomatis et al 2005 Phys. Med. Biol. 50 1675-1687   doi: 10.1088/0031-9155/50/8/004  Help

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Stefano Tomatis1, Mauro Carrara1, Aldo Bono2, Cesare Bartoli3, Manuela Lualdi1, Gabrina Tragni4, Ambrogio Colombo1 and Renato Marchesini1
1 Department of Medical Physics, Istituto Nazionale per lo Studio e la Cura dei Tumori, via Venezian, 1.20133 Milan, Italy
2 Melanoma and Sarcoma Unit, Istituto Nazionale per lo Studio e la Cura dei Tumori, via Venezian, 1.20133 Milan, Italy
3 Day Surgery Unit, Istituto Nazionale per lo Studio e la Cura dei Tumori, via Venezian, 1.20133 Milan, Italy
4 Department of Pathology and Cytopathology, Istituto Nazionale per lo Studio e la Cura dei Tumori, via Venezian, 1.20133 Milan, Italy
E-mail: stefano.tomatis@istitutotumori.mi.it

Abstract. The aim of this research was to evaluate the performance of a new spectroscopic system in the diagnosis of melanoma. This study involves a consecutive series of 1278 patients with 1391 cutaneous pigmented lesions including 184 melanomas. In an attempt to approach the 'real world' of lesion population, a further set of 1022 not excised clinically reassuring lesions was also considered for analysis. Each lesion was imaged in vivo by a multispectral imaging system. The system operates at wavelengths between 483 and 950 nm by acquiring 15 images at equally spaced wavelength intervals. From the images, different lesion descriptors were extracted related to the colour distribution and morphology of the lesions. Data reduction techniques were applied before setting up a neural network classifier designed to perform automated diagnosis. The data set was randomly divided into three sets: train (696 lesions, including 90 melanomas) and verify (348 lesions, including 53 melanomas) for the instruction of a proper neural network, and an independent test set (347 lesions, including 41 melanomas). The neural network was able to discriminate between melanomas and non-melanoma lesions with a sensitivity of 80.4% and a specificity of 75.6% in the 1391 histologized cases data set. No major variations were found in classification scores when train, verify and test subsets were separately evaluated. Following receiver operating characteristic (ROC) analysis, the resulting area under the curve was 0.85. No significant differences were found among areas under train, verify and test set curves, supporting the good network ability to generalize for new cases. In addition, specificity and area under ROC curve increased up to 90% and 0.90, respectively, when the additional set of 1022 lesions without histology was added to the test set. Our data show that performance of an automated system is greatly population dependent, suggesting caution in the comparison with results reported in the literature. In our opinion, scientific reports should provide, at least, the median values of thickness and dimension of melanomas, as well as the number of small (≤6 mm) melanomas.

Print publication: Issue 8 (21 April 2005)
Received 29 November 2004, in final form 2 February 2005
Published 30 March 2005

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