2017
DOI: 10.1016/j.jaad.2016.07.038
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Development and validation of a noninvasive 2-gene molecular assay for cutaneous melanoma

Abstract: BackgroundClinical and histopathologic assessment of pigmented skin lesions remains challenging even for experts. Differentiated and accurate noninvasive diagnostic modalities are highly desirable.ObjectiveWe sought to provide clinicians with such a tool.MethodsA 2-gene classification method based on LINC00518 and preferentially expressed antigen in melanoma (PRAME) gene expression was evaluated and validated in 555 pigmented lesions (157 training and 398 validation samples) obtained noninvasively via adhesive… Show more

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Cited by 127 publications
(190 citation statements)
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“…In contrast to the current pathway, the PLA also has a very high NPV (>99%), 26 which reduces the likelihood that a melanoma will be missed and subject to a delayed diagnosis. Melanomas with a delayed diagnosis have higher stage-related treatment costs.…”
Section: Discussionmentioning
confidence: 99%
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“…In contrast to the current pathway, the PLA also has a very high NPV (>99%), 26 which reduces the likelihood that a melanoma will be missed and subject to a delayed diagnosis. Melanomas with a delayed diagnosis have higher stage-related treatment costs.…”
Section: Discussionmentioning
confidence: 99%
“…The PLA is based on a new platform technology for noninvasive genomic testing of the skin, which allows the analysis of samples collected from adhesive patches. 11,22,[24][25][26][27] In contrast to the current VAH pathway, the PLA has a very high NPV (>99%) that reduces the probability of missing melanomas from about 17% using the current standard of care (NPV of 83%) to less than 1%. 26,27 In addition, the noninvasive sampling leads to dramatic reduction in surgical biopsies and subsequent excisions.…”
Section: -14mentioning
confidence: 99%
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“…5a). Among these was the tumor-specific LINC00518 gene that has been proposed as a two-gene classifier for melanoma detection together with the tumor associated antigen PRAME 47 .…”
Section: Identification Of Tumor-specific Nonchlaipmentioning
confidence: 99%
“…Among the most upregulated genes in NRAS-mutant melanoma were PRAME and NES. PRAME encodes an antigen that is predominantly expressed in melanoma and has been used in gene expression-based, non-invasive diagnostic assay for melanoma (Gerami et al, 2017). NES is a stem cell/progenitor lineage marker that is highly expressed in both large CMN and superficial spreading melanoma (Charbel et al, 2015).…”
Section: Genomic Analysis Of Metastatic Melanoma In An Adult With Giamentioning
confidence: 99%