Detection of micrometastases in sentinel lymph nodes from melanoma patients

Rimoldi, Donata; Lemoine, Robert; Kurt, Anne-Marie; Salvi, Suzanne; Berset, Magali; Matter, Maurice; Roche, Bruno; Cerottini, Jean‐Philippe; Guggisberg, D.; Krischer, Joachim; Braun, Ralph P.; Willi, Jean-Pierre; Antonescu, Cristian; Slosman, Daniel O.; Lejeune, Ferdy J.; Líénard, Danielle; Lémanique, Groupe Mélanome

doi:10.1097/00008390-200310000-00010

Cited by 32 publications

(1 citation statement)

References 39 publications

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“…Despite their shared origin as melanocytic malignancies, UM and CM involve different genetic and molecular pathophysiologic mechanisms (Table 1). The most common mutations found in CM are BRAF, NRAS, and KIT, which are rarely found in UM [15]. UM also lacks CM's hallmark environmental risk factor of ultraviolet (UV) radiation exposure, as evidenced by UM's lower burden of UV radiationinduced somatic mutations [16].…”

Section: Uveal Melanoma Versus Cutaneous Melanomamentioning

confidence: 99%

Uveal melanoma: laboratory advances and new frontiers in patient care

Moser

Dalvin

2021

Current Opinion in Ophthalmology

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Purpose of reviewTo review recent advancements in the genetic understanding, diagnosis, prognosis, and treatment of uveal melanoma (UM). Recent findingsUM is a molecularly distinct melanocytic malignancy driven by mutations in GNAQ or GNA11, with mitogen-activated protein kinase pathway upregulation. Earlier diagnosis and treatment are important factors for improving life prognosis. These goals can be aided by more objective multimodal imaging risk factors for the prediction of malignant nevus transformation and novel treatment strategies such as customized radiation fields and nanoparticle therapy to reduce vision-threatening treatment side effects. The risk for metastatic disease can be reliably predicted through gene expression profiling or the Cancer Genome Atlas project classification, and combined use of clinical tumor features with molecular data allows for highly individualized patient prognosis. Patients with high-risk UM should be considered for clinical trials of adjuvant therapy to prevent metastatic disease. For patients with clinically evident metastasis, combination immunotherapy regimens, T cell-based therapies, and focal adhesion kinase inhibitors offer hope for improved clinical response rates.

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Section: Uveal Melanoma Versus Cutaneous Melanomamentioning

confidence: 99%