Noel Turner scite author profile

Melanoma is a malignant neoplasm of melanocytes that accounts for the majority of skin cancer deaths despite comprising less than 5% of all cutaneous malignancies. Its incidence has increased faster than that of any other cancer over the past half-century and the annual costs of treatment in the United States alone have risen rapidly. Although the majority of primary melanomas are cured with local excision, metastatic melanoma historically carries a grim prognosis, with a median survival of 9 months and a long-term survival rate of 10%. Given the urgent need to develop treatment strategies for metastatic melanoma and the explosion of genetic technologies over the past 20 years, there has been extensive research into the genetic alterations that cause melanocytes to become malignant. More recently, efforts have focused on the genetic changes that drive melanoma metastasis. This review aims to summarize the current knowledge of the genetics of primary cutaneous and ocular melanoma, the genetic changes associated with metastasis in melanoma and other cancer types, and non-genetic factors that may contribute to metastasis.

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B cell depletion or absence does not impede anti-tumor activity of PD-1 inhibitors

Damsky¹,

Jilaveanu²,

Turner³

et al. 2019

j. immunotherapy cancer

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Background PD-1 inhibitors are approved for multiple malignancies and function by stimulating T cells. However, the role of B cells in the anti-tumor activity of these drugs is unknown, as is their activity in patients who have received B cell depleting drugs or with immunoglobulin deficiencies. Methods We studied B cell content in 40 melanomas from patients treated with pembrolizumab or nivolumab and assessed the association with response to therapy. Murine MC38 colon cancer and YUMMER1.7 melanoma models were used to determine whether concomitant anti-CD20 antibody injections diminish the anti-tumor effects of anti-PD-1. Results were validated in mu MT mice, which lack B cells. Results B cells were sparse in most melanomas and B cell content was not associated with response to anti-PD-1 or overall survival. Employing MC38 and YUMMER1.7 models, we demonstrated that anti-CD20 antibodies reduce tumor-infiltrating B cells yet had no effect on tumor growth, response to PD-1 inhibition, or survival. In mu MT mice, T-cell dependent tumor rejection and anti-PD-1 responses were no different than in wildtype C57BL/6 J mice. Conclusions The degree of tumor infiltrating B cell content is not associated with response to anti-PD-1 inhibitors in melanoma. PD-1 inhibitors cause tumor shrinkage in murine cancer models even when B cells are absent or are depleted. PD-1 inhibitors are likely to be active in patients with impaired B cell function, such as patients undergoing B cell depletion with drugs including rituximab for conditions such as B cell malignancies or autoimmune disorders. Electronic supplementary material The online version of this article (10.1186/s40425-019-0613-1) contains supplementary material, which is available to authorized users.

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Recurrent Cutaneous Exophiala Phaeohyphomycosis in an Immunosuppressed Patient

Turner¹,

Kibbi

Panse

et al. 2020

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Atezolizumab‐associated vitiligo‐like leukoderma in a patient with transitional cell carcinoma

Turner

Leventhal

2018

Int J Dermatology

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Noel Turner

Subepidermal blistering eruptions, including bullous pemphigoid, following COVID-19 vaccination

Genetics of metastasis: melanoma and other cancers

B cell depletion or absence does not impede anti-tumor activity of PD-1 inhibitors

Recurrent Cutaneous Exophiala Phaeohyphomycosis in an Immunosuppressed Patient

Atezolizumab‐associated vitiligo‐like leukoderma in a patient with transitional cell carcinoma

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