Publications by authors named "Richard Marais"

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  • Scientists found that a specific marker in melanoma (a type of skin cancer), called ALDH1A3, works with another protein called ACSS2 to help cancer cells use sugar (glucose) better and change their genes.
  • They discovered that acetaldehyde, which is a toxic substance, plays a role in this process and can help change gene activity in cancer cells.
  • In experiments with zebrafish that have melanoma, they showed that blocking ALDH1A3 can stop cancer cells from becoming resistant to treatment and may help doctors find new ways to fight the disease.
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  • Mucosal (MM) and acral melanomas (AM) are rare types of melanoma that often have KIT mutations, which could be treated with targeted small-molecule inhibitors, though none are currently approved for melanoma.
  • A Phase II clinical trial (NICAM) assessed the safety and effectiveness of nilotinib in patients with KIT-mutant MM and AM; 18% of screened patients had KIT mutations, with some showing promising results.
  • The trial found that nilotinib demonstrated activity in treating these mutations, suggesting the need for further research on its use in managing KIT-mutated melanoma.
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  • Scientists are studying how the tiny living things in our gut (gut microbiome) can affect cancer treatment, specifically with a method called immune checkpoint blockade (ICB).
  • They looked at 175 patients with a type of skin cancer called melanoma to see how changes in the gut microbiome relate to how well the treatment works over time.
  • They found that certain types of gut bacteria can help predict if patients will do better or worse with the treatment, and understanding these changes can help doctors improve therapies in the future.
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Introduction: We aimed to study the frequency (prevalence) and histology of benign melanocytic naevus cells in regional lymph nodes in relation to age and sex and nodal location.

Material And Methods: Histopathology reports of sentinel lymph node (SLN) biopsies from melanoma patients, 2002 - 2014, and from breast cancer patients, 2010- 2019, were obtained from records of a single hospital in England. All sections were similarly processed and examined.

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Congenital disorders of glycosylation (CDG) are rare genetic disorders with a spectrum of clinical manifestations caused by abnormal N-glycosylation of secreted and cell surface proteins. Over 130 genes are implicated and next generation sequencing further identifies potential disease drivers in affected individuals. However, functional testing of these variants is challenging, making it difficult to distinguish pathogenic from non-pathogenic events.

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Introduction: There appear to be several variants of naevoid melanoma suspected as having different outcomes, but follow-up studies have been few. We aimed to assess the prognosis of naevoid melanomas in a multi-centre study.

Material And Methods: From histopathology records we ascertained patients in the UK, Australia and Italy diagnosed with maturing naevoid melanoma (n = 65; 14; 7 respectively) and nodular/papillomatous naevoid melanoma (12; 6; 0), and patients with superficial spreading melanoma (SSM) from UK (73) and Australia (26).

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Over the past decade, melanoma has led the field in new cancer treatments, with impressive gains in on-treatment survival but more modest improvements in overall survival. Melanoma presents heterogeneity and transcriptional plasticity that recapitulates distinct melanocyte developmental states and phenotypes, allowing it to adapt to and eventually escape even the most advanced treatments. Despite remarkable advances in our understanding of melanoma biology and genetics, the melanoma cell of origin is still fiercely debated because both melanocyte stem cells and mature melanocytes can be transformed.

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  • Immune cells are crucial for the effectiveness of checkpoint inhibitors in cancer treatment, but their exact roles are not well understood.
  • This study used single-cell analysis of melanoma biopsies and blood samples to investigate the importance of various immune cell types in response to these treatments.
  • Results showed that specific B cell maturation and abundance can predict patient outcomes, suggesting that B cells play a significant role in anti-tumor immunity and may serve as a potential biomarker for assessing treatment risk in melanoma patients.
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  • Research shows that the gut microbiome may influence how patients with advanced melanoma respond to immune checkpoint inhibitors (ICIs), but there’s no clear agreement on which specific microbiome traits are beneficial.
  • A study that sequenced stool samples from 165 ICI-naive patients and combined these with 147 samples from earlier research found that microbiome characteristics linked to treatment response varied by patient group.
  • While some bacteria, like Bifidobacterium pseudocatenulatum and Akkermansia muciniphila, were associated with positive responses to ICIs, no single species reliably indicated treatment success, highlighting the complexity of this relationship and suggesting more research is needed.
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Background: The use of indoor tanning devices causes melanoma and other skin cancers with resulting morbidity, mortality and increased healthcare costs. Policymakers require robust economic evidence to inform decisions about a possible ban of such devices to mitigate these burdens.

Objectives: To assess the health costs and consequences of introducing a policy-based intervention across England to ban commercial indoor tanning with an accompanying public information campaign.

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Background: Precision immuno-oncology approaches are needed to improve cancer care. We recently demonstrated that in patients with metastatic melanoma, an increase of clonality or diversity of the T cell receptor (TCR) repertoire of peripheral T cells following one cycle of immunotherapy is coincident with response to immune-checkpoint blockade (ICB). We also identified a subset of peripheral CD8 immune-effector memory T cells (T cells) whose expansion was associated with response to ICB and increased overall survival.

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Conjunctival melanoma (ConjMel) is a potentially deadly ocular melanoma, originating from partially sunlight-exposed mucosa. We explored the mutational landscape of ConjMel and studied the correlation with etiological factors. We collected 47 primary ConjMel samples and performed next-generation sequencing of 400 genes.

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Fibroblasts display extensive transcriptional heterogeneity, yet functional annotation and characterization of their heterocellular relationships remains incomplete. Using mass cytometry, we chart the stromal composition of 18 murine tissues and 5 spontaneous tumor models, with an emphasis on mesenchymal phenotypes. This analysis reveals extensive stromal heterogeneity across tissues and tumors, and identifies coordinated relationships between mesenchymal and immune cell subsets in pancreatic ductal adenocarcinoma.

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  • The study investigates the growth rates of primary cutaneous melanomas (≥1 mm thickness) and their link to aggressiveness, focusing on fast-growing melanomas (FGMM) versus slower ones.
  • Researchers evaluated the mutational profiles of these melanomas, finding that FGMM displayed a higher number of harmful mutations and poorer relapse-free survival rates.
  • Key factors associated with FGMM include ulceration, increased thickness, lower sun exposure, and specific mutations in the FGFR2 gene, suggesting that testing for FGFR2 could help identify patients at higher risk for aggressive disease.
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Tumor infiltration by T cells is paramount for effective anti-cancer immune responses. We hypothesized that the T cell receptor (TCR) repertoire of tumor infiltrating T lymphocytes could therefore be indicative of the functional state of these cells and determine disease course at different stages in cancer progression. Here we show that the diversity of the TCR of tumor infiltrating T cell at baseline is prognostic in various cancers, whereas the TCR clonality of T cell infiltrating metastatic melanoma pre-treatment is predictive for activity and efficacy of PD1 blockade immunotherapy.

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Article Synopsis
  • In 1967, Sandy Posey declared sunglasses as a must-have for beachgoers.
  • Recent whole-genome sequencing research shows that ultraviolet radiation (UVR) can lead to melanomas in the eye's iris and conjunctiva.
  • This research gives a scientific basis for the importance of wearing sunglasses to shield our eyes from harmful UVR exposure.
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There is a lack of appropriate melanoma models that can be used to evaluate the efficacy of novel therapeutic modalities. Here, we discuss the current state of the art of melanoma models including genetically engineered mouse, patient-derived xenograft, zebrafish, and ex vivo and in vitro models. We also identify five major challenges that can be addressed using such models, including metastasis and tumor dormancy, drug resistance, the melanoma immune response, and the impact of aging and environmental exposures on melanoma progression and drug resistance.

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Although identified as the key environmental driver of common cutaneous melanoma, the role of ultraviolet radiation (UVR)-induced DNA damage in mucosal melanoma is poorly defined. We analyze 10 mucosal melanomas of conjunctival origin by whole genome sequencing and our data shows a predominance of UVR-associated single base substitution signature 7 (SBS7) in the majority of the samples. Our data shows mucosal melanomas with SBS7 dominance have similar genomic patterns to cutaneous melanomas and therefore this subset should not be excluded from treatments currently used for common cutaneous melanoma.

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Background: Combination treatments targeting the MEK-ERK pathway and checkpoint inhibitors have improved overall survival in melanoma. Resistance to treatment especially in the brain remains challenging, and rare disease subtypes such as acral melanoma are not typically included in trials. Here we present analyses from longitudinal sampling of a patient with metastatic acral melanoma that became resistant to successive immune and targeted therapies.

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Background: The academia-industry interface is important, and, despite challenges that inevitably occur, bears the potential for positive synergies to emerge. Perceived barriers to wider collaboration in academia-industry oncology research in Europe need to be addressed, current academic cooperative group and industry models for collaboration need to be discussed, and a common terminology to facilitate understanding of both sectors' concerns needs to be established with an eye towards improving academia-industry partnerships on clinical trials for the benefit of patients with cancer.

Methodology: CAREFOR (Clinical Academic Cancer Research Forum), a multi-stakeholder platform formed to improve the direction for academic clinical trials in the field of oncology in Europe, formed the CAREFOR-Industry Working Group comprised of experienced professionals from European academic cooperative groups joined by industry representatives selected based on their activities in the area of medical oncology.

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