Reduced expression of autotaxin predicts survival in uveal melanoma

Singh, Arun D.; Sisley, Karen; Xu, Yaomin; Li, Jianbo; Faber, Pieter; Plummer, Sarah J.; Mudhar, Hardeep Singh; Rennie, I G; Kessler, Patricia M.; Casey, Graham; Williams, Bryan R.G.

doi:10.1136/bjo.2007.116947

Cited by 37 publications

(25 citation statements)

References 44 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…It was shown that ATX is differentially expressed in non-cancerous (low) and cancerous (high) tissues, suggesting that ATX could be a marker of the process [105]. It has been suggested that serum ATX might be used as a marker in follicular lymphoma [61], uveal melanoma [106] or chronic hepatitis C [52,107].…”

Section: Autotaxin and Physio-pathologymentioning

confidence: 99%

Autotaxin

Boutin

Ferry

2009

Cell. Mol. Life Sci.

View full text Add to dashboard Cite

Autotaxin is a protein of approximately 900 amino acids discovered in the early 1990s. Over the past 15 years, a strong association between cancer cells and autotaxin production has been observed. Recent publications indicate that autotaxin and the capacity of cancer to metastasise are intimately linked. The discovery of new molecular targets in pharmacology is a mixture of pure luck, hard work and industrial strategy. Despite a crucial and desperate need for new therapeutic tools, many targets are approached in oncology, but only a few are validated and end up at the patient bed. Outside the busy domain of kinases, few targets have been discovered that can be useful in treating cancer, particularly metastatic processes. The fortuitous relationship between autotaxin and lysophosphatidic acid renders the results of observations made in the diabetes/obesity context considerably important. The literature provides observations that may aid in redesigning experiments to validate autotaxin as a potential oncology target.

show abstract

Section: Autotaxin and Physio-pathologymentioning

confidence: 99%

Autotaxin

Boutin

Ferry

2009

Cell. Mol. Life Sci.

View full text Add to dashboard Cite

show abstract

“…High-throughput technologies, including cDNA microarrays and aCGH array analysis, have been the focus of many recent papers that have identiWed various "molecular-genetic signatures" for this particular neoplasm Zuidervaart et al 2003;Onken et al 2004;Marshall et al 2007;Meir et al 2007;Singh et al 2007). While these papers have presented very consistent data that identify signiWcant chromosomal aberrations in chromosome 3, 6 and 8 (Aalto et al 2001;White et al 2006;Onken et al 2007;Mensink et al 2008;van Gils et al 2008), the tissue used for these transcriptional studies were mostly fresh frozen and are more diYcult to acquire due to the fact that enucleation is no longer the primary treatment for UM.…”

Section: Introductionmentioning

confidence: 99%

Expression profiling of formalin-fixed paraffin embedded primary human uveal melanomas using DASL matrices

Cesare

Nantel

Marshall

et al. 2009

J Cancer Res Clin Oncol

View full text Add to dashboard Cite

“…When two gene signatures of 25 uveal melanomas were compared with respect to a 92-month survival probability, gene expression profiling was found to be associated with survival [25]. Singh et al [26] studied gene expression data of 27 uveal melanoma samples and showed that a poor patient survival was related to the expression of genes encoding the histocompatibility complex class I and class II, as well as other immune response genes (e.g. the nuclear factor of activated T cells, macrophage stimulating pseudogene 9).…”

Section: Genome-wide Microarray Analysismentioning

confidence: 99%

Uveal Melanoma: The Inflammatory Microenvironment

Bronkhorst

Jager²

2012

J Innate Immun

View full text Add to dashboard Cite

Uveal melanoma is a highly malignant intraocular tumor with quite homogeneous tumor tissue and a diffuse leukocytic infiltration. In contrast with many other malignancies, the presence of infiltrating macrophages and T cells is associated with a poor prognosis rather than a good one. The clear link between inflammation and cancer in this malignancy provides a paradigm for macrophage plasticity and function. Macrophages in uveal melanoma have an M2-like phenotype and are associated with the loss of one specific chromosome – monosomy 3. The central players involved in this process and discussed in this review include macrophages, T lymphocytes, chemokines and cytokines, including the macrophage-attraction molecules. When a tumor acquires the ability to release significant amounts of macrophage-attraction molecules it causes the expansion of a population of myeloid immature cells that may not only help the tumor to suppress immune reactions but also aid in the construction of new blood vessels for tumor growth. A better understanding of the molecular basis of a local myelomonocytic cell population will bring a better understanding of the immunopathology of this disease and will lead to therapeutic interventions in uveal melanoma. This review focuses on the roles of the local inflammatory microenvironment in the development and progression of uveal melanoma.

show abstract

Reduced expression of autotaxin predicts survival in uveal melanoma

Cited by 37 publications

References 44 publications

Autotaxin

Autotaxin

Expression profiling of formalin-fixed paraffin embedded primary human uveal melanomas using DASL matrices

Uveal Melanoma: The Inflammatory Microenvironment

Contact Info

Product

Resources

About