Development of new therapeutic options for the treatment of uveal melanoma

Author:

Wang Janney Z.1,Lin Vivian2,Toumi Elsa2,Wang Ke3,Zhu Hong4ORCID,Conway R. Max56,Madigan Michele C.67,Murray Michael8,Cherepanoff Svetlana9,Zhou Fanfan1ORCID,Shu Wenying110

Affiliation:

1. Faculty of Medicine and Health Sydney Pharmacy School The University of Sydney NSW Australia

2. Faculty of Medicine The University of New South Wales Sydney NSW Australia

3. Key Laboratory of Nuclear Medicine Ministry of Health Jiangsu Key Laboratory of Molecular Nuclear Medicine Jiangsu Institute of Nuclear Medicine Wuxi China

4. Zhejiang Province Key Laboratory of Anti‐Cancer Drug Research College of Pharmaceutical Sciences Zhejiang University Hangzhou China

5. Ocular Oncology Unit Sydney Eye Hospital and The Kinghorn Cancer Centre NSW Australia

6. Save Sight Institute The University of Sydney NSW Australia

7. School of Optometry and Vision Sciences University of New South Wales Sydney NSW Australia

8. Discipline of Pharmacology Faculty of Medicine and Health The University of Sydney NSW Australia

9. SydPath Department of Anatomical Pathology St Vincent's Hospital Darlinghurst NSW Australia

10. Department of Pharmacy Affiliated Cancer Hospital & Institute of Guangzhou Medical University China

Abstract

Uveal melanoma (UM) is the most common primary intraocular malignancy in adults. Important cytogenetic and genetic risk factors for the development of UM include chromosome 3 monosomy, mutations in the guanine nucleotide‐binding proteins GNAQ/GNA11, and loss of the BRACA1‐associated protein 1 (BAP 1). Most primary UMs are treated conservatively with radiotherapy, but enucleation is necessary for large tumours. Despite the effectiveness of local control, up to 50% of UM patients develop metastasis for which there are no effective therapies. Attempts to utilise the targeted therapies that have been developed for the treatment of other cancers, including a range of signal transduction pathway inhibitors, have rarely produced significant outcomes in UM. Similarly, the application of immunotherapies that are effective in cutaneous melanoma to treat UM have also been disappointing. Other approaches that have been initiated involve proteasomal inhibitors and histone deacetylase inhibitors which are approved for the treatment of other cancers. Nevertheless, there have been occasional positive outcomes from these treatments in UM. Moreover, combination approaches in UM have also yielded some positive developments. It would be valuable to identify how to apply such therapies efficiently in UM, potentially via individualised tumour profiling. It would also be important to characterise UM tumours to differentiate the potential drivers of progression from those in other types of cancers. The recent identification of novel kinases and metastatic genes in UM tumours makes the development of new UM‐specific treatments feasible.

Funder

University of Sydney

Government of Jiangsu Province

Publisher

Wiley

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