Journal article
Clinical and pathological associations of the activating RAC1 P29S mutation in primary cutaneous melanoma
VJ Mar, SQ Wong, A Logan, T Nguyen, J Cebon, JW Kelly, R Wolfe, A Dobrovic, C Mclean, GA Mcarthur
Pigment Cell and Melanoma Research | Published : 2014
DOI: 10.1111/pcmr.12295
Abstract
Activating mutations in the GTPase RAC1 are a recurrent event in cutaneous melanoma. We investigated the clinical and pathological associations of RAC1P29S in a cohort of 814 primary cutaneous melanomas with known BRAF and NRAS mutation status. The RAC1P29S mutation had a prevalence of 3.3% and was associated with increased thickness (OR=1.6 P = 0.001), increased mitotic rate (OR=1.3 P = 0.03), ulceration (OR=2.4 P = 0.04), nodular subtype (OR=3.4 P = 0.004), and nodal disease at diagnosis (OR=3.3 P = 0.006). BRAF mutant tumors were also associated with nodal metastases (OR=1.9 P = 0.004), despite being thinner at diagnosis than BRAF WT (median 1.2 mm versus 1.6 mm, P < 0.001). Immunohistoch..
View full abstractRelated Projects (2)
Grants
Awarded by Victorian Government through the Victorian Cancer Agency Translational Research Program
Awarded by National Health and Medical Research Council of Australia (NHMRC)
Funding Acknowledgements
This project was enabled by the Melbourne Melanoma Project funded by the Victorian Government through the Victorian Cancer Agency Translational Research Program Grant (EOI09_27). Professor Grant A McArthur is also supported by a Program Grant APP1053792 and Practitioner Fellowship 1002654 of the National Health and Medical Research Council of Australia (NHMRC). Victoria J Mar was supported by an NHMRC PhD Scholarship. The authors wish to acknowledge Sonia Mailer, Sue Sturrock, Karen Scott, Anne Fennessy, and Joanne Hawking for their assistance with data and specimen collection.