Molecular & Cancer Biomarkers

Biography

Biography: Devika Agarwal

Abstract

Despite immense success in the diagnosis and treatment of  breast cancer (BC), effective delivery of personalised medicine is needed. This requires the discovery of novel therapeutic targets in subgroups of BC and improvements in treatment efficiency by identifying biomarkers that can predict an individuals response to therapy.  Although chemotherapy is offered in combination with other targeted therapies to 60% of BC patients, it reduces recurrence and mortality rates by only 30%. Given that all the prognostic power of majority of  commercial gene assays for guiding therapy comes from genes related to cell proliferation, a St Gallens Expert consensus have recommended the use of proliferation markers/gene assays when choosing an optimal systemic treatment. However, the decision for the the best molecular test/marker to be used continues to be debated. The use of novel non-linear computational approaches with sufficient power are urgently needed to identify biomarkers with high specificity and sensitivity. An aritificial neural network based integrative data mining approach was  applied to multiple BC gene expressions studies (n=2000), using factors (e.g. Grade) that are associated with proliferation as clinical class questions and individual genes as predictors.  This analysis identified the marker SPAG5 , among the 30 most common genes for the top 100 ranked genes for the proliferation factors across the datasets. Further clinical validation in excess of 10,000 patients revealed amplication of SPAG5 in 10-20% of BC , SPAG5 gene CNAs , mRNA and protein expression are associated with poor clinical outcome and predictors of response to chemotherapy.