A twitter explainer for our latest #teamscience study rdcu.be/KwgV congrats Josh @stephanie_mul @dliu_ccb @nikolausschultz Arul @CharlesSawyers et al @PCFnews @SU2C @DanaFarber @broadinstitute @MSKCC_OncoNotes @NatureGenet [1/n]

About two years ago, @stephanie_mul tallied the whole exome data we had & mapped it against theoretical power calculations @gaddyg set forth for discovering significant cancer genes in any cancer type (see: ncbi.nlm.nih.gov/pubmed/24390350)

Turned out we had a lot! So we started wondering, "If you have enough tumor genomics in any one cancer type, can you find mutations in genes that invoke *all* Cancer Hallmarks, even those never seen in that cancer?" (see: cell.com/abstract/S0092…)

After numerous analyses, realigning, re-re-aligning, re-analysis, etc, we had a refined set of 1,013 #prostatecancer exomes - in 2018, we also now have many cancer genomics & biology priors to apply with a statistical framework (h/t @MarkARubin1) and learn!

Main finding: A true “long tail” of significantly mutated genes in #prostatecancer, including genes/pathways we had no idea were involved & rare, but helped us cover the remaining territory of the Cancer Hallmarks (e.g. SF3B1/splicing, Ras signaling)

We also saw an entire subclass of prostate cancer with mutations exclusively in epigenetic genes, raising new therapeutic & tumor-immune hypotheses, plus new collabs with @kadochlab @CKadoch et al cc: @SKCCDirector

With a bigger cohort, we also could take a better swing at defining a genomic “signature” of metastatic vs. primary prostate cancer – we are still a long way from a clinical test, but the potential is vast, e.g. wsj.com/articles/prost… @LucetteLagnado

Of course, we hope to augment this cohort (exclusively from academic sites via traditional means) with the patient-driven Metastatic Prostate Cancer Project cohort → 3 months in & 100s of men have said “Count Me In!” mpcproject.org @PrCaProject @corrie_painter et al