I have downloaded all the VCF files for one cancer type from the TCGA. Upon annotation using Annovar, I notice that there are a lot more variants than I expected. So I have a few questions:

1. How should I process these downstream? I've already reduced the list based on those that passed.
2. I particularly wanted the mutation profiles of individuals before MutSig. Is using the VCF files the best way to do this, or should I just get the MAF file? My assumption was that the MAF file was MutSig processed.

Thank you.

TCGA VCFs are raw mutation lists, straight out of the automated variant calling pipelines. TCGA MAFs are also mutation lists, but have (usually) undergone expert curation to remove false-positives, or recover known calls missed by the automated pipelines. This post should give you a good intro to TCGA VCFs and MAFs - Working with MAF files (Mutation Annotation Format) from the TCGA (The Cancer Genome Atlas). The MAF is usually the best place to start for good science, unless you are confident that the VCFs contain data you need, that was removed in the corresponding MAF. Take a look at this post to find and re-annotate the MAF for your cancer type - Annotating TCGA MAFs with the latest Ensembl/Gencode transcripts