Hello, everyone:

I want to get some annotations on some snps, using ucsc as primary annotation source.

As i know, UCSC defined some important regulators, such as Yale TFBS, and regulatory elements.

In some paper, i found that the author tended to consider some trascription factors as most important, such as c-Myc sirt6 c-Fox MAX...

it is true that TFBS of these transcription factors are very important, but how can we just consider these facotrs while neglecting the others? is there any evidence or reference could tell me the criteria of this classification?

and for regulatory elements such as cpgislandext...?

ps:i have used ANNOVAR doing the annotation of these snps, but i seemed that it was not clear enough to explain the exact reason linking to my investigated cancer target.

Thanks for sparing your time!

Why those transcription factors (TFs)? Because they are important and popular and tools are available to test them (antibodies, well characterized binding sites, known/interesting biology, etc.). However, these are by no means the only important TFs. Look at FANTOM and their work - they have some 1000 TFs in mind for the human genome. ENCODE and company would like to map binding sites for all TFs and just started with what you see in the databases.

Maybe for the cell type or biological process that interests you or your research group a handful of other TFs are important and override the need to look at MYC, NFKB1, FOS and others. So, take a step back to the biological question you're addressing and see which resources are available to answer that question. It may turn out that you need to upload into UCSC (as custom tracks) a set of TF data other than what they already have. These new data may come from a study on one of your key TFs because it is just what you need.

If you want all TFBSs, you'll have to wait and hunt. Wait: Not all TFBSs are known for the 1000 or so human TFs. Hunt: Many more are known than are commonly displayed, but you'll have to hunt them down from various resources.