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curious to know whether only 3-helix binder protein could be design if using scaffold-based binder design.

Open Huilin-Li opened this issue 1 year ago • 1 comments

Firstly I used de novo binder design --> only 1-helix binder protein will be designed. Then, I am using scaffold-based binder design by using the given 1000 scaffolds --> only 3-helix binder protein are designed. (inference.num_designs=10000).

Is it normal?

Huilin-Li avatar May 08 '24 04:05 Huilin-Li

Helical and helical bundle proteins are indeed favored by RFdiffusion, as it's slightly easier to diffuse into helices than beta sheets. However, RFdiffusion should be able to generate a large number of different topologies, so it's a bit surprising you don't see any variation over 10,000 designs.

My only thought is that if you have a particularly short protein, it may be hard for RFdiffusion to create a well-defined protein core with anything besides a short alpha helix or small helical bundle. You may want to try increasing your protein length (80-100 aa is often what's used for de novo design, but longer gives RFdiffusion more room to play around) to see if that increases the topological variation.

roccomoretti avatar Oct 09 '24 12:10 roccomoretti