2004/09/02
DFP Roadmap
We would like to thank all of our users for their participation in the CASP 6 experiment. We have managed to predict a total of eight targets using DFP. While this is only a small fraction of the targets that were available, we chose some of the hardest ones to predict, and are anxious to see how the present method compares with our other more manual method, as well as other protein folding approaches, after the meeting in December.
After having put forth all our resources towards participation in CASP 6, we now need to step back and conduct a thorough analysis of our results, as well as an in-depth evaluation of all the methods used, including Distributed Folding.
Having limited resources available in our Structure group, we are faced with the following options:
Continue running DFP with the current algorithm, tweaking code in the process
Implement Boris Steipe's protein fragment libraries into the Phase II algorithm
Modify the Phase II algorithm into a true genetic algorithm
Shut down the DF project entirely to focus on development and improvement of our core algorithm via data analysis of available results
We feel that the project would benefit most from taking a break, namely the latter option, while we put our efforts towards providing you with a more robust, scientifically cutting edge platform.
We would like to extend our sincere thanks to all the users who have participated in the project over the past two and a half years. We are grateful for the countless CPU hours you have given us, for your improvement ideas, and for relentlessly testing any changes we made as we progressed towards better software. We have learned much about writing robust software, and we hope you have learned a little about the exciting world of protein folding.
With your help, we have been able to generate large amounts of scientifically significant data that has advanced our understanding of protein folding, and has enabled us to improve our folding algorithms, which may one day allow us to predict protein structure and folding pathways from sequence.
However, due to the aforementioned reasons, we have decided to bring the
Distributed Folding Project to an end upon reaching the 10 billion target on the current protein or on October 1, 2004, whichever comes last. We truly hope that our loyal user community keeps checking back for future distributed projects, as we certainly intend to return with newer and better ideas.
With gratitude,
Christopher Hogue, Howard Feldman and the Distributed Folding team
DFP Roadmap
We would like to thank all of our users for their participation in the CASP 6 experiment. We have managed to predict a total of eight targets using DFP. While this is only a small fraction of the targets that were available, we chose some of the hardest ones to predict, and are anxious to see how the present method compares with our other more manual method, as well as other protein folding approaches, after the meeting in December.
After having put forth all our resources towards participation in CASP 6, we now need to step back and conduct a thorough analysis of our results, as well as an in-depth evaluation of all the methods used, including Distributed Folding.
Having limited resources available in our Structure group, we are faced with the following options:
Continue running DFP with the current algorithm, tweaking code in the process
Implement Boris Steipe's protein fragment libraries into the Phase II algorithm
Modify the Phase II algorithm into a true genetic algorithm
Shut down the DF project entirely to focus on development and improvement of our core algorithm via data analysis of available results
We feel that the project would benefit most from taking a break, namely the latter option, while we put our efforts towards providing you with a more robust, scientifically cutting edge platform.
We would like to extend our sincere thanks to all the users who have participated in the project over the past two and a half years. We are grateful for the countless CPU hours you have given us, for your improvement ideas, and for relentlessly testing any changes we made as we progressed towards better software. We have learned much about writing robust software, and we hope you have learned a little about the exciting world of protein folding.
With your help, we have been able to generate large amounts of scientifically significant data that has advanced our understanding of protein folding, and has enabled us to improve our folding algorithms, which may one day allow us to predict protein structure and folding pathways from sequence.
However, due to the aforementioned reasons, we have decided to bring the
Distributed Folding Project to an end upon reaching the 10 billion target on the current protein or on October 1, 2004, whichever comes last. We truly hope that our loyal user community keeps checking back for future distributed projects, as we certainly intend to return with newer and better ideas.
With gratitude,
Christopher Hogue, Howard Feldman and the Distributed Folding team