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Toward real-time modeling of human heart ventricles at cellular resolution: Simulation of drug-induced arrhythmias
Author(s) -
A.A. Mirin,
David F. Richards,
James N. Glosli,
Erik W. Draeger,
Bor Chan,
JeanLuc Fattebert,
William D. Krauss,
Tomas Oppelstrup,
John Jeremy Rice,
John A. Gunnels,
Viatcheslav Gurev,
Changhoan Kim,
J. H. Magerlein,
Matthias Reumann,
Hui-Fang Wen
Publication year - 2012
Publication title -
international conference for high performance computing, networking, storage and analysis
Language(s) - English
Resource type - Conference proceedings
SCImago Journal Rank - 0.363
H-Index - 56
ISSN - 2167-4337
ISBN - 978-1-4673-0804-5
DOI - 10.1109/sc.2012.108
Subject(s) - scalability , computer science , cardiac electrophysiology , sudden cardiac death , ibm , national laboratory , simulation , cardiology , medicine , electrophysiology , physics , materials science , operating system , nanotechnology , engineering physics
We have developed a highly efficient and scalable cardiac electrophysiology simulation capability that supports groundbreaking resolution and detail to elucidate the mechanisms of sudden cardiac death from arrhythmia. We can simulate thousands of heartbeats at a resolution of 0.1 mm, comparable to the size of cardiac cells, thereby enabling scientific inquiry not previously possible. Based on scaling results from the partially deployed Sequoia IBM Blue Gene/Q machine at Lawrence Livermore National Laboratory and planned optimizations, we estimate that by SC12 we will simulate 8--10 heartbeats per minute --- a time-to-solution 400--500 times faster than the state-of-the-art. Performance between 8 and 11 PFlop/s on the full 1,572,864 cores is anticipated, representing 40--55 percent of peak. The power of the model is demonstrated by illuminating the subtle arrhythmogenic mechanisms of anti-arrhythmic drugs that paradoxically increase arrhythmias in some patient populations.

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