Antiarrhythmic treatment strategies remain suboptimal due to our inability to predict how drug interactions with ion channels will affect the ability of the tissues to initiate and sustain an arrhythmia. We built a multiscale molecular model of the N

Chung, Woenho

Mangold, Kathryn

Moreno, Jonathan D

Silva, Jonathan R

Zhu, Wandi

English

Digital Commons@Becker

A molecularly detailed Na V 1.5 model reveals a new Class I antiarrhythmic target

https://digitalcommons.wustl.edu/cgi/viewcontent.cgi?article=9370&context=open_access_pubs

A molecularly detailed Na V 1.5 model reveals a new Class I antiarrhythmic target

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