Sema3a Maintains Normal Heart Rhythm Through Sympathetic Innervation Patterning

Overview

Journal Nat Med

Specialties General Medicine
Molecular Biology

Date 2007 Apr 10

PMID 17417650

Citations 105

Authors

Masaki Ieda

Hideaki Kanazawa

Kensuke Kimura

Fumiyuki Hattori

Yasuyo Ieda

Masahiko Taniguchi

Jong-Kook Lee

Keisuke Matsumura

Yuichi Tomita

Shunichiro Miyoshi

Kouji Shimoda

Shinji Makino

Motoaki Sano

Itsuo Kodama

Satoshi Ogawa

Keiichi Fukuda

Affiliations

Soon will be listed here.

Abstract

Sympathetic innervation is critical for effective cardiac function. However, the developmental and regulatory mechanisms determining the density and patterning of cardiac sympathetic innervation remain unclear, as does the role of this innervation in arrhythmogenesis. Here we show that a neural chemorepellent, Sema3a, establishes cardiac sympathetic innervation patterning. Sema3a is abundantly expressed in the trabecular layer in early-stage embryos but is restricted to Purkinje fibers after birth, forming an epicardial-to-endocardial transmural sympathetic innervation patterning. Sema3a(-/-) mice lacked a cardiac sympathetic innervation gradient and exhibited stellate ganglia malformation, which led to marked sinus bradycardia due to sympathetic dysfunction. Cardiac-specific overexpression of Sema3a in transgenic mice (SemaTG) was associated with reduced sympathetic innervation and attenuation of the epicardial-to-endocardial innervation gradient. SemaTG mice demonstrated sudden death and susceptibility to ventricular tachycardia, due to catecholamine supersensitivity and prolongation of the action potential duration. We conclude that appropriate cardiac Sema3a expression is needed for sympathetic innervation patterning and is critical for heart rate control.

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