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Contractile abnormalities of mouse muscles expressing hyperkalemic periodic paralysis mutant NaV1.4 channels do not correlate with Na+ influx or channel content.

Authors :
Lucas, Brooke
Ammar, Tarek
Khogali, Shiemaa
DeJong, Danica
Barbalinardo, Michael
Nishi, Cameron
Hayward, Lawrence J.
Renaud, Jean-Marc
Source :
Physiological Genomics. 6/1/2014, Vol. 46 Issue 11, p385-397. 13p.
Publication Year :
2014

Abstract

Hyperkalemic periodic paralysis (HyperKPP) is characterized by myotonic discharges that occur between episodic attacks of paralysis. Individuals with HyperKPP rarely suffer respiratory distress even though diaphragm muscle expresses the same defective Na+ channel isoform (NaV1.4) that causes symptoms in limb muscles. We tested the hypothesis that the extent of the HyperKPP phenotype (low force generation and shift toward oxidative type I and IIA fibers) in muscle is a function of 1) the NaV1.4 channel content and 2) the Na+ influx through the defective channels [i.e., the tetrodotoxin (TTX)-sensitive Na+ influx]. We measured NaV1.4 channel protein content, TTXsensitive Na+ influx, force generation, and myosin isoform expression in four muscles from knock-in mice expressing a NaV1.4 isoform corresponding to the human M1592V mutant. The HyperKPP flexor digitorum brevis muscle showed no contractile abnormalities, which correlated well with its low NaV1.4 protein content and by far the lowest TTX-sensitive Na+ influx. In contrast, diaphragm muscle expressing the HyperKPP mutant contained high levels of NaV1.4 protein and exhibited a TTX-sensitive Na+ influx that was 22% higher compared with affected extensor digitorum longus (EDL) and soleus muscles. Surprisingly, despite this high burden of Na+ influx, the contractility phenotype was very mild in mutant diaphragm compared with the robust abnormalities observed in EDL and soleus. This study provides evidence that HyperKPP phenotype does not depend solely on the NaV1.4 content or Na+ influx and that the diaphragm does not depend solely on Na+-K+ pumps to ameliorate the phenotype. [ABSTRACT FROM AUTHOR]

Details

Language :
English
ISSN :
10948341
Volume :
46
Issue :
11
Database :
Academic Search Index
Journal :
Physiological Genomics
Publication Type :
Academic Journal
Accession number :
103743302
Full Text :
https://doi.org/10.1152/physiolgenomics.00166.2013