Jessa L Aldridge, Emily Davis Alexander, Allison A Franklin, Chad R Frasier
{"title":"管理活性氧增加的能力下降可能是缺乏 Scn1b 的小鼠易患心律失常的原因。","authors":"Jessa L Aldridge, Emily Davis Alexander, Allison A Franklin, Chad R Frasier","doi":"10.1152/ajpheart.00265.2024","DOIUrl":null,"url":null,"abstract":"<p><p><i>Scn1b</i> plays essential roles in the heart, where it encodes β<sub>1</sub>-subunits that serve as modifiers of gene expression, cell surface channel activity, and cardiac conductivity. Reduced β<sub>1</sub> function is linked to electrical instability in various diseases with cardiac manifestations and increased susceptibility to arrhythmias. Recently, we demonstrated that loss of <i>Scn1b</i> in mice leads to compromised mitochondria energetics and reactive oxygen species (ROS) production. In this study, we examined the link between increased ROS and arrhythmia susceptibility in <i>Scn1b</i><sup>-/-</sup> mice. In addition, ROS-scavenging capacity can be overwhelmed during prolonged oxidative stress, increasing arrhythmia susceptibility. Therefore, we isolated whole hearts and cardiomyocytes from <i>Scn1b</i><sup>-/-</sup> and <i>Scn1b<sup>+/+</sup></i> mice and subjected them to an oxidative challenge with diamide, a glutathione oxidant. Next, we analyzed gene expression and activity of antioxidant enzymes in <i>Scn1b<sup>-/-</sup></i> hearts. Cells isolated from <i>Scn1b<sup>-/-</sup></i> hearts died faster and displayed higher rates of ROS accumulation preceding cell death compared with those from <i>Scn1b<sup>+/+</sup></i>. Furthermore, <i>Scn1b<sup>-/-</sup></i> hearts showed higher arrhythmia scores and spent less time free of arrhythmia. Lastly, we found that protein expression and enzymatic activity of glutathione peroxidase is increased in <i>Scn1b<sup>-/-</sup></i> hearts compared with wild type. Our results indicate that <i>Scn1b<sup>-/-</sup></i> mice have decreased capability to manage ROS during prolonged oxidative stress. ROS accumulation is elevated and appears to overwhelm ROS scavenging through the glutathione system. This imbalance creates the potential for altered cell energetics that may underlie increased susceptibility to arrhythmias or other adverse cardiac outcomes.<b>NEW & NOTEWORTHY</b> Using an oxidative challenge, we demonstrated that isolated cells from <i>Scn1b<sup>-/-</sup></i> mice are more susceptible to cell death and surges in reactive oxygen species accumulation. At the whole organ level, they were also more susceptible to the formation of cardiac arrhythmias. This may in part be due to changes to the glutathione antioxidant system.</p>","PeriodicalId":7692,"journal":{"name":"American journal of physiology. Heart and circulatory physiology","volume":" ","pages":"H723-H732"},"PeriodicalIF":4.1000,"publicationDate":"2024-10-01","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"https://www.ncbi.nlm.nih.gov/pmc/articles/PMC11482272/pdf/","citationCount":"0","resultStr":"{\"title\":\"Decreased ability to manage increases in reactive oxygen species may underlie susceptibility to arrhythmias in mice lacking <i>Scn1b</i>.\",\"authors\":\"Jessa L Aldridge, Emily Davis Alexander, Allison A Franklin, Chad R Frasier\",\"doi\":\"10.1152/ajpheart.00265.2024\",\"DOIUrl\":null,\"url\":null,\"abstract\":\"<p><p><i>Scn1b</i> plays essential roles in the heart, where it encodes β<sub>1</sub>-subunits that serve as modifiers of gene expression, cell surface channel activity, and cardiac conductivity. Reduced β<sub>1</sub> function is linked to electrical instability in various diseases with cardiac manifestations and increased susceptibility to arrhythmias. Recently, we demonstrated that loss of <i>Scn1b</i> in mice leads to compromised mitochondria energetics and reactive oxygen species (ROS) production. In this study, we examined the link between increased ROS and arrhythmia susceptibility in <i>Scn1b</i><sup>-/-</sup> mice. In addition, ROS-scavenging capacity can be overwhelmed during prolonged oxidative stress, increasing arrhythmia susceptibility. Therefore, we isolated whole hearts and cardiomyocytes from <i>Scn1b</i><sup>-/-</sup> and <i>Scn1b<sup>+/+</sup></i> mice and subjected them to an oxidative challenge with diamide, a glutathione oxidant. Next, we analyzed gene expression and activity of antioxidant enzymes in <i>Scn1b<sup>-/-</sup></i> hearts. Cells isolated from <i>Scn1b<sup>-/-</sup></i> hearts died faster and displayed higher rates of ROS accumulation preceding cell death compared with those from <i>Scn1b<sup>+/+</sup></i>. Furthermore, <i>Scn1b<sup>-/-</sup></i> hearts showed higher arrhythmia scores and spent less time free of arrhythmia. Lastly, we found that protein expression and enzymatic activity of glutathione peroxidase is increased in <i>Scn1b<sup>-/-</sup></i> hearts compared with wild type. Our results indicate that <i>Scn1b<sup>-/-</sup></i> mice have decreased capability to manage ROS during prolonged oxidative stress. ROS accumulation is elevated and appears to overwhelm ROS scavenging through the glutathione system. This imbalance creates the potential for altered cell energetics that may underlie increased susceptibility to arrhythmias or other adverse cardiac outcomes.<b>NEW & NOTEWORTHY</b> Using an oxidative challenge, we demonstrated that isolated cells from <i>Scn1b<sup>-/-</sup></i> mice are more susceptible to cell death and surges in reactive oxygen species accumulation. At the whole organ level, they were also more susceptible to the formation of cardiac arrhythmias. 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Decreased ability to manage increases in reactive oxygen species may underlie susceptibility to arrhythmias in mice lacking Scn1b.
Scn1b plays essential roles in the heart, where it encodes β1-subunits that serve as modifiers of gene expression, cell surface channel activity, and cardiac conductivity. Reduced β1 function is linked to electrical instability in various diseases with cardiac manifestations and increased susceptibility to arrhythmias. Recently, we demonstrated that loss of Scn1b in mice leads to compromised mitochondria energetics and reactive oxygen species (ROS) production. In this study, we examined the link between increased ROS and arrhythmia susceptibility in Scn1b-/- mice. In addition, ROS-scavenging capacity can be overwhelmed during prolonged oxidative stress, increasing arrhythmia susceptibility. Therefore, we isolated whole hearts and cardiomyocytes from Scn1b-/- and Scn1b+/+ mice and subjected them to an oxidative challenge with diamide, a glutathione oxidant. Next, we analyzed gene expression and activity of antioxidant enzymes in Scn1b-/- hearts. Cells isolated from Scn1b-/- hearts died faster and displayed higher rates of ROS accumulation preceding cell death compared with those from Scn1b+/+. Furthermore, Scn1b-/- hearts showed higher arrhythmia scores and spent less time free of arrhythmia. Lastly, we found that protein expression and enzymatic activity of glutathione peroxidase is increased in Scn1b-/- hearts compared with wild type. Our results indicate that Scn1b-/- mice have decreased capability to manage ROS during prolonged oxidative stress. ROS accumulation is elevated and appears to overwhelm ROS scavenging through the glutathione system. This imbalance creates the potential for altered cell energetics that may underlie increased susceptibility to arrhythmias or other adverse cardiac outcomes.NEW & NOTEWORTHY Using an oxidative challenge, we demonstrated that isolated cells from Scn1b-/- mice are more susceptible to cell death and surges in reactive oxygen species accumulation. At the whole organ level, they were also more susceptible to the formation of cardiac arrhythmias. This may in part be due to changes to the glutathione antioxidant system.
期刊介绍:
The American Journal of Physiology-Heart and Circulatory Physiology publishes original investigations, reviews and perspectives on the physiology of the heart, vasculature, and lymphatics. These articles include experimental and theoretical studies of cardiovascular function at all levels of organization ranging from the intact and integrative animal and organ function to the cellular, subcellular, and molecular levels. The journal embraces new descriptions of these functions and their control systems, as well as their basis in biochemistry, biophysics, genetics, and cell biology. Preference is given to research that provides significant new mechanistic physiological insights that determine the performance of the normal and abnormal heart and circulation.
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