Literature DB >> 22695420

Nitrite reduces ischemia/reperfusion-induced muscle damage and improves survival rates in rat crush injury model.

Isamu Murata1, Ryo Nozaki, Kazuya Ooi, Kazuo Ohtake, Soichiro Kimura, Hideo Ueda, Genya Nakano, Kunihiro Sonoda, Yutaka Inoue, Hiroyuki Uchida, Ikuo Kanamoto, Yasunori Morimoto, Jun Kobayashi.   

Abstract

BACKGROUND: Nitrite is an intrinsic signaling molecule with potential therapeutic implications in mammalian ischemia/reperfusion (I/R) injury of the heart, liver, and kidney. Although limb muscle compression and subsequent reperfusion are the causative factors in developing crush syndrome (CS), there has been no report evaluating the therapeutic effects of nitrite on CS. We therefore tested whether nitrite could be a therapeutic agent for the treatment of CS.
METHODS: To create a CS model, anesthetized rats were subjected to bilateral hind limb compression with rubber tourniquets for 5 hours, followed by reperfusion for 0 hour to 6 hours while monitoring blood pressure. Saline for the CS group or sodium nitrite (NaNO(2)-100, 200, and 500 μmol/kg) for the nitrite-treated CS groups was intravenously administered immediately before reperfusion. Blood and tissue samples were collected for biochemical analysis.
RESULTS: Tissue nitrite levels in injured muscles were significantly reduced in the CS group compared with the sham group during I/R injury. Nitrite administration to CS rats restored nitric oxide bioavailability by enhancing nitrite levels of the muscle, resulting in a reduction of rhabdomyolysis markers such as potassium, lactate dehydrogenase, and creatine phosphokinase. Nitrite treatment also reduced plasma levels of interleukin-6 and myeloperoxidase activities in muscle and lung tissues, finally resulting in a dose-dependent improvement of survival rate from 24% (CS group) to 36% (NaNO(2)-100 group) and 64% (NaNO(2)-200 and 500 groups).
CONCLUSION: These results indicate that nitrite reduces I/R-induced muscle damage through its cytoprotective action and contributes to improved survival rate in a rat CS model.
Copyright © 2012 by Lippincott Williams & Wilkins.

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Year:  2012        PMID: 22695420     DOI: 10.1097/TA.0b013e31824a76b5

Source DB:  PubMed          Journal:  J Trauma Acute Care Surg        ISSN: 2163-0755            Impact factor:   3.313


  16 in total

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2.  The macrophage stimulating anti-cancer agent, RRx-001, protects against ischemia-reperfusion injury.

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4.  Beneficial effects of bardoxolone methyl, an Nrf2 activator, on crush-related acute kidney injury in rats.

Authors:  Emine Kadıoğlu; Yasemin Tekşen; Cengiz Koçak; Fatma Emel Koçak
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Authors:  Isamu Murata; Ryota Kawanishi; Syo Inoue; Moeko Iwata; Jun Kobayashi; Yutaka Inoue; Ikuo Kanamoto
Journal:  Eur J Trauma Emerg Surg       Date:  2018-07-27       Impact factor: 3.693

Review 6.  Nitrite in organ protection.

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Journal:  Br J Pharmacol       Date:  2014-01       Impact factor: 8.739

7.  Alterations of biochemical marker levels and myonuclear numbers in rat skeletal muscle after ischemia-reperfusion.

Authors:  Motoharu Itoh; Noriaki Shimokawa; Yuki Tajika; Tohru Murakami; Nobutaka Aotsuka; Ronny Lesmana; Reni Farenia; Toshiharu Iwasaki; Junichi Okda; Hiroshi Yorifuji; Noriyuki Koibuchi
Journal:  Mol Cell Biochem       Date:  2012-10-13       Impact factor: 3.396

8.  Systemic Inflammatory Response and Multiple Organ Dysfunctions Following Crush Injury: a New Experimental Model in Rabbits.

Authors:  Peng Xu; Fei Wang; Xian-Long Zhou; Lei Li; Dan Xiong; Yong-Quan Yong; Yan Zhao; Wang-Xiang Jiang
Journal:  Inflammation       Date:  2018-02       Impact factor: 4.092

9.  β1-Blocker improves survival and ventricular remodelling in rats with lethal crush injury.

Authors:  Mengyang Yu; Qi Lv; Jie Shi; Yahua Liu; Haojun Fan; Hui Ding; Ziquan Liu; Juan Cao; Yanhua Gong; Shike Hou
Journal:  Eur J Trauma Emerg Surg       Date:  2020-06-02       Impact factor: 3.693

10.  Therapeutic Potential of the Nitrite-Generated NO Pathway in Vascular Dysfunction.

Authors:  Michael Madigan; Brian Zuckerbraun
Journal:  Front Immunol       Date:  2013-07-02       Impact factor: 7.561

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