nitric oxide is necessary for diazoxide protection against ischemic injury in skeletal muscle

Authors

hossein farahini department of orthopedic surgery, tehran university of medical sciences, tehran, iran.

marjan ajami department of nutrition, school of public health, tehran university of medical sciences, tehran, iran. physiology research center, tehran univercity of medical sciences, tehran, iran.

jalaledin mirzay razaz nano medicine and tissue engineering center, shahid beheshti university of medical sciences, tehran, iran.

nahid azad cellular and molecular research center, tehran university of medical sciences, tehran, iran.

abstract

ischemia reperfusion injury (ir injury) is a common problem in clinical conditions. researches have frequently revealed that atp- sensitive potassium (katp) channels and nitric oxide plays a role in protection against ischemic injury in skeletal muscle. the present study aimed at evaluating the possible link between this two pathways. sixty-eight male wistar rats, were pretreated with saline, diazoxide (katp opener; 45 mg/kg, ip), glibenclamide (katp inhibitor; 5 mg/kg), or l-name (inos inhibitor; 20 mg/kg, ip) before 3 h ischemia and 2 h reperfusion. activities of antioxidant enzymes superoxide dismutase (sod) and catalase (cat), and the level of malondialdehyde (mda) and expression of inos were measured in muscle tissue. tissue mda content was significantly increased by ir (p < 0.001). diazoxide significantly decreased the ir-induced elevation of tissue mda level (p < 0.05) and glibenclamide increased mda (p < 0.05 vs. ir group). l-name inhibited the effect of diazoxide on decreasing mda (p < 0.01 vs., diazoxide+ir group) and ir decreased the activity of sod and cat (p < 0.01), while pretreatment with diazoxide increased activity of sod and cat (p < 0.01). glibenclamide decreased sod and cat activity after ir (p < 0.05). l-name pretreatment in diazoxide-treated rats abolished the effect of diazoxide on increasing the activity of sod and cat (p < 0.05 vs. diaz+ir). expression of inos was increased by ir (p < 0.01 vs. sham group). diazoxide significantly decreased inos expression after ir (p < 0.05 vs. ir). l-name significantly decreased inos expression after ir (p < 0.01) in diazoxide-treated rats (p < 0.01 vs. diaz+ir).

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Journal title:
iranian journal of pharmaceutical research

جلد ۱۱، شماره ۱، صفحات ۳۷۵-۳۸۱

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