Attenuation of Skeletal Muscle and Renal Injury to the Lower Limb following Ischemia-Reperfusion Using mPTP Inhibitor NIM-811

Garcı́a-Dorado, David; Turóczi, Zsolt; Arányi, Péter; Fülöp, András; Oliver, Roland; Hermesz, Edit; Ferencz, Ágnes; Lotz, Gábor; Harsányi, László; Szíjártó, Attila

doi:10.1371/journal.pone.0101067

Cited by 38 publications

(33 citation statements)

References 60 publications

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“…In young rats, we previously observed that CsA restored skeletal muscle mitochondrial coupling and reduced ROS production during hindlimb IR [23]. Similarly, CsA enhanced mitochondrial recovery after lattissimus dorsi flaps IR in pigs [22] and a nonimmunosuppressive CsA derivative (NIM-811) reduced skeletal muscle injury after IR [24]. Remarkably, the protective effects provided by 10 mg/kg intravenous CsA, given 5 min before reperfusion (reduced muscle infarction, reduced myeloperoxidase activity, and reduced muscle calcium content), were abolished when a mPTP opener atractyloside was injected [22] supporting that CsA is still able to maintain the mPTP in the 'closed' mode, even when provided after ischemia.…”

Section: Effects Of Cyclosporinementioning

confidence: 88%

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Skeletal muscle ischemia–reperfusion injury and cyclosporine A in the aging rat

Pottecher

Kindo

Chamaraux-Tran

et al. 2016

Fundamemntal Clinical Pharma

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Old patients exhibit muscle impairments and increased perioperative risk during vascular surgery procedures. Although aging generally impairs protective mechanisms, data are lacking concerning skeletal muscle in elderly. We tested whether cyclosporine A (CsA), which protects skeletal muscle from ischemia-reperfusion (IR) in young rats, might reduce skeletal muscle mitochondrial dysfunction and oxidative stress in aging rats submitted to hindlimb IR. Wistar rats aged 71-73 weeks were randomized to IR (3 h unilateral tourniquet application and 2 h reperfusion) or IR + CsA (10 mg/kg cyclosporine IV before reperfusion). Maximal oxidative capacity (VM ax ), acceptor control ratio (ACR), and relative contribution of the mitochondrial respiratory chain complexes II, III, IV (VS ucc ), and IV (VTMPD /Asc ), together with calcium retention capacity (CRC) a marker of apoptosis, and tissue reactive oxygen species (ROS) production were determined in gastrocnemius muscles from both hindlimbs. Compared to the nonischemic hindlimb, IR significantly reduced mitochondrial coupling, VMax (from 7.34 ± 1.50 to 2.87 ± 1.22 μMO2 /min/g; P < 0.05; -70%), and VS ucc (from 6.14 ± 1.07 to 3.82 ± 0.83 μMO2 /min/g; P < 0.05; -42%) but not VTMPD /Asc . IR also decreased the CRC from 15.58 ± 3.85 to 6.19 ± 0.86 μMCa(2+) /min/g; P < 0.05; -42%). These alterations were not corrected by CsA (-77%, -49%, and -32% after IR for VM ax, VS ucc , and CRC, respectively). Further, CsA significantly increased ROS production in both hindlimbs (P < 0.05; +73%). In old rats, hindlimb IR impairs skeletal muscle mitochondrial function and increases oxidative stress. Cyclosporine A did not show protective effects.

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Section: Effects Of Cyclosporinementioning

confidence: 88%

“…CsA inhibits mitochondrial transition pore (mPTP) opening and therefore antagonizes apoptosis. CsA given at the onset of reperfusion was shown to protect myocardial [21] and skeletal muscles [22][23][24] from IR-induced injury in adult patients and rats, respectively.…”

Section: Introductionmentioning

confidence: 99%

Skeletal muscle ischemia–reperfusion injury and cyclosporine A in the aging rat

Pottecher

Kindo

Chamaraux-Tran

et al. 2016

Fundamemntal Clinical Pharma

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“…There is an increase in local injury, necrosis and rhabdomyolysis, as well as of their systemic repercussions. The metabolics and pro-inflammatory cytokines originating from muscular injury may induce Systemic Inflammatory Response Syndrome, and may affect distant organs, such as kidneys, lung and gastrointestinal tract -multiple organ dysfunction 13 . Among these organs, the lung was the one analyzed in the present study.…”

Section: ■ Discussionmentioning

confidence: 99%

The influence of allopurinol and post-conditioning on lung injuries induced by lower-limb ischemia and reperfusion in Wistar rats

Akahane

Gomes²,

Paludo³

et al. 2017

Acta Cir. Bras.

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1 AbstractPurpose: To analyze the effects of allopurinol and of post-conditioning on lung injuries induced by lower-limb ischemia and reperfusion. Methods: Thirty rats were used. They were divided in 5 groups: (1) group A: abdominal aortic dissection only, (2) group B: ischemia and reperfusion, (3) group C: administered allopurinol (100mg/Kg) a few hours before procedure, (4) group D: post-conditioned and (5) group E: administered allopurinol and post-conditioned. With the exception of group A, all groups were submitted to infrarenal aortic ischemia for 2 hours, and reperfusion for 72 hours. After euthanasia, lungs were removed for histological analysis. They were graded under two scores: pulmonary injury (neutrophil infiltration, interstitial edema, vascular congestion, and destruction of lung architecture) and lymphocytic score (neutrophil infiltration, lymphoid aggregate and secondary follicle). Results: On the pulmonary injury score, the degree of injury was smaller than in groups D and E, when compared to group B, p<0.05. Group C did not obtain the same result (p>0,05). On the lymphocytic score, there was no statistic difference among groups, p>0.05. Conclusion: Both post-conditioning and the combination of allopurinol and post-conditioning were effective in remote lung protection induced by lower-limbs I/R. When used in isolation, allopurinol showed no protective effect.

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“…They reported that muscle mitochondrial viability proved to be significantly higher and renal function parameters significantly better in the treatment group (18).…”

Section: Discussionmentioning

confidence: 98%

The reno-protective effects of atorvastatin in crush syndrome and rhabdomyolysis:is there a dilemma?

Acar¹,

Gülpembe²,

Yıldız³

et al. 2017

Turk J Med Sci

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Background/aim: We aim to determine the effects of low-dose atorvastatin treatment together with crush fluid resuscitation on renal functions and muscle enzyme levels in a rat model of crush syndrome. Materials and methods:The study involved female Wistar Albino rats weighing 250-300 g that were housed with free access to food and water. The crush model was obtained by compression. Rats were randomly divided into four groups: control (C) group, atorvastatin + crush fluid (ACF) group, crush fluid (CF) group, and hypertonic saline (%3) + mannitol + sodium bicarbonate (SM) group. Blood was obtained at 24, 48, and 72 h, and serum creatinine kinase, myoglobin, urea, creatinine, and lactate dehydrogenase levels were studied.Results: All parameters were statistically significantly higher in the control group than in the treatment groups at all hours. However, there was no statistically significant difference among treatment groups regarding any of the parameters. Conclusion:This is the first study determining the role of atorvastatin in the treatment of renal ischemia/reperfusion injury in a crush syndrome and rhabdomyolysis model setting. Larger studies with different atorvastatin doses are required to define the role of this drug in the treatment of renal ischemia/reperfusion injury during crush syndrome.

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Attenuation of Skeletal Muscle and Renal Injury to the Lower Limb following Ischemia-Reperfusion Using mPTP Inhibitor NIM-811

Cited by 38 publications

References 60 publications

Skeletal muscle ischemia–reperfusion injury and cyclosporine A in the aging rat

Skeletal muscle ischemia–reperfusion injury and cyclosporine A in the aging rat

The influence of allopurinol and post-conditioning on lung injuries induced by lower-limb ischemia and reperfusion in Wistar rats

The reno-protective effects of atorvastatin in crush syndrome and rhabdomyolysis:is there a dilemma?

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