Your search keyword '"Utkina-Sosunova, I"' showing total 14 results

1. Molsidomine provides neuroprotection against vincristine-induced peripheral neurotoxicity through soluble guanylyl cyclase activation

Author

Utkina-Sosunova, I, Chiorazzi, A, de Planell-Saguer, M, Li, H, Meregalli, C, Pozzi, E, Carozzi, V, Canta, A, Monza, L, Alberti, P, Fumagalli, G, Karan, C, Moayedi, Y, Przedborski, S, Cavaletti, G, Lotti, F, Utkina-Sosunova, Irina, Chiorazzi, Alessia, de Planell-Saguer, Mariangels, Li, Hai, Meregalli, Cristina, Pozzi, Eleonora, Carozzi, Valentina Alda, Canta, Annalisa, Monza, Laura, Alberti, Paola, Fumagalli, Giulia, Karan, Charles, Moayedi, Yalda, Przedborski, Serge, Cavaletti, Guido, Lotti, Francesco, Utkina-Sosunova, I, Chiorazzi, A, de Planell-Saguer, M, Li, H, Meregalli, C, Pozzi, E, Carozzi, V, Canta, A, Monza, L, Alberti, P, Fumagalli, G, Karan, C, Moayedi, Y, Przedborski, S, Cavaletti, G, Lotti, F, Utkina-Sosunova, Irina, Chiorazzi, Alessia, de Planell-Saguer, Mariangels, Li, Hai, Meregalli, Cristina, Pozzi, Eleonora, Carozzi, Valentina Alda, Canta, Annalisa, Monza, Laura, Alberti, Paola, Fumagalli, Giulia, Karan, Charles, Moayedi, Yalda, Przedborski, Serge, Cavaletti, Guido, and Lotti, Francesco

Abstract

Peripheral neurotoxicity is a dose-limiting adverse reaction of primary frontline chemotherapeutic agents, including vincristine. Neuropathy can be so disabling that patients drop out of potentially curative therapy, negatively impacting cancer prognosis. The hallmark of vincristine neurotoxicity is axonopathy, yet its underpinning mechanisms remain uncertain. We developed a comprehensive drug discovery platform to identify neuroprotective agents against vincristine-induced neurotoxicity. Among the hits identified, SIN-1-an active metabolite of molsidomine-prevents vincristine-induced axonopathy in both motor and sensory neurons without compromising vincristine anticancer efficacy. Mechanistically, we found that SIN-1's neuroprotective effect is mediated by activating soluble guanylyl cyclase. We modeled vincristine-induced peripheral neurotoxicity in rats to determine molsidomine therapeutic potential in vivo. Vincristine administration induced severe nerve damage and mechanical hypersensitivity that were attenuated by concomitant treatment with molsidomine. This study provides evidence of the neuroprotective properties of molsidomine and warrants further investigations of this drug as a therapy for vincristine-induced peripheral neurotoxicity.

Published

2024

2. Molsidomine reduces the severity of Vincristine-induced peripheral neurotoxicity in rats

Author

Chiorazzi, A., Carozzi, V., Paola Alberti, Canta, A., Meregalli, C., Fumagalli, G., Monza, L., Pozzi, E., Oggioni, N., Utkina-Sosunova, I., Przedborski, S., Cavaletti, G., Lotti, F., Chiorazzi, A, Carozzi, V, Alberti, P, Canta, A, Meregalli, C, Fumagalli, G, Monza, L, Pozzi, E, Oggioni, N, Utkina-Sosunova, I, Przedborsk, S, Cavaletti, G, and Lotti, F

Subjects

Peripheral Neurotoxicity, Animal models, Neuroprotection, Translational Medicine, Cancer, Neuropathy, Vincristine

Published

2019

3. Molsidomide provides neuroprotection against vincristine-induced peripheral neurotoxicity

Author

Lotti, F, Utkina Sosunova, I, Chiorazzi, A, Carozzi, VA, Canta, A, Monza, L, Alberti, P, Fumagalli, G, Przedborski, S, Cavaletti, G, Lotti, F, Utkina Sosunova, I, Chiorazzi, A, Carozzi, V, Canta, A, Monza, L, Alberti, P, Fumagalli, G, Przedborski, S, and Cavaletti, G

Subjects

axonal biology, pre-clinical studies, pain, axonal regeneration

Abstract

Peripheral neuropathy is the principal dose-limiting adverse reaction of the major frontline chemotherapeutic agents. Neuropathy can be so disabling that many patients will drop out of potentially curative therapy, negatively impacting cancer prognosis. Chemotherapy-induced peripheral neuropathy (CIPN) is refractory to treatment and persists in about 50% of cancer survivors limiting their quality of life. Vincristine is highly active, but its use is limited by the severe neurotoxicity leading to autonomic, sensory and motor impairment. The hallmark of vincristine peripheral neurotoxicity is axonopathy. Yet the underpinning mechanisms of vincristine-induced axonopathy remains uncertain. We hypothesize that agents preventing vincristine-induced axonopathy will effectively mitigate CIPN symptoms, hence improving cancer treatment outcomes and survivors’ quality of life. Based on this premise, we developed a comprehensive drug discovery pipeline to identify small molecules with neuroprotective activity against vincristine-induced axon degeneration. Among the hits identified, SIN-1 – an active metabolite of molsidomine (Covaryl) – prevents VCR-induced axon loss in both motor and sensory neurons, and it does so without compromising vincristine anti-cancer potency. To determine the neuroprotective effect of molsidomine, we used an extensively validated rat model of vincristine-induced peripheral neuropathy. Vincristine (0.2mg/kg/week) was administered via the tail vein for 4 weeks and molsidomine (10mg/kg/day or 20mg/kg/day) was administered orally for 4 weeks, starting the first day of vincristine treatment. As expected, the selected schedule of vincristine administration induced severe sensory and motor nerve damage. Importantly, vincristine-treated rats showed a significant decrease in the sensory threshold determined by the dynamic test that was prevented by molsidomine administration in a dose-dependent manner. A similar protective effect of molsidomine was evident on digital nerve amplitude and velocity. This study provides preliminary evidence of the neuroprotective properties of molsidomine and opens the way to further investigations of this drug as a therapeutic agent to prevent vincristine-induced peripheral neuropathy.

Published

2019

4. Molsidomine reduces the severity of Vincristine-induced peripheral neurotoxicity in rats

Author

Chiorazzi, A, Carozzi, V, Alberti, P, Canta, A, Meregalli, C, Fumagalli, G, Monza, L, Pozzi, E, Oggioni, N, Utkina-Sosunova, I, Przedborsk, S, Cavaletti, G, Lotti, F, Carozzi, VA, Chiorazzi, A, Carozzi, V, Alberti, P, Canta, A, Meregalli, C, Fumagalli, G, Monza, L, Pozzi, E, Oggioni, N, Utkina-Sosunova, I, Przedborsk, S, Cavaletti, G, Lotti, F, and Carozzi, VA

Published

2019

5. The Oxygen Free Radicals Originating from Mitochondrial Complex I Contribute to Oxidative Brain Injury Following Hypoxia-Ischemia in Neonatal Mice

Author

Niatsetskaya, Z. V., primary, Sosunov, S. A., additional, Matsiukevich, D., additional, Utkina-Sosunova, I. V., additional, Ratner, V. I., additional, Starkov, A. A., additional, and Ten, V. S., additional

Published

2012

6. The state of systemic circulation, collapsed or preserved defines the need for hyperoxic or normoxic resuscitation in neonatal mice with hypoxia-ischemia.

Author

Matsiukevich D, Randis TM, Utkina-Sosunova I, Polin RA, Ten VS, Matsiukevich, Dzmitry, Randis, Tara M, Utkina-Sosunova, Irina, Polin, Richard A, and Ten, Vadim S

Abstract

Background: The return of spontaneous circulation (ROSC) is a primary goal of resuscitation. For neonatal resuscitation the International Liaison Committee on Resuscitation (ILCOR) recommends oxygen concentrations ranging from 21% to 100%.Aims and Methods: This study (a) compared the efficacy of resuscitation with room air (RA) or 100% O(2) in achieving ROSC in 46 neonatal mice with circulatory collapse induced by lethal hypoxia-ischemia (HI) and (b) determined whether re-oxygenation with RA or 100% O(2) alters the extent of HI cerebral injury in mice with preserved systemic circulation (n=31). We also compared changes in generation of reactive oxygen species (ROS) in cerebral mitochondria in response to re-oxygenation with RA or 100% O(2).Result: In HI-mice with collapsed circulation re-oxygenation with 100% O(2) versus RA resulted in significantly greater rate of ROSC. In HI-mice with preserved systemic circulation and regional (unilateral) cerebral ischemia the restoration of cerebral blood flow was significantly faster upon re-oxygenation with 100% O(2), than RA. However, no difference in the extent of brain injury was detected. Regardless of the mode of re-oxygenation, reperfusion in these mice was associated with markedly accelerated ROS production in brain mitochondria.Conclusion: In murine HI associated with circulatory collapse the resuscitation limited to re-oxygenation with 100% O(2) is superior to the use of RA in achievement of the ROSC. However, in HI-mice with preserved systemic circulation hyperoxic re-oxygenation has no benefit over the normoxic brain recovery. [ABSTRACT FROM AUTHOR]

Published

2010

7. Molsidomine provides neuroprotection against vincristine-induced peripheral neurotoxicity through soluble guanylyl cyclase activation.

Author

Utkina-Sosunova I, Chiorazzi A, de Planell-Saguer M, Li H, Meregalli C, Pozzi E, Carozzi VA, Canta A, Monza L, Alberti P, Fumagalli G, Karan C, Moayedi Y, Przedborski S, Cavaletti G, and Lotti F

Subjects

Animals, Rats, Humans, Male, Peripheral Nervous System Diseases chemically induced, Peripheral Nervous System Diseases prevention & control, Peripheral Nervous System Diseases drug therapy, Rats, Sprague-Dawley, Neurotoxicity Syndromes drug therapy, Neurotoxicity Syndromes prevention & control, Neurotoxicity Syndromes metabolism, Neurotoxicity Syndromes etiology, Vincristine adverse effects, Vincristine pharmacology, Vincristine toxicity, Neuroprotective Agents pharmacology, Soluble Guanylyl Cyclase metabolism, Molsidomine pharmacology, Molsidomine analogs & derivatives

Abstract

Peripheral neurotoxicity is a dose-limiting adverse reaction of primary frontline chemotherapeutic agents, including vincristine. Neuropathy can be so disabling that patients drop out of potentially curative therapy, negatively impacting cancer prognosis. The hallmark of vincristine neurotoxicity is axonopathy, yet its underpinning mechanisms remain uncertain. We developed a comprehensive drug discovery platform to identify neuroprotective agents against vincristine-induced neurotoxicity. Among the hits identified, SIN-1-an active metabolite of molsidomine-prevents vincristine-induced axonopathy in both motor and sensory neurons without compromising vincristine anticancer efficacy. Mechanistically, we found that SIN-1's neuroprotective effect is mediated by activating soluble guanylyl cyclase. We modeled vincristine-induced peripheral neurotoxicity in rats to determine molsidomine therapeutic potential in vivo. Vincristine administration induced severe nerve damage and mechanical hypersensitivity that were attenuated by concomitant treatment with molsidomine. This study provides evidence of the neuroprotective properties of molsidomine and warrants further investigations of this drug as a therapy for vincristine-induced peripheral neurotoxicity., (© 2024. The Author(s).)

Published

2024

8. Patterns of TDP-43 Deposition in Brains with LRRK2 G2019S Mutations.

Author

Agin-Liebes J, Hickman RA, Vonsattel JP, Faust PL, Flowers X, Utkina Sosunova I, Ntiri J, Mayeux R, Surface M, Marder K, Fahn S, Przedborski S, and Alcalay RN

Subjects

Humans, Brain, DNA-Binding Proteins genetics, Leucine-Rich Repeat Serine-Threonine Protein Kinase-2 genetics, Mutation genetics, Protein Serine-Threonine Kinases genetics, Parkinson Disease genetics, Parkinsonian Disorders genetics

Abstract

Objective: To assess for TDP-43 deposits in brains with and without a LRRK2 G2019S mutation., Background: LRRK2 G2019S mutations have been associated with parkinsonism and a wide range of pathological findings. There are no systematic studies examining the frequency and extent of TDP-43 deposits in neuropathological samples from LRRK2 G2019S carriers., Methods: Twelve brains with LRRK2 G2019S mutations were available for study from the New York Brain Bank at Columbia University; 11 of them had samples available for TDP-43 immunostaining. Clinical, demographic, and pathological data are reported for 11 brains with a LRRK2 G2019S mutation and compared to 11 brains without GBA1 or LRRK2 G2019S mutations with a pathologic diagnosis of Parkinson's disease (PD) or diffuse Lewy body disease. They were frequency matched by age, gender, parkinsonism age of onset, and disease duration., Results: TDP-43 aggregates were present in 73% (n = 8) of brains with a LRRK2 mutation and 18% (n = 2) of brains without a LRRK2 mutation (P = 0.03). In one brain with a LRRK2 mutation, TDP-43 proteinopathy was the primary neuropathological change., Conclusions: Extranuclear TDP-43 aggregates are observed with greater frequency in LRRK2 G2019S autopsies compared to PD cases without a LRRK2 G2019S mutation. The association between LRRK2 and TDP-43 should be further explored. © 2023 International Parkinson and Movement Disorder Society., (© 2023 International Parkinson and Movement Disorder Society.)

Published

2023

9. Retromer dysfunction in amyotrophic lateral sclerosis.

Author

Pérez-Torres EJ, Utkina-Sosunova I, Mishra V, Barbuti P, De Planell-Saguer M, Dermentzaki G, Geiger H, Basile AO, Robine N, Fagegaltier D, Politi KA, Rinchetti P, Jackson-Lewis V, Harms M, Phatnani H, Lotti F, and Przedborski S

Subjects

Animals, Disease Models, Animal, Humans, Mice, Mice, Transgenic, Spinal Cord metabolism, Superoxide Dismutase-1 genetics, Superoxide Dismutase-1 metabolism, Amyotrophic Lateral Sclerosis metabolism, Vesicular Transport Proteins genetics, Vesicular Transport Proteins metabolism

Abstract

Retromer is a heteropentameric complex that plays a specialized role in endosomal protein sorting and trafficking. Here, we report a reduction in the retromer proteins-vacuolar protein sorting 35 (VPS35), VPS26A, and VPS29-in patients with amyotrophic lateral sclerosis (ALS) and in the ALS model provided by transgenic (Tg) mice expressing the mutant superoxide dismutase-1 G93A. These changes are accompanied by a reduction of levels of the α-amino-3-hydroxy-5-methyl-4-isoxazolepropionic acid receptor subunit GluA1, a proxy of retromer function, in spinal cords from Tg SOD1 G93A mice. Correction of the retromer deficit by a viral vector expressing VPS35 exacerbates the paralytic phenotype in Tg SOD1 G93A mice. Conversely, lowering Vps35 levels in Tg SOD1 G93A mice ameliorates the disease phenotype. In light of these findings, we propose that mild alterations in retromer inversely modulate neurodegeneration propensity in ALS.

Published

2022

10. Paclitaxel-induced peripheral neuropathy is caused by epidermal ROS and mitochondrial damage through conserved MMP-13 activation.

Author

Cirrincione AM, Pellegrini AD, Dominy JR, Benjamin ME, Utkina-Sosunova I, Lotti F, Jergova S, Sagen J, and Rieger S

Subjects

Animals, Axons drug effects, Axons pathology, Enzyme Activation drug effects, Epidermis metabolism, Mitochondria pathology, Peripheral Nervous System Diseases chemically induced, Up-Regulation drug effects, Zebrafish, Epidermis drug effects, Matrix Metalloproteinase 13 metabolism, Mitochondria drug effects, Paclitaxel adverse effects, Peripheral Nervous System Diseases metabolism, Peripheral Nervous System Diseases pathology, Reactive Oxygen Species metabolism

Abstract

Paclitaxel induces peripheral neuropathy as a side effect of cancer treatment. The underlying causes are unclear, but epidermal, unmyelinated axons have been shown to be the first to degenerate. We previously utilized an in vivo zebrafish model to show that the epidermal matrix-metalloproteinase 13 (MMP-13) induces degeneration of unmyelinated axons, whereas pharmacological inhibition of MMP-13 prevented axon degeneration. However, the precise functions by which MMP-13 is regulated and affects axons remained elusive. In this study, we assessed mitochondrial damage and reactive oxygen species (ROS) formation as possible inducers of MMP-13, and we analyzed MMP-13-dependent damage. We show that the small ROS, H 2 O 2 , is increased in basal keratinocytes following treatment with paclitaxel. Cytoplasmic H 2 O 2 appears to derive, at least in part, from mitochondrial damage, leading to upregulation of MMP-13, which in turn underlies increased epidermal extracellular matrix degradation. Intriguingly, also axonal mitochondria show signs of damage, such as fusion/fission defects and vacuolation, but axons do not show increased levels of H 2 O 2 . Since MMP-13 inhibition prevents axon degeneration but does not prevent mitochondrial vacuolation, we suggest that vacuolization occurs independently of axonal damage. Finally, we show that MMP-13 dysregulation also underlies paclitaxel-induced peripheral neuropathy in mammals, indicating that epidermal mitochondrial H 2 O 2 and its effectors could be targeted for therapeutic interventions.

Published

2020

11. Isoflurane anesthesia initiated at the onset of reperfusion attenuates oxidative and hypoxic-ischemic brain injury.

Author

Sosunov SA, Ameer X, Niatsetskaya ZV, Utkina-Sosunova I, Ratner VI, and Ten VS

Subjects

Anesthetics, Inhalation, Animals, Blood Gas Analysis, Cerebrovascular Circulation drug effects, Disease Models, Animal, Hydrogen Peroxide metabolism, Hypoxia-Ischemia, Brain blood, Hypoxia-Ischemia, Brain drug therapy, Isoflurane administration & dosage, Mice, Mitochondria metabolism, Neuroprotective Agents administration & dosage, Neuroprotective Agents pharmacology, Reactive Oxygen Species metabolism, Reperfusion Injury blood, Reperfusion Injury drug therapy, Respiration, Artificial, Hypoxia-Ischemia, Brain metabolism, Isoflurane pharmacology, Oxidative Stress drug effects, Reperfusion, Reperfusion Injury metabolism

Abstract

This study demonstrates that in mice subjected to hypoxia-ischemia (HI) brain injury isoflurane anesthesia initiated upon reperfusion limits a release of mitochondrial oxidative radicals by inhibiting a recovery of complex-I dependent mitochondrial respiration. This significantly attenuates an oxidative stress and reduces the extent of HI brain injury. Neonatal mice were subjected to HI, and at the initiation of reperfusion were exposed to isoflurane with or without mechanical ventilation. At the end of HI and isoflurane exposure cerebral mitochondrial respiration, H2O2 emission rates were measured followed by an assessment of cerebral oxidative damage and infarct volumes. At 8 weeks after HI navigational memory and brain atrophy were assessed. In vitro, direct effect of isoflurane on mitochondrial H2O2 emission was compared to that of complex-I inhibitor, rotenone. Compared to controls, 15 minutes of isoflurane anesthesia inhibited recovery of the compex I-dependent mitochondrial respiration and decreased H2O2 production in mitochondria supported with succinate. This was associated with reduced oxidative brain injury, superior navigational memory and decreased cerebral atrophy compared to the vehicle-treated HI-mice. Extended isoflurane anesthesia was associated with sluggish recovery of cerebral blood flow (CBF) and the neuroprotection was lost. However, when isoflurane anesthesia was supported with mechanical ventilation the CBF recovery improved, the event associated with further reduction of infarct volume compared to HI-mice exposed to isoflurane without respiratory support. Thus, in neonatal mice brief isoflurane anesthesia initiated at the onset of reperfusion limits mitochondrial release of oxidative radicals and attenuates an oxidative stress. This novel mechanism contributes to neuroprotective action of isoflurane. The use of mechanical ventilation during isoflurane anesthesia counterbalances negative effect of isoflurane anesthesia on recovery of cerebral circulation which potentiates protection against reperfusion injury.

Published

2015

12. Mild intermittent hypoxemia in neonatal mice causes permanent neurofunctional deficit and white matter hypomyelination.

Author

Juliano C, Sosunov S, Niatsetskaya Z, Isler JA, Utkina-Sosunova I, Jang I, Ratner V, and Ten V

Subjects

2',3'-Cyclic-Nucleotide Phosphodiesterases metabolism, Animals, Animals, Newborn, Caspase 3 metabolism, Cerebrovascular Circulation physiology, Disease Models, Animal, Heart Rate physiology, Hypoxia therapy, Mice, Mice, Inbred C57BL, Muscle Strength physiology, Myelin Basic Protein metabolism, Nerve Fibers, Myelinated metabolism, Nerve Fibers, Myelinated pathology, Nerve Fibers, Myelinated ultrastructure, Oxygen administration & dosage, Psychomotor Performance physiology, Statistics, Nonparametric, Time Factors, Gene Expression Regulation, Developmental physiology, Hypoxia complications, Leukoencephalopathies etiology, Nervous System Diseases etiology

Abstract

Very low birth weight (VLBW) premature infants experience numerous, often self-limited non-bradycardic episodes of intermittent hypoxemia (IH). We hypothesized that these episodes of IH affect postnatal white matter (WM) development causing hypomyelination and neurological handicap in the absence of cellular degeneration. Based on clinical data from ten VLBW neonates; a severity, daily duration and frequency of non-bradycardic IH episodes were reproduced in neonatal mice. Changes in heart rate and cerebral blood flow during IH were recorded. A short-term and long-term neurofunctional performance, cerebral content of myelin basic protein (MBP), 2'3' cyclic-nucleotide 3-phosphodiesterase (CNPase), electron microscopy of axonal myelination and the extent of cellular degeneration were examined. Neonatal mice exposed to IH exhibited no signs of cellular degeneration, yet demonstrated significantly poorer olfactory discrimination, wire holding, beam and bridge crossing, and walking-initiation tests performance compared to controls. In adulthood, IH-mice demonstrated no alteration in navigational memory. However, sensorimotor performance on rota-rod, wire-holding and beam tests was significantly worse compared to naive littermates. Both short- and long-term neurofunctional deficits were coupled with decreased MBP, CNPase content and poorer axonal myelination compared to controls. In neonatal mice mild, non-ischemic IH stress, mimicking that in VLBW preterm infants, replicates a key phenotype of non-cystic WM injury: permanent hypomyelination and sensorimotor deficits. Because this phenotype has developed in the absence of cellular degeneration, our data suggest that cellular mechanisms of WM injury induced by mild IH differ from that of cystic periventricular leukomalacia where the loss of myelin-producing cells and axons is the major mechanism of injury., (Copyright © 2014 Elsevier Inc. All rights reserved.)

Published

2015

13. Hypoxic stress exacerbates hyperoxia-induced lung injury in a neonatal mouse model of bronchopulmonary dysplasia.

Author

Ratner V, Slinko S, Utkina-Sosunova I, Starkov A, Polin RA, and Ten VS

Subjects

Animals, Bronchopulmonary Dysplasia metabolism, Disease Models, Animal, Female, Glutathione metabolism, Humans, Infant, Newborn, Lung metabolism, Lung pathology, Lung physiopathology, Male, Mice, Mice, Inbred C57BL, Oxidative Stress physiology, Oxygen metabolism, Protein Carbonylation physiology, Pulmonary Alveoli metabolism, Pulmonary Alveoli pathology, Pulmonary Alveoli physiopathology, Animals, Newborn physiology, Bronchopulmonary Dysplasia etiology, Bronchopulmonary Dysplasia physiopathology, Hyperoxia complications, Hyperoxia physiopathology, Hypoxia physiopathology

Abstract

Background: Premature infants with lung injury often experience intermittent episodes of hypoxemia., Objective: This study investigates whether intermittent hypoxemia exacerbates oxidative stress and lung injury in neonatal mice in a hyperoxia-induced model of bronchopulmonary dysplasia (BPD)., Methods: For the BPD model, 3-day-old C57Bl/6J mice were exposed to hyperoxia (65% O(2)) for 4 weeks (O(2) group) or to hyperoxia and intermittent (10 min daily) hypoxia (O(2) + H group). Upon completion of O(2) or O(2) + H exposure, the degree of pulmonary alveolarization and granulocytic infiltration were examined. The severity of oxidative injury in lungs was defined by tissue glutathione and protein carbonyl content. Data were compared to those in naïve mice and mice subjected only to intermittent hypoxia., Results: Hyperoxia-exposed mice exhibited a dramatic (p < 0.0001) decrease of alveolarization, significantly increased granulocytic infiltration (p < 0.0001) and increased protein carbonyl content (p = 0.04) compared to naïve mice. However, O(2) + H mice demonstrated significantly (p = 0.03) fewer alveoli compared to their O(2) counterparts. This was associated with a significantly (p = 0.02) decreased pulmonary total/oxidized glutathione ratio and a significant (p = 0.03) elevation of protein carbonyl content., Conclusions: Thus, intermittent hypoxic stress during hyperoxic induction of BPD in mice potentiates oxidative stress in lung tissue and exacerbates alveolar developmental arrest., ((c) 2008 S. Karger AG, Basel.)

Published

2009

14. An isolation method for assessment of brain mitochondria function in neonatal mice with hypoxic-ischemic brain injury.

Author

Caspersen CS, Sosunov A, Utkina-Sosunova I, Ratner VI, Starkov AA, and Ten VS

Subjects

Adenosine Triphosphate metabolism, Animals, Animals, Newborn, Brain cytology, Brain ultrastructure, Cell Respiration, Humans, Hypoxia-Ischemia, Brain pathology, Mice, Oxygen Consumption, Brain metabolism, Cell Fractionation methods, Hypoxia-Ischemia, Brain metabolism, Mitochondria metabolism, Mitochondria ultrastructure

Abstract

This work was undertaken to develop a method for the isolation of mitochondria from a single cerebral hemisphere in neonatal mice. Mitochondria from the normal mouse brain hemisphere isolated by the proposed method exhibited a good respiratory control ratio of 6.39 +/- 0.53 during glutamate-malate-induced phosphorylating respiration. Electron microscopy showed intact mitochondria. The applicability of this method was tested on mitochondria isolated from naïve mice and their littermates subjected to hypoxic-ischemic insult. Hypoxic-ischemic insult prior to reperfusion resulted in a significant (p < 0.01) inhibition of phosphorylating respiration compared to naïve littermates. This was associated with a profound depletion of the ATP content in the ischemic hemisphere. The expression for Mn superoxide dismutase and cytochrome C (markers for the integrity of the mitochondrial matrix and outer membrane) was determined by Western blot to control for mitochondrial integrity and quantity in the compared samples. Thus, we have developed a method for the isolation of the cerebral mitochondria from a single hemisphere adapted to neonatal mice. This method may serve as a valuable tool to study mitochondrial function in a mouse model of immature brain injury. In addition, the suggested method enables us to examine the mitochondrial functional phenotype in immature mice with a targeted genetic alteration., (2008 S. Karger AG, Basel.)

Published

2008