Glutathione Peroxidase Activity, Plasma Total Antioxidant Capacity, and Urinary F2‐ Isoprostanes as Markers of Oxidative Stress in Anemic Dogs

Kendall, A. Richard; Woolcock, Andrew D; Brooks, Aimee C.; Moore, George E.

doi:10.1111/jvim.14847

Cited by 23 publications

(31 citation statements)

References 39 publications

(122 reference statements)

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“…Several tests are available for the measurement of oxidative stress processes in plasma or serum and to assess changes in antioxidant status. These include measurement of total oxidant status (TOS), total antioxidant status (TAS), and the oxidative stress index (OSI) . TAS and TOS are generally used for more accurate evaluation of in vivo oxidative stress .…”

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confidence: 99%

“…These include measurement of total oxidant status (TOS), total antioxidant status (TAS), and the oxidative stress index (OSI) . TAS and TOS are generally used for more accurate evaluation of in vivo oxidative stress . Biochemical parameters such as TAS, TOS, and OSI therefore exhibit perfect sensitivity in the analysis of oxidative stress .…”

mentioning

confidence: 99%

“…13,14 TAS and TOS are generally used for more accurate evaluation of in vivo oxidative stress. 14,15 Biochemical parameters such as TAS, TOS, and OSI therefore exhibit perfect sensitivity in the analysis of oxidative stress. 16,17 The OSI and the ratio of TOS to TAS are parameters evaluating the balance between antioxidants and oxidants.…”

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confidence: 99%

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Effects of gadolinium‐based MRI contrast agents on liver tissue

Mercantepe

Tümkaya

Çeliker

et al. 2018

Magnetic Resonance Imaging

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Effects of gadolinium‐based MRI contrast agents on liver tissue

Mercantepe

Tümkaya

Çeliker

et al. 2018

Magnetic Resonance Imaging

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“…Необхідно також враховувати, що на активність GPx у крові тварин впливають різні фактори. Так, у крові анемічних собак активність ензиму значно ниж-ча, ніж у здорових тваринами (Kendall et al, 2017). Також показана залежність цього показника від форми анемії у собак (Gultekin and Voyvoda, 2017), але не виявлено статистично вірогідних відмінностей в активності GPx у собак з серцевою недостатністю (Verk et al, 2017).…”

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Glutathione peroxidase of blood of dogs and cats with mammary tumors

2018

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For timely diagnostics and successful treatment of mammary tumors in human and animals a necessary search of compounds that can be the biomarkers of this disease is needed. The aim of our work was to measure the activity of glutathione peroxidase (GPx) in blood plasma and erythrocytes of dogs and cats with mammary tumors and healthy animals for establishment of intercommunication between enzyme's activity and tumors. For researches took away blood at three groups of animals: 1) four healthy females of dogs (Canis familiaris) – the German Shepherd dogs by age 3, 6, 7 and 7; 2) four females of dogs with mammary tumors – the Russian Spaniel dog by age 8, Boxer dog by age 9 and the German Shepherd crossbred dogs by age 11 and 12; 3) four females of cats (Felis catus) with mammary tumors – crossbred cats by age 6, 8 and 10 and the Persian crossbred cat by age 13. Activity of GPx was determined by decrease of reduced glutathione in a presence of hydrogen peroxide for time unit with a count on the gramme of protein in blood plasma, or haemoglobin in erythrocytes. In the sick dogs’ erythrocytes the activity of GPx presents 30.45 ± 3.08 mmol GSH/min×g haemoglobin and it is more than for the healthy animals of 27.84 ± 5.24 mmol GSH/min×g haemoglobin, these differences aren't statistically reliable however. This index is the highest for the sick German Shepherd crossbred dog aged 11 and presents 38.5 mmol GSH/min×g haemoglobin. In sick dogs’ activity of GPx in blood plasma is 7.45 ± 1.60 mmol GSH/min×g protein and it is statistically reliable less than the healthy animals of 12.77 ± 1.18 mmol GSH/min×g protein. This index is the lowest for the the 12 years old sick German Shepherd crossbred dog and it is 3.41 mmol GSH/min×g protein. In sick cats activity of GPx in erythrocytes is 41.57 ± 4.10 mmol GSH/min×g haemoglobin, and the greatest it is in the sick crossbred cat age 10 – 52.52 mmol GSH/min×g haemoglobin. The activity of the enzyme in blood plasma of sick cats is 11.58 ± 1.99 mmol GSH/min×g protein and this index is similar to the healthy dogs. Activity of GPx of the erythrocytes of dogs and blood plasma of cats with mammary tumors did not differ from healthy dogs. The activity of GPx of sick dogs only in blood plasma is less than in healthy ones. It can be the consequence of this “exhaustion” of the enzyme and its involving in the process of neutralizing of active forms of reactive oxygen species in those tissues of organism where oxidizing stress develops. Next to the study of expression on the future it is necessary to pay attention to the study of polymorphism of GPx.

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“…For example, glutathione (GSH) depletion correlates with illness severity and outcome (Viviano et al 2009). Additional veterinary studies have recognised an association between oxidative stress and several canine disease states, including liver disease, congestive heart failure, intervertebral disk disease, anaemia and parvoviral enteritis , Freeman et al 2005, McMichael et al 2006, Kendall et al 2017, Gaykwad et al 2018. Given the data in people, it is tempting to speculate that AS may ameliorate oxidative stress in dogs.…”

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confidence: 99%

Antioxidant supplementation during illness in dogs: effect on oxidative stress and outcome, an exploratory study

Hagen¹,

Ekena

Geesaman

et al. 2019

J of Small Animal Practice

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Objectives To assess whether combination antioxidant supplementation for 30 days in systemically ill dogs alters antioxidant status, degree of lipid peroxidation, clinical score and survival. Materials and Methods Forty client‐owned systemically‐ill hospitalised dogs were eligible for inclusion. Dogs were randomised to no supplementation (NS; n=19) or supplementation with N‐acetylcysteine/S‐adenosylmethionine/silybin and vitamin E (AS; n=20) for 30 days. Clinical score and oxidative biomarkers including glutathione, cysteine, vitamin E, selenium and urine isoprostanes/creatinine (F2‐IsoPs/Cr) were determined on days 0 and 30. Glutathione, cysteine, vitamin E and urine F2‐IsoPs/Cr were quantified by high‐performance liquid chromatography, and selenium concentrations determined using atomic absorption spectroscopy. Results Thirty‐two dogs completed the study (NS, n=16; AS, n=16). Vitamin E concentrations were significantly greater in the supplemented compared to the non‐supplemented group. No other markers of oxidative stress significantly changed with supplementation. There was no difference in Day 30 clinical scores or survival between the two groups. Clinical Significance In this population of systemically‐ill hospitalised dogs, combination antioxidant supplementation did not alter redox state or clinical outcome.

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Glutathione Peroxidase Activity, Plasma Total Antioxidant Capacity, and Urinary F2‐ Isoprostanes as Markers of Oxidative Stress in Anemic Dogs

Cited by 23 publications

References 39 publications

Effects of gadolinium‐based MRI contrast agents on liver tissue

Effects of gadolinium‐based MRI contrast agents on liver tissue

Glutathione peroxidase of blood of dogs and cats with mammary tumors

Antioxidant supplementation during illness in dogs: effect on oxidative stress and outcome, an exploratory study

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