COVID-19 as an oxygen-deprivation disease

Among vertebrates able to tolerate periods of oxygen deprivation, the painted and red-eared slider turtles ( Chrysemys picta and Trachemys scripta) and the crucian carp ( Carassius carassius) are the most extreme and can survive even months of total lack of oxygen during winter. The key to hypoxia survival resides in concerted physiological responses, including strong metabolic depression, protection against oxidative damage and–in air-breathing animals–redistribution of blood flow. Each of these responses is known to be tightly regulated by nitric oxide (NO) and during hypoxia by its metabolite nitrite. The aim of this review is to highlight recent work illustrating the widespread roles of NO and nitrite in the tolerance to extreme oxygen deprivation, in particular in the red-eared slider turtle and crucian carp, but also in diving marine mammals. The emerging picture underscores the importance of NO and nitrite signaling in the adaptive response to hypoxia in vertebrate animals.

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Effect of Oxygen Deprivation and Reoxygenation on Endothelin-Induced Contractions of Porcine Coronary Artery1

Endothelium-Derived Contracting Factors ◽

10.1159/000418367 ◽

2015 ◽

pp. 221-231

Author(s):

David J. Schmidt ◽

Denise Koth ◽

Denise Jubenville ◽

Robert F. Highsmith

Keyword(s):

Oxygen Deprivation ◽

Effect Of Oxygen

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EFFECTS OF GLUCOSE AND OXYGEN DEPRIVATION ON FUNCTION OF ISOLATED MAMMALIAN RETINA

Journal of Neurophysiology ◽

10.1152/jn.1963.26.4.617 ◽

1963 ◽

Vol 26 (4) ◽

pp. 617-634 ◽

Cited By ~ 87

Author(s):

A. Ames ◽

B. S. Gurian

Keyword(s):

Oxygen Deprivation ◽

Mammalian Retina

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Short-term serum supplementation improves glucose-oxygen deprivation in primary cortical cultures grown under serum-free conditions

Methods in Cell Science ◽

10.1007/s11022-004-9121-9 ◽

2004 ◽

Vol 25 (3-4) ◽

pp. 227-236

Author(s):

Jan Lewerenz ◽

Susanne Thomsen ◽

Julius A. Steinbeck ◽

Axel Methner

Keyword(s):

Oxygen Deprivation ◽

Short Term ◽

Serum Free ◽

Serum Supplementation ◽

Cortical Cultures ◽

Serum Free Conditions

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Abstract W P218: Interleukin 21 receptor: A Major Modulator of Infarct Volume

Stroke ◽

10.1161/str.45.suppl_1.wp218 ◽

2014 ◽

Vol 45 (suppl_1) ◽

Author(s):

Han Kyu Lee ◽

Sehoon Keum ◽

Donald C Lo ◽

Douglas A Marchuk

Keyword(s):

Infarct Volume ◽

Brain Slices ◽

Oxygen Deprivation ◽

Cerebral Infarct ◽

Adult Brain ◽

Chromosome 7 ◽

Mouse Strains ◽

Circulatory Effects ◽

A Genome ◽

Interleukin 21

Using the permanent middle cerebral artery occlusion (MCAO) model of stroke, we have demonstrated that different inbred mouse strains show profound differences in infarct volume, indicating that infarction is under strong genetic control. To identify natural genetic determinants modulating infarction, we employed quantitative trait locus (QTL) linkage analysis and a genome-wide association study of cerebral infarct volume. We identified a locus on distal chromosome 7 that contributes over 50% of the variation in infarct volume, as well as other loci of smaller effect. Using interval-specific ancestral haplotype analysis, we fine-mapped the chromosome 7 locus to only 12 candidate genes. To identify the gene(s) underlying this locus, we determined the strain-specific transcript levels of all 12 genes in relevant tissues that included P1 and adult brain cortex, and embryonic macrophages, the latter due to their importance in the development of the cerebrovascular system. One gene, interleukin 21 receptor (Il21r), showed a 7-fold expression difference between strains and harbors a coding SNP difference that segregates with infarct volume. To determine whether Il21r is a major modulator of infarction, we examined Il21r in mice for their cerebrovascular anatomy as well as the cerebral infarct volume after MCAO. While Il21r-/- mice show a moderate reduction in collateral vessel connections compared to wild-type littermate mice cerebral infarct volume in Il21r-/- mice is increased 3-fold. This suggests that Il21r has effects on both cerebrovascular anatomy and innate neuroprotection. To examine the latter, we performed an ex vivo study of brain slices under in vitro oxygen deprivation. In this system devoid of any potential circulatory effects, but retaining appropriate tissue architecture, Il21r-/- brain slices showed an increase in oxygen-deprivation induced cell death, showing that Il21r is also involved in cerebrovascular-independent neuroprotection. Biochemical studies of the brain slices show that Il21R regulates ischemia-induced apoptosis. The identification of Il21R as a cerebrovascular-independent modulator of infarct volume provides a fundamental advance in the understanding of genetic modulation of ischemic stroke.

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Vertebral malformation in the mouse foetus caused by X-radiation of the mother during pregnancy

Development ◽

10.1242/dev.12.4.841 ◽

1964 ◽

Vol 12 (4) ◽

pp. 841-850

Author(s):

Ujihiro Murakami ◽

Yoshiro Kameyama

Keyword(s):

Early Pregnancy ◽

Vertebral Column ◽

Strain Differences ◽

In Utero ◽

Oxygen Deprivation ◽

Experimental Animals ◽

Vertebral Malformation ◽

Pregnant Mice ◽

Maternal Hypoxia ◽

In Pregnancy

Maternal hypoxia in early pregnancy can result in malformations of the vertebrae of mouse foetuses, and there is a tendency for more posterior vertebrae to be affected the later in pregnancy the oxygen deprivation occurs (Murakami & Kameyama, 1963). Ingalls et al. (1957) and Degenhardt (1954, 1959) had earlier obtained similar results. We have also exposed pregnant mice to X-radiation and studied the consequent malformations. The effects on the extremities have already been described (Murakami, Kameyama & Nogami, 1963), and in the present paper we shall describe the effects on the vertebral column. Vertebral malformations in animals irradiated in utero have been described by Job, Leibold & Fitzmaurice (1935), Warkany and Schraffenberger (1947), Russell. (1950, 1954), and Russell & Russell (1954). In order to obtain results comparable with those of our experiments with hypoxia, no less than to detect inter-strain differences, we used mice of the ddN and CF1 strains originally supplied by the Central Laboratories for Experimental Animals, Tokyo (Zikkendobutsu Chuo Kenkyujo).

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TRPM4 activation by chemically- and oxygen deprivation-induced ischemia and reperfusion triggers neuronal death

Channels ◽

10.1080/19336950.2017.1375072 ◽

2017 ◽

Vol 11 (6) ◽

pp. 624-635 ◽

Cited By ~ 7

Author(s):

Elías Leiva-Salcedo ◽

Denise Riquelme ◽

Oscar Cerda ◽

Andrés Stutzin

Keyword(s):

Neuronal Death ◽

Oxygen Deprivation ◽

Ischemia And Reperfusion

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Differential Regulation of Degradation and Immune Pathways Underlies Adaptation of the Ectosymbiotic Nematode Laxus Oneistus to Oxic-Anoxic Interfaces

10.21203/rs.3.rs-1107288/v1 ◽

2021 ◽

Author(s):

Gabriela F. Paredes ◽

Tobias Viehboeck ◽

Stephanie Markert ◽

Michaela A. Mausz ◽

Yui Sato ◽

...

Keyword(s):

Ribosome Biogenesis ◽

Oxygen Deprivation ◽

Molecular Physiology ◽

Cellular Energy ◽

Mucin Genes ◽

Sulfur Oxidizing ◽

Innate Immunity Pathway ◽

Cellular Components ◽

Transfer Chain ◽

Oxygen Shortage

Abstract Eukaryotes may experience oxygen deprivation under both physiological and pathological conditions. Because oxygen shortage leads to a reduction in cellular energy production, all eukaryotes studied so far conserve energy by suppressing their metabolism. However, the molecular physiology of animals that naturally and repeatedly experience anoxia is underexplored. One such animal is the marine nematode Laxus oneistus. It thrives, invariably coated by its sulfur-oxidizing symbiont Candidatus Thiosymbion oneisti, in anoxic sulfidic or hypoxic sand. Here, transcriptomics and proteomics showed that, whether in anoxia or not, L. oneistus mostly expressed genes involved in ubiquitination, energy generation, oxidative stress response, immune response, development, and translation. Importantly, ubiquitination genes were also highly expressed when the nematode was subjected to anoxic sulfidic conditions, together with genes involved in autophagy, detoxification and ribosome biogenesis. We hypothesize that these degradation pathways were induced to recycle damaged cellular components (mitochondria) and misfolded proteins into nutrients. Remarkably, when L. oneistus was subjected to anoxic sulfidic conditions, lectin and mucin genes were also upregulated, potentially to promote the attachment of its thiotrophic symbiont. Furthermore, the nematode appeared to survive oxygen deprivation by using an alternative electron carrier (rhodoquinone) and acceptor (fumarate), to rewire the electron transfer chain. On the other hand, under hypoxia, genes involved in costly processes (e.g., amino acid biosynthesis, development, feeding, mating) were upregulated, together with the worm’s Toll-like innate immunity pathway and several immune effectors (e.g., Bacterial Permeability Increasing proteins, fungicides). In conclusion, we hypothesize that, in anoxic sulfidic sand, L. oneistus upregulates degradation processes, rewires oxidative phosphorylation and by reinforces its coat of bacterial sulfur-oxidizers. In upper sand layers, instead, it appears to produce broad-range antimicrobials and to exploit oxygen for biosynthesis and development.

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