Subtype-selective regulation of IP3 receptors by thimerosal via cysteine residues within the IP3-binding core and suppressor domain

Khan, Seema; Rossi, Ana M.; Riley, Andrew M.; Potter, Barry V. L.; Taylor, Colin W.

doi:10.1042/bj20121600

Cited by 22 publications

(14 citation statements)

References 53 publications

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“…Superoxide anions may cause oxidation of the IP 3 receptor and sensitization of Ca 2+ release. Various exogenously added oxidants, such as thimerosal ( 97 – 99 ), t -butylhydroperoxide ( 100 ), and diamide ( 101 , 102 ), each stimulate IP 3 R-mediated Ca 2+ release. Mitochondria, by providing a source of ROS, may thus maintain IP 3 -evoked Ca 2+ release.…”

Section: Discussionmentioning

confidence: 99%

Mitochondrial ATP production provides long-range control of endothelial inositol trisphosphate–evoked calcium signaling

Wilson

Lee

Heathcote

et al. 2019

Journal of Biological Chemistry

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Endothelial cells are reported to be glycolytic and to minimally rely on mitochondria for ATP generation. Rather than providing energy, mitochondria in endothelial cells may act as signaling organelles that control cytosolic Ca2+ signaling or modify reactive oxygen species (ROS). To control Ca2+ signaling, these organelles are often observed close to influx and release sites and may be tethered near Ca2+ transporters. In this study, we used high-resolution, wide-field fluorescence imaging to investigate the regulation of Ca2+ signaling by mitochondria in large numbers of endothelial cells (∼50 per field) in intact arteries from rats. We observed that mitochondria were mostly spherical or short-rod structures and were distributed widely throughout the cytoplasm. The density of these organelles did not increase near contact sites with smooth muscle cells. However, local inositol trisphosphate (IP3)-mediated Ca2+ signaling predominated near these contact sites and required polarized mitochondria. Of note, mitochondrial control of Ca2+ signals occurred even when mitochondria were far from Ca2+ release sites. Indeed, the endothelial mitochondria were mobile and moved throughout the cytoplasm. Mitochondrial control of Ca2+ signaling was mediated by ATP production, which, when reduced by mitochondrial depolarization or ATP synthase inhibition, eliminated local IP3-mediated Ca2+ release events. ROS buffering did not significantly alter local Ca2+ release events. These results highlight the importance of mitochondrial ATP production in providing long-range control of endothelial signaling via IP3-evoked local Ca2+ release in intact endothelium.

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Section: Discussionmentioning

confidence: 99%

Mitochondrial ATP production provides long-range control of endothelial inositol trisphosphate–evoked calcium signaling

Wilson

Lee

Heathcote

et al. 2019

Journal of Biological Chemistry

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“…In the same study, the IP3R3 channel function remained unchanged by thimerosal [ 96 ]. Another study suggested that thimerosal selectively sensitizes IP3R1 and IP3R2 to IP3 by stabilizing an active conformation of the receptors through modification of cysteine residues [ 97 ].…”

Section: Mutual Interplay Between Ros and Ca 2+mentioning

confidence: 99%

Interrelation between ROS and Ca2+ in aging and age-related diseases

2020

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Calcium (Ca 2+ ) and reactive oxygen species (ROS) are versatile signaling molecules coordinating physiological and pathophysiological processes. While channels and pumps shuttle Ca 2+ ions between extracellular space, cytosol and cellular compartments, short-lived and highly reactive ROS are constantly generated by various production sites within the cell. Ca 2+ controls membrane potential, modulates mitochondrial adenosine triphosphate (ATP) production and affects proteins like calcineurin (CaN) or calmodulin (CaM), which, in turn, have a wide area of action. Overwhelming Ca 2+ levels within mitochondria efficiently induce and trigger cell death. In contrast, ROS comprise a diverse group of relatively unstable molecules with an odd number of electrons that abstract electrons from other molecules to gain stability. Depending on the type and produced amount, ROS act either as signaling molecules by affecting target proteins or as harmful oxidative stressors by damaging cellular components. Due to their wide range of actions, it is little wonder that Ca 2+ and ROS signaling pathways overlap and impact one another. Growing evidence suggests a crucial implication of this mutual interplay on the development and enhancement of age-related disorders, including cardiovascular and neurodegenerative diseases as well as cancer.

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“…Not breaking the signaling and metabolic pathways, ROS implement the "orthogonal regulation" of metabolism through modulation of kinetic characteristics of biochemical reactions [239]. Redox modulation is specifically localized and depends on the size and redox potential of ROS or other oxidants (electrophile); its concentration, and availability of the targets, consisted mainly of amino acids [246]. It is important to note here that the so-called antioxidants are perhaps the most ambiguous and speculative group of dietary supplements.…”

Section: Concluding Remarks and Future Directionsmentioning

confidence: 99%

Markers and Biomarkers of Endothelium: When Something Is Rotten in the State

Гончаров

Nadeev

Jenkins

et al. 2017

Oxidative Medicine and Cellular Longevity

159

115

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Endothelium is a community of endothelial cells (ECs), which line the blood and lymphatic vessels, thus forming an interface between the tissues and the blood or lympha. This strategic position of endothelium infers its indispensable functional role in controlling vasoregulation, haemostasis, and inflammation. The state of endothelium is simultaneously the cause and effect of many diseases, and this is coupled with modifications of endothelial phenotype represented by markers and with biochemical profile of blood represented by biomarkers. In this paper, we briefly review data on the functional role of endothelium, give definitions of endothelial markers and biomarkers, touch on the methodological approaches for revealing biomarkers, present an implicit role of endothelium in some toxicological mechanistic studies, and survey the role of reactive oxygen species (ROS) in modulation of endothelial status.

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Subtype-selective regulation of IP3 receptors by thimerosal via cysteine residues within the IP3-binding core and suppressor domain

Cited by 22 publications

References 53 publications

Mitochondrial ATP production provides long-range control of endothelial inositol trisphosphate–evoked calcium signaling

Mitochondrial ATP production provides long-range control of endothelial inositol trisphosphate–evoked calcium signaling

Interrelation between ROS and Ca2+ in aging and age-related diseases

Markers and Biomarkers of Endothelium: When Something Is Rotten in the State

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