Prostaglandin E2 as a mediator of fever: synthesis and catabolism

Ivanov, Andrei I.; Romanovsky, Andrej A.

doi:10.2741/1383

Cited by 217 publications

(187 citation statements)

References 152 publications

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“…The role of PGE 2 in induction of fever in mammals was already reported in 1971 by Milton and Wendlandt (1971) who demonstrated that microinjection of PGE 2 into the third ventricle of conscious cats and rabbits cause a rise of body temperature. The subsequent studies using inhibitors of PGE 2 synthesis clearly confirmed that PGE 2 plays essential role in fever expressed by mammals (reviewed by Ivanov and Romanovsky, 2004;Blatteis et al, 2005). PGE 2 biosynthesis involves three successive enzymatic reactions (Pecchi et al, 2009): firstly, arachidonic acid (AA) is released by the action of phospholipase A2 (PLA2) on the cell membrane phospholipids; secondly, AA is metabolized in PGG 2 then converted to PGH 2 by the action of COX; thirdly, PGH 2 is finally metabolized in PGE 2 by the mPGES1.…”

Section: The Key Role Of Pgementioning

confidence: 87%

“…In addition to the PGE 2 locally produced in the brain, PGE 2 can also be secreted at the periphery predominantly by hepatic and pulmonary macrophages (Li et al, 2006;Simm et al, 2016;Steiner et al, 2006). This peripheral PGE 2 binds to albumin which protects it from enzymatic degradation during its journey to the brain via the bloodstream (Ivanov and Romanovsky, 2004). Independently of its peripheral or cerebral origin, PGE 2 bind to a PGE 2 receptors on a specific group of neurons in the median preoptic nucleus (MnPO).…”

Section: The Key Role Of Pgementioning

confidence: 99%

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Behavioral fever in ectothermic vertebrates

Rakus

Ronsmans

Vanderplasschen

2017

Developmental & Comparative Immunology

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a b s t r a c tFever is an evolutionary conserved defense mechanism which is present in both endothermic and ectothermic vertebrates. Ectotherms in response to infection can increase their body temperature by moving to warmer places. This process is known as behavioral fever. In this review, we summarize the current knowledge on the mechanisms of induction of fever in mammals. We further discuss the evolutionary conserved mechanisms existing between fever of mammals and behavioral fever of ectothermic vertebrates. Finally, the experimental evidences supporting an adaptive value of behavioral fever expressed by ectothermic vertebrates are summarized.

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Section: The Key Role Of Pgementioning

confidence: 87%

Section: The Key Role Of Pgementioning

confidence: 99%

Behavioral fever in ectothermic vertebrates

Rakus

Ronsmans

Vanderplasschen

2017

Developmental & Comparative Immunology

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“…In general, fever-generating PGE 2 is thought to be produced in the brain (16). Nevertheless, it is shown that substantial amounts of peripheral PGE 2 enter hypothalamic structures (17), and recent data support the idea of blood-derived PGE 2 's playing an important role in fever (18,19). The authors showed that in a rat fever model, the main enzymes that lead to generation of PGE 2 are dramatically upregulated in liver and lung (and hypothalamus) (20).…”

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confidence: 88%

Prostaglandin E2 Inhibits Its Own Renal Transport by Downregulation of Organic Anion Transporters rOAT1 and rOAT3

Sauvant¹,

Holzinger²,

Gekle³

2006

Journal of the American Society of Nephrology

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Prostaglandin E 2 (PGE 2 ) is the principal mediator of fever and inflammation. Recently, evidence emerged that during febrile response, PGE 2 that is generated in the periphery enters the hypothalamus and contributes to the maintenance of fever. In a rat model of fever generation, peripheral PGE 2 is increased, whereas clearance by metabolism of peripheral PGE 2 is downregulated. The major route of PGE 2 excretion is via the renal proximal tubular organic anion secretory system, where basolateral uptake that is mediated by renal organic anion transporter 1 (rOAT1) and rOAT3 is rate limiting. Therefore, it was hypothesized that PGE 2 itself will abolish its excretion by rOAT1 or rOAT3. Fluorescein was used as a prototypic organic anion, and NRK-52E cells from rat served as a proximal tubular model system. PGE 2 time-dependently downregulates basolateral organic anion uptake, without affecting cell volume or cell protein, recirculation of counter ions, or proximal tubular transport systems in general. In addition, PGE 2 diminishes expression of both rOAT1 and rOAT3. Both organic anion uptake and expression of rOAT1 and rOAT3 are dose-dependently downregulated by PGE 2 . These findings suggest that during fever or inflammation, renal secretory transport of PGE 2 is reduced, contributing to elevated PGE 2 levels in blood. These data fit into the hypothetical concept of peripheral PGE 2 's playing a significant role in fever. The described regulatory mechanism may also be of relevance in chronic inflammatory events. Moreover, the data presented could explain why increased plasma urate levels occur in diseases that go along with increased levels of PGE 2 .J Am Soc Nephrol 17: 46 -53, 200646 -53, . doi: 10.1681 T he organic anion transport system of the renal proximal tubule plays a crucial role in the excretion of a variety of potentially toxic compounds. This system consists of organic anion exchangers that are located at the basolateral membrane and a less well-characterized transport step at the apical membrane. The classical basolateral organic anion exchanger is the terminal step in a tertiary active transport system, dependent on an inward-directed Na ϩ gradient to drive the uptake of ␣-ketoglutarate, which then is exchanged for organic anions. It has been shown that OAT1 represents characteristics of the basolateral, polyspecific transporter for organic anions, which had been functionally described for some time (1). Recently, new evidence has indicated that organic anion transporter 3 (OAT3) (2), which also is located in the basolateral renal proximal tubular membrane, also works as an appropriate exchanger for organic anions and dicarboxylates (3,4). Moreover, additional homologues have been cloned and were called OAT2 (5), OAT4 (6), OAT5 (7), and OAT6 (8). These clones show 40 to 60% homology in amino acid sequence compared with OAT1 or OAT3, and they differ in substrate specificity and expression pattern. Furthermore, these latter proteins are not anion exchangers like OAT1 or OAT3 but seem to work as fac...

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“…mPGES-1 expression profiles were similar to COX-2, which isn't surprising given their direct involvement with each other. mPGES-1, a PGE 2 synthase enzyme, is functionally coupled with COX-2 (58); however, mPGES-1 continues to be expressed once COX-2 has declined (36). Furthermore, mPGES-1 is increased during inflammation and is downregulated by glucocorticoids (35,41).…”

Section: Cr Sickness Behavior and A Potential Mechanismmentioning

confidence: 99%

Calorie restriction attenuates LPS-induced sickness behavior and shifts hypothalamic signaling pathways to an anti-inflammatory bias

MacDonald

Radler

Paolini

et al. 2011

American Journal of Physiology-Regulatory, Integrative and Comp

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MacDonald L, Radler M, Paolini AG, Kent S. Calorie restriction attenuates LPS-induced sickness behavior and shifts hypothalamic signaling pathways to an anti-inflammatory bias. Am J Physiol Regul Integr Comp Physiol 301: R172-R184, 2011. First published April 27, 2011 doi:10.1152/ajpregu.00057.2011 has been demonstrated to alter cytokine levels; however, its potential to modify sickness behavior (fever, anorexia, cachexia) has not. The effect of CR on sickness behavior was examined in male C57BL/6J mice fed ad libitum or restricted 25% (CR25%) or restricted 50% (CR50%) in food intake for 28 days and injected with 50 g/kg of LPS on day 29. Changes in body temperature, locomotor activity, body weight, and food intake were determined. A separate cohort of mice were fed ad libitum or CR50% for 28 days, and hypothalamic mRNA expression of inhibitory factor B-␣ (I B-␣), cyclooxygenase-2 (COX-2), prostaglandin E 2 (PGE2), suppressor of cytokine signaling 3 (SOCS3), IL-10, neuropeptide Y (NPY), leptin, proopiomelanocortin (POMC), and corticotrophin-releasing hormone (CRH) were determined at 0, 2, and 4 h post-LPS. CR50% mice did not develop fevers, whereas the CR25% mice displayed a fever shorter in duration but with the same peak as the controls. Both CR25% and CR50% mice showed no sign of anorexia and reduced cachexia after LPS administration. Hypothalamic mRNA expression of NPY and CRH were both increased by severalfold in CR50% animals preinjection compared with controls. The CR50% mice did not demonstrate the expected rise in hypothalamic mRNA expression of COX-2, microsomal prostaglandin E synthase-1, POMC, or CRH 2 h post-LPS, and leptin expression was decreased at this time point. Increases in SOCS3, IL-10, and I B-␣ expression in CR50% animals were enhanced compared with ad libitum-fed controls at 4 h post-LPS. CR results in a suppression of sickness behavior in a dose-dependent manner, which may be due to CR attenuating proinflammatory pathways and enhancing anti-inflammatory pathways. fever; suppressor of cytokine signaling 3; cyclooxygenase-2; microsomal prostaglandin E synthase-1; leptin CALORIE RESTRICTION (CR), a dietary regimen low in calories, while avoiding malnutrition, is the only manipulation that has consistently been shown to extend the mean and maximum life span in a range of species (2,42,71,76). In addition to an increase in life span, CR attenuates the normal immunosenscence seen with age (52), along with reducing the occurrence of other age-related diseases (14,39,43,53,54,79).It has been postulated that the mechanism by which CR extends the mean and maximum life span is by reducing oxidative stress caused by unregulated increases in reactive oxygen species (3,19,31,42,69), as well as by limiting the age-related increase in basal pro-inflammatory cytokine levels (73). One possible mechanism by which CR exerts its antiinflammatory effect are glucocorticoids, which are increased after CR (33, 47) and act to increase the transcription of anti-inflammatory cytokines and decrease the transcripti...

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Prostaglandin E2 as a mediator of fever: synthesis and catabolism

Cited by 217 publications

References 152 publications

Behavioral fever in ectothermic vertebrates

Behavioral fever in ectothermic vertebrates

Prostaglandin E2 Inhibits Its Own Renal Transport by Downregulation of Organic Anion Transporters rOAT1 and rOAT3

Calorie restriction attenuates LPS-induced sickness behavior and shifts hypothalamic signaling pathways to an anti-inflammatory bias

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