Detection of hydrogen sulfide in plasma and knee‐joint synovial fluid from rheumatoid arthritis patients: relation to clinical and laboratory measures of inflammation

Whiteman, Matthew; Haigh, Richard; Tarr, Joanna M.; Gooding, Karen M.; Shore, Angela C.; Winyard, Paul G.

doi:10.1111/j.1749-6632.2010.05556.x

Cited by 68 publications

(59 citation statements)

References 22 publications

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“…In the CFA arthritis model ), CFA injection induced synovial H 2 S synthesis fluid (SF), in agreement with in vitro studies using human joint cells Fox et al 2012;Burguera et al 2014) and observations with human SF from patients with various inflammatory arthritides (Whiteman and Winyard 2011;Whiteman et al 2010c). GYY4137 (50 mg/kg i.p.)…”

Section: Gyy4137: Anti-inflammatory Effectssupporting

confidence: 55%

“…The ratio of blood/sputum H 2 S levels has been proposed as a novel biomarker for airway disease (Chung 2014;Saito et al 2013Saito et al , 2014Wang et al 2011a). Similarly, synovial fluid H 2 S levels are elevated relative to disease controls in patients with rheumatoid arthritis (Whiteman et al 2010c) and inflammatory joint disease (Whiteman and Winyard 2011). Early studies generally showed inhibition of endogenous H 2 S synthesis attenuated pro-inflammatory signalling in vitro and inflammation in vivo (reviewed in Whiteman and Winyard (2011)), although it should be noted that pharmacological inhibitors of CSE, CBS and 3-MST are non-specific necessitating their use at very high concentrations (reviewed in detail in ) and the addition of NaSH to cultured cells in vitro (Whiteman et al 2010b;Zhang et al 2008;Zhi et al 2007;Kloesch et al 2012a, b).…”

Section: Gyy4137: Anti-inflammatory Effectsmentioning

confidence: 94%

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Phosphinodithioate and Phosphoramidodithioate Hydrogen Sulfide Donors

Whiteman

Perry

Zhou³

et al. 2015

Chemistry, Biochemistry and Pharmacology of Hydrogen Sulfide

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Hydrogen sulfide is rapidly emerging as a key physiological mediator and potential therapeutic tool in numerous areas such as acute and chronic inflammation, neurodegenerative and cardiovascular disease, diabetes, obesity and cancer. However, the vast majority of the published studies have employed crude sulfide salts such as sodium hydrosulfide (NaSH) and sodium sulfide (Na2S) as H2S "donors" to generate H2S. Although these salts are cheap, readily available and easy to use, H2S generated from them occurs as an instantaneous and pH-dependent dissociation, whereas endogenous H2S synthesis from the enzymes cystathionine γ-lyase, cystathionine-β-synthase and 3-mercaptopyruvate sulfurtransferase is a slow and sustained process. Furthermore, sulfide salts are frequently used at concentrations (e.g. 100 μM to 10 mM) far in excess of the levels of H2S reported in vivo (nM to low μM). For the therapeutic potential of H2S is to be properly harnessed, pharmacological agents which generate H2S in a physiological manner and deliver physiologically relevant concentrations are needed. The phosphorodithioate GYY4137 has been proposed as "slow-release" H2S donors and has shown promising efficacy in cellular and animal model diseases such as hypertension, sepsis, atherosclerosis, neonatal lung injury and cancer. However, H2S generation from GYY4137 is inefficient necessitating its use at high concentrations/doses. However, structural modification of the phosphorodithioate core has led to compounds (e.g. AP67 and AP105) with accelerated rates of H2S generation and enhanced biological activity. In this review, the therapeutic potential and limitations of GYY4137 and related phosphorodithioate derivatives are discussed.

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Section: Gyy4137: Anti-inflammatory Effectssupporting

confidence: 55%

Section: Gyy4137: Anti-inflammatory Effectsmentioning

confidence: 94%

Phosphinodithioate and Phosphoramidodithioate Hydrogen Sulfide Donors

Whiteman

Perry

Zhou³

et al. 2015

Chemistry, Biochemistry and Pharmacology of Hydrogen Sulfide

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“…Over the years, H 2 S is emerging as an important mediator in acute and chronic inflammation [8]. It has been reported that the increased H 2 S circulation detected in the burn injury [36] and its levels correlated with inflammatory and clinical indices in rheumatoid arthritis patients [37]. Moreover, multiple lines of studies, in multiple experimental models, showing that therapeutic elevation of H 2 S concentrations or H 2 S donors can exert anti-inflammation and decrease the mortality caused by endotoxemia [38][39][40].…”

Section: Figmentioning

confidence: 99%

Endogenous Hydrogen Sulfide Ameliorates NOX4 Induced Oxidative Stress in LPS-Stimulated Macrophages and Mice

Wang

Pan

Long

et al. 2018

Cell Physiol Biochem

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Background/Aims: Sepsis is a severe and complicated syndrome that is characterized by dysregulation of host inflammatory responses and organ failure. Cystathionine-γ-lyase (CSE)/ hydrogen sulfide (H₂S) has potential anti-inflammatory activities in a variety of inflammatory diseases. NADPH oxidase 4 (Nox4), a member of the NADPH oxidases, is the major source of reactive oxygen species (ROS) and its expression is increased in sepsis, but its function in CSE-mediated anti-inflammatory activities remains unknown. Methods: Macrophages were either transfected with CSE, Nox4 siRNA or transduced with lentiviral vector encoding CSE or Nox4, and then stimulated with lipopolysaccharide (LPS). The expression of inflammatory mediators and signaling pathway activation were measured by quantitative PCR (qPCR), ELISA, and immunoblotting. LPS-induced shock severity in WT, Nox4 knockdown and CSE knockout (CSE^-/-) mice was assessed. Results: Here we showed that CSE and Nox4 were upregulated in macrophage and mouse in response to LPS. After LPS stimulation, the inflammatory responses were significantly ameliorated by lentiviral Nox4 shRNA knockdown, but were exacerbated by lentiviral overexpressing Nox4. Furthermore, Nox4 mediated inflammation through PI3K/Akt and p-p38 mitogen-activated protein kinase signal pathway. Notably, CSE knockout served to amplify the inflammatory cascade by increasing Nox4-ROS signaling activation in septic mice and macrophage. Similarly, the enhanced production of inflammatory mediators by macrophages was reduced by CSE overexpression. Conclusion: Thus, we demonstrated that CSE/H₂S attenuated LPS-induced sepsis against oxidative stress and inflammation damage probably largely through mediated Nox4 pathway.

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“…Dentre os doadores de H 2 S disponíveis comercialmente, empregados em modelos inflamatórios e sensitivos, estão os doadores de H 2 S de liberação espontânea/rápida: hidrossulfeto de sódio (NaHS), sulfeto de sódio (Na 2 S), o reagente de Lawesson, os de liberação lenta (Benetti et al, 2013;Campos et al, 2016;Coavoy-Sánchez et al, 2016;Ekundi et al, 2010;Li et al, 2009;Rodrigues et al, 2016;Wang, 2012;Whiteman et al, 2010;) e os doadores híbridos (H 2 S associado a uma molécula anti-inflamatória não esteroide; Ekundi-Valentim et al, 2013;Gemici et al, 2015).…”

Section: Pancreatite E Sulfeto De Hidrogêniounclassified

“…Postula-se que as ações tóxicas/deletérias do H 2 S descritas em alguns estudos podem ser explicadas pelo fato que a taxa de liberação de H 2 S dos doadores espontâneos/rápidos, como o NaHS, é extremamente alta e em curto período de tempo, enquanto a taxa de liberação de H 2 S por GYY4137 é muito menor (cerca de 200 X), mas de forma constante e prolongada (Whiteman et al, 2010), mimetizando assim a liberação de H 2 S endógeno em sistemas fisiológicos. Em concentrações fisiológicas, o H 2 S causa relaxamento muscular por ação direta em canais de K ATP , assim como intensifica a ação relaxante do óxido nítrico (Wang et al, 2014).…”

Section: Pancreatite E Sulfeto De Hidrogêniounclassified

Análise farmacológica comparativa da pancreatite experimental induzida por fosfolipase A2 secretória do veneno de serpente Crotalus durissus terrificus e fosfolipase A2 de mamífero em ratos: papel das fibras C e do sulfeto de hidrogênio.

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Detection of hydrogen sulfide in plasma and knee‐joint synovial fluid from rheumatoid arthritis patients: relation to clinical and laboratory measures of inflammation

Cited by 68 publications

References 22 publications

Phosphinodithioate and Phosphoramidodithioate Hydrogen Sulfide Donors

Phosphinodithioate and Phosphoramidodithioate Hydrogen Sulfide Donors

Endogenous Hydrogen Sulfide Ameliorates NOX4 Induced Oxidative Stress in LPS-Stimulated Macrophages and Mice

Análise farmacológica comparativa da pancreatite experimental induzida por fosfolipase A<sub>2 </sub>secretória do veneno de serpente <i>Crotalus durissus terrificus</i> e fosfolipase A<sub>2</sub> de mamífero em ratos: papel das fibras C e do sulfeto de hidrogênio.

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