Targeting Hydrogen Sulfide Modulates Dexamethasone-Induced Muscle Atrophy and Microvascular Rarefaction, through Inhibition of NOX4 and Induction of MGF, M2 Macrophages and Endothelial Progenitors

Adel, Mohamed; Elsayed, Hassan; El-Nablaway, Mohammad; Hamed, Shereen; Eladl, Amira; Fouad, Samah; Nashar, Eman Mohamad El; Al-Otaibi, Mohammed Lafi; Rabei, Mohammed R.

doi:10.3390/cells11162500

“…In agreement with these findings, different studies have observed that exogenous administration of H 2 S attenuates M1 polarization, including reduction of CD86 [ 24 ], CD11c [ 60 ], and iNOS [ 77 ] expression. H 2 S has also been indicated to lead to the polarization of macrophages from M1 to M2 phenotype [ 77 ], increasing the expression of M2 markers like CD206 [ 13 , 77 ] and CD163 [ 1 ]. In our study, GYY-4137 co-treatment failed to recover the reduction in gene expression of CD206 triggered by LPS, whereas protein levels were barely detected.…”

Section: Discussionmentioning

confidence: 99%

Study of hydrogen sulfide biosynthesis in synovial tissue from diabetes-associated osteoarthritis and its influence on macrophage phenotype and abundance

Lendoiro-Cino,

Rodríguez-Coello,

Saborido

et al. 2023

J Physiol Biochem

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Type 2 diabetes (DB) is an independent risk factor for osteoarthritis (OA). However, the mechanisms underlying the connection between both diseases remain unclear. Synovial macrophages from OA patients with DB present a marked pro-inflammatory phenotype. Since hydrogen sulphide (H2S) has been previously described to be involved in macrophage polarization, in this study we examined H2S biosynthesis in synovial tissue from OA patients with DB, observing a reduction of H2S-synthetizing enzymes in this subset of individuals. To elucidate these findings, we detected that differentiated TPH-1 cells to macrophages exposed to high levels of glucose presented a lower expression of H2S-synthetizing enzymes and an increased inflammatory response to LPS, showing upregulated expression of markers associated with M1 phenotype (i.e., CD11c, CD86, iNOS, and IL-6) and reduced levels of those related to M2 fate (CD206 and CD163). The co-treatment of the cells with a slow-releasing H2S donor, GYY-4137, attenuated the expression of M1 markers, but failed to modulate the levels of M2 indicators. GYY-4137 also reduced HIF-1α expression and upregulated the protein levels of HO-1, suggesting their involvement in the anti-inflammatory effects of H2S induction. In addition, we observed that intraarticular administration of H2S donor attenuated synovial abundance of CD68+ cells, mainly macrophages, in an in vivo model of OA. Taken together, the findings of this study seem to reinforce the key role of H2S in the M1-like polarization of synovial macrophages associated to OA and specifically its metabolic phenotype, opening new therapeutic perspectives in the management of this pathology.

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A Potentiometric Dual‐Channel Microsensor Reveals that Fluctuation of H₂S is Less pH‐Dependent During Spreading Depolarization in the Rat Brain

Liu,

Zhang,

Zeng

et al. 2024

Angewandte Chemie

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Spreading depolarization (SD) is one of the most common neuropathologic phenomena in the nervous system, relating to numerous diseases. However, real‐time monitoring the rapid chemical changes during SD to probe the molecular mechanism remains a great challenge. We develop a potentiometric dual‐channel microsensor for simultaneous monitoring of H2S and pH featuring excellent selectivity and spatiotemporal resolution. Using this microsensor we firstobserve real time changes of H2S and pH in the rat brain induced by SD. This changes of H2S are completely suppressed when the rat pre‐treats with aminooxyacetic acid (AOAA), a blocker to inhibit the H2S‐producing enzyme, indicating H2S fluctuation might be related to enzyme‐dependent pathway during SD and less pH‐dependent. This study provides a new perspective for studying the function of H2S and the molecular basis of SD‐associated diseases.

show abstract

A Potentiometric Dual‐Channel Microsensor Reveals that Fluctuation of H₂S is Less pH‐Dependent During Spreading Depolarization in the Rat Brain

Liu,

Zhang,

Zeng

et al. 2024

Angew Chem Int Ed

0

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Spreading depolarization (SD) is one of the most common neuropathologic phenomena in the nervous system, relating to numerous diseases. However, real‐time monitoring the rapid chemical changes during SD to probe the molecular mechanism remains a great challenge. We develop a potentiometric dual‐channel microsensor for simultaneous monitoring of H2S and pH featuring excellent selectivity and spatiotemporal resolution. Using this microsensor we firstobserve real time changes of H2S and pH in the rat brain induced by SD. This changes of H2S are completely suppressed when the rat pre‐treats with aminooxyacetic acid (AOAA), a blocker to inhibit the H2S‐producing enzyme, indicating H2S fluctuation might be related to enzyme‐dependent pathway during SD and less pH‐dependent. This study provides a new perspective for studying the function of H2S and the molecular basis of SD‐associated diseases.

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Targeting Hydrogen Sulfide Modulates Dexamethasone-Induced Muscle Atrophy and Microvascular Rarefaction, through Inhibition of NOX4 and Induction of MGF, M2 Macrophages and Endothelial Progenitors

Cited by 8 publications

References 53 publications

Study of hydrogen sulfide biosynthesis in synovial tissue from diabetes-associated osteoarthritis and its influence on macrophage phenotype and abundance

Study of hydrogen sulfide biosynthesis in synovial tissue from diabetes-associated osteoarthritis and its influence on macrophage phenotype and abundance

A Potentiometric Dual‐Channel Microsensor Reveals that Fluctuation of H₂S is Less pH‐Dependent During Spreading Depolarization in the Rat Brain

A Potentiometric Dual‐Channel Microsensor Reveals that Fluctuation of H₂S is Less pH‐Dependent During Spreading Depolarization in the Rat Brain

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Targeting Hydrogen Sulfide Modulates Dexamethasone-Induced Muscle Atrophy and Microvascular Rarefaction, through Inhibition of NOX4 and Induction of MGF, M2 Macrophages and Endothelial Progenitors

Cited by 8 publications

References 53 publications

Study of hydrogen sulfide biosynthesis in synovial tissue from diabetes-associated osteoarthritis and its influence on macrophage phenotype and abundance

Study of hydrogen sulfide biosynthesis in synovial tissue from diabetes-associated osteoarthritis and its influence on macrophage phenotype and abundance

A Potentiometric Dual‐Channel Microsensor Reveals that Fluctuation of H2S is Less pH‐Dependent During Spreading Depolarization in the Rat Brain

A Potentiometric Dual‐Channel Microsensor Reveals that Fluctuation of H2S is Less pH‐Dependent During Spreading Depolarization in the Rat Brain

Contact Info

Product

Resources

About

A Potentiometric Dual‐Channel Microsensor Reveals that Fluctuation of H₂S is Less pH‐Dependent During Spreading Depolarization in the Rat Brain

A Potentiometric Dual‐Channel Microsensor Reveals that Fluctuation of H₂S is Less pH‐Dependent During Spreading Depolarization in the Rat Brain