Flufenamic acid promotes angiogenesis through AMPK activation

Ge, Ruowen; Hu, Lei; Tai, Yilin; Xue, Feng; Yuan, Lei; Wei, Gongtian; Wang, Yi

doi:10.3892/ijo.2013.1891

Cited by 6 publications

(3 citation statements)

References 47 publications

(49 reference statements)

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“…For further investigation of intracellular mechanisms that influence SGLT-1 activity, epithelia were incubated with 3 mM AMG in the mucosal buffer solution and 10 mM glucose in the serosal buffer solution. Epithelia were preincubated with either 0.1 mM ouabain, an inhibitor of Na ϩ -K ϩ -ATPase (4); 20 M compound C, an inhibitor of AMPK (13); 20 mM 5-aminoimidazole-4-carboxamide (AICAR) (purchased from Santa Cruz Biotechnology) and 0.2 mM flufenamic acid (FFA) (purchased from Sigma-Aldrich), both known as activators of AMPK (10,18,37,45,47); or the respective solvent as control for 30 min before subjecting part of the epithelia to hypoxia. After 45 min of hypoxia, 0.2 mM phlorizin, an inhibitor of SGLT-1 (39), were added to the mucosal buffer solution and the decrease in the slope of Isc (i.e., the loss of net charge transport across the epithelium) was measured.…”

Section: Methodsmentioning

confidence: 99%

Glucose transport across lagomorph jejunum epithelium is modulated by AMP-activated protein kinase under hypoxia

Dengler

Rackwitz

Pfannkuche

et al. 2017

Journal of Applied Physiology

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The gastrointestinal epithelium possesses adaptation mechanisms to cope with huge variations in blood flow and subsequently oxygenation. Since sufficient energy supply is crucial under hypoxic conditions, glucose uptake especially must be regulated by these adaptation mechanisms. Therefore, we investigated glucose transport under hypoxic conditions. Jejunal epithelia of rabbits were incubated in Ussing chambers under short-circuit current conditions. Hypoxia was simulated by gassing with 1% O instead of 100% O. The activity of sodium-coupled glucose transporter-1 (SGLT-1) was assessed by measuring the increase of short circuit current ( I) after the addition of 2 mM glucose to the mucosal buffer solution. We observed decreased activity of SGLT-1 after hypoxia compared with control conditions. To investigate underlying mechanisms, epithelia were exposed to agonists and antagonists of AMP-activated protein kinase (AMPK) before assessment of SGLT-1-mediated transport and the pAMPK/AMPK protein ratio. Preincubation with the antagonist restored SGLT-1 activity under hypoxic conditions to the level of control conditions, indicating an involvement of AMPK in the downregulation of SGLT-1 activity under hypoxia, which was confirmed in Western blot analysis of pAMPK/AMPK. Transepithelial flux studies using radioactively labeled glucose, ortho-methyl-glucose, fructose, and mannitol revealed no changes after hypoxic incubation. Therefore, we could exclude a decreased transepithelial glucose transport rate and increased paracellular conductance under hypoxia. In conclusion, our study hints at a decreased activity of SGLT-1 under hypoxic conditions in an AMPK-dependent manner. However, transepithelial transport of glucose is maintained. Therefore, we suggest other transport mechanisms, especially glucose transporter 1 and/or 2 to substitute SGLT-1 under hypoxia. NEW & NOTEWORTHY To our knowledge, this is the first approach to simulate hypoxia and study its effects in the jejunal epithelium using the Ussing chamber technique. We were able show that AMPK plays a role in the downregulation of SGLT-1 and that there seems to be an upregulation of other glucose transport mechanisms in the apical membrane of lagomorph jejunum epithelium under hypoxia, securing the epithelial energy supply and thus integrity.

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Section: Methodsmentioning

confidence: 99%

Glucose transport across lagomorph jejunum epithelium is modulated by AMP-activated protein kinase under hypoxia

Dengler

Rackwitz

Pfannkuche

et al. 2017

Journal of Applied Physiology

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“…Recent reports have documented a range of beneficial effects of FFA beyond its direct anti-inflammatory activity, including its ability to promote carbonyl reductase 1 ( CBR1 ) upregulation and thereby protect against pulmonary damage induced by sepsis ( 23 ). It can also reportedly downregulate the expression of osteoclastogenesis-related genes while activating mitogen-activated protein kinase (MAPK) signaling and thereby preventing osteoporosis ( 24 , 25 ), in addition to inducing the AMP-activated protein kinase (AMPK) activation and thereby enhancing angiogenic activity in vitro and in vivo ( 26 ). The pleiotropic properties of FFA may thus offer substantial benefits to treated patients.…”

Section: Discussionmentioning

confidence: 99%

Flufenamic Acid, a Promising Agent for the Sensitization of Colistin-Resistant Gram-Negative Bacteria to Colistin

et al. 2023

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“…Another study showed that the knockdown of AKR1C3 overcame doxorubicin resistance by promoting autophagy in gastrointestinal cancer cells 34 . In addition, FLU, an AKR1C3 inhibitor, has been reported to activate AMPK signaling, which directly regulates autophagy via ULK1 phosphorylation 43 , 44 . These findings led us to examine whether LD accumulation by ARK1C3 depends on autophagy.…”

Section: Discussionmentioning

confidence: 99%

AKR1C3-dependent lipid droplet formation confers hepatocellular carcinoma cell adaptability to targeted therapy

Wu¹,

Dai²,

Li³

et al. 2022

Theranostics

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Rationale: Increased lipid droplet (LD) formation has been linked to tumor metastasis, stemness, and chemoresistance in various types of cancer. Here, we revealed that LD formation is critical for the adaptation to sorafenib in hepatocellular carcinoma (HCC) cells. We aim to investigate the LD function and its regulatory mechanisms in HCC. Methods:The key proteins responsible for LD formation were screened by both metabolomics and proteomics in sorafenib-resistant HCC cells and further validated by immunoblotting and immunofluorescence staining. Biological function of AKR1C3 was evaluated by CRISPR/Cas9-based gene editing. Isotopic tracing analysis with deuterium 3 -labeled palmitate or carbon13-labeled glucose was conducted to investigate fatty acid (FA) and glucose carbon flux. Seahorse analysis was performed to assess the glycolytic flux and mitochondrial function. Selective AKR1C3 inhibitors were used to evaluate the effect of AKR1C3 inhibition on HCC tumor growth and induction of autophagy. Results: We found that long-term sorafenib treatment impairs fatty acid oxidation (FAO), leading to LD accumulation in HCC cells. Using multi-omics analysis in cultured HCC cells, we identified that aldo-keto reductase AKR1C3 is responsible for LD accumulation in HCC. Genetic loss of AKR1C3 fully depletes LD contents, navigating FA flux to phospholipids, sphingolipids, and mitochondria. Furthermore, we found that AKR1C3-dependent LD accumulation is required for mitigating sorafenib-induced mitochondrial lipotoxicity and dysfunction. Pharmacologic inhibition of AKR1C3 activity instantly induces autophagy-dependent LD catabolism, resulting in mitochondrial fission and apoptosis in sorafenib-resistant HCC clones. Notably, manipulation of AKR1C3 expression is sufficient to drive the metabolic switch between FAO and glycolysis. Conclusions: Our findings revealed that AKR1C3-dependent LD formation is critical for the adaptation to sorafenib in HCC through regulating lipid and energy homeostasis. AKR1C3-dependent LD accumulation protects HCC cells from sorafenib-induced mitochondrial lipotoxicity by regulating lipophagy. Targeting AKR1C3 might be a promising therapeutic strategy for HCC tumors.

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Flufenamic acid promotes angiogenesis through AMPK activation

Cited by 6 publications

References 47 publications

Glucose transport across lagomorph jejunum epithelium is modulated by AMP-activated protein kinase under hypoxia

Glucose transport across lagomorph jejunum epithelium is modulated by AMP-activated protein kinase under hypoxia

Flufenamic Acid, a Promising Agent for the Sensitization of Colistin-Resistant Gram-Negative Bacteria to Colistin

AKR1C3-dependent lipid droplet formation confers hepatocellular carcinoma cell adaptability to targeted therapy

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