Soft TCPTP Agonism—Novel Target to Rescue Airway Epithelial Integrity by Exogenous Spermidine

Ghisalberti, Carlo Angelo; Borzı̀, Rosa Maria; Cetrullo, Silvia; Flamigni, Flavio; Cairo, Gaetano

doi:10.3389/fphar.2016.00147

Cited by 9 publications

(6 citation statements)

References 115 publications

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“…After 24 h starvation, the cells were pretreated with SPD (Sigma S2501, spermidine trihydrochloride), 100 nM, 24 h. The starvation step was useful to reduce the endogenous polyamine pool so to better highlight the effect of 100 nM exogenous SPD pre-treatment. This subμmolar dose was selected on the basis of previous literature hints that indicate a narrow useful dosage window in which addition of exogenous SPD may support cell homeostatic activities by increasing the unbound pool without exerting inflammation or apoptosis promoting effects [32]. Previous work from our group showed that 1-10 μmolar doses instead promote chondrocyte terminal differentiation [33], in keeping with previous observations of high SPD levels in the extracellular matrix of the ossifying cartilage [34].…”

Section: Culture and Treatment Of Chondrocyte Primary Culturesmentioning

confidence: 54%

Spermidine rescues the deregulated autophagic response to oxidative stress of osteoarthritic chondrocytes

D’Adamo

Cetrullo

Guidotti

et al. 2020

Free Radical Biology and Medicine

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Oxidative stress (OS) contributes to Osteoarthritis (OA) pathogenesis and its effects are worsened by the impairment of homeostatic mechanisms such as autophagy in OA chondrocytes. Rescue of an efficient autophagic flux could therefore reduce the bulk of damaged molecules, and at the same time improve cell function and viability. As a promising dietary or intra-articular supplement to rescue autophagy in OA chondrocytes, we tested spermidine (SPD), known to induce autophagy and to reduce OS in several other cellular models. Chondrocytes were obtained from OA cartilage and seeded at high-density to keep their differentiated phenotype. The damaging effects of OS and the chondroprotective activity of SPD were assessed by evaluating the extent of cell death, oxidative DNA damage and caspase 3 activation. The autophagy promoting activity of SPD was evaluated by assessing pivotal autophagic effectors, i.e. Beclin-1 (BECN-1), microtubule-associated protein 1 light chain 3 II (LC3-II) and p62. BECN-1 protein expression was significantly increased by SPD and reduced by H 2 O 2 treatment. SPD also rescued the impaired autophagic flux consequent to H 2 O 2 exposure by increasing mRNA and protein expression of LC3-II and p62. SPD induction of mitophagy was revealed by immunofluorescent co-localization of LC3-II and TOM20. The key protective role of autophagy was confirmed by the loss of SPD chondroprotection upon autophagy-related gene 5 (ATG5) silencing. Significant SPD tuning of the H 2 O 2-dependent induction of degradative (MMP-13) inflammatory (iNOS, COX-2) and hypertrophy markers (RUNX2 and VEGF) was revealed by Real Time PCR and pointed at the SPD ability of reducing NF-κB activation through autophagy induction. Conversely, blockage of autophagy led to parallel increases of oxidative markers and p65 nuclear translocation. SPD also increased the proliferation of slow-proliferating primary cultures.Taken together, our findings highlight the chondroprotective, anti-oxidant and anti-inflammatory activity of SPD and suggest that the protection afforded by SPD against OS is exerted through the rescue of the autophagic flux.

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Section: Culture and Treatment Of Chondrocyte Primary Culturesmentioning

confidence: 54%

Spermidine rescues the deregulated autophagic response to oxidative stress of osteoarthritic chondrocytes

D’Adamo

Cetrullo

Guidotti

et al. 2020

Free Radical Biology and Medicine

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“…Spermine compacts DNA more actively than spermidine 52 . Furthermore, inside the cells spermidine is primarily complexed to anionic molecules and macromolecules (phospholipids of the cell membrane, ATP, RNA, DNA wrapped with histones) and only a fraction of the intracellular content represents the “free pool” 53 . Slight variation of this pool is achieved by treatment of the cells with low- µmolar/sub-µmolar amounts of spermidine, that have been shown to promote anti-inflammatory effects via triggering of T-cell protein tyrosine phosphatase (TCPTP) 54 or autophagy 55 .…”

Section: Discussionmentioning

confidence: 99%

“…Slight variation of this pool is achieved by treatment of the cells with low- µmolar/sub-µmolar amounts of spermidine, that have been shown to promote anti-inflammatory effects via triggering of T-cell protein tyrosine phosphatase (TCPTP) 54 or autophagy 55 . TCPTP is a phosphatase that exerts an anti-inflammatory role being able to down-regulate multiple signaling transduction pathways in the cells, acting at multiple levels 53 . An in vitro high throughput assay identified spermidine (at the same concentration used in the present work) and other 5 small molecules among 64280 potential candidates screened to tease out the best selective TCPTP agonists 56 .…”

Section: Discussionmentioning

confidence: 99%

Polyamine supplementation reduces DNA damage in adipose stem cells cultured in 3-D

Minguzzi

Guidotti

Platano

et al. 2019

Sci Rep

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According to previous research, natural polyamines exert a role in regulating cell committment and differentiation from stemness during skeletal development. In order to assess whether distinct polyamine patterns are associated with different skeletal cell types, primary cultures of stem cells, chondrocytes or osteoblasts were dedicated for HPLC analysis of intracellular polyamines. Spermine (SPM) and Spermidine (SPD) levels were higher in adipose derived stem cells (ASC) compared to mature skeletal cells, i.e. chondrocytes and osteoblasts, confirming the connection of polyamine content with stemness. To establish whether polyamines can protect ASC against oxidative DNA damage in a 3-D differentiation model, the level of γH2AX was measured by western blot, and found to correlate with age and BMI of patients. Addition of either polyamine to ASC was able to hinder DNA damage in the low micromolecular range, with marked reduction of γH2AX level at 10 µM SPM and 5 µM SPD. Molecular analysis of the mechanisms that might underlie the protective effect of polyamine supplementation evidences a possible involvement of autophagy. Altogether, these results support the idea that polyamines are able to manage both stem cell differentiation and cell oxidative damage, and therefore represent appealing tools for regenerative and cell based applications.

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“…36 We saw higher levels of spermidine, a product of ORN that plays a role in the regulation of cell proliferation and nucleic acid synthesis. 37,38 Previous studies report higher levels of ARG in muscles of COPD patients, but not in arterial blood. 12,13 In stable patients with moderate-to-severe COPD, endogenous ARG and CIT production is upregulated but no difference in whole body NO production was detectable (ARG-to-CIT flux).…”

Section: Amino Acids Involved In Nitrogen Removalmentioning

confidence: 96%

<p>Smokers with COPD Show a Shift in Energy and Nitrogen Metabolism at Rest and During Exercise</p>

Holz¹,

DeLuca²,

Roepcke³

et al. 2020

COPD

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There is an ongoing demand for easily accessible biomarkers that reflect the physiological and pathophysiological mechanisms of COPD. To test if an exercise challenge could help to identify clinically relevant metabolic biomarkers in COPD. Patients and Methods: We performed two constant-load exercise challenges separated by 4 weeks including smokers with COPD (n=23/19) and sex-and age-matched healthy smokers (n=23/20). Two hours after a standardized meal venous blood samples were obtained before, 5 mins after the start, at the end of submaximal exercise, and following a recovery of 20 mins. Data analysis was performed using mixed-effects model, with the metabolite level as a function of disease, time point and interaction terms and using each individual's resting level as reference. Results: Exercise duration was longer in healthy smokers but lactate levels were comparable between groups at all four time points. Glucose levels were increased in COPD. Glutamine was lower, while glutamate and arginine were higher in COPD. Branched-chain amino acids showed a stronger decline during exercise in healthy smokers. Carnitine and the acylcarnitines C16 and C18:1 were increased in COPD. These metabolite levels and changes were reproducible in the second challenge. Conclusion: Higher serum glucose, evidence for impaired utilization of amino acids during exercise and a shift of energy metabolism to enhanced consumption of lipids could be early signs for a developing metabolic syndrome in COPD. In COPD patients, deviations of energy and nitrogen metabolism are amplified by an exercise challenge.

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Soft TCPTP Agonism—Novel Target to Rescue Airway Epithelial Integrity by Exogenous Spermidine

Cited by 9 publications

References 115 publications

Spermidine rescues the deregulated autophagic response to oxidative stress of osteoarthritic chondrocytes

Spermidine rescues the deregulated autophagic response to oxidative stress of osteoarthritic chondrocytes

Polyamine supplementation reduces DNA damage in adipose stem cells cultured in 3-D

<p>Smokers with COPD Show a Shift in Energy and Nitrogen Metabolism at Rest and During Exercise</p>

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