Implications of Senescent Cell Burden and NRF2 Pathway in Uremic Calcification: A Translational Study

Laget, Jonas; Hobson, Sam; Muyor, Karen; Duranton, Flore; Cortijo, Irene; Bartochowski, Piotr; Jover, Bernard; Lajoix, Anne‐Dominique; Söderberg, Magnus; Ebert, Thomas; Stenvinkel, Peter; Argilés, Àngel; Kublickiene, Karolina; Gayrard, Nathalie

doi:10.3390/cells12040643

Cited by 5 publications

(10 citation statements)

References 79 publications

(81 reference statements)

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“…Interventional therapies have yet to be developed; however, the fact that free radical generation persists after generation of both toxins is of clinical importance. Using a novel animal model of 5/6 nephrectomised rats, we reported dysregulated NRF2 is linked to ectopic vascular calcification 48 . Hence therapeutically targeting the NRF2 pathway using NRF2 agonists may have positive clinical implications.…”

Section: Discussionmentioning

confidence: 97%

“…Strengths of the current study include a reasonably large kidney failure cohort that was carefully phenotyped. We also implemented a translational approach to test our hypothesis in a clinical cohort and an in vitro calcification model, as recapitulating uremic components in vitro has been difficult 48 . In addition, we assessed the magnitude of calcification in two separate locations of the vascular tree—coronary and epigastric arteries.…”

Section: Discussionmentioning

confidence: 99%

“…Using a novel animal model of 5/6 nephrectomised rats, we reported dysregulated NRF2 is linked to ectopic vascular calcification. 48 Hence therapeutically targeting the NRF2 pathway using NRF2 agonists may have positive clinical implications. However, further experimental studies are needed to determine the optimal window of intervention.…”

Section: Discussionmentioning

confidence: 99%

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Phenylacetylglutamine and trimethylamine N‐oxide: Two uremic players, different actions

Hobson,

Qureshi,

Ripswedan

et al. 2023

Eur J Clin Investigation

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BackgroundChronic kidney disease (CKD) patients exhibit a heightened cardiovascular (CV) risk which may be partially explained by increased medial vascular calcification. Although gut‐derived uremic toxin trimethylamine N‐oxide (TMAO) is associated with calcium‐phosphate deposition, studies investigating phenylacetylglutamine's (PAG) pro‐calcifying potential are missing.MethodsThe effect of TMAO and PAG in vascular calcification was investigated using 120 kidney failure patients undergoing living‐donor kidney transplantation (LD‐KTx), in an observational, cross‐sectional manner. Uremic toxin concentrations were related to coronary artery calcification (CAC) score, epigastric artery calcification score, and markers of established non‐traditional risk factors that constitute to the ‘perfect storm’ that drives early vascular aging in this patient population. Vascular smooth muscle cells were incubated with TMAO or PAG to determine their calcifying effects in vitro and analyse associated pathways by which these toxins may promote vascular calcification.ResultsTMAO, but not PAG, was independently associated with CAC score after adjustment for CKD‐related risk factors in kidney failure patients. Neither toxin was associated with epigastric artery calcification score; however, PAG was independently, positively associated with 8‐hydroxydeoxyguanosine. Similarly, TMAO, but not PAG, promoted calcium‐phosphate deposition in vitro, while both uremic solutes induced oxidative stress.ConclusionsIn conclusion, our translational data confirm TMAO's pro‐calcifying effects, but both toxins induced free radical production detrimental to vascular maintenance. Our findings suggest these gut‐derived uremic toxins have different actions on the vessel wall and therapeutically targeting TMAO may help reduce CV‐related mortality in CKD.

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Section: Discussionmentioning

confidence: 97%

Section: Discussionmentioning

confidence: 99%

See 1 more Smart Citation

Phenylacetylglutamine and trimethylamine N‐oxide: Two uremic players, different actions

Hobson,

Qureshi,

Ripswedan

et al. 2023

Eur J Clin Investigation

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“…Aging is associated with an accumulation of senescent cells resistant to apoptosis, contributing to medial calcification and increased expression of osteogenic markers 7,42 . Silencing Nrf2 has been found to speed up the senescence of vascular cells 43,44 , with both senescent cell accumulation and Nrf2 dysregulation implicated in medial VC pathogenesis 20 . The burgeoning body of evidence suggests that activating NRF2 could provide protective effects against age-related VC by mitigating cellular senescence.…”

Section: Discussionmentioning

confidence: 99%

“…However, it is imperative to acknowledge that NRF2 activators lack specificity and may induce activation of alternative pathways, such as the NF-κB signaling pathway, which has also been implicated in inhibiting VC 18,19 . Interestingly, NRF2 levels are higher in animal models of CKD and in end-stage renal disease (ESRD) patients with VC, even though uremic serum from these patients paradoxically increases VSMC calcification and decreases NRF2 20 . Molecules associated with NRF2, both upstream and downstream, have been identified as inhibitors of VC.…”

Section: Introductionmentioning

confidence: 99%

The NRF2/ID2 Axis in Vascular Smooth Muscle Cells: Novel Insights into the Interplay between Vascular Calcification and Aging

Xu,

Wei,

Wang

et al. 2024

Preprint

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OBJECTIVEVascular calcification (VC) significantly contributes to cardiovascular morbidity and mortality and escalates with age. However, effective pharmaceutical interventions are lacking, and the molecular mechanisms linking aging to VC remain elusive. This study explores the role of nuclear factor erythroid 2-related factor 2 (NRF2) in VC, specifically focusing on the interplay between vascular senescence and oxidative stress (OS).APPROACH AND RESULTSUsing a chronological aging mouse model, we noted a significant decline in the expression and activity of Nrf2 in the aortas of aged mice, coinciding with increased medial VC. Administering NRF2 activators effectively reduced this calcification. In the vascular smooth muscle cell (VSMC)-specific Nrf2 knockout (Nrf2SMCKO) models, created using adenine and Vitamin D, there was an increase in calcium deposition within the aortic medial layer, alongside heightened VSMC senescence and OS. Furthermore, NRF2 knockout exacerbated VC in aortic rings and primary VSMCs in high-phosphate conditions, while Nrf2 overexpression in VSMCs inhibited calcium deposition by alleviating cell senescence and OS. RNAseq analysis of the aortas fromNrf2SMCKOand control mice highlighted a significant downstream regulator of Inhibitor of DNA Binding 2 (ID2). Our results show that reduced NRF2 levels lead to increased VSMC senescence, characterized by heightened p16 expression and diminished ID2 expression. Inhibiting ID2 negated NRF2’s protective effects against VSMC senescence and VC.CONCLUSIONThis study emphasizes the critical role of NRF2 dysfunction in the nexus of vascular senescence, OS, and VC. It proposes the NRF2-ID2 axis in VSMCs as a promising therapeutic target for reducing VC and mitigating age-related cardiovascular diseases.HighlightsDecline in NRF2 activity is linked to increased vascular calcification (VC) and aging.VSMC-specificNrf2knockout causes a remarkable exacerbation of arterial calcification.NRF2 alleviates VC by inhibiting oxidative stress and VSMC senescence.ID2 contributes to the protective role of NRF2 in VSMC senescence and VC.

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STING1-accelerated vascular smooth muscle cell senescence-associated vascular calcification in diabetes is ameliorated by oleoylethanolamide via improved mitochondrial DNA oxidative damage

Chen,

Li,

Sun

et al. 2024

Free Radical Biology and Medicine

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Implications of Senescent Cell Burden and NRF2 Pathway in Uremic Calcification: A Translational Study

Cited by 5 publications

References 79 publications

Phenylacetylglutamine and trimethylamine N‐oxide: Two uremic players, different actions

Phenylacetylglutamine and trimethylamine N‐oxide: Two uremic players, different actions

The NRF2/ID2 Axis in Vascular Smooth Muscle Cells: Novel Insights into the Interplay between Vascular Calcification and Aging

STING1-accelerated vascular smooth muscle cell senescence-associated vascular calcification in diabetes is ameliorated by oleoylethanolamide via improved mitochondrial DNA oxidative damage

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