Sex-related differences in matrix remodeling and early osteogenic markers in aortic valvular interstitial cells

Masjedi, Shirin; Lei, Ying; Patel, Jenny; Ferdous, Zannatul

doi:10.1007/s00380-016-0909-8

Cited by 32 publications

(20 citation statements)

References 49 publications

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“…High levels of ERK phosphorylation were detected in calcified and stenotic human valves [ 72 ]. In support of the hypothesis of early occurrence of sex-specific differences in CAVD pathogenesis, another study using VICs obtained from male and female rat and porcine aortic valves showed that there is a sex-related difference in the events associated with osteogenic differentiation of the aortic VICs, where male VICs are more prone to calcification than female ones [ 73 ]. Human VICs undergo osteoblastic differentiation in response to specific mediators such as BMPs and TGF-β [ 74 ].…”

Section: The Experimental Evidence Indicating Sex-related Differenmentioning

confidence: 96%

Sex-Specific Features of Calcific Aortic Valve Disease

Summerhill

Moschetta

Orekhov

et al. 2020

IJMS

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Calcific aortic valve disease (CAVD) is the most common valvular heart disease in developed countries predominantly affecting the elderly population therefore posing a large economic burden. It is a gradually progressive condition ranging from mild valve calcification and thickening, without the hemodynamic obstruction, to severe calcification impairing leaflet motion, known as aortic stenosis (AS). The progression of CAVD occurs over many years, and it is extremely variable among individuals. It is also associated with an increased risk of coronary events and mortality. The recent insights into the CAVD pathophysiology included an important role of sex. Accumulating evidence suggests that, in patients with CAVD, sex can determine important differences in the relationship between valvular calcification process, fibrosis, and aortic stenosis hemodynamic severity between men and women. Consequently, it has implications on the development of different valvular phenotypes, left ventricular hypertrophy, and cardiovascular outcomes in men and women. Along these lines, taking into account the sex-related differences in diagnosis, prognosis, and treatment outcomes is of profound importance. In this review, the sex-related differences in patients with CAVD, in terms of pathobiology, clinical phenotypes, and outcomes were discussed.

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Section: The Experimental Evidence Indicating Sex-related Differenmentioning

confidence: 96%

Sex-Specific Features of Calcific Aortic Valve Disease

Summerhill

Moschetta

Orekhov

et al. 2020

IJMS

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“…Supporting the hypothesis that sex-specific divergence of CAVD etiology may occur early on is a growing body of evidence indicating intrinsic cellular-scale differences between men and women [6] that also yield differences in the cellular response to pathological stimuli. For example, VIC culture in hormone-free osteogenic medium is associated with an increase in calcification in male VICs compared to female VICs [9]. The discovery that men and women exhibit different CAVD pathogenesis has the potential to provoke transformative changes in the approach used to investigate CAVD etiology as well as the clinical treatment of this disease.…”

Section: Implications For the Study And Treatment Of Cavdmentioning

confidence: 99%

Calcific Aortic Valve Disease

Porras

McCoy

Masters

2017

Circulation Research

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“…These results have led to a growing interest to better understand the regulatory role of TNF‐α in AVS. Recent studies suggest that TNF‐α induces VIC calcification through both apoptotic and osteogenic mechanisms 38‐41 . For example, VIC mineralization in human valves depends on apoptotic signaling through death receptor 4 caused by increasing expression of the TNF ligand superfamily member 10 (TNF10 or TRAIL) 42 .…”

Section: Introductionmentioning

confidence: 99%

Tumor necrosis factor‐α promotes and exacerbates calcification in heart valve myofibroblast populations

et al. 2021

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Pro‐inflammatory cytokines play critical roles in regulating valvular interstitial cell (VIC) phenotypic changes that can cause heart valve fibrosis and calcification. Tumor necrosis factor alpha (TNF‐α) is a cytokine known to influence VIC behavior and has been reported at high levels in calcified valves ex vivo. We sought to understand the specific effects of TNF‐α on VIC phenotypes (eg, fibroblast, profibrotic activated myofibroblasts) and its link with heart valve disorders. We characterize human aortic valve tissue from patients with valve disorders and identify a high variability of fibrotic and calcific markers between tissues. These results motivated in vitro studies to explore the effects of TNF‐α on defined VIC fibroblasts and profibrotic activated myofibroblasts, induced via FGF‐2 and TGF‐β1 treatment. Using 3D hydrogels to culture VICs, we measure the effect of TNF‐α (0.1‐10 ng/mL) on key markers of fibrosis (eg, αSMA, COL1A1) and calcification (eg, RUNX2, BMP2, and calcium deposits). We observe calcification in TNF‐α‐treated VIC activated myofibroblasts and identify the MAPK/ERK signaling cascade as a potential pathway for TNF‐α mediated calcification. Conversely, VIC fibroblasts respond to TNF‐α with decreased calcification. Treatment of VIC profibrotic activated myofibroblast populations with TNF‐α leads to increased calcification. Our in vitro findings correlate with findings in diseased human valves and highlight the importance of understanding the effect of cytokines and signaling pathways on specific VIC phenotypes. Finally, we reveal MAPK/ERK as a potential pathway involved in VIC‐mediated matrix calcification with TNF‐α treatment, suggesting this pathway as a potential pharmaceutical target for aortic valve disease.

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Sex-related differences in matrix remodeling and early osteogenic markers in aortic valvular interstitial cells

Cited by 32 publications

References 49 publications

Sex-Specific Features of Calcific Aortic Valve Disease

Sex-Specific Features of Calcific Aortic Valve Disease

Calcific Aortic Valve Disease

Tumor necrosis factor‐α promotes and exacerbates calcification in heart valve myofibroblast populations

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