Elastin-Derived Peptides Are New Regulators of Insulin Resistance Development in Mice

Blaise, Sébastien; Romier, Béatrice; Kawecki, Charlotte; Ghirardi, Maxime; Rabenoelina, Fanja; Baud, Stéphanie; Duca, Laurent; Maurice, Pascal; Heinz, Andrea; Schmelzer, Christian E.H.; Tarpin, Michel; Martiny, Laurent; Garbar, Christian; Dauchez, Manuel; Debelle, Laurent; Durlach, V.

doi:10.2337/db13-0508

Cited by 95 publications

(127 citation statements)

References 41 publications

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“…9,10 In addition to this structural role, elastin-derived peptides have been shown to contribute to insulin resistance by blocking glucose uptake in muscle and adipose tissue. 11 The degradation of the ECM proteins such as collagen and elastin is controlled by proteinases that include matrix metalloproteinases (MMPs) and their endogenous inhibitors such as tissue inhibitors of metalloproteinases (TIMPs). [12][13][14] Of these, MMP-12 is a metalloelastase that has the capacity to degrade elastin and plays important roles in tissue fibrosis and injury.…”

Section: Introductionmentioning

confidence: 99%

Obesity-induced remodeling of the adipose tissue elastin network is independent of the metalloelastase MMP-12

et al. 2015

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The extracellular matrix (ECM) plays important roles in maintaining adequate adipose tissue function and in metabolic regulation. Here we have examined the organization of a relatively unexplored adipose tissue ECM component, elastin and its response to diet induced obesity in mice. Additionally, we have explored the regulation and requirement of macrophage metalloelastase, MMP-12, in adipose tissue ECM remodeling in obesity. In visceral fat depots, elastin fibers form a mesh-like net that becomes denser with diet-induced obesity. In contrast, the elastin fibers in subcutaneous adipose depots are more linear in organization, and are tightly associated with adipose tissue macrophages (ATMs). We found that Mmp12 is produced predominantly by ATMs and can be induced with both short-and long-term high fat diet challenge and rapid remodeling induced by lipolysis. This contrasts with Mmp14 and Timp1 which are further induced only after chronic obesity in non-ATM populations. We examined obese transgenic Mmp12 ¡/¡ mice and found an increase in gene expression of ECM genes with diet-induced obesity, but showed few significant differences in metabolic parameters, elastin matrix density, or in adipose tissue inflammation. Together, these studies reveal the architecture and diet-induced regulation of the elastin matrix and suggest that MMP-12 is not required for elastin matrix remodeling or for the metabolic dysfunction that occurs with obesity.

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Section: Introductionmentioning

confidence: 99%

Obesity-induced remodeling of the adipose tissue elastin network is independent of the metalloelastase MMP-12

et al. 2015

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“…29,30 Indeed, ≈29 different peptides were identified in kE mixtures by mass spectrometry analysis with one third containing the bioactive GxxPG motif (not shown). 14 In contrast, the scrambled VVGPGA is unable to adopt the type VIII β-turn conformation because of the lack of GxxPG motif. 30 However, previous studies have reported that simple proline-containing peptides, such as PG, WP, and PGP (putative fragments of collagen and elastin), possess significant antithrombotic and anticoagulant effects in vitro and in vivo.…”

Section: Discussionmentioning

confidence: 99%

“…These 3 subunits form a functional receptor in human platelets that is able to trigger an increase in sialidase activity on binding to EDP. In contrast to PPCA, the catalytic activity of Neu-1 has been shown to be essential for ERC-mediated effects both in vitro 19,32 and in vivo 13,14 by catalyzing the local conversion of GM 3 ganglioside into lactosylceramide. 19,32 Expression of Neu-1 and PPCA has been already reported in platelets.…”

Section: Discussionmentioning

confidence: 99%

“…[9][10][11]21,22 A growing body of evidences now suggests that these extracellular matrix degradation products can also affect adjacent/circulating cells and contribute to the progression of age-associated vascular diseases. 21,23 In this context, we recently demonstrated that chronic injection of EDP in mice potentiates atherosclerosis development and promotes insulin resistance, 14,24 2 events that mainly occur during aging. Results are expressed are mean±SEM of 4 to 6 independent experiments, each run in triplicate, and normalized to the control (w/o, without kE).…”

Section: Discussionmentioning

confidence: 99%

“…This peptide was used at a 4-fold higher concentration than kE (400 μg/mL) because it has been demonstrated that a 4-fold higher concentration is necessary to achieve the equivalent physiological stimulation levels of bioactive elastin peptides released after elastin degradation. 13,14,16 As negative control, a scrambled VVGPGA peptide was used. 17,18 As shown in Figure 2A and 2C, VGVAPG significantly decreased the area covered by platelets from 30 seconds of perfusion.…”

Section: Edp and Vgvapg Reduce Thrombus Formation In Vitro Under Flowmentioning

confidence: 99%

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Elastin-Derived Peptides Are New Regulators of Thrombosis

Kawecki

Hézard

Bocquet

et al. 2014

ATVB

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Objective-Elastin is the major structural extracellular matrix component of the arterial wall that provides the elastic recoil properties and resilience essential for proper vascular function. Elastin-derived peptides (EDP) originating from elastin fragmentation during vascular remodeling have been shown to play an important role in cell physiology and development of cardiovascular diseases. However, their involvement in thrombosis has been unexplored to date. In this study, we investigated the effects of EDP on (1) platelet aggregation and related signaling and (2) thrombus formation. We also characterized the mechanism by which EDP regulate thrombosis. Approach and Results-We show that EDP, derived from organo-alkaline hydrolysate of bovine insoluble elastin (kappaelastin), decrease human platelet aggregation in whole blood induced by weak and strong agonists, such as ADP, epinephrine, arachidonic acid, collagen, TRAP, and U46619. In a mouse whole blood perfusion assay over a collagen matrix, kappa-elastin and VGVAPG, the canonical peptide recognizing the elastin receptor complex, significantly decrease thrombus formation under arterial shear conditions. We confirmed these results in vivo by demonstrating that both kappa-elastin and VGVAPG significantly prolonged the time for complete arteriole occlusion in a mouse model of thrombosis and increased tail bleeding times. Finally, we demonstrate that the regulatory role of EDP on thrombosis relies on platelets that express a functional elastin receptor complex and on the ability of EDP to disrupt plasma von Willebrand factor interaction with collagen. Conclusions-These

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Elastin molecular aging promotes MDA‐MB‐231 breast cancer cell invasiveness

et al. 2018

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Elastin is a long‐lived extracellular matrix protein responsible for the structural integrity and function of tissues. Breast cancer elastosis is a complex phenomenon resulting in both the deposition of elastotic masses and the local production of elastin fragments. In invasive human breast cancers, an increase in elastosis is correlated with severity of the disease and age of the patient. Elastin‐derived peptides ( EDP s) are a hallmark of aging and are matrikines – matrix fragments having the ability to regulate cell physiology. They are known to promote processes linked to tumor progression, but their effects on breast cancer cells remain unexplored. Our data show that EDP s enhance the invasiveness of MDA ‐ MB ‐231 breast cancer cells through the engagement of matrix metalloproteases 14 and 2. We therefore suggest that elastosis and/or an aged stroma could promote breast cancer cell invasiveness.

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Elastin-Derived Peptides Are New Regulators of Insulin Resistance Development in Mice

Cited by 95 publications

References 41 publications

Obesity-induced remodeling of the adipose tissue elastin network is independent of the metalloelastase MMP-12

Obesity-induced remodeling of the adipose tissue elastin network is independent of the metalloelastase MMP-12

Elastin-Derived Peptides Are New Regulators of Thrombosis

Elastin molecular aging promotes MDA‐MB‐231 breast cancer cell invasiveness

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