François-Xavier Maquart’s research while affiliated with Université de Reims Champagne-Ardenne and other places

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Publications (136)


Figure 8. a) Effects of Cu-Met at different levels and cold temperature on TIMP-2 level in
Oral copper-methionine decreases matrix metalloproteinase-2 activity in the liver and brain of broiler chickens subjected to cold stress for ascites incidence
  • Preprint
  • File available

October 2023

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41 Reads

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Rahman Jahanian

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Francois-Xavier Maquart

Copper plays an antioxidant role in biological reactions. This study examined the impact of copper-methionine supplementation on the matrix metalloproteinase-2 (MMP-2) activity and gene expression in the liver and brain of broiler chickens subjected to cold temperature. A total of 480 broiler chickens were assigned to 6 groups and reared under either low (15-19 C) or normal temperature (25-28 C) and fed a basal diet enriched with different concentrations of copper-methionine (Cu-Met) supplementation (0, 100 or 200 mg.kg-1). Ascites was exclusively observed in broiler chickens kept in low temperature and fed with basal diet without Cu-Met during the seventh week, identified by the presence of abdominal fluid accumulation. Broilers' livers and brains were separated for MMP-2 and tissue inhibitor of metalloproteinase-2 (TIMP-2) analysis. Results of gelatin zymography on these samples demonstrated that incidence of ascites was associated with increased MMP-2 levels in liver and brain. MMP-2 activity assay confirmed the results obtained by zymography. RT-qPCR experiments revealed an upregulation in the mRNA expression of MMP-2. In contrast, the treatments did not induce significant alterations in TIMP-2 levels. Results suggest that oral copper-methionine can decrease the ascites occurrence and might be useful for prevention of ascites in broiler chickens. Key words: Matrix metalloproteinase-2 (MMP-2); Tissue inhibitor of metalloproteinase-2 (TIMP-2); Copper-methionine; Liver; Brain; Broiler chicken; Ascites; Cold stress

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The Glypican-1/HGF/C-Met and Glypican-1/VEGF/VEGFR2 Ternary Complexes Regulate Hair Follicle Angiogenesis

December 2021

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174 Reads

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14 Citations

The hair renewal involves changes in the morphology of the hair follicle and its micro-vascularization. In alopecia, the hair cycle is accelerated, resulting in the formation of thinner and shorter hair. In addition, alopecia is associated with a decrease in the micro-vascularization of the hair follicles. In this study, the role of glypicans (GPCs) was analyzed in the regulation of the angiogenesis of human dermal microvascular endothelial cells (HDMEC). The analysis of glypican gene expression showed that GPC1 is the major glypican expressed by human keratinocytes of outer root sheath (KORS), human hair follicle dermal papilla cells (HHFDPC) and HDMEC. KORS were demonstrated to secrete VEGF and HGF. The HDMEC pseudotube formation was induced by KORS conditioned media (KORS CM ). It was totally abrogated after GPC1 siRNA transfection of HDMEC. Moreover, when cleaved by phospholipase C (PLC), GPC1 promotes the proliferation of HDMEC. Finally, GPC1 was shown to interact directly with VEGFR2 or c-Met to regulate angiogenesis induced by the activation of these receptors. Altogether, these results showed that GPC1 is a key regulator of microvascular endothelial cell angiogenesis induced by VEGF and HGF secreted by KORS. Thus, GPC1 might constitute an interesting target to tackle alopecia in dermatology research.


F4, a collagen XIX-derived peptide, inhibits tumor angiogenesis through αvβ3 and α5β1 integrin interaction

January 2021

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149 Reads

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8 Citations

We previously demonstrated that F4 peptide (CNPEDCLYPVSHAHQR) from collagen XIX was able to inhibit melanoma cell migrationin vitro and cancer progression in a mouse melanoma model. The aim of the present work was to study the anti-angiogenic properties of F4 peptide. We demonstrated that F4 peptide inhibited VEGF-induced pseudo-tube formation on Matrigel by endothelial cells and endothelial sprouting in a rat aortic ring assay. By affinity chromatography, we identified αvβ3 and α5β1 integrins as potential receptors for F4 peptide on endothelial cell surface. Using solid phase assays, we proved the direct interaction between F4 and both integrins. Taken together, our results demonstrate that F4 peptide is a potent antitumor agent inhibiting both angiogenesis and tumor cell migration.


Fig. 5 VGVAPG and AGVPGLGVG synthetic elastin peptides induced membrane bleb formation. HT-1080 cells were treated with three different synthetic peptides at concentrations ranging from 10 −11 to 10 −3 M for 40 min. The quantification of the blebbing cell number was evaluated by counting 10 fields per well under a phase contrast optical microscope. Results were expressed as mean ± S.E.M. Data from one experiment, representative of three independent experiments, are shown
Tumour cell blebbing and extracellular vesicle shedding: key role of matrikines and ribosomal protein SA

February 2019

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255 Reads

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29 Citations

British Journal of Cancer

Background: Carcinogenesis occurs in elastin-rich tissues and leads to local inflammation and elastolytic proteinase release. This contributes to bioactive matrix fragment (Matrikine) accumulation like elastin degradation products (EDP) stimulating tumour cell invasive and metastatic properties. We previously demonstrate that EDPs exert protumoural activities through Hsp90 secretion to stabilised extracellular proteinases. Methods: EDP influence on cancer cell blebbing and extracellular vesicle shedding were examined with a videomicroscope coupled with confocal Yokogawa spinning disk, by transmission electron microscopy, scanning electron microscopy and confocal microscopy. The ribosomal protein SA (RPSA) elastin receptor was identified after affinity chromatography by western blotting and cell immunolocalisation. mRNA expression was studied using real-time PCR. SiRNA were used to confirm the essential role of RPSA. Results: We demonstrate that extracellular matrix degradation products like EDPs induce tumour amoeboid phenotype with cell membrane blebbing and shedding of extracellular vesicle containing Hsp90 and proteinases in the extracellular space. EDPs influence intracellular calcium influx and cytoskeleton reorganisation. Among matrikines, VGVAPG and AGVPGLGVG peptides reproduced EDP effects through RPSA binding. Conclusions: Our data suggests that matrikines induce cancer cell blebbing and extracellular vesicle release through RPSA binding, favouring dissemination, cell-to-cell communication and growth of cancer cells in metastatic sites.



Conformation-dependent binding of a Tetrastatin peptide to avB3 integrin decreases melanoma progression through FAK/PI3K/Akt pathway inhibition.

June 2018

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514 Reads

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23 Citations

Tetrastatin, a 230 amino acid sequence from collagen IV, was previously demonstrated to inhibit melanoma progression. In the present paper, we identified the minimal active sequence (QKISRCQVCVKYS: QS-13) that reproduced the anti-tumor effects of whole Tetrastatin in vivo and in vitro on melanoma cell prolifération, migration and invasion. We demonstrated that QS-13 binds to SK-MEL-28 melanoma cells through the αvβ3 integrin using blocking antibody and β3 integrin subunit siRNAs strategies. Relevant QS-13 conformations were extracted from molecular dynamics simulations and their interactions with αVβ3 integrin were analyzed by docking experiments to determine the binding areas and the QS-13 amino acids crucial for the binding. The in silico results were confirmed by in vitro experiments. Indeed, QS-13 binding to SK-MEL-28 was dependent on the presence of a disulfide-bound as shown by mass spectroscopy and the binding site on αVβ3 was located in close vicinity to the RGD binding site. QS-13 binding inhibits the FAK/ PI3K/Akt pathway, a transduction pathway that is largely involved in tumor cell proliferation and migration. Taken together, our results demonstrate that the QS-13 peptide binds αvβ3 integrin in a conformation- dependent manner and is a potent antitumor agent that could target cancer cells through αVβ3.



Lumican as a multivalent effector in wound healing

March 2018

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95 Reads

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66 Citations

Advanced Drug Delivery Reviews

Wound healing, a complex physiological process, is responsible for tissue repair after exposure to destructive stimuli, without resulting in complete functional regeneration. Injuries can be stromal or epithelial, and most cases of wound repair have been studied in the skin and cornea. Lumican, a small leucine-rich proteoglycan, is expressed in the extracellular matrices of several tissues, such as the cornea, cartilage, and skin. This molecule has been shown to regulate collagen fibrillogenesis, keratinocyte phenotypes, and corneal transparency modulation. Lumican is also involved in the extravasation of inflammatory cells and angiogenesis, which are both critical in stromal wound healing. Lumican is the only member of the small leucine-rich proteoglycan family expressed by the epithelia during wound healing. This review summarizes the importance of lumican in wound healing and potential methods of lumican drug delivery to target wound repair are discussed. The involvement of lumican in corneal wound healing is described based on in vitro and in vivo models, with critical emphasis on its underlying mechanisms of action. Similarly, the expression and role of lumican in the healing of other tissues are presented, with emphasis on skin wound healing. Overall, lumican promotes normal wound repair and broadens new therapeutic perspectives for impaired wound healing.


Fig. 1. Secondary structure, surface representation and N-glycosylation positions on human fibromodulin. (A) Cartoon representation: the fibromodulin backbone is colored according to the secondary structure of the core protein. The residues bearing the N-glycosylations are displayed using orange Van der Waals motifs. Bi-antennary glycosylated chains were modeled with gray licorice. (B) Surface representation: it considers the occupancy of the glycosylated chains which were modeled with gray surfaces.
Fig. 2. Schematic diagram demonstrating postulated mediators of the action of lumican in modulating key cellular functions. (A) The interaction of lumican with integrins was proposed to activate signaling pathways regulating cell growth, apoptosis, adhesion, cell motility, invasion, EMT and metastasis. Lumican is also involved in the inhibition of MMP-14 activity via a direct binding to the catalytic domain regulating cell motility, invasion, EMT and metastasis. (B) Lumican was shown to interact with TGF-β, sequestering the growth factor in the ECM, in a way that modulates TGF-β binding to the respective receptors and resulting in regulation of cell adhesion and EMT. (C) Lumican was also reported to interact with CD14 on macrophages, enhancing phagocytosis, or to interact with lipopolysaccharide and Toll-Like Receptor-4, regulating the immune response. (D) Lumican was also shown to interact with Fas-Fas ligand, mediating apoptosis and the immune response. Hpx, hemopexin domain. Adapted from a figure originally published in FEBS J, Brézillon et al. [96].
Fig. 3. Structure of MMP-14. (A) Domain structure of MMP-14 (MT1-MMP). (B) Surface representation of MMP-14 catalytic domain. The coordinates extracted from the pdb structure 1BQQ present a catalytic site (green) and the MT-LOOP (red). The Asn229 is highlighted in yellow as a possible N-glycosylation site.
Structural characteristics of human SLRPs.
Small leucine-rich proteoglycans and matrix metalloproteinase-14: Key partners?

December 2017

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996 Reads

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62 Citations

Matrix Biology

Small leucine-rich proteoglycans (SLRPs) are important regulators of extracellular matrix assembly and cell signaling. They are a family of proteoglycans that are present in extracellular matrix and that share in common multiple repeats of a leucine-rich structural motif. SLRPs have been identified as inhibitors of cancer progression by affecting MMPs, especially MMP-14 activity. Lumican, a member of the SLRPs family, and its derived peptides were shown to possess anti-tumor activity. Interestingly, it was demonstrated recently that lumican interacts directly with the catalytic domain of MMP-14 and inhibits its activity. The aim of this review was to summarize the interactions between SLRPs and MMPs with a special interest to lumican.


Tau protein as a possible marker of cerebrospinal fluid leakage in cerebrospinal fluid rhinorrhoea: A pilot study

October 2017

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265 Reads

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6 Citations

Biochemia Medica

Introduction The management of posttraumatic cerebrospinal fluid (CSF) rhinorrhoea remains a clinical challenge. Cerebrospinal fistula is a dural defect responsible for possible CSF leakage into the contiguous air-filled cavities located at the skull base. The risk of central nervous system infection in these conditions is severe and can be life threatening. Consequently, a specific CSF biomarker might be used in case of difficult diagnosis of CSF rhinorrhoea. CSF Tau protein is a neuronal protein, commonly assessed for diagnosis of Alzheimer Disease (AD). The aim of this study was to determine whether the Tau protein could be a relevant marker of CSF leakage. Materials and methods Tau protein measurement was performed by enzyme-linked immunosorbent assay in 13 patients with CSF leakage (CSF rhinorrhoea group), and 8 patients with spontaneous aqueous rhinorrhoea (non-CSF leakage group). The serum concentration of Tau protein was measured by ELISA in both CSF rhinorrhoea group and non-CSF leakage group. Results In patients with CSF leakage, CSF Tau protein median concentration was 479 ng/L (197 - 2325 ng/L). On the other hand, the Tau protein concentration was below the lower limit of quantification (LLoQ) (< 87 ng/L) in non-CSF leakage group. Serum Tau protein concentration by ELISA was also below LLoQ (< 87 ng/L) for all subjects. Conclusion ELISA measurement of Tau protein in rhinorrhoea fluid may be a reliable and relevant marker for detecting the presence of CSF in the nasal discharge and sign the existence of a CSF leakage.


Citations (67)


... Hair renewal involves changes in microvessel formation, and hair loss is strongly associated with reduced microvascular formation in hair follicles [27]. Based on this, we examined the effect of DOP on the biological functions of MVECs at the cellular level. ...

Reference:

Dendrobium officinale polysaccharide promotes angiogenesis as well as follicle regeneration and hair growth through activation of the WNT signaling pathway
The Glypican-1/HGF/C-Met and Glypican-1/VEGF/VEGFR2 Ternary Complexes Regulate Hair Follicle Angiogenesis

... However, some studies have also examined the biochemical role of collagen in neo-angiogenesis, investigating the pathways in which this protein is involved. More specifically, some of its peptide derivatives exhibit anti-angiogenic effects involving integrins αvβ3 and α5β1 [86]. Other peptides, including those derived from type IV collagen, inhibit endothelial cell proliferation stimulated by basic fibroblast growth factor (bFGF) or induce apoptosis in endothelial cells via a Fas-dependent mechanism [87], confirming the pleiotropic nature of tumor-associated collagen. ...

F4, a collagen XIX-derived peptide, inhibits tumor angiogenesis through αvβ3 and α5β1 integrin interaction

... A few years ago, the name "matrikines" was coined to refer to peptide products of partial proteolysis of ECM macromolecules capable of regulating cellular activity [6,7]. However, recent data indicate that some of these peptides may modulate proliferation, migration or apoptosis and play an important role in controlling tumor progression. ...

Les matrikines anti-tumorales : intérêt potentiel en cancérologie
  • Citing Article
  • March 2010

Bulletin de l Académie Nationale de Médecine

... The ECM plays a transcendental role not only during reepithelialization, but also during every phase of the wound healing process (reviewed in Olczyk et al., 2014;Maquart, 2015;Xue and Jackson, 2015;Tracy et al., 2016;Rousselle et al., 2019). The secretion of ECM components occurs in a coordinated fashion in response to specific inflammatory and growth factors. ...

La matrice extracellulaire : un partenaire majeur de la cicatrisation des plaies
  • Citing Article
  • October 2015

Bulletin de l Académie Nationale de Médecine

... A 2023 study suggested an unconventional nuclear mechanism by which uS2/RPSA strengthens the host's NF-κB-mediated antiviral signaling [43]. uS2/RPSA, also known as the 37/67-kDa laminin receptor, has been linked to a wide range of pathological conditions [75][76][77][78], including infections, oncogenesis, DNA damage repair, and neurodegenerative diseases. However, its role in modulating the NF-κB signaling pathway was not previously studied. ...

Tumour cell blebbing and extracellular vesicle shedding: key role of matrikines and ribosomal protein SA

British Journal of Cancer

... Zgodnie z literaturą, ten typ kolagenu może także wywierać odmienne działanie w tkance nowotworowej. Wykazano bowiem, że jedna z domen kolagenu typu IV posiada anty-nowotworowe właściwości, obniżając proliferację oraz inwazyjność komórek czerniaka [46]. Zawartość tego białka w metastatycznej tkance raka jelita grubego okazuje się być jednak zdecydowanie niższa niż w tkance zdrowej [25]. ...

Conformation-dependent binding of a Tetrastatin peptide to avB3 integrin decreases melanoma progression through FAK/PI3K/Akt pathway inhibition.

... Lumican is a small leucine-rich proteoglycan which is involved in the maintenance of tissue homeostasis and cell proliferation, migration and differentiation 58 . More specifically, it is involved in wound healing 59 , in the regulation of collagen fibrillogenesis 58 , has anti-angiogenesis function 60 and is possibly also involved in muscle 61 and bone formation 62 . BPIFA2 (also called parotid secretory protein, PSP) is a salivary protein that can bind to bacterial lipopolysaccharide 63 and it has been shown to have antibacterial functions 64 , but many of its functions are still unknown. ...

Lumican as a multivalent effector in wound healing
  • Citing Article
  • March 2018

Advanced Drug Delivery Reviews

... Originally thought to be mainly important in bone growth, they have been found to be involved in a wide range of cellular functions. These include promoting autophagy (decorin), modulation of the immune system by interacting with toll like receptors and also cytokines such as tumour necrosis factor α, and in the formation of the ECM architecture [16,[26][27][28][29][30][31]48]. Created with BioRender.com. ...

Small leucine-rich proteoglycans and matrix metalloproteinase-14: Key partners?

Matrix Biology

... This differs from the transient hyperphosphorylation of tau during development and during anesthesia and hypothermia. Therefore, the level of tau in cerebrospinal fluid (CSF), in particular phosphorylated tau, is a biomarker for AD diagnosis and can be used for staging of the disease [62,63]. Nevertheless, whether NFTs are the precursors of neuron death or the expression of intracellular adaptability of neurons, as well as the nature of the neurotoxic role of tau protein and the role of tau hyperphosphorylation in the progression of AD remain unresolved. ...

Tau protein as a possible marker of cerebrospinal fluid leakage in cerebrospinal fluid rhinorrhoea: A pilot study

Biochemia Medica

... On the other hand, extracellular matrix (ECM) and secreted proteins constitute part of the complex array of the TME [19]. Importantly, GB-induced CMA in murine PCs has been shown to increase the secretion of molecules such as Osteopontin (OPN) [18], which supports tumor growth [20][21][22][23], while the inhibition of this CMA upregulation leads to the release of molecules with anti-tumor properties, such as Lumican [18,[24][25][26][27][28][29]. Thus, a better understanding of the relationship between the secretion of these two proteins and the GB-induced CMA status in human PCs could let us validate these possible prognostic markers in GB patients. ...

Lumican effectively regulates the estrogen receptors-associated functional properties of breast cancer cells, expression of matrix effectors and epithelial-to-mesenchymal transition