Your search keyword '"Lopez-Sanz, Laura"' showing total 6 results

1. Fcγ receptor activation mediates vascular inflammation and abdominal aortic aneurysm development.

Author

Lopez‐Sanz, Laura, Bernal, Susana, Jimenez‐Castilla, Luna, Prieto, Ignacio, La Manna, Sara, Gomez‐Lopez, Sergio, Blanco‐Colio, Luis Miguel, Egido, Jesus, Martin‐Ventura, Jose Luis, and Gomez‐Guerrero, Carmen

Subjects

*ABDOMINAL aortic aneurysms, *VASCULAR smooth muscle, *ELASTASES, *IMMUNE complexes, *MUSCLE cells, *DRUG target, *FC receptors

Abstract

Background: Abdominal aortic aneurysm (AAA), a degenerative vascular pathology characterized by permanent dilation of the aorta, is considered a chronic inflammatory disease involving innate/adaptive immunity. However, the functional role of antibody‐dependent immune response against antigens present in the damaged vessel remains unresolved. We hypothesized that engagement of immunoglobulin G (IgG) Fc receptors (FcγR) by immune complexes (IC) in the aortic wall contributes to AAA development. We therefore evaluated FcγR expression in AAA lesions and analysed whether inhibition of FcγR signaling molecules (γ‐chain and Syk kinase) influences AAA formation in mice. Methods: FcγR gene/protein expression was assessed in human and mouse AAA tissues. Experimental AAA was induced by aortic elastase perfusion in wild‐type (WT) mice and γ‐chain knockout (γKO) mice (devoid of activating FcγR) in combination with macrophage adoptive transfer or Syk inhibitor treatment. To verify the mechanisms of FcγR in vitro, vascular smooth muscle cells (VSMC) and macrophages were stimulated with IgG IC. Results: FcγR overexpression was detected in adventitia and media layers of human and mouse AAA. Elastase‐perfused γKO mice exhibited a decrease in AAA incidence, aortic dilation, elastin degradation, and VSMC loss. This was associated with (1) reduced infiltrating leukocytes and immune deposits in AAA lesions, (2) inflammatory genes and metalloproteinases downregulation, (3) redox balance restoration, and (4) converse phenotype of anti‐inflammatory macrophage M2 and contractile VSMC. Adoptive transfer of FcγR‐expressing macrophages aggravated aneurysm in γKO mice. In vitro, FcγR deficiency attenuated inflammatory gene expression, oxidative stress, and phenotypic switch triggered by IC. Additionally, Syk inhibition prevented IC‐mediated cell responses, reduced inflammation, and mitigated AAA formation. Conclusion: Our findings provide insight into the role and mechanisms mediating IgG‐FcγR‐associated inflammation and aortic wall injury in AAA, which might represent therapeutic targets against AAA disease. [ABSTRACT FROM AUTHOR]

Published

2021

2. Protective effect of suppressor of cytokine signalling 1‐based therapy in experimental abdominal aortic aneurysm.

Author

Bernal, Susana, Lopez‐Sanz, Laura, Jimenez‐Castilla, Luna, Prieto, Ignacio, Melgar, Ana, La Manna, Sara, Martin‐Ventura, Jose Luis, Blanco‐Colio, Luis Miguel, Egido, Jesus, and Gomez‐Guerrero, Carmen

Subjects

*ABDOMINAL aortic aneurysms, *SUPPRESSORS of cytokine signaling, *INVESTIGATIONAL therapies, *VASCULAR smooth muscle, *ELASTASES, *MUSCLE cells, *MACROPHAGES

Abstract

Background and Purpose: Abdominal aortic aneurysm (AAA) is a multifactorial disease characterized by chronic inflammation, oxidative stress and proteolytic activity in the aortic wall. Targeting JAK/signal transducer and activator of transcription (JAK/STAT) pathway is a promising strategy for chronic inflammatory diseases. We investigated the vasculo‐protective role of suppressor of cytokine signalling‐1 (SOCS1), the negative JAK/STAT regulator, in experimental AAA. Experimental Approach A synthetic, cell permeable peptide (S1) mimic of SOCS1 kinase inhibitory domain to suppress STAT activation was evaluated in the well‐established mouse model of elastase‐induced AAA by monitoring changes in aortic diameter, cellular composition and gene expression in abdominal aorta. S1 function was further evaluated in cultured vascular smooth muscle cells (VSMC) and macrophages exposed to elastase or elastin‐derived peptides. Key Results: S1 peptide prevented AAA development, evidenced by reduced incidence of AAA, aortic dilation and elastin degradation, partial restoration of medial VSMC and decreased inflammatory cells and oxidative stress in AAA tissue. Mechanistically, S1 suppressed STAT1/3 activation in aorta, down‐regulated cytokines, metalloproteinases and altered the expression of cell differentiation markers by favouring anti‐inflammatory M2 macrophage and contractile VSMC phenotypes. In vitro, S1 suppressed the expression of inflammatory and oxidative genes, reduced cell migration and reversed the phenotypic switch of macrophages and VSMC. By contrast, SOCS1 silencing promoted inflammatory response. Conclusion and Implications: This preclinical study demonstrates the therapeutic potential of SOCS1‐derived peptide to halt AAA progression by suppressing JAK/STAT‐mediated inflammation and aortic dilation. S1 peptide may therefore be a valuable option for the treatment of AAA. [ABSTRACT FROM AUTHOR]

Published

2021

3. Cyclic mimetics of kinase-inhibitory region of Suppressors of Cytokine Signaling 1: Progress toward novel anti-inflammatory therapeutics.

Author

La Manna, Sara, Lopez-Sanz, Laura, Bernal, Susana, Fortuna, Sara, Mercurio, Flavia A., Leone, Marilisa, Gomez-Guerrero, Carmen, and Marasco, Daniela

Subjects

*SUPPRESSORS of cytokine signaling, *BIOLOGICAL assay, *PHOSPHORYLATION, *OXIDATIVE stress, *CATALYTIC domains

Abstract

Herein we investigated the structural and cellular effects ensuing from the cyclization of a potent inhibitor of JAK2 as mimetic of SOCS1 protein, named PS5. The introduction of un-natural residues and a lactam internal bridge, within SOCS1-KIR motif, produced candidates that showed high affinity toward JAK2 catalytic domain. By combining CD, NMR and computational studies, we obtained valuable models of the interactions of two peptidomimetics of SOCS1 to deepen their functional behaviors. Notably, when assayed for their biological cell responses mimicking SOCS1 activity, the internal cyclic PS5 analogues demonstrated able to inhibit JAK-mediated tyrosine phosphorylation of STAT1 and to reduce cytokine-induced proinflammatory gene expression, oxidative stress generation and cell migration. The present study well inserts in the field of low-molecular-weight proteomimetics with improved longtime cellular effects and adds a new piece to the puzzled way for the conversion of bioactive peptides into drugs. [Display omitted] • Effects of cyclization on a potent mimetic of SOCS1 protein, PS5. • Structural model of interaction of cycles and JAK2. • Internal cyclic PS5 as inhibitors of JAK-mediated tyrosine phosphorylation of STAT1. • New inhibitors of proinflammatory gene expression, oxidative stress and migration. [ABSTRACT FROM AUTHOR]

Published

2021

4. Targeting NF-κB by the Cell-Permeable NEMO-Binding Domain Peptide Improves Albuminuria and Renal Lesions in an Experimental Model of Type 2 Diabetic Nephropathy.

Author

Opazo-Ríos, Lucas, Plaza, Anita, Sánchez Matus, Yenniffer, Bernal, Susana, Lopez-Sanz, Laura, Jimenez-Castilla, Luna, Carpio, Daniel, Droguett, Alejandra, Mezzano, Sergio, Egido, Jesús, and Gomez-Guerrero, Carmen

Subjects

DIABETIC nephropathies, TYPE 2 diabetes, BASAL lamina, ANIMAL models in research, BODY weight

Abstract

Diabetic nephropathy (DN) is a multifactorial disease characterized by hyperglycemia and close interaction of hemodynamic, metabolic and inflammatory factors. Nuclear factor-κB (NF-κB) is a principal matchmaker linking hyperglycemia and inflammation. The present work investigates the cell-permeable peptide containing the inhibitor of kappa B kinase γ (IKKγ)/NF-κB essential modulator (NEMO)-binding domain (NBD) as therapeutic option to modulate inflammation in a preclinical model of type 2 diabetes (T2D) with DN. Black and tan, brachyuric obese/obese mice were randomized into 4 interventions groups: Active NBD peptide (10 and 6 µg/g body weight); Inactive mutant peptide (10 µg/g); and vehicle control. In vivo/ex vivo fluorescence imaging revealed efficient delivery of NBD peptide, systemic biodistribution and selective renal metabolization. In vivo administration of active NBD peptide improved albuminuria (>40% reduction on average) and kidney damage, decreased podocyte loss and basement membrane thickness, and modulated the expression of proinflammatory and oxidative stress markers. In vitro, NBD blocked IKK-mediated NF-κB induction and target gene expression in mesangial cells exposed to diabetic-like milieu. These results constitute the first nephroprotective effect of NBD peptide in a T2D mouse model that recapitulates the kidney lesions observed in DN patients. Targeting IKK-dependent NF-κB activation could be a therapeutic strategy to combat kidney inflammation in DN. [ABSTRACT FROM AUTHOR]

Published

2020

5. Cyclic mimetics of kinase-inhibitory region of Suppressors of Cytokine Signaling 1: Progress toward novel anti-inflammatory therapeutics

Author

Laura Lopez-Sanz, Carmen Gomez-Guerrero, Sara La Manna, Susana Bernal, Daniela Marasco, Marilisa Leone, Flavia Anna Mercurio, Sara Fortuna, La Manna, Sara, Lopez-Sanz, Laura, Bernal, Susana, Fortuna, Sara, Mercurio, Flavia A., Leone, Marilisa, Gomez-Guerrero, Carmen, Marasco, Daniela, La Manna, S., Lopez-Sanz, L., Bernal, S., Fortuna, S., Mercurio, F. A., Leone, M., Gomez-Guerrero, C., and Marasco, D.

Subjects

Peptidomimetic, Mimetic peptides, Cytokine signaling, JAK/STAT, SOCS1, Oxidative stress, Inflammation, medicine.medical_treatment, Anti-Inflammatory Agents, 01 natural sciences, Proinflammatory cytokine, Mice, Structure-Activity Relationship, 03 medical and health sciences, chemistry.chemical_compound, Suppressor of Cytokine Signaling 1 Protein, Mimetic peptide, Drug Discovery, medicine, Animals, Protein Kinase Inhibitors, Cells, Cultured, 030304 developmental biology, Pharmacology, 0303 health sciences, Dose-Response Relationship, Drug, Molecular Structure, 010405 organic chemistry, Kinase, Chemistry, Suppressor of cytokine signaling 1, Organic Chemistry, JAK-STAT signaling pathway, Cell migration, Tyrosine phosphorylation, General Medicine, 0104 chemical sciences, Cell biology, Cytokine, Oxidative stre, Peptidomimetics

Abstract

Herein we investigated the structural and cellular effects ensuing from the cyclization of a potent inhibitor of JAK2 as mimetic of SOCS1 protein, named PS5. The introduction of un-natural residues and a lactam internal bridge, within SOCS1-KIR motif, produced candidates that showed high affinity toward JAK2 catalytic domain. By combining CD, NMR and computational studies, we obtained valuable models of the interactions of two peptidomimetics of SOCS1 to deepen their functional behaviors. Notably, when assayed for their biological cell responses mimicking SOCS1 activity, the internal cyclic PS5 analogues demonstrated able to inhibit JAK-mediated tyrosine phosphorylation of STAT1 and to reduce cytokine-induced proinflammatory gene expression, oxidative stress generation and cell migration. The present study well inserts in the field of low-molecular-weight proteomimetics with improved longtime cellular effects and adds a new piece to the puzzled way for the conversion of bioactive peptides into drugs.

Published

2021

6. Chimeric Peptidomimetics of SOCS 3 Able to Interact with JAK2 as Anti-inflammatory Compounds

Author

Carmen Gomez-Guerrero, Marilisa Leone, Laura Lopez-Sanz, Daniela Marasco, Sara Fortuna, Sara La Manna, Flavia Anna Mercurio, La Manna, S., Lopez-Sanz, L., Mercurio, F. A., Fortuna, S., Leone, M., Gomez-Guerrero, C., Marasco, D., La Manna, Sara, Lopez-Sanz, Laura, Mercurio, Flavia Anna, Fortuna, Sara, Leone, Marilisa, Gomez-Guerrero, Carmen, and Marasco, Daniela

Subjects

Peptidomimetic, Microscale thermophoresis, Chemistry, medicine.medical_treatment, Organic Chemistry, digestive, oral, and skin physiology, Mimetic peptides, cytokine signaling, JAK-STAT, SOCS3, inflammation, JAK-STAT signaling pathway, Glycoprotein 130, Biochemistry, Proinflammatory cytokine, Cell biology, Cytokine, Mimetic peptide, Drug Discovery, medicine, Ternary complex

Abstract

[Image: see text] The immunomodulatory effects of Suppressor of Cytokine Signaling (SOCS) proteins, that control the JAK/STAT pathway, indicate them as attractive candidates for immunotherapies. Recombinant SOCS3 protein suppresses the effects of inflammation, and its deletion in neurons or in immune cells increases pathological blood vessels growth. Recently, on the basis of the structure of the ternary complex among SOCS3, JAK2, and gp130, we focused on SOCS3 interfacing regions and designed several interfering peptides (IPs) that were able to mimic SOCS3 biological role in triple negative breast cancer (TNBC) models. Herein, to explore other protein regions involved in JAK2 recognition, several new chimeric peptides connecting noncontiguous SOCS3 regions and including a strongly aromatic fragment were investigated. Their ability to recognize the catalytic domain of JAK2 was evaluated through MST (microscale thermophoresis), and the most promising compound, named KIRCONG chim, exhibited a low micromolar value for dissociation constant. The conformational features of chimeric peptides were analyzed through circular dichroism and NMR spectroscopies, and their anti-inflammatory effects were assessed in cell cultures. Overall data suggest the importance of aromatic contribution in the recognition of JAK2 and that SOCS3 peptidomimetics could be endowed with a therapeutic potential in diseases with activated inflammatory cytokines.

Published

2020