Publications by authors named "Bailon E"

Article Synopsis
  • Increased angiogenesis in chronic lymphocytic leukemia (CLL) is linked to advanced disease, with CLL cells showing a pro-angiogenic gene expression pattern influenced by their environment.
  • MMP-9, a component of the microenvironment, was found to enhance MMP-9 expression and secretion in CLL cells, leading to increased endothelial cell proliferation.
  • MMP-9 also altered the expression of angiogenic-related genes, particularly decreasing TSP-1 and increasing VEGF, by involving specific molecular pathways, highlighting its role in CLL pathology.
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  • α4β1 integrin and VEGFR2 work together as a receptor complex that interacts with VEGF in chronic lymphocytic leukemia (CLL) cells.
  • This interaction suggests that α4β1 integrin has a new and significant role in the development of CLL.
  • The findings highlight how understanding these receptors could lead to better insights into CLL pathology and potential treatments.
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  • MMP-9 plays a significant role in the pathology of Chronic Lymphocytic Leukemia (CLL) by regulating cell survival, migration, and inducing cell arrest when expressed at high levels.
  • A study identified that MMP-9 alters the gene expression of specific genes in CLL cells, notably including CD99, which affects cell adhesion and migration.
  • The research highlights CD99 as a new therapeutic target that, when influenced by MMP-9, regulates CLL cell behavior and could lead to new treatment strategies.
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  • Researchers found that MMP-9, when overexpressed, hinders the movement of chronic lymphocytic leukemia (CLL) cells, leading to studies on a mutant form of MMP-9 that doesn't break down proteins (MMP-9MutE).
  • In mouse models, these MMP-9MutE cells showed reduced ability to migrate to key areas like the spleen and bone marrow compared to control cells.
  • The study identified changes in cellular signaling pathways; MMP-9MutE cells had higher levels of PTEN and lower p-ERK, indicating that non-proteolytic functions of MMP-9 are important in CLL cell migration and may affect disease progression.
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  • CLL is currently an incurable disease, but arsenic trioxide (ATO) shows promise as an effective therapy by inducing cell death in CLL cells.
  • ATO affects gene expression related to oxidative stress, notably increasing the levels of the gene HMOX1 and the protein MMP-9, which are involved in the response to treatment.
  • HMOX1 has a pro-apoptotic role that enhances the cytotoxic effects of ATO, making it a potential new therapeutic target when combined with ATO for CLL treatment.
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Degradation and remodeling of the extracellular matrix by matrix metalloproteinases (MMPs) plays important roles in normal development, inflammation, and cancer. MMP-9 efficiently degrades the extracellular matrix component gelatin, and the hemopexin domain of MMP-9 (PEX9) inhibits this degradation. To study the molecular basis of this inhibition, we generated GST fusion proteins containing PEX9 or truncated forms corresponding to specific structural blades (B1-B4) of PEX9.

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Article Synopsis
  • CLL (Chronic Lymphocytic Leukemia) remains incurable despite new treatments; arsenic trioxide (ATO) shows promise in killing CLL cells but resistance occurs in the presence of bone marrow stromal cells.
  • Stromal cells enhance the resistance of CLL cells to ATO through the activation of specific signaling pathways (Lyn, ERK, PI3K, PKC, NF-κB, and STAT3) and upregulation of proteins like Mcl-1, Bcl-xL, and Bfl-1.
  • Targeting the pathways with inhibitors like idelalisib and sotrastaurin can disrupt the resistance, making CLL cells more sensitive to ATO,
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This study addresses the role of (pro)MMP-9 overexpression in CLL cell migration. We have used primary CLL cells and CLL-derived MEC-1 cells transfected with empty (mock cells) or proMMP-9-encoding (MMP-9 cells) lentiviral vectors. The constitutive (pro)MMP-9 expression in mock cells and primary CLL cells was similar, whereas in MMP-9 cells, expression resembled that of CLL cells incubated with proMMP-9.

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Article Synopsis
  • MMP-9 plays a role in chronic lymphocytic leukemia (CLL) by regulating cell movement and inhibiting apoptosis, and this study investigates its effect on CLL's response to chemotherapy drugs like arsenic trioxide (ATO) and fludarabine.
  • CLL cells showed an increase in MMP-9 in response to these drugs before they began to undergo apoptosis, and inhibiting apoptosis with a specific agent blocked this increase, suggesting a connection between MMP-9 and the apoptotic process.
  • The presence of MMP-9 was linked to drug resistance in CLL cells; higher levels of anti-apoptotic proteins were found in cells with increased MMP-9, and using anti-MMP
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(pro)MMP-9 binds to CLL cells through the PEX9 domain and contributes to CLL progression. To biochemically characterize this interaction and identify potential therapeutic targets, we prepared GST-PEX9 forms containing structural blades B1B2 or B3B4. We recently described a sequence in blade B4 (P3 sequence) that bound α4β1 integrin and partially impaired cell adhesion and migration.

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This study addresses the role of (pro)MMP-9 overexpression in CLL cell migration. We have used primary CLL cells and CLL-derived MEC-1 cells transfected with empty (mock cells) or proMMP-9-encoding (MMP-9 cells) lentiviral vectors. The constitutive (pro)MMP-9 expression in mock cells and primary CLL cells was similar, whereas in MMP-9 cells, expression resembled that of CLL cells incubated with proMMP-9.

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Background: Previous studies have indicated that colitis increases intestinal permeability to food antigens. This condition also generates an immunoreactive milieu in the gut, which may exacerbate or counteract allergy reactions. This, along with the fact that both colitis and allergy are being codiagnosed more frequently, means the scientific interest on the immune relation between these pathologies is increasing.

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We previously showed that pro-matrix metalloproteinase-9 (proMMP-9) binds to B chronic lymphocytic leukemia (B-CLL) cells and contributes to B-CLL progression by regulating cell migration and survival. Induction of cell survival involves a non-proteolytic mechanism and the proMMP-9 hemopexin domain (PEX9). To help design specific inhibitors of proMMP-9-cell binding, we have now characterized B-CLL cell interaction with the isolated PEX9.

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Myeloma cell adhesion dependent on α4β1 integrin is crucial for the progression of multiple myeloma (MM). The α4β1-dependent myeloma cell adhesion is up-regulated by the chemokine CXCL12, and pharmacological blockade of the CXCL12 receptor CXCR4 leads to defective myeloma cell homing to bone marrow (BM). Sphingosine-1-phosphate (S1P) regulates immune cell trafficking upon binding to G-protein-coupled receptors.

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Cow's milk protein allergy (CMPA) is one of the most prevalent human food-borne allergies, particularly in children. Experimental animal models have become critical tools with which to perform research on new therapeutic approaches and on the molecular mechanisms involved. However, oral food allergen sensitization in mice requires several weeks and is usually associated with unspecific immune responses.

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Nosema ceranae has been suggested to be replacing Nosema apis in some populations of Apis mellifera honeybees. However, this replacement from one to the other is not supported when studying the distribution and prevalence of both microsporidia in professional apiaries in Spanish territories (transverse study), their seasonal pattern in experimental hives with co-infection or their prevalence at individual level (either in worker bees or drones). Nevertheless, N.

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The present study analysed the effects of the flavanol (-)-epicatechin in rats after chronic inhibition of NO synthesis with NG-nitro-L-arginine methyl ester (L-NAME), at doses equivalent to those achieved in the studies involving human subjects. Wistar rats were randomly divided into four groups: (1) control-vehicle, (2) L-NAME, (3) L-NAME-epicatechin 2 (L-NAME-Epi 2) and (4) L-NAME-epicatechin 10 (L-NAME-Epi 10). Rats were daily given by oral administration for 4 weeks: vehicle, (-)-epicatechin 2 or 10 mg/kg.

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Background: The dinitrofluorobenzene/dinitrosulfonic acid (DNFB/DNS) model was originally described as an experimental model of intestinal inflammation resembling human ulcerative colitis (UC). Due to the absence of acceptable UC experimental models for pharmacological preclinical assays, here we examine the immune response induced in this model.

Methods: Balb/c mice were sensitized by skin application of DNFB on day 1, followed by an intrarectal challenge with DNS on day 5.

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Activation of nuclear hormone receptor peroxisome proliferator-activated receptor β/δ (PPARβ) has been shown to improve insulin resistance and plasma high-density lipoprotein levels, but nothing is known about its effects in genetic hypertension. We studied whether the PPARβ agonist GW0742 might exert antihypertensive effects in spontaneously hypertensive rats (SHRs). The rats were divided into 4 groups, Wistar Kyoto rat-control, Wistar Kyoto rat-treated (GW0742, 5 mg · kg(-1) · day(-1) by oral gavage), SHR-control, and SHR-treated, and followed for 5 weeks.

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Background And Purpose: Dersalazine sodium (DS) is a new chemical entity formed by combining, through an azo bond, a potent platelet activating factor (PAF) antagonist (UR-12715) with 5-aminosalicylic acid (5-ASA). DS has been demonstrated to have anti-inflammatory effects on trinitrobenzene sulphonic acid (TNBS)-induced colitis in rats and recently in UC patients in phase II PoC. There is Increasing evidence that Th17 cells have an important role in the pathogenesis of inflammatory bowel disease (IBD).

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Purpose: The aim of this study was to better characterise the biological effects of Lactobacillus salivarius ssp. salivarius CECT5713, a probiotic with immunomodulatory properties.

Methods: Live or dead probiotic was assayed in the TNBS model of rat colitis to determine whether viability was a requisite to exert the beneficial effects.

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Some antibiotics, including minocycline, have recently been reported to display immunomodulatory properties in addition to their antimicrobial activity. The use of a compound with both immunomodulatory and antibacterial properties could be very interesting in the treatment of inflammatory bowel disease (IBD), so the aim of our study was to evaluate the anti-inflammatory effect of minocycline in several experimental models of IBD. Firstly, the immunomodulatory activity of the antibiotic was tested in vitro using Caco-2 intestinal epithelial cells and RAW 264.

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Different types of dietary fiber can be distinguished considering their rate of fermentability, thus determining the location of the large intestine where they exert their beneficial effect. Their combination could be interesting to obtain health-promoting effects throughout the entire colon. The aim of the present study was to evaluate the synergistic effect of two dietary fibers with different fermentation patterns, fructooligosaccharides (FOS) (Beneo(®)-95) and resistant starch (Fibersol(®)-2), after their administration to healthy rats or in trinitrobenzenesulphonic acid-(TNBS) colitic rats, with an altered colonic immune response.

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In the present study we describe the preparation and chemical characterization of a caramel with a high (70%) content of difructose dianhydrides (DFAs) and glycosylated derivatives (DFAs). This product was obtained by thermal activation (90 degrees C) of highly concentrated (90% w/v) aqueous D-fructose solutions using the sulfonic acid ion-exchange resin Lewatit S2328 as caramelization catalyst. DFAs represent a unique family of cyclic fructans with prebiotic properties already present in low proportions (<15%) in commercial caramel.

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