Your search keyword '"Mannose-Binding Lectins"' showing total 419 results

1. From Organotypic Mouse Brain Slices to Human Alzheimer Plasma Biomarkers: A Focus on Microglia.

Author

Steiner, Katharina, Yilmaz, Sakir Necat, Gern, Alessa, Marksteiner, Josef, Faserl, Klaus, Villunger, Mathias, Sarg, Bettina, and Humpel, Christian

Subjects

ALZHEIMER'S disease, ALZHEIMER'S patients, MANNOSE-binding lectins, PROTEIN C, PLASMA focus

Abstract

Alzheimer's disease is a severe neurodegenerative disorder, and the discovery of biomarkers is crucial for early diagnosis. While the analysis of biomarkers in cerebrospinal fluid is well accepted, there are currently no blood biomarkers available. Our research focuses on identifying novel plasma biomarkers for Alzheimer's disease. To achieve this, we employed a technique that involves coupling human plasma to mouse organotypic brain slices via microcontact prints. After culturing for two weeks, we assessed Iba1-immunopositive microglia on these microcontact prints. We hypothesized that plasma from Alzheimer's patients contains factors that affect microglial migration. Our data indicated that plasma from Alzheimer's patients significantly inhibited the migration of round Iba1-immunoreactive microglia (13 ± 3, n = 24, p = 0.01) compared to healthy controls (50 ± 16, n = 23). Based on these findings, we selected the most promising plasma samples and conducted mass spectrometry using a differential approach, and we identified four potential biomarkers: mannose-binding protein C, macrophage receptor MARCO, complement factor H-related protein-3, and C-reactive protein. Our method represents a novel and innovative approach to translate research findings from mouse models to human applications. [ABSTRACT FROM AUTHOR]

Published

2024

2. Characterization of novel extracellular proteases produced by Acanthamoeba castellanii after contact with human corneal epithelial cells and their relevance to pathogenesis.

Author

Loufouma-Mbouaka, Alvie, Martín-Pérez, Tania, Köhsler, Martina, Danisman, Zeynep, Schwarz, Maya, Mazumdar, Rounik, Samba-Louaka, Ascel, and Walochnik, Julia

Subjects

ACANTHAMOEBA castellanii, EPITHELIAL cells, MANNOSE-binding lectins, MATRIX metalloproteinases, SERINE proteinases, PROTEOLYTIC enzymes

Abstract

Background: Proteases produced by Acanthamoeba spp. play an important role in their virulence and may be the key to understanding Acanthamoeba pathogenesis; thus, increasing attention has been directed towards these proteins. The present study aimed to investigate the lytic factors produced by Acanthamoeba castellanii during the first hours of in vitro co-culture with human corneal epithelial cells (HCECs). Methods: We used one old and one recent Acanthamoeba isolate, both from patients with severe keratitis, and subsets of these strains with enhanced pathogenic potential induced by sequential passaging over HCEC monolayers. The proteolytic profiles of all strains and substrains were examined using 1D in-gel zymography. Results: We observed the activity of additional proteases (ranging from 33 to 50 kDa) during the early interaction phase between amoebae and HCECs, which were only expressed for a short time. Based on their susceptibilities to protease inhibitors, these proteases were characterized as serine proteases. Protease activities showed a sharp decline after 4 h of co-incubation. Interestingly, the expression of Acanthamoeba mannose-binding protein did not differ between amoebae in monoculture and those in co-culture. Moreover, we observed the activation of matrix metalloproteinases in HCECs after contact with Acanthamoeba. Conclusions: This study revealed the involvement of two novel serine proteases in Acanthamoeba pathogenesis and suggests a pivotal role of serine proteases during Acanthamoeba-host cell interaction, contributing to cell adhesion and lysis. [ABSTRACT FROM AUTHOR]

Published

2024

3. Discovering the Radiation Biomarkers in the Plasma of Total-Body Irradiated Leukemia Patients.

Author

Gabriela, Rydlova, Vera, Vozandychova, Pavel, Rehulka, Helena, Rehulkova, Igor, Sirak, Marie, Davidkova, Marketa, Markova, Alena, Myslivcova-Fucikova, and Ales, Tichy

Subjects

TOTAL body irradiation, PLASMA radiation, PROTEOMICS, COMPLEMENT (Immunology), BLOOD proteins, MANNOSE-binding lectins

Abstract

The increased risk of acute large-scale radiological exposure for the world's population underlines the need for optimal radiation biomarkers. Ionizing radiation triggers a complex response by the genome, proteome, and metabolome, all of which have been reported as suitable indicators of radiation-induced damage in vivo. This study analyzed peripheral blood samples from total-body irradiation (TBI) leukemia patients through mass spectrometry (MS) to identify and quantify differentially regulated proteins in plasma before and after irradiation. In brief, samples were taken from 16 leukemic patients prior to and 24 h after TBI (2 × 2.0 Gy), processed with Tandem Mass Tag isobaric labelling kit (TMTpro-16-plex), and analyzed by MS. In parallel, label-free relative quantification was performed with a RP-nanoLC-ESI-MS/MS system in a Q-Exactive mass spectrometer. Protein identification was done in Proteome Discoverer v.2.2 platform (Thermo). Data is available via ProteomeXchange with identifier PXD043516. Using two different methods, we acquired two datasets of up-regulated (ratio ≥ 1.2) or down-regulated (ratio ≤ 0.83) plasmatic proteins 24 h after irradiation, identifying 356 and 346 proteins in the TMT-16plex and 285 and 308 label-free analyses, respectively (P ≤ 0.05). Combining the two datasets yielded 15 candidates with significant relation to gamma-radiation exposure. The majority of these proteins were associated with the inflammatory response and lipid metabolism. Subsequently, from these, five proteins showed the strongest potential as radiation biomarkers in humans (C-reactive protein, Alpha amylase 1A, Mannose-binding protein C, Phospholipid transfer protein, and Complement C5). These candidate biomarkers might have implications for practical biological dosimetry. [ABSTRACT FROM AUTHOR]

Published

2024

4. Complement MASP-1 Modifies Endothelial Wound Healing.

Author

Németh, Zsuzsanna, Demeter, Flóra, Dobó, József, Gál, Péter, and Cervenak, László

Subjects

MANNOSE-binding lectins, WOUND healing, CARDIOVASCULAR system, ENDOTHELIAL cells

Abstract

Endothelial wound-healing processes are fundamental for the maintenance and restoration of the circulatory system and are greatly affected by the factors present in the blood. We have previously shown that the complement protein mannan-binding lectin-associated serine protease-1 (MASP-1) induces the proinflammatory activation of endothelial cells and is able to cooperate with other proinflammatory activators. Our aim was to investigate the combined effect of mechanical wounding and MASP-1 on endothelial cells. Transcriptomic analysis showed that MASP-1 alters the expression of wound-healing-related and angiogenesis-related genes. Both wounding and MASP-1 induced Ca2+ mobilization when applied individually. However, MASP-1-induced Ca2+ mobilization was inhibited when the treatment was preceded by wounding. Mechanical wounding promoted CREB phosphorylation, and the presence of MASP-1 enhanced this effect. Wounding induced ICAM-1 and VCAM-1 expression on endothelial cells, and MASP-1 pretreatment further increased VCAM-1 levels. MASP-1 played a role in the subsequent stages of angiogenesis, facilitating the breakdown of the endothelial capillary network on Matrigel®. Our findings extend our general understanding of endothelial wound healing and highlight the importance of complement MASP-1 activation in wound-healing processes. [ABSTRACT FROM AUTHOR]

Published

2024

5. Plasma levels of mannan-binding lectin-associated serine proteases are increased in type 1 diabetes patients with insulin resistance.

Author

Kietsiriroje, Noppadol, Scott, Georgia E, Ajjan, Ramzi A, Brôz, Jan, Schroeder, Verena, and Campbell, Matthew D

Subjects

TYPE 1 diabetes, SERINE proteinases, INSULIN resistance, PEOPLE with diabetes, MANNOSE-binding lectins, GALACTOMANNANS, ECULIZUMAB

Abstract

Activation of the lectin pathway of the complement system, as demonstrated by elevated levels of mannan-binding lectin proteins (MBL), contributes to vascular pathology in type 1 diabetes (T1D). Vascular complications are greatest in T1D individuals with concomitant insulin resistance (IR), however, whether IR amplifies activiation of the lectin pathway in T1D is unknown. We pooled pretreatment data from two RCTs and performed a cross-sectional analysis on 46 T1D individuals. We employed estimated glucose disposal rate (eGDR), a validated IR surrogate with cut-points of: <5.1, 5.1–8.7, and > 8.7 mg/kg/min to determine IR status, with lower eGDR values conferring higher degrees of IR. Plasma levels of MBL-associated proteases (MASP-1, MASP-2, and MASP-3) and their regulatory protein MAp44 were compared among eGDR classifications. In a subset of 14 individuals, we assessed change in MASPs and MAp44 following improvement in IR. We found that MASP-1, MASP-2, MASP-3, and MAp44 levels increased in a stepwise fashion across eGDR thresholds with elevated MASPs and MAp44 levels conferring greater degrees of IR. In a subset of 14 patients, improvement in IR was associated with significant reductions in MASPs, but not MAp44, levels. In conclusion, IR in T1D amplifies levels of MASP-1/2/3 and their regulator MAp44, and improvement of IR normalizes MASP-1/2/3 levels. Given that elevated levels of these proteins contribute to vascular pathology, amplification of the lectin pathway of the complement system may offer mechanistic insight into the relationship between IR and vascular complications in T1D. Plasma levels of mannan-binding lectin-associated serine proteases are increased in type 1 diabetes patients with insulin resistance. Graphical Abstract [ABSTRACT FROM AUTHOR]

Published

2024

6. The mannose‐binding protein from Agaricus bisporus inhibits the growth of MDA‐MB‐231 spheroids.

Author

Azzahra, Fauzia, Amalia, Riezki, Karsono, Agung Heru, Tjandrawinata, Raymond Rubianto, Ismaya, Wangsa Tirta, and Rachmawati, Heni

Subjects

MANNOSE-binding lectins, CULTIVATED mushroom, WNT signal transduction, CELL morphology, CELL proliferation, CELL growth

Abstract

A mannose‐binding protein from the mushroom Agaricus bisporus (Abmb) inhibits the growth of MDA‐MB‐231 cells, which is of an aggressive breast cancer subtype. This ability was observed in a monolayer cell (2D) culture setup, which often is unable to capture changes in cell morphology, polarity and division. That shortcoming may overestimate Abmb potency for its development as a pharmaceutical agent and its use in a therapy. Hence, Abmb's inhibition to the cell growth was performed in the 3D cell (spheroid) culture, which is more representative to the situation in vivo. The result showed that, although the presence of Abmb at ~14.7 μM already disrupted the MDA‐MB‐231 cell morphology in the 2D culture, its presence at ~16.5 μM only ceased the growth of the MDA‐MB‐231 spheroid. Further, Abmb is unique because structurally it belongs to the R‐type lectin (RTL) family; most of mannose‐binding protein is of the C‐type lectin (CTL). As the natural ligand of Abmb is unknown thus the mechanism of action is unclear, Abmb effect on the cancer cells was assessed via observation of the altered expression of genes involved in the Wnt/β‐catenin signalling, which is one of the canonical pathways in the proliferation of cancer cells. The results suggested that Abmb did not alter the pathway upon exerting its anti‐proliferative activity to the MDA‐MB‐231 cells. [ABSTRACT FROM AUTHOR]

Published

2024

7. Mannose-Binding Lectins as Potent Antivirals against SARS-CoV-2.

Author

Grosche, Victória Riquena, Souza, Leandro Peixoto Ferreira, Ferreira, Giulia Magalhães, Guevara-Vega, Marco, Carvalho, Tamara, Silva, Romério Rodrigues dos Santos, Batista, Karla Lilian Rodrigues, Abuna, Rodrigo Paolo Flores, Silva, João Santana, Calmon, Marília de Freitas, Rahal, Paula, da Silva, Luis Cláudio Nascimento, Andrade, Bruno Silva, Teixeira, Claudener Souza, Sabino-Silva, Robinson, and Jardim, Ana Carolina Gomes

Subjects

MANNOSE-binding lectins, PLANT lectins, SARS-CoV-2, CELL receptors, SARS-CoV-2 Omicron variant, LECTINS, VIRUS diseases

Abstract

The SARS-CoV-2 entry into host cells is mainly mediated by the interactions between the viral spike protein (S) and the ACE-2 cell receptor, which are highly glycosylated. Therefore, carbohydrate binding agents may represent potential candidates to abrogate virus infection. Here, we evaluated the in vitro anti-SARS-CoV-2 activity of two mannose-binding lectins isolated from the Brazilian plants Canavalia brasiliensis and Dioclea violacea (ConBR and DVL). These lectins inhibited SARS-CoV-2 Wuhan-Hu-1 strain and variants Gamma and Omicron infections, with selectivity indexes (SI) of 7, 1.7, and 6.5, respectively for ConBR; and 25, 16.8, and 22.3, for DVL. ConBR and DVL inhibited over 95% of the early stages of the viral infection, with strong virucidal effect, and also protected cells from infection and presented post-entry inhibition. The presence of mannose resulted in the complete lack of anti-SARS-CoV-2 activity by ConBR and DVL, recovering virus titers. ATR-FTIR, molecular docking, and dynamic simulation between SARS-CoV-2 S and either lectins indicated molecular interactions with predicted binding energies of −85.4 and −72.0 Kcal/Mol, respectively. Our findings show that ConBR and DVL lectins possess strong activities against SARS-CoV-2, potentially by interacting with glycans and blocking virus entry into cells, representing potential candidates for the development of novel antiviral drugs. [ABSTRACT FROM AUTHOR]

Published

2023

8. Sublethal Exposure to Plasma-Activated Water Influences the Morphological Characteristics, Phagocytic Ability, and Virulence of Acanthamoeba castellanii.

Author

Bahrami, Somayeh, Darvishi, Mojtaba, Zarei, Mehdi, Sabaeian, Mohammad, and Henriquez, Fiona L.

Subjects

ACANTHAMOEBA castellanii, DISULFIDES, OXIDANT status, MANNOSE-binding lectins, SUPEROXIDE dismutase, TROPHOZOITES

Abstract

Purpose: This study aimed to examine the ultrastructure, cytotoxicity, phagocytosis, and antioxidant responses of Acanthamoeba castellanii trophozoites exposed to sublethal plasma-activated water. Methods: Trophozoites were exposed to a sublethal treatment of PAW and compared to untreated viable trophozoites via adhesion assays on macrophage monolayers, osmo- and thermotolerance tests. Bacterial uptake was assessed in treated cells to evaluate their phagocytic characteristics. Oxidative stress biomarkers and antioxidant activities were compared in treated and untreated trophozoites. Finally, the expression of the mannose-binding protein (MBP), cysteine protease 3 (CP3), and serine endopeptidase (SEP) genes was determined in cells. Results: In PAW-treated trophozoites, cytopathic effects were more extensive and resulted in the detachment of macrophage monolayers. Treated trophozoites could not grow at high temperatures (43 °C). Moreover, they showed osmotolerance to 0.5 M d-mannitol but not to 1 M. Results demonstrated a higher bacterial uptake rate by PAW-treated trophozoites than untreated cells. Activities of superoxide dismutase and catalase and catalase were significantly greater in the treated trophozoites, and the glutathione and glutathione/glutathione disulfide were significantly lower in the PAW-treated cells. Exposure to PAW also significantly increased the malondialdehyde level and total antioxidant capacity. Treatment with PAW led to significantly higher expression of virulent genes like MBP, CP3, and SEP. Conclusion: PAW is a double-edged sword against A. castellanii. PAW is an effective antiamoebic agent in proper usage, whereas its sublethal exposure may reduce its effectiveness and increase amoebas' pathogenicity. An agent's adequate concentration and exposure time are essential to achieve optimum results. [ABSTRACT FROM AUTHOR]

Published

2023

9. Complement Dysregulation in Obese Versus Nonobese Polycystic Ovary Syndrome Patients.

Author

Butler, Alexandra E., Moin, Abu Saleh Md, Sathyapalan, Thozhukat, and Atkin, Stephen L.

Subjects

POLYCYSTIC ovary syndrome, COMPLEMENT (Immunology), CD55 antigen, MANNOSE-binding lectins, B cells, INDUCED ovulation, INSULIN, OBESITY

Abstract

Introduction: Upregulation of complement system factors are reported to be increased in polycystic ovary syndrome (PCOS) and may be due to obesity and insulin resistance rather than inherently due to PCOS. We directly compared complement factors from an obese, insulin-resistant PCOS population to a nonobese, non-insulin-resistant PCOS population in a proteomic analysis to investigate this. Methods: Plasma was collected from 234 women (137 with PCOS and 97 controls) from a biobank cohort and compared to a nonobese, non-insulin-resistant population (24 with PCOS and 24 controls). Slow off-rate modified aptamer (SOMA) scan plasma protein measurement was undertaken for the following complement system proteins: C1q, C1r, C2, C3, C3a, iC3b, C3b, C3d, C3adesArg, C4, C4a, C4b, C5, C5a, C5b-6 complex, C8, properdin, factor B, factor D, factor H, factor I, Mannose-binding protein C (MBL), complement decay-accelerating factor (DAF) and complement factor H-related protein 5 (CFHR5). Results: The alternative pathway of the complement system was overexpressed in both obese and nonobese PCOS, with increased C3 (p < 0.05) and properdin (p < 0.01); additionally, factor B increased in obese PCOS (p < 0.01). For inhibitors of this pathway, factor I was increased (p < 0.01) in both slim and obese PCOS, with an increase in CFHR5 and factor H in obese PCOS (p < 0.01). Complement factors iC3b, C3d and C5a, associated with an enhanced B cell response and inflammatory cytokine release, were increased in both slim and obese PCOS (p < 0.05). C3a and its product, C3adesArg, were both significantly elevated in nonobese PCOS (<0.01) but not altered in obese PCOS. Hyperandrogenemia correlated positively with properdin and iC3b in obese PCOS (p < 0.05) but not in nonobese PCOS. There was no association with insulin resistance. BMI correlated positively in both groups with factor B, factor H and C5a. Additionally, in obese PCOS, BMI correlated with C3d, factor D, factor I, CFHR5 and C5a (p < 0.05), and in nonobese PCOS, BMI correlated with properdin, iC3b, C3, C3adesArg, C3a, C4, C5, C5a and C1q. In obese controls, BMI correlated with C3, C3desArg, C3a, C3d, C4, factor I, factor B, C5a and C5, whilst in nonobese controls, BMI only correlated negatively with C1q. Comparison of nonobese and obese PCOS showed that properdin, C3b, iC3b, C4A, factor D, factor H and MBL differed. Conclusion: The upregulation of the alternative complement pathway was seen in nonobese PCOS and was further exacerbated in obese PCOS, indicating that this is an inherent feature of the pathophysiology of PCOS that is worsened by obesity and is reflected in the differences between the nonobese and obese PCOS phenotypes. However, the increase in the complement proteins associated with activation was counterbalanced by upregulation of complement inhibitors; this was evident in both PCOS groups, suggesting that insults, such as a cardiovascular event or infection, that cause activation of complement pathways may be amplified in PCOS. [ABSTRACT FROM AUTHOR]

Published

2023

10. Cooperation of Complement MASP-1 with Other Proinflammatory Factors to Enhance the Activation of Endothelial Cells.

Author

Németh, Zsuzsanna, Debreczeni, Márta L., Kajdácsi, Erika, Dobó, József, Gál, Péter, and Cervenak, László

Subjects

ENDOTHELIAL cells, HISTAMINE receptors, MANNOSE-binding lectins, BRADYKININ receptors, GENE expression, BRADYKININ

Abstract

Endothelial cells play an important role in sensing danger signals and regulating inflammation. Several factors are capable of inducing a proinflammatory response (e.g., LPS, histamine, IFNγ, and bradykinin), and these factors act simultaneously during the natural course of the inflammatory reaction. We have previously shown that the complement protein mannan-binding lectin-associated serine protease-1 (MASP-1) also induces a proinflammatory activation of the endothelial cells. Our aim was to investigate the possible cooperation between MASP-1 and other proinflammatory mediators when they are present in low doses. We used HUVECs and measured Ca2+ mobilization, IL-8, E-selectin, VCAM-1 expression, endothelial permeability, and mRNA levels of specific receptors. LPS pretreatment increased the expression of PAR2, a MASP-1 receptor, and furthermore, MASP-1 and LPS enhanced each other's effects in regulating IL-8, E-selectin, Ca2+ mobilization, and changes in permeability in a variety of ways. Cotreatment of MASP-1 and IFNγ increased the IL-8 expression of HUVECs. MASP-1 induced bradykinin and histamine receptor expression, and consequently, increased Ca2+ mobilization was found. Pretreatment with IFNγ enhanced MASP-1-induced Ca2+ mobilization. Our findings highlight that well-known proinflammatory mediators and MASP-1, even at low effective doses, can strongly synergize to enhance the inflammatory response of endothelial cells. [ABSTRACT FROM AUTHOR]

Published

2023

11. Exposure to sublethal concentrations of chlorine enhances the cytotoxicity of Acanthamoeba castellanii.

Author

Bahrami, Somayeh, Asadi, Zeinab, Zarei, Mehdi, Hamidinejat, Hossein, and Henriquez, Fiona L.

Subjects

ACANTHAMOEBA castellanii, OXIDANT status, MANNOSE-binding lectins, CHLORINE, GENE expression

Abstract

Free-living amoebae belonging to the genus Acanthamoeba are the causative agents of infections in humans and animals. Many studies are being conducted to find effective compounds against amoebae, but their sublethal concentration effects on surviving amoebae seem to have been overlooked. Chlorine is a common disinfection agent commonly added to public water facilities and supplies. In this study, the cytopathic and phagocytic properties of Acanthamoeba castellanii trophozoites following exposure to sublethal concentrations of chlorine were examined. Two hours of exposure to 5 ppm hypochlorite calcium was considered the sublethal concentration for A. castellanii trophozoites. To compare the pathogenic potential of treated and untreated Acanthamoeba trophozoites, cytotoxicity, adhesion assays in RAW 264.7 macrophages, osmo, and thermotolerance tests were carried out. Bacterial uptake was assessed in treated cells to evaluate their phagocytic characteristics. Oxidative stress biomarkers and antioxidant activities were compared in treated and untreated trophozoites. Finally, the mRNA expression of the mannose-binding protein (MBP), cysteine protease 3 (CP3), and serine endopeptidase (SEP) genes was determined in cells. In all the experiments, untreated trophozoites were considered the control. In comparison to untreated trophozoites, in chlorine-treated trophozoites, cytopathic effects were more extensive and resulted in the detachment of macrophage monolayers. Treated trophozoites could not grow at high temperatures (43 °C). Besides, they showed osmotolerance to 0.5 M D-mannitol but not to 1 M. Results demonstrated a higher bacterial uptake rate by chlorine-treated trophozoites than untreated cells. The treated and untreated cells had significantly different glutathione and glutathione/glutathione disulfide ratios. Antioxidant enzyme activities, total antioxidant capacity, and malondialdehyde levels were increased significantly in chlorine-treated cells. Quantifying mRNA expression in chlorine-treated trophozoites revealed that virulence genes were upregulated. Chlorine can form resistance and virulent amoebae if it is not used at a proper concentration and exposure time. Identification of stress responses, their mechanisms in Acanthamoeba, and their relation to amoeba virulence would give us a better perception of their pathophysiology. [ABSTRACT FROM AUTHOR]

Published

2023

12. Mannose-binding lectin (MBL) levels in children with Hashimoto's thyroiditis.

Author

Gul, Ali, Hatipoglu, Nihal, Yilmaz, Resul, and Ates, Haci Omer

Subjects

AUTOIMMUNE thyroiditis, MANNOSE-binding lectins, ETIOLOGY of diseases, OUTPATIENT medical care, HYPOTHYROIDISM, CHILD patients

Abstract

OBJECTIVE: Hashimoto's thyroiditis (HT) was described many years ago, but the etiopathogenesis remains unclear. Mannose-binding lectin (MBL) initiates complement activation in the lectin pathway. We determined MBL levels in children with HT and the associations thereof with thyroid hormone and thyroid autoantibody levels. METHODS: Thirty-nine patients with HT and 41 controls were enrolled from the pediatric outpatient clinics. Subjects were grouped according to their thyroid functions: Euthyroid, marked hypothyroidism and clinical/subclinical hyperthyroidism. MBL levels were compared among these groups. Serum MBL levels of the subjects were determined using MBL Human ELISA kit. RESULTS: Serum MBL levels were studied in serum samples from the 80 subjects (48 (60.0%) females). MBL levels in HT and control groups were 50.787±34.718 and 50.593±44.28 ng/ml (p=0,983), respectively. In HT group, there was no significant difference in MBL levels between thyroid function groups (p=0.869). In addition, gender was not detected as a factor for serum MBL levels. Also we found negative correlation between WBC and serum MBL levels (r=-0.532; p=0.050). Otherwise there was no correlation between TSH, anti-TPO and anti-TG with serum MBL levels. CONCLUSION: MBL levels did not decrease in HT patients. Further research is needed to elucidate more fully any role for MBL in the development of autoimmune thyroid disease. [ABSTRACT FROM AUTHOR]

Published

2023

13. Acanthamoeba Mannose and Laminin Binding Proteins Variation across Species and Genotypes.

Author

Corsaro, Daniele

Subjects

CARRIER proteins, MEMBRANE glycoproteins, ACANTHAMOEBA, MANNOSE-binding lectins, MANNOSE, LECTINS

Abstract

Acanthamoeba is a ubiquitous free-living amoeba capable of being an opportunistic pathogen in humans and animals. A critical step in infection is the adhesion of the amoeba to host cells and tissues, and two major parasite adhesins, mannose-binding protein (MBP) and laminin-binding protein (LBP), are known to recognize the cell surface glycoproteins and those of the extracellular matrix, respectively. In this study, the available genomes of Acanthamoeba were analysed to recover the sequences of MBP and LBP using previously published genetic data. Genes for both proteins were successfully obtained from strains belonging to various genotypes (T4A, T4D, T4G, T4F, T2, T5, T10, T22, T7 and T18), resulting in a single gene for LBP but identifying two types of MBP, MBP1 and MBP2. Phylogenetic analysis based on deduced amino acid sequences shows that both MBP and LBP have a branching pattern that is consistent with that based on 18S rDNA, indicating that changes in both proteins occurred during diversification of Acanthamoeba lines. Notably, all MBPs possess a conserved motif, shared with some bacterial C-type lectins, which could be the recognition site for mannose binding. [ABSTRACT FROM AUTHOR]

Published

2022

14. Applications of mannose-binding lectins and mannan glycoconjugates in nanomedicine.

Author

Gupta, Anita and Gupta, G. S.

Subjects

MANNOSE-binding lectins, NANOMEDICINE, PLANT lectins, GALACTOMANNANS, TARGETED drug delivery, GLYCOCONJUGATES, DRUG delivery systems, CELL receptors

Abstract

Glycosylated nanoparticles (NPs) have drawn a lot of attention in the biomedical field over the past few decades, particularly in applications like targeted drug delivery. Mannosylated NPs and mannan-binding lectins/proteins (MBL/MBP) are emerging as promising tools for delivery of drugs, medicines, and enzymes to targeted tissues and cells as nanocarriers, enhancing their therapeutic benefits while avoiding the adverse effects of the drug. The occurrence of plenty of lectin receptors and their mannan ligands on cell surfaces makes them multifaceted carriers appropriate for specific delivery of bioactive drug materials to their targeted sites. Thus, the present review describes the tethering of mannose (Man) to several nanostructures, like micelles, liposomes, and other NPs, applicable for drug delivery systems. Bioadhesion through MBL-like receptors on cells has involvements applicable to additional arenas of science, for example gene delivery, tissue engineering, biomaterials, and nanotechnology. This review also focuses on the role of various aspects of drug/antigen delivery using (i) mannosylated NPs, (ii) mannosylated lectins, (iii) amphiphilic glycopolymer NPs, and (iv) natural mannan-containing polysaccharides, with most significant applications of MBL-based NPs as multivalent scaffolds, using different strategies. Mannosylated NPs and/or MBL/MBP are coming up as viable and versatile tools as nanocarriers to deliver drugs and enzymes precisely to their target tissues or cells. The presence of abundant number of lectin receptors and their mannan ligands on cell surfaces makes them versatile carriers suitable for the targeted delivery of bioactive drugs. [ABSTRACT FROM AUTHOR]

Published

2022

15. Acanthamoeba Mannose and Laminin Binding Proteins Variation across Species and Genotypes.

Author

Corsaro, Daniele

Subjects

CARRIER proteins, MEMBRANE glycoproteins, ACANTHAMOEBA, MANNOSE-binding lectins, MANNOSE, LECTINS

Abstract

Acanthamoeba is a ubiquitous free-living amoeba capable of being an opportunistic pathogen in humans and animals. A critical step in infection is the adhesion of the amoeba to host cells and tissues, and two major parasite adhesins, mannose-binding protein (MBP) and laminin-binding protein (LBP), are known to recognize the cell surface glycoproteins and those of the extracellular matrix, respectively. In this study, the available genomes of Acanthamoeba were analysed to recover the sequences of MBP and LBP using previously published genetic data. Genes for both proteins were successfully obtained from strains belonging to various genotypes (T4A, T4D, T4G, T4F, T2, T5, T10, T22, T7 and T18), resulting in a single gene for LBP but identifying two types of MBP, MBP1 and MBP2. Phylogenetic analysis based on deduced amino acid sequences shows that both MBP and LBP have a branching pattern that is consistent with that based on 18S rDNA, indicating that changes in both proteins occurred during diversification of Acanthamoeba lines. Notably, all MBPs possess a conserved motif, shared with some bacterial C-type lectins, which could be the recognition site for mannose binding. [ABSTRACT FROM AUTHOR]

Published

2022

16. Components of the Complement Cascade Differ in Polycystic Ovary Syndrome.

Author

Butler, Alexandra E., Moin, Abu Saleh Md, Sathyapalan, Thozhukat, and Atkin, Stephen L.

Subjects

COMPLEMENT (Immunology), POLYCYSTIC ovary syndrome, COMPLEMENT activation, INDUCED ovulation, CD55 antigen, MANNOSE-binding lectins, COMPLEMENT receptors, TALL-1 (Protein)

Abstract

Complement pathway proteins are reported to be increased in polycystic ovary syndrome (PCOS) and may be affected by obesity and insulin resistance. To investigate this, a proteomic analysis of the complement system was undertaken, including inhibitory proteins. In this cohort study, plasma was collected from 234 women (137 with PCOS and 97 controls). SOMALogic proteomic analysis was undertaken for the following complement system proteins: C1q, C1r, C2, C3, C3a, iC3b, C3b, C3d, C3adesArg, C4, C4a, C4b, C5, C5a, C5b-6 complex, C8, properdin, factor B, factor D, factor H, factor I, mannose-binding protein C (MBL), complement decay-accelerating factor (DAF) and complement factor H-related protein 5 (CFHR5). The alternative pathway of the complement system was primarily overexpressed in PCOS, with increased C3 (p < 0.05), properdin and factor B (p < 0.01). In addition, inhibition of this pathway was also seen in PCOS, with an increase in CFHR5, factor H and factor I (p < 0.01). Downstream complement factors iC3b and C3d, associated with an enhanced B cell response, and C5a, associated with an inflammatory cytokine release, were increased (p < 0.01). Hyperandrogenemia correlated positively with properdin and iC3b, whilst insulin resistance (HOMA-IR) correlated with iC3b and factor H (p < 0.05) in PCOS. BMI correlated positively with C3d, factor B, factor D, factor I, CFHR5 and C5a (p < 0.05). This comprehensive evaluation of the complement system in PCOS revealed the upregulation of components of the complement system, which appears to be offset by the concurrent upregulation of its inhibitors, with these changes accounted for in part by BMI, hyperandrogenemia and insulin resistance. [ABSTRACT FROM AUTHOR]

Published

2022

17. Plasma level of mannose-binding lectin is associated with the risk of recurrent pregnancy loss but not pregnancy outcome after the diagnosis.

Author

Nørgaard-Pedersen, C, Rom, L H, Steffensen, R, Kesmodel, U S, and Christiansen, O B

Subjects

MANNOSE-binding lectins, BLOOD plasma, ABORTION

Abstract

STUDY QUESTION Are low or high plasma mannose-binding lectin (p-MBL) levels associated with recurrent pregnancy loss (RPL) and the reproductive and perinatal outcomes before and after RPL? SUMMARY ANSWER The prevalence of low p-MBL levels was significantly higher in RPL patients, while high levels were significantly less prevalent. No association was found between p-MBL level and reproductive and perinatal outcomes before and after RPL. WHAT IS KNOWN ALREADY Mannose-binding lectin (MBL) is an important component in the innate immune system. Low p-MBL levels have been associated with RPL, while the correlation with high levels has been poorly studied. Adverse perinatal outcomes are generally more frequent among RPL patients, but reports concerning the association between maternal p-MBL levels and perinatal outcomes, including birth weight (BW) and gestational age (GA), are conflicting. STUDY DESIGN, SIZE, DURATION This study was a combined cross-sectional and cohort study of 267 RPL patients admitted to the RPL Center of Western Denmark between January 2016 and March 2020. RPL patients were followed until birth of a liveborn child or until end of follow-up, March 2021. A sample of 185 healthy female blood donors of reproductive age was used as a MBL reference group. PARTICIPANTS/MATERIALS, SETTING, METHODS All RPL patients had ≥3 consecutive pregnancy losses, a regular menstrual cycle and no known significant chromosomal or uterine malformations. At the first consultation, routine blood samples including p-MBL measurement and detailed obstetrical and perinatal information were collected. p-MBL levels in RPL patients were compared to the MBL reference group. A logistic regression analysis adjusted for relevant confounders assessed the association between low p-MBL levels and an unsuccessful reproductive outcome in RPL patients in first pregnancy after admission. Perinatal outcomes before and after RPL were compared between RPL subgroups according to low (≤500 µg/l), intermediate (501–3000 µg/l) and high (>3000 µg/l) p-MBL levels. MAIN RESULTS AND THE ROLE OF CHANCE Significantly more RPL patients had low p-MBL levels (prevalence proportion ratio (PPR): 1.79, 95% CI: 1.34–2.38) and fewer had high p-MBL levels (PPR: 0.56, 95% CI: 0.40–0.79) compared to the reference group, while the prevalence of intermediate p-MBL level was not different between the groups (PPR: 0.86, 95% CI: 0.69–1.08). In the prospective study, low p-MBL level was not a significant risk factor for a pregnancy loss in the first pregnancy after admission after adjustment for age, BMI and smoking. Neither before nor after the RPL diagnosis were maternal p-MBL levels significantly associated with BW or GA. LIMITATIONS, REASONS FOR CAUTION Only 161 (60.3%) patients had given birth after RPL during the follow-up period, which limited the possibility to detect clear associations between p-MBL levels and perinatal outcomes after RPL. WIDER IMPLICATIONS OF THE FINDINGS In agreement with several previous studies, low p-MBL levels are strongly associated with RPL, while this study for the first time documents that high levels may play a protective role, which suggests a causal relationship. We suggest that larger prospective studies evaluate the association between p-MBL levels and RPL prognosis. STUDY FUNDING/COMPETING INTEREST(S) No external funding was received. We acknowledge the Department of Obstetrics and Gynaecology at Aalborg University Hospital for financial support. U.S.K. has reported personal fees from Merck, consulting fees from IBSA Nordic, and a grant from Gedeon Richter, Merck and IBSA Nordic outside of the submitted work. TRIAL REGISTRATION NUMBER ID from clinicaltrials.gov is NCT04017754. [ABSTRACT FROM AUTHOR]

Published

2022

18. Measurement of erythrocyte membrane mannoses to assess splenic function.

Author

Cao, Huan, Mathur, Abhinav, Robertson, Charlotte, Antonopoulos, Aristotelis, Henderson, Sadie, Girard, Louis‐Pierre, Wong, Jin Hien, Davie, Adam, Wright, Sonja, Brewin, John, Rees, David C., Dell, Anne, Haslam, Stuart M., and Vickers, Mark A.

Subjects

ERYTHROCYTE membranes, SPLENECTOMY, ERYTHROCYTES, MANNOSE-binding lectins, SICKLE cell anemia, CELL membranes, LECTINS, GLYCANS

Abstract

Summary: Red blood cells (RBCs) lose plasma membrane in the spleen as they age, but the cells and molecules involved are yet to be identified. Sickle cell disease and infection by Plasmodium falciparum cause oxidative stress that induces aggregates of cross‐linked proteins with N‐linked high‐mannose glycans (HMGs). These glycans can be recognised by mannose‐binding lectins, including the mannose receptor (CD206), expressed on macrophages and specialised phagocytic endothelial cells in the spleen to mediate the extravascular haemolysis characteristic of these diseases. We postulated this system might also mediate removal of molecules and membrane in healthy individuals. Surface expression of HMGs on RBCs from patients who had previously undergone splenectomy was therefore assessed: high levels were indeed observable as large membrane aggregates. Glycomic analysis by mass spectrometry identified a mixture of Man5‐9GlcNAc2 structures. HMG levels correlated well with manual pit counts (r = 0.75–0.85). To assess further whether HMGs might act as a splenic reticuloendothelial function test, we measured levels on RBCs from patients with potential functional hyposplenism, some of whom exhibited high levels that may indicate risk of complications. [ABSTRACT FROM AUTHOR]

Published

2022

19. Recognition of Cell Wall Mannosylated Components as a Conserved Feature for Fungal Entrance, Adaptation and Survival Within Trophozoites of Acanthamoeba castellanii and Murine Macrophages.

Author

Ferreira, Marina da Silva, Mendoza, Susana Ruiz, Gonçalves, Diego de Souza, Rodríguez-de la Noval, Claudia, Honorato, Leandro, Nimrichter, Leonardo, Ramos, Luís Felipe Costa, Nogueira, Fábio C. S., Domont, Gilberto B., Peralta, José Mauro, and Guimarães, Allan J.

Subjects

FUNGAL cell walls, ACANTHAMOEBA castellanii, CELLULAR recognition, MANNOSE-binding lectins, INTRACELLULAR pathogens, MACROPHAGES, TROPHOZOITES

Abstract

Acanthamoeba castellanii (Ac) is a species of free-living amoebae (FLAs) that has been widely applied as a model for the study of host-parasite interactions and characterization of environmental symbionts. The sharing of niches between Ac and potential pathogens, such as fungi, favors associations between these organisms. Through predatory behavior, Ac enhances fungal survival, dissemination, and virulence in their intracellular milieu, training these pathogens and granting subsequent success in events of infections to more evolved hosts. In recent studies, our group characterized the amoeboid mannose binding proteins (MBPs) as one of the main fungal recognition pathways. Similarly, mannose-binding lectins play a key role in activating antifungal responses by immune cells. Even in the face of similarities, the distinct impacts and degrees of affinity of fungal recognition for mannose receptors in amoeboid and animal hosts are poorly understood. In this work, we have identified high-affinity ligands for mannosylated fungal cell wall residues expressed on the surface of amoebas and macrophages and determined the relative importance of these pathways in the antifungal responses comparing both phagocytic models. Mannose-purified surface proteins (MPPs) from both phagocytes showed binding to isolated mannose/mannans and mannosylated fungal cell wall targets. Although macrophage MPPs had more intense binding when compared to the amoeba receptors, the inhibition of this pathway affects fungal internalization and survival in both phagocytes. Mass spectrometry identified several MPPs in both models, and in silico alignment showed highly conserved regions between spotted amoeboid receptors (MBP and MBP1) and immune receptors (Mrc1 and Mrc2) and potential molecular mimicry, pointing to a possible convergent evolution of pathogen recognition mechanisms. [ABSTRACT FROM AUTHOR]

Published

2022

20. Comparative Genomics of Lactiplantibacillus plantarum : Insights Into Probiotic Markers in Strains Isolated From the Human Gastrointestinal Tract and Fermented Foods.

Author

Garcia-Gonzalez, Natalia, Bottacini, Francesca, van Sinderen, Douwe, Gahan, Cormac G. M., and Corsetti, Aldo

Subjects

RAW milk, COMPARATIVE genomics, FERMENTED foods, PROBIOTICS, PENTOSE phosphate pathway, MANNOSE-binding lectins, BACTERIAL genomes, PLANT cell walls

Abstract

Lactiplantibacillus (Lpb.) plantarum is a versatile species commonly found in a wide variety of ecological niches including dairy products and vegetables, while it may also occur as a natural inhabitant of the human gastrointestinal tract. Although Lpb. plantarum strains have been suggested to exert beneficial properties on their host, the precise mechanisms underlying these microbe–host interactions are still obscure. In this context, the genome-scale in silico analysis of putative probiotic bacteria represents a bottom–up approach to identify probiotic biomarkers, predict desirable functional properties, and identify potentially detrimental antibiotic resistance genes. In this study, we characterized the bacterial genomes of three Lpb. plantarum strains isolated from three distinct environments [strain IMC513 (from the human GIT), C904 (from table olives), and LT52 (from raw-milk cheese)]. A whole-genome sequencing was performed combining Illumina short reads with Oxford Nanopore long reads. The phylogenomic analyses suggested the highest relatedness between IMC513 and C904 strains which were both clade 4 strains, with LT52 positioned within clade 5 within the Lpb. plantarum species. The comparative genome analysis performed across several Lpb. plantarum representatives highlighted the genes involved in the key metabolic pathways as well as those encoding potential probiotic features in these new isolates. In particular, our strains varied significantly in genes encoding exopolysaccharide biosynthesis and in contrast to strains IMC513 and C904, the LT52 strain does not encode a Mannose-binding adhesion protein. The LT52 strain is also deficient in genes encoding complete pentose phosphate and the Embden–Meyerhof pathways. Finally, analyses using the CARD and ResFinder databases revealed that none of the strains encode known antibiotic resistance loci. Ultimately, the results provide better insights into the probiotic potential and safety of these three strains and indicate avenues for further mechanistic studies using these isolates. [ABSTRACT FROM AUTHOR]

Published

2022

21. Analysis of Mannose‑Binding Lectin Protein Levels and their MIC Profile in Patients with Dermatophytosis.

Author

Hemanth, Veena, Kindo, Anupma J., Rengasamy, Madhu, Sankarasubramaian, Anandan, and S., Adhikrishnan

Subjects

MANNOSE-binding lectins, PARASITIC diseases, ANTIFUNGAL agents, RINGWORM

Published

2023

22. A patent review of the antimicrobial applications of lectins: Perspectives on therapy of infectious diseases.

Author

Carneiro, Diego C., Fernandez, Luzimar G., Monteiro‐Cunha, Joana P., Benevides, Raquel G., and Cunha Lima, Suzana T.

Subjects

LECTINS, PLANT lectins, MANNOSE-binding lectins, COMMUNICABLE diseases, MICROBIAL sensitivity tests, AMINO acid sequence, VIRUS diseases

Abstract

Patents of lectins with antiviral, antibacterial and antifungal applications were searched and reviewed. Lectins are proteins that reversibly bind to specific carbohydrates and have the potential for therapy of infectious diseases as biopharmaceuticals, biomedical tools or in drug design. Given the rising concerns over drug resistance and epidemics, our patent review aims to add information, open horizons and indicate our view of the future perspectives about the antimicrobial applications of lectins. Patents with publications until December 2020 were retrieved from Espacenet using defined search terms and Boolean operators. The documents were used to identify the geographical and temporal distribution of the patents, characterize their lectins, and classify and summarize their antiviral, antibiotic and antifungal applications. Lectins are promising antiviral agents against viruses with epidemics and drug resistance concerns. Mannose‐binding lectins were the most suggested antiviral agents since glycans with mannose residues are commonly involved in viral entry mechanisms. They were also immobilized onto surfaces to trap viral particles and inhibit their spread and replication. Many patents described the extraction, isolation, amino acid and nucleotide sequences, and expression vectors of lectins with antibiotic and/or antifungal activities in terms of MIC and IC50 for in vitro assays. The inventions also included lectins as biological tools in nanosensors for antibiotics susceptibility tests, drug‐delivery systems for the treatment of resistant bacteria, diagnostics of viral diseases and as a vaccine adjuvant. Although research and development of new medicines is highly expensive, antimicrobial lectins may be worth investments given the emergence of epidemics and drug resistance. For this purpose, less invasive routes should be developed as alternatives to the parenteral administration of biologics. While anti‐glycan neutralizing antibodies are difficult to develop due to the low immunogenicity of carbohydrates, lectins can be produced more easily and have a broad‐spectrum activity. Protein engineering technologies may make the antimicrobial applications of lectins more successful. [ABSTRACT FROM AUTHOR]

Published

2022

23. Viral Evasion of Innate Immune Defense: The Case of Resistance of Pandemic H1N1 Influenza A Virus to Human Mannose-Binding Proteins.

Author

White, Mitchell R., Nikolaidis, Nikolaos M., McCormack, Francis, Crouch, Erika C., and Hartshorn, Kevan L.

Subjects

MANNOSE-binding lectins, INFLUENZA A virus, INFLUENZA A virus, H1N1 subtype, PANDEMICS, LECTINS, PULMONARY surfactant-associated protein D

Abstract

Mannose-binding lectins effectively inhibit most seasonal strains of influenza A virus and contribute to the innate host defense vs. these viruses. In contrast, pandemic IAV strains are largely resistant to these lectins, likely contributing to increased spread and worse outcomes. In this paper, we evaluated the inhibition of IAV by mannose-binding lectins of human, bacterial, and fungal origin to understand and possibly increase activity vs. the pandemic IAV. A modified version of the human surfactant protein D (SP-D) neck and carbohydrate recognition domain (NCRD) with combinatorial substitutions at the 325 and 343 positions, previously shown to inhibit pandemic H3N2 IAV in vitro and in vivo , and to inhibit pandemic H1N1 in vitro , failed to protect mice from pandemic H1N1 in vivo in the current study. We attempted a variety of maneuvers to improve the activity of the mutant NCRDs vs. the 2009 pandemic H1N1, including the formation of full-length SP-D molecules containing the mutant NCRD, cross-linking of NCRDs through the use of antibodies, combining SP-D or NCRDs with alpha-2-macroglobulin, and introducing an additional mutation to the double mutant NCRD. None of these substantially increased the antiviral activity for the pandemic H1N1. We also tested the activity of bacterial and algal mannose-binding lectins, cyanovirin, and griffithsin, against IAV. These had strong activity against seasonal IAV, which was largely retained against pandemic H1N1. We propose mechanisms to account for differences in activity of SP-D constructs against pandemic H3N2 and H1N1, and for differences in activity of cyanovirin vs. SP-D constructs. [ABSTRACT FROM AUTHOR]

Published

2021

24. A case of persistent recurrent herpes zoster ophthalmicus in a patient with primary mannose binding lectin deficiency.

Author

Maltsev, D. V.

Subjects

OPHTHALMIC zoster, MANNOSE-binding lectins, PROTEIN deficiency, KERATOCONJUNCTIVITIS, ANTIALLERGIC agents

Abstract

In the current paper, we present an example case of persistent recurrent herpes zoster ophthalmicus with the development of chronic keratoconjunctivitis, corneal opacity, secondary eczema herpeticum and resistance both to antiviral drugs and to antiallergic medications in a female patient with primary MBL deficiency. Particularly, we demonstrate how the elucidation of the causative immune deficiency and the related administration of specific replacement immunotherapy has become the cornerstone of the achievement of clinical success in the difficult-to-treat patient. Immunological tests demonstrated that the patient had a significantly reduced MBL level (167 ng/ml compared to a norm of 450 ng/ml), whereas other studied immune status characteristics where within normal range. We identified two pathological polymorphisms in the promoter and structural region of MBL-2 (particularly, -550 G/C and 221 C/G), which indicated that the patient had a primary MBL deficiency. It was the fact that the patient had the above genetic immunodeficiency disease that an atypical and unfavorable course of varicella zoster virus infection was associated in this case. The identification of primary MBL deficiency opened the door for new ways of therapy for the difficult-to-treat infectious disease through the specific replacement immunotherapy with the aim of improving immune control of the opportunistic agent through compensation of primary immunodeficiency. [ABSTRACT FROM AUTHOR]

Published

2021

25. Production of a monoclonal antibody against a galactose-binding protein of Acanthamoeba castellanii and its cytotoxicity.

Author

Kim, Dong-Youn, Son, Dae-Hyun, Matin, Abdul, and Jung, Suk-Yul

Subjects

ACANTHAMOEBA castellanii, MONOCLONAL antibodies, ANTIBODY formation, MANNOSE-binding lectins, CELL fusion, ANTIBODY titer

Abstract

In this study, it was confirmed whether the galactose-binding protein (GBP) was present in Acanthamoeba castellanii, and its function on a target cell was confirmed by production of an antibody against the GBP. Since the genes for GBP have not yet been identified at all, the purification of GBP was done using galactose-beads from amoebial lysates, and monoclonal antibodies were produced using cell fusion. GBP was confirmed to have a size of about 35 kDa. After the third immunization with purified GBP in BALB/c mice, monoclonal antibody production was analyzed. The clone cultured before limiting dilution was named 2AB2 and showed the highest antibody titer in the culture supernatant of a 24-well plate. AF6 clone cultured after limiting dilution showed an antibody titer of 0.259 in a 75-T flask. Antibodies generated by collecting ascites by injecting monoclonal colonies into the abdominal cavity of mice were confirmed through gel analysis and were observed to belong to the isotype of the IgM having kappa chains. Since the cytotoxicity of A. castellanii was inhibited by about 26% by the monoclonal antibody against GBP, it was confirmed that the antibody against GBP had an inhibitory effect on cytotoxicity. This study was the first report on GBP isolated and purified from A. castellanii, and similarly to a mannose-binding protein (MBP), its involvement in contact-dependent cytotoxicity was demonstrated with monoclonal antibody production. [ABSTRACT FROM AUTHOR]

Published

2021

26. Medical University of Plovdiv Researchers Provide Details of New Studies and Findings in the Area of Membranous Nephropathy (Mannose-Binding Lectin Deposition in Membranous Nephropathy and Differentiation of Primary from Secondary Forms).

Subjects

MANNOSE-binding lectins, PHOSPHOLIPASE A2, COLLECTINS, REPORTERS & reporting, RENAL biopsy

Abstract

Researchers from the Medical University of Plovdiv in Bulgaria have conducted a study on membranous nephropathy (MN), a kidney disease. The study aimed to differentiate between primary and secondary forms of MN, which is crucial for determining appropriate treatment options. The researchers found that the lack of mannose-binding lectin (MBL) deposition can be used as a marker for secondary MN in the early stages of the disease. However, IgG4 deposition, another biomarker, was present in both primary and secondary MNs. This research provides valuable insights into the diagnosis and management of MN. [Extracted from the article]

Published

2024

27. Findings from Department of Orthopedics Broaden Understanding of Spinal Tuberculosis (Combined clinical significance of MRI and serum mannose-binding lectin in the prediction of spinal tuberculosis).

Subjects

GRAM-positive bacterial infections, SPINAL tuberculosis, MYCOBACTERIAL diseases, MAGNETIC resonance imaging, MANNOSE-binding lectins, ORTHOPEDICS

Abstract

A recent study conducted by the Department of Orthopedics explored the diagnostic value of MRI combined with mannose-binding lectin (MBL) for spinal tuberculosis (STB). The study included 124 patients suspected of having STB, who were divided into STB and non-STB groups based on their pathological diagnosis. The results showed that both MRI and MBL had diagnostic value for STB, but their combined use resulted in higher diagnostic accuracy than using either one alone. The sensitivity of MRI combined with MBL diagnosis was 96.61%, and the specificity was 92.31%. [Extracted from the article]

Published

2024

28. Status of mannose-binding lectin (MBL) and complement system in COVID-19 patients and therapeutic applications of antiviral plant MBLs.

Author

Gupta, Anita and Gupta, G. S.

Abstract

Coronavirus disease 2019 (COVID-19) is an infectious disease caused by a virus called "Severe Acute Respiratory Syndrome Coronavirus 2 (SARS-CoV-2)." In the majority of patients, infection with COVID-19 may be asymptomatic or may cause only mild symptoms. However, in some patients, there can also be immunological problems, such as macrophage activation syndrome (CSS) that results in cytokine storm syndrome (CSS) and acute respiratory distress syndrome (ARDS). Comprehension of host-microbe communications is the critical aspect in the advancement of new therapeutics against infectious illnesses. Endogenous animal lectins, a class of proteins, may perceive non-self glycans found on microorganisms. Serum mannose-binding lectin (sMBL), as a part of the innate immune framework, recognizes a wide range of microbial microorganisms and activates complement cascade via an antibody-independent pathway. Although the molecular basis for the intensity of SARS-CoV-2 infection is not generally understood, scientific literature indicates that COVID-19 is correlated with unregulated activation of the complement in terms of disease severity. Disseminated intravascular coagulation (DIC), inflammation, and immune paralysis contribute to unregulated complement activation. Pre-existing genetic defects in MBL and their association with complement play a major role in immune response dysregulation caused by SARS-CoV-2. In order to generate anti-complement-based therapies in Covid-19, an understanding of sMBL in immune response to SARS-CoV-2 and complement is therefore essential. This review highlights the role of endogenous sMBL and complement activation during SARS-CoV-2 infection and their therapeutic management by various agents, mainly plant lectins, since antiviral mannose-binding plant lectins (pMBLs) offer potential applications in the prevention and control of viral infections. [ABSTRACT FROM AUTHOR]

Published

2021

29. Mevo lectin specificity toward high-mannose structures with terminal αMan(1,2)αMan residues and its implication to inhibition of the entry of Mycobacterium tuberculosis into macrophages.

Author

Sivaji, Nukathoti, Harish, Nikitha, Singh, Samsher, Singh, Amit, Vijayan, Mamannamana, and Surolia, Avadhesha

Subjects

LECTINS, MYCOBACTERIUM tuberculosis, MANNOSE-binding lectins, ISOTHERMAL titration calorimetry, GLYCAN structure, MYCOBACTERIUM smegmatis, MACROPHAGES

Abstract

Mannose-binding lectins can specifically recognize and bind complex glycan structures on pathogens and have potential as antiviral and antibacterial agents. We previously reported the structure of a lectin from an archaeal species, Mevo lectin, which has specificity toward terminal α1,2 linked manno-oligosaccharides. Mycobacterium tuberculosis expresses mannosylated structures including lipoarabinomannan (ManLAM) on its surface and exploits C-type lectins to gain entry into the host cells. ManLAM structure has mannose capping with terminal αMan(1,2)αMan residues and is important for recognition by innate immune cells. Here, we aim to address the specificity of Mevo lectin toward high-mannose type glycans with terminal αMan(1,2)αMan residues and its effect on M. tuberculosis internalization by macrophages. Isothermal titration calorimetry studies demonstrated that Mevo lectin shows preferential binding toward manno-oligosaccharides with terminal αMan(1,2)αMan structures and showed a strong affinity for ManLAM, whereas it binds weakly to Mycobacterium smegmatis lipoarabinomannan, which displays relatively fewer and shorter mannosyl caps. Crystal structure of Mevo lectin complexed with a Man7D1 revealed the multivalent cross-linking interaction, which explains avidity-based high-affinity for these ligands when compared to previously studied manno-oligosaccharides lacking the specific termini. Functional studies suggest that M. tuberculosis internalization by the macrophage was impaired by binding of Mevo lectin to ManLAM present on the surface of M. tuberculosis. Selectivity shown by Mevo lectin toward glycans with terminal αMan(1,2)αMan structures, and its ability to compromise the internalization of M. tuberculosis   in vitro , underscore the potential utility of Mevo lectin as a research tool to study host-pathogen interactions. [ABSTRACT FROM AUTHOR]

Published

2021

30. Prediction of the Mannose-Binding Site in the Agaricus bisporus Mannose-Binding Protein.

Author

Ismaya, Wangsa Tirta, Tjandrawinata, Raymond Rubianto, and Rachmawati, Heni

Subjects

MANNOSE-binding lectins, CULTIVATED mushroom, AMINO acid sequence, CARRIER proteins, GALACTOSE, LECTINS, MOLECULAR docking, PLANT lectins

Abstract

Agaricus bisporus mannose-binding protein (Abmb) was discovered as part of mushroom tyrosinase (PPO3) complex. Apart from its presence, nothing is known about its function or activity in the mushroom. The protein is evolutionarily related to lectins with β-trefoil fold, which are glucose or galactose (and their derivatives) binding proteins. Abmb is also recently showed to display the typical agglutination activity of lectin when in complex with PPO3; this further supports Abmb similarity to its structural homologs from lectin with β-trefoil fold. However, Abmb has no affinity towards glucose or galactose but for mannose, thus its binding to the sugar may be different from its homologs. To date, the natural ligand of Abmb is unknown and the structure of Abmb in the presence of a ligand is not available. Therefore, the mannose-binding site of Abmb was predicted using molecular docking, which was consulted with the information from its structural homologs. This conservative approach would prevent over-speculation. The mannose-binding site of Abmb is likely located in the same region to that of Abmb structural homologs but with a shift in position due to the presence of additional surface loop. In addition, benefiting from the information from an in vitro study on Abmb sugar specificity, the mannose poses suggested that the sugar might interact with the side chains of Arg15, Thr45, Gln48, Asp49, Asp51 and Arg51. Most of these residues were equally present in Abmb structural homologs despite variation of their positions in the amino acid sequence. The variation probably originates from alteration of its amino acid sequence during evolution. [ABSTRACT FROM AUTHOR]

Published

2021

31. An Aromatic Micelle‐Based Saccharide Cluster with Changeable Fluorescent Color and its Protein Interactions.

Author

Narita, Haruna, Catti, Lorenzo, and Yoshizawa, Michito

Subjects

PROTEIN-protein interactions, FLUORESCENT proteins, SACCHARIDES, MANNOSE-binding lectins, FLUORESCENT dyes

Abstract

To develop a new type of synthetic saccharide clusters with changeable fluorescent colors, we herein designed a multisaccharide‐coated aromatic micelle. The new cluster forms in water through the quantitative assembly of bent polyaromatic amphiphiles bearing three mannose groups. The spherical assembly, with a 2 nm‐sized polyaromatic core and ca. 18 saccharide pendants, is stable even under high dilution conditions (up to 0.02 mM). The emission intensity and color of the saccharide cluster can be altered from moderate blue (ΦF=19 %) to strong red, orange, and green (ΦF up to 67 %) upon encapsulation of hydrophobic fluorescent dyes in water. Moreover, the present fluorescent clusters, both with and without the dyes, display selective interactions with mannose‐binding proteins in vitro. [ABSTRACT FROM AUTHOR]

Published

2021

32. An Aromatic Micelle‐Based Saccharide Cluster with Changeable Fluorescent Color and its Protein Interactions.

Author

Narita, Haruna, Catti, Lorenzo, and Yoshizawa, Michito

Subjects

PROTEIN-protein interactions, FLUORESCENT proteins, SACCHARIDES, MANNOSE-binding lectins, FLUORESCENT dyes

Abstract

To develop a new type of synthetic saccharide clusters with changeable fluorescent colors, we herein designed a multisaccharide‐coated aromatic micelle. The new cluster forms in water through the quantitative assembly of bent polyaromatic amphiphiles bearing three mannose groups. The spherical assembly, with a 2 nm‐sized polyaromatic core and ca. 18 saccharide pendants, is stable even under high dilution conditions (up to 0.02 mM). The emission intensity and color of the saccharide cluster can be altered from moderate blue (ΦF=19 %) to strong red, orange, and green (ΦF up to 67 %) upon encapsulation of hydrophobic fluorescent dyes in water. Moreover, the present fluorescent clusters, both with and without the dyes, display selective interactions with mannose‐binding proteins in vitro. [ABSTRACT FROM AUTHOR]

Published

2021

33. Thermodynamic and structural aspects of molecular recognition in mannose-binding protein complexes: a theoretical study over HRP-ArtinM association.

Author

Santo, Anderson Aparecido do Espírito and Feliciano, Gustavo Troiano

Subjects

MANNOSE-binding lectins, MOLECULAR recognition, GIBBS' free energy, GLYCOSYLATED hemoglobin, AMINO acid residues, VAN der Waals forces, JACKFRUIT, LECTINS

Abstract

The biomolecular recognition of D-mannose-binding lectin from Artocarpus heterophyllus (ArtinM) by Horseradish Peroxidase (HRP) mediated by glycosylation allows their application in a multitude of biological systems. The present work describes the use of molecular dynamics (MD) to assess the Gibbs free energy associated with the formation of a ArtinM-HRP conjugate mediated by a glycosylation molecule. For the enthalpy term, we applied the molecular mechanics Poisson-Boltzmann surface area (MM-PBSA) method and for the vibrational entropy term, we use the quasi-harmonic approximation. Our results show that, even without glycosylation, the binding free energy between ArtinM and HRP is − 196.154 kJmol− 1, an extremely high affinity with low selectivity, originated mainly through the van der Waals energy terms. The binding free energy between ArtinM and the glycosylated HRP (gHRP) was calculated at − 66.156 kJmol− 1, an absolute and considerably lower value, however, originated from electrostatic energy terms, which increases the selectivity of molecular recognition. Our work has shown that the HRP active site region has a high affinity and low selectivity for other biomolecules. The presence of glycosylation plays a role in increasing this selectivity for this region. Thus, we conclude that performing mutagenesis of amino acid residues near the entrance of the catalytic site, can improve the activity of non-glycosylated HRPs. This illustrates new insights that can be applied to carbohydrate-based immunochemistry. [ABSTRACT FROM AUTHOR]

Published

2021

34. Platelet‐derived extracellular vesicles are increased in sera of Alzheimer's disease patients, as revealed by Tim4‐based assays.

Author

Odaka, Haruki, Hiemori, Keiko, Shimoda, Asako, Akiyoshi, Kazunari, and Tateno, Hiroaki

Subjects

EXOSOMES, ALZHEIMER'S patients, EXTRACELLULAR vesicles, BILAYER lipid membranes, MANNOSE-binding lectins, ALZHEIMER'S disease, NEUROFIBRILLARY tangles

Abstract

Alzheimer's disease (AD) is the most common form of dementia, characterized by the accumulation of β‐amyloid plaques and the formation of neurofibrillary tangles. Extracellular vesicles (EVs) are small vesicles surrounded by a lipid bilayer membrane, which may be involved in the progression of AD. Glycans are essential building blocks of EVs, and we hypothesized that EV glycans may reflect pathological conditions of various diseases. Here, we performed glycan profiling of EVs prepared from sera of three AD patients (APs) compared to three healthy donors (HDs) using lectin microarray. Distinct glycan profiles were observed. Mannose‐binding lectins exhibited significantly higher signals for AP‐derived EVs than HD‐derived EVs. Lectin blotting using mannose‐binding lectin (rPALa) showed a single protein band at ~ 80 kDa exclusively in AP‐derived EVs. LC‐MS/MS analysis identified a protein band precipitated by rPALa as CD61, a marker of platelet‐derived exosomes (P‐Exo). Sandwich assays using Tim4 with specificity for phosphatidylserine on EVs and antibodies against P‐Exo markers (CD61, CD41, CD63, and CD9) revealed that P‐Exo is significantly elevated in sera of APs (n = 16) relative to age‐ and sex‐matched HDs (n = 16). Tim4‐αCD63 showed the highest value for the area under the curve (0.957) for discriminating APs from HDs, which should lead to a better understanding of AD pathology and may facilitate the development of a novel diagnostic method for AD. [ABSTRACT FROM AUTHOR]

Published

2021

35. Genetic Association With Pseudomonas aeruginosa Acquisition in Cystic Fibrosis: Influence of Surfactant Protein D and Mannose-Binding Lectin.

Author

Nourkami-Tutdibi, Nasenien, Freitag, Klemens, Zemlin, Michael, and Tutdibi, Erol

Subjects

PULMONARY surfactant-associated protein D, MANNOSE-binding lectins, PSEUDOMONAS aeruginosa, CYSTIC fibrosis, PSEUDOMONAS diseases

Abstract

Background: Pseudomonas aeruginosa (PA) infection in cystic fibrosis (CF) is associated with poor prognosis. Surfactant protein-D (SFTPD) and mannose-binding lectin (MBL) play a critical role in innate immunity and response to bacterial infections. We investigated serum levels and genetic variants of SFTPD and MBL in CF patients. Method: Thirty-five Caucasian patients homozygous for ΔF508del were genotyped for functional relevant polymorphisms within MBL2 (promoter−221 Y/X, codons 52, 54, and 57) and SFTPD genes (Met11Thr, Ala160Thr, and Ser270Thr). Serum levels of collectins, clinical characteristics, and PA status were correlated with genetic data. Results: Patients age, gender, and PA status did not affect MBL and SFTPD serum concentrations. MBL concentrations were correlated with MBL haplotypes. Patients with chronic Pseudomonas aeroginosa infection (PAC) and MBL insufficiency had a shorter interval between first PA infection and onset of PAC (0.01 vs. 4.6 years, p < 0.04) as well as a lower median age at transition to PAC (9.8 vs. 16.4 years, p < 0.03) compared to MBL sufficient patients with PAC. SFTPD serum level and FEV1% (Spearman r = −0.41, p < 0.03) showed a negative correlation irrespective of PA infection status. The hazard ratio to PA acquisition was increased in carriers of the SFTPD haplotype 11Thr-160Ala-270Ser compared to carriers of the common 11Met-160Thr-270Ser haplotype [HR 3.0 (95%CI: 1.1–8.6), p < 0.04]. Conclusion: MBL insufficiency leads to a shorter interval between first PA infection and onset of chronic infection. Susceptibility to PA acquisition is associated with SFTPD genetic variants with 11Thr-160Ala-270Ser as risk haplotype for early PA infection. This may be due to presence of threonine associated with oligomeric structure of SFTPD and binding ability to bacteria. [ABSTRACT FROM AUTHOR]

Published

2021

36. Identification of sugar moieties in chief cells of the rat fundic gastric glands.

Author

Gómez-Santos, Laura, Alonso, Edurne, Crende, Olatz, Ibarretxe, Gaskon, Madrid, Juan Francisco, and Sáez, Francisco José

Subjects

GASTRIC mucosa, MANNOSE-binding lectins, MOIETIES (Chemistry), GLYCOCONJUGATES, GALACTOSE, LECTINS, GLUCOSE oxidase, ZYMOGENS

Abstract

Many studies have been conducted to determine the composition of the glycoconjugates of the mucus-secreting cells of the fundic glands of the stomach. However, the chief cells of these glands have been largely ignored because they secrete mainly zymogens with a lower glycosylation. The aim of this work was to analyze the glycoconjugates of the gastric chief cells by a battery of 17 different lectins, recognizing Fucose, N-acetylgalactosamine, Galactose, N-acetylneuraminic acid, N-acetylglucosamine and Mannose containing oligosaccharides. Histochemical techniques were performed with several lectins and also combined with two pre-treatments; β-elimination, which removes O-linked oligosaccharides, and incubation with Peptide-N-Gycosidase F, which removes N-linked oligosaccharides. In addition, acid hydrolysis was performed before WGA histochemistry, and incubation with glucose oxidase before Con A labeling. Many lectins did not stain the chief cells. In addition, the presence of O-glycans in the apical cell membrane was demonstrated with the lectins AAL, HPA, MPA/MPL, PNA, RCA-I, and WGA. Some of these O-glycans were resistant to short-term β-elimination pre-treatments. Mannose-binding lectins stained the basal cytoplasm of the chief cells. The level of glycosylation of the chief cells was lower than that of the mucous cells. The presence of O-glycans in the apical cell membrane is consistent with the presence of mucins such as MUC1 in the apical membrane of chief cells. Moreover, Mannose-binding lectins revealed N-glycosylation in the basal cytoplasm. The knowledge of gastric chief cell glycoconjugates is relevant because of their potential involvement not only in in physiological but also in pathological processes, such as cancer. [ABSTRACT FROM AUTHOR]

Published

2021

37. An integrated microfluidic system for early detection of sepsis-inducing bacteria.

Author

Fang, Yen-Ling, Wang, Chih-Hung, Chen, Yi-Sin, Chien, Chun-Chih, Kuo, Feng-Chih, You, Huey-Ling, Lee, Mel S., and Lee, Gwo-Bin

Subjects

ERYTHROCYTES, LEUCOCYTES, MANNOSE-binding lectins, BACTERIAL typing, BACTERIAL proteins

Abstract

Since early diagnosis of sepsis may assist clinicians in initiating timely, effective, and prognosis-improving antibiotic therapy, we developed an integrated microfluidic chip (IMC) for rapid isolation of both Gram-positive and Gram-negative bacteria from blood. The device comprised a membrane-based filtration module (90 min operating time), a bacteria-capturing module using a micro-mixer containing magnetic beads coated with "flexible neck" regions of mannose-binding lectin proteins for bacteria capture (20 min), and a miniature polymerase chain reaction (PCR) module for bacteria identification (90 min via TaqMan® probe technology). The filter separated all white blood cells and 99.5% of red blood cells from bacteria, which were captured at rates approaching 85%. The PCR assay's limit of detection was 5 colony-forming units (CFU) per reaction, and the entire process was completed in only 4 h. Since this is far less than that for culture-based approaches, this IMC may serve as a promising device for detection of sepsis. [ABSTRACT FROM AUTHOR]

Published

2021

38. Plasma complement activation mechanisms differ in ornate (Terrapene ornata ornata) and eastern box turtles (Terrapene carolina carolina).

Author

Adamovicz, Laura, Baker, Sarah J., Merchant, Mark, Darville, Lancia, and Allender, Matthew C.

Subjects

COMPLEMENT activation, SODIUM dodecyl sulfate, MANNOSE-binding lectins, TURTLES, POLYACRYLAMIDE gel electrophoresis

Abstract

Eastern (Terrapene carolina carolina) and ornate (Terrapene ornata ornata) box turtles have robust plasma antibacterial activity, however, the mechanism behind this activity is unknown. We used sheep red blood cell (SRBC) hemolysis assays, mannan‐affinity chromatography, sodium dodecyl sulfate polyacrylamide gel electrophoresis (SDS‐PAGE), and matrix‐assisted laser desorption ionization time‐of‐flight (MALDI‐TOF) to explore the mechanisms of complement activity in box turtles. Plasma from both species demonstrated volume, time, and temperature‐dependent SRBC hemolysis, with significantly greater hemolytic activity in ornate box turtle plasma. Hemolytic activity was highly attenuated following treatment with heat, EDTA, and salicylaldoxime in both species, but was unchanged after treatment with methylamine and ammonium hydroxide. Two abundant mannan‐binding proteins (presumed C‐type lectins) were identified in eastern box turtle plasma using SDS‐PAGE and MALDI‐TOF, but ornate box turtles did not express either protein. Eastern box turtles appear to rely on the lectin pathway of complement activation while ornate box turtles utilize the alternative pathway. This study provides further evidence that mechanisms underlying immune function are not always conserved between closely related species. This finding may have important implications for explaining species differences in susceptibility to emerging threats such as disease, toxicants, and climate change. Research Highlights: Box turtle plasma lyses sheep erythrocytes in a volume, time, and temperature‐dependent manner using the complement cascade.Eastern box turtles use the lectin pathway of complement activation while ornate box turtles use the alternative pathway. [ABSTRACT FROM AUTHOR]

Published

2020

39. The potential and efficacy of Allium sativum leaf lectin (ASAL) against sap-sucking insect pests of transgenic maize.

Author

Bhatti, Muhammad Umar, Riaz, Saman, Toufiq, Nida, Adeyinka, Olawale Samuel, Khan, Anwar, Yousaf, Iqra, Tariq, Muhammad, Murtaza, Shahid, Nasir, Idrees Ahmad, and Tabassum, Bushra

Subjects

CORN, MANNOSE-binding lectins, APHID control, TRANSGENE expression, RHOPALOSIPHUM, GARLIC, KIDNEY bean, INSECT pest control

Abstract

The gene sequence encoding the mannose-binding homodimeric protein Allium sativum leaf agglutinin (ASAL) was introduced into maize inbred lines to achieve resistance against sap-sucking corn leaf aphids in transgenic lines. Maize transformants were generated after the co-cultivation of immature maize embryos with the Agrobacterium strain LB4404 harbouring a recombinant Ti-binary ASAL construct driven by the polyubiquitin promoter. The preliminary screening of maize transformants was performed via GUS histochemical analysis, and PCR and Southern blotting confirmed the insertion of the transgene and its stable integration in five transgenic maize lines. Transcript abundance was quantified by a quantitative real-time PCR assay, which revealed variable expression of the ASAL transgene among five transgenic maize lines. The highest mRNA expression of the ASAL gene was found in the A23 transgenic maize line, while the lowest expression was found in the AU1 transgenic maize line. In planta bioassays in the T1 progeny of the transgenic maize lines revealed high resistance against corn leaf aphids compared to the control non-transgenic line. The mortality of the infesting aphids (Rhopalosiphum maidi) was found to vary from 40 to 71% compared to that of the non-transgenic control maize line. [ABSTRACT FROM AUTHOR]

Published

2020

40. ANA-associated uveitis in the presence of reactivated HHV-7 infection in a patient with MBL deficiency.

Author

Maltsev, D. V. and Hurzhii, O. O.

Subjects

UVEITIS, MANNOSE-binding lectins, POLYMERASE chain reaction, RITUXIMAB, METHOTREXATE

Abstract

Bilateral, ANA-positive uveitis developed in a patient with primary total mannose binding lectin (MBL) deficiency during human herpes virus type 7 (HHV-7) reactivation from latently infected salivary glands. The diagnosis of uveitis was confirmed based on eye examination, findings of optical coherence tomography, and elevated serum antinuclear antibody titer (1:320). HHV-7 reactivation from persistence was verified by blood white cell polymerase chain reaction (PCR) and eye swab PCR. The patient was diagnosed with primary MBL deficiency based on the results of enzyme-linked immunosorbent assay and special genetic testing. The serum MBL level was zero, but all other studied characteristics were within respective reference ranges. We identified three pathologic polymorphisms (223 C/T, 230 G/A, and 239 A/G) in the MBL-2 gene, which indicated a genetic origin for the detected immunodeficiency. The results of these tests provided a rationale for administering a comprehensive treatment for suppression of the autoimmune process (rituximab and methotrexate), elimination of HHV-7 DNA from blood white cells and ocular smears (valganciclovir) and compensation of primary immunodeficiency by replacement therapy with intravenous infusion of solvent-detergent-treated fresh frozen plasma containing MBL. Our comprehensive approach to treatment led not only to a complete remission of uveitis, but also to compensation of other autoimmune, allergic and infectious symptoms and signs of the immunodeficiency. The data from this report expand our knowledge on the heterogeneity of clinical signs and symptoms of primary MBL deficiency in humans and provide pathways to studies on new potential pathogenetic mechanisms of autoimmune lesions in this genetic immune dysfunction which is one of the most common in the population. [ABSTRACT FROM AUTHOR]

Published

2020

41. Extended Spectrum Beta-Lactamase and Metallo Beta-Lactamase Producing Pseudomonas Species Isolated From Fish Pond Water in Ibadan, Nigeria.

Author

Falodun, Olutayo Israel and Ikusika, Emmanuel Olugbenga

Subjects

FISH ponds, PSEUDOMONAS, BETA lactam antibiotics, BETA lactamases, DRUG resistance in bacteria, GRAM-negative bacteria, MANNOSE-binding lectins

Abstract

Gram-negative bacteria that produce Extended-spectrum beta-lactamase (ESBL) and metallo beta-lactamase (MBL) show resistance to beta-lactam antibiotics. This study was to determine Beta-lactamases-producing Pseudomonas species in fish ponds. Pseudomonas species isolated from aquaculture water samples using Pseudomonas base agar were characterised biochemically. The detection of ESBL and MBL was made by double disc synergy and imipenem-EDTA combined disc methods, respectively. Antimicrobial susceptibility was by disc diffusion method. The 94 Pseudomonas species isolated comprised P. aeruginosa (62.8%), P. stutzeri (14.9%), P. putida (9.8%) and P. fluorescens (12.8%). P. aeruginosa 16 (16.3%) and P. stutzeri 4 (4.3%) produced ESBL, but 2 (10%) P. aeruginosa and 1 (5%) P. stutzeri produced MBL. Resistance of ESBL producers to trimethoprim was 55.5% and 7 (35.0%) were multidrug resistant. Detection of ESBL and MBL in Pseudomonas spp. from this study implies environmental health risk. Antibiotics misuse in aquaculture and discharge of untreated aquaculture wastewater into the environment should be discouraged. [ABSTRACT FROM AUTHOR]

Published

2020

42. GENETIC STUDIES FOR WOMEN WITH RECURRENT MISCARRIAGE.

Author

Al-Zuhairi, Ibrahim H., A-Salih, Raid M. H., and Al-Naser, Alaa H.

Subjects

RECURRENT miscarriage, GENOTYPES, MANNOSE-binding lectins, ALLELES, GENETICS

Abstract

The controls and patients were divided into three groups, a control group was healthy recurrent miscarriage women. The explained group was recurrent miscarriage women with RM. The unexplained group was recurrent miscarriage women with RM.The results showed genotypes CC, TT and allele C frequencies increased in patients (33.33%, 20.00% and 56.66%, respectively) than in control (13.33%, 13.33% and 50%, respectively) and this positive relation were insignificant (P= 0.39,0.62 and 0.796, respectively). On other hand, the genotype CT and allele T showed decreased frequencies in patients (46.66 and 43.33%, respectively) than in the control (73.33% and 50%, respectively). The genotype CC and C allele showed a higher frequency in patients (73.33% and 83.3%, respectively) than in the control (13.33% and 50%, respectively). While, the genotype GT, TT, and T allele showed decreased frequencies in patients(20.00%, 6.66% and 16.66%, respectively) than in the control (73.33%, 13.33% and 50%, respectively). [ABSTRACT FROM AUTHOR]

Published

2020

43. Targeting the Mutational Landscape of Bystander Cells: Drug-Promoted Blood Cancer From High-Prevalence Pre-neoplasias in Patients on BRAF Inhibitors.

Author

Simnica, Donjete, Ittrich, Harald, Bockemeyer, Carsten, Stein, Alexander, and Binder, Mascha

Subjects

HEMATOLOGIC malignancies, CHRONIC lymphocytic leukemia, BLOOD cells, MANNOSE-binding lectins, NUCLEOTIDE sequencing, FLUDARABINE

Abstract

Drug-promoted cancers are increasingly recognized as a serious clinical problem in patients receiving BRAF inhibitory treatment. Here we report on a patient with BRAF mutant hairy cell leukemia and monoclonal B-cell lymphocytosis (MBL), who responded durably to BRAF/MEK inhibitors (BRAFi/MEKi) but experienced transformation of a RAS mutant MBL to chronic lymphocytic leukemia (CLL) with accelerated nodal progression. Hypothesizing that BRAFi triggered excessive MEK-ERK signaling in the MBL/CLL clone via the CRAF/RAS complex as previously described for BRAFi-induced cancers, BRAFi was discontinued inducing a rapid remission of the CLL on MEKi alone. Liquid biopsy monitoring showed a continuous increase of the MBL/CLL clone from the start of BRAFi/MEKi treatment followed by a rapid decline upon BRAFi withdrawal. Next-generation sequencing of a cohort of patients with MBL and monoclonal gammopathy of unclear significance (MGUS) revealed that almost one third of these cases harbored RAS mutations. In view of the population frequency of lymphatic pre-malignant conditions and the prevalence of RAS mutations in such cases, vigilant surveillance remains critical in patients treated with BRAF inhibitors. [ABSTRACT FROM AUTHOR]

Published

2020

44. Fasciola hepatica Extracellular Vesicles isolated from excretory-secretory products using a gravity flow method modulate dendritic cell phenotype and activity.

Author

Murphy, Anna, Cwiklinski, Krystyna, Lalor, Richard, O'Connell, Barry, Robinson, Mark W., Gerlach, Jared, Joshi, Lokesh, Kilcoyne, Michelle, Dalton, John P., and O'Neill, Sandra M.

Subjects

EXTRACELLULAR vesicles, FASCIOLA hepatica, GLYCOPROTEIN analysis, DENDRITIC cells, GLYCANS, MANNOSE-binding lectins, IMMUNE response

Abstract

Parasite-released extracellular vesicles (EVs) deliver signals to the host immune system that are critical to maintaining the long-term relationship between parasite and host. In the present study, total EVs (FhEVs) released in vitro by adults of the helminth parasite Fasciola hepatica were isolated using a recently described gravity flow method that protects their structural integrity. The FhEVs molecular cargo was defined using proteomic analysis and their surface topology characterised by glycan microarrays. The proteomic analysis identified 618 proteins, 121 of which contained putative N-linked glycosylation sites while 132 proteins contained putative O-linked glycosylation sites. Glycan arrays revealed surface-exposed glycans with a high affinity for mannose-binding lectins indicating the predominance of oligo mannose-rich glycoproteins, as well as other glycans with a high affinity for complex-type N-glycans. When added to bone-marrow derived dendritic cells isolated FhEV induced a novel phenotype that was categorised by the secretion of low levels of TNF, enhanced expression of cell surface markers (CD80, CD86, CD40, OX40L, and SIGNR1) and elevation of intracellular markers (SOCS1 and SOCS3). When FhEV-stimulated BMDCs were introduced into OT-II mice by adoptive transfer, IL-2 secretion from skin draining lymph nodes (sdLN) and spleen cells was inhibited in response to both specific and non-specific antigen stimulation. Immunisation of mice with a suspension of FhEV did not elicit significant immune responses; however, in the presence of alum, FhEVs induced a mixed Th1/Th2 immune response with high antigen specific antibody titres. Thus, we have demonstrated that FhEVs induce a unique phentotype in DC capable of suppressing IL-2 secretion from T-cells. Our studies add to the growing immuno-proteomic database that will be an important source for the discovery of future parasite vaccines and immunotherapeutic biologicals. Author summary: Parasite-released extracellular vesicles (EVs) deliver signals to the host immune system that are critical to maintaining the long-term relationship between parasite and host. This study isolated total EVs (FhEVs) released in vitro by the adult stages of the parasitic worm Fasciola hepatica using a gravity flow method that protects the structural integrity of the vesicles. Proteomic analysis identified 618 proteins, 121 of which contained putative N-linked glycosylation sites while 132 proteins contained putative O-linked glycosylation sites while glycan arrays revealed surface-exposed glycans were predominantly oligo mannose-rich glycoproteins, and glycans with a high affinity for complex-type N-glycans. Since the EV molecular cargo can influence host immune cells, FhEVs were added to bone-marrow derived dendritic cells, inducing a novel cell phenotype that when adoptive transferred into OT-II mice inhibited IL-2 secretion from skin draining lymph nodes (sdLN) and spleen cells. Immunisation of mice with FhEV did not elicit significant immune responses; however, in the presence of alum, FhEVs induced a mixed Th1/Th2 immune response with high antigen specific antibody titres. This studied sheds like on the biological activity of FhEVs and added to the growing immuno-proteomic database that will be an important source for the discovery of future therapeutics. [ABSTRACT FROM AUTHOR]

Published

2020

45. Multiphysical sensing of light, sound and microwave in a microcavity Brillouin laser.

Author

Yang, Jianfan, Qin, Tian, Zhang, Fangxing, Chen, Xianfeng, Jiang, Xiaoshun, and Wan, Wenjie

Subjects

MICROCAVITY lasers, RADIATION pressure, MICROWAVE imaging, MICROWAVES, ACTIVE medium, MICROWAVE photonics, SOUND mixers & mixing, MANNOSE-binding lectins

Abstract

Light, sound, and microwave are important tools for many interdisciplinary applications in a multi-physical environment, and they usually are inefficient to be detected simultaneously in the same physical platform. However, at the microscopic scale, these waves can unexpectedly interact with the same microstructure through resonant enhancement, making it a unique hybrid micro-system for new applications across multiple physical channels. Here we experimentally demonstrate an optomechanical microdevice based on Brillouin lasing operation in an optical microcavity as a sensitive unit to sense external light, sound, and microwave signals in the same platform. These waves can induce modulations to the microcavity Brillouin laser (MBL) in a resonance-enhanced manner through either the pressure forces including radiation pressure force or thermal absorption, allowing several novel applications such as broadband non-photovoltaic detection of light, sound-light wave mixing, and deep-subwavelength microwave imaging. These results pave the way towards on-chip integrable optomechanical solutions for sensing, free-space secure communication, and microwave imaging. [ABSTRACT FROM AUTHOR]

Published

2020

46. Tracing Extreme Updrafts in Hurricane Wilma (2005) to Their Boundary Layer Roots Using Trajectories: A Thermodynamic and Structural Analysis.

Author

MILLER, WILLIAM and DA-LIN ZHANG

Subjects

BOUNDARY layer (Aerodynamics), LATENT heat of fusion, BUOYANT ascent (Hydrodynamics), HURRICANES, STRATIFIED flow, MANNOSE-binding lectins, HYGROTHERMOELASTICITY, BUOYANCY

Abstract

This study uses a recently developed trajectory model to trace eyewall updrafts in a high-resolution Hurricane Wilma (2005) prediction to their roots in the maritime boundary layer (MBL) in order to better understand their thermodynamics and how they interact with the swirling winds. Out of 97 020 four-hour backward trajectories seeded from the upper troposphere, the 45% of them originating from the MBL are stratified into five subsamples binned by peak vertical velocity wMAX. Of particular interest are the thermodynamic characteristics of parcels belonging to the wMAX-Extreme subsample (i.e., those with wMAX exceeding 20 m s-1 ) that ascend through Wilma’s strongest convective burst (CB) cores. A vertical momentum budget computed along a selected wMAX-Extreme trajectory confirms that the parcel possesses large positive buoyancy that more than compensates for negative hydrometeor loading to yield an uppertropospheric wMAX ; 30 m s-1 . Comparing all 1170 wMAX-Extreme trajectories with all 19 296 secondary circulation trajectories shows that the former tends to originate from the MBL where equivalent potential temperature θe and ocean surface heat and moisture fluxes are locally enhanced. The wMAX-Extreme parcels become further differentiated from the background ascent in terms of their (i) greater updraft width and smaller θe reduction while ascending into the midtroposphere, implying lower environmental entrainment rates, and (ii) less hydrometeor loading in the z 5 3–5-km layer. The Lagrangian analysis herein bridges two previous studies that focused separately on the importance of high SSTs and fusion latent heat release to the development of CBs, the latter of which may facilitate upper-level warm core development through their compensating subsidence. [ABSTRACT FROM AUTHOR]

Published

2020

47. Prevalence and Immunophenotypic Characteristics of Monoclonal B-Cell Lymphocytosis in Healthy Korean Individuals With Lymphocytosis.

Author

In Young Yoo, Sung Hoan Bang, Dae Jin Lim, Seok Jin Kim, Kyunga Kim, Hee Jin Kim, Sun-Hee Kim, and Duck Cho

Subjects

CHRONIC lymphocytic leukemia, LYMPHOCYTOSIS, ASIANS, LYMPHOCYTE count, MANNOSE-binding lectins, EAST Asians

Abstract

Epidemiological studies of monoclonal B-cell lymphocytosis (MBL) have been conducted in limited geographical regions. Little is known about the prevalence of MBL in Asia. We investigated the prevalence and immunophenotypic characteristics of MBL in Koreans who had idiopathic lymphocytosis (lymphocyte count >4.0×109/L) and were =40 years of age. A total of 105 leftover peripheral blood samples met these criteria among those from 73,727 healthy individuals who visited the Health Promotion Center, Samsung Medical Center, Korea, from June 2018 to August 2019. The samples were analyzed using eight-color flow cytometry with the following monoclonal antibodies: CD45, CD5, CD10, CD19, CD20, CD23, and kappa and lambda light chains. The overall prevalence of MBL in the study population was 2.9% (3/105); there was one case of chronic lymphocytic leukemia (CLL)-like MBL (CD5+CD23+), one case of atypical CLL-like MBL (CD5+CD23-), and one case of CD5-MBL with a lambda restriction pattern. This is the first study on the MBL prevalence in an East Asian population, and it reveals a relatively low prevalence of MBL in healthy Korean individuals with lymphocytosis. [ABSTRACT FROM AUTHOR]

Published

2020

48. Mannose-Binding Lectin and Risk of Cardiovascular Events and Mortality in Type 2 Diabetes: A Danish Cohort Study.

Author

Gedebjerg, Anne, Bjerre, Mette, Kjaergaard, Alisa Devedzic, Steffensen, Rudi, Nielsen, Jens Steen, Rungby, Jørgen, Friborg, Søren Gunnar, Brandslund, Ivan, Thiel, Steffen, Beck-Nielsen, Henning, Sørensen, Henrik Toft, Hansen, Troels Krarup, and Thomsen, Reimar Wernich

Subjects

TYPE 2 diabetes, CARDIOVASCULAR diseases, ANGINA pectoris, COHORT analysis, MANNOSE-binding lectins

Abstract

Objective: Mannose-binding lectin (MBL) is linked to risk of cardiovascular disease (CVD) in diabetes, but the nature of the association is unclear. We investigated the association between MBL and the risk of cardiovascular events (CVE) and all-cause mortality in type 2 diabetes.Research Design and Methods: In a cohort study of 7,588 patients with type 2 diabetes, we measured serum MBL in 7,305 patients and performed MBL expression genotyping in 3,043 patients. We grouped serum MBL and MBL expression genotypes into three categories: low, intermediate, and high. Outcomes were CVE (myocardial infarction, stroke, coronary revascularization, unstable angina, or cardiovascular death) and all-cause mortality. The association with outcomes was examined by spline and Cox regression analyses.Results: Serum MBL and CVE showed a U-shaped association. Compared with the intermediate serum MBL category, the adjusted hazard ratio (HR) for CVE was 1.82 (95% CI 1.34-2.46) for the low-MBL category and 1.48 (95% CI 1.14-1.92) for the high-MBL category. We found a similar U-shaped association for all-cause mortality, but with lower risk estimates. Compared with the intermediate MBL expression genotype, the adjusted HR for CVE was 1.40 (95% CI 0.87-2.25) for the low-expression genotype and 1.44 (95% CI 1.01-2.06) for the high-expression genotype. MBL expression genotype was not associated with all-cause mortality.Conclusions: Both serum MBL and MBL expression genotype showed a U-shaped association with CVE risk in individuals with type 2 diabetes. Our findings suggest that serum MBL is a risk factor for CVD in this population. [ABSTRACT FROM AUTHOR]

Published

2020

49. Interactions Between Acanthamoeba culbertsoni and Pathogenic Bacteria and their Inhibition by Lectin- Antibodies.

Author

Suk-Yul Jung

Subjects

ACANTHAMOEBA, MANNOSE-binding lectins, IMMUNOGLOBULINS, MONOCLONAL antibodies, AMOEBA, KLEBSIELLA pneumoniae

Abstract

In this study, using pathogenic and non-pathogenic bacteria, it was analyzed whether a polyclonal serum and a monoclonal antibody to A. culbertsoni mannose-binding protein (MBP) could inhibit its interaction. The association of the amoeba with E. coli O157:H7 was very strong at a level of over 100%, but the non-pathogenic E. coli strain was about five times lower at 22%. Pathogenic K. pnueumoniae also showed high association with amoeba by about 92% as compared with pathogenic E. coli O157:H7 and S. agalactiae. The polyclonal serum to MBP inhibited E. coli O157:H7 association to amoeba 2.5 times more than untreated E. coli O157:H7. Monoclonal antibody to MBP also inhibited bacterial association with amoeba but was not stronger than the polyclonal serum. Pathogenic E. coli O157:H7 showed about 88% invasion into amoeba and decreased about 22% as compared with associated E. coli O157:H7. Polyclonal serum to MBP inhibited about 55%, 50%, and 44% in E. coli O157:H7, K. pneumoniae and S. agalactiae, respectively. The invasion of K. pneumoniae and S. agalactiae was not high as polyclonal serum but was about 8% to 10% weaker than polyclonal serum. The pathogenic strains of K. pneumoniae and S. agalactiae showed less decrease in survival as shown at invasion than E. coli O157:H7 without antibody. This study provided the information that the pathogenic bacteria could be more interactive with A. culbertsoni trophozoites as a reservoir host than non-pathogenic E. coli, and the amoeba should interact with bacteria by the MBP lectin. [ABSTRACT FROM AUTHOR]

Published

2020

50. Principles and current strategies targeting metallo‐β‐lactamase mediated antibacterial resistance.

Author

Yan, Yu‐Hang, Li, Gen, and Li, Guo‐Bo

Subjects

MANNOSE-binding lectins, METAL ions, DRUG resistance in bacteria, PERMEABILITY, ANTIBACTERIAL agents, CARBAPENEMS

Abstract

Resistance to β‐lactam antibacterials is commonly associated with the production of the serine β‐lactamases (SBLs) and/or metallo‐β‐lactamases (MBLs). Although clinically useful inhibitors for the SBLs have been developed, no equivalent inhibitors are available for the MBLs, which can hydrolyze almost all β‐lactam antibiotics, including the so‐called "last resort" carbapenems. It is still a challenging task to develop a clinically useful inhibitor that should be broad‐spectrum targeting multiple clinically relevant MBL enzymes that differ in their active site features. This review provides a detailed description of interaction modes of substrates and small‐molecule inhibitors with various MBL enzymes and highlights the importance of metal‐ and "anchor residue"‐binding features to achieve broad‐spectrum MBL inhibition. Recently emerging active site interference strategies include metal ion deprivation, metal ion replacement, and cysteine modification as challenging, but worth experimenting directions for inhibitor development. The metalloenzyme selectivity, metal‐binding pharmacophore, and cellular permeability and accumulation should be properly considered in the further development of clinically useful inhibitors to combat MBL‐mediated antibacterial resistance. [ABSTRACT FROM AUTHOR]

Published

2020