Your search keyword '"Jacalin"' showing total 94 results

1. Jacalin-Curcumin Complex Sensitizes the Breast Cancer MDA-MB-231 Cell Line.

Author

Petrova, Lidiya, Gergov, Nikolay, Stoup, Marie, Zapryanova, Silvina, Van Damme, Els J. M., Lebègue, Nicolas, Liberelle, Maxime, Zasheva, Diana, and Bogoeva, Vanya

Subjects

*CANCER cells, *TRIPLE-negative breast cancer, *BREAST cancer, *CELL lines, *CELL physiology, *BREAST

Abstract

Protein–drug interactions are crucial for understanding drug delivery and cell functions. Jacalin is a suitable molecule for such targeting, as it specifically recognizes the tumor-associated Thomsen–Friedenreich (TF) antigen that is expressed on the glycosylated proteins in cancer cells. The present paper describes the interaction of curcumin and jacalin, a possible carrier molecule for the delivery of antitumor drugs due to its ability to recognize tumor cells. Our results have shown that both steady-state fluorescence and fluorescent labelling of jacalin are two reliable methods to determine jacalin-curcumin interactions. The affinity of jacalin for curcumin is consistently within the micromolar range (using fluorescence and microscale thermophoresis) showing high-affinity binding of the complex. In vitro experiments on triple-negative breast cancer MDA-MB-231 cells indicated inhibition of cell growth after treating with the jacalin-curcumin complex for 48 h. The cell survival fraction was significantly reduced to 50% after combined treatment. In this paper, we report for the first time about the jacalin-curcumin interaction. We quantified this unique biomolecular interaction and gathered additional information on the binding event. We observed that the jacalin-curcumin complex inhibits the proliferation of the triple-negative breast cancer MDA-MB-231 cells. [ABSTRACT FROM AUTHOR]

Published

2023

2. OsJRL40 , a Jacalin-Related Lectin Gene, Promotes Salt Stress Tolerance in Rice.

Author

Gao, Qinmei, Yin, Xiaolin, Wang, Feng, Hu, Shuchang, Liu, Weihao, Chen, Liangbi, Dai, Xiaojun, and Liang, Manzhong

Subjects

*SALT, *IMMOBILIZED proteins, *RICE breeding, *RICE quality, *TRANSCRIPTION factors

Abstract

High salinity is a major stress factor affecting the quality and productivity of rice (Oryza sativa L.). Although numerous salt tolerance-related genes have been identified in rice, their molecular mechanisms remain unknown. Here, we report that OsJRL40, a jacalin-related lectin gene, confers remarkable salt tolerance in rice. The loss of function of OsJRL40 increased sensitivity to salt stress in rice, whereas its overexpression enhanced salt tolerance at the seedling stage and during reproductive growth. β-glucuronidase (GUS) reporter assays indicated that OsJRL40 is expressed to higher levels in roots and internodes than in other tissues, and subcellular localization analysis revealed that the OsJRL40 protein localizes to the cytoplasm. Further molecular analyses showed that OsJRL40 enhances antioxidant enzyme activities and regulates Na+-K+ homeostasis under salt stress. RNA-seq analysis revealed that OsJRL40 regulates salt tolerance in rice by controlling the expression of genes encoding Na+/K+ transporters, salt-responsive transcription factors, and other salt response-related proteins. Overall, this study provides a scientific basis for an in-depth investigation of the salt tolerance mechanism in rice and could guide the breeding of salt-tolerant rice cultivars. [ABSTRACT FROM AUTHOR]

Published

2023

3. Growing Maize Root: Lectins Involved in Consecutive Stages of Cell Development.

Author

Aglyamova, Aliya, Petrova, Natalia, Gorshkov, Oleg, Kozlova, Liudmila, and Gorshkova, Tatyana

Subjects

LECTINS, PLANT cell walls, CORN growth, RECEPTOR-like kinases, PROTEIN domains, PLANT development, MORPHOGENESIS, CORN

Abstract

Proteins that carry specific carbohydrate-binding lectin domains have a great variety and are ubiquitous across the plant kingdom. In turn, the plant cell wall has a complex carbohydrate composition, which is subjected to constant changes in the course of plant development. In this regard, proteins with lectin domains are of great interest in the context of studying their contribution to the tuning and monitoring of the cell wall during its modifications in the course of plant organ development. We performed a genome-wide screening of lectin motifs in the Zea mays genome and analyzed the transcriptomic data from five zones of primary maize root with cells at different development stages. This allowed us to obtain 306 gene sequences encoding putative lectins and to relate their expressions to the stages of root cell development and peculiarities of cell wall metabolism. Among the lectins whose expression was high and differentially regulated in growing maize root were the members of the EUL, dirigent–jacalin, malectin, malectin-like, GNA and Nictaba families, many of which are predicted as cell wall proteins or lectin receptor-like kinases that have direct access to the cell wall. Thus, a set of molecular players was identified with high potential to play important roles in the early stages of root morphogenesis. [ABSTRACT FROM AUTHOR]

Published

2022

4. Evaluation of Jacalin lectin sorbents for the extraction of the human chorionic gonadotropin glycoforms prior to analysis by nano liquid chromatography-high resolution mass spectrometry.

Author

Goumenou, Anastasia, Chendo, Christophe, Combès, Audrey, Fournier, Thierry, Pichon, Valérie, and Delaunay, Nathalie

Subjects

*CHORIONIC gonadotropins, *SOLID phase extraction, *MASS spectrometry, *PROTEIN analysis, *LIQUID chromatography

Abstract

Human chorionic gonadotropin (hCG) is a dimeric, highly glycosylated hormone with a total of 4 N- and 4 O-glycosylation sites in its two subunits, hCGα and hCGβ. Recently, we developed a novel nano liquid chromatography coupled to high resolution mass spectrometry (nanoLC-HRMS) method for the analysis and thus the detection of the intact glycoforms of hCG. Here, a sorbent functionalized with the Jacalin lectin was evaluated in solid-phase extraction (SPE) for its potential to fractionate the hCG glycoforms prior to their nanoLC-HRMS analysis at the intact level, which may facilitate the detection of low-abundance glycoforms and may lead to a more detailed characterization of the hormone glycosylation. A commercial sorbent based on Jacalin immobilized on Sepharose and having a lectin density of 4.5 mg per ml of gel was selected to carry out SPE and its capacity was estimated to be of some tens of μg of hCG per ml of lectin sorbent. Next, the SPE protocol was modified to improve the extraction recoveries. Especially, it was noticed that an extensive pre-conditioning procedure prior to the first use of a cartridge was necessary to remove the residual non-grafted lectins. Indeed, if non-grafted lectins are not eliminated, they may bind a part of hCG glycoforms preventing their retention by the sorbent, leading to low extraction recoveries (around 10 %). With the extensive pre-conditioning procedure, the average extraction recoveries for both hCGα and hCGβ glycoforms were about 50 %, with either recombinant or urinary hCG. Qualitatively, the fractionation of hCG glycoforms between the washing and elution fractions was achieved with the urinary hCG sample by determining the number of glycoforms detected in each fraction. It appears that 12 hCGα glycoforms have a low affinity (detected only in the washing fraction), 1 a low-medium affinity (detected in washing and elution 1 fractions), 16 a medium affinity (detected in washing, elution 1 and 2 fractions), and 12 a high affinity (detected only in elution 1 and 2 fractions). For the hCGβ glycoforms, similarly, 3 have a low affinity and 12 a low-medium affinity. Additionally, the 3 hCGβ glycoforms were detected better. A different behavior was observed with the recombinant hCG sample, which indicates glycosylation differences between the two hCG samples. This shows the potential of lectin-based affinity fractionation before nanoLC-HRMS analysis to better characterize the glycosylation state of hCG at the intact level. • Capacity of Jacalin sorbents were evaluated with recombinant and urinary hCG. • the SPE procedure was developed to improve extraction recoveries. • SPE with Jacalin sorbents led to recoveries of around 50 % for hCG glycoforms. • Jacalin SPE enabled fractionation of hCG glycoforms as a function of their affinity. • lectin SPE and intact protein analysis by nanoLC-HRMS improves hCG characterization. [ABSTRACT FROM AUTHOR]

Published

2025

5. A plant mannose‐binding lectin and fluconazole: Key targets combination against Candida albicans.

Author

Del Rio, Marianela, Radicioni, Melisa B., Mello, Érica O., Ribeiro, Suzanna F. F., Taveira, Gabriel B., Carvalho, André O., de la Canal, Laura, Gomes, Valdirene M., and Regente, Mariana

Subjects

*CANDIDA albicans, *PLANT lectins, *FUNGAL morphology, *CELL morphology, *MICROBIAL cells, *CELL membranes, *FUNGAL growth

Abstract

Aims: This study aimed to evaluate the combined effect of a mannose‐binding lectin Helja with fluconazole (FLC) on Candida albicans and to get insights about the joint action mechanism. Methods and Results: The fungal growth was assessed following the optical density at 630 nm. Fungal cell morphology and nucleus integrity were analysed by flow cytometry and confocal laser scanning microscopy using Calcofluor White (CFW) and 4′,6‐diamidino‐2‐phenylindole (DAPI) staining respectively. The basis of Helja + FLC action on cell wall and plasma membrane was analysed using perturbing agents. The Helja + FLC combination exhibited an inhibitory effect of fungal growth about three times greater than the sum of both compounds separately and inhibited fungal morphological plasticity, an important virulence attribute associated with drug resistance. Cells treated with Helja + FLC showed morphological changes, nucleus disintegration and formation of multimera structures, leading to cell collapse. Conclusions: Our findings indicate that the Helja + FLC combination exhibited a potent antifungal activity based on their simultaneous action on different microbial cell targets. Significance and Impact of Study: The combination of a natural protein with conventional drugs might be helpful for the design of effective therapeutic strategies against Candida, contributing to minimize the development of drug resistance and host cell toxicity. [ABSTRACT FROM AUTHOR]

Published

2022

6. Ghrelin and Jacalin Localization in Developing Rat Kidney.

Author

Rashwan, Ahmed M., Noreldin, Ahmed E., Mahmoud, Sahar F., Elewa, Yaser H. A., and Nomir, Ahmed G.

Subjects

*GHRELIN, *CARRIER proteins, *KIDNEYS, *RATS, *GLYCOPROTEINS

Abstract

Introduction: Lectins are hormone consists of carbohydrate binding proteins that perceive explicit epitopes present on certain glycoproteins and play roles in metabolism. Materials and Methods: Here we examined the localization of two different lectins, ghrelin and jacalin, in rat kidney of both sexes at neonatal 20 days and postnatal 1, 2, 4, 6, 8 and 12 weeks by immunohistochemistry. Results: Ghrelin and jacalin were found in the intrarenal kidney from neonatal day 20. Ghrelin immunoreactivity was mild in the proximal convoluted tubule (PCT), slightly stronger in the distal convoluted tubule (DCT), and absent in the renal corpuscle (RC). In contrast, jacalin immunoreactivity was intense in the RC but absent in the PCT and DCT. At postnatal one week, the ghrelin intensity increased and started to appear in the glomerular capillary of the RC and collecting duct (CD), while the jacalin immunoreactivity was intense in the RC, collecting tubules (CT), and loop of Henle. At postnatal two weeks, ghrelin immunoreactivity was intense in the DCT, CT, and loop of Henle, while jacalin immunoreactivity was intense in the RC, CD, and CT. It was also high in the DCT but mild in the PCT. From four weeks until 12 weeks, the localization of the two lectins was the same, and the immunoreactivity increased with age. Conlusions: Our research elucidates the neonatal and postnatal intra-renal localization of ghrelin and jacalin. [ABSTRACT FROM AUTHOR]

Published

2022

7. Immunomodulatory Effects of Jacalin, a Dietary Plant Lectin on the Peripheral Blood Mononuclear Cells (PBMCs).

Author

Lavanya, V., Bommanabonia, Anil Kumar, Ahmed, Neesar, and Jamal, Shazia

Abstract

The tumor microenvironment that refers to the tumor's surroundings is a key modulator of tumor growth and invasion. The tumor-derived signals are known to downregulate the anti-tumor effects of the effector cells present in the TME. Thus, the cross-talk between the tumor cells with the surrounding immune cells helps in evading the tumor surveillance as well as aiding in tumor growth and proliferation. Hence, knowledge regarding the effects of drugs/compound on the tumor-stromal interactions is gaining importance. In the present study, the effects of jacalin, a dietary lectin on the proliferation and cytokine production of peripheral blood mononuclear cells (PBMCs), are investigated. Jacalin was shown to act as a mitogen of PBMCs, the key cytokine secreting immune cells. Also, jacalin initially induced increased mRNA expression of pro-inflammatory cytokine IFN-γ; however, prolonged stimulation of PBMCs resulted in increased expression of anti-inflammatory cytokine, mainly TGF-β. Furthermore, 6 h jacalin prestimulated PBMCs (Jac-PBMCs) were shown to inhibit HeLa cell proliferation while 24 h Jac-PBMCs were found to favor tumor growth. Thus, it may be postulated that while jacalin initially polarizes the PBMCs to hinder the tumor growth, after a stipulated time point, interaction of jacalin with PBMCs can lead to an immunosuppressive TME that may probably assist in tumor growth and progression. [ABSTRACT FROM AUTHOR]

Published

2022

8. Effect of Key Parameters on Jacalin Extraction from Aqueous Phase into Anionic Reverse Micelles

Author

Sharifah Fathiyah Sy Mohamad, Farhan Mohd Said, Mimi Sakinah Abdul Munaim, and Shahril Mohamad

Subjects

Reverse micelles, sodium bis(2-ethylhexyl) sulfosuccinate (AOT), Jacalin, Forward extraction efficiency (FEE), Chemistry, QD1-999

Abstract

This study demonstrates the extraction of jacalin from crude extract of jackfruit seeds using anionic surfactant based reverse micellar system, sodium bis(2-ethylhexyl) sulfosuccinate (AOT) in isooctane. Effects of various parameters, such as, NaCl concentration (0.05 – 1 M), pH of aqueous phase (pH 4 – 10), AOT concentration (5 – 150 mM), contact time (5 – 30 min) and phase volume ratio (0.5-5) on the transfer efficiency of jacalin was evaluated by changing one factor at a time (OFAT) while keeping the other parameters constant. A maximum of 83% of protein transfer was achieved after equal volume of organic and aqueous phase was stirred for 20 min using 20 mM AOT at pH 5 aqueous phase containing 0.1 M NaCl. The findings demonstrated AOT reverse micellar system as a promising and effective method to extract and purify jacalin from crude protein mixture.

Published

2019

9. Gene Expression Patterns for Proteins With Lectin Domains in Flax Stem Tissues Are Related to Deposition of Distinct Cell Wall Types

Author

Natalia Petrova, Alsu Nazipova, Oleg Gorshkov, Natalia Mokshina, Olga Patova, and Tatyana Gorshkova

Subjects

plant lectins, flax, jacalin, malectin, amaranthin, gene expression, Plant culture, SB1-1110

Abstract

The genomes of higher plants encode a variety of proteins with lectin domains that are able to specifically recognize certain carbohydrates. Plants are enriched in a variety of potentially complementary glycans, many of which are located in the cell wall. We performed a genome-wide search for flax proteins with lectin domains and compared the expression of the encoding genes in different stem tissues that have distinct cell wall types with different sets of major polysaccharides. Over 400 genes encoding proteins with lectin domains that belong to different families were revealed in the flax genome; three quarters of these genes were expressed in stem tissues. Hierarchical clustering of the data for all expressed lectins grouped the analyzed samples according to their characteristic cell wall type. Most lectins differentially expressed in tissues with primary, secondary, and tertiary cell walls were predicted to localize at the plasma membrane or cell wall. These lectins were from different families and had various architectural types. Three out of four flax genes for proteins with jacalin-like domains were highly upregulated in bast fibers at the stage of tertiary cell wall deposition. The dynamic changes in transcript level of many genes for lectins from various families were detected in stem tissue over the course of gravitropic response induced by plant gravistimulation. The data obtained in this study indicate a large number of lectin-mediated events in plants and provide insight into the proteins that take part in tissue specialization and reaction to abiotic stress.

Published

2021

10. Increased ERK phosphorylation and caveolin-1 expression on K562 human chronic myelogenous leukemia cells by jacalin, a dietary plant lectin.

Author

V, Lavanya, Jamal, Shazia, and Ahmed, Neesar

Abstract

The potential antitumor effects of jacalin, the plant lectin that specifically recognizes the tumor-associated Thomsen-Friedenreich antigen has been extensively studied. We had earlier reported jacalin to be mitogenic to K562, the Bcr-Abl expressing erythroleukemia cell line. The dearth of studies highlighting the proliferative effects of jacalin and other lectins motivated us to unveil the mechanism underlying the mitogenic effects of jacalin. Caveolin-1 (cav-1) is an integral membrane protein, known to play a crucial role in cell signaling, lipid transport, and membrane trafficking. The role of cav-1 in tumorigenesis is considered to be controversial as it can suppress as well as promote tumor growth, depending on the cellular context. In the present study, we propose that cav-1 plays the central role in the mitogenic effects of jacalin on the K562 cells. In accordance, the mRNA, as well as protein expression of cav-1 was found to be upregulated in the jacalin-treated K562 cells as compared to the untreated control. Further, jacalin stimulation also increased the phosphorylation of ERK and Akt. The rationale that leads to the initial conjecture about cav-1 was that the sequence of jacalin possesses a cav-1-binding site. [ABSTRACT FROM AUTHOR]

Published

2021

11. Gene Expression Patterns for Proteins With Lectin Domains in Flax Stem Tissues Are Related to Deposition of Distinct Cell Wall Types.

Author

Petrova, Natalia, Nazipova, Alsu, Gorshkov, Oleg, Mokshina, Natalia, Patova, Olga, and Gorshkova, Tatyana

Subjects

PROTEIN domains, GENE expression, PLANT lectins, PROTEIN expression, LECTINS, FLAX, CULTIVARS

Abstract

The genomes of higher plants encode a variety of proteins with lectin domains that are able to specifically recognize certain carbohydrates. Plants are enriched in a variety of potentially complementary glycans, many of which are located in the cell wall. We performed a genome-wide search for flax proteins with lectin domains and compared the expression of the encoding genes in different stem tissues that have distinct cell wall types with different sets of major polysaccharides. Over 400 genes encoding proteins with lectin domains that belong to different families were revealed in the flax genome; three quarters of these genes were expressed in stem tissues. Hierarchical clustering of the data for all expressed lectins grouped the analyzed samples according to their characteristic cell wall type. Most lectins differentially expressed in tissues with primary, secondary, and tertiary cell walls were predicted to localize at the plasma membrane or cell wall. These lectins were from different families and had various architectural types. Three out of four flax genes for proteins with jacalin-like domains were highly upregulated in bast fibers at the stage of tertiary cell wall deposition. The dynamic changes in transcript level of many genes for lectins from various families were detected in stem tissue over the course of gravitropic response induced by plant gravistimulation. The data obtained in this study indicate a large number of lectin-mediated events in plants and provide insight into the proteins that take part in tissue specialization and reaction to abiotic stress. [ABSTRACT FROM AUTHOR]

Published

2021

12. Artocarpus Heterophyllus: Review Study on Potential Activities

Author

Haleel, Mohammed P M, Rashid, K, and Kumar, C. Senthil

Published

2018

13. Targeting the glycan of receptor binding domain with jacalin as a novel approach to develop a treatment against COVID-19

Author

Senthilnathan Rajendaran, Arunchalam Jothi, and Veerappan Anbazhagan

Subjects

jacalin, COVID-19, receptor-binding domain, in silico binding, hydroxychloroquine, human angiotensin-converting enzyme 2, Science

Abstract

In silico analysis revealed that a lectin, jacalin from jackfruit seeds, recognizes a glycosylated region of the receptor-binding domain (RBD) of SARS-CoV2. Jacalin binding induces conformational changes in RBD and significantly affects its interaction with human angiotensin-converting enzyme 2. The result may open up exploration of lectin-based strategies against COVID-19.

Published

2020

14. Immunomodulatory action of jacalin from Artocarpus integrifolia and mannoprotein from Saccharomyces uvarum on the humoral immunity of laying hens

Author

Marco Aurélio Chiara Silva, Miriele Caroline da Silva, João Waine Pinheiro, Raul Jorge Hernan Castro-Goméz, Alice Eiko Murakami, Wagner Loyola, and Emerson José Venancio

Subjects

Artocarpus integrifolia, chickens, IgY, jacalin, mannoprotein, humoral immune response, Saccharomyces uvarum, Agriculture, Agriculture (General), S1-972

Abstract

ABSTRACT: Advances in the fields of glycobiology and immunology have provided many insights into the role of carbohydrate-protein interactions in the immune system. Jacalin of Artocarpus integrifolia (JCA) and structural mannoprotein of Saccharomyces uvarum (MPS) are molecules with immunomodulatory properties. JCA is an IgA human lectin binding molecule that causes the mitogenic stimulation of immune cells, production of cytokines, chemotaxis, and activation of leukocytes. Studies on the immunomodulatory properties of JCA and MPS in mammals and fish suggest that they have an action on antibody production. The aim of this study was to investigate the possible action of JCA and MPS on the production of specific antibodies in laying hens. For this, laying hens were inoculated with an intra abdominal injection of sheep red blood cells (SRBC) with either JCA (0.075 µg, 0.75 µg, and 7.5 µg) or MPS (20 µg and 100 µg). Levels of anti-SRBC antibodies of the IgY, IgM, and IgA classes were evaluated by ELISA. Results showed that JCA and MPS have immunomodulatory effects on levels of anti-SRBC IgM, IgA, and IgY. An immunostimulatory effect of JCA was observed in primary immune response on anti-SRBC IgY, while an inhibitory effect of JCA and MPS was observed in secondary immune response on the production of IgM and IgA anti-SRBC. These results suggested that MPS and JCA have immunomodulatory effects on antibody production and could be used in future studies on humoral immune response in poultry.

Published

2020

15. Immunomodulatory action of jacalin from Artocarpus integrifolia and mannoprotein from Saccharomyces uvarum on the humoral immunity of laying hens.

Author

Silva, Marco Aurélio Chiara, Silva, Miriele Caroline da, Pinheiro, João Waine, Castro-Goméz, Raul Jorge Hernan, Murakami, Alice Eiko, Loyola, Wagner, and Venancio, Emerson José

Subjects

*HENS, *HUMORAL immunity, *ARTOCARPUS, *SACCHAROMYCES, *ANTIBODY formation, *IMMUNOGLOBULIN M, *CHEMOTAXIS

Abstract

Advances in the fields of glycobiology and immunology have provided many insights into the role of carbohydrate--protein interactions in the immune system. Jacalin of Artocarpus integrifolia (JCA) and structural mannoprotein of Saccharomyces uvarum (MPS) are molecules with immunomodulatory properties. JCA is an IgA human lectin binding molecule that causes the mitogenic stimulation of immune cells, production of cytokines, chemotaxis, and activation of leukocytes. Studies on the immunomodulatory properties of JCA and MPS in mammals and fish suggest that they have an action on antibody production. The aim of this study was to investigate the possible action of JCA and MPS on the production of specific antibodies in laying hens. For this, laying hens were inoculated with an intra abdominal injection of sheep red blood cells (SRBC) with either JCA (0.075 µg, 0.75 µg, and 7.5 µg) or MPS (20 µg and 100 µg). Levels of anti-SRBC antibodies of the IgY, IgM, and IgA classes were evaluated by ELISA. Results showed that JCA and MPS have immunomodulatory effects on levels of anti-SRBC IgM, IgA, and IgY. An immunostimulatory effect of JCA was observed in primary immune response on anti-SRBC IgY, while an inhibitory effect of JCA and MPS was observed in secondary immune response on the production of IgM and IgA anti-SRBC. These results suggested that MPS and JCA have immunomodulatory effects on antibody production and could be used in future studies on humoral immune response in poultry [ABSTRACT FROM AUTHOR]

Published

2020

16. CYTOTOXICITY ON MCF7 CELL LINES EXPOSED TO AN EXTRACT OF THE JACALIN FROM JACKFRUIT SEED

Author

M. A, B. Akbar, and Y. Kamaruzzaman

Subjects

Jacalin, jackfruit seed, cytotoxicity, MCF7, crude extract, Science (General), Q1-390

Abstract

Jacalin is a major lectin present in jackfruit seeds, obtained by crude protein recovery. Its lectin symbol is AIL and it belongs to the galactose family of N-acetylglucosamine binding lectins, which are recognized to be cancer cell inhibitor. There have been many pharmacological research studies focusing intensively on jacalin, however their scope was restricted to the application of jacalin in pharmacology. Jacalin or lectin extract from jackfruit seed were induced cell cycle arrest in human breast cancer cell, MCF7, in comparison of crude extract, purified jacalin and jacalin standard. IC50 for MCF7 was achieved at concentration 125 µg/mL, comparable to jacalin standard with only 1.60 % contradictions

Published

2017

17. Cell wall layers delimit cell groups derived from cell division in the foliose trebouxiophycean alga Prasiola japonica.

Author

Mine, Ichiro, Kinoshita, Urara, Kawashima, Shigetaka, and Sekida, Satoko

Subjects

*PLANT cell walls, *CELL division, *PRASIOLA, *MULTICELLULAR organisms, *AGGLUTININS, *PLANTS

Abstract

The cells in the foliose thallus of trebouxiophycean alga Prasiola japonica apparently develop into 2 × 2 cell groups composed of two two-celled groups, each of which is a pair of derivative cells of the latest cell division. In the present study, the structural features of cell walls of the alga P. japonica concerning the formation of the cell groups were investigated using histochemical methods. Thin cell layers stained by Calcofluor White appeared to envelope the two-celled and four-celled groups separately and, hence, separated them from neighboring cell groups, and the Calcofluor White-negative gaps between neighboring four-celled groups were specifically stained by lectins, such as soybean agglutinin, jacalin, and Vicia villosa lectin conjugated with fluorescein. These results indicated that the Calcofluor White-positive cell wall layer of parent cell that existed during two successive cell divisions structurally distinguished two-celled and four-celled groups from others in this alga. Moreover, the results suggested that the cell wall components of the Calcofluor White-negative gaps would possibly contribute to the formation of the planar thallus through lateral union of the cell groups. [ABSTRACT FROM AUTHOR]

Published

2018

18. Electrochemical Characterization of CdSe Monolayers Modified with Glycosilated Molecules.

Author

La Ferla, B., D'Orazio, G., Zotti, G., and Vercelli, B.

Subjects

*CADMIUM selenide, *THIN films, *ELECTROCHEMISTRY, *LECTINS, *MOLECULAR self-assembly, *NANOCRYSTALS

Abstract

Abstract: Ultrathin films of CdSe nannocrystals (CdSe‐NCs) modified with glycosilated molecules have shown interesting electrochemical properties which lead to the detection of lectin Jacalin. [ABSTRACT FROM AUTHOR]

Published

2018

19. Jacalin-copper sulfide nanoparticles complex enhance the antibacterial activity against drug resistant bacteria via cell surface glycan recognition.

Author

Ahmed, Khan Behlol Ayaz, Subramaniyan, Siva Bala, Banu, Sanaulla Farisa, Nithyanand, Paramasivam, and Veerappan, Anbazhagan

Subjects

*COPPER sulfide, *NANOPARTICLES, *DRUG resistance in bacteria, *GLYCAN structure, *FLUORESCENCE quenching

Abstract

In any therapeutic modality the usage of drug in high doses often leads to serious side-effects. Herein, we demonstrated a method to enhance the antibacterial efficacy of CuS NPs at lower concentration through interacting with jackfruit seed lectin, jacalin. Fluorescence quenching studies revealed that jacalin form complex with CuS NPs and the association constant was 1.91 × 10 4  M −1 . Upon complex with jacalin, the bacterial minimum inhibitory concentration (MIC) of CuS NPs drastically decreases from 12.5 μM to 0.78 μM. The addition of jacalin specific sugar, galactose to jacalin-CuS NPs complex (JCuS NPs) reverses the MIC from 0.78 μM to 25 μM. Mechanistic study suggests that JCuS NPs kills bacteria in part by reactive oxygen species and membrane damage, but galactose prevents the action of JCuS NPs at 0.78 μM. JCuS NPs successfully reduce (14 fold) A. hydrophila colonization in an infected zerbra fish and rescue them completely from the infection, but galJCuS NPs and CuS NPs were ineffective at 0.78 μM. Collectively, our studies demonstrates that the enhance antibacterial activity of JCuS NPs is likely due to the interaction between the galactose binding site of jacalin and the bacterial strains, as a result NPs are targeted and delivered sufficiently. [ABSTRACT FROM AUTHOR]

Published

2018

20. Sub-Micellar Concentration of Sodium Dodecyl Sulphate Prevents Thermal Denaturation Induced Aggregation of Plant Lectin, Jacalin.

Author

Lavanya, V., Anil Kumar, B., Jamal, Shazia, Khan, Md., and Ahmed, Neesar

Subjects

*SODIUM, *SULFATES, *LECTINS, *PROTEINS, *HEMAGGLUTININ

Abstract

The irreversible thermal unfolding of jacalin, the lectin purified from jackfruit seeds was accompanied by aggregation, where intermolecular interactions among the subunits are favoured over intramolecular interactions. The extent of aggregation increased as a function of temperature, time and protein concentration. The anionic surfactant, sodium dodecyl sulphate (SDS) significantly suppressed the formation of aggregates as observed by turbidity measurements and Rayleigh scattering assay. Moreover, far UV-CD spectra indicate that the protein β sheet transforms into α helical structure, when denatured in the presence of 3 mM SDS. Further, jacalin when heated in the presence of SDS partially retained the hemagglutination activity when jacalin-SDS mixture was diluted to 1:8 factor since 3 mM SDS was found to lyse the red blood cells. Thus, SDS only altered the aggregation behaviour of jacalin by preventing intermolecular hydrogen bonding among the exposed residues but did not completely stabilize the native conformation. [ABSTRACT FROM AUTHOR]

Published

2017

21. Interaction of cadmium sulfide quantum dots with jacalin for specific recognition of cancer cells.

Author

Ayaz Ahmed, Khan Behlol, Raja, Mamilla R. Charan, Mahapatra, Santanu Kar, and Anbazhagan, Veerappan

Subjects

*CADMIUM sulfide, *QUANTUM dots, *CANCER cells, *SURFACE chemistry, *OPTOELECTRONIC devices

Abstract

Surface functionalizations of quantum dots (QDs) are expected to improve their optoelectronic properties and advance their targeting nature, which is highly warranted for application in molecular imaging and biomedical diagnostics. Therefore, an understanding the interaction between surface functionalization agents and QDs is a prerequisite for their application. Herein, we investigated the interaction between cadmium sulfide (CdS) QDs and dietary T-antigen binding lectin (jacalin) isolated from Indian jack fruit seeds. Fluorescence spectroscopy study showed that CdS QDs effectively quenched the intrinsic fluorescence of jacalin. Analysis of fluorescence quenching at a different temperature indicated that the mechanism of interaction is static and a non-radiation energy transfer occurred within the molecules. The obtained binding constant, K a value in the order of 10 4 M −1 at the tested temperature range suggested that the binding affinity between jacalin and CdS QDs is in the same range as those obtained for the interaction of lectin with carbohydrate. Thermodynamic analysis of the binding data, Δ H 0 =−44.24±1.21 kJ mol −1 , Δ S 0 =−60.92±4.10 J mol − 1 K −1 and Δ G 0 =−26.21±0.1 kJ mol −1 suggested that the binding reaction is enthalpy-driven spontaneous process. Hemagglutination activity of jacalin is well preserved even after binding to CdS QDs, indicating that the jacalin-CdS QDs complex can recognize T-antigens of the malignant tissues. To support the claim, we demonstrated selective fluorescence labeling of chronic myeloid leukemia cells, K562 with jacalin-CdS QDs complex. [ABSTRACT FROM AUTHOR]

Published

2017

22. Anti-Neuroblastoma Properties of a Recombinant Sunflower Lectin.

Author

Pinedo, Marcela, Genoula, Melanie, Silveyra, María Ximena, De Oliveira Carvalho, André, Regente, Mariana, Del Río, Marianela, Ribeiro Soares, Júlia, Moreira Gomes, Valdirene, and De La Canal, Laura

Subjects

*AGGLUTININS, *CANCER treatment, *NEUROBLASTOMA, *LECTINS, *ENTEROKINASE

Abstract

According to their sugar recognition specificity, plant lectins are proposed as bioactive proteins with potential in cancer treatment and diagnosis. Helja is a mannose-specific jacalin-like lectin from sunflower which was shown to inhibit the growth of certain fungi. Here, we report its recombinant expression in a prokaryotic system and its activity in neurobalstoma cells. Helja coding sequence was fused to the pET-32 EK/LIC, the enterokinase/Ligation-independent cloning vector and a 35 kDa protein was obtained in Escherichia coli representing Helja coupled to thioredoxin (Trx). The identity of this protein was verified using anti-Helja antibodies. This chimera, named Trx-rHelja, was enriched in the soluble bacterial extracts and was purified using Ni+2-Sepharose and D-mannose-agarose chromatography. Trx-rHelja and the enterokinase-released recombinant Helja (rHelja) both displayed toxicity on human SH-SY5Y neuroblastomas. rHelja decreased the viability of these tumor cells by 75% according to the tetrazolium reduction assay, and microscopic analyses revealed that the cell morphology was disturbed. Thus, the stellate cells of the monolayer became spheroids and were isolated. Our results indicate that rHelja is a promising tool for the development of diagnostic or therapeutic methods for neuroblastoma cells, the most common solid tumors in childhood. [ABSTRACT FROM AUTHOR]

Published

2017

23. Serodiagnosis of human neurocysticercosis using antigenic components of Taenia solium metacestodes derived from the unbound fraction from jacalin affinity chromatography

Author

Gleyce Alves Machado, Heliana Batista de Oliveira, Margareth Leitão Gennari-Cardoso, José Roberto Mineo, and Julia Maria Costa-Cruz

Subjects

neurocysticercosis, Taenia solium, jacalin, Triton X-114, diagnosis, Microbiology, QR1-502, Infectious and parasitic diseases, RC109-216

Abstract

The aim of the present study was to analyse Taenia solium metacestode antigens that were derived from the unbound fraction of jacalin affinity chromatography and subsequent tert-octylphenoxy poly (oxyethylene) ethanol Triton X-114 (TX-114) partitioning in the diagnosis of human neurocysticercosis (NCC). Immunoassays were designed to detect T. solium-specific IgG antibodies by ELISA and immunoblot. Serum samples were collected from 132 individuals who were categorised as follows: 40 had NCC, 62 presented Taenia spp or other parasitic diseases and 30 were healthy individuals. The jacalin-unbound (J unbound ) fraction presented higher sensitivity and specificity rates than the jacalin-bound fraction and only this fraction was subjected to subsequent TX-114 partitioning, resulting in detergent (DJ unbound ) and aqueous (AJ unbound ) fractions. The ELISA sensitivity and specificity were 85% and 84.8% for J unbound , 92.5% and 93.5% for DJ unbound and 82.5% and 82.6% for AJ unbound . By immunoblot, the DJ unbound fraction showed 100% sensitivity and specificity and only serum samples from patients with NCC recognised the 50-70 kDa T. solium-specific components. We conclude that the DJ unbound fraction can serve as a useful tool for the differential immunodiagnosis of NCC by immunoblot.

Published

2013

24. Serological reactivity of different antigenic preparations of Leishmania (Leishmania) amazonensis and the Leishmania braziliensis complex Reatividade sorológica frente a diferentes preparações antigênicas de Leishmania (Leishmania) amazonensis e do complexo Leishmania braziliensis

Author

Adriano Gomes-Silva, Maria Aparecida Souza, Sandra Regina Afonso-Cardoso, Lívia Resende Andrade, Reynaldo Dietze, Elenice Lemos, Alejandro Belli, Silvio Favoreto Júnior, and Marcelo Simão Ferreira

Subjects

Leishmaniose tegumentar americana, Antígenos de isolados Leishmania braziliensis, Antígenos Leishmania amazonensis, Concanavalina-A, Jacalina, American tegmentary leishmaniasis, Antigens from Leishmania braziliensis isolates, Leishmania amazonensis antigens, Concanavalin-A, Jacalin, Arctic medicine. Tropical medicine, RC955-962

Abstract

Total antigen from Leishmania (Leishmania) amazonensis and isolates from the Leishmania braziliensis complex, along with their respective antigenic fractions obtained by affinity chromatography on concanavalin-A-Sepharose and jacalin-agarose columns evaluated using immunoenzymatic ELISA assay. For this, serum samples from 229 patients were used, grouped as American tegmental leishmaniasis (nº=58), visceral leishmaniasis (nº=28), Chagas disease (nº=49), malaria (nº=32), tuberculosis (nº=13) and healthy volunteers (nº=49). Samples from American tegmentary leishmaniasis showed higher reactivity with antigens isolated from the Leishmania braziliensis complex than with antigens from Leishmania amazonensis (pAntígeno total de Leishmania (Leishmania) amazonensis e isolado do complexo Leishmania brazilienis, assim como suas respectivas frações antigênicas obtidas por cromatografia de afinidade em coluna de concanavalina-A ligada a sepharose e Jacalina ligada a agarose foram avaliadas por ensaio imunoenzimático ELISA. Para tanto, foram utilizadas amostras de soros de 229 pacientes agrupadas em leishmaniose tegumentar americana (nº=58), leishmaniose visceral (nº=28), doença de Chagas (nº=49), malaria (nº=32), tuberculose (nº=13) e voluntários saudáveis (nº=49). Houve maior reatividade das amostras de leishmaniose tegumentar americana com a utilização dos antígenos obtidos do isolado do complexo Leishmania braziliensis quando comparado com antígenos de Leishmania amazonensis (p

Published

2008

25. Sustained mitogenic effect on K562 human chronic myelogenous leukemia cells by dietary lectin, jacalin.

Author

Lavanya, V., Ahmed, Neesar, Khan, Md, and Jamal, Shazia

Abstract

Dietary lectins have been shown to affect the proliferation of human cancer cell lines. The anti-proliferative effects of lectins from varied sources have been extensively studied and in some cases, the underlying mechanism has been explored. Except for peanut agglutinin (PNA), the mitogenic effects of no other lectins have been studied in detail. In the present study, we have shown that jacalin, lectin purified from jackfruit ( Artocarpus integrifolia) seeds act as a mitogen for K562, the Bcr-Abl expressing erythroleukemia cell line (K562) and the effect was found to be dose dependent. K562 cells remained in the proliferative state for a longer period even after the withdrawal of jacalin stimulation, thus jacalin was found to induce sustained mitogenic effect on K562 cells. Further, conditioned media from K562 cells treated with jacalin were observed to have the similar mitogenic effect even in the presence of galactose. Importantly, galactose which is a known ligand for jacalin will interact with functionally active jacalin present in the conditioned media and neutralise its effect. In addition, jacalin treatment also resulted in increased mRNA expression levels of pro-inflammatory cytokines including IL-1β, IL-6 and IFN-γ. Our results indicate that jacalin induces secretion of soluble molecules, which maybe responsible for this observed increased proliferation of K562 cells. [ABSTRACT FROM AUTHOR]

Published

2016

26. Detection of Leukemic Cells by using Jacalin as the Biorecognition Layer: A New Strategy for the Detection of Circulating Tumor Cells.

Author

Cancino ‐ Bernardi, Juliana, Marangoni, Valeria S., Faria, HENrique A. M., and Zucolotto, ValtENcir

Subjects

CANCER cells, LEUKEMIA, CANCER diagnosis, ELECTROCHEMISTRY, INDIUM tin oxide

Abstract

The possibility of early cancer diagnosis has inspired the development of electrochemical systems that could improve both cell detection and activity monitoring, especially for circulating tumor cells. In this study, we propose an impedimetric leukemia sensor based on the use of immobilized jacalin, which is a lectin overexpressed in most types of human cancers. The biosensor is prepared through the chemical adsorption of (3-aminopropil)trimetoxisilano on indium tin oxide electrodes, followed by immersion in a jacalin solution. The performance of the jacalin-modified electrodes toward monocytic leukemic cells, THP-1, and myeloblastic leukemic cells, OCI-AMI3, was investigated through electrochemical impedance spectroscopy. Our results revealed that, upon using the jacalin biorecognition layer, the sensors were able to differentiate leukemic cells from healthy monocyte cells, even at low percentage ranges, with limits of detection of 4±1 cells mL−1 for OCI-AMI3 and 3±1 cells mL−1 for THP-1. [ABSTRACT FROM AUTHOR]

Published

2015

27. Interaction of sugar stabilized silver nanoparticles with the T-antigen specific lectin, jacalin from Artocarpus integrifolia.

Author

Ayaz Ahmed, Khan Behlol, Mohammed, Ansari Sulthan, and Veerappan, Anbazhagan

Subjects

*SILVER nanoparticles, *ANTIGENS, *LECTINS, *ARTOCARPUS, *GALACTOSE, *ENERGY transfer

Abstract

The advances in nanomedicine demonstrate the anticancer properties of silver nanoparticles (AgNPs) and considered as an alternative to the available chemotherapeutic agents. Owing to the preferential interaction of Artocarpus integrifolia lectin (jacalin) with Gal β1-3 GalNAc α (a chemically well-defined tumor associated antigen), a study was undertaken to understand the interaction mechanism of AgNPs with jacalin in presence of specific sugar, galactose. Fluorescence spectroscopic analysis revealed that the AgNPs binding significantly quenched the intrinsic fluorescence of jacalin through a static quenching mechanism, and a non-radiative energy transfer occurred within the molecules. Association constants obtained from the interaction of different sugar-stabilized AgNPs with jacalin are in the order of 10 4 M −1 , this is in the same range as those obtained for the interaction of lectin with carbohydrate and hydrophobic ligand. Each subunit of the tetrameric jacalin binds one AgNPs, and the stoichiometry was unaffected by the presence of the specific sugar, galactose. Hemagglutination assay shows that sugar stabilized AgNPs interacts to jacalin at a site that is different from the saccharide-binding site. Analysis of the FTIR spectra of jacalin indicates that the binding of AgNPs does not alter the secondary structure of jacalin. More importantly, AgNPs exists in nano form even after interacting with the lectin. These results suggest that the development of lectin–AgNPs conjugate would be possible for diagnosis and treatment of cancer. [ABSTRACT FROM AUTHOR]

Published

2015

28. From individual proteins to proteomic samples: characterization of O-glycosylation sites in human chorionic gonadotropin and human-plasma proteins.

Author

Bai, Xue, Li, Daoyuan, Zhu, Jing, Guan, Yudong, Zhang, Qunye, and Chi, Lianli

Subjects

*CHORIONIC gonadotropins, *BLOOD proteins, *PROTEIN analysis, *PROTEOMICS, *GLYCOSYLATION, *LIQUID chromatography-mass spectrometry

Abstract

O-glycosylation-site characterization of individual glycoproteins is a major challenge because of the heterogeneity of O-glycan core structures. In proteomic studies, O-glycosylation-site analysis is even more difficult because of the complexity of the sample. In this work, we designed a rapid and convenient workflow for characterizing the O-glycosylation sites of individual proteins and the human-plasma proteome. A mixture of exoglycosidases was used to partially remove O-glycan chains and leave an N-acetylgalacosamine (GalNAc) residue attached to the Ser or Thr residues. The O-glycosylated peptides could then be identified by using liquid chromatography-tandem mass spectrometry (LC-MS-MS) to detect the 203 Da mass increase. Jacalin was used to selectively isolate O-GalNAc glycopeptides before LC-MS-MS analysis, which is optional for individual proteins and necessary for complex human-plasma proteins. Bovine fetuin and human chorionic gonadotropin (hCG) were used to test the analytical workflow. The workflow indicated superior sensitivity by not only covering most previously known O-glycosylation sites but also discovering several novel sites. Using only one drop of blood, a total of 49 O-GalNAc-linked glycopeptides from 36 distinctive glycoproteins in human plasma were identified unambiguously. The approach described herein is simple, sensitive, and global for site analysis of core 1 through core 4 O-glycosylated proteins. [ABSTRACT FROM AUTHOR]

Published

2015

29. Spectroscopic investigation on the interaction of ruthenium complexes with tumor specific lectin, jacalin.

Author

Ayaz Ahmed, Khan Behlol, Reshma, Elamvazhuthi, Mariappan, Mariappan, and Anbazhagan, Veerappan

Subjects

*RUTHENIUM, *METAL complexes, *LECTINS, *ANTINEOPLASTIC agents, *PHARMACEUTICAL chemistry, *METALS in medicine

Abstract

Several ruthenium complexes are regarded as anticancer agents and considered as an alternative to the widely used platinum complexes. Owing to the preferential interaction of jacalin with tumor-associated T-antigen, we report the interaction of jacalin with four ruthenium complex namely, tris(1,10-phenanthroline)ruthenium(II)chloride, bis(1,10-phenanthroline)(N-[1,10]phenanthrolin-5-yl-pyrenylmethanimine)ruthenium(II)chloride, bis(1,10-phenanthroline)(dipyrido[3,2- a :2′,3′- c ]-phenazine)ruthenium(II)chloride, bis(1,10-phenanthroline)(11-(9-acridinyl)dipyrido[3,2-a:2′,3′-c]phenazine)ruthenium(II) chloride. Fluorescence spectroscopic analysis revealed that the ruthenium complexes strongly quenched the intrinsic fluorescence of jacalin through a static quenching procedure, and a non-radiative energy transfer occurred within the molecules. Association constants obtained for the interaction of different ruthenium complexes with jacalin are in the order of 10 5 M −1 , which is in the same range as those obtained for the interaction of lectin with carbohydrate and hydrophobic ligand. Each subunit of the tetrameric jacalin binds one ruthenium complex, and the stoichiometry is found to be unaffected by the presence of the specific sugar, galactose. In addition, agglutination activity of jacalin is largely unaffected by the presence of the ruthenium complexes, indicating that the binding sites for the carbohydrate and the ruthenium complexes are different. These results suggest that the development of lectin–ruthenium complex conjugate would be feasible to target malignant cells in chemo-therapeutics. [ABSTRACT FROM AUTHOR]

Published

2015

30. A modified assay for measuring thymocyte co-stimulatory activity

Author

Sergio R. Dalmau, Claudia S. Freitas, and Wilson Savino

Subjects

thymocyte, co-stimulatory assays, interleukin 1, interleukin 2, MTT, Jacalin, Microbiology, QR1-502, Infectious and parasitic diseases, RC109-216

Abstract

The observation that murine thymocytes increase their proliferation to interleukin 1 (IL-1) in the presence of phytohemagglutinin (PHA) when pre-incubated with interleukin 2 (IL-2) allowed the introduction of a modified assay for the measurement of IL-1 or the search of thymocyte-inducing proliferative activities in biological samples. Pre-incubation of thymocytes for 24 hr with 50 u/ml IL-2, followed by washings, elicited their maximal response to IL-1 in the usual lymphocyte activating factor (LAF) assay. This suggests that sequential events lead to thymocyte activation. The responsiveness is three to five fold greater than, and the total time of assay is the same as that of the LAF assay. Interestingly, pre-incubation with IL-2 renders thymocytes more sensitive than responsive to crude monocyte conditioned media. The use of the MTT colorimetric method for the assessment of thymocyte proliferation, and of the lectin jacalin as a co-mitogen are suggested as alternatives to be used in co-stimulatory assays.

Published

1993

31. Synthesis and characterization of jacalin-gold nanoparticles conjugates as specific markers for cancer cells.

Author

Marangoni, Valeria S., Paino, Ieda M., and Zucolotto, Valtencir

Subjects

*CHEMICAL synthesis, *GOLD nanoparticles, *BIOCONJUGATES, *BIOMARKERS, *NANOPARTICLES, *ENTROPY

Abstract

Highlights: [•] Jacalin was efficiently conjugated with gold nanoparticles. [•] The nanoconjugate formation is driven by an entropic process. [•] The nanoconjugate exhibited high affinity and specificity against K562 cells. [ABSTRACT FROM AUTHOR]

Published

2013

32. ApoB-INDEPENDENT ENZYME IMMUNOASSAY FOR LIPOPROTEIN(a) BY CAPTURE ON IMMOBILIZED LECTIN (JACALIN).

Author

Sreekumar, Anuradha, Mandagini, Geetha, Subramanian, SabarinathP., and Sankunni, AppukuttanP.

Subjects

*ENZYME-linked immunosorbent assay, *LIPOPROTEIN A, *PEROXIDASE, *MICROPLATES, *APOLIPOPROTEIN B, *GLYCANS, *SERUM

Abstract

Enzyme immunoassay for lipoprotein(a) [Lp(a)] using antibodies to both apoB and apo(a) subunits (a-B assay) is shown to be affected by differential masking of apoB by apo(a) and the presence of LDL-Lp(a) adducts. An apoB-independent immunoassay by capturing Lp(a) through its O-glycans on microplate-coated lectin jacalin and quantitation using peroxidase-labeled anti-apo(a) (J-a assay) is described. J-a assay response is linear, more than twice as sensitive as a-B assay, and is suppressed only 18 ± 5% by non-Lp(a) O-glycan-containing proteins of serum. Wide variations in IgA did not significantly affect Lp(a) binding to jacalin (CV = 6.4%). [ABSTRACT FROM PUBLISHER]

Published

2013

33. Green synthesis of silver nanoparticles using Artocarpus heterophyllus Lam. seed extract and its antibacterial activity

Author

Jagtap, Umesh B. and Bapat, Vishwas A.

Subjects

*JACKFRUIT, *SILVER nanoparticles, *ANTIBACTERIAL agents, *PLANT extracts, *BOTANICAL chemistry, *BIOSYNTHESIS

Abstract

Abstract: A novel approach for the green synthesis of silver nanoparticles (AgNPs) from aqueous solution of silver nitrate (AgNO3) by using Artocarpus heterophyllus Lam. seed powder extract (ASPE), as a reducing agent has been reported in the present work. The seed contains Jacalin, a lectin which is a single major protein representing more than 50% of the proteins from the jackfruit crude seed extract having several biological activities. The reaction of ASPE and AgNO3 was carried out in an autoclave at 15psi, 121°C for 5min and the biosynthesis of the AgNPs in solution was monitored by measuring the UV–vis spectroscopy. The morphology and crystalline phase of the NPs were determined using transmission electron microscopy (TEM), selected area electron diffraction (SAED), scanning electron microscopy (SEM) with X-ray energy dispersive spectrophotometer (EDAX) and Fourier transform infrared spectroscopy (FTIR). The AgNPs synthesized were generally found to be irregular in shapes with an average size 10.78nm. The FTIR spectra indicated the role of amino acids, amides group I in the synthetic process. The AgNPs thus obtained showed highly potent antibacterial activity toward Gram-positive (Bacillus cereus, Bacillus subtilis and Staphyloccocus aureus) and Gram-negative (Pseudomonas aeruginosa) microorganisms. The results confirmed that the ASPE is a very good eco friendly and nontoxic source for the synthesis of AgNPs as compared to the conventional chemical/physical methods. Therefore, A. heterophyllus seed provides future opportunities in nanomedicine by tagging nanoparticles with jacalin. [Copyright &y& Elsevier]

Published

2013

34. Recombinant jacalin-like plant lectins are produced at high levels in Nicotiana benthamiana and retain agglutination activity and sugar specificity

Author

Fernandez-del-Carmen, Asun, Juárez, Paloma, Presa, Silvia, Granell, Antonio, and Orzáez, Diego

Subjects

*PLANT lectins, *NICOTIANA benthamiana, *PLANT proteins, *GLYCOSYLATION, *RECOMBINANT proteins, *PHYLOGENY, *PLANT diversity, *MANNOSE

Abstract

Abstract: The plant kingdom is an underexplored source of valuable proteins which, like plant lectins, display unique interacting specificities. Furthermore, plant protein diversity remains under-exploited due to the low availability and heterogeneity of native sources. All these hurdles could be overcome with recombinant production. A narrow phylogenetic gap between the native source and the recombinant platform is likely to facilitate proper protein processing and stability; therefore, the plant cell chassis should be specially suited for the recombinant production of many plant native proteins. This is illustrated herein with the recombinant production of two representatives of the plant jacalin-related lectin (JRLs) protein family in Nicotiana benthamiana using state-of-the-art magnICON technology. Mannose-specific Banlec JRL was produced at very high levels in leaves, reaching 1.0mg of purified protein per gram of fresh weight and showing strong agglutination activity. Galactose-specific jacalin JRL, with its complicated processing requirements, was also successfully produced in N. benthamiana at levels of 0.25mg of purified protein per gram of fresh weight. Recombinant Jacalin (rJacalin) proved efficient in the purification of human IgA1, and was able to discriminate between plant-made and native IgA1 due to their differential glycosylation status. Together, these results show that the plant cell factory should be considered a primary option in the recombinant production of valuable plant proteins. [Copyright &y& Elsevier]

Published

2013

35. Recombinant IgA production: Single step affinity purification using camelid ligands and product characterization

Author

Reinhart, David, Weik, Robert, and Kunert, Renate

Subjects

*IMMUNOGLOBULIN A, *LIGANDS (Biochemistry), *METHOTREXATE, *TETRAHYDROFOLATE dehydrogenase, *CELL lines, *CELL culture

Abstract

Abstract: Immunoglobulins of isotype A (IgA) mediate a key role in mucosal immunity and are promising new immunotherapeutic candidates, but difficulties in obtaining enough material often hamper their in vivo exploration. We established recombinant Chinese hamster ovary (CHO) cells which stably expressed two IgA1 antibodies under serum-free conditions. The two cell lines achieved significantly different specific productivities of 16pg per cell and day and 100 times less, a common phenomenon in recombinant antibody expression which challenges the production and purification process. Polymeric IgA in crude culture supernatants was assembled with J chain and showed expected specificity. We employed an immobilized camelid anti-human alpha-chain VHH ligand and isolated both recombinant IgAs at high purity and yield in a single chromatographic step. The described method was irrespective of the light chain and specificity and may be used as a generic capture step for the isolation of any IgA. Results were compared with a multistep purification process consisting of an affinity step based on immobilized jacalin followed by anion exchange and hydrophobic interaction chromatography. [Copyright &y& Elsevier]

Published

2012

36. Jacalin interaction with human immunoglobulin A1 and bovine immunoglobulin G1: Affinity constant determined by piezoelectric biosensoring.

Author

Pedroso, Mariele M, Pesquero, Naira C, Thomaz, Sandra MO, Roque-Barreira, Maria C, Faria, Ronaldo C, and Bueno, Paulo R

Subjects

*ARTOCARPUS, *CHEMICAL composition of plants, *PROTEIN-protein interactions, *LECTINS, *GALACTOSE, *IMMUNOGLOBULIN A, *IMMUNOGLOBULIN G, *PIEZOELECTRIC devices, *BIOSENSORS, *PIEZOELECTRIC transducers

Abstract

The affinity of the d-galactose-binding lectin from Artocarpus heterophyllus lectin, known as jacalin, with immonuglobulins (Igs) was determined by biofunctionalization of a piezoelectric transducer. This piezoelectric biofunctionalized transducer was used as a mass-sensitive analytical tool, allowing the real-time binding analysis of jacalin–human immunoglobulin A1 (IgA1) and jacalin–bovine IgG1 interactions from which the apparent affinity constant was calculated. The strategy was centered in immobilizing jacalin on the gold electrode's surface of the piezoelectric crystal resonator using appropriate procedures based on self-assembling of 11-mercaptoundecanoic acid and 2-mercaptoethanol thiol's mixture, a particular immobilization strategy by which it was possible to avoid cross-interaction between the proteins over electrode's surface. The apparent affinity constants obtained between jacalin–human IgA1 and jacalin–bovine IgG1 differed by 1 order of magnitude [(8.0 ± 0.9) × 105 vs (8.3 ± 0.1) × 106 L mol−1]. On the other hand, the difference found between human IgA1 and human IgA2 interaction with jacalin, eight times higher for IgA1, was attributed to the presence of O-linked glycans in the IgA1 hinge region, which is absent in IgA2. Specific interaction of jacalin with O-glycans, proved to be present in the human IgA1 and hypothetically present in bovine IgG1 structures, is discussed as responsible for the obtained affinity values. [ABSTRACT FROM PUBLISHER]

Published

2012

37. Human ZG16p recognizes pathogenic fungi through non-self polyvalent mannose in the digestive system.

Author

Tateno, Hiroaki, Yabe, Rikio, Sato, Takashi, Shibazaki, Azusa, Shikanai, Toshihide, Gonoi, Tohru, Narimatsu, Hisashi, and Hirabayashi, Jun

Subjects

*ZYMOGENS, *PATHOGENIC fungi, *MANNOSE, *DIGESTIVE organs, *CARRIER proteins, *PROTEIN microarrays, *CHROMATOGRAPHIC analysis

Abstract

Human zymogen granule protein 16 (ZG16p) contains a Jacalin-like lectin domain, although its glycan-binding properties are not fully understood. Here, we screened the glycan-binding specificity of ZG16p by recently developed glycoconjugate microarray. ZG16p appeared to exhibit selective binding to α- and β-linked mannose-polyacrylamide-biotin probes. In more quantitative analysis using frontal affinity chromatography, dissociation constants to two types of polyvalent mannose, i.e. high-density mannose and yeast mannan, were determined to be 1.3 and 1.7 µM, respectively. Mutation of the evolutionarily conserved amino acid Asp151, which is involved in sugar binding among the Jacalin-related lectins (JRLs), abolished binding activity to mannose. By immunohistochemical staining, ZG16p was specifically detected in mucus-secreting cells of the digestive system such as serosanguineous acinar cells of the parotid gland, acinar cells of the pancreas and goblet cells of the intestine. Finally, we showed that ZG16p recognizes pathogenic Candida and Malassezia species in a polyvalent mannose-dependent manner. We propose that ZG16p is a novel member of mannose-specific JRLs, which recognizes pathogenic fungi through non-self polyvalent mannose in the digestive system. [ABSTRACT FROM PUBLISHER]

Published

2012

38. ArtinM, a d-mannose-binding lectin from Artocarpus integrifolia, plays a potent adjuvant and immunostimulatory role in immunization against Neospora caninum

Author

Cardoso, Mariana R.D., Mota, Caroline M., Ribeiro, Dâmaso P., Santiago, Fernanda M., Carvalho, Julianne V., Araujo, Ester C.B., Silva, Neide M., Mineo, Tiago W.P., Roque-Barreira, Maria C., Mineo, José R., and Silva, Deise A.O.

Subjects

*MANNOSE, *LECTINS, *ARTOCARPUS, *IMMUNOLOGICAL adjuvants, *IMMUNE response, *MORTALITY, *LABORATORY mice

Abstract

Abstract: ArtinM and Jacalin (JAC) are lectins from the jackfruit (Artocarpus integrifolia) that have important role in modulation of immune responses to pathogens. Neospora caninum is an Apicomplexa parasite that causes neuromuscular disease in dogs and reproductive disorders in cattle, with economic impact on the livestock industry. Hence, we evaluated the adjuvant effect of ArtinM and JAC in immunization of mice against neosporosis. Six C57BL/6 mouse groups were subcutaneously immunized three times at 2-week intervals with Neospora lysate antigen (NLA) associated with lectins (NLA+ArtinM and NLA+JAC), NLA, ArtinM and JAC alone, and PBS (infection control). Animals were challenged with lethal dose of Nc-1 isolate and evaluated for morbidity, mortality, specific antibody response, cytokine production by spleen cells, brain parasite burden and inflammation. Our results demonstrated that ArtinM was able to increase NLA immunogenicity, inducing the highest levels of specific total IgG and IgG2a/IgG1 ratio, ex vivo Th1 cytokine production, increased survival, the lowest brain parasite burden, along with the highest inflammation scores. In contrast, NLA+JAC immunized group showed intermediate survival, the highest brain parasite burden and the lowest inflammation scores. In conclusion, ArtinM presents stronger immunostimulatory and adjuvant effect than Jacalin in immunization of mice against neosporosis, by inducing a protective Th1-biased pro-inflammatory immune response and higher protection after parasite challenge. [Copyright &y& Elsevier]

Published

2011

39. Denatured-jacalin derivatives with selective recognition for O-linked glycosides (ST, T, Tn, and STn Type) on IgA1 hinge region

Author

Miyamoto, Keiichi, Kawasaki, Ayaka, Nagata, Yuko, Uraya, Masanori, Kojima, Hisayoshi, Ito, Takanori, Horiuchi, Takashi, Asakawa, Nagisa, and Nomura, Shinsuke

Subjects

*GLYCOSIDES, *LECTINS, *IMMUNOGLOBULIN A, *CHRONIC kidney failure, *KIDNEY diseases, *BLOOD sugar, *ENZYME-linked immunosorbent assay

Abstract

Abstract: Immunoglobulin A1 (IgA1) concentration in the plasma of patients with IgA nephropathy (IgAN) as the cause of renal failure is higher than that in the plasma of normal controls. IgA1 with abnormal sugars is considered to deposit in the glomerular mesangium, aggravating nephritis in IgAN. Jacalin is a lectin that recognizes sugars on IgA1. However, its selective-recognition for normal-type (ST type, NeuAc-α(2,3)-Gal-β(1,3)-GalNAc) and abnormal-type (T type, Gal-β(1,3)-GalNAc; Tn type, GalNAc; STn type, NeuAc-α(2,6)-GalNAc) sugars α-O-linked to serine/threonine in IgA1 is weak. Therefore, jacalin cannot be used for recognizing specific sugar types on IgA1. We attempted to develop a new recognition method for specific sugar types on IgA1 by utilizing the multirecognition capability of jacalin. Its binding abilities were regulated by heat denaturation with suitable template sugar (galactose or N-acetylgalactosamine). Further, we successfully prepared denatured-jacalin derivatives, which recognized ST-/T-type sugars on IgA1, by sugar-immobilized affinity chromatography. Enzyme-linked immunosorbent assay of denatured-jacalin derivatives, showed the ratios of abnormal sugars on IgA1 in the plasma of IgAN patients and normal controls to be approximately 60% and 20%, respectively. The results proved that profiling of sugar types in IgAN can successfully be performed by solely using jacalin derivatives. [ABSTRACT FROM AUTHOR]

Published

2011

40. Immobilization of carbohydrate epitopes for surface plasmon resonance using the Staudinger ligation

Author

Loka, Ravi S. and Cairo, Christopher W.

Subjects

*SURFACE plasmon resonance, *LECTINS, *MICROBIOLOGICAL assay, *WHEAT germ, *DIMETHYL sulfoxide, *ETHYLENEDIAMINE, *AZIDES

Abstract

Abstract: The detection of carbohydrate–protein interactions is often performed using techniques that require surface immobilization of the lectin or the glycan. A commonly used assay for lectin binding is surface plasmon resonance (SPR). We describe an implementation of the Staudinger ligation as a method to immobilize carbohydrate epitopes to a biosensor surface. This was accomplished by first introducing an azide functionality to a carboxymethyldextran surface, followed by reaction with a phosphane-modified carbohydrate ligand. The chemistry employed is extremely mild and was easily adapted to a commercial biosensor system. Using this approach, we investigated the binding of jacalin and wheat germ agglutinin (WGA) to galactose, lactose, and N-acetyl-lactosamine. We observed that WGA binding shows evidence of multivalent interaction with the surface. Additionally, we found that jacalin binding was influenced by the presence of a flexible and hydrophobic galactosyl aglycone. [ABSTRACT FROM AUTHOR]

Published

2010

41. Interaction of aromatic imino glycoconjugates with jacalin: experimental and computational docking studies

Author

Kumar, Amit, Ramanujam, Balaji, Singhal, Nitin Kumar, Mitra, Atanu, and Rao, Chebrolu Pulla

Subjects

*AROMATIC compounds, *GLYCOCONJUGATES, *CARBOHYDRATES, *CHEMISTRY experiments, *AGGLUTINATION, *CALORIMETRY, *IMINES

Abstract

Abstract: Altering the lectin properties by chemically modified glycoconjugates can have profound effect on their biological applications. In the present case, jacalin has been chosen to study the binding aspects toward glycoconjugates modified by connecting aromatic moieties through imine conjugation at their C-1- or C-2-positions. Out of 10 glycoconjugates, the galactosyl–naphthyl imine (1c) was found to be most effective toward agglutination inhibition (260 times better than galactose), quenching fluorescence intensity, and exhibiting greater binding (K a, 1.3×104 M−1) with jacalin. The specific binding of galactose conjugates and the nonspecific binding of other conjugates have been demonstrated based on ITC. Changes in the secondary structures have been addressed by far- and near-UV CD spectroscopy. The present studies demonstrated that galactose-based conjugates bind at carbohydrate recognition domain (CRD) mainly through polar interactions in addition to exhibiting some nonpolar/hydrophobic interactions, whereas the conjugates other than galactose primarily interact through hydrophobic interactions. Binding of galactosyl conjugates at CRD has been further demonstrated by rigid docking. [ABSTRACT FROM AUTHOR]

Published

2010

42. Modulation of PP2A activity by Jacalin: is it through caveolae and ER chaperones?

Author

Ahmed, Neesar, Pany, Satyabrata, Rahman, Aejazur, Srivastava, Saumya, Sneh, Amita, and Krishnasastry, Musti

Abstract

Plant lectins have been reported to affect the proliferation of different human cancer cell line probably by binding to the specific carbohydrate moieties. In the present study, Badan labeled single cysteine mutant (present in the caveolin-1 binding motif) of jacalin (rJacalin) was found to penetrate the target membrane, indicating a protein-protein or protein-membrane interaction apart from its primary mode of binding i.e. protein-carbohydrate interaction. Further, Jacalin treatment has resulted in the movement of the GFP-Caveolin-1 predominantly at the cell-cell contact region with much restricted dynamics. Jacalin treatment has resulted in the perinuclear accumulation of PP2A and dissociation of the PHAP1/PP2A complex. PP2A was found to act as a negative regulator of ERK signaling and a significant decrease in the phosphorylation level of MEK and AKT (T308) in A431. In addition, we have also identified several ER resident proteins including molecular chaperones like ORP150, Hsp70, Grp78, BiP of A431 cells, which were bound to the Jacalin-sepharose column. Among various ER chaperones that were identified, ORP150 was found to present on the cell surface of A431 cells. [ABSTRACT FROM AUTHOR]

Published

2010

43. Artocarpus: A review of its traditional uses, phytochemistry and pharmacology

Author

Jagtap, U.B. and Bapat, V.A.

Subjects

*ARTOCARPUS, *BOTANICAL chemistry, *PHARMACOLOGY, *TRADITIONAL medicine, *PHENOLS

Abstract

The genus Artocarpus (Moraceae) comprises about 50 species of evergreen and deciduous trees. Economically, the genus is of appreciable importance as a source of edible fruit, yield fairly good timber and is widely used in folk medicines. The aim of the present review is to present comprehensive information of the chemical constituents, biological and pharmacological research on Artocarpus which will be presented and critically evaluated. The close connection between traditional and modern sources for ethnopharmacological uses of Artocarpus species, especially for treatment against inflammation, malarial fever, diarrhoea, diabetes and tapeworm infection. Artocarpus species are rich in phenolic compounds including flavonoids, stilbenoids, arylbenzofurons and Jacalin, a lectin. The extracts and metabolites of Artocarpus particularly those from leaves, bark, stem and fruit possess several useful bioactive compounds and recently additional data are available on exploitation of these compounds in the various biological activities including antibacterial, antitubercular, antiviral, antifungal, antiplatelet, antiarthritic, tyrosinase inhibitory and cytotoxicity. Several pharmacological studies of the natural products from Artocarpus have conclusively established their mode of action in treatment of various diseases and other health benefits. Jacalin, a lectin present in seeds of this plant has a wide range of activities. Strong interdisciplinary programmes that incorporate conventional and new technologies will be critical for the future development of Artocarpus as a promising source of medicinal products. In the present review, attempts on the important findings have been made on identification; synthesis and bioactivity of metabolites present in Artocarpus which have been highlighted along with the current trends in research on Artocarpus. [Copyright &y& Elsevier]

Published

2010

44. Group epitope mapping considering relaxation of the ligand (GEM-CRL): Including longitudinal relaxation rates in the analysis of saturation transfer difference (STD) experiments

Author

Kemper, Sebastian, Patel, Mitul K., Errey, James C., Davis, Benjamin G., Jones, Jonathan A., and Claridge, Timothy D.W.

Subjects

*LIGAND binding (Biochemistry), *GENE mapping, *EPITOPES, *MOLECULAR relaxation, *PROTEINS, *NUCLEAR magnetic resonance spectroscopy, *MAGNETIZATION

Abstract

Abstract: In the application of saturation transfer difference (STD) experiments to the study of protein–ligand interactions, the relaxation of the ligand is one of the major influences on the experimentally observed STD factors, making interpretation of these difficult when attempting to define a group epitope map (GEM). In this paper, we describe a simplification of the relaxation matrix that may be applied under specified experimental conditions, which results in a simplified equation reflecting the directly transferred magnetisation rate from the protein onto the ligand, defined as the summation over the whole protein of the protein–ligand cross-relaxation multiplied by with the fractional saturation of the protein protons. In this, the relaxation of the ligand is accounted for implicitly by inclusion of the experimentally determined longitudinal relaxation rates. The conditions under which this “group epitope mapping considering relaxation of the ligand” (GEM-CRL) can be applied were tested on a theoretical model system, which demonstrated only minor deviations from that predicted by the full relaxation matrix calculations (CORCEMA-ST) . Furthermore, CORCEMA-ST calculations of two protein–saccharide complexes (Jacalin and TreR) with known crystal structures were performed and compared with experimental GEM-CRL data. It could be shown that the GEM-CRL methodology is superior to the classical group epitope mapping approach currently used for defining ligand–protein proximities. GEM-CRL is also useful for the interpretation of CORCEMA-ST results, because the transferred magnetisation rate provides an additional parameter for the comparison between measured and calculated values. The independence of this parameter from the above mentioned factors can thereby enhance the value of CORCEMA-ST calculations. [Copyright &y& Elsevier]

Published

2010

45. Specific interaction of jacalin with phycocyanin, a fluorescent phycobiliprotein

Author

Pandey, Gunjan, Fatma, Tasneem, Cowsik, Sudha M., and Komath, Sneha Sudha

Subjects

*PROTEIN-protein interactions, *PLANT lectins, *PHYCOBILIPROTEINS, *PHOTOCHEMOTHERAPY, *PORPHYRINS, *CANCER cells

Abstract

Abstract: Recent research has shown that, like porphyrins, phycocyanin (PC) too can produce singlet oxygen upon excitation with the appropriate radiation and hence could be useful in photodynamic therapy (PDT) for cancer. Unlike porphyrins, PC has the advantage of being a non-toxic, non-carcinogenic, soluble protein. However, the challenge would be to target the fluorescent phycobiliprotein to malignant cells. We report here that the tumor-specific lectin, jacalin, binds PC specifically in a carbohydrate-independent manner and with affinities better than that for porphyrins. Hence the lectin could prove to be a useful carrier for targeted delivery of PC. The interaction involves both ionic and hydrophobic interactions and more than one contact site. [Copyright &y& Elsevier]

Published

2009

46. Surface analysis of pure and complex mucin coatings on a real-type substrate using individual and combined mBCA, ELLA, and ELISA

Author

Sandberg, Tomas, Mellin, Lisa, Gelius, Ulrik, and Caldwell, Karin D.

Subjects

*SURFACE chemistry, *MUCINS, *SURFACE coatings, *SUBSTRATES (Materials science), *BIOLOGICAL assay, *ENZYME-linked immunosorbent assay, *LECTINS, *QUANTITATIVE chemical analysis

Abstract

Abstract: In the past, we introduced the idea of using mucin coatings to improve biomaterials performance. Here, we evaluate non-radioactive methods for the analysis of pure and human host protein-containing (complex) mucin coatings on a real-type substrate (Thermanox). A common protein quantification assay (mBCA) was combined with mass-calibrated, enzyme-amplified assays based on lectin (ELLA) and antibody (ELISA) recognition, to determine the total and specific amounts of surface-associated proteins. Model studies showed the mBCA assay to be of limited use at low mass loads, and steric effects to influence the ELLA at high surface layer densities. Non-specific responses due to substrate interaction were low for the ELLA and ELISAs. Cross-reactions were observed during ELLA analysis of analytes sharing high degree of O-glycosylation. Combined mBCA–ELLA–ELISA analysis suggested that mucin desorption was low upon protein addition and that low concentrations of ELISA-determined protein for the complex coatings could be explained in terms of low accessibility of proteins to the bulk environment. Specifically, a methodology is presented for the determination of the fraction of surface-exposed, presumed bioactive proteins in a complex mucin coating. Finally, X-ray photoelectron spectroscopy and infrared reflectance spectroscopy combined with multivariate data analysis were proven useful in the evaluation of mucin-based coatings. [Copyright &y& Elsevier]

Published

2009

47. Rhizoid differentiation of Spirogyra is regulated by substratum.

Author

Ikegaya, Hisato, Sonobe, Seiji, Murakami, Kohei, and Shimmen, Teruo

Subjects

*SPIROGYRA, *RHIZOIDS, *ZYGNEMATACEAE, *MORPHOLOGY, *LECTINS

Abstract

Some species of Spirogyra can anchor to substratum with rod- or rosette-shaped rhizoid (hapteron). The rhizoid differentiation can be induced by cutting algal filaments in a laboratory. Requirement of contact stimulation for rhizoid differentiation has been reported (Nagata in Plant Cell Physiol 14:531–541, ). However, the control mechanism of rhizoid morphology has not been elucidated. When cut filaments were incubated on the glass surface, start of tip growth, secretion of lectin-binding material and callose synthesis were observed. In the absence of contact to the glass surface, none of above phenomena was induced. Systematic analysis showed that rosette-shaped rhizoid was formed only on the hydrophobic substratum. On the hydrophobic substratum, both Bandeiraea (Griffonia) simplicifolia lectin and jacalin strongly stained the rhizoids. On the hydrophilic substratum, however, only Bandeiraea (Griffonia) simplicifolia lectin strongly stained the rhizoids. [ABSTRACT FROM AUTHOR]

Published

2008

48. THESES.

Abstract

The article presents abstracts of neuropsychiatry research including the primary headaches and generalized anxiety disorder comorbidity, the role of melatonin in migraine and comorbidities and the evaluation of taenia saginata metacestodes antigenic fractions for the diagnosis of human neurocysticercosis.

Published

2008

49. Galectin-1, an endogenous lectin produced by arterial cells, binds lipoprotein(a) [Lp(a)] in situ: Relevance to atherogenesis

Author

Chellan, Bijoy, Narayani, Jayakumari, and Appukuttan, Padinjaradath S.

Subjects

*GLYCOSYLATION, *IMMUNE complexes, *CARRIER proteins, *BLOOD vessels

Abstract

Abstract: Lipoprotein(a) [Lp(a)], a modified LDL molecule, is implicated in atherogenesis. Mechanisms of the accumulation of [Lp(a)] in atherosclerotic vessels is lacking in literature. We sought to investigate the complementarities of the carbohydrate structures on Lp(a) and LDL with galectin-1(a carbohydrate binding protein) and whether endogenous galectin-1 binds Lp(a) in situ. We investigated T-antigen structures on Lp(a) and LDL by enzyme-linked lectin assay using T-antigen specific lectins, galectin-1 and jacalin. Both jacalin and galectin-1 bound strongly to Lp(a) and to a much lesser extent, to LDL. Galectin-1 recognition of the lipoproteins was abolished when the O-linked sugars were selectively removed. Localization of endogenous galectin-1 within histological sections of human internal mammary artery and in vitro binding of Lp(a) to the tissues was analyzed by immunohistochemical staining. The Lp(a)-binding pattern was found to overlap with the localization of galectin-1. The poor Lp(a)-binding on inhibiting tissue galectin-1 with lactose, suggested the binding of Lp(a) to galectin-1. This may be suggestive of a mechanism by which Lp(a) accumulates within arterial walls in atherogenesis. [Copyright &y& Elsevier]

Published

2007

50. Isolation of Bovine Immunoglobulins Resistant to Peptic Digestion: New Perspectives in the Prevention of Failure in Passive Immunization of Neonatal Calves.

Author

Porto, A. C. R. C., Oliveira, L. L., Ferraz, L. C., Ferraz, L. E. S., Thomaz, S. M. O., Rosa, J. C., and Roque-Barreira, M. C.

Subjects

*IMMUNIZATION, *DIGESTION, *CALVES, *LECTINS, *IMMUNOGLOBULINS, *PEPTIDES, *IMMUNOTHERAPY, *COLOSTRUM

Abstract

In calves, neonatal mortality and disease susceptibility are greatly influenced by failure in passive immunization, normally provided by colostrum ingestion just after birth. Formulations projected to replace natural colostrum have not been successful, and one of the possible reasons for such failure is that orally administered Ig are probably digested in the gastrointestinal tract, so they are not absorbed as intact functional molecules. With the aim of finding an adequate colostrum substitute, we used columns of immobilized jacalin, a lectin known by its ability to bind O-linked oligosaccharides, to obtain a colostral Ig population putatively protected against enzymatic cleavage by the presence of sugar chains. Immunoglobulin G1 is a major constituent of colostrum Ig bound to jacalin (JB-Ig). This preparation contains 10% of the total colostral Ig and is typically 3 to 6 times more resistant to pepsin digestion than the Ig contained in the fraction that is not bound to jacalin, which presumably does not contain O-glycans. Mass spectrometry analysis demonstrated that the tryptic peptides obtained from JB-Ig and unbound Ig were similar, indicating that their distinct susceptibility to enzyme hydrolysis was associated with differences in their sugar chains. Therefore, the present research suggests that the bovine colostrum JB-Ig has potential application in the immunotherapy of neonatal calves that have not been supplied with colostrum. [ABSTRACT FROM AUTHOR]

Published

2007