Your search keyword '"Sulfation"' showing total 5,940 results

1. Sulfated galactofucan from Sargassum fusiforme protects against postmenopausal osteoporosis by regulating bone remodeling.

Author

Yizhong, Bao, Chen, Fen, Jin, Weihua, Dai, Jihua, Mao, Genxiang, and Song, Boshan

Subjects

*OSTEOPOROSIS in women, *BONE diseases, *OLDER women, *BONE remodeling, *SULFATION

Abstract

Osteoporosis is a degenerative bone disease highly prevalent in older women, causing high morbidity and mortality rates. Fourteen kinds of fucoidan were isolated from Sargassum fusiforme through acid (named as SFS), alkaline (SFJ) and water (SFW). SFW was passed through an anion exchange column to obtain SFW-0, SFW-0.5 and SFW-2. SFW-0.5 and SFW-2 were degraded to obtain different sulfate group contents SFW-x-M/S/O (x for 0.5 or 2). We further confirmed SFW-0.5-O was the most effective fraction of SFW. SFW-0.5-O may have alternating backbones of (Gal)n and (Fuc)n, and the main sulfation may be at C2/C3 of the Fuc/Gal residues. SFW-0.5-O inhibition of OC differentiation was associated with IRF-8 signaling; meanwhile, SFW-0.5-O promoted osteoblast differentiation and bone mineral nodule formation. SFW-0.5-O also effectively ameliorated osteoporosis symptom caused by estrogen deprivation in vivo. We uncovered that the fucoidan active fraction SFW-0.5-O demonstrated effective bone protection, may be exploited for osteoporosis therapy. Fucoidan active ingredient SFW-0.5-O can effectively inhibit osteoclastogenesis, promote osteoblast differentiation, and improve osteoporosis symptoms caused by estrogen deprivation. [ABSTRACT FROM AUTHOR]

Published

2024

2. Systematic Characteristics of Fucoidan: Intriguing Features for New Pharmacological Interventions.

Author

Jeong, Seungjin, Lee, Seokmin, Lee, Geumbin, Hyun, Jimin, and Ryu, Bomi

Subjects

*BROWN algae, *BIODIVERSITY, *SULFATION, *MOLECULAR weights, *DRUG therapy

Abstract

Fucoidan, a sulfated polysaccharide found primarily in brown algae, is known for exhibiting various biological activities, many of which have been attributed to its sulfate content. However, recent advancements in techniques for analyzing polysaccharide structures have highlighted that not only the sulfate groups but also the composition, molecular weight, and structures of the polysaccharides and their monomers play a crucial role in modulating biological effects. This review comprehensively provides the monosaccharide composition, degree of sulfation, molecular weight distribution, and linkage of glycosidic bonds of fucoidan, focusing on the diversity of its biological activities based on various characteristics. The implications of these findings for future applications and potential therapeutic uses of fucoidan are also discussed. [ABSTRACT FROM AUTHOR]

Published

2024

3. 硫酸化修饰对椰子吸器多糖结构和 抗氧化活性的影响.

Author

阚金涛, 皮正林, 杨锴莉, 赵津好, 刘笑焱, and 张玉锋

Subjects

IRON ions, HYDROXYL group, POLYSACCHARIDES, URONIC acids, SULFATION

Abstract

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Published

2024

4. Site-specific sulfations regulate the physicochemical properties of papillomavirus-heparan sulfate interactions for entry.

Author

Bano, Fouzia, Soria-Martinez, Laura, van Bodegraven, Dominik, Throsteinsson, Konrad, Brown, Anna M., Fels, Ines, Snyder, Nicole L., Bally, Marta, and Schelhaas, Mario

Subjects

*HUMAN papillomavirus, *SULFATION, *HEPARAN sulfate, *OROPHARYNGEAL cancer, *CAPSIDS, *VIRAL tropism

Abstract

Certain human papillomaviruses (HPVs) are etiological agents for several anogenital and oropharyngeal cancers. During initial infection, HPV16, the most prevalent cancer-causing type, specifically interacts with heparan sulfates (HSs), not only enabling initial cell attachment but also triggering a crucial conformational change in viral capsids termed structural activation. It is unknown, whether these HPV16-HS interactions depend on HS sulfation patterns. Thus, we probed potential roles of HS sulfations using cell-based functional and physicochemical assays, including single-molecule force spectroscopy. Our results demonstrate that N-sulfation of HS is crucial for virus binding and structural activation by providing high-affinity sites, and that additional 6O-sulfation is required to mechanically stabilize the interaction, whereas 2O-sulfation and 3O-sulfation are mostly dispensable. Together, our findings identify the contribution of HS sulfation patterns to HPV16 binding and structural activation and reveal how distinct sulfation groups of HS synergize to facilitate HPV16 entry, which, in turn, likely influences the tropism of HPVs. [ABSTRACT FROM AUTHOR]

Published

2024

5. A Comparison Study on the Recovery of REEs from Red Mud by Sulfation Roasting–Water Leaching and Citric Acid Leaching.

Author

Shalchian, Hossein, Hajizadeh Navakh, Mohsen, Birloaga, Ionela, Babakhani, Abolfazl, and Vegliò, Francesco

Subjects

*RARE earth metals, *CITRIC acid, *SOLVENT extraction, *ACID solutions, *SULFATION

Abstract

In this study, the recovery of rare earth elements (REEs) from red mud (bauxite residue) was explored through a combination of citric acid leaching and sulfation roasting–water leaching processes, introducing an innovative approach to the field. The research uniquely investigates the influence of citric acid on the leaching behavior of REEs and impurities in both untreated red mud and red mud subjected to sulfation roasting, providing a direct comparison of these methodologies. A novel aspect of this study is the evaluation of solvent extraction efficiency using DEHPA, highlighting the selective recovery of REEs over impurities from both citric acid and water-leaching solutions. Furthermore, a comprehensive phase analysis using X-ray diffraction (XRD) was conducted to track the transformations of minerals during the sulfation roasting process, an original contribution to the literature. The findings revealed that over 85% of REEs and major elements such as Fe, Al, Ca, and Ti dissolved in water after sulfation at 105 °C, while iron and titanium dissolution significantly decreased following roasting at 725 °C. Importantly, terbium, neodymium, and gadolinium extraction efficiencies were notably affected by roasting temperature. Citric acid leaching results demonstrated that the direct leaching of red mud leads to higher leaching efficiency than leaching it after the roasting process. Solvent extraction demonstrated lower terbium and neodymium recovery from citric acid solutions compared to water leaching solution. Finally, stripping experiments illustrated that 6M H2SO4 solution is capable of stripping more than 80% of rare earth elements, except terbium. [ABSTRACT FROM AUTHOR]

Published

2024

6. Chemokine Receptor N-Terminus Charge Dictates Reliance on Post-Translational Modifications for Effective Ligand Capture and Following Boosting by Defense Peptides.

Author

Xu, Ting, Schou, Anne Sophie, Lackman, Jarkko J., Barrio-Calvo, Marina, Verhallen, Lisa, Goth, Christoffer Knak, Jensen, Benjamin Anderschou Holbech, Veldkamp, Christopher T., Volkman, Brian F., Peterson, Francis C., and Hjortø, Gertrud Malene

Subjects

*LIGAND binding (Biochemistry), *POST-translational modification, *ELECTROSTATIC interaction, *SULFATION, *PEPTIDES, *CHEMOKINE receptors

Abstract

The chemokine receptors CCR1 and CCR5 display overlapping expression patterns and ligand dependency. Here we find that ligand activation of CCR5, not CCR1, is dependent on N-terminal receptor O-glycosylation. Release from O-glycosylation dependency is obtained by increasing CCR5 N-terminus acidity to the level of CCR1. Ligand activation of CCR5, not CCR1, drastically improves in the absence of glycosaminoglycans (GAGs). Ligand activity at both CCR1 and CCR5 is boosted by positively charged/basic peptides shown to interact with acidic chemokine receptor N-termini. We propose that receptors with an inherent low N-terminus acidity rely on post-translational modifications (PTMs) to efficiently compete with acidic entities in the local environment for ligand capture. Although crucial for initial ligand binding, strong electrostatic interactions between the ligand and the receptor N-terminus may counteract following insertion of the ligand into the receptor binding pocket and activation, a process that seems to be aided in the presence of basic peptides. Basic peptides bind to the naked CCR1 N-terminus, not the CCR5 N-terminus, explaining the loss of boosting of ligand-induced signaling via CCR5 in cells incapable of glycosylation. [ABSTRACT FROM AUTHOR]

Published

2024

7. Extracellular Matrix Sulfation in the Tumor Microenvironment Stimulates Cancer Stemness and Invasiveness.

Author

Kuşoğlu, Alican, Örnek, Deniz, Dansık, Aslı, Uzun, Ceren, Nur Özkan, Sena, Sarıca, Sevgi, Yangın, Kardelen, Özdinç, Şevval, Sorhun, Duygu Turan, Solcan, Nuriye, Doğanalp, Efe Can, Arlov, Øystein, Cunningham, Katherine, Karaoğlu, Ismail C., Kizilel, Seda, Solaroğlu, Ihsan, Bulutay, Pınar, Fırat, Pınar, Erus, Suat, and Tanju, Serhan

Subjects

*FOCAL adhesion kinase, *PROTEIN-tyrosine kinases, *EXTRACELLULAR matrix, *SULFATION, *LUNG tumors

Abstract

Tumor extracellular matrices (ECM) exhibit aberrant changes in composition and mechanics compared to normal tissues. Proteoglycans (PG) are vital regulators of cellular signaling in the ECM with the ability to modulate receptor tyrosine kinase (RTK) activation via their sulfated glycosaminoglycan (sGAG) side chains. However, their role on tumor cell behavior is controversial. Here, it is demonstrated that PGs are heavily expressed in lung adenocarcinoma (LUAD) patients in correlation with invasive phenotype and poor prognosis. A bioengineered human lung tumor model that recapitulates the increase of sGAGs in tumors in an organotypic matrix with independent control of stiffness, viscoelasticity, ligand density, and porosity, is developed. This model reveals that increased sulfation stimulates extensive proliferation, epithelial‐mesenchymal transition (EMT), and stemness in cancer cells. The focal adhesion kinase (FAK)‐phosphatidylinositol 3‐kinase (PI3K) signaling axis is identified as a mediator of sulfation‐induced molecular changes in cells upon activation of a distinct set of RTKs within tumor‐mimetic hydrogels. The study shows that the transcriptomic landscape of tumor cells in response to increased sulfation resembles native PG‐rich patient tumors by employing integrative omics and network modeling approaches. [ABSTRACT FROM AUTHOR]

Published

2024

8. Metabolic and Pharmacokinetic Profiling Studies of N, N-Dimethylaniline-Heliamine in Rats by UHPLC-Q-Orbitrap MS/MS.

Author

Xi, Ruqi, Abdulla, Rahima, Sherzod, Jurakulov, Ivanovna, Vinogradova Valentina, Habasi, Maidina, and Liu, Yongqiang

Subjects

*BLOOD volume, *CAUSES of death, *SULFATION, *METABOLITES, *GLUCURONIDATION

Abstract

Cardiovascular disease is the first cause of death worldwide and kills more people each year than any other cause of death. N, N-dimethylaniline-heliamine (DH), a synthetic tetrahydroisoquinoline alkaloid, has shown notable antiarrhythmic activity. However, the metabolic processes and pharmacokinetic characteristics of DH in rats have not been studied. This study aims to identify its metabolites, as well as develop and validate a rapid and efficient bioanalytical method for quantifying DH in rat plasma over a wide range of concentrations. Its metabolites were characterized in silico, in vitro, and in vivo. A series of 16 metabolites were identified, of which 12 were phase I metabolites and 4 were phase II metabolites. A low probability of DH binding to DNA, protein, and glutathione is predicted by the in silico model. The main metabolic processes of DH were demethylation, dehydrogenation, glucuronidation, and sulfation. Concentration–time profiles were generated by analyzing the plasma, and the outcomes were analyzed via non-compartmental analysis to identify the pharmacokinetic parameters. Among the detected parameters were the volume of distribution, estimated at 126,728.09 ± 56,867.09 mL/kg, clearance at 30,148.65 ± 15,354.27 mL/h/kg, and absolute oral bioavailability at 16.11%. The plasma distribution volume of DH was substantially higher than the overall plasma volume of rats, which suggests that DH has a specific tissue distribution in rats. This study suggests that DH is appropriately bioavailable and excreted via a variety of routes and has low toxicity. [ABSTRACT FROM AUTHOR]

Published

2024

9. Enhanced Photocatalytic Degradation of Herbicide 2,4-Dichlorophenoxyacetic Acid Using Sulfated CeO 2.

Author

Rodríguez, Carlos, Castañeda, Claudia, Sosa, Edwin, Martínez, José J., Mancipe, Sonia, Rojas, Hugo, Tzompantzi, Francisco, and Gómez, Ricardo

Subjects

*PRECIPITATION (Chemistry), *SULFATION, *CERIUM oxides, *PHOTODEGRADATION, *INFRARED spectroscopy

Abstract

The present study presents the results obtained from evaluating the photocatalytic behavior of a series of sulfated CeO2 materials in the photocatalytic degradation of the herbicide 2,4-dichlorophenoxyacetic acid. The CeO2 photocatalytic support was prepared using the precipitation synthesis method. Subsequently, the support was wetly impregnated with different contents of sulfate ions (0.5, 1.0, and 2.0 wt.%). The materials were characterized using X-ray diffraction, nitrogen physisorption, infrared spectroscopy, diffuse reflectance UV–Vis spectrophotometry, and thermal analysis. The characterization results showed that the sulfation of the material promoted an increase in the surface area and a decrease in the average size of the crystallites. Likewise, it was possible to demonstrate the surface sulfation of the support through bidentate coordination of the sulfate groups to the semiconductor metal. Concerning photoactivity, the convenience of the surface modification of CeO2 was confirmed because the sulfate groups acted as capturers of the electrons generated during the photocatalytic process, reducing the frequency of recombination of the charge carriers and allowing the availability of the gaps to favor the degradation reaction of the contaminant. Finally, it was evident that a percentage of 1.0 wt.% of the sulfate anion is the optimal content to improve the photocatalytic properties of CeO2. [ABSTRACT FROM AUTHOR]

Published

2024

10. Effects of Sulfated Modification on the Structural Characterization and Antioxidant Activities of Coconut (Cocos nucifera L.)Haustorium Polysaccharide

Author

Jintao KAN, Zhenglin PI, Kaili YANG, Jinhao ZHAO, Xiaoyan LIU, and Yufeng ZHANG

Subjects

coconut haustorium polysaccharide, sulfation, substitution degree, antioxidant activity, structure property, Food processing and manufacture, TP368-456

Abstract

To investigate the effect of sulfated modification on the structure and function of coconut haustorium polysaccharide (CHP), three kinds of sulfated coconut haustorium polysaccharides (SCHP-2, SCHP-3, and SCHP-4) were prepared using sulfation reagents containing different ratios of chlorosulfonic acid and pyridine (v/v, mL/mL: 1/2, 1/3, and 1/4) after extracting CHP from the raw materials of coconut haustorium, and their basic chemical compositions, structural characteristics and antioxidant activity in vitro were compared and analyzed. Results showed that all three sulfation reagents were able to modify CHP (characteristic peaks of S=O and C-O-S were observed near 1100~1250 cm−1 and 820 cm−1 in infrared spectra, respectively), and the degree of substitution (DS) was the highest (0.75) at the ratio of chlorosulfonic acid and pyridine for 1/2. The total sugar, uronic acid content, and molecular weight of the three SCHP decreased, and the molar content of monosaccharides also changed when comparing with that of CHP. The thermal stability had slightly weakened as well (the degradation temperature of polysaccharides decreased from 211.17 ℃ and 282.01 ℃ of CHP to 194.86~207.70 ℃ and 233.35~262.46 ℃ of SCHP, respectively). The results of antioxidant experiments in vitro showed that the scavenging activity of SCHP on DPPH and hydroxyl radicals was lower than that of CHP, and the larger the DS was, the more obvious the decrease in activity was. In terms of the ABTS+ radicals scavenging ability and ferrous ions chelating activity, increasing DS could enhance the activity of SCHP. At 8 mg/mL, the ABTS+ radicals scavenging rate (54.82%) and ferrous ions chelating rate (15.59%) of SCHP-2 were significantly (P

Published

2024

11. Enzymatically cross-linkable sulfated bacterial polyglucuronic acid as an affinity-based carrier of FGF-2 for therapeutic angiogenesis.

Author

Goto, Ryota, Sakai, Shinji, Delattre, Cédric, Petit, Emmanuel, El Boutachfaiti, Redouan, and Nakahata, Masaki

Subjects

*HORSERADISH peroxidase, *HEMATOPOIESIS, *AQUEOUS solutions, *NEOVASCULARIZATION, *SULFATION

Abstract

The fibroblast growth factor-2 (FGF-2) is a critical protein for biological processes such as angiogenesis and tissue regeneration. Recently, hydrogels based on semi-synthetic sulfated polysaccharides have been developed for the controlled delivery of FGF-2. These affinity-based FGF-2 carriers utilizing hydrogels based on sulfated polysaccharides enable sustained delivery of FGF-2, yet choice of materials is limited. Here, we demonstrate a novel synthetic sulfated polysaccharide-based hydrogel based on bacterial polyglucuronic acid (PGU). We synthesized phenol-grafted sulfated PGU (PGUS-Ph), an enzymatically cross-linkable PGU derivative that exhibited an enhanced affinity for FGF-2. The aqueous solution of PGUS-Ph, when combined with FGF-2, could be injected into affected sites and form a hydrogel in a minimally invasive manner. The FGF-2 released from the PGUS-Ph hydrogel induced blood vessel formation, as proven by a chick embryo-based angiogenesis assay. Our results indicate that the PGUS-Ph has the potential as an enzymatically cross-linkable and minimally invasively injectable affinity-based FGF-2 delivery system. [ABSTRACT FROM AUTHOR]

Published

2024

12. Commercially available carrageenans show broad variation in their structure, composition, and functionality.

Author

Hale, Julia, Gerhäuser, Julian, Gaukel, Volker, and Wefers, Daniel

Subjects

*FOOD additives, *RED algae, *DISACCHARIDES, *POLYSACCHARIDES, *SULFATION, *CARRAGEENANS

Abstract

Carrageenans are polysaccharides from red algae which are widely used as food additives and in other applications. Their structure is often described by different disaccharide repeating units, although it was already demonstrated that reality is more complex. In many studies, commercial carrageenans were used to establish structure function relationships, but a structural and compositional analysis was rarely conducted. Therefore, the aim of our study was to systematically and comprehensively characterize a broad collection of commercial carrageenans with different specifications from different manufacturers. For a more detailed characterization, an analytical approach based on partial enzymatic hydrolysis in combination with HPLC–MS and HPSEC-RI was developed and applied. Furthermore, rheology was used to gain detailed insights into the functionality of selected samples. Our results demonstrate that significant structural variation can be observed for commercial carrageenans. The samples contained different cations and the carrageenan type specified by the manufacturer did not always represent the structure of the corresponding polysaccharides. This was especially true for λ-carrageenans: Of the six commercial samples analyzed, none contained structural elements from the λ-type. Instead, the corresponding carrageenans contained κ-, ι- and ν-units. The application of the developed enzymatic-chromatographic approach showed that different hybrid carrageenans are present. In addition, the rheological analysis of the commercial carrageenan samples showed clear differences in the gelling properties upon calcium addition which could influence their behavior in different applications. Our results demonstrate that before an investigation of structure–function relationships, commercial carrageenan samples should be analyzed for their structure and composition. We also showed that the enzymatic-chromatographic approach described in this study is well suited for this purpose. [ABSTRACT FROM AUTHOR]

Published

2024

13. Steroidomics in Men with Schizophrenia.

Author

Hill, Martin, Velíková, Marta, Hovorková, Tereza, Bulant, Josef, Janšáková, Katarína, and Valeš, Karel

Subjects

*CORTISONE, *SULFATION, *PREGNENOLONE, *SCHIZOPHRENIA, *HYDROCORTISONE

Abstract

Schizophrenia is associated with numerous abnormalities, including imbalances in all hormonal axes, among which steroids play a major role. Steroidomic studies therefore represent a promising tool for early diagnosis and appropriate treatment of schizophrenia. A total of 51 adult male schizophrenics aged 27 (22, 34) years (shown as median with quartiles) and 16 healthy controls (HCs) aged 28 (25, 32) years were enrolled into this study. Our results showed the effective differentiation of men with schizophrenia from controls based on steroidomic profiles. We also found an altered metabolic pathway from pregnenolone and its sulfate (PREG/S) to cortisol in schizophrenics with several metabolic bottlenecks such as lower PREG levels due to increased PREG sulfation and/or suppressed PREGS desulfation and attenuated conversion of 17-hydroxy-PREG to 17-hydroxy-progesterone, as well as the results suggestive of suppressed CYP11B1 activity. In contrast, steroid molar ratios suggested two counterregulatory steps involving increased conversion of PREG/S to 17-hydroxy-PREG/S and decreased conversion of cortisol to cortisone, which may maintain unchanged basal cortisol levels but may not ensure a sufficient cortisol response to stress. Our data also indicated a trend to higher 7α-, 7β-, and 16α-hydroxylation that may counteract the autoimmune complications and proinflammatory processes accompanying schizophrenia. Finally, a possible suppression of HSD17B3 activity was suggested, resulting in decreased circulating testosterone levels with increased androstenedione levels. [ABSTRACT FROM AUTHOR]

Published

2024

14. Decoding the Role of O-GlcNAcylation in Hepatocellular Carcinoma.

Author

Zhou, Xinyu, Hang, Sirui, Wang, Qingqing, Xu, Liu, and Wang, Peter

Subjects

*PROTEIN stability, *HEPATOCELLULAR carcinoma, *SULFATION, *TREATMENT effectiveness, *UBIQUITINATION

Abstract

Post-translational modifications (PTMs) influence protein functionality by modulating protein stability, localization, and interactions with other molecules, thereby controlling various cellular processes. Common PTMs include phosphorylation, acetylation, ubiquitination, glycosylation, SUMOylation, methylation, sulfation, and nitrosylation. Among these modifications, O-GlcNAcylation has been shown to play a critical role in cancer development and progression, especially in hepatocellular carcinoma (HCC). This review outlines the role of O-GlcNAcylation in the development and progression of HCC. Moreover, we delve into the underlying mechanisms of O-GlcNAcylation in HCC and highlight compounds that target O-GlcNAc transferase (OGT) and O-GlcNAcase (OGA) to improve treatment outcomes. Understanding the role of O-GlcNAcylation in HCC will offer insights into potential therapeutic strategies targeting OGT and OGA, which could improve treatment for patients with HCC. [ABSTRACT FROM AUTHOR]

Published

2024

15. Sulfation of Various Polysaccharide Structures: Different Methods and Perspectives.

Author

Berezhnaya, Yaroslava D., Kazachenko, Aleksandr S., Kazachenko, Anna S., Malyar, Yuriy N., and Borovkova, Valentina S.

Subjects

*TARGETED drug delivery, *SULFUR trioxide, *SULFATION, *DRUG solubility, *POLYMERS, *POLYSACCHARIDES

Abstract

Sulfated polysaccharides have a variety of important biologically active properties, such as anticoagulant, hypolipidemic, antiviral activity, the ability to be a means of targeted drug delivery and to improve the water solubility of certain drugs. Initial and sulfated polysaccharides' biological activity depends on the method of their preparation, composition and structure. Currently, there is an extensive body of literature data on methods for the sulfation of various natural polysaccharides. However, modern reviews on this topic mainly focus on the biological activity and application of sulfated polymers, rather than on synthesis methods. The latest comprehensive review on methods for the synthesis of sulfated polysaccharides was performed by Caputo in 2019. To further study this area, you need to know the latest trends in this topic. Based on this, we decided to create a new, up-to-date review covering most of the existing methods for the synthesis of sulfated polysaccharides. This work examined methods for the synthesis of biologically active polysaccharide sulfates and their effect on polymer characteristics, as well as the advantages and disadvantages of each method. Traditional methods for sulfating polysaccharides were reviewed such as using a complex of sulfur trioxide with pyridine, and new methods based on the use of toxic free and corrosive free reagents. Some data on the biological activity of the obtained polysaccharides are considered. [ABSTRACT FROM AUTHOR]

Published

2024

16. Extraction, Purification, Sulfated Modification, and Biological Activities of Dandelion Root Polysaccharides.

Author

Wu, Xiao, Li, Na, Dong, Zeng, Yin, Qin, Zhou, Tong, Zhu, Lixiang, Yan, Hanxi, Chen, Ziping, and Zhai, Kefeng

Subjects

LACTOBACILLUS acidophilus, LACTOBACILLUS plantarum, HELICAL structure, AMMONIUM sulfate, MOLECULAR weights, MONOSACCHARIDES

Abstract

In this study, polysaccharides were extracted at a rate of 87.5% ± 1.5% from native dandelion roots, and the dandelion root polysaccharides (DRPs) were then chemically modified to obtain sulfated polysaccharides (SDRPs) with a degree of substitution of 1.49 ± 0.07. The effects of modification conditions, physicochemical characterizations, structural characteristics, antioxidant properties, hypoglycemic activity, and proliferative effects on probiotics of DRP derivatives were further investigated. Results showed that the optimum conditions for sulfation of DRPs included esterification reagents (concentrated sulfuric acid: n-butanol) ratio of 3:1, a reaction temperature of 0 °C, a reaction time of 1.5 h, and the involvement of 0.154 g of ammonium sulfate. The DRPs and SDRPs were composed of six monosaccharides, including mannose, glucosamine, rhamnose, glucose, galactose, and arabinose. Based on infrared spectra, the peaks of the characteristic absorption bands of S=O and C-O-S appeared at 1263 cm−1 and 836 cm−1. Compared with DRPs, SDRPs had a significantly lower relative molecular mass and a three-stranded helical structure. NMR analysis showed that sulfated modification mainly occurred on the hydroxyl group at C6. SDRPs underwent a chemical shift to higher field strength, with their characteristic signal peaking in the region of 1.00–1.62 ppm. Scanning electron microscopy (SEM) analysis indicated that the surface morphology of SDRPs was significantly changed. The structure of SDRPs was finer and more fragmented than DRPs. Compared with DRPs, SDRPs showed better free radical scavenging ability, higher Fe2+chelating ability, and stronger inhibition of α-glucosidase and α-amylase. In addition, SDRPs had an excellent promotional effect on the growth of Lactobacillus plantarum 10665 and Lactobacillus acidophilus. Therefore, this study could provide a theoretical basis for the development and utilization of DRPs. [ABSTRACT FROM AUTHOR]

Published

2024

17. The Influence of Sulfation Degree of Glycosaminoglycan-Functionalized 3D Collagen I Networks on Cytokine Profiles of In Vitro Macrophage–Fibroblast Cocultures.

Author

Ullm, Franziska, Renner, Alexander, Freudenberg, Uwe, Werner, Carsten, and Pompe, Tilo

Subjects

SULFATION, GLYCOSAMINOGLYCANS, COLLAGEN, MACROPHAGES, FIBROBLASTS

Abstract

Cell–cell interactions between fibroblasts and immune cells, like macrophages, are influenced by interaction with the surrounding extracellular matrix during wound healing. In vitro hydrogel models that mimic and modulate these interactions, especially of soluble mediators like cytokines, may allow for a more detailed investigation of immunomodulatory processes. In the present study, a biomimetic extracellular matrix model based on fibrillar 3D collagen I networks with a functionalization with heparin or 6-ON-desulfated heparin, as mimics of naturally occurring heparan sulfate, was developed to modulate cytokine binding effects with the hydrogel matrix. The constitution and microstructure of the collagen I network were found to be stable throughout the 7-day culture period. A coculture study of primary human fibroblasts/myofibroblasts and M-CSF-stimulated macrophages was used to show its applicability to simulate processes of progressed wound healing. The quantification of secreted cytokines (IL-8, IL-10, IL-6, FGF-2) in the cell culture supernatant demonstrated the differential impact of glycosaminoglycan functionalization of the collagen I network. Most prominently, IL-6 and FGF-2 were shown to be regulated by the cell culture condition and network constitution, indicating changes in paracrine and autocrine cell–cell communication of the fibroblast–macrophage coculture. From this perspective, we consider our newly established in vitro hydrogel model suitable for mechanistic coculture analyses of primary human cells to unravel the role of extracellular matrix factors in key events of tissue regeneration and beyond. [ABSTRACT FROM AUTHOR]

Published

2024

18. Genome-wide analysis and characterization of the peptides containing tyrosine sulfation (PSY) gene family in Triticum aestivum L. unraveling their contributions to both plant development and diverse stress responses.

Author

Kesawat, Mahipal Singh, Kherawat, Bhagwat Singh, Ram, Chet, Manohar, Swati, Kumar, Santosh, Chung, Sang-Min, Alharbi, Sulaiman Ali, Ansari, Mohammad Javed, and Lenka, Sangram K.

Subjects

GENE families, PLANT development, SULFATION, GENE expression, TYROSINE, WHEAT, PLANT hormones, GENES

Abstract

Background: Small-secreted peptides are increasingly recognized as a novel class of intracellular signal molecules, playing crucial roles in plant growth and development. However, the precise role and mechanism governed by peptides containing Tyrosine Sulfation (PSY) are still under investigation. Currently, there is a lack of accessible information concerning the PSY gene family in wheat. Results: Therefore, in this investigation, we identified 29 PSY genes in Triticum aestivum, with the aim of unraveling their significance in plant development processes and their response to a variety of stress conditions. Phylogenetic analysis showed that TaPSY genes clustered into five groups. Additionally, an analysis of the gene structure of TaPSYs displayed a conserved evolutionary path. The syntenic relationship demonstrated the 69 orthologous gene pairs in T. dicoccoides, Ae. tauschii, T. turgidum, and H. vulgare, respectively. Furthermore, the Ka/Ks analysis indicated that TaPSY genes have experienced purifying selection during their evolutionary processes. The promoters of TaPSY genes were found to contain numerous CAREs, and these elements are known to perform essential functions in various development processes, phytohormone responses, as well as defense and stress mechanisms. In addition, the identification of potential miRNAs targeting TaPSY genes was followed by an examination of their expression patterns across various tissues. Among the 29 TaPSY genes, twenty miRNAs were discovered to target eighteen of them. Moreover, TaPSY genes displayed a distinct expression across different tissues and stress conditions. Conclusions: Hence, these discoveries offer a significant reference point for forthcoming molecular investigations and hold promise for bolstering wheat yield and stress resilience through targeted genetic enhancements and strategic breeding approaches. Highlights: ➢ Signaling peptides, particularly those with Tyrosine Sulfation (PSY) gene family members, have been extensively researched in Arabidopsis. However, there is scarce information available regarding PSY genes in other crops such as wheat. ➢ In this study, we have identified 29 PSY genes in wheat for the first time, shedding light on their significance in plant development and stress response. ➢ Phylogenetic analysis categorized TaPSY genes into five clusters, exhibiting conserved gene structures and notable purifying selection. ➢ Further, the presence of multiple cis-acting regulatory elements (CAREs) in TaPSY promoters and out of the 29 TaPSY genes, 18 TaPSY genes were targeting by miRNAs highlight their roles in various developmental and stress processes. ➢ These discoveries offer invaluable insights for future molecular investigations aimed at boosting wheat yield and enhancing stress tolerance through targeted genetic improvements. [ABSTRACT FROM AUTHOR]

Published

2024

19. Classification and Molecular Functions of Heparan Sulfate Proteoglycans and Their Molecular Mechanisms with the Receptor.

Author

Matsuzaka, Yasunari and Yashiro, Ryu

Subjects

*HEPARAN sulfate proteoglycans, *GLUCURONIC acid, *SULFATION, *PROTEOGLYCANS, *CHEMOKINES

Abstract

Heparan sulfate proteoglycans are highly glycosylated proteins in which heparan sulfate, a glycosaminoglycan sugar chain, is an acidic sugar chain consisting of a repeating disaccharide structure of glucuronic acid and N-acetylglucosamine is locally sulfated. Syndecan, one of the transmembrane HSPGs, functions as a receptor that transmits signals from the extracellular microenvironment to the inside of the cell. In the vascular system, heparan sulfate proteoglycans, a major component of the glycocalyx, enable the binding of various plasma-derived molecules due to their diversity, epimerization of glycosaminoglycans chains, long chains, and sulfation. Heparan sulfate proteoglycans present in the extracellular matrix serve as a reservoir for bioactive molecules such as chemokines, cytokines, and growth factors. Aberrant expression of heparan sulfate proteoglycans, heparanase, and sulfatase is observed in many pathological conditions. Therefore, it can be applied to therapeutic strategies for a wide range of fields including Alzheimer's disease, heart failure, cancer, organ transplants, diabetes, chronic inflammation, aging, and autoimmune diseases. [ABSTRACT FROM AUTHOR]

Published

2024

20. In Vitro Metabolism and Transport Characteristics of Zastaprazan.

Author

Lee, Min Seo, Lee, Jihoon, Pang, Minyoung, Kim, John, Cha, Hyunju, Cheon, Banyoon, Choi, Min-Koo, Song, Im-Sook, and Lee, Hye Suk

Subjects

*ORGANIC anion transporters, *ORGANIC cation transporters, *BIOCHEMICAL substrates, *CYTOCHROME P-450, *SULFATION, *HYDROXYLATION

Abstract

Zastaprazan (JP-1366), a novel potassium-competitive acid blocker, is a new drug for the treatment of erosive esophagitis. JP-1366 is highly metabolized in human, mouse, and dog hepatocytes but moderately metabolized in rat and monkey hepatocytes when estimated from the metabolic stability of this compound in hepatocyte suspension and when 18 phase I metabolites and 5 phase II metabolites [i.e., N-dearylation (M6), hydroxylation (M1, M19, M21), dihydroxylation (M7, M8, M14, M22), trihydroxylation (M13, M18), hydroxylation and reduction (M20), dihydroxylation and reduction (M9, M16), hydrolysis (M23), hydroxylation and glucuronidation (M11, M15), hydroxylation and sulfation (M17), dihydroxylation and sulfation (M10, M12), N-dearylation and hydroxylation (M3, M4), N-dearylation and dihydroxylation (M5), and N-dearylation and trihydroxylation (M2)] were identified from JP-1366 incubation with the hepatocytes from humans, mice, rats, dogs, and monkeys. Based on the cytochrome P450 (CYP) screening test and immune-inhibition analysis with CYP antibodies, CYP3A4 and CYP3A5 played major roles in the metabolism of JP-1366 to M1, M3, M4, M6, M8, M9, M13, M14, M16, M18, M19, M21, and M22. CYP1A2, 2C8, 2C9, 2C19, and 2D6 played minor roles in the metabolism of JP-1366. UDP-glucuronosyltransferase (UGT) 2B7 and UGT2B17 were responsible for the glucuronidation of M1 to M15. However, JP-1366 and active metabolite M1 were not substrates for drug transporters such as organic cation transporter (OCT) 1/2, organic anion transporter (OAT) 1/3, organic anion transporting polypeptide (OATP)1B1/1B3, multidrug and toxic compound extrusion (MATE)1/2K, P-glycoprotein (P-gp), and breast cancer-resistant protein (BCRP). Only M1 showed substrate specificity for P-gp. The findings indicated that drug-metabolizing enzymes, particularly CYP3A4/3A5, may have a significant role in determining the pharmacokinetics of zastaprazan while drug transporters may only have a small impact on the absorption, distribution, and excretion of this compound. [ABSTRACT FROM AUTHOR]

Published

2024

21. Unveiling the lithium deintercalation mechanisms in spent lithium-ion batteries via sulfation roasting.

Author

He, Minyu, Cao, Wen, Teng, Liumei, Liu, Weizao, Ji, Sitong, Yu, Wenhao, Ding, Chunlian, Wu, Hongli, and Liu, Qingcai

Subjects

*SULFATION, *LITHIUM, *FERRIC oxide, *LITHIUM-ion batteries, *ROASTING (Metallurgy), *CHONDROITIN sulfates

Abstract

[Display omitted] • Pyrite ore as the only additive is used for sulfation reaction of LiCoO 2. • The mechanism of the sulfation reaction of LiCoO 2 was obtained. • Lithium deintercalation has been verified through density functional theory calculations. • High purity Li 2 CO 3 could be produced from the lithium sulfate leaching solution. Recovery of valuable metals from spent lithium-ion batteries (LIBs) is of great importance for resource sustainability and environmental protection. This study introduced pyrite ore (FeS 2) as an alternative additive to achieve the selective recovery of Li 2 CO 3 from spent LiCoO 2 (LCO) batteries. The mechanism study revealed that the sulfation reaction followed two pathways. During the initial stage (550 °C–800 °C), the decomposition and oxidation of FeS 2 and the subsequent gas–solid reaction between the resulting SO 2 and layered LCO play crucial roles. The sulfation of lithium occurred prior to cobalt, resulting in the disruption of layered structure of LCO and the transformation into tetragonal spinel. In the second stage (over 800 °C), the dominated reactions were the decomposition of orthorhombic cobalt sulfate and its combination with rhombohedral Fe 2 O 3 to form CoFe 2 O 4. The deintercalation of Li from LCO by the substitution of Fe and conversion of Co(III)/Fe(II) into Co 3 O 4 /CoFe 2 O 4 were further confirmed by density functional theory (DFT) calculation results. This fundamental understanding of the sulfation reaction facilitated the future development of lithium extraction methods that utilized additives to substantially reduce energy consumption. [ABSTRACT FROM AUTHOR]

Published

2024

22. Effect of Incorporation of Sulfation in Columnar Modeling of Oxidized Copper Minerals on Predictions of Leaching Kinetics.

Author

Bruce, Elena, Sepúlveda, Rossana, Castillo, Jonathan, and Saldana, Manuel

Subjects

SULFATION, ECCENTRIC loads, LEACHING, SOMATOMEDIN, COPPER ores, MINERALS

Abstract

Mathematical modeling of columnar leaching is a useful tool for predicting and evaluating the kinetics of copper extraction. One commonly used model for this process is the shrinking core model (SCM). In this study, the aim was to develop a model for column leaching of oxidized copper ore based on the SCM, which incorporates the ore sulfation stage before leaching. In sulfation and leaching laboratory-scale tests, we studied the effect of acid dosage (at 22.8, 34.2, and 45.6 kg/t), humidity (at 90%, 100%, and 110% of the saturation humidity of the mineral), ore granulometry (−3/4″ and −3/8″), and rest time (at 24, 48, 72, and 96 h) on sulfation. We found that the highest sulfation reached 49.7% for both granulometries in studies. In the column tests, the effects of acid dosage (at 34.2, 45.6 kg/t), ore granulometry (−3/4″, −3/8″), and rest time (at 24, 48 h) were studied. When the SCM was applied to these tests, we obtained fit qualities within 63.4% and 74.9%. By incorporating the sulfation factor into the SCM predictions, we observed an average increase in adjustment between 24% and 28%. This method is effective for minerals and operating conditions different from the ones studied. [ABSTRACT FROM AUTHOR]

Published

2024

23. The role of genetic polymorphisms in the sulfation of pregnenolone by human cytosolic sulfotransferase SULT2B1a

Author

Eid Alatwi and Ahsan F. Bairam

Subjects

Pregnenolone, Sulfation, SULT2B1a, SNPs, Medicine, Science

Abstract

Abstract Pregnenolone is a key intermediate in the biosynthesis of many steroid hormones and neuroprotective steroids. Sulfotransferase family cytosolic 2B member 1 (SULT2B1a) has been reported to be highly selective to sulfate pregnenolone. This study aimed to clarify the effect of missense single nucleotide polymorphisms (SNPs) of the human SULT2B1 gene on the sulfating activity of coded SULT2B1a allozymes toward Pregnenolone. To investigate the effects of single nucleotide polymorphisms of the SULT2B1 gene on the sulfation of pregnenolone by SULT2B1a allozymes, 13 recombinant SULT2B1a allozymes were generated, expressed, and purified using established procedures. Human SULT2B1a SNPs were identified by a comprehensive database search. 13 SULT2B1a nonsynonymous missense coding SNPs (cSNPs) were selected, and site-directed mutagenesis was used to generate the corresponding cDNAs, packaged in pGEX-2TK expression vector, encoding these 13 SULT2B1a allozymes, which were bacterially expressed in BL21 E. coli cells and purified by glutathione-Sepharose affinity chromatography. Purified SULT2B1a allozymes were analyzed for sulfating activities towards pregnenolone. In comparison with the wild-type SULT2B1a, of the 13 allozymes, 11 showed reduced activity toward pregnenolone at 0.1 µM. Specifically, P134L and R259Q allozymes, reported to be involved in autosomal-recessive congenital ichthyosis, displayed low activity (1–10%) toward pregnenolone. The findings of this study may demonstrate the impact of genetic polymorphism on the sulfation of pregnenolone in individuals with different SULT2B1 genotypes.

Published

2024

24. Bone Phenotype is Always Present But Androgen Excess is Less Frequently Seen in PAPSS2 Deficiency

Author

Didem Helvacıoğlu and Tülay Güran

Subjects

papss2, androgen excess, sulfation, brachyolmia, semd, dheas, Pediatrics, RJ1-570, Diseases of the endocrine glands. Clinical endocrinology, RC648-665

Abstract

3'-Phosphoadenosine 5'-phosphosulfate synthase 2 (PAPSS2) deficiency is a rare disorder due to biallelic pathogenic variants in the PAPSS2 gene. This disorder was first described in 1998 by Ahmad et al. and Faiyaz ul Haque et al. To date, 79 patients with PAPSS2 deficiency have been reported. The main reported features of these patients are related to bone abnormalities and clinical/biochemical androgen excess. Disproportionate short stature and symptoms associated with spondylar skeletal dysplasia are the most common clinical features that require clinical attention. Androgen excess has been described much less commonly. This review summarizes the currently published clinical, molecular, and biochemical features of patients with PAPSS2 deficiency.

Published

2024

25. Sulfation of chondroitin and bile acids converges to antagonize Wnt/β-catenin signaling and inhibit APC deficiency-induced gut tumorigenesis

Author

Pengfei Xu, Yue Xi, Jong-Won Kim, Junjie Zhu, Min Zhang, Meishu Xu, Songrong Ren, Da Yang, Xiaochao Ma, and Wen Xie

Subjects

Colon cancer, APC, Wnt/β-catenin, PAPSS2, Chondroitin sulfate, Sulfation, Therapeutics. Pharmacology, RM1-950

Abstract

Sulfation is a crucial and prevalent conjugation reaction involved in cellular processes and mammalian physiology. 3′-Phosphoadenosine 5′-phosphosulfate (PAPS) synthase 2 (PAPSS2) is the primary enzyme to generate the universal sulfonate donor PAPS. The involvement of PAPSS2-mediated sulfation in adenomatous polyposis coli (APC) mutation-promoted colonic carcinogenesis has not been reported. Here, we showed that the expression of PAPSS2 was decreased in human colon tumors along with cancer stages, and the lower expression of PAPSS2 was correlated with poor prognosis in advanced colon cancer. Gut epithelial-specific heterozygous Apc deficient and Papss2-knockout (ApcΔgut-HetPapss2Δgut) mice were created, and the phenotypes were compared to the spontaneous intestinal tumorigenesis of ApcΔgut-Het mice. ApcΔgut-HetPapss2Δgut mice were more sensitive to gut tumorigenesis, which was mechanistically accounted for by the activation of Wnt/β-catenin signaling pathway due to the suppression of chondroitin sulfation and inhibition of the farnesoid X receptor (FXR)-transducin-like enhancer of split 3 (TLE3) gene regulatory axis. Chondroitin sulfate supplementation in ApcΔgut-HetPapss2Δgut mice alleviated intestinal tumorigenesis. In summary, we have uncovered the protective role of PAPSS2-mediated chondroitin sulfation and bile acids–FXR–TLE3 activation in the prevention of gut carcinogenesis via the antagonization of Wnt/β-catenin signaling. Chondroitin sulfate may be explored as a therapeutic agent for Papss2 deficiency-associated colonic carcinogenesis.

Published

2024

26. Gut microbiota metabolite indole-3-acetic acid maintains intestinal epithelial homeostasis through mucin sulfation

Author

Mengfan Li, Yiyun Ding, Jingge Wei, Yue Dong, Jingyi Wang, Xin Dai, Jing Yan, Feifei Chu, Kexin Zhang, Fanyi Meng, Jiahui Ma, Weilong Zhong, Bangmao Wang, Yunhuan Gao, Rongcun Yang, Xinjuan Liu, Xiaomin Su, and Hailong Cao

Subjects

Inflammatory bowel disease, indole-3-acetic acid, aryl hydrocarbon receptor, mucin, sulfation, Diseases of the digestive system. Gastroenterology, RC799-869

Abstract

The global incidence and prevalence of inflammatory bowel disease (IBD) are gradually increasing. A high-fat diet (HFD) is known to disrupt intestinal homeostasis and aggravate IBD, yet the underlying mechanisms remain largely undefined. Here, a positive correlation between dietary fat intake and disease severity in both IBD patients and murine colitis models is observed. A HFD induces a significant decrease in indole-3-acetic acid (IAA) and leads to intestinal barrier damage. Furthermore, IAA supplementation enhances intestinal mucin sulfation and effectively alleviates colitis. Mechanistically, IAA upregulates key molecules involved in mucin sulfation, including 3’-phosphoadenosine 5’-phosphosulfate synthase 2 (Papss2) and solute carrier family 35 member B3 (Slc35b3), the synthesis enzyme and the transferase of 3’-phosphoadenosine-5’-phosphosulfate (PAPS), via the aryl hydrocarbon receptor (AHR). More importantly, AHR can directly bind to the transcription start site of Papss2. Oral administration of Lactobacillus reuteri, which can produce IAA, contributes to protecting against colitis and promoting mucin sulfation, while the modified L. reuteri strain lacking the iaaM gene (LactobacillusΔiaaM) and the ability to produce IAA fail to exhibit such effects. Overall, IAA enhances intestinal mucin sulfation through the AHR-Papss2-Slc35b3 pathway, contributing to the protection of intestinal homfeostasis.

Published

2024

27. Sulfated Hydrogels as Primary Intervertebral Disc Cell Culture Systems.

Author

Bermudez-Lekerika, Paola, Crump, Katherine B., Wuertz-Kozak, Karin, Le Maitre, Christine L., and Gantenbein, Benjamin

Subjects

HYDROGELS, INTERVERTEBRAL disk, CELL culture, SULFATION, CELL survival

Abstract

The negatively charged extracellular matrix plays a vital role in intervertebral disc tissues, providing specific cues for cell maintenance and tissue hydration. Unfortunately, suitable biomimetics for intervertebral disc regeneration are lacking. Here, sulfated alginate was investigated as a 3D culture material due to its similarity to the charged matrix of the intervertebral disc. Precursor solutions of standard alginate, or alginate with 0.1% or 0.2% degrees of sulfation, were mixed with primary human nucleus pulposus cells, cast, and cultured for 14 days. A 0.2% degree of sulfation resulted in significantly decreased cell density and viability after 7 days of culture. Furthermore, a sulfation-dependent decrease in DNA content and metabolic activity was evident after 14 days. Interestingly, no significant differences in cell density and viability were observed between surface and core regions for sulfated alginate, unlike in standard alginate, where the cell number was significantly higher in the core than in the surface region. Due to low cell numbers, phenotypic evaluation was not achieved in sulfated alginate biomaterial. Overall, standard alginate supported human NP cell growth and viability superior to sulfated alginate; however, future research on phenotypic properties is required to decipher the biological properties of sulfated alginate in intervertebral disc cells. [ABSTRACT FROM AUTHOR]

Published

2024

28. A General Method to Access Underexplored Ylideneamino Sulfates as Interrupted Beckmann-Type Rearrangement Intermediates.

Author

Zhou, Yifei and Jones, Alan M.

Subjects

*BECKMANN rearrangement, *SULFATES, *SCISSION (Chemistry), *SULFURIC acid, *AMIDES, *SODIUM bicarbonate, *BETAINE

Abstract

The Beckmann rearrangement of ketoximes to their corresponding amides, using a Brønsted acid-mediated fragmentation and migration sequence, has found wide-spread industrial application. We postulated that the development of a methodology to access ylideneamino sulfates using tributylsulfoammonium betaine (TBSAB) would afford isolable Beckmann-type intermediates and competent partners for subsequent rearrangement cascades. The ylideneamino sulfates generated, isolated as their tributylammonium salts, are sufficiently activated to undergo Beckmann rearrangement without additional reagent activation. The generation of sulfuric acid in situ from the ylideneamino sulfate giving rise to a routine Beckmann rearrangement and additional amide bond cleavage to the corresponding aniline was detrimental to reaction success. The screening of bases revealed inexpensive sodium bicarbonate to be an effective additive to prevent classic Brønsted acid-mediated fragmentation and achieve optimal conversions of up to 99%. [ABSTRACT FROM AUTHOR]

Published

2024

29. Rearrangement of Arylsulfamates and Sulfates to Para -Sulfonyl Anilines and Phenols.

Author

Zhou, Yifei and Jones, Alan M.

Subjects

*ANILINE, *DRUG discovery, *PHENOLS, *INTRAVENOUS anesthetics, *SULFATES, *BETAINE

Abstract

The C(sp2)-aryl sulfonate functional group is found in bioactive molecules, but their synthesis can involve extreme temperatures (>190 °C or flash vacuum pyrolysis) and strongly acidic reaction conditions. Inspired by the 1917 Tyrer industrial process for a sulfa dye that involved an aniline N(sp2)-SO3 intermediate en route to a C(sp2)-SO3 rearranged product, we investigated tributylsulfoammonium betaine (TBSAB) as a milder N-sulfamation to C-sulfonate relay reagent. Initial investigations of a stepwise route involving TBSAB on selected anilines at room temperature enabled the isolation of N(sp2)-sulfamate. Subsequent thermal rearrangement demonstrated the intermediary of a sulfamate en route to the sulfonate; however, it was low-yielding. Investigation of the N-sulfamate to C--sulfonate mechanism through control experiments with variation at the heteroatom positions and kinetic isotope experiments (KIEH/D) confirmed the formation of a key N(sp2)-SO3 intermediate and further confirmed an intermolecular mechanism. Furthermore, compounds without an accessible nitrogen (or oxygen) lone pair did not undergo sulfamation- (or sulfation) -to-sulfonation under these conditions. A one-pot sulfamation and thermal sulfonation reaction was ultimately developed and explored on a range of aniline and heterocyclic scaffolds with high conversions, including N(sp2)-sulfamates (O(sp2)-sulfates) and C(sp2)-sulfonates, in up to 99 and 80% (and 88% for a phenolic example) isolated yield, respectively. Encouragingly, the ability to modulate the ortho-para selectivity of the products obtained was observed under thermal control. A sulfonated analog of the intravenous anesthetic propofol was isolated (88% yield), demonstrating a proof-of-concept modification of a licensed drug alongside a range of nitrogen- and sulfur-containing heterocyclic fragments used in drug discovery. [ABSTRACT FROM AUTHOR]

Published

2024

30. The Genetics behind Sulfation: Impact on Airway Remodeling.

Author

Ntenti, Charikleia, Papakonstantinou, Eleni, Fidani, Liana, Stolz, Daiana, and Goulas, Antonis

Subjects

*VENTRICULAR remodeling, *SULFATION, *GENETICS, *SMOKING, *CIGARETTE smoke, *GENETIC polymorphisms

Abstract

In COPD, chronic inflammation and exposure to irritants, such as cigarette smoke, lead to the thickening of bronchial walls. This results from increased deposition of collagen and other extracellular matrix components, contributing to the narrowing of airways. Nevertheless, it is widely recognized that COPD is an inflammatory disorder marked by partially reversible airflow limitation wherein genetic factors interact with the environment. In recent years, numerous investigations have substantiated the correlation between gene polymorphisms and COPD. SUMF1 has been implicated in diverse cellular processes, including lysosomal function and extracellular matrix maintenance, both of which play pivotal roles in respiratory health. The genetic variations in SUMF1 could lead to an imbalanced sulfation in the extracellular matrix of lung tissue, potentially playing a role in the onset of COPD. Recent studies have uncovered a potential link between dysregulation of SUMF1 and COPD progression, shedding light on its involvement in the abnormal sulfatase activity observed in COPD patients. Through a comprehensive review of current literature and experimental findings, this article aims to contribute to the growing body of knowledge surrounding the genetic intricacies concerning sulfation of airway remodeling and possible pharmacological applications in COPD and asthma management. [ABSTRACT FROM AUTHOR]

Published

2024

31. Carboxymethylated and Sulfated Furcellaran from Furcellaria lumbricalis and Its Immobilization on PLA Scaffolds.

Author

Štěpánková, Kateřina, Ozaltin, Kadir, Sáha, Petr, Vargun, Elif, Domincová-Bergerová, Eva, Vesel, Alenka, Mozetič, Miran, and Lehocký, Marian

Subjects

*SULFATION, *POLYETHYLENE glycol, *CARBOXYMETHYLATION, *SURFACE roughness, *ELEMENTAL analysis

Abstract

This study involved the creation of highly porous PLA scaffolds through the porogen/leaching method, utilizing polyethylene glycol as a porogen with a 75% mass ratio. The outcome achieved a highly interconnected porous structure with a thickness of 25 μm. To activate the scaffold's surface and improve its hydrophilicity, radiofrequency (RF) air plasma treatment was employed. Subsequently, furcellaran subjected to sulfation or carboxymethylation was deposited onto the RF plasma treated surfaces with the intention of improving bioactivity. Surface roughness and water wettability experienced enhancement following the surface modification. The incorporation of sulfate/carboxymethyl group (DS = 0.8; 0.3, respectively) is confirmed by elemental analysis and FT-IR. Successful functionalization of PLA scaffolds was validated by SEM and XPS analysis, showing changes in topography and increases in characteristic elements (N, S, Na) for sulfated (SF) and carboxymethylated (CMF). Cytocompatibility was evaluated by using mouse embryonic fibroblast cells (NIH/3T3). [ABSTRACT FROM AUTHOR]

Published

2024

32. Bioinformatic Analysis of Sulfotransferases from an Unexplored Gut Microbe, Sutterella wadsworthensis 3_1_45B: Possible Roles towards Detoxification via Sulfonation by Members of the Human Gut Microbiome.

Author

Langford, Lauryn and Shah, Dhara D.

Subjects

*SULFOTRANSFERASES, *GUT microbiome, *HUMAN microbiota, *SULFONATION, *MICROBIAL enzymes, *GLUTATHIONE transferase

Abstract

Sulfonation, primarily facilitated by sulfotransferases, plays a crucial role in the detoxification pathways of endogenous substances and xenobiotics, promoting metabolism and elimination. Traditionally, this bioconversion has been attributed to a family of human cytosolic sulfotransferases (hSULTs) known for their high sequence similarity and dependence on 3′-phosphoadenosine 5′-phosphosulfate (PAPS) as a sulfo donor. However, recent studies have revealed the presence of PAPS-dependent sulfotransferases within gut commensals, indicating that the gut microbiome may harbor a diverse array of sulfotransferase enzymes and contribute to detoxification processes via sulfation. In this study, we investigated the prevalence of sulfotransferases in members of the human gut microbiome. Interestingly, we stumbled upon PAPS-independent sulfotransferases, known as aryl-sulfate sulfotransferases (ASSTs). Our bioinformatics analyses revealed that members of the gut microbial genus Sutterella harbor multiple asst genes, possibly encoding multiple ASST enzymes within its members. Fluctuations in the microbes of the genus Sutterella have been associated with various health conditions. For this reason, we characterized 17 different ASSTs from Sutterella wadsworthensis 3_1_45B. Our findings reveal that SwASSTs share similarities with E. coli ASST but also exhibit significant structural variations and sequence diversity. These differences might drive potential functional diversification and likely reflect an evolutionary divergence from their PAPS-dependent counterparts. [ABSTRACT FROM AUTHOR]

Published

2024

33. Histone H3Y99sulf regulates hepatocellular carcinoma responding to hypoxia.

Author

Sibi Yin, Weixing Yu, Runxin Zhou, Xiao Zeng, Li Jiang, Yu Wang, Dingyuan Guo, Fuqiang Tong, Leya He, Jun Zhao, and Yugang Wang

Subjects

*HYPOXIA-inducible factor 1, *HEPATOCELLULAR carcinoma, *HYPOXIA-inducible factors, *PROMOTERS (Genetics), *HYPOXEMIA, *SULFATION

Abstract

Histone H3 tyrosine-99 sulfation (H3Y99sulf) is a recently identified histone mark that can cross-talk with H4R3me2a to regulate gene transcription, but its role in cancer biology is less studied. Here, we report that H3Y99sulf is a cancer-associated histone mark that can mediate hepatocellular carcinoma (HCC) cells responding to hypoxia. Hypoxia-stimulated SNAIL pathway elevates the expression of PAPSS2, which serves as a source of adenosine 30-phosphate 50-phos-phosulfate for histone sulfation and results in upregulation of H3Y99sulf. The transcription factor TDRD3 is the downstream effector of H3Y99sulf-H4R3me2a axis in HCC. It reads and co-localizes with the H3Y99sulf-H4R3me2a dual mark in the promoter regions of HIF1A and PDK1 to regulate gene transcription. Depletion of SULT1B1 can effectively reduce the occurrence of H3Y99sulf-H4R3me2a-TDRD3 axis in gene promoter regions and lead to downregulation of targeted gene transcription. Hypoxia-inducible factor 1-alpha and PDK1 are master regulators for hypoxic responses and cancer metabolism. Disruption of the H3Y99sulf-H4R3me2a-TDRD3 axis can inhibit the expression and functions of hypoxia-inducible factor 1-alpha and PDK1, resulting in suppressed proliferation, tumor growth, and survival of HCC cells suffering hypoxia stress. The present study extends the regulatory and functional mechanisms of H3Y99sulf and improves our understanding of its role in cancer biology. [ABSTRACT FROM AUTHOR]

Published

2024

34. Crystal structure of tick tyrosylprotein sulfotransferase reveals the activation mechanism of the tick anticoagulant protein madanin.

Author

Misa Yoshimura, Takamasa Teramoto, Hirai Asano, Yuka Iwamoto, Mariko Kondo, Etsuko Nishimoto, and Yoshimitsu Kakuta

Subjects

*SULFOTRANSFERASES, *CRYSTAL structure, *TICKS, *SULFATION, *ANTICOAGULANTS, *PROTEIN S

Abstract

Ticks pose a substantial public health risk as they transmit various pathogens. This concern is related to the adept blood-sucking strategy of ticks, underscored by the action of the anticoagulant, madanin, which is known to exhibit an approximately 1000-fold increase in anticoagulant activity following sulfation of its two tyrosine residues, Tyr51 and Tyr54. Despite this knowledge, the molecular mechanism underlying sulfation by tick tyrosylprotein sulfotransferase (TPST) remains unclear. In this study, we successfully prepared tick TPST as a soluble recombinant enzyme. We clarified the method by which this enzyme proficiently sulfates tyrosine residues in madanin. Biochemical analysis using a substrate peptide based on madanin and tick TPST, along with the analysis of the crystal structure of the complex and docking simulations, revealed a sequential sulfation process. Initial sulfation at the Tyr51 site augments binding, thereby facilitating efficient sulfation at Tyr54. Beyond direct biochemical implications, these findings considerably improve our understanding of tick bloodsucking strategies. Furthermore, combined with the utility of modified tick TPST, our findings may lead to the development of novel anticoagulants, promising avenues for thrombotic disease intervention and advancements in the field of public health. [ABSTRACT FROM AUTHOR]

Published

2024

35. Bone Phenotype is Always Present But Androgen Excess is Less Frequently Seen in PAPSS2 Deficiency.

Author

Helvacıoğlu, Didem and Güran, Tülay

Subjects

*SPINE radiography, *BONES, *ANDROGENS, *HYPERANDROGENISM, *MUSCULOSKELETAL system abnormalities, *DEHYDROEPIANDROSTERONE, *GENE expression, *STATURE, *GENETIC mutation, *SOMATOMEDIN, *GROWTH disorders, *PHENOTYPES, *LUMBAR pain

Abstract

3'-Phosphoadenosine 5'-phosphosulfate synthase 2 (PAPSS2) deficiency is a rare disorder due to biallelic pathogenic variants in the PAPSS2 gene. This disorder was first described in 1998 by Ahmad et al. and Faiyaz ul Haque et al. To date, 79 patients with PAPSS2 deficiency have been reported. The main reported features of these patients are related to bone abnormalities and clinical/biochemical androgen excess. Disproportionate short stature and symptoms associated with spondylar skeletal dysplasia are the most common clinical features that require clinical attention. Androgen excess has been described much less commonly. This review summarizes the currently published clinical, molecular, and biochemical features of patients with PAPSS2 deficiency. [ABSTRACT FROM AUTHOR]

Published

2024

36. Sulfation of chondroitin and bile acids converges to antagonize Wnt/β-catenin signaling and inhibit APC deficiency-induced gut tumorigenesis.

Author

Xu, Pengfei, Xi, Yue, Kim, Jong-Won, Zhu, Junjie, Zhang, Min, Xu, Meishu, Ren, Songrong, Yang, Da, Ma, Xiaochao, and Xie, Wen

Subjects

SULFATION, ADENOMATOUS polyposis coli, BILE acids, CHONDROITIN, FARNESOID X receptor, CHONDROITIN sulfates

Abstract

Sulfation is a crucial and prevalent conjugation reaction involved in cellular processes and mammalian physiology. 3′-Phosphoadenosine 5′-phosphosulfate (PAPS) synthase 2 (PAPSS2) is the primary enzyme to generate the universal sulfonate donor PAPS. The involvement of PAPSS2-mediated sulfation in adenomatous polyposis coli (APC) mutation-promoted colonic carcinogenesis has not been reported. Here, we showed that the expression of PAPSS2 was decreased in human colon tumors along with cancer stages, and the lower expression of PAPSS2 was correlated with poor prognosis in advanced colon cancer. Gut epithelial-specific heterozygous Apc deficient and Papss2 -knockout (Apc Δgut-Het Papss2 Δgut) mice were created, and the phenotypes were compared to the spontaneous intestinal tumorigenesis of Apc Δgut-Het mice. Apc Δgut-Het Papss2 Δgut mice were more sensitive to gut tumorigenesis, which was mechanistically accounted for by the activation of Wnt/ β -catenin signaling pathway due to the suppression of chondroitin sulfation and inhibition of the farnesoid X receptor (FXR)-transducin-like enhancer of split 3 (TLE3) gene regulatory axis. Chondroitin sulfate supplementation in Apc Δgut-Het Papss2 Δgut mice alleviated intestinal tumorigenesis. In summary, we have uncovered the protective role of PAPSS2-mediated chondroitin sulfation and bile acids–FXR–TLE3 activation in the prevention of gut carcinogenesis via the antagonization of Wnt/ β -catenin signaling. Chondroitin sulfate may be explored as a therapeutic agent for Papss2 deficiency-associated colonic carcinogenesis. Intestinal PAPSS2 or sulfation represents a potential therapeutic target for colon cancer and chondroitin sulfate may be explored for its use in the prevention and treatment of PAPSS2 deficiency-associated colon cancer. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2024

37. A poly‐proline II helix in YadA from Yersinia enterocolitica serotype O:9 facilitates heparin binding through electrostatic interactions.

Author

Meuskens, Ina, Kristiansen, Per Eugen, Bardiaux, Benjamin, Koynarev, Vladimir Rosenov, Hatlem, Daniel, Prydz, Kristian, Lund, Reidar, Izadi‐Pruneyre, Nadia, and Linke, Dirk

Subjects

*YERSINIA enterocolitica, *HEPARIN, *ELECTROSTATIC interaction, *HEPARAN sulfate, *N-terminal residues, *SULFATION

Abstract

Poly‐proline II helices are secondary structure motifs frequently found in ligand‐binding sites. They exhibit increased flexibility and solvent exposure compared to the strongly hydrogen‐bonded α‐helices or β‐strands and can therefore easily be misinterpreted as completely unstructured regions with an extremely high rotational freedom. Here, we show that the adhesin YadA of Yersinia enterocolitica serotype O:9 contains a poly‐proline II helix interaction motif in the N‐terminal region. The motif is involved in the interaction of YadAO:9 with heparin, a host glycosaminoglycan. We show that the basic residues within the N‐terminal motif of YadA are required for electrostatic interactions with the sulfate groups of heparin. Biophysical methods including CD spectroscopy, solution‐state NMR and SAXS all independently support the presence of a poly‐proline helix allowing YadAO:9 binding to the rigid heparin. Lastly, we show that host cells deficient in sulfation of heparin and heparan sulfate are not targeted by YadAO:9‐mediated adhesion. We speculate that the YadAO:9–heparin interaction plays an important and highly strain‐specific role in the pathogenicity of Yersinia enterocolitica serotype O:9. [ABSTRACT FROM AUTHOR]

Published

2024

38. Tyrosine Sulfation at Antibody Light Chain CDR-1 Increases Binding Affinity and Neutralization Potency to Interleukine-4.

Author

D'Antona, Aaron M., Lee, Julie M., Zhang, Melvin, Friedman, Clarence, He, Tao, Mosyak, Lidia, Bennett, Eric, Lin, Laura, Silverman, Maddison, Cometa, Funi, Meade, Caryl, Hageman, Tyler, Sousa, Eric, Cohen, Justin, Marquette, Kimberly, Ferguson, Darren, and Zhong, Xiaotian

Subjects

*SULFATION, *POST-translational modification, *TYROSINE, *IMMUNOGLOBULINS, *SODIUM chlorate, *MONOCLONAL antibodies, *VIRAL antibodies, *FC receptors

Abstract

Structure and function of therapeutic antibodies can be modulated by a variety of post-translational modifications (PTM). Tyrosine (Tyr) sulfation is a type of negatively charged PTM that occurs during protein trafficking through the Golgi. In this study, we discovered that an anti-interleukin (IL)-4 human IgG1, produced by transiently transfected HEK293 cells, contained a fraction of unusual negatively charged species. Interestingly, the isolated acidic species exhibited a two-fold higher affinity to IL-4 and a nearly four-fold higher potency compared to the main species. Mass spectrometry (MS) showed the isolated acidic species possessed an +80-Dalton from the expected mass, suggesting an occurrence of Tyr sulfation. Consistent with this hypothesis, we show the ability to control the acidic species during transient expression with the addition of Tyr sulfation inhibitor sodium chlorate or, conversely, enriched the acidic species from 30% to 92% of the total antibody protein when the IL-4 IgG was co-transfected with tyrosylprotein sulfotransferase genes. Further MS and mutagenesis analysis identified a Tyr residue at the light chain complementarity-determining region-1 (CDRL-1), which was sulfated specifically. These results together have demonstrated for the first time that Tyr sulfation at CDRL-1 could modulate antibody binding affinity and potency to a human immune cytokine. [ABSTRACT FROM AUTHOR]

Published

2024

39. Seaweed Polysaccharides as Potential Biostimulants in Turnip Greens Production.

Author

Mamede, Mariana, Cotas, João, Pereira, Leonel, and Bahcevandziev, Kiril

Subjects

POLYSACCHARIDES, TURNIPS, RAPESEED, SUSTAINABLE agriculture, MARINE algae, POTAMOGETON, MARINE plants

Abstract

Seaweed polysaccharides can act as substitutes for synthetic compounds present in commercial stimulants and fertilizers used in agriculture to improve crop yields and vigor. In this study, three different polysaccharides (alginate, agar, and carrageenan) were extracted from one brown seaweed, Saccorhiza polyschides, and two red seaweeds, Gracilaria gracilis and Chondrus crispus, respectively, and applied to potted turnip greens (Brassica napus L.), with the intention to analyze their impact on plant growth, development, and metabolism. Turnip greens treated with polysaccharides, especially carrageenan of C. crispus, showed the best results in improving the crop productivity in terms of plant length and weight, number of leaves, nutrient and pigment content, and soil fertility compared with turnip greens from the negative control or those treated with a commercial leaf fertilizer. λ-carrageenan extracted from the tetrasporophyte generation of C. crispus had the highest bioactivity and positive effect on turnip greens among all treatments. λ-carrageenan has been shown to improve plant growth; increase the plant's biomass (plant leaves: CC(T) (40.80 ± 5.11 g) compared to the positive control (15.91 ± 15.15 g)) and root system; enhance photosynthetic activity; increase the uptake of soil nutrients; and protect plants against abiotic and biotic stresses, stimulating the production of secondary metabolites and managing its defense pathways. Seaweed-extracted polysaccharides have the potential to be used in sustainable agriculture. [ABSTRACT FROM AUTHOR]

Published

2024

40. The Discovery of the Fucoidan-Active Endo-1→4-α-L-Fucanase of the GH168 Family, Which Produces Fucoidan Derivatives with Regular Sulfation and Anticoagulant Activity.

Author

Silchenko, Artem S., Taran, Ilya V., Usoltseva, Roza V., Zvyagintsev, Nikolay V., Zueva, Anastasiya O., Rubtsov, Nikita K., Lembikova, Dana E., Nedashkovskaya, Olga I., Kusaykin, Mikhail I., Isaeva, Marina P., and Ermakova, Svetlana P.

Subjects

*SULFATION, *RODENTICIDES, *BROWN algae, *ANTICOAGULANTS, *MARINE bacteria, *HEPARIN

Abstract

Sulfated polysaccharides of brown algae, fucoidans, are known for their anticoagulant properties, similar to animal heparin. Their complex and irregular structure is the main bottleneck in standardization and in defining the relationship between their structure and bioactivity. Fucoidan-active enzymes can be effective tools to overcome these problems. In the present work, we identified the gene fwf5 encoding the fucoidan-active endo-fucanase of the GH168 family in the marine bacterium Wenyingzhuangia fucanilytica CZ1127T. The biochemical characteristics of the recombinant fucanase FWf5 were investigated. Fucanase FWf5 was shown to catalyze the endo-type cleavage of the 1→4-O-glycosidic linkages between 2-O-sulfated α-L-fucose residues in fucoidans composed of the alternating 1→3- and 1→4-linked residues of sulfated α-L-fucose. This is the first report on the endo-1→4-α-L-fucanases (EC 3.2.1.212) of the GH168 family. The endo-fucanase FWf5 was used to selectively produce high- and low-molecular-weight fucoidan derivatives containing either regular alternating 2-O- and 2,4-di-O-sulfation or regular 2-O-sulfation. The polymeric 2,4-di-O-sulfated fucoidan derivative was shown to have significantly greater in vitro anticoagulant properties than 2-O-sulfated derivatives. The results have demonstrated a new type specificity among fucanases of the GH168 family and the prospects of using such enzymes to obtain standard fucoidan preparations with regular sulfation and high anticoagulant properties. [ABSTRACT FROM AUTHOR]

Published

2024

41. Ultra‐Fast Recyclable and Value‐Added Desulfation Method for Spent Lead Paste via Dual Intensification Processes.

Author

Chai, Lulu, Li, Zhiyu, Wang, Keyu, Liu, Xiaowei, Dai, Shaozhen, Liu, Xiaoguang, Sun, Yanzhi, and Pan, Junqing

Subjects

*EMISSIONS (Air pollution), *LIQUID films, *COST accounting, *SULFATION, *MANUFACTURING processes

Abstract

The new low‐cost clean pre‐desulfation technology is very important in pyrometallurgy and hydrometallurgy. However, traditional reactors have low space‐time yield and desulfation rate, resulting in high energy consumption and SO2 emissions in the industrial desulfation processes. Herein, dual rotating liquid film reactors (RLFRs) and lime are proposed to construct a recyclable, ultra‐fast, and value‐added desulfation method. Parameter optimization and kinetic calculations prove that the above reactions are controlled by internal diffusion, revealing that RLFR promotes the mass transfer and reaction rate. The new process greatly shortens the desulfation time of lead paste from 40 min to 10 s with a high desulfation rate of 99.7%, and the sulfation time of lime from 30 min to 30 s with a sulfation rate of 98.6% with a net profit of 55.99 ¥/ton by cost accounting. Moreover, ten batches of continuous scale‐up experiments demonstrate the stability of processes, the desulfation and sulfation rates are kept at 99.7% and 98.2%, which greatly reduces the emissions of waste desulfate liquor. This work provides a new universal strategy for a sustainable, low‐cost, and clean desulfation method of waste resources to achieve technical and economic feasibility. [ABSTRACT FROM AUTHOR]

Published

2023

42. Copper Sulfation from Enargite Roasting Using Coal and Fayalite Slag Mixture.

Author

Véliz, Miguel, Aracena, Alvaro, Jerez, Oscar, Pérez-Tello, Manuel, and Balladares, Eduardo

Subjects

*ROASTING (Metallurgy), *SULFATION, *ARSENIC removal (Water purification), *COPPER slag, *SLAG, *COPPER, *COAL

Abstract

In this work, the roasting of an enargite mix was carried out in oxidative conditions. The temperature range of the study was 773–973 K. The mixture had a 4:6:6 molar ratio of enargite, magnetite and coal, respectively. The roasting was made in an open atmosphere. The time was 1 h for each isothermal test. The effect of temperature and weight loss were studied. The results indicate that the temperature affects the products. At 773–873 K, the copper phases were sulfates. When the temperature was increased to 973 K, all the present phases were oxidized, and no arsenic phase was encountered in the XRDs. Therefore, this process is an excellent alternative for roasting copper concentrates with enargite, removing arsenic in the gas phase and generating a calcine that could then go to lixiviation to finally recover the copper through electrowinning. [ABSTRACT FROM AUTHOR]

Published

2023

43. Effect of sucrose-based carbon foams as negative electrode additive on the performance of lead-acid batteries under high-rate partial-state-of-charge condition

Author

Fazhi Xie, Yujia Ma, Meng Zhang, Shaohua Yang, Yuan Dai, Liang Fang, and Yonggang Shao

Subjects

Lead-acid battery, Porous material, Sulfation, Cycle life, High-rate partial-state-of-charge (HRPSoC), Science (General), Q1-390, Social sciences (General), H1-99

Abstract

Lead-acid batteries are noted for simple maintenance, long lifespan, stable quality, and high reliability, widely used in the field of energy storage. However, during the use of lead-acid batteries, the negative electrode is prone to irreversible sulfation, failing to meet the requirements of new applications such as maintenance-free hybrid vehicles and solar energy storage. In this study, in order to overcome the sulfation problem and improve the cycle life of lead-acid batteries, active carbon (AC) was selected as a foaming agent and foam fixing agent, and carbon foams (CF) with layered porous structure was prepared by mixing with molten sucrose. Sucrose as raw material is green and cheap, and the material preparation process is simple. The prepared CF material was then added as an additive to the negative electrode plate, and the electrochemical performance of the electrode plate and the battery was studied. The results proved that the addition of CF could effectively inhibit the sulfate formation of the negative electrode plate, with the 1.0 % CF negative electrode plate showing the best electrochemical performance. Specifically, according to the result of battery cycle testing, the simulated battery with CF had a cycle life of 3642 times, which was 2.87 times that of the blank group and 2.39 times of the AC group. Meanwhile, rate testing showed that the simulated battery with CF could maintain a high capacity even under high-rate discharge conditions.

Published

2024

44. Extraction, Purification, Sulfated Modification, and Biological Activities of Dandelion Root Polysaccharides

Author

Xiao Wu, Na Li, Zeng Dong, Qin Yin, Tong Zhou, Lixiang Zhu, Hanxi Yan, Ziping Chen, and Kefeng Zhai

Subjects

dandelion root polysaccharide (DRP), sulfation, structural characteristics, biological activity, Chemical technology, TP1-1185

Abstract

In this study, polysaccharides were extracted at a rate of 87.5% ± 1.5% from native dandelion roots, and the dandelion root polysaccharides (DRPs) were then chemically modified to obtain sulfated polysaccharides (SDRPs) with a degree of substitution of 1.49 ± 0.07. The effects of modification conditions, physicochemical characterizations, structural characteristics, antioxidant properties, hypoglycemic activity, and proliferative effects on probiotics of DRP derivatives were further investigated. Results showed that the optimum conditions for sulfation of DRPs included esterification reagents (concentrated sulfuric acid: n-butanol) ratio of 3:1, a reaction temperature of 0 °C, a reaction time of 1.5 h, and the involvement of 0.154 g of ammonium sulfate. The DRPs and SDRPs were composed of six monosaccharides, including mannose, glucosamine, rhamnose, glucose, galactose, and arabinose. Based on infrared spectra, the peaks of the characteristic absorption bands of S=O and C-O-S appeared at 1263 cm−1 and 836 cm−1. Compared with DRPs, SDRPs had a significantly lower relative molecular mass and a three-stranded helical structure. NMR analysis showed that sulfated modification mainly occurred on the hydroxyl group at C6. SDRPs underwent a chemical shift to higher field strength, with their characteristic signal peaking in the region of 1.00–1.62 ppm. Scanning electron microscopy (SEM) analysis indicated that the surface morphology of SDRPs was significantly changed. The structure of SDRPs was finer and more fragmented than DRPs. Compared with DRPs, SDRPs showed better free radical scavenging ability, higher Fe2+chelating ability, and stronger inhibition of α-glucosidase and α-amylase. In addition, SDRPs had an excellent promotional effect on the growth of Lactobacillus plantarum 10665 and Lactobacillus acidophilus. Therefore, this study could provide a theoretical basis for the development and utilization of DRPs.

Published

2024

45. Effect of Incorporation of Sulfation in Columnar Modeling of Oxidized Copper Minerals on Predictions of Leaching Kinetics

Author

Elena Bruce, Rossana Sepúlveda, Jonathan Castillo, and Manuel Saldana

Subjects

column modeling, sulfation, leaching kinetics, Mining engineering. Metallurgy, TN1-997

Abstract

Mathematical modeling of columnar leaching is a useful tool for predicting and evaluating the kinetics of copper extraction. One commonly used model for this process is the shrinking core model (SCM). In this study, the aim was to develop a model for column leaching of oxidized copper ore based on the SCM, which incorporates the ore sulfation stage before leaching. In sulfation and leaching laboratory-scale tests, we studied the effect of acid dosage (at 22.8, 34.2, and 45.6 kg/t), humidity (at 90%, 100%, and 110% of the saturation humidity of the mineral), ore granulometry (−3/4″ and −3/8″), and rest time (at 24, 48, 72, and 96 h) on sulfation. We found that the highest sulfation reached 49.7% for both granulometries in studies. In the column tests, the effects of acid dosage (at 34.2, 45.6 kg/t), ore granulometry (−3/4″, −3/8″), and rest time (at 24, 48 h) were studied. When the SCM was applied to these tests, we obtained fit qualities within 63.4% and 74.9%. By incorporating the sulfation factor into the SCM predictions, we observed an average increase in adjustment between 24% and 28%. This method is effective for minerals and operating conditions different from the ones studied.

Published

2024

46. Optimization of Preparation Technology and Anti-Mammary Gland Hyperplasia of Polysaccharide Sulfate from Atractylodes macrocephala

Author

Changxu LI, Shuo LI, Yike ZHANG, Zejun QI, Weiwei TANG, Qi GAO, Jiayue LIU, Mengting SHAO, Yanyan WANG, and Hong ZHAO

Subjects

response surface, atractylodes macrocephala polysaccharide, sulfation, structure identification, antioxidant, mammary gland hyperplasia, Food processing and manufacture, TP368-456

Abstract

Objective: To establish a preparation method of Atractylodes macrocephala Koidz polysaccharide (AMP) sulfate with anti-hyperplasia of mammary. Methods: AMP were sulfated by sulfated method, and the optimal conditions for the sulfated modification were determined by response surface methodology. The structures of AMP and SAMP were initially analyzed by infrared spectroscopy (IR) and High-Performance Gel Chromatography (HPGPC). The anti-oxidative activity in vitro of polysaccharide was investigated by testing the DPPH, ABTS+, OH free radical scavenging ability of AMP and SAMP. Rat model of mammary gland hyperplasia was established by intramuscular injection of estradiol benzoate and progesterone. The rats weight and breast diameter were recorded and the pathological organization form of mammary gland of rats were observed. Results: The optimum preparation conditions were as follows: Ratio of conditions of volume ratio of sulfuric acid and n-butanol 2:1, reaction temperature −4 ℃, reaction time 21 min. The degree of substitution of SAMP was 0.59±0.00391. The HPGPC results showed the relative molecular weights for AMP and SAMP were 2719 and 33524 Da, respectively. The IR spectra showed that SAMP had characteristic absorption peaks of S=O and C-O-S appeared near 833 and 1226 cm−1, indicating that the sulfated was successful. When the sample concentration was 0.5 mg/mL, the DPPH, ABTS+, OH free radical scavenging activities of SAMP were 54.91% , 38.21%, and 42.23%, respectively. Compared with the model group, the diameter of the nipples of the rats in the SAMP group decreased (P

Published

2023

47. Preparation of Sulfated Xylans and Its in Vitro Proliferation of Probiotics

Author

Xia LI, Qiying ZHANG, Yuan GUAN, Jing LI, Haishan CHEN, and Lifen LI

Subjects

xylan (xyl), sulfation, probiotics, in vitro proliferation, prebiotics, Food processing and manufacture, TP368-456

Abstract

This study aimed to determine the effect of sulfated xylans on the growth of probiotics. Xylan (Xyl) was chemically modified using the sulfamic acid-N,N-dimethylformamide method to produce sulfated xylan (SXY). The SXY was characterized by Fourier infrared spectroscopy (FT-IR), scanning electron microscope (SEM) and Congo red experiment. The Xyl and SXY were tested for their in vitro prebiotic effects using four strains of intestinal microflora, including Lactobacillus delbrueckii subsp. bulgaricus (GIM1.155), L. plantarum (GIM1.191), L. brevis (GIM1.773), and Streptococcus thermophilus (GIM1.540). From the recorded infrared spectra, vibrational bands for SXY were observed at 894, 1052 and 1243 cm−1, they could be assigned to the C—O—S vibration of a C—O—SO3, C—O stretched and S＝O stretching vibrations. The results of scanning electron microscopy showed that the surface structure of SXY increased smoothness. Congo red experiment revealed that SXY had a triple helix structure. The substitution degree of SXY measured using a BaCl2-gelatin turbidimeter was 0.341. In vitro experiment showed that the optimum concentration of SXY for the in vitro probiotic growth was 2.0%, rapid growth and increased proliferation were observed after 10 h of culture. The results obtained suggest that SXY could promote probiotic growth. It is an alternate source of prebiotics for maintaining gut health.

Published

2023

48. Sulfation on polysaccharides from Zizania latifolia extracted using ultrasound: Characterization, antioxidant and anti-non-small cell lung cancer activities

Author

Yang Zhang, Rongnan Nie, Wenxuan Liu, Shuaiyi Dong, Jingchun Yang, Xinyu Wang, Yang Wang, and Lixue Zheng

Subjects

Zizania latifolia, Polysaccharides, Yield- and antioxidation-guided strategy, Ultrasonic-assisted extraction, Sulfation, Anti-non-small cell lung cancer activity, Chemistry, QD1-999, Acoustics. Sound, QC221-246

Abstract

Zizania latifolia is a highly nutritious vegetable being praised as “Ginseng in Water”. Polysaccharides are the main bioactive ingredients in Z. latifolia, but there have been no reports on the yield- and activity-guided ultrasonic-assisted extraction (UAE), sulfation and anti-non-small cell lung cancer (NSCLC) activity. In this study, Z. latifolia polysaccharides (ZLP) were extracted using UAE under an optimized power, followed by sulfation to give three derivatives (SZLP-1 ∼ 3). After characterization, the antioxidant and anti-NSCLC activities were evaluated. The optimal ultrasonic power for ZLP extraction was screened out to be 300 W, under which the yield was 16.9 ± 2.10 %, and the scavenging rate against 2, 2-diphenyl-1-picrylhydrazyl (DPPH) radical was 63.3 ± 5.71 %, significantly higher than those of other powers and hot-water extraction. A series of characterizations fully confirmed the sulfated modification of ZLP. Sulfation improved the antioxidation of ZLP and was positively proportional to the degree of substitution (DS), of which SZLP-2 with a DS of 15.1 ± 2.50 elicited strong hydroxyl and DPPH radicals-scavenging capacities. Meanwhile, SZLP-2 also exerted promising anti-NSCLC potency via inhibiting A549 cell proliferation, with a median inhibition concentration (IC50) of 0.57 ± 0.01 mg/mL at 72 h, markedly smaller than that of unmodified ZLP (0.78 ± 0.04 mg/mL). In summary, the yield- and activity-guided UAE led to the ZLP with high yield and strong antioxidation. Further sulfation enhanced the bioactivities and produced the promising SZLP-2, which showed great potential in the development of novel antioxidant and anti-NSCLC drug.

Published

2024

49. The role of genetic polymorphisms in the sulfation of pregnenolone by human cytosolic sulfotransferase SULT2B1a

Author

Alatwi, Eid and Bairam, Ahsan F.

Published

2024

50. Stereocontrolled Synthesis and Conformational Analysis of a Series of Disaccharides α,β-d-GlcA-(1→3)-α-L-Fuc.

Author

Gerbst, Alexey G., Vinnitsky, Dmitry Z., Tokatly, Alexandra I., Dmitrenok, Andrey S., Krylov, Vadim B., Ustuzhanina, Nadezhda E., and Nifantiev, Nikolay E.

Subjects

*DISACCHARIDES, *SPIN-spin coupling constants, *QUANTUM chemistry, *CONFORMATIONAL analysis, *SULFATION, *CHONDROITIN sulfates

Abstract

D-Glucuronic acid is a fundamental building block of many biologically important polysaccharides, either in its non-substituted form or bearing a variety of substituents, among them sulfates. We have previously performed a study of the effects of exhaustive sulfation on the conformational behavior of β-gluronopyranosides. Herein, we report an investigation comparing α- and β-derivatives of this monosaccharide within the title disaccharides using NMR and quantum chemistry approaches. It was found that for α-linked disaccharides, the introduction of sulfates did not greatly affect their conformational behavior. However, for β-derivatives, considerable conformational changes were observed. In general, they resemble those that took place for the monosaccharides, except that NOESY experiments and calculations of intra-ring spin–spin coupling constants suggest the presence of a 1S5 conformer along with 3S1 in the fully sulfated disaccharide. During the synthesis of model compounds, hydrogen bond-mediated aglycone delivery was used as an α-directing stereocontrol approach in the glucuronidation reaction. [ABSTRACT FROM AUTHOR]

Published

2023