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1. Sortase-click strategy for defined protein conjugation on a heptavalent cyclodextrin scaffold.

Author

Shikha Singh, Kanchan Gupta, Shagun Shukla, Srinivasa-Gopalan Sampathkumar, and Rajendra P Roy

Subjects
Medicine, Science
Abstract

Multivalent proteins or protein dendrimers are useful for clinical and biotechnological applications. However, assembly of chemically defined protein dendrimers is a challenging endeavor. In the past, majority of protein dendrimers have been developed on branched lysine scaffolds and are usually limited to a valency of two to four. The naturally occurring cyclodextrin (CD) scaffold composed of 6-8 glucose units offers the possibility of expanding the valency. Here we have adapted a chemoenzymatic-click strategy for displaying heptavalent peptides and large proteins on the β-cyclodextrin (β-CD) scaffold. We demonstrate that recombinant proteins (engineered with a LPXTG pentapeptide motif at the carboxy terminus), labeled with an alkyne moiety by sortase-mediated ligation, can be easily clicked on to the azide-derivatized β-cyclodextrin through the Huisgen cycloaddition reaction yielding a well-defined heptavalent display of proteins.

Published
2019
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2. PeracetylN-cyclobutanoyl-D-mannosamine enhances expression of sialyl-Lewis X (sLeX / CD15s) and adhesion of leukocytes

Author

Anam Tasneem, Shubham Parashar, Simran Aittan, Tanya Jain, Charu Chauhan, Jyoti Rautela, Zahoor Ahmad Bhat, Kaisar Raza, Arumugam Madhumalar, and Srinivasa-Gopalan Sampathkumar

Abstract

Sialyl-Lewis-X (sLeX/CD15s) epitopes regulate cell adhesionviainteractions with selectins. High levels of sLeX are associated with chronic inflammation. Intense efforts have been devoted for the development of sLeX mimetics for the prevention of atherosclerosis. By contrast, low levels of sLeX are associated with leukocyte adhesion deficiency (LAD) disorders. In this context, we employed metabolic glycan engineering to alter the fine structures of sialoglycans. Treatment of HL-60 (human acute myeloid leukemia) cells with peracetylN-cyclobutanoyl-D-mannosamine (Ac4ManNCb) resulted in a four-fold increase in both sLeX levels and adhesion to E-selectin-Fc chimera. Enhanced sLeX levels on CD162/PSGL-1, CD43, and CD44 were observed through immunoprecipitation. Molecular dynamics (MD) simulations on interactions with E-selectin revealed dramatic differentials in the conformational dynamics of sLeX-Cb compared to sLeX, highlighting the significance of remoteN-acyl side chains of sialic acids in facilitating bio-active conformations. These results provide opportunities for pharmacological interventions in both LAD and chronic inflammation.Table of ContentsRemote substituents on the tetrasaccharide sialyl-Lewis X (sLeX / CD15s) influence ensembles of bio-active conformations and alter biological outcomes. Treatment with peracetylN-cyclobutanoyl-D-mannosamine (Ac4ManNCb) results in four-fold enhancement in the expression of sialyl-Lewis-X (sLeX / CD15s) and adhesion to E-selectin (CD62E). Molecular dynamics simulations show that the sLeX-Cb prefers a flatter bio-active conformation (gray) compared to wild-type sLeX (cyan).Institute and/or researcher Twitter usernames: @NImmunology @Gops_GlycoIndia

Published
2021

3. An expeditious synthesis of novel DNA nucleobase mimics of (+)-anisomycin

Author

Umesh K, Mishra, Yogesh S, Sanghvi, R, Abhiraj, Srinivasa-Gopalan, Sampathkumar, and Namakkal G, Ramesh

Subjects
Organic Chemistry, Humans, Nucleosides, DNA, General Medicine, Biochemistry, Anisomycin, HeLa Cells, Analytical Chemistry
Abstract

A glycal based expeditious synthesis of novel nucleoside analogues of (+)-anisomycin is reported. Readily available tri-O-benzyl-D-glucal was converted to a partially protected trihydroxypyrrolidine that is used as a common scaffold for the introduction of various nucleobases at the primary hydroxyl centre. Nucleoside analogues possessing all four DNA bases have been synthesized. Selective acetylation at C3 position was carried out with two of these unnatural nucleosides in order to mimic the structure of (+)-anisomycin. Cytotoxicity studies of some of these nucleosides showed that they display weaker activity on HeLa cells than Ara-C.

Published
2022

4. Efficient Inhibition of O-glycan biosynthesis using the hexosamine analog Ac5GalNTGc

Author

Aristotelis Antonopoulos, Alan E. Friedman, Monika Garg, Joseph T.Y. Lau, Xinheng Yu, Sriram Neelamegham, Shuen-Shiuan Wang, Virginia del Solar, Anne Dell, Mehrab Nasirikenari, Srinivasa-Gopalan Sampathkumar, Syed Meheboob Ahmed, Ahana Addya, Kavita Agarwal, and Stuart M. Haslam

Subjects
Glycan, Glycosylation, biology, medicine.diagnostic_test, Cell, Inflammation, Small molecule, carbohydrates (lipids), chemistry.chemical_compound, medicine.anatomical_structure, Biosynthesis, chemistry, Western blot, Biochemistry, medicine, biology.protein, medicine.symptom, Promyelocyte
Abstract

SUMMARYThere is a critical need to develop small molecule inhibitors of mucin-type O-linked glycosylation. The best known reagent currently is peracetylated benzyl-GalNAc, but it is only effective at millimolar concentrations. This manuscript demonstrates that Ac5GalNTGc, a peracetylated C-2 sulfhydryl substituted GalNAc, fulfills this unmet need. When added to cultured leukocytes, breast and prostate cells, Ac5GalNTGc increased cell surface VVA-binding by ~10-fold, indicating truncation of O-glycan biosynthesis. Cytometry, mass spectrometry and Western blot analysis of HL-60 promyelocytes demonstrate that 50-80μM Ac5GalNTGc prevented elaboration of 30-60% of the O-glycans beyond the Tn-antigen (GalNAcα1-Ser/Thr) stage. The effect of the compound on N-glycans and glycosphingolipids was small. Glycan inhibition induced by Ac5GalNTGc resulted in 50-80% reduction in leukocyte sialyl-Lewis-X expression, and L-/P-selectin mediated rolling under flow. Ac5GalNTGc was pharmacologically active in mouse. It reduced neutrophil infiltration to sites of inflammation by ~60%. Overall, Ac5GalNTGc may find diverse applications as a potent inhibitor of O-glycosylation.

Published
2020

5. Differential inhibition of mucin-type O-glycosylation (MTOG) induced by peracetyl N-thioglycolyl-d-galactosamine (Ac5GalNTGc) in myeloid cells

Author

Kavita Agarwal, Vandita Dwivedi, Srinivasa-Gopalan Sampathkumar, Anam Tasneem, and Pratima Saini

Subjects
0301 basic medicine, Glycan, Glycosylation, Glycoconjugate, Cell, Biophysics, Biochemistry, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, medicine, Molecular Biology, chemistry.chemical_classification, CD43, biology, Myeloid leukemia, Cell Biology, Cell biology, carbohydrates (lipids), 030104 developmental biology, medicine.anatomical_structure, chemistry, Cell culture, 030220 oncology & carcinogenesis, biology.protein, Glycoprotein
Abstract

Investigations on the structure and functional roles of glycosylation - an intricate, complex, and dynamic post translational modification on proteins - in biological processes has been a challenging task. Glycan modifications vary depending on the specific cell type, its developmental stage, and resting or activated state. In the present study, we aim to understand the differences between the mucin-type O-glycosylation (MTOG) of two functionally divergent human cell lines, K562 (chronic myeloid leukemia) and U937 (histiocytic lymphoma), having myeloid origins. MTOG is initiated by the addition of N-acetyl-α-d-galactosamine (GalNAc) to Ser/Thr of glycoproteins. We exploited the metabolic glycan engineering (MGE) strategy using the peracetyl N-thioglycolyl-d-galactosamine (Ac5GalNTGc), a synthetic GalNAc analogue, to engineer the glycoconjugates. Ac5GalNTGc was metabolized and incorporated as N-thioglycolyl-d-galactosamine (GalNTGc) in cell surface glycoproteins in both the cell lines with varying degrees of efficiency. Notably, metabolic incorporation of GalNTGc resulted in differential inhibition of MTOG. It was observed that endogenous glycosylation machinery of K562 is relatively more stringent for selecting GalNTGc whereas U937 is flexible towards this selection. Additionally, we studied how the glycan modifications vary on a given CD antigen in these cell lines. Particularly, MTOG on CD43 was differentially inhibited in K562 and U937 as revealed by glycan-dependent and glycan-independent antibodies. It was observed that the effect of MGE on CD43 was similar to global effects on both cell lines. Consequences of MGE using GalNAc analogues depend on the expression and activity of various glycosyl transferases which determine global glycosylation on cell surface as well as on specific glycoproteins.

Published
2018

6. Efficient inhibition of O-glycan biosynthesis using the hexosamine analog Ac

Author

Shuen-Shiuan, Wang, Virginia Del, Solar, Xinheng, Yu, Aristotelis, Antonopoulos, Alan E, Friedman, Kavita, Agarwal, Monika, Garg, Syed Meheboob, Ahmed, Ahana, Addhya, Mehrab, Nasirikenari, Joseph T, Lau, Anne, Dell, Stuart M, Haslam, Srinivasa-Gopalan, Sampathkumar, and Sriram, Neelamegham

Subjects
carbohydrates (lipids), Male, Mice, Inbred C57BL, Mice, Glycosylation, Polysaccharides, Carbohydrate Conformation, Animals, Humans, Female, Hexosamines, Cells, Cultured, Article
Abstract

There is a critical need to develop small molecule inhibitors of mucin-type O-linked glycosylation. The best-known reagent currently is benzyl-GalNAc, but it is only effective at millimolar concentrations. This manuscript demonstrates that Ac(5)GalNTGc, a peracetylated C-2 sulfhydryl substituted GalNAc, fulfills this unmet need. When added to cultured leukocytes, breast and prostate cells, Ac(5)GalNTGc increased cell surface VVA-binding by ~10-fold, indicating truncation of O-glycan biosynthesis. Cytometry, mass spectrometry and Western blot analysis of HL-60 promyelocytes demonstrated that 50-80μM Ac(5)GalNTGc prevented elaboration of 30-60% of the O-glycans beyond the Tn-antigen (GalNAcα1-Ser/Thr) stage. The effect of the compound on N-glycans and glycosphingolipids was small. Glycan inhibition induced by Ac(5)GalNTGc resulted in 50-80% reduction in leukocyte sialyl-Lewis-X expression, and L-/P-selectin mediated rolling under flow. Ac(5)GalNTGc was pharmacologically active in mouse. It reduced neutrophil infiltration to sites of inflammation by ~60%. Overall, Ac(5)GalNTGc may find diverse applications as a potent inhibitor of O-glycosylation.

Published
2019

7. Sortase-click strategy for defined protein conjugation on a heptavalent cyclodextrin scaffold

Author

Rajendra P. Roy, Srinivasa-Gopalan Sampathkumar, Shagun Shukla, Shikha Singh, and Kanchan Gupta

Subjects
Models, Molecular, Reversed-Phase High Performance Liquid Chromatography, Protein Expression, Organic chemistry, 02 engineering and technology, Protein Engineering, 01 natural sciences, Pentapeptide repeat, Biochemistry, chemistry.chemical_compound, Sortase, Peptide synthesis, Moiety, Vitamin C, Peptide sequence, chemistry.chemical_classification, Liquid Chromatography, Multidisciplinary, Cyclodextrin, Cycloaddition Reaction, Sulfates, Chromatographic Techniques, Vitamins, 021001 nanoscience & nanotechnology, Aminoacyltransferases, Recombinant Proteins, Chemistry, Cysteine Endopeptidases, Alkynes, Physical Sciences, Medicine, Fimbriae Proteins, 0210 nano-technology, Research Article, Peptide Biosynthesis, Dendrimers, Science, Size-Exclusion Chromatography, 010402 general chemistry, Research and Analysis Methods, Protein Chemistry, Bacterial Proteins, Dendrimer, Organic compounds, Gene Expression and Vector Techniques, Amino Acid Sequence, Molecular Biology Techniques, Molecular Biology, Molecular Biology Assays and Analysis Techniques, Cyclodextrins, Chemical Compounds, Biology and Life Sciences, Proteins, Reversed Phase Chromatography, Combinatorial chemistry, High Performance Liquid Chromatography, Hydrocarbons, 0104 chemical sciences, chemistry, Salts, Click Chemistry, Peptides
Abstract

Multivalent proteins or protein dendrimers are useful for clinical and biotechnological applications. However, assembly of chemically defined protein dendrimers is a challenging endeavor. In the past, majority of protein dendrimers have been developed on branched lysine scaffolds and are usually limited to a valency of two to four. The naturally occurring cyclodextrin (CD) scaffold composed of 6-8 glucose units offers the possibility of expanding the valency. Here we have adapted a chemoenzymatic-click strategy for displaying heptavalent peptides and large proteins on the β-cyclodextrin (β-CD) scaffold. We demonstrate that recombinant proteins (engineered with a LPXTG pentapeptide motif at the carboxy terminus), labeled with an alkyne moiety by sortase-mediated ligation, can be easily clicked on to the azide-derivatized β-cyclodextrin through the Huisgen cycloaddition reaction yielding a well-defined heptavalent display of proteins.

Published
2019

8. Efficient inhibition of O-glycan biosynthesis using the hexosamine analog Ac5GalNTGc

Author

Sriram Neelamegham, Virginia del Solar, Joseph T.Y. Lau, Xinheng Yu, Stuart M. Haslam, Ahana Addhya, Monika Garg, Anne Dell, Shuen-Shiuan Wang, Kavita Agarwal, Syed Meheboob Ahmed, Alan E. Friedman, Srinivasa-Gopalan Sampathkumar, Mehrab Nasirikenari, and Aristotelis Antonopoulos

Subjects
Pharmacology, Glycan, Glycosylation, 010405 organic chemistry, Clinical Biochemistry, Mucin, Inflammation, Biology, 01 natural sciences, Biochemistry, 0104 chemical sciences, carbohydrates (lipids), chemistry.chemical_compound, Sialyl-Lewis X, Biosynthesis, chemistry, Drug Discovery, medicine, biology.protein, Molecular Medicine, medicine.symptom, Cell adhesion, Molecular Biology, Selectin
Abstract

Summary There is a critical need to develop small-molecule inhibitors of mucin-type O-linked glycosylation. The best-known reagent currently is benzyl-GalNAc, but it is effective only at millimolar concentrations. This article demonstrates that Ac5GalNTGc, a peracetylated C-2 sulfhydryl-substituted GalNAc, fulfills this unmet need. When added to cultured leukocytes, breast cells, and prostate cells, Ac5GalNTGc increased cell-surface VVA binding by ∼10-fold, indicating truncation of O-glycan biosynthesis. Cytometry, mass spectrometry, and western blot analysis of HL-60 promyelocytes demonstrated that 50–80 μM Ac5GalNTGc prevented elaboration of 30%–60% of the O-glycans beyond the Tn-antigen (GalNAcα1-Ser/Thr) stage. The effect of the compound on N-glycans and glycosphingolipids was small. Glycan inhibition induced by Ac5GalNTGc resulted in 50%–80% reduction in leukocyte sialyl-Lewis X expression and L-/P-selectin-mediated rolling under flow conditions. Ac5GalNTGc was pharmacologically active in mouse. It reduced neutrophil infiltration to sites of inflammation by ∼60%. Overall, Ac5GalNTGc may find diverse applications as a potent inhibitor of O-glycosylation.

Published
2021

9. Differential inhibition of mucin-type O-glycosylation (MTOG) induced by peracetyl N-thioglycolyl-d-galactosamine (Ac

Author

Vandita, Dwivedi, Pratima, Saini, Anam, Tasneem, Kavita, Agarwal, and Srinivasa-Gopalan, Sampathkumar

Subjects
Acetylgalactosamine, Glycosylation, Leukosialin, Mucins, Gene Expression, Monocytes, Jurkat Cells, Metabolic Engineering, Organ Specificity, Cell Line, Tumor, Humans, N-Acetylgalactosaminyltransferases, K562 Cells, Glycoconjugates, Protein Processing, Post-Translational, Glycoproteins
Abstract

Investigations on the structure and functional roles of glycosylation - an intricate, complex, and dynamic post translational modification on proteins - in biological processes has been a challenging task. Glycan modifications vary depending on the specific cell type, its developmental stage, and resting or activated state. In the present study, we aim to understand the differences between the mucin-type O-glycosylation (MTOG) of two functionally divergent human cell lines, K562 (chronic myeloid leukemia) and U937 (histiocytic lymphoma), having myeloid origins. MTOG is initiated by the addition of N-acetyl-α-d-galactosamine (GalNAc) to Ser/Thr of glycoproteins. We exploited the metabolic glycan engineering (MGE) strategy using the peracetyl N-thioglycolyl-d-galactosamine (Ac

Published
2018

10. Chemical and biological methods for probing the structure and functions of polysialic acids

Author

Shubham Parashar, Vandita Dwivedi, Asif Shajahan, Srinivasa-Gopalan Sampathkumar, and Surbhi Goswami

Subjects
0301 basic medicine, Glycobiology, Polysialic acid, Central nervous system, Biology, Blood–brain barrier, Embryonic stem cell, General Biochemistry, Genetics and Molecular Biology, Cell biology, Sialic acid, 03 medical and health sciences, chemistry.chemical_compound, 030104 developmental biology, 0302 clinical medicine, medicine.anatomical_structure, chemistry, medicine, Neural cell adhesion molecule, General Agricultural and Biological Sciences, 030217 neurology & neurosurgery, Gene knockout
Abstract

Owing to its poly-anionic charge and large hydrodynamic volume, polysialic acid (polySia) attached to neural cell adhesion molecule regulates axon–axon and axon–substratum interactions and signalling, particularly, in the development of the central nervous system (CNS). Expression of polySia is spatiotemporally regulated by the action of two polysialyl transferases, namely ST8SiaII and ST8SiaIV. PolySia expression peaks during late embryonic and early post-natal period and maintained at a steady state in adulthood in neurogenic niche of the brain. Aberrant polySia expression is associated with neurological disorders and brain tumours. Investigations on the structure and functions, over the past four decades, have shed light on the physiology of polySia. This review focuses on the biological, biochemical, and chemical tools available for polySia engineering. Genetic knockouts, endo-neuraminidases that cleave polySia, antibodies, exogenous expression, and neuroblastoma cells have provided deep insights into the ability of polySia to guide migration of neuronal precursors in neonatal brain development, neuronal clustering, axonal pathway guidance, and axonal targeting. Advent of metabolic sialic acid engineering using ManNAc analogues has enabled reversible and dose-dependent modulation polySia in vitro and ex vivo. In vivo, ManNAc analogues readily engineer the sialoglycans in peripheral tissues, but show no effect in the brain. A recently developed carbohydrate-neuroactive hybrid strategy enables a non-invasive access to the brain in living animals across the blood–brain barrier. A combination of recent advances in CNS drugs and imaging with ManNAc analogues for polySia modulation would pave novel avenues for understanding intricacies of brain development and tackling the challenges of neurological disorders.

Published
2018

11. Rifampicin reduces advanced glycation end products and activates DAF-16 to increase lifespan in Caenorhabditis elegans

Author

Sandeep B. Golegaonkar, Mashanipalya G. Jagadeeshaprasad, Srinivasa-Gopalan Sampathkumar, Mahesh J. Kulkarni, Sneha B. Bansode, Shalini Sethurathinam, Syed Shamsh Tabrez, Awadhesh Pandit, and Arnab Mukhopadhyay

Subjects
Glycation End Products, Advanced, Aging, medicine.medical_treatment, Longevity, DAF-16, Biology, rifampicin, Transcription (biology), Glycation, In vivo, Daf-16, medicine, PTEN, Animals, Insulin, Caenorhabditis elegans, Caenorhabditis elegans Proteins, Antibiotics, Antitubercular, advanced glycation end products, Forkhead Transcription Factors, Cell Biology, Original Articles, biology.organism_classification, 3. Good health, Cell biology, Biochemistry, Mutation, biology.protein, glycation, Signal transduction, Rifampin, lifespan, Signal Transduction
Abstract

Advanced glycation end products (AGEs) are formed when glucose reacts nonenzymatically with proteins; these modifications are implicated in aging and pathogenesis of many age-related diseases including type II diabetes, atherosclerosis, and neurodegenerative disorders. Thus, pharmaceutical interventions that can reduce AGEs may delay age-onset diseases and extend lifespan. Using LC-MS(E), we show that rifampicin (RIF) reduces glycation of important cellular proteins in vivo and consequently increases lifespan in Caenorhabditis elegans by up to 60%. RIF analog rifamycin SV (RSV) possesses similar properties, while rifaximin (RMN) lacks antiglycation activity and therefore fails to affect lifespan positively. The efficacy of RIF and RSV as potent antiglycating agents may be attributed to the presence of a p-dihydroxyl moiety that can potentially undergo spontaneous oxidation to yield highly reactive p-quinone structures, a feature absent in RMN. We also show that supplementing rifampicin late in adulthood is sufficient to increase lifespan. For its effect on longevity, rifampicin requires DAF-18 (nematode PTEN) as well as JNK-1 and activates DAF-16, the FOXO homolog. Interestingly, the drug treatment modulates transcription of a different subset of DAF-16 target genes, those not controlled by the conserved Insulin-IGF-1-like signaling pathway. RIF failed to increase the lifespan of daf-16 null mutant despite reducing glycation, showing thereby that DAF-16 may not directly affect AGE formation. Together, our data suggest that the dual ability to reduce glycation in vivo and activate prolongevity processes through DAF-16 makes RIF and RSV effective lifespan-extending interventions.

Published
2015

13. Inhibition of Mucin-Type O-Glycosylation through Metabolic Processing and Incorporation of N-Thioglycolyl-<scp>d</scp>-galactosamine Peracetate (Ac5GalNTGc)

Author

Asif Shajahan, Monika Garg, Kavita Agarwal, Rachna Kaul, Saroj Kumar Jha, and Srinivasa-Gopalan Sampathkumar

Subjects
Glycan, Acetylgalactosamine, Glycosylation, Leukosialin, biology, Immunoprecipitation, Mucins, Galactosamine, General Chemistry, Biochemistry, Jurkat cells, Small molecule, Catalysis, Epitope, carbohydrates (lipids), Jurkat Cells, chemistry.chemical_compound, Colloid and Surface Chemistry, chemistry, Antigen, biology.protein, Humans
Abstract

Mucin-type O-glycans form one of the most abundant and complex post-translational modifications (PTM) on cell surface proteins that govern adhesion, migration, and trafficking of hematopoietic cells. Development of targeted approaches to probe functions of O-glycans is at an early stage. Among several approaches, small molecules with unique chemical functional groups that could modulate glycan biosynthesis form a critical tool. Herein, we show that metabolism of peracetyl N-acyl-D-galactosamine derivatives carrying an N-thioglycolyl (Ac5GalNTGc, 1) moiety-but not N-glycolyl (Ac5GalNGc, 2) and N-acetyl (Ac4GalNAc, 3)-through the N-acetyl-D-galactosamine (GalNAc) salvage pathway induced abrogation of MAL-II and PNA epitopes in Jurkat cells. Mass spectrometry of permethylated O-glycans from Jurkat cells confirmed the presence of significant amounts of elaborated O-glycans (sialyl-T and disialyl-T) which were inhibited upon treatment with 1. O-Glycosylation of CD43, a cell surface antigen rich in O-glycans, was drastically reduced by 1 in a thiol-dependent manner. By contrast, only mild effects were observed for CD45 glycoforms. Direct metabolic incorporation of 1 was confirmed by thiol-selective Michael addition reaction of immunoprecipitated CD43-myc/FLAG. Mechanistically, CD43 glycoforms were unperturbed by peracetylated N-(3-acetylthiopropanoyl) (4), N-(4-acetylthiobutanoyl) (5), and N-methylthioacetyl (6) galactosamine derivatives, N-thioglycolyl-D-glucosamine (7, C-4 epimer of 1), and α-O-benzyl 2-acetamido-2-deoxy-D-galactopyranoside (8), confirming the critical requirement of both free sulfhydryl and galactosamine moieties for inhibition of mucin-type O-glycans. Similar, yet differential, effects of 1 were observed for CD43 glycoforms in multiple hematopoietic cells. Development of small molecules that could alter glycan patterns in an antigen-selective and cell-type selective manner might provide avenues for understanding biological functions of glycans.

Published
2013

14. Development of delivery methods for carbohydrate-based drugs: controlled release of biologically-active short chain fatty acid-hexosamine analogs

Author

Jie Fu, Christopher Weier, Benjamin C. Tang, Kevin J. Yarema, M. Adam Meledeo, Ming Yang, Srinivasa-Gopalan Sampathkumar, Sung Yun Chung, Mark B. Jones, Udayanath Aich, and Justin Hanes

Subjects
Chemistry, Pharmaceutical, Antineoplastic Agents, Biochemistry, Article, Polyethylene Glycols, chemistry.chemical_compound, Drug Delivery Systems, In vivo, Dicarboxylic Acids, Molecular Biology, Chromatography, High Pressure Liquid, Chemistry, Short-chain fatty acid, Hexosamines, Biological activity, Cell Biology, Decanoic acid, Carbohydrate, Fatty Acids, Volatile, Controlled release, Drug development, Delayed-Action Preparations, Drug delivery, Nanoparticles, Polyvinyls, Decanoic Acids
Abstract

Carbohydrates are attractive candidates for drug development because sugars are involved in many, if not most, complex human diseases including cancer, immune dysfunction, congenital disorders, and infectious diseases. Unfortunately, potential therapeutic benefits of sugar-based drugs are offset by poor pharmacologic properties that include rapid serum clearance, poor cellular uptake, and relatively high concentrations required for efficacy. To address these issues, pilot studies are reported here where 'Bu(4)ManNAc', a short chain fatty acid-monosaccharide hybrid molecule with anti-cancer activities, was encapsulated in polyethylene glycol-sebacic acid (PEG-SA) polymers. Sustained release of biologically active compound was achieved for over a week from drug-laden polymer formulated into microparticles thus offering a dramatic improvement over the twice daily administration currently used for in vivo studies. In a second strategy, a tributanoylated ManNAc analog (3,4,6-O-Bu(3)ManNAc) with anti-cancer activities was covalently linked to PEG-SA and formulated into nanoparticles suitable for drug delivery; once again release of biologically active compound was demonstrated.

Published
2010

15. Chemical Labels Metabolically Installed Into the Glycoconjugates of the Target Cell Surface Can Be Used to Track Lymphocyte/Target Cell Interplay via Trogocytosis: Comparisons with Lipophilic Dyes and Biotin

Author

Sandrine Daubeuf, Xavier Préville, Srinivasa-Gopalan Sampathkumar, Anne Aucher, Kevin J. Yarema, and Denis Hudrisier

Subjects
CD4-Positive T-Lymphocytes, Glycosylation, Trogocytosis, Glycoconjugate, Immunology, Biotin, Context (language use), Cell Communication, CD8-Positive T-Lymphocytes, Biology, Mice, chemistry.chemical_compound, Antigen, Animals, Coloring Agents, chemistry.chemical_classification, B-Lymphocytes, Vaccination, General Medicine, T lymphocyte, Cell biology, CTL, chemistry, Biochemistry, Biotinylation, Glycoconjugates, T-Lymphocytes, Cytotoxic
Abstract

Trogocytosis, the process whereby lymphocytes capture membrane components from the cells they interact with, is classically evidenced by the transfer of fluorescent lipophilic compounds or biotinylated proteins from target cells to T or B cells. A particular class of molecules, not studied explicitly so far in the context of trogocytosis is glycoconjugates. Here, we used a method to metabolically install chemical labels in target cell glycoconjugates. Working with those target cells, we describe the conditions allowing CTL to be detected based on glycoconjugate trogocytosis triggered by antigen or stimulatory antibodies. Accordingly, we used this method to monitor the CTL response triggered in mice after vaccination. In addition, we documented the applicability of this approach to the detection of CD4(+) T and B cells. Overall, glycoconjugates were transferred between target cells and lymphocytes during trogocytosis with efficiencies comparable or higher than measured for biotinylated proteins or lipophilic dyes incorporated into general membrane lipids. From a technological point of view, our approach can be employed to detect reactive lymphocytes via glycoconjugate trogocytosis. More generally, we believe that the ever-growing ability to employ chemistry in living systems to label particular compounds will be powerful in unraveling the contributions of glycosylation to various aspects of T and B cells biology.

Published
2007

16. Targeting Glycosylation Pathways and the Cell Cycle: Sugar-Dependent Activity of Butyrate-Carbohydrate Cancer Prodrugs

Author

Kaoru Hida, Prasra Gomutputra, M. Adam Meledeo, Steven R. Head, Kevin J. Yarema, Tim Gilmartin, Anthony Sheh, Mark B. Jones, Srinivasa-Gopalan Sampathkumar, Sean S S. Choi, and Christopher T. Campbell

Subjects
Glycosylation, Cell cycle checkpoint, medicine.drug_class, Clinical Biochemistry, Apoptosis, Butyrate, Biology, Biochemistry, Jurkat Cells, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Cell Line, Tumor, Drug Discovery, medicine, Humans, Prodrugs, Molecular Biology, 030304 developmental biology, Pharmacology, 0303 health sciences, Reporter gene, Molecular Structure, Cell Cycle, Histone deacetylase inhibitor, Hexosamines, General Medicine, Cell cycle, 3. Good health, Cell biology, Butyrates, chemistry, Acetylation, 030220 oncology & carcinogenesis, Cancer cell, Molecular Medicine, Drug Screening Assays, Antitumor, HeLa Cells, Signal Transduction
Abstract

SummaryShort-chain fatty acid (SCFA)-carbohydrate hybrid molecules that target both histone deacetylation and glycosylation pathways to achieve sugar-dependent activity against cancer cells are described in this article. Specifically, n-butyrate esters of N-acetyl-d-mannosamine (But4ManNAc, 1) induced apoptosis, whereas corresponding N-acetyl-d-glucosamine (But4GlcNAc, 2), d-mannose (But5Man, 3), or glycerol (tributryin, 4) derivatives only provided transient cell cycle arrest. Western blots, reporter gene assays, and cell cycle analysis established that n-butyrate, when delivered to cells via any carbohydrate scaffold, functioned as a histone deacetylase inhibitor (HDACi), upregulated p21WAF1/Cip1 expression, and inhibited proliferation. However, only 1, a compound that primed sialic acid biosynthesis and modulated the expression of a different set of genes compared to 3, ultimately killed the cells. These results demonstrate that the biological activity of butyrate can be tuned by sugars to improve its anticancer properties.

Published
2006
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17. Synthesis of non-natural ManNAc analogs for the expression of thiols on cell-surface sialic acids

Author

Adrienne V. Li, Srinivasa-Gopalan Sampathkumar, and Kevin J. Yarema

Subjects
Cell, Mutagenesis, Cell Culture Techniques, Drug design, Hexosamines, Protein engineering, Transfection, Biology, Glycocalyx, General Biochemistry, Genetics and Molecular Biology, carbohydrates (lipids), Glycomics, medicine.anatomical_structure, Solubility, Biochemistry, Gene expression, Sialic Acids, medicine, Protein biosynthesis, Animals, Sulfhydryl Compounds
Abstract

The sialic acid biosynthetic pathway in mammalian cells utilizes N-acetyl-D-mannosamine (ManNAc) as a natural metabolic precursor and has the remarkable ability to biosynthetically process non-natural ManNAc analogs. Herein, we describe a recipe-style protocol for the synthesis of the novel peracetylated analog Ac5ManNTGc (1) that contains a pendant acetylthio- group and enables incorporation of thiol functionalities into the glycocalyx of living cells. We also describe the synthesis of the oxygen analog Ac5ManNGc (2), which serves as an appropriate control compound for biological experiments with 1. Both 1 and 2 were prepared from a reported, common intermediate 8, which is selectively acetylated at the hydroxyl groups. In contrast to previous methods, this synthetic approach introduces O-acetyl groups first, followed by N-acylation. Starting from the commercially available D-mannosamine hydrochloride (5), gram quantities of both 1 and 2 can be prepared over five steps in about 2-3 weeks.

Published
2006

18. Synthesis of hexa- to tridecasaccharides related to Shigella dysenteriae type 1 for incorporation in experimental vaccines

Author

Vince Pozsgay, Göran Ekborg, and Srinivasa-Gopalan Sampathkumar

Subjects
chemistry.chemical_classification, Glycosylation, Shigella dysenteriae, biology, Stereochemistry, Molecular Sequence Data, Organic Chemistry, O Antigens, Oligosaccharides, General Medicine, Oligosaccharide, HEXA, biology.organism_classification, Polysaccharide, Biochemistry, Analytical Chemistry, chemistry.chemical_compound, Carbohydrate Sequence, Shigella Vaccines, chemistry, Polysaccharides, Tetra, Tetrasaccharide, Trisaccharide
Abstract

Hexa- to tridecasaccharides corresponding to the O-specific polysaccharide (O-SP) of the Gram-negative bacterium Shigella dysenteriae type 1 were synthesized in solution phase. The syntheses utilized tetra-, octa-, and dodecasaccharide intermediates that represent one to three contiguous tetrasaccharide repeating units of the O-SP [Synlett2003, 743]. These compounds were glycosylated with mono-, di-, and trisaccharide trichloroacetamidates, which were synthesized in this study. The excellent stereodirecting effect of 4,6-O-benzophenone ketals in glycosylation reactions of 2-azido-2-deoxy-glucopyranosyl donors was demonstrated. The free oligosaccharides were characterized by 1H and 13C NMR spectroscopy and by high-resolution mass spectrometry. The oligosaccharides described herein contain the 5-(methoxycarbonyl)pentyl aglycon for eventual attachment to immunogenic carriers using a recently published protocol [J. Org. Chem.2005, 70, 6987].

Published
2006

19. Deciphering glycan linkages involved in Jurkat cell interactions with gold-coated nanofibers via sugar-displayed thiols

Author

Udayanath Aich, Pao Lin Che, Elaine Tan, Srinivasa-Gopalan Sampathkumar, Hyo Jun Kim, Jian Du, and Kevin J. Yarema

Subjects
Glycan, Glycosylation, Clinical Biochemistry, Carbohydrates, Nanofibers, Pharmaceutical Science, Biochemistry, Jurkat cells, Article, N-Acetylgalactosamine, Glycocalyx, chemistry.chemical_compound, 3D cell culture, Jurkat Cells, Polysaccharides, Drug Discovery, Humans, Sulfhydryl Compounds, Molecular Biology, chemistry.chemical_classification, biology, Organic Chemistry, Oligosaccharide, Sialic acid, chemistry, Cell culture, biology.protein, Microscopy, Electron, Scanning, Molecular Medicine, Gold
Abstract

Metabolic oligosaccharide engineering (MOE) provides a method to install novel chemical functional groups into the glycocalyx of living cells. In this Letter we use this technology to compare the impact of replacing natural sialic acid, GalNAc, and GlcNAc with their thiol-bearing counterparts in Jurkat and HL-60 cells. When incubated in the presence of gold-coated nanofibers, only Jurkat cells incubated with Ac5ManNTGc—an analogue that installs thiols into sialosides—experienced a distinctive ‘spreading’ morphology. The comparison of Ac5ManNTGc with Ac5GalNTGc and Ac5GlcNTGc in the two cell lines implicated sialosides of N-linked glycans as critical molecular mediators of the unusual responses evoked in the Jurkat line.

Published
2011

20. Targeting Pro-Invasive Oncogenes with Short Chain Fatty Acid-Hexosamine Analogs Inhibits the Mobility of Metastatic MDA-MB-231 Breast Cancer Cells

Author

Mary M. Wen, Sean S. Choi, Katharina Maisel, Udayanath Aich, Jean J. Wang, Srinivasa-Gopalan Sampathkumar, Kevin J. Yarema, Christopher T. Campbell, and Christopher Weier

Subjects
Receptors, CXCR4, Chemistry, Pharmaceutical, Antineoplastic Agents, Breast Neoplasms, CXCR4, Models, Biological, Article, Metastasis, Epigenesis, Genetic, Transcription (biology), Cell Line, Tumor, Drug Discovery, medicine, Humans, Neoplasm Metastasis, MUC1, Chemistry, Fatty Acids, NF-kappa B, Cancer, Biological activity, Hexosamines, medicine.disease, Biochemistry, Aminosugar, Matrix Metalloproteinase 9, Cell culture, Drug Design, Cancer research, Molecular Medicine
Abstract

Per-butanoylated N-acetyl-D-mannosamine (Bu(4)ManNAc), a SCFA-hexosamine cancer drug candidate with activity manifest through intact n-butyrate-carbohydrate linkages, reduced the invasion of metastatic MDA-MB-231 breast cancer cells unlike per-butanoylated-D-mannose (Bu(5)Man), a clinically tested compound that did not alter cell mobility. To gain molecular-level insight, therapeutic targets implicated in metastasis were investigated. The active compound Bu(4)ManNAc reduced both MUC1 expression and MMP-9 activity (via down-regulation of CXCR4 transcription), whereas "inactive" Bu(5)Man had counterbalancing effects on these oncogenes. This divergent impact on transcription was linked to interplay between HDACi activity (held by both Bu(4)ManNAc and Bu(5)Man) and NF-kappaB activity, which was selectively down-regulated by Bu(4)ManNAc. Overall, these results establish a new therapeutic end point (control of invasion) for SCFA-hexosamine hybrid molecules, define relative contributions of molecular players involved in cell mobility and demonstrate that Bu(4)ManNAc breaks the confounding link between beneficial HDACi activity and the simultaneous deleterious activation of NF-kappaB often found in epigenetic drug candidates.

Published
2008

21. Dendrimers in Cancer Treatment and Diagnosis

Author

Kevin J. Yarema and Srinivasa-Gopalan Sampathkumar

Subjects
Biodistribution, Materials science, Biocompatibility, Biological property, Dendrimer, Drug delivery, Cancer therapy, Nanotechnology, Gene delivery, Combinatorial chemistry, Cancer treatment
Abstract

The sections in this article are Overview Introduction Basic Properties and Applications of Dendrimers Structural Features and Chemical and Biological Properties Basic Features of Dendritic Macromolecules are Inspired by Nature Comparison of the Properties of Dendrimers and Conventional Synthetic Polymers Comparison of the Properties of Dendrimers and Proteins (a Biological Polymer) Dendritic Macromolecules Possess a Wealth of Possible Applications Methods for Dendrimer Synthesis History and Basic Strategies Cascade Reactions are the Foundation of Dendrimer Synthesis Dendrimer Synthesis has Expanded Dramatically in the Past Two Decades Strategies, Cores, and Building Blocks for Dendritic Macromolecules Dendrimers are Constructed from Simple “Building Blocks” The Synthesis of Dendrimers Follows Either a Divergent or Convergent Approach Heterogeneously-functionalized Dendrimers Basic Description and Synthetic Considerations Glycosylation is an Example of Surface Modification with Multiple Bioactivities Dendrimers in Drug Delivery Dendrimers are Versatile Nano-devices for the Delivery of Diverse Classes of Drugs Dendritic Drug Delivery: Encapsulation of Guest Molecules Dendrimers have Internal Cavities that can Host Encapsulated Guest Molecules Using Dendrimers for Gene Delivery Release of Encapsulated “Pro-drugs” Covalent Conjugation Strategies Dendrimers Overcome many Limitations Inherent in Polymeric Conjugation Strategies Dendrimer Conjugates can be Used as Vaccines Release of Covalently-delivered “Pro-drugs” Fine-tuning Dendrimer Properties to Facilitate Delivery and Ensure Bioactivity Delivery Requires Avoiding Non-specific Uptake “Local” Considerations: Contact with, and Uptake by, the Target Cell Drug Delivery: Ensuring the Biocompatibility of Dendritic Delivery Vehicles Biocompatibility Entails Avoiding “Side Effects” such as Toxicity and Immunogenicity Water Solubility and Immunogenicity Inherent and Induced Toxicity Dendrimers in Cancer Diagnosis and Treatment Dendrimers have Attractive Properties for Cancer Treatment Dendrimer-sized Particles Passively Accumulate at the Sites of Tumors Multifunctional Dendrimers can Selectively Target Biomarkers found on Cancer Cells Methods for Targeting Specific Biomarkers of Cancer Targeting by Folate, a Small Molecule Ligand Targeting by Monoclonal Antibodies Dendrimers in Cancer Diagnosis and Imaging Labeled Dendrimers are Important Research Tools for Biodistribution Studies Towards Clinical Use: MRI Imaging Agents Steps Towards the Clinical Realization of Dendrimer-based Cancer Therapies The Stage is now set for Dendrimer-based Cancer Therapy Boron Neutron Capture Therapy Innovations Promise to Speed Progress “Mix-and-Match” Strategy of Bifunctional Dendritic Clusters Towards Therapeutic Exploitation of Glycosylation Abnormalities found in Cancer Towards Targeting Metabolically-engineered Carbohydrate Epitopes Concluding Remarks Acknowledgments

Published
2007

22. Metabolic expression of thiol-derivatized sialic acids on the cell surface and their quantitative estimation by flow cytometry

Author

Kevin J. Yarema, Mark B. Jones, and Srinivasa-Gopalan Sampathkumar

Subjects
Oligosaccharides, Jurkat cells, General Biochemistry, Genetics and Molecular Biology, Flow cytometry, Cell membrane, chemistry.chemical_compound, Jurkat Cells, medicine, Humans, Sulfhydryl Compounds, Fluorescein, chemistry.chemical_classification, biology, medicine.diagnostic_test, Cell Membrane, Hexosamines, Flow Cytometry, N-Acetylneuraminic Acid, Sialic acid, medicine.anatomical_structure, chemistry, Biochemistry, Thiol, biology.protein, N-Acetylneuraminic acid, Oxidation-Reduction, Avidin
Abstract

The N-acetyl-D-mannosamine (ManNAc) analog Ac5ManNTGc, a non-natural metabolic precursor for the sialic acid biosynthetic pathway, can be used to display thiols on the cell surface. Sugar-expressed cell-surface thiols are readily accessible compared to their protein counterparts, making them ideal for exploitation in cell-adhesion and tissue-engineering applications. This report describes a protocol for the incubation of Jurkat (human acute T-cell leukemia) cells with Ac5ManNTGc and the quantitative estimation of the resulting sialic acid displayed thiols by flow cytometry after a reaction with a water-soluble biotin-conjugated maleimide reagent and fluorescein isothiocyanate-conjugated (FITC) avidin staining. These methods, with minimal optimization, are generally also applicable to other human cell lines. The labeling and flow cytometry steps of this protocol can be performed in five to eight hours.

Published
2007

23. Sialic acid and the central nervous system: perspectives on biological functions, detection, imaging methods and manipulation

Author

Kevin J. Yarema, Srinivasa-Gopalan Sampathkumar, and Adrienne V. Li

Subjects
Central Nervous System, Diagnostic Imaging, Modern medicine, Glycosylation, Central nervous system, Biology, chemistry.chemical_compound, Gangliosides, medicine, Animals, Humans, Glycoproteins, Pharmacology, Brain Chemistry, medicine.diagnostic_test, Glycobiology, Brain Diseases, Metabolic, General Neuroscience, Brain, Magnetic resonance imaging, N-Acetylneuraminic Acid, Sialic acid, Functional imaging, medicine.anatomical_structure, chemistry, Positron emission tomography, Molecular Probes, Neural function, Cell Surface Extensions, Neuroscience
Abstract

Glycobiology, broadly defined as the study of sugars in living systems, is becoming increasingly important for understanding the basic biology of the central nervous system (CNS) and diagnosing and devising new treatments for neurological disorders. Decades of research have uncovered many roles for both glycolipids and glycoproteins in the proper functioning of the brain; moreover many diseases are characterized by abnormalities in either the biosynthesis or catabolism of these cellular components. In many cases, however, only a rudimentary understanding of the basic biological roles of sugars in neural function exists. Similarly, methods to detect and diagnose glycosylation disorders are far from state-of-the-art compared to many facets of modern medicine. This review focuses on sialic acid, arguably the most important monosaccharide in CNS, and describes how recent advances in its manipulation by chemical and metabolic methods hold the possibility to converge with advanced instrumentation such as magnetic resonance imaging, positron emission tomography, diffusion tensor imaging, and single photon emission computerized tomography now used for imaging of the CNS in human subjects. Specifically, methods are under development for tagging sialic acids in living systems with contrast agents suitable for magnetic resonance imaging, in essence allowing for the functional imaging of sugars at a molecular level. One of these methods, biochemical engineering of sialic acids by use of small molecule metabolic substrates, also holds promise for the manipulation of sialic acids for the development of novel therapies for neurological disorders.

Published
2006

24. Metabolic installation of thiols into sialic acid modulates adhesion and stem cell biology

Author

Mark B. Jones, Adrienne V. Li, Zhonghui Sun, Kevin J. Yarema, and Srinivasa-Gopalan Sampathkumar

Subjects
Surface Properties, Molecular Conformation, Biology, Cell morphology, Ligands, Jurkat cells, Glycocalyx, chemistry.chemical_compound, Jurkat Cells, Tissue engineering, Cell Adhesion, Humans, Sulfhydryl Compounds, Molecular Biology, beta Catenin, chemistry.chemical_classification, Stem Cells, Cell Membrane, Cell Differentiation, Hexosamines, Cell Biology, Adhesion, Oligosaccharide, N-Acetylneuraminic Acid, Cell biology, Sialic acid, Up-Regulation, chemistry, Gold, Stem cell
Abstract

Metabolic 'oligosaccharide engineering' methods based on N-acetyl-D-mannosamine (ManNAc) analogs allow the glycocalyx of living cells to be remodeled. Herein we report the analog Ac(5)ManNTGc (1) that enables thiols to be expressed in surface sialic acids. By locating this versatile functional group on the outer periphery of normally nonadhesive human Jurkat cells, we obtained spontaneous cell-cell clustering and attachment to complementary maleimide-derivatized substrates. When analyzed in human embryoid body-derived (hEBD) stem cells, Ac(5)ManNTGc induced beta-catenin expression and altered cell morphology, consistent with neuronal differentiation. Notably, these effects were modulated by the growth substrate of the cells, with a stronger response observed on a gold surface than on glass. Together, these results establish sugar analogs as small-molecule tools for tissue engineering by providing a method for attaching cells to scaffolds via their surface carbohydrates as well as offering a means to influence stem cell fates.

Published
2005

25. Targeting cancer cells with dendrimers

Author

Srinivasa-Gopalan Sampathkumar and Kevin J. Yarema

Subjects
Zipper, Clinical Biochemistry, Receptors, Cell Surface, Biology, Biochemistry, chemistry.chemical_compound, Dendrimer, Neoplasms, Drug Discovery, Polyamines, Moiety, Humans, Bifunctional, Molecular Biology, Pharmacology, Drug Carriers, Folate Receptors, GPI-Anchored, General Medicine, DNA, Combinatorial chemistry, chemistry, Folate receptor, Cancer cell, Molecular Medicine, Fluorescein, Carrier Proteins
Abstract

Bifunctional PAMAM-based dendrimers that selectively target cancer cells are described in this issue of Chemistry & Biology [1]. The targeting moiety for folate receptor is complexed to an imaging or therapeutic agent by a DNA "zipper"—a versatile strategy to create libraries of novel drugs.

Published
2005

26. Establishment of N-acetylmannosamine (ManNAc) analogue-resistant cell lines as improved hosts for sialic acid engineering applications

Author

Mark B. Jones, Jun Kyu Rhee, Kevin J. Yarema, Eun Jeong Kim, and Srinivasa-Gopalan Sampathkumar

Subjects
Cell Survival, Cell, Drug Resistance, Apoptosis, Biology, law.invention, chemistry.chemical_compound, Jurkat Cells, Species Specificity, law, N-Acetylmannosamine, medicine, Staurosporine, Humans, Cell Proliferation, Dose-Response Relationship, Drug, Hexosamines, N-Acetylneuraminic Acid, Sialic acid, medicine.anatomical_structure, Genetic Enhancement, Biochemistry, chemistry, Gene Expression Regulation, Cell culture, Recombinant DNA, DNA fragmentation, Biotechnology, medicine.drug
Abstract

Metabolic substrate-based sialic acid engineering techniques, where exogenously supplied N-acetylmannosamine (ManNAc) analogues are utilized by the sialic acid biosynthetic pathway, allow the cell surface to be endowed with novel physical and chemical properties and show promise for increasing the quality of recombinant glycoproteins. The in vitro toxicity of many ManNAc analogues, however, hinders the large-scale adoption of this technology. In this study, we used a selection strategy where cells were subjected to progressively higher levels of ManNAc analogues to establish novel cell lines that showed decreased sensitivity to analogue-induced in vitro toxicity. The decreased sensitivity to sugar analogue-induced apoptosis, demonstrated by the Annexin V-FITC detection method and DNA fragmentation assays, corresponded to increased sialic acid production in the resistant cell lines. The ManNAc analogue-resistant cell lines exhibited cross-resistance to apoptosis induced by staurosporine and an apoptosis-activating Fas antibody. We propose that the selection strategy employed to develop these novel cell lines, which serve as superior hosts for substrate-based sialic acid engineering applications, will generally apply to the development of host cell lines for biotechnology applications.

Published
2004

27. Electrochemically active, anti-biofouling polymer adlayers on indium-tin-oxide electrodes

Author

Kevin J. Yarema, Srinivasa-Gopalan Sampathkumar, Eun Jeong Kim, Daekyung Sung, Kyuwon Kim, Sangyong Jon, Sangjin Park, Hee Young Shin, and Sung-Yool Choi

Subjects
Optics and Photonics, Materials science, Polymers, Inorganic chemistry, Catalysis, Coupling reaction, Polyethylene Glycols, Adsorption, Electrochemistry, Materials Chemistry, Organosilicon Compounds, Biomass, Electrodes, chemistry.chemical_classification, Metals and Alloys, Tin Compounds, Self-assembled monolayer, General Chemistry, Polymer, Surfaces, Coatings and Films, Electronic, Optical and Magnetic Materials, Microelectrode, chemistry, Covalent bond, Electrode, Ceramics and Composites, Methacrylates, Surface modification, Oxidation-Reduction
Abstract

Here we report the synthesis of a novel electrochemically active polymer, preparation of adlayers of the polymer on optically transparent electrodes, and an application of the adlayers to immobilization of engineered cells through a direct covalent coupling reaction.

Published
2008

30. Electrochemically active, anti-biofouling polymer adlayers on indium-tin-oxide electrodes.

Author

Eun Jeong Kim, Hee-Young Shin, Sangjin Park, Daekyung Sung, Sangyong Jon, Srinivasa-Gopalan Sampathkumar, Kevin J. Yarema, Sung-Yool Choi, and Kyuwon Kim

Subjects
ELECTROCHEMISTRY, CHEMICAL reactions, POLYMERS, ELECTRODES
Abstract

Here we report the synthesis of a novel electrochemically active polymer, preparation of adlayers of the polymer on optically transparent electrodes, and an application of the adlayers to immobilization of engineered cells through a direct covalent coupling reaction. [ABSTRACT FROM AUTHOR]

Published
2008
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