Your search keyword '"Metkar, Sunil S."' showing total 4 results

1. A Novel Mechanism for Protein Delivery.

Author

Raja, Srikumar M., Metkar, Sunil S., Höning, Stefan, Baikun Wang, Russin, William A., Pipalia, Nina H., Menaa, Cheikh, Belting, Mattias, Xuefang Cao, Dressel, Raif, and Froelich, Christopher J.

Subjects

*PROTEINS, *GLYCOSAMINOGLYCANS, *MUCOPOLYSACCHARIDES, *T cells, *BINDING sites, *LYMPHOCYTES

Abstract

The molecular interaction of secreted granzyme B-serglycin complexes with target cells remains undefined. Targets exposed to double-labeled granzyme Bserglycin complexes show solely the uptake of granzyme B. An in vitro model demonstrates the exchange of the granzyme from serglycin to immobilized, sulfated glycosaminoglycans. Using a combination of cell binding and internalization assays, granzyme B was found to exchange to sulfated glycosaminoglycans and, depending on the cell type, to higher affinity sites. Apoptosis induced by purified granzyme B and cytotoxic T-cells was diminished in targets with reduced cell surface glycosaminoglycan content. A mechanism of delivery is proposed entailing electrostatic transfer of granzyme B from serglycin to cell surface proteins. [ABSTRACT FROM AUTHOR]

Published

2005

2. Detection of functional cell surface perforin by flow cytometry

Author

Metkar, Sunil S., Wang, Baikun, and Froelich, Christopher J.

Subjects

*CELL membranes, *PROTEOGLYCANS, *GLYCOPROTEINS, *KILLER cells

Abstract

Abstract: How perforin (PFN) delivers the granzymes during cytotoxic granule mediated apoptosis remains a mystery. A major obstacle has been the inability to visualize PFN in either monomeric or polymeric form after interaction with the target cell surface. An antibody based technique is described which detects cell surface PFN on intact cells by flow cytometry. The methodology requires the presence of calcium (Ca2+) at a concentration which supports binding but not polymerization of PFN. Functionality was ensured by showing the cell surface PFN was able to deliver GrB causing caspase-3 activation and mitochondrial depolarization. The technique demonstrates a role for heparan sulfate proteoglycans in PFN binding. Further, the variable sensitivity of effector versus target cell lines to the permeabilizing effects of PFN could not be attributed to differential binding of PFN. [Copyright &y& Elsevier]

Published

2005

3. Cytotoxic granule-mediated apoptosis: unraveling the complex mechanism

Author

Raja, Srikumar M, Metkar, Sunil S, and Froelich, Christopher J

Subjects

*APOPTOSIS, *CYTOPLASMIC granules, *ANTINEOPLASTIC antibiotics, *PROTEOGLYCANS

Abstract

The molecular details of cytotoxic granule-mediated apoptosis have been gleaned from the study of the effects of isolated granzymes and perforin on target cells. Recent evidence indicates that the physiological apoptosis-inducing form is a multi-component macro-complex consisting of cationic granule proteins non-covalently linked to the chondroitin-sulfate proteoglycan, serglycin. [Copyright &y& Elsevier]

Published

2003

4. Human perforin permeabilizing activity, but not binding to lipid membranes, is affected by pH

Author

Praper, Tilen, Beseničar, Mojca Podlesnik, Istinič, Helena, Podlesek, Zdravko, Metkar, Sunil S., Froelich, Christopher J., and Anderluh, Gregor

Subjects

*PROTEINS, *BILAYER lipid membranes, *HYDROGEN-ion concentration, *NATURAL immunity, *IMMUNE response, *SURFACE plasmon resonance, *T cells, *EPIDERMAL growth factor

Abstract

Abstract: The various steps that perforin (PFN), a critical mediator of innate immune response, undertakes to form a transmembrane pore remains poorly understood. We have used surface plasmon resonance (SPR) to dissect mechanism of pore formation. The membrane association of PFN was calcium dependent irrespective of pH. However, PFN does not permeabilize large or giant unilamellar vesicles (GUV) at pH 5.5 even though the monomers bind to the membranes in the presence of calcium. It was possible to activate adsorbed PFN and to induce membrane permeabilization by simply raising pH to a physiological level (pH 7.4). These results were independently confirmed on GUV and Jurkat cells. The conformational state of PFN at either pH was further assessed with monoclonal antibodies Pf-80 and Pf-344. Pf-344 maps to a linear epitope within region 373–388 of epidermal growth factor (EGF)-like domain while the Pf-80 appears to recognize a conformational epitope. Pf-344 interacts with the EGF-like domain after PFN monomers undergo pore formation, the site recognized by Pf-80 is only accessible at acidic but not neutral pH. Thus, the Pf-80 mAb likely interacts with a region of the monomer that participates in oligomerization prior to insertion of the monomer into the lipid bilayer and thus may have therapeutic utility against PFN-mediated immunopathology. [ABSTRACT FROM AUTHOR]

Published

2010