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Dive into the research topics where Ramnath Sasisekharan is active.

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Featured researches published by Ramnath Sasisekharan.


Biotechnology and Bioengineering | 1999

Regional heparinization via simultaneous separation and reaction in a novel Taylor-Couette flow device

Guillermo A. Ameer; S. Raghavan; Ramnath Sasisekharan; William E. Harmon; Charles L. Cooney; Robert Langer

The development of a safe and efficient bioreactor design has remained a challenge for the clinical application of immobilized enzymes. Specifically, the use of immobilized heparinase I has been the target of many studies to make heparin anticoagulation therapy safer for the critically ill patient with kidney failure or heart disease. We have investigated the use of Taylor-Couette flow for a novel type of bioreactor. In a previous study, we showed that the fluidization of agarose immobilized heparinase within Taylor vortices in whole blood can lead to extensive blood damage in the form of cell depletion and hemolysis. Based on these findings, we designed and developed a reactor, referred to as vortex-flow plasmapheretic reactor (VFPR), that incorporated plasmapheresis and fluidization of the agarose in the reactive compartment, separate from the whole-blood path. In the present study, immobilized heparinase I was tested as a means of achieving regional heparinization of a closed circuit. This is a method in which heparin is infused into the extracorporeal circuit predialyzer and neutralized postdialyzer. Saline studies were performed with an immobilized heparinase I-packed bed and with the VFPR. An in vitro feasibility study was performed with the VFPR using human blood. The VFPR achieved heparin conversions of 44 +/- 0.5% and 34 +/- 2% in saline and blood, respectively. In addition, the VFPR caused no blood damage. We report a novel method to achieve fluidization which depended on secondary, circumferencial flow, and was independent of the primary flow through the device.


Biochemical Journal | 1996

Expression in Escherichia coli, purification and characterization of heparinase I from Flavobacterium heparinum.

Steffen Ernst; Ganesh Venkataraman; Winkler S; Ranga Godavarti; Robert Langer; Charles L. Cooney; Ramnath Sasisekharan


Archive | 1996

Rationally designed polysaccharide lyases derived from heparinase i

Ranganathan Godavarti; Ramnath Sasisekharan; Steffen Ernst; Ganesh Venkataraman; Charles L. Cooney; Robert Langer


Archive | 1995

Method for inhibiting angiogenesis using heparinase

Ramnath Sasisekharan; Marsha A. Moses; Matthew A. Nugent; Charles L. Cooney; Robert Langer


Archive | 1992

Heparinase gene from flavobacterium heparinum

Ramnath Sasisekharan; Kelley W. Moremen; Charles L. Cooney; Joseph J. Zimmermann; Robert Langer


Archive | 1993

Purification, composition and specificity of heparinase I, II, and III from flavobacterium heparinum

Ramnath Sasisekharan; Daniel L. Lohse; Charles L. Cooney; Robert J. Linhardt; Robert Langer


Archive | 1992

Purification of heparinase I, II, and III from Flavobacterium heparinum

Ramnath Sasisekharan; Daniel L. Lohse; Charles L. Cooney; Robert J. Linhardt; Robert Langer


Biotechnology and Bioengineering | 1999

Investigation of a whole blood fluidized bed Taylor–Couette flow device for enzymatic heparin neutralization

Guillermo A. Ameer; William E. Harmon; Ramnath Sasisekharan; Robert Langer


Archive | 1995

Method for obtaining a modified heparinase gene

Ramnath Sasisekharan; Kelley W. Moremen; Charles I. Cooney; Joseph J. Zimmermann; Robert Langer


Biochemical Journal | 1999

Oligomeric self-association of basic fibroblast growth factor in the absence of heparin-like glycosaminoglycans

Joseph Davis; Ganesh Venkataraman; Zachary Shriver; Raj Pa; Ramnath Sasisekharan

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Robert Langer

Massachusetts Institute of Technology

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Charles L. Cooney

Massachusetts Institute of Technology

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Daniel L. Lohse

Massachusetts Institute of Technology

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Joseph J. Zimmermann

Massachusetts Institute of Technology

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Robert J. Linhardt

Rensselaer Polytechnic Institute

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Ganesh Venkataraman

Massachusetts Institute of Technology

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Marsha A. Moses

Boston Children's Hospital

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