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Volume 7, Issue 1 (Suppl)

J Biotechnol Biomater

ISSN: 2155-952X JBTBM, an open access journal

March 20-21, 2017 Rome, Italy

&

15

th

World Congress on

2

nd

International Conference on

Biotechnology And Biotech Industries Meet

Enzymology and Molecular Biology

Enzymology & Mol. Biology 2017

Biotechnology Congress 2017

March 20-21, 2017

Metabolic engineering strategies for effective use of glycosyltransferases in oligosaccharide synthesis

Rachel Chen

Georgia Institute of Technology, USA

A

s one of the four building blocks of life, sugar molecules permeate almost all aspects of life. The widespread occurrence of

glycosylation and its broad impact in biological processes underscores the importance of studying glycosylation. To study glycans

and probe their roles in a biological system significant amount of pure molecules are needed. Besides basic research, there are a wide

range of opportunities of utilizing oligosaccharides, polysaccharides and glycoproteins and other glyco-conjugates for diagnosis,

vaccine development, as new drug entities and many other medical applications. Unfortunately, these potential applications are all

impeded by the lack of large scale synthesis technology for these molecules. Metabolic engineering, since its inception in late 80’s,

has grown to be a field impactful in the synthesis of a variety of molecules of commercial and societal importance. Opportunities

abound at the interface of glycosciences and metabolic engineering. In fact, all sugar moieties in biological components, small or big,

free or bound, are important targets for metabolic engineering. Over the past decades, its use in the synthesis of sugar-containing

molecules has gained significance. Glycosidic bond formation catalyzed by glycosyltransferase enzyme is in the center of the synthesis

of most glycan structures in nature. Oligosaccharides, polysaccharides and glycoproteins share the commonality that requires

glycosyltransferases in their synthesis, differing only in the nature of the acceptors. Therefore, from a metabolic engineering point

of view, they share much of the synthesis challenges. These include the high energy demand due to the need for sugar nucleotides as

precursors, the complexity of metabolic pathways and regulations involved and the adequate supply of acceptors when and where

the glycosyltransferases are most active. Represented by 2’-fucosyllactose, the success in bringing highly valuable oligosaccharides

to commercial production demonstrates the power of metabolic engineering. On the other hand, given the enormous diversity and

significant complexity of saccharide-containing structures, a handful of molecules attaining commercial success can only qualify

as a promising beginning. In fact, the surface of the gigantic glyco-sphere has barely scratched. Providing scientists with hundreds

and thousands of glycans in quantities sufficient to probe their structure and functional relationships and supplying clinicians with

selective compounds (such as Globo H and heparin in Kg quantities) for clinical studies in a cost effective manner are challenges

before metabolic engineers and synthetic biologists. The inherent challenges in complex carbohydrates demands innovative metabolic

engineering strategies beyond a simple extension of those used in successful examples. In this presentation, metabolic engineering

challenges common to glycosyltransferase-catalyzed synthesis of oligosaccharides are analyzed and successful examples from Chen

labs are showcased to emphasize the power of metabolic engineering as an enabling technology.

Biography 

Rachel Chen has done her PhD from California Institute of Technology in 1994 and subsequently worked as a Research Scientist in Bristol-Myers Squibb. She

began her independent academic career in Virginia Commonwealth University and continued at Georgia Institute of Technology. Her research interfaces biology,

chemistry and engineering with major focus on applying molecular engineering tools in the synthesis of molecules that are not attainable with conventional means.

She has published over 80 peer-reviewed papers and has been serving as an Associate Editor for

Microbial Cell Factories

and on Editorial Boards of

Biotechnology

and Bioengineering, AIMS Bioengineering

and

AIMS Microbiology

.

rchen@chbe.gatech.edu

Rachel Chen, J Biotechnol Biomater 2017, 7:1(Suppl)

http://dx.doi.org/10.4172/2155-952X.C1.070