SBIR-STTR Award

Adherence of pathogens to their host cells is the obligatory first step in infection and is frequently mediated by specific molecular interactions [1, 2]. Virulent Campylobacter species and pathogenic strains of Norwalk virus, the leading bacterial and viral causes of human infectious diarrhea [3], adhere to gut epithelial surfaces through binding to 1(1, 2) fucosylated cellular receptors [4, 5]. 1(1, 2) fucosylated glycans, which are abundant in human breast milk [6, 7], have been shown both in vitro and in vivo effectively to prevent binding and infection by these pathogens [4,5]. These molecules therefore represent a new class of agent with potential to prevent infectious diarrhea, a condition which is the cause annually of over 2 million deaths worldwide [8]. However the production of a(1, 2) fucosylated glycans as anti-infective agents in sufficient quantities to impact global diarrhea incidence remains a significant challenge. Chemical syntheses are possible, but are limited by stereo-specificity issues, product impurities, and high overall cost [9-11]. In vitro enzymatic syntheses are also possible but are limited by a requirement for expensive nucleotide-sugar precursors. Glycosyn Inc.'s broad goal is to develop ways to manufacture a(1,2) fucosylated glycans cheaply and in bulk through microbial fermentation, and three classes of potential anti-infective products are envisaged: 1) purified a(1,2) fucosylated oligosaccharides, 2) yeast strains expressing a(1,2) fucosylated glycans on their cell surface, and 3) purified a(1,2) fucosylated glycoproteins. The goal of the studies outlined in this application are to synthesize, purify, and test as a nutritional supplement, an example of the first of these product classes, namely a purified a(1,2) fucosylated oligosaccharide, 2-fucosyllactose (2FL). Glycan synthetic pathways in the common dairy yeast Kluyveromyces lactis will be engineered through a combination of endogenous gene manipulation and the introduction of heterologous genes encoding desired activities. Specifically, K.lactis will be engineered to synthesize the key precursor sugar, GDP-fucose, and subsequently to make 2-fucosyllactose in the cell cytoplasm. Yields of product will be optimized, and extraction and purification schemes will be developed. Purified 2-fucosyllactose produced in K.lactis will be tested for efficacy both in vitro and in vivo in models of infection.

Public Health Relevance:
Worldwide, infectious diarrhea [12] is responsible for approximately 20% of all mortality in children under the age of 5, and for an estimated 2.5 millions deaths annually [8]. In the United States infectious diarrhea has an annual incidence of over 200 million cases and is responsible for approximately 900,000 hospitalizations and 5,000 deaths per year [3, 13]. Infection by Norwalk-like viruses is by far the single largest cause of infectious diarrhea in the US, with the single largest bacterial cause being infection by Campylobacter species. The surface a(1,2) fucosylated probiotic K.lactis that is the subject of this application will target both Norwalk-like viruses and C.jejuni, as well as other fucose-binding enteropathogens.

Public Health Relevance:
This Public Health Relevance is not available.

Thesaurus Terms:
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Adherence of pathogens to their host cells is the obligatory first step of infection and is frequently mediated by specific molecular interactions [1][2]. Virulent Campylobacter species, Vibrio cholerae, enteropathogenic E.coli (EPEC), enterohemorrhagic E.coli (EHEC) and pathogenic strains of Norwalk virus, the leading bacterial and viral causes of human infectious diarrhea [3], adhere to gut epithelial surfaces through binding to 1(1,2) fucosylated cellular receptors[4][5]. 1(1,2) fucosylated glycans, which are abundant in human breast milk[6][7], have been shown both in vitro and in vivo effectively to prevent binding and infection by these pathogens[4][5]. These molecules therefore represent a new class of agent with potential to prevent infectious diarrhea, a condition that is the cause annually of over 2 million deaths worldwide [8]. However the production of 1(1,2) fucosylated glycans as anti-infective agents in sufficient quantities to impact global diarrhea incidence remains a significant challenge. Chemical syntheses are possible, but are limited by stereo-specificity issues, product impurities, and high overall cost[9][10][11]. In vitro enzymatic syntheses are also possible but are limited by a requirement for expensive nucleotide-sugar precursors. Glycosyn Inc.
Public Health Relevance:
Worldwide, infectious diarrhea[12] is responsible for approximately 20% of all mortality in children under the age of 5, and for an estimated 2 million deaths annually[8]. In the developing world bacterial infections cause more than 50% of all cases of diarrhea, and of these, infections by Campylobacter and diarrheagenic E.coli together account for about half. Campylobacter is the most common cause of culture-proven bacterial gastroenteritis in both developed and developing countries, and is responsible for 400 to 500 million cases of diarrhea each year. By far the highest incidence of Campylobacter infections is in children <5 yrs of age[13][14][15]. Unfortunately, prevention and treatment options for bacterial diarrhea are limited. Vaccines are currently unavailable, and if developed, would be costly and of limited availability in rural poor populations where unmet need is highest. Moreover vaccines are typically pathogen-specific, but infectious diarrhea can be caused by numerous diverse pathogens. The use of antibiotics for treatment of diarrhea is also becoming increasingly problematic, since such use is driving the emergence of resistant strains. For example, clinical isolates of Campylobacter are now often resistant to quinolones [16] and erythromycin-resistant strains are rapidly emerging [17]. Conventional antimicrobial agents are designed to inhibit a pathogen
Thesaurus Terms:
0-11 Years Old; Accounting; Achievement; Achievement Attainment; Adherence; Adherence (Attribute); Adhesives; Age; Anti-Adhesion Agent; Anti-Infective Agents; Anti-Infective Drugs; Anti-Infectives; Anti-Infective Preparation; Antiinfective Drugs; Antiinfectives; Antibiotic Therapy; Antibiotic Treatment; Antiinfective Agents; Applications Grants; Automobile Driving; Bacterial Gastroenteritis; Bacterial Infections; Benign; Binding; Binding (Molecular Function); Bioreactors; Breast Milk; C. Jejuni; C.Jejuni; Campylobacter; Campylobacter Infection; Campylobacter Jejuni; Campylobacteriosis; Cell Survival; Cell Viability; Cell Surface; Cells; Cessation Of Life; Cheese; Child; Child Youth; Children (0-21); Clinical; Cytoplasm; D-Mannose; Death; Dehydratases; Deoxygalactose; Developing Countries; Developing Nations; Diarrhea; Diet; Drivings, Automobile; E-Mycin; Ehec; Ehec, Escherichia Coli; Epec; Etec; Engineering; Engineerings; Enterohemorrhagic E Coli; Enterohemorrhagic E. Coli; Enterohemorrhagic E.Coli; Enterohemorrhagic Escherichia Coli; Enterohemorrhagic Strain Of E Coli; Enterohemorrhagic Strain Of E. Coli; Enterohemorrhagic Strain Of Escherichia Coli; Enzyme Precursors; Enzymes; Epithelial; Epithelium; Equilibrium; Ery-Tab; Eryc; Eryderm; Erythrocin; Erythromycin; Erythromycin A; Escherichia Coli Ehec; Fda; Fermentation; Food And Drug Administration; Food And Drug Administration (U.S.); Fucose; Fucosyltransferase 2; Gdp Fucose; Galactoside 2-Alpha-L-Fucosyltransferase 2; Generalized Growth; Genes; Genome; Glycans; Glycoproteins; Goals; Grant; Grant Proposals; Grants, Applications; Growth; Guanosine 5'-(Trihydrogen Diphosphate), P'-(6-Deoxy-Beta-L-Galactopyranosyl) Ester; Guanosine Diphosphate Fucose; Guanosine Diphosphofucose; Human; Human Milk; Human Mother's Milk; Human, Child; Human, General; Hydrases; Hydro-Lyases; Ilotycin; In Vitro; Incidence; Infection; Infection Prevention; Kluyveromyces; Less-Developed Countries; Less-Developed Nations; Ligase; Literature; Mammary Gland Milk; Man (Taxonomy); Man, Modern; Mannopyranose; Mannopyranoside; Mannose; Mediating; Methods; Milk, Human; Modeling; Molecular Interaction; Mortality; Mortality Vital Statistics; Norwalk Agent; Norwalk Virus; Oligosaccharides; Oral; Organism; Pathway Interactions; Pediamycin; Performance; Phase; Polysaccharides; Population; Pressure; Pressure- Physical Agent; Prevent Infection; Prevention; Procedures; Production; Proenzymes; Progress Reports; Proliferating; Public Health; Qualifying; Quinolone Resistant; Rp-Mycin; Receptor Protein; Research; Research Activity; Resistance; Resistance Development; Resistant Development; Robimycin; Running; Rural; Sbir; Sbirs (R43/44); Stec; Secretor Blood Group Alpha-2-Fucosyltransferase; Shiga Toxin-Producing E Coli; Shiga Toxin-Producing E. Coli; Shiga Toxin-Producing E.Coli; Shiga Toxin-Producing Escherichia Coli; Small Business Innovation Research; Small Business Innovation Research Grant; Specificity; Surface; Synthetases; System; System, Loinc Axis 4; Testing; Third-World Countries; Third-World Nations; Tissue Growth; Usfda; Under-Developed Countries; Under-Developed Nations; United States Food And Drug Administration; V. Cholerae; V.Cholerae; Vaccines; Vibrio Cholerae; Vibrio Comma; Viral; Virulent; Yeasts; Zymogens; Alpha-Fucose; Anti-Microbial Agent; Anti-Microbial Drug; Antimicrobial Agent; Antimicrobial Drug; Bacterial Disease; Balance; Balance Function; Chemical Synthesis; Children; Commercialization; Communicable Disease Control Agent; Cost; Design; Designing; Developing Resistance; Driving; Efficacy Testing; Enteropathogenic E. Coli; Enteropathogenic E.Coli; Enteropathogenic Escherichia Coli; Enterotoxigenic E. Coli; Enterotoxigenic E.Coli; Enterotoxigenic Escherichia Coli; Genetic Manipulation; Improved; In Vivo; Living System; Microbial; Novel; Ontogeny; Pathogen; Pathway; Pressure; Prevent; Preventing; Public Health Medicine (Field); Public Health Relevance; Quinolone Resistance; Receptor; Resistance To Quinolone; Resistant; Resistant Strain; Resistant To Quinolone; Sugar; Sugar Nucleotide; Synthetic Enzyme; Treatment Of Bacterial Diseases; Treatment Of Bacterial Infectious Disease; Youngster