Abstract

Sialic acids, which are the outermost sugars on the glycoproteins and glycolipids of mammalian cells, can be substituted at the 4,7,8, and 9 positions with O-acetyl esters (or other less common substitutions) in a tissue-specific fashion. However, little is known about the biological roles of thes ester groups. This proposal is a continuation of a detailed study of the biosynthesis and regulation of O-acetylated sialic acids. We have previously developed new methods to study O-acetylated sialic acids, discovered the phenomenon of O-acetyl migration, discovered neuraminidases that can release O-acetylated sialic acids and identified tissue culture cell lines that synthesize them. We have partially purified a sialic-acid-specific O-acetyl-esterase from human red blood cells and found that it is identical to the """"""""non-specific"""""""" esterased (which is tightly linked to the """"""""retinoblastoma gene"""""""" and the Wilson's disease gene on chromosome 13). We plan to further study this enzyme, particularly in retinoblastoma cells that are deficient in it, and to search for other sialic-acid-apecific esterases that could be involved in regulating O-acetylation. We have discovered a rat liver Golgi acetyl-coenzyme A transporter that provides the donor for the O-acetylation reaction; we plan to further study this transporter by affinity labelling, purification and re-constitution. We have begun studies aimed at purifying, characterizing and ultimately achieving the genetic cloning of the sialic acid-specific O-acetyltransferaseis) from E.Coli and from rat liver Golgi. We also propose approaches to generating """"""""high-acetylator"""""""" cell lines, and studies to directly demonstrate the subcellular sites of the O-acetylation reaction in such cells. The tools, probes and information generated from these studies will be used to understand the mechansims of regulation of O-acetylation in specific biological systems. For example, we have discovered that the sialic acids of rat and human colon become O-acetylated primarily after birth. We will further define the basis for this phenomenon, and pursue the hypothesis the change is induced by products arising from bacterial colonisation. In parallel studies we discovered O-acetylated GD3 (recognized by amuring monoclonal antibody D1.1) a developmentally regulated brain ganglioside also expressed in human melanoma cells. The biological basis for this expression can also be explored. A long-range goal is to use the genetic probes arising from these studies to attempt abrogation of O-acetylation in tissue-culture cells and in intact animals. These studies could have implications for the understanding of a wide variety of biological and pathological processes, such as cell surface involvement in development and malignant transformation, bacterial antigenicity and pathogenicity, alternate pathway complement activation and the generation of tumor antigens.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
5R01GM032373-08
Application #
3281145
Study Section
Pathobiochemistry Study Section (PBC)
Project Start
1983-08-01
Project End
1991-07-31
Budget Start
1990-08-01
Budget End
1991-07-31
Support Year
8
Fiscal Year
1990
Total Cost
Indirect Cost

  Institution

Name
University of California San Diego
Department
Type
Schools of Medicine
DUNS #
077758407
City
La Jolla
State
CA
Country
United States
Zip Code
92093

  Publications

Meng, Caicai; Sasmal, Aniruddha; Zhang, Yan et al. (2018) Chemoenzymatic Assembly of Mammalian O-Mannose Glycans. Angew Chem Int Ed Engl 57:9003-9007
Okerblom, Jonathan; Fletes, William; Patel, Hemal H et al. (2018) Human-like Cmah inactivation in mice increases running endurance and decreases muscle fatigability: implications for human evolution. Proc Biol Sci 285:
Samraj, Annie N; Bertrand, Kimberly A; Luben, Robert et al. (2018) Polyclonal human antibodies against glycans bearing red meat-derived non-human sialic acid N-glycolylneuraminic acid are stable, reproducible, complex and vary between individuals: Total antibody levels are associated with colorectal cancer risk. PLoS One 13:e0197464
Ram, Sanjay; Gulati, Sunita; Lewis, Lisa A et al. (2018) A Novel Sialylation Site on Neisseria gonorrhoeae Lipooligosaccharide Links Heptose II Lactose Expression with Pathogenicity. Infect Immun 86:
Alisson-Silva, Frederico; Liu, Janet Z; Diaz, Sandra L et al. (2018) Human evolutionary loss of epithelial Neu5Gc expression and species-specific susceptibility to cholera. PLoS Pathog 14:e1007133
Fong, Jerry J; Tsai, Chih-Ming; Saha, Sudeshna et al. (2018) Siglec-7 engagement by GBS ?-protein suppresses pyroptotic cell death of natural killer cells. Proc Natl Acad Sci U S A 115:10410-10415
Siddiqui, Shoib S; Springer, Stevan A; Verhagen, Andrea et al. (2017) The Alzheimer's disease-protective CD33 splice variant mediates adaptive loss of function via diversion to an intracellular pool. J Biol Chem 292:15312-15320
Varki, Ajit (2017) Are humans prone to autoimmunity? Implications from evolutionary changes in hominin sialic acid biology. J Autoimmun 83:134-142
Okerblom, Jonathan J; Schwarz, Flavio; Olson, Josh et al. (2017) Loss of CMAH during Human Evolution Primed the Monocyte-Macrophage Lineage toward a More Inflammatory and Phagocytic State. J Immunol 198:2366-2373
Bergfeld, Anne K; Lawrence, Roger; Diaz, Sandra L et al. (2017) N-glycolyl groups of nonhuman chondroitin sulfates survive in ancient fossils. Proc Natl Acad Sci U S A 114:E8155-E8164

Showing the most recent 10 out of 145 publications