Biolubrication: Structural investigation of lubricin and its glycosylation
Sammanfattning
The sliding articular cartilage surfaces of the human diarthrodial joints are surrounded by
biolubricating synovial fluid (SF), creating a perfect low friction biological biobearing
structure with excellent lubrication and wear resistance, even during motion. Lubrication is
predominately provided by surface adhered biomolecules including phospholipids,
hyaluronic acid and synovial lubricin. Inflammation, such as arthritis and injury, changes
the joint assembly resulting in detachment of essential surface molecules, increasing
friction and wear of the sliding articular cartilage. Changes in the composition and
distribution of these surface molecules is suggested to aggravate the disease. The
lubricative, heavily glycosylated mucin-like synovial glycoprotein, lubricin, has previously
been observed to contain glycosylation changes related to rheumatoid arthritis and
osteoarthritis. Therefore, a structural investigation of lubricin and its glycosylation was
initiated in order to better understand the biolubricating ability of lubricin and its
pathological involvement in arthritis diseases. An investigation was undertaken to better
understand the nature of the dominant glycan structure, sialic acid. Sialidase specific for
α2-3 linked sialic acid and subsequent UniCarb-DB fragment spectra comparison of the
resultant structure indicated the exclusive 3-linked nature of core 2 sialylation. However,
core 1 structures had both 3 and 6 linked sialylation. In arthritis, lubricin has been shown to
degrade as identified by its fragments in the synovial fluid. This may open up a new
possibility for identification of disease specific biomarker. The mass spectrometric
glycopeptide analysis showed that lubricin contains an extended serine, threonine and
proline (STP) rich domain composed of imperfect tandem repeats (EPAPTTPK), the target
for O-glycosylation. The N-acetylgalactosaminyltransferase (GALNTs) expression analysis
of the fibroblast-like synoviocytes showed high expression of the less understood GALNT5
and 15 in addition to the ubiquitously expressed GALNT1 and 2. This indicated that
lubricin required a unique combination of transferase genes for its glycosylation.
Overall, this study revealed that negatively charged sialic acid in the mucin-like domain
makes the lubricin molecule amphoteric in nature, as the arginine and lysine rich protein
core is positively charged. The number of glycosylation sites and sialylation were shown to
be essential for this amphoteric nature and may be important for its function as an
amphoteric biolubricator.
Delarbeten
I. Ali, L., Kenny, D.T., Hayes, C.A., and Karlsson, N.G. (2012) Structural
Identification of O-Linked Oligosaccharides Using Exoglycosidases and
MSn Together with UniCarb-DB fragment Spectra Comparison.
Metabolites. 2(4): 648-666. ::doi::10.3390/metabo2040648 II. Ali, L., Jin, C., and Karlsson, N.G. (2012) Glycoproteomics of Lubricin-
Implication of Important Biological Glyco- and Peptide-Epitopes in
Synovial Fluid, In Rheumatoid Arthritis –Etiology Consequences and Co-
Morbidities. Intech. 131-150. ::doi::10.5772/25657 III. Flowers, S.A., Ali, L., Lane, C.S., Olin, M., and Karlsson, N.G. (2013) Selected
reaction monitoring to differentiate and relatively quantitate isomers of
sulfated and unsulfated core 1 O-glycans from salivary MUC7 protein in
rheumatoid arthritis. Mol. Cell. Proteomics. 12: 921-931. ::doi::10.1074/mcp.M113.028878 IV. Ali, L., Flowers, S.A., Jin, C., Bennet, E.P., Ekwall, A.K., and Karlsson, N.G.
(2014) The O-glycomap of Lubricin, a Novel Mucin Responsible for Joint
Lubrication, Identified by Site-Specific Glycopeptide Analysis. Mol. Cell.
Proteomics. Accepted. ::pii::mcp.M114.040865
Examinationsnivå
Doctor of Philosophy (Medicine)
Universitet
University of Gothenburg. Sahlgrenska Academy
Institution
Institute of Biomedicine. Department of Medical Biochemistry and Cell Biology
Disputation
Torsdagen den 20 November 2014, kl 13:00, Hörsal Ragnar Sandberg, Medicinaregatan 7A, Göteborg
Datum för disputation
2014-11-20
E-post
liaqat.ali@medkem.gu.se
Datum
2014-11-04Författare
Ali, Liaqat
Nyckelord
Lubricin, mass spectrometry, EPAPTTPK, GALNTs, biolubricator
Publikationstyp
Doctoral thesis
ISBN
978-91-628-9206-7
978-91-628-9207-4 (electronic)
Språk
eng