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Author
- Briggs, David C3
- Milner, Caroline M3
- Banerji, Suneale2
- Birchenough, Holly L2
- Enghild, Jan J2
- Jackson, David G2
- Jowitt, Thomas A2
- Lawrance, William2
- Ali, Tariq1
- Baldock, Clair1
- Bhattacharjee, Shaumick1
- Coulson-Thomas, Vivien J1
- Dushek, Omer1
- Dyer, Douglas P1
- Fawcett, James W1
- Fuster, Mark M1
- Handel, Tracy M1
- Hascall, Vincent C1
- Ievoli, Elena1
- Johns, Scott C1
- Kielty, Cay M1
- Langford-Smith, Alexander WW1
- Lauer, Mark E1
- Metcalfe, Clive1
Keyword
- hyaluronan5
- extracellular matrix2
- glycosaminoglycan2
- inflammation2
- LYVE-12
- proteoglycan2
- reproduction2
- TSG-62
- astrocyte1
- avidity1
- cell adhesion1
- cell migration1
- chemokine1
- chemokine-binding protein1
- complex1
- CUB module structure1
- cumulus-oocyte complex expansion1
- dimer1
- disulfide1
- endothelial cell1
- endothelium1
- glial scar1
- Inter-α-inhibitor Heavy Chain1
- TNF-stimulated gene 6 (TSG-6)1
- X-ray crystallography1
Glycobiology and Extracellular Matrices
6 Results
- Glycobiology and Extracellular MatricesOpen Access
Inter-α-inhibitor heavy chain-1 has an integrin-like 3D structure mediating immune regulatory activities and matrix stabilization during ovulation
Journal of Biological ChemistryVol. 295Issue 16p5278–5291Published online: March 6, 2020- David C. Briggs
- Alexander W.W. Langford-Smith
- Holly L. Birchenough
- Thomas A. Jowitt
- Cay M. Kielty
- Jan J. Enghild
- and others
Cited in Scopus: 12Inter-α-inhibitor is a proteoglycan essential for mammalian reproduction and also plays a less well-characterized role in inflammation. It comprises two homologous “heavy chains” (HC1 and HC2) covalently attached to chondroitin sulfate on the bikunin core protein. Before ovulation, HCs are transferred onto the polysaccharide hyaluronan (HA) to form covalent HC·HA complexes, thereby stabilizing an extracellular matrix around the oocyte required for fertilization. Additionally, such complexes form during inflammatory processes and mediate leukocyte adhesion in the synovial fluids of arthritis patients and protect against sepsis. - Glycobiology and Extracellular MatricesOpen Access
Homodimerization of the Lymph Vessel Endothelial Receptor LYVE-1 through a Redox-labile Disulfide Is Critical for Hyaluronan Binding in Lymphatic Endothelium
Journal of Biological ChemistryVol. 291Issue 48p25004–25018Published online: October 12, 2016- Suneale Banerji
- William Lawrance
- Clive Metcalfe
- David C. Briggs
- Akira Yamauchi
- Omer Dushek
- and others
Cited in Scopus: 24The lymphatic vessel endothelial receptor LYVE-1 is implicated in the uptake of hyaluronan (HA) and trafficking of leukocytes to draining lymph nodes. Yet LYVE-1 has only weak affinity for hyaluronan and depends on receptor clustering and higher order ligand organization for durable binding in lymphatic endothelium. An unusual feature of LYVE-1 not found in other HA receptors is the potential to form disulfide-linked homodimers. However, their influence on function has not been investigated. Here we show LYVE-1 homodimers are the predominant configuration in lymphatic endothelium in vitro and in vivo, and formation solely requires the unpaired cysteine residue Cys-201 within the membrane-proximal domain, yielding a 15-fold higher HA binding affinity and an ∼67-fold slower off-rate than the monomer. - Glycobiology and Extracellular MatricesOpen Access
Tumor Necrosis Factor-stimulated Gene-6 (TSG-6) Is Constitutively Expressed in Adult Central Nervous System (CNS) and Associated with Astrocyte-mediated Glial Scar Formation following Spinal Cord Injury
Journal of Biological ChemistryVol. 291Issue 38p19939–19952Published online: July 19, 2016- Vivien J. Coulson-Thomas
- Mark E. Lauer
- Sara Soleman
- Chao Zhao
- Vincent C. Hascall
- Anthony J. Day
- and others
Cited in Scopus: 47Tumor necrosis factor (TNF)-stimulated gene-6 (TSG-6) binds to hyaluronan and can reorganize/stabilize its structure, also enhancing the binding of this glycosaminoglycan to its cell surface receptor, CD44. TSG-6 is rapidly up-regulated in response to inflammatory cytokines protecting tissues from the damaging effects of inflammation. Despite TSG-6 treatment having been shown to improve outcomes in an experimental model of traumatic brain injury, TSG-6 expression has not been extensively studied in the central nervous system (CNS). - Glycobiology and Extracellular MatricesOpen Access
The Anti-inflammatory Protein TSG-6 Regulates Chemokine Function by Inhibiting Chemokine/Glycosaminoglycan Interactions
Journal of Biological ChemistryVol. 291Issue 24p12627–12640Published online: April 4, 2016- Douglas P. Dyer
- Catherina L. Salanga
- Scott C. Johns
- Elena Valdambrini
- Mark M. Fuster
- Caroline M. Milner
- and others
Cited in Scopus: 70TNF-stimulated gene-6 (TSG-6) is a multifunctional protein secreted in response to pro-inflammatory stimuli by a wide range of cells, including neutrophils, monocytes, and endothelial cells. It has been shown to mediate anti-inflammatory and protective effects when administered in disease models, in part, by reducing neutrophil infiltration. Human TSG-6 inhibits neutrophil migration by binding CXCL8 through its Link module (Link_TSG6) and interfering with the presentation of CXCL8 on cell-surface glycosaminoglycans (GAGs), an interaction that is vital for the function of many chemokines. - Glycobiology and Extracellular MatricesOpen Access
Binding of Hyaluronan to the Native Lymphatic Vessel Endothelial Receptor LYVE-1 Is Critically Dependent on Receptor Clustering and Hyaluronan Organization
Journal of Biological ChemistryVol. 291Issue 15p8014–8030Published online: January 28, 2016- William Lawrance
- Suneale Banerji
- Anthony J. Day
- Shaumick Bhattacharjee
- David G. Jackson
Cited in Scopus: 72The lymphatic endothelial receptor LYVE-1 has been implicated in both uptake of hyaluronan (HA) from tissue matrix and in facilitating transit of leukocytes and tumor cells through lymphatic vessels based largely on in vitro studies with recombinant receptor in transfected fibroblasts. Curiously, however, LYVE-1 in lymphatic endothelium displays little if any binding to HA in vitro, and this has led to the conclusion that the native receptor is functionally silenced, a feature that is difficult to reconcile with its proposed in vivo functions. - Glycobiology and Extracellular MatricesOpen Access
Metal Ion-dependent Heavy Chain Transfer Activity of TSG-6 Mediates Assembly of the Cumulus-Oocyte Matrix
Journal of Biological ChemistryVol. 290Issue 48p28708–28723Published online: October 14, 2015- David C. Briggs
- Holly L. Birchenough
- Tariq Ali
- Marilyn S. Rugg
- Jon P. Waltho
- Elena Ievoli
- and others
Cited in Scopus: 38Background: TSG-6 (TNF-stimulated gene-6)-dependent transfer of heavy chains from inter-α-inhibitor onto hyaluronan is critical for ovulation.Results: A calcium ion and chelating glutamate within TSG-6 mediate formation of the covalent heavy chain-TSG-6 intermediate.Conclusion: TSG-6 transferase activity rather than hyaluronan binding drives cumulus expansion.Significance: The role of metal ions in hyaluronan-heavy chain formation has been determined.