BaseSpace
Correlation Engine 2.0
Import Your Data
Literature

FAQ

More FAQs

Back to top
Clear Search sequence regions
(e.g. Holistic medicine, Doxycycline, rs2230926, KLK3, Metabolism of xenobiotics, Retina)
Bookmark Forward

Kinetic regulation of the binding of prothrombin to phospholipid membranes.

Emma Smith, Rina Vekaria, Katherine A Brown, Colin Longstaff

Molecular and cellular biochemistry 2013 Oct


filter terms:
  • elisa (3)
  • factors (1)
  • humans (1)
  • lipid bilayers (2)
  • phospholipid (7)
  • prothrombin (9)
  • spr (4)
    • Sizes of these terms reflect their relevance to your search.

    A wide range of equilibrium and kinetic constants exist for the interaction of prothrombin and other coagulation factors with various model membranes from a variety of techniques. We have investigated the interaction of prothrombin with pure dioleoylphosphatidylcholine (DOPC) membranes and dioleoylphosphatidlyserine (DOPS)-containing membranes (DOPC:DOPS, 3:1) using surface plasmon resonance (SPR, with four different model membrane presentations) in addition to isotheral titration calorimetry (ITC, with suspensions of phospholipid vesicles) and ELISA methods. Using ITC, we found a simple low-affinity interaction with DOPC:DOPS membranes with a K(D) = 5.1 μM. However, ELISA methods using phospholipid bound to microtitre plates indicated a complex interaction with both DOPC:DOPS and DOPC membranes with K(D) values of 20 and 58 nM, respectively. An explanation for these discrepant results was developed from SPR studies. Using SPR with low levels of immobilised DOPC:DOPS, a high-affinity interaction with a K(D) of 18 nM was obtained. However, as phospholipid and prothrombin concentrations were increased, two distinct interactions could be discerned: (i) a kinetically slow, high-affinity interaction with K(D) in the 10(-8) M range and (ii) a kinetically rapid, low-affinity interaction with K(D) in the 10(-6 )M range. This low affinity, rapidly equilibrating, interaction dominated in the presence of DOPS. Detailed SPR studies supported a heterogeneous binding model in agreement with ELISA data. The binding of prothrombin with phospholipid membranes is complex and the techniques used to measure binding will report K D values reflecting the mixture of complexes detected. Existing data suggest that the weaker rapid interaction between prothrombin and membranes is the most important in vivo when considering the activation of prothrombin at the cell surface.

    Citation

    Emma Smith, Rina Vekaria, Katherine A Brown, Colin Longstaff. Kinetic regulation of the binding of prothrombin to phospholipid membranes. Molecular and cellular biochemistry. 2013 Oct;382(1-2):193-201

    Expand section icon Mesh Tags

    Expand section icon Substances


    PMID: 23812842

    View Full Text
    • Copyright © 2024 Illumina Inc. All rights reserved.