Binding of anti-platelet factor 4/heparin antibodies depends on the thermodynamics of conformational changes in platelet factor 4.

[heparin-induced thrombocytopenia]

The chemokine platelet factor 4 (PF 4 ) undergoes conformational changes when complexing with polyanions . This can induce the antibody-mediated adverse drug effect of heparin-induced thrombocytopenia (HIT ). Understanding why the endogenous protein PF 4 becomes immunogenic when complexing with heparin is important for the development of other negatively charged drugs and may also hint toward more general mechanisms underlying the induction of autoantibodies to other proteins . By circular dichroism spectroscopy , atomic force microscopy , and isothermal titration calorimetry we characterized the interaction of PF 4 with unfractionated heparin (UFH ), its 16 -, 8 -, and 6 -mer subfractions , low -molecular-weight heparin (LMWH ), and the pentasaccharide fondaparinux . To bind anti-PF 4 /heparin antibodies , PF 4 /heparin complexes require (1 ) an increase in PF 4 antiparallel β-sheets exceeding ∼30 % (achieved by UFH , LMWH , 16 -, 8 -, 6 -mer ), (2 ) formation of multimolecular complexes (UFH , 16 -, 8 -mer ), and (3 ) energy (needed for a conformational change ), which is released by binding of ≥11 -mer heparins to PF 4 , but not by smaller heparins . These findings may help to synthesize safer heparins . Beyond PF 4 and HIT , the methods applied in the current study may be relevant to unravel mechanisms making other endogenous proteins more vulnerable to undergo conformational changes with little energy requirement (eg , point mutations and post-translational modifications ) and thereby predisposing them to become immunogenic .