Pathogenic PF4/Polyvinylsulfonate ELISA-negative Antibodies in HIT

  1. Adam J. Kanack
  2. Noah P. Splinter
  3. Emily E. Mauch
  4. Leben Tefera
  5. Morayma Reyes Gil
  6. Sakshi Jasra
  7. Andrew Goodwin
  8. Kristi J Smock
  9. Hadiyah Ahmad
  10. Aneel Ashrani
  11. Nathaniel L. Robinson
  12. Ana I. Casanegra
  13. Curtis G. Jones
  14. Shannon M. Pechauer
  15. Erin Yttre
  16. Richard H. Aster
  17. Mindy C. Kohlhagen
  18. Rachel R. Leger
  19. David L. Murray
  20. Lu Zhou
  21. Demin Wang
  22. Renren Wen
  23. Dong Chen
  24. Rajiv K. Pruthi
  25. Anand Padmanabhan
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Abstract

BACKGROUND

Platelet factor 4-polyanion enzyme-linked immunosorbent assays (ELISAs) are considered highly sensitive for diagnosing heparin-induced thrombocytopenia (HIT), such that current practice guidelines recommend use of ELISA-negative results to exclude HIT. Once HIT is ruled out, alternative, non-heparin-based anticoagulant treatments are ceased, and heparin reintroduction frequently occurs.

METHODS

Antigen-based and PF4-dependent functional testing were used to study PF4/polyvinyl sulfonate ELISA-negative platelet-activating antibodies in HIT-suspected patients and mice immunized with PF4/heparin.

RESULTS

Three patients with clinical presentations consistent with HIT tested negative in an ELISA using PF4-polyvinylsulfonate (PF4/PVS), an antigenic target very commonly used for HIT antibody detection. All three patients demonstrated PF4-dependent platelet activation in functional testing that was sensitive to blockade of platelet FcγRIIa receptors and inhibited by high concentrations of heparin, consistent with pathogenic HIT antibodies. Functional testing-based screening of 500 ELISA-negative patients identified three patients whose sera activated platelets in a PF4- and FcγRIIa-dependent manner, and had clinical histories consistent with HIT. Five of the six ELISA-negative HIT patients were re-exposed to heparin, which precipitated a decrease in platelet counts in all re-exposed patients, and one patient developed a new thrombus. To advance the study of ELISA-negative HIT antibodies, mice were immunized with PF4/heparin, and functional and antigenic assays were simultaneously used to successfully identify an ELISA-negative, PF4-dependent platelet-activating murine monoclonal antibody that recapitulated the serological characteristics of ELISA-negative HIT patients.

CONCLUSIONS

Recognition of ELISA-negative HIT is critical to avoid harm due to the cessation of alternative anticoagulation therapy and re-exposure of these patients to heparin.

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  1. Version published to 10.1101/2025.10.29.25338884 on medRxiv