Treatment with soluble CD24 attenuates COVID-19-associated systemic immunopathology

  1. No-Joon Song
  2. Carter Allen
  3. Anna E. Vilgelm
  4. Brian P. Riesenberg
  5. Kevin P. Weller
  6. Kelsi Reynolds
  7. Karthik B. Chakravarthy
  8. Amrendra Kumar
  9. Aastha Khatiwada
  10. Zequn Sun
  11. Anjun Ma
  12. Yuzhou Chang
  13. Mohamed Yusuf
  14. Anqi Li
  15. Cong Zeng
  16. John P. Evans
  17. Donna Bucci
  18. Manuja Gunasena
  19. Menglin Xu
  20. Namal P. M. Liyanage
  21. Chelsea Bolyard
  22. Maria Velegraki
  23. Shan-Lu Liu
  24. Qin Ma
  25. Martin Devenport
  26. Yang Liu
  27. Pan Zheng
  28. Carlos D. Malvestutto
  29. Dongjun Chung
  30. Zihai Li

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Abstract

Background

Severe Acute Respiratory Syndrome Coronavirus 2 (SARS-CoV-2) causes coronavirus disease 2019 (COVID-19) through direct lysis of infected lung epithelial cells, which releases damage-associated molecular patterns and induces a pro-inflammatory cytokine milieu causing systemic inflammation. Anti-viral and anti-inflammatory agents have shown limited therapeutic efficacy. Soluble CD24 (CD24Fc) blunts the broad inflammatory response induced by damage-associated molecular patterns via binding to extracellular high mobility group box 1 and heat shock proteins, as well as regulating the downstream Siglec10-Src homology 2 domain–containing phosphatase 1 pathway. A recent randomized phase III trial evaluating CD24Fc for patients with severe COVID-19 (SAC-COVID; NCT04317040) demonstrated encouraging clinical efficacy.

Methods

Using a systems analytical approach, we studied peripheral blood samples obtained from patients enrolled at a single institution in the SAC-COVID trial to discern the impact of CD24Fc treatment on immune homeostasis. We performed high dimensional spectral flow cytometry and measured the levels of a broad array of cytokines and chemokines to discern the impact of CD24Fc treatment on immune homeostasis in patients with COVID-19.

Results

Twenty-two patients were enrolled, and the clinical characteristics from the CD24Fc vs. placebo groups were matched. Using high-content spectral flow cytometry and network-level analysis, we found that patients with severe COVID-19 had systemic hyper-activation of multiple cellular compartments, including CD8 + T cells, CD4 + T cells, and CD56 + natural killer cells. Treatment with CD24Fc blunted this systemic inflammation, inducing a return to homeostasis in NK and T cells without compromising the anti-Spike protein antibody response. CD24Fc significantly attenuated the systemic cytokine response and diminished the cytokine coexpression and network connectivity linked with COVID-19 severity and pathogenesis.

Conclusions

Our data demonstrate that CD24Fc rapidly down-modulates systemic inflammation and restores immune homeostasis in SARS-CoV-2-infected individuals, supporting further development of CD24Fc as a novel therapeutic against severe COVID-19.

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  1. Version published to 10.1186/s13045-021-01222-y
  2. ScreenIT

    SciScore for 10.1101/2021.08.18.21262258: (What is this?)

    Please note, not all rigor criteria are appropriate for all manuscripts.

    Table 1: Rigor

    EthicsIRB: The Western Institutional Review Board approved trial and protocol.
    Sex as a biological variablenot detected.
    RandomizationConsented and enrolled patients were randomized in a double-blinded fashion to receive either CD24Fc antibody (480 mg IV infusion) or placebo control (IV saline)
    Blindingnot detected.
    Power Analysisnot detected.

    Table 2: Resources

    No key resources detected.

    Results from OddPub: We did not detect open data. We also did not detect open code. Researchers are encouraged to share open data when possible (see Nature blog).

    Results from LimitationRecognizer: An explicit section about the limitations of the techniques employed in this study was not found. We encourage authors to address study limitations.

    Results from TrialIdentifier: We found the following clinical trial numbers in your paper:

    IdentifierStatusTitle
    NCT04317040CompletedCD24Fc as a Non-antiviral Immunomodulator in COVID-19 Treatm…
    NCT04315948Active, not recruitingTrial of Treatments for COVID-19 in Hospitalized Adults

    Results from Barzooka: We did not find any issues relating to the usage of bar graphs.

    Results from JetFighter: We did not find any issues relating to colormaps.

    Results from rtransparent:
    • Thank you for including a conflict of interest statement. Authors are encouraged to include this statement when submitting to a journal.
    • Thank you for including a funding statement. Authors are encouraged to include this statement when submitting to a journal.
    • No protocol registration statement was detected.

    Results from scite Reference Check: We found no unreliable references.

    About SciScore

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  3. Version published to 10.1101/2021.08.18.21262258 on medRxiv