Impact of the Presence of Anti-interferon Autoantibodies on the Viral Load in Severe Respiratory Infections

Last updated: September 24, 2025
Sponsor: Hospices Civils de Lyon
Overall Status: Active - Recruiting

Phase

N/A

Condition

Respiratory Syncytial Virus (Rsv) Infection

Treatment

Serum anti-IFN-I antibodies

Clinical Study ID

NCT05536219
69HCL22_0674
  • All Genders

Study Summary

Type I interferons (IFN-I) production is induced by the detection of viral molecules, such as RNA or DNA viral strands, through pattern recognition receptors (PRR) present on many immune cell types. Despite a minimal concentration, IFN-I secretion activate the secretion, by neighbouring cells, of more than 700 proteins with antiviral properties (inhibition of viral replication, destabilization of virus membranes, etc.). IFN-I constitute therefore one of the major first line of defence established by the immune system in response to viral infection. Briefly, during the Coronavirus disease (COVID-19) pandemic, several teams including ours, highlighted a lack of IFN-I response in approximately one in five individuals presenting a severe form of COVID-19.

Interestingly, within a large part of them, in vitro investigations revealed the presence of autoantibodies presenting neutralizing capacities against alpha and/or omega interferons This finding confirms the deleterious role of anti-IFN-I autoantibodies on the antiviral immune response and the key role of IFN-I pathway regarding defences against COVID-19 infection. Furthermore, those observations pave the way to interesting research that would allow understanding the underlying pathophysiological mechanisms of severe viral respiratory infection.

The research hypothesis are:

i) IFN-I deficiency could induce severe forms of viral infections which could lead to intensive care admission ii) IFN-I deficiency could increase viral loads in nasopharyngeal samples, and be associated with protracted viral clearance iii) The frequency of viral co-infections may be higher in case of IFN-I antiviral pathway blockade, iv) severe forms of respiratory viruses' infections could be induced by other anti-cytokine autoantibodies.

In addition to confirming research hypotheses recently mentioned, the aim of this clinical protocol will be to assess the impact of antiviral innate immune response alterations in severe respiratory infections.

Eligibility Criteria

Inclusion

Inclusion Criteria:

For adult patients :

  • Patients with acute respiratory failure requiring the administration of oxygen* tomaintain peripheral oxygen saturation at at least 90%
  • in patients with chronic respiratory failure, an oxygen flow higher than the usualflow or a duration of non-invasive ventilation longer than the usual duration willbe required.
  • Patients with influenza, RSV or SARS-CoV-2 infection diagnosed by ReverseTranscription Polymerase Chain Reaction (RT-PCR) or antigen test in the last 7 days

  • Patients hospitalized in participating intensive care units

For pediatric patient :

  • In respiratory distress placed on oxygen with signs suggestive of viral infection:
  1. moderate or absent fever or nasopharyngeal congestion or cough

  2. signs of acute respiratory distress (polypnea > 2DS of the normal value,intercostal drawing, thoraco-abdominal sway) with more or less marked hypoxia (SpO2 < 92% under ambient air),

  3. and/or significant apnea (associated with bradycardia or desaturation),

  4. and/or dietary difficulties (reduction of rations to less than 50% of the usualration).

  • Hospitalized in the pediatric emergency and intensive care unit of Hôpital FemmeMère Enfant (HFME)

Exclusion

Exclusion Criteria:

  • Opposition of the patient or his close family/friend to inclusion in the study

  • Patient under legal protection measure

  • Patient who was included in this study during a previous stay

  • Immunodepression defined by: bone marrow allograft less than 24 months old,chemotherapy for less than 6 months, HIV infection with CD4<200/mm3 or <15%,corticosteroid therapy for more than 2 weeks with a daily dose greater than 10mg of prednisolone equivalent, immunosuppressive treatment administered in theprevious 3 months (6 months for rituximab), aplasia, asplenia or splenectomy.

  • Patient under 30 kg (for adults) and less than 3 kg (for children)

Study Design

Total Participants: 360
Treatment Group(s): 1
Primary Treatment: Serum anti-IFN-I antibodies
Phase:
Study Start date:
November 08, 2022
Estimated Completion Date:
August 08, 2027

Connect with a study center

  • Hôpital Femme Mère et enfant

    Bron, Rhone 69500
    France

    Site Not Available

  • Hôpital Femme Mère et enfant

    Bron 3029931, Rhone 69500
    France

    Active - Recruiting

  • Hopital Lyon Sud

    Pierre-Bénite, Rhone 69110
    France

    Site Not Available

  • Hopital Lyon Sud

    Pierre-Bénite 2987314, Rhone 69110
    France

    Active - Recruiting

  • Hôpital Croix Rousse

    Lyon, Rhône 69004
    France

    Site Not Available

  • Hôpital Croix Rousse

    Lyon 2996944, Rhône 69004
    France

    Active - Recruiting

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