Clinical Trial Details
— Status: Completed
Administrative data
NCT number |
NCT04334850 |
Other study ID # |
APHP200392 |
Secondary ID |
2020-001324-33 |
Status |
Completed |
Phase |
N/A
|
First received |
|
Last updated |
|
Start date |
April 20, 2020 |
Est. completion date |
June 23, 2021 |
Study information
Verified date |
July 2021 |
Source |
Assistance Publique - Hôpitaux de Paris |
Contact |
n/a |
Is FDA regulated |
No |
Health authority |
|
Study type |
Interventional
|
Clinical Trial Summary
The novel coronavirus SARS-CoV-2 (COVID-19) is an emerging respiratory virus that causes
pneumonia. WHO data reported admission to the intensive care unit (ICU) for 6% of patients,
with a mortality rate reaching 45%. To date, apart from therapeutic trials, ICU management is
symptomatic, based on organ failure support therapies. In the initial phase, the therapeutic
management also includes empiric antimicrobial therapy (90% of patients, in accordance with
LRTI guidelines (ATS 2019) and SRLF Guidelines (2020). One challenge for the ICU physicians
is the timing for discontinuation of antimicrobial treatment, especially in case of shock or
ARDS, considering that a substantial proportion of COVID-19 pneumonia patients may have
pulmonary bacterial coinfection/superinfection. In order to avoid unnecessary prolonged
antimicrobial therapy, and subsequent selective pressure, two tests could be combined in a
personalized antibiotic strategy:
- Procalcitonin (PCT): PCT is a useful tool to guide antibiotics discontinuation in
community-acquired pneumonia) and viral pneumonia (PMID24612487).
- Respiratory multiplex PCR FA-PPP (Biomérieux®): panel has been enlarged, including 8
viruses and 18 bacteria (quantitative analysis). The turnaround time is short.
Sensitivity is high (99%, PMID32179139). It may contribute, in combination with
conventional tests, to accelerate and improve the microbiological diagnosis during
severe COVID-19 pneumonia.
The hypothesize of the study is that the combination of the mPCR FA-PPP and PCT could be used
to reduce antibiotics exposure in patients with severe confirmed COVID-19 pneumonia, with a
higher clinical efficacy and safety as compared with a conventional strategy.
Description:
Inclusion (D0_H0) is performed in ICU as soon as possible, once the diagnosis of COVID-19
pneumonia is confirmed. Therefore, inclusion might be performed either on ICU admission (if
the COVID-19 pneumonia has been confirmed in the pre-ICU wards) or during the ICU stay (if
the COVID-19 pneumonia was confirmed after ICU admission). Conventional microbiological
investigations are left at the discretion of the physicians, and may include blood cultures,
Streptococcus pneumoniae and Legionella pneumophila urinary antigen assays, and a respiratory
tract sample for Gram stain examination and 2 days-long culture (if not already done in the
past 24 hours). Usual biology includes procalcitonin measurement. Empirical antimicrobial
therapy combines a third-generation cephalosporin and a macrolide, or broader-spectrum
antibiotics if risk factors for resistant bacteria are identified.
Randomization is performed immediately after the inclusion.
- In the intervention arm, a broad panel respiratory Mpcr FA-PPP is performed on
respiratory tract sample (tracheal aspirate, BAL or sputum), collected 12 hours after
inclusion. An algorithm of early antibiotic adaptation and discontinuation, based on the
microbiological results, including the mPCR FA-PPP results, and the procalcitonin values
and kinetics will be used. This algorithm will be applied as soon as possible after
inclusion, and repeated day after day until D7.
- In the control arm, the antimicrobial therapy is left at the discretion of the
physicians, as in usual practice.
Evaluation criteria are collected at hospital discharge or at D28, and D90. The vital status
may be obtained by phone call at D28 (if the patient has been discharged before D28) and at
D90.