Cystic Fibrosis Clinical Trial
Official title:
Epidemiology and Clinical Characteristics of Non-Tuberculous Mycobacteria Infections in Cystic Fibrosis Patients.
An increase in the prevalence of infections due to non-tuberculous mycobacteria (NTM) is
observed in many countries and recent data suggest the circulation of dominant clones with a
possibility of human-to-human contamination. The hypothesis is made that these infections are
also increasing in France and that dominant NTM clones are circulating. The last French study
carried out in 2004 already showed prevalences of up to 10% in certain French regions. It is
essential to know the prevalence 8 years later, taking advantage of the new recommendations
for the management of patients and samples, which will homogenize practices on French
territory.
No data are currently available in France on the prevalence of positive serological responses
in cystic fibrosis patients. Serological analyzes of the sera collected during this study
will enable us to evaluate the performance of serology in mycobacterial culture and to
identify patients with no positive respiratory specimen in culture but with positive serology
indicating potential contact with a mycobacterium. The establishment of a serological
follow-up of these patients will allow to correlate this result with a clinical evolution and
/ or the detection of NTM in subsequent samples. Serology is an innovative aspect of the
CIMENT study.
Non-tuberculous mycobacteria (NTM) are important new pathogens in cystic fibrosis, with
prevalence estimates ranging from 6% to 13%. The diagnosis of the disease in cystic fibrosis
patients is difficult because the infection may remain indolent in some cases without
evidence of clinical consequence, while in other patients NTM are associated with significant
morbidity and mortality. Treatment requires antibiotic therapy over a prolonged period (at
least 12 to 18 months) with several drugs and varies according to NTM and their antibiotic
resistance profile. The development of a specialized approach (clinicians / biologists) in
the management of this infection, combined with the diagnosis and treatment of NTM
infections, in cystic fibrosis patients is a research priority. It is an indispensable
long-term strategy for this high-risk population.
Two main elements confirm the interest of a prevalence survey of NTM infections in cystic
fibrosis (CF) patients: the diagnostic difficulty of "true" infections (as opposed to simple
colonizations) to NTM, and the clinical impact on respiratory functions of NTM present in
these patients. Two recent contradictory studies on the impact of NTM infections in CF
patients have recently been published. The German monocentric study suggests a greater
deterioration of respiratory function in CF patients not infected with NTM compared to CF
patients infected with NTM. 26 patients were infected with NTM: 14/26 with M. avium complex
(MAC), 10/26 with M. abscessus complex and 2/26 with M. gordonae. Only 5 patients out of a
dozen positive to M. abscessus and 1 in 14 positive to MAC were treated. Comparatively, the
other study found a significant deterioration in respiratory function (maximum expired volume
in 1 seconde) of CF patients infected with M. abscessus. This Scandinavian national study
reinforced its argument by the fact that an effective treatment made it possible to find
changes in maximum expired volume in 1 seconde close to that observed before the infection.
Some differences are observed in these two studies; including the age of the subjects
included, older in the German study, and the number of positive lung samples per patient. The
German study retained the criteria of the American Thoracic Society (ATS) / Infectious
Disease Society of America (IDSA) for interpreting respiratory specimens positive for MNT.
However, these criteria remain very difficult to apply for CF patients because the clinical
and radiological manifestations of cystic fibrosis and mycobacterial infection are confounded
and other criteria are necessary, such as the number of positive pulmonary samples: 5 vs. 2
to 4 or the decline in maximum expired volume in 1 seconde in the year prior to colonization
/ MNT infection (-5.8% per year vs. 0.7% per year). We see here the necessity of
complementary studies, in order to be able to identify the diagnostic difficulties and the
impacts of the therapeutics administered in these patients. Indeed, on the one hand the
therapeutic impact is very difficult to evaluate in the face of the very weak correlation
between the results of the "antibiograms" and therefore in vitro and the therapeutic effect
in vivo. On the other hand, precise diagnostic interpretation remains essential, as published
observational studies show real discrepancies, largely due to diagnostic biases. Recently,
under the auspices of the American Foundation and the European Cystic Fibrosis Society,
guidelines for the management of NTM infections in CF patients have been published. To this
is added the references of Microbiology.
Several authors have shown that this diagnosis is an alternative in the context of NTM
infections in cystic fibrosis patients. Indeed, as mentioned above, the microbiological
diagnosis is often faulted, due to the difficulty of culturing the samples and their low
yield in the context of NTM infections. An indirect diagnostic approach can only reinforce
the screening of cystic fibrosis patients who have had contact with a NTM. Any serological
response, although unable to date an infection, is the result of a potentially protective
response of the host undergoing infection, and evidence of antibodies directed against the
agent's bacterial products pathogen in circulating blood. A simple colonization does not
allow the appearance of antibodies. An infectious process, even inapparent, must have taken
place.
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