Official Title
Real-life Observatory of Efficacy and Resistance to Anti CMV Molecules in Stem Cell Recipients
Brief Title
AntiCMV molécules Monitoring in Real-life in Stem Cell Recipients
Protocol ID
NCT04690933
Lead Sponsor
University Hospital, Limoges
Brief Summary
Cytomegalovirus (CMV) is a ubiquitous herpesvirus that represent a major cause of
morbidity in haematopoietic stem cell transplants (HSCT) recipients, mostly through
reactivation of the recipient's virus.
If left untreated, 40 to 80% of patients will develop CMV infection, leading to CMV
disease in 30 to 35 % patients, and associated with considerable morbi-mortality.
Interstitial pneumonia is the most severe and specific manifestation, although CMV
replication by itself has also indirect effects such as triggering graft versus host
disease and increasing immunosuppression. The current burden of CMV infection increases
by 25 to 30% the cost of the graft in France. This also includes the burden for
refractory - infections, that represent up to 13% of recipients with CMV infection,
including 3% of cases with virological resistance in France (data from the Reference
Center cohorts).
Ganciclovir, or valganciclovir preemptive treatment, guided by CMV viral load follow-up
allowed significant reduction of CMV disease to 2-6% but did not prevent CMV indirect
effects. In addition, hematotoxicity can compromise post-transplant haematological
reconstitution, thus preventing its use as prophylaxis in France. Foscarnet,
iv-administered and nephrotoxic, remains less used. There is thus a high expectation from
less toxic molecules for prophylaxis The development letermovir recently available for
prophylaxis of CMV infection in high risk patients will modify the patients care and
follow-up. This new molecule targeting CMV terminases (developed by Merck) was recently
marketed in France (Jan 2020). However, the analysis of the letermovir phase III study
and further publications show that the risk of emergence of resistance is low, but may
occur in case of breakthrough and thus post AMM monitoring is required.
A "real-life" evaluation of these new molecules in terms of efficacy, emergence of
resistance, tolerance and morbimortality related to CMV infection, is useful, to propose
recommendations on management strategies, in particular for the most at-risk patients
i.e. CMV-seropositive recipients. To this purpose, the National Reference Center in
collaboration with the French Society for marrow graft and cell therapy (SFGMTC) set up a
cohort of surveillance of allografted patients, receiving, in prevention or treatment,
old and new molecules.
Detailed Description
Cytomegalovirus (CMV) is a ubiquitous herpesvirus that represent a major cause of
morbidity in haematopoietic stem cell transplants (HSCT) recipients, mostly through
reactivation of the recipient's virus.
If left untreated, 40 to 80% of patients will develop CMV infection, leading to CMV
disease in 30 to 35 % patients, and associated with considerable morbi-mortality.
Interstitial pneumonia is the most severe and specific manifestation, although CMV
replication by itself has also indirect effects such as triggering graft versus host
disease and increasing immunosuppression. The current burden of CMV infection increases
by 25 to 30% the cost of the graft in France. This also includes the burden for
refractory - infections, that represent up to 13% of recipients with CMV infection,
including 3% of cases with virological resistance in France (data from the Reference
Center cohorts).
Ganciclovir, or valganciclovir preemptive treatment, guided by CMV viral load follow-up
allowed significant reduction of CMV disease to 2-6% but did not prevent CMV indirect
effects. In addition, hematotoxicity can compromise post-transplant haematological
reconstitution, thus preventing its use as prophylaxis in France. Foscarnet,
iv-administered and nephrotoxic, remains less used. There is thus a high expectation from
less toxic molecules for prophylaxis The development letermovir recently available for
prophylaxis of CMV infection in high risk patients will modify the patients care and
follow-up. This new molecule targeting CMV terminases (developed by Merck) was recently
marketed in France (Jan 2020). However, the analysis of the letermovir phase III study
and further publications show that the risk of emergence of resistance is low, but may
occur in case of breakthrough and thus post AMM monitoring is required.
A "real-life" evaluation of these new molecules in terms of efficacy, emergence of
resistance, tolerance and morbimortality related to CMV infection, is useful, to propose
recommendations on management strategies, in particular for the most at-risk patients
i.e. CMV-seropositive recipients. To this purpose, the National Reference Center in
collaboration with the French Society for marrow graft and cell therapy (SFGMTC) set up a
cohort of surveillance of allografted patients, receiving, in prevention or treatment,
old and new molecules.
Study Period
-
Enrollment Count
400 participants
Eligibility Criteria
Inclusion Criteria :
• Candidate (adult) for an allograft of hematopoietic stem cells for which a decision of
transplant is made and willing to participate in the cohort.
Exclusion Criteria :
- CMV-seronegative patient receiving a negative CMV donor graft ;
- Patient having signed the consent but not grafted ;
- Patient included in a clinical study on an anti-CMV molecule ;
- Non-insured social patient ;
Filters
Hematopoietic Stem Cell Transplantation
Cytomegalovirus Infections
Antivirals
Antiviral Drug Resistance
COMPLETED
ADULT
OLDER_ADULT