Incidence and Risks Factors of CMV Reactivation in Patients Receiving of CAR-T Cells for Acute Leukemia and Lymphoma Relapse, a Cohort Study Analysis

Assistance Publique - Hôpitaux de Paris250 enrolled

Overview

Letermovir is approved for the primary prevention of Cytomegalovirus (CMV) reactivation and infection in hematopoietic stem cell transplant recipients. Letermovir may be beneficial in other clinical presentation where CMV reactivates and may alter clinical outcomes. Recently Chimeric Antigen Receptor (CAR) T cells have been used for the treatment of refractory acute leukemia and B cell lymphoma. Reactivation of chronic viral infections, in particular those belonging to the Herpesviridae family can therefore be observed following CAR-T cells treatment.According to first reports, Cytomegalovirus seems to be the main virus detected. Uncontrolled CMV reactivation leads to CMV disease requiring the use of antiviral drugs associated with either hematological toxicity (ganciclovir) or renal toxicity (foscarnet) and is usually associated with poor outcomes. In addition, CMV interplays with the immune system and decreases the immunosurveillance of tumor cells and facilitates the growth or reactivation of other opportunistic infections. Therefore, CMV reactivation could also impact the outcome of CART cells treatment by increasing the existing risk of opportunistic infections in CART cells recipients and thus by increasing morbidity, length stay or require intensive care. Imbalance of the immune system usually correlates with reactivation of persistent virus like Torquetenovirus (TTV), redondovirus or pegivirus found more frequently in Hematopoietic stem-cell transplantation (HSCT) patients or patients requiring intensive care. Whether reactivations of those persistent viruses are associated or precede CMV reactivation deserve careful investigation to identify as early as possible patients at high risk and who could benefit from antiviral preventive treatment. The objective of this trial is to determine the incidence of CMV reactivation within 3 months after infusion of CAR-T cells in CMV seropositive patients with refractory acute leukemia or B-cell lymphoma.

Study Type

OBSERVATIONAL

Enrollment

250

Conditions

Cytomegalovirus Infections

Eligibility

Sex: ALLMin age: 1 YearMax age: 100 Years

Medical Language ↔ Plain English

Common inclusion criteria : * Paediatric (1 to 18 years old) receiving CART-T cells treatment for refractory acute leukemia or B-cell lymphoma * Adult receiving CART-T cells treatment for refractory acute leukemia or B-cell lymphoma * CMV seropositive patients Inclusion criteria : retrospective part * Provide written non-opposition from the patient signed by investigator * If the patient is a minor, provide written non-opposition from both parents and child (if age appropriate to collect their non-objection) or child and the legal representative in case only one parent is alive, signed by investigator Inclusion criteria : prospective part * Provide written consent form signed by patient and investigator * If the patient is a minor, provide written consent form signed by investigator and both parents or signed by investigator and the legal representative in case only one parent is alive Exclusion Criteria: * CMV seronegative patients * Lack of affiliation to a social security scheme (as a beneficiary or assignee) * Patients under guardianship / curatorship * Patient under AME (state medical aid)

Outcomes

Primary Outcomes

Rate of CMV reactivation

Rate of CMV reactivation occurring within the first 3 months after CAR-T-cell infusion in paediatric and adult patients treated for refractory B cell acute lymphoblastic leukemia (B-ALL) and diffuse large B-cell lymphoma (DLBCL).

Time frame: Up to 3 months after inclusion

Secondary Outcomes

Rate of CMV disease

Time frame: Up to 3 months

Rate of anellovirus infection

Time frame: Up to 3 months

Rate of pegivirus infection

Time frame: Up to 3 months

Rate of redondovirus infection

Time frame: Up to 3 months

Correlation between CMV reactivation and the occurrence of other bacterial or fungal infections

Time frame: Up to 3 months

Correlation between CMV reactivation and the expansion of CAR-T cells

Time frame: Up to 3 months

Correlation between CMV reactivation and other early viral persistent reactivations (anellovirus, pegivirus, redondovirus)

Time frame: Up to 3 months

Rate of CMV reactivation in patients with acute leukemia

Time frame: Up to 3 months

Rate of CMV reactivation in patients with lymphoma

Time frame: Up to 3 months

Detection of mutations in the CMV DNA polymerase gene in patients under acyclovir or valacyclovir prophylaxis

Time frame: Up to 3 months

Health related quality of life (HRQL)) of the study population with or without CMV activation

EQ-5D-5L scale (adult) EQ-5D-Y scale (child) First part describes 5 dimensions (mobility, self-care, usual activities, pain/discomfort, anxiety/depression) Second part is a visual analogue scale with a score varying from 0 to 100; the higher the score the better the state of health.

Time frame: Up to 3 months

Cost of illness of CMV disease

Illness of CMV disease is defined by prolonged initial hospitalization, additional hospitalizations, increased surveillance in case of reactivation (consults and biological sampling), treatments)

Time frame: Up to 3 months

Incidence and Risks Factors of CMV Reactivation in Patients Receiving of CAR-T Cells for Acute Leukemia and Lymphoma Relapse, a Cohort Study Analysis

Overview

Conditions

Eligibility

Locations (3)

Outcomes

Primary Outcomes

Secondary Outcomes

Central Contacts