Patients treated for DLBCL are at high risk of developing AICD. This adverse event is
characterized by irreversible damage to the heart muscle with a loss of cardiomyocytes
and subsequent decline in cardiac pumping capacity. Thereby patients treated for this
malignancy are at double the risk of developing symptomatic heart failure /
cardiomyopathy when compared to the general population. This corresponds to a cumulative
incidence of 5-10% within 5-years after receiving R-CHOP. In the elderly, an incidence of
26% has been reported after 8-years of follow-up. Among patients who die in complete
remission, heart failure has been described to be one of the most important causes of
death. ANTICIPATE aims to evaluate if dexrazoxane can prevent AICD in DLBCL patients and
identify those at highest risk of AICD. Of all patients treated with anthracyclines in a
first-line setting, DLBCL patients were chosen for this trial for two primary reasons.
Firstly, these patients have a favourable oncological prognosis with a 5-year relative
survival in the Netherlands of 64-78% in those aged 18-74 years increasing the importance
of preventing long-term toxicity. Secondly, the cumulative anthracycline dose used for
the treatment of DLBCL is higher than the dose used in breast cancer. The cumulative
anthracycline dose is the most important risk factor for AICD known.
Study sponsor and potential other locations can be found on ClinicalTrials.gov for NCT06220032.
HO170 DLBCL-ANTICIPATE: "Prevention of ANThracycline-Induced Cardiac dysfunction by
dexrazoxane In PATients with diffusE large B-cell lymphoma" is a national randomized
controlled trial that will be conducted across 25 Dutch hospitals. This study will
include adult patients with DLBCL in which first-line treatment with 6 cycles of R-CHOP
(rituximab, cyclophosphamide, doxorubicin, vincristine, prednisone) is planned
(cumulative doxorubicin dose 300 mg/m2). In this trial, we have chosen to include
patients with a normal cardiac function before chemotherapy because cardiac dysfunction
is a contra-indication for administration of anthracyclines. A total of 324 DLBCL
patients will prior to treatment be randomized in a 1:1 ratio to either (1) intravenous
dexrazoxane administration in a 10:1 dexrazoxane:doxorubicin ratio prior to each
doxorubicin infusion or (2) no cardioprotective treatment (current standard of care). Due
to the low pH of the dexrazoxane solution that would jeopardize the blinding no placebo
is used. Cardiac function will be screened with echocardiography prior to the initiation
of chemotherapy and followed-up at 4- and 12-months post randomization. The primary end
point of the study will be the incidence of AICD, defined as a left ventricular ejection
fraction (LVEF) decline of ≥10 percentage points from baseline and below 50% (normal
reference value for two-dimensional (2D) echocardiography). The secondary endpoint will
be the percentage of patients with complete metabolic remission (CMR) after R-CHOP
chemotherapy, to reassure that dexrazoxane does not influence the antineoplastic efficacy
of doxorubicin. To declare ANTICIPATE successful, the trial must show both the
superiority of addition of dexrazoxane on the primary endpoint and non-inferiority on the
secondary endpoint. Deep-phenotyping of patient- and treatment-related factors will be
performed to evaluate their prognostic value.
Lead OrganizationStichting Hemato-Oncologie voor Volwassenen Nederland
Principal InvestigatorA. van Rhenen
