Immunosuppression Clinical Trial
Official title:
New Strategies to Improve Immunosuppressive Therapy Management in Heart Transplantation: a Pilot Study
Cardiac allograft rejection (CAR) occurs in 30% to 40% of transplant recipients within the
first year post-transplant, and carries an increased risk of both acute graft failure and
reduced graft longevity. Because of the high morbidity of CAR when diagnosed after symptoms
develop, surveillance endomyocardial biopsy (EMB) has been included in heart transplantation
guidelines since 1990. Although EMB is the established gold standard for the diagnosis of
CAR, the clinical utility of EMB using standard hematoxylin and eosin (H&E) histologic
analysis is limited by marked inter-observer variability and significant discordance between
the histologic grade and clinical impression of CAR severity.
On the other hand, Tacrolimus (TAC), one of the most important immunosuppressant drug and
widely used for the prevention of rejection after solid organ transplantation (SOT), is
considered a critical dose drug: too low exposure to TAC may result in
under-immunosuppression and acute rejection, whereas overexposure puts patients at risk for
toxicity. Tac concentrations, in whole-blood, are considered therapeutic when maintained in
the range 5 and 20 ng/mL. In addition to being highly variable inter-individually, TAC
pharmacokinetics can also be variable within individual patients.
Although in recent years significant decrease of rejection post SOT has been observed, there
is space for further modulation of immunosuppressive therapy, in order to reduce the most
common adverse side effects (nephrotoxicity, diabetes, osteoporosis, cardiovascular disease,
infections and malignancies), to improve the patients quality of life and to better
individualize their therapies. Tac. Unfortunately, a clear correlation between TAC whole
blood concentration and acute rejection risk has not yet been defined.
Monocentric and Observational Study
- Longitudinal Prospective
The study considers the collection of the following samples:
- a single whole blood sample, 3-5 mL in EDTA for Pharmacogenetics,
- 10 mL whole blood sample in lithium-heparin for Tac quantification in PBMC collected at
each time-point scheduled for routine follow-up visits: day +15 and month 1, 3, 6, 12
post transplant
- About 1 mg cardiac tissue samples (from cardiac biopsies), collected by standard
procedure adopted at the Transplant Center of CardiacSurgery at each time-point
scheduled for routine follow-up visits: day +15 and month 1, 3, 6, 12 post transplant
Each blood sample and biopsy specimen will be identified and labeled with an alphanumeric
code, whose decoding matrix will be kept by dedicated personnel at the U.O.C. Cardiac
Surgery, Department of Intensive Medicine.
In general, each patient will be defined as "TAC + progressive enrollment number" (example:
TAC1, TAC2, TAC3 ...).
Each sample sent to the laboratories for the analyzes in the different matrices and for the
different activities foreseen by the protocol (measurements of tacrolimus and pharmacogenetic
concentrations) must always contain the identification code assigned to the patient followed
by the type of analysis + sampling time. For example, patient collection # 2 for tacrolimus
assay to be performed in PBMC, whole blood and EMB at month 3, will be identified as:
TAC2-PBMC-M3 TAC2-WB-M3 TAC2-BEM-M3
The storage of the codes that will allow the patients' identification will be kept by dr.
Carlo Pellegrini and dr. Barbara Cattadori (U.O.C. Cardiosurgery).
All samples will be investigated within the Foundation: blood samples for the quantification
of Tacrolimus in blood mononuclear cells (PBMC) and in whole blood will be transferred to the
Clinical and Experimental Pharmacokinetic Laboratory. Blood samples for pharmacogenetic
investigations will be transferred to the Biochemical and Genetic Laboratory of Respiratory
Diseases.
The proponents of the study will keep any residual samples at the investigations planned by
the study in a safe place with limited access, ie in a freezer -80 °C located in a locked
room (room n.11a, Lab Clinical and Experimental Pharmacokinetics, Pavilion 13). These samples
can be used for scientific purposes directly related to those of the main study
;
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