Renal Failure Clinical Trial
Official title:
Pilot Study of In Vitro Immunosuppressive Effects of Mycophenolate Mofetil and Valganciclovir in Kidney Transplant Recipients
Valganciclovir (VGCV) has recently been approved by the Food and Drug Administration (FDA)
for the treatment and prevention of cytomegalovirus (CMV) retinitis in HIV patients. It is
under review for the prevention of CMV disease following organ transplantation.
Mycophenolate mofetil (MMF), the morpholinoethyl ester of mycophenolic acid (MPA) is
currently the most widespread used immunosuppressant in kidney transplantation. These drugs
exerts their effects by blocking the production of DNA primarily in lymphocytes.
Recent studies have suggested that combining both MMF and GCV in vitro may have a beneficial
effect on the treatment of CMV infections. However, the effect of these two drugs in
combination on the effects of the immune system both in vitro and in vivo have not been
studied. Preliminary studies in our lab show that a combination of these two drugs have an
additive effect on the level of immunosuppression of both the growth and differentiation of
progenitor bone marrow cells as well as lymphocyte proliferation.
This study is designed to test patients degree of immune reactivity both on and off VGCV
when used in combination with MMF. Patients will have blood drawn as several time points and
an immune assay will be performed to show if VGCV when used in combination with MMF exerts
immunosuppressive effects.
Recruitment and screening of subjects will be performed between 4 and 8 weeks after
transplantation at which time consent will be obtained. Per clinical standard of care at
Indiana University, VGCV is routinely stopped at 12 weeks post transplantation. At week 10
and the day of discontinuation of their prophylaxis the patients will be seen by the study
physician. The subjects will also be seen at 2 and 4 weeks after discontinuing VGCV. At each
study visit, the subject will have a limited history and physical (H&P) performed, one 3ml
light green top (lithium heparin) tube, one 3ml dark green top (sodium heparin) tube, and
one 5ml purple top (EDTA) tube will be obtained by phlebotomy during their regularly
scheduled blood draw times. This blood will then be used for the Cylex® assay, Flow
cytometry and MMF and GCV trough level. The patient’s complete blood count and differential
as well as drug levels, and medication dosages will be recorded. This information will be
used for assure that Cylex® results are not being influenced by changes in immunosuppressive
drug levels. The complete blood count and differential will be used to determine absolute
neutrophil counts. After the week sixteen visit, the subjects will have completed the
protocol. Pregnancy tests will not be performed as patients are not directly receiving any
treatment secondary to this study. Flow cytometry will be performed to measure absolute CD4
counts, CD4/CD8 ratios, and look at several activation markers on lymphocytes.
Signed IRB approved informed consent must be obtained from all subjects prior to screening
assessments. The following evaluations will be performed prior to initiation of phlebotomy
for purposes of this study.
Medical history including age, gender, race, and renal disease, immunosuppressive regimen
including dose, level and use of antibody treatment at time of transplant will be noted.
Physical examination including: vital signs, cardiac, and lung evaluation.
Laboratory testing which will be performed as part of standard of care because of the
transplant are:
Hematology: complete blood count. Drug level: tacrolimus, cyclosporine and/or sirolimus.
Evaluations during treatment and post treatment
Patients will be followed by surgical co-investigators throughout the entire study.
A limited history and physical examination will be performed as indicated in the schedule of
assessments.
Clinical laboratory testing Additional clinical laboratory testing beyond standard of care
that will be done for this protocol includes adding a differential to the complete blood
count. CBC and drug levels will be noted from already scheduled clinic appointments and post
transplant protocols. Research blood levels for GCV and MPA will be run from a 3ml lithium
heparin and a 5ml EDTA tube in the research laboratory or at outside laboratory.
Transplant laboratory testing On the testing days an additional 3ml sodium heparin blood
tube will be drawn in phlebotomy at the same time the scheduled labs are obtained. Flow
cytometric analysis will be performed at times listed above. A 5 tube panel using three
color analysis will be performed using approximately 500_L of whole blood from the sodium
heparinized tube. The panel will consist of the following staining protocol
Tube 1 – CD 45 FITC / CD 14 PE – Used to locate lymphocyte population as well as determine
purity of specimen and monocyte contamination
Tube 2 – _1a FITC/ _1a PE/ _1a PerCP – Isotype control to check for background staining.
Tube 3 – CD 4 FITC/ CD 8 PE / CD 20 PerCP – Used to determine CD4/CD8 ratio as well as
determining B cell population counts.
Tube 4 – CD 4 FITC/ CD 25 PE/ HLA – DR PerCP – Check for specific activation markers on CD 4
cells.
Tube 5 – CD 4 FITC/ CD 69 PE/ CD 3 PerCP – Used to get true CD4 counts on T-cells as well as
look at another activation marker on CD4 cells.
Cylex immune assay will be run as listed above. This assay requires minimal amount of whole
sodium heparinized blood and will be used from same tube as flow analyses. The whole blood
is diluted with a saline base diluent. It is then stimulated overnight with
phytohemagglutinin. The CD4+ or CD3+ T cells are then isolated using magnetic beads. They
are lysed and ATP production is recorded using a luciferase based reaction.
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Allocation: Non-Randomized, Endpoint Classification: Pharmacokinetics/Dynamics Study, Intervention Model: Crossover Assignment, Masking: Open Label, Primary Purpose: Diagnostic
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