Clinical Trial Details
— Status: Completed
Administrative data
| NCT number |
NCT01081405 |
| Other study ID # |
TLI-001-2007 |
| Secondary ID |
2007-005563-10 |
| Status |
Completed |
| Phase |
N/A
|
| First received |
|
| Last updated |
|
| Start date |
November 2007 |
| Est. completion date |
November 2022 |
Study information
| Verified date |
March 2024 |
| Source |
Fondazione EMN Italy Onlus |
| Contact |
n/a |
| Is FDA regulated |
No |
| Health authority |
|
| Study type |
Interventional
|
Clinical Trial Summary
To exploit the curative potential of allografting, the ultimate clinical goal is to separate
GVL from GVHD. In murine preclinical models, recipients of allogeneic hematopoietic cell
transplants after a preparative regimen of total lymphoid irradiation (TLI) and antithymocyte
globulin (ATG) did not develop GVHD. The murine TLI/ATG study was turned into a clinical
phase I protocol for patients with hematological malignancies, and a reduction of acute GVHD
to < 3% was observed (Lowsky R et al, N Engl J Med). This suggests that specific immune
mechanisms control GVHD and preserve GVL. The study will include patients with lympho and
myeloproliferative diseases. The conditioning regimen will consist of TLI [ten 80 cGy
fractions on day -11 through day -7 and on day -4 through day -1; the radiation field (four
fields-two anterior and two posterior) involves all major lymphoid organs including the
thymus, spleen and lymph nodes] and ATG (five i.v. doses at 1.5 mg/kg/day from day -11
through day -7). G-CSF mobilised hematopoietic cells, collected on days -1 and 0, from
HLA-identical siblings or unrelated donors will be infused on day 0. Post-transplant
immunosuppression will consist of oral cyclosporine (at 6.25 mg/kg/d) from day -3 and
micophenolate mophetile (at 15 mg/Kg bid) from day +1. The clinical primary objective is to
reduce the incidence of GVHD to < 5%, with better survival and quality of life.
Description:
PATIENT ENROLMENT.
It is expected that about 15 patients / year will be enrolled in this phase I-II protocol.
Patient selection will be based on the following criteria:
Eligibility Criteria:
1. Any patient with one of the following lympho or myeloproliferative malignancies or
syndromes in whom allogeneic NST is warranted. Patients with other selected
malignancies/disorders may also be considered but must be approved by the transplant
team and the Principal Investigator.
2. Patient age > 50 years, or for patients <50 years of age but because of pre-existing
medical conditions or prior therapy are considered to be at high risk for
regimen-related toxicity associated with conventional myeloablative transplants.
3. an HLA-identical sibling or matched unrelated donor is available. Patients with one
antigen mismatched donors can be considered but only after discussion with the
transplant team and the Principal Investigator.
STEM CELL TRANSPLANTATION:
(A) TLI Administration: see "brief description" (B) ATG: Thymoglobulin will be administered
five times intravenously at 1.5 mg/kg/day from day -11 through day -7 for a total dose of 7.5
mg/kg. Thymoglobulin doses will be based on the adjusted ideal body weight. Premedication for
thymoglobulin will include solumedrol 1.0 mg/kg.
Mobilized PBPC: The minimum cell doses (based on recipient body weight) for transplants are >
5x106 CD34+ cells/kg. Cells collected on days -1 and 0 will be pooled and processed for
infusion on day 0. Fresh cells (not frozen) are to be infused. For related donor transplants,
if the target cell dose is not achieved then a third apheresis procedure may be performed on
day+1 and the cells infused on the same day. Collection of cells for unrelated donor
transplants will be coordinated through the Italian bone Marrow Transplant Registry and
subject to the rules of that Program. If mobilized PBPC is not available through certain
collection centers then bone marrow will be used.
(F) Cyclosporine (CSP): CSP is given at 6.25 mg/kg p.o. b.i.d (9 a.m and 9 p.m.) from day -3
until after the day +56 chimerism results are obtained. CSP will be tapered after the day +56
chimerism results are obtained. If the day +56 chimerism results show >40% donor cells in the
CD3+ lineage, and the patient is without evidence of GVHD then CSP taper will begin. The CSP
will be tapered at 6% every week. Modifications of the taper schedule may be indicated if
significant disease progression occurs early post-transplantation or the patient develops
GVHD.
(G) Mycophenylate mofetil (MMF): Administration of MMF will begin at 15 mg/kg po on day 0, at
5-10 hours after mobilized PBPC infusion is complete. Thereafter,beginning on day +1 MMF is
taken at 15 mg/kg po b.i.d. (30 mg/kg/day) if transplantation was using a matched related
donor and 15 mg/kg po t.i.d if from a matched unrelated donor or a one antigen mismatched
donor. Doses will be rounded up to the nearest 250 mg (capsules are 250 mg). MMF will be
stopped on day +28 for matched related donors and for one antigen mismatched or unrelated
donors beginning day +40 MMF will be tapered by 10% weekly till off, typically by day +96.
POST-TRANSPLANT FOLLOW-UP
Clinical: The incidence, severity and extent of acute and chronic GVHD will be monitored and
scored according to standard criteria. As well, documented and presumed post-transplant
infectious complications, rate of relapse, event-free and overall survival and transplant
related mortality will be recorded.
Assessment of Disease Response: Since the diseases treated on this protocol are heterogenous,
appropriate disease specific studies will be performed to evaluate response to transplant.
Responses will be classified as continued complete remission (CCR), achieved complete
remission (CRa), partial response (PR), progressive disease (PD), or no response (NR).
Disease response will be according to accepted criteria. All cases of progressive disease
should be discussed with the Principal Investigators. If patients show evidence of
progressive disease then they may be candidates for donor lymphocyte infusion.
