Lymphoma Clinical Trial
Official title:
A Two Step Approach to Allogeneic Hematopoietic Stem Cell Transplantation for Patients With Hematologic Malignancies in Remission From HLA Partially-Matched Related Donors
The primary hypothesis of this research study is that patients in remission undergoing myeloablative haploidentical hematopoietic stem cell transplantation (HSCT) on the Thomas Jefferson University (TJU) 2 Step treatment regimen will have a disease-free survival (DFS) rate at 1 year that is the same or better than the historical DFS of patients with similar diagnoses and ages undergoing matched sibling HSCT. Based on a review of the literature a DFS rate of 50% or better at 1 year would meet the criterion for an effective alternative therapy. A DFS rate of 75% or better would imply superior efficacy of the TJU 2 Step approach over T-replete matched sibling HSCT.
The primary rationale for the development of this research study is to find out if the
Thomas Jefferson University (TJU) 2 Step approach to stem cell transplant is an effective
treatment for patients with blood cancers who require transplant for long-term survival but
are without an available matched-sibling donor. Historically, survival rates for patients
undergoing half-matched stem cell transplant have been much lower than those observed after
matched sibling stem cell transplant. This may be due to the poor-risk disease features of
the patients by the time they are referred for hematopoietic stem cell transplantation
(HSCT). Survival post half-matched stem cell transplant has also been affected by the
requirement to remove or soothe donor T cells resulting in higher rates of infection and
relapse. Newer approaches to haploidentical HSCT, such as the TJU 2 Step approach, utilize
cyclophosphamide (CY) to tolerize donor lymphocytes instead of removing them completely from
the donor product. This has resulted in less infection without concomitant increase in
severe graft-versus-host disease (GVHD) and has increased overall survival as compared to
older haploidentical treatment approaches due to decreases in regimen-related morbidity.
Because of the historically low overall survival (OS) after haploidentical HSCT, it has
become a procedure of last resort with most centers unwilling to consider it unless all
other options are exhausted. With the recent development of regimens such as the TJU 2 Step
approach which provide safe, alternative platforms for HSCT, it is now feasible, and
ethically more acceptable, for patients without matched sibling donors to undergo HSCT prior
to being heavily pretreated or developing resistant disease. In this setting, i.e.
equivalent regimen safety profiles and more homogenous patient comparison groups, it is
possible to more accurately compare antitumor effects between matched sibling donors and
haploidentical donors. There is ample evidence in the literature that HLA mismatching causes
GVHD. There is not a large body of evidence supporting the notion that HLA mismatching
provides superior tumor control translating into greater relapse free survival. As compared
to more common types of transplants where donor T cells are given to the recipient, the
investigators would surmise that the T cell tolerization associated with the TJU 2 Step
approach may decrease the anti-tumor effects of the donor immune system. Conversely, the
greater degree of human leukocyte antigen (HLA) mismatch with exploitation of NK effects may
mitigate some of the attenuated T cell alloreactivity.
Thus, in the context of comparable regimen-related toxicity, our major aim in this research
study is to compare graft versus tumor effects as measured by disease-free survival (DFS)
between matched sibling HSCT and the TJU 2 Step haploidentical HSCT. If DFS is similar
despite T cell tolerization, than the TJU 2 Step haploidentical approach should be
considered an effective alternative therapy for those patients in remission without a
matched sibling donor. The widespread benefit of this outcome would be the enfranchisement
of segments of the population who are without available matched donors resulting in a delay
or a failure to receive this potentially life-saving therapy. If DFS survival after
treatment on the TJU 2 Step haploidentical approach is superior to what would be expected
after matched sibling HSCT, then one could conclude that haploidentical HSCT confers greater
tumor control forming the basis for future studies regarding the potential benefits of
utilizing haploidentical donors over matched sibling donors when both types of donors are
available.
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Endpoint Classification: Efficacy Study, Intervention Model: Single Group Assignment, Masking: Open Label, Primary Purpose: Treatment
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