Blood and Marrow Transplantation Reviews: Volume 12, Issue 2
Introduction: Antithymocyte Globulin: Teaching Old Dogs New Tricks
by John R. Wingard, MD
Editor
Antithymocyte globulin (ATG) has been used in hematopoietic stem
cell transplantation (HSCT) for several decades. Its important
role in the treatment of aplastic anemia was noted early, and its
usefulness has remained through the decades both as part of the
conditioning regimen for some HSCT applications and as a therapy
for acute graft-versus-host disease (GVHD). Multiple polyclonal
and monoclonal antibody preparations have been developed over the
years. There are differences in these various products, but the
clinical significance of these differences is uncertain.
Comparative trials have not been conducted, and today it remains
unclear as to whether one product might be more suited for a
specific application than another. Moreover, comparative trials
have been made difficult by the lack of clear convertibility of
different doses and dose schedules of the various products.
There are important differences between the anti-T-cell antibody
products and pharmacologic agents that suppress T-cell function.
The prolonged presence of antibody in the circulation and its
ongoing activity in vivo for days to weeks is a clear-cut
difference. This activity could have a beneficial effect by
dampening deleterious immunopathologic reactions. In some
situations, however, this prolonged action can have
disadvantageous effects such as increasing susceptibility to
infection or lymphomas.
These proceedings of a symposium held at the 2002 Tandem BMT
Meetings present new data from pilot studies to evaluate the role
of ATG in new HSCT applications. Dr. Nash discusses ATG use in
the conditioning regimen of patients undergoing high-dose
immunosuppressive (not cytotoxic) therapy prior to stem cell
infusions as therapy for immunologic disorders. Dr. Blazar
presents a compilation of data from the University of Minnesota
regarding the use of ATG as therapy for patients with refractory
acute GVHD and examines factors that influence outcome. Dr.
Spitzer considers the role of ATG in nonablative transplantation
conditioning regimens. Finally, Dr. Laughlin reports outcome data
from patients undergoing cord blood transplantation in which ATG
was incorporated into the conditioning regimen.
These presentations have the unifying theme of examining the
utility of a time-tested biological preparation for new HSCT
applications. These data suggest that ATG will continue to have
an important role in HSCT decades later. Is horse ATG a better
agent for suppression of T-cell function than other biologic
preparations or pharmacologic agents developed to accomplish the
same purpose? Unfortunately, these datasets do not answer this
question, which must be addressed using controlled trials, larger
sample sizes, and different study designs to probe the individual
contribution of ATG. Notwithstanding, these data are helpful in
setting the stage for consideration of such issues in subsequent
studies and in clarifying both the benefits and limitations of
these agents in current HSCT practice.
In this issue:
Introduction John R. Wingard, MD
Membership Application
ASBMT News
The Evolving Role of Equine Antithymocyte Globulin in
Hematopoietic Stem Cell Transplantation
High-Dose Immunosuppression in the Autoimmune Transplantation
Setting: Lessons Learned Richard A. Nash, MD
The Early Use of Equine ATG in Nonmyeloablative Stem Cell
Transplantation Bruce R. Blazar, MD
The Role of Equine ATG in Nonmyeloablative Stem Cell
Transplantation Tom Spitzer, MD
Hematopoietic Engraftment and Survival after Unrelated Donor
Umbilical Cord Blood Transplantation in Adults Mary Laughlin, MD
Journal Watch
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