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Query: UMLS:C0018133 (
graft-versus-host disease
)
18,032
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
We evaluated demographic characteristics and graft composition as risk factors for acute
graft-versus-host disease
(
GVHD
) in 160 adult recipients of HLA-identical allogeneic blood stem cell transplants. The patients received a median nucleated cell dose of 7.9 x 10(8)/kg and median C34(+) cell dose of 5.6 x 10(6)/kg.
GVHD
prophylaxis consisted of cyclosporine (CSA) and steroids, tacrolimus (
FK506
) and steroids, or
FK506
and methotrexate. Grades 2 to 4
GVHD
occurred in 31% (95% CI, 23% to 39%), and grades 3 to 4
GVHD
in 14% (95% CI, 8% to 20%). In univariate analyses,
GVHD
prophylaxis with CSA and high CD34(+) cell doses were significant risk factors for grades 2 to 4
GVHD
, but diagnosis, age, use of total body irradiation, donor sex, female donor for male recipient, donor parity, donor alloimmunization, viral serology, nucleated cell dose, CD3(+) cell dose, and CD56(+) cell dose did not alter the incidence of
GVHD
significantly. With a CD34(+) cell dose less than 8 x 10(6) CD34(+) cells/kg, the risk of grades 2 to 4
GVHD
was significantly higher for those who received CSA (39%, 95% CI, 21% to 47%) in comparison with those on
FK506
(18%, 95% CI, 10% to 26%) (P =.03), but
GVHD
prophylaxis regimen had less impact with a higher CD34(+) cell dose (overall grades 2 to 4
GVHD
rate 52%, 95% CI, 37% to 67%).
GVHD
prophylaxis and CD34(+) cell dose are independent risk factors for acute
GVHD
after allogeneic blood stem cell transplantation.
...
PMID:Risk factors for acute graft-versus-host disease after allogeneic blood stem cell transplantation. 1043 35
Pneumocystis carinii pneumonia (PCP) is a life-threatening but preventable infection that may occur after bone marrow transplantation (BMT). Although various prophylactic regimens have been used in this setting to prevent active infection, their efficacy, toxicity profile, and impact on outcomes are poorly described in this patient group. We undertook a retrospective cohort study in which we reviewed the records of 451 adult patients who underwent BMT for hematologic malignancies, aplastic anemia, or myelodysplasia over a 7-year period at the Brigham and Women's Hospital. Post-BMT PCP prophylaxis consisted of aerosolized pentamidine (AP) 150 mg every 2 weeks or 300 mg per month, trimethoprim/sulfamethoxazole (TMP/SMX) 160/800 mg orally b.i.d. 3 times per week, or dapsone 100 mg orally each day. Prophylaxis was continued for 1 year post-BMT in all patients when clinically feasible. One hundred twenty-one patients were unevaluable because of death or relapse <60 days after BMT (n = 89), loss to follow-up upon hospital discharge (n = 20), or other reasons (n = 12). Three eligible patients did not receive any prophylaxis and were not further evaluated. Of the 327 patients analyzed, 133 underwent autologous BMT, 4 syngeneic BMT, 159 related allogeneic BMT, and 31 unrelated allogeneic BMT.
Graft-versus-host disease
prophylaxis in the 190 patients receiving allogeneic BMT consisted of T-cell depletion with anti-CD5 and complement in 58 patients and cyclosporine/methotrexate or
FK506
with or without steroids in 132 patients. Eight of 327 (2.4%) documented PCP cases were identified, 0 of 105 in patients receiving only TMP/SMX. Four cases occurred in patients receiving only AP (4/44, 9.1%; odds ratio [OR] relative to TMP/SMX 23.4, 95% confidence interval [CI] 1.2, 445.2); 1 in patients receiving only dapsone (1/31, 3.2%; OR not significant); 2 in patients receiving more than 1 prophylactic regimen (2/147 1.4%; OR not significant); and 1 >1 year post-BMT in a patient who was off PCP prophylaxis. Although the patients receiving only AP had a significantly lower probability of treatment-related toxicity than those receiving TMP/SMX (OR 0.19 [95% CI 0.04, 0.851), the probability of their acquiring other serious non-PCP infections was increased (OR 2.2 [95% CI 1.0, 4.6]), and the probability of their dying by 1 year post-BMT was significantly higher (OR 5.2 [95% CI 2.4, 26.6]), even when adjusted for variables such as type of BMT (autologous versus allogeneic; high versus low risk) and sex. Although AP is associated with fewer toxicities, the data show that it is inferior to TMP/SMX in preventing PCP in the post-BMT setting and is associated with an increased risk of other infections and a higher mortality at 1 year after BMT.
...
PMID:Aerosolized pentamidine as pneumocystis prophylaxis after bone marrow transplantation is inferior to other regimens and is associated with decreased survival and an increased risk of other infections. 1070 97
A hybrid human protein was produced in E. coli by fusing the genes encoding human pancreatic RNase1 (hpRNase1) and human IL-2 (hIL-2). The recombinant hpRNase1-hIL-2 inhibited protein synthesis in HTLV-1-infected, malignant T cells, which hyperproduce high affinity IL-2 receptors, with an IC(50)of 2x10(-8) M, whereas no inhibition was detectable in control cells with lower affinity receptors. HpRNase1 alone had an IC(50)of almost 10(-3) M. A molar excess of hIL-2 blocked the protein synthesis inhibition dose-dependently. In a human mixed lymphocyte culture, hpRNase1-hIL-2 inhibited the proliferation of responder cells with potency comparable to that of cyclosporine, while non-effective doses of
FK506
importantly improved its potency. Despite its short half-life in animals, hpRNase1-hIL-2 rapidly enters cells in a few minutes and arrests the protein translation in less than 10 h. Thus, hpRNase1-hIL-2 may be useful to selectively eliminate activated lymphocytes hyperproducing high affinity IL-2 receptors, as in allograft rejection,
graft-versus-host disease
, autoimmune disorders, adult T cell leukaemia and other lymphoproliferative or retroviral malignancies including HIV infection, without inducing general immunosuppression. As an entirely human "immunotoxin analogue" it may alleviate the dose limiting toxicity and immunogenicity of conventional immunotoxins.
...
PMID:Targeting activated lymphocytes with an entirely human immunotoxin analogue: human pancreatic RNase1-human IL-2 fusion. 1084 65
Forty-eight patients who underwent bone marrow transplantation (BMT) from serologically HLA-matched unrelated donors received tacrolimus (
FK506
) alone or with methotrexate (MTX) and/or methylprednisolone (mPSL) to prevent
graft-versus-host disease
(
GVHD
). We analyzed retrospectively the efficacy of
FK506
for
GVHD
prophylaxis, and its toxicity, by comparing three groups of patients: those given
FK506
alone, those given
FK506
+ mPSL, and those given
FK506
+ MTX + mPSL. Grade III and IV acute
GVHD
occurred in five of 10 patients given
FK506
alone and in 11 of 30 patients given
FK506
+ mPSL. In these groups, severe acute
GVHD
was commonly seen in the patients who discontinued
FK506
administration early after BMT and in those who received bone marrow from genotypically HLA-mismatched donors. Early withdrawal of
FK506
was due mainly to severe nephrotoxicity. The incidence of nephrotoxicity was very high in patients who received high-dose
FK506
as well as melphalan-containing preconditioning (80% and 50%). None of eight patients who received
FK506
+ mPSL + MTX developed grade III-IV acute
GVHD
even though five of them received bone marrow from genotypically HLA-mismatched donors. In patients receiving bone marrow from unrelated donors, adjustment of the initial dose of
FK506
seems essential in order to avoid severe nephrotoxicity, and combination of MTX and
FK506
is useful for preventing severe acute
GVHD
.
...
PMID:[Prophylaxis with FK-506 for graft-versus-host disease after transplantation of bone marrow from unrelated donors]. 1087 6
A 10-year-old girl presented with massive pericardial/pleural effusion with anasarca 216 days after an allogeneic bone marrow transplantation from her HLA-matched sibling for relapsed acute lymphoblastic leukemia. She did not show any other symptoms of chronic
graft-versus-host disease
(
GVHD
). The antinucleolar antibody was elevated in the blood and the pleural fluid. The lymphocytes in the fluid were mostly CD8+/HLA-DR+, and a majority of CD8+ cells in the blood expressed CD57. These data suggested that she had chronic
GVHD
. Immunosuppressive therapy including prednisolone, cyclosporin A, high-dose methylprednisolone, tacrolimus (
FK506
), and methotrexate had no effect, and the patient died of Aspergillus pneumonia 183 days after the presentation of the disease. Although it has not been described before, isolated serositis with edema should be recognized as a clinical feature of chronic
GVHD
.
...
PMID:Massive pericardial and pleural effusion with anasarca following allogeneic bone marrow transplantation. 1090 62
Currently, limited data exist on the role of tacrolimus (
FK506
) in pediatric allogeneic marrow transplantation. Forty-one patients who received tacrolimus as prophylaxis were reviewed, with a median age of 9 years (range 0.2-16 years). Twenty-one patients underwent related donor transplants and 20 underwent unrelated donor transplants. All patients received tacrolimus beginning the day prior to transplant at a dose of 0.03 mg/kg/day by continuous i.v. infusion. When clinically possible, patients were switched to oral therapy in two divided doses, at four times the intravenous dose. Tacrolimus levels were monitored twice a week, and dosages adjusted to maintain serum levels 5-15 ng/ml. Common adverse effects included hypomagnesemia (98%), hypertension (49%), nephrotoxicity (34%), and tremors (32%). Less common side-effects (<10% cases) included seizures and hyperglycemia. The median time to ANC recovery (ANC >500 x 106/l) was 15 days. For the related donor group, the incidence of grade II-IV acute
GVHD
was 33%, and grade III-IV
GVHD
19%. For the unrelated donor group, the incidence of grade II-IV acute
GVHD
was 55%, and grade III-IV
GVHD
30%. Overall, tacrolimus therapy was well tolerated as prophylaxis for acute
GVHD
in pediatric patients undergoing allogeneic transplantation.
...
PMID:Tacrolimus (FK506) and methotrexate as prophylaxis for acute graft-versus-host disease in pediatric allogeneic stem cell transplantation. 1091 26
GVHD
continues to be a major complication after allogeneic hematopoietic stem cell transplantation even when the recipient is given immunosuppression for the prophylaxis of this severe disease. There have been many advances in the prevention and treatment of
GVHD
, using compounds such as cyclosporine,
FK506
, mycophenolate mofetil or monoclonal IL-2 receptor antagonist. New strategies seem to include sequential therapy involving the blocking of both endogenous cytokines and alloreactive donor cells. However, further clinical and laboratory studies are needed in order to improve the therapy of established
GVHD
.
...
PMID:New strategies in the treatment of graft-versus-host disease. 1093 79
The macrolide lactone, tacrolimus (
FK506
), is utilized in bone marrow transplantation (BMT) to prevent
graft-versus-host disease
(
GVHD
). In the current study, we evaluated the ability of
FK506
to modify the function of dendritic cells (DCs) derived from CD34+ hematopoietic progenitor cells (HPCs). Comparable to DCs obtained in the absence of
FK506
, DCs cultured in the presence of
FK506
(FK-DCs) had higher expression of CD1a+ and formed a greater number of DC colonies. Despite the same expression of costimulatory molecules, FK-DCs displayed a reduced capacity to stimulate an allogeneic T cell response, and showed significantly lower interleukin (IL)-12 production. While normal DCs pulsed with the exogenous antigen, keyhole limpet hemocyanin (KLH) induced specific Th1-like interferon-gamma(IFN-gamma) producing CD4+ T cell line, FK-DCs induced Th2-like interleukin-4 (IL-4) producing CD4+ T cell line. These data demonstrate the ability of
FK506
to induce Th2-promoting function in developing DCs.
...
PMID:Tacrolimus (FK506) treatment of CD34+ hematopoietic progenitor cells promote the development of dendritic cells that drive CD4+ T cells toward Th2 responses. 1107 1
We report a case of cerebral hemorrhage associated with cyclosporin A (CsA)/
FK506
-related encephalopathy that developed in a 16-year-old woman after allogeneic bone marrow transplantation. Hematopoietic engraftment occurred on day 15, and the patient developed systemic convulsions after CsA was replaced by
FK506
for the treatment of acute
graft-versus-host disease
(
GVHD
). Based on magnetic resonance imaging, laboratory findings and cerebrospinal fluid studies, she was diagnosed as having CsA/
FK506
-related encephalopathy with cerebral hemorrhagic infarction. Although she recovered completely after discontinuation of
FK506
, she developed convulsions again 15 days after re-administration of
FK506
. A computed tomography scan showed cerebral hemorrhage. She died of respiratory failure. Vascular damage induced by immunosuppressive drugs and enhanced by acute
GVHD
seemed to be the cause of the cerebral hemorrhage. Since hypertension, which was present during both of the central nervous system events, seemed to have contributed to the development of the cerebral hemorrhage, it is proposed that CsA and
FK506
should be reduced or discontinued when patients who have risk factors of hypertension become hypertensive even if they have no symptoms of neurotoxicity.
...
PMID:Fatal cerebral hemorrhage associated with cyclosporin-A/FK506-related encephalopathy after allogeneic bone marrow transplantation. 1110 Jul 53
The increasing number of allogeneic stem cell transplants, particularly those involving donors other than HLA-identical siblings, has made the management of acute and chronic
graft-versus-host disease
(
GVHD
) a continuing problem for transplant experts. There have been improvements in the prevention of acute
GVHD
with cyclosporine- and
FK506
-based combination therapies, as well as lymphocyte depletion. However, fewer than 50% of patients have durable improvement after initial treatment.
FK506
and mycophenolate mofetil (MMF) are promising salvage therapies in steroid-resistant
GVHD
, as are the anti-cytokine antibodies and the purine nucleoside analog, pentostatin. The incidence of chronic
GVHD
has unfortunately not decreased, despite advances in treatment of acute
GVHD
. Treatment of chronic
GVHD
involves treatment of the underlying immunologic process and supportive therapies. Initial therapy has tended to be cyclosporine and prednisone. Refractory patients have hope with combination MMF and
FK506
, etretinate, plaquenil, and nonpharmacologic approaches, such as PUVA. Supportive care is an integral part of chronic
GVHD
management with emphasis on infection control and symptom control. Death in chronic
GVHD
is still largely attributable to infection. The progress in therapies for
GVHD
has been encouraging, but the future of
GVHD
management lies in a better understanding of its pathogenesis.
...
PMID:Management of graft-versus-host disease. 1112 7
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