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BioOncology Watch Timely Information for Practicing
Physicians |
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august 2002 Non-Hodgkin's Lymphoma (NHL) Ibritumomab tiuxetan
radioimmunotherapy. Gregory
Wiseman et al. conducted a multicenter phase II study in which 30 mildly
thrombocytopenic (100-149 x 109/L) patients with relapsed or
refractory low-grade NHL were treated with a reduced dose of 90Y
ibritumomab tiuxetan (0.3 instead of 0.4 mCi/kg). Grade 4 hematologic toxicity was observed, but it was transient
and reversible. The incidence of
grade 4 neutropenia, thrombocytopenia, and anemia was 33%, 13%, and 3%, respectively. The overall response rate was 83% with an
estimated median time to progression of 9.4 months (range, 1.7-24.6
months). These results demonstrate
that a reduced dose of 90Y ibritumomab tiuxetan is well tolerated
and has significant clinical activity in thrombocytopenic patients with
relapsed or refractory low-grade NHL.
(Wiseman GA, et al. Blood 2002;99:4336-4342) Molecular profiling. Andreas Rosenwald and colleagues
retrospectively reviewed tumor biopsy specimens and clinical data from 240
patients with previously untreated diffuse large B-cell lymphoma (DLBCL). All
patients had received prior anthracycline-based chemotherapy. Lymphochip DNA
microarrays were used to quantitate the expression of messenger RNA in the
lymphomas. Hierarchical clustering
grouped the DLBCLs into 3 large subgroups: germinal-center B-cell-like;
activated B-cell-like; and type 3 DLBCL. Bcl-2 translocation and
c-rel amplification were detected in only the germinal-center B-cell-like
subgroup and patients in this subgroup had the greatest 5-year survival rate
(60% vs. 35% vs. 39%; p<0.001). Four gene-expression signatures
(comprising 16 genes; 3 germinal center B-cell genes, 4 MHC class II genes, 6
lymph-node genes, and 3 proliferation genes) were found to predict survival. BMP6
was the only individual gene found to increase the predictive value for
survival of the 4 gene-expression signatures. Thus, these 17 genes were used
to construct a predictor of overall survival after chemotherapy, and this
gene-based tool and the standard international prognostic index were found to
be independent prognostic indicators. This study shows that DNA microarrays
can be used to formulate molecular predictors of survival. (Rosenwald A, et
al. N Eng J Med 2002;346:1937-1947) Epstein-Bar Virus-Lymphoproliferative Disease
(EBV-LPD) Preemptive rituximab. Joost van Esser and colleagues recently
monitored 49 recipients of TCD allogeneic SCT for EBV reactivation and
treated 15 of these patients who showed EBV reactivation to ³1000
geq/mL with a single infusion of rituximab (375 mg/m2). Fourteen patients had a complete clearance
of EBV-DNA from plasma in a median of 8 days (range, 1-46 days). One patient developed EBV-LPD but achieved
a complete remission after further rituximab and donor lymphocyte
infusions. Comparison with historical
controls (n=26) demonstrated a decrease in EBV-LPD-related mortality at 6
months with preemptive rituximab therapy (0% vs. 26% ±10%;
p=0.04). These preliminary findings
show that rituximab is an effective treatment for the prevention of
EBV-LPD-related mortality in high-risk patients. (van Esser JWJ, et al. Blood 2002;99:4364-4369) Relapsed Chronic Myelogenous Leukemia (CML) Donor lymphocyte infusion (DLI). Cesare Guglielmi and investigators with
the Chronic Leukemia Working Party of the European Group for Blood and Marrow
Transplantation retrospectively analyzed data from 298 relapsed CML patients
treated at 51 centers with DLI and found a lower ICD to be associated with
improved outcomes. Patients who received
£0.2 x 108
mononuclear cells/kg, compared to those who received either >0.2 to 2.0 or
>2.0 x 108 mononuclear cells/kg, had less myelosuppression
(p=0.01) and less graft versus host disease (p<0.001) while achieving a
similar response rate. These results translated to a greater 3-year survival
rate (84% vs. 63% vs. 58%) and a lower DLI-related mortality rate (5% vs. 20%
vs. 22%) for patients receiving the lower ICD. The data suggest that the first DLI cell dose should not exceed
0.2 x 108 mononuclear cells/kg.
(Gugliemi C, et al. Blood 2002;100:397-405) Idiopathic
Thrombocytopenia (ITP) Effect of pegylated recombinant
human megakaryocyte growth and development factor (PEG-rHuMGDF). Shosaku Nomura and coworkers report the
treatment of 4 patients with ITP refractory to standard therapy (platelet
count <30 x 109/L) with PEG-rHuMGDF 0.5 ug/kg/day intravenously
for up to 7 days. Platelet counts
were increased in 3 patients. In
addition, reticulated (indicating newly produced) platelets were observed resulting
in decreased bleeding episodes even in patients for whom platelet counts
remained low. Two patients developed
thrombocytosis (platelet count >700 x 109/L) a week after the
last administration of PEG-rHuMGDF.
Platelet counts returned to baseline levels within 4-6 weeks in all
cases. These very early results
suggest that PEG-rHuMGDF may be an effective therapy for patients with ITP.
Further clinical studies are needed.
(Nomura S, et al. Blood 2002;100:728-730) Cytomegalovirus (CMV) InfectionRole of Campath-1H. Suparno
Chakrabarti and colleagues used PCR-based assays in a multicenter study to
monitor the incidence and pattern of CMV infection in 101 patients undergoing
nonmyeloablative conditioning containing Campath-1H. CMV infection occurred in 51 patients
(50%) at a median of 27 days after SCT.
The median time to CD4+ T-cell count >200/uL was 9 months in the 48
patients tested and a low CD4+ T-cell count at 3 months was found to be a
risk factor for late recurrence of CMV infection. The results demonstrate an association of Campath-1H treatment
with prolonged immune deficiency and a high incidence of CMV infection. (Chakrabarti S, et al. Blood
2002;99:4357-4363) |
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