Background: IFN-γ is crucial in the pathogenesis of GVHD and higher levels are reported to be elevated in patients with active chronic GVHD. Immune-monitoring of INF-levels after alloHSCT could help in the management of GVHD. A recent ELISA based test (QuantiFERON®-CMV) could measure specific (anti-CMV) and aspecific production of IFN-γ in whole blood. Preliminary data suggests that aspecific production of IFN-γ should be associated with GVHD. The aim of this study is to confirm the reliability of QuantiFERON®-CMV for association and prediction of GVHD. Methods: the study was performed in 2 phases. In the fisrt phase of the study, 92 whole blood specimen were collected and analyzed from 29 patients undergoing alloHSCT in order to confirm the preliminary data. QuantiFERON® CMV is an in vitro diagnostic test that use an antigenic human cytomegalovirus proteins (CMV) peptide cocktail to stimulate cells from whole blood. Detection of interferon-γ (IFN-γ) by ELISA is used to identify responses to these peptide antigens. The IFN-γ response in the CMV Ag tube is considered positive if > 0.2 UI/mL as defined by the manufacturer. The Mitogen-stimulated (PHA) plasma sample is used as an IFN-γ positive control for each specimen tested. In order to assess the association between IFN-γ response due to PHA stimulation and GVHD, the positivity of the test was determined according to 2 different cut-off: #1) 0,5 IU/mL as defined by manufacturer, #2) 9 IU/mL as experimentally defined by the median of the observations in our data set. GVHD extension was defined by Seattle criteria and/or the number of involved sites, Chi-square test was used to assess the statistical correlation between IFN-γ production and clinical outcomes. In the second phase 10 patients were observed prospectively with collection of blood samples every 2-3 weeks since engraftment until 4-6 months after SCT in order to study the PHA stimulated IFN-γ production in relationship with the onset of chronic GVHD. Results: among 92 samples 70 were positive for the PHA stimulated IFN-γ production according to the cut-off #1; 61% (43/70) were associated with GVHD whereas 27% (6/22) with lower PHA stimulated IFN-γ production were associated with GVHD: this difference was proved to be significant (p=0.005). Among 92 samples 46 were positive for the PHA stimulated IFN-γ production according to the cut-off #2; 71% (33/46) were associated with GVHD whereas 34% (16/46) with lower PHA stimulated IFN-γ production were associated with GVHD: this difference was proved to be significant (p=0.000). Among the 10 patients observed prospectively during the first 6 months after alloHSCT 7 became positive for the PHA stimulated IFN-γ production: 6/7 developed GVHD in a median time of 100 days according to the cutoff #1 and after a median time of 33 days according the cutoff#2. Four patients received steroid treatment for extensive chronic GVHD and their PHA stimulated IFN-γ production dropped after treatment (figure 1). Conclusions: The PHA stimulated IFN-γ production is strictly associated to GVHD, seems to predict its onset and could help in the modulation of immunesuppressive treatment. However, larger prospective studies are needed.
IFN-γ induced by PHA stimulation as new marker for GVHD prediction in patients undergoing Allogeneic Hematopoietic Stem Cell Transplantation
MORELLO, Enrico;MONSURRO', Vladia;COIN, Silvia;TRIDENTE, Giuseppe;
2008-01-01
Abstract
Background: IFN-γ is crucial in the pathogenesis of GVHD and higher levels are reported to be elevated in patients with active chronic GVHD. Immune-monitoring of INF-levels after alloHSCT could help in the management of GVHD. A recent ELISA based test (QuantiFERON®-CMV) could measure specific (anti-CMV) and aspecific production of IFN-γ in whole blood. Preliminary data suggests that aspecific production of IFN-γ should be associated with GVHD. The aim of this study is to confirm the reliability of QuantiFERON®-CMV for association and prediction of GVHD. Methods: the study was performed in 2 phases. In the fisrt phase of the study, 92 whole blood specimen were collected and analyzed from 29 patients undergoing alloHSCT in order to confirm the preliminary data. QuantiFERON® CMV is an in vitro diagnostic test that use an antigenic human cytomegalovirus proteins (CMV) peptide cocktail to stimulate cells from whole blood. Detection of interferon-γ (IFN-γ) by ELISA is used to identify responses to these peptide antigens. The IFN-γ response in the CMV Ag tube is considered positive if > 0.2 UI/mL as defined by the manufacturer. The Mitogen-stimulated (PHA) plasma sample is used as an IFN-γ positive control for each specimen tested. In order to assess the association between IFN-γ response due to PHA stimulation and GVHD, the positivity of the test was determined according to 2 different cut-off: #1) 0,5 IU/mL as defined by manufacturer, #2) 9 IU/mL as experimentally defined by the median of the observations in our data set. GVHD extension was defined by Seattle criteria and/or the number of involved sites, Chi-square test was used to assess the statistical correlation between IFN-γ production and clinical outcomes. In the second phase 10 patients were observed prospectively with collection of blood samples every 2-3 weeks since engraftment until 4-6 months after SCT in order to study the PHA stimulated IFN-γ production in relationship with the onset of chronic GVHD. Results: among 92 samples 70 were positive for the PHA stimulated IFN-γ production according to the cut-off #1; 61% (43/70) were associated with GVHD whereas 27% (6/22) with lower PHA stimulated IFN-γ production were associated with GVHD: this difference was proved to be significant (p=0.005). Among 92 samples 46 were positive for the PHA stimulated IFN-γ production according to the cut-off #2; 71% (33/46) were associated with GVHD whereas 34% (16/46) with lower PHA stimulated IFN-γ production were associated with GVHD: this difference was proved to be significant (p=0.000). Among the 10 patients observed prospectively during the first 6 months after alloHSCT 7 became positive for the PHA stimulated IFN-γ production: 6/7 developed GVHD in a median time of 100 days according to the cutoff #1 and after a median time of 33 days according the cutoff#2. Four patients received steroid treatment for extensive chronic GVHD and their PHA stimulated IFN-γ production dropped after treatment (figure 1). Conclusions: The PHA stimulated IFN-γ production is strictly associated to GVHD, seems to predict its onset and could help in the modulation of immunesuppressive treatment. However, larger prospective studies are needed.I documenti in IRIS sono protetti da copyright e tutti i diritti sono riservati, salvo diversa indicazione.