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  • 1
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    Relapse risk after umbilical cord blood transplantation: enhanced graft-versus-leukemia effect in recipients of 2 units
    American Society of Hematology ; 2009
    In:  Blood Vol. 114, No. 19 ( 2009-11-05), p. 4293-4299
    Details
    In: Blood, American Society of Hematology, Vol. 114, No. 19 ( 2009-11-05), p. 4293-4299
    Abstract: Umbilical cord blood (UCB) transplantation is potentially curative for acute leukemia. This analysis was performed to identify risk factors associated with leukemia relapse following myeloablative UCB transplantation. Acute leukemia patients (n = 177; 88 with acute lymphoblastic leukemia and 89 with acute myeloid leukemia) were treated at a single center. Patients received a UCB graft composed of either 1 (47%) or 2 (53%) partially human leukocyte antigen (HLA)–matched unit(s). Conditioning was with cyclophosphamide and total body irradiation with or without fludarabine. The incidence of relapse was 26% (95% confidence interval [CI], 19%-33%). In multivariate analysis, relapse was higher in advanced disease patients (≥ third complete remission [CR3] ; relative risk [RR], 3.6; P 〈 .01), with a trend toward less relapse in recipients of 2 UCB units (RR = 0.6; P = .07). However, relapse was lower for CR1-2 patients who received 2 UCB units (RR 0.5; P 〈 .03). Leukemia-free survival was 40% (95% CI, 30%-51%) and 51% (95% CI, 41%-62%) for single- and double-unit recipients, respectively (P = .35). Although it is known that transplantation in CR1 and CR2 is associated with less relapse risk, this analysis reveals an enhanced graft-versus-leukemia effect in acute leukemia patients after transplantation with 2 partially HLA-matched UCB units. This trial was registered at http://clinicaltrials.gov as NCT00309842.
    Type of Medium: Online Resource
    ISSN: 0006-4971 , 1528-0020
    URL: Article
    DOI: 10.1182/blood-2009-05-220525
    RVK:
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    Language: English
    Publisher: American Society of Hematology
    Publication Date: 2009
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  • 2
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    Elevated Absolute Lymphocyte Counts Following Acute Graft Vs. Host Disease Treatment Is Associated with Therapeutic Responses and Lower Non-Relapse Mortality Following Umbilical Cord Blood Transplant,
    American Society of Hematology ; 2011
    In:  Blood Vol. 118, No. 21 ( 2011-11-18), p. 4085-4085
    Details
    In: Blood, American Society of Hematology, Vol. 118, No. 21 ( 2011-11-18), p. 4085-4085
    Abstract: Abstract 4085 Acute graft vs. host diseases (aGVHD) is a life threatening complication of allogeneic hematopoietic cell transplantation (allo-HCT). In a large series of patients undergoing allo-HCT (n=863) we recently demonstrated that following the initiation of corticosteroids, a clinical response at day 28 was associated with an increased likelihood of overall treatment response and a reduction in treatment related mortality (TRM) (MacMillan, Blood, 2010). We have also shown that patients who have rapid lymphocyte recovery following umbilical cord blood transplantation (UCBT) have improved outcomes (Burke, BBMT, 2010). To date, no study has addressed the influence of absolute lymphocyte count (ALC) on aGVHD treatment responses. We hypothesized that high ALC might predict favorable responses to aGVHD therapy. To test this hypothesis we reviewed the ALC at the time of aGVHD diagnosis and weekly following the initiation of corticosteroid therapy (48 mg/m2 × 14 days followed by a 10% taper over 8 weeks). ALCs were collected on patients who had clinical laboratory data available in the electronic medical record and who had available data on clinical response to corticosteroid therapy. There were 211 patients transplanted at our center from 2001–2007 who fit the above criteria. Median age was 42 years (range 0.2–69 yrs). Thirty nine patients (19%) were 〈 18 years of age and 135 (64%) were 〉 35 years old. The majority of patients underwent UCBT (n=134, 64%) and most others received a sibling PBSC transplant (n=71, 34%). Myeloablative conditioning was used in 55% of patients. GVHD prophylaxis was mainly with CSA/MMF (n=142, 67%) or MTX/CSA (n=42, 22%). Median time to aGVHD onset was 37 days (11–92). Patterns of aGVHD included skin only (n=91, 43%), gut only (n=36, 17%) or multi-organ involvement (n=82, 39%). At the time of GVHD diagnosis, ALC was not predictive of response to therapy. Likewise, there was no association with the ALC at D7 (after the start of steroid treatment) and therapeutic response. The D14 post-treatment ALC showed an association with clinical response at D28 (a time point previously associated with long-term responses and NRM). Patients with an ALC of 0–0.14, 0.15–0.34 and 〉 0.35 at D+14 after corticosteroid therapy had a 40%, 54% and 68% chance of a clinical response at D28 (p 〉 0.01). This translated into a reduction in non-relapse mortality for patients with higher ALC (0–0.14 vs. 〉 0.15; 33% [19–47%] vs 23% [17–29%] , p=0.04). Subgroup analysis showed that these observations were mainly driven by the myeloablatve UCB group. Treating ALC as a continuous variable and using a repeated measures approach, we observed that for every unit increase in ALC between the day of diagnosis and D14, there was a 2.26 higher increased likelihood of having a complete clinical response at D28 (p 〉 0.001). Similar results were seen for NRM (OR=0.89 [0.81–9.8], p=0.01). In multivariate analysis, repeated measures of ALC (from D0-14) remained significant for both D28 clinical response (p=0.001) and NRM (p=0.05). Patients with steroid refractory aGVHD (n=17) were treated with ATG. Because steroid refractory aGVHD has poor outcomes and because ATG can negatively impact ALC, we removed these patients from the analysis to determine the impact of ALC. In this subgroup analysis, ALC at D14 after aGVHD treatment remained associated with D28 clinical response in multivariate analysis (OR=3.01, 95%CI[1.24–7.35] , p=0.02). Using repeated analysis, the change in ALC from aGVHD treatment day D0 to 14 was associated with D28 treatment response (OR=4.42 [1.88–10.37], p 〈 0.001). Collectively, these results show that absolute ALC at D14 and increases in ALC from the day of treatment to day 14were associated with D28 clinical response and NRM. ALC maybe a simple and cost effective method to monitor response to aGVHD therapy. Disclosures: No relevant conflicts of interest to declare.
    Type of Medium: Online Resource
    ISSN: 0006-4971 , 1528-0020
    URL: Article
    DOI: 10.1182/blood.V118.21.4085.4085
    RVK:
    XA 33000
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    XA 10000
    Language: English
    Publisher: American Society of Hematology
    Publication Date: 2011
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  • 3
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    Higher CSA Levels After Umbilical Cord Blood Transplant For Acute Leukemia Result In Improved Survival
    American Society of Hematology ; 2013
    In:  Blood Vol. 122, No. 21 ( 2013-11-15), p. 2097-2097
    Details
    In: Blood, American Society of Hematology, Vol. 122, No. 21 ( 2013-11-15), p. 2097-2097
    Abstract: Cyclosporine A (CSA) is commonly used after bone marrow transplantation for graft versus host disease (GVHD) prophylaxis. There have been conflicting reports regarding dosing of CSA and its effects on relapse and GVHD. Higher doses of CSA after bone marrow transplantation have been associated with greater leukemia relapse. Because it was unknown whether umbilical cord blood transplantation (UCBT) has a similar risk, we studied the impact of CSA levels on UCBT outcomes in patients with acute leukemia. Patients and Methods We reviewed the records of 242 consecutive patients with acute leukemia who received UCBT and CSA for GVHD prophylaxis at our institution from 2004-2011. Eighty (33%) patients had acute lymphoblastic leukemia and 162 (67%) had acute myelogenous leukemia. Fifty-seven patients (24%) had a single UCBT; one hundred fifty-four patients (64%) underwent myeloablative conditioning. The median age at transplant was 30 (1-71) years and median follow-up 4.95 (0.56-10.29) years. Serum CSA levels were collected at least once a week around day -1 and continuing through ∼day 180. We hypothesized that early CSA levels would have the greatest impact on both graft vs. host disease (GVHD) and graft vs. leukemia (GVL) reactions. For the purpose of this study, we examined CSA levels during the first 6 weeks of administration and determined the median CSA level both early (day -3-20) and late (day 21-42). A median of 13 (range was 4-28) CSA levels were drawn during this time period. The median CSA level determined from day-3-20 was 273.5 and the median CSA from days 21-42 was 249.5. Based on the medians in each three week period, patients were divided into four different groups based CSA level and whether it was above or below the median (low-low; low-high; high-low and high-high). Results In multivariate analysis for patients with ALL, disease free survival (DFS) at one year and three years was significantly improved in patients that maintained high levels of CSA from days 21-42 (p=0.02 for low-high and p=0.01 for high-high). Overall survival (OS) was improved at one year for patients with high CSA levels late (p= 〈 0.01 for low-high and high-high) but at three years was improved in only patients that had maintained high CSA levels throughout the entire 6 weeks (p=0.03 for high-high). Patients with high levels of CSA from days 21-42 were also associated with less transplant related mortality (TRM) (p=0.04 for low-high and p=0.01 for high-high). There was no association of CSA levels and relapse or acute GVHD grades II-IV for ALL patients. In multivariate analysis of AML patients, we found that DFS at one year was significantly improved in patients that maintained high CSA levels at any time during the six weeks (p=0.01 for high-low, low-high and high-high) whereas at 3 years, patients that maintained high CSA levels early had a better chance of DFS (p=0.02 for high-low and high-high). OS at three years was also significantly greater in patients with high levels of CSA early (p=0.05 for high-low and high-high). TRM was decreased in patients that had high levels of CSA early (p=0.02 for high-low and high-high). Interestingly, in multivariate analysis, relapse was improved in patients that maintained initially low levels and then high levels of CSA (p=0.05). Acute GVHD grades II-IV was significantly improved in AML patients with high CSA levels for the entire 6 weeks (p=0.04 for high-high). Conclusions Taken together, these data suggest that high median CSA levels in the first six weeks is critical to ensure improved DFS and OS in patients with acute leukemia undergoing UCBT. Interestingly, in ALL patients, the improvement was seen in patients that maintained high CSA levels late, whereas in AML patients, it was seen in those that maintained high CSA levels early. This implies that the interaction between CSA dose and GVL may be different between myelogenous and lymphoid leukemia following UCBT. Disclosures: Wagner: Novartis: Research Funding.
    Type of Medium: Online Resource
    ISSN: 0006-4971 , 1528-0020
    URL: Article
    DOI: 10.1182/blood.V122.21.2097.2097
    RVK:
    XA 33000
    RVK:
    XA 10000
    Language: English
    Publisher: American Society of Hematology
    Publication Date: 2013
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  • 4
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    Next Generation XPO1 Inhibitor Shows Improved Efficacy and In Vivo Tolerability in Hematologic Malignancies
    American Society of Hematology ; 2015
    In:  Blood Vol. 126, No. 23 ( 2015-12-03), p. 317-317
    Details
    In: Blood, American Society of Hematology, Vol. 126, No. 23 ( 2015-12-03), p. 317-317
    Abstract: Restoring nuclear localization of tumor suppressors by blocking exportin 1 (XPO1) holds promise as a new therapeutic paradigm in many cancers, including chronic lymphocytic leukemia (CLL) and acute myeloid leukemia (AML). Oral selective inhibitor of nuclear export (SINE) compounds that covalently modify XPO1 were recently discovered and are exciting new compounds to implement this strategy. Selinexor, the clinical lead SINE, has made progress in Phase I/II clinical trials and is generally well tolerated, but limited to twice weekly dosing, with supportive care. The discovery of novel SINE compounds with improved tolerability is therefore of considerable clinical interest and represents a significant contribution beyond the targeted therapies currently available for hematologic malignancies and a variety of other cancers where upregulation of XPO1 is observed. Presented herein is the discovery of KPT-8602, the next generation SINE compound that shows lower brain penetration, improved tolerability allowing continuous dosing, and improved efficacy beyond any current XPO1 inhibitor. Results: Our crystallography data revealed that KPT-8602 binds covalently to XPO1 through a Michael acceptor that is activated by an electron withdrawing pyrimidyl moiety, allowing a 2-fold increased reversible interaction with XPO1 compared to earlier SINE compounds. The crystal structure of the KPT-8602-XPO1 complex showed interactions between XPO1 and the activating pyrimidyl group. In vitro pull-downs using immobilized GST-nuclear export sequences and purified recombinant XPO1 demonstrated greater reversible binding of KPT-8602 compared to KPT-330 (selinexor). In vivo toxicology studies demonstrated that KPT-8602 possesses lower brain penetration compared to KPT-330 allowing for continuous dosing and improved tolerability. Our results also showed that KPT-8602 induced a comparable level of cytotoxicity as well as inhibition of cell proliferation compared to KPT-330 in primary CLL tumors and in a representative panel of DLBCL cell lines. Furthermore, KPT-8602 inhibited proliferation and induced apoptosis in AML cell lines and primary AML blasts while inducing nuclear accumulation of p53 and NPM1. We hypothesized that these improved pharmacological parameters would allow daily KPT-8602 to abrogate disease progression in CLL and AML animal models. The Eµ-TCL1-C57BL/6 transplant model of CLL was used to evaluate the therapeutic benefit of continuous dosing of KPT-8602. Eµ-TCL1-engrafted mice were treated with KPT-8602 given daily or 2x/week. The KPT-8602 daily cohort had significantly improved survival with a median overall survival of 70 vs 50 days (vs vehicle 33 days), compared to those treated only 2x/week with KPT-8602 (p=0.001). Mice treated with KPT-330 2x/week showed a similar survival to mice treated with KPT-8602 2x/week. Mice given daily KPT-8602 had significantly smaller spleens and reduced circulating leukemic cells compared to all the other groups (p 〈 0.001 for all comparisons). We recently showed the combination of KPT-330 and ibrutinib (bruton tyrosine kinase inhibitor) increases survival compared to ibrutinib alone in Eµ-TCL1-engrafted mice. We therefore tested the effect of KPT-330+ibrutinib or KPT-8602+ibrutinib in a cohort of Eµ-TCL1-engrafted mice compared to any agent alone. Notably, the combination of KPT-8602 to ibrutinib was able to further improve the survival induced by KPT-330+ibrutinib (p=0.008). We next assessed the activity of KPT-8602 in a human leukemia xenograft model of AML where NOD/SCID γ mice were inoculated with MV4-11 cells obtained from spleens of primary MV4-11 xenografts. Recipient mice given KPT-8602 5x/week showed strikingly better outcomes with a median survival of 58 vs 35 days compared to KPT-8602 2x/week (p 〈 0.0001) and KPT-330 2x/week (p 〈 0.0001). Conclusion: Consistent with the in vitro finding of a two-fold enhanced reversibility of XPO1-KPT-8602 binding and lower brain penetration, our data indicate that KPT-8602 allows a prolonged frequent dosing schedule, which leads to an excellent therapeutic benefit and less toxicity in animal models of CLL and AML. These data suggest that KPT-8602 represents a new treatment paradigm and warrants further evaluation in clinical trials of patients with hematologic malignancies, particularly in combination with ibrutinib or other second generation Btk inhibitors. Disclosures Baloglu: Karyopharm Therapeutics Inc.: Employment, Equity Ownership. Shacham:Karyopharm: Employment, Equity Ownership. Kauffman:Karyopharm: Employment, Equity Ownership. Byrd:Acerta Pharma BV: Research Funding. Chook:Karyopharm Therapeutics Inc.: Consultancy.
    Type of Medium: Online Resource
    ISSN: 0006-4971 , 1528-0020
    URL: Article
    DOI: 10.1182/blood.V126.23.317.317
    RVK:
    XA 33000
    RVK:
    XA 10000
    Language: English
    Publisher: American Society of Hematology
    Publication Date: 2015
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  • 5
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    Follistatin and Endoglin: Potential Biomarkers of Endothelial Damage and Non-Relapse Mortality after Myeloablative Allogeneic Hematopoietic Cell Transplantation in Blood and Marrow Transplant Clinical Trials Network (BMT CTN) 0402
    American Society of Hematology ; 2016
    In:  Blood Vol. 128, No. 22 ( 2016-12-02), p. 63-63
    Details
    In: Blood, American Society of Hematology, Vol. 128, No. 22 ( 2016-12-02), p. 63-63
    Abstract: Introduction: Inflammation and angiogenesis are linked biologic processes influencing the onset and recovery of acute graft-versus-host disease (aGVHD) after allogeneic hematopoietic cell transplantation (HCT). In aGVHD, angiogenic factors (AF) contributing to tissue healing/repair (e.g. epidermal growth factor [EGF]) versus AF associated with tissue damage/inflammation (e.g. follistatin [FS] ) exist in a dysregulated balance. Whether these AF are associated with, or predictive of, non-relapse mortality (NRM) in the absence of aGVHD, is not understood. Given that regimen-related tissue injury plays a role in NRM, we hypothesized that elevated levels of inflammation-associated AF early after HCT would be associated with NRM even in patients without aGVHD. Methods: We studied plasma samples from patients enrolled on Blood and Marrow Transplant Clinical Trials Network (BMT CTN) aGVHD prophylaxis study 0402, a randomized trial of tacrolimus/methotrexate vs tacrolimus/sirolimus after matched sibling peripheral blood stem cell transplantation with myeloablative conditioning. Levels of AF (angiopoietin-2 [Ang2], EGF, FS, vascular endothelial growth factor [VEGF] -A and -B, endoglin [sEng], placental growth factor [PlGF] , and soluble VEGF receptor [sVEGFR]-1 and -2) were quantified by MILLIPLEX magnetic bead panels. We analyzed factors associated with NRM in univariate analysis and used multivariate analysis to develop composite AF scores to predict NRM. In calculating the composite scores, we extrapolated the individual probabilities of NRM based upon regression models, and sorted the individual probabilities into 3 composite scores based on: 1) estimated probability of NRM 〈 10%, 2) probability of NRM between 10-19%, 3) probability of NRM 〉 20%. Results: 221 patients from BMT CTN 0402 had pre-transplant plasma samples and samples at day +28 available for analysis. Univariate analysis showed associations of raw levels of Ang2, FS, sEng, and sVEGFR1 on day +28 with NRM. Of these, only higher levels of log-transformed FS (p=0.01) and of sEng (p=0.04) showed a correlation with NRM; these two AF were selected for the final model. In multivariate analysis, patients with the highest levels of day +28 FS and sEng (score 3, n=32, Figure) had a 4.6-fold higher relative risk (RR) of NRM (95% confidence interval 1.7-12.3, p 〈 0.01, Table). The prognostic value of the composite score was stronger than either individual factor alone (RR log[FS]=2.1, p=0.03, and RR log[sEng] =2.3, p=0.07). Grade III-IV aGVHD and patient age 〉 50 years were also independently associated with 1-year NRM. There was no effect of patient gender, disease status, CMV serostatus, or type of GVHD prophylaxis (tacrolimus/methotrexate versus tacrolimus/sirolimus) on NRM. There was no significant effect of the composite score, grade III-IV aGVHD, or age on the competing risk of relapse. FS and sEng measured before HCT were not associated with 1-year NRM (p=0.91 and p=0.62, respectively). There was only a weak correlation between the day 0 and day 28 FS and sEng (Spearman's rho 0.36 and 0.38, respectively). Among the 221 cohort patients, there were 25 deaths due to NRM, including 5 deaths occurring prior to day 56. Death was more likely to be from organ toxicity in patients with composite score 3 (5/9, 56%) vs those with a composite score of 1 (1/8, 12%) or 2 (3/8, 37%). Conclusions: A composite score using day 28 plasma levels of FS and sEng predicts the risk of 1-year NRM after HCT, providing further evidence that endothelial dysfunction is a relevant biological problem in HCT. Pre-HCT measurements of FS and sEng were not associated with NRM, suggesting that elevations in these factors may reflect susceptibility to regimen-related toxicity. We have previously shown that elevated levels of FS and sEng at the onset of aGVHD are associated with poor survival. Here, we show that these factors are predictive of NRM independent of aGVHD. Follistatin modulates inflammatory responses following tissue injury via interaction with the transforming growth factor β superfamily and may reflect endothelial cell damage. sEng is upregulated in proliferating endothelial cells, in inflammation and tissue ischemia, and can influence leukocyte adhesion and endothelial transmigration. Measurement of these predictive AF may highlight prospective opportunities to intervene and prevent subsequent complications thereby limiting NRM after allogeneic HCT. Disclosures No relevant conflicts of interest to declare.
    Type of Medium: Online Resource
    ISSN: 0006-4971 , 1528-0020
    URL: Article
    DOI: 10.1182/blood.V128.22.63.63
    RVK:
    XA 33000
    RVK:
    XA 10000
    Language: English
    Publisher: American Society of Hematology
    Publication Date: 2016
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  • 6
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    Allele Level HLA Matching On Outcomes After Double Umbilical Cord Blood (dUCB) Transplantation for Hematological Malignancies: Stronger Graft Vs. Leukemia with HLA Mismatch
    American Society of Hematology ; 2012
    In:  Blood Vol. 120, No. 21 ( 2012-11-16), p. 1976-1976
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    In: Blood, American Society of Hematology, Vol. 120, No. 21 ( 2012-11-16), p. 1976-1976
    Abstract: Abstract 1976 Multiple single center and registry reports have documented the critical impact of donor-recipient HLA match on engraftment, transplant-related mortality (TRM) and survival after umbilical cord blood (UCB) transplantation. However, nearly all reports have only considered HLA A and B at antigen level and HLA DRB1 at allele level typing without consideration of HLA C or DQ. Therefore, we retrospectively performed allele level HLA typing for HLA-A, B, C, DRB1, DQB1 for UCB donor-recipient pairs in order to assess the importance of high resolution HLA typing on transplant outcomes. After 2002, most patients received a dUCB transplant in order to achieve the desired cell doses of ≥3, ≥4 and ≥5 × 10e7 NC/kg for grafts that were HLA 6/6, 5/6 and 4/6 matched by original typing resolution, respectively. Therefore, the analysis was limited to 275 recipients of dUCBT for hematological malignancy and whom DNA from both units was available. The effect of HLA match was based on the HLA type of the predominant long term engrafting unit. The median recipient age and weight was 44 years (range, 0.6–69) and 76.9 kg (range, 7.1–148), respectively. Conditioning was myeloablative (40%) consisting of cyclophosphamide (CY) 120 mg/kg, fludarabine (FLU) 75 mg/m2 and total body irradiation (TBI) 1320 cGy, or non-myeloablative (60%) consisting of CY 50 mg/kg, FLU 200 mg/m2, TBI 200 cGy with 95% receiving cyclosporine A (CsA) and mycophenolate mofetil (MMF) immunosuppression. Patients had acute leukemia (62%), standard risk disease (62%), cytomegalovirus seropositive (59%), and received at least one UCB unit that was sex mismatched to the recipient (78%). Results reported are based on the long-term predominant UCB unit. Notably, survival was not adversely affected by HLA mismatch. The probability of survival at 5 years was 46% (95%CI, 33–58%), 47% (95%CI, 38–54%) and 29% (95%CI, 13–47%) in patients engrafting with a 3–5/10, 6–8/10 and 9–10/10 HLA-matched UCB grafts, respectively (p=.47). In multivariable analysis after adjusting for disease risk, CMV serostatus, and KPS, there was similar risk of overall mortality for all groups regardless of HLA matching level. All other transplant outcomes including the incidence of acute and chronic GVHD were similar for all HLA-matching groups (data not shown). In the subset with acute leukemia (n=174), however, greater HLA mismatch was associated with a significantly lower risk of relapse without a deleterious effect on risk of TRM, resulting in a benefit in LFS (inverse of treatment failure) as shown below. Transplant Outcome for Acute Leukemia HLA 3–5/10 match (n=84) RR (95%CI), p-value HLA 6–8/10 match (n=168) RR (95%CI), p-value HLA 9–10/10 match (n=34) RR (95%CI), p-value TRM at 2 years 1.0 1.1 (0.6–2.4)
 P=.73 1.1 (0.6–2.4)
 P=.73 Leukemia Relapse 1.0 1.9 (0.9–4.3)
 P=.11 3.5 (1.3–9.5)
 P=.01 Treatment failure 1.0 1.4 (0.8–2.4)
 P=.19 2.2 (1.1–4.2)
 P=.02 Together these data indicate that UCB units with greater HLA mismatch may confer greater GVL effect without greater TRM compared to HLA better-matched UCB grafts. These results suggest importance of evaluating allele level HLA typing in the setting of dUCB transplantation. If confirmed, these results could have major implications not only on graft selection (ie avoidance of HLA matched units), but also the target size of the international UCB banking inventory. Disclosures: No relevant conflicts of interest to declare.
    Type of Medium: Online Resource
    ISSN: 0006-4971 , 1528-0020
    URL: Article
    DOI: 10.1182/blood.V120.21.1976.1976
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    Language: English
    Publisher: American Society of Hematology
    Publication Date: 2012
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  • 7
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    Promising Progression Free and Overall Survival Using a Novel (CY/FLU/TBI) Reduced-Intensity Conditioning (RIC) Regimen for Allogeneic Sibling Stem Cell Transplantation (SCT).
    American Society of Hematology ; 2006
    In:  Blood Vol. 108, No. 11 ( 2006-11-16), p. 2999-2999
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    In: Blood, American Society of Hematology, Vol. 108, No. 11 ( 2006-11-16), p. 2999-2999
    Abstract: RIC regimens permit older and less fit patients to receive allogeneic stem cell transplantation (SCT). We designed a novel RIC regimen (cyclophosphamide, fludarabine, TBI [CY/FLU/TBI]) to achieve sufficient anti-neoplastic potency for cytoreduction and adequate immunosuppression for engraftment yet have limited treatment related mortality (TRM). We report the results of 72 patients (58% male) receiving sibling donor HLA-identical (n=66; 92%) or single antigen mismatched (n=6; 8%) G-CSF mobilized peripheral blood SCT from 2002–2005. Eligible patients were 〉 55 years or had prior SCT, ongoing but controlled infections, ventricular ejection fraction 35–45% or corrected DLCO 30–50%. All patients had chemotherapy sensitive disease or remission. Most patients had lymphoma (n=29; 40%) or acute leukemia/MDS (n=23; 32%); others (28%) had multiple myeloma, CML, CLL, aplastic anemia, or renal cell carcinoma. All acute leukemia patients were in CR (CR1=14, ≥CR2=4). All lymphoma patients were chemosensitive; 4 were in CR. All patients received conditioning with FLU 40 mg/m2/day × 5 days, CY 50 mg/kg and 200 cGy TBI. Equine ATG 90 mg/kg plus methylprednisolone were given to those without recent combination chemotherapy (29%). GVHD prophylaxis included mycophenolate mofetil 1 gm BID and cyclosporine. The median age was 55 years (range, 11–65). The median graft cell dose infused was 5.4 × 106 CD34+ cells/kg (range, 0.6–15.5). Seventeen (24%) had previous SCT (14 autologous, 3 allogeneic). Neutrophil engraftment occurred at a median of 7 days (range, 0–13) and median time to platelet recovery 〉 20K and 〉 50K was 9 days (range, 0–51) and 14 days (range, 0–68), respectively. Median bone marrow chimerism by day 28 was 100% (range, 50–100); only 11 patients were 〈 90%. The cumulative incidence (95% CI) of Grade 2–4 acute GVHD was 47% (35–59) and Grade 3–4 acute GVHD was 24% (14–33). Chronic GVHD at 2 years was 48% (34–62). Treatment related mortality at 100 days and 1 year was low [100 day (95% CI): 11% (4–18%); 1 year: 17% (8–25)]. Causes of death (n=29) included relapse (52%), GVHD (21%), organ toxicity (24%), and fungal infection (3%). The cumulative incidence (95% CI) of relapse/progression for all patients was 37% (25–49) at 2 years [acute leukemia/MDS, 47% (24–71); lymphoma, 37% (18–55)] . After a median 29 months (range, 6–48) follow-up of survivors, progression-free (PFS) and overall (OS) survival were encouraging: [PFS: 1 year, 51% (39–62); 3 years, 43% (31–55); OS: 1 year 68% (57–79); 3 years, 58% (45–70)]. Importantly, almost no events (relapse or death) have occurred beyond 2 years yielding a plateau in PFS and OS. This novel CY/FLU/TBI conditioning regimen is well tolerated, effective, and associated with promising PFS and OS. Further application and testing in multi-center studies is warranted. Figure Figure
    Type of Medium: Online Resource
    ISSN: 0006-4971 , 1528-0020
    URL: Article
    DOI: 10.1182/blood.V108.11.2999.2999
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    Language: English
    Publisher: American Society of Hematology
    Publication Date: 2006
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    Monocyte Subpopulation Recovery and Outcomes Following Hematopoietic Cell Transplantation
    American Society of Hematology ; 2016
    In:  Blood Vol. 128, No. 22 ( 2016-12-02), p. 2232-2232
    Details
    In: Blood, American Society of Hematology, Vol. 128, No. 22 ( 2016-12-02), p. 2232-2232
    Abstract: Introduction: Monocyte recovery following allogeneic hematopoietic cell transplantation (allo-HCT) has previously been correlated with improved overall survival (OS). Three distinct monocyte subpopulations have been identified based on CD14 and CD16 surface expression, including: CD14+CD16++ (non-classical), CD14+CD16+ (intermediate), and CD14++CD16- (classical). Among these subpopulations, non-classical monocytes have greater capacity to produce inflammatory cytokines, whereas classical monocytes have phagocytic activity, are less inflammatory and produce counter regulatory cytokines (i.e., IL-10), and intermediate monocytes are a transitionary population sharing features of both non-classical and classical monocytes. To date, there has not been a direct comparison between stem cell source and monocyte recovery, nor has there been an analysis of monocyte subpopulation recovery and HCT outcomes. We hypothesized that recovery of monocytes and their subpopulations would vary based on stem cell source and that recovery of the monocyte subpopulations would be associated with clinical outcomes. Methods: This analysis included individuals who underwent a first allo-HCT at the University of Minnesota between 2010-2014 and who enrolled onto an institutional immune reconstitution protocol. Absolute monocyte count (AMC), as well as the absolute counts of non-classical, intermediate and classical monocyte subpopulations were assessed at days 28, 60, 100 and 365 post-HCT. Optimal cut points of each monocyte subpopulation at day 28 were calculated using the Contal and OQuigley method and were used for analysis. This time point was selected because the outcomes of interest were unlikely to have occurred prior to this time. Individuals who experienced acute graft versus host disease (aGVHD) prior to day 28 were excluded from the aGVHD analysis (n=39). Patient demographics, disease and treatment characteristics were included in univariable analyses to determine associations between monocyte subpopulations and transplant outcomes, including 2-year OS, 1-year transplant related mortality (TRM), 2-year disease free survival (DFS), 2-year relapse, 180-day aGVHD and chronic GVHD. Factors with P-values 〈 0.15 were included in multivariable models. Results: Among 318 individuals with available day 28 data, median age at HCT was 38 years, and median follow up was 531 days. Conditioning was myeloablative for 45% and reduced intensity for 55%. Stem cell source was: BM (n=80), PBSC (n=79), single UCB (SUCB) (n=54) and double UCB (DUCB) (n=105). Although monocyte subpopulation recovery did not differ across stem cell sources at day 28, AMC, classical and intermediate monocyte recovery was greater among UCB recipients compared to other stem cell sources at days 60, 100 and 365 (Table). In multivariable models, after controlling for each monocyte subpopulation, stem cell source, disease and treatment characteristics, an absolute classical monocyte count of 〉 /= 0.25x 109/L at day 28 was associated with improved OS (HR=0.33, 95% CI 0.12-0.86, P=0.02) (Figure) and DFS (HR=0.36, 95% CI 0.15-0.85, P=0.02). Absolute numbers of non-classical monocytes 〉 /=0.02 x 109/L at day 28 was associated with decreased rates of grade II-IV aGVHD (HR=0.58, 95% CI 0.34-0.99, P=0.04) and decreased cGVHD (HR=0.48, 95% CI 0.26-0.90, P=0.02). None of the day 28 monocyte subpopulation counts were associated with TRM or relapse. Conclusions: Monocyte recovery differs among stem cell sources. UCB recipients experience more robust monocyte recovery, specifically within the intermediate and classical monocyte subpopulations, at day 60 and at all measured time points beyond, compared to other stem cell sources. Early monocyte recovery is associated with HCT outcomes. Increased classical monocyte count at day 28 is independently associated with improved OS and DFS. Paradoxically, despite their inflammatory properties, increased non-classical monocyte count predicts decreased acute and chronic GVHD within this large series of patients. If reproduced, these findings could allow for enhanced outcome prediction models and could lead to novel interventions to improve transplant outcomes. Disclosures Cooley: Fate Therapeutics: Research Funding. Miller:Oxis Biotech Scientific Advisory Board: Membership on an entity's Board of Directors or advisory committees.
    Type of Medium: Online Resource
    ISSN: 0006-4971 , 1528-0020
    URL: Article
    DOI: 10.1182/blood.V128.22.2232.2232
    RVK:
    XA 33000
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    XA 10000
    Language: English
    Publisher: American Society of Hematology
    Publication Date: 2016
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  • 9
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    Validation of Amphiregulin As a Monitoring Biomarker during Treatment of Life-Threatening Acute Gvhd: A Secondary Analysis of 2 Prospective Clinical Trials
    American Society of Hematology ; 2021
    In:  Blood Vol. 138, No. Supplement 1 ( 2021-11-05), p. 259-259
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    In: Blood, American Society of Hematology, Vol. 138, No. Supplement 1 ( 2021-11-05), p. 259-259
    Abstract: Background: Patients with life-threatening acute graft-versus-host disease (aGVHD) often have severe symptoms related to organ/tissue damage, elevated blood biomarkers of aGVHD, or both. Monitoring such patients can be challenging due to unpredictable variations in symptoms that may not be related to aGVHD pathogenesis, such as dietary changes, medication side effects, or infections. In our previously published phase 1 study of urinary-derived human chorionic gonadotropin/epidermal growth factor (uhCG/EGF) for the treatment of life-threatening aGVHD (NCT02525029), we recognized amphiregulin (AREG) as a potential GVHD monitoring biomarker that is elevated at the start of treatment and decreases in patients who respond to treatment. Here we show the results of AREG as a monitoring biomarker in our larger uhCG/EGF treated cohort and validate them in an independent cohort of patients with steroid-refractory aGVHD receiving ruxolitinib as second-line therapy in the REACH1 study. Methods: Longitudinal plasma samples were cryopreserved at study baseline and on study Days 7, 14, 28, and 56 from patients enrolled in both NCT02525029 (N=51) and REACH1 (N=60). In samples collected during NCT02525029, AREG was measured using enzyme-linked immunosorbent assay (R & D Systems, Minneapolis, MN), and ST2 and REG3a were measured using a multiplex Luminex-based array (R & D Systems). Samples from REACH1 were analyzed for concentrations of AREG, ST2, and REG3a using the ProteinSimple Ella platform (Bio-Techne, San Jose, CA). Comparisons of biomarker concentrations between response groups were performed using nonparametric one-way analysis of variance (Kruskal-Wallis test). Analyses of change of biomarkers from baseline to subsequent study days were performed using nonparametric matched pairs analysis (Wilcoxon signed rank test). Biomarker cutoffs relevant for overall survival at study baseline were identified using recursive partitioning on the NCT02525029 dataset and tested in the REACH1 dataset. Results: In patients with a complete response (CR) at Day 28 to uhCG/EGF, AREG decreased 3-fold from baseline to Day 56 (mean, 98 vs 32 pg/mL, P=0.006, Figure 1A). AREG did not significantly change over time in patients with a partial response (PR) or no response (NR) to uhCG/EGF. Similarly, in patients with a Day 28 CR to ruxolitinib, AREG decreased 2.8-fold from baseline to Day 56 (mean, 174.7 vs 63.6 pg/mL, P=0.007, Figure 1B). AREG also decreased 2.0-fold over time in patients treated with ruxolitinib who had a PR to treatment (mean baseline 288.2 vs 146.1 pg/mL at Day 56, P=0.017) but no change in those with progressive disease (PD). ST2 declined with CR, but to a lesser extent, over time in patients with a CR in both studies (1.4-fold decrease in NCT02525029, P=0.04 and 2.2-fold decrease in REACH1, P=0.021). REG3a did not significantly change over time in responders in either clinical trial. Biomarker cutoffs associated with a rapidly fatal course were identified in NCT02525029 for AREG ( & gt;212 pg/mL associated with a median survival of 62 days, P=0.006, Figure 1C), ST2 ( & gt;292 ng/mL associated with a median survival of 239 days, P & lt;0.001), and REG3a ( & gt;13.5 ng/mL associated with a median survival of 416 days, P=0.01). These cutoffs were not statistically significant in REACH1, although patients with a baseline AREG & gt;212 pg/mL had a median survival of 165 days vs not reached (P=0.1, Figure 1D) in REACH1. Conclusions: Using samples collected during 2 prospective clinical trials on 2 different measurement platforms, we conclude that AREG is a useful longitudinal monitoring biomarker for patients with life-threatening aGVHD. AREG levels were generally higher in REACH1 than NCT02525029, which could reflect differences in assay, severity of illness, or both. Patients with a high baseline AREG are at high risk of early death and should be monitored on a consistent platform during serial assessments. Figure 1 Figure 1. Disclosures Pratta: Incyte: Current Employment. Betts: Patent Disclosures: Patents & Royalties: B.C.B. holds a patent (WO2015120436A2) related to CD4+ T cell pSTAT3 as a marker and therapeutic target of acute GVHD. B.C.B. additionally holds a provisional patent (WO2017058950A1) related to the use of JAK inhibitors for rejection and GVHD prevention. . Galvin: Incyte: Current Employment. MacMillan: Equilium: Other: DSMB member; Incyte: Consultancy; Jazz Pharmaceuticals: Consultancy. Weisdorf: Fate Therapeutics: Research Funding; Incyte: Research Funding. Holtan: Generon: Consultancy; Incyte: Consultancy, Research Funding. OffLabel Disclosure: uhCG/EGF has orphan drug designation for the treatment of acute GVHD
    Type of Medium: Online Resource
    ISSN: 0006-4971 , 1528-0020
    URL: Article
    DOI: 10.1182/blood-2021-150867
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    XA 33000
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    Language: English
    Publisher: American Society of Hematology
    Publication Date: 2021
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  • 10
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    Alternative Donor Hematopoietic Cell Transplantation for Patients with Fanconi Anemia.
    American Society of Hematology ; 2012
    In:  Blood Vol. 120, No. 21 ( 2012-11-16), p. 3081-3081
    Details
    In: Blood, American Society of Hematology, Vol. 120, No. 21 ( 2012-11-16), p. 3081-3081
    Abstract: Abstract 3081 Hematopoietic cell transplantation (HCT) is the only proven curative therapy for the hematological abnormalities in patients with Fanconi anemia (FA). In the mid-1990s, survival after alternative donor (AD)-HCT was reported to be 18% with excessive rates of regimen-related toxicity, graft failure, graft-versus-host-disease (GVHD) and opportunistic infections (OI). Between 1990 and 2010, 127 FA patients underwent AD-HCT at the University of Minnesota using one of 5 consecutive, prospective phase I-II total body irradiation (TBI) containing clinical trials, representing the largest single center experience. All patients received cyclophosphamide (CY, 40 mg/kg) and single fraction TBI. Sequential changes were made to prevent GVHD, graft failure and OI and ultimately enhance survival; in 1994, all patients received T cell depleted (TCD) bone marrow (BM) or umbilical cord blood (UCB) to reduce GVHD; in 1999, fludarabine (FLU) was added to enhance engraftment; in 2003, thymic shielding (TS) was added to reduce OI risk; and in 2006, TBI dose reduction was evaluated to reduce toxicity. Over this time period, HLA-matched unrelated donor BM was the donor of choice with partially HLA matched BM and UCB only used as alternatives. Neutrophil recovery was twice as likely after FLU-containing regimens than non-FLU containing regimens and was not deleteriously affected by TS or reducing TBI dose to 300cGy. Grade II-IV acute GVHD was significantly reduced by the use of TCD (18%) compared to T replete BM or UCB (50% and 38%, respectively: p 〈 0.01). Similarly, chronic GVHD was significantly lower with TCD BM (9%) vs T replete BM or UCB (25% and 15%, respectively; p=0.04). For the entire cohort of 127 patients, the probability of survival was 61% at 1 year and 54% at 5 years with a median follow-up of 9 years. Mortality was higher in recipients who were older ( 〉 10 years) or CMV seropositive, received any transfusions before HCT, or developed OI before HCT (Table). Mortality was lowest using CY/FLU/ATG, TBI 300 cGy with TS (Trial 5, relative risk [RR] 0.1; p 〈 0.01). For 10 patients on Trial 5 who had no prior history of transfusions or OI, incidences of neutrophil and platelet are 100% and 100%, acute and chronic GVHD 17% and 0%, and probability of survival is 92%. Table: Factors associated with 3 year mortality: Multivariate analysis Factors Relative Risk of Mortality (95% CI) P-value Trial*     2: CY/ATG/TBI 450-600, CSA/MP 1.0     3: CY/FLU/ATG/TBI 450, CSA/MP 0.3 (0.1–.7) 〈 0.01     4: CY/FLU/ATG/TBI 450+TS, CSA/MP 0.2 (0.1–0.7) 0.01     5: CY/FLU/ATG/TBI 300+TS, CSA/MP or MMF 0.1 (0.04–0.3) 〈 0.01 Donor Type     Matched URD Marrow 1.0     Mismatched URD Marrow 0.3 (0.1–0.8) 〈 0.01     Mismatched RD Marrow 0.3 (0.1–2.3) 0.22     Single or Double UCB 2.0 (0.9–4.6) 0.08 Age at Transplant      〈 10 years 1.0     10–17 years 2.4 (1.2–5.0) 0.01     18+ years 3.1 (1.4–7.0) 〈 0.01 Prior OI     None 1.0     Yes 3.2 (1.5–6.9) 〈 0.01 Prior Transfusions     None     Yes 2.4 (1.0–5.8) 0.05 CMV Serostatus     Patient negative/donor negative 1.0     Patient negative/donor positive 1.5 (0.7–3.4) 0.34     Patient positive 2.2 (1.1–4.3) 0.03 * Trial 1 (CY/TBI 450, MTX/MP or CSA) was excluded as there were only 8 patients in this group and a number of demographic and disease factors were unknown. Substantial progress has been made in the successful application of AD-HCT for FA. These data support the urgency of transplant prior to the onset of severe pancytopenia when risk of OI and transfusions are more likely, particularly when a suitable BM donor is available. While other regimens are being explored, CY/FLU/ATG/TBI300 with TS should be considered a new standard of care for FA patients undergoing AD-HCT. Disclosures: No relevant conflicts of interest to declare.
    Type of Medium: Online Resource
    ISSN: 0006-4971 , 1528-0020
    URL: Article
    DOI: 10.1182/blood.V120.21.3081.3081
    RVK:
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    XA 10000
    Language: English
    Publisher: American Society of Hematology
    Publication Date: 2012
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