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A Phase I Dose Escalation Trial of Donor T Cells Sensitized with Pentadecapeptides of the CMV-pp65 Protein for the Treatment of CMV Infections Following Allogeneic Hematopoietic Stem Cell Transplants.

Koehne, Guenther ; Doubrovina, Ekaterina ; Hasan, Aisha ; [weitere]

American Society of Hematology ; 2009

In: Blood Vol. 114, No. 22 ( 2009-11-20), p. 2262-2262

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In: Blood, American Society of Hematology, Vol. 114, No. 22 ( 2009-11-20), p. 2262-2262

Kurzfassung: Abstract 2262 Poster Board II-239 We have developed a novel alternative method of generating donor-derived T-cell lines specific for CMV-pp65 peptides for use in adoptive immunotherapy. In this approach, 138 pentadecapeptides (15-mers), with 11 amino acid overlaps spanning the entire 561 amino acid sequence of the CMV protein pp65 were synthesized and manufactured under conditions ensuring their purity and sterility for application in clinical trials. A pool of the 138 pentadecapeptides is loaded onto monocyte-derived dendritic cells derived from seropositive donors and the same donor's T cells are sensitized under GMP conditions. In our preclinical studies, we have been able to generate CMV-pp65 specific T-cell lines from each seropositive donor tested, irrespective of HLA genotype. During the culture period of 21-28 days, populations of T cells specific for CMV-pp65 selectively expanded 200-300 fold while T cells reactive against major or minor alloantigens were depleted. Currently, 9 patients (pts) with persistent/refractory CMV antigenemia, one pt with CMV pneumonia diagnosed four weeks after treatment, have been treated using cells manufactured by this method on a clinical trial approved by the FDA. One pt was treated on a single patient IND prior to final FDA approval; 8 pts were enrolled onto the clinical trial - 3 pts at a T cell dose of 5×105/kg; 3 pts at dose level II of 1×106/kg and 2 pts at dose level III of 2×106/kg. We report here the results of the first 7 pts, (the 2 latter pts are too early in treatment to be included at time of abstract admission). CMV specific CTLs were generated from HLA-identical unrelated donors (3 pts) or from HLA-identical siblings (6 pts) for 2 pts who underwent non-myeloablative conventional and 7 pts who received myeloablative T-cell depleted allogeneic transplants. Pts were eligible if they had persistent CMV antigenemia despite treatment with antiviral drugs or had toxicities precluding further treatment with antiviral agents. Prior to infusion, the T cells were tested to be CMV specific by cytotoxicity, intracellular Interferon gamma (IFN-g) production and MHC-tetramer staining (if available). Cells were also assayed to establish lack of alloreactivity, microbiological sterility and low endotoxin levels. The cytotoxic T cells demonstrated cytolytic activity against peptide-loaded autologous PHA blasts, but exhibited no cytotoxicity against non-pulsed HLA-matched or pulsed HLA-mismatched target cells. The HLA-restriction and the specific pp65-derived epitopes of the CMV-specific T-cells were characterized prior to the infusion. CMV-specific frequencies of the CD8+ cells measured by intracellular IFN-g or MHC tetramers ranged from 2 -70%. Post infusion, an increase in the absolute lymphocyte count correlated with an increase in CMV-specific T-cell frequencies to levels as high as 12% of CD8+ cells. These persisted for at least 7 months (10% of CD8+ cells) following the infusion. Notably, the same pp65-derived epitopes and their HLA-restrictions, which characterized the pre-infusion CTLs were detected in the pt specimens post infusion. Freshly isolated T cells from the blood of HLA-A*0201 positive pts obtained 3 months post infusion showed significant lysis of CMV infected and peptide-pulsed MRC-5 fibroblasts, while non infected/pulsed fibroblasts and pulsed HLA-mismatched targets were not lysed. Three of the treated pts exhibited an HLA-A*0201 as well as HLA-B*0701 allele. In all three pts, epitope-specific T cells for the HLA-A*0201 restricted NLVPMVATV peptide and the B*0701 restricted RPHERNGFTV peptide were detected and monitored in pre and post infusion T-cell populations. All 7 pts who were treated for persistent CMV antigenemia tolerated treatment well. None developed early signs or symptoms of GvHD at the dose levels tested. Six of the 7 pts cleared CMV viremia by 2-4 weeks following the T-cell infusions. One of the pts died six weeks after the CTL infusion of respiratory failure despite clearing CMV from blood and bronchial aspirates. The one pt who remained viremic following the CTL infusion continued on oral Valgancyclovir and subsequently became CMV antigen negative. The clearance of CMV antigenemia was preceded by an initial spike of CMV antigenemia and/or CMV PCR in all pts. These results from the first 7 pts on this trial indicate that donor T cells sensitized with this pool of synthetic overlapping CMV pp65 15-mers are safe and clear CMV viremia resistant to standard therapy. Disclosures: No relevant conflicts of interest to declare.

Materialart: Online-Ressource

ISSN: 0006-4971 , 1528-0020

URL: Article

DOI: 10.1182/blood.V114.22.2262.2262

RVK:

XA 33000

RVK:

XA 10000

Sprache: Englisch

Verlag: American Society of Hematology

Publikationsdatum: 2009

ZDB Id: 1468538-3

ZDB Id: 80069-7

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Off-the-shelf EBV-specific T cell immunotherapy for rituximab-refractory EBV-associated lymphoma following transplantation

Prockop, Susan ; Doubrovina, Ekaterina ; Suser, Stephanie ; [weitere]

American Society for Clinical Investigation ; 2020

In: Journal of Clinical Investigation Vol. 130, No. 2 ( 2020-1-6), p. 733-747

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In: Journal of Clinical Investigation, American Society for Clinical Investigation, Vol. 130, No. 2 ( 2020-1-6), p. 733-747

Materialart: Online-Ressource

ISSN: 0021-9738 , 1558-8238

URL: Article

DOI: 10.1172/JCI121127

DOI: 10.1172/JCI121127DS1

DOI: 10.1172/JCI121127DS2

Sprache: Englisch

Verlag: American Society for Clinical Investigation

Publikationsdatum: 2020

ZDB Id: 2018375-6

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Disease-Free Survival After Cord Blood (CB) Transplantation Is Not Different to That After Related or Unrelated Donor Transplantation in Patients with Hematologic Malignancies.

Ponce, Doris ; Zheng, Junting ; Gonzales, Anne Marie ; [weitere]

American Society of Hematology ; 2009

In: Blood Vol. 114, No. 22 ( 2009-11-20), p. 2296-2296

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In: Blood, American Society of Hematology, Vol. 114, No. 22 ( 2009-11-20), p. 2296-2296

Kurzfassung: Abstract 2296 Poster Board II-273 CB transplantation (CB-T) may be curative for patients with high-risk or advanced hematologic malignancies. However, given there are no randomized trials comparing survival after CBT with the more traditional approach of matched related donor transplantation (MRD-T) or unrelated donor transplantation (URD-T), how CB-T compares to MRD-T and URD-T transplantation is not established. Therefore, we conducted a retrospective study comparing survival after CB-T (n=67) with MRD-T (n=96) and URD-T (n=163) performed 10/05-3/09 for the treatment of hematologic malignancies. Our hypothesis was that 1 year survival is comparable between hematopoietic stem cell (HSC) sources. Consecutive adult and pediatric recipients of first allograft for the treatment of acute leukemia in remission (CR1-3), myelodysplasia (MDS, ≤5% blasts at work-up), or non-Hodgkins or Hodgkin lymphoma were eligible for analysis. The median age of CB-T recipients (37 years, range & lt;1-66) was not different to that of MRD-T (46 years, range & lt;1-71) and URD-T (47 years, range 1-71) recipients (p=0.151). A lower percentage of CB-T recipients (n=36, 54%) had acute leukemia or MDS as compared to 69 (72%) MRD-T and 116 (71%) URD-T recipients (p=0.022), and a lower percentage received ablative conditioning (n=47, 70%) as compared to 81 (84%) MRD-T and 141 (87%) URD-T recipients (p & lt;0.001). While MRD grafts were HLA-identical, URD grafts were 8-10/10 HLA-allele matched (99 10/10, 47 9/10, 17 8/10). CB grafts were 4-6/6 HLA-A,-B antigen, DRB1 allele matched, with all CBT recipients receiving double unit grafts (median infused TNC larger unit 2.57 × 107/kg; smaller unit 1.93 × 107/kg) to augment engraftment. GVHD prophylaxis was calcineurin inhibitor based in 67 (100%) of CB-T but only 37 (39%) of MRD-T and 52 (32%) of URD-T recipients, with remaining patients receiving T cell depleted grafts. Median follow-up of survivors is 22 months (range 5-46) and was similar between HSC sources. We found no difference in the cumulative incidence (CI) of transplant-related mortality (TRM) at day 100 between HSC sources: 15% (95%CI: 6-24) in CB-T as compared to 7% (95%CI: 2-13) for MRD-T and 10% (95%CI: 5-14) for URD-T recipients (p=0.742). Further, there was no difference in the CI of relapse at 1 year: 19% (95%CI: 9-29) in CB-T as compared to 16% (95%CI: 9-24) for MRD-T and 16% (95%CI: 10-22) for URD-T recipients (p=0.930). Finally, by log-rank analysis there was no significant difference between HSC sources for either overall survival (p=0.778) or disease-free survival (DFS, p=0.381, Figure 1). While outcomes within subgroups could differ according to HSC source as well as donor-recipient HLA-match, recipient co-morbidities, diagnosis, disease risk, conditioning intensity, and GVHD prophylaxis, this encouraging preliminary data supports the use of double unit CB grafts as an alternative HSC source in patients lacking suitably HLA-matched peripheral blood HSC or marrow donors. Disclosures: No relevant conflicts of interest to declare.

Materialart: Online-Ressource

ISSN: 0006-4971 , 1528-0020

URL: Article

DOI: 10.1182/blood.V114.22.2296.2296

RVK:

XA 33000

RVK:

XA 10000

Sprache: Englisch

Verlag: American Society of Hematology

Publikationsdatum: 2009

ZDB Id: 1468538-3

ZDB Id: 80069-7

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Clofarabine, Melphalan, and Thiotepa, Followed by Allogeneic Unmodified Bone Marrow or Peripheral Blood Stem Cell Transplant, by Unmodified Double Cord Blood Transplant, or by CD34+ T-Cell Depleted Stem Cell Transplant for the Treatment of Hematologic Malignancies.

Boulad, Farid ; Koehne, Guenther ; Kernan, Nancy A. ; [weitere]

American Society of Hematology ; 2012

In: Blood Vol. 120, No. 21 ( 2012-11-16), p. 3144-3144

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In: Blood, American Society of Hematology, Vol. 120, No. 21 ( 2012-11-16), p. 3144-3144

Kurzfassung: Abstract 3144 Based on encouraging results with the use of clofarabine (CLO) for reinduction treatment of acute leukemias, we have developed two allograft protocols for patients with hematologic malignancies with a cytoreductive regimen, using CLO in combination with melphalan (Mel) and thiotepa (Thio). Patients on protocol #1 received unmodified bone marrow (BMT), peripheral blood stem cells (PBSCT), or unmodified double unit cord blood (dCBT). Patients on protocol #2 received CD34+ T-cell depleted stem cells (TCD-SCT). Cytoreduction consisted of CLO 20 mg/m2/day × 5, Thio 10 mg/Kg/day × 1 and Mel 70 mg/m2/day × 2. Graft-versus-host disease (GvHD) prophylaxis consisted of tacrolimus (Tacro) and methotrexate (MTX) with unmodified BMT or PBSCT, tacro and mycophenolate mofetil (MMF) with unmodified dCBT, and none with TCD-SCT. Rabbit ATG at 2.5 mg/Kg × 2 or 3 doses was used for the prevention of rejection with the TCD-SCT. To date, 64 pts were treated with this regimen including: unmodified BMT/PBSCT 27 patients, dCBT 15 patients, and TCD-SCT 22 patients. The median age for patients was 10.2 years (range 0.9–58.7) for unmodified SCT and 41.5 (range 0.6–67.2) for TCD-SCT. This was the second SCT for 13 of 27 pts in the BMT-PBSCT group, 2 of 15 pts in the CBT group, and 4 of 22 pts in the TCD group. Patient diagnoses included acute lymphoblastic leukemia (ALL) (N=36), acute myelogenous leukemia (AML) (N=23), and myelodysplastic syndrome (MDS) (N=5). Patients with ALL or AML in first remission (CR1) or CR2 and MDS in CR1 or refractory anemia (RA) were categorized as having good risk disease (GRD), while all other pts were considered to have poor risk disease (PRD), irrespective of all other factors. There were 15 of 27 pts with PRD in the BMT/PBSCT group, 10 of 15 pts in the CBT group, and 9 of 22 pts in the TCD-SCT group. For the unmodified BMT/PBSCT group, donors were HLA-matched related (N=11), mismatched related (N=1), matched unrelated (N=12), or mismatched unrelated (N=3). All CBT recipients received double-unit grafts from 2 mismatched unrelated donors. For the TCD-SCT group, donors were HLA-matched related (N=8), mismatched related (N=1), matched unrelated (N=4), or mismatched unrelated (N=9). Engraftment occurred in 59 of 61 evaluable pts; three pts died before engraftment. One pt recipient of unmodified BMT/PBSCT suffered a late graft failure, and one pt recipient of CBT suffered an early graft failure in the context of sepsis. Grade 2–4 acute GvHD occurred in 8/26 (31%) evaluable pts in the BMT/PBSCT group, 5/13 (38%) evaluable pts in the CBT group, and 4/20 (20%) evaluable pts in the TCD-SCT group. With a median follow-up of 20.5 months for the unmodified SCT groups and 15.4 months for the TCD group, the overall survival (OS) and disease-free survival (DFS) rates were: 53.7% and 41.0% for the BMT/PBSCT group, 51.3% and 41.5% for the CBT group, and 64.1% and 60.7% for the TCD-SCT group. This cytoreductive regimen represents a promising approach for the transplantation of patients with acute leukemias without the use of total body irradiation. This regimen is also sufficiently immunosuppressive to insure consistent engraftment of T-cell depleted transplants. Lastly, it appears to be relatively well tolerated for younger pts requiring a second SCT. Disclosures: Off Label Use: Clofarabine.

Materialart: Online-Ressource

ISSN: 0006-4971 , 1528-0020

URL: Article

DOI: 10.1182/blood.V120.21.3144.3144

RVK:

XA 33000

RVK:

XA 10000

Sprache: Englisch

Verlag: American Society of Hematology

Publikationsdatum: 2012

ZDB Id: 1468538-3

ZDB Id: 80069-7

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Adoptive Immune Cell Therapy Using Third Party T-Cell Donors In the Treatment of EBV Related Diseases In Immunodeficient Recipients

Prockop, Susan ; Doubrovina, Ekaterina ; Boulad, Farid ; [weitere]

American Society of Hematology ; 2010

In: Blood Vol. 116, No. 21 ( 2010-11-19), p. 487-487

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In: Blood, American Society of Hematology, Vol. 116, No. 21 ( 2010-11-19), p. 487-487

Kurzfassung: Abstract 487 Adoptive transfer of donor-derived EBV-specific T-cells can induce complete and durable regressions of EBV lymphomas complicating allogeneic hematopoietic progenitor cell transplants (HSCT). However, this treatment has not been broadly applicable due to 1) lack of immediate access to such T-cells and 2) lack of adequate donor cells to generate the virus-specific T-cells required, either because of donor unavailability (e.g. cord blood or some unrelated donors) or seronegativity. To address this we have developed a bank of EBV-specific cells of defined HLA restriction, and are now evaluating the potential of these HLA-partially matched, third party EBV-specific T-cells. We here report results for the first 13 patients treated by this approach, including pts who developed clonal EBV lymphomas following HLA matched (n=2) or disparate (n=1) T-cell depleted HSCT (N=3) or HLA-disparate cord blood transplants (N=3); pts with chemotherapy refractory EBV PTLD (n=2) or EBV+ leiomyosarcomas (LS) (n=3) complicating organ transplants (N=5) and pts with EBV+ CNS lymphomas complicating AIDS or prolonged immunosuppression (N=2). These patients received infusions of third party EBV-CTLs after the failure of a median of 2 prior therapies (0 – 4) including rituximab in all but one case. Three patients had also failed prior infusions with autologous (1) or HSCT donor (2) EBV-CTLs. T-cells from consenting EBV seropositive HLA typed normal donors were sensitized in vitro for at least 28 days with irradiated autologous EBV BLCL transformed with the EBV strain B95.8, and were then tested for sterility virus-specificity and lack of alloreactivity and stored cryopreserved prior to use. The donors were selected based on matching for at least 2 HLA alleles and in most instances, known restriction of the EBV-specific T-cells for epitopes presented by HLA alleles shared by the EBV+ malignancy. Up to 4 courses of T-cells were administered in 3 weekly I.V. infusions of 1 × 106 T cells/kg, each course separated by a 3 week observation period. T cell infusions were well tolerated. One patient developed minor skin GvHD. No other patient developed GVHD or organ allograft rejection. Results for the 13 pts are summarized in Table 1. Those pts achieving CR, PR or SD had rapid increments in the frequencies of EBV CTLP detected that persisted 14–21 days after each course. Of the 4 pts with PD, none exhibited increases in the frequency of EBV CTLPs in the blood post T-cell infusion. No increase in EBV CTLPs was observed in a patient who progressed after treatment with EBV-specific T-cells from his haplotype disparate HSCT donor. In this case, the donor's EBV-specific T-cells were restricted by an HLA allele not shared by the host-type lymphoma. This patient was then treated with EBV-specific T-cells from a third party donor restricted by an HLA allele shared by the host-type lymphoma. These T-cells expanded post infusion, resulting in a durable CR. Overall, 9 of 13 survive either in CR or sustained PR or SD 〉 6 to 〉 60 months post treatment. These results provide evidence that third party EBV-specific T-cells, that are partially HLA-matched, and appropriately HLA restricted can induce regressions of EBV-associated lymphomas, PTLD and LS complicating transplantation or prolonged immunodeficiency. A bank of such T-cells can provide an immediately accessible source of T-cells for adoptive therapy for a large proportion of patients developing these life threatening disorders. N CR PR SD PD Survival EBV+ Lymphoma Post HSCT or CBT 6 4 0 0 2 4 in CR EBV+ PTLD Post Organ Transplant 2 0 1 0 1 1 in PR EBV+ CNS Lymphoma in Immunodeficiency 2 1 0 0 1 1 in CR EBV+ Leiomyosarcoma Post Transplant 3 0 1 2 0 3 in PR or SD 13 5 3 2 4 9 Disclosures: No relevant conflicts of interest to declare.

Materialart: Online-Ressource

ISSN: 0006-4971 , 1528-0020

URL: Article

DOI: 10.1182/blood.V116.21.487.487

RVK:

XA 33000

RVK:

XA 10000

Sprache: Englisch

Verlag: American Society of Hematology

Publikationsdatum: 2010

ZDB Id: 1468538-3

ZDB Id: 80069-7

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A Phase I-II Dose Escalation Trial of Clofarabine Plus Melphalan and Thiotepa Followed by Unmodified Allogeneic Stem Cell Transplant (SCT) for the Treatment of High Risk or Advanced Acute Leukemia

Boulad, Farid ; Kernan, Nancy A ; Prockop, Susan E ; [weitere]

American Society of Hematology ; 2010

In: Blood Vol. 116, No. 21 ( 2010-11-19), p. 2354-2354

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In: Blood, American Society of Hematology, Vol. 116, No. 21 ( 2010-11-19), p. 2354-2354

Kurzfassung: Abstract 2354 High-risk or advanced acute leukemias are associated with poor outcome even with the use of stem cell transplantation (SCT) with or without total body irradiation (TBI). Based on encouraging results with the use of clofarabine (CLO) for reinduction treatment of acute leukemias, we have developed a phase I/II protocol using this agent with melphalan (Mel) and thiotepa (Thio) followed by unmodified SCT for the treatment of patients (pts) with high-risk (HR) leukemias. To date, 28 consecutive pts were treated on, or as per protocol, with 26 pts evaluable for follow-up. There were 15 males and 11 females aged 1–58 years (median 5.3 years). Cytoreduction consisted of CLO at dose level I of 20 mg/m2/day × 5 days (n=23) or at dose level II of 30 mg/m2/day × 5 (n=3), Thio 10 mg/Kg/day × 1 day and Mel 70 mg/m2/day × 2 days. Graft-versus-host disease (GvHD) prophylaxis consisted of tacrolimus and mycophenolate mofetil (MMF), or tacrolimus and methotrexate. Twenty pts had acute lymphoblastic leukemia (ALL) in complete remission (CR1; n=5), CR2 (n=5), CR3 (n=9), or relapse (n=1). Five pts had acute myeloid leukemia (AML), in CR1 (n=1), CR2 (n=2), or CR3 (n=2). One pt had myelodysplastic syndrome (MDS) in RAEB. For the pts with ALL in CR1, very HR features included: Infant MLL (N=2), Philadelphia (Ph1) chromosome (N=2) and Induction failure (N=1). For the pts with ALL in CR2, HR features included: Infant MLL (N=1), 2nd SCT (N=1), Ph1 and 2nd SCT (N=2), while 1 pt had prior CNS infarcts precluding the use of TBI. The one pt with AML in CR1 had M7-AML. This was a first SCT for 14 pts, a 2nd SCT for 11 pts and 3rd SCT for 1 pt, with time from previous SCT to the present one being 5–73 months (median 11.3 mo) for those 12 pts. Donors were HLA-matched siblings (n=8), HLA matched unrelated donors (n=8), or HLA mismatched unrelated donors (N=10). Stem cell grafts were bone marrow (n=12), peripheral blood (n=7) or double cord blood (n=7) stem cells. Twenty four of the 26 evaluable pts engrafted, while 2 pts died prior to engraftment. Toxicity of the SCT cytoreduction included elevation of hepatic transaminases in 17 of 26 evaluable pts (AST elevation of 5–19 fold and ALT elevation of 7–16 fold), with a subsequent normalization in all pts. Mucositis was mostly at acceptable grade 1–2 levels. Two pts developed a syndrome of renal and hepatic insufficiency leading to hepatic veno-occlusive disease (VOD) (1 pt at each of the 2 dose levels). Non-relapse mortality included: VOD (N=2), infections (N=3), treatment related sarcoma, a malignancy secondary to the irradiation received with a prior transplant (N=1). With a follow-up of 3–57 mos (median 21 mos), 15 of the 26 pts are alive, disease-free. Five pts relapsed and 4 died subsequently of disease, while 6 pts died of non-relapse morality. Overall (OS) and disease-free survival (DFS) at 2 years were both 58%. DFS was 56% for pts 〉 18 years and 53% for pts 〈 18 years (p =0.36); it was 64% for recipients of a first HSCT and 41% (p=0.97) for recipients of a second or third HSCT. Five pts (4 recipients of unrelated donor SCT; 3 from mismatched donors) developed Grade 2–4 acute GvHD. Four of these pts went on to develop chronic GvHD. Immune reconstitution was rapid; for the evaluable pts, it included absolute CD4 counts 〉 200 cells/L at 1–3 mos for 15 pts and at 4–8 mos for 4 pts. This cytoreductive regimen represents a promising approach for the transplantation of patients with high risk acute leukemias. It was well tolerated for pts requiring a second SCT and is also associated with rapid immune recovery. Ultimately, a large scale study would need to be done to determine if this approach could offer equal or superior results to TBI containing regimens for ALL or AML. Disclosures: No relevant conflicts of interest to declare.

Materialart: Online-Ressource

ISSN: 0006-4971 , 1528-0020

URL: Article

DOI: 10.1182/blood.V116.21.2354.2354

RVK:

XA 33000

RVK:

XA 10000

Sprache: Englisch

Verlag: American Society of Hematology

Publikationsdatum: 2010

ZDB Id: 1468538-3

ZDB Id: 80069-7

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