Your search keyword '"Prentice, H. G."' showing total 114 results

1. The risk of early and late CMV DNAemia associated with Campath use in stem cell transplant recipients.

Author

Buyck, H. C., Prentice, H. G. F., Griffiths, P. D., and Emery, V. C.

Subjects

STEM cell transplantation, CYTOMEGALOVIRUSES, PATIENTS, RADIOTHERAPY, DISEASE risk factors

Abstract

The risks associated with in vivo and ex vivo use of Campath-1H and -1G in a cohort of 206 stem cell transplant recipients for human CMV (HCMV) DNAemia have been quantified. DNAemia showed a biphasic incidence pattern with an inflexion at day 60. The first phase had a linear risk rate for HCMV DNAemia of 0.3% per day, whereas the second phase had a substantially lower risk rate of 0.058% per day. In multivariable analyses, risk factors for early DNAemia were HCMV serostatus, radiotherapy-based conditioning and CD34 stem cell dose, with the use of in vivo Campath-1H having the most significant risk (hazards ratio=3.68; 95% CI=2.02–6.72; P<0.001). Ex vivo use of Campath was not associated with an increased risk for HCMV DNAemia. Patients receiving either in vivo Campath-1H or -1G experienced HCMV DNAemia earlier (27 and 33 days, respectively) compared with patients receiving no Campath (time to DNAemia, 51 days; P=0.0006). Multivariable analysis of risk factors for HCMV DNAemia occurring beyond 100 days after transplant were older age, acute GVHD>grade II and a lower CD34 stem cell dose, whereas Campath-1H use was not associated with late HCMV DNAemia. [ABSTRACT FROM AUTHOR]

Published

2010

2. A study to determine the safety profile and maximum tolerated dose of micafungin (FK463) in patients undergoing haematopoietic stem cell transplantation.

Author

Sirohi, B., Powles, R. L., Chopra, R., Russell, N., Byrne, J. L., Prentice, H. G., Potter, M., and Koblinger, S.

Subjects

ANTIFUNGAL agents, PHARMACODYNAMICS, DRUG administration, STEM cell transplantation, HEMATOPOIETIC stem cells, NEUTROPENIA, DRUG dosage

Abstract

This open-label, dose-escalation study assessed the maximum tolerated dose (MTD) of the new antifungal micafungin in patients undergoing haematopoietic stem cell transplantation (HSCT). Participants received 3, 4, 6 or 8 mg/kg/day micafungin intravenously from 7 days to a maximum of 28 days or until neutropaenia resolved. The MTD was defined as the highest dose not causing the same Grade 3 or 4 adverse event in three or more patients. All 36 participants received 8 days treatment for a median of 18 days (range: 8–28); 1 patient withdrew consent and a further 11 discontinued to receive another systemic antifungal agent for a suspected infection. No case of confirmed invasive fungal infection occurred. Adverse events were those expected for patients undergoing HSCT and showed no evidence of dose-related toxicity. Criteria for MTD were not met; no patient had a Grade 3 or 4 adverse event considered causally related to micafungin. Thus, the MTD of micafungin can be inferred to be 8 mg/kg/day or higher.Bone Marrow Transplantation (2006) 38, 47–51. doi:10.1038/sj.bmt.1705398; published online 22 May 2006 [ABSTRACT FROM AUTHOR]

Published

2006

3. Validation and Clinical Application of Molecular Methods for the Identification of Molds in Tissue.

Author

Paterson, P. J., Seaton, S., McHugh, T. D., McLaughlin, J., Potter, M., Prentice, H. G., and Kibbler, C. C.

Subjects

TISSUE culture, MYCOSES, MOLECULAR biology, INFECTION, PATIENTS, BIOMOLECULES

Abstract

Background. Invasive fungal infections due to less-common molds are an increasing problem, and accurate diagnosis is difficult. Methods. We used our previously established molecular method, which allows species identification of molds in histological tissue sections, to test sequential specimens from 56 patients with invasive fungal infections who were treated at our institution from 1982 to 2000. Results. The validity of the method was demonstrated with the establishment of a molecular diagnosis in 52 cases (93%). Confirmation of the causative organism was made in all cases in which a mold had been cultured from the tissue specimen. Less-common molds were identified in 7% of cases and appear to be an increasing problem. Conclusions. Our previously established method has proven to be of value in determining the incidence of invasive infection caused by less-common molds. Institutions should continue to pursue diagnosis of invasive fungal infections by means of tissue culture and microbiologic analysis. [ABSTRACT FROM AUTHOR]

Published

2006

4. Factors affecting reconstitution of the T cell compartment in allogeneic haematopoietic cell transplant recipients.

Author

Fallen, P R, McGreavey, L, Madrigal, J A, Potter, M, Ethell, M, Prentice, H G, Guimarães, A, and Travers, P J

Subjects

T cells, HEMATOPOIETIC stem cell transplantation, THYMUS, GRAFT versus host disease, IMMUNODEFICIENCY

Abstract

Summary:The factors affecting T cell reconstitution post haematopoietic cell transplantation (HCT) are not well characterised. We carried out a longitudinal analysis of T cell reconstitution in 32 HCT recipients during the first 12 months post transplant. We analysed reconstitution of naïve, memory and effector T cells, their diversity and monitored thymic output using TCR rearrangement excision circles (TRECs). Thymic-independent pathways were responsible for the rapid reconstitution of memory and effector T cells less than 6 months post HCT. Thymic-dependent pathways were activated between 6 and 12 months in the majority of patients with naïve T cell numbers increasing in parallel with TREC levels. Increasing patient age, chronic GVHD and T cell depletion (with or without pretransplant Campath-1H) predicted low TREC levels and slow naïve T cell recovery. Furthermore, increasing patient age also predicted high memory and effector T cell numbers. The effects of post HCT immunosuppression, total body irradiation, donor leucocyte infusions, T cell dose and post HCT infections on T cell recovery were also analysed. However, no effects of these single variables across a variety of different age, GVHD and T cell depletion groups were apparent. This study suggests that future analysis of the factors affecting T cell reconstitution and studies aimed at reactivating the thymus through therapeutic intervention should be analysed in age-, GVHD- and TCD-matched patient groups.Bone Marrow Transplantation (2003) 32, 1001-1014. doi:10.1038/sj.bmt.1704235 [ABSTRACT FROM AUTHOR]

Published

2003

5. Identification of non-naïve CD4+CD45RA+ T cell subsets in adult allogeneic haematopoietic cell transplant recipients.

Author

Fallen, P R, Duarte, R F, McGreavey, L, Potter, M, Ethell, M, Prentice, H G, Madrigal, J A, and Travers, P J

Subjects

HEMATOPOIETIC stem cells, TRANSPLANTATION of organs, tissues, etc., T cell receptors, PHENOTYPES, HOMEOSTASIS

Abstract

Summary:The study of thymic-dependent pathways of T cell reconstitution in T cell replete haematopoietic cell transplant (HCT) recipients in previous studies was complicated by the transfer of naïve CD4+CD45RA+ T cells with the stem cell graft. However, direct quantification of thymic output has been enabled by measurement of T cell receptor excision circles (TREC). We analysed T cell reconstitution using T cell phenotyping and TREC quantification in 12 T cell-replete HCT recipients 6-53 years of age during the first 12 months post transplant. We have identified a novel subpopulation of CD4+CD45RA+ T cells in the peripheral blood of these HCT recipients with expansions of this subset being more pronounced in older recipients. The recovery of classical naïve CD4+CD45RA+ T cells was dependent on thymic output whereas this novel CD4+CD45RA+ subpopulation arose independently of thymic output and displayed effector function and phenotype. These results suggest that CD4+CD45RA+ effector populations exist, similar to the CD8+CD45RA+ effector subset, and that the CD45RA antigen should not be used alone to define naïve CD4+ T cells when monitoring T cell reconstitution in T cell replete HCT recipients. Furthermore, these results raise important questions regarding the role of the thymus in regulating T cell homeostasis in older HCT recipients and normal individuals.Bone Marrow Transplantation (2003) 32, 609-616. doi:10.1038/sj.bmt.1704185 [ABSTRACT FROM AUTHOR]

Published

2003

6. Acute myeloid leukaemia cells secrete a soluble factor that inhibits T and NK cell proliferation but not cytolytic function – implications for the adoptive immunotherapy of leukaemia.

Author

Orleans-Lindsay, J. K., Barber, L. D., Prentice, H. G., and Lowdell, M. W.

Subjects

ACUTE myeloid leukemia, T cells, KILLER cells, LYMPHOCYTES

Abstract

Evidence of an immune mediated graft-versus-leukaemia effect has led to the belief that T and NK cell based adoptive immunotherapy can constitute effective treatment for relapsed leukaemias. However, work on solid tumours has shown this strategy may be hampered, by an immune escape mechanism in which tumour secreted immunosuppressive factors compromise T and NK cell function. Indeed, acute myeloid leukaemia (AML) cells secrete immunosuppressive factors that block the synthesis of Th1 type cytokines in T cells. We demonstrate here that this immunosuppression, mediated by both HL60 AML cell line and primary AML blasts, inhibits T and NK cell proliferation but not cytolytic activity. Supernatants from HL60 cell line and primary AML blasts inhibited T cell proliferation to mitogenic and alloantigen stimulation but had no effect on cytolytic function. Similarly, the proliferation of NK cells to IL-2 and IL-15 stimulation was inhibited whilst their cytolytic function, shown by lysis of AML blasts, K562 and Daudi cells remained unaffected. The failure of T and NK cells to proliferate was not due to effector cell apoptosis. Indeed, removal of lymphocytes from the immunosuppressive environment partially restored their capacity to respond to mitogenic stimulation. T cells exposed to immunosuppressive supernatants did not increase expression of mitotic inhibitory proteins that arrest cell division, thereby ruling this out as a mechanism of operation for this immunosuppression. T cell expansion requires antigen stimulation, usually provided in the form of AML blasts, therefore our data suggest that NK cells may be more practical for the immunotherapy of AML. [ABSTRACT FROM AUTHOR]

Published

2001

7. Treatment of relapse after allogeneic bone marrow transplantation with reduced intensity conditioning (FLAG ± Ida) and second allogeneic stem cell transplant.

Author

Pawson, R., Potter, M. N., Theocharous, P., Lawler, M., Garg, M., Yin, J. A. Liu, Rezvani, K., Craddock, C., Rassam, S., and Prentice, H. G.

Subjects

STEM cell transplantation, BONE marrow transplantation, DISEASE relapse

Abstract

Acute leukaemias in relapse after allogeneic stem cell transplantation (SCT) respond poorly to donor leucocyte infusions (DLI) compared with chronic myeloid leukaemia (CML), at least in part because of faster disease kinetics. Fludarabine-containing ‘non-myeloablative’ chemotherapy followed by further allo SCT may offer more rapid and effective disease control. We report 14 patients with relapse after allo SCT for acute leukaemia [seven acute myeloid leukaemia (AML), five acute lymphoblastic leukaemia (ALL)] or refractory anaemia with excess blasts in transformation (RAEB-t, n = 2) treated with fludarabine, high-dose cytosine arabinoside (ara-C) and granulocyte colony-simulating factor (G-CSF) with (n = 10) or without (n = 2) idarubicin (FLAG ± Ida) or DaunoXome (FLAG-X) (n = 2) and second allo SCT from the original donor. Donors were fully human leucocyte antigen (HLA) -matched in 13 cases with a single class A mismatch in one. Actuarial overall survival was 60% and disease-free survival was 26% at 58 months. Remissions after the second SCT were longer than those after the first bone marrow transplantation (BMT) in eight of the 13 assessable patients to date. Haematopoietic recovery was rapid. Transplants were well tolerated with no treatment-related deaths. The major complication was graft-versus-host disease (GvHD, acute >= grade II-2 cases, chronic – eight cases, two limited, six extensive) although there have been no deaths attributable to this. FLAG ± Ida and second allo SCT is a safe and useful approach and may be more effective than DLI in the treatment of acute leukaemias relapsing after conventional allo SCT. [ABSTRACT FROM AUTHOR]

Published

2001

8. Intravenous Itraconazole Followed by Oral Itraconazole in the Treatment of Invasive Pulmonary Aspergillosis in Patients with Hematologic Malignancies, Chronic Granulomatous Disease, or AIDS.

Author

Caillot, D., Bassaris, H., McGreer, A., Arthur, C., Prentice, H. G., Seifert, W., and De Beule, K.

Subjects

TRIAZOLES, PULMONARY aspergillosis, MYCOSES, DRUG efficacy, THERAPEUTICS

Abstract

Determines the efficacy and safety of intravenous or oral dosing regimen of the triazole antifungal drug itraconazole in the treatment of pulmonary aspergillosis in immunocompromised patients. Incidence of invasive fungal infection at autopsy in patients with hematologic malignancies; Percentage of patients who showed complete or partial response to itraconazole treatment; Adverse events in itraconazole treatment.

Published

2001

9. Heterogeneity of VH-JH gene rearrangement patterns: an insight into the biology of B cell precursor ALL.

Author

Moreira, I, Papaioannou, M, Mortuza, F Y, Gameiro, P, Palmisano, G L, Harrison, C J, Prentice, H G, Mehta, A B, Hoffbrand, A V, and Foroni, L

Subjects

LYMPHOBLASTIC leukemia, IMMUNOGLOBULINS, CELL proliferation, CELL metabolism, B cell lymphoma, CELLS, CHROMOSOME abnormalities, CHROMOSOMES, COMPARATIVE studies, CYTOGENETICS, GENETICS, LONGITUDINAL method, RESEARCH methodology, MEDICAL cooperation, POLYMERASE chain reaction, RESEARCH, DISEASE relapse, EVALUATION research, TREATMENT effectiveness, SEQUENCE analysis

Abstract

Oligoclonal B cell proliferation, as defined by the presence of more than one leukemic clone, has been detected in approximately 20% to 30% of patients with acute lymphoblastic leukemia (ALL) using PCR or Southern blotting. An accurate assessment of these populations is required to avoid false negative measurements of minimal residual disease (MRD) in follow-up bone marrow (BM) samples of ALL patients. In this study, we analysed 29 ALL patients with two or more immunoglobulin heavy (IGH) chain gene rearrangements in the presentation samples using IGH fingerprinting PCR and sequence analysis. Thirty-nine (51%) of 76 sequences (from 15 patients), shared no VNDNJ homology (ie different CDR3 regions). In the remaining 14 patients, at least two related VH sequences were identified in each patient (identical DNJ sequences). Numerical abnormalities of chromosome 14 was detected in 10 patients. Eight patients were analysed at presentation and relapse. In four of them, expansion of a minor presentation-clone was detected at relapse while the major presentation clone disappeared, confirming 'subclonal evolution'. Finally, in our cohort of patients, the presence of related or unrelated IGH clones did not influence overall survival. [ABSTRACT FROM AUTHOR]

Published

2001

10. The combination of oral amphotericin B with azoles prevents the emergence of resistant Candida species in neutropenic patients.

Author

Paterson, P. J., McWhinney, P. H. M., Potter, M., Kibbler, C. C., and Prentice, H. G.

Subjects

AMPHOTERICIN B, CANDIDIASIS treatment, CANDIDA

Abstract

The role of antifungal prophylaxis remains controversial and concerns exist that the use of azoles may potentiate the emergence of resistant Candida species. We used a strategy of combining the latest azole/triazole with oral amphotericin B to reduce this risk. We analysed data on Candida colonization and candidaemia in neutropenic patients from four prophylaxis periods (1985/6: ketoconazole and amphotericin B suspension; 1991/2 & 1997: fluconazole and amphotericin B suspension; 1998/9: itraconazole) to look for evidence of the emergence of potentially resistant species. Overall, the percentage of patients colonized with Candida fell significantly (69·3%, 57·5%, 43·2% and 46%, respectively, P < 0·001) due to a decrease in colonization with C. albicans (49%, 23·1%, 22·2% and 25·2%, respectively, P < 0·001). However, in 1998/9, increased colonization, particularly with C. glabrata in the lower gastrointestinal tract, was noted to coincide with the omission of oral amphotericin B. Despite an increasing population of ‘high risk’ patients, the incidence of candidaemia has not changed significantly (2%, 1·4%, 1·2% and 2% respectively). However, species causing candidaemia have changed, with resistant organisms now predominating. Our findings support the use of azole prophylaxis although, in view of the trends noted when itraconazole was used alone, we would recommend the additional use of oral amphotericin B. [ABSTRACT FROM AUTHOR]

Published

2001

11. Defibrotide for the treatment of hepatic veno-occlusive disease: results of the European compassionate-use study.

Author

Chopra, R., Eaton, J. D., Grassi, A., Potter, M., Shaw, B., Salat, C., Neumeister, P., Finazzi, G., Iacobelli, M., Bowyer, K., Prentice, H. G., and Barbui, T.

Subjects

DNA, LIVER diseases, VEIN diseases, THERAPEUTICS

Abstract

Severe hepatic veno-occlusive disease (VOD) is a recognized complication of autologous and allogeneic stem cell transplantation (SCT) that is often fatal. Defibrotide (DF) is a polydeoxyribonucleotide that has been found to have anti-thrombotic, anti-ischaemic and thrombolytic properties without causing significant anticoagulation. Preliminary studies have demonstrated activity for DF in the treatment of VOD, with minimal associated toxicity. In the present study, 40 patients who fulfilled established criteria for VOD were treated with DF on compassionate grounds in 19 European centres; 28 patients met risk criteria predicting progression of VOD and fatality or had evidence of multiorgan failure (MOF), and were defined as ‘poor-risk’. DF was commenced intravenously at a median of 14 d (range, -2 d to 53 d) post SCT at doses ranging from 10 to 40 mg/kg. The median duration of therapy was 18 d (range, 2–71 d). Twenty-two patients showed a complete response (CR) (bilirubin < 34·2 μmol/l and resolution of signs/symptoms of VOD and end-organ dysfunction) [CR = 55%, confidence interval (CI) 40–70%] and 17 patients (43%) are alive beyond d +100. Ten poor-risk patients showed a complete response (CR = 36%, CI 21–51%). These results demonstrate that DF is an active treatment for VOD following SCT and a randomized trial is now underway in order to further evaluate its role. [ABSTRACT FROM AUTHOR]

Published

2000

12. Is there a graft-versus-leukaemia effect in the absence of graft-versus-host disease in patients undergoing bone marrow transplantation for acute leukaemia?

Author

Ringdén, O., Labopin, M., Gorin, N. C., Schmitz, N., Schaefer, U. W., Prentice, H. G., Bergmann, L., Jouet, J. P., Mandelli, F., Blaise, D., Fouillard, L., and Frassoni, F.

Subjects

BONE marrow transplant complications, GRAFT versus host disease, LEUKEMIA, FAMILIAL diseases

Abstract

During a 13-year period, 5200 autografts, 1039 HLA-identical sibling transplants without acute or chronic graft-vs.-host disease (GVHD) and 67 twins were reported to the European Group for Blood and Marrow Transplantation EBMT. Follow-up time was a median of 32 months. Diagnoses were acute myeloid leukaemia (AML, 4521) and acute lymphoblastic leukaemia (ALL, 1785) in first complete remission. The probability of relapse at 5 years was 51 ± 1% in the autografts, 45 ± 8% in the twins and 34 ± 2% among the HLA-identical siblings (auto vs. sibs, P < 0·0001). In multivariate analyses, the following factors were significantly associated with an increased risk of relapse: ALL vs. AML M3 [relapse rate (RR) 2·29, P < 0·0001], AML non-M3 vs. AML M3 (RR 1·8, P < 0·0001), autograft vs. sibling transplant (RR 1·76, P < 0·0001), interval diagnosis to transplantation < 261 d (RR 1·45, P < 0·001) and other conditioning vs. total body irradiation (RR 1·16, P = 0·001). Transplant-related mortality was the same in the three groups at approximately 10% at 2 years. Five-year leukaemia-free survival was 42 ± 1% in the autografts, 44 ± 8% in the twins and 58 ± 2% among the siblings (auto vs. sibs, P < 0·0001). The factors significant for relapse were also significant in multivariate analyses for leukaemia-free survival. In addition, children had a significantly better leukaemia-free survival than adults (RR 0·82, P < 0·0001). Recipients of bone marrow from HLA-identical siblings without GVHD had a lower risk of relapse and a better leukaemia-free survival than recipients of autografts. This may be as a result of a graft-vs.-leukaemia effect in the absence of GVHD. [ABSTRACT FROM AUTHOR]

Published

2000

13. Management of Invasive Pulmonary Aspergillosis in Hematology Patients: A Review of 87 Consecutive...

Author

Yeghen, T., Kibbler, C. C., Prentice, H. G., Berger, L. A., Wallesby, R. K., McWhinney, P. H. M., Lampe, F. C., and Gillespie, S.

Subjects

PULMONARY aspergillosis, FUNGAL lung diseases

Abstract

Reports on the identification of patients with hematologic malignancies and invasive pulmonary aspergillosis (IPA) between 1982 and 1995. Positive predictive value for IPA as shown by the presence of lesion with imaging suggestive of aspergillosis; Association of relapsed hematologic disease with death.

Published

2000

14. Malignant neoplasms in long-term survivors of bone marrow transplantation. Late Effects Working Party of the European Cooperative Group for Blood and Marrow Transplantation and the European Late Effect Project Group.

Author

Kolb, H.J., Socie, Gerard, Socié, G, Duell, T, Van Lint, M T, Tichelli, A, Apperley, J F, Nekolla, E, Ljungman, P, Jacobsen, N, van Weel, M, Wick, R, Weiss, M, and Prentice, H G

Subjects

BONE marrow transplant complications, TUMOR diagnosis, CYCLOSPORINE, DRUG side effects

Abstract

Background: Patients who receive bone marrow transplants have increased risk for new malignant conditions because of several risk factors, including conditioning with radiation and chemotherapy, immune stimulation, and malignant primary disease. The occurrence of and risk factors for malignant neoplasm in long-term survivors must be assessed.Objective: To determine the risk and define potential risk factors for new malignant conditions in long-term survivors after marrow transplantation.Design: Retrospective multicenter study.Setting: Study of the Late Effects Working Party with 45 transplantation centers cooperating in the European Cooperative Group for Blood and Marrow Transplantation.Patients: 1036 consecutive patients who underwent transplantation for leukemia, lymphoma, inborn diseases of the hematopoietic and immune systems, or severe aplastic anemia. Transplantation was done before December 1985, and patients had survived more than 5 years.Measurements: Reports on malignant neoplasms were evaluated, and the incidence was compared to that in the general population. Patient age and sex, primary disease and status at transplantation, histocompatibility of the donor, conditioning regimen, type of prophylaxis of graft-versus-host disease, development of acute and chronic graft-versus-host disease, and treatment of chronic graft-versus-host disease were evaluated as variables.Results: Median follow-up since transplantation was 10.7 years (range, 5 to 22.1 years). Malignant neoplasms were seen in 53 patients; the actuarial incidence (+/- SE) was 3.5% +/- 0.6% at 10 years and 12.8% +/- 2.6% at 15 years. The rate of new malignant disease was 3.8-fold higher than that in an age-matched control population (P < 0.001). The most frequent malignant diseases were neoplasms of the skin (14 patients), oral cavity (7 patients), uterus (including cervix) (5 patients), thyroid gland (5 patients), breast (4 patients), and glial tissue (3 patients). Median age of patients and their donors was 21 years. Malignant neoplasms were more frequent in older patients and in patients with chronic graft-versus-host disease. Older patient age and treatment of chronic graft-versus-host disease with cyclosporine were significant risk factors for new malignant neoplasms after bone marrow transplantation.Conclusions: The spectrum of neoplasms and immunosuppressive treatment with cyclosporine for chronic graft-versus-host disease as dominant risk factors indicate that immunosuppression is the major cause of malignant neoplasms in patients receiving marrow transplants. [ABSTRACT FROM AUTHOR]

Published

1999

15. Autologous haematopoietic stem cell transplants for autoimmune disease – feasibility and transplant-related mortality.

Author

Tyndall, A., Fassas, A., Passweg, J., de Elvira, C. Ruiz, Attal, M., Brooks, P., Black, C., Durez, P., Finke, J., Forman, S., Fouillard, L., Furst, D., Holmes, J. A., Joske, D., Jouet, J. P., Kötter, I., Locatelli, F., Prentice, H. G., Marmont, A. M., and McSweeney, P.

Subjects

AUTOIMMUNE diseases, BONE marrow transplantation

Abstract

This ongoing multicentre prospective phase I/II trial enrolled 74 consecutive patients from 22 centres worldwide with severe autoimmune disease, 35 with rheumatological disorders, 31 with neurological, five with haematological and three with vasculitides. They were treated with autologous peripheral blood or bone marrow transplants according to predetermined criteria. Two patients died after mobilisation before transplant. Seventy-two patients were given 73 transplants, seven bone marrow, and 66 mobilised peripheral blood stem cell transplants. The graft was manipulated to remove T and/or B cells in 43 cases. All 73 transplants engrafted. Five patients died of transplant-related complications: two from bleeding, three from infections. Two patients died of progressive disease. The transplant-related mortality at 1 year of 9% (1–17%; 95% CI) is comparable to the transplant-related mortality of 6% (3–9%; 95% CI) in patients transplanted during the same period in Europe for non-Hodgkin’s lymphoma in sensitive relapse (P = 0.39). Sixty patients are evaluable for response, 40 patients (65%) showed some improvement in their disease. Haematopoietic stem cell transplants are feasible for patients with severe refractory autoimmune disease. Transplant-related mortality is comparable to results in patients with non-Hodgkin’s lymphoma in responsive relapse. Two-thirds of the patients show at least some response. These preliminary data are promising. Although associated with considerable risk, randomised trials comparing autologous stem cell transplants to conventional therapy are warranted. [ABSTRACT FROM AUTHOR]

Published

1999

16. Allogeneic bone marrow transplant or second autograft in patients with acute leukemia who relapse after an autograft.

Author

Ringdén, O, Labopin, M, Frassoni, F, Sanz, G F, Demeocq, F, Prentice, H G, Cahn, J-Y, Barbui, T, Meloni, G, Schaefer, U W, Reiffers, J, and Gorin, N C

Subjects

BONE marrow transplantation, AUTOGRAFTS, LEUKEMIA

Abstract

Among 2752 patients with acute leukemia who had recurrent leukemia after autograft in remission and were reported to the EBMT, 94 underwent an allogeneic bone marrow transplant and 74 received a second autograft. Recipients of HLA-mismatched related or unrelated bone marrow had an increased transplant-related mortality (TRM, P = 0.017) and a decreased leukemia-free survival (LFS, P = 0.03), compared to recipients of HLA matched related or unrelated bone marrow. Outcome in recipients of HLA-compatible related or unrelated bone marrow was compared to those receiving a second autograft. TRM at 2 years was 51 ± 8% in recipients of matched allografts and 26 ± 6% following a 2nd autograft (P < 0.05). two-year lfs was 27 ± 7% and 35 ± 6% in the two groups, respectively (ns). multivariate analysis in these two groups showed that trm was increased in patients who were in 2nd or later remission at 1st autograft (P < 0.05) and allograft recipients (P < 0.05). relapse was more common in patients with all (P < 0.001), above 25 years of age (P < 0.02), autograft performed later than 1991 (P < 0.05), and in second autografts (P < 0.05). lfs was decreased in patients >25 years of age (P < 0.01), if the interval from first autograft to relapse was 8 months or less (P < 0.01) and if tbi was used at first autograft (P < 0.05). [ABSTRACT FROM AUTHOR]

Published

1999

17. Selective removal of alloreactive cells from haematopoietic stem cell grafts: graft engineering for GVHD prophylaxis.

Author

Koh, M B C, Prentice, H G, and Lowdell, M W

Subjects

HEMATOPOIETIC stem cells, GRAFT versus host disease, T cells, CD antigens, BONE marrow transplantation

Abstract

One of the main goals in allogeneic bone marrow transplantation is the abrogation of graft-versus-host disease with the preservation of antileukaemia and antiviral activity. We have established a novel system for the selective removal of alloreactive lymphocytes from donor grafts while retaining an effective allogeneic response to third-party stimulator cells. Initial feasibility studies were done with unrelated HLA-mismatched pairs and then extended into the matched setting. Mononuclear cells from HLA-matched donors were cocultured with irradiated recipient cells prestimulated with cytokines (γ-IFN and TNF-α) in a modified mixed lymphocyte culture (MLC). Alloreactive donor lymphocytes were identified by expression of CD69, an early activation marker and selectively removed by paramagnetic bead sorting. The remaining ‘non-alloreactive’ lymphocytes were tested in proliferative assays against the original matched recipient and to a third-party donor. A mean depletion of proliferative capacity to 11.5 ± 9.9% of the original matched recipient response was achieved while the residual third-party response was largely preserved at 77.8 ± 20.9% which should translate into improved immune reconstitution and preservation of antiviral activity. The non-alloreactive lymphocytes could also possess functional antileukaemia activity. Moreover, the alloreactive cells are easily recoverable in this selective T cell depletion strategy for cryopreservation and ready for immediate access as therapeutic donor lymphocyte infusions in cases of frank relapse post transplant. [ABSTRACT FROM AUTHOR]

Published

1999

18. FLAG-idarubicin and allogeneic stem cell transplantation for Ph-positive ALL beyond first remission.

Author

Deane, M, Koh, M, Foroni, L, Galactowicz, G, Hoffbrand, A V, Lawler, M, Secker-Walker, L, and Prentice, H G

Subjects

REPORTING of diseases, BONE marrow transplantation, CELL transplantation, CYTOGENETICS, DRUG therapy

Abstract

We describe a single centre experience of eight consecutive patients with relapsed or refractory Ph+ ALL treated with the FLAG/idarubicin regimen followed by BMT or PBSCT. Following FLAG/idarubicin, one achieved a partial response and seven CR. All patients subsequently received allogeneic transplants: one sibling BMT, three matched unrelated (MUD) BMT and four sibling PBSCT. Two patients received second transplants with PBSC from their original BM donors following FLA/Ida with no further conditioning. Three patients are alive in CR 9, 24 and 32 months after transplant. Seven of eight patients had a cytogenetic response following FLAG/Ida induction and one of seven became bcr-abl negative. All eight patients had a complete cytogenetic response following transplant. Four of five assessable patients became p190 bcr-abl negative after transplant; three of these subsequently relapsed. Both patients with the p210 bcr-abl transcript remained bcr-abl positive in CR after transplant. FLAG/Ida was well tolerated and appears to be effective in inducing remission in relapsed Ph+ ALL. The use of FDR-containing chemotherapy without further conditioning prior to PBSCT deserves further study in heavily pre-treated patients and, in patients with relapsed ALL following BMT, may be a safer option than DLI (donor lymphocyte infusion) by avoiding the associated risk of aplasia. [ABSTRACT FROM AUTHOR]

Published

1998

19. Respiratory infections in immunocompromised patients.

Author

Barry, Simon M., Lipman, Marc C.I., Johnson, Margaret A., Prentice, H. Grant, Barry, S M, Lipman, M C, Johnson, M A, and Prentice, H G

Published

1999

20. Standardization of the Processing of Human Bone Marrow for Allogeneic Transplantation.

Author

Gilmore, M. J. M. L. and Prentice, H. G.

Published

1986

21. A Technique for the Concentration of Nucleated Bone Marrow Cells for in vitro Manipulation or Cryopreservation Using the IBM 2991 Blood Cell Processor.

Author

Gilmore, M. J. M. L., Prentice, H. G., Corringham, R.E., Blacklock, H.A., and Hoffbrand, A. V.

Published

1983

22. The impact of age on outcome in lymphoblastic leukaemia; MRC UKALL X and XA compared: a report from the MRC Paediatric and Adult Working Parties.

Author

Chessells, J M, Hall, E, Prentice, H G, Durrant, J, Bailey, C C, and Richards, S M

Subjects

LYMPHOBLASTIC leukemia treatment, CANCER prognosis, TUMORS in children

Abstract

The purpose of the study was to examine the influence of age on outcome in a large cohort of children and adults with lymphoblastic leukaemia who were treated on two similar trials. Factors influencing outcome were examined in 2204 patients aged over 1 year treated between 1985 and 1992 on the parallel Medical Research Council Trials UKALL X and XA, for children and adults, respectively. There was a progressive worsening in survival with increasing age from 85% (95% CI 83-87) at 5 years for children aged 1-9 to 24% (CI 17-31) for patients over 40. Induction failures, deaths in remission and bone marrow relapses increased significantly with age. Analysis of clinical and biological features showed dominance of early B-ALL in childhood and increasing incidence of the Ph' chromosome with age. Over 80% of eligible children, but a much lower proportion of adults especially those over 40, was entered. Compliance was stricter in the paediatric trial but most deviations in adults involved giving more treatment. Analysis of results in a proportional hazards model confirmed the overwhelming independent influence of age; with all other factors equal a 10 year old had half the risk of treatment failure of a 20 year old and a 44 year old double the risk. Selective entry to therapeutic trials and increased treatment-related toxicity are features of adult ALL but age itself remains a dominant prognostic factor. While improved supportive care and refinements of conventional therapy may have some effect on prognosis, new understandings and treatment approaches to adult ALL are needed. [ABSTRACT FROM AUTHOR]

Published

1998

23. Molecular detection of minimal residual disease in adult and childhood acute lymphoblastic leukaemia reveals differences in treatment response.

Author

Foroni, L, Coyle, L A, Papaioannou, M, Yaxley, J C, Sinclair, MF Cole, Chim, J S, Cannell, P, Secker-Walker, L M, Mehta, A B, Prentice, H G, Hoffbrand, A V, and Sinclair, M F

Subjects

IMMUNOGLOBULINS, LYMPHOBLASTIC leukemia, LYMPHOBLASTIC leukemia treatment, LYMPHOBLASTIC leukemia diagnosis, CARCINOGENESIS, ALLELES, CHROMOSOME abnormalities, CLINICAL trials, COMPARATIVE studies, DNA fingerprinting, DNA probes, RESEARCH methodology, MEDICAL cooperation, POLYMERASE chain reaction, RESEARCH, TIME, EVALUATION research, TREATMENT effectiveness

Abstract

Immunoglobulin heavy chain gene (IgH gene) rearrangements are found in the majority of patients with B lineage acute lymphoblastic leukaemia (ALL). Two hundred and three bone marrow samples from 54 patients (33 adults and 21 children) were analysed by PCR within specific time-points after diagnosis (ie 1, 2-3, 4-6 and 7-12 months) using FR1 and JH primers (fingerprinting with a sensitivity > or =1:5 x 10[3]). CDR3-derived allele specific oligoprimers (ASO to achieve a sensitivity between 1:10[4] and 1:10[5]) were applied to 12 children and 18 adults, while size of CDR3 region, oligoclonality and background problems prevented their application to the remaining patients. All patients were followed clinically for > or =24 months. Thirty adults and 16 children presented as newly diagnosed ALL, while the remaining eight patients were analysed in first or subsequent relapse. Patients destined to relapse showed a higher proportion of positive tests (> or =50%), particularly after 1 month, than in the remission group, irrespective of age. Among patients staying in remission, a decrease in MRD-positive tests occurred during the first 12 months in both age groups. However, the proportion of positive tests dropped below 15% at a later stage in adults (4-6 months) than in children (2-3 months). Among children, only patients destined to relapse were MRD positive beyond 1 month, with the exception of only one patient, still positive at 2-3 months in the remission group. The difference in MRD positivity between relapse and remission patients was statistically significant in children (P < 0.03) at any time of testing, but only at 4-6 months in adults (P < 0.01). These data suggest that resolution of MRD in ALL occurs more rapidly in children compared to adults, particularly within the first 6 months. Children and adults, studied in first or subsequent relapse, showed a higher proportion of positive tests during reinduction compared to newly diagnosed patients. [ABSTRACT FROM AUTHOR]

Published

1997

24. High-dose melphalan with autologous bone marrow transplant. Treatment of poor prognosis tumors.

Author

Corringham, Robert, Gilmore, Martin, Prentice, H. Grant, Boesen, Evelyn, Corringham, R, Gilmore, M, Prentice, H G, and Boesen, E

Published

1983

25. Efficacy of amphotericin B encapsulated in liposomes (AmBisome) in the treatment of invasive fungal infections in immunocompromised patients.

Author

Ringdén, O., Meunier, F., Tollemar, J., Ricci, P., Tura, S., Kuse, E., Viviani, M. A., Gorin, N. C., Klastersky, J., Fenaux, P., Prentice, H. G., and Ksionski, G.

Abstract

One hundrtd and twenty-six patients were treated for 137 episodts of fungal infection with liposomal amphotericin B (AmBisome) at 43 investigational centres. Among the patients were 72 with malignancies, 17 organ transplant recipients, 20 patients with immunological disorders and 17 others. AmBisome treatment was instituted after toxicity from previous amphotericin B treatment in 49 cases, nephrotoxicity or renal insuffciency in 40 and failure of previous antifungal treatment in 41. One hundred and eight episodes were clinically evaluable; among these 52 were caused byCandido spp and 34 by Aspergillus spp. Ninety-nine patients were treated for at least eight days with a maximum dose of 0·7–5 mg/kg/day. Among 64 cases with proven invasive fungal infection 58% were cured. Fungi were eradicated in 35 of 54 (65) mycologically evaluable cases. The cumulative dose was 3·2 ± 3·2 (mean±S.D.) in cases where fungi were eradicated in comparison with 3·3 ± 2·3 g in cases where fungi persisted. The eradication rate was 83% for Candida spp. compared with 41% forAspergilus spp. (P <0·01). Among 24 cases with presumptive invasive fungal infections 14 (58) were cured.Candida spp. were eradicated in seven of ten of these cases. Among 11 cases with superficial fungal infections eight were cured and three improved.Candida spp. were eradicated in four of five patients.It is concluded that AmBisome is an effective antifungal agent in a majority of patients with invasive or superficial fungal infections [ABSTRACT FROM PUBLISHER]

Published

1991

26. Liposomal amphotericin B (AmBisome): safety data from a phase II/III clinical trial.

Author

Meunier, F., Prentice, H. G., and Ringdén, O.

Abstract

AmBisome is commmercially available preparation of amphotericin B incorporated in small unilamellar lipsomes. The analysis of safely data provided in a multicentre compassionate phase II/III study evaluating 133 episodes of therapy with AmBisome in patients with server underlying dieses is very encouraging. Rapid (30–60 min) administration of a high daily does of AmBisome is feasible without the well known side effects observed with the conventional formulation of amphotericin B (Fungizone). Although eleven of 71 patients with initially normal serum creatinine concentration showed increased values after AmBisome therapy, 17 patients among 50 with initially high creatinine concentrations recovered normal renal function during AmBisome treatment. Hypokalaemia was observed 24 episodes of treatment (18%). Increases in serum glutamyl oxaloacetic transaminase and alkaline phosphatase were also quit common in this selected population with severe underlying disease and the contribution of AmBisome appears a safe alrnative to conventional amphotericin B, and its eficacy should be further investigated. [ABSTRACT FROM PUBLISHER]

Published

1991

27. A comparison of double beta-lactam combinations with netilmicin/ureidopenicillin regimens in the empirical therapy of febrile neutropenic patients.

Author

Kibbler, C C, Prentice, H G, Sage, R J, Hoffbrand, A V, Brenner, M K, Mannan, P, Warner, P, Bhamra, A, and Noone, P

Abstract

In a randomized trial ceftazidime plus piperacillin or azlocillin, and netilmicin plus piperacillin or azlocillin were used as initial empirical therapy in 202 febrile neutropenic episodes. Netilmicin plus azlocillin was the most effective combination with a clinical response rate of 81% in clinically and microbiologically documented infections compared with 63% for ceftazidime plus piperacillin. All of the episodes of Gram-negative bacteraemia treated with azlocillin responded compared with 43% of those treated with piperacillin. Gram-positive organisms accounted for 52% of all bacteriologically documented infections and 40% of the febrile episodes were treated with vancomycin for presumptive or documented Gram-positive infection. Patients treated with netilmicin had significantly more nephrotoxicity than those given the double beta-lactam combinations (14.8% vs 3.5%; P less than 0.05). However, this difference was not shown in those patients who did not receive concurrent vancomycin or amphotericin. The double beta-lactam combinations were associated with more hypokalaemia (58.2% vs. 37.7%; P less than 0.05) and more colonization with yeasts (24% vs. 10.4%; P less than 0.05) but there was no evidence that their use was associated with prolongation of neutropenia. These results indicate that ceftazidime plus a ureidopenicillin would be adequate empirical therapy in situations where the concomitant use of nephrotoxic agents precludes the use of aminoglycoside containing combinations. [ABSTRACT FROM AUTHOR]

Published

1989

28. A randomized trial of empirical antibiotic therapy with one of four beta-lactam antibiotics in combination with netilmicin in febrile neutropenic patients.

Author

Sage, Roger, Hann, Ian, Prentice, H. Grant, Devereux, Stephen, Corringham, Robert, Hoffbrand, A. Victor, Blacklock, Hilary, Stirling, Louise, Guimaraes, Maria, Trikka, Eleftheria, Bhamra, Amrat, Warner, Pauline, Noone, Paul, Sage, R, Hann, I, Prentice, H G, Devereux, S, Corringham, R, Hoffbrand, A V, and Blacklock, H

Abstract

Over a two year period 174 evaluable episodes of fever in neutropenic patients were treated in a randomized study comparing four beta-lactam antibiotics, each given in combination with netilmicin. Exclusions included episodes due to viral or fungal infection, and trial violations. Most patients were receiving treatment for leukaemia, including 18% undergoing bone marrow transplantation. The overall response rate (EORTC criteria) was 66%, ranging from 56% for cefoperazone to 76% for mezlocillin. Microbial documentation was obtained in 31% of episodes; Gram-positive isolates were most frequent but Pseudomonas aeruginosa was found in 18 patients. In patients with microbiologically documented infection 70% improved, overall--from 40% with cefoperazone to 80% with piperacillin (P less than 0.05). Nephrotoxicity was seen in 6.7% and was associated with severe documented sepsis. Hypokalaemia was seen in 29% and was most marked in patients receiving ticarcillin. Rashes occurred in 6.6% overall, with no difference between the groups. Ototoxicity, shown by serial audiograms, was seen in 4.7% of patients. No evidence of vestibular dysfunction was seen in 62 patients studied. Of thirteen deaths due to the primary infection, seven were caused by Ps. aeruginosa and five by fungi. [ABSTRACT FROM AUTHOR]

Published

1988

29. The pharmacokinetics of ketoconazole in severely immunocompromised patients.

Author

Hann, I. M., Prentice, H. G., Keaney, M., Corringham, R., Blacklock, H. A., Fox, J., Gascoigne, E., Van Custem, J., and Van Cutsem, J

Abstract

Forty patients severely immunocompromised because of the nature of their underlying disease (marrow aplasia, acute leukaemia or solid tumour) and/or the treatment they were receiving, received ketoconazole 400 mg daily. All patients also received gut decontamination with non-absorbable antibiotics, skin antisepsis, sterile food and oral co-trimoxazole. Mean (±S.D.) peak serum ketoconazole levels of 5·14±1·4 mg/l occurred 3 h after drug intake. In patients not receiving an allogeneic bone marrow transplant (BMT), the mean serum level at 2 h post-dose remained in the range of 3 to 5 mg/l during prolonged therapy. In contrast, serum ketoconazole levels in allogeneic BMT patients declined during continued treatment. In addition, the incidence of fungal infections was significantly higher in allogeneic-BMT patients than in the other group (<0·005). [ABSTRACT FROM PUBLISHER]

Published

1982

30. The effect of T cell depletion with Campath-1M on immune reconstitution after chemotherapy and allogeneic bone marrow transplant as treatment for leukaemia.

Author

Lowdell, M W, Craston, R, Ray, N, Koh, M, Galatowicz, G, and Prentice, H G

Subjects

T cells, GRAFT versus host disease, STEM cell transplantation

Abstract

The prophylactic use of T cell depletion (TCD) strategies for the prevention of graft-versus-host disease (GVHD) following allogeneic stem cell transplantation remains widespread. Initial reports of high incidence of graft rejection after TCD BMT led to a move away from this approach but improved conditioning regimens have reduced this risk substantially. The use of TCD has also been associated with higher relapse risk post-BMT although the success of donor leukocyte infusion (DLI) as treatment for relapse has reduced this problem, especially in chronic myeloid leukaemia (CML). Currently the use of TCD BMT is increasing particularly due to the relative increase in BMT from non-related donors for whom TCD is the optimal GVHD prophylaxis. However, doubts remain over the long-term effect on the reconstituted immune system of recipients of TCD BMT, particularly in adult recipients. In this study we have undertaken a detailed sequential analysis in 23 patients who received allo-grafts from HLA-identical sibling donors after high-dose chemo/radiotherapy for acute or chronic leukaemia. Of these patients, 11 received non-manipulated grafts, five received ‘partially TCD’ (PTCD) and a further seven received ‘fully TCD’ (FTCD) bone marrow. T cell depletion was performed ex vivo by Campath-1M plus autologous serum as a source of complement. Partial TCD describes grafts with a T cell reduction of 1–2 log. Full TCD refers to grafts with a reduction of >2.5 log. The decision regarding the optimal degree of TCD was clinical and was based upon the perceived relative risk of relapse based upon the disease and remission status. All patients were monitored for up to 12 months post-BMT with regard to reconstitution of T and NK cell subsets. T cell depletion at either level was associated with a slower recovery of CD4 cells. This was most marked in the FTCD recipients and lasted throughout the period of study. CD8 cell recovery was also slower in... [ABSTRACT FROM AUTHOR]

Published

1998

31. Longitudinal fluctuations in cytomegalovirus load in bone marrow transplant patients: relationship between peak virus load, donor/recipient serostatus, acute GVHD and CMV disease.

Author

Gor, D, Sabin, C, Prentice, H G, Vyas, N, Man, S, Griffiths, P D, and Emery, V C

Subjects

CYTOMEGALOVIRUS diseases, BONE marrow transplantation, GRAFT versus host disease

Abstract

Quantitative competitive PCR was used to monitor the quantity of cytomegalovirus (HCMV) in 1647 blood samples from 110 BMT recipients. DNAemia was detected in 49/110 (45%) of the patients, of whom 15/49 experienced HCMV disease. Peak virus load during surveillance was elevated in symptomatic (median 4.5 log10 genomes/ml) vs asymptomatic patients (median 3.6 log10 genomes/ml, P = 0.002) and was also significantly elevated in HCMV seropositive recipients of seronegative marrow, (R+D-, median 5.0 log10), compared to those in the R-D- and R+D+ groups (P < 0.01 and <0.005). odds ratios for disease per 0.25 log10 increase in viral load, recipient seropositivity and aGVHD were 1.43 (P = 0.004), 6.60 (P = 0.05) and 3.17 (P = 0.08), respectively. In multivariate logistic regression analysis only elevated viral load remained a significant risk factor for HCMV disease. The computed disease probability viral load curve showed a rapid increase in disease risk at viral loads between 3.8 and 5.5 log10 genomes/ml in blood, and odds ratios for disease were determined for different threshold viral loads. These data demonstrate the central role of viral load in the pathogenesis of HCMV in BMT recipients and provide an additional marker for targeting and monitoring therapy. [ABSTRACT FROM AUTHOR]

Published

1998

32. Use of intravenous immune globulin in addition to antiviral therapy in the treatment of CMV gastrointestinal disease in allogeneic bone marrow transplant patients: a report from the European Group for Blood and Marrow Transplantation (EBMT).

Author

Ljungman, P, Cordonnier, C, Einsele, H, Bender-Götze, C, Bosi, A, Dekker, A, De la Camara, R, Gmür, J, Newland, A C, Prentice, H G, Robinson, A J, Rovira, M, Rösler, W, and Veil, D

Subjects

CYTOMEGALOVIRUS diseases, GASTROINTESTINAL diseases, GLOBULINS, GANCICLOVIR

Abstract

The best treatment of CMV gastrointestinal disease has been controversial, with some centers adding intravenous (i.v.) Ig to antiviral chemotherapy. The aim of this retrospective survey was to compare the outcome of antiviral chemotherapy with or without i.v. Ig. A questionnaire was sent to centers belonging to the EBMT. Thirty-three patients with CMV gastrointestinal disease were reported, 22 patients were given antiviral chemotherapy alone and 11 patients a combination of antiviral chemotherapy and i.v. Ig. Eighteen of 33 (55%) patients responded to therapy, 13 of those treated with antiviral chemotherapy alone and five (45%) of those treated with the combination (P = NS). Patients with acute GVHD of grades II–IV had significantly worse outcomes than patients with acute GVHD grades 0–I. In a Cox proportional hazards model corrected for acute GVHD there was no difference in outcome of CMV gastrointestinal disease with or without addition of Ig. Survival at 100 days after diagnosis of CMV gastro- intestinal disease was 64%. There was no difference in survival in patients treated with or without i.v. Ig. The results of this retrospective survey indicate that addition of i.v. Ig to antiviral chemotherapy might not improve outcome in patients with biopsy-proven CMV gastrointestinal disease. [ABSTRACT FROM AUTHOR]

Published

1998

33. European results of matched unrelated donor bone marrow transplantation for chronic myeloid leukemia. Impact of HLA class II matching.

Author

Devergie, A, Apperley, J F, Labopin, M, Madrigal, A, Jacobsen, N, Carreras, E, Prentice, H G, Jouet, J P, Kolb, H J, Herstenstein, B, Bacigalupo, A, Evensen, S A, Ljungman, P, de Witte, T, Reiffers, J, Nagler, A, Clark, R E, Goldman, J M, and Gratwohl, A

Subjects

ORGAN donation, BONE marrow transplantation, MYELOID leukemia

Abstract

We have retrospectively analyzed the impact of prognostic factors on the outcome of serologically HLA-matched unrelated donor (UD) BMT for CML. For this purpose, we have studied a cohort of 366 patients transplanted in Europe between January 1985 and December 1994. The median age of the 211 males and 155 females was 34 years; 238 patients were transplanted in first chronic phase and 116 in advanced phases. The median interval from diagnosis to BMT was 827 days. GVHD prophylaxis consisted of CsA and MTX in 202 patients or of ex vivo or in vivo T cell depletion (TCD) in 129. Recently, DNA-based methods of HLA-class II typing have been used to improve donor selection. We obtained complete data on 300 donor/recipient (D/R) pairs. Among them, we have identified three groups of patients, according to specific HLA-DRB1 D/R compatibility. Two hundred and ten patients received marrow from donors identical for HLA-DRB1 (group 1). Thirty-one patients received BMT from a donor who was HLA-DRB1 mismatched (group 2) and 59 from a donor in whom specific HLA-DRB1 typing was not performed (group 3). The overall survival was 37 ± 3% at 2 years and leukemia-free survival (LFS) was 31 ± 3%. In univariate analysis, five variables had a favorable effect on LFS: transplant in first chronic phase (P = 0.0001), time interval from diagnosis to BMT shorter than the median (P = 0.01), prophylaxis of GVHD without TCD (P = 0.001), acute GVHD

Published

1997

34. The in vitro detection of anti-leukaemia-specific cytotoxicity after autologous bone marrow transplantation for acute leukaemia.

Author

Lowdell, M W, Ray, N, Craston, R, Corbett, T, Deane, M, and Prentice, H G

Subjects

LEUKEMIA, BONE marrow transplantation

Abstract

Anti-leukaemia activity after allogeneic bone marrow transplantation has been studied extensively but its antigen specificity and effector cell phenotype remain unknown. Here we report a study in three recipients of autologous bone marrow transplantation done as part of the treatment for acute leukaemia, in whom we were able to detect innate specific anti-leukaemia activity post-transplant. One patient maintained selective cell-mediated cytolytic activity against her autologous leukaemic cells in the absence of cytolysis of her normal bone marrow mononuclear cells (BMMC). She remains in complete remission 3 years after ABMT for acute myeloid leukaemia (M5). A second patient was transplanted for acute lymphoblastic leukaemia and had detectable anti-leukaemia activity up to 20 weeks post-ABMT. At this point anti-leukaemia activity could no longer be demonstrated and the patient suffered a relapse 2 weeks later. A third patient was transplanted for AML (M4 Eo) and lacked detectable leukaemia- specific immune reactivity at 1, 3 and 6 months post-ABMT. She relapsed 6 months after her ABMT and returned to complete remission after further chemotherapy. She commenced treatment with alpha interferon and regained NK function. Furthermore, she developed high level cytolytic activity against her autologous leukaemic cells in the absence of activity against her remission bone marrow samples. She remains in complete remission 17 months after her initial relapse. This is the first report of an apparent association between in vitro leukaemia-specific cytolytic activity in individual patients after ABMT and clinical outcome. It encourages the theory that autologous immuno- modulation may be useful in the future treatment of leukaemia. [ABSTRACT FROM AUTHOR]

Published

1997

35. Long-term survival in allogeneic bone marrow transplant recipients following acyclovir prophylaxis for CMV infection.

Author

Prentice, H G, Gluckman, E, Powles, R L, Ljungman, P, Milpied, N J, Camara, R, Mandelli, F, Kho, P, Kennedy, L, and Bell, A R

Subjects

CYTOMEGALOVIRUS diseases, ACYCLOVIR, BONE marrow transplantation

Abstract

Recipients of HLA-matched, related or unrelated allogeneic BMT who were CMV seropositive or those receiving unmanipulated marrow from a seropositive donor were randomised to receive one of three treatment regimens, i.v. acyclovir 500 mg/m2 three times a day from 5 days before transplant to 30 days after transplant followed by oral acyclovir 800 mg four times a day for a further 6 months, i.v. acyclovir followed by placebo, or 400 mg oral acyclovir four times a day followed by placebo (control). This paper reports the 1 year data on the same cohort of patients which was previously reported. Intravenous acyclovir (IV/PCB) significantly reduced the risk of CMV infection when compared to the control group. The frequency of adverse events reported was comparable among the three groups. The mortality rate was significantly reduced by the sequential use of i.v. acyclovir followed by oral acyclovir, resulting in a 19% survival advantage at 1 year from transplant. [ABSTRACT FROM AUTHOR]

Published

1997

36. Clinical strategies for the management of cytomegalovirus infection and disease in allogeneic bone marrow transplant.

Author

Prentice, H G and Kho, P

Subjects

CYTOMEGALOVIRUS diseases, BONE marrow transplantation

Abstract

Four clinical strategies are proposed for the management of CMV disease: prophylaxis, suppression, pre-emptive therapy and treatment. The degree of risk of developing CMV disease and the safety profile of the presently available drugs need to be considered when deciding on the most appropriate approach. We conclude that a prophylactic strategy employing a drug with a safe toxicity profile followed by pre-emptive treatment with an effective antiviral drug for failure of prophylaxis gives the best outcome in allogeneic HLA matched bone marrow transplant recipients. [ABSTRACT FROM AUTHOR]

Published

1997

37. Can lung function measurements be used to predict which patients will be at risk of developing interstitial pneumonitis after bone marrow transplantation?

Author

Milburn, H J, Prentice, H G, and du Bois, R M

Subjects

BLOOD gases analysis, BONE marrow transplantation, CARBON monoxide, LUNGS, PROGNOSIS, PULMONARY fibrosis, RESPIRATORY measurements, VITAL capacity (Respiration), LUNG volume measurements

Abstract

Background: Lung function often deteriorates after bone marrow transplantation for haematological malignancies. Whether pulmonary function measurements are useful for monitoring patients' progress after transplantation and for alerting clinicians to the development of pneumonitis is uncertain.Methods: Serial pulmonary function measurements were made in 39 patients with a haematological malignancy, and the values from 18 recipients of T cell depleted allogeneic (n = 17) or autologous (n = 1) bone marrow transplants who developed interstitial pneumonitis were compared retrospectively with values from 21 recipients of allogeneic (n = 17) or autologous (n = 4) transplants who did not develop pneumonitis. Lung function was measured at the onset of a further 18 episodes of pneumonitis.Results: Measurements made before transplantation showed no difference in forced expiratory volume in one second (FEV1), transfer factor for carbon monoxide (TLCO), or total lung capacity between the two groups, but the forced vital capacity (FVC) was slightly higher in those who developed pneumonitis (mean (SD)% predicted 104 (12)) than in those who did not (93 (17%)). Six weeks and three months after transplantation all pulmonary function measurements had fallen slightly in both groups but TLCO had fallen considerably more in those who later developed pneumonitis, being 71% (SD 11%) and 77% (7%) of pretransplant values in patients who later developed pneumonitis compared with 109% (38%) and 96% (26%) in those who did not. All lung function measurements were significantly lower at the onset of pneumonitis than three months after transplantation, even in patients with no abnormal signs and a normal chest radiograph.Conclusions: Serial measurements of gas transfer before and after bone marrow transplantation may be useful for predicting which patients will be at risk of developing pneumonitis and may help to diagnose pneumonitis in breathless patients with no abnormal signs. [ABSTRACT FROM AUTHOR]

Published

1992

38. Pulmonary cell populations in recipients of bone marrow transplants with interstitial pneumonitis.

Author

Milburn, H J, Poulter, L W, Prentice, H G, and du Bois, R M

Abstract

The immunological basis of the inflammatory response in the lungs of patients with pneumonitis after bone marrow transplantation has been investigated by means of bronchoalveolar lavage. Ten episodes of pneumonitis associated with cytomegalovirus and nine episodes due to various other infectious and non-infectious causes were investigated in 16 patients (three patients had two episodes of pneumonitis). Total lavage cell counts and differential cell counts were determined and compared with results from normal control subjects. In most patients with pneumonitis the total cell yield was greater than normal (mean 6.8 (SD 6.0) x 10(5) cells/ml; normal 1-2 x 10(5) cells/ml). The percentage distribution of these cells was 71.9 (17) macrophage like cells, 24.1 (15.8) lymphocytes, 5.0 (5.0) polymorphonuclear cells, and 0.7 (1.0) eosinophils. None of the patients had peripheral lymphocytosis despite the increased number of lymphocytes in the lavage fluid. Further analysis of the lymphocyte population using monoclonal antibodies with immunocytochemical techniques showed that B cells were generally present in normal proportions, whereas the proportion of cells expressing T lymphocyte markers (CD2+, CD5+, CD8) were reduced in nine out of 19 cases. In 10 of the 19 episodes there were substantial numbers of cells expressing none of the B or T cell antigens studied ("null" cells). These abnormalities bore no relation to survival. The total cell yield, the proportion and number of lymphocytes, and the proportion and number of T cells in the bronchoalveolar lavage fluid were all lower in the group with cytomegalovirus infections than in those with pneumonitis from other causes. These results suggest that the pneumonitis in recipients of bone marrow transplants is associated with a local immune response despite the fact that the individuals are otherwise immunosuppressed. [ABSTRACT FROM PUBLISHER]

Published

1989

39. Apparent pulmonary mycetoma following invasive aspergillosis in neutropenic patients.

Author

Kibbler, C C, Milkins, S R, Bhamra, A, Spiteri, M A, Noone, P, and Prentice, H G

Subjects

ASPERGILLOSIS treatment, AGRANULOCYTOSIS, ASPERGILLOSIS, HEMOPTYSIS, FUNGAL lung diseases, NEUTROPENIA, PROGNOSIS, DISEASE complications

Abstract

After the death from massive haemoptysis of two neutropenic patients who had developed apparent pulmonary mycetomas, two subsequent patients underwent successful resection of similar lesions. Histological examination of these lesions confirmed that these so called mycetomas were masses of devitalized lung tissue infiltrated with fungus. The term mycotic lung sequestrum is therefore proposed to distinguish this condition from a fungus ball arising in a previously formed cavity. A review of 34 similar cases reported previously showed that haemoptysis occurred in about half of the cases and was fatal in just over half of these. Medical treatment appears to have little impact on survival and early consideration of surgical intervention is important. [ABSTRACT FROM PUBLISHER]

Published

1988

40. Role of bronchoalveolar lavage in the evaluation of interstitial pneumonitis in recipients of bone marrow transplants.

Author

Milburn, H J, Prentice, H G, and du Bois, R M

Abstract

Forty episodes of pneumonitis in 30 recipients of allogeneic bone marrow transplants were investigated by fibreoptic bronchoscopy and bronchoalveolar lavage. A positive diagnosis was made in 32 episodes of pneumonitis (24 patients), giving a diagnostic yield of 80%. In 31 of these the diagnosis was made within 24 hours of bronchoscopy and this enabled the appropriate treatment to be instituted early. Eighteen patients recovered from their primary infection, although two died subsequently of respiratory failure due to postpneumonic lung destruction. Ten patients later developed a second episode of pneumonitis and a diagnosis was made in nine of these. Only three survived a second episode. Bronchoalveolar lavage was well tolerated by all patients and there was no morbidity or mortality that could be directly attributed to the procedure. Bronchoalveolar lavage is a safe and valuable early diagnostic procedure for the investigation of pulmonary complications in patients who have received bone marrow transplants. [ABSTRACT FROM PUBLISHER]

Published

1987

41. Terminal Transferase Enzyme Assay and Immunological Membrane Markers in the Diagnosis of Leukaemia: a Multiparameter Analysis of 300 Cases.

Author

Janossy, G., Hoffbrand, A. V., Greaves, M. F., Ganeshaguru, K., Pain, Carol, Bradstock, K. F., Prentice, H. G., Kay, H. E. M., and Lister, T. A.

Published

1980

42. Is the measurement of virus-specific antibody in the lungs of transplant recipients with cytomegalovirus pneumonitis of diagnostic or prognostic value?

Author

Milburn, Heather J., Grundy, Jane E., Bois, R. M. Du, Prentice, H. G., and Griffiths, P. D.

Published

1988

43. Seroepidemiologic studies on the acquisition of antibodies to cytomegalovirus, herpes simplex virus, and human immunodeficiency virus among general hospital patients and those attending a clinic for sexually transmitted diseases.

Author

Berry, N. J., Burns, D. MacDonald, Wannamethee, G., Grundy, J. E., Lui, S. F., Prentice, H. G., and Griffiths, P. D.

Published

1988

44. Virological and serological diagnosis of cytomegalovirus infection in bone marrow allograft recipients.

Author

Panjwani, D. D., Ball, M. G., Berry, N. J., Wimperis, J. Z., Blacklock, H. A., Prentice, H. G., Hoffbrand, A. V., and Griffiths, P. D.

Published

1985

45. Impact of Previous Aspergillosis on the Outcome of Bone Marrow Transplantation.

Author

Offner, F., Cordonnier, C., Ljungman, P., Prentice, H. G., Engelhard, D., De Bacquer, D., Meunier, F., and De Pauw, B.

Abstract

A retrospective analysis of 48 patients with documented or probable invasive aspergillosis (IA) prior to bone marrow transplantation (BMT) was conducted in 16 centers. Treatment of primary IA was medical in all 48 patients and surgical in 20; clinicoradiological resolution of IA occurred in 30 of 48 patients. Pretransplantation risk factors for relapse IA, total mortality, and IA-related mortality were analyzed by multivariate logistic regression with the following dichotomous risk factors: surgery as part of the initial treatment, resolution of IA by the time of BMT, donor type, conditioning regiment, total-body irradiation, T cell depletion, immunosuppressive therapy, type of antifungal prophylaxis, and growth factor prophylaxis. Conditioning with busulfan/cyclophosphamide was associated with a beneficial outcome for total survival and reduced IA-related mortality. Posttransplantation risk factors such as the development of graft-vs.-host disease (GVHD), therapy for GVHD, and the duration of neutropenia did not have a significant effect on relapse IA, IArelated mortality, or total mortality. The overall incidence of relapse IA was lower than expected (33% [16 of 48 patients]), but the mortality rate among relapsed patients was 88% (14 of 16). Patients receiving prophylaxis with absorbable or intravenous antifungals had less relapses of IA than did those not receiving prophylaxis (12 of 41 vs. four of seven, respectively). This finding reflects the need for better prophylaxis and new antifungal treatments for patients undergoing BMT who have a history of IA. [ABSTRACT FROM PUBLISHER]

Published

1998

46. ANTIVIRAL THERAPY IN THE IMMUNOCOMPROMISED PATIENT.

Author

Prentice, H G and Hann, I M

Published

1985

47. Minimal Residual Disease in Acute Lymphoblastic Leukaemia-PCR Analysis of Immunoglobulin Gene Rearrangements.

Author

Cole-Sinclair, M., Foroni, L., Wright, F., Mehta, A., Prentice, H. G., and Hoffbrand, A. V.

Published

1993

48. Flow Cytometric Assessment of Multidrug Resistance (MDR) Phenotype in Acute Myeloid Leukaemia.

Author

Hart, S. M., Ganeshaguru, K., Lyttelton, M. P. A., Prentice, H. G., Hoffbrand, A. V., and Mehta, A. B.

Published

1993

49. Plasma Soluble Interleukin 2 Receptor Levels in Patients with Malignant Lymphoma are Correlated with Disease Activity but not Cellular Immunosuppression.

Author

Hamon, M. D., Unal, E., Macdonald, I., Shamim, F., Boesen, E., and Prentice, H. G.

Published

1993

50. Multidrug Resistance in Acute Leukaemia: A Comparative Study of Immunocytochemical and RNA Slot Blot Detection of P-glycoprotein Expression.

Author

Lyttelton, M. P. A., Hart, S., Ganeshaguru, K., Prentice, H. G., Hoffbrand, A. V., and Mehta, A. B.

Published

1991