Your search keyword '"Goldman J"' showing total 180 results

1. Border-associated macrophages mediate the neuroinflammatory response in an alpha-synuclein model of Parkinson disease.

Author

Schonhoff, A. M., Figge, D. A., Williams, G. P., Jurkuvenaite, A., Gallups, N. J., Childers, G. M., Webster, J. M., Standaert, D. G., Goldman, J. E., and Harms, A. S.

Subjects

PARKINSON'S disease, ANTIGEN presenting cells, T cells, MACROPHAGES, ALPHA-synuclein, ANTIGEN presentation

Abstract

Dopaminergic cell loss due to the accumulation of α-syn is a core feature of the pathogenesis of Parkinson disease. Neuroinflammation specifically induced by α-synuclein has been shown to exacerbate neurodegeneration, yet the role of central nervous system (CNS) resident macrophages in this process remains unclear. We found that a specific subset of CNS resident macrophages, border-associated macrophages (BAMs), play an essential role in mediating α-synuclein related neuroinflammation due to their unique role as the antigen presenting cells necessary to initiate a CD4 T cell response whereas the loss of MHCII antigen presentation on microglia had no effect on neuroinflammation. Furthermore, α-synuclein expression led to an expansion in border-associated macrophage numbers and a unique damage-associated activation state. Through a combinatorial approach of single-cell RNA sequencing and depletion experiments, we found that border-associated macrophages played an essential role in immune cell recruitment, infiltration, and antigen presentation. Furthermore, border-associated macrophages were identified in post-mortem PD brain in close proximity to T cells. These results point to a role for border-associated macrophages in mediating the pathogenesis of Parkinson disease through their role in the orchestration of the α-synuclein-mediated neuroinflammatory response. Neuroinflammatory mechanisms are implicated in Parkinson disease. Here we identify border-associated macrophages (BAMs), as essential for the α-synuclein-mediated neuroinflammatory response via class II antigen presentation, and T cell infiltration. [ABSTRACT FROM AUTHOR]

Published

2023

2. Escalating-dose HLA-mismatched DLI is safe for the treatment of leukaemia relapse following alemtuzumab-based myeloablative allo-SCT.

Author

Innes, A J, Beattie, R, Sergeant, R, Damaj, G, Foroni, L, Marin, D, Kanfer, E, Mielke, S, Milojkovic, D, MacDonald, D, Pavlu, J, Rahemtulla, A, Roberts, I, Slade, D, Bray, E, Goldman, J, Apperley, J, Szydlo, R, Dazzi, F, and Rezvani, K

Subjects

PATIENTS, LEUKEMIA, GENES, CANCER, SAFETY

Abstract

Although the feasibility of using HLA-mismatched unrelated donors as an alternate graft source for haematopoietic SCT (HSCT) has been shown, little is known about the safety of HLA-mismatched DLI for the treatment of relapse. We examined the outcome of 58 consecutive leukaemia patients who received escalating-dose DLI for treatment of relapse after alemtuzumab-conditioned myeloablative unrelated donor HSCT at our institution. High-resolution HLA typing on stored DNA samples revealed mismatches in 28/58 patients who were considered HLA-matched at the time of transplantation. Following DLI from HLA-matched (10/10) (n=30) or -mismatched (7-9/10) (n=28) unrelated donors, we found no significant difference in the incidence of acute GVHD (17.2% versus 23.1%, P=0.59), probability of remission at 3 years (62.1% versus 63.9%, P=0.89) or 5-year OS (89.8% versus 77.7%, P=0.22). We conclude that escalating-dose DLI can be safely given to HLA-mismatched recipients following T-depleted myeloablative HSCT. [ABSTRACT FROM AUTHOR]

Published

2013

3. Prognostic factors for outcomes in allogeneic transplantation for CML in the imatinib era: a CIBMTR analysis.

Author

Khoury, H J, Kukreja, M, Goldman, J M, Wang, T, Halter, J, Arora, M, Gupta, V, Rizzieri, D A, George, B, Keating, A, Gale, R P, Marks, D I, McCarthy, P L, Woolfrey, A, Szer, J, Giralt, S A, Maziarz, R T, Cortes, J, Horowitz, M M, and Lee, S J

Subjects

HEMATOPOIETIC agents, TREATMENT of chronic myeloid leukemia, IMATINIB, BONE marrow transplantation, BLOOD transfusion

Abstract

Allogeneic hematopoietic SCT is an effective treatment in accelerated (AP) or blast phase (BP) CML. Imatinib (IM) has transient but significant activity in advanced phases of CML, which may permit early allografting for responding patients. To identify prognostic factors in allograft recipients previously treated with IM, we analyzed 449 allogeneic hematopoietic SCTs performed from 1999 to 2004 in advanced-phase CML, using the data reported to the Center for International Blood and Marrow Transplant Research. CML patients in second chronic phase (CP2, n=184), AP (n=185) and BP (n=80) received HLA-identical sibling (27%), related (3%), or matched or mismatched unrelated donor (70%), peripheral blood (47%) or BM (53%) hematopoietic SCT after myeloablative (78%) or non-myeloablative (22%) conditioning. In all, 52% in CP2, 49% in AP and 46% in BP received IM before hematopoietic SCT. Disease-free survival was 35-40% for CP2, 26-27% for AP and 8-11% for BP. Cumulative incidence of acute and chronic GVHD and TRM were not affected by the stages of CML or pre-hematopoietic SCT IM exposure. Multivariate analyses showed that conventional prognostic indicators remain the strongest determinants of transplant outcomes. In conclusion, there are no new prognostic indicators of the outcomes of allogeneic hematopoietic SCT for advanced-phase CML in the IM era. [ABSTRACT FROM AUTHOR]

Published

2012

4. Uptake and outcome of assisted reproductive techniques in long-term survivors of SCT.

Author

Babb, A, Farah, N, Lyons, C, Lindsay, K, Reddy, N, Goldman, J, Apperley, J F, and Salooja, N

Subjects

STEM cell transplantation, HEMATOLOGY -- Technique, SPERMATOZOA, HUMAN reproductive technology, SPERM banks, SPERM donation, INFERTILITY, CONCEPTION, PATIENTS

Abstract

We have audited the invitation for uptake and outcome of artificial reproductive techniques in patients undergoing SCT for haematological malignancy, with the aim of improving our pre-transplant counselling. A postal survey was sent to 434 patients in our centre surviving a minimum of 2 years after allo-SCT, of whom 221 patients responded. Of 112 male patients, 79 were offered sperm storage, 42 banked sperm and 25 subsequently attempted parenthood with stored sperm. A total of 18 were successful, with 29 children born a median of 8 years (range 1-22 years) following SCT. Of 72 females <42 years old, 33 were offered storage of embryos/eggs/ovarian tissue and 12 accepted. Following SCT, four women attempted pregnancy using cryopreserved embryos, with two successes. The majority of patients who were not counselled about infertility or not offered fertility-preservation options provided a likely reason, with completion of family being the most frequent. Nonetheless, 16 patients (11/72 women and 5/112 men) could not provide a reason for the lack of information/invitation. In conclusion, uptake of gamete/embryo storage is high when offered and collected material is used frequently. Pregnancies in partners of male patients were usually successful and our data highlight the value of prolonged cryostorage. [ABSTRACT FROM AUTHOR]

Published

2012

5. Long-term safety of intramuscular gene transfer of non-viral FGF1 for peripheral artery disease.

Author

Niebuhr, A, Henry, T, Goldman, J, Baumgartner, I, van Belle, E, Gerss, J, Hirsch, A T, and Nikol, S

Subjects

PERIPHERAL vascular diseases, GENETIC transformation, DISEASE progression, VIRAL genetics, GENE therapy, FIBROBLAST growth factors, GENE expression, NEOVASCULARIZATION

Abstract

Peripheral artery disease is a progressive disease. Primary ischemic leg symptoms are muscle fatigue, discomfort or pain during ambulation, known as intermittent claudication. The most severe manifestation of peripheral artery disease is critical limb ischemia (CLI). The long-term safety of gene therapy in peripheral artery disease remains unclear. This four center peripheral artery disease registry was designed to evaluate the long-term safety of the intramuscular non-viral fibroblast growth factor-1 (NV1FGF), a plasmid-based angiogenic gene for local expression of fibroblast growth factor-1 versus placebo in patients with peripheral artery disease who had been included in five different phase I and II trials. Here we report a 3-year follow-up in patients suffering from CLI or intermittent claudication. There were 93 evaluable patients, 72 of them in Fontaine stage IV (47 NV1FGF versus 25 placebo) and 21 patients in Fontaine stage IIb peripheral artery disease (15 NV1FGF versus 6 placebo). Safety parameters included rates of non-fatal myocardial infarction (MI), stroke, death, cancer, retinopathy and renal dysfunction. At 3 years, in 93 patients included this registry, there was no increase in retinopathy or renal dysfunction associated with delivery of this angiogenic factor. There was also no difference in the number of strokes, MI or deaths, respectively, for NV1FGF versus placebo. In the CLI group, new cancer occurred in two patients in the NV1FGF group. Conclusions that can be drawn from this relatively small patient group are limited because of the number of patients followed and can only be restricted to safety. Yet, data presented may be valuable concerning rates in cancer, retinopathy, MI or strokes following angiogenesis gene therapy in the absence of any long-term data in angiogenesis gene therapy. It may take several years until data from larger patient populations will become available. [ABSTRACT FROM AUTHOR]

Published

2012

6. KIR2DS1 genotype predicts for complete cytogenetic response and survival in newly diagnosed chronic myeloid leukemia patients treated with imatinib.

Author

Marin, D, Gabriel, I H, Ahmad, S, Foroni, L, Lavallade, H de, Clark, R, O'Brien, S, Sergeant, R, Hedgley, C, Milojkovic, D, Khorashad, J S, Bua, M, Alsuliman, A, Khoder, A, Stringaris, K, Cooper, N, Davis, J, Goldman, J M, Apperley, J F, and Rezvani, K

Subjects

CHRONIC myeloid leukemia, GENETIC research, GENETIC polymorphisms, PROTEIN-tyrosine kinases, AMINO acids

Abstract

Natural killer (NK) cells are expanded in chronic myeloid leukemia (CML) patients on tyrosine kinase inhibitors (TKI) and exert cytotoxicity. The inherited repertoire of killer immunoglobulin-like receptors (KIR) may influence response to TKI. We investigated the impact of KIR-genotype on outcome in 166 chronic phase CML patients on first-line imatinib treatment. We validated our findings in an independent patient group. On multivariate analysis, KIR2DS1 genotype (RR=1.51, P=0.03) and Sokal risk score (low-risk RR=1, intermediate-risk RR=1.53, P=0.04, high-risk RR=1.69, P=0.034) were the only independent predictors for failure to achieve complete cytogenetic response (CCyR). Furthermore, KIR2DS1 was the only factor predicting shorter progression-free (PFS) (RR=3.1, P=0.03) and overall survival (OS) (RR=2.6, P=0.04). The association between KIR2DS1 and CCyR, PFS and OS was validated by KIR genotyping in 174 CML patients on first-line imatinib in the UK multi-center SPIRIT-1 trial; in this cohort, KIR2DS1(+) patients had significantly lower 2-year probabilities of achieving CCyR (76.9 vs 87.9%, P=0.003), PFS (85.3 vs 98.1%, P=0.007) and OS (94.4 vs 100%, P=0.015) than KIR2DS1(−) patients. The impact of KIR2DS1 on CCyR was greatest when the ligand for the corresponding inhibitory receptor, KIR2DL1, was absent (P=0.00006). Our data suggest a novel role for KIR-HLA immunogenetics in CML patients on TKI. [ABSTRACT FROM AUTHOR]

Published

2012

7. Feasibility testing of an automated image-capture method to aid dietary recall.

Author

Arab, L, Estrin, D, Kim, D H, Burke, J, and Goldman, J

Subjects

FEASIBILITY studies, IMAGING systems, DIET, INGESTION, CAMERA phones, WEBSITES, IMAGE processing, SELF-consciousness (Awareness)

Abstract

Background/Objectives:The accuracy of dietary recalls might be enhanced by providing participants with photo images of foods they consumed during the test period.Subjects/Methods:We examined the feasibility of a system (Image-Diet Day) that is a user-initiated camera-equipped mobile phone that is programmed to automatically capture and transmit images to a secure website in conjunction with computer-assisted, multipass, 24-h dietary recalls in 14 participants during 2007. Participants used the device during eating periods on each of the three independent days. Image processing filters successfully eliminated underexposed, overexposed and blurry images. The captured images were accessed by the participants using the ImageViewer software while completing the 24-h dietary recall on the following day.Results:None of the participants reported difficulty using the ImageViewer. Images were deemed 'helpful' or 'sort of helpful' by 93% of participants. A majority (79%) of users reported having no technical problems, but 71% rated the burden of wearing the device as somewhat to very difficult, owing to issues such as limited battery life, self-consciousness about wearing the device in public and concerns about the field of view of the camera.Conclusion:Overall, these findings suggest that automated imaging is a promising technology to facilitate dietary recall. The challenge of managing the thousands of images generated can be met. Smaller devices with a broader field of view may aid in overcoming self-consciousness of the user with using or wearing the device. [ABSTRACT FROM AUTHOR]

Published

2011

8. Safety of a non-viral plasmid-encoding dual isoforms of hepatocyte growth factor in critical limb ischemia patients: a phase I study.

Author

Henry, T D, Hirsch, A T, Goldman, J, Wang, Y L, Lips, D L, McMillan, W D, Duval, S, Biggs, T A, and Keo, H H

Subjects

ISCHEMIA, PLASMID genetics, HEPATOCYTE growth factor, INTRAMUSCULAR injections, MYOCARDIAL revascularization, PAIN tolerance, FOLLOW-up studies (Medicine), DNA, GENE therapy

Abstract

We aimed to evaluate in a phase I dose-escalation study, the safety of intramuscular injections of a novel non-viral plasmid DNA expressing two isoforms of human hepatocyte growth factor (HGF) (VM202) in patients with critical limb ischemia (CLI). In total, 12 patients with CLI and unsuitable for revascularization were consecutively assigned to increasing doses (2 to 16 mg) of VM202 administered into the ischemic calf muscle at days 1 and 15. Patients were evaluated for safety and tolerability, changes in ankle- and toe brachial index (ABI and TBI), and pain severity score using a visual analog scale (VAS) throughout a 12-month follow-up period. Median age was 72 years and 53% of the patients were male. VM202 was safe and well tolerated with no death during the 12-month follow-up. Median ABI and TBI significantly increased from 0.35 to 0.52 (P=0.005) and from 0.15 to 0.24 (P=0.01) at 12 months follow-up. Median VAS decreased from 57.5 to 16.0 mm at 6 months follow-up (P=0.03). In this first human clinical trial, VM202, which expresses two isoforms of human HGF, appear to be safe and well tolerated with encouraging clinical results and thus supports the performance of a phase II randomized controlled trial. [ABSTRACT FROM AUTHOR]

Published

2011

9. Optimized planar Penning traps for quantum information studies.

Author

Goldman, J. and Gabrielse, G.

Subjects

*QUANTUM theory, *ION traps, *QUANTUM computers, *ELECTRON configuration, *ELECTRON capture, *NUCLEAR physics, *MATHEMATICAL optimization

Abstract

Single electron qubits are attractive for quantum information processing because they offer, for example, the possibility of extremely long coherence times. For scaling up to a large number of coupled qubits, an array of planar Penning traps is a much more promising option than the cylindrical Penning traps within which one-quantum transitions have been observed. This report summarizes optimized trap configurations, discussed at length in Goldman and Gabrielse (Phys Rev A 81:052335, ), which promise to make it possible to realize one-electron qubits in a scalable configuration for the first time. [ABSTRACT FROM AUTHOR]

Published

2011

10. Diverging effects of HLA-DPB1 matching status on outcome following unrelated donor transplantation depending on disease stage and the degree of matching for other HLA alleles.

Author

Shaw, B. E., Mayor, N. P., Russell, N. H., Apperley, J. F., Clark, R. E., Cornish, J., Darbyshire, P., Ethell, M. E., Goldman, J. M., Little, A.-M., Mackinnon, S., Marks, D. I., Pagliuca, A., Thomson, K., Marsh, S. G. E., and Madrigal, J. A.

Subjects

LEUKEMIA, HLA histocompatibility antigens, BONE marrow, CANCER patients, MULTIVARIATE analysis, LEUKEMIA treatment, ALLELES, COMPARATIVE studies, GRAFT versus host disease, HEMATOPOIETIC stem cell transplantation, HISTOCOMPATIBILITY testing, RESEARCH methodology, MEDICAL cooperation, ORGAN donors, RESEARCH, HLA-B27 antigen, DISEASE relapse, EVALUATION research

Abstract

Disease stage and recipient/donor human leukocyte antigen (HLA) matching are important determinants of outcome in transplantation using volunteer-unrelated donors (VUD). Matching for HLA-A, -B, -C, -DRB1, -DQB1 is beneficial, whereas the importance of DPB1 matching is more controversial. The impact of HLA matching status may differ dependent on disease stage. We investigated the outcome according to the degree of HLA matching at 6 loci, in 488 recipients of predominantly T-cell depleted bone marrow VUD transplants for leukaemia. Survival was significantly better in 12/12-matched transplants in those with early leukaemia (5 years: 63 versus 41% in 10/10 matched, P=0.006), but not late stage disease. Conversely, within the HLA-mismatched group (< or =9/10), there was a significant survival advantage to DPB1 mismatching (5 years: 39 versus 21% in DPB1 matched, P=0.008), particularly in late leukaemia (P=0.01), persisting in multivariate analysis (odds ratio 0.478; 95% confidence interval 0.30, 0.75; P=0.001). These novel findings suggest that the best outcome for patients with early leukaemia, with a 10/10-matched donor, is achieved by matching for DPB1. Conversely, our results suggest that in patients receiving an HLA-mismatched graft, the outcome is significantly better if they are also mismatched for DPB1. We recommend validation of these results in independent datasets. [ABSTRACT FROM AUTHOR]

Published

2010

11. Chronic myeloproliferative diseases with and without the Ph chromosome: some unresolved issues.

Author

Goldman, J. M., Green, A. R., Holyoake, T., Jamieson, C., Mesa, R., Mughal, T., Pellicano, F., Perrotti, D., Skoda, R., and Vannucchi, A. M.

Subjects

*CHRONIC myeloid leukemia, *LEUKEMIA, *PROTEIN-tyrosine kinases, *STEM cells, *CANCER

Abstract

Ph-positive chronic myeloid leukemia (CML) and Ph-negative chronic myeloproliferative diseases (MPDs), characterized in many cases by the presence of the JAK2V617F mutation, have many features in common and yet also show fundamental differences. In this review, we pose five discrete and related questions relevant to both categories of hematological malignancy, namely: What are the mechanisms that underlie disease progression from a relatively benign or chronic phase? By what therapeutic methods might one target residual leukemia stem cells in CML? Is JAK2V617F the original molecular event in MPD? What epigenetic events must have a role in dictating disease phenotype in MPDs? And finally, Will the benefits conferred by current or future JAK2V617F inhibitors equal or even surpass the clinical success that has resulted from the use of tyrosine kinase inhibitors in CML? These and others questions must be addressed and in some cases should be answered in the foreseeable future. [ABSTRACT FROM AUTHOR]

Published

2009

12. Recommendations for a standard UK approach to incorporating umbilical cord blood into clinical transplantation practice: conditioning protocols and donor selection algorithms.

Author

Shaw, B. E., Veys, P., Pagliuca, A., Addada, J., Cook, G., Craddock, C. F., Gennery, A. R., Goldman, J., Mackinnon, S., Madrigal, J. A., Marks, D. I., Navarrete, C., Potter, M. N., Querol, S., Regan, F., Russell, N. H., and Hough, R. E.

Subjects

UMBILICAL cord, HEMATOPOIETIC growth factors, CELL transplantation, BLOOD transfusion, BONE marrow transplantation

Abstract

Allogeneic haematopoietic cell transplantation is an established curative treatment modality for patients with malignant and non-malignant haematological disorders. Since the first related umbilical cord blood transplant (UCBT) in 1988, the use of UCB as a stem cell source for transplantation has become a standard practice in many countries, with approximately 8000 such transplants having been performed worldwide to date.Bone Marrow Transplantation (2009) 44, 7–12; doi:10.1038/bmt.2008.420; published online 12 January 2009 [ABSTRACT FROM AUTHOR]

Published

2009

13. Six-year follow-up of patients receiving imatinib for the first-line treatment of chronic myeloid leukemia.

Author

Hochhaus, A., O'Brien, S. G., Guilhot, F., Druker, B. J., Branford, S., Foroni, L., Goldman, J. M., Müller, M. C., Radich, J. P., Rudoltz, M., Mone, M., Gathmann, I., Hughes, T. P., and Larson, R. A.

Subjects

CHRONIC myeloid leukemia, IMATINIB, ANTINEOPLASTIC agents, INTERFERONS, GLYCOPROTEINS, PATIENTS

Abstract

Imatinib mesylate is considered standard of care for first-line treatment of chronic phase chronic myeloid leukemia (CML-CP). In the phase III, randomized, open-label International Randomized Study of Interferon vs STI571 (IRIS) trial, previously untreated CML-CP patients were randomized to imatinib (n=553) or interferon-α (IFN) plus cytarabine (n=553). This 6-year update focuses on patients randomized to receive imatinib as first-line therapy for newly diagnosed CML-CP. During the sixth year of study treatment, there were no reports of disease progression to accelerated phase (AP) or blast crisis (BC). The toxicity profile was unchanged. The cumulative best complete cytogenetic response (CCyR) rate was 82%; 63% of all patients randomized to receive imatinib and still on study treatment showed CCyR at last assessment. The estimated event-free survival at 6 years was 83%, and the estimated rate of freedom from progression to AP and BC was 93%. The estimated overall survival was 88%––or 95% when only CML-related deaths were considered. This 6-year update of IRIS underscores the efficacy and safety of imatinib as first-line therapy for patients with CML.Leukemia (2009) 23, 1054–1061; doi:10.1038/leu.2009.38; published online 12 March 2009 [ABSTRACT FROM AUTHOR]

Published

2009

14. BCR-ABL1-positive CML and BCR-ABL1-negative chronic myeloproliferative disorders: some common and contrasting features.

Author

Cross, N. C. P., Daley, G. Q., Green, A. R., Hughes, T. P., Jamieson, C., Manley, P., Mughal, T., Perrotti, D., Radich, J., Skoda, R., Soverini, S., Vainchenker, W., Verstovsek, S., Villeval, J.-L., and Goldman, J. M.

Subjects

MYELOPROLIFERATIVE neoplasms, CHRONIC myeloid leukemia, PROTEIN-tyrosine kinase inhibitors, CHRONIC leukemia, MYELOID leukemia, PROTEIN metabolism, TREATMENT of chronic myeloid leukemia, CHRONIC diseases, CLINICAL trials, GENETIC mutation, PROTEINS, THERAPEUTICS

Abstract

The article discusses the common and different features of BCR-ABL1-positive chronic myeloid leukemia (CML) and BCR-ABL1-negative chronic myeloproliferative disorders. The BCR-ABL1-positive and the JAK2-positive MPNs provide important information on the earliest stages of tumorigenesis. Moreover, study of their molecular pathogenesis shows their differences in certain cases like determining molecular abnormalities. Meanwhile, tyrosine kinase inhibitors (TKIs) has been effective in CML treatment.

Published

2008

15. Hematopoietic stem cells and progenitors of chronic myeloid leukemia express leukemia-associated antigens: implications for the graft-versus-leukemia effect and peptide vaccine-based immunotherapy.

Author

Yong, A. S. M., Keyvanfar, K., Eniafe, R., Savani, B. N., Rezvani, K., Sloand, E. M., Goldman, J. M., and Barrett, A. J.

Subjects

HEMATOPOIETIC stem cells, CHRONIC myeloid leukemia, MINOR histocompatibility antigens, IMMUNOTHERAPY, VACCINES, PROTEIN-tyrosine kinase inhibitors, PROTEIN analysis, ANTIGENS, HISTOCOMPATIBILITY antigens, STEM cells, TRANSPLANTATION immunology, TUMOR antigens, CANCER vaccines, CASE-control method

Abstract

The cure of chronic myeloid leukemia (CML) patients following allogeneic stem cell transplantation (SCT) is attributed to graft-versus-leukemia (GVL) effects targeting alloantigens and/or leukemia-associated antigens (LAA) on leukemia cells. To assess the potential of LAA-peptide vaccines in eliminating leukemia in CML patients, we measured WT1, PR3, ELA2 and PRAME expression in CD34+ progenitor subpopulations in CML patients and compared them with minor histocompatibility antigens (mHAgs) HA1 and SMCY. All CD34+ subpopulations expressed similar levels of mHAgs irrespective of disease phase, suggesting that in the SCT setting, mHAgs are the best target for GVL. Furthermore, WT1 was consistently overexpressed in advanced phase (AdP) CML in all CD34+ subpopulations, and mature progenitors of chronic phase (CP) CML compared to healthy individuals. PRAME overexpression was limited to more mature AdP-CML progenitors only. Conversely, only CP-CML progenitors had PR3 overexpression, suggesting that PR1-peptide vaccines are only appropriate in CP-CML. Surface expression of WT1 protein in the most primitive hematopoietic stem cells in AdP-CML suggest that they could be targets for WT1 peptide-based vaccines, which in combination with PRAME, could additionally improve targeting differentiated progeny, and benefit patients responding suboptimally to tyrosine kinase inhibitors, or enhance GVL effects in SCT patients. [ABSTRACT FROM AUTHOR]

Published

2008

16. Chronic myeloid leukemia – some topical issues.

Author

Mughal, T, Cortes, J, Cross, N C P, Donato, N, Hantschel, O, Jabbour, E, Kantarjian, H, Melo, J V, Skorski, T, Silver, R T, and Goldman, J M

Subjects

MYELOID leukemia, IMATINIB, PROTEIN-tyrosine kinases, TUMOR suppressor genes, HEART failure

Abstract

The article presents an editorial looking at chronic myeloid leukemia. The article discusses the part genomic instability plays in causing the BCR-ABL fusion, the PP2A tumor suppressor gene, resistance to imatinib mesylate, the possible association between imatinib mesylate and cardiac failure, the U.S. Food and Drug Administration's approval of dasatinib, and the therapeutic use of tyrosine kinase.

Published

2007

17. Response to donor lymphocyte infusions for chronic myeloid leukemia is dose-dependent: the importance of escalating the cell dose to maximize therapeutic efficacy.

Author

Simula, M. P., Marktel, S., Fozza, C., Kaeda, J., Szydlo, R. M., Nadal, E., Bua, M., Rahemtulla, A., Kanfer, E., Marin, D., Olavarria, E., Goldman, J. M., Apperley, J. F., and Dazzi, F.

Subjects

TREATMENT of chronic myeloid leukemia, LEUKEMIA, LYMPHOCYTES, INTERLEUKINS, LEUCOCYTES, PATIENTS

Abstract

Donor lymphocyte infusions (DLI) are an effective treatment for patients with chronic myeloid leukemia (CML) in relapse after allografting but the optimal cell dose has yet to be identified. To address this question, we investigated the factors affecting the dose required to achieve remission (effective cell dose, (ECD)) in 81 patients treated with an escalating dose regimen. The overall proportion of patients who achieved a molecular remission was 88%. The cumulative proportion of remitters increased significantly at each dose level. With a CD3+ cell dose 107/kg, 56% of patients in molecular/cytogenetic relapse obtained molecular remission, whereas only 20% of those in hematologic relapse did so. At the same cell dose, 58% of patients who received lymphocytes from volunteer unrelated donors achieved remission, as compared to 29% of those who received DLI from sibling donors. We conclude that the response to DLI is dose-dependent and that the ECD is influenced by the quantity and phase of CML at relapse and degree of donor/recipient histocompatibility.Leukemia (2007) 21, 943–948. doi:10.1038/sj.leu.2404641; published online 15 March 2007 [ABSTRACT FROM AUTHOR]

Published

2007

18. Rationale for the recommendations for harmonizing current methodology for detecting BCR-ABL transcripts in patients with chronic myeloid leukaemia.

Author

Branford, S., Cross, N. C. P., Hochhaus, A., Radich, J., Saglio, G., Kaeda, J., Goldman, J., and Hughes, T.

Subjects

CHRONIC myeloid leukemia, IMATINIB, POLYMERASE chain reaction, PATIENT monitoring, PLASMIDS, GENETIC testing

Abstract

Molecular monitoring for patients with chronic myeloid leukaemia (CML) has become an important practice in the era of imatinib therapy. For successful widespread introduction into the mainstream patient monitoring schedule, many procedural aspects of the complex real-time quantitative polymerase chain reaction (RQ-PCR) technique for measuring BCR-ABL transcripts require optimization. Recommendations for harmonizing the differing methodologies have recently been proposed. These recommendations were designed to maximize reliability of analysis for clinical decision making and proposed the adoption of an International Scale of measurement. The purpose of this review is to present the evidence and supporting data for specific recommendations. These recommendations include use of the same source of cells, either blood or marrow, for analysis; for validation of equal PCR amplification efficiencies of cDNA and standards when using a plasmid to construct standard curves and for ensuring ongoing high-level performance by undertaking a quality assurance programme. Clinicians must know the measurement reliability of an RQ-PCR assay to be able to determine the significance of a change in BCR-ABL level. An assay with poor precision limits the clinical usefulness of results. International harmonization should establish RQ-PCR measurement of BCR-ABL as the best method for monitoring treatment response for patients with CML.Leukemia (2006) 20, 1925–1930. doi:10.1038/sj.leu.2404388; published online 14 September 2006 [ABSTRACT FROM AUTHOR]

Published

2006

19. Topical issues in unrelated donor haematopoietic stem cell transplants: a report from a workshop convened by the Anthony Nolan Trust in London – 2005.

Author

Duarte, R F, Pamphilon, D, Cornish, J, Shaw, B E, Samson, D, Craddock, C, Marks, D, Mufti, G J, Powles, R L, Apperley, J F, Madrigal, J A, and Goldman, J M

Subjects

ORGAN donors, HEMATOPOIETIC stem cells, BONE marrow, ORGAN donation, TRANSPLANTATION of organs, tissues, etc., SEMINARS, CHARITABLE uses, trusts, & foundations

Abstract

Over more than three decades, The Anthony Nolan Trust (ANT) has provided an unrelated donor (UD) for over 4000 children and adults lacking a suitable family member donor, and has remained at the forefront of developments in haematopoietic stem cell transplantation (HSCT) and bone marrow register management. These three decades have seen major changes in clinical practice of UD-HSCT, including new indications, increased use of alternative haematopoietic cell sources, significant improvement of the outcome as a result of better support care, less-toxic conditioning regimens, and better donor selection, and expansion to older patients with higher comorbidities. In order to foster our goal of improving UD-HSCT availability and outcome in a progressively more complex clinical scenario, a new initiative from ANT was launched in 2005 to convene an experts workshop to address the topical issues in this field. Four consecutive panels addressed factors influencing donor selection and transplant outcome, the use of cord blood, regulatory and accreditation issues, and future developments in this field. This report summarizes the discussions held in this workshop, which will likely develop into a periodic event where transplant clinicians, scientists and registry members will meet to share their experience and vision in the field of UD-HSCT.Bone Marrow Transplantation (2006) 37, 901–908. doi:10.1038/sj.bmt.1705365 [ABSTRACT FROM AUTHOR]

Published

2006

20. The presence of a BCR-ABL mutant allele in CML does not always explain clinical resistance to imatinib.

Author

Khorashad, J. S., Anand, M., Marin, D., Saunders, S., Al-Jabary, T., Iqbal, A., Margerison, S., Melo, J. V., Goldman, J. M., Apperley, J. F., and Kaeda, J.

Subjects

CHRONIC myeloid leukemia, MYELOID leukemia, IMATINIB, GENETIC mutation, CLONE cells, CELL culture

Abstract

The expansion of a leukemia clone bearing a Bcr-Abl kinase domain mutation is associated with acquired resistance to imatinib and may also predict disease progression in patients with Philadelphia-positive chronic myeloid leukemia (CML). Here we report results of pyrosequencing to quantitate the non-mutated and mutant alleles in 12 CML patients monitored over periods ranging from 11 to 58 months, and describe three contrasting kinetic patterns: Group 1 – in four patients total BCR-ABL transcript numbers remained high with the mutant allele predominating; Group 2 – in four patients the total number of BCR-ABL transcripts fell to low levels but the mutant allele predominated; and Group 3 – in four other patients the total level of transcripts remained high (n=2) or fell (n=2) but the mutant clone persisted at relatively low level. In Group 2 the mutant leukemia clone was presumably still relatively sensitive to imatinib but in Group 1 the leukemia could be classified as resistant. In Group 3 patients the imatinib sensitivity of the leukemia was variable. We conclude that a mutant clone does not necessarily have a proliferative advantage and its presence does not always account for resistance to imatinib. Other mechanisms underlie resistance in at least some patients.Leukemia (2006) 20, 658–663. doi:10.1038/sj.leu.2404137; published online 9 February 2006 [ABSTRACT FROM AUTHOR]

Published

2006

21. Monitoring patients in complete cytogenetic remission after treatment of CML in chronic phase with imatinib: patterns of residual leukaemia and prognostic factors for cytogenetic relapse.

Author

Marin, D., Kaeda, J., Szydlo, R., Saunders, S., Fleming, A., Howard, J., Andreasson, C., Bua, M., Olavarria, E., Rahemtulla, A., Dazzi, F., Kanfer, E., Goldman, J. M., and Apperley, J. F.

Subjects

CHRONIC myeloid leukemia, PATIENT monitoring, HUMAN cytogenetics, DISEASE relapse, LEUKEMIA, IMATINIB, ANTINEOPLASTIC agents

Abstract

We monitored BCR-ABL transcript levels by quantitative real-time PCR in 103 patients treated with imatinib for chronic myeloid leukaemia in chronic phase for a median of 30.3 months (range 5.5-49.9) after they achieved complete cytogenetic remission (CCyR). The patients could be divided into three groups: (1) in 32 patients transcript levels continued to decline during the period of observation (nadir BCR-ABL/ABL ratio 0.015%); in five of these patients BCR-ABL transcripts became undetectable on repeated testing, (2) in 42 patients the transcript levels reached a plateau and (3) in 26 patients transcript numbers increased and the initial CCyR was lost. Three patients were not evaluable. Patients who remained in CCyR for at least 24 months appeared to have a low risk of subsequent cytogenetic relapse. We conclude that the pattern of‘residual’disease after achieving CCyR on imatinib is variable: some patients in CCyR show a progressive reduction in the level of residual disease, some reach a plateau where transcript numbers are relatively stable and others relapse with Ph-positive metaphases.Leukemia (2005) 19, 507-512. doi:10.1038/sj.leu.2403664 Published online 10 February 2005 [ABSTRACT FROM AUTHOR]

Published

2005

22. Autologous/syngeneic stem cell transplantation to treat refractory GvHD.

Author

Passweg, J. R., Orchard, K., Buergi, A., Gratwohl, A., Powles, R., Goldman, J., Apperley, J., and Mehta, J.

Subjects

GRAFT versus host disease, ADRENOCORTICAL hormones, STEM cell transplantation, TRANSPLANTATION of organs, tissues, etc., CELL transformation, BONE marrow transplant complications

Abstract

Summary:Severe graft-versus-host disease (GvHD) refractory to corticosteroids responds poorly to experimental treatment and is often fatal. Attempts have been made to‘rescue’such patients by transfusing autologous cells in order to ablate the lymphoid component of the graft or to introduce regulatory cells capable of suppressing the GvHD. Here, we report details of eight patients with severe grade III-IV acute GvHD (n=7) or extensive chronic GvHD (n=1) who after failing a median of four lines of treatment were then treated with either autologous or syngeneic nucleated cell transfusions. Patients received standard conditioning (n=3), low intensity (n=2) or no conditioning (n=3) before the rescue procedure. In four of the five patients who received some form of conditioning, mixed chimerism or complete recipient hematopoiesis was restored. The GvHD resolved in four patients, of whom one died subsequently of multiorgan failure and two died of leukemia; one is still alive. A fifth patient had transient improvement in GvHD, which recurred when the corticosteroids were reduced. Three patients obtained no benefit from the procedure. We conclude that‘rescue’by transfusion of autologous or syngeneic nucleated cells may be valuable to treat severe refractory GvHD; the best approach to conditioning remains to be defined.Bone Marrow Transplantation (2004) 34, 995-998. doi:10.1038/sj.bmt.1704658 Published online 18 October 2004 [ABSTRACT FROM AUTHOR]

Published

2004

23. Imatinib inhibits the activation and proliferation of normal T lymphocytes in vitro.

Author

Cwynarski, K., Laylor, R., Macchiarulo, E., Goldman, J., Lombardi, G., Melo, J. V., and Dazzi, F.

Subjects

IMATINIB, LYMPHOCYTE transformation, T cells, CELL transformation, CELL proliferation, STEM cell transplantation

Abstract

The ABL tyrosine kinase inhibitor imatinib mesylate is highly effective in the treatment of CML and is increasingly used in the stem cell transplantation (SCT) setting. Since ABL-dependent intracellular signaling molecules are involved in T-cell activation, imatinib may affect T-cell responses in vivo, thus affecting T-cell function in CML patients, disrupting immune reconstitution after allogeneic SCT and/or impeding the graft-versus-leukemia effect. Here we demonstrate that imatinib inhibits PHA-induced proliferation of normal peripheral blood mononuclear cells at in vitro concentrations (1-5?µmol/l) representative of the pharmacological doses used therapeutically in vivo. The effect is not dependent on antigen-presenting cells because CD3/CD28-induced T-cell stimulation was similarly inhibited by imatinib. Dose-dependent inhibition of the proliferative response of purified CD8+ and CD4+ T lymphocytes to anti-CD3/CD28 was similarly observed and associated with reduction in IFN-? production. The inhibitory effect could not be ascribed to an increased rate of apoptosis but the expression of activation markers on CD3+ T cells was significantly reduced in the presence of imatinib (1-5?µmol/L). Inhibition of T-cell proliferation was reversible after removal of the drug from the cultures. Thus, imatinib inhibits T-cell proliferation in vitro, an effect that is APC-independent, reversible, and does not involve apoptosis induction.Leukemia (2004) 18, 1332-1339. doi:10.1038/sj.leu.2403401 Published online 10 June 2004 [ABSTRACT FROM AUTHOR]

Published

2004

24. Efficacy of dual-specific Bcr-Abl and Src-family kinase inhibitors in cells sensitive and resistant to imatinib mesylate.

Author

Tipping, A. J., Baluch, S., Barnes, D. J., Veach, D. R., Clarkson, B. M., Bornmann, W. G., Mahon, F. X., Goldman, J. M., and Melo, J. V.

Subjects

MYELOID leukemia, PYRIMIDINES, HETEROCYCLIC compounds, DRUG resistance, THERAPEUTICS, NONLYMPHOID leukemia, BONE marrow diseases

Abstract

Monotherapy of chronic myeloid leukemia (CML) with imatinib mesylate has been cast into shadow by the evolution of clinical resistance during therapy. Resistance to imatinib can arise by multiple mechanisms including amplification or mutation of Bcr-Abl, and continuity of imatinib therapy is probably a poor option for either of these patient groups. Recently, however, a structurally distinct new class of drugs, the pyrido[2,3-d]pyrimidines, has been described, and these compounds are predicted to make different molecular contacts in the Abl kinase domain. These drugs potently target both the Bcr-Abl and Src-family kinase activities, both of which are thought to be relevant to survival of the leukemic cell. We asked whether these drugs could selectively induce cell death in murine cell line models of CML cells sensitive and resistant to imatinib by different mechanisms. We show that whereas the pyrido[2,3-d] pyrimidines are indeed highly potent in suppressing proliferation of Bcr-Abl-overexpressing imatinib-resistant cells, they are almost completely ineffective against cells expressing the T315I mutant. This implies that despite structural differences from imatinib, these drugs are unlikely to be useful in patients expressing this mutant Bcr-Abl protein, but may be effective in cases where selection of cells overexpressing the oncoprotein leads to refractoriness to imatinib. [ABSTRACT FROM AUTHOR]

Published

2004

25. Autologous stem cell transplantation normalizes abnormal bone remodeling and sRANKL/osteoprotegerin ratio in patients with multiple myeloma.

Author

Terpos, E., Politou, M., Szydlo, R., Nadal, E., Avery, S., Olavarria, E., Kanfer, E., Goldman, J. ., Apperley, J. F., and Rahemtulla, A.

Subjects

STEM cell transplantation, BONE remodeling, BONE metabolism, CELL transplantation, MULTIPLE myeloma, PLASMACYTOMA

Abstract

The osteoprotegerin (OPG)/receptor activator of NF-kappa B ligand (RANKL) system has a major role in the pathogenesis of bone disease in myeloma (MM). The effect of autologous stem cell transplantation (ASCT) on bone turnover in MM was evaluated in 51 patients (35M/16F). Markers of bone resorption (NTX, TRACP-5b), bone formation (bone-alkaline phosphatase (bALP), osteocalcin), OPG and sRANKL were measured pre- and every month post-ASCT. The median follow-up period was 12 months. Four patients were transplanted in CR, 44 were transplanted in PR and three patients had progressive/resistant disease. All patients received bisphosphonates both pre- and post-ASCT. At baseline the majority of patients had increased NTX, TRACP-5b levels, and sRANKL/OPG ratio, while markers of bone formation were strongly suppressed. ASCT produced a significant reduction of sRANKL/OPG ratio, with a concomitant decrease of NTX, and TRACP-5b levels, starting the second month post-ASCT. Bone formation markers, osteocalcin and bALP, started to increase after the 9th and 11th month post-ASCT, respectively, while the increase of OPG preceded this. These results provide biochemical evidence that ASCT normalizes the abnormal bone resorption in MM patients possibly through the decrease of RANKL/OPG ratio, while bone formation requires a longer period to return to normal.Leukemia (2004) 18, 1420-1426. doi:10.1038/sj.leu.2403423 Published online 24 June 2004 [ABSTRACT FROM AUTHOR]

Published

2004

26. Prognostic factors for patients with chronic myeloid leukaemia in chronic phase treated with imatinib mesylate after failure of interferon alfa.

Author

Marin, D, Marktel, S, Bua, M, Szydlo, R M, Franceschino, A, Nathan, I, Foot, N, Crawley, C, Na Nakorn, T, Olavarria, E, Lennard, A, Neylon, A, O'Brien, S G, Goldman, J M, and Apperley, J F

Subjects

MYELOID leukemia, IMATINIB, PROGNOSIS

Abstract

We assessed clinical results in 145 patients with chronic myeloid leukaemia in chronic phase who satisfied criteria for interferon-a failure and were thus eligible for treatment with imatinib at the Hammersmith Hospital. We used univariate and multivariate analyses to develop a risk score based on features defined after treatment for 3 months. We identified a low neutrophil count and poor cytogenetic response (<35% Ph-negative marrow metaphases) at 3 months as principal independent predictive factors and incorporated them into a three-tier prognostic scoring system for individual patients. For patients in the low-, intermediate- and high-risk groups, the probabilities of survival at 24 months were 100, 82 and 40% (P<0.0001) and progression-free survival 100, 66 and 15% (P<0.0001), respectively. This Hammersmith prognostic scoring system was validated with an independent cohort of patients treated at another UK centre. [ABSTRACT FROM AUTHOR]

Published

2003

27. The degree of matching at HLA-DPB1 predicts for acute graft-versus-host disease and disease relapse following haematopoietic stem cell transplantation.

Author

Shaw, B E, Potter, M N, Mayor, N P, Pay, A L, Smith, C, Goldman, J M, Prentice, H Grant, Marsh, S G E, and Madrigal, J A

Subjects

STEM cell transplantation, HLA histocompatibility antigens, GRAFT versus host disease, DISEASE relapse, COMPLICATIONS from organ transplantation

Abstract

Summary:The importance of matching for HLA-DPB1 in unrelated donor haematopoietic stem cell (HSC) transplantation is little understood. Most transplant centres do not, currently, prospectively match for DPB1, but emerging data show that DPB1 matching does play a role in determining outcome. We studied the impact of HLA-DPB1 matching on outcome in 143 recipients of T-cell depletion transplants, who matched with their respective unrelated donors (allelic level) at HLA-A, -B, -C, -DRB1 and -DQB1. Of those matched at DPB1, 47.2% (17/36) developed acute graft-versus-host disease (aGvHD) as compared to 66.3% (55/83) of those who were mismatched. This led to a 19.1% (95% CI 0.1-38.3%) increase in the chance of developing aGvHD in mismatched patients (P=0.049). Relapse of the original disease occurred in 51 recipients; 23 of 37 (62%) matched at both DPB1 alleles, 28 of 82 (34%) were mismatched at one or two DPB1 alleles. Thus, there was a significantly higher relapse rate (P=0.0011) in transplant recipients who matched at both DPB1 alleles. In conclusion, a donor/recipient DPB1 match was associated with a significantly lower incidence of aGvHD and a significantly higher incidence of disease relapse. This study provides further evidence for an immunogenic role of HLA-DPB1 in HSC transplants.Bone Marrow Transplantation (2003) 31, 1001-1008. doi:10.1038/sj.bmt.1704029 [ABSTRACT FROM AUTHOR]

Published

2003

28. Autologous stem cell transplantation in multiple myeloma: improved survival in nonsecretory multiple myeloma but lack of influence of age, status at transplant, previous treatment and conditioning regimen. A single-centre experience in 127 patients.

Author

Terpos, E, Apperley, J F, Samson, D, Giles, C, Crawley, C, Kanfer, E, Olavarria, E, Goldman, J M, and Rahemtulla, A

Subjects

MULTIPLE myeloma, AUTOTRANSPLANTATION, CELL transplantation

Abstract

High-dose therapy with autologous stem cell transplantation (ASCT) has become the treatment of choice for symptomatic eligible patients with multiple myeloma (MM). We report our centre experience and analyse retrospectively the prognostic influence of pretransplant characteristics and transplant modalities on response and survival. A total of 127 MM patients (median age: 55.2 years) were transplanted between 1994 and 2001. In all, 69 patients had IgG, 28 IgA, 23 light chain, one IgD and six non secretory MM. At the time of autograft, 6% of patients were in complete remission (CR), 73% in partial remission (PR), 12% showed minor response to previous treatment and 9% had stable or refractory disease. Prior to autograft, 79% of cases had received only one line of chemotherapy and 21% two or more lines. All patients received PBSC support after conditioning with 200?mg/m2 melphalan alone (100 patients) or melphalan and TBI (27 patients). We evaluated the influence of age (using as cutoff value the ages of 55, 60 and 65 years), type of MM, status pre- and post-ASCT, number of lines of previous regimens, time of ASCT from diagnosis, year of autograft, dose of reinfused CD34+ cells, plasma cell infiltration and ?2-microglobulin at diagnosis on overall (OS) and progression-free survivals (PFS) to define patients with better prognosis. Following ASCT, 15% of patients were in CR and 81% in PR, while only two patients progressed. Median OS and PFS from transplantation were 50.4 and 23.5 months, respectively. Median OS from diagnosis was 79.7 months. Transplant-related mortality was 2.3%. Low levels of ?2-microglobulin and the achievement of CR post-transplant correlated with longer PFS (P<0.03 and <0.01, respectively). The median PFS was 36.1, 23.9, 21.1 and 16.4 months for nonsecretory, IgG, IgA and light chain subtypes, respectively. Age was not an important prognostic factor at a cutoff value of 55 or 60 years. We conclude that... [ABSTRACT FROM AUTHOR]

Published

2003

29. Solid-State Silicon NMR Quantum Computer.

Author

Abe, E., Itoh, K., Ladd, T., Goldman, J., Yamaguchi, F., and Yamamoto, Y.

Abstract

A solid-state quantum computer composed entirely of semiconductor silicon is proposed. Qubits are nuclear spins, I = 1/2, of 29Si stable isotopes in the form of atomic chains embedded in a nuclear-spin free matrix of 28Si stable isotopes. Each 29Si nuclear spin in a chain can be accessed selectively with a different resonant frequency (rf) due to a large magnetic field gradient created by a nearby micromagnet, i.e., unitary operations needed for quantum computing can be performed by fine tuning of the rf. Ensemble readout of qubits from 105 copies of the atomic chain is accomplished by magnetic resonance force microscopy. [ABSTRACT FROM AUTHOR]

Published

2003

30. Drug responses of imatinib mesylate-resistant cells: synergism of imatinib with other chemotherapeutic drugs.

Author

Tipping, A J, Mahon, F X, Zafirides, G, Lagarde, V, Goldman, J M, and Melo, J V

Subjects

MYELOID leukemia, LEUKEMIA treatment, DRUG therapy, DRUG resistance

Abstract

Imatinib mesylate (STI571, Glivec, Gleevec) is a powerful inhibitor of the tyrosine kinase activity of Bcr-Abl, the oncoprotein responsible for chronic myeloid leukemia (CML). The drug shows great efficacy in chronic phase, but is less effective in maintaining hematologic remissions in blast crisis patients. Our group has previously described several cell lines made resistant to imatinib. We now examine the question of cross-resistance to other chemotherapeutic drugs used in CML. Four paired imatinib-sensitive/resistant CML cell lines were assessed by caspase-3 and MTS assays for their proliferative response to cytosine arabinoside (Ara-C), daunorubicin (DNR), homoharringtonine (HHT) and hydroxyurea (HU), either alone or in combination with imatinib. Primary blasts from advanced-stage CML patients refractory to imatinib therapy were studied by semi-solid media clonogenic assays. We found that these drugs are generally capable of major inhibition of proliferation of the CML cell lines, although differential responses to DNR and HHT were noted between some sensitive and resistant cell line pairs, implying that resistance to imatinib may confer a growth advantage under such conditions. The four drugs were also effective in preventing the formation of progenitor cell colonies from CML patients both before treatment with imatinib, and after relapse on the drug. Isobolographic analysis implied that these drugs will generally combine well with imatinib, and in some cases will be synergistic. We conclude that Ara-C, DNR or HHT, either alone or in combination with imatinib, are likely to be the best therapeutic alternatives in the management of patients who become resistant to imatinib monotherapy.Leukemia (2002) 16, 2349–2357. doi:10.1038/sj.leu.2402775 [ABSTRACT FROM AUTHOR]

Published

2002

31. Mecamylamine (Inversine®): an old antihypertensive with new research directions.

Author

Shytle, R.D., Penny, E., Silver, A.A., Goldman, J., and Sanberg, P.R.

Subjects

MECAMYLAMINE, SMOKING prevention

Abstract

Reviews the research available regarding the possible use of mecamylamine as an aid to smoking cessation. Proposed testable hypotheses that could be studies in recalcitrant smokers with mild to moderate hypertension; Mecamylamine as the first orally available ganglionic blocker developed for severe hypertension.

Published

2002

32. A possible role of initial cell death due to mechanical stretch in the regulation of subsequent cell proliferation in experimental vein grafts.

Author

Liu, S. Q., Ruan, Y. Y., Tang, D., Li, Y. C., Goldman, J., and Zhong, L.

Abstract

The proliferation of vascular cells contributes to the formation of neointima and hypertrophy of the blood vessel wall. Here we show that mechanical stretch possibly regulates the proliferation of vascular cells via the mediation of cell death in a rat vein graft model. The wall of vein grafts is subject to a suddenly increased mechanical stretch due to exposure to arterial blood pressure. Such a stretch induces rapid cell death with a reduction in cell density by ∼60% within the first day after surgery. The initial cell death was followed by an increase in the percentage of proliferating cells, as shown by a BrdU incorporation assay (1.55 ± 1.27%, 8.48 ± 2.27%, 11.93 ± 2.36%, 6.36 ± 1.77%, and 5.60 ± 1.46% at days 1, 5, 10, 20, and 30, respectively). When mechanical stretch was reduced by restraining the vein graft using a polytetrafluoroethylene sheath, the percentage of proliferating cells reduced significantly (0.76 ± 0.76%, 1.70 ± 0.46%, 1.29 ± 0.56%, 0.99 ± 0.83%, and 0.47±0.52% at days 1, 5, 10, 20, and 30, respectively). A further reduction in cell density, induced by local administration of a cell death inducer ceramide to experimental vein grafts (without sheath), enhanced subsequent cell proliferation. In contrast, a prevention of cell death, induced by local administration of a cell death inhibitor tetrapeptide-aldehyde DEVD-CHO to experimental vein grafts (without sheath), significantly reduced subsequent cell proliferation. These results suggest that mechanical stretch induces cell death, which possibly mediates subsequent cell proliferation in the present model. [ABSTRACT FROM AUTHOR]

Published

2002

33. Immune haemolytic anaemia following T cell-depleted allogeneic bone marrow transplantation for chronic myeloid leukaemia: association with leukaemic relapse and treatment with donor lymphocyte infusions.

Author

Cwynarski, K, Goulding, R, Pocock, C, Dazzi, F, Craddock, C, Kaeda, J, Olavarria, E, Kanfer, E, Apperley, J, Lawler, M, and Goldman, J M

Subjects

HEMOLYTIC anemia, T cells, BONE marrow transplantation, MYELOID leukemia, LYMPHOCYTES

Abstract

Immune haemolytic anaemia (IHA) is a recognised complication after allogeneic stem cell transplantation (SCT) and occurs more frequently if marrow cells have been subjected to T cell depletion (TCD). Among 58 consecutive patients who underwent TCD-allogeneic SCT from volunteer unrelated donors for the treatment of CML at the Hammersmith Hospital during a 3-year period (1 March 1996 to 28 February 1999) we identified nine cases of IHA. All patients had a strongly positive direct and indirect antiglobulin test and in eight patients the serological findings were typical of warm-type haemolysis often with antibody specificities within the Rh system. All nine cases had clinically significant haemolysis and were treated initially with prednisolone and immunoglobulin. The onset of IHA coincided with the occurrence of leukaemic relapse in six cases, and the presence of host haemopoiesis confirmed by lineage-specific chimerism in all four cases studied. Five patients received donor lymphocyte infusions (DLI); in three molecular remission and the restoration of full donor chimerism coincided with resolution of haemolysis. We conclude that in the context of leukaemic relapse, DLI is an effective therapy for IHA following allografts involving TCD. Bone Marrow Transplantation (2001) 28, 581–586. [ABSTRACT FROM AUTHOR]

Published

2001

34. Peripheral blood progenitor cell mobilisation alters myeloid, but not erythroid, progenitor cell self-renewal kinetics.

Author

Marley, S B, Lewis, J L, Zheng, B, Davidson, R J, Davis, J G, McDonald, C, Alenzi, F Q B, Goldman, J M, and Gordon, M Y

Subjects

MYELOID metaplasia, ERYTHROCYTES, BONE marrow transplantation

Abstract

Transplantation of progenitor cells which have been mobilised into the bloodstream (PBPC) following the administration of G-CSF results in more rapid neutrophil recovery than transplantation of bone marrow (BM). The reasons for the accelerated neutrophil engraftment are not clear, but would be explained by increased self-replication of myeloid progenitor cells (CFU-GM). We have used a CFU-GM replating assay to investigate myeloid progenitor self-replication, and quantification of subcolony formation during erythroid burst formation to quantify erythroid progenitor self-renewal. Secondary colony formation by CFU-GM, grown from PBPC and then replated was increased compared with secondary colony formation by BM CFU-GM (P = 0.0001); erythroid subcolony formation was not altered. There was no difference between the replating abilities of PBPC CFU-GM derived from allogeneic donors (normal individuals) and autologous donors (patients with malignant disease) although differences were found between subgroups of autologous donors. The increased replication of PBPC could not be accounted for by a reduction in progenitor cell apoptosis; PBPC CFU-GM contained slightly fewer apoptotic CD34+ cells than BM CFU-GM. The increased replication by PBPC CFU-GM was reversible because it declined when CFU-GM colonies were passaged through three sequential CFU-GM replating cycles. This decline in self-replication was more rapid than the decline seen in replated BM CFU-GM. The self-replication of PBPC CFU-GM, and subcolony formation by BFU-E could be further enhanced by exposure to cytokines in vitro. We conclude that mobilisation alters the replication kinetics of myeloid, but not of erythroid, progenitor cells, that mobilisation-induced events are of limited duration and that in vitro exposure to cytokines may modify PBPC progenitor cell kinetics. Bone Marrow Transplantation (2001) 27, 241–248. [ABSTRACT FROM AUTHOR]

Published

2001

35. A phase I/II study of multiple-dose intravenous busulfan as myeloablation prior to stem cell transplantation.

Author

Olavarria, E, Hassan, M, Eades, A, Nilsson, C, Timms, A, Matthews, J, Craddock, C, Kanfer, E, Apperley, J, and Goldman, J

Subjects

STEM cell transplantation, DRUG dosage

Abstract

Busulfan has been previously only available in an oral formulation due to its poor water solubility. We report the results of a phase I study of multiple escalating doses of intravenous busulfan (Spartaject Busulfan, Orphan Europe, Paris, France) for myeloablation prior to stem cell transplantation (SCT) in 12 patients with chronic myeloid leukemia, acute myeloid leukemia or acute lymphocytic leukemia. One patient received allogeneic SCT; the other 11 patients received autologous SCT. The first six patients received i.v. busulfan diluted in 50 ml of 0.9% normal saline and the last six patients received busulfan in a 500-ml 5% dextrose solution. All patients experienced profound myelosuppression and all but one demonstrated hematopoietic engraftment. Toxicity was mild or moderate and there were no toxic deaths attributable to busulfan. Of note, there were no cases of veno-occlusive disease of the liver. Busulfan plasma concentrations were determined by gas chromatography with electron capture detection and showed little intrapatient variability. In most cases there was no significant difference between the first and last dose PK parameters. These data suggest that dose adjustment based on first dose PK data could allow uniformity of busulfan dosing for patients receiving SCT. [ABSTRACT FROM AUTHOR]

Published

2000

36. Masimo signal extraction pulse oximetry.

Author

Goldman, Julian, Petterson, Michael, Kopotic, Robert, Barker, Steven, Goldman, J M, Petterson, M T, Kopotic, R J, and Barker, S J

Abstract

Objective.To describe a new pulse oximetry technology and measurement paradigm developed by Masimo Corporation. Introduction.Patient motion, poor tissue perfusion, excessive ambient light, and electrosurgical unit interference reduce conventional pulse oximeter (CPO) measurement integrity. Patient motion frequently generates erroneous pulse oximetry values for saturation and pulse rate. Motion-induced measurement error is due in part to wide spread implementation of a theoretical pulse oximetry model which assumes that arterial blood is the only light-absorbing pulsatile component in the optical path. Methods.Masimo Signal Extraction Technology(SET®) pulse oximetry begins with conventional red and infrared photoplethysmographic signals, and then employs a constellation of advanced techniques including radiofrequency and light-shielded optical sensors, digital signal processing, and adaptive filtration, to measure SpO2 accurately during challenging clinical conditions. In contrast to CPO which calculates O2 saturation from the ratio of transmitted pulsatile red and infrared light, Masimo SET pulse oximetry uses a new conceptual model of light absorption for pulse oximetry and employs the discrete saturation transform (DST) to isolate individual “saturation components” in the optical pathway. Typically, when the tissue under analysis is stationary, only the single saturation component produced by pulsatile arterial blood is present.In contrast, during patient motion, movement of non-arterial components (for example, venous blood) can be identified as additional saturation components (with a lower O2 saturation). When conditions of the Masimo model are met, the saturation component corresponding to the highest O2 saturation is reported by the instrument as SpO2. Conclusion.The technological strategies implemented in Masimo SET pulse oximetry effectively permit continuous monitoring of SpO2 during challenging clinical conditions of motion and poor tissue perfusion. [ABSTRACT FROM AUTHOR]

Published

2000

37. Combination of interferon alpha with either Ara-C or ATRA in vitro reduces the selective action of interferon against CML CFU-GM.

Author

Marley, S B, Davidson, R J, Goldman, J M, and Gordon, M Y

Subjects

MYELOID leukemia, INTERFERONS

Abstract

Although interferon (IFN)-alpha has no specific inhibitory effect on the plating efficiency of granulocyte-macrophage colony-forming cells (CFU-GM) from patients with chronic myeloid leukaemia (CML), it does selectively inhibit the replating ability (secondary colony formation) of CML CFU-GM. Thus, amplification of CFU-GM may be a target for IFN-alpha and other agents used in the treatment of CML. Here we examined whether cytarabine (Ara-C) or all-trans retinoic acid (ATRA) exert similar effects and whether they might in combination with IFN-alpha enhance its efficacy. We found that Ara-C preferentially inhibits the formation of CML CFU-GM compared to normal CFU-GM, but this inhibition was not increased by addition of IFN-alpha. When Ara-C was added to cultures containing IFN-alpha, the inhibition of replating by CML progenitors was abrogated. ATRA increased significantly the plating efficiency of normal CFU-GM. The addition of IFN-alpha to ATRA had no effect on CML or normal colony numbers. However, addition of ATRA to cultures containing IFN-alpha reversed the selective inhibition of CML CFU-GM replating seen in cultures containing IFN-alpha alone. In four IFN-alpha/Ara-C experiments, secondary CML patient-derived colonies were examined by fluorescence in situ hybridisation (FISH). All of them were Ph chromosome positive. No significant effects on CFU-GM production were observed when CML primitive haemopoietic progenitor cells were investigated in a delta (delta) assay. Thus we conclude that combining IFN-alpha with Ara-C or ATRA neutralises the effect of IFN-alpha on CML CFU-GM. This observation provides a rationale for treating patients with alternating courses of IFN-alpha and Ara-C or ATRA, rather than giving either of these two agents in combination with IFN-alpha. [ABSTRACT FROM AUTHOR]

Published

2000

38. Identification of PML/RARalpha rearrangements in suspected acute promyelocytic leukemia using fluorescence in situ hybridization of bone marrow smears: a comparison with cytogenetics and RT-PCR in MRC ATRA trial patients. MRC Adult Leukaemia Working Party.

Author

Iqbal, S, Grimwade, D, Chase, A, Goldstone, A, Burnett, A, Goldman, J M, and Swirsky, D

Subjects

LETTERS to the editor, PERIODICALS

Abstract

Presents several letters to the editor published in the May 2000 issue of the periodical 'Leukemia.' Identification of PML/RARα rearrangements in suspected acute promyelocytic leukemia using fluorescence in situ hybridization of bone marrow smears; Administration of low-dose melphalan in elderly acute myeloid leukemia.

Published

2000

39. Cytogenetic status pre-transplant as a predictor of outcome post bone marrow transplantation for chronic myelogenous leukaemia.

Author

Konstantinidou, P, Szydlo, R M, Chase, A, and Goldman, J M

Subjects

CYTOGENETICS, MYELOID leukemia, BONE marrow transplantation, CHROMOSOMES, DISEASE relapse

Abstract

We have analysed pre-transplant cytogenetic findings in 418 patients with CML in pre-blastic phase who underwent allogeneic BMT between February 1981 and January 1998. Five different patient groups were identified: A = Philadelphia (Ph)+; B = Ph-, BCR-ABL+; C = variant Ph (VPh); D = Ph chromosome plus at least one of: trisomy 8, +Ph, chromosome 17 abnormalities and E = other abnormalities in addition to the Ph chromosome. There were two principal conclusions. Firstly, Ph- patients showed a better outcome, and VPh patients a worse outcome, than those with a standard Ph, both in terms of leukaemia-free survival (LFS) (76.9%, 22.1% and 31.9%) and the risk of treatment failure relative to those with a standard Ph (relative risks of 0.49 and 1.92, respectively). One contributing factor may be relapse: no Ph- patients relapsed, whereas all other groups showed similar probabilities of relapse at 5 years (range 33.0–44.0%). Secondly, those with the additional changes of +8, +Ph and i(17q) did not show a worse outcome than those with no additional changes (5 year survival of 44.7% vs 51.8%; 5 year LFS of 40.6% vs 31.9%), whereas those with other additional changes may fare worst of all (40.4% and 16.0%, respectively). Bone Marrow Transplantation (2000) 25, 143–146. [ABSTRACT FROM AUTHOR]

Published

2000

40. Liposomal amphotericin (AmBisome) in the prophylaxis of fungal infections in neutropenic patients: a randomised, double-blind, placebo-controlled study.

Author

Kelsey, S M, Goldman, J M, McCann, S, Newland, A C, Scarffe, J H, Oppenheim, B A, and Mufti, G J

Subjects

*LIPOSOMES, *NEUTROPENIA, *PLACEBOS

Abstract

Liposomal amphotericin (AmBisome) 2 mg/kg three times weekly was compared with placebo as prophylaxis against fungal infection in patients undergoing chemotherapy or bone marrow transplantation (BMT) for haematological malignancies. Prophylaxis began on day 1 of chemotherapy and continued until neutrophils regenerated or infection was suspected. Of 161 evaluable patients, 74 received AmBisome and 87 received placebo. Proven fungal infections developed in no patients on AmBisome and in three on placebo (3.4%) (P = NS). Suspected fungal infections requiring intervention with systemic antifungal therapy (usually amphotericin B) occurred in 31 patients on AmBisome (42%) and in 40 on placebo (46%) (P = NS). Suspected deep-seated infections developed in 21 (28.3%) and 31 (35.6%) patients, respectively (P = NS). Time to develop a suspected or proven deep-seated infection showed a trend in favour of AmBisome (P = 0.11). Fifty patients had fungal colonisation (48 with Candida spp, two with Aspergillus spp) of at least one body site during prophylaxis; 15 patients while receiving AmBisome (20%) and 35 while on placebo (40%) (P < 0.01). time to colonisation was significantly delayed in the group receiving ambisome (P < 0.05). treatment-related toxicity was modest and no additional toxicity was observed in patients receiving ambisome. ambisome 2 mg/kg three times weekly is safe and reduces fungal colonisation in patients receiving intensive chemotherapy or bmt. however, despite encouraging trends, prophylactic ambisome did not lead to a significant reduction in fungal infection or in requirement for systemic antifungal therapy. [ABSTRACT FROM AUTHOR]

Published

1999

41. Cell biology of CML cells.

Author

Gordon, M. Y., Dazzi, F., MarleY, S. B., Lewis, J. L., Nguyen, D., Grand, F. H., Davidson, R. J., and Goldman, J. M.

Subjects

CHRONIC myeloid leukemia, CANCER cells, HEMATOPOIESIS, APOPTOSIS, CHRONIC leukemia, CYTOLOGY

Abstract

At the cellular level, expansion of haemopoiesis in chronic myeloid leukaemia (CML) must involve some imbalance in cell production along the myeloid maturation pathway. The relevant kinetic parameters are cell loss by apoptosis and differentiation and cell gain by proliferation (self-renewal). In spite of the predominance of the BCR-ABL-positive leukaemic cells, some BCR-ABL-negative, presumably normal, progenitor cells remain for long periods in chronic phase CML. Thus, understanding the kinetics of CML and normal progenitor cells may lead to therapeutic strategies capable of reducing malignant cell growth and reactivating normal haemopoiesis. [ABSTRACT FROM AUTHOR]

Published

1999

42. A comparison of prophylactic vs pre-emptive ganciclovir to prevent cytomegalovirus disease after T-depleted volunteer unrelated donor bone marrow transplantation.

Author

Stocchi, R, Szydlo, R, Craddock, C, Kanfer, E, Apperley, J F, Goldman, J M, and Ward, K N

Subjects

CYTOMEGALOVIRUS diseases, BONE marrow transplantation

Abstract

The prophylactic and pre-emptive use of ganciclovir (GCV) both reduce significantly the incidence of CMV disease after sibling BMT but it is unclear which of these strategies is best for volunteer unrelated donor (VUD) BMT patients. We reviewed 49 consecutive patients, who received a T-depleted VUD BMT (from March 1990 to March 1996) for the treatment of CML in chronic phase, and were CMV seropositive before transplant or had a CMV seropositive donor. Patients were conditioned with cyclophosphamide (120 mg/kg for 2 days) and total body irradiation (13.2–14.4 Gy). Prophylaxis for GVHD was cyclosporin A and methotrexate with ex vivo or in vivo T cell depletion. Twenty-seven patients received pre-emptive GCV if CMV infection was detected by short-term culture before day +120 post BMT. Twenty-two patients received prophylactic GCV from engraftment until day +120 post BMT. The probabilities of CMV infection and disease occurring by 1 year post-BMT were greater in the pre-emptive GCV group than in the prophylactic GCV group (73.8% and 64.0% vs 53.1% and 30.0%, respectively; P = 0.04 and 0.07). The incidence of death from CMV disease was similar in both groups (3/12 (25%) vs 3/10 (30%), respectively) and there was no difference in 1 year survival (55.6% vs 54.2%, respectively). New strategies are urgently required for the prevention of CMV disease after T-depleted VUD BMT. [ABSTRACT FROM AUTHOR]

Published

1999

43. Optimal timing for processing and cryopreservation of umbilical cord haematopoietic stem cells for clinical transplantation.

Author

Shlebak, A A, Marley, S B, Roberts, I A G, Davidson, R J, Goldman, J M, and Gordon, M Y

Subjects

CORD blood, CRYOPRESERVATION of organs, tissues, etc.

Abstract

Some of the factors that may influence the number and quality of cord blood haematopoietic progenitor cells available for transplantation have been investigated including site of collection, delayed processing after collection and cryopreservation protocol. We used the granulocyte–macrophage progenitor (CFU-GM) and erythroid burst-forming unit (BFU-E) assays to quantify progenitors. The capacity of CFU-GM to produce secondary colonies was used as a measure of progenitor cell quality. We found that: (1) there were no significant differences in total nucleated cells (TNC), mononuclear cells (MNC), CFU-GM or BFU-E numbers in paired specimens from the umbilical vein or veins at the base of the placenta. The potential of the CFU-GM to produce secondary colonies from the two sites was similar; (2) storing cord blood at room temperature or at 4°C resulted in a significant reduction in progenitor cell numbers beyond 9 h; and (3) cryopreservation following either controlled rate freezing or passive cooling reduced MNC numbers, viability and CFU-GM survival insignificantly but the potential of CFU-GM to produce secondary colonies was significantly reduced post cryopreservation (P = 0.04). We conclude that the yield of CB progenitor cells is not affected by the site of collection, but is adversely affected by delays between collection and cryopreservation. Furthermore, cryo- preservation reduced the CFU-GM potential to produce secondary colonies. Measures of progenitor cell quality as well as quantity may be relevant to assessing CB blood collections. [ABSTRACT FROM AUTHOR]

Published

1999

44. Improvement of depression following transcranial magnetic stimulation.

Author

George, Mark, Nahas, Ziad, Kozel, F., Goldman, Juliet, Molloy, Monica, Oliver, Nicholas, George, M S, Nahas, Z, Kozel, F A, Goldman, J, Molloy, M, and Oliver, N

Subjects

BRAIN physiology, CEREBRAL cortex, THERAPEUTICS, MENTAL depression, NEURAL physiology, COMPARATIVE studies, ELECTROTHERAPEUTICS, RESEARCH methodology, MEDICAL cooperation, RESEARCH, RESEARCH funding, SCALP, TRANSCRANIAL magnetic stimulation, EVALUATION research

Abstract

Psychiatry as a field was transformed by the discovery and introduction of electroconvulsive therapy (ECT) as a treatment in the early part of this century. ECT demonstrated that depression was a disease of the brain and that it could be treated with a direct brain intervention. Psychiatry's evolution continued in 1958 with the discovery of the antidepressant activity of the monoamine oxidase inhibitors. Interestingly, although the area of neuropsychopharmacology has continued to advance, the realm of physical somatic interventions in psychiatry has lagged behind. With perhaps the exception of light therapy, there were no advances in somatic interventions in psychiatry. However, in 1985, Barker et al. developed a brief high intensity electromagnet capable of depolarizing cortical neurons, called transcranial magnetic stimulation (TMS). There has been much interest in the past 10 years in whether TMS might have antidepressant actions, similar to ECT but without causing a seizure and with no apparent cognitive side effects. This review examines the basic principles underlying TMS, and describes how TMS differs from electrical stimulation and the other uses of magnets. [ABSTRACT FROM AUTHOR]

Published

1999

45. Allogeneic and autologous transplantation for haematological diseases, solid tumours and immune disorders: current practice in Europe in 1998.

Author

Goldman, J M, Schmitz, N, Niethammer, D, and Gratwohl, A

Subjects

*GRAFT versus host disease, *AUTOTRANSPLANTATION, *BONE marrow transplantation, *HEMATOPOIETIC stem cell transplantation

Abstract

In 1996, the Accreditation Sub-Committee of the EBMT published a special report summarising current practice in Europe in relation to haemopoietic stem cell transplants for haematological diseases, solid tumours and immune disorders. An updated report is presented here. The major change has been the recognition that transplant practice is appreciably different between children and adults, who should therefore be considered in separate categories. The autoimmune disorders for which autografting may be useful are now specified. Non-CML myeloproliferative disorders and AL amyloidosis have been added to the list of indications for transplant procedures in adults. Other changes have been incorporated into the revised tables. [ABSTRACT FROM AUTHOR]

Published

1998

46. Brief child assessment battery to assist with treatment planning and program evaluation.

Author

Goldman J, Sorensen E, and Ward M

Abstract

A brief battery of self-report measures was constructed to discriminate effectively 45 matched clinic versus nonclinic subjects, ages 8 to 15. The battery consisted of measures from six domains, including externalizing problems, child and parent report of internalizing problems, peer relations, school functioning, and family relationships. Data on subjects and their families were provided by various sources, including parents, teachers, and the children. In an effort to facilitate interpretation and use of this information by unsophisticated staff, within domain scores were converted to bivariate risk scores. Results indicated effective classification (82%) of groups using the bivariate risk scores alone. This constituted only a small loss of information when the risk scores replaced t-scores. Implications for the use of the risk scores to facilitate treatment planning and program evaluation are discussed. [ABSTRACT FROM AUTHOR]

Published

1995

47. BCR/ABL-negative progenitors are enriched in the adherent fraction of CD34+ cells circulating in the blood of chronic phase chronic myeloid leukemia patients.

Author

Grand, F H, Marley, S B, Chase, A, Titley, I, Healy, L, Spencer, A, Reiter, A, Goldman, J M, and Gordon, M Y

Subjects

LEUKEMIA, CANCER cells

Abstract

Philadelphia chromosome-positive (Ph+) hemopoietic cells predominate in patients with chronic myeloid leukemia (CML) in chronic phase, but some Ph presumably normal stem cells persist in most patients. Ph cells are relatively frequent, compared to mature cell populations, in primitive hemopoietic cell populations from CML patients. We have purified CD34+ cells from chronic phase CML blood and separated them into two fractions on the basis of adherence or non-adherence to tissue culture plastic. We also separated CD34+ CML cell populations into HLA-DR(hi) and HLA-DR(lo) fractions and CD38(hi) and CD38(lo) fractions by flow cytometry. The CD34+ cells that adhered to plastic were predominantly CD33-, CD38- and HLA(-)-DR; cells with these phenotypic properties were significantly rarer in the CD34+ non-adherent cell population (P = 0.008-0.02). Expression of p210 BCR/ABL mRNA by adherent, non-adherent, HLA-DR(hi) and HLA-DR(lo)CD34+ cell subpopulations was demonstrated by RT-PCR. Using fluorescence in situ hybridization (FISH) in conjunction with BCR and ABL probes we detected Ph+ and Ph- cells in both adherent and non-adherent CD34+ cell fractions of 15/15 patients studied and in the HLA-DR(lo) or CD38(lo) sorted CD34+ cell fractions. The concentration of Ph- cells in the adherent CD34+ cell fraction was three-fold higher than in the non-adherent fraction (P = 0.001). Ph- adherent cells were detected in untreated CML patients and as late as 6 years after diagnosis of CML in patients treated with hydroxyurea (HU) or interferon-alpha (IFN-alpha). We conclude that whilst appreciable numbers of Ph- primitive hemopoietic progenitors are present in the circulation in untreated patients and also in treated patients in late chronic phase, the majority of cells expressing CD34 but not CD33, CD38 or HLA-DR antigens, are part of the CML clone. [ABSTRACT FROM AUTHOR]

Published

1997

48. Rarity of dominant-negative mutations of the G-CSF receptor in patients with blast crisis of chronic myeloid leukemia or de novo acute leukemia.

Author

Carapeti, M, Soede-Bobok, A, Hochhaus, A, Sill, H, Touw, I P, Goldman, J M, Cross, N C P, and Cross, N C

Subjects

GENETIC mutation, MYELOID leukemia, PATIENTS

Abstract

It is likely that leukemia results, at least in part, from mutations that lead to a block in the normal process of differentiation. A defined region of the cytoplasmic domain of the granulocyte colony-stimulating factor receptor (G-CSF-R) transmits signals for maturation or differentiation of myeloid progenitor cells. Mutations in this region have been found in some patients with severe congenital neutropenia (SCN) who subsequently evolved to acute myeloid leukemia (AML). To determine if mutations of the G-CSF-R are more widespread in hematological malignancies, we have investigated a total of 47 patients, including 29 patients with blast crisis of chronic myeloid leukemia (CML-BC) and 18 patients with de novo acute leukemia as well as 19 normal controls, by RT-PCR and SSCP analysis. Two point mutations were found in a single individual with secondary AML (FAB type M1). The first was heterozygous and is predicted to replace the normal glutamine at position 718 with a stop codon, leading to a truncated protein. An identical mutation has been described previously and shown to act in a dominant negative manner. The second mutation was homozygous and would substitute a lysine for the normal glutamic acid at position 785. No mutations were found in any other patient or control samples. We conclude that mutations in the cytoplasmic domain of the G-CSF-R are infrequent in CML-BC or acute leukemia but may contribute to malignant transformation in some cases. [ABSTRACT FROM AUTHOR]

Published

1997

49. Expression of interferon regulatory factor (IRF) genes and response to interferon-alpha in chronic myeloid leukaemia.

Author

Hochhaus, A, Yan, X H, Willer, A, Hehlmann, R, Gordon, M Y, Goldman, J M, and Melo, J V

Subjects

INTERFERONS, GENES, MYELOID leukemia, ANTINEOPLASTIC agents, TREATMENT of chronic myeloid leukemia, RNA analysis, COMPARATIVE studies, DOCUMENTATION, GENE expression, RESEARCH methodology, MEDICAL cooperation, NUCLEOTIDES, PHOSPHOPROTEINS, PROTEINS, RESEARCH, TRANSCRIPTION factors, DNA-binding proteins, EVALUATION research, CHRONIC myeloid leukemia

Abstract

Interferon regulatory factors (IRF) 1 and 2 are DNA-binding proteins which control interferon (IFN) gene expression. IRF1 functions as an activator for IFN and IFN-inducible genes, whereas IRF2 represses the action of IRF1. Expression of the two regulatory genes is itself IFN-inducible. Because therapeutic responses of chronic myeloid leukaemia (CML) patients to IFN-alpha may be determined by intracellular levels of these two mutually antagonistic transcription factors, we have devised a competitive reverse-transcription polymerase chain reaction (RT-PCR) assay which provides an estimate of the ratio of IRF1 to IRF2 expression in a given cell population. Analysis of peripheral blood leucocytes from 25 normal individuals showed that the IRF1:IRF2 ratio varied between 1.13 and 2.30 (mean +/- s.d. 1.49 +/- 0.33). Similar values were obtained for normal bone marrow specimens, with no significant difference between CD34+ and CD34- cells. In contrast, the IRF1:IRF2 ratio in leucocytes from CML patients showed a much wider variation (0.53-5.11). Eleven out of 130 patients in chronic phase had ratios above the normal range, whereas none of the 33 blast crisis samples had a ratio >2.5. Analysis of diagnostic specimens in 59 CML patients treated subsequently with IFN-alpha showed a high IRF1:IRF2 ratio of 5.11 in one of two patients who became complete responders; all the 53 patients with minimal or no cytogenetic response had ratios below 2.5. In a separate series of 97 CML patients studied after IFN-alpha therapy a highly significant correlation was found between the IRF1:IRF2 ratio and both the cytogenetic and the molecular response (ie low concentration of BCR-ABL transcripts) to treatment: 53 out of 115 prospectively analysed samples of good cytogenetic responders had ratios above 2.0, as opposed to only 13 out of 91 samples from poor responders (P < 0.0001; chi2 test). We conclude that a high ratio of IRF1/IRF2 expression may be associated with good cytogenetic and molecular response to IFN-alpha in CML. [ABSTRACT FROM AUTHOR]

Published

1997

50. Clonal instability preceding lymphoid blastic transformation of chronic myeloid leukemia.

Author

Spencer, A, Vulliamy, T, Kaeda, J, Goldman, J M, and Melo, J V

Subjects

POLYMERASE chain reaction, MYELOID leukemia, IMMUNOGLOBULIN genes, BLOOD cells, BONE marrow, CELLS, COMPARATIVE studies, DNA, GENES, GENETICS, IMMUNOGLOBULINS, RESEARCH methodology, MEDICAL cooperation, PROTEINS, RESEARCH, STEM cells, EVALUATION research, CHRONIC myeloid leukemia, RETROSPECTIVE studies, DISEASE progression

Abstract

We have sought the presence of rearrangements of the immunoglobulin heavy chain gene locus in 13 patients with chronic myeloid leukemia (CML) in lymphoid blastic transformation (L-BT) using the polymerase chain reaction (PCR). The lymphoid nature of the transformation was confirmed by immunophenotyping and/or Southern blot hybridization with a J(H) probe. Clonal rearrangements were detected in 85% of cases and two or more rearrangements were visible in 64% of informative cases. The pattern of V(H) gene family utilization revealed an apparent reduction in V(H)4 family gene usage but otherwise reflected the known proportion of each gene family in the germline repertoire. In six cases the third complementary determining regions (CDR3) of the predominant blast crisis clone/s were sequenced revealing minimal evidence of somatic mutation. No clonal changes were detected in the chronic phase leukemia cells collected more than 6 months before the onset of L-BT in three of these patients. Of the other three patients studied in chronic phase from 1 to 6 months before L-BT, two showed clonal rearrangements which differed in size from those present at L-BT. In one patient a V(H)3 to V(H)5-D(H)-J(H) substitution had occurred at least 3 months prior to L-BT. In the other patient, however, the sequence of the rearrangement present 5 months prior to L-BT was unrelated to the rearrangements at the time of L-BT indicating a pattern of clonal succession. We conclude that: (1) IgH gene rearrangements are detectable in the majority of patients with L-BT using PCR and the lymphoid lineage of blastic CML is most readily confirmed using consensus primers to the framework 3 region; (2) somatic mutation is uncommon; and (3) B lymphoid clones distinct from those identified later may be detected before overt lymphoid BT. The identification of such 'abortive' clones is evidence for clonal instability before the onset of transformation and might have prognostic value. [ABSTRACT FROM AUTHOR]

Published

1997