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5. Clearance of marrow infiltration after 1 week of therapy for childhood lymphoblastic leukaemia: clinical importance and the effect of daunorubicin. The Medical Research Council's Working Party on Childhood Leukaemia

Author

Lilleyman, JS, Gibson, BE, Stevens, RF, Will, AM, Hann, IM, Richards, SM, and Hill, FG

Abstract

At the commencement of UKALL XI, a national MRC trial for childhood lymphoblastic leukaemia (ALL), the therapy included a bolus of daunorubicin (DR) on the first 2 d of the protocol. This component of treatment was subsequently withdrawn because of concern about long-term cardiotoxicity. All children both before and after this change of policy had their marrow status at the end of the first week assessed by central review as part of the trial to examine the clinical importance of the rate of disease clearance. This also afforded an opportunity to observe the effect of DR on gross residual disease at an early stage of therapy. 1419 children were studied: 342 received DR ('recipients'), 1077 did not. 44% of the recipients completely cleared their marrow of blast cells after 8 d compared with 13% of the non-recipients (chi2 = 158.2, P < 0.0001). The difference in the proportion with massive residual disease (>80% blasts) was less impressive but there was still a difference in favour of DR recipients (DR 9%, no DR 15%; chi2 = 7.7, P = 0.006). The rate of disease clearance correlated with disease-free survival for both recipients and non-recipients, but there was no significant difference in outcome when comparing the two groups with each other, either in terms of disease-free or relapse-free survival. DR accelerated the rate of blast cell disappearance from the marrow but the difference this made to disease free survival is small or non-existent. It appears to be the relative speed of response to a given therapeutic regimen that is prognostically important rather than the absolute rate of response when comparing one treatment with another.

Published
2016

8. Results of treatment of children with refractory anaemia with excess blasts (RAEB) and RAEB in transformation (RAEBt) in Great Britain 1990-99

Author

Webb, DK, Passmore, SJ, Hann, IM, Harrison, G, Wheatley, K, and Chessells, JM

Abstract

Between 1990 and 1999, 36 children with refractory anaemia with excess blasts (RAEB) and RAEB in transformation (RAEBt), not associated with Down's syndrome, were diagnosed in Britain. A total of 31 children received intensive chemotherapy, six of whom proceeded to a bone marrow allograft in first remission, whereas two received an autograft. Of the 23 given chemotherapy only, four died of toxicity, 10 relapsed and nine are alive in first remission. Out of the 10 who relapsed, four are alive and disease-free following an allograft. Out of the 6 children given an allograft in first remission, two died of disease and four are alive in first remission. Both children given an autograft died of disease. Two children received an allograft without prior chemotherapy but died of toxicity. Three children received supportive care only, and one child survived. The overall survival was 51% at 5 years, and was superior in children with RAEBt (63%) compared with RAEB (28%, P = 0.03). Cytogenetics were available in 35 cases. Monosomy 7 was the most common abnormality (33% of cases). Survival in children with monosomy 7 was 22% at 5 years compared with 66% for the other patients (P = 0.05). Allowing for cytogenetics, outcomes of therapy appear similar to those for de novo acute myeloid leukaemia (AML), and it is appropriate for children with RAEB/RAEBt to be registered in AML trials.

Published
2016

9. Analysis of the immunophenotype of children treated on the Medical Research Council United Kingdom Acute Lymphoblastic Leukaemia Trial XI (MRC UKALLXI). Medical Research Council Childhood Leukaemia Working Party

Author

Hann, IM, Richards, SM, Eden, OB, and Hill, FG

Abstract

Despite many years of meticulous immunophenotyping of childhood acute lymphoblastic leukaemia (ALL) cases the prognostic significance of some subtypes remains unclear. The Medical Research Council UKALLXI trial (1990-1996) in which uniform treatment has been given to 2090 children with ALL below the age of 18 years and above the age of 1 year, has afforded the opportunity to review these issues. Children with ALL of mature B cell type were not entered into this trial. Immunophenotype analysis was performed in each individual trial centre, but results were centrally reviewed in all cases, and were both available and considered adequate in 1934 (93%) of the first 2090 patients entered. The main diagnostic categories were early pre-B or null reported in 60 cases (3.1%), common ALL in 1242 (64.2%), pre-B in 252 (13.0%), 'common' or pre-B in 172 (8.9%) and T cell in 207 (10.7%) cases. Children with T cell disease were significantly more likely to be over the age of 10 years, with central nervous system disease at diagnosis and to be CD34 negative. They also had a higher incidence of high white cell count and were more likely to be of the French-American-British (FAB) L2 morphological subtype. Patients with 'null' cell disease tended to be less than 2 years or greater than 10 years of age, and CD13 and CD33 positive. CD10 was associated with lower white cell count (WBC) at diagnosis, younger age and FAB L1 morphological subtype. The presence of cytoplasmic immunoglobulin in pre-B cells was not associated with any specific clinical or laboratory features. CD34 positivity was less common in T cell patients and was associated with low WBC. Disease-free survival (DFS) and 95% confidence intervals (CI) at 5 years from diagnosis was 52% (95% CI: 44-59%) for T cell disease, 58% (95% CI: 43-73%) for early pre-B (or null cell) disease and 65% (95% CI: 62-68%) for common or pre-B disease; there being no significant difference between common and pre-B disease with regard to disease outcome. Patients with T cell disease had a worse prognosis than any other immunophenotype group (P < 0.00005). However this worse outcome was no longer significant after allowing for the other principal prognostic factors of age, gender and white cell count at diagnosis except for the very small number with WBC

Published
2016

10. Intraocular relapse of childhood acute lymphoblastic leukaemia

Author

Somervaille, TC, Hann, IM, Harrison, G, Eden, TO, Gibson, BE, Hill, FG, Mitchell, C, Kinsey, SE, Vora, AJ, and Lilleyman, JS

Abstract

Relapse of childhood acute lymphoblastic leukaemia (ALL) involving the eye is a rare but challenging problem. Twenty cases occurred in patients treated on the Medical Research Council United Kingdom Acute Lymphoblastic Leukaemia XI and ALL97 trials between 1991 and 2001, representing 2.2% of ALL relapses. Seventeen occurred as a first relapse, either in isolation or combined with relapse at another site, and three occurred as a second relapse. All patients with intraocular disease at first relapse were treated with both chemotherapy and radiotherapy, but the doses and protocols used varied. Eleven of these 17 patients are alive and in complete remission with a median follow up of 4 years 2 months from relapse. All 11 children that were treated with a full chemotherapy relapse protocol, together with local radiotherapy have survived. Patients treated with chemotherapy of shorter duration and intensity, despite radiotherapy and/or bone marrow transplantation, did poorly with only one survivor, currently in chronic relapse. Consequently, we suggest that children with eye relapse of ALL be treated with an intensive relapse chemotherapy protocol with local ocular radiotherapy, whether the relapse occurs in isolation or in combination with relapse at another site.

Published
2016

11. Predicting microbiologically defined infection in febrile neutropenic episodes in children: global individual participant data multivariable meta-analysis

Author

Phillips, RS, Sung, L, Amman, RA, Riley, RD, Castagnola, E, Haeusler, GM, Klaassen, R, Tissing, WJE, Lehrnbecher, T, Chisholm, J, Hakim, H, Ranasinghe, N, Paesmans, M, Hann, IM, Stewart, LA, Phillips, RS, Sung, L, Amman, RA, Riley, RD, Castagnola, E, Haeusler, GM, Klaassen, R, Tissing, WJE, Lehrnbecher, T, Chisholm, J, Hakim, H, Ranasinghe, N, Paesmans, M, Hann, IM, and Stewart, LA

Abstract

BACKGROUND: Risk-stratified management of fever with neutropenia (FN), allows intensive management of high-risk cases and early discharge of low-risk cases. No single, internationally validated, prediction model of the risk of adverse outcomes exists for children and young people. An individual patient data (IPD) meta-analysis was undertaken to devise one. METHODS: The 'Predicting Infectious Complications in Children with Cancer' (PICNICC) collaboration was formed by parent representatives, international clinical and methodological experts. Univariable and multivariable analyses, using random effects logistic regression, were undertaken to derive and internally validate a risk-prediction model for outcomes of episodes of FN based on clinical and laboratory data at presentation. RESULTS: Data came from 22 different study groups from 15 countries, of 5127 episodes of FN in 3504 patients. There were 1070 episodes in 616 patients from seven studies available for multivariable analysis. Univariable analyses showed associations with microbiologically defined infection (MDI) in many items, including higher temperature, lower white cell counts and acute myeloid leukaemia, but not age. Patients with osteosarcoma/Ewings sarcoma and those with more severe mucositis were associated with a decreased risk of MDI. The predictive model included: malignancy type, temperature, clinically 'severely unwell', haemoglobin, white cell count and absolute monocyte count. It showed moderate discrimination (AUROC 0.723, 95% confidence interval 0.711-0.759) and good calibration (calibration slope 0.95). The model was robust to bootstrap and cross-validation sensitivity analyses. CONCLUSIONS: This new prediction model for risk of MDI appears accurate. It requires prospective studies assessing implementation to assist clinicians and parents/patients in individualised decision making.

Published
2016

12. Predicting microbiologically defined infection in febrile neutropenic episodes in children: global individual participant data multivariable meta-analysis (vol 114, pg 623, 2016)

Author

Phillips, RS, Sung, L, Ammann, RA, Riley, RD, Castagnola, E, Haeusler, GM, Klaassen, R, Tissing, WJE, Lehrnbecher, T, Chisholm, J, Hakim, H, Ranasinghe, N, Paesmans, M, Hann, IM, Stewart, LA, Phillips, RS, Sung, L, Ammann, RA, Riley, RD, Castagnola, E, Haeusler, GM, Klaassen, R, Tissing, WJE, Lehrnbecher, T, Chisholm, J, Hakim, H, Ranasinghe, N, Paesmans, M, Hann, IM, and Stewart, LA

Published
2016

14. The United Kingdom Childhood Cancer Study: objectives, materials and methods. UK Childhood Cancer Study Investigators

Author

Boulton, A, Boyd, P, Cheng, KK, Cook, J, Gilman, EA, Lunt, D, Mahler, H, Walker, C, Wardroper, M, Darbyshire, PJ, Hill, FGH, Mann, JR, Morland, B, Raafat, F, Stevens, MCG, Ahmed, A, Amos, P, Bone, V, Bonney, S, Bray, M, Cambouropoulos, P, Cook, S, Day, N, Elkins, S, Hensel, F, Lucas, P, Pettinger, J, Pugsley, M, Ruja, E, Skinner, J, Williams, D, Braodbent, V, Williams, M, Alcock, M, Bell, K, Buchan, M, Cartwright, R, Cusack, H, Fear, N, Griffiths, S, Jarvis, J, Johnson, P, Kane, E, Law, G, Moorman, A, Prajapati, J, Roberts, P, Roman, E, Simpson, J, Sinclair, V, Staines, A, Thackrah, C, Thistlethwaite, S, Waller, B, Bailey, C, Kinsey, S, Lewis, I, Picton, S, Squire, R, Taylor, R, Beck, JM, Doran, RML, Livingston, JH, Van Hille, P, Beddis, I, Cameron, MM, Craft, A, Hale, J, Kernahan, J, Reid, M, Windebank, K, Pearson, A, Skinner, R, Marks, S, Achilles, J, Alam, S, Birch, JM, Blair, V, Buckley, B, Clarkson, M, Eden, OB, Howell, S, Kellaway, C, Lashford, L, Leeke, S, Leggett, P, Murphy, AV, O'Rorke, C, Panton, S, Paxon, J, Pots, H, Roberts, C, Rothwell, J, Stephenson, W, Whelpton, B, Caswell, M, McDowell, H, Pizer, BL, Gattamaneri, R, Brock, J, Kelsey, AM, Stevens, R, Will, A, Brennan, B, Brydon, J, Dodds, C, Findlay, E, Finucane, J, Fraser, J, Harkness, E, Heary, A, Hunter, N, Juszczak, E, Lang, M, Lapsley, E, McArthur, A, MacCalman, A, McKinney, PA, Proudfoot, K, Smith, C, Smith, K, Stockton, D, Thomson, CS, Vickers, R, Wilkie, R, King, D, Mackinlay, G, Shaw, P, Thomas, A, Wallace, H, Carachi, R, Gibson, BS, Simpson, E, Cruickshank, G, Hide, TAH, Gregor, A, Steers, AJW, Barrett, A, Hamblen, DL, Kaye, SB, Mackie, R, Allen, A, Jones, AA, Beeby, S, Bignall, V, Breeze, L, Deacon, J, MacDonald, M, Matthews, F, Meggitt, C, Peto, J, Sharpe, E, Spencer, C, Swales, J, Thorne, M, Trowbridge, P, Webster-King, J, Williams, E, Bell, BA, Johnston, FG, Marsh, HT, Uttley, D, Bartlett, J, Evans, A, Gullan, RW, Glaser, MG, Peterson, D, Southcott, BM, Cavanagh, N, Pearl, K, Scott, D, Darby, CW, Chessels, J, Evans, J, Gaze, M, Hann, IM, Harkness, W, Hayward, R, Michalski, A, Passmore, J, Phillips, M, Pritchard, J, Clark, KGA, MacDonald, EA, Neville, BGR, Robb, SA, Robinson, RO, Hardwidge, C, Padgham, N, Lobo, VJ, Keen, C, Hindmarsh, PC, Kilby, AM, Souhami, RL, Tuft, S, Thomas, RM, Ward, P, Scott, M, Hoffbrand, AV, Prentice, HG, Gutteridge, CG, Newland, AC, Brada, M, Henk, JM, Meller, S, Pinkerton, R, Jones, KP, Cannon, S, Murrell, DS, Hungerford, JL, Kingston, JE, Plowman, PN, Young, B, Ball, SE, Capps, SNJ, Davies, EG, Holmes, SJK, Carr, R, Mercer, DM, Smith, MA, Andrews, VE, Hughes, RG, Ansell, P, Baker, K, Beral, V, Black, J, Boon, S, Burge, C, Burge, F, Cliff, A, Deciaccio, D, Dorman, P, Heydon, F, Langley, N, Pelerin, M, Roemmele, J, Sayers, K, Townshend, P, Harman, S, Loftus, J, Roth, S, Lee, B, Buchdahl, R, Dunger, DB, Mitchell, C, Moncrieff, MKM, Tam, PKH, Wheeler, K, Reiser, J, Joss, V, Moir, DJ, Darmady, J, Daish, P, Liberman, MM, Al-Izzi, MS, Adams, CBT, Kerr, RSC, Teddy, PJ, Barton, CJ, Newman, CL, Gabriel, CM, O'Hea, M, Sherrin, S, Watson, A, Douek, E, Connell, JA, Kelly, S, Beswick, A, Eldridge, B, Elwood, P, Hughes, J, Webb, D, Alexander, FE, Bennett-Lloyd, B, Davis, A, Dunn, R, Little, J, Longdon, S, Mitchell, M, Muir, S, Sturitis, J, Kennedy, C, Kohler, J, Lang, D, Radford, M, Foreman, N, Foot, A, Mott, M, Noblett, H, Oakhill, A, Sandeman, D, Baumer, J, McNinch, A, Gilbertson, N, Bosley, A, Richardson, S, Challacombe, D, French, T, Bate, L, Chilvers, CED, Faulkner, G, Hawtin, P, Jenkinson, C, Kelham, P, Mackie, I, Mackie, M, Muir, KR, O'Dwyer, J, Williams, A, Nelson, C, Howarth, C, Madi, M, Shannon, R, Forman, K, Hewitt, M, Punt, J, Walker, D, Gerrard, M, Lilleyman, JS, Vora, A, Draper, G, Harrison, C, Doll, R, Richards, S, Ayres, M, Carter, R, Dearden, SP, Hussain, A, Kennedy, J, Ravetto, P, Ruprai, A, Taylor, GM, Taylor, J, Watson, PD, Colman, SM, Greaves, MF, Price, CM, Goodhead, DT, Allen, S, Bartlett, D, Blackwell, RP, Fry, F, Maslanyj, M, Mee, T, Miles, J, Adams, G, and Investigat, UKCCS

Abstract

An investigation into the possible causes of childhood cancer has been carried out throughout England, Scotland and Wales over the period 1991-1998. All children known to be suffering from one or other type of the disease over periods of 4-5 years have been included, and control children matched for sex, age and area of residence have been selected at random from population registers. Information about both groups of children (with and without cancer) has been obtained from parental questionnaires, general practitioners' and hospital records, and from measurement of the extent of exposure to radon gas, terrestrial gamma radiation, and electric and magnetic fields. Samples of blood have also been obtained from the affected children and their parents and stored. Altogether 3,838 children with cancer, including 1,736 with leukaemia, and 7,629 unaffected children have been studied. Detailed accounts are given of the nature of the information obtained in sections describing the general methodology of the study, the measurement of exposure to ionizing and non-ionizing radiation, the classification of solid tumours and leukaemias, and the biological material available for genetic analysis.

Published
2000

19. Enrichment of pluripotent hemopoietic progenitor cells from human bone marrow

Author

Bodger, MP, Hann, IM, Maclean, RF, and Beard, ME

Abstract

Pluripotent hemopoietic progenitor cells (CFU-GEMM, cells forming mixed hemopoietic colonies in methylcellulose) from human bone marrow were enriched 90-fold by positive selection on the fluorescence-activated cell sorter using monoclonal antibody RFB-1. Bone marrow cells were separated by cell size, using log 90 degrees light scatter, and the cell fraction containing CFU-GEMM was further separated by relative fluorescence intensity for the RFB-1 antigen. Further enrichment, up to 150-fold, was achieved by depleting bone marrow of T cells and mature myeloid cells prior to RFB-1 selection. These procedures yield a cell fraction containing 51% blast cells, 2% promyelocytes, and 47% undifferentiated (lymphocyte-like) mononuclear cells, although only 1% of the cells formed a mixed colony. CFU-GEMM are strongly positive for the RFB-1 antigen, whereas morphologically identifiable erythroblasts, myeloblasts, and promyelocytes are weakly RFB-1+. This suggests that the relative concentration of the RFB-1 antigen on bone marrow cells is inversely related to their maturity. The greatly increased recovery of CFU-GEMM after the separation of bone marrow by log 90 degrees light scatter and the removal of T cells and mature myeloid cells suggested that accessory cells that normally regulate the cloning efficiency of CFU-GEMM were removed.

Published
1984
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20. Development of pluripotent hematopoietic progenitor cells in the human fetus

Author

Hann, IM, Bodger, MP, and Hoffbrand, AV

Abstract

Pluripotent hematopoietic progenitor cells (CFU-GEMM), myeloid progenitor cells (CFU-GM), and erythroid progenitors (BFU-E) were studied in midtrimester human fetuses using the mixed colony assay. All three progenitor cell populations were detected at high levels in the fetal liver from 12 to 23 wk of gestation. Stem cells were first observed in the bone marrow at 15–16 wk of gestation, although bone marrow cultures from earlier fetuses showed heavy growths of stromal cells. Spleen cultures first showed growth of stem cells at 18–19 wk, but fetal thymus showed no hematopoietic activity. Peripheral blood from four fetuses aged 13, 18, 20, and 21 wk showed very high levels of all 3 progenitor cells. The results demonstrate that hematopoietic development in the human fetus parallels that of the mouse. The observation that stromal cell development in the bone marrow precedes the appearance of hematopoietic progenitor cells suggests that they may be closely involved in stem cell growth.

Published
1983
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24. Two novel activating mutations in the Wiskott-Aldrich syndrome protein result in congenital neutropenia.

Author

Ancliff PJ, Blundell MP, Cory GO, Calle Y, Worth A, Kempski H, Burns S, Jones GE, Sinclair J, Kinnon C, Hann IM, Gale RE, Linch DC, and Thrasher AJ

Subjects
Animals, Bone Marrow Cells cytology, Bone Marrow Cells metabolism, COS Cells, Cell Proliferation, Child, Child, Preschool, Chlorocebus aethiops, Humans, Leukocyte Elastase metabolism, Lymphocytes cytology, Male, Neutropenia metabolism, U937 Cells, Wiskott-Aldrich Syndrome Protein metabolism, Mutation, Neutropenia congenital, Neutropenia genetics, Wiskott-Aldrich Syndrome Protein genetics
Abstract

Severe congenital neutropenia (SCN) is characterized by neutropenia, recurrent bacterial infections, and maturation arrest in the bone marrow. Although many cases have mutations in the ELA2 gene encoding neutrophil elastase, a significant proportion remain undefined at a molecular level. A mutation (Leu270Pro) in the gene encoding the Wiskott-Aldrich syndrome protein (WASp) resulting in an X-linked SCN kindred has been reported. We therefore screened the WAS gene in 14 young SCN males with wild-type ELA2 and identified 2 with novel mutations, one who presented with myelodysplasia (Ile294Thr) and the other with classic SCN (Ser270Pro). Both patients had defects of immunologic function including a generalized reduction of lymphoid and natural killer cell numbers, reduced lymphocyte proliferation, and abrogated phagocyte activity. In vitro culture of bone marrow progenitors demonstrated a profound reduction in neutrophil production and increased levels of apoptosis, consistent with an intrinsic disturbance of normal myeloid differentiation as the cause of the neutropenia. Both mutations resulted in increased WASp activity and produced marked abnormalities of cytoskeletal structure and dynamics. Furthermore, these results also suggest a novel cause of myelodysplasia and that male children with myelodysplasia and disturbance of immunologic function should be screened for such mutations.

Published
2006
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25. Treatment for myeloid leukaemia of Down syndrome: population-based experience in the UK and results from the Medical Research Council AML 10 and AML 12 trials.

Author

Rao A, Hills RK, Stiller C, Gibson BE, de Graaf SS, Hann IM, O'Marcaigh A, Wheatley K, and Webb DK

Subjects
Adolescent, Amsacrine administration & dosage, Child, Child, Preschool, Cytarabine administration & dosage, Cytogenetic Analysis, Daunorubicin administration & dosage, Down Syndrome mortality, Drug Administration Schedule, Etoposide administration & dosage, Female, Humans, Infant, Leukemia, Myeloid mortality, Leukocyte Count, Male, Mitoxantrone administration & dosage, Thioguanine administration & dosage, Treatment Outcome, United Kingdom, Antineoplastic Combined Chemotherapy Protocols therapeutic use, Down Syndrome complications, Down Syndrome drug therapy, Leukemia, Myeloid complications, Leukemia, Myeloid drug therapy
Abstract

Down syndrome (DS) children are at an increased risk of developing myelodysplasia and acute myeloid leukaemia (AML). We retrospectively analysed the population-based data on 81 children with myeloid leukaemia of Down syndrome (ML-DS) from the UK National Registry of Childhood Tumours and experience in the Medical Research Council (MRC) AML 10 and AML 12 trials, which enrolled 46 children with ML-DS from 1988 to 2002. Eight per cent of UK children with AML had DS, but DS children comprised only 5% of children registered in MRC trials. The unique clinical characteristics of ML-DS were confirmed. Overall survival (OS) of ML-DS at 5 years increased from 47% in UK children diagnosed from 1988 to 1995 to 75% in children diagnosed from 1996 to 2002. OS for DS children registered in AML 10 and AML 12 was 74% in 5 years and improved from AML 10 to AML 12 (56% vs. 83%) There was no significant difference in OS between DS and non-DS children (OS: 74% vs. 62%, P = 0.4) in the trials, but this result masked a significant increase in early death amongst DS children, with a significant reduction in mortality later on. Relapse was significantly reduced (3% vs. 39%, P = 0.0003), leading to the improved disease-free survival (83% vs. 56%, P = 0.02). Given the increased number of early treatment-related deaths, future treatment protocols should aim to reduce chemotherapy dosage or intensity whilst maintaining low rates of resistant and recurrent disease.

Published
2006
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26. Treatment strategy and long-term results in paediatric patients treated in consecutive UK AML trials.

Author

Gibson BE, Wheatley K, Hann IM, Stevens RF, Webb D, Hills RK, De Graaf SS, and Harrison CJ

Subjects
Acute Disease, Adolescent, Antineoplastic Combined Chemotherapy Protocols toxicity, Bone Marrow Transplantation mortality, Central Nervous System Neoplasms drug therapy, Central Nervous System Neoplasms prevention & control, Child, Child, Preschool, Dose-Response Relationship, Drug, Follow-Up Studies, Humans, Infant, Infant, Newborn, Injections, Spinal, Leukemia, Myeloid mortality, Remission Induction methods, Risk Assessment, Survival Analysis, Treatment Outcome, Antineoplastic Combined Chemotherapy Protocols therapeutic use, Antineoplastic Protocols standards, Leukemia, Myeloid therapy
Abstract

Between 1988 and 2002, 758 children with acute myeloid leukaemia (AML) were treated on Medical Research Council (MRC) AML 10 and AML 12. MRC AML 10 tested the role of bone marrow transplantation following four blocks of intensive chemotherapy and found that while both allogeneic bone marrow transplant (allo-BMT) and autologous bone marrow transplant (A-BMT) significantly reduced the relapse risk (RR), this did not translate into a significant improvement in overall survival (OS). A risk group stratification based on cytogenetics and response to the first course of chemotherapy derived from MRC AML 10 was used to deliver risk-directed therapy in MRC AML 12. Allo-BMT was limited to standard and poor risk patients and A-BMT was not employed. Instead, the benefit of an additional block of treatment was tested by randomising children to receive either four or five blocks of treatment in total. While the results of MRC AML 12 remain immature, there appears to be no survival advantage for a fifth course of treatment. The 5 year OS, disease-free survival (DFS), event-free survival (EFS) and RR in MRC AML 12 are 66, 61, 56 and 35%, respectively; at present superior to MRC AML 10, which had a 5-year OS, DFS, EFS and RR of 58, 53, 49 and 42%, respectively. MRC AML trials employ a short course of triple intrathecal chemotherapy alone for CNS-directed treatment and CNS relapse is uncommon. Improvements in supportive care have contributed to improved outcomes and the number of deaths in remission fell between trials. Anthracycline-related cardiotoxicity remains a concern and the current MRC AML 15 trial tests the feasibility of reducing anthracycline dosage without compromising outcome by comparing standard MRC anthracycline-based consolidation with high-dose ara-C. MRC studies suggest that the role of allo-BMT is limited in 1st CR and that there may be a ceiling of benefit from current or conventional chemotherapy.

Published
2005
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27. Prospective gene expression analysis accurately subtypes acute leukaemia in children and establishes a commonality between hyperdiploidy and t(12;21) in acute lymphoblastic leukaemia.

Author

van Delft FW, Bellotti T, Luo Z, Jones LK, Patel N, Yiannikouris O, Hill AS, Hubank M, Kempski H, Fletcher D, Chaplin T, Foot N, Young BD, Hann IM, Gammerman A, and Saha V

Subjects
Acute Disease, Analysis of Variance, Child, Chromosome Banding, Core Binding Factor Alpha 2 Subunit, DNA-Binding Proteins genetics, Diagnosis, Differential, Gene Rearrangement, Humans, Immunophenotyping, In Situ Hybridization, Fluorescence, Karyotyping, Leukemia genetics, Leukemia, Myeloid diagnosis, Leukemia, Myeloid genetics, Nuclear Proteins genetics, Ploidies, Precursor Cell Lymphoblastic Leukemia-Lymphoma diagnosis, Principal Component Analysis, Prospective Studies, Proto-Oncogene Proteins genetics, Proto-Oncogene Proteins c-ets, Repressor Proteins genetics, Reproducibility of Results, Reverse Transcriptase Polymerase Chain Reaction, Telomeric Repeat Binding Protein 2 genetics, Transcription Factors genetics, Translocation, Genetic, ETS Translocation Variant 6 Protein, Chromosome Aberrations, Chromosomes, Human, Pair 12, Chromosomes, Human, Pair 21, Gene Expression Profiling, Oligonucleotide Array Sequence Analysis, Precursor Cell Lymphoblastic Leukemia-Lymphoma genetics
Abstract

We have prospectively analysed and correlated the gene expression profiles of children presenting with acute leukaemia to the Royal London and Great Ormond Street Hospitals with morphological diagnosis, immunophenotype and karyotype. Total RNA extracted from freshly sorted blast cells was obtained from 84 lymphoblastic [acute lymphoblastic leukaemia (ALL)], 20 myeloid [acute myeloid leukaemia (AML)] and three unclassified acute leukaemias and hybridised to the high density Affymetrix U133A oligonucleotide array. Analysis of variance and significance analysis of microarrays was used to identify discriminatory genes. A novel 50-gene set accurately identified all patients with ALL and AML and predicted for a diagnosis of AML in three patients with unclassified acute leukaemia. A unique gene set was derived for each of eight subtypes of acute leukaemia within our data set. A common profile for children with ALL with an ETV6-RUNX1 fusion, amplification or deletion of ETV6, amplification of RUNX1 or hyperdiploidy with an additional chromosome 21 was identified. This suggests that these rearrangements share a commonality in biological pathways that maintains the leukaemic state. The gene TERF2 was most highly expressed in this group of patients. Our analyses demonstrate that not only is microarray analysis the single most effective tool for the diagnosis of acute leukaemias of childhood but it has the ability to identify unique biological pathways. To further evaluate its prognostic value it needs to be incorporated into the routine diagnostic analysis for large-scale clinical trials in childhood acute leukaemias.

Published
2005
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28. Three distinct subgroups of hypodiploidy in acute lymphoblastic leukaemia.

Author

Harrison CJ, Moorman AV, Broadfield ZJ, Cheung KL, Harris RL, Reza Jalali G, Robinson HM, Barber KE, Richards SM, Mitchell CD, Eden TO, Hann IM, Hill FG, Kinsey SE, Gibson BE, Lilleyman J, Vora A, Goldstone AH, Franklin IM, Durrant J, and Martineau M

Subjects
Adolescent, Adult, Child, Disease-Free Survival, Female, Follow-Up Studies, Humans, Karyotyping, Male, Middle Aged, Prognosis, Survival Analysis, Aneuploidy, Chromosomes, Human genetics, Precursor Cell Lymphoblastic Leukemia-Lymphoma genetics
Abstract

This study of children and adults with acute lymphoblastic leukaemia (ALL) is the largest series of patients with hypodiploidy (<46 chromosomes) yet reported. The incidence of 5% was independent of age. Patients were subdivided by the number of chromosomes; near-haploidy (23-29 chromosomes), low hypodiploidy (33-39 chromosomes) and high hypodiploidy (42-45 chromosomes). The near-haploid and low hypodiploid groups were characterized by their chromosomal gains and a doubled hyperdiploid population. Structural abnormalities were more frequent in the low hypodiploid group. Near-haploidy was restricted to children of median age 7 years (range 2-15) whereas low hypodiploidy occurred in an older group of median age 15 years (range 9-54). Patients with 42-45 chromosomes were characterized by complex karyotypes involving chromosomes 7, 9 and 12. The features shared by the few patients with 42-44 chromosomes and the large number with 45 justified their inclusion in the same group. Survival analysis showed a poor outcome for the near-haploid and low hypodiploid groups compared to those with 42-45 chromosomes. Thus cytogenetics, or at least a clear definition of the modal chromosome number, is essential at diagnosis in order to stratify patients with hypodiploidy into the appropriate risk group for treatment.

Published
2004
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29. MRC trials in childhood acute myeloid leukaemia.

Author

Hann IM, Webb DK, Gibson BE, and Harrison CJ

Subjects
Child, Chromosome Aberrations, Clinical Trials as Topic, Disease-Free Survival, Humans, Leukemia, Myeloid genetics, Leukemia, Myeloid mortality, Prognosis, Recurrence, Survival Analysis, Treatment Outcome, Leukemia, Myeloid therapy
Abstract

The modern approach to therapy for acute myeloid leukaemia (AML) in children began in the late 80's and in the MRC series led to a 30% improvement in survival, up to levels of about 50%. Since 1995 the most recent trial AML 12 has taken those figures to two thirds event free survival and similar overall survival. Resistant disease rates remain at 4% overall but the death rate in complete remission has fallen from 11% to 6% despite increasing intensity of therapy, and due to advances in supportive care including nutrition and antibiotics/antifungals. However, although relapse rates have continued to fall, the biggest challenge is to reduce the currently one third relapse rate. We are much better at predicting who is likely to relapse, based mainly on primary resistance to therapy and karyotype. Analysis of 629 out of the last 808 cases in whom cytogenetic testing was successful (78%) has shown very clearly that t(8;21), t(15;17), inv(16) are independent good risk features. Additionally, loss of a sex chromosome in the 8;21 group defines a group which does exceptionally well, with 93% EFS at 5 years. Chromosome 7 abnormalities also remain of independent prognostic significance when age, WHO classification and white cell count are taken into account, with monosomy 7 doing even worse than 7q abnormalities. The current trial MRC AML 15 investigates the role of fludarabine--idarubicin combination therapy in the induction courses and the role of high dose cytarabine during consolidation; the aim being to increase efficacy and reduce toxicity, particularly that involving the heart. New approaches such as targeted antibody therapy will be explored when toxicity data for children permits.

Published
2004
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30. Long-term follow-up of relapsed childhood acute lymphoblastic leukaemia.

Author

Chessells JM, Veys P, Kempski H, Henley P, Leiper A, Webb D, and Hann IM

Subjects
Child, Child, Preschool, Clinical Protocols, Disease-Free Survival, Female, Follow-Up Studies, Humans, Infant, Male, Precursor Cell Lymphoblastic Leukemia-Lymphoma drug therapy, Precursor Cell Lymphoblastic Leukemia-Lymphoma mortality, Recurrence, Remission Induction, Risk Assessment, Survival Rate, Treatment Failure, Bone Marrow Transplantation, Precursor Cell Lymphoblastic Leukemia-Lymphoma therapy
Abstract

We have reviewed the outcome after relapse in a cohort of 505 children with acute lymphoblastic leukaemia (ALL) seen at a single institution. The majority of relapses (74%) occurred within 3 years from diagnosis, and most involved the bone marrow alone or with overt extramedullary relapse. Early relapse was more common in children with T-ALL and those with unfavourable cytogenetics. Factors influencing second remission included length of first remission and type of relapse. Children who had not received previous cranial irradiation had a superior survival. The German relapse score involving length of first remission, site of relapse and immunophenotype was highly predictive of outcome: event-free survival with 95% confidence intervals at 6 years for patients who received modern treatment [intensive chemotherapy or bone marrow transplantation (BMT)] was 78% (51-92%) for standard risk, 41% (33-49%) for intermediate risk and 19% (10-31%) for highest risk. Retrospective comparison of BMT with chemotherapy showed no difference in the intermediate-risk group but a possible advantage in the highest risk group. Follow-up of 235 patients who relapsed after chemotherapy and received a third course of treatment showed an extremely high early attrition rate, but a small number of patients survived in third remission. We conclude that new approaches are needed to individualize therapy in intermediate-risk patients and to improve the outcome for those in the highest risk group. Only a small number of children can be treated effectively in third remission.

Published
2003
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31. Outcome heterogeneity in childhood high-hyperdiploid acute lymphoblastic leukemia.

Author

Moorman AV, Richards SM, Martineau M, Cheung KL, Robinson HM, Jalali GR, Broadfield ZJ, Harris RL, Taylor KE, Gibson BE, Hann IM, Hill FG, Kinsey SE, Eden TO, Mitchell CD, and Harrison CJ

Subjects
Adolescent, Age Factors, Child, Child, Preschool, Disease-Free Survival, Female, Humans, In Situ Hybridization, Fluorescence, Infant, Karyotyping, Male, Multivariate Analysis, Precursor Cell Lymphoblastic Leukemia-Lymphoma mortality, Prognosis, Proportional Hazards Models, Sex Factors, Time Factors, Treatment Outcome, Trisomy, Diploidy, Precursor Cell Lymphoblastic Leukemia-Lymphoma drug therapy, Precursor Cell Lymphoblastic Leukemia-Lymphoma genetics
Abstract

High hyperdiploidy (HeH) (51 to 65 chromosomes) is found in one third of children with acute lymphoblastic leukemia and is associated with a good prognosis. Cytogenetic features may further refine this prognosis and identify patients with a poor outcome. We examined the effect of sex, age, individual trisomies, modal number, and structural abnormalities on survival among 700 children with HeH. Univariate analysis showed that age. sex, +4, +10, +18, and a high modal number were associated with survival. Multivariate analysis however, revealed that only age, sex, +4, and +18 were independent indicators. Hazard scores for predicting relapse and mortality were constructed. Three risk groups with 5-year event-free survival (EFS) rates of 86%, 75%, and 50% (P <.0001) were identified. The high-risk group comprised boys older than 9 years, boys aged 1 through 9 years without +18, and girls older than 9 years without +18, while girls aged 1 through 9 years with +18 had the best EFS. In terms of mortality, those younger than age 10 years with both +4 and +18 had an improved survival (96% vs 84% at 5 years, P <.0001). These findings confirm that the outcome of children with HeH is heterogeneous and that specific trisomies can identify patients with the greatest and least risk of treatment failure.

Published
2003
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32. Paediatric myelodysplastic syndromes and juvenile myelomonocytic leukaemia in the UK: a population-based study of incidence and survival.

Author

Passmore SJ, Chessells JM, Kempski H, Hann IM, Brownbill PA, and Stiller CA

Subjects
Adolescent, Child, Child, Preschool, Female, Humans, Incidence, Infant, Infant, Newborn, Leukemia, Myeloid therapy, Male, Myelodysplastic Syndromes therapy, Prognosis, Survival Analysis, Survival Rate, United Kingdom epidemiology, Leukemia, Myeloid mortality, Myelodysplastic Syndromes mortality
Abstract

We aimed to identify and classify cases of paediatric myelodysplastic syndromes (MDS) occurring in Britain to estimate the incidence of this rare group of diseases, investigate the results of therapy and identify prognostic risk factors. Patients aged below 15 years at diagnosis were collected from England, Scotland and Wales, inclusively between 1990 and 1999. One hundred and thirty-five patients were accepted as de novo MDS or juvenile myelomonocytic leukaemia (JMML). The incidence for this period was 1.35 per million (age standardized rate) which is below that reported outside the UK. The overall survival was 45%[standard error (SE) = 4%] at 5 years: 40% (SE = 6%) for JMML and 50% (SE = 6%) for other MDS. Significant adverse prognostic factors for JMML were a platelet count < 40 x 10(9)/l, raised fetal haemoglobin, FPC score and age above 2 years at diagnosis, for other MDS only monosomy 7 was significant. To conclude, the incidence of MDS/JMML in children in the UK appears to be lower than that reported outside the UK. This may be either a real difference in incidence or variation in reporting. Monosomy 7 is associated with poor outcome in MDS other than JMML. The prognosis of JMML depends on age, platelet count and fetal haemoglobin.

Published
2003
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33. Intraocular relapse of childhood acute lymphoblastic leukaemia.

Author

Somervaille TC, Hann IM, Harrison G, Eden TO, Gibson BE, Hill FG, Mitchell C, Kinsey SE, Vora AJ, and Lilleyman JS

Subjects
Antineoplastic Combined Chemotherapy Protocols therapeutic use, Bone Marrow Cells pathology, Central Nervous System pathology, Child, Child, Preschool, Combined Modality Therapy, Databases, Factual, Female, Follow-Up Studies, Humans, Infant, Male, Precursor Cell Lymphoblastic Leukemia-Lymphoma drug therapy, Precursor Cell Lymphoblastic Leukemia-Lymphoma radiotherapy, Recurrence, Survival Rate, United Kingdom, Eye pathology, Leukemic Infiltration, Precursor Cell Lymphoblastic Leukemia-Lymphoma pathology
Abstract

Relapse of childhood acute lymphoblastic leukaemia (ALL) involving the eye is a rare but challenging problem. Twenty cases occurred in patients treated on the Medical Research Council United Kingdom Acute Lymphoblastic Leukaemia XI and ALL97 trials between 1991 and 2001, representing 2.2% of ALL relapses. Seventeen occurred as a first relapse, either in isolation or combined with relapse at another site, and three occurred as a second relapse. All patients with intraocular disease at first relapse were treated with both chemotherapy and radiotherapy, but the doses and protocols used varied. Eleven of these 17 patients are alive and in complete remission with a median follow up of 4 years 2 months from relapse. All 11 children that were treated with a full chemotherapy relapse protocol, together with local radiotherapy have survived. Patients treated with chemotherapy of shorter duration and intensity, despite radiotherapy and/or bone marrow transplantation, did poorly with only one survivor, currently in chronic relapse. Consequently, we suggest that children with eye relapse of ALL be treated with an intensive relapse chemotherapy protocol with local ocular radiotherapy, whether the relapse occurs in isolation or in combination with relapse at another site.

Published
2003
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34. Prognostic factors and outcome for children after second central nervous system relapse of acute lymphoblastic leukaemia.

Author

Morris EC, Harrison G, Bailey CC, Hann IM, Hill FG, Gibson BE, Richards S, and Webb DK

Subjects
Child, Child, Preschool, Clinical Trials as Topic, Female, Follow-Up Studies, Humans, Infant, Infant, Newborn, Male, Prognosis, Survival Analysis, Central Nervous System Neoplasms therapy, Neoplasm Recurrence, Local etiology, Precursor Cell Lymphoblastic Leukemia-Lymphoma therapy
Abstract

The Medical Research Council acute lymphoblastic leukaemia trials (UKALL X and XI) recruited 3,702 children with ALL between January 1985 and March 1997. Seventy-nine children had central nervous system (CNS) involvement in their first two relapses. Fourteen children survived at a median follow-up of 22 months from second relapse; seven (9%) in third remission, two in later remissions and five with disease. Factors predictive of survival from second relapse were site (isolated CNS was better than combined CNS, P = 0.02) and time from diagnosis to second CNS relapse (longer time was better, P = 0.004). Prognosis after second CNS relapse is extremely poor, and palliative therapy is appropriate.

Published
2003
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35. Failure of a new protocol to improve treatment results in paediatric lymphoblastic leukaemia: lessons from the UK Medical Research Council trials UKALL X and UKALL XI.

Author

Chessells JM, Harrison G, Richards SM, Gibson BE, Bailey CC, Hill FG, and Hann IM

Subjects
Adolescent, Child, Child, Preschool, Clinical Protocols, Disease-Free Survival, Female, Follow-Up Studies, Humans, Infant, Leukocyte Count, Male, Randomized Controlled Trials as Topic, Risk Assessment, Risk Factors, Treatment Failure, Antineoplastic Combined Chemotherapy Protocols therapeutic use, Precursor Cell Lymphoblastic Leukemia-Lymphoma drug therapy
Abstract

The impact of various types of intensification therapy was examined in a cohort of 3617 children aged 1-14 years with acute lymphoblastic leukaemia (ALL) enrolled in the Medical Research Council (MRC) UKALL X (1985-90) and UKALL XI (1990-97) trials. UKALL XI was modified in 1992 to incorporate the "best arm" of UKALL X with two 5-d intensification blocks at 5 and 20 weeks, and an additional randomization in respect of a third intensification at 35 weeks but omission of two consecutive injections of daunorubicin during induction. All children were eligible for randomization irrespective of risk group. The impact of the various types of intensification therapy was examined in a stratified analysis. At a median follow up of 102 months, both trials had an identical event-free survival of 61% (95% CI 58-63%) at 8 years. Survival at 8 years in UKALL XI was significantly better in than in UKALL X, 81% (79-83%) compared with 74% (72-76%) (P = < 0.001), owing to improved management of relapse. There was a highly significant trend in reduction of the number of relapses and deaths with increased intensity of therapy both for children with initial leucocyte count < 50 x 10(9)/l (P = < 0.001) and > or = 50 x 10(9)/l (P = 0.002). Introduction of a third late intensification block compensated for omission of anthracyclines during induction but produced little additional benefit. These results show, in a large cohort of patients, that minor modifications of therapy may influence relapse rate and obviate the benefit of previous randomized trials. The failure to adapt treatment for higher risk children contributed to these disappointing results.

Published
2002
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36. The value of allogeneic bone marrow transplant in patients with acute myeloid leukaemia at differing risk of relapse: results of the UK MRC AML 10 trial.

Author

Burnett AK, Wheatley K, Goldstone AH, Stevens RF, Hann IM, Rees JH, and Harrison G

Subjects
Acute Disease, Adolescent, Adult, Child, Child, Preschool, Disease-Free Survival, Female, Histocompatibility Testing methods, Humans, Infant, Infant, Newborn, Male, Middle Aged, Recurrence, Risk Assessment, Risk Factors, Survival Analysis, Transplantation, Homologous, Treatment Outcome, Bone Marrow Transplantation methods, Leukemia, Myeloid therapy
Abstract

Patients under 55 years in the United Kingdom Medical Research Council Acute Myeloid Leukaemia 10 trial who entered complete remission were tissue typed (n = 1063). Four hundred and nineteen had a matched sibling donor and 644 had no match. When compared on a donor versus no donor basis the relapse risk was reduced in the donor arm (36%vs 52%; P = 0.001) and the disease-free survival (DFS) improved (50%vs 42%; P = 0.01), but overall survival (OS) was not different (55%vs 50%; P = 0.1). Sixty-one per cent of patients with a donor underwent transplantation. When patients were subdivided into risk groups based on cytogenetics alone or with the addition of blast response to course 1, a reduction in relapse risk was seen in all risk groups and in three age cohorts (0-14, 15-34 and 35+ years). Significant benefit in DFS was only seen in the intermediate-risk cytogenetic group (50%vs 39%; P = 0.004). The OS benefit was only seen in intermediate-risk patients (55%vs 44%; P = 0.02). The reduction in relapse risk in good-risk patients was attributable to patients with t(15;17) and not to patients with t(8;21) or inv(16). Allogeneic transplantation given after intensive chemotherapy was able to reduce relapse in all risk and age groups. However, due to the competing effects of procedural mortality and an inferior response to chemotherapy if relapse does occur, there was a survival advantage only in patients of intermediate risk. This trial found no survival advantage in children, patients over 35 years or good-risk disease.

Published
2002
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37. Paternal mosaicism proves the pathogenic nature of mutations in neutrophil elastase in severe congenital neutropenia.

Author

Ancliff PJ, Gale RE, Watts MJ, Liesner R, Hann IM, Strobel S, and Linch DC

Subjects
Adult, Child, Preschool, DNA Mutational Analysis, Fathers, Female, Humans, Leukopoiesis genetics, Male, Neutropenia etiology, Neutrophils enzymology, T-Lymphocytes enzymology, Leukocyte Elastase genetics, Mosaicism genetics, Mutation, Neutropenia congenital, Neutropenia enzymology
Abstract

Heterozygous mutations in neutrophil elastase have been detected in many sporadic cases of congenital neutropenia. However, a convincing pathogenetic mechanism has not been established, and it is unclear whether the effects of the mutant enzyme occur within the cell of production or are paracrine in nature. The healthy father of a patient was demonstrated to be mosaic for his daughter's Cys42Arg elastase mutation. Using semiquantitative polymerase chain reaction, approximately half of his T cells were shown to carry the mutation in contrast to less than 10% of neutrophils. Individual hematopoietic colonies grown from peripheral blood were heterozygous for the mutation or were homozygous wild type. These results demonstrate that precursors containing the mutation are selectively lost during myelopoiesis or fail to develop into neutrophils. This is the first in vivo confirmation of the pathogenic nature of elastase mutations in humans. The normal neutrophil count in the father suggests that the mutant elastase does not have paracrine effects.

Published
2002
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38. Results of treatment of children with refractory anaemia with excess blasts (RAEB) and RAEB in transformation (RAEBt) in Great Britain 1990-99.

Author

Webb DK, Passmore SJ, Hann IM, Harrison G, Wheatley K, and Chessells JM

Subjects
Acute Disease, Adolescent, Anemia, Refractory, with Excess of Blasts genetics, Anemia, Refractory, with Excess of Blasts mortality, Child, Child, Preschool, Chromosomes, Human, Pair 7, Female, Humans, Infant, Leukemia, Myeloid mortality, Leukemia, Myeloid therapy, Male, Monosomy, Patient Selection, Randomized Controlled Trials as Topic, Survival Rate, Transplantation, Homologous, Treatment Outcome, Anemia, Refractory, with Excess of Blasts therapy, Bone Marrow Transplantation
Abstract

Between 1990 and 1999, 36 children with refractory anaemia with excess blasts (RAEB) and RAEB in transformation (RAEBt), not associated with Down's syndrome, were diagnosed in Britain. A total of 31 children received intensive chemotherapy, six of whom proceeded to a bone marrow allograft in first remission, whereas two received an autograft. Of the 23 given chemotherapy only, four died of toxicity, 10 relapsed and nine are alive in first remission. Out of the 10 who relapsed, four are alive and disease-free following an allograft. Out of the 6 children given an allograft in first remission, two died of disease and four are alive in first remission. Both children given an autograft died of disease. Two children received an allograft without prior chemotherapy but died of toxicity. Three children received supportive care only, and one child survived. The overall survival was 51% at 5 years, and was superior in children with RAEBt (63%) compared with RAEB (28%, P = 0.03). Cytogenetics were available in 35 cases. Monosomy 7 was the most common abnormality (33% of cases). Survival in children with monosomy 7 was 22% at 5 years compared with 66% for the other patients (P = 0.05). Allowing for cytogenetics, outcomes of therapy appear similar to those for de novo acute myeloid leukaemia (AML), and it is appropriate for children with RAEB/RAEBt to be registered in AML trials.

Published
2002
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39. Mutations in the ELA2 gene encoding neutrophil elastase are present in most patients with sporadic severe congenital neutropenia but only in some patients with the familial form of the disease.

Author

Ancliff PJ, Gale RE, Liesner R, Hann IM, and Linch DC

Subjects
Adult, Case-Control Studies, Child, Chromosomes, Human, Pair 19, DNA Mutational Analysis, Family Health, Female, Genes, Dominant, Genes, Recessive, Genetic Linkage, Humans, Male, Middle Aged, Neutropenia congenital, Neutropenia enzymology, Pedigree, Leukocyte Elastase genetics, Mutation, Neutropenia genetics
Abstract

Severe congenital neutropenia (SCN) was originally described as an autosomal recessive disorder. Subsequently, autosomal dominant and sporadic forms of the disease have been recognized. All forms are manifest by persistent severe neutropenia and recurrent bacterial infection. In contrast, cyclical hematopoiesis is characterized by periodic neutropenia inter-spaced with (near) normal neutrophil counts. Recently, linkage analysis on 13 affected pedigrees identified chromosome 19p13.3 as the likely position for mutations in cyclical hematopoiesis. Heterozygous mutations in the ELA2 gene encoding neutrophil elastase were detected in all families studied. Further work also demonstrated mutations in ELA2 in sporadic and autosomal dominant SCN. However, all mutations described to date are heterozygous and thus appear to act in a dominant fashion, which is inconsistent with an autosomal recessive disease. Therefore, the current study investigated whether mutations in ELA2 could account for the disease phenotype in classical autosomal recessive SCN and in the sporadic and autosomal dominant types. All 5 exons of ELA2 and their flanking introns were studied in 18 patients (3 autosomal recessive, 5 autosomal dominant [from 3 kindreds], and 10 sporadic) using direct automated sequencing. No mutations were found in the autosomal recessive families. A point mutation was identified in 1 of 3 autosomal dominant families, and a base substitution was identified in 8 of 10 patients with the sporadic form, though 1 was subsequently shown to be a low-frequency polymorphism. These results suggest that mutations in ELA2 are not responsible for classical autosomal recessive Kostmann syndrome but provide further evidence for the role of ELA2 in SCN.

Published
2001
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40. Down's syndrome and acute lymphoblastic leukaemia: clinical features and response to treatment.

Author

Chessells JM, Harrison G, Richards SM, Bailey CC, Hill FG, Gibson BE, and Hann IM

Subjects
Child, Child, Preschool, Chromosome Aberrations, Chromosome Disorders, Clinical Trials as Topic, Cytogenetic Analysis, Disease-Free Survival, Down Syndrome genetics, Down Syndrome mortality, Female, Follow-Up Studies, Humans, Immunosuppressive Agents therapeutic use, Infant, Male, Methotrexate therapeutic use, Precursor Cell Lymphoblastic Leukemia-Lymphoma drug therapy, Precursor Cell Lymphoblastic Leukemia-Lymphoma mortality, Randomized Controlled Trials as Topic, Survival Rate, Down Syndrome complications, Patient Selection, Precursor Cell Lymphoblastic Leukemia-Lymphoma complications
Abstract

Aims: To examine the clinical and biological features of acute lymphoblastic leukaemia in children with Down's syndrome (DS), to compare their survival with other children, and to determine if entry to trials and survival has improved., Methods: Examination of presenting features and response to treatment in patients treated in two consecutive national trials, MRC UKALL X and XI., Results: The proportion of children with DS was significantly higher in UKALL XI (1.9%) than UKALL X (0.9%). Children with DS tended to be under 10 years and to have the common ALL subtype. Cytogenetic analysis showed that favourable features, such as high hyperdiploidy and t(12;21) were less frequent but also that there was a lack of translocations associated with a poor prognosis. Children with DS showed no increase in risk of relapse at any site but their survival and event free survival were inferior to other children. These results were caused by an increased number of infective deaths during remission (11% compared to 2%). At five years overall survival was 73% in DS children compared with 82% in other children; event free survival was 53% compared to 63% in non-DS children., Conclusions: Entry of children with DS to national trials has increased and survival has improved. However they remain at risk of relapse and also of treatment related mortality. These findings emphasise the need for both intensive chemotherapy and optimal supportive care.

Published
2001
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41. Oral ciprofloxacin plus colistin: prophylaxis against bacterial infection in neutropenic patients. A strategy for the prevention of emergence of antimicrobial resistance.

Author

Prentice HG, Hann IM, Nazareth B, Paterson P, Bhamra A, and Kibbler CC

Subjects
Adolescent, Adult, Aged, Bone Marrow Transplantation, Humans, Middle Aged, Neomycin therapeutic use, Neutropenia therapy, Statistics, Nonparametric, Transplantation Conditioning, Treatment Outcome, Antibiotic Prophylaxis, Bacterial Infections prevention & control, Ciprofloxacin therapeutic use, Colistin therapeutic use, Drug Therapy, Combination therapeutic use, Neutropenia drug therapy
Abstract

Following a 2-year study, the combination of oral ciprofloxacin and colistin has been used continuously for 10 years without the emergence of resistance. During a 2-year period (1987-1989), we compared ciprofloxacin + colistin (CIP + COL) with neomycin + colistin (NEO + COL) in a randomized trial--combinations chosen because of the potential for prophylaxis of Gram-negative infection by ciprofloxacin, with colistin given to reduce the risk of emergence of resistance. Sixty-four patients with similar demographics in each arm were evaluable for efficacy analysis. Patients on CIP + COL had a significantly lower proportion of neutropenic days with fever (P < 0.001) and neutropenic days on intravenous antibiotics (P < 0.001) than patients on NEO + COL. A total of 54 (15 bacteriologically documented) pyrexial episodes occurred in patients on CIP + COL and 77 (41 bacteriologically documented) in patients on NEO + COL. Only two Gram-negative bacterial infections occurred in the CIP + COL arm compared with 16 in the NEO + COL arm. No Staphylococcus aureus infections occurred in the CIP + COL group compared with 10 in the other patients. Two CIP-resistant Gram-negative bacilli were isolated from patients on CIP + COL compared with 13 NEO-resistant Gram-negative bacilli from patients on NEO + COL. Following a subsequent decade of unchanged use of this prophylactic strategy in neutropenic patients, a 2-year follow-up study between 1 January 1998 and 31 December 1999 showed 66 significant infections during 700 [corrected] neutropenic episodes. Thirty-five of the 111 (31%) isolates were ciprofloxacin-resistant, involving 5% of the neutropenic episodes [corrected].

Published
2001
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42. Relationships between age at diagnosis, clinical features, and outcome of therapy in children treated in the Medical Research Council AML 10 and 12 trials for acute myeloid leukemia.

Author

Webb DK, Harrison G, Stevens RF, Gibson BG, Hann IM, and Wheatley K

Subjects
Acute Disease, Adolescent, Age Factors, Child, Child, Preschool, Cytogenetic Analysis, Disease-Free Survival, Female, Humans, Infant, Infant, Newborn, Leukemia, Myeloid mortality, Male, Prognosis, Recurrence, Survival Rate, Treatment Outcome, Leukemia, Myeloid diagnosis, Leukemia, Myeloid drug therapy
Abstract

Between May 1988 and June 2000, 698 children were treated in the Medical Research Council acute myeloid leukemia 10 and 12 trials. The presenting features and outcomes of therapy in these children were compared by age. Although there was no single cutoff in age, younger children were more likely to have intermediate risk and less likely to have favorable cytogenetics (P <.001), and they had a higher incidence of translocations involving chromosome 11q23 (P <.001). The distribution of French-American-British (FAB) types also varied with age; FAB types M5 (P <.001) and M7 (P <.001) were more common in early childhood, whereas older children were more likely to have FAB types M0 (P =.03), M1 (P =.04), M2 (P =.005), and M3 (P <.001). Involvement of the central nervous system at diagnosis was also more common in the youngest children (P =.01). Younger children had more severe diarrhea (P =.002), whereas older children had worse nausea and vomiting (P =.01) after chemotherapy. When adjusted for other important factors, complete remission rates were similar (P =.5) and although there was less resistant disease in younger children (P =.003), this was partially balanced by a slight increase in deaths during induction therapy in younger patients (P =.06). On multivariate analysis overall survival (P =.02), event-free survival (P =.02), and disease-free survival were better (P =.06) in younger children due to a lower relapse rate (P =.02) especially in the bone marrow (P =.02).

Published
2001
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43. Outcome of relapsed or refractory childhood B-cell acute lymphoblastic leukaemia and B-cell non-Hodgkin's lymphoma treated with the UKCCSG 9003/9002 protocols.

Author

Atra A, Gerrard M, Hobson R, Imeson JD, Hann IM, and Pinkerton CR

Subjects
Antineoplastic Combined Chemotherapy Protocols administration & dosage, Bone Marrow Transplantation, Burkitt Lymphoma radiotherapy, Burkitt Lymphoma therapy, Child, Combined Modality Therapy, Cyclophosphamide administration & dosage, Cytarabine therapeutic use, Doxorubicin administration & dosage, Etoposide therapeutic use, Follow-Up Studies, Humans, Lymphoma, B-Cell radiotherapy, Lymphoma, B-Cell therapy, Palliative Care, Precursor Cell Lymphoblastic Leukemia-Lymphoma radiotherapy, Precursor Cell Lymphoblastic Leukemia-Lymphoma therapy, Prednisone administration & dosage, Recurrence, Treatment Outcome, Vincristine administration & dosage, Antineoplastic Combined Chemotherapy Protocols therapeutic use, Burkitt Lymphoma drug therapy, Lymphoma, B-Cell drug therapy, Precursor Cell Lymphoblastic Leukemia-Lymphoma drug therapy
Abstract

Twenty-six children with B-cell acute lymphoblastic leukaemia (B-ALL) or Murphy Stage III or IV B-cell non-Hodgkin's lymphoma (B-NHL) progressed or relapsed after first-line therapy with a short, intensive multiagent chemotherapy regimen [United Kingdom Childhood Cancer Study Group (UKCCSG) 9003] (n = 62) or a slightly less intensive regimen (UKCCSG 9002) (n = 112). Eight patients (4.6%) never achieved complete remission (CR) and 18 (10.3%) relapsed. Second-line therapy resulted in remission for eight patients (30%). All patients initially treated with the 9003 protocol died. Three patients (11.5%) in the 9002 group, including one who never achieved CR in the primary site, are alive after second-line therapy. This study confirms that the prognosis of relapsed or refractory B-ALL/B-NHL is poor and exceptionally so if relapse occurred less than 6 months from diagnosis. High-dose therapy with stem cell rescue was used in only seven patients; its role needs to be studied further.

Published
2001
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44. Lipid-based amphotericin B: a review of the last 10 years of use.

Author

Hann IM and Prentice HG

Subjects
Amphotericin B economics, Antifungal Agents economics, Clinical Trials as Topic, Costs and Cost Analysis, Hematologic Diseases complications, Humans, Mycoses complications, Neoplasms complications, Neutropenia complications, Randomized Controlled Trials as Topic, Amphotericin B therapeutic use, Antifungal Agents therapeutic use, Mycoses therapy
Abstract

The last decade has been remarkable for the dramatic increase in the prevalence of serious fungal infections in patients with haematological disorders and neutropenic cancer patients. The mortality rate of deep-seated infection has been in excess of 90% and there is no doubt that this is one of the greatest challenges currently facing haematologists and oncologists. The development of the lipid-based drugs - liposomal amphotericin (AmBisome(R)), amphotericin B lipid complex, ABLC (Abelcet(R)), amphotericin B colloidal dispersion, Amphocil (ABCD(R)), has meant that doses of amphotericin B can be safely escalated for the first time whilst the problems of nephrotoxicity, infusion related reactions (including chills, rigors, fevers and hypoxia) can be reduced. These toxicities are variably reduced with AmBisome more than Abelcet and more than Amphocil and there is little information from randomised trials other than for AmBisome. AmBisome used in the setting of persistent fever and neutropenia not responding after 3-4 days of intravenous antibiotics, is associated with less breakthrough systemic fungal infections. There is also much less need for premedication, including steroids, compared with amphotericin B and Abelcet. The use of intermittent doses of Ambisome given prophylactically is now being explored. A new and exciting era of antifungal therapy is opening up with new compounds, such as itraconazole voriconazole, posaconazole and echinocandins, being investigated and for the first time, we also have options for combination therapy and prophylaxis.

Published
2001
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45. Hermansky-Pudlak syndrome presenting with subdural haematoma and retinal haemorrhages in infancy.

Author

Russell-Eggitt IM, Thompson DA, Khair K, Liesner R, and Hann IM

Subjects
Birth Injuries complications, Child Abuse diagnosis, Diagnosis, Differential, Hematoma, Subdural diagnosis, Hermanski-Pudlak Syndrome diagnosis, Humans, Infant, Male, Retinal Hemorrhage diagnosis, Hematoma, Subdural etiology, Hermanski-Pudlak Syndrome complications, Retinal Hemorrhage etiology
Published
2000
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46. Bone marrow transplantation versus chemotherapy in the treatment of very high-risk childhood acute lymphoblastic leukemia in first remission: results from Medical Research Council UKALL X and XI.

Author

Wheeler KA, Richards SM, Bailey CC, Gibson B, Hann IM, Hill FG, and Chessells JM

Subjects
Adolescent, Child, Child, Preschool, Disease-Free Survival, Histocompatibility Testing, Humans, Infant, Leukocyte Count, Philadelphia Chromosome, Ploidies, Precursor Cell Lymphoblastic Leukemia-Lymphoma mortality, Recurrence, Remission Induction, Risk Factors, United Kingdom, Antineoplastic Combined Chemotherapy Protocols therapeutic use, Bone Marrow Transplantation, Precursor Cell Lymphoblastic Leukemia-Lymphoma drug therapy, Precursor Cell Lymphoblastic Leukemia-Lymphoma surgery
Abstract

The role of bone marrow transplantation (BMT) in first remission of children with high-risk acute lymphoblastic leukemia (ALL) remains unclear. There were 3676 patients (aged 1 to 15 years) entered into the United Kingdom (UK) Medical Research Council (MRC) trials UKALL X and XI from 1985 to 1997. Of these patients, 473 patients (13%) were classified as very high (VH) risk and were eligible for a transplantation from a matched histocompatible sibling donor (MSD). We tissue-typed 286 patients; 99 patients had a matched related donor, and 76 patients received transplantations. Additionally, 25 children received transplantations from a matched unrelated donor (MUD) despite trial guidelines for MSD transplantations only. The median time to transplantation was 5 months (range, 2 to 19 months), and the median follow-up was 8 years. The 10-year event-free survival (EFS) adjusted for the time to transplantation, diagnostic white blood cell (WBC) count, Ph chromosome status, and ploidy was 6. 0% higher (95% confidence interval (CI), -10.5% to 22.5%) for 101 patients who received a first-remission transplantation (MSD and MUD) than for the 351 patients treated with chemotherapy (transplantation, 45.3%, vs chemotherapy, 39.3%). The transplantation group had fewer relapses (31%) compared to relapses in the chemotherapy group (55%); however, the transplantation group had more remission deaths (18%) compared to remission deaths in the chemotherapy group (3%). In contrast the adjusted 10-year EFS was 10. 7% higher (95% CI, -2.6% to 24.0%) for patients without a human leukocyte antigen (HLA)-matched donor than for those patients with a donor (no donor, 50.4%, vs donor, 39.7%). In conclusion, for the majority of children with VH-risk ALL, the first-remission transplantation has not improved EFS.

Published
2000

47. Management of infection in children with bone marrow failure.

Author

Hann IM

Subjects
Bacterial Infections drug therapy, Bacterial Infections etiology, Bacterial Infections prevention & control, Child, Hematopoietic Cell Growth Factors therapeutic use, Humans, Mycoses drug therapy, Mycoses etiology, Mycoses prevention & control, Virus Diseases drug therapy, Virus Diseases etiology, Virus Diseases prevention & control, Antineoplastic Agents adverse effects, Infections drug therapy, Infections etiology, Leukemia drug therapy, Neutropenia complications, Neutropenia etiology
Abstract

The development of new and often more successful regimens of treatment for childhood blood and malignant diseases has usually been associated with a parallel increase in infectious problems. This is because these successes have often, in the absence of new effective drugs, been achieved by increasing drug dose intensity to new limits. This chapter is not intended to deal with every possible infection, but rather to be a practical guide to the current management of infection. The last few years have seen major improvements in the development of haematopoietic growth factors, new antifungal agents, new antibiotics and new ways to use aminoglycosides. Attempts are being made to identify good and poor risk factors for the outcome of infection in order to facilitate shorter courses and possibly home or day care use of antimicrobial agents. In addition the different needs of children are being recognized in view of the restricted use of quinolones in this group and the different organisms and types of infection that they experience.

Published
2000
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48. Central venous access devices in children with congenital coagulation disorders: complications and long-term outcome.

Author

McMahon C, Smith J, Khair K, Liesner R, Hann IM, and Smith OP

Subjects
Adolescent, Blood Coagulation Disorders congenital, Catheters, Indwelling adverse effects, Child, Child, Preschool, Drug Hypersensitivity etiology, Equipment Failure, Female, Hemorrhage etiology, Humans, Infant, Infant, Newborn, Length of Stay, Male, Retrospective Studies, Staphylococcal Infections etiology, Treatment Outcome, Blood Coagulation Disorders therapy, Catheterization, Central Venous adverse effects
Abstract

Reliable venous access is essential to facilitate the administration of prophylactic factor concentrate or blood products in children with congenital coagulation disorders and immune tolerance therapy (ITT) regimens in those who develop high responding inhibitors. Poor venous access is even more problematic in very young children, the vast majority of whom will require the insertion of central venous access devices (CVADs). Previous studies have suggested that infection rates are low and that there are few long-term complications associated with CVAD usage. We have reviewed 86 CVADs that have been inserted, since 1988, in 58 children with congenital bleeding disorders, aged 6 d to 16.5 years, attending Great Ormond Street Hospital, London, and the National Children's Hospital, Dublin. The devices have remained in situ for 2 weeks to 92 months (median 22.5 months). Early (0-2 weeks) complications of CVAD insertion included nine bleeding episodes, one extravasation of factor concentrate, three allergic reactions to factor concentrate and five catheter infections. Overall, CVAD infection was the commonest problem encountered, with 52 devices (60%) becoming infected. Twenty-seven CVADs (31%) required removal. Infection rates in children without inhibitors (29/68) were 1/20 patient-months or 1. 6 infections/1000 patient-days, but infection rates for those with inhibitors were 1/8.5 patient-months or 4.3/1000 patient-days. Staphylococcus epidermidis was the predominant organism (25/52) isolated. Blockage of CVAD (four) and catheter disconnection (four) were the most frequently occurring non-infectious long-term complications. Skin erosion of the port was also seen in three children, in one child at 20 months, in one at 29 months and in one at 34 months after insertion. This study demonstrates a high CVAD infection rate and highlights the long-term complications of CVAD usage.

Published
2000
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49. Improved outcome in children with advanced stage B-cell non-Hodgkin's lymphoma (B-NHL): results of the United Kingdom Children Cancer Study Group (UKCCSG) 9002 protocol.

Author

Atra A, Imeson JD, Hobson R, Gerrard M, Hann IM, Eden OB, Carter RL, and Pinkerton CR

Subjects
Adolescent, Analysis of Variance, Bone Marrow pathology, Child, Child, Preschool, Cyclophosphamide administration & dosage, Disease-Free Survival, Doxorubicin administration & dosage, Female, Follow-Up Studies, Humans, L-Lactate Dehydrogenase blood, Lymphoma, B-Cell pathology, Male, Methotrexate administration & dosage, Multivariate Analysis, Neoplasm Staging, Prednisone administration & dosage, Prognosis, Survival Rate, Time Factors, Treatment Outcome, Vincristine administration & dosage, Antineoplastic Combined Chemotherapy Protocols therapeutic use, Lymphoma, B-Cell drug therapy
Abstract

From July 1990 to March 1996, 112 children with stage III or IV B-cell non-Hodgkin's lymphoma (B-NHL) with up to 70% FAB L3-type blasts (n = 42) in the bone marrow without central nervous system (CNS) disease were treated on the United Kingdom Children Cancer Study Group (UKCCSG) 9002 protocol (identical to the French LMB 84). The median age was 8.3 years. There were 81 boys and 31 girls. According to the extent of the primary disease, patients were sub-staged into three groups: IIIA with unresectable abdominal tumour (n = 39); IIIB with abdominal multiorgan involvement (n = 57) and IIIX with extra-abdominal primary lymphoma often presenting as pleural effusion (n = 16). Univariate and multivariate analyses were carried out to evaluate the prognostic significance of lactate dehydrogenase (LDH) level at diagnosis, the sub-stage and the time to achieve complete remission (CR). With a median follow up of 48 months (range 12-92), the overall and event free survival (EFS) is 87% (95% confidence interval (CI) 79.2-92.1 %) and 83.7% (95% CI 76.3-89.2%) respectively. Six patients (5.4%) never achieved CR, of whom one is alive following high-dose therapy. Eight patients (7.1%) relapsed after achieving CR, three are alive after second-line therapy. There were three early toxic deaths (2.7%), mainly from infection, and one late death from a second cancer. There was no significant difference in EFS according to LDH level at diagnosis, the sub-stage or the time to CR. This study confirms the overall good prognosis and low rate of toxic deaths in patients with advanced B-NHL treated with this intensive regimen. No significant difference in EFS according to the sub-stage, the time to achieve CR or LDH level at diagnosis making it difficult to identify a group that should not receive intensive therapy.

Published
2000
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50. A simple, robust, validated and highly predictive index for the determination of risk-directed therapy in acute myeloid leukaemia derived from the MRC AML 10 trial. United Kingdom Medical Research Council's Adult and Childhood Leukaemia Working Parties.

Author

Wheatley K, Burnett AK, Goldstone AH, Gray RG, Hann IM, Harrison CJ, Rees JK, Stevens RF, and Walker H

Subjects
Acute Disease, Adolescent, Adult, Child, Child, Preschool, Chromosome Aberrations, Female, Humans, Infant, Infant, Newborn, Leukemia, Myeloid pathology, Male, Middle Aged, Prognosis, Recurrence, Risk Assessment, Risk Factors, Survival Analysis, Leukemia, Myeloid therapy
Abstract

Data on 1711 patients, aged up to 55 years, in the MRC AML 10 trial were used to create a prognostic index for use in risk-directed therapy decision making for younger patients with acute myeloid leukaemia (AML). Two parameters, response after course 1 and cytogenetics, were strongly predictive of outcome. For patients with complete remission, partial remission and resistant disease, 5-year survival from the start of course 2 was 53%, 44% and 22% and relapse rates were 46%, 48% and 69% respectively, and for patients with favourable, intermediate and adverse karyotypic abnormalities, survival was 72%, 43% and 17% and relapse rates were 34%, 51% and 75% respectively (all P < 0.0001). Patients with FAB type M3 but no cytogenetic t(15;17) also had a low relapse rate (29%). These three factors were combined to give three risk groups: good (favourable karyotype or M3, irrespective of response status or presence of additional abnormalities), standard (neither good nor poor), poor (adverse karyotype or resistant disease, and no good-risk features). Survival for these three groups was 70%, 48% and 15% respectively and relapse rates were 33%. 50% and 78% (both P < 0.0001). The index is simple (based on just three parameters), robust (derived from 1711 patients), highly discriminatory (55% survival difference between good and poor risk) and validated, so can be applied in the clinical setting to assist with therapeutic decisions as in the current AML 12 trial.

Published
1999
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