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Dive into the research topics where Archie Prentice is active.

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Featured researches published by Archie Prentice.


British Journal of Haematology | 2006

In meta-analysis itraconazole is superior to fluconazole for prophylaxis of systemic fungal infection in the treatment of haematological malignancy

Archie Prentice; Axel Glasmacher; Benjamin Djulbegovic

biology of Transfusion Medicine (ed. by G. Garratty), pp. 493–521. Marcel Dekker, New York. Gehrs, B.C. & Friedberg, R.C. (2002) Autoimmune hemolytic anemia. American Journal of Hematology, 69, 258–271. Gilliland, B.C., Baxter, E. & Evans, R.S. (1971) Red-cell antibodies in acquired hemolytic anemia with negative antiglobulin serum tests. New England Journal of Medicine, 285, 252–256. Mollison, P.L. & Hughes-Jones, N.C. (1967) Clearance of Rh-positive red cells by low concentrations of Rh antibody. Immunology, 12, 63–67. Nathalang, O., Chuansumrit, A., Prayoonwiwat, W., Siripoonya, P. & Sriphaisal, T. (1997) Comparison between the conventional tube technique and the gel technique in direct antiglobulin test. Vox Sanguinis, 72, 169–171.


Leukemia & Lymphoma | 2010

Chronic lymphocytic leukemia can cause acute renal failure even in early stage patients

Claire Lentaigne; Clare Craig; Kate Cwynarski; Archie Prentice; Christopher McNamara

An 80-year-old lady was diagnosed with Rai stage 0 chronic lymphocytic leukemia (CLL) on the basis of a peripheral blood lymphocyte count of 9 × 109/L with a typical phenotype by flow cytometry. Sh...


Medical Mycology | 2006

The debate: The trials have told us very little

Archie Prentice

The original trials of empiric intravenous amphotericin-B in the 1980s failed to prove conclusively its efficacy in the treatment of febrile neutropenia. Despite that, all subsequent studies of the therapy of presumed, possible, probable and proven invasive aspergillosis have assumed that this drug, either as deoxycholate or in lipid-based form, is the gold standard treatment against which all newcomers should be compared. This has led to a series of further inconclusive randomized controlled trials of empiric therapy as a result of which the most we can say is that nearly all new drugs are less toxic but also no more effective than amphotericin-B deoxycholate. The toxicity of the non-lipid formulation of this drug should have led us to withdraw it from both RCTs and routine clinical practice some years ago in view of the increasing evidence of equivalent efficacy and lower toxicity of other agents including lipid amphotericin formulations.Recent studies of the use of newer diagnostic techniques (i.e., CT and serology) reinforce the need to abandon the empiric trial approach in which we have repeatedly shown lack of superiority in the treatment of an infection which most patients do not have. Even in the small number of trials of the therapy of proven or probable invasive aspergillosis, results have been inconclusive or at best confusing in trying to find a better option than amphotericin-B. The trial of voriconazole versus amphotericin-B deoxycholate for this indication is a model for study for all those interested in the difficulties of designing trials which lead to convincing results.Effective prophylaxis trials and their analyses began by following a more rational pathway, first showing convincingly that fluconazole reduced the risk of C. albicans systemic infection in transplant patients. Unfortunately the widespread faith in the ability of this drug to prevent a wider range of systemic fungal infections in a wider range of patients is simply not supported by the data from many subsequent single trials and meta-analyses. This attachment to fluconazole has been mirrored by unwillingness to accept the evidence that itraconazole is superior in prophylaxis to fluconazole which is inactive against Aspergillus spp. In this case the trials have not told us enough because we have not believed the results. Results of trials of extended range azoles such as posaconazole are interesting but there are insufficient data to claim that posaconazole is superior to itraconazole.The progress in therapy and prophylaxis of systemic fungal infection has been unsatisfactory and slow. A new approach is needed for the design of clinical trials for these indications. There is good evidence that supportive investigations should now be used routinely in clinical practice and trials to increase certainty about the presence of invasive infection, to limit unnecessary use of expensive and toxic drugs and to improve analysis of efficacy of old and new antifungal agents.


Blood | 2009

Attempts to Optimise Induction and Consolidation Chemotherapy in Patients with Acute Myeloid Leukaemia: Results of the MRC AML15 Trial.

Alan Kenneth Burnett; Robert Kerrin Hills; Donald Milligan; Ann Hunter; Anthony H. Goldstone; Archie Prentice; Brenda Gibson; Lars Kjeldsen; John A. Liu Yin; Keith Wheatley; Nigel H. Russell


Blood | 2009

Induction of Noxa Via Generation of Reactive Oxygen Species Plays a Key Role in Induction of CLL Cell Apoptosis by Two Novel p53-Independent Cytotoxic Agents.

Andrew Steele; Archie Prentice; A Chanalaris; A. V. Hoffbrand; Kate Cwynarski; Rg Wickremasinghe


Blood | 2005

Rituximab Does Not Increase the Complication Rate, Particularly Perforation, When Added to Chemotherapy for Patients with Primary B-Cell Lymphomas of the Gastrointestinal Tract.

Shireen A. Kassam; Anthony H. Goldstone; A. V. Hoffbrand; Miguel Perez-Machado; Nicola Cooper; Panos Kottaridis; Archie Prentice; Derralyn Hughes; Christopher McNamara


Blood | 2005

Itraconazole for Antifungal Prophylaxis in Neutropenic Patients: An Update of a Meta-Analysis with Now 3846 Patients.

Axel Glasmacher; Corinna Hahn; Marie von Lilienfeld-Toal; Katjana Orlopp; Ingo Schmidt-Wolf; Archie Prentice


Blood | 2012

Phenethyl Isothiocyanate (PEITC) Regulates Autophagy in Chronic Lymphocytic Leukemia.

J Adams; Rg Wickremasinghe; Archie Prentice; Jon C. Strefford; Andrew S Duncombe; Francesco Forconi; Freda K. Stevenson; Graham Packham; Andrew Steele


In: (Proceedings) 51st Annual Scientific Meeting of the British-Society-for-Haematology. (pp. p. 72). WILEY-BLACKWELL (2011) | 2011

CD160: a novel approach to minimal residual disease (MRD) assessment in chronic lymphocytic leukaemia (CLL)

Timothy Farren; Feng-Ting Liu; Marion G. Macey; Michael Jenner; Archie Prentice; Amit C. Nathwani; Samir G. Agrawal


Clinical Lymphoma, Myeloma & Leukemia | 2011

4.17 A Novel Approach to Minimal Residual Disease Assessment in Chronic Lymphocytic Leukaemia Utilizing the Tumour Specific Antigen CD160

Timothy Farren; Feng-Ting Liu; Marion G. Macey; Michael Jenner; Archie Prentice; Amit C. Nathwani; Samir G. Agrawal

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Andrew Steele

University of Southampton

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Feng-Ting Liu

Queen Mary University of London

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Michael Jenner

Queen Mary University of London

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Samir G. Agrawal

Queen Mary University of London

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Timothy Farren

Queen Mary University of London

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