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Health Technology Assessment 2008; Vol. 12: No. 16 Ranibizumab and pegaptanib for the treatment of age-related macular degeneration: a systematic review and economic evaluation JL Colquitt, J Jones, SC Tan, A Takeda, AJ Clegg and A Price Feedback The HTA Programme and the authors would like to know your views about this report. The Correspondence Page on the HTA website (http://www.hta.ac.uk) is a convenient way to publish your comments. If you prefer, you can send your comments to the address below, telling us whether you would like us to transfer them to the website. We look forward to hearing from you. May 2008 The National Coordinating Centre for Health Technology Assessment, Alpha House, Enterprise Road Health Technology Assessment Southampton Science Park Chilworth NHS R&D HTA Programme HTA Southampton SO16 7NS, UK. www.hta.ac.uk Fax: +44 (0) 23 8059 5639 Email: HTA How to obtain copies of this and other HTA Programme reports. 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Contact details are as follows: HTA Despatch Email: Ranibizumab and pegaptanib for the treatment of age-related macular degeneration: a systematic review and economic evaluation * JL Colquitt, J Jones, SC Tan, A Takeda, AJ Clegg and A Price Southampton Health Technology Assessments Centre (SHTAC), Wessex Institute for Health Research and Development (WIHRD), University of Southampton, UK * Corresponding author Declared competing interests of authors: none Published May 2008 This report should be referenced as follows: Colquitt JL, Jones J, Tan SC, Takeda A, Clegg AJ, Price A. Ranibizumab and pegaptanib for the treatment of age-related macular degeneration: a systematic review and economic evaluation. Health Technol Assess 2008;12(16). Health Technology Assessment is indexed and abstracted in Index Medicus/MEDLINE, Excerpta Medica/EMBASE and Science Citation Index Expanded (SciSearch®) and Current Contents®/Clinical Medicine. NIHR Health Technology Assessment Programme he Health Technology Assessment (HTA) Programme, part of the National Institute for Health TResearch (NIHR), was set up in 1993. It produces high-quality research information on the effectiveness, costs and broader impact of health technologies for those who use, manage and provide care in the NHS. ‘Health technologies’ are broadly defined as all interventions used to promote health, prevent and treat disease, and improve rehabilitation and long-term care. The research findings from the HTA Programme directly influence decision-making bodies such as the National Institute for Health and Clinical Excellence (NICE) and the National Screening Committee (NSC). HTA findings also help to improve the quality of clinical practice in the NHS indirectly in that they form a key component of the ‘National Knowledge Service’. The HTA Programme is needs-led in that it fills gaps in the evidence needed by the NHS. 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The research reported in this issue of the journal was commissioned and funded by the HTA Programme on behalf of NICE as project number 04/24/01. The protocol was agreed in May 2006. The assessment report began editorial review in November 2006 and was accepted for publication in January 2008. The authors have been wholly responsible for all data collection, analysis and interpretation, and for writing up their work. The HTA editors and publisher have tried to ensure the accuracy of the authors’ report and would like to thank the referees for their constructive comments on the draft document. However, they do not accept liability for damages or losses arising from material published in this report. The views expressed in this publication are those of the authors and not necessarily those of the HTA Programme or the Department of Health. Editor-in-Chief: Professor Tom Walley Series Editors: Dr Aileen Clarke, Dr Peter Davidson, Dr Chris Hyde, Dr John Powell, Dr Rob Riemsma and Professor Ken Stein Programme Managers: Sarah Llewellyn Lloyd, Stephen Lemon, Kate Rodger, Stephanie Russell and Pauline Swinburne ISSN 1366-5278 © Queen’s Printer and Controller of HMSO 2008 This monograph may be freely reproduced for the purposes of private research and study and may be included in professional journals provided that suitable acknowledgement is made and the reproduction is not associated with any form of advertising. Applications for commercial reproduction should be addressed to: NCCHTA, Alpha House, Enterprise Road, Southampton Science Park, Chilworth, Southampton SO16 7NS, UK. Published by Gray Publishing, Tunbridge Wells, Kent, on behalf of NCCHTA. Printed on acid-free paper in the UK by St Edmundsbury Press Ltd, Bury St Edmunds, Suffolk. T Health Technology Assessment 2008; Vol. 12: No. 16 Abstract Ranibizumab and pegaptanib for the treatment of age-related macular degeneration: a systematic review and economic evaluation * JL Colquitt, J Jones, SC Tan, A Takeda, AJ Clegg and A Price Southampton Health Technology Assessments Centre (SHTAC), Wessex Institute for Health Research and Development (WIHRD), University of Southampton, UK * Corresponding author Objectives: To assess the clinical effectiveness and or more (a clinically important outcome having a cost-effectiveness of ranibizumab and pegaptanib for significant impact on quality of life) was statistically subfoveal choroidal neovascularisation (CNV) significantly greater in the pegaptanib group for doses associated with wet age-related macular degeneration of 0.3 and 1.0 mg but not for 3.0 mg, and for all (AMD). ranibizumab groups compared to the sham injection Data sources: Electronic databases were searched groups or PDT. This was also statistically significant for from inception to September 2006. Experts in the field patients receiving 0.5 mg ranibizumab plus PDT were consulted and manufacturers’ submissions were compared with PDT plus sham injection. Pegaptanib examined. patients lost statistically significantly fewer letters after Review methods: The quality of included studies was 12 months of treatment than the sham group [mean assessed using standard methods and the clinical letters lost: 7.5 (0.3 mg), 6.5 (1.0 mg) or 10 (3.0 mg) vs effectiveness data were synthesised through a narrative 14.5 (sham)]. In the MARINA and ANCHOR trials, review with full tabulation of results. A model was ranibizumab patients gained letters of visual acuity at developed to estimate the cost-effectiveness of 12 months whereas patients with sham injection or ranibizumab and of pegaptanib (separately), compared PDT lost about 10 letters (p < 0.001) and in the PIER with current practice or best supportive care, from the study, ranibizumab patients lost significantly fewer than perspective of the NHS and Personal Social Services. the sham injection group. Significantly fewer patients Two time horizons were adopted for each model. The receiving pegaptanib or ranibizumab deteriorated to first adopted time horizons determined by the available legal blindness compared with the control groups. trial data. The second analysis extrapolated effects of Adverse events were common for both pegaptanib treatment beyond the clinical trials, adopting a time and ranibizumab but most were mild to moderate. horizon of 10 years. Drug costs for 1 year of treatment were estimated as Results: The combined analysis of two randomised £4626 for pegaptanib and £9134 for ranibizumab. Non- controlled trials (RCTs) of pegaptanib [0.3 mg (licensed drug costs accounted for an additional £2614 for dose), 1.0 mg and 3.0 mg] versus sham injection in pegaptanib and £3120 for ranibizumab. Further costs patients with all lesion types was reported by three are associated with the management of injection- publications (the VISION study). Three published RCTs related adverse events, from £1200 to £2100. For of ranibizumab were identified (MARINA, ANCHOR, pegaptanib compared with usual care, the incremental FOCUS), and an additional unpublished RCT was cost-effectiveness ratio (ICER) ranged from £163,603 provided by the manufacturer (PIER). Significantly more for the 2-year model to £30,986 for the 10-year model. patients lost less than 15 letters of visual acuity at 12 Similarly, the ICERs for ranibizumab for patients with months when taking pegaptanib (0.3 mg: 70% of minimally classic and occult no classic lesions, patients; 1.0 mg: 71% of patients; 3.0 mg: 65% of compared with usual care, ranged from £152,464 for patients) or ranibizumab (0.3 mg: 94.3–94.5%; 0.5 mg: the 2-year model to £25,098 for the 10-year model. 94.6–96.4%) than sham injection patients (55% versus Conclusions: Patients with AMD of any lesion type pegaptanib and 62.2% versus ranibizumab) or, in the benefit from treatment with pegaptanib or ranibizumab case of ranibizumab, photodynamic therapy (PDT) on measures of visual acuity when compared with sham (64.3%). The proportion of patients gaining 15 letters injection and/or PDT. Patients who continued iii © Queen’s Printer and Controller of HMSO 2008. All rights reserved. Abstract treatment with either drug appeared to maintain investigate the role of verteporfin PDT in combination benefits after 2 years of follow-up. When comparing with these drugs. Studies are also needed to assess pegaptanib and ranibizumab, the evidence was less adverse events outside the proposed RCTs, to consider clear due to the lack of direct comparison through the optimal dosing regimes of these drugs and the head-to-head trials and the lack of opportunity for benefits of re-treatment after initial treatment, and to indirect statistical comparison due to heterogeneity. review costing in more detail. Health state utilities and The cost-effectiveness analysis showed that the two their relationship with visual acuity and contrast drugs offered additional benefit over the comparators sensitivity, the relationship between duration of vision of usual care and PDT but at increased cost. Future loss and the quality of life and functional impact of research should encompass trials to compare vision loss, behavioural studies of those genetically at pegaptanib with ranibizumab and bevacizumab, and to risk are other topics requiring further research. iv Health Technology Assessment 2008; Vol. 12: No. 16 Contents Glossary and list of abbreviations ............. vii Appendix 3 Quality assessment ................ 121 Executive summary .................................... ix Appendix 4 Data extraction tables ............ 123 1 Background ................................................ 1 Appendix 5 List of selected excluded Description of health problem ................... 1 studies ......................................................... 147 Current service provision ........................... 11 Description of technology under Appendix 6 List of eligible abstracts ......... 149 assessment .................................................. 13 Appendix 7 List of ongoing studies .......... 151 2 Definition of the decision problem ............ 17 Decision problem ....................................... 17 Appendix 8 Critique of industry Overall aims and objectives of submissions ................................................. 153 assessment .................................................. 17 Appendix 9 Ocular adverse events in study 3 Assessment of clinical effectiveness .......... 19 eye: CIC information from ranibizumab Methods for reviewing effectiveness .......... 19 studies ......................................................... 157 Results ........................................................ 20 Discussion of clinical effectiveness ............. 38 Appendix 10 Non-ocular adverse events: Summary of clinical effectiveness .............. 39 CIC information from ranibizumab studies ......................................................... 159 4 Assessment of cost-effectiveness .............. 43 Introduction ............................................... 43 Appendix 11 Summary of measures Systematic review of existing reported in studies included in the review cost-effectiveness evidence ......................... 43 of quality of life in AMD ............................ 161 Independent economic assessment ........... 58 Appendix 12 Critical appraisal checklist 5 Assessment of factors relevant to the of economic evaluation in Pfizer NHS and other parties .............................. 87 submission .................................................. 165 6 Discussion ................................................... 89 Appendix 13 Critical appraisal checklist Statement of principal findings ................. 89 of economic evaluation in Novartis Strengths and limitations of the submission .................................................. 167 assessment .................................................. 93 Uncertainties .............................................. 94 Appendix 14 Variables included in Other relevant factors ................................ 94 probabilistic sensitivity analysis .................. 169 7 Conclusions ................................................ 97 Appendix 15 Additional analysis Implications for service provision .............. 97 commissioned by the NHS R&D HTA Suggested research priorities ..................... 98 Programme on behalf of the National Institute for Health and Clinical Acknowledgements .................................... 99 Excellence ................................................... 171 References .................................................. 101 Health Technology Assessment reports published to date ....................................... 203 Appendix 1 Protocol methods .................. 109 Health Technology Assessment Appendix 2 Literature search strategies ..... 113 Programme ................................................ 219 v Health Technology Assessment 2008; Vol. 12: No. 16 Glossary and list of abbreviations Technical terms and abbreviations are used throughout this report. The meaning is usually clear from the context, but a glossary is provided for the non-specialist reader. In some cases, usage differs in the literature, but the term has a constant meaning throughout this review. Glossary Vascular endothelial growth factor (VEGF, contributors to physiological or pathological VEGF-A) This is a protein that plays a critical conditions that can stimulate the formation of role in angiogenesis (development of new new blood vessels. blood vessels) and serves as one of the List of abbreviations ACD Appraisal Consultation Document FA fluorescein angiography AMD age-related macular degeneration FDA Food and Drug Administration AREDS Age-related Eye Disease Study ICD International Classification of Diseases ARM age-related maculopathy ICER incremental cost-effectiveness ratio ARMD age-related macular degeneration ITT intention-to-treat BNF British National Formulary IVI Impact of Vision Impairment CI confidence interval MAR minimum angle of resolution CIC commercial-in-confidence CNV choroidal neovascularisation MLRM multinomial logistic regression model CRD Centre for Reviews and Dissemination NEI-VFQ National Eye Institute Visual Function Questionnaire CVI Certificate of Vision Impairment NICE National Institute for Health and DA optic disc area (measurement of Clinical Excellence lesion size: DA = 2.54 mm2) OCT optical coherence tomography ETDRS Early Treatment Diabetic Retinopathy Study PDT photodynamic therapy continued vii © Queen’s Printer and Controller of HMSO 2008. All rights reserved. Glossary and list of abbreviations List of abbreviations continued POMS Profile of Mood States SF-36 Short Form with 36 Items PSS Personal Social Services SPC Summary of Product Characteristics QALY quality-adjusted life-year TAP Treatment of Age-related Macular QWB Quality of Well-Being Degeneration with Photodynamic Therapy RCT randomised controlled trial TTO time trade-off RNIB Royal National Institute for the Blind VAR visual acuity rating RPE retinal pigment epithelium VEGF, vascular endothelial growth factor VEGF-A (-A). SD standard deviation VIP Verteporfin in Photodynamic SG standard gamble Therapy SF-12 Short Form with 12 Items All abbreviations that have been used in this report are listed here unless the abbreviation is well known (e.g. NHS), or it has been used only once, or it is a non-standard abbreviation used only in figures/tables/appendices in which case the abbreviation is defined in the figure legend or at the end of the table. viii

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