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Gout, Hyperuricaemia and Crystal-Associated Disease Network (G-CAN) consensus statement regarding labels and definitions of disease states of gout
  1. David Bursill1,
  2. William J Taylor2,3,
  3. Robert Terkeltaub4,
  4. Abhishek Abhishek5,
  5. Alexander K So6,
  6. Ana Beatriz Vargas-Santos7,
  7. Angelo Lino Gaffo8,
  8. Ann Rosenthal9,10,
  9. Anne-Kathrin Tausche11,
  10. Anthony Reginato12,
  11. Bernhard Manger13,
  12. Carlo Sciré14,15,
  13. Carlos Pineda16,
  14. Caroline van Durme17,
  15. Ching-Tsai Lin18,
  16. Congcong Yin19,
  17. Daniel Arthur Albert20,
  18. Edyta Biernat-Kaluza21,
  19. Edward Roddy22,
  20. Eliseo Pascual23,24,
  21. Fabio Becce25,
  22. Fernando Perez-Ruiz26,27,28,
  23. Francisca Sivera29,
  24. Frédéric Lioté30,31,
  25. Georg Schett32,
  26. George Nuki33,
  27. Georgios Filippou34,
  28. Geraldine McCarthy35,36,
  29. Geraldo da Rocha Castelar Pinheiro37,
  30. Hang-Korng Ea38,
  31. Helena De Almeida Tupinambá39,
  32. Hisashi Yamanaka40,41,
  33. Hyon K Choi42,
  34. James Mackay43,
  35. James R ODell44,
  36. Janitzia Vázquez Mellado45,
  37. Jasvinder A Singh46,47,48,
  38. John D Fitzgerald49,
  39. Lennart T H Jacobsson50,
  40. Leo Joosten51,
  41. Leslie R Harrold52,53,
  42. Lisa Stamp54,
  43. Mariano Andrés55,56,
  44. Marwin Gutierrez57,
  45. Masanari Kuwabara58,59,
  46. Mats Dehlin60,
  47. Matthijs Janssen61,
  48. Michael Doherty5,
  49. Michael S Hershfield62,
  50. Michael Pillinger63,
  51. N Lawrence Edwards64,
  52. Naomi Schlesinger65,
  53. Nitin Kumar66,
  54. Ole Slot67,
  55. Sebastien Ottaviani68,
  56. Pascal Richette69,
  57. Paul A MacMullan70,
  58. Peter T Chapman71,
  59. Peter E Lipsky72,
  60. Philip Robinson73,
  61. Puja P Khanna74,
  62. Rada N Gancheva75,
  63. Rebecca Grainger76,77,
  64. Richard J Johnson78,
  65. Ritch Te Kampe17,
  66. Robert T Keenan79,
  67. Sara K Tedeschi80,81,
  68. Seoyoung Kim82,
  69. Sung Jae Choi83,
  70. Theodore R Fields84,
  71. Thomas Bardin85,
  72. Till Uhlig86,
  73. Tim Jansen87,
  74. Tony Merriman88,
  75. Tristan Pascart89,
  76. Tuhina Neogi90,
  77. Viola Klück91,
  78. Worawit Louthrenoo92,
  79. Nicola Dalbeth93
  1. 1 Department of Health and Medical Sciences, The University of Adelaide, Adelaide, South Australia, Australia
  2. 2 Department of Medicine, University of Otago, Wellington, New Zealand
  3. 3 Wellington Regional Rheumatology Unit, Hutt Valley District Health Board, Lower Hutt, New Zealand
  4. 4 Department of Rheumatology, UCSD/ VA Medical Center, San Diego, California, USA
  5. 5 Department of Academic Rheumatology, University of Nottingham, Nottingham, UK
  6. 6 Department of Musculoskeletal Medicine, Service de RMR, Lausanne, Switzerland
  7. 7 Department of Internal Medicine, Rheumatology Unit, State University of Rio de Janeiro, Rio de Janeiro, Brazil
  8. 8 Department of Medicine, University of Alabama at Birmingham, Birmingham, Alabama, USA
  9. 9 Division of Rheumatology, Medical College of Wisconsin, Milwaukee, Wisconsin, USA
  10. 10 Translational Research Unit, Clement J Zablocki VA Medical Center, Milwaukee, Wisconsin, USA
  11. 11 Department of Rheumatology, University Hospital 'Carl Gustav Carus' of the Technical University Dresden, Dresden, Germany
  12. 12 Division of Rheumatology, The Warren Alpert School of Medicine at Brown University, Providence, Rhode Island, USA
  13. 13 Rheumatology and Immunology, Universität Erlangen-Nürnberg, Erlangen, Germany
  14. 14 Section of Rheumatology, Department of Medical Sciences, University of Ferrara, Ferrara, Italy
  15. 15 Epidemiology Unit, Italian Society for Rheumatology, Milan, Italy
  16. 16 Department of Rheumatology, Instituto Nacional de Rehabilitación Luis Guillermo Ibarra Ibarra, Mexico City, Mexico
  17. 17 Department of Internal Medicine, Division of Rheumatology, Maastricht University Medical Centre, Maastricht, The Netherlands
  18. 18 Division of Allergy, Immunology and Rheumatology, Taichung Veterans General Hospital, Taichung, Taiwan
  19. 19 Department of Immunology and Dermatology, Henry Ford Health System, Detroit, Michigan, USA
  20. 20 Department of Rheumatology, Dartmouth-Hitchcock Medical Center, Hanover, New Hampshire, USA
  21. 21 Outpatient Rheumatology Clinic, Nutritional and Lifestyle Medicine Centre, ORLIK, Warsaw, Poland
  22. 22 Research Institute for Primary Care and Health Sciences, Keele University, Keele, UK
  23. 23 Department of Rheumatology, Hospital General Universitario de Alicante, Alicante, Spain
  24. 24 Departamento de Medicina Clínica, Universidad Miguel Hernández, Alicante, Spain
  25. 25 Department of Diagnostic and Interventional Radiology, University of Lausanne, Lausanne, Switzerland
  26. 26 Rheumatology Division, Cruces University Hospital, Baracaldo, Spain
  27. 27 Department of Medicine, University of the Basque Country, Biscay, Spain
  28. 28 Investigation Group for Arthritis, Biocruces Health Research Institute, Baracaldo, Spain
  29. 29 Department of Rheumatology, Hospital General Universitario Elda, Elda, Spain
  30. 30 Department of Rhumatologie, Hôpital Lariboisière, Assistance Publique-Hopitaux de Paris, Paris, France
  31. 31 Department of Rhumatologie, INSERM UMR-1132 and Université Paris Diderot, Paris, France
  32. 32 Department of Internal Medicine III, Friedrich-Alexander University Erlangen-Nürnberg and Universitatsklinikum Erlangen, Erlangen, Germany
  33. 33 Insititute of Genetics and Molecular Medicine, University of Edinburgh, Edinburgh, UK
  34. 34 Section of Rheumatology, Department of Medical Sciences, University of Ferrara, Ferrara, Italy
  35. 35 Department of Rheumatology, Mater Misericordiae University Hospital, Dublin, Ireland
  36. 36 School of Medicine and Medical Science, University College Dublin, Dublin, Ireland
  37. 37 Department of Internal Medicine, Rheumatology Unit, State University of Rio de Janeiro, Rio de Janeiro, Brazil
  38. 38 Department of Rheumatology, Hôpital Lariboisière, Paris, France
  39. 39 Rheumatology, State University of Rio de Janeiro, Rio de Janeiro, Brazil
  40. 40 Institute of Rheumatology, Tokyo Women's Medical University Hospital, Tokyo, Japan
  41. 41 School of Medicine, Tokyo Women’s Medical University, Tokyo, Japan
  42. 42 Section of Rheumatology and Clinical Epidemiology, Harvard Medical School and Massachusetts General Hospital, Boston, Massachusetts, USA
  43. 43 President and CEO, Aristea Therapeutics, San Diego, California, USA
  44. 44 Division of Rheumatology, University of Nebraska Medical Center, Omaha, Nebraska, USA
  45. 45 Department of Rheumatology, Hospital General de Mexico and Universidad Nacional Autónoma de México, Mexico City, Mexico
  46. 46 Department of Medicine at School of Medicine, University of Alabama at Birmingham, Birmingham, Alabama, USA
  47. 47 Medicine Service, Birmingham Veterans Affairs Medical Center, Birmingham, Alabama, USA
  48. 48 Division of Epidemiology at School of Public Health, University of Alabama at Birmingham, Birmingham, Alabama, USA
  49. 49 Department of Medicine/Rheumatology, David Geffen School of Medicine at the University of California, Los Angeles, Los Angeles, California, USA
  50. 50 Department of Rheumatology and Inflammation Research, Institute of Medicine, The Sahlgrenska Academy, University of Gothenburg, Gothenburg, Sweden
  51. 51 Department of Internal Medicine, Radboud University Medical Center Nijmegen, Nijmegen, The Netherlands
  52. 52 Department of Medicine, University of Massachusetts Medical School, Worcester, Massachusetts, USA
  53. 53 Chief Scientific Officer, Corrona, LLC, Southborough, Massachusetts, USA
  54. 54 Department of Medicine, Otago University, Christchurch, New Zealand
  55. 55 Department of Rheumatology, Hospital Universitario de Alicante, Alicante, Spain
  56. 56 Departamento de Medicina Clínica, Universidad Miguel Hernández, Alicante, Spain
  57. 57 Division of Musculoskeletal and Rheumatic Diseases, Instituto Nacional Rehabilitación, México City, México
  58. 58 Division of Renal Diseases and Hypertension, University of Colorado Denver School of Medicine, Aurora, Colorado, USA
  59. 59 Department of Cardiology, Toranomon Hospital, Minato-ku, Japan
  60. 60 Department of Rheumatology and Inflammation Research, Sahlgrenska Academy, University of Göteborg, Göteborg, Sweden
  61. 61 Department of Rheumatology, VieCuri Medical Centre, Venlo, The Netherlands
  62. 62 Division of Rheumatology, Duke University Medical Center, Durham, North Carolina, USA
  63. 63 Department of Rheumatology/Medicine, New York University School of Medicine, New York City, New York, USA
  64. 64 College of Medicine, University of Florida, Gainesville, Florida, USA
  65. 65 Department of Medicine, Rutgers-Robert Wood Johnson Medical School, New Brunswick, New Jersey, USA
  66. 66 Department of Internal Medicine, Division of Cardiovascular Medicine, University of Michigan, Ann Arbor, Detroit, Michigan, USA
  67. 67 Department of Rheumatology, Copenhagen Center for Arthritis Research, Center for Rheumatology and Spinal Disorders, Rigshospitalet Glostrup, Glostrup, Denmark
  68. 68 Department of Rheumatology, Bichat-Claude Bernard Hospital, University of Sorbonne Paris Cité, Paris, France
  69. 69 Service de Rhumatologie, Hôpital Lariboisière, Assistance Publique-Hopitaux de Paris, and INSERM UMR-1132 and Université de Paris, Paris, France
  70. 70 Division of Rheumatology, University of Calgary, Calgary, Alberta, Canada
  71. 71 Department of Rheumatology, Immunology and Allergy, Canterbury District Health Board, Christchurch, New Zealand
  72. 72 CEO and CMO, AMPEL BioSolutions, LLC, Charlottesville, Virginia, USA
  73. 73 School of Clinical Medicine, Faculty of Medicine, The University of Queensland, Brisbane, Queensland, Australia
  74. 74 Department of Rheumatology, University of Michigan, Ann Arbor, Michigan, USA
  75. 75 Clinic of Rheumatology, University Hospital ‘St. Ivan Rilski’, Sofia, Bulgaria
  76. 76 Department of Medicine, University of Otago, Wellington, Wellington, New Zealand
  77. 77 Wellington Regional Rheumatology Unit, Hutt Valley District Health Board, Lower Hutt, New Zealand
  78. 78 Division of Renal Diseases and Hypertension, University of Colorado Denver, Denver, Colorado, USA
  79. 79 Division of Rheumatology, Duke University School of Medicine, Durham, North Carolina, USA
  80. 80 Division of Rheumatology, Immunology and Allergy, Brigham and Women's Hospital, Boston, Massachusetts, USA
  81. 81 Arthritis Center, Harvard Medical School, Boston, Massachusetts, USA
  82. 82 Department of Medicine, Brigham and Women's Hospital, Boston, Massachusetts, USA
  83. 83 Division of Rheumatology, Department of Internal Medicine, Korea University Medical College, Ansan, South Korea
  84. 84 Weill Cornell Medical College, Hospital for Special Surgery, New York City, New York, USA
  85. 85 Department of Rheumatology, Hôpital Lariboisière, Assistance Publique-Hopitaux de Paris, and INSERM UMR-1132 and Université de Paris, Paris, France
  86. 86 Department of Rheumatology, Diakonhjemmet Hospital, Oslo, Norway
  87. 87 Department of Rheumatology, VieCuri Medical Centre, Venlo, The Netherlands
  88. 88 Department of Biochemistry, University of Otago, Dunedin, New Zealand
  89. 89 Department of Rheumatology, Lille Catholic University, Saint-Philibert Hospital, Lomme, France
  90. 90 Section of Rheumatology, Department of Medicine, Boston University School of Medicine, Boston, Massachusetts, USA
  91. 91 Department of Internal Medicine, Radboud Institute for Molecular Life Sciences, Radboud University Medical Center, Nijmegen, The Netherlands
  92. 92 Division of Rheumatology, Department of Internal Medicine, Faculty of Medicine, Chiang Mai University, Chiang Mai, Thailand
  93. 93 Department of Medicine, Faculty of Medical and Health Sciences, University of Auckland, Auckland, New Zealand
  1. Correspondence to Dr David Bursill, Health and Medical Sciences, The University of Adelaide, Adelaide, SA 5005, Australia; davebursill{at}bigpond.com

Abstract

Objective There is a lack of standardisation in the terminology used to describe gout. The aim of this project was to develop a consensus statement describing the recommended nomenclature for disease states of gout.

Methods A content analysis of gout-related articles from rheumatology and general internal medicine journals published over a 5-year period identified potential disease states and the labels commonly assigned to them. Based on these findings, experts in gout were invited to participate in a Delphi exercise and face-to-face consensus meeting to reach agreement on disease state labels and definitions.

Results The content analysis identified 13 unique disease states and a total of 63 unique labels. The Delphi exercise (n=76 respondents) and face-to-face meeting (n=35 attendees) established consensus agreement for eight disease state labels and definitions. The agreed labels were as follows: ‘asymptomatic hyperuricaemia’, ‘asymptomatic monosodium urate crystal deposition’, ‘asymptomatic hyperuricaemia with monosodium urate crystal deposition’, ‘gout’, ‘tophaceous gout’, ‘erosive gout’, ‘first gout flare’ and ‘recurrent gout flares’. There was consensus agreement that the label ‘gout’ should be restricted to current or prior clinically evident disease caused by monosodium urate crystal deposition (gout flare, chronic gouty arthritis or subcutaneous tophus).

Conclusion Consensus agreement has been established for the labels and definitions of eight gout disease states, including ‘gout’ itself. The Gout, Hyperuricaemia and Crystal-Associated Disease Network recommends the use of these labels when describing disease states of gout in research and clinical practice.

  • gout
  • urate
  • hyperuricemia
  • monosodium urate crystals
  • nomenclature
  • language
  • terminology

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Key messages

What is already known about this subject?

  • The language used to describe gout is characterised by a lack of consistent terminology and definitions.

What does this study add?

  • Consensus agreement has been reached about the labels and definitions of disease states of gout.

  • The agreed labels are as follows: ‘asymptomatic hyperuricaemia’, ‘asymptomatic monosodium urate crystal deposition’, ‘asymptomatic hyperuricaemia with monosodium urate crystal deposition’, ‘gout’, ‘tophaceous gout’, ‘erosive gout’, ‘first gout flare’ and ‘recurrent gout flares’.

  • The label ‘gout’ should be restricted to current or prior clinically evident disease caused by monosodium urate crystal deposition.

How might this impact on clinical practice or future developments?

  • The Gout, Hyperuricaemia and Crystal-Associated Disease Network recommends the use of these labels when communicating in the scientific literature and in professional practice.

Introduction

The language used to describe gout is characterised by a lack of consistent terminology and definitions.1 2 In particular, many different terms are used interchangeably to describe different disease states and their constituent features. This lack of agreement and clarity has implications for how disease-related concepts are communicated in both clinical and research settings.3–5 Notably, there is no universally accepted definition of ‘gout’ itself.6

The Gout, Hyperuricaemia and Crystal-Associated Disease Network (G-CAN) is an international, multidisciplinary network for collaborative research, committed to advancing all aspects of the crystal deposition-associated disorders. G-CAN has supported a project to establish consensus agreement on the nomenclature of hyperuricaemia and gout, its primary objective being the promotion of accurate, well defined terms that facilitate understanding of disease-related concepts. The intended audience is healthcare professionals and non-physician scientists in clinical and research settings.

In the first stage of the G-CAN gout nomenclature project, consensus agreement was reached on the labels and definitions of the disease elements of gout. The content analysis of the literature and subsequent G-CAN-endorsed consensus statement have been published, with the results of the latter summarised in table 1.1 7 This initial work provided labels and definitions for clinical elements including gout flare, chronic gouty arthritis and subcutaneous tophus, as well as imaging elements such as gouty bone erosion. Using these results as a framework, the objective of this second stage of the G-CAN gout nomenclature project was to reach agreement on the nomenclature of disease states of gout. For the purpose of this project, a disease state was defined as ‘a clinically meaningful cluster of the presence, or absence, of two or more disease elements’. Here, we describe the process and outcomes of this project addressing the labels and definitions of the disease states of gout.

Table 1

G-CAN endorsed labels and definitions of the disease elements of gout7

Methods

This work consisted of three components: a content analysis of the literature, a Delphi exercise and a face-to-face consensus meeting. The content analysis of the literature was performed to identify the language currently used to represent disease states of gout. The results of this analysis were then used as the basis for two group consensus exercises—a Delphi exercise and a face-to-face meeting—with the overall objective of reaching agreement on a nomenclature for disease states of gout. A schematic representation of these project components is shown in figure 1.

Figure 1

Outline of the project to develop the G-CAN consensus statement regarding the labels and definitions of disease states of gout. G-CAN, Gout, Hyperuricaemia and Crystal-Associated Disease Network.

Content analysis of the literature

This component of the project had two aims: first, to establish the range of disease states described in the contemporary gout-related and hyperuricaemia-related literature; and second, to identify the labels currently used to denote these disease states. Articles were extracted from the 10 highest-ranked general rheumatology journals, and the five highest-ranked general internal medicine journals (according to Impact Factor, 2016 Thomson-Reuters Journal Citation Reports) published between first January 2013 and 31 January 2018. These journals are shown in supplementary table S1. Relevant articles within each journal were identified through MEDLINE using the search terms ‘gout’ or ‘urate’ or ‘hyperuricaemia’ without exclusion criteria. This methodology was used to provide a suitably large representation of contemporary literature for the extraction of disease states and their labels, with the intention of reflecting the current language of gout and hyperuricaemia, rather than its progression over time.

For the purpose of this project, a disease state was defined as a ‘clinically meaningful cluster of the presence, or absence, of two or more disease elements’. The G-CAN-endorsed labels and definitions for the disease elements of gout are summarised in table 1. A cluster was considered ‘meaningful’ if the co-occurrence of these disease elements had the potential to impact either disease prognosis or management. Articles were manually searched for passages of text referring to the collective presence, or absence, of two or more disease elements. Labels for each identified disease state were extracted to determine the range and frequency of unique labels. Disease state labels were taken verbatim from the examined text, except where the labels for component disease elements were modified to comply with existing G-CAN consensus statement for disease elements (as shown in table 1). Labels were considered ‘unique’ if they used different words or phrases to describe a disease state. For each article, the use of a unique label was recorded only once. All articles were analysed by a single investigator (DB). To ensure the accuracy of the disease state and label identification, the first 10 articles examined were jointly reviewed by a second investigator (ND) with 98% agreement on identified disease element clusters.

Delphi exercise

The Delphi exercise was conducted as a series of three web-based surveys using Survey MonkeyTM software (SurveyMonkey, San Mateo, CA, USA). Physicians and non-physician scientists with expertise in gout were identified through their membership of G-CAN and invited by email to participate in the first round of the survey. Subsequent rounds were only made available to those who had engaged in the previous surveys. In each survey, respondents were presented with disease states identified by the content analysis of the literature, represented by the disease element clusters. Respondents were first asked if each proposed disease state was meaningful for disease prognosis or management. Next, respondents were asked to select and rank their preferred labels for each disease state from a list of options derived from the content analysis of the literature; labels were included if present in at least two of the articles analysed, with the frequency with which they occurred in the literature also shown. In the first round, respondents were also able to nominate their own preferred disease states or labels that had not already been presented; these were included as voting options in the second round of the Delphi if nominated by at least two respondents. Respondents were given the option to comment on disease states or labels that they felt either strongly for or against; a thematic summary of these comments was provided as group feedback in subsequent rounds according to Delphi principles. Disease state label options were refined as the Delphi rounds progressed. Voting on whether a disease state was meaningful, and for its preferred label, ceased once consensus agreement was achieved, defined as at least 80% agreement.

Face-to-face meeting

The face-to-face meeting took place on 20 October 2018 in Chicago, IL. All G-CAN members were invited to attend irrespective of their involvement in the Delphi exercise. There were two main objectives for this meeting. The first objective was to address those disease states for which consensus agreement was not met at the conclusion of the Delphi exercises, either for whether they were meaningful, or for the preferred label. The second objective was to agree on a definition for each disease state included in the final consensus statement. Attendees were provided pre-reading that included a summary of the content analysis of the literature, results of the Delphi exercise and draft definitions of the disease states as a starting point for discussion. The meeting was conducted as a facilitated discussion, moderated by two investigators (DB and ND). Key points raised by attendees were summarised, refined by group discussion and then brought forward for voting by show of hands. Consensus agreement was defined as at least 80% agreement by those present at the time of voting.

The group was first asked to consider which of the proposed disease states should be included in the nomenclature based on the results of the Delphi exercise. It was agreed that only those disease states that had achieved consensus agreement as being meaningful following the three rounds of the Delphi exercise would be included. Next, disease state labels for which consensus agreement had not been reached during the Delphi exercise were discussed and voted on. Finally, the definitions for each disease state were developed and iteratively modified until consensus agreement was reached.

G-CAN endorsement

The results of the project and consensus nomenclature statement have been reviewed and endorsed by the G-CAN Board of Directors.

Results

Content analysis of the literature

A total of 539 articles were extracted using the search criteria. Analysis of these articles identified 13 disease states that were categorised into pre-clinical states, clinical states and states describing the disease course of gout (table 2). In total, there were 63 unique labels identified for these 13 disease states. A detailed description of these results is shown in the supplementary material.

Table 2

Results of the content analysis of 539 gout-related and hyperuricaemia-related articles: disease element clusters identified as potentially meaningful disease states of gout and characteristics of their labels

Delphi exercise

In all, 76 G-CAN members responded to the first round of the survey; of these, 72 (95%) completed all three rounds. The respondents included 34 members from Europe (45%), 24 from North America (32%), 13 from the Asia-Pacific region (17%) and five from Latin America (7%). The majority of respondents were rheumatologists (n=67, 88%); other physician specialists (n=4, 5%) and non-physician scientists (n=5, 7%) also participated.

Of the 13 disease states identified from the content analysis of the literature, nine were deemed to be meaningful by consensus agreement (table 3). Of these nine disease states deemed to be meaningful, seven disease states reached consensus agreement on their preferred label: ‘asymptomatic hyperuricaemia’, ‘asymptomatic monosodium urate crystal deposition’, ‘severe gout’, ‘tophaceous gout’, ‘erosive gout’, ‘first gout flare’ and ‘recurrent gout flares’ (table 4). A detailed description of the Delphi exercise results regarding whether disease states were meaningful and preferred labels is shown in the supplementary material.

Table 3

Results of the Delphi exercise for agreement about whether the proposed gout disease states are meaningful*

Table 4

Results of the Delphi exercise and face-to-face consensus meeting for agreement on the labels for the disease states of gout

Face-to-face meeting

A total of 35 G-CAN members attended the face-to-face meeting, the majority of whom were rheumatologists (n=33, 94%). Of those attending, 32 (91%) had also participated in all three rounds of the Delphi exercise. The panel included 18 members from Europe (51%), 11 from North America (31%), 4 from the Asia-Pacific region (11%) and 2 from Latin America (6%). The number of attendees participating in voting activities during the meeting varied from 28 to 35.

Agreement about which disease states are meaningful

The first item raised was the proposal that only disease states reaching consensus agreement as being meaningful during the Delphi exercise should be included within the final disease state consensus statement. This proposal was unanimously agreed on (35 of 35 voting in favour), reducing the total number of disease states for consideration to nine; this was further reduced to eight when it was unanimously agreed to eliminate the disease state ‘the presence of monosodium urate crystals with any of the following: frequent recurrent gout flares, chronic gouty arthritis, subcutaneous tophi or imaging disease elements of gout’. This disease state, labelled ‘severe gout’ through the Delphi exercise, was thought to be a broad, non-specific state that would be difficult to define in clinical and research settings. It was also considered to be potentially misleading for gout treatment; for example, it might imply that patients not fulfilling this definition have ‘non-severe gout’ and that urate lowering therapy is not warranted in this case. For the cluster of disease elements, ‘hyperuricaemia with imaging evidence of monosodium urate crystal deposition but without clinical disease elements of gout’, consensus agreement on this state being meaningful was achieved through the Delphi exercise. However, a number of respondents commented that this state was similar to the disease state, ‘asymptomatic monosodium urate crystal deposition’, and therefore may be redundant. After being put to vote, it was unanimously agreed (35/35 in favour) that this represented a unique and meaningful disease state, distinct from ‘asymptomatic monosodium urate crystal deposition’ which could represent a state of asymptomatic crystal deposition irrespective of serum urate concentration. The final eight disease states deemed meaningful by consensus agreement at the conclusion of both the Delphi exercise and face-to-face meeting are shown in table 5.

Table 5

G-CAN endorsed labels and definitions for the disease states of gout

Disease state labels

Consensus agreement was achieved on two disease state labels that remained unresolved after the Delphi exercise. These consensus labels were: ‘asymptomatic hyperuricaemia with monosodium urate crystal deposition’ and ‘gout’ (table 4). Further details on voting results are shown in supplementary table S2.

For the disease state referring to ‘hyperuricaemia with imaging evidence of monosodium urate crystal deposition but without clinical disease elements of gout’, the label ‘asymptomatic hyperuricaemia with monosodium urate crystal deposition’ was very close to reaching consensus following the Delphi exercise with 79% agreement; after being put to vote, consensus agreement was reached with 33 of 35 (94%) in favour of this label.

The second disease state label that remain unresolved following the Delphi exercise concerned the disease state ‘the presence of monosodium urate crystals with clinical disease elements of gout’. The two most preferred labels for this disease state following the Delphi exercise were ‘gout’ (56% agreement) and ‘symptomatic gout’ (43% agreement). This situation raised the fundamental question of whether ‘gout’ refers to the underlying pathophysiological process of monosodium urate crystal deposition or the clinically evident sequelae of crystal deposition. Consensus agreement for the label ‘gout’ to describe the disease state ‘the presence of monosodium urate crystals with clinical disease elements of gout’ was achieved with 34 of 34 (100%, one abstention) voting in favour. Thus, consensus was reached that the label ‘gout’ should be reserved for clinically evident disease.

Disease state definitions

Consensus agreement was achieved for the definitions of all eight disease states of gout (table 5). Relevant issues arising from group discussions on the composition of these definitions are outlined here. Further details on voting results are shown in supplementary table S2.

When considering the definition of the disease state of gout, it was considered important to include reference to ‘a disease caused by monosodium urate crystal deposition’ resulting in clinical disease elements. Therefore ‘gout’, according to this definition, requires current or prior clinically evident symptoms or signs resulting from monosodium urate crystal deposition. The issue was also raised as to whether ‘monosodium urate crystal-proven’ should be used as a modifier for the label ‘gout’. Although use of this descriptor is popular in clinical practice, it strictly refers to method of diagnosis, which can be achieved through a number of modalities, including synovial fluid analysis, ultrasound or dual-energy CT (DECT). As this does not represent a separate disease state, it was not included in the recommended nomenclature.

Disease state labels not specifically addressed by the nomenclature

Throughout discussions, it was acknowledged that disease states are not necessarily mutually exclusive and that the potential for overlap exists. It was also recognised that a consensus nomenclature cannot formally address all combinations of disease elements of gout. This led to the suggestion of a hierarchical approach to address those disease states that are not formally included in the agreed nomenclature. Specifically, the following recommendation was proposed: ‘Where there is more than one disease state present, these can be combined (eg, ‘tophaceous and erosive gout’). Where there are additional elements present, not recognised as disease states, these will be labelled as the recognised disease state with or without additional disease elements (eg, ‘tophaceous gout with chronic gouty arthritis’)’. This proposal was unanimously agreed on with 27 of 27 voting in favour (100%, one abstention).

Discussion

In this project, we have achieved consensus agreement on the labels and definitions for disease states of gout. This project builds on the G-CAN-endorsed nomenclature for the disease elements of gout,7 which provided a foundation for both the extraction of disease element clusters in the content analysis of the literature, and for the formulation of disease state terminology. The G-CAN endorsed labels for disease elements and for disease states should be used concurrently where appropriate. These technical language labels and definitions for disease states which have been endorsed by G-CAN have been developed for use by healthcare professionals and non-physician scientists in clinical and research settings.

Our content analysis of the literature demonstrated that the existing terminology of the disease states of gout is deficient in a number of key areas. Disease states were, in general, infrequently mentioned, poorly defined or inconsistently labelled in the large body of contemporary gout-related literature that was analysed. With the exception of ‘asymptomatic hyperuricaemia’, little mention was made of pre-clinical disease states defined by the presence of monosodium urate crystal deposition on imaging and the absence of clinical disease elements of gout. Increasing availability of advanced imaging such as ultrasound and DECT will inevitably lead to increased detection of monosodium urate crystal deposition prior to the development of clinical disease. While further research is required regarding the sensitivity and specificity of these imaging modalities, and the implications of these findings for disease management, there is a need to consistently label and define these pre-clinical states. This project has provided consensus labels and definitions for two further pre-clinical disease states: ‘asymptomatic monosodium urate crystal deposition’ and ‘asymptomatic hyperuricaemia with monosodium urate crystal deposition’.

One of the key outcomes of this project was defining the label ‘gout’. There was much discussion about what constitutes ‘gout’, whether it is the presence of monosodium urate crystal deposition, or more specifically, the clinical manifestations resulting from this crystal deposition. In this consensus statement, we recommend the label ‘gout’ be used only when there are current or prior clinical symptoms or signs of monosodium urate crystal deposition (including gout flare, chronic gouty arthritis or subcutaneous tophus). The prognostic significance of asymptomatic monosodium urate crystal deposition is currently uncertain and we recommend that the label ‘gout’ is not used in the absence of current or prior clinical symptoms or signs caused by monosodium urate crystal deposition. Another key outcome was the rejection of non-specific labels of the clinical features of gout, such as ‘severe gout’, which are, despite their ambiguity, present in a number of international gout management guidelines.8–11 Where cluster of elements cannot be described using a single label, guidance has been provided for the use of consistent nomenclature.

In summary, this consensus statement presents recommended labels and definitions for disease states of gout. The G-CAN recommends the use of these labels when communicating in the scientific literature and in professional practice.

Acknowledgments

We wish to thank Pamela Love (G-CAN Executive Director and Board Secretary), Sharon Andrews (G-CAN Executive Assistant) and Andrea Love for assisting in the organisation of the face-to-face consensus meeting.

References

Footnotes

  • Handling editor Josef S Smolen

  • Contributors ND (the guarantor) accepts full responsibility for the work and the conduct of the project, had access to the data and controlled the decision to publish. ND, DB, WJT and RT conceived of the project. DB and ND were responsible for devising the Delphi exercise surveys and the running of the face-to-face meeting, including the analysis of results. All authors participated in either or both of the Delphi exercise and face-to-face consensus meeting. DB and ND drafted the first version of the manuscript. All authors contributed to manuscript revisions and approved the final manuscript.

  • Funding Work by DB was supported by an Australian Rheumatology Association/Arthritis South Australia Post-Graduate Rheumatology grant.RT reports research grants from the VA Research Service (I01 BX001660-06), NIH (AR060772).

  • Competing interests AKT has received speaking fees and honoraria for advisory boards from Berlin Chemie Menarini, Novartis, Grünenthal and AstraZeneca. JAS has received consultant fees from Crealta/Horizon, Medisys, Fidia, UBM LLC, Medscape, WebMD, the National Institutes of Health and the American College of Rheumatology. JAS owns stock options in Amarin pharmaceuticals and Viking therapeutics. JAS is a member of the executive of OMERACT, an organisation that develops outcome measures in rheumatology and receives arms-length funding from 36 companies. JAS is a member of the Veterans Affairs Rheumatology Field Advisory Committee. JAS is the editor and the Director of the UAB Cochrane Musculoskeletal Group Satellite Center on Network Meta-analysis. JAS previously served as a member of the following committees: member, the American College of Rheumatology's (ACR) Annual Meeting Planning Committee (AMPC) and Quality of Care Committees, the Chair of the ACR Meet-the-Professor, Workshop and Study Group Subcommittee and the co-chair of the ACR Criteria and Response Criteria subcommittee. ND has received speaking fees from Pfizer, Horizon, Janssen, and AbbVie, consulting fees from Horizon, AstraZeneca, Dyve Biosciences, Hengrui, and Kowa, and research funding from Amgen and AstraZeneca.

  • Patient consent for publication Not required.

  • Provenance and peer review Not commissioned; externally peer reviewed.

  • Data availability statement Data are available upon reasonable request.