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Recommendation
First Latin American clinical practice guidelines for the treatment of systemic lupus erythematosus: Latin American Group for the Study of Lupus (GLADEL, Grupo Latino Americano de Estudio del Lupus)–Pan-American League of Associations of Rheumatology (PANLAR)
  1. Bernardo A Pons-Estel1,
  2. Eloisa Bonfa2,
  3. Enrique R Soriano3,
  4. Mario H Cardiel4,
  5. Ariel Izcovich5,
  6. Federico Popoff5,
  7. Juan M Criniti5,
  8. Gloria Vásquez6,
  9. Loreto Massardo7,
  10. Margarita Duarte8,
  11. Leonor A Barile-Fabris9,
  12. Mercedes A García10,
  13. Mary-Carmen Amigo11,
  14. Graciela Espada12,
  15. Luis J Catoggio3,
  16. Emilia Inoue Sato13,
  17. Roger A Levy14,
  18. Eduardo M Acevedo Vásquez15,
  19. Rosa Chacón-Díaz16,
  20. Claudio M Galarza-Maldonado17,
  21. Antonio J Iglesias Gamarra18,
  22. José Fernando Molina19,
  23. Oscar Neira20,
  24. Clóvis A Silva21,
  25. Andrea Vargas Peña22,
  26. José A Gómez-Puerta23,
  27. Marina Scolnik3,
  28. Guillermo J Pons-Estel1,24,
  29. Michelle R Ugolini-Lopes2,
  30. Verónica Savio25,
  31. Cristina Drenkard26,
  32. Alejandro J Alvarellos27,
  33. Manuel F Ugarte-Gil28,29,
  34. Alejandra Babini25,
  35. André Cavalcanti30,
  36. Fernanda Athayde Cardoso Linhares22,
  37. Maria Jezabel Haye Salinas27,
  38. Yurilis J Fuentes-Silva31,
  39. Ana Carolina Montandon de Oliveira e Silva32,
  40. Ruth M Eraso Garnica33,
  41. Sebastián Herrera Uribe34,
  42. Diana Gómez-Martín35,
  43. Ricardo Robaina Sevrini36,
  44. Rosana M Quintana1,24,
  45. Sergio Gordon37,
  46. Hilda Fragoso-Loyo35,
  47. Violeta Rosario38,
  48. Verónica Saurit27,
  49. Simone Appenzeller39,
  50. Edgard Torres dos Reis Neto13,
  51. Jorge Cieza40,
  52. Luis A González Naranjo6,
  53. Yelitza C González Bello41,
  54. María Victoria Collado42,
  55. Judith Sarano42,
  56. Soledad Retamozo27,
  57. María E Sattler43,
  58. Rocio V Gamboa-Cárdenas28,
  59. Ernesto Cairoli36,
  60. Silvana M Conti24,
  61. Luis M Amezcua-Guerra44,
  62. Luis H Silveira45,
  63. Eduardo F Borba2,
  64. Mariana A Pera10,
  65. Paula B Alba Moreyra46,
  66. Valeria Arturi10,
  67. Guillermo A Berbotto43,
  68. Cristian Gerling37,
  69. Carla A Gobbi46,
  70. Viviana L Gervasoni24,
  71. Hugo R Scherbarth37,
  72. João C Tavares Brenol47,
  73. Fernando Cavalcanti30,
  74. Lilian T Lavras Costallat39,
  75. Nilzio A Da Silva32,
  76. Odirlei A Monticielo47,
  77. Luciana Parente Costa Seguro2,
  78. Ricardo M Xavier47,
  79. Carolina Llanos48,
  80. Rubén A Montúfar Guardado49,
  81. Ignacio Garcia de la Torre50,
  82. Carlos Pineda51,
  83. Margarita Portela Hernández52,
  84. Alvaro Danza53,
  85. Marlene Guibert-Toledano54,
  86. Gil Llerena Reyes54,
  87. Maria Isabel Acosta Colman8,
  88. Alicia M Aquino8,
  89. Claudia S Mora-Trujillo40,
  90. Roberto Muñoz-Louis38,
  91. Ignacio García Valladares41,
  92. María Celeste Orozco55,
  93. Paula I Burgos48,
  94. Graciela V Betancur55,
  95. Graciela S Alarcón56,57
  96. on behalf of the Grupo Latino Americano de Estudio del Lupus (GLADEL) and Pan-American League of Associations of Rheumatology (PANLAR)
  1. 1 Departamento de Medicina Interna, Grupo Oroño-Centro Regional de Enfermedades Autoinmunes y Reumáticas (GO-CREAR), Rosario, Argentina
  2. 2 Rheumatology Division, Faculdade de Medicina, Hospital das Clinicas HCFMUSP, Universidade de São Paulo, São Paulo, Brazil
  3. 3 Sección de Reumatología, Servicio de Clínica Médica, Instituto Universitario, Escuela de Medicina, and Fundación Dr Pedro M Catoggio para el Progreso de la Reumatología, Hospital Italiano de Buenos Aires, Buenos Aires, Argentina
  4. 4 Centro de Investigación Clínica de Morelia, SC, Morelia, México
  5. 5 Servicio de Clínica Médica del Hospital Alemán de Buenos Aires, Hospital Alemán de Buenos Aires, Ciudad Autónoma de Buenos Aires, Argentina
  6. 6 Grupo de Inmunología Celular e Inmunogenética, Universidad de Antioquia, Hospital Universitario, Fundación San Vicente, Medellín, Colombia
  7. 7 Centro de Biología Celular y Biomedicina, Facultad de Medicina y Ciencia. Universidad San Sebastián, Santiago, Chile
  8. 8 Departamento de Reumatología, Hospital de Clínicas, Facultad de Ciencias Médicas, Universidad Nacional de Asunción, Asunción, Paraguay
  9. 9 Hospital Angeles del Pedregal, Ciudad de México, México
  10. 10 Servicio de Reumatología, HIGA General San Martín, La Plata, Argentina
  11. 11 Servicio de Reumatología, Centro Médico ABC, Ciudad de México, México
  12. 12 Servicio de Reumatología Infantil, Hospital de Niños Dr Ricardo Gutiérrez, Buenos Aires, Argentina
  13. 13 Escola Paulista de Medicina, Universidade Federal de São Paulo, São Paul, Brazil
  14. 14 Discipline of Rheumatology, University of the State of Rio de Janeiro, Rio de Janeiro, Brasil
  15. 15 Facultad de Medicina., Universidad Nacional Mayor de San Marcos. Servicio de Reumatología. Clínica San Felipe, J. María., Lima, Perú.
  16. 16 Servicio de Reumatología, Policlínica Méndez Gimón, Caracas, Venezuela
  17. 17 Unidad de Enfermedades Reumáticas y Autoinmunes (UNERA), Corporación Médica Monte Sinaí., Cuenca, Ecuador
  18. 18 Universidad Nacional de Colombia, Bogotá, Colombia
  19. 19 Centro Integral de Reumatología, Reumalab, Medellín, Colombia
  20. 20 Sección de Reumatología, Hospital del Salvador. Universidad de Chile. Unidad de Reumatología. Clínica Alemana de Santiago, Facultad de Medicina Clínica Alemana, Universidad del Desarrollo., Santiago, Chile
  21. 21 Pediatric Department, Faculdade de Medicina, Children’s Institute, Hospital das Clinicas HCFMUSP, Universidade de São Paulo, São Paulo, Brazil
  22. 22 Clínica Reumatológica, Universidad de la República, and Unidad Docente Asistencial, Hospital Pasteur, Instituto Nacional de Reumatología., Montevideo, Uruguay
  23. 23 Servicio de Reumatología, Hospital Clinic, Barcelona, Spain
  24. 24 Servicio de Reumatología, Hospital Provincial de Rosario, Rosario, Argentina
  25. 25 Servicio de Reumatología, Hospital Italiano de Córdoba, Córdoba, Argentina
  26. 26 Division of Rheumatology, Department of Medicine, Emory School of Medicine, Atlanta, Georgia, USA
  27. 27 Servicio de Reumatología, Hospital Privado Universitario de Córdoba, Córdoba, Argentina
  28. 28 Servicio de Reumatología, Hospital General Guillermo Almenara Irigoyen, EsSalud., Lima, Perú
  29. 29 Universidad Científica del Sur, Lima, Perú
  30. 30 Serviço de Reumatologia do Hospital das Clínicas da Universidade Federal de Pernambuco (HC-UFPE), Recife, Brazil
  31. 31 Unidad de Reumatología, Departamento de Medicina, Universidad de Oriente, Complejo Hospitalario Universitario Ruiz y Páez, Ciudad Bolívar, Venezuela
  32. 32 Serviço de Reumatologia, Departamento de Clinica Medica, Faculdade de Medicina, Hospital das Clínicas, Universidade Federal de Goiás, Goiânia, Brazil
  33. 33 Departamento de Pediatría, Facultad de Medicina, Universidad de Antioquia, Hospital Pablo Tobón Uribe, Medellín, Colombia
  34. 34 Servicio de Reumatología, Hospital General de Medellín ‘Luz Castro de Gutierrez’ ESE, ARTMEDICA, Medellín, Colombia
  35. 35 Departamento de Inmunología y Reumatología, Instituto Nacional de Ciencias Médicas y Nutrición, Salvador Zubirán, Ciudad de México, Mexico
  36. 36 Unidad de Enfermedades Autoinmunes Sistémicas, Facultad de Medicina, Clínica Médica ‘C’, Hospital de Clínicas, Universidad de la República, Montevideo, Uruguay
  37. 37 Unidad de Reumatología y Enfermedades Autoinmunes Sistémicas, HIGA Dr Oscar Alende, Mar del Plata, Argentina
  38. 38 Servicio de Reumatología, Enfermedades Reumatológicas e Investigación Clínica (ERIC), Hospital Docente Padre Billini, Santo Domingo, Dominican Republic
  39. 39 Departamento de Clínica Médica, Disciplina de Reumatologia, Faculdade de Ciências Medicas da UNICAMP, Universidade Estadual de Campinas, Campinas, Brazil
  40. 40 Servicio de Reumatología, Departamento de Especialidades Médicas, Hospital Nacional Edgardo Rebagliati Martins, EsSalud., Lima, Perú
  41. 41 Servicio de Reumatología, CEIBAC, SC, Guadalajara, México
  42. 42 Servicio de Inmunología, Instituto de Investigaciones Médicas "Alfredo "Lanari", Ciudad Autónoma de Buenos Aires, Argentina
  43. 43 Servicio de Reumatología, Hospital Escuela "Eva Perón", Granadero Baigorria, Argentina
  44. 44 Departamento de Inmunología, Instituto Nacional de Cardiología Ignacio Chávez, Ciudad de México, Mexico
  45. 45 Departamento de Reumatología, Instituto Nacional de Cardiología "Ignacio Chávez", Ciudad de México, México
  46. 46 Unidad de Reumatología, Cátedra de Clínica Médica I, Hospital Córdoba. Cátedra de Semiología, Facultad de Ciencias Médicas, Universidad Nacional de Córdoba., Córdoba, Argentina
  47. 47 Rheumatology Division, Department of Internal Medicine, Hospital de Clínicas de Porto Alegre, Universidade Federal do Rio Grande do Sul, Porto Alegre, Brazil
  48. 48 Departamento de Inmunología Clínica y Reumatología, Escuela de Medicina, Pontificia Universidad Católica de Chile, Santiago, Chile
  49. 49 Departamento de Reumatología, Consultorio de Especialidades del Instituto Salvadoreño de la Seguridad Social, San Salvador, El Salvador
  50. 50 Departamento de Inmunología y Reumatología, Hospital General de Occidente., Zapopan, Jalisco, México.
  51. 51 Instituto Nacional de Rehabilitación Luis Guillermo Ibarra Ibarra, Ciudad de México, Mexico
  52. 52 Departamento de Reumatología, Hospital de Especialidades CMN SXXI, IMSS, Ciudad de México, Mexico
  53. 53 Grupo de Trabajo en Enfermedades Autoinmunes Sistémicas, Servicio de Clínica Médica, Facultad de Medicina, Universidad de la Republica, Hospital Pasteur, Administración de Servicios de Salud del Estado, Montevideo, Uruguay
  54. 54 Servicio Nacional de Reumatología, Centro de Investigaciones Médico Quirúrgicas (CIMEQ)., La Habana, Cuba
  55. 55 Servicio de Reumatología, Instituto de Rehabilitación Psicofísica (IREP), Ciudad Autónoma de Buenos Aires, Argentina
  56. 56 Division of Clinical Immunology and Rheumatology, Department of Medicine, School of Medicine, The University of Alabama at Birmingham, Birmingham, Alabama, USA
  57. 57 Department of Medicine, School of Medicine, Universidad Peruana Cayetano Heredia, Lima, Peru
  1. Correspondence to Dr Mario H Cardiel, Centro de Investigación Clínica de Morelia SC. Morelia, México; mhcardiel{at}hotmail.com

Abstract

Systemic lupus erythematosus (SLE), a complex and heterogeneous autoimmune disease, represents a significant challenge for both diagnosis and treatment. Patients with SLE in Latin America face special problems that should be considered when therapeutic guidelines are developed. The objective of the study is to develop clinical practice guidelines for Latin American patients with lupus. Two independent teams (rheumatologists with experience in lupus management and methodologists) had an initial meeting in Panama City, Panama, in April 2016. They selected a list of questions for the clinical problems most commonly seen in Latin American patients with SLE. These were addressed with the best available evidence and summarised in a standardised format following the Grading of Recommendations Assessment, Development and Evaluation approach. All preliminary findings were discussed in a second face-to-face meeting in Washington, DC, in November 2016. As a result, nine organ/system sections are presented with the main findings; an ‘overarching’ treatment approach was added. Special emphasis was made on regional implementation issues. Best pharmacologic options were examined for musculoskeletal, mucocutaneous, kidney, cardiac, pulmonary, neuropsychiatric, haematological manifestations and the antiphospholipid syndrome. The roles of main therapeutic options (ie, glucocorticoids, antimalarials, immunosuppressant agents, therapeutic plasma exchange, belimumab, rituximab, abatacept, low-dose aspirin and anticoagulants) were summarised in each section. In all cases, benefits and harms, certainty of the evidence, values and preferences, feasibility, acceptability and equity issues were considered to produce a recommendation with special focus on ethnic and socioeconomic aspects. Guidelines for Latin American patients with lupus have been developed and could be used in similar settings.

  • systemic lupus erythematosus
  • treatment
  • lupus nephritis

This is an open access article distributed in accordance with the Creative Commons Attribution Non Commercial (CC BY-NC 4.0) license, which permits others to distribute, remix, adapt, build upon this work non-commercially, and license their derivative works on different terms, provided the original work is properly cited, appropriate credit is given, any changes made indicated, and the use is non-commercial. See: http://creativecommons.org/licenses/by-nc/4.0/.

https://doi.org/10.1136/annrheumdis-2018-213512

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    Introduction

    Systemic lupus erythematosus (SLE) is a complex multisystemic autoimmune disease resulting, oftentimes, in irreversible damage, diminished quality of life and reduced life expectancy.1–3 Genetic and environmental factors play important roles in its pathogenesis.4–8 Disease manifestations and severity vary according to the patients’ racial/ethnic background and socioeconomic status (SES).1 9 10 Data from Grupo Latino Americano de Estudio del Lupus (GLADEL), Lupus in Minorities: Nature vs Nurture (LUMINA) and the Lupus Family Registry and Repository cohorts have demonstrated that Latin American and North American Mestizo patients (mixed Amerindian and European ancestry), African descendants and Native Americans develop lupus earlier11 12 although diagnostic delays may occur.1 They also experience more severe disease, have higher disease activity levels,1 accrue more organ damage2 and have higher mortality rates,1 succumbing mainly to disease activity and/or infections.1 3 13–15

    Although guidelines for SLE treatment do exist and there is scarce evidence to support specific therapies for Latin American patients with lupus,16–21 this regional effort has considered the impact of racial/ethnic background1 10 22–28 and SES3 9 on lupus outcomes and treatment response.25 26 Other medication variables such as cost and availability were also taken into account since they affect adherence and are relevant in decision-making.27 28 GLADEL and the Pan-American League of Associations of Rheumatology have joined efforts to produce these guidelines,29 which are presented by organ systems, although manifestations usually occur in more than one. Nevertheless, treatment is usually tailored to the more severe manifestation(s), which usually benefits the less severe.

    Methods

    Two working teams on logistics and methodological issues constituted by experienced Latin American rheumatologists and experts in the Grading of Recommendations Assessment, Development and Evaluation (GRADE) guideline system developed a framework for these guidelines. Nine organ/system sections were prepared with the main findings. Special emphasis was placed on reviewing local problems and regional publications.

    The GRADE approach was followed in the process (http://www.gradeworkinggroup.org) answering the clinical questions voted most relevant by the panel. The description of the methodology followed to develop these guidelines has already been published.29 All authors listed in this manuscript have participated in planning, drafting, reviewing, final approval and are accountable for all aspects of the manuscript. No ethical approval was required by institutions. We present the final recommendations and their supporting information. Comments from three patients with SLE were also considered.

    Results

    For each of the subheadings listed below, the panel considered interventions based on experience, availability, affordability and a stepwise therapeutic approach of the different alternatives. Standard of care (SOC) was defined as the use of hydroxychloroquine (HCQ) and, if clinically indicated, low-dose glucocorticoids (GC) (prednisone ≤7.5 mg or equivalent for the shortest time).24 Chloroquine remains an alternative for some of the Latin American countries where HCQ is not available and careful monitoring of eye side effect is recommended. Overarching principles are shown in box 1. Tables summarising the evidence that was considered in the process are shown in online supplementary tables in https://doi.org/10.5061/dryad.bg8452h.

    Box 1

    GLADEL–PANLAR Latin American guidelines for the treatment of systemic lupus erythematosus

    Overarching principles

    1. Treatment should be individualised, specialists and generalists should work together and the active involvement of patients and their family members on the overall therapeutic plan should be emphasised.

    2. The therapeutic goal should be to reach and maintain remission or low-disease activity as soon as the diagnosis is made and for as long as possible.

    3. Treatment should include photo-protection, osteoporosis, cardiovascular, metabolic syndrome and infection prevention, psychological support and pregnancy counselling.

    4. All patients with lupus should receive AMs, except those who refuse them or who have absolute contraindications to take them.

    5. GCs, if clinically needed, regardless of patient’s disease manifestations, should be prescribed at the lowest possible dose and for the shortest period of time.

    • AM, antimalarials; GC, glucocorticoid; GLADEL, Grupo Latino Americano de Estudio del Lupus; PANLAR, Pan-American League of Associations of Rheumatology.

    Supplemental material

    Musculoskeletal manifestations

    1. Which is the best treatment for adult patients with SLE and musculoskeletal (MSK) manifestations?

    Interventions considered

    (1) SOC; (2) SOC plus methotrexate (MTX); (3) SOC plus leflunomide (LFN); (4) SOC plus belimumab; (5) SOC plus abatacept (ABT); (6) other options: azathioprine (AZA), mycophenolate mofetil (MMF), cyclosporine A (CsA) or rituximab (RTX) (online supplementary tables S2.1.1, S2.1.4, S2.1.6, S2.1.7, S2.2.11, S2.1.11, S2.1.12, S2.1.14, S2.1.15, S2.1.17, S2.2.1, S2.2.2, S2.2.4, S3.1.1, S3.1.3–S3.1.6, S3.2.1, S3.2.2, S12.2–S12.5, S12.8–S12.10).

    Benefits and harms

    Although the panel judged that compared with SOC alone, adding MTX, LFN, belimumab or ABT is possibly associated with beneficial effects, a significant proportion of patients will achieve adequate symptom control with SOC and could be spared the adverse effects/excess costs associated to those other options.

    Recommendation

    The panel suggests SOC alone over adding other immunosuppressant (IS) in adult patients with SLE with MSK manifestations (weak recommendation based on low certainty of the evidence). It suggests also adding either MTX, LFN, belimumab or ABT to those failing to respond to SOC (weak recommendation based on low to moderate certainty of the evidence). Cost and availability may favour MTX (table 1).

    View this table:
    Table 1

    GLADEL–PANLAR recommendations for musculoskeletal and cutaneous manifestations in patients with systemic lupus erythematosus

    Cutaneous manifestations

    1. Which is the best treatment for adult patients with different manifestations of cutaneous lupus?

    Interventions considered

    (1) SOC; (2) SOC plus MTX; (3) SOC plus AZA; (4) SOC plus MMF; (5) SOC plus CsA; (6) SOC plus belimumab; (7) SOC plus ABT; (8) SOC plus acitretin; (9) SOC plus atacicept; (10) SOC plus cyclophosphamide (CYC) (online supplementary tables S4.1.1–S4.1.7, S4.2.1–S4.2.5, S4.3.1, S4.4.1, S4.4.2, S4.5.1–S4.5.13).

    Benefits and harms

    The panel judged that a significant proportion of patients will achieve adequate symptom control with SOC and could be spared the adverse effects/costs of the other therapies.

    Recommendation

    The panel suggests SOC alone over adding other IS in adult patients with SLE with cutaneous manifestations (weak recommendation based on low certainty of the evidence). It also suggests adding MTX, AZA, MMF, CsA, CYC or belimumab to patients failing to respond to SOC (weak recommendation based on low to moderate certainty of the evidence). Cost and availability may favour MTX and AZA (table 1).

    Adult kidney manifestations

    1. Which is the best induction treatment for adult patients with lupus nephritis?

    Interventions considered

    (1) GCs; (2) GCs plus high-dose CYC; (3) GCs plus low-dose CYC; (4) GCs plus MMF; (5) GCs plus RTX plus MMF; (6) GCs plus tacrolimus (TAC); (7) GCs plus AZA (online supplementary tables S1.1.1.2, S1.1.1.7, S1.1.1.8, S1.1.1.10, S1.1.2.2, S1.1.2.5, S1.1.2.7, S1.1.3.2, S1.1.4.1, S1.2.6).

    Benefits and harms

    Based on the identified evidence the panel concluded that compared with GCs alone, the addition of other IS (CYC, MMF or TAC) is associated with significant benefits, higher remission rates and lower progression rates to end-stage renal disease (ESRD). Head-to-head comparisons between MMF, TAC and high-dose CYC showed that MMF and TAC are associated with less adverse effects than high-dose CYC. Between low and high-dose CYC the balance favours the former because of better safety profile and comparable efficacy, although this conclusion is based on one trial that included predominantly Caucasians. RTX did not provide additional benefits when combined with MMF.

    Recommendation

    The panel recommends SOC (GCs and antimalarials (AM)) in addition to an IS (CYC in high or low doses, MMF or TAC) over GCs alone, for induction in patients with SLE-related kidney disease (strong recommendation based on moderate certainty of the evidence). Although more African-American descendants and Hispanic patients responded to MMF than CYC (25), limited access to MMF and TAC in several Latin American countries, due primarily to cost issues, makes CYC the best alternative for induction (high or low dose) in these regions (table 2).

    ­

    1. Which is the best maintenance treatment for adult patients with lupus nephritis?

    View this table:
    Table 2

    GLADEL–PANLAR recommendations for adult and childhood-onset lupus nephritis

    Interventions considered

    Recommendations are applicable to patients showing partial or total remission after induction therapy aiming at sustaining renal remission, preventing relapses and achieving the best long-term outcome. The following interventions were considered: (1) AZA; (2) MMF; (3) CYC; (4) TAC; and (5) CsA (online supplementary tables S1.1.1.7, S1.1.2.1, S1.1.2.2, S1.2.1, S1.2.3, S1.2.4, S1.2.5, S1.2.6, S1.2.7).

    Benefits and harms

    The panel concluded that long-term IS agents during maintenance therapy prolong stable renal function, reduce proteinuria, extend renal survival and minimise the toxicity of GCs. AZA, CYC, MMF and CsA seem to be equivalent regarding efficacy but MMF and AZA have a better safety profile, particularly regarding gonadal toxicity and blood pressure control. We found very low certainty of the evidence for TAC as maintenance therapy, with studies mostly restricted to Asian populations.

    Recommendation

    The panel recommends AZA or MMF over CYC for maintenance in patients with SLE-related nephritis (strong recommendation based on low certainty of the evidence, since certainty in better efficacy of MMF or AZA over CYC is low but certainty of fewer adverse effects is high). Cost and availability issues may favour AZA (table 2).

    Childhood-onset lupus nephritis

    1. Which is the best induction treatment for childhood-onset lupus nephritis (cLN)?

    Interventions considered

    (1) MMF plus GCs; (2) CYC plus GCs; (3) GCs (online supplementary table S9.2.3).

    Benefits and harms

    The panel concluded that both MMF plus high-dose GCs (prednisone 1–2 mg/kg/day, maximum 60 mg/day) and CYC plus high-dose GCs are associated with significant benefits in comparison to GCs alone. No significant differences between these two alternatives were noted. The panel pointed that differential pharmacokinetic effects of MMF in cLN may exist, which could require dosing increase.30 Risk of reduction of ovarian reserve and sperm abnormalities should be considered in patients with cLN treated with CYC.

    Recommendation

    The panel suggests high-dose GCs plus MMF or CYC over high-dose GCs alone in patients with cLN as induction therapy (weak recommendation based on low certainty of the evidence). Cost and availability may favour CYC despite the risk of gonadal toxicity (table 2).

    ­

    1. Which is the best maintenance treatment for cLN?

    Interventions considered

    (1) SOC plus MMF; (2) SOC plus AZA (online supplementary table S9.2.3).

    Benefits and harms

    The panel concluded that MMF or AZA decreases the occurrence of ESRD without significant adverse events, as maintenance therapy for cLN. The panel pointed that differential pharmacokinetic effects of MMF in cLN may exist, which may require dosing increase.30

    Recommendation

    The panel suggests MMF or AZA over CYC for patients with cLN who responded, partially or completely, to induction therapy (weak recommendation based on low certainty of the evidence). Cost and availability may favour AZA (table 2).

    Cardiac manifestations

    1. Which is the best treatment for adult patients with lupus-related acute pericarditis?

    Interventions considered

    (1) SOC plus colchicine; (2) SOC plus non-steroidal anti-inflammatory drugs (NSAID); (3) SOC plus belimumab; (4) low to moderate dose of GCs for 4 weeks and slow tapering (online supplementary tables S6.2.1 and S6.3.1).

    Benefits and harms

    Based on the identified evidence the panel concluded that the use of SOC combined with colchicine is associated with significant benefits (decrease in pericarditis recurrence rate) compared with SOC alone. Belimumab probably made little or no difference in pericarditis-related symptom improvement.

    Recommendation

    The panel suggests SOC plus colchicine over SOC plus NSAIDs or belimumab for patients with acute SLE-related pericarditis (weak recommendation based on low certainty of the evidence) (table 3).

    View this table:
    Table 3

    GLADEL–PANLAR recommendations for cardiac and pulmonary manifestations

    Pulmonary manifestations

    1. Which is the best treatment for lupus-related diffuse alveolar haemorrhage (DAH)?

    Interventions considered

    (1) High-dose GCs plus CYC; (2) high-dose GCs plus intravenous immunoglobulins (Ig); (3) high-dose GCs plus therapeutic plasma exchange (TPE); (4) high-dose GCs plus RTX (online supplementary tables S6.1.1 and S6.1.2).

    Benefits and harms

    In the absence of trustworthy evidence regarding the effects of the different interventions in this scenario and considering DAH’s high mortality rate, the panel decided that intense and early approach is mandatory without prioritising one intervention over another.

    Recommendation

    The panel recommends that patients with SLE-related DAH be treated with intravenous GCs plus CYC and/or intravenous Ig and/or TPE and/or RTX over GCs alone (strong recommendation based on very low certainty of the evidence, since possible benefits exist in a life-threatening situation). Cost and availability may favour GC plus CYC (table 3).

    Neuropsychiatric manifestations

    1. Which is the best treatment for adult patients with lupus-related severe, acute neuropsychiatric manifestations?

    Interventions considered

    (1) High-dose GCs; (2) high-dose GCs plus CYC; and (3) high-dose GCs plus RTX (online supplementary tables S5.1.1, S5.1.2, S5.1.3, S5.1.6, S5.2.1, S5.2.3, S5.3.3, S5.4.1, S5.4.3, S5.5.1, S5.5.2, S5.6.1).

    Benefits and harms

    The panel concluded that both options (GCs plus CYC and GCs plus RTX) were associated with large benefits and moderate harms in comparison to GCs plus placebo in patients with acute neurological manifestations. No studies comparing these two options were identified. In terms of SLE and severe neurological manifestations, clinical trials with GCs plus CYC focused on both general neurologic manifestations, and on seizures, psychosis, myelitis, peripheral neuropathy, brain stem disease and optic neuritis, specifically. No data were found regarding other neuropsychiatric manifestations. The panel significantly weighted the fact that the certainty of the evidence was better for CYC than RTX and that RTX was only evaluated in refractory patients.

    Recommendation

    The panel suggests using GCs plus CYC over GCs alone or GCs plus RTX for the treatment of severe neurologic manifestations in patients with SLE (weak recommendation based on low certainty of the evidence). Cost and availability may favour CYC (table 4).

    View this table:
    Table 4

    GLADEL–PANLAR recommendations for neuropsychiatric and haematological manifestations

    Haematological manifestations

    1. Which are the best interventions for patients with severe acute lupus-related haemolytic anaemia (haemoglobin ≤8 g/dL)?

    Interventions considered

    (1) High-dose GCs; (2) GCs plus RTX (online supplementary tables S7.1.12 and S7.1.13).

    Benefits and harms

    The panel concluded that compared with GCs as the first-line therapy, the addition of RTX provided moderate beneficial effects (reducing the risk of flare) and moderate harms (increasing the risk of infections). However, the panel significantly weighted the risks associated with RTX as well as availability and cost issues.

    Recommendation

    The panel suggests using high-dose GCs for patients with severe haemolytic anaemia (weak recommendation based on low certainty of the evidence).

    It also suggests RTX for patients with life-threatening haemolytic anaemia and/or for those in whom high-dose GC treatment fails (weak recommendation based on low certainty of the evidence). Cost and availability, however, may prompt the use of IS instead of RTX although no data support this assertion (table 4).

    ­

    1. Which are the best interventions for patients with severe lupus-related thrombocytopenia (platelet count ≤ 30 x10^9/L)?

    Interventions considered

    (1) High-dose GCs; (2) high-dose GCs plus RTX; (3) high-dose GCs plus intravenous Ig (online supplementary tables S7.1.12, S7.1.13, S7.1.15).

    Benefits and harms

    The panel concluded that compared with GCs as the first-line therapy, RTX and intravenous Ig provided moderate beneficial effects (increasing the platelet count). The harmful effects were judged as moderate for RTX (increase in infections) and small for intravenous Ig (infusion reactions).

    The panel significantly weighted the risks associated with RTX as well as availability and cost issues. In life-threatening situations, the panel significantly weighted intravenous Ig’s and RTX’s beneficial effect on platelet count.

    Recommendations

    The panel suggests using high-dose GCs in patients with lupus with severe lupus thrombocytopenia (weak recommendation based on moderate certainty of the evidence).

    It also recommends intravenous Ig with/without GCs or RTX plus GCs for patients who are refractory to high-dose GCs, those with life-threatening bleeding, those requiring urgent surgery and those with infections (strong recommendation based on moderate certainty of the evidence). Cost and availability, however, may prompt the use of IS instead of RTX although there are no data to support this assertion (table 4).

    Antiphospholipid syndrome

    1. Which is the best treatment for adult patients with SLE with antiphospholipid syndrome (APS) and venous thromboembolic disease (VTD)?

    Interventions considered

    (1) Extended anticoagulation (AC) with vitamin K antagonist (compared with not-extended AC); (2) high-intensity AC (international normalised ratio (INR) 3–4.5) compared with moderate-intensity AC (INR 2–3) (online supplementary tables S10.2.1 and S10.2.2).

    Benefits and harms

    The panel judged the effect of extended AC as a large benefit, reducing VTD with increase in bleeding risk as a moderate harm. For the comparisons of different AC intensities, the panel decided to use the evidence from observational studies because it judged that it probably better reflects reality given that the randomised controlled trials (RCT) are severely flawed (indirectness of intervention as most patients did not reach the INR >3 goal). They judged the reduction in VTD as a large benefit and the bleeding increase as a large harm. Hence, the panel considered that the balance could favour the intervention only when the risk of VTD recurrence is particularly high.

    Recommendation

    The panel recommends extended AC with vitamin K antagonist therapy for patients with APS with VTD (strong recommendation based on moderate certainty of evidence).

    The panel recommends standard (INR 2.0–3.0) over high-intensity (INR 3.0–4.0) AC for patients with APS with VTD (strong recommendation based on very low certainty of the evidence, since certainty of the effect on VTD recurrence is very low but certainty in bleeding risk is high (significant increase in major bleeding with INR 3.0–4.0)).

    ­

    1. Which is the best treatment for adult patients with SLE with APS and stroke?

    Interventions considered

    Extended antithrombotic therapy with: (1) vitamin K antagonist; (2) low-dose aspirin (LDA: 81–100 mg/day); (3) vitamin K antagonist plus LDA; (4) high-intensity AC (INR 3–4.5) (online supplementary tables S10.3.1 and S10.3.2).

    Benefits and harms

    The panel decided to use the body of evidence provided by observational studies because it probably better reflects reality as the RCTs are severely flawed (indirectness of population as most patients were inadequately diagnosed with APS). The panel judged the observed reduction in arterial thrombosis with high-intensity AC as a large benefit, and the bleeding increase as a large harm. Also, it was noted that the observed basal risk (risk with LDA) of thromboembolic recurrence in patients with APS and arterial events was particularly high, compared with the risk of recurrence in patients with VTD.

    Recommendation

    The panel suggests extended high-intensity (INR 3.0–4.0) over standard-intensity AC (INR 2.0–3.0) or LDA alone for patients with SLE with APS and stroke (weak recommendation based on very low certainty of the evidence).

    1. Which is the best treatment for pregnant SLE women with antiphospholipid antibodies and recurrent pregnancy loss?

    Interventions considered

    (1) HCQ plus LDA; (2) HCQ plus LDA plus heparin; (3) HCQ plus intravenous Ig (online supplementary tables S10.5.1, S10.5.2, S10.5.3, S10.5.4, S10.5.5, S10.5.6, S10.5.7, S10.5.8).

    Benefits and harms

    The panel judged the observed reduction in pregnancy loss with the addition of heparin to LDA as a large benefit. This intervention was not associated with significant harms. The addition of GCs or intravenous Ig to heparin plus LDA was associated with large harms (significant increase in premature delivery) without relevant benefits. Regarding heparin administration, the panel considered the reduction in pregnancy loss with low molecular weight heparin (LMWH) in comparison with unfractionated heparin (UFH) as a large benefit without significant adverse effects. No additional benefits were observed with LMWH-enoxaparin 80 mg compared with 40 mg.

    Recommendation

    The panel recommends HCQ plus LMWH plus LDA over HCQ plus LDA or adding GCs or intravenous Ig for pregnant patients with SLE with antiphospholipid antibodies and recurrent pregnancy loss (strong recommendation based on moderate certainty of the evidence (LMWH plus LDA vs other alternatives) and very low certainty of the evidence (GCs and intravenous Ig vs other alternatives), since high certainty of harms related to GCs (increased premature delivery) and intravenous Ig (costs increase, burden related to drug administration) exists).

    It also suggests LMWH at a dose of 40 mg/day over UFH or higher doses of LMWH (weak recommendation based on low certainty of the evidence) (table 5).

    View this table:
    Table 5

    GLADEL–PANLAR recommendations for adult patients with SLE with antiphospholipid antibodies or antiphospholipid syndrome

    Discussion

    Treatment of SLE in Latin America remains a challenge despite several guidelines published on the management of this disease.16–21 The distinct epidemiology, healthcare resources, socioeconomic issues and priorities were considered to develop these guidelines.

    Although these guidelines consider region limitations, the inclusion of alternative approaches for tailoring treatment did not exclude the task of providing physicians with the state-of-the-art findings in the field. This was a major advantage of the present work since highlighting these advances provides valuable basis for future requirement of government authorisation of new drugs in these countries.

    Of note, problems faced by Latin American countries are shared by several developing nations. Therefore, it is expected that these guidelines will also be very useful for them. Furthermore, due to ever increasing globalisation and the increase of migratory movements of people from countries with more susceptible SLE groups in terms of frequency and disease severity both in terms of race/ethnicity (Mestizos, Asians, Africans) and low SES to countries with better life opportunities, we consider that these guidelines may be used by physicians anywhere in the world, even in developed countries, where such individuals may migrate to and seek care for their lupus.

    We acknowledge as a limitation that certainty of the evidence was not as high as desirable for most recommendations and probably biased by few randomised clinical trials. Although regional information was published on several topics1 4 10 11 23 24 31–49 we recognise that these guidelines should be updated as research-based changes in our understanding of SLE emerge. Regardless, the publication of these guidelines must be followed by health system engagement and implementation by specialists, major steps towards improvement of lupus treatment in Latin America and low/middle-income countries.

    Acknowledgments

    The authors are deeply grateful to Miss Teresa Cattoni (Buenos Aires, Argentina), Laura Athie (Mexico City, Mexico) and Kim Schofield (Atlanta, USA), the three patients with SLE who carefully reviewed this manuscript and provided very useful comments and suggestions.

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    View Abstract

    Footnotes

    • BAP-E, EB, ERS and MHC contributed equally.

    • Handling editor Josef S Smolen

    • Contributors All authors listed in this manuscript have participated in planning, drafting, reviewing, final approval and are accountable for all aspects of the manuscript.

    • Funding PANLAR financed the development of these guidelines. PANLAR received unrestricted funds from GlaxoSmithKline (GSK) and UCB Pharma for this endeavour.

    • Disclaimer None of the entities influenced the content of the guidelines.

    • Competing interests LBF, BAPE and OAM have been speakers for GlaxoSmithKline (GSK). JCTB has received research grants from GSK. RMX, ON and JFM have received support grants for meetings from GSK. JAGP has been a lecturer for Roche. ERS has received research grants and has been a lecturer for Roche. JFM has been a clinical researcher for Anthera. MHC has received research grants from Roche and is an advisor for Eli Lilly.

    • Patient consent Not required.

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

    • Correction notice This article has been corrected since it published Online First. The author affiliations have been updated.

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