The ASIA syndrome: basic concepts (2024)

Journal List
Mediterr J Rheumatol
v.28(2); 2017 Jun
PMC7046028

As a library, NLM provides access to scientific literature. Inclusion in an NLM database does not imply endorsem*nt of, or agreement with, the contents by NLM or the National Institutes of Health.
Learn more: PMC Disclaimer | PMC Copyright Notice

Mediterr J Rheumatol. 2017 Jun; 28(2): 64–69.

Published online 2017 Jun 27. doi:10.31138/mjr.28.2.64

PMCID: PMC7046028

PMID: 32185259

Abdulla Watad,^1,² Kassem Sharif,^1,² and Yehuda Shoenfeld²

Author information Article notes Copyright and License information PMC Disclaimer

Abstract

The autoimmune/inflammatory syndrome induced by adjuvants (ASIA), also known as Shoenfeld’s syndrome, encompasses several autoimmune conditions/phenomena that are induced following the exposure to substances with adjuvant activity. The disease spectrum is heterogeneous in respect to clinical presentation as well as severity of the clinical manifestations. Adjuvants are included in vaccination formulations for their immunogenic properties. Despite being generally well tolerated, safe and effective, some genetically predisposed individuals can develop generalized non-specific constitutional symptoms, autoantibody production, new onset, or worsening of disease presentation. In this review, we focus on the current knowledge presented in the literature on ASIA syndrome, increasing physician awareness about the basic concepts of ASIA syndrome and highlight the devastating amount of data accumulated in the last few years concerning the relationship between various adjuvants and autoimmunity.

Keywords: ASIA syndrome, autoimmune/inflammatory syndrome induced by adjuvants, adjuvants, vaccine, autoantibodies, silicone, autoimmunity

INTRODUCTION

Autoimmune/Inflammatory syndrome induced by adjuvants (ASIA) is a disease entity that was first introduced by Shoenfeld et al. in 2011.¹The authors have proposed several major and minor criteria that may aid in the diagnosis of ASIA syndrome (Table 1). It constitutes a set of closely related immune mediated diseases that share a common clinical picture as well as a history of a previous exposure to an adjuvant agent.²These common denominators were prominent in individuals who developed macrophagic myofasciitis syndrome (MMF), post vaccination phenomenon, Gulf War syndrome (GWS), and siliconosis.¹Post-vaccination phenomena and MMF are thought to mainly develop following the use of aluminum-based adjuvants.²In contrast, the incidence of GWS was contributed to squalene adjuvant exposure.⁴From a clinical standpoint, these four diseases present with classical constitutional manifestations that include myalgia, arthralgia, chronic fatigue and dry mouth as well as neurological manifestations such as cognitive disturbances, memory loss and neurologic disabilities.⁵Resembling other autoimmune disease entities, the etiopathogenesis of these conditions involves a multifactorial interplay between environmental factors and genetic predisposition as noted by the association with certain HLA haplotypes.⁶Since its emergence as a disease entity, more than 4000 documented cases of ASIA syndrome have been reported with various clinical severity and diverse history of adjuvant exposure.⁷In this review we sought to summarize the current literature on ASIA syndrome and its relation to vaccines and silicone. We aim to highlight basic concepts in order to increase physician awareness and therefore facilitate early diagnosis and prevent the exposure to adjuvants to those subjects with high risk for autoimmunity.

Table 1.

Suggested criteria for the diagnosis of ‘ASIA’

THE ROLE OF ADJUVANTS

Adjuvants are immunological molecules that function through potentiating antigen specific immune responses.⁸While adjuvants themselves do not mount an immune response, they aid in the production of a robust reaction against their inoculated antigens. Adjuvants are frequently employed in the field of medicine, more specifically in vaccination production.⁸The utilization of adjuvants contribute towards a heightened immunogenicity response resulting in a reduced frequency and amount of vaccination required to attain adequate preventive immunity.⁹Additionally, adjuvants act as a depot facilitating a prolonged antigen presence in the blood, as well as a delivering vehicle carrying inoculated antigens to lymphocyte rich areas including lymph nodes.¹⁰Both of these mechanisms strengthen the resultant immune response; a response that is not strongly provoked otherwise.¹⁰

Broadly, adjuvants influence both the adaptive and the innate arms of the immune system via various mechanisms which results in initiation as well as substantiation of immune response by the activation of pattern recognition receptors, more specifically toll like receptors (TLR), NOD-like receptors (NOR), and C-type lectin receptors.¹¹The activation of these molecules subsequently leads to a recruitment and downstream protein activation that contributes toward cytokine generation.¹¹Furthermore, adjuvants promote certain aspects of dendritic cells chemotaxis and antigen presenting cells activation which further potentiates antigen transfer to B-cell and T-cell rich environments and thus enhancing adaptive immune response to antigen.¹²

According to Edelman, adjuvants can be classified to three distinct groups; active immune stimulants that potentiate immune response to the antigen, carriers which enable T-cell help, and vehicle adjuvants which inoculate the antigens and facilitated immune response activation.¹³

Adjuvants can usually be produced from a myriad of substances including for example: oils, mineral salts, lipopolysaccharides and peptidoglycan.¹¹

In spite of its beneficial effects, the application of adjuvants in medicine was shown to induce non-specific generalized constitutional musculoskeletal symptoms.¹²Moreover, in genetically susceptible individuals, adjuvant administration can lead to overt autoimmune disease induction, as well as autoantibody production.^14,15These incidences were repeatedly reported and documented by observational studies and experimental animal studies following adjuvant administration.^16,17

POST-VACCINATION EFFECT AND ASIA

The breakthrough in vaccination development is one of the greatest public health movements in the last century. Vaccinations provide protection against the formerly known infectious diseases that in many cases led to disabling consequences as well as high morbidity and mortality rates.¹⁸Although generally well tolerated, occasionally vaccine administration led to autoimmune manifestation induction as well as autoantibody production.¹⁹Further, patients with preexisting rheumatologic diseases witnessed a worsening in their disease process subsequent to vaccinations.²⁰

The post vaccination phenomena have been postulated to be largely attributed to the immunological characteristics of adjuvants that are concurrently administered with vaccination.²⁰Adjuvant formulations have been widely studied with the intention of finding preparations with high stability, strong immunogenicity, and sufficient bioavailability while still being well tolerated.²¹Aluminum salts, mostly aluminum phosphate or hydroxide, are one of the most frequently used adjuvants which were shown to enhance antigen presentation, complement activation, innate immune system stimulation and T-helper cells (TH)1 and TH2 activation.²²Vaccines with aluminum based adjuvants where associated with post vaccination phenomena and ASIA-related symptoms.²³Animal models showed a higher seroconversion and antibody levels for systemic lupus erythematosus (SLE) following hepatitis B virus (HBV) vaccination in genetically susceptible mice.²⁴Moreover, alum-based adjuvant administration in mice led to the development of Sjögren-like disease resulting in the development of higher antibody levels, decreased saliva volume, and documented histological inflammatory acinar response.²⁵

Comparable to the results witnessed in the animal models, multiple studies have been carried with the purpose of documenting autoimmune adverse effect patterns associated with vaccination administration.^26,27These studies were based on safety surveillance data made available by database system in the United States, which is known as vaccine adverse event reporting system (VAERS). A case control study revealed that over a 6 year vaccination period with the quadrivalent HPV vaccine, a reported increased risk of arthritis, vasculitis, SLE and neurological conditions were documented as compared to the general population.²⁶These effects mostly occurred on average 1 to 7 weeks after vaccination. The quadrivalent HPV vaccine is prepared by inoculation of virus-like particles of the constituent four serotypes HPV type 6,11,16 and 18 in aluminum-based adjuvant.²⁶Numerous other associations between vaccination and autoimmune phenomenon have been documented of which include: Guillain-Barre syndrome outbreak after H1N1 vaccination and HBV vaccination, idiopathic thrombocytopenic purpura (ITP) in subsequence to Measles-mumps-rubella (MMR) and varicella zoster vaccination, arthritis following diphtheria tetanus-pertussis (DTP) and MMR vaccinations,²⁷and influenza vaccine preceding Hashimoto’s thyroiditis.²⁸Furthermore, multiple cases of giant cell arthritis (GCA) were documented in otherwise healthy individuals who received adjuvanted influenza vaccination during the previous three months.²⁹

Other than the postulated role of adjuvants in the resultant autoimmune response, other vaccine components exampled by neomycin and polymyxin have been implicated in mounting certain immunological responses, which occur as a result of influencing certain immunologic responses.³⁰

Several mechanisms have been suggested by which infections can induce autoimmune diseases. One of these mechanisms is the molecular mimicry that requires both antigen and immunologic adjuvant. This phenomenon normally induces autoimmune diseases in those with genetically predisposition for autoimmunity. The demyelinating disease induced by the HBV vaccine is a good example to illustrate and clarify these phenomena.³¹When a structural similarity exists between some viral antigen (or other component of the vaccine) and a self-antigen. This similarity may be the trigger to the autoimmune reaction. Other mechanism by which vaccines may induce autoimmunity is the increase in immune complexes which can in turn cause the vasculitis noted in several cases, or the exacerbation of existing autoimmune symptoms.¹⁷At large, the individual role of each independent complement is still to be elucidated; yet, emerging data supports the notion of the existence of autoimmune response following vaccination administration. Although most epidemiological studies do not indicate apparent vaccine safety concerns, awareness of ASIA syndrome development as well as identification of certain high-risk attributes could prevent such adverse reactions.

MACROPHAGIC MYOFASCIITIS SYNDROME (MMF) AND ADJUVANT ADMINISTRATION

Another closely related disease in the ASIA syndrome spectrum is MMF, which is noted to develop after certain vaccine administration. As suggested by the disease name, the accumulation of agglomerate forming alum nano-crystalline molecules in the macrophages between muscle fibers leads to autoimmune inflammation and induces non-specific clinical symptoms including myalgia, fatigue, and CNS involvement with reported decreased memory function, disturbed mood, and attention deficit.³²In addition to those constitutional symptoms, close to one-fifth of MMF patients developed a contemporaneous well-defined autoimmune disease, most frequently Hashimoto’s thyroiditis, dermatomyositis, myasthenia gravis, autoimmune myopathy, inclusion body myositis and multiple sclerosis-like demyelinating disease.³²Histologic findings showed a strongly periodic acid-schiff staining macrophages, a prominent CD8 positive infiltrating T cells, and positive hematoxylin staining aluminum crystals.³³In contrast, surrounding myofibers are typically left intact, unless an additional autoimmune disease process is present. In 457 studied MMF patients, Gheradi et al³documented a mean of 5.3 alum containing vaccine administration, with 85% of the studied sample reporting previous vaccination against HBV. The average latency of symptoms appeared to be around 7 months after vaccine administration. Interestingly, these patients had no previous distinctive aluminum exposure other than their exposure to adjuvant-associated alum compounds including Hepatitis A virus, HBV and tetanus toxoid vaccines.³Such findings stand in agreement with the increased vaccination against HBV during the same period as well as the use of intramuscular route of HBV vaccination, replacing the older subcutaneous route of administration.⁴

The integral role of genetic susceptibility and MMF development was supported by the relative rarity of the condition as compared to the widespread usage of aluminum hydroxide. In fact, a case control study involving 9 MMF patients and 230 controls demonstrated an increased HLA-DRB1*01 haplotype presence among patients with MMF as compared to healthy control (Odds ratio: 9.8, 95%CI:2.0–62.0, p<0.03).³⁴

GULF WAR SYNDROME (GWS) AND ASIA

The appearance of systematic constitutional symptoms including fatigue, muscle weakness and arthralgia in military veterans and civil workers during the Gulf War period led to the emergence of GWS entity. To explain this phenomenon, certain exposure to hazards were identified during this war including the exposure to pyridostigmine, radioactive munition and military vaccination protocol.³⁵Remarkably, veterans deployed to war had to be vaccinated with a six shot regimen for anthrax vaccine; a preparation that was adjuvanted with alum and squalene.¹²

Squalene, which is an oil-based adjuvant, increases antigen uptake by APC and leads to adaptive immune system activation.³⁶Although safe and well tolerated in humans, exposure to squalene have been shown to be possibly implicated with provoking chronic fatigue syndrome; a response that is postulated to be mediated by TH2-cell response.³⁶In animal models, squalene exposure in mice led to the development of immune mediated arthritis in all of the tested subjects, which was detected by the appearance of signs of synovitis including pannus formation, osteolysis and chondrolysis noted in histological examination.³⁷

The relationship between exposure to squalene and GWS development was supported by a case control study involving 144 Gulf War veterans, of which 95% of deployed GWS patients had antibodies to squalene. In the subcategory of GWS patients who received the vaccinations yet did not deploy to service, the presence of squalene antibodies was documented in 100% of these patients. On the other hand, healthy adults, or patients with other autoimmune syndromes, and vaccinated veterans without clinical signs of GWS did not form squalene antibodies.³⁸

While an exact causal relationship still requires elucidation, the evidence of an association between adjuvant administration and GWS is present, a finding that necessitates caution regarding the induced side effects after vaccination administration.

SILICONE AND ASIA SYNDROME

Silicone as an adjuvant material has been long thought to be an inert material, and therefore has been used for more than 5 decades in medical implants including heart valves, testicular prostheses, intraocular lenses and breast implants.³⁹Although considered otherwise safe, reports are emerging regarding the development of autoimmune-like phenomena in patients as well as animal models exposed to silicone.⁴⁰Silicone as an adjuvant potentiates the immune response by promoting adaptive immune cell proliferation and cytokine release that leads to T cell proliferation and polarization.⁴¹Additionally, silicone is notable for enhancing immnoreactivity by its reaction with components of the connective tissue including mucopolysaccardies and naturally occurring silicone substances.⁴²

As with previously mentioned diseases, exposure to silicone adjuvants led to immunologically-mediated immune responses that manifested as arthralgia, arthritis, malaise and pyrexia, headaches, fatigue and generalized weakness.⁴⁰

Although the constellation of these symptoms satisfied certain criteria of fibromyalgia and chronic fatigue syndrome, they lacked the presence of the prominent symptoms characterizing those diseases. Moreover, all these symptoms did not fulfill a distinctive rheumatological disease diagnostic criteria.

Several research groups set to investigate the relationship of silicone and the appearance of the autoimmune-associated clinical manifestation. Vasey et al.⁴³documented a statistically significant increase of the reported constitutional symptoms including pain and fatigue in patients with silicone implants and silicone implant ruptures. In line with this study, a large study conducted by Fryzek et al.⁴⁴showed statistically significant reports of constitutional symptoms and rheumatological symptoms in 1546 patients as compared with 2496 controls that underwent breast reduction surgeries. In another study, 69% of women had improvement of constitutional symptoms following silicone implant extraction.⁴⁵All of these findings stand in agreement of the possible relationship between silicone and the grouping of these symptoms – ASIA syndrome. Other factors have also been seen to play a role in the development of autoantibodies. In a cohort study, vitamin D levels in silicone-implanted breast patients were shown to be inversely related to antibody levels (Relative risk 3.14, 95%CI: 1.24–7.59).⁴⁶This result suggests the possible beneficial role of the immunomodulatory action of vitamin D in preventing the subsequent antibody formation in silicone-implanted patients.

CONCLUSION

ASIA syndrome, also known as Shoenfeld’s syndrome, has been frequently reported since its emergence as a disease entity. Genetic predisposition and environmental exposure to adjuvants seem to be the largest factors in disease pathogenesis. Due to the presence of reported severe ASIA cases, more efforts should be put towards clarifying and understating the governing relationship between adjuvant administration and autoimmunity. The awareness of the diseases as well as its manifestations is essential for the prevention and the treatment of cases that develop subsequent to adjuvant exposure.

CONFLICT OF INTEREST

The authors declare no conflict of interest.

REFERENCES

1. Shoenfeld Y, Agmon-Levin N.‘ASIA’ - autoimmune/inflammatory syndrome induced by adjuvants. J Autoimmun2011;36:4–8. [PubMed] [Google Scholar]

2. Watad A, Quaresma M, Brown S, Cohen Tervaert J W, Rodriguez-Pint I, Cervera R, et al.Autoimmune/inflammatory syndrome induced by adjuvants (Shoenfeld’s syndrome) - An update. Lupus2017:961203316686406. [PubMed] [Google Scholar]

3. Gherardi R K, Authier F.Macrophagic myofasciitis: characterization and pathophysiology. Lupus2012;21:184–9. [PMC free article] [PubMed] [Google Scholar]

4. Whitehouse M.Oily adjuvants and autoimmunity: now time for reconsideration?Lupus2012;21:217–22. [PubMed] [Google Scholar]

5. Cojocaru M, Chicos B.ASIA or Shoenfeld’s syndrome--an autoimmune syndrome induced by adjuvants. Rom J Intern Med2013;51:131–4. [PubMed] [Google Scholar]

6. Shoenfeld Y.Video Q&A: what is ASIA? An interview with Yehuda Shoenfeld. BMC Med2013;11:118. [PMC free article] [PubMed] [Google Scholar]

7. Jara L J, Garcia-Collinot G, Medina G, Cruz-Dominguez M D, Vera-Lastra O, Carranza-Muleiro RA, et al.Severe manifestations of autoimmune syndrome induced by adjuvants (Shoenfeld’s syndrome). Immunol Res2016:1–9. [Google Scholar]

8. Bomford R.Will adjuvants be needed for vaccines of the future?Dev Biol Stand1998;92:13–7. [PubMed] [Google Scholar]

9. McElrath M J.Selection of potent immunological adjuvants for vaccine construction. Semin Cancer Biol1995;6:375–85. [PubMed] [Google Scholar]

10. Awate S, Babiuk L A, Mutwiri G.Mechanisms of Action of Adjuvants. Front Immunol2013;4. [PMC free article] [PubMed] [Google Scholar]

11. Coffman R L, Sher A, Seder R A.Vaccine adjuvants: putting innate immunity to work. Immunity2010;33:492–503. [PMC free article] [PubMed] [Google Scholar]

12. Israeli E, Agmon-Levin N, Blank M, Shoenfeld Y.Adjuvants and autoimmunity. Lupus2009;18:1217–25. [PubMed] [Google Scholar]

13. Edelman R.Vaccine adjuvants. Rev Infect Dis1980;2:370–83. [PubMed] [Google Scholar]

14. Pellegrino P, Clementi E, Radice S.On vaccine’s adjuvants and autoimmunity: Current evidence and future perspectives. Autoimmun Rev2015;14:880–8. [PubMed] [Google Scholar]

15. Guimaraes L E, Baker B, Perricone C, Shoenfeld Y.Vaccines, adjuvants and autoimmunity. Pharmacol Res2015;100:190–209. [PMC free article] [PubMed] [Google Scholar]

16. Ruiz J T, Lujan L, Blank M, Shoenfeld Y.Adjuvants- and vaccines-induced autoimmunity: animal models. Immunol Res2017;65(1):55–65. [PubMed] [Google Scholar]

17. Shoenfeld Y, Aron-Maor A.Vaccination and autoimmunity-’vaccinosis’: a dangerous liaison?J Autoimmun2000;14:1–10. [PubMed] [Google Scholar]

18. Folb P I, Bernatowska E, Chen R, Clemens J, Dodoo A N O, Ellen-berg S S, et al.A Global Perspective on Vaccine Safety and Public Health: The Global Advisory Committee on Vaccine Safety. Am J Public Health2004;94:1926–31. [PMC free article] [PubMed] [Google Scholar]

19. Toplak N, Avčin T.Autoantibodies Induced by Vaccine. Vaccines and Autoimmunity: John Wiley & Sons, Inc; 2015;93–102. [Google Scholar]

20. Israeli E, Blank M, Shoenfeld Y.Role of Adjuvants in Infection and Autoimmunity. Vaccines and Autoimmunity: John Wiley & Sons, Inc; 2015;9–24. [Google Scholar]

21. Petrovsky N, Aguilar J C.Vaccine adjuvants: Current state and future trends. Immunol Cell Biol2004;82:488–96. [PubMed] [Google Scholar]

22. Walls R S.Eosinophil response to alum adjuvants: involvement of T cells in non-antigen-dependent mechanisms. Proc Soc Exp Biol Med (New York, NY)1977;156:431–5. [PubMed] [Google Scholar]

23. Tomljenovic L, Shaw C A.Mechanisms of aluminum adjuvant toxicity and autoimmunity in pediatric populations. Lupus2012;21:223–30. [PubMed] [Google Scholar]

24. Hanslik T, Vaillant J N, Audrain L, Jubault V, Prinseau J, Baglin A, et al.[Systemic lupus erythematosus and risk of hepatitis B vaccination: from level of evidence to prescription]. Rev Med Interne2000;21:785–90. [PubMed] [Google Scholar]

25. Bagavant H, Nandula S R, Kaplonek P, Rybakowska P D, Deshmukh U S.Alum, an aluminum-based adjuvant, induces Sjogren’s syndrome-like disorder in mice. Clin Exp Rheumatol2014;32:251–5. [PMC free article] [PubMed] [Google Scholar]

26. Geier D A, Geier M R.A case-control study of quadrivalent human papillomavirus vaccine-associated autoimmune adverse events. Clin Rheumatol2015;34:1225–31. [PMC free article] [PubMed] [Google Scholar]

27. McGarvey P B, Suzek B E, Baraniuk J N, Rao S, Conkright B, Lababidi S, et al.In silico analysis of autoimmune diseases and genetic relationships to vaccination against infectious diseases. BMC Immunol2014;15:61. [PMC free article] [PubMed] [Google Scholar]

28. Watad A, David P, Brown S, Shoenfeld Y.Autoimmune/Inflammatory Syndrome Induced by Adjuvants and Thyroid Autoimmunity. Front Endocrinol (Lausanne)2017;7:150. [PMC free article] [PubMed] [Google Scholar]

29. Soriano A, Verrecchia E, Marinaro A, Giovinale M, Fonnesu C, Landolfi R, et al.Giant cell arteritis and polymyalgia rheumatica after influenza vaccination: report of 10 cases and review of the literature. Lupus2012;21:153–7. [PubMed] [Google Scholar]

30. Cantrell H F, Lombardy E E, Duncanson F P, Katz E, Barone JS.Declining susceptibility to neomycin and polymyxin B of pathogens recovered in otitis externa clinical trials. South Med J2004;97:465–71. [PubMed] [Google Scholar]

31. Waisbren B A., SrAcquired autoimmunity after viral vaccination is caused by molecular mimicry and antigen complimentarity in the presence of an immunologic adjuvant and specific HLA patterns. Med Hypotheses2008;70:346–8. [PubMed] [Google Scholar]

32. Gherardi R K, Authier F J.Aluminum inclusion macrophagic myofasciitis: a recently identified condition. Immunol Allergy Clin North Am2003;23:699–712. [PubMed] [Google Scholar]

33. Gherardi R K, Coquet M, Cherin P, Belec L, Moretto P, Dreyfus P A, et al.Macrophagic myofasciitis lesions assess long-term persistence of vaccine-derived aluminium hydroxide in muscle. Brain2001;124:1821–31. [PubMed] [Google Scholar]

34. Guis S, Pellissier J F, Nicoli F, Reviron D, Mattei J P, Gherardi R K, et al.HLA-DRB1*01 and macrophagic myofasciitis. Arthritis Rheum2002;46:2535–7. [PubMed] [Google Scholar]

35. Gulf War illness and the health of Gulf War veterans, scientific findings and recommendations. US Department of Veterans Affairs; 2008:50. [Google Scholar]

36. Salemi S, D’ Amelio R.Could autoimmunity be induced by vaccination?Int Rev Immunol2010;29:247–69. [PubMed] [Google Scholar]

37. Holm B C, Svelander L, Bucht A, Lorentzen J C.The arthritogenic adjuvant squalene does not accumulate in joints, but gives rise to pathogenic cells in both draining and non-draining lymph nodes. Clin Exp Immunol2002;127:430–5. [PMC free article] [PubMed] [Google Scholar]

38. Asa P B, Cao Y, Garry R F.Antibodies to squalene in Gulf War syndrome. Exp Mol Pathol2000;68:55–64. [PubMed] [Google Scholar]

39. Barilaro G, Spaziani Testa C, Cacciani A, Donato G, Dimko M, Mariotti A.ASIA syndrome, calcinosis cutis and chronic kidney disease following silicone injections. A case-based review. Immunol Res2016;64:1142–9. [PubMed] [Google Scholar]

40. Baldwin C M, Jr, Kaplan E N.Silicone-induced human adjuvant disease?Ann Plast Surg1983;10:270–3. [PubMed] [Google Scholar]

41. Sun H H, Sachanandani N S, Jordan B, Myckatyn T M.Sarcoidosis of the Breasts following Silicone Implant Placement. Plast Reconstr Surg2013;131:939e–40e. [PubMed] [Google Scholar]

42. Teuber S S, Rowley M J, Yoshida S H, Ansari A A, Gershwin M E.Anti-collagen autoantibodies are found in women with silicone breast implants. J Autoimmun1993;6:367–77. [PubMed] [Google Scholar]

43. Vasey F B, Zarabadi S A, Seleznick M, Ricca L.Where there’s smoke there’s fire: the silicone breast implant controversy continues to flicker: a new disease that needs to be defined. J Rheumatol2003;30:2092–4. [PubMed] [Google Scholar]

44. Fryzek J P, Signorello L B, Hakelius L, Feltelius N, Ringberg A, Blot W J, et al.Self-reported symptoms among women after cosmetic breast implant and breast reduction surgery. Plast Reconstr Surg2001;107:206–13. [PubMed] [Google Scholar]

45. Maijers M C, de Blok C J, Niessen F B, van der Veldt A A, Ritt M J, Winters H A, et al.Women with silicone breast implants and unexplained systemic symptoms: a descriptive cohort study. Neth J Med2013;71:534–40. [PubMed] [Google Scholar]

46. Colaris M J, van der Hulst R R, Tervaert J W.Vitamin D deficiency as a risk factor for the development of autoantibodies in patients with ASIA and silicone breast implants: a cohort study and review of the literature. Clin Rheumatol2017:1–3. [PMC free article] [PubMed] [Google Scholar]

47. Young V L, Nemecek J R, Schwartz B D, Phelan D L, Schorr M W.HLA typing in women with breast implants. Plast Reconstr Surg1995;96:1497–519; discussion 520. [PubMed] [Google Scholar]

Articles from Mediterranean Journal of Rheumatology are provided here courtesy of Greek Rheumatology Society and Professional Association of Rheumatologists