key: cord-0707749-h87bv6gd authors: Padiyar, Shivraj; Kamath, Navaneeth; Mathew, John; Chandu, A. S.; Deodhar, Divya; Shastry, B. A.; Shashikala, T.; Ganapati, Arvind title: New-onset Adult-onset Still’s disease-like syndrome after ChAdOx1 nCoV-19 vaccination—a case series with review of literature date: 2022-01-18 journal: Clin Rheumatol DOI: 10.1007/s10067-022-06065-7 sha: 9e223c806689131b25633400a2ef016a1223a116 doc_id: 707749 cord_uid: h87bv6gd We report a series of 3 Adult-onset Still’s disease (AOSD)-like presentations in previously healthy females following vaccination with the ChAdOx1 nCoV-19 vaccine, and also compare them with similar cases reported in literature through a PubMed database search. Our first patient had a high spiking bi-quotidian type of fever with myalgia, sore throat, and arthritis with onset 10-day post-vaccination, with laboratory features of hyper inflammation responding to only naproxen. She was off treatment after 2 months. The second patient, with onset 3-week post-vaccination, had a more severe illness, requiring high dose immunosuppression. In our third case, the onset of illness was slightly delayed i.e., 3-month post-vaccination, but she had the most severe disease with macrophage activation syndrome at presentation requiring immunosuppression and biologicals. The underlying mechanism may be linked to the activation of Toll-like receptors (TLR)—TLR-7 and TLR-9—leading to a robust immune response. These 3 cases highlight the immunogenicity of COVID-19 vaccines, with the possibility of occurrence of new-onset systemic hyper-inflammation illness which can happen a few days following the vaccination, sometimes even delayed to months, and can range in severity from mild to even life-threatening. More cases need to be studied to understand the profile and prognosis of these syndromes in the long run. The spread of COVID-19 infection has led to unprecedented rapid growth in vaccine development with a subsequent increase in the vaccination against COVID 19, with many countries having vaccinated more than 50 percent of their population [1] . India also has completed 1000 million vaccinations since the inception of the vaccination program in Feb 2021 [2] . Fever, chills, myalgia fatigue, and arthralgia can occur following COVID-19 vaccination; however, most of these symptoms are mild to moderate in severity, occurring within the first 3 days of vaccination and resolve within 1 or 2 days [3] . Although deemed safe in the general population, systemic rheumatic diseases have been shown to have flare-ups after vaccination [4] . In addition to this, there are reports of new-onset systemic rheumatological diseases [5, 6] . The adjuvanticity of the available SARS-CoV-2 vaccines is based on either TLR-7/8 or TLR-9 agonism, which is a distinct mechanism from previous vaccines [7] . ChAdOx1 nCoV-19 (Covishield) vaccine, one of the many vaccines available in our country, consists of simian adenovirus vector ChAdOx1, with fulllength spike protein of SARS-CoV-2 [8] Here we report a series of 3 cases of new-onset Adult-onset Still's disease (AOSD)-like syndrome following vaccination with ChAdOx1 nCoV-19 vaccine. A 20-year-old previously healthy female, asymptomatic 4 weeks before admission, presented with high-grade fever (102 degrees Fahrenheit), without chills. The fever was bi-quotidian in nature, with asymptomatic phases in between the fever spikes. This was also associated with throat pain, generalized myalgia, and ankle arthralgia. In a week, she also developed an evanescent maculopapular rash over the neck, abdomen, and thigh during the height of the fever. She had received her first dose of ChAdOx1 nCoV-19 vaccine 10 days before the onset of symptoms. Her clinical examination at the time of admission was unremarkable. On evaluation in an outside hospital, she was found to have neutrophilic leukocytosis (Total WBC count 15,600, N-72%) with elevated C-reactive peptides (71 mg/L) and elevated ferritin levels (3500 ng/ml). The investigations at presentation to us have been summarized in Table 1 . Infectious disease (including polymerase chain reaction for SARS-CoV2 and blood culture) and malignancy workup with Positron Emission Tomography-Computerized Tomography (PET-CT)/bone marrow examination were normal. Serological workup for other autoimmune diseases was negative. She was diagnosed with AOSD based on the Fautrel's criteria [9] . She was initiated on Tab. Naproxen 250 mg twice daily which she had immediate resolution of symptoms of fever and myalgia. She remained afebrile during the remaining stay in the hospital. She had improvement in her inflammatory parameters at discharge (Table 1) . She was continued on anti-inflammatory agents for 4 weeks. She was reviewed telephonically 2 months later and reported to be asymptomatic and has remained off medications since. The course of the patient's clinical presentation and management has been summarized in Fig. 1 . A 47-year-old, previously healthy woman presented with high-grade fever (101 degrees F), quotidian in nature for the last 2 months. This was associated with small and large joint inflammatory arthritis, without any rash. She also had a history of associated significant weight loss and loss of appetite of the same duration. She had a history of ChAdOx1 nCoV-19 vaccine 3 weeks before the onset of symptoms. She had a partial response to oral methylprednisolone therapy 16 mg/day prescribed by a general practitioner. She also gives a positive history of rheumatoid arthritis (RA) in her elder sister. Clinical examination revealed pyrexia with tachycardia (Pulse rate -104 beats per minute) and swollen and painful knee and wrist joints. On evaluation, she was found to have a hemoglobin of 8.1 g/dL, platelet count of 5.54 lakh/mm 3 , and a white blood cell count of 12,100 cells/mm 3 with a neutrophil predominance. She was also found to have elevated liver enzymes and elevated inflammatory markers (Table 1) . Her nasopharyngeal swab for SARS COV 2 by RT-PCR was negative. Cross-sectional imaging of the thorax and abdomen did not show hepatosplenomegaly and bone marrow examination ruled out the possibility of infection or malignancy. An echocardiogram showed mild pericardial effusion. Serology for autoimmune diseases was negative. After excluding infectious, malignant, and autoimmune etiologies, a possibility of AOSD was considered based on Fautrel's criteria [9] . Her fever resolved following 20 mg/kg naproxen; however, arthritis needed 0.5 mg/kg oral prednisolone. Since the patient refused consent for higher doses of steroids, she was started on Inj Tocilizumab 162 mg subcutaneously every 2 weeks with low dose methotrexate. She was reviewed after 1 month telephonically at which point, she had remarkable improvement in her symptoms. A decision regarding further tocilizumab will be done at 3 months review. The course of the patient's clinical presentation and management has been summarized in Fig. 2 . A 35-year-old lady with no previous co-morbidities presented to us with high-grade fever, sore throat, evanescent skin rash on the trunk/extremities, and arthralgias for 2 weeks. There was a history of associated weight loss [10] . She had multi-organ dysfunction in the form of acute respiratory distress syndrome (ARDS) due to diffuse alveolar hemorrhage (DAH) requiring non-invasive ventilation and hepatic failure (AST 515 IU/L, ALT 1294 IU/L, ALP 308 IU/L). She was immediately started on intravenous (IV) pulse methylprednisolone (MP) of 1 g for 3 days with intravenous immunoglobulin (IVIg) 2 g/ kg over the next 5 days. We followed up this therapy with oral dexamethasone of 10 mg/m 2 as per the HLH-2004 protocol [11] . She improved 5 days following this management with rapid clearance of her DAH accompanied by a rise in hemoglobin and blood counts; however, there was no improvement in liver function tests. She further received 480 mg (8 mg/kg) of IV tocilizumab, following which there was a significant improvement in liver function tests. She was discharged on oral prednisolone 1 mg/kg and planned for tocilizumab therapy for the next 3 months. The course of patient management has been summarized in Fig. 3 . AOSD is a multisystem inflammatory disorder of unknown etiology commonly affecting young adults. This is mainly a diagnosis of exclusion, done by a constellation of clinical and laboratory criteria. The cardinal symptoms consist of fever, arthritis, evanescent rash, sore throat, hepatosplenomegaly, and even life-threatening complications, including fulminant hepatitis and macrophage activation syndrome (MAS) [12] . The predominant laboratory abnormalities include anemia, thrombocytosis, neutrophilic leukocytosis, transaminitis, and hyperferritinemia. Abnormal activation of the innate and adaptive immune system leading to uncontrolled production of cytokines, including IL-1β, IL-6, IL-18, and TNF-α, has been recognized as a cornerstone in AOSD pathogenesis [13] . SARS-CoV-2 infection similarly provokes a hyperinflammatory state driven by IL-6, IL-1α, IL-1β, and TNF-α [14] . There have been studies comparing the similarity and differences among AOSD and cytokine storm of COVID-19 [15] . Severe COVID-19 associated cytokine storm is also a hyperferritinemia state which further enhances pro-inflammatory cytokine release [16, 17] . Various autoimmune and rheumatological disorders have been reported among the COVID-19 affected patients and also flare-up of certain underlying rheumatological conditions [6] . Conversely, AOSD is a multisystem auto-inflammatory disorder that can be triggered by viral infections, bacterial infections, or rarely even vaccines in a genetically susceptible individual. Wan-Hee-Yo in his cover letter to the editor also reports a case of AOSD following influenza vaccination [18] . A few differences however do exist between the two disease states. AOSD has a higher female preponderance which is consistent in our case series. All the 3 cases reported by the authors are female patients [19, 20] . One of the oddities was normal platelet counts in cases 1 and 3. Although thrombocytosis is common in AOSD, it is not a must for diagnosis. There have been many cases reported in the literature where platelet counts are normal [29] . The proportion of elevated liver enzymes and elevated C-reactive peptides was higher in AOSD patients compared to COVID-19 cytokine storm patients. AOSD is characterized by much more elevated ferritin levels compared to the COVID-19 cytokine storm [15] . The cytokines like IL-1, IL-6, and IL-10 were higher in severe COVID-19 compared to AOSD. The common role of IL-1 and IL-6 in the pathogenesis of AOSD and COVID-19 could explain the close similarities between both diseases. cases reported in the literature on the development of AOSD after COVID-19 infection [21, 22] . Apart from the COVID infection, vaccination per se can also cause a new onset AOSD-like syndrome. A PubMed database search done on 2/1/2022 using key words "Still's disease and COVID vaccination" yielded 3 case reports that have been published in literature [23] [24] [25] (Table 2) . Two main mechanisms have been postulated in the development of autoimmunity to vaccines: one is molecular mimicry and the other is nonspecifically known as "bystander activation" [26] . Studies have shown that the SARS-CoV-2 spike protein can act as a pathogen-associate molecular pattern (PAMP), thereby causing an overproduction of cytokines via the TLR-mediated pathways and also the inflammasome pathway [27, 28] . Activation of TLR-7 and 9 can lead to upregulation of Interferon stimulated Genes (ISG) leading to robust innate immune responses. The symptom onset in all 3 of our cases being later than 1 week following vaccination and symptom constellation lasting > 3 weeks emphasizes the point of these presentations being likely due to a distinct immunological hyperactivation entity, unlike the immediate post-vaccination immunological phenomena. Our first patient had a less severe disease that responded to only naproxen; however, the second patient had a more severe disease. The third patient had a life-threatening presentation requiring intravenous immunoglobulin, pulse steroids, and anti-cytokine therapy to control the disease activity. The time difference between the COVID vaccination and AOSD-like presentation was relatively short (days to weeks) in the first two cases; however, it was slightly delayed (3 months) in Case 3. The delayed onset as in Case 3 is also in contrast to the recently reported cases of AOSD-like state following COVID vaccination, which had onset ranging from 5-to 13-day post-vaccination [22] [23] [24] . Such observations highlight the point that hyperinflammatory state following COVID19 vaccination can be variable in severity from mild to life-threatening disease and can present early (in days/few weeks) or occur as a delayed presentation (up to 3 months). At this point, the nomenclature of the abovementioned presentations seems difficult and could be debatable. Such presentations could turn out to be a monophasic illness in contrast to the variable course of AOSD. However, similar cases from across the globe need to be reported and longterm follow-up of our patients is imperative to conclude on this aspect. With this case series, we can only postulate the COVID vaccination to be the most probable inciting trigger for an AOSD like presentation; however, a definite causal relationship can only be established with the help of epidemiological studies from countries with good data-keeping and surveillance for vaccine-induced immunological adverse events and population data of annual incidence of AOSD. Clinicians must be alert to the possible occurrence of new-onset early or delayed presentation of an AOSD-like syndrome following ChAdOx1 nCoV-19 vaccination. The presentation can range from being mild to extremely lifethreatening. 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