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BRIEF ARTICLE 
 

Adult-Onset Still's Disease with an Atypical Cutaneous 
Manifestation 

Shae Margulies, BS1, Nicole Nagrani, MD2, Paul Rodriguez-Waitkus, MD, PhD2, Lilia Correa-
Selm, MD2 
 

1 University of Florida College of Medicine, Gainesville, FL 
2 University of South Florida Morsani College of Medicine, Department of Dermatology and Cutaneous Surgery, 
Tampa, FL 
 

 

 
 

 
 
Adult-onset Still’s disease (AOSD) is a rare 
systemic inflammatory disorder that is 
characterized by daily fevers, arthralgias, and 
rash without evidence of infection. AOSD can 
present itself in various ways, making the 
diagnosis a difficult one to make. More 
recently, there has been an increasing 
number of cases reported with atypical 
cutaneous presentations. Herein, we 
describe a case of AOSD with an atypical 

cutaneous presentation in a black female to 
add to the growing body of literature. 
 

 
 
A 37-year-old skin type Fitzpatrick VI female 
with past medical history significant for 
obesity, solitary kidney, and paranoid 
personality disorder presented to the hospital 
with complaints of subjective fevers, cough, 
and lower extremity pain following a motor 
vehicle accident which occurred 15 days prior 

ABSTRACT 

Adult-onset Still’s disease (AOSD) is a rare systemic inflammatory disorder, characterized by 
daily fevers, arthralgias, and rash without evidence of infection. Recently there has been a 
growing number of cases reported with atypical cutaneous manifestations. We present a 37-
year-old type VI Fitzpatrick skin type female who was seen in the hospital for a pruritic rash 
on her chest, back, and legs. Skin examination was significant for hyperpigmented papules 
coalescing into plaques on the chest, and hyperpigmented linear patches and excoriated 
plaques on the back and legs. Punch biopsy showed acanthosis and numerous apoptotic 
keratinocytes in the upper layers of the epidermis, which was characteristic of AOSD. As of 
recently, there is a growing body of evidence describing an atypical eruption of persistent, 
pruritic papules and plaques with typical histologic findings of AOSD. Further, these atypical 
features may be associated with more severe symptoms, higher incidence of macrophage 
activation syndrome, and possible delayed malignancy. Due to the scarcity of atypical 
cutaneous manifestations reported in the literature, these eruptions have not been included in 
the diagnostic criteria and can therefore be overlooked and misdiagnosed. Prompt 
recognition of these atypical eruptions is imperative to prevent a worsening prognosis and 
serious adverse effects. 

INTRODUCTION 

CASE PRESENTATION 



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to presentation. Within a few days of 
admission, she developed a pruritic rash that 
involved the face, chest, abdomen, legs, and 
hands. Dermatology was consulted. 
 
Skin examination was significant for 
hyperpigmented papules coalescing into 
plaques on the chest in a V-shaped 
distribution (Figure 1). On the back and legs 
there were hyperpigmented linear patches 
intermixed with linear excoriations (Figure 2). 
Additional clinical findings included cyclical 
fevers, diffuse lymphadenopathy, elevated 
ferritin, pericardial effusion and pulmonary 
infiltrates. Laboratory evaluation revealed an 
elevated ferritin of 16,580 ng/mL, an elevated 
erythrocyte sedimentation rate (ESR) of >130 
mm/h, and an elevated c-reactive protein 
(CRP) of 19.25 mg/L. All infectious etiologies 
were ruled out. A punch biopsy of the chest 
showed skin with acanthosis and numerous 
apoptotic keratinocytes predominantly 
located in the upper layers of the epidermis. 
Within the dermis, there is a superficial 
perivascular inflammatory infiltrate 
composed of lymphocytes, neutrophils and 
scattered melanophages. No interface 
changes were identified. 
 

 
Figure 1. Hyperpigmented papules coalescing 
into plaques in a V-shaped distribution 

 

 
Figure 2. Hyperpigmented linear patches and 
linear excoriations 

 
In the setting of fever, polyarthralgia, 
pericardial effusion, elevated ESR, CRP, and 
ferritin, rash, and characteristic biopsy 
findings, she was diagnosed with AOSD. She 
was treated with a prednisone taper, 
colchicine 0.6mg twice daily, as well as 
triamcinolone 0.5% twice daily as needed for 
her pruritic rash. Prednisone taper consisted 
of 50mg twice daily for 10 days, then 60mg 
daily decreased by 10mg each week until she 
reached 20mg, where it was then tapered by 
5mg weekly. She showed very mild 
improvement of the pruritus and rash in the 
hospital. On outpatient rheumatology follow 
up, she had no recurrent flares of the rash, 
and her inflammatory markers were trending 
down. At this time, her prednisone taper was 
being decreased by 5mg weekly, and during 
follow up she was taking 15mg daily with 
complete resolution of her rash. Systemic 
therapy, such as anakinra, may be needed in  



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Table 1. Yamaguchi criteria for the diagnosis of AOSD1 

Diagnosis is made with  5 criteria present,  2 being major criteria with no exclusion criteria present   

Major Criteria Fever 39 for  1 week 

 Arthralgia or arthritis  2 weeks 

 Typical nonpruritic salmon-colored rash 

 Leukocytosis  10,000/mm3 

Minor Criteria Pharyngitis 

 Lymphadenopathy 

 Hepatomegaly and/or splenomegaly 

 Liver dysfunction 

 Negative rheumatoid factor and antinuclear antibody 

Exclusion Criteria Infection, malignancy, or other rheumatic diseases 



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the future if she is unable to taper off the 
steroids. 
 

 
 
AOSD is a rare, multisystem inflammatory 
condition with an unknown etiology. Due to its 
uncommon occurrence and variable 
presentation, diagnosis of AOSD may be 
delayed. There is a broad differential 
diagnosis for patients with overlapping 
features of AOSD, including infection, 
autoimmune disease, autoinflammatory 
disease, and malignancy. The proposed 
Yamaguchi major criteria for AOSD, 
summarized in Table 1, consists of fever, 
arthralgias, typical rash, and leukocytosis, 
while the minor criteria include pharyngitis, 
lymphadenopathy and/or splenomegaly, liver 
dysfunction, and the absence of rheumatoid 
factor and antinuclear antibody.1 The typical 
rash of AOSD is characterized by nonpruritic, 
salmon-pink macules, papules, and plaques 
that coincide with fever spikes.  
 
As of recently, more cases of AOSD have 
been reported in the literature with atypical 
cutaneous presentations. There is a growing 
body of evidence describing the atypical 
eruption of persistent, pruritic papules and 
plaques in patients with AOSD.2-8 These 
persistent lesions have characteristic findings 
on histology, including dyskeratotic cells in 
the upper epidermis and a lymphocytic 
infiltrate in the papillary dermis.2 In patients 
who develop linear lesions with the 
appearance of excoriations, as seen in our 
patient, histology remains consistent, and 
this therefore represents Koebner’s 
phenomenon.9 Skin findings differ from the 
typical rash in both morphology and time 
course, leading to further difficulty making the 
diagnosis of AOSD.  
 

Moreover, these atypical features may be 
associated with more severe symptoms and 
are theorized to be a negative prognostic 
factor for disease.10-12 A cohort study 
including 150 patients with AOSD found that 
those with atypical persistent pruritic 
eruptions had higher levels of lactate 
dehydrogenase and ferritin and a higher rate 
of macrophage activation syndrome than 
patients with the typical evanescent rash.10 

Dyskeratotic cells on histology in persistent 
pruritic eruptions have been linked to an 
increase in IL-18 and subsequently a worse 
prognosis.11 Further, AOSD has been 
increasingly associated with delayed 
malignancies, commonly breast cancer and 
lymphoma.13 In a review of 19 patients with 
atypical presentations of AOSD, diagnostic 
workup for malignancy showed 
hepatosplenomegaly in 26%, 
lymphadenopathy in 11%, and pleural and 
pericardial effusion in 5%.13 
 

 
 
Early recognition of AOSD is important as to 
not delay treatment in patients with diffuse 
systemic disease. Due to the scarcity of 
atypical cutaneous manifestations reported in 
the literature, these eruptions have not been 
included in the diagnostic criteria and can 
therefore be overlooked and misdiagnosed. 
Prompt recognition of these atypical 
eruptions is imperative to prevent a 
worsening prognosis and serious adverse 
effects such as macrophage activation 
syndrome or delayed recognition of 
malignancy. 
 
Conflict of Interest Disclosures: Dr. Correa is a 
consultant for Accutec Blades and a consultant and a 
researcher for Novartis Pharmaceutical. 
 
Funding: None 
 
Corresponding Author: 
Lilia Correa-Selm, MD  

DISCUSSION 

CONCLUSION 



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Department of Dermatology and Cutaneous Surgery  
University of South Florida College of Medicine  
13220 USF Laurel Drive, 5th floor 
Tampa, FL 33612 
Phone: (813) 974-4270 
Email: Lcorrea1@usf.edu 

 
 
References: 
1. Yamaguchi, M., Ohta, A., Tsunematsu, T., et al. 

(1992). Preliminary criteria for classification of 
adult Still’s disease. The Journal of 
Rheumatology, 19(3), 424–430. 

2. Fernández Camporro, Á., Rodríguez Diaz, E., 
BetetaGorriti, V., Gonzalvo Rodríguez, P., & 
Álvarez Cuesta, C. (n.d.). Still’s disease with 
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activation syndrome. Clinical and Experimental 
Dermatology, n/a(n/a). 
https://doi.org/10.1111/ced.15294 

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(2022). Fever and flagellate dermatosis in an 
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1509. https://doi.org/10.1016/j.jaad.2021.02.005  

11. Maeda-Aoyama, N., Hamada-Ode, K., Taniguchi, 
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https://doi.org/10.1097/MD.0000000000019051 

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https://doi.org/10.1097/MD.0000000000019051
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