The clinical history should aim to delineate the specific subtype of AFND, which are the following:

• Classical
• Malignancy associated
• Drug-induced

History of fever, sore throat, or any other infection, significant weight loss, current or previous malignancy, or a new drug administration should be sought.

The classical clinical appearance is that of erythematous, tender, non-pruritic, papules, nodules, and plaques with predominantly head, neck, and upper trunk distribution patterns.

The plaques are often studded with multiple closely grouped translucent papules giving an illusion of vesiculation. These pseudo-vesicles and pseudo-pustules impart a mamillated appearance to the surface of the plaques and are considered one of the suggestive manifestations of AFND. Subsequent ulceration may occur, which resembles a superficial pyoderma gangrenosum that has been described in association with acute myeloid leukemia. Targetoid appearance, facial erysipelas like presentation, and giant cellulitis like appearance are the morphological variants.

Papulonodular lesions of lower limbs closely resemble erythema nodosum and can be differentiated histopathologically. Oral and genital involvements are usually uncommon. However, aphthous ulceration has been reported. Ocular involvement is relatively common in the form of episcleritis and conjunctivitis.

Systemic manifestations: The presence of fever and leukocytosis is the most common, followed by arthralgias and arthritis. Arthritis is typically asymmetric, non-erosive, and sterile.

The specific involvement of visceral organs is known as extracutaneous Sweet syndrome. This includes neutrophilic alveolitis, multifocal sterile osteomyelitis, mesangial glomerulonephritis, acute myositis, hepatitis, pancreatitis, and colitis.

CNS involvement, also known as neuro-Sweets disease, may range from aseptic meningitis to brain stem involvement and benign encephalitis.

In about 30% of cases, the skin lesions show spontaneous resolution by 3 months. However, fluctuating course with relapse and remission is more frequently observed.

Clinical variants:

• Neutrophilic dermatosis of dorsal hands- it is characterized by bluish violaceous or hemorrhagic papules, bullae, and nodules on the dorsal hands. It may be accompanied by typical lesions of Sweet syndrome over other areas of the body. This variant may have a greater association with occult or hematological malignancy. It closely mimics a bullous pyoderma gangrenosum.
• A subcutaneous Sweet syndrome-this entity presents with erythema nodosum like lesions on the shins.[1][10]

As such, there are no specific diagnostic tests for acute febrile neutrophilic dermatosis. Su and Liu proposed the diagnostic criteria for Sweet syndrome, which are as follows:

Major criteria

1. Abrupt onset of typical cutaneous lesions
2. Histopathology consistent with Sweet syndrome

Minor criteria

• Preceded by one of the associated infections or vaccinations, accompanied by one of the associated malignancies or drug exposure or pregnancy
• Fever >38 C
• Abnormal laboratory values at presentation (3 out of the 4 required) a. erythrocyte sedimentation rate (ESR)>20mm/hour, b. leukocytes>8000/mm3, c. neutrophils>70%, d. Elevated C reactive protein (CRP)
• Dramatic response to systemic corticosteroids or potassium iodide (KI)

Based on these criteria, the essential investigations include a skin biopsy, complete blood count, ESR, CRP, liver, and renal function tests. Additional tests include thyroid function tests, rheumatoid factor, and antistreptolysin-O antibody titer.

Complete lymph node examination, examination of breasts and pelvic in female and prostate, and testicles in males, sigmoidoscopy, and positron emission tomography (PET) scan comprise the workup to rule out occult malignancy.

Although elevated levels of C-ANCA have been noted, it is no longer considered of any significance.[1][11]

For mild localized disease, potent, topical or intralesional corticosteroids may be effective. However, the majority of cases warrant the use of systemic corticosteroid therapy in the dose of 0.5mg to 1mg per kg of prednisolone equivalent for 4-6 weeks.

Treatment with low dose steroids may have to be continued for a longer time to prevent exacerbations. If remission is not achieved by 3 months, a second line steroid-sparing agent must be added.

The main second-line steroid-sparing agents include dapsone (50 to 100mg/day), KI (300mg 3 times a day), and colchicine (0.5mg 3 times a day).

A baseline G6PD activity should be done in patients before starting dapsone.

Miscellaneous drugs that have been reported to be efficacious in various studies include cyclophosphamide, cyclosporine, thalidomide, clofazimine, IVIG, and TNF-alpha antagonists.[1]

Clinical: Erysipelas, cellulitis, and leprosy

Other neutrophilic dermatoses like pyoderma gangrenosum, Bechet disease, and bowel associated dermatitis arthritis syndrome (BADAS)

Cutaneous vasculitis including erythema elevatum diutinum, cutaneous polyarteritis nodosa, granuloma faciale, and cockade purpura

Reactive erythemas such as annular urticaria and erythema multiforme

Panniculitis including lupoid panniculitis and erythema nodosum

Eosinophilic cellulitis (Wells syndrome)

Granulomatous disorders such as sarcoidosis, inflammatory granuloma annulare, and palisaded neutrophilic granulomatous dermatitis.

Histopathological: Leukemia cutis, neutrophilic eccrine hidradenitis, and leukocytoclastic vasculitis[1][8][12][13]

The cutaneous lesions of acute febrile neutrophilic dermatosis or Sweet syndrome eventually show spontaneous resolution along with the associated extracutaneous manifestations. However, periodic exacerbations may occur, representing underlying paraneoplastic conditions. In a patient with a treated malignancy, recurrence of lesions of Sweet syndrome heralds a relapse. In the case of local cutaneous complications such as scarring and acquired cutis laxa, the prognosis is poor as they seldom respond to any modality.[14]

Even though lesions usually resolve with mild post-inflammatory hyperpigmentation, various localized complications such as scarring in the case of ulcerative lesions and atrophy in cases of panniculitis have been observed. Postinflammatory elastolysis presenting as acquired cutis laxa, also called Marshal syndrome, is a frequently encountered finding.[14]

In patients diagnosed with acute febrile neutrophilic dermatosis or Sweet syndrome, detailed counseling regarding the need to rule out underlying systemic diseases or malignancies should be carried out. Regular consultation with the dermatologist is recommended. In patients with treated malignancy, the reappearance of lesions should not be ignored as they can signal a relapse.[10]

Sweet syndrome is one of the great mimickers in dermatology. The key to diagnosing this syndrome is to have a high index of suspicion. Prompt referral to a dermatologist for tender erythematous papulonodular lesions with fever, which show an inadequate therapeutic response to analgesics and antibiotics, is necessary. More importantly, primary clinicians should obtain routine investigations such as a complete blood count, ESR, and CRP in suspected cases. Sweet syndrome heralds underlying infectious, immunological, or malignant disease hence, prompt diagnosis and a thorough evaluation by an interprofessional team are necessary for ruling out underlying systemic illnesses.[1][10] [Level 5]