Dermatology: Practical and Conceptual


Observation  |  Dermatol Pract Concept 2016;6(3):11 55

DERMATOLOGY PRACTICAL & CONCEPTUAL
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Case presentation

A 72-year-old male with a recent diagnosis of acute myeloid 

leukemia (AML) had been commenced on chemotherapy—

daunorubicin and cytarabine. He was also on ciprofloxacin, 

posaconazole and acyclovir for antimicrobial prophylaxis.

Within forty-eight hours of starting chemotherapy, he 

developed fever of 40oC and was commenced on pipera-

cillin-tazobactam. On day 4 of chemotherapy a rash was 

noted. He was pancytopenic with an absolute neutrophil 

count of 0.34x109/L and a platelet count of 20x109/L. C-re-

active protein was raised at 322mg/L and a septic screen 

Two neutrophilic dermatoses captured 
simultaneously on histology
Christina Wlodek1, Nidhi Bhatt2, Cameron Kennedy1

1 Department of Dermatology, Bristol Royal Infirmary, Bristol, UK

2 Department of Pathology, Bristol Royal Infirmary, Bristol, UK

Key words: neuturopilic dermatosis, neutrophilic eccrine hidradenitis, Sweet’s syndrome

Citation: Wlodek C, Bhatt N, Kennedy C. Two neutrophilic dermatoses captured simultaneously on histology. Dermatol Pract Concept 
2016;6(3):11. doi: 10.5826/dpc.0603a11

Received: December 14, 2015; Accepted: May 27, 2016; Published: July 31, 2016

Copyright: ©2016 Wlodek et al. This is an open-access article distributed under the terms of the Creative Commons Attribution License, 
which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.

Funding: None.

Competing interests: The authors have no conflicts of interest to disclose.

All authors have contributed significantly to this publication.

Corresponding author: Christina Wlodek, BSc, MBBS, Bristol Royal Infirmary, Department of Dermatology, Upper Maudlin Street, Bristol 
BS2 8HW, United Kingdom. Tel. 0117 923 000; Fax. 0117 342 2845. Email: christina.wlodek@gmail.com

A number of neutrophilic dermatoses are associated with malignancies and their treatment. These 
rarely occur together in the same patient. 

A Caucasian 72-year-old male was treated for acute myeloid leukemia (AML) with chemotherapy 
including daunorubicin and cytarabine. Within 48 hours of commencing treatment, he developed 
pyrexia and, two days later, disseminated non-tender pink plaques on the limbs and trunk. A skin 
biopsy showed a dermal interstitial infiltrate of lymphocytes, histiocytoid cells and predominantly 
neutrophils. This extended into the subcutis, where a neutrophilic lobular panniculitis was seen. These 
findings are consistent with Sweet’s syndrome. In addition, a neutrophilic and lymphocytic infiltrate 
was also present around eccrine coils and lower ducts. The eccrine epithelium showed squamous 
metaplasia with dyskeratosis and sloughing into the lumen. These latter findings are consistent with 
neutrophilic eccrine hidradenitis (NEH).

These two histologically distinct entities form part of the neutrophilic dermatoses that have been 
described in oncology patients with reports of concurrent or sequential occurrence of various neutro-
philic dermatoses in the same patient. Ours, however, is only the second reported case of simultane-
ously captured Sweet’s and NEH in the setting of AML. The most likely explanation is that of an 
epiphenomenon, whereby the neutrophilic infiltrate extended around the sweat glands in the context 
of the neutrophilic dermatosis.

ABSTRACT



56 Observation  |  Dermatol Pract Concept 2016;6(3):11

(Figure 2b) with dyskeratosis and sloughing into the lumen. 

Surrounding these changes there was a neutrophilic and 

lymphocytic infiltrate. Fungal, bacterial and mycobacterial 

cultures were negative.

To our knowledge this is only the second reported case 

of concomitant Sweet-like neutrophilic dermatosis and neu-

trophilic eccrine hidradenitis (NEH) in the setting of AML.

Since the original description by R. D. Sweet in 1964, acute 

febrile neutrophilic dermatosis (Sweet’s syndrome) is known 

to be associated with leukemia and in particular the acute 

myelomonocytic type [1]. Histology typically demonstrates a 

dense infiltrate of mature neutrophils in the upper half of the 

dermis but the location of the infiltrate can vary. Less com-

monly the neutrophils are perivascular. Neutrophils can also 

migrate into the epidermis or underlying adipose tissue [2]. To 

the best of our knowledge there are no literature reports of the 

neutrophilic infiltrate involving the eccrine glands.

was negative. Granulocyte-colony stimulating factor was 

not administered.

At the time of dermatology review, the patient had been 

pyrexial for four days. He had disseminated non-tender pink 

plaques on the limbs and trunk. Some lesions were immi-

nently vesicular while others hemorrhagic. Since the rash was 

asymptomatic no treatment was felt necessary. An incisional 

biopsy was performed. Within 7 days the eruption resolved.

The skin biopsy showed subepidermal edema (Figure 

1a), with no interface damage. There was extensive red cell 

extravasation in the dermis and an interstitial infiltrate of 

lymphocytes, histiocytoid cells and predominantly neutro-

phils. This extended into the subcutis, where a neutrophilic 

lobular panniculitis was seen. There was no evidence of 

vasculitis (Figure 1b). A second striking abnormality was 

centered around the eccrine coils and lower ducts (Figure 

2a). The eccrine epithelium showed squamous metaplasia 

Figure 1. (a) A scanning power view showing subepidermal edema and a diffuse infiltrate throughout the dermis and subcutis. (b) High 

power view of neutrophils within the dermis. Note the absence of vasculitis. Hematoxylin and eosin, original magnification (a) x40 (b) x100. 

[Copyright: ©2016 Wlodek et al.]

Figure 2. (a) High power view of neutrophilic infiltration of eccrine sweat glands (arrows) and epithelial necrosis (circled) together with 

intraluminal necrotic eosinophilic debris (*). (b) Upper part of eccrine duct showing squamous metaplasia (circled). Hematoxylin and eosin, 

original magnification (a) x200 (b) x300. [Copyright: ©2016 Wlodek et al.]



Observation  |  Dermatol Pract Concept 2016;6(3):11 57

of pathological changes described has expanded. There can 

be variability in the composition of the infiltrate as well as 

its depth. We could hypothesize that this case describes yet a 

further expansion of the pathological description. However, 

the occurrence of these two entities concurrently, in this 

same patient, is not entirely unexpected. The patient had 

a hematological malignancy well known to be associated 

with Sweet’s syndrome and at the same time was receiving 

an agent, cytarabine, that has a well-established association 

with NEH. Thus we feel the most likely explanation is that 

of an epiphenomenon, where by the neutrophilic infiltrate 

has extended around the sweat glands in the context of the 

neutrophilic dermatosis.

References

1. Cohen PR. Sweet’s syndrome—a comprehensive review of an acute 

febrile neutrophilic dermatosis. Orphanet J Rare Dis 2007;2(1):34. 

PMID: 17655751. DOI: 10.1186/1750-1172-2-34.

2. Cohen PR, Kurzrock R. Sweet’s syndrome revisited: a review of 

disease concepts. Int J Dermatol 2003;42(10):761-78. PMID: 

14521689. DOI: 10.1046/j.1365-4362.2003.01891.x.

3. Greer KE, Cooper PH. Sweet’s syndrome (acute febrile neutrophilic 

dermatosis). Clin Rheum Dis 1982;8(2):427-41. PMID: 6754235.

4. Harrist TJ, Fine JD, Berman RS, Murphy GF, Mihm MC, Jr. Neu-

trophilic eccrine hidradenitis. A distinctive type of neutrophilic 

dermatosis associated with myelogenous leukemia and chemo-

therapy. Arch Dermatol 1982;118(4):263-6. PMID: 6950689. DOI: 

10.1001/archderm.1982.01650160053024.

5. Allegue F, Soria C, Rocamora A, Munoz E, et al. Neutrophilic ec-

crine hidradenitis in two neutropenic patients. J Am Acad Dermatol 

1990;23(6 Pt 1):1110-3. PMID: 2273110.

6. Kuttner BJ, Kurban RS. Neutrophilic eccrine hidradenitis in the 

absence of an underlying malignancy. Cutis 1988;41(6):403-5. 

PMID: 3391045.

7. Cohen PR. Neutrophilic dermatoses occurring in oncology pa-

tients. Int J Dermatol 2007;46(1):106-11. PMID: 17214733. DOI: 

10.1111/j.1365-4632.2006.02605.x.

8. Gross PR, Margolis D. Neutrophilic dermatosis versus neutrophilic 

eccrine hidradenitis. N Engl J Med 1999;340(17):1371. PMID: 

10223880. DOI: 10.1056/NEJM199904293401718.

9. Zehani A, Chelly I, Abdelmalek R, et al. [Adult idiopathic neu-

trophilic eccrine hidradenitis mimicking Sweet’s syndrome]. Tunis 

Med 2013;91(5):366-7 PMID: 23716340.

A few lymphocytes are typically present in older lesions, 

in a perivascular pattern. Vasculitis is usually absent [3], 

although a secondary leukocytoclastic vasculitis has been 

described in several cases [2].

NEH is a more recently characterized entity—first 

reported in a patient treated with cytarabine for AML [4]. 

Since then, other malignancies and chemotherapeutic agents 

have been implicated. The histological hallmark is a neu-

trophilic infiltrate around and within eccrine secretory coils 

often associated with vacuolar degeneration and even necro-

sis of the secretory epithelium. The NEH literature does not 

report any neutrophilic infiltrates away from the eccrine 

sweat glands. In the setting of neutropenia the infiltrate may 

be sparse [5]. Squamous metaplasia is occasionally seen.

The pathologic mechanism of NEH remains unclear. It 

was postulated to be linked to the high concentrations of 

chemotherapy drugs secreted into eccrine glands, however 

cases of NEH have been seen in the absence of chemotherapy 

and AML [6].

These two histologically distinct entities form part of the 

neutrophilic dermatoses that have been described in oncol-

ogy patients. There are reports of concurrent or sequential 

occurrence of various neutrophilic dermatoses in the same 

patient [7]. However, ours is the second reported case of 

simultaneous Sweet-like neutrophilic dermatosis and NEH. 

There is a case similar to ours where there was a background 

of AML treated with chemotherapy, including cytarabine, in 

a patient with both Sweet’s and NEH. The patient suffered 

a recurrence of the eruption when a relapse of the AML was 

treated with chemotherapy, but did not have a recurrence 

when consolidation chemotherapy was given during remis-

sion [8]. Our patient did have a recurrence of AML 8 weeks 

after completing his second cycle of chemotherapy. Since 

then he has been on azacitidine (an antimetabolite) to control 

disease progression. To date he has not experienced a recur-

rence of the cutaneous eruption. Another case of concomitant 

Sweet’s plus NEH reported in the Tunisian literature appeared 

to be idiopathic [9].

Conclusion
Since Sweet’s syndrome was initially recognized, the spectrum