Dermatology: Practical and Conceptual


DERMATOLOGY PRACTICAL & CONCEPTUAL
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Observation  |  Dermatol Pract Concept 2014;4(1):6 47

Introduction

Kikuchi-Fujimoto disease (KFD) or histiocytic necrotizing 

lymphadenitis is a rare, benign, and self-limited disorder 

characterized by regional cervical lymphadenopathy, mild 

fever, and night sweats. It has a worldwide distribution, with 

higher prevalence among young Asian females [1]. Recogni-

tion of KFD is crucial especially because it can be mistaken 

for lymphoma, tuberculosis or even, for carcinoma. Prognosis 

is favorable with spontaneous recovery occurring in 1 to 4 

months. Treatment is symptomatic and includes analgesics-

antipyretics, non-steroidal anti-inflammatory drugs and, 

rarely, corticosteroids.

KFD can occur isolated, or associated with severe and 

autoimmune diseases including mixed connective tissue dis-

eases and systemic lupus erythematosus (SLE). In particular 

KFD can precede, postdate or coincide with the diagnosis of 

SLE [2]. Here we report a case of necrotizing lymphadenitis 

preceding the occurrence of subacute cutaneous erythemato-

sus lupus (SCLE) in a 42-year-old woman.

Subacute cutaneous lupus erythematosus onset 
preceded by Kikuchi-Fujimoto disease

Vito Di Lernia1, Gianluigi Bajocchi2, Simonetta Piana3

1 Dermatology Unit, Arcispedale Santa Maria Nuova-IRCCS, Reggio Emilia, Italy

2 Rheumatology Unit, Arcispedale Santa Maria Nuova-IRCCS, Reggio Emilia, Italy

3 Pathology Unit, Arcispedale Santa Maria Nuova-IRCCS, Reggio Emilia, Italy

Keywords: Kikuchi-Fujimoto disease, skin, lymphadenitis

Citation: Di Lernia V, Bajocchi G, Piana S. Subacute cutaneous lupus erythematosus onset preceded by Kikuchi-Fujimoto disease. Dermatol 
Pract Concept. 2014;4(1):6. http://dx.doi.org/10.5826/dpc.0401a06

Received: June 27, 2013; Accepted: September 16, 2013; Published: January 31, 2014

Copyright: ©2014 Di Lernia 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: Dr. Vito Di Lernia, Unit of Dermatology, Arcispedale S. Maria Nuova-IRCCS, viale Risorgimento 80, 42100 Reggio 
Emilia, Italy. Email: vito.dilernia@asmn.re.it

Kikuchi-Fujimoto disease (KFD) is an uncommon clinicopathological entity characterized by fever and 
lymphadenopathy, predominantly involving cervical lymph nodes, accompanied by chills and leuko-
penia. The diagnosis relies primarily on the presence of typical morphological features in the swelling 
lymph nodes. KFD can occur as a benign and self-limiting lymphadenopathy, but it can sporadically 
precede, postdate or coincide with the diagnosis of systemic lupus erythematosus (SLE). The authors 
report a case of subacute cutaneous lupus erythematosus (SCLE) in a 42-year-old female preceded by 
prolonged fever, anemia, leukopenia, and cervical necrotizing lymphadenopathy. About two months 
later, the patient developed facial and scalp plaques suggestive of lupus skin disease. Histologic and 
immunologic investigations lead to the diagnosis of SCLE. It is not clear whether KFD associated with 
lupus skin disease are true KFD or a histopathologic feature of SLE.

ABSTRACT



48 Observation  |  Dermatol Pract Concept 2014;4(1):6

papulo-squamous lesions on her scalp, ears, face, and trunk, 

she was referred to the dermatology department.

Skin examination showed papular and scaly plaques on 

the face, the scalp, the V-area of the neck, upper chest, back 

and shoulder in a photodistributed pattern. No malar rash 

was noted. Skin lesions were biopsied with a presumptive 

diagnosis of lupus.

At histology, the epidermis was thinned and displayed 

focal parakeratosis and vacuolar degeneration of basal kera-

tinocytes, with occasional cytoid bodies. The dermis showed 

conspicuous interstitial mucin deposits, dense perivascular 

and perifollicular lymphocytic infiltrates with interface der-

matitis (Figure 2) and superficial nuclear debris with kary-

orrhexis. Direct immunofluorescence failed to demonstrate 

immunoglobulin or complement deposits along the dermo-

epidermal junction or around the vessels. Immunologic serum 

investigations showed absence of antinuclear antibodies, 

antibodies (anti)-LA/SS-B, anti-ds DNA, anti-phospholipids, 

anti-pANCA, anti-Jo1, anti-Scl-70, anti-RNP. Antibodies 

anti-Ro/SS-A (E.I.A) were 59 (normal value: 0-10), ENA 

(E.I.A) 18.7 (normal value: 0-3). The patient’s complement 

levels were low with C3 71 mg/dL (normal values: 88–201 

mg/dL), C4 5 mg/dL (normal values: 16–47 mg/dL). On the 

basis of clinical, laboratory and histology findings, a diagno-

sis of SCLE was made.

The patient was given prednisone 25 mg per day and 

hydroxychloroquine. Skin lesions improved rapidly and 

healed without scarring. The dosage of corticosteroids was 

gradually tapered without relapse of skin lesions. After 

Case report

A 42-year-old Moroccan female was admitted to the hospital 

with fever lasting one month, night sweats and left cervical 

lymphadenopathy. Laboratory exams showed leukocytes 

3300/mm3, erythrocytes 4.370.000/mm3, hemoglobin 12.7 g/

dl, thrombocytes 156.000/mm3, LDH 843U/l (normal values: 

230-460). Other laboratory findings were all within normal 

ranges. Serologic investigations excluded viral, bacterial and 

parasitic infections, including syphilis and cytomegalovirus, 

Epstein-Barr virus, HIV, Rickettsia coronii, Brucella spp, 

Salmonella typhi, Salmonella paratyphi, toxoplasma, Leish-

mania donovani infections. Blood and throat cultures were 

negative. QuantiFERON TB Gold (ESAT-6, CFP-10, TB7.7 

antigens) was negative. Chest X-ray was normal. Chest com-

puted tomography (CT) showed multiple, small-sized bilat-

eral hilar and mediastinal lymphadenopathies. Abdominal CT 

revealed additional small interaortocaval, para-aortic mesen-

theric and iliac lymphadenopathies. Due to the presence of 

multiple lymphadenopathies, a bone marrow biopsy was per-

formed to exclude a lymphoma. Bone marrow examination 

was considered normal. Histology showed a mild reactive T 

lymphocytosis, consisting of a regular number of interstitial 

lymphocytes which showed mainly a CD3+, CD 20- pheno-

type. Bronchial aspiration with microbiologic cultures for 

Mycobacterium tuberculosis were negative. A cervical lymph 

node biopsy was performed. The lymph node structure was 

completely effaced by diffuse necrotic areas with abundant 

karyorrhectic debris (Figure 1); the search for DNA of Myco-

bacterium tuberculosis was negative. A mediastinal lymph 

node biopsy and a liver biopsy showed normal histological 

findings. At this time a definitive diagnosis was not available. 

After two months new laboratory investigations showed a 

leukocyte count of 3830/mm3, erythrocytes 3360000/mm3, 

Hgb 9,2 g/dL, thrombocytes 353.000/mm3, AST 44 U/I, ALT 

45 U/I, LDH 138 U/l. Since the patient developed recurrent 

Figure 1. Lymph node showing evident loss of architecture with 

widespread apoptosis and necrosis (inset, at high power). [Copy-

right: ©2014 Di Lernia et al.]

Figure 2. At low power, the epidermis is hyperkeratotic and the bas-

al membrane is focally thickened. The dermis shows scattered aggre-

gates of granulocytes (A). Interstitial mucin deposits are highlighted 

with Alcian PAS stain (B). [Copyright: ©2014 Di Lernia et al.]



Observation  |  Dermatol Pract Concept 2014;4(1):6 49

ies were not found. Laboratory findings were unremarkable 

except for neutropenia, anemia and elevated LDH. Two 

months later our patient developed a SCLE. She presented 

leukopenia and photosensitivity, but she did not fulfill ACR 

(American College of Rheumatology) criteria for the diagno-

sis of SLE. However, since we have a 38-month follow-up, a 

clinical evolution of our patient’s SCLE toward SLE in the 

future cannot be definitely excluded.

SCLE has exceptionally been reported in association with 

KFD [11]. KFD may be the initial diagnosis in patients who 

go on to develop SLE later on. A lag time of 10 months to 3 

years has been observed between the diagnosis of KFD and 

the subsequent onset of SLE [12]. Pathological features of 

KFD and LL show significant overlap. Thus patients with 

necrotizing lymphadenitis should be monitored long term for 

SLE. It is suitable to test for autoimmune disease repeatedly 

even if ANAs are initially negative.

References
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38-month follow up the patient is free of skin and systemic 

symptoms. Now she is taking hydroxychloroquine 400 mg/

day. Laboratory investigations are all within normal value, 

except for persistent complement deficiency in C3 and C4.

Discussion

The etiology of KFD is unknown and controversial. The viral 

origin remains still a hypothesis that has not definitely been 

proven. Common presentation signs are acute symmetrical 

painful swelling of predominantly cervical lymph nodes, fever 

and systemic signs. The nature of the clinical and pathophysi-

ological relationships between KFD and SLE remains a matter 

of debate, in particular whether KFD can be considered an 

atypical manifestation of SLE [3].

Both conditions share the predilection for young females 

and similar clinical features, including lymphadenopathy, 

mainly in the cervical lymph nodes, fever, arthralgia, and 

leukopenia [4].

Histopathologic findings of KFD are crucial in character-

ization of this condition. Diagnosis is generally made upon 

on pathological examination of the excised lymph nodes. 

Typical morphological features include apoptotic necrosis 

in paracortical areas with abundant karyorrhectic debris, 

infiltration of histiocytes, CD123+ plasmacytoid dendritic 

cells, CD8+ T cells, and the absence of neutrophils [5]. Lupus 

lymphadenitis (LL) is characterized by prominent necrosis, 

strikingly similar to that described in patients with KFD. 

Some histological findings, such as the presence of hematoxy-

lin bodies, prominent plasma cells and neutrophils support 

the diagnosis of LL [6]. However histology alone may be not 

enough to distinguish between KFD and LL [7].

When KFD occurs with skin involvement, there are two 

major possibilities. The first one is a SLE with cutaneous and 

lymph-node involvement, mainly if histopathology of skin 

lesions show interface dermatitis [8]. In this case KFD may in 

fact be a histopathologic characteristic of SLE supporting the 

hypothesis that KFD is a rare manifestation of SLE [3]. The 

second one is benign, self-limited KFD with transient cutaneous 

involvement. Extra-nodal involvement in KFD is uncommon; 

skin manifestations are observed in 5–30% of patients [9]. Var-

ious skin lesions, such as urticaria-like erythematous papules, 

nodules, plaques, and indurate lesions, have been reported. In 

addition, also lupus-typical skin manifestations, as malar rash 

and photosensitivity, have been observed [10]. In such cases, 

histopathology of skin lesions usually show lymphohistiocytic 

infiltrates accompanied by non-neutrophilic karyorrhetic 

debris, similar to those observed in the involved lymph nodes.

In our patient a necrotizing lymphadenitis preceded the 

onset of lupus skin disease. The lymph node biopsy showed 

extensive necrosis suggesting the possibility of LL, however 

aggregates of nuclear debris or so-called hematoxylin bod-