Introduction
Langerhans cell histiocytosis (LCH) is characterized
by the proliferation of abnormal dendritic antigen-presenting
histiocytes. LCH may involve almost any organ. The clinical
presentation of LCH therefore varies and is frequently misdiagnosed
(1–3). We report a patient who was initially
admitted to the liver department with sclerosing cholangitis (SC),
but was eventually diagnosed with multisystem LCH.
Case report
A 35-year-old Chinese male was admitted to our
hospital with a 2-year history of jaundice and pruritus. The
patient’s laboratory test results are shown in Table I. Magnetic resonance
cholangiopancreatography (MRCP) and the pathology of a liver biopsy
supported the diagnosis of SC by a local hospital. The patient
received treatment with ursodeoxycholic acid (UDCA) at a dose of
750 mg/day, with no marked response. The patient had no history of
smoking, alcohol consumption or blood transfusions, and no family
history of similar symptoms. Physical examinations revealed mildly
icteric sclera and skin, coarse breath sounds in the lungs and
enlargement of the spleen accompanied by percussion pain. A
1.0×1.0-cm defect was detected in the patient’s occipital bone,
which had occasionally caused pain over the previous 8 months.
 | Table IComparison of figures at admission and
following chemotherapy. |
Table I
Comparison of figures at admission and
following chemotherapy.
| 2 years ago | At admission | Following
chemotherapy | Normal range |
|---|
| ALT (U/l) | 134 | 110 | 52 | 0–40 |
| AST (U/l) | 78 | 81 | 30 | 0–40 |
| GGT (U/l) | 698 | 73 | 113 | 8–55 |
| ALP (U/l) | 538 | 431 | 303 | 30–150 |
| TBIL (μmol/l) | 17 | 67 | 34 | 3.42–17.1 |
| DBIl (μmol/l) | 6.5 | 38.7 | 13 | 0–6.84 |
| ESR (mm/h) | 35 | 26 | 10 | 0–20 |
| Immunoglobin IgG
(mg/dl) | 1890 | 1920 | 1550 | 723–1685 |
The laboratory examination showed a normal complete
blood count, positive urine bilirubin and urobilinogen, a normal
stool test and an erythrocyte sedimentation rate (ESR) of 26 mm/h.
Liver function test results are shown in Table I. Viral hepatitis markers were
negative. Immunoglobulin (IgG) was 1,920.0 mg/dl. Antinuclear
antibody (1:80) (normal <1:80) was positive. Anti-smooth muscle,
anti-liver/kidney microsome, anti-soluble liver antigen and liver
cytosol antigen type I antibody were all negative.
Anti-mitochondrial antibody subtype-2, extractable nuclear antigen
and double-stranded DNA (ds-DNA) were negative. α-fetoprotein,
carcinoembryonic antigen and CA19-9 concentrations were also
normal. Body mass index was normal.
An X-ray examination showed multifocal osteolytic
bone lesions, including the right occipital bone (Fig. 1A), left iliac bone, left neck of the
femur (Fig. 1B) and the seventh
posterior segment of the rib. Chest radiography (Fig. 1C) and computed tomography (CT) scans
of the lungs (Fig. 1D) revealed
marked reticular opacities and diffuse small cysts. CT showed
multiple low-density lesions in the liver. The lesions were shown
as hyperechoic areas on ultrasound examination, while isointense
intensity areas on the T1-weighted image and low intensity areas
without enhancement on the axial fat-suppressed T2-weighted image
were visualized by magnetic resonance imaging (MRI) (Fig. 2A). This observation suggested the
possibility of fat deposition on the liver. MRCP (Fig. 2B) was highly suggestive of SC,
including segmental intrahepatic bile duct dilatation and stenosis,
and proximal strictures of the right and left hepatic ducts.
However, the common hepatic duct exhibited no stenosis or
dilatation.
Fine-needle liver biopsy under ultrasound guidance
and hematoxylin-eosin staining showed interstitial fibrosis and
inflammatory infiltrates in the portal area, epithelial injury and
reactive hyperplasia of small bile ducts with cholestatic features,
phagocyte aggregation and lipid granuloma formation (Fig. 2C and D), suggesting chronic
intrahepatic cholestasis and moderate steatosis. However,
eosinophils or macrophages were not found and immunohistochemical
stains for CD1a and S-100 protein were negative. The occipital bone
biopsy revealed bone granulomas consisting predominantly of
macrophages, intermixed with eosinophils (Fig. 3A). The macrophages were strongly
positive for antibodies to CD1a (Fig.
3B) and S100 (Fig. 3C)
antigens. Immunohistochemical analysis showed that 10% of cells
were positive for the proliferation marker Ki-67 (Fig. 3D). We also investigated the
involvement of other organs. Bone marrow puncture showed bone
reactive hyperplasia. Brain MRI revealed no abnormalities of the
hypothalamic-pituitary region. No thyroid lesions were detected by
ultrasonography, and gastroscopy and colonoscopy revealed no
involvement of the gastrointestinal tract.
The patient was diagnosed with multisystem,
high-risk organ LCH and was referred to the hematological
department for specific treatment. A first course of chemotherapy
(vinblastine 6 mg/m2 i.v. bolus; prednisone 40
mg/m2/day orally, weekly reduction after week 4) was
administered. Although the patient developed adverse effects of
chemotherapy, such as bacterial infection, chemotherapy was
continued and supportive treatment lead to bone pain being
relieved, liver function improving and normalization of ESR
(Table I).
Discussion
LCH often presents as a puzzling syndrome and is
difficult to diagnose in adults. The incidence of LCH in adults may
reach 1–2 cases per million and is thus significantly lower than
that in children (4). The
35-year-old patient came to the liver department with liver
dysfunction as the first symptom, and the patient’s history and
laboratory examination excluded the common causes of liver
dysfunction. SC and multifocal osteolytic bone lesions made us
consider the possibility of a single disease with multisystem
involvement.
However, the immunohistochemical analysis of the
liver biopsy yielded negative results for CD1a and S-100, possibly
as the disease process is usually found around the major bile
ducts, and a blind liver biopsy may therefore miss the LCH
infiltration, and as the number of Langerhans cells varies in
different lesions, with limited numbers observed in the liver,
spleen, gastrointestinal or central nervous system tissues
(5). Secondly, the liver biopsy and
results of MRCP supported a diagnosis of SC. When LCH infiltrates
the liver, it shows a propensity for the biliary ducts, leading to
the development of cholestasis with an increase in GGT and ALP. The
TB levels do not appear to vary in correlation to GGT or ALP. The
pathological pattern ranges from mild cholestasis to more severe
periportal infiltration with consequent hepatocellular injury in
LCH. Bile duct involvement is capable of progressing to a SC-type
image, fibrosis and eventually to liver failure. Although SC
patients typically present with a cholestatic biochemical profile
with 3–10 times the upper limit of serum ALP, this finding is
neither specific nor mandatory (6).
The serum levels increase with fluctuations due to
choledocholithiasis or dominant stenoses with progression of the
disease.
This progressive damage may continue, despite the
regression of the LCH (6,7). Diagnostic imaging was able to
visualize areas of LCH infiltration that may have been missed by
biopsy. Imaging findings of liver involvement may vary depending on
the progressive histological phase: proliferative, granulomatous,
xanthomatous or fibrous phases (8).
Diagnostic imaging results of this study have shown that the liver
damage in this patient was in the xanthomatous stage.
Various treatment strategies have been employed in
adult LCH patients, depending on the degree of organ involvement
and the clinical course. Treatment of multisystem LCH normally
benefits from systemic therapy, which usually reduces morbidity and
mortality (3,9). Our patient received an initial 6-week
course of therapy (prednisone 40 mg/m2/day orally,
weekly reduction after week 4, vinblastine 6 mg/m2 i.v.
bolus, weekly) according to the Histiocyte Society Evaluation and
Treatment Guidelines (10).
Although the patient achieved partial remission following the first
course of chemotherapy, the patient’s prognosis remained uncertain.
A number of studies have reported high mortality (30–50%) when
high-risk organs including the liver, spleen, lungs and
hematopoietic system are involved, compared with the situation when
these areas are not involved (<10%). The 3-year survival rate
with liver involvement is 51.8%, compared with that of 96.7%
without liver involvement (11).
In conclusion, our case is a rare presentation of
multisystem LCH with liver dysfunction as the first presentation in
an adult. Particular attention should be paid to osteolytic skull
lesions associated with liver dysfunction or pulmonary symptoms in
order to gain a better understanding of the pathophysiology of LCH
and improve diagnosis and treatment.
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