Introduction
Extraskeletal myxoid chondrosarcoma, also referred
to as chondroid sarcoma, is a rare malignant soft tissue sarcoma
that accounts for 2.5% of all soft tissue sarcomas and exhibits a
multinodular structure that is rich in mucus (1). This type of tumor was first reported by
Enzinger et al (2) in 1972 as
a unique clinical case. Extraskeletal myxoid chondrosarcoma has the
potential for multiple differentiation and was traditionally
classified as a low-grade malignancy. However, long-term follow-up
revealed that extraskeletal myxoid chondrosarcoma was associated
with a high rate of local recurrence, metastasis and mortality. In
2005, it was categorised as a soft tissue tumour with uncertain
differentiation by the WHO Classification of Soft Tissue Tumours
(3). We herein report a case of
mandibular extraskeletal myxoid chondrosarcoma and investigate its
clinical and pathological characteristics, differential diagnosis,
treatment and prognosis via a literature review.
Case report
This study was conducted according to the principles
of the Declaration of Helsinki and approved by the Ethics Committee
of the Shanghai Ninth People's Hospital. The images included in
this article were captured by a hospital-based photographer at
Shanghai Ninth People's Hospital, Shanghai Jiao Tong University
School of Medicine. Permission to use these images for this study
has been obtained from the patient.
A male patient, aged 22 years, had identified a
gingival tumour in the lower left premolar region 2 years earlier.
The tumor was 3×2 cm in size, with no history of growth, pain or
symptoms of numbness in the teeth or gums, and occasional bleeding.
A clinical examination revealed a mass in the buccal gingiva of
teeth 34 and 35, sized 3×2 cm, with a dark red colour, a clear
boundary and firm texture. The mass was not mobile and was not
tender or painful on palpation. Whole-jaw panoramic radiographs
revealed a hypodense shadow in the mesiodistal area near the root
of teeth 34 and 35, with a clear boundary. A maxillofacial computed
tomography (CT) scan revealed a mass in the lower left premolar
soft tissue, with a shadow indicating bone destruction, a clear
boundary and uniform density. The patient sought treatment in the
Oral Surgery outpatient department of our hospital on December 17,
2014, complaining of a ‘tumour in the lower left posterior gingiva
with loosening of the teeth for >2 years’. The tumor was
preliminarily diagnosed as 34–35 epulis in the outpatient
department. Following discussion, a surgical plan was developed. On
December 24, 2014, the patient underwent surgery for 34–35 gingival
tumour resection, 34 and 35 extraction, and 34 and 35 immediate
implantation. Intraoperatively, a cystic tumour was identified,
with an intact capsule, no adhesions to the mandible, and a grey
jelly-like surface on cross-section. A consultation regarding the
postoperative pathological results was performed by experts in
multiple hospitals, and the final diagnosis was cellular type
extraskeletal myxoid chondrosarcoma of the lower left mandible. As
extraskeletal myxoid chondrosarcoma is rare and exhibits uncertain
differentiation, the patient was referred to the Department of Head
and Neck Oncology of our hospital. On January 27, 2015, under
general anaesthesia, the patient underwent lower left mandibular
block and segmental resection, submandibular triangle dissection,
vessel disassociation and musculocutaneous flap repair in the oral
and maxillofacial defect area, titanium implantation in the
mandibular defect, and fibular graft procurement. Symptomatic
anti-inflammatory (Cephalosporins), anti-edematous (Prednisone) and
hemostatic (ZhiKang; Chinese Traditional Medicine) treatment was
provided postoperatively. The surgical specimen was fixed in 10%
formalin, dehydrated, and embedded in paraffin to prepare
conventional sections for haematoxylin and eosin staining and
immunohistochemistry. The patient was followed up for 9 months,
without complaints of discomfort. Tumour recurrence was not
observed on whole-jaw panoramic radiographs and CT examination.
The pathological results revealed a mass sized
1.6×1.5×1.2 cm in the lower left mandible, with a pale colour and a
cauliflower-like surface. The tumour cells exhibited nodular growth
with a cartilage-like matrix. Some cells were heteromorphous, and
mitotic activity was observed. The immunohistochemical markers
showed positive staining for vimentin, CD99, S-100, protein gene
product 9.5, glial fibrillary acidic protein and MYB and Ki67
(~20%), and showed negative staining for cytokeratin (CK)8,
calponin, CK19, CAM5.2, CKp, P63, smooth muscle actin, CD34,
epithelial membrane antigen (EMA), CD57 and chromogranin A (CgA).
The pathological diagnosis was cellular type extraskeletal myxoid
chondrosarcoma of the lower left mandible.
Discussion
Clinical manifestations
Extraskeletal myxoid chondrosarcoma often occurs in
adults aged 50–60 years, with an average onset age of 52 years.
Only few cases have been reported in children and adolescents
(4). The male:female ratio is 2:1.
Approximately 80% of the cases occur in the deep soft tissues of
the proximal extremities and limb girdles and most commonly involve
the thigh, which accounts for ~69% of the cases. Approximately 20%
of the cases are located in the trunk, mainly in skeletal muscles,
tendons and the deep subcutis; a few cases involve the skin and
bone tissue, whereas rare sites include the vulva and the breast
(5). In recent years, individual
cases occurring intracranially (hypothalamus) and in the buccal
mucosa have been reported (6,7). According to a review of the literature,
no case of extraskeletal myxoid chondrosarcoma occurring in the
mandible has been reported to date. The main clinical manifestation
is a slow-growing tumour; local pain and dysfunction may be present
in some cases. Tumours located in joints may limit movement;
tumours located in the brain may cause headaches or visual
disorders, whereas tumours located more superficially may lead to
an increase in skin tension, superficial varicose veins, or skin
ulcers. Tumour sizes range from 1 to 25 cm, with an average size of
7 cm, and have a nodular appearance with a clear boundary.
Pathological characteristics
As discussed in Oliveira et al, the surface
of extraskeletal myxoid chondrosarcomas is myxoid or jelly-like,
with a localised myxoid-like transparent appearance; cysts,
haemorrhage, or necrosis may be observed. Under a light microscope,
extraskeletal myxoid chondrosarcomas usually exhibit a nodular
structure with abundant myxoid stroma (8). The tumour cells are circular or
polygonal and arranged in a strip-like, sieve-like and fibrous
network structures, with abundant cytoplasm that is strongly
eosinophilic or lightly stained. The nuclei are relatively uniform,
with small and inconspicuous nucleoli, and the mitotic figures are
2–3/10 high-power fields (HPFs) (8).
In the present case, immunohistochemical examination of the tumour
revealed that vimentin was continuously expressed, with S-100 and
EMA focally expressed in several lesions, whereas neurofilament
protein, neuron-specific enolase and CgA are expressed in cases
with neuroendocrine differentiation.
Differential diagnosis
Epulis
As discussed in Kfir et al, epulis is more
common among young and middle-aged individuals and female patients.
It often occurs in the buccal labial gingival papillae and most
commonly in the premolar area (9).
The tumour is relatively limited, varying in size, usually
spherical or elliptical, and may sometimes be lobulated,
polypoid-like, or have a broad sessile base. Vascular and
granulomatous type tumours are soft and red; fibrous type tumours
have a firm and hard texture with a pink colour. Generally, the
tumour grows slowly and is usually pain-free, unless ulceration
occurs on the tumour surface. The pathological characteristics of
granulomatous epulis include newly generated capillaries and
fibroblasts accompanied by inflammatory cell infiltration, mainly
consisting of lymphocytes and plasma cells, and the gingival
epithelium often shows false intraepithelial hyperplasia.
Pathologically, fibrous type epulis exhibits fibrosis of the
granulation tissue, with a reduction in the cellular and vascular
components (9). In the present case,
a small amount of chronic inflammatory cell infiltration was
observed in the coarse collagen fibres, which may calcify or ossify
within the fibre bundle, presenting as irregular trabecular bone
without dental epithelial structures.
Haemangioma
As discussed in Wyke, haemangiomas that occur in the
oral and maxillofacial area account for 60% of all haemangiomas in
the body (10). They are mostly
located on the facial skin, subcutaneous tissue and oral mucosa,
such as the tissues of the tongue, lips and floor of the mouth,
while a few cases have been reported in the jaw or deep tissues.
Cavernous haemangioma is a slow-growing soft mass with no
subjective symptoms. When the head is in a low position, the tumour
expands due to hyperaemia, and if the head returns to the normal
position, the shape of the tumour is restored. Superficial tumours
produce a blue-purple colour on the skin surface or mucous
membranes. The skin colour is normal when the tumour is located
deeper. The tumour is soft on palpation, with no clear boundary and
no tenderness. The tumour size is decreased by extrusion and
returns to the original size after the pressure is released. The
histopathological characteristics of the tumour include the
presence of irregular cavities in the lower part of the dermis and
the subcutaneous tissue, which contains red blood cells and fibrous
tissue. The cavity wall is a monolayer of endothelial cells.
Endothelial cell hyperplasia may be observed in the larger vascular
compartment, resulting in a thickened wall (10).
Fibrosarcoma
As discussed in Prat and Scully (11), fibrosarcoma is common in young adults.
Tumours located in the mouth and jaw are usually found in the gum
and the surface of the jaw, have a spherical or lobulated shape and
exhibit a purple-red colour, often with ulceration and haemorrhage.
Invasion of the surrounding tissue may lead to bone destruction and
loosening of the teeth or tooth loss. Peripheral type tumours may
present as a local mass in the early stage, followed by pain. On
histopathological examination, the tumour is composed of spindle
fibroblasts and most skin fibrosarcomas are well-differentiated,
with few mitoses, no obvious spiral structures and reduced fibre
generation. When these phenomena are present, they indicate that
the tumour is invasive and the prognosis is poor.
Treatment and prognosis
As the prognosis of extraskeletal myxoid
chondrosarcoma is good, most scholars originally classified it as a
low-grade malignancy. However, long-term follow-up revealed that,
although the behaviour of this tumour is inert, it was associated
with a high rate of local recurrence, metastasis and mortality. The
local recurrence rate was 48%, and in such cases, 58% of tumours
exhibited multifocal recurrence. The metastasis rate was 46%, and
the most common metastatic site was the lung, accounting for 63% of
the cases; however, extrapulmonary metastasis and diffuse
metastasis may also occur (12). It
has been reported that the 5-, 10- and 15-year survival rates are
82, 65 and 58%, respectively (13).
The adverse factors for poor prognosis of extraskeletal myxoid
chondrosarcoma include a tumour diameter >10 cm, abundant cells,
tumour atypia, a mitotic figure count >2/10 HPFs, and tumour
metastasis.
Extraskeletal myxoid chondrosarcoma is refractory to
radiotherapy and chemotherapy (14,15). Wide
surgical resection is currently the preferred treatment, and
incomplete tumour resection is considered a major cause of
recurrence. Postoperative localised radiotherapy and systematic
chemotherapy may be applied to reduce the rate of recurrence and
metastasis. Currently, the optimal chemotherapy regimen for
extraskeletal myxoid chondrosarcoma has not been determined and
further investigation is required in this field. In recent years,
with the development of gene therapy, researchers have found that
regulating the specific proteins of extraskeletal myxoid
chondrosarcoma may be a potential treatment, but this method
remains in the clinical trial stage (16).
References
|
1
|
Meis-Kindblom JM, Bergh P, Gunterberg B
and Kindblom LG: Extraskeletal myxoid chondrosarcoma: A reappraisal
of its morphologic spectrum and prognostic factors based on 117
cases. Am J Surg Pathol. 23:636–650. 1999. View Article : Google Scholar : PubMed/NCBI
|
|
2
|
Enzinger FM and Shiraki M: Extraskeletal
myxoid chondrosarcoma. An analysis of 34 cases. Hum Pathol.
3:421–435. 1972. View Article : Google Scholar : PubMed/NCBI
|
|
3
|
Fletcher CDM, Bridge JA, Hogendoorn P and
Mertens F: WHO classification of tumours of soft tissue and bone.
WHO Classification of Tumours. 5:(4th). IARC press. (Lyon).
223–224. 2013.
|
|
4
|
Yi JW, Park YK, Choi YM, Hong HP and Chang
SG: Bulbous urethra involved in perineal extraskeletal myxoid
chondrosarcoma in a child. Int J Urol. 11:436–439. 2004. View Article : Google Scholar : PubMed/NCBI
|
|
5
|
Fotiadis C, Charalambopoulos A,
Chatzikoklis S, Zografos GC, Genetzakis M and Tringidou R:
Extraskeletal myxoid chondrosarcoma metastatic to the pancreas: A
case report. World J Gastroenterol. 11:2203–2205. 2005. View Article : Google Scholar : PubMed/NCBI
|
|
6
|
Angiero F: Extraskeletal myxoid
chondrosarcoma of the left buccal mucosa. Anticancer Res.
32:3345–3350. 2012.PubMed/NCBI
|
|
7
|
Park JH, Kim MJ, Kim CJ and Kim JH:
Intracranial extraskeletal myxoid chondrosarcoma: Case report and
literature review. J Korean Neurosurg Soc. 52:246–249. 2012.
View Article : Google Scholar : PubMed/NCBI
|
|
8
|
Oliveira AM, Sebo TJ, McGrory JE, Gaffey
TA, Rock MG and Nascimento AG: Extraskeletal myxoid chondrosarcoma:
a clinicopathologic, immunohistochemical, and ploidy analysis of 23
cases. Mod Pathol. 13:900–909. 2000. View Article : Google Scholar : PubMed/NCBI
|
|
9
|
Kfir Y, Buchner A and Hansen LS: Reactive
lesions of the gingiva. A clinicopathological study of 741 cases. J
Periodontol. 51:655–661. 1980. View Article : Google Scholar : PubMed/NCBI
|
|
10
|
Wyke BD: Primary hemangioma of skull rare
cranial tumor review of the literature and report of case with
special reference to roentgenographic appearance. Am J Roentgenol
Radium Ther. 61:302–316. 1949.PubMed/NCBI
|
|
11
|
Prat J and Scully RE: Cellular fibromas
and fibrosarcomas of the ovary: a comparative clinicopathologic
analysis of seventeen cases. Cancer. 47:2663–2670. 1981. View Article : Google Scholar : PubMed/NCBI
|
|
12
|
Gupta R, Sharma MC, Attri S and Guleria S:
Testicular metastasis of extraskeletal myxoid chondrosarcoma:
Report of first case. Urology. 71:984.e1–e4. 2008. View Article : Google Scholar
|
|
13
|
Drilon AD, Popat S, Bhuchar G, D'Adamo DR,
Keohan ML, Fisher C, Antonescu CR, Singer S, Brennan MF, Judson I
and Maki RG: Extraskeletal myxoid chondrosarcoma: A retrospective
review from 2 referral centers emphasizing long-term outcomes with
surgery and chemotherapy. Cancer. 113:3364–3371. 2008. View Article : Google Scholar : PubMed/NCBI
|
|
14
|
Stacchiotti S, Dagrada CP, Morosi C, Negri
T, Romanini A, Pilotti S, Gronchi A and Casali PG: Extraskeletal
myxoid chondrosarcoma: Tumor response to sunitinib. Clin Sarcoma
Res. 2:222012. View Article : Google Scholar : PubMed/NCBI
|
|
15
|
Han K, Sun YJ, Shan Z, Zhang JJ, Lin F,
Zhao H, Meerani S and Yao Y: Extraskeletal myxoid chondrosarcoma: A
case report of complete remission by chemotherapy and review of the
literature. BMJ Case Rep. 2010:bcr07.2009.21282010.PubMed/NCBI
|
|
16
|
Stacchiotti S, Dagrada GP, Morosi C, Negri
T, Romanini A, Pilotti S, Gronchi A and Casali PG: Extraskeletal
myxoid chondrosarcoma: Tumor response to sunitinib. Clin Sarcoma
Res. 2:22–33. 2012. View Article : Google Scholar : PubMed/NCBI
|
