Giant Cell Tumor of the Mandible

Article information

Clin Exp Otorhinolaryngol. 2012;5(1):49-52
Publication date (electronic) : 2011 February 23
doi : https://doi.org/10.3342/ceo.2012.5.1.49
Department of Otorhinolaryngology, Yonsei Head and Neck Cancer Clinic, Yonsei University Health System, Seoul, Korea.
Corresponding author: Eun Chang Choi, MD. Department of Otorhinolaryngology, Yonsei Head and Neck Cancer Clinic, Yonsei University Health System, 250 Seongsan-no, Seodaemun-gu, Seoul 120-752, Korea. Tel: +82-2-2228-3608, Fax: +82-2-393-0580, eunchangmd@yuhs.ac
Received 2009 May 22; Revised 2009 November 02; Accepted 2009 November 26.

Abstract

A 53-year-old woman presented with left mandibular area pain, trismus, and facial numbness that had persisted for 4 years. Physical examination revealed a 3×5 cm, hard, non-tender, and round mass on the left mandibular area. Computed tomography and magnetic resonance imaging revealed an expansile tumor involving the left mandibular ramus and temporomandibular joint area with bone destruction, extending to the base of middle cranial fossa and left zygomatic bone. The mass at the segment of left mandible and zygomatic bone, and base of middle cranial fossa was removed. Pathological examination of the mass revealed a giant cell tumor. The defect was reconstructed with iliac bone for the mandible and temporal bone and fascia for the cranial bone and dura. The case is described along with a review of the literature.

INTRODUCTION

Giant cell tumors (GCTs) are benign bone tumors arising from bone marrow, which account for about 5% of all biopsied primary bone tumors (1-3). GCTs arising in the head and neck region constitute approximately 2% of all GCTs, with the majority occurring in the sphenoid, ethmoid, or temporal bones (4, 5). To date, only a few reports of GCT arising from the craniofacial skeleton have been published, including from the parieto-occipital bones (6, 7), maxilla (8, 9), zygomatic bone (10, 11), and laryngeal cartilages (12). Only two studies have addressed treatment of the mandible giant cell tumors, especially with skull base extension (13, 14). We present a case of GCT arising from the mandible.

CASE REPORT

A 53-year-old female was referred to our head and neck cancer clinic for a mass lesion at the mandibular area. The patient presented with left mandibular area pain, trismus, and facial numbness that had persisted for 4 years. The patient had a medical history of osteoarthritis and osteoporosis. Physical examination revealed a 3×5 cm, hard, non-tender, and round mass on the left mandibular area. No other otorhinolaryngological and systemic abnormalities were evident.

Computed tomography (CT) revealed an expansile tumor involving the left mandibular ramus and temporomandibular joint area with bone destruction, extending to the base of middle cranial fossa (Fig. 1). The tumor also extended to the left zygomatic bone. Magnetic resonance imaging (MRI) showed a 3×5 cm, heterogenous, well-defined, and expansile mass displacing the lateral pterygoid and temporalis muscle laterally, and involving the dura at the base of the middle cranial fossa (Fig. 2). On positron emission tomography-CT, elevated uptake of fludeoxyglucose was noted at the left masticator space, and no metastatic lesion was observed. We initially considered ameloblastoma, lymphoma, chondrosarcoma, and giant cell tumor. The patient did not undergo preoperative biopsy because an imaging study and preoperative biopsy including fine needle aspiration is often not sufficient for a diagnosis. Based on the clinical and radiographic criteria, this case was classified as an aggressive form (15). Therefore, we planned wide complete excision and reconstruction.

Fig. 1

CT findings showing the TMJ lesion (arrow) and extension to the base of middle cranial fossa (arrowhead).

Fig. 2

Facial MRI findings revealing 5×3 cm sized heterogenous, well-defined and expansile mass is located at the condylar fossa (arrow).

The patient underwent mass excision using a modified Blair and cervical incisions to preserve the parotid gland. The mass was resected with a segment of the left mandible and zygomatic bone (Fig. 3). The mass at the base of middle cranial fossa was also removed. The defect was reconstructed with iliac bone for mandible and temporal bone, and with fascia for cranial bone and dura (Fig. 4). No perioperative complications occurred.

Fig. 3

(A) The mass lesion is exposed from infraparotid space (i) and from supraparotid space (ii). (B) After mass resection and segmental mandibulectomy, the defect is observed from infraparotid space (i) and from supraparotid space (ii).

Fig. 4

(A) Reconstruction of cranial bone and dura with left temporalis bone and fascia. (B) Reconstruction of mandible A with iliac bone.

Microscopic examination revealed evenly distributed multinucleated giant cells with surrounding stroma made up of spindle cells. The giant cells displayed nucleoli that were similar to the surrounding spindle cells, suggestive of an osteoclastic type, which was consistent with a GCT (Fig. 5). The tumor involvement of the dura was confirmed and resection margins at the surrounding area were free.

Fig. 5

Evenly distributed multinucleated giant cell with surrounding stroma made up of spindle cells are shown, which were consistent with GCT.

During a 1-year serial clinical and radiological follow-up, there was no evidence of recurrence (Fig. 6). The facial contour and masticatory function was well-preserved, though lateralization of the mandible was observed on the opening of mouth due to pterygoid muscle injury.

Fig. 6

(A) Postoperative CT taken 1 year after the operation reveals no sign of recurrence. (B) The facial contour and masticatory function was well preserved, except for the lateralization of the mandible on the opening of mouth.

DISCUSSION

GCT is a true neoplastic process originating from the undifferentiated mesenchymal cells of the bone marrow (10). It is generally considered as benign (6) but severe bony destruction may result occasionally depending on the location and clinical presentation of the tumor, making tumor management very challenging (9). GCTs are usually mono-ostotic, although they may occasionally present in a polyostotic form, which is usually of a high grade (16).

Patients with head and neck GCT may present with diverse symptoms depending on the location of primary lesion; symptoms include swelling, pain, epistaxis, neurological deficits, proptosis, visual defects, tinnitus, and hearing loss. In this case, GCT arising from the mandible caused temporo-mandibular pain and trismus.

Radiologic examination of GCT usually reveals a well-circumscribed lytic lesion surrounded by little or no sclerosis. The tumors may infrequently break through the cortex and invade the soft tissue or the articular space (4, 17). A CT scan can provide a detailed assessment of GCT, showing the soft tissue mass of the lesion, cortical perforation, amount of bony destruction, and extension toward important adjacent anatomic structures such as the cranial base (9). MRI is superior to CT in delineating the extent of soft tissue tumor because of its improved contrast resolution (9). Bone scintigraphy shows increased radionuclide uptake in the majority of GCTs (9).

The differential diagnosis of GCT includes aneurismal bone cyst, chondroblastoma, dermoid cyst, chondrosarcoma, giant cell reparative granuloma, and pigmented villonodular synovitis (4, 17). When an aggressive growth pattern is evident, the possibility of chondrosarcoma, osteosarcoma, and metastatic lesion cannot be ruled out until confirmation by histologic examination.

The final diagnosis is established only on the basis of a biopsy (5). Histologically, GCTs are composed of multinucleated giant cells in a vascular stroma of epitheloid or spindle-shaped mononuclear cells (18). The pathologic differential diagnosis of GCT is also extensive, including giant cell reparative granuloma, brown tumor of hyperparathyroidism, osteoblastoma, chondroblastoma, aneurismal bone cyst, non-ossifying fibroma, foreign body reaction, and osteosarcoma with abundant giant cells. These can be difficult to distinguish from one another, particularly at fine needle aspiration or with frozen section specimens (9).

Although it is regarded as benign, the giant cell tumor is locally aggressive, and can even metastasize to the lung (17). Malignant giant cell tumors have been reported (6), usually resulting from secondary malignant transformation after radiation treatment (19). They present with marked atypia and pleomorphism with mitotic activity and vascular invasion (20).

The treatment of choice of GCT is surgical excision (10). Regardless of the site of presentation, partial resection or curretage results in a recurrence rate of up to 70%, whereas recurrence after wide resection is about 7% (21). Radiotherapy is generally avoided and is reserved for GCTs that are considered inoperable, due to the risk of sarcomatous transformation (9), although some authors have advocated the use of radiotherapy in the management of GCT. Other treatment modalities including cryotherapy, chemotherapy, and curretage with adjuvant agents have been tried, but have yielded less effective results (10). GCTs generally recur within the first 3 years if recurrence occurs. But, continuous evaluation up to 5 years is recommended, since late distant metastasis have been reported (9).

After extended GCT resection, reconstruction of the defect is often required for functional and esthetical reasons. Osteoarticular autograft, allograft, and prosthetic reconstruction have been described (9, 22). A previous report suggested that the use of autologous tissue enables the rapid incorporation with a lower risk of infection, especially with vascularized grafts (9).

In conclusion, GCT arising from the mandible is a rare disease whose diagnosis is difficult. Imaging and preoperative biopsy including fine needle aspiration is often not sufficient to make the diagnosis. Therefore, the possibility of GCT should be included in the differential diagnosis of a bony lesion of craniofacial bones until a final diagnosis is made using a permanent pathologic specimen. Wide complete excision is required since incomplete excision results in a high incidence of recurrence.

Notes

No potential conflict of interest relevant to this article was reported.

References

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Article information Continued

Fig. 1

CT findings showing the TMJ lesion (arrow) and extension to the base of middle cranial fossa (arrowhead).

Fig. 2

Facial MRI findings revealing 5×3 cm sized heterogenous, well-defined and expansile mass is located at the condylar fossa (arrow).

Fig. 3

(A) The mass lesion is exposed from infraparotid space (i) and from supraparotid space (ii). (B) After mass resection and segmental mandibulectomy, the defect is observed from infraparotid space (i) and from supraparotid space (ii).

Fig. 4

(A) Reconstruction of cranial bone and dura with left temporalis bone and fascia. (B) Reconstruction of mandible A with iliac bone.

Fig. 5

Evenly distributed multinucleated giant cell with surrounding stroma made up of spindle cells are shown, which were consistent with GCT.

Fig. 6

(A) Postoperative CT taken 1 year after the operation reveals no sign of recurrence. (B) The facial contour and masticatory function was well preserved, except for the lateralization of the mandible on the opening of mouth.