Low-Grade Myofibroblastic Sarcoma of the Tongue: Case Report and Review of Literature

Abstract

Introduction: Low-grade myofibroblastic sarcoma (LGMS) is one of the ultra-rare malignant soft tissue tumors, with an annual incidence of less than 1 per 1,000,000. However, due to its rarity, there is currently no standardized treatment guideline. The therapeutic approaches remain under investigation with the ongoing accumulation of clinical experience. Case Report: A 55-year-old female with no significant medical history presented with a two-week history of a tongue mass and associated numbness. Physical examination revealed a 1.4 cm, firm, non-tender lesion on the ventral surface of the tongue. An excisional biopsy was performed, and the tumor was identified as an LGMS, characterized by spindle-shaped cells infiltrating adjacent skeletal muscle. Immunohistochemistry showed positive staining for α-SMA and negative results for desmin, cytokeratin, P63, CD34, S100, and Ki67. A PET-CT scan revealed focal FDG uptake in the tongue, likely related to postoperative changes, with no distant metastasis. The clinical stage was T1N0M0. In this report, a review of the literature was conducted, summarizing the interpretation of immunohistochemistry and discussing relevant studies on the treatment of LGMS. Conclusion: LGMS should be considered in the differential diagnosis of tongue tumors, with biopsy being crucial for confirming the diagnosis. Due to its rarity, there are no standardized treatment protocols, but surgical excision remains the primary approach. Given the risk of recurrence, regular follow-up is recommended.

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Shih, H. and Lee, C. (2025) Low-Grade Myofibroblastic Sarcoma of the Tongue: Case Report and Review of Literature. International Journal of Otolaryngology and Head & Neck Surgery, 14, 145-151. doi: 10.4236/ijohns.2025.143017.

1. Introduction

Low-grade myofibroblastic sarcoma (LGMS) is classified as an ultra-rare soft tissue malignant tumor. Ultra-rare sarcomas, defined as an annual incidence of less than 1 per 1,000,000, poses challenges for well-powered prospective studies due to its rarity [1].

This tumor has been reported on various sites of the body. According to previous studies, the most common sites of LGMS vary, with some studies identifying the extremities and trunk as the most frequent location [2], while others suggest a higher prevalence in the head and neck region [3].

The diagnosis of LGMS depends on pathological examination of surgical specimens. Due to its rarity, there is no current standardized treatment guideline for LGMS. According to the literature, proposed treatment modalities include surgical intervention, radiotherapy, chemotherapy, and target therapy [4]-[6].

Here, we describe the clinical, histological, immunohistochemical, and radiographic features of an LGMS of the tongue and review the different managements of LGMS.

2. Case Report

A 55-year-old female with no significant systemic diseases presented to our clinic with a tongue mass accompanied by a numbness sensation for two weeks. She denied experiencing pain, and there was no discharge from the lesion. She reported no history of smoking, betel nut chewing, or alcohol consumption. She came to our hospital for help and physical examination revealed a palpable 1.4 cm tumor on the ventral surface of the tongue. The lesion was firm in consistency and non-tender.

We performed the operation of excisional biopsy under local anesthesia. The tumor measured approximately 1.4 × 1.0 × 0.8 cm in size. It appeared white tan and was firm to the touch. Microscopically, the tumor was composed of spindle-shaped cells with slightly enlarged nuclei. The tumor cells were arranged in fascicles and infiltrated into the adjacent skeletal muscle. The mitotic index was 3 per square millimeters. Further immunohistochemical staining was performed for differential diagnosis. The tumor cells were positive for alpha-smooth muscle actin (α-SMA). However, they were negative for desmin, cytokeratin (CK), P63, CD34, S100, and Ki67 (Figure 1). Based on these pathological features, a diagnosis of LGMS was favored.

The patient experienced only mild postoperative pain with no other complications. A whole-body positron emission tomography-computed tomography (PET-CT) scan was performed for cancer staging (Figure 2). The imaging report only indicated focal increased fluorodeoxyglucose (FDG) uptake in the tongue, likely due to postoperative changes. There was no evidence of distant metastasis. The clinical stage was T1N0M0. Unfortunately, the patient had lost follow-up at our hospital.

Figure 1. Histological staining and Immunohistochemistry. (a) Hematoxylin and eosin staining demonstrated that the tumor primarily consisted of spindle-shaped cells; (b) Immunohistochemically, LGMS showed positive staining for α-SMA and negative staining for; (c) desmin; (d) CK; (e) P63; (f) CD34; (g) S100; (h) Ki67 (a-h: ×200).

Figure 2. PET-CT reported clinical stage of T1N0M0. (a) Axial; (b) Coronal; (c) Sagittal view.

3. Discussion

LGMS is an ultra-rare malignant soft tissue sarcoma with a low prevalence [1]. It most commonly arises from the head and neck region or the extremities [2] [3] [7] [8]. LGMS can occur across a wide age range, with case reports documenting cases from 2 to 85 years old [9]. Clinically, it typically presents as a painless mass [10]. Definitive diagnosis requires histopathological examination through excisional biopsy.

LGMS exhibits diverse immunophenotypic profiles, including smooth muscle actin (SMA) positivity with desmin negativity, desmin positivity with SMA negativity, or co-expression of both markers [11]. On immunohistochemistry, the tumor cells of our patient were positive for α-SMA but negative for desmin, CK, CD34, and S100. We conducted a literature review on tongue LGMS and summarized the immunohistochemical staining results (Table 1). Desmin was positive in 4 of 10 cases, and α-SMA was positive in 9 of 10 cases.

Table 1. Immunohistochemical summary of previously reported cases of LGMS in tongue.

Year

Location

Gender

Age

Size (cm)

α-SMA

desmin

CK

CD34

S100

References

2006

tongue

Female

24

2

+

-

[12]

2007

tongue

Male

41

1.5

+

+

-

-

[13]

2007

tongue

Male

53

2

+

-

[14]

2009

tongue

Female

61

2

+

-

[8]

2010

tongue

Male

56

4.2

-

+

-

-

[15]

2015

tongue

Male

74

4.1

+

-

-

-

[16]

2018

tongue

Female

38

1.5

+

[17]

2019

tongue

Male

41

2

+

+

[18]

2022

tongue

Male

73

4

+

+

+

[19]

2025

tongue

Female

55

1.4

+

-

-

-

-

Present case

LGMS are more likely to recur locally than metastasis to distant sites [20]. Although LGMS typically exhibits indolent growth, clinical follow-up is still necessary due to its associated recurrence rate. Maruyama et al. reported local recurrence and distant metastasis rates of 29% and 2%, respectively [21].

Because LGMS is very rare, a standardized treatment guideline has not yet been established. According to several previous studies, surgical excision may be the most effective therapy [4] [6] [7]. A 2021 study reported that surgical intervention was associated with significantly improved overall survival in LGMS patients, whereas the absence of surgery was a poor prognostic factor [6]. The role of radiotherapy and chemotherapy in LGMS is still uncertain. Some reports have documented notable clinical improvement with adjuvant chemotherapy in cases with metastases, leading to extended progression-free survival [22]. One systematic review concluded that adjuvant radiation therapy showed no benefit in reducing recurrence rates [23]. It has also been recommended to avoid radiotherapy after the resection of LGMS, as it may contribute to tumor recurrence [21]. Besides, target therapy with apatinib may be a potential treatment for LGMS [5]. Additional studies, incorporating long-term follow-up data and comprehensive clinical information, are needed to establish new treatment protocols for LGMS.

4. Conclusion

When encountering a tongue tumor, LGMS should be considered as a potential diagnosis, and a biopsy is essential to confirm the pathological diagnosis. There are no standardized treatment protocols for LGMS due to its rarity. According to current research, surgical excision is the primary treatment. Furthermore, given the potential for recurrence, it is recommended that patients undergo regular follow-up.

Ethical Approval

The study was reviewed and approved by the Ethics Committee of Shin Kong Wu-Ho-Su Memorial Hospital (Number: PJ2025032901).

Abbreviations

LGMS: Low-grade myofibroblastic sarcoma

α-SMA: Alpha smooth muscle actin

SMA: Smooth muscle actin

CK: Cytokeratin

PET-CT: Positron emission tomography-computed tomography

FDG: Fluorodeoxyglucose

Conflicts of Interest

The authors declare no conflicts of interest regarding the publication of this paper.

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