1. The oral tongue is freely mobile and composed mainly of skeletal muscle. It has a dorsal (exposed) surface, ventral surface, and tip. The dorsal surface contains numerous papillae that have specialized taste receptors. The floor of the mouth lies beneath the tongue and is divided into sides by the midline frenulum (mucosal fold) of the tongue. It contains ostia of the submandibular and sublingual salivary glands, whereas the main duct of the parotid gland (Stensen’s duct) enters the oral cavity through the buccal mucosa. The hard palate forms the roof of the oral cavity and consists of portions of the maxillary and palatine bones.

2. The oral cavity is lined by stratified squamous mucosa with prominent mucoserous glands in the submucosa. Most of the mucosa is nonkeratinizing with the exception of the hard palate, gingiva, and dorsal tongue, which become keratinized due to the friction of mastication.

1. Open procedure specimens are widely variable depending on the location of the tumor. Because many lesions encroach upon or invade the bone of the mandible or maxilla, composite resections with bone and soft tissue are common. As a generalization, all specimens need to be oriented appropriately, the soft tissue margins inked, and mucosal and soft tissue margins evaluated followed by sectioning of the tumor relative to cartilage/bone and tissue margins. Margins should be evaluated by either shave or radial sections, depending on the nature of the specimen. If the tumor is relatively distant from a margin, 1- to 2-mm shave sections are preferred. If the tumor grossly approximates a margin to <1 to 2 mm, radial sections should be taken.

2. Partial resections with a CO₂ laser under an operating microscope are becoming more common. Because the inherent approach of this procedure is to excise the tumor piece by piece, the surgeon inks the individual pieces as he/she alone knows what constitutes the true margin. In the gross room all that is therefore required is to measure the pieces provided, describe them, and submit them entirely in sections perpendicular to the ink. If there is an additional orienting marker such as a suture, then one should submit the sections sequentially from that end to the opposite end.

1. Lichen planus. This disorder commonly affects the oral mucosa. Whereas skin involvement is usually self-limited, oral lichen planus follows a more protracted waxing and waning course. The oral lesions are typically asymptomatic unless ulceration occurs.

Any oral mucosal surface may be involved, and several patterns can be seen. The classic pattern is reticular with intersecting white keratotic streaks (Wickham’s striae); the lesions are ill-defined, and the background may be erythematous due to mucosal atrophy. Some lesions may be mostly erythematous with minimal keratotic streaks, whereas others may show extensive keratinization and/or ulceration or form bullae. Microscopically, a dense submucosal band of lymphocytes is present, which may be less distinct in ulcerated lesions (e-Fig. 1.1).^* The rete ridges may be hyperplastic (saw-toothed) or flattened. There is loosening of the basal layer of the epithelium, with degeneration of individual keratinocytes that may form eosinophilic colloid (dyskeratotic, cytoid, or Civatte) bodies (e-Fig. 1.2). The surface may show hyperor parakeratosis. Although the histologic findings of lichen planus have been well defined, they are nonetheless not specific; for example, some oral lesions with a similar histologic picture may be due to a contact hypersensitivity reaction. In addition, a lichenoid infiltrate may accompany dysplastic lesions.

Asymptomatic patients require no treatment, but steroids (particularly topical) are often used for erosive or erythematous lesions. Some data suggest that there is an increased risk of malignant transformation in the erythematous, ulcerative, and bullous forms of oral lichen planus. Although this proposed risk of malignancy is controversial, these lesions at least require closer clinical follow-up.

2. Pemphigus vulgaris. This is an uncommon disorder that causes superficial ulceration of the skin and mucous membranes. Involvement of the oral mucosa may precede the development of skin lesions. The disease is caused by autoantibodies to desmogleins 1 and 3, cellular transmembrane proteins involved in the assembly of desmosomes. Cell-to-cell adhesion is impaired in the suprabasal epithelium, leading to clefting and ulceration. Flaccid bullae that easily rupture to form painful erosions can be seen on any oral mucosal surface. The lesions heal without scarring. Microscopically, intraepithelial separation with edema and acantholysis, which imparts a “tombstone” appearance to the remaining attached basal cell layer (e-Fig. 1.3), is seen at the edge of the ulcer. Acute and chronic inflammation are frequently present in the submucosa. Direct immunofluorescence is positive for immunoglobulin G (IgG) along cell membranes throughout the epidermis.

Paraneoplastic pemphigus, which is associated with an underlying malignancy, may be distinguished from pemphigus vulgaris by the identification of a different pattern of antibody staining by direct immunofluorescence.

3. Cicatricial or mucous membrane pemphigoid. This is a rare disease caused by various antibodies that target the basement membrane of mucous membranes and occasionally the skin. The oral mucosa is almost always involved, most commonly the gingiva. In contrast to pemphigus vulgaris, the variably sized bullae are not flaccid, and ruptured bullae heal with scarring. Microscopically, there is clefting between the epithelium and the basement membrane, and the space may be filled with serous fluid containing sparse inflammatory cells. Direct immunofluorescence shows a linear band of IgG and C3 on the
basement membrane. Treatment is with immunosuppression, but the disease is often progressive despite therapy.

1. Fungal. Candida species cause most of the fungal infections of the oral cavity. Other fungal infections that occur less frequently in the oral cavity include histoplasmosis, blastomycosis, and coccidiomycosis. Candida species are a part of the normal oral flora; candidiasis occurs due to overgrowth, usually in the setting of a predisposing factor, and Candida albicans is the most frequently isolated species. Local and systemic factors that favor overgrowth include immunosuppression, use of steroids or antibiotics, radiation therapy, xerostomia, use of dentures, and anemia. The extremes of age are more often affected as well, and infection may be acute or chronic. Symptoms include a burning sensation or foul odor, although the infection may be asymptomatic.

Several clinical patterns of oral candidiasis are seen. White plaques that are easily scraped off underlying erythematous mucosa are called pseudomembranous candidiasis (oral thrush). This is the most common type of oral candidiasis. Erythematous candidiasis appears as a red patch due to atrophy of the mucosa. Median rhomboid glossitis is a type of erythematous candidiasis that occurs in a specific location, namely a rhomboid-shaped area on the midline dorsal tongue, which over time may develop a nodular appearance. Angular cheilitis causes red fissuring and scaling at the labial commissures; predisposing factors include drooling and ill-fitting dentures. Chronic hyperplastic candidiasis presents as asymptomatic, white patches (due to the thickened, hyperplastic mucosa) that cannot be removed by scraping. This pattern is more common in immunocompetent individuals and may predispose to the development of carcinoma, although a causal relationship between the two has not been clearly demonstrated.

Microscopically, an intraepithelial infiltrate of neutrophils is seen in all types of candidal infection. The epithelium may be ulcerated, although in chronic hyperplastic candidiasis it is thickened and hyperkeratotic (e-Fig. 1.4). Fungal pseudohyphae may be difficult to identify on routine H&E-stained slides. However, methenamine silver or periodic acid-Schiff (PAS) stains will highlight the fungal elements within the keratin and in the superficial squamous epithelium (e-Fig. 1.4, inset A).

2. Viral. Oral viral infections are highly prevalent, although frequently asymptomatic.

3. Bacterial. Cervicofacial actinomycosis (“lumpy jaw”). Actinomyces are gram positive, saprophytic anaerobes that are part of the normal oral flora. The organisms are often incidentally found in sections of the tonsillar crypts. Occasionally, they are introduced into the soft tissues through trauma, particularly from dental manipulations, where an acute or chronic infection may ensue. Actinomyces israeli is the most common pathogenic species.

Acute infections are suppurative, creating a nontender fluctuant mass. In the chronic phase, infections may form a more extensive firm fibrous mass mimicking a neoplasm. Sinus tracts may exit either the skin or mucosa (e-Fig. 1.9) and often discharge yellow clusters of tightly adherent Actinomyces bacteria that have the appearance of sulfur granules. Osteomyelitis may develop in adjacent bone. Microscopically, collections of radiating, filamentous organisms are seen in a background of neutrophils with surrounding granulation tissue and/or fibrosis. Cultures are often negative due to overgrowth of other organisms. Treatment with prolonged antibiotics is usually successful, although incision and drainage may be necessary.

1. Fibrous lesions. A number of different types of fibrous lesions occur in and around the oral cavity.

2. Inflammatory papillary hyperplasia is a denture-associated lesion and is typically located beneath a denture base in the hard palate and alveolar ridges. Occasionally, it is seen in patients without dentures and may be associated with poor oral hygiene.

Clinically, the mucosa looks “pebbly” with numerous, small, papular projections. Microscopically, the mucosa may be atrophic or demonstrate pseudoepitheliomatous hyperplasia. The underlying submucosa may vary from edematous to fibrotic, with mild chronic inflammation. Individual nodules may resemble an irritation fibroma or pyogenic granuloma. The condition is not premalignant, may subside with less denture wear, or may require surgical excision.

3. Torus palatinus, torus mandibularis, and buccal exostosis are common developmental anomalies that continue to grow throughout life and typically present in adulthood. They are site-specific. Torus palatinus occurs in the midline of the hard palate, torus mandibularis occurs on the lingual surface of the mandible near the bicuspid teeth, and buccal exostosis is found on the facial surface of the alveolar bone. Any identical appearing bony proliferations at other oral sites are generically termed “bony exostosis” or “osteoma” and are not developmental, but rather trauma-related or true neoplasms that can be associated with Gardner syndrome.

Grossly, these lesions are broad-based, single, or lobulated masses with smooth surfaces (e-Fig. 1.13). Microscopically, they are composed of dense lamellar bone with scattered osteocytes and variable amounts of marrow. Ischemic changes with marrow fibrosis and loss of osteocytes from lacunae may be seen. Resection is not necessary except for cosmetic reasons or if the lesions become large. There is little risk of recurrence, and the lesions have no malignant potential.

4. Fordyce granules. Sebaceous glands are normally found in the skin associated with hair follicles. When they are ectopically present in the oral mucosa, they are called Fordyce granules. They are common (present in up to 80% of adults) and can occur on any oral mucosal surface, although the buccal mucosa is most common. Most appear as scattered, 1 to 3 mm, white to yellow papules. Microscopically, normal sebaceous glands are present in the submucosa without associated hair follicles; occasionally, Fordyce granules coalesce to form the larger cauliflower-like lesion termed sebaceous hyperplasia. No treatment is necessary unless for cosmetic reasons (biopsies are rarely performed as the diagnosis is usually clinically apparent).

5. Cysts. Included here are several of the more common soft tissue true cysts that have an epithelial lining. Odontogenic cysts, bone cysts, and salivary
gland-derived pseudocysts (lacking a true epithelial lining) are discussed in Chapter 4.

6. Pseudoepitheliomatous hyperplasia is a generic term for benign, downward proliferation of the epithelium that is important to distinguish from invasive, well-differentiated SCC. Pseudoepitheliomatous hyperplasia is characteristically seen in association with specific lesions including inflammatory papillary hyperplasia, submucosal granular cell tumors, and fungal infections. It can also be seen adjacent to ulcers or be seen associated with myriad other lesions. Microscopically, irregular and pseudoinfiltrative nests of keratinizing squamous epithelium are sometimes seen beneath a markedly thickened surface epithelium. The papillae of the squamous epithelium may be markedly elongated and extend deeply into the submucosa (e-Fig. 1.14). However, in contrast to squamous dysplasia and carcinoma, cytologic atypia is absent.