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Variasi Normal Rongga Mulut

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N o r m a l Var i a t i o n s o f O r a l

Anatomy and Common Oral


Soft Tissue Lesions
Evaluation and Management

a b,
Farideh M. Madani, DMD , Arthur S. Kuperstein, DDS *

KEYWORDS
 Leukoedema  Fordyce granules  Linea alba  White sponge nevus  Ankylogossia
 Lingual thyroid  Hairy tongue  Fissured tongue

KEY POINTS
 Physicians should be able to recognize normal variations of oral and oropharyngeal anatomy.
 Physicians should be able to recognize common soft tissue lesions of the oral and oropha-
ryngeal structures.
 Physicians should be able to determine if referral to an oral health care provider for further
evaluation and management is warranted based on physical examination findings.

BUCCAL AND LABIAL MUCOSA


Cheek Biting (Morsicatio Buccarum)
Habitual, repetitive, parafunctional masticatory activity against the delicate nonkerati-
nized buccal mucosal tissue may result in a whitish, ragged surface and irregularly
textured area of varying size known as morsicatio buccarum (chronic cheek biting).1–4
These areas are found unilaterally or bilaterally, in the vicinity of and lateral to the
occlusal surfaces of the dentition. Histologic appearance is consistent with
hyperkeratosis.

Management
Typically, there is no treatment other than reassurance, but use of an occlusal guard
may be indicated to protect the buccal mucosa from chronic trauma (Fig. 1).5–7

Disclosures: No disclosures to be made.


a
Department of Oral Medicine, University of Pennsylvania School of Dental Medicine, 240
South 40th Street, Philadelphia, PA 19104, USA; b Oral Medicine Clinical Services, Department
of Oral Medicine, University of Pennsylvania School of Dental Medicine, 240 South 40th Street,
Philadelphia, PA 19104, USA
* Corresponding author.
E-mail address: arthurk@dental.upenn.edu

Med Clin N Am - (2014) -–-


http://dx.doi.org/10.1016/j.mcna.2014.08.004 medical.theclinics.com
0025-7125/14/$ – see front matter Ó 2014 Elsevier Inc. All rights reserved.
2 Madani & Kuperstein

Fig. 1. Chronic cheek biting has resulted in this diffuse right buccal mucosal lesion. (Courtesy
of A. Kuperstein, DDS, Philadelphia, PA.)

Leukoedema
Leukoedema is a common benign mucosal alteration of unknown cause that is
considered to be a normal variation. It is usually discovered as an incidental finding
during routine oral examination. In the United States it is present in about 70% to
90% of African-American adults and 50% of African-American children. It is observed
less frequently in whites, and overall is commonly seen in males.8–10
Leukoedema is characterized by accumulation of the fluid within the epithelial cells of
the buccal mucosa. Leukoedema usually start to appear around age 2 to 5; however,
it is not often noticeable until adulthood.11 Clinically leukoedema presents as an asymp-
tomatic, grayish white semitransparent mucosal alteration, located in the buccal
mucosa bilaterally. Occasionally, folds or white lines crisscross the affected area.
The buccal mucosa is the most common site for leukoedema; however, it can
extend to the labial mucosa, floor of the mouth, and pharyngeal areas. Other mucosal
surfaces can be affected, such as vagina and larynx. Leukoedema cannot be wiped
off; however, it can be eliminated temporarily by stretching of the mucosa, which is
referred to as clinical stretch test.12–17 Differential diagnoses of leukoedema include
white sponge nevus, smoker’s tobacco, frictional keratosis, candidiasis, lichen pla-
nus, and hereditary benign intraepithelial dyskeratosis. Leukoedema can be easily
diagnosed clinically by not being temporarily eliminated.

Management
Leukoedema is considered to be a normal variation; therefore, no treatment is required
for this condition. There is no relationship between leukoedema and dysplasia and
malignancy (Fig. 2).18
Oral Anatomy and Common Oral Soft Tissue Lesions 3

Fig. 2. A classic manifestation of leukoedema of the left buccal mucosa. Stretching the
mucosa causes the grayish coloring to temporarily disappear. (Courtesy of F. Madani, DMD,
Philadelphia, PA.)

Fordyce Granules
Fordyce first described these ectopic sebaceous glands or sebaceous choristomas
(normal tissue in abnormal location) within the oral mucosa in 1896.19 Normally,
sebaceous glands are seen within the skin, in association with hair follicles; however,
Fordyce granules do not exhibit any association with hair structures in the oral cavity.
The condition is considered to be a variation of normal and is seen in approximately
80% to 90% of the adult population. Clinically, they present as multiple asymptom-
atic, slightly elevated, yellowish or yellowish white maculopapular structures that
measure 1 to 2 mm in diameter. The lesions generally are symmetrically distributed
and the sites of predilection include the buccal mucosa and the vermilion of the
upper lip. They tend to become obvious after puberty, possibly because of hormonal
changes and the number usually increases with age. Fordyce granules are asymp-
tomatic and are often discovered incidentally by the patient or by the practitioner
during a routine oral examination. Fordyce granules are neither related to smoking
nor systemic atherosclerosis, and there is no race or gender predilection for these
lesions.20–22

Management
No treatment is indicated for this particular condition and because the clinical
appearance is virtually diagnostic, no biopsy is usually required. Fordyce granules
on the vermilion border of the upper lip may require surgical removal for esthetic rea-
sons. Rare cases of pseudocysts and sebaceous cell hyperplasia and adenoma have
been reported.23 Differential diagnosis of Fordyce granules includes pseudomembra-
nous candidiasis. However, these conditions can be differentiated easily because
Fordyce granules do not wipe off, whereas plaques associated with pseudomembra-
nous candidiasis can be easily removed (Fig. 3).
4 Madani & Kuperstein

Fig. 3. The patient’s right buccal mucosa is covered by a diffuse collection of Fordyce gran-
ules. (Courtesy of F. Madani, DMD, Philadelphia, PA.)

Linea Alba
Linea alba is a white, linear elevation of buccal mucosa at the level of occlusal plane
of the teeth. It usually extends from the angle of the mouth toward the pterygomandib-
ular raphe and terminates at the most posterior teeth that are in occlusion. The hyper-
keratotic area is associated with repetitive pressure, frictional trauma, or other
parafunctional habits from buccal surfaces of the dentition. The clinical appearance
is typically diagnostic.
Management
No treatment is required for linea alba, which may disappear if the offending source of
friction is mitigated (Fig. 4).7

Traumatic Ulcer
A solitary ulcer of the mucosa may be the direct result of a physical, mechanical,
chemical, or thermal injury. It is not uncommon for patients to inadvertently bite their
lips or buccal mucosa while eating or after a dental visit if local anesthesia was

Fig. 4. Located along the occlusal line of the patient’s left maxilla and mandible is the linear
white line (arrow) of linea alba. (Courtesy of A. Kuperstein, DDS, Philadelphia, PA.)
Oral Anatomy and Common Oral Soft Tissue Lesions 5

administered. A traumatic ulcer may be caused by repetitive biting, secondary to or-


thodontic or other oral appliances, or malpositioned or irregularly contoured or frac-
tured teeth. A traumatic ulcer of the palate is commonly caused by thermal injury
from eating or drinking extremely hot foods or beverages. Unintentional application
of caustic medicaments and/or chemicals during dental treatment or inappropriate
topical use of aspirin, by the patient, may cause a burn. However, nonresolving
mucosal ulcerations may imply underlying infection, systemic disease, immunocom-
promised status, or even a neoplasm.24–26
Management
Typically, palliative care is sufficient for management of a traumatic ulcer. If the ulcer
is refractory to palliative care and is present for greater than 2 weeks, further investi-
gation including biopsy is warranted (Fig. 5).

TONGUE
Ankyloglossia
Ankyloglossia, or “tongue-tie,” is a developmental anomaly characterized by an
abnormally short and anteriorly positioned lingual frenum that results in restricted
tongue movement. Ankyloglossia can range in severity from mild cases with little clin-
ical significance (common) to complete ankyloglossia, in which the tongue is anatom-
ically attached to the floor of the mouth. Complete ankyloglossia is rare and occurs in
two to three cases of every 10,000 births.27
Complications associated with complete ankyloglossia may include eating prob-
lems (particularly during infancy, such as breastfeeding or sucking problems), peri-
odontal problems caused by high mucogingival attachment of the lingual frenum,
speech defects, and mandibular midline diastema.
Management
Treatment ranges from no treatment to lingual frenectomy, if it causes functional or
periodontal problems (Fig. 6).28–36

Fig. 5. A large, deep traumatic ulcer of the left buccal mucosa (arrow), secondary to chronic
repetitive mechanical trauma from fractured sharp teeth. (Courtesy of A. Kuperstein, DDS,
Philadelphia, PA.)
6 Madani & Kuperstein

Fig. 6. Ankyloglossia. Note the stretched shortened lingual frenum (arrow) as the tongue is
retracted posteriorly. (Courtesy of A. Kuperstein, DDS, Philadelphia, PA.)

Lingual Thyroid
Lingual thyroid tissue is a rare anomaly characterized by the development of a submu-
cosal mass of thyroid tissue on the midposterior dorsum of the tongue. Embryologi-
cally, the thyroid gland anlage arises at the site of foramen cecum and migrates
inferiorly along the thyroglossal tract to its ultimate destination in the anterior neck.
If all or part of the thyroid anlage fails to migrate, remnants of thyroid tissue can
develop along its path of migration. A lingual thyroid nodule represents a thyroid
remnant in the region of the thyroid gland’s origin. Of all ectopic thyroids, 90% are
found in this region.11 Microscopic examination of human tongues removed at
autopsy reveals that despite the absence of a clinically apparent thyroid nodule, as
many as 10% exhibited remnants of thyroid tissue within the tongue.37,38 Lingual
thyroid occurs more commonly among females and may range from a small asymp-
tomatic nodule to a large mass that can obstruct the airway. The most common clinical
symptoms are dysphagia, dysphonia, and dyspnea.
Hypothyroidism has been reported in up to 33% of patients with lingual thyroid,
possibly as a secondary phenomenon to compensate for thyroid hypofunction, and
as many as 75% of patients with infantile hypothyroidism have some ectopic thyroid
tissue.39–43
The clinical appearance is variable. Diagnosis is best established by thyroid scan
using iodine isotope or technetium 99m.44 Computed tomography and magnetic reso-
nance imaging can be helpful in delineating the size and the extent of the lesion.45,46
Biopsy is often avoided because of risk of hemorrhage due to the vascular nature of
these lesions and because the mass may represent the patient’s only functioning
thyroid tissue. However, in some cases, incisional biopsy might be indicated to
confirm the diagnosis and to rule out malignant changes.

Management
No treatment except for periodic follow-up is required for asymptomatic lingual
thyroid. In symptomatic patients the use of suppressive hormonal therapy with levo-
thyroxine47 may reduce the size of the lesion. If hormone therapy does not eliminate
symptoms, surgical removal or ablation with radioactive iodine-131 can be performed.
If the mass is surgically excised, autotransplantation to another body site can be
Oral Anatomy and Common Oral Soft Tissue Lesions 7

attempted to maintain functional thyroid tissue and to prevent hypothyroidism. Rare


examples of carcinoma arising from lingual thyroid have been reported (Fig. 7).5
Hairy Tongue
Hairy tongue is a consequence of the elongation of the filiform papillae on the dorsum
of the tongue resulting in hairlike appearance. It is related to marked accumulation of
keratin on the filiform papillae caused by increase in keratin production or decrease in
normal keratin desquamation. The elongated papillae are generally confined to the
posterior third of the dorsal tongue, but may include the middle third in lesser
amounts. The color ranges from white to yellow, brown, and black as a result of over-
growth of pigment-producing bacteria or staining from food or tobacco. The cause of
hairy tongue is unknown in most of cases; however, most patients are heavy smokers.
Other predisposing factors for this condition include neglected oral hygiene, dryness
of the oral cavity, antibiotics, immunosuppressive drugs, systemic diseases, radiation
treatment, excess use of mouthwashes containing peroxidase, and candidiasis.48
The condition is typically asymptomatic, although patients may complain of a gagging
sensation or bad taste.49–52 Diagnosis is made by clinical appearance and biopsy is
unnecessary. Hairy tongue is found in about 0.5% of adults.53
Management
Treatment of hairy tongue is focused on reduction or elimination of predisposing
factors and excellent oral hygiene should be encouraged. Desquamation of the hyper-
keratotic papillae can be promoted by periodic (gentle) scraping or brushing with a
toothbrush or tongue scraper. This condition is often mistakenly diagnosed as oral
candidiasis, and patients are often prescribed antifungal agents unnecessarily. If the
clinician suspects a diagnosis of oral candidiasis, further investigations should be
conducted (ie, exfoliative cytology) to rule this out as a cause for the patient’s condi-
tion (Fig. 8).
Fissured Tongue
Fissured tongue is relatively common and affects 2% to 5% of the overall population.54
It is characterized by deep grooves and fissures on the dorsal surface of the tongue.
It can be seen in children and adults; however, severity and prevalence increases with
age. There is a strong association between fissured tongue and geographic tongue,

Fig. 7. Lingual thyroid presenting as a large mass behind the tongue or area near the fora-
men cecum (arrow). Patient complained of constant dysphagia. (Courtesy of A. Kuperstein,
DDS, Philadelphia, PA.)
8 Madani & Kuperstein

Fig. 8. Black hairy tongue is represented in this photograph. Patient is a smoker with poor
oral hygiene. (Courtesy of Dr A. Houston, Philadelphia, PA.)

and most individuals have both of these conditions at the same time.55 The cause of
fissured tongue is uncertain but heredity seems to play an important role.56 Aging and
local environmental factors may contribute to its development. Fissured tongue is usu-
ally asymptomatic, although some patients may complain of burning sensation or mild
soreness, particularly after eating hot or spicy foods. Fissured tongue has been seen
more in individuals with Down syndrome than the general population.57 Fissured
tongue is a component of Melkerson-Rosenthal syndrome, characterized by the
classic triad of facial palsy, facial swelling, and fissured tongue.56,58–60 Fissured
tongue is a benign condition and no specific treatment is indicated. Patients should
be encouraged to brush the tongue, because food or debris entrapped in the grooves
may act as a source of irritation. If the patient is symptomatic, clinicians may consider
use of topical anesthetics for palliative treatment. There is a report of fissured tongue
responding to biologics during the treatment of psoriasis (Fig. 9).61

Geographic Tongue (Benign Migratory Glossitis–Erythema Migrans)


Geographic tongue, which is also called benign migratory glossitis or erythema mi-
grans, is a common condition that primarily affects the tongue. This condition is usu-
ally recognized as an incidental finding on routine oral examination. It affects 1% to
3% of the population, and females are affected more commonly than males by a
2:1 ratio.62 The cause of geographic tongue is unknown, yet heredity and environ-
mental factors may play a role in pathogenesis of geographic tongue. There is a strong
association between geographic tongue and fissured tongue.63–66
Geographic tongue is primarily located on the dorsal anterior two-thirds of the
tongue. The lesions appear as well-demarcated red zones secondary to atrophy of
the filiform papillae. The erythematous zones are completely or partially surrounded
by a slightly elevated white serpentine or scalloped border. The peripheral zone dis-
appears after some time, and healing of the erythematous area begins. The lesions
can appear on the lateral or ventral surface of the tongue; however, in most patients,
it is accompanied by similar lesions on the dorsal surface of the tongue. This condition
can also affect other oral mucosal surfaces, such as labial mucosa, buccal mucosa,
soft palate, and gingiva.

Management
Geographic tongue is usually asymptomatic and no treatment is required; however,
some patients may complain of a burning sensation or sensitivity to hot or spicy foods.
Oral Anatomy and Common Oral Soft Tissue Lesions 9

Fig. 9. Fissured tongue of the dorsal surface. Tongue also presents with an associated
benign migratory glossitis distributed over the dorsal surface (selectively indicated by
arrows). (Courtesy of T. Musbah, BDS, Philadelphia, PA.)

In those patients, topical steroids and/or anesthetic may be beneficial in some cases.
Patients should be assured of the benign nature of their condition (Fig. 10).54,65,67,68
Lateral Lingual Tonsil
Lateral lingual tonsil is an aggregate of lymphoid tissue that is located at the posterior
lateral portion of the tongue, related to foliate papillae. Coloration of the nontender
submucosal masses is often red-yellow. They usually are bilateral, generally asymp-
tomatic, and discovered on routine oral examination.11
Management
Typically they require no treatment except for reassurance of the patient. However,
asymmetrical presentation may be suggestive of lymphoma and further evaluation
and management, including biopsy, may be warranted (Fig. 11).69–72
Oral Varicosities (Varices)
Oral varicosities or varices are abnormally dilated or tortuous veins, with an unknown
cause. This condition is rare among children so it is thought to represent a physical
manifestation of the aging process. Lingual varicosities appear as tortuous, blue,
red, and purple elevations that course over the ventrolateral surface of the tongue.
They represent a degenerative change in the adventitia of the venous wall and are
10 Madani & Kuperstein

Fig. 10. Benign migratory glossitis distributed on the ventral and lateral borders of the
tongue. Note the circumferential white borders surrounding the atrophic central regions.
(Courtesy of A. Kuperstein, DDS, Philadelphia, PA.)

of no clinical consequence.68,73–75 They are painless and are not thought to be subject
to rupture and/or hemorrhage.76
A focal dilatation of a vein or group of venules is known as varix. These lesions also
tend to occur in elderly persons and are primarily located on the lower lip, appearing as
a focal raised blue, red, or purple nodule.
Management
These conditions do not require any treatment unless they become calcified or create
an esthetic problem Fig. 12.

Crenation of Lateral Tongue


Crenations or scalloping of the lateral border, and occasionally the tip of the tongue, is
a common finding. It may be associated with stress-related chronic pressure exerted

Fig. 11. Lateral lingual tonsil tissue (arrow) located at the right posterior tongue. (Courtesy
of F. Madani, DMD, Philadelphia, PA.)
Oral Anatomy and Common Oral Soft Tissue Lesions 11

Fig. 12. Bilateral lingual varicosities along the ventral tongue (large arrows). Labial varix of
lower lip at the left commissure (small arrow). (Courtesy of A. Kuperstein, DDS, Philadel-
phia, PA.)

by the tongue musculature against the curved lingual surfaces of the dentition, impart-
ing the scalloped margin. Occasionally, it may be associated with systemic disease,
such as macroglossia associated with acromegaly. There have been some indications
of association with obstructive sleep apnea.77–79

Management
Typically no treatment is necessary (Fig. 13).

GINGIVA
Amalgam Tattoo
An amalgam tattoo represents an exogenous pigmentation, which may be identified
on the buccal mucosa, gingiva, ventral tongue, floor of mouth, or hard palate. The
color may vary from a light gray to a dark blue-black hue. The cause is inadvertent
embedding or migration of amalgam restorative material into the mucosa. Over time
the foreign material may disperse into surrounding tissue, which may lighten the area’s
color. Amalgam tattoo must be differentiated from other pigmented lesions including
malignant melanoma.79–81

Management
No treatment is required for suspected amalgam tattoos. However, if there is clinical
suspicion for other etiologies of the pigmented lesion, referral to a dentist for further
evaluation and management is recommended (Fig. 14).

Physiologic Pigmentation
The oral mucosa may present with variations in physiologic pigmentation. Association
with varying skin color seems to be variably related with oral physiologic pigmentation.
The spectrum of pigmentation, from light to a darker brown, typically presents on the
labial gingiva, but also may be observed on the dorsum of the tongue, the gingival
surfaces, lips and palate, and buccal mucosa.
12 Madani & Kuperstein

Fig. 13. Crenations, scalloping of the lateral borders and tip of the tongue (arrows).
(Courtesy of A. Kuperstein, DDS, Philadelphia, PA.)

Fig. 14. Amalgam tattoo (arrow) located buccal to the maxillary alveolar ridge at the site
of a previously extracted and amalgam restored molar. (Courtesy of A. Kuperstein, DDS,
Philadelphia, PA.)
Oral Anatomy and Common Oral Soft Tissue Lesions 13

Management
Physiologic pigmentation is often observed in infancy, young children, and adolescence
with pubertal darkening. If adult onset is noted, a biopsy may be indicated, because
the presentation may represent underlying systemic disease, neoplasm, trauma, and/
or reactive pigmentation. Endocrinopathies, such as Addison disease, may present
with oral mucosal pigmentation.82 The clinical presentation of endocrinopathy-
associated pigmentation in the oral cavity is usually a diffuse but dappled melanosis
of multiple mucosal surfaces. A medical work-up including biopsy, serum cortisol,
and electrolyte levels should be performed if endocrinopathy-associated pigmentation
is suspected (Fig. 15).83,84

PALATE, ALVEOLAR PROCESS


Tori, Exostoses
These osseous structures have a relatively high frequency of presentation and the
manner in which they impact the overlying oral mucosa. Tori are nonneoplastic,
exophytic, often nodular, dense cortical bony structures that may be located in the
midline of the hard palate (torus palatinus), typically bilaterally along the lingual
cortical plate of the mandible (torus mandibularis), and beneath the buccal and labial
alveolar mucosa (exostoses). Typically thin oral mucosa overlies the underlying bony
mass giving the mucosa a pale yellow-white coloration, when actually its translu-
cency permits the bone color to be visualized through it. Nevertheless, the practi-
tioner should be cognizant of the potential for the bony expansion associated with
dentoalveolar infection, Paget disease, or the fibro-osseous lesions of fibrous
dysplasia.

Management
Typically no treatment is indicated unless there is persistent trauma to the overlying
mucosa or dental prosthetic are indicated. In cases in which dental prostheses are
indicated, the exophytic osseous growths may need to be excised or recontoured
to accommodate the restoration (Figs. 16–18).68,85,86

Fig. 15. Physiologic melanotic pigmentation of the maxillary and to a lesser degree, mandib-
ular labial gingiva. (Courtesy of A. Kuperstein, DDS, Philadelphia, PA.)
14 Madani & Kuperstein

Fig. 16. Torus palatinus. Note two-lobed structure of the bony mass (arrow). The translu-
cency of the mucosa can be readily observed. (Courtesy of F. Madani, DMD, Philadelphia,
PA; and A. Kuperstein, DDS, Philadelphia, PA.)

Fig. 17. Bilateral torus mandibularis (small arrows) and buccal exostoses (large arrows). The
translucency of the mucosa can be observed. (Courtesy of T. Musbah, BDS, Philadelphia, PA.)

Fig. 18. Torus mandibularis. Typical bilateral presentation of the bony exophytic mass
(arrows). The translucency of the mucosa can be observed as on the palatal lesion. (Courtesy
of J. Thoppay, BDS, Philadelphia, PA.)
Oral Anatomy and Common Oral Soft Tissue Lesions 15

SUMMARY

This article highlights the importance of recognizing common variations of normal oral
anatomy and clinical findings that may suggest association with systemic, psycholog-
ical, and behavioral health conditions. Physicians should have an understanding of
these findings to provide appropriate patient care.

REFERENCES

1. Vargas CM, Arevalo O. How dental care can preserve and improve oral health.
Dent Clin North Am 2009;53(3):399–420.
2. Lankarani KB, Sivandzadeh GR, Hassanpour S. Oral manifestation in inflamma-
tory bowel disease: a review. World J Gastroenterol 2013;19(46):8571–9.
3. Padovani MC, Barbosa PS, Baeder F, et al. Oral manifestations of systemic
alterations in early childhood. J Contemp Dent Pract 2013;14(2):327–31.
4. Islam NM, Bhattacharyya I, Cohen DM. Common oral manifestations of systemic
disease. Otolaryngologic Clinics of North America 2011;44(1):161–82.
5. Greenberg MS, Ship JA, Glick M. Burket’s oral medicine. 11th edition. Hamilton
(Canada): BC Decker; 2011.
6. Woo SB, Lin D. Morsicatio mucosae oris: a chronic oral frictional keratosis, not a
leukoplakia. J Oral Maxillofac Surg 2009;67(1):140–6.
7. Neville BW, Damm DD, Allen CM, et al. Physical and chemical injuries. In: Oral
and maxillofacial pathology. 3rd edition. St Louis (MO): WB Saunders; 2009.
8. Martin JL, Crump EP. Leukoedema of the buccal mucosa in children and youth.
Oral Surg Oral Med Oral Pathol 1972;34(1):49–58.
9. Axéll T, Henricsson V. Leukoedema: an epidemiologic study with special refer-
ence to the influence of tobacco habits. Community Dent Oral Epidemiol
1981;9(3):142–6.
10. Martin JL. Leukoedema: an epidemiological study in white and African American.
J Tenn Dent Assoc 1997;77:18–21.
11. Bouquot BW, Neville DD, Damm CM, et al. Oral & maxillofacial pathology.
2nd edition. Philadelphia: WB Saunders; 2002.
12. Sandstead HR, Lowe JW. Leukoedema and keratosis in relation to leukoplakia of
the buccal mucosa in man. J Natl Cancer Inst 1953;14(2):423–37.
13. Durocher RT, Thalman R, Fiore-Donno G. Leukoedema of the oral mucosa. J Am
Dent Assoc 1972;85(5):1105–9.
14. Bánóczy J. Oral leukoplakia and other white lesions of the oral mucosa related
to dermatological disorders. J Cutan Pathol 1983;10(4):238–56.
15. Martin JL. Nutrition: a non-factor in leukoedema. Ann Dent 1977;36(1):24–8.
16. Waitzer S, Fisher BK. Oral leukoedema. Arch Dermatol 1984;120(2):264–6.
17. Van Wyk CW, Ambrosio SC, van der Vyver PC. Abnormal keratohyalin-like forms
in leukoedema. J Oral Pathol 1984;13(3):271–81.
18. Scully C. Oral and maxillofacial medicine: the basis of diagnosis and treatment.
Edinburgh (United Kingdom): Churchill Livingstone; 2013. p. 388.
19. Fordyce J. A peculiar affection of the mucous membrane of the lip and oral cavity.
J Cutan Genito-Urin Dis 1896;14:413–9.
20. Miles AE. Sebaceous glands in the lip and cheek mucosa of man. Br Dent J
1958;105:235–9.
21. Miller AS, McCrea MW. Sebaceous gland adenoma of the buccal mucosa.
J Oral Surg 1968;26:593–5.
22. Scully C. Oral and maxillofacial medicine: the basis of diagnosis and treatment,
vol. 170. Edinburgh (United Kingdom): Churchill Livingstone; 2013. p. 392.
16 Madani & Kuperstein

23. Gorsky M, Buchner A, Fondoianu-Dayan D, et al. Fordyce’s granules in the oral


mucosa of adult Israeli Jews. Community Dent Oral Epidemiol 1986;14:231–2.
24. Compilato D, Cirillo N, Termine N, et al. Long-standing oral ulcers: proposal for a
new ‘S-C-D classification system’. J Oral Pathol Med 2009;38(3):241–53.
25. Bascones-Martı́nez A, Figuero-Ruiz E, Esparza-Gómez GC. Oral ulcers. Med
Clin (Barc) 2005;125(15):590–7 [in Spanish].
26. Hegde ND, Hegde MN, Puri A, et al. Differential diagnosis of long term tongue
ulcers. Int Res J Pharm 2012;3(8):145–8.
27. Messner AH, Lalakea ML. The effect of ankyloglossia on speech in children.
Otolaryngol Head Neck Surg 2002;127(6):539–45.
28. Messner AH, Lalakea ML. Ankyloglossia: controversies in management. Int J
Pediatr Otorhinolaryngol 2000;54:123–31.
29. Lalakea M, Lauren M, Anna H. Frenotomy and frenuloplasty: if, when, and how.
Operative Techniques in Otolaryngol Head Neck Surg 2002;13:93.
30. Wallace H, Clarke S. Tongue-tie division in infants with breast-feeding diffi-
culties. Int J Pediatr Otorhinolaryngol 2006;70(7):1257–61.
31. Ruffoli R, Giambelluca MA, Scavuzzo MC, et al. Ankyloglossia: a morphofunc-
tional investigation in children. Oral Dis 2005;11(3):170–4.
32. Breward S. Tongue tie and breastfeeding: assessing and overcoming the diffi-
culties. Community Pract 2006;79(9):298–9.
33. Lalakea ML, Messner AH. Ankyloglossia: does it matter? Pediatr Clin North Am
2003;50(2):381–97.
34. Yoon PJ. Tongue-tie (ankyloglossia): current diagnosis and treatment: pediat-
rics. 20th edition. New York: McGraw-Hill; 2011. p. 485.
35. Messner AH, Lalakea L, Aby J, et al. Ankyloglossia: incidence and associated
feeding difficulties. Arch Otolaryngol Head Neck Surg 2000;126(1):36–9.
36. Ricke LA, Baker NJ, Madlon-Kay DJ, et al. Newborn tongue-tie, prevalence and
effect on breast-feeding. J Am Board Fam Pract 2005;18(1):1–7.
37. Baik SH, Choi JH, Lee HM. Dual ectopic thyroid. Eur Arch Otorhinolaryngol
2002;259:105–7.
38. Paludetti G, Galli J, Almadori G, et al. Ectopic thyroid gland. Acta Otorhinolar-
yngol Ital 1991;11:117–33.
39. Chanin LR, Greenberg LM. Pediatric upper airway obstruction due to ectopic
thyroid: classification and case reports. Laryngoscope 1988;98:422–7.
40. Hazarika P, Siddiqui SA, Pujary K, et al. Dual ectopic thyroid: a report of two
cases. J Laryngol Otol 1998;12:393–5.
41. Huang TS, Chen HY. Dual thyroid ectopia with a normally located pretracheal
thyroid gland: case report and literature review. Head Neck 2007;29:885–8.
42. Mussak EN, Kacker A. Surgical and medical management of midline ectopic
thyroid. Otolaryngol Head Neck Surg 2007;136:870–2.
43. Alderson DJ, Lannigan FJ. Lingual thyroid presenting after previous thyroglossal
cyst excision. J Laryngol Otol 1994;108:341–3.
44. Willinsky RA, Kassel EE, Cooper PW, et al. Computed tomography of lingual
thyroid. J Comput Assist Tomogr 1987;11(1):182–3.
45. Shah HR, Boyd CM, Williamson M, et al. Lingual thyroid: unusual appearance on
computed tomography. Comput Med Imaging Graph 1988;12(4):263–6.
46. Takashima S, Ueda M, Shibata A, et al. MR imaging of the lingual thyroid.
comparison to other submucosal lesions. Acta Radiol 2001;42(4):376–82.
47. Pinto A, Glick M. Management of patients with thyroid disease: oral health
considerations. J Am Dent Assoc 2002;133(7):849–58.
48. Nally F. Diseases of the tongue. Practitioner 1991;235(1498):65–71.
Oral Anatomy and Common Oral Soft Tissue Lesions 17

49. Redman RS. Prevalence of geographic tongue, fissured tongue, median rhom-
boid glossitis, and hairy tongue among 3,611 Minnesota schoolchildren. Oral
Surg Oral Med Oral Pathol 1970;30(3):390–5.
50. Kostka E, Wittekindt C, Guntinas-Lichius O. Tongue coating, mouth odor, gusta-
tory sense disorder: earlier and new treatment options by means of tongue
scraper. Laryngorhinootologie 2008;87(8):546–50.
51. Lawoyin D, Brown RS. Drug-induced black hairy tongue: diagnosis and man-
agement challenges. Dent Today 2008;27(1):60, 62–3.
52. Pigatto PD, Spadari F, Meroni L, et al. Black hairy tongue associated with
long-term oral erythromycin use. J Eur Acad Dermatol Venereol 2008;22(10):
1269–70.
53. Thompson DF, Kessler TL. Drug-induced black hairy tongue. Pharmacotherapy
2010;30(6):585–93.
54. Reamy BV, Derby R, Bunt CW. Common tongue conditions in primary care. Am
Fam Physician 2010;81(5):627–34.
55. Liu R, Yu S. Melkersson-Rosenthal syndrome: a review of seven patients. J Clin
Neurosci 2013;20(7):993–5.
56. Eidelman E, Chosack A, Cohen T. Scrotal tongue and geographic tongue: poly-
genic and associated traits. Oral Surg Oral Med Oral Pathol 1976;42(5):591–6.
57. Dar-Odeh NS, Hayajneh WA, Abu-Hammad OA, et al. Orofacial findings in
chronic granulomatous disease: report of twelve patients and review of the liter-
ature. BMC Res Notes 2010;3(1):37.
58. Stein SL, Mancini AJ. Melkersson-Rosenthal syndrome in childhood: successful
management with combination steroid and minocycline therapy. J Am Acad
Dermatol 1999;41:746–8.
59. Alioglu Z, Caylan R, Adanir M, et al. Melkersson-Rosenthal syndrome: report of
three cases. Neurol Sci 2000;21(1):57–60.
60. Nakane T, Hatakeyama K, Nakamura K, et al. Melkersson-Rosenthal syndrome
with isolated immunoglobulin E hypogammaglobulinaemia. J Int Med Res 2007;
35(6):922–5.
61. D’Erme AM, Agnoletti AF, Prignano F. Fissured tongue responding to biologics
during the treatment of psoriasis: the importance of detecting oral involvement
of psoriasis. Dermatol Ther 2013;26(4):364–6.
62. Neville BW, Damm DD, Allen CA, et al. Oral & maxillofacial pathology. 2nd
edition. Philadelphia: WB Saunders; 2002. p. 677–9.
63. Greenberg MS, Glick M, Ship JA. Burket’s oral medicine. 11th edition. BC
Decker; 2008. p. 103–4.
64. Scully C. Oral and maxillofacial medicine: the basis of diagnosis and treatment.
2nd edition. Edinburgh: Churchill Livingstone; 2013. p. 205–6.
65. Shulman JD, Carpenter WM. Prevalence and risk factors associated with
geographic tongue among US adults. Oral Dis 2006;12(4):381–6.
66. Zhu JF, Kaminski MJ, Pulitzer DR, et al. Psoriasis: pathophysiology and oral
manifestations. Oral Dis 1996;2(2):135–44.
67. Ching V, Grushka M, Darling M, et al. Increased prevalence of geographic
tongue in burning mouth complaints: a retrospective study. Oral Surg Oral
Med Oral Pathol Oral Radiol 2012;114(4):444–8.
68. Canaan TJ, Meehan SC. Variations of structure and appearance of the oral
mucosa. Dent Clin North Am 2005;49:1–14.
69. Kenna MA, Amin A. Anatomy and physiology of the oral cavity. In: Snow JB,
Wackym PA, editors. Ballenger’s otorhinolaryngology head and neck surgery.
17th edition. Shelton (CT): BC Decker Inc; 2009. p. 769–74.
18 Madani & Kuperstein

70. Wiatrak BJ, Woolley AL. Pharyngitis and adenotonsillar disease. Cummings
otolaryngology head and neck surgery. 3rd edition. London: Mosby; 1998.
p. 188–215.
71. William JL, Lawrence SS, Steven P, et al. Human embryology. 3rd edition.
Philadelphia: Elsevier; 2001. p. 375–6.
72. Robb PJ. The adenoid and adenoidectomy. Gleeson’s otorhinolaryngology,
head and neck surgery. 7th edition. London: Hodder Arnold; 2008. p. 1094–101.
73. Neville BW, Damm DD, Allen CM, et al. Oral & maxillofacial pathology. Philadelphia:
Saunders; 2002. p. 337–69.
74. Kleinman HZ. Lingual varicosities. Oral Surg Oral Med Oral Pathol 1967;23:546–8.
75. Colby RA, Kerr DA, Robson HB. Color atlas of oral pathology. 2nd edition.
Philadelphia: JBLippincott Company; 1961. p. 125.
76. Viswanath V, Nair S, Chavan N, et al. Caviar tongue. Indian J Dermatol Venereol
Leprol 2011;77(1):78–9.
77. Zonato AI, Martinho FL, Bittencourt LR, et al. Head and neck physical examina-
tion: comparison between nonapneic and obstructive sleep apnea patients.
Laryngoscope 2005;115(6):1030–4.
78. Patel M. Amyloidosis, not to be taken lightly. Society of Hospital Medicine
[abstracts]. J Hosp Med 2012;7:1.
79. Al-Mobeeriek A. Oral health status among psychiatric patients in Riyadh, Saudi
Arabia. West Indian Med J 2012;61(5):549–54.
80. Tran HT, Anandasabapathy N, Soldano AC. Amalgam tattoo. Dermatol Online J
2008;14:19.
81. Lewandowski B, Niedziela W. Amalgam staining of the oral mucosa as a simu-
lation of melanoma. Family Medicine and Primary Care Review 2010;12(4):
1095–8.
82. Eisen D. Disorders of pigmentation in the oral cavity. Clin Dermatol 2000;18(5):
579–87.
83. Alawi F. Pigmented lesions of the oral cavity: an update. Dent Clin North Am
2013;57:699–710.
84. Lawson W. Pigmented oral lesions: Clues to identifying the potentially malignant.
Consultant 2012;52(5):347–52.
85. Antoniades DZ, Belazi M, Papanayiotou P. Concurrence of torus palatinus with
palatal and buccal exostoses: case report and review of the literature. Oral
Surg Oral Med Oral Pathol Oral Radiol Endod 1998;8(5):552–7.
86. Sawair FA, Shayyab MH, Al-Rabab’ah MA, et al. Prevalence and clinical charac-
teristics of tori and jaw exostoses in a teaching hospital in Jordan. Saudi Med J
2009;30(12):1557–62.

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