Regezi Oral Pathology 2 Midterm Reviewer PDF

Summary

This document is a reviewer for a midterm exam in oral pathology. It covers the diagnosis process, patient engagement with health care system, and viral diseases such as herpes simplex virus (HSV) infections. The information includes chief complaints, differential diagnoses, and treatment considerations.

Full Transcript

ORAL PATHOLOGY 2 5. Working diagnosis = always communicate to
narrow your differential diagnosis until you
 Professor: Dra. Katrina Bianca B. Cruz-Natividad
come up with your working diagnosis
 From San Mateo Morong, Rizal 6. Clinical History and Interview = strengthen
your rapport and bond with your patient
7. Physical exam = hands on observational
DIAGNOSIS PROCESS examination of the patients, observe patient`s
 Tic Douloureux = Trigeminal Neuralgia, severe demeanor
stabbing pain to one side of the face  Gait of patient = inconsistent height
 Diagnosis = process of establishing the nature of measurement, abnormal walking
an abnormality or disease that produces signs 8. Diagnostic Testing = can confirm suspected
and symptoms diagnosis
 Correct diagnosis the first step to successful  When in doubt you can always ask for second
treatment opinion
9. Referral and Consultation = refer or consult to
The Diagnostic Process a specialist
1. Patient Experiences a Health Problem = patient  Obturator is used to a patient with cleft palate
only come for check up when in pain or there is 10. Communication of Diagnosis = execution of
inflammation treatment plan, have a signed consent form
 Always cater the right treatment plan 11. Treatment = schedule, rate of treatment
 Our diagnosis starts on patient chief complaint  Always treat first the chief complaint
 Chief complaint = reason why the patient is 12. Outcome = feedback of patient satisfaction
seeking medical attention
 Patient own words
 Deepen your interview and ask why questions VESICULOBULLOUS DISEASE
 Differential diagnosis = occurs when a
pathology have many similar signs and  VIRAL DISEASES:
1) HERPES SIMPLEX VIRUS (HSV)
symptoms
INFECTIONS:
2. Patient Engages with Health care system
Herpes simplex virus (HSVs) infections are common
Influenced by Many Factors:
vesicular eruptions of the skin and mucosa that occur in
 Symptoms two forms—primary (systemic) as the result of initial
 Access infection in a previously uninfected person and
 Cost secondary (localized) as the result of viral reactivation in
 Trust in the System a previously infected individual.
3. Information Gathering = Medical History, family
history,, dental history, social history
 Signs – Objective
 Symptoms – Subjective
 Chief Complaint – History of Present Illness
 When -> How long -> What questions

Diagnostic Instruments : Imaging, CBC, Stool
Sample ETIOLOGY
 Two forms of infection:
4. Information, Integration, Interpretation =
working diagnosis might change. This 3Is o Primary (systemic): Occurs with initial
depend on clinicians medical knowledge infection in a previously uninfected
person.
 o Secondary (localized): Results from o Infection: HSV infection of the
reactivation of the virus in a previously finger(s), either primary or secondary.
infected individual. o Cause: Inoculation through a break in
skin integrity,
PATHOGENESIS o Symptoms: Pain, redness, swelling,
vesicles or pustules that become ulcers,
possible lymphadenopathy. Last 4-6
 Occurs mainly through physical contact with
weeks.
an infected person or exposure to body
fluids.
HISTOPATHOLOGY:
 Symptomatic individuals develop
vesiculoulcerative eruptions (primary
gingivostomatitis) in oral and perioral o Microscopic Findings: Intraepithelial
tissues. vesicles with exudate, inflammatory
 Reactivation can be triggered by sunlight, cells, and virus-infected epithelial cells.
colds, trauma, menstrual cycle, stress, or
immunosuppression. DIFFERENTIAL DIAGNOSIS:

 Types of HSV:  Primary Herpetic Gingivostomatitis:..
o HSV1: Typically affects the orofacial o Differentiation from Other
region. Conditions:
o HSV2: Affects the genital region but  Streptococcal Pharyngitis:
can cause oral lesions through oral- Erythema Multiforme:
genital contact.  Acute Necrotizing Ulcerative
o Previous HSV1 infection may offer Gingivitis (ANUG):
some protection against HSV2 due to o Secondary Herpes vs. Aphthous
antibody cross-reactivity. Stomatitis:
 Herpes
 Aphthous Stomatitis:
CLINICAL FEATURES

 Primary Herpetic Gingivostomatitis: TREATMENT
o Usually occurs in children, exposure. By
age 15, about half of the population is Antiviral Drugs:
infected.
o Vesicular eruptions on skin, vermilion  Acyclovir & Analogs:
border, and oral mucous membranes.  Acyclovir & Penciclovir:
Can appear on any mucosal surface.  Docosanol:
o Accompanying Symptoms: Fever,
arthralgia, malaise, anorexia, headache, Systemic Antiviral Agents:
cervical lymphadenopathy.
o Healing: Lesions heal without scarring  Acyclovir (400 mg, 3x/day) or Valacyclovir
after 7-10 days (1000 mg, 2x/day):
 Secondary (Recurrent) Herpes Simplex o Effective for primary genital herpes.
Infection: o Less effective for primary oral herpetic
o Cause: Reactivation of latent virus, gingivostomatitis.
rarely from exogenous reinfection.  Supportive Therapy: Fluids, rest, oral lavage,
o Tingling, burning, pain at the site of analgesics, and antipyretics are essential
lesion appearance. components.
o Multiple fragile vesicles that quickly  Secondary Herpes: Controlled to some degree
form superficial ulcers, healing without by systemic acyclovir
scarring in 1-2 weeks.
o Location: Most commonly appears on 2) VARICELLA ZOSTER INFECTION
the vermilion border and surrounding
skin (herpes labialis);and hard palate or In seronegative individuals, primary varicella-zoster
gingiva. virus (VZV) infection is known as varicella or chickenpox,
 Herpetic Whitlow: while secondary or reactivated disease is known as
herpes zoster or shingles o Rash progresses to vesicular eruption,
pustular lesions, and eventually ulcers.
o Lesions appear in crops, causing
multiple stages of development at once.
o Oral mucous membranes may show
multiple shallow ulcers.
o Pruritic: Intense itching often leads to
secondary bacterial infections and
potential scarring.
 Complications:
o Rare but can include pneumonitis,
encephalitis, and inflammation of other
organs.
ETIOLOGY
Herpes Zoster (Shingles):
 Varicella-Zoster Virus (VZV):
o Similar in structure to Herpes Simplex  Affected Population: Primarily older adults and
Virus (HSV). immunocompromised individuals.
o Causes two forms of disease:  Symptoms:
 Primary Infection: Known as o Prodromal symptoms of pain/paresthesia
varicella (chickenpox). in the affected dermatome.
 Reactivation: Known as herpes o A unilateral maculopapular rash that
zoster (shingles). becomes vesicular, pustular, and
ulcerative.
PATHOGENESIS o Systemic symptoms may occasionally
accompany the rash.
 Primarily through direct contact via droplets  Complications:
from skin lesions or inhalation of aerosolized o Post-herpetic neuralgia (may be difficult
virus. Highly contagious. to treat).

 Incubation: 2 weeks. HISTOPATHOLOGY
 Reactivation: Can be triggered by
immunosuppression (e.g., malignancies, HIV,  VZV and HSV Morphology: Similar
drug administration), radiation, spinal surgery, histopathological features.
or local trauma.
DIFFERENTIAL DIAGNOSIS
 Disease Progression:
o Vesicular skin eruption → Pustular  Similar Conditions: Primary HSV infection
lesions → Ulceration. and hand-foot-and-mouth (HFM) disease.
o Duration: 2 to 3 weeks.  Herpes Zoster Confusion: Often mistaken for
 Post-Herpetic Neuralgia: recurrent HSV infection.
o Occurs in ~15% of patients, can take  Herpes Zoster Features:
several months to resolve. o Longer duration and more intense
prodromal symptoms.
CLINICAL FEATURES o Unilateral lesion distribution with abrupt
midline ending.
Varicella (Chickenpox): o Presence of post-herpetic neuralgia.

 Vaccine: Attenuated live vaccine developed in TREATMENT
the 1970s by Dr. Michiaki Takahashi.
 Symptoms:  Supportive therapy.
o Fever, chills, malaise, headache.  Require antiviral therapies.
o Rash primarily on the trunk, head, and  Effective Antiviral Drugs: Acyclovir,
neck. vidarabine, interferon.
  Vaccination: Live attenuated vaccine since HISTOPATHOLOGY:
1995; reduced cases, hospitalizations, and
disease burden.  Vesicle enlargement due to destruction of
keratinocytes, filled with proteinaceous debris
Herpes Zoster Treatment: and inflammatory cells.

 Effective Antiviral: Oral acyclovir (800 mg 5 DIFFERENTIAL DIAGNOSIS:
times daily for 7-10 days)
 Pain Management: Analgesics provide limited  Consider primary herpetic gingivostomatitis and
relief; varicella.
 Distinguishing features: mild symptoms,
3) HAND FOOT AND MOUTH DISEASE cutaneous lesions, epidemic spread.

One of the subdivisions of the family of viruses known TREATMENT:
as picornavirus (literally, small “pico” RNA virus) is the
Coxsackie A group  General Approach: Symptomatic treatment
Severe Cases: Monitor for complications like
dehydration and encephalitis,
 Symptom Relief: Bland mouth rinses (e.g.,
sodium bicarbonate in warm water)
 Hospitalization: May be needed if dehydration
occurs.

4) HERPANGINA

Herpangina is an acute viral infection caused by another
Coxsackie type A virus (types A1-6, A8, A10, A22, B3,
ETIOLOGY and possibly others).

 Virus Family: Coxsackie A group, part of
picornavirus family.
 Causing Agents: Primarily Coxsackie type A16
and enterovirus 71; other types include A5, A9,
A10, B2, B5.

PATHOGENESIS
 Direct contact with nasal secretions, saliva,
blister fluid, or fecal-oral contamination.
 Mucous membranes (buccal mucosa, tongue),
hands, feet, and buttocks. ETIOLOGY

CLINICAL FEATURES  Caused by Coxsackie type A viruses (A1-6, A8,
A10, A22, B3, possibly others).
 Primarily affects children under 5 years old.
 Symptoms: Low-grade fever, malaise, PATHOGENESIS
lymphadenopathy, sore mouth.
 Oral Lesions: Begin as vesicles, quickly rupture  Transmission through contaminated saliva and
to form ulcers with a yellow fibrinous membrane occasionally feces.
and erythematous halo; commonly on palate,
tongue, and buccal mucosa. CLINICAL FEATURES:
 Cutaneous Lesions: Multiple maculopapular
lesions on feet, toes, hands, and fingers; progress  Vesicular Enanthem: Rash on mucous
to vesicular state, ulcerate, and encrust without membranes, typically on soft palate, faucial
scarring. pillars, and tonsils.
 Occurrence: Common in children aged 3-10;
  Symptoms: Malaise, fever, dysphagia, sore o Prodromal Symptoms: Fever, malaise,
throat; diffuse erythematous pharyngitis. coryza, conjunctivitis, photophobia,
 Duration: Vesicular eruption persists for 4-6 cough.
days o Koplik’s Spots: Pathognomonic small
erythematous macules with white
DIFFERENTIAL DIAGNOSIS: centers in buccal mucosa; Rash
Progression: Starts on head and neck,
 Herpetic gingivostomatitis, HFM disease, moves to trunk and extremities.
varicella. o Complications: Encephalitis,
 Streptococcal pharyngitis (diffuse pharyngitis). thrombocytopenic purpura, secondary
 Aphthous stomatitis (systemic symptoms). infections like otitis media and
pneumonia.
TREATMENT:
HISTOPATHOLOGY:
 Local measures usually sufficient.
 Infected Epithelial Cells: Necrotic with
 Complications: Rare, so extensive treatment is
typically not required. inflamed connective tissue beneath.

5) MEASLES (RUBELLA) DIFFERENTIAL DIAGNOSIS:

 Key Features: Prodromal symptoms, Koplik’s
Measles is a highly contagious viral infection caused by
spots, and rash.
a member of the genus morbillivirus, a member of the
paramyxovirus family of viruses.
TREATMENT:

 Supportive care including bed rest, fluids,
adequate diet, and analgesics.
 MMR Vaccine: Live attenuated viruses for
measles, mumps, and rubella; effective and safe.

 IMMUNOLOGIC DISEASE

1) PEMPHIGUS VULGARIS
Pemphigus is a group of autoimmune mucocutaneous
diseases characterized by intraepithelial blister
ETIOLOGY formation that results from a breakdown or loss of
intercellular keratinocyte adhesion, thus producing
o Virus: Measles virus, an RNA- epithelial cell separation known as acantholysis of the
enveloped virus from the morbillivirus skin and mucous membranes.
genus, related to mumps and influenza
viruses

PATHOGENESIS

o Spread by airborne droplets through the
respiratory epithelium.
o Rash: Early pinpoint elevations in the
soft palate, coalescing with pharyngeal
involvement and bright erythema;
possible Herman spots (bluish-gray ETIOLOGY
areas on tonsils).
 CLINICAL FEATURES:  Autoimmune mucocutaneous diseases causing
intraepithelial blister formation due to loss of
 intercellular keratinocyte adhesion o Paraneoplastic Pemphigus
(acantholysis). o Aphthous Ulcers
 Consequences: Painful debilitation, fluid loss, o Pemphigus Vegetans (Subset of
electrolyte imbalance, and historically, sepsis Pemphigus Vulgaris):
and death.
TREATMENT
Types of Pemphigus:
 Systemic Corticosteroids: Intermediate-dose
 Pemphigus Vulgaris: Affects suprabasal prednisone is the cornerstone of treatment; high-
epithelium and oral mucosa; potentially involves dose regimen used for severe cases.
skin.  Nonsteroidal Immunosuppressive Agents:
 Pemphigus Foliaceus: Affects the upper prickle Used in combination with corticosteroids; may
cell layer of the skin; does not involve oral include azathioprine, dapsone, mycophenolate,
mucosa. or cyclophosphamide.
 IgA Pemphigus: Less common; characterized  Plasmapheresis
by IgA autoantibodies.  Immunoadsorption
 Pemphigus Vegetans: Rare variant of  Intravenous Immunoglobulin (IVIg)
pemphigus vulgaris.  Biologic Agents (e.g., Rituximab)
 Paraneoplastic Pemphigus: Associated with 2) MUCOUS MEMBRANE PEMPHIGOID
malignancy; involves extensive mucocutaneous
disease patterns and potentially internal organs.
Mucous membrane pemphigoid (MMP) is a chronic
blistering or vesiculobullous disease that affects
PATHOGENESIS: predominantly oral and ocular mucous membranes
 Antibodies disrupt desmosomal junctions,
leading to loss of cell-to-cell adhesion.

CLINICAL FEATURES:

 Lesions: Painful ulcers preceded by flaccid,
short-lived intraoral vesicles and bullae.
 Bullae: Rapidly rupture, leaving painful,
ulcerated bases with friable epithelial borders.
ETIOLOGY
 Ranges from small aphthous-like lesions to
large, irregular map-like lesions.
 Chronic blistering or vesiculobullous disease
 Nikolsky Sign: Gentle traction on unaffected
primarily affecting oral and ocular mucous
mucosa may cause stripping of epithelium.
membranes.
 Discomfort: In soft palate, buccal mucosa, floor
 Known by various names, including cicatricial
of the mouth, and oropharynx.
pemphigoid, benign mucous membrane
 Age: Most common in the fourth and fifth
pemphigoid, ocular pemphigus, childhood
decades of life; can occur from childhood to
pemphigoid, and mucosal pemphigoid.
elderly age.
 Autoimmune disease with unknown stimulus or
etiology.
HISTOPATHOLOGY:
PATHOGENESIS
 Intraepithelial Clefting: Characterized by
keratinocyte acantholysis.
 Antigenic targets include laminin 332 (epiligrin,
laminin 5) and BP180 (bullous pemphigoid
DIFFERENTIAL DIAGNOSIS antigen 180).
 Must be distinguished from other
CLINICAL FEATURES
vesiculobullous diseases:
o Mucous Membrane Pemphigoid
 Primarily affects adults and the elderly, with a
o Erythema Multiforme
higher prevalence in women.
o Erosive Lichen Planus
  Affects Oral mucosa, conjunctiva, nasopharynx, Bullous pemphigoid and its closely related mucosal
larynx, esophagus, and anogenital region. counterpart, MMP, appear to share similar etiologic and
 Oral lesions: Typically present as superficial pathogenetic factors.
ulcers, often limited to the gingiva. Chronic,
persistent, and may heal with scarring. ETIOLOGY
 Bullae: Fragile and short-lived, often not
observed.  Bullous pemphigoid shares similar factors with
 Gingival lesions: Bright red, friable patches or mucous membrane pemphigoid (MMP).
ulcers with mild to moderate discomfort; may  Autoantibodies target basement membrane zone
extend to unattached gingiva. antigens (BP230, BP180) found in
 Positive Nikolsky sign may be observed (easy hemidesmosomes and lamina lucida
stripping of intact epithelium).
PATHOGENESIS.
HISTOPATHOLOGY
 Binding of autoantibodies activates the
 MMP is characterized by subepithelial clefting complement cascade, attracting neutrophils and
without acantholysis. eosinophils.
 Early stages: Few lymphocytes are present.
 Later stages: The infiltrate becomes denser and
CLINICAL FEATURES:
more mixed.
 Primarily affects the elderly, with peak
DIFFERENTIAL DIAGNOSIS
incidence in the 70s and 80s.
 Characterized by tense vesicles and bullae, often
 Pemphigus vulgaris preceded by erythematous papular eruptions.
 Erosive lichen planus  Skin lesions commonly appear on the trunk and
 Atrophic lichen planus (when attached gingiva is limbs.
exclusively involved)  Oral mucosal lesions are similar to those of
 Linear IgA disease MMP, including bullae and erosions on the
 Discoid lupus erythematosus gingiva, soft palate, buccal mucosa, and floor of
 Contact allergy the mouth.
TREATMENT HISTOPATHOLOGY

 Corticosteroids are the main treatment, with  Bullae are subepithelial and cleave at the lamina
prednisone for moderate to severe cases and lucida.
topical steroids for mild cases.
 High-potency topical steroids include clobetasol, TREATMENT:
betamethasone dipropionate, fluocinonide, and
desoximetasone.
 Systemic corticosteroids are the main treatment.
 Custom-made mouth guards can help keep  Nonsteroidal immunosuppressive agents,
topical medication in place for gingival antibiotics (tetracycline, erythromycin), and
involvement. niacinamide may be used.
 Good oral hygiene, including chlorhexidine  Biologic agents, including rituximab
rinses, enhances treatment effectiveness.  Periods of clinical remission can occur.
 Systemic agents like tetracycline, niacinamide,
sulfapyridine, and dapsone may be used when 4) DERMATITIS HERPETIFORMIS
standard therapy fails.
Dermatitis herpetiformis is a cutaneous vesiculobullous
 Immunosuppressive agents (azathioprine, disease characterized by intense pruritus.
cyclophosphamide, methotrexate,
mycophenolate, and cyclosporine) are added to
reduce steroid use in severe cases. ETIOLOGY AND PATHOGENESIS:
 Rituximab is effective in recalcitrant or relapsed
cases.  Dermatitis herpetiformis is a vesiculobullous
disease with intense pruritus.
3 ) BULLOUS PEMPHIGOID
  Associated with granular IgA deposits in the membrane tissue and antibodies to type VII
papillary dermis and epidermal collagen.
transglutaminase.  Hereditary Forms: Includes dystrophic,
 Often linked with celiac disease, which involves junctional, and simplex types, with varying
autoantibodies to tissue transglutaminase. genetic origins (autosomal dominant or
recessive) and involving defects in basal cells,
CLINICAL FEATURES: hemidesmosomes, or anchoring filaments.

 Chronic disease mostly seen in young and CLINICAL FEATURES:
middle-aged adults, with a slight male
predominance.  Common Feature: Formation of blisters with
 Characterized by papular, erythematous, minor trauma, especially on stress areas (e.g.,
vesicular lesions that are intensely pruritic. elbows, knees).
 Lesions are usually symmetric, affecting  Onset: Infancy or early childhood for hereditary
extensor surfaces (elbows, shoulders, sacrum, forms; adulthood for acquired type.
buttocks) and may involve scalp and face.  Severity: Greater in inherited recessive forms,
 Oral involvement is rare with possible widespread blisters, scarring, and
dystrophic nails.
HISTOPATHOLOGY  Oral Manifestations: Common and severe in
recessive forms, including bullae, scarring,
 Neutrophils, eosinophils, and fibrin are present constricted oral orifice, and hypoplastic teeth.
at the tips of dermal papillae.
TREATMENT AND PROGNOSIS:
TREATMENT AND PROGNOSIS:
 Treatment: Focuses on trauma avoidance and
 Treated with dapsone, sulfoxone, or supportive care; options include corticosteroids,
sulfapyridine. vitamin E, phenytoin, retinoids, dapsone, and
 Gluten-free diet helps in managing associated immunosuppressive agents.
enteropathy and reduces small bowel pathology.
 Lifelong condition with long periods of WHITE LESIONS
remission; often requires ongoing dietary
restrictions or drug treatment.  White Lesions:
o Appear due to scattering of light through
 HEREDITARY DISEASE thickened keratin, epithelial hyperplasia,
intracellular edema, or reduced
1) EPIDERMOLYSIS BULLOSA vascularity.
Epidermolysis bullosa is a general term that o Can also result from fibrinous exudate,
encompasses one acquired and as many as 20 submucosal deposits, surface debris, or
genetic or hereditary varieties (dystrophic, fungal colonies.
junctional or simplex) of diseases that are
characterized by the formation of blisters at sites of  HEREDITARY CONDITIONS
minor trauma.
LEUKOEDEMA:

Leukoedema is a generalized mild opacification of the
buccal mucosa that is common enough to be regarded
as a variation of normal.

ETIOLOGY AND PATHOGENESIS:

 Acquired Form: Epidermolysis bullosa
acquisita, often triggered by specific drugs,
characterized by IgG deposits in sub-basement
 o ETIOLOGY AND PATHOGENESIS: known as Witkop disease or Witkop-von Sallmann
 Cause unknown; factors like syndrome, is a rare, hereditary condition (autosomal
smoking, tobacco, alcohol, dominant).
infection, and cannabis use
implicated but not proven. o ETIOLOGY:
o CLINICAL FEATURES:  Autosomal-dominant condition
 Asymptomatic, gray-white, linked to a mutation in NLRP1
diffuse, filmy/milky surface, on chromosome 17p13.2.
typically in buccal mucosa. o CLINICAL FEATURES:
o HISTOPATHOLOGY:  Early onset of bulbar
 Parakeratotic and acanthotic conjunctivitis and oral white
epithelium with marked lesions, usually in the first year
intracellular edema of spinous of life.
cells.  Oral lesions: soft,
o TREATMENT: asymptomatic, white
 No treatment needed folds/plaques of spongy
mucosa.
WHITE SPONGE NEVUS (WSN): o HISTOPATHOLOGY:
 Epithelial hyperplasia and
White sponge nevus (WSN) is an autosomal-dominant acanthosis with intracellular
inherited condition that is due to point mutations for edema and dyskeratotic
genes coding for keratin 4 and/or 13. elements.
o TREATMENT:
 No treatment needed

FOLLICULAR KERATOSIS (DARIER’S
DISEASE):

Follicular keratosis (Darier’s disease, Darier-White
disease) is an autosomal-dominant disorder that results
o ETIOLOGY:
in desmosomal defects and dysfunction by way of
 Autosomal-dominant
inheritance due to mutations in altered epithelial cell adhesion
keratin 4 and/or 13.
o CLINICAL FEATURES: o ETIOLOGY:
 Asymptomatic, thickened,  Autosomal-dominant disorder
spongy white lesions, bilaterally caused by mutations in ATP2A2
and symmetrically on buccal on chromosome 12q23-24,
mucosa. affecting calcium-dependent
 Typically appears before cell processes.
puberty, sparing skin. o CLINICAL FEATURES:
o HISTOPATHOLOGY:  Onset between ages 6-20 years;
 Thickened epithelium with mainly affects the skin.
spongiosis, acanthosis,  Oral lesions: small, whitish
parakeratosis, and marked papules on the attached gingiva
hydropic changes. and hard palate.
o TREATMENT: o HISTOPATHOLOGY:
 No treatment required  Formation of suprabasal lacunae
with acantholytic cells, basal
HEREDITARY BENIGN layer proliferation, vertical
INTRAEPITHELIAL DYSKERATOSIS clefts, and presence of corps
(HBID): ronds and grains.
o TREATMENT:
 Topical corticosteroids and
Hereditary benign intraepithelial dyskeratosis (HBID),
retinoic acid to improve skin
also
lesions and reduce symptoms.
  Chronic, slowly progressive inflammation and keratosis with potential
disease; some remissions dysplastic changes.
possible.  CLINICAL FEATURES: White lesions
develop in areas where tobacco is placed, often
 REACTIVE LESIONS in the mucobuccal fold; may appear granular,
wrinkled, or folded; usually painless.
FOCAL (FRICTIONAL) HYPERKERATOSIS  HISTOPATHOLOGY: Shows parakeratosis,
epithelial changes, and potential dysplasia;
inflammatory infiltrate is common.
Focal (frictional) hyperkeratosis is a white lesion that is
 TREATMENT AND PROGNOSIS: Lesions
related to chronic rubbing or friction against an oral
may resolve with cessation of tobacco use
mucosal surface.
NICOTINE STOMATITIS

Nicotine stomatitis is a common tobacco-related form
of keratosis.

 ETIOLOGY: White lesion caused by chronic
rubbing or friction against oral mucosa, similar
to a callus on the skin.
 CLINICAL FEATURES: Commonly occurs
on lips, lateral tongue, buccal mucosa, and
edentulous alveolar ridges; may result from
cheek/lip chewing or trauma from dentures.  ETIOLOGY: Associated with pipe and cigar
 HISTOPATHOLOGY: Shows hyperkeratosis smoking; related to the direct topical effect of
with a few chronic inflammatory cells in the smoke and heat.
underlying tissue.  CLINICAL FEATURES: Begins with
 DIAGNOSIS: Based on history and erythematous change and progresses to
examination; resolves with cessation of the keratinization; red dots surrounded by white
causative habit. rings appear on the palate.
 TREATMENT: Observation; habit control  HISTOPATHOLOGY: Shows epithelial
leads to improvement; no malignant potential. hyperplasia, hyperkeratosis, and inflammation of
minor salivary glands.
WHITE LESIONS ASSOCIATED WITH  TREATMENT AND PROGNOSIS: Rarely
SMOKELESS TOBACCO leads to malignancy, except in reverse smokers;
indicates a higher risk of dysplasia and neoplasia
A causal relationship has been documented between elsewhere.
smokeless tobacco and white tissue changes.
HAIRY LEUKOPLAKIA

In 1984, an unusual white lesion along the lateral
margins of the tongue, predominantly in gay men, was
first described.

 ETIOLOGY: Caused by the use of smokeless
tobacco, particularly snuff; involves
 Dentifrice-associated slough is a relatively common
phenomenon that has been associated with the use of
several different brands of toothpaste

 ETIOLOGY AND PATHOGENESIS: Related
to Epstein-Barr virus (EBV); commonly seen in
HIV-infected individuals or those with other
forms of immunosuppression.
 CLINICAL FEATURES: Presents as a well-
demarcated white lesion on the lateral margins  ETIOLOGY: Superficial chemical burn or
of the tongue; may be unilateral or bilateral, flat, reaction to toothpaste components like
or corrugated. detergents or flavoring agents.
 HISTOPATHOLOGY: Characterized by  CLINICAL FEATURES: Presents as a
hyperparakeratosis, viral inclusions, and painless, superficial whitish slough on the buccal
ballooning degeneration of keratinocytes. mucosa, easily swiped away; resolves with a
 TREATMENT AND PROGNOSIS: No switch to a blander toothpaste.
specific treatment; linked to HIV and other  TREATMENT AND PROGNOSIS: Switching
immunosuppressive conditions. to another toothpaste or mouth rinse resolves the
issue; benign condition.
HAIRY TONGUE
 PRENEOPLASTIC AND NEOPLASTIC
Hairy tongue is a clinical term referring to a condition of LESIONS
filiform papillary overgrowth on the dorsal surface of
the tongue of variable color. ACTINIC CHEILITIS (AC)

Actinic, or solar, cheilitis represents accelerated tissue
degeneration of the vermilion (dry mucous membrane)
of the lips, especially the lower lip, as a result of chronic
exposure to sunlight;

 ETIOLOGY: Linked to antibiotic use,
smoking, radiation therapy, and poor oral
hygiene; caused by overgrowth of filiform
papillae and microbial proliferation.
DEFINITION:
 CLINICAL FEATURES: Appears as a thick,
matted surface on the dorsal tongue; color varies
from white to black; usually asymptomatic but  Degeneration of the vermilion (lip) tissue due to
may cause gagging. chronic sun exposure; potentially premalignant.
 HISTOPATHOLOGY: Shows elongated
filiform papillae with surface contamination by PATHOGENESIS:
microorganisms.
 TREATMENT AND PROGNOSIS:  Caused by UVB rays (2900-3200 nm), affecting
Discontinuing causative agents and practicing both epithelium and connective tissue.
good oral hygiene
CLINICAL FEATURES
DENTIFRICE-ASSOCIATED SLOUGH
  Appearance: Lips appear atrophic, pale, silvery  CLINICAL FEATURES: Common in middle-
gray, glossy; fissuring, wrinkling, and swelling aged and older adults; predominant sites include
are common. mandibular and buccal mucosa.
 Advanced Cases: Poorly defined vermilion-skin  HISTOPATHOLOGY: Varies from
junction, epidermization, hyperpigmentation, hyperkeratosis to invasive carcinoma; dysplasia
keratosis, scaling, cracking, ulceration may be mild, moderate, or severe.
 TREATMENT: Periodic exams, rebiopsy,
HISTOPATHOLOGY excision of dysplastic lesions, with options like
cryosurgery, laser surgery, or topical agents.
 Epithelium: Atrophic, hyperkeratotic, with
potential dysplasia.  DIFFERENTIAL DIAGNOSIS: Consider if
 Connective Tissue: Solar elastosis (basophilic the lesion can be removed or if it is bilaterally
changes) and telangiectasia. present; biopsy non-removable lesions.

TREATMENT  OTHER WHITE LESIONS

 Prevention: Avoid sun exposure; use lip balm GEOGRAPHIC TONGUE (ERYTHEMA
with sunscreen (PABA, titanium dioxide, zinc IGRANS/BENIGN MIGRATORY GLOSSITIS)
oxide).
 Advanced Cases: Biopsy of persistent ulcers; Geographic tongue, also known as erythema
vermilionectomy or wedge excision for migrans and benign migratory glossitis, is a
suspicious lesions; options include laser surgery, condition of unknown cause.
cryosurgery

ACTINIC KERATOSES (AK)

Actinic keratoses of the skin, the cutaneous counterpart
of actinic cheilitis, are epithelial changes noted typically
in lightcomplexioned individuals who have had long-
term exposure to sunlight.

 Relation to AC: AK is the cutaneous
counterpart of AC, often found in sun-exposed  Etiology: Geographic tongue is a condition with
areas like the face and neck. an unknown cause, often more prevalent in
 Appearance: Oval plaques, rough texture, color whites and blacks compared to Mexican
varies from yellow-brown to red. Americans.
 Risk: A small percentage may develop into  Clinical Features: The condition is
squamous cell carcinoma. characterized by atrophic patches on the tongue
 Treatment: Cryotherapy, topical 5-fluorouracil, surrounded by elevated keratotic margins, which
curettage, surgical excision, and biopsy for appear red and may be slightly tender. The
suspicious lesions. pattern changes over days or weeks, seemingly
moving across the tongue.
IDIOPATHIC LEUKOPLAKIA  Histopathology: Geographic tongue features
atrophy of the filiform papillae, hyperkeratosis,
and acanthosis at the lesion's margins.
Leukoplakia is a descriptive clinical term indicating a
 Differential Diagnosis include candidiasis,
white patch or plaque of oral mucosa that cannot be
leukoplakia, lichen planus, and lupus
rubbed off and cannot be characterized clinically as any erythematosus.
other disease  Treatment and Prognosis: Treatment is
generally unnecessary due to the self-limiting
 Definition: White oral mucosal patch that and asymptomatic nature of geographic tongue.
cannot be rubbed off or identified as another
disease; may range from benign hyperkeratosis LICHEN PLANUS
to invasive squamous cell carcinoma.
 ETIOLOGY: Often related to tobacco use,
alcohol, trauma, or C. albicans infection.
Lichen planus is a chronic mucocutaneous disease o Systemic (Acute) Lupus
of unknown cause, with oral lesions occurring most Erythematosus (SLE): Affects multiple
commonly in women between 30 and 60 years of organs, more severe.
age o Discoid (Chronic) Lupus
Erythematosus (DLE): Mainly affects
the skin, especially the face; rarely
progresses to SLE.
o Subacute Cutaneous Lupus
Erythematosus: Intermediate between
SLE and DLE; mild systemic
involvement with skin lesions.
 ETIOLOGY AND PATHOGENESIS:
o Autoimmune disease involving both
humoral and cell-mediated immune
responses.
 CLINICAL FEATURES:
 ETIOLOGY AND PATHOGENESIS: Lichen o DLE:
planus is a chronic mucocutaneous disease with  Common in middle-aged
an unknown cause, commonly affecting women women.
between 30 and 60 years old. It is believed to be  Lesions typically on face and
an immunologically mediated process, scalp; may cause scarring and
resembling a hypersensitivity reaction. permanent hair loss.
 CLINICAL FEATURES: Stress may influence o SLE:
disease severity, but it is not a sole cause. An  Milder skin and mucosal
association with hepatitis C has been suggested lesions; multisystem
 HISTOPATHOLOGY: Microscopic features involvement dominates.
include hyperkeratosis, basal layer  Classic "butterfly" rash on the
vacuolization, and a lymphophagocytic infiltrate face; other body areas may also
at the epithelium-connective tissue interface. be affected.
DIFFERENTIAL DIAGNOSIS: include  Systemic symptoms include
lichenoid drug reactions, lupus erythematosus, fever, weight loss, and malaise.
white sponge nevus, hairy leukoplakia, cheek  HISTOPATHOLOGY:
chewing, graft-versus-host disease, candidiasis, o DLE: Basal cell destruction,
idiopathic leukoplakia, and squamous cell hyperkeratosis, epithelial atrophy,
carcinoma. o SLE: Similar to DLE but with less
 TREATMENT AND PROGNOSIS: Lichen intense inflammation
planus cannot be cured, but symptoms can be  DIFFERENTIAL DIAGNOSIS:
managed with corticosteroids o Oral LE lesions may resemble erosive
lichen planus but are less symmetrical.
SYSTEMIC ERYTHEMTOSUS (LE) o Other differential diagnoses include
mucous membrane pemphigoid,
erythematous lichen planus,
Lupus erythematosus (LE) may be seen in one of
erythematous candidiasis, and contact
two wellrecognized forms: systemic (acute) lupus hypersensitivity.
erythematosus (SLE) and discoid (chronic) lupus  TREATMENT:
erythematosus (DLE), both of which may have oral o DLE: Treated with topical
manifestations. corticosteroids; refractory cases may
require antimalarials or sulfones.
o SLE: Systemic steroids like prednisone,
often combined with
immunosuppressants; antimalarials and
NSAIDs may also be used.

CANDIDIASIS
Candidiasis is a common opportunistic oral mycotic oFungal hyphae penetrate the
infection that develops in the presence of one of epithelium; neutrophilic infiltration is
several predisposing conditions. common.
 DIFFERENTIAL DIAGNOSIS:
o Candidal lesions should be
differentiated from chemical burns,
syphilis, white keratotic lesions, and
others.
 TREATMENT AND PROGNOSIS:
o Topical antifungals like nystatin or
clotrimazole are effective for most
cases.

 ETIOLOGY AND PATHOGENESIS: MUCOSAL BURNS
o Caused by C. albicans and, less
commonly, other species like C. The most common form of superficial burn of the oral
parapsilosis, C. tropicalis, etc. mucosa is associated with topical applications of
o Exists in three forms: yeast chemicals, such as aspirin or caustic agents
(blastospores), pseudohyphae, and
chlamydospores.
o Infection usually remains superficial,
affecting oral mucosa or skin.
 CLINICAL FEATURES:
o Acute Pseudomembranous Candidiasis
(Thrush):
 Common in infants, elderly,
patients with cancer, or those
undergoing chemotherapy.
 White, soft plaques on the oral
mucosa; painful when wiped
away.  ETIOLOGY:
o Acute Erythematous Candidiasis: o Caused by topical application of
chemicals (e.g., aspirin, caustic agents,
 May result from persistent
drugs).
pseudomembranous
o Accidental dental procedures (e.g.,
candidiasis. phosphoric acid) or overuse of alcohol-
 Associated with antibiotic use; based mouth rinses.
manifests as red lesions with o Thermal burns from hot foods/liquids,
erosions. commonly on the hard palate.
o Chronic Erythematous Candidiasis:  CLINICAL FEATURES:
 Common in geriatric patients o Localized mild erythema to white
with dentures; primarily affects slough/membrane due to surface
the palate. necrosis.
 Causes bright red, velvety  HISTOPATHOLOGY:
mucosa; can lead to angular o Coagulative necrosis of the epithelium;
cheilitis. fibrinous exudate; intense inflammation.
o Chronic Hyperplastic Candidiasis:  TREATMENT:
 Resembles leukoplaki o Symptomatic therapy (e.g., sodium
 Includes median rhomboid bicarbonate rinses, analgesics).
o Avoid alcohol-based mouth rinses;
glossitis and nodular papillary
lesions.
o Mucocutaneous Candidiasis:
SUBMUCOUS FIBROSIS
 Persistent candidiasis affecting
oral mucosa, skin, and nails.
 HISTOPATHOLOGY:
Several factors contributing to submucous fibrosis oLobules of sebaceous glands around
include general nutritional or vitamin deficiencies and excretory ducts; glands appear
hypersensitivity to various dietary constituents. functional.
 TREATMENT:
 ETIOLOGY: o No treatment necessary
o Caused by chewing areca (betel) nut,
nutritional deficiencies, and chronic ECTOPIC LYMPHOID TISSUE
irritants.
o Impaired collagen degradation and Lymphoid tissue may be found in numerous oral
increased collagen cross-linking. locations, most notably in the region surrounding the
 CLINICAL FEATURES: oropharynx termed Waldeyer’s ring.
o Common in Southeast Asia; associated
with areca nut and tobacco use.  ETIOLOGY:
o Whitish-yellow mucosal changes o Lymphoid tissue found in various oral
leading to fibrosis, trismus, and locations, part of Waldeyer’s ring.
difficulty eating.  CLINICAL FEATURES:
o Often affects buccal mucosa and soft o Small, dome-shaped yellow or yellow-
palate; possible extension to pharynx white elevations.
and esophagus. o Typically uninflamed and
 HISTOPATHOLOGY: asymptomatic.
o Epithelial atrophy and fibrosis with mild o Sometimes leads to "lymphoepithelial
to moderate inflammation. cysts" due to crypt obstruction.
 TREATMENT:  TREATMENT:
o Eliminate causative agents; use of o No biopsy needed unless cystic changes
chymotrypsin, hyaluronidase, are suspected.
dexamethasone injections.
o Surgical excision and grafts; condition is GINGIVAL CYSTS
generally irreversible.
o High risk of progression to squamous
Gingival cysts of odontogenic origin occur in adults, as
cell carcinoma.
well as in infants (Bohn’s nodules).
FORDYCE’S GRANULES
 ETIOLOGY:
o Neonatal gingival cysts arise from
Fordyce’s granules represent ectopic sebaceous glands dental lamina remnants; adult cysts
or sebaceous choristomas (normal tissue in an likely from dental lamina remnants or
abnormal location). traumatic implantation.
o Epstein’s pearls (midline palatal cysts)
result from epithelial entrapment during
palatal fusion.
 CLINICAL FEATURES:
o Neonatal cysts: off-white nodules on
alveolar crests; midline palatal cysts
along the palatal raphe.
 ETIOLOGY: o Adult cysts: painless growths on the
o Ectopic sebaceous glands; considered a attached gingiva, often in the
developmental variation of normal. mandibular premolar region.
 CLINICAL FEATURES:  HISTOPATHOLOGY:
o Multiple yellow or yellow-white o Neonatal cysts: stratified squamous
granules, often in aggregates. epithelium lined with keratinaceous
o Common on buccal mucosa and upper debris.
lip vermilion. o Adult cysts: thin cuboidal or flattened
o Asymptomatic and typically noticed in epithelium with focal clear cell change.
routine examinations.  TREATMENT:
 HISTOPATHOLOGY: o Neonatal cysts: no treatment needed
o Adult cysts: require surgical excision.
PARULIS  The exact cause of Paget's disease is unknown,
but possible factors include infection by
A parulis, or “gum boil,” represents a focus of pus in the paramyxovirus, environmental influences, and
gingiva genetic mutations, which affects osteoclast
development.

PATHOGENESIS:

 Paget's disease involves abnormal bone
remodeling due to altered osteoclast and
osteoblast functions. The disease progresses
through stages: Resorptive Phase, Vascular
Phase, Sclerotic Phase:

CLINICAL FEATURES:
 ETIOLOGY:
o Represents pus from an acute infection  Typically affects individuals over 50 years old.
at the base of a periodontal pocket or  Common sites include the pelvis, skull, tibia,
nonvital tooth. vertebrae, humerus, sternum, and jaws
 CLINICAL FEATURES: (especially the maxilla).
o Yellow-white gingival swelling with  Symptoms include bone pain (deep and aching),
associated erythema; pain relieved when deformity, increased skin temperature over
pus escapes. affected areas, and neurologic issues (e.g.,
 TREATMENT: headache, hearing and vision disturbances,
o Address underlying periodontal pocket vertigo).
or nonvital tooth infection to resolve the  Oral signs include jaw enlargement, diastemas,
abscess. ill-fitting dentures, patchy radiographic
opacities, and hypercementosis.
LIPOMA
HISTOPATHOLOGY:
Lipoma appears as a yellow or yellow-white uninflamed
submucosal mass of adipose tissue. I  Initial phase shows random overactive
osteoclastic resorption.
 ETIOLOGY:
o A submucosal mass of adipose tissue, DIFFERENTIAL DIAGNOSIS:
typically yellow or yellow-white and
uninflamed.  Fibrous dysplasia, osteopetrosis, and
osteosarcoma, among others.

TREATMENT:
METABOLIC AND GENETIC
 Treatment is typically indicated for symptomatic
DISEASE patients or those with elevated alkaline
phosphatase levels.
 METABOLIC CONDITIONS  Bisphosphonates and calcitonin are used to
control bone resorption and deposition.
PAGET'S DISEASE (OSTEITIS DEFORMANS)
HYPERPARATHYROIDISM
Paget’s disease, or osteitis deformans, is a chronic,
slowly progressive metabolic disorder of bone of Hyperparathyroidism may be one of three types:
undetermined cause primary, secondary, or hereditary

ETIOLOGY:  ETIOLOGY:
  Primary Hyperparathyroidism: Caused by Hyperfunction of the thyroid gland, or hyperthyroidism,
hypersecretion of parathyroid hormone (PTH) encompasses several conditions.
 Secondary Hyperparathyroidism:
Compensatory response to low serum calcium  ETIOLOGY:
due to conditions like renal failure,
malabsorption, or vitamin D deficiency.  Graves’ disease
 Hereditary Hyperparathyroidism:  Excess stimulation via the hypothalamic-
Autosomal-dominant condition (e.g., multiple pituitary axis.
endocrine neoplasia types 1 and 2A).
 PATHOGENESIS:
 PATHOGENESIS:
 Excessive production of thyroid hormones T3
 Elevated PTH leads to increased osteoclast and T4.
activity, resulting in bone resorption, elevated
serum calcium,
 Secondary hyperparathyroidism occurs due to  CLINICAL FEATURES:
hypocalcemia from chronic renal failure or
malabsorption,  Systemic: Heat intolerance, hyperhidrosis,
palmar erythema, fine motor tremor, muscle
weakness, palpitations, atrial fibrillation,
 CLINICAL FEATURES:
diarrhea, anxiety, irritability, weight loss,
menstrual dysfunction.
 Asymptomatic in many cases, detected through  Dermatologic: Altered complexion, thinning
elevated serum calcium. and brittle hair.
 Symptoms may include fatigue, weakness, bone  Ocular: Upper lid retraction, lid lag,
pain, headaches, nausea, anorexia, polyuria, exophthalmos (bright-eyed stare).
thirst, depression, and constipation.  Other: Pretibial myxedema, acropachy (soft
 "Stones, bones, groans, and moans" (renal tissue enlargement, finger clubbing).
calculi, bone pathology, duodenal ulcers,  Cardiac: Increased stroke volume, pulse rate,
neuropsychiatric symptoms). and cardiac output.
 Oral manifestations include loosening of teeth,  Oral: Premature exfoliation of deciduous teeth,
osteoporotic appearance of the jaw, and rapid eruption of permanent teeth (children),
radiolucencies. osteoporosis of the mandible and maxilla
(adults), burning tongue, increased dental
 HISTOPATHOLOGY: erosion.

 Bone lesions show osteoclastic resorption and  HISTOPATHOLOGY:
formation of osteoid trabeculae by osteoblasts.
 Hyperplastic thyroid tissue with follicular
 DIFFERENTIAL DIAGNOSIS: hyperplasia.

 Conditions like central giant cell granuloma,  DIFFERENTIAL DIAGNOSIS:
osteitis fibrosa cystica, and other metabolic bone
disorders should be considered.  Toxic multinodular goiter.
 Thyroiditis.
 TREATMENT:  Other forms of thyrotoxicosis.

 Primary Hyperparathyroidism: Surgical  TREATMENT:
removal of the affected parathyroid glands;
medical management with bisphosphonates in  Symptom Control: Beta-blockers to manage
some cases. symptoms like tachycardia and tremors.
 Secondary Hyperparathyroidism:  Thyroid Hormone Reduction: Thyroid-
Management of underlying renal disease, use of suppressive drugs (e.g., propylthiouracil,
vitamin D analogs, methimazole)
 Surgery: Thyroidectomy with caution
HYPERTHYROIDISM
HYPOTHYROIDISM Hypophosphatasia represents a deficiency of alkaline
phosphatase
Hypothyroidism is a systemic condition that is caused by
reduced production of thyroid hormone.  ETIOLOGY:

 ETIOLOGY:  Caused by a deficiency of alkaline phosphatase.
 Rare hereditary disorder transmitted in an
 Congenital defect. autosomal-recessive manner.
 Iodine deficiency goiter.
 Autoimmune (Hashimoto’s thyroiditis).  PATHOGENESIS:
 Diseases of the pituitary and hypothalamus
(central hypothyroidism).  Leads to inadequate formation of dentin and
cementum in teeth.
 PATHOGENESIS:  Results in disordered bone mineralization,
causing rickets, osteomalacia, fractures, and
 Reduced production of thyroid hormones (T3 other skeletal abnormalities.
and T4).  Affects long bones, leading to inadequate
 Primary hypothyroidism: Low T4, high TSH mineralization and wide osteoid seams.
(compensatory pituitary response).
 Secondary hypothyroidism: Low T4 and low  CLINICAL FEATURES:
TSH (pituitary malfunction).
 Dental Features:
 CLINICAL FEATURES: o Premature loss of primary dentition,
primarily involving anterior teeth.
 Children: Cretinism (delayed skeletal and o Enlarged pulp chambers, alveolar bone
dental development, sexual immaturity). loss, abnormal root cementum, and
 Adults: Myxedema (edema of face, eyes, lips, hypoplastic enamel defects.
tongue).  Skeletal Features:
 General: Fatigue, lethargy, slow pulse, anemia, o Delayed skeletal development,
hyperlipidemia. especially in congenital and early
infantile types.
 HISTOPATHOLOGY:
 HISTOPATHOLOGY:
 Hypofunctional thyroid tissue with reduced
follicular activity.  Decreased tissue levels of alkaline phosphatase.

 DIFFERENTIAL DIAGNOSIS:  DIFFERENTIAL DIAGNOSIS:

 Central hypothyroidism.  Cyclic neutropenia, idiopathic histiocytosis,
 Euthyroid sick syndrome. juvenile periodontitis, acrodynia, rickets,
 Depressive disorders (due to similar lethargy Papillon-Lefèvre syndrome (conditions
symptoms). associated with premature tooth exfoliation).
 Anemia (due to fatigue and lethargy).
 TREATMENT:
 TREATMENT:
 No successful treatment
 Gradual replacement with synthetic or natural  Management focuses on controlling
thyroid hormone preparations. hypercalcemia, large doses of vitamin D.
 Monitor and adjust drug dosages (opiates,
hypnotics, anticoagulants) INFANTILE CORTICAL HYPERTOSIS

HYPOPHOSPHATASIA Infantile cortical hyperostosis, or Caffey’s disease, is a
very rare, self-limited, short-lived proliferative bone
disease of genetic origin which usually manifests in bone secondary to a non-neoplastic vascular-lymphatic
early infancy. proliferation

 ETIOLOGY:  ETIOLOGY:

 Rare, self-limited, proliferative bone disease of  Also known as massive osteolysis or vanishing
genetic origin. bone disease.
 Typically manifests in early infancy.  Rare, non-neoplastic condition characterized by
progressive localized destruction of bone.
 PATHOGENESIS:
 PATHOGENESIS:
 Characterized by cortical-subperiosteal
thickening of various bones,  Bone destruction occurs slowly and
 Swelling of overlying soft tissues is common. progressively, often following trauma or
 Pain, fever, and hyperirritability are frequent spontaneously.
symptoms.
 Diagnostic triad: swelling, bone lesions, and  CLINICAL FEATURES:
irritability.
 Bone Involvement:
 CLINICAL FEATURES: o Can affect nearly any bone in the body,
with the maxillofacial region involved in
 Bone Involvement: some cases.
o Mandible most commonly affected, o Usually develops before the fourth
especially in sporadic cases ( decade of life, although it can affect
o Other affected bones may include individuals from 18 months to 72 years
clavicles, long bones, maxilla, ribs, and of age.
scapulae. o Progressive atrophy of the affected bone
 Radiographic Features: leads to significant deformity.
o Expansile hyperostotic process visible o In severe cases, the affected bone may
over the cortical surface. completely disappear.
o Rounding or blunting of the mandibular  Symptoms:
coronoid process. o Pain is usually absent unless a
pathological fracture occurs.
 DIAGNOSIS: o Swelling and variable levels of
osteolysis may be present.
 Technetium (99mTc) scans can facilitate early
diagnosis, often positive before routine  RADIOGRAPHIC FEATURES:
radiographic detection.
 Early signs include intermedullary subcortical
 TREATMENT: radiolucencies with indistinct margins and thin
radiopaque borders.
 Primarily supportive care
 Systemic corticosteroids and NSAIDs  DIAGNOSIS:
 The disease course may include relapses and
remissions;  No known genetic basis or specific ethnic or
gender predilection.
PHANTOM BONE DISEASE (GORHAM`S
DISEASE)  TREATMENT:

Phantom bone disease, also known as massive  No standardized effective treatment is available.
osteolysis, Gorham’s disease, or vanishing bone disease,  Surgical interventions, such as bone grafts, are
is an unusual process characterized by posttraumatic or often unsuccessful as the disease can affect the
spontaneous slow, progressive, localized destruction of graft.
 Moderate doses of radiation therapy
ACROMEGALY
 GENETIC ABNORMALITIES
This disease is characterized by bony and soft tissue
overgrowth and metabolic disturbances. CHERUBISM

 ETIOLOGY: Cherubism is a benign hereditary condition that affects
the jaws only and is transmitted as an autosomal-
 Over 90% of cases are due to a benign pituitary dominant trait.
adenoma that secretes excessive GH.
 ETIOLOGY:
 PATHOGENESIS
 Genetic Basis:
 Pituitary adenomas may also produce other o The condition is linked to mutations in
hormones, including prolactin, TSH, or ACTH. the SH3BP2 gene on chromosome
4p16.3.
o The condition has been classified by
 CLINICAL FEATURES:
some as an autoinflammatory disease.
 Typically presents in the fourth decade of life,
with an insidious onset leading to delayed  CLINICAL FEATURES:
diagnosis.
 Younger patients often have more aggressive  Usually detected in children by the age of 5.
tumors.  Symmetric enlargement of the mandible and/or
maxilla.
 Most commonly affects the mandibular angle,
Symptoms:
ascending ramus, retromolar region, and
posterior maxilla.
 Hyperhidrosis, coarse body hair, muscle  Bilateral swelling of the lower face with full
weakness, paresthesia/carpal tunnel syndrome, cheeks and upward-gazing eyes, giving a
large joint arthropathy, and dysmenorrhea. "cherubic" appearance.
 Thickened skin, sleep apnea, hypertension, and  Hard, nontender swellings in affected areas.
heart disease. Premature loss of primary teeth, displacement of
 Skin tags, which may be indicative of colonic developing tooth follicles, ectopic eruption, and
polyps. impaction of permanent teeth.
 Facial changes including frontal bossing, nasal  Well-defined multilocular radiolucencies in the
bone hypertrophy, and mandibular prognathism. jaws, often giving a "soap bubble" appearance.
 Enlarged paranasal sinuses and laryngeal
hypertrophy leading to a deep, resonant voice.
 Enlargement of the mandible and maxilla,  HISTOPATHOLOGY:
leading to dental malocclusion, macroglossia,
and prominent lips.  Vascularized fibrous stroma with multinucleated
giant cells, resembling central giant cell
granuloma.
 DIAGNOSIS:

 Nonsuppressible GH levels after glucose loading  DIFFERENTIAL DIAGNOSIS:
is diagnostic.
 MRI or CT of the sella turcica to detect pituitary  Include ossifying fibroma, giant cell granuloma,
tumors. giant cell tumor, fibrous dysplasia, and Paget’s
disease.
 TREATMENT:
 TREATMENT AND PROGNOSIS:
 Transsphenoidal surgery to remove the pituitary
adenoma is the primary treatment.  Conservative curettage and bone recontouring
 Conventional or radiosurgery, used especially in may be performed if necessary to improve
recurrent or persistent cases. function, prevent debility, or address cosmetic
 Somatostatin receptor ligands (e.g., octreotide). concerns.
OSTEOPETROSIS  DIFFERENTIAL DIAGNOSIS:

Osteopetrosis, also known as Albers-Schönberg disease, o Includes osteomalacia, Paget’s disease,
is a rare hereditary bone condition clinically hyperparathyroidism, acromegaly, and
characterized by a generalized symmetric increase in malignant bone disease.
skeletal density due to defective bone resorption.
OSTEOGENESIS IMPERFECTA
 Etiology
Osteogenesis imperfecta represents a genetically and
 Osteopetrosis, also known as Albers-Schönberg phenotypically heterogeneous group (nine major
disease, is a rare hereditary bone disorder subtypes) of heritable defects of connective tissue with
characterized by increased skeletal density due an estimated incidence of 1:20,000 births
to defective bone resorption.
 Etiology:
 PATHOGENESIS
 Genetic disorder with mutations in collagen
o Reduced osteoclastic activity despite genes (COL1A1 and COL1A2).
increased osteoclast numbers.  Autosomal dominant and autosomal recessive
o Lack of bone resorption due to inheritance patterns.
insufficient acid secretion by
osteoclasts.  Pathogenesis:
o Results in increased bone mass and
skeletal disturbances like sclerosis of the  Defects in collagen synthesis or structure lead to
bone marrOW fragile bones.
 Abnormal bone formation and increased fracture
 CLINICAL FEATURES: risk due to impaired bone matrix integrity.

 Bone pain.  Clinical Features:
 Cranial nerve compression leading to blindness,
deafness, anosmia, ageusia, and facial paralysis.  Type I: Osteoporosis, bone fragility, blue
 Normal bone is replaced by dense, poorly sclerae,
structured, and fragile bone, prone to pathologic  Type II: Severe bone fragility, short stature,
fractures. broad thighs,
 Delayed eruption of teeth.  Type III: Severe bone fragility, multiple
 Premature exfoliation due to periodontal fractures,
ligament defects.  Type IV: Osteopenia, bone fragility, bluish
 Malformed and unerupted teeth. sclerae at birth,
 Enamel hypoplasia and increased caries index.
 Bone-within-bone presentation due to defective
 Histopathology:
metaphyseal remodeling.
 Mandible less frequently involved compared to
 Bone Structure: Disrupted collagen matrix
other bones.
leading to brittle bones.
 HISTOPATHOLOGY:
 Differential Diagnosis:
o Normal bone production with defective
 Osteomalacia
resorption.
 Paget’s disease
o Disrupted endochondral bone formation.
 Hyperparathyroidism
 Acromegaly
 TREATMENT AND PROGNOSIS:  Malignant bone disease
o Potential treatments include in utero
 Treatment:
stem cell therapy,
o Bone marrow transplantation has been
 Bisphosphonates to improve bone density.
used to provide osteoclast precursors.
  Fracture management, physical therapy, surgery  TREATMENT:
for deformities and kyphoscoliosis.
 Management of dentinogenesis imperfecta with  Genetic Counseling: Important for
potential full crown coverage. understanding inheritance and management.
 Genetic counseling and patient support groups  Surgical extraction of supernumerary and
for emotional support. overretained primary teeth, surgical exposure of
unerupted teeth, orthodontic treatment.
CLEIDOCRANIAL DYSPLASIA  Protective headgear, orthognathic surgery for
facial deformity correction, and prosthetic
Cleidocranial dysplasia (CCD) is notable for aplasia or rehabilitation for severe cases.
hypoplasia of the clavicles, characteristic craniofacial
malformations, and the presence of numerous CROUZON’S SYNDROME (CRANIOFACIAL
supernumerary and unerupted teeth. DYSOSTOSIS)

 ETIOLOGY: Crouzon’s syndrome is characterized by variable
degrees of cranial deformity, maxillary hypoplasia, and
 Autosomal dominant inheritance with high shallow orbits with exophthalmos and divergent
penetrance; recessive form reported. strabismus
 Caused by mutations in the RUNX2 gene, which
regulates bone differentiation.  ETIOLOGY

 PATHOGENESIS:  Inheritance: Autosomal dominant with
complete penetrance and variable expressivity.
 Intramembranous and endochondral bones
affected, leading to abnormal skull and clavicle PATHOGENESIS:
development.
 Delayed closure of fontanelles and sutures,  Premature fusion of cranial sutures leads to
resulting in cranial deformities. increased intracranial pressure, cranial
 Deficiency in clavicle formation contributes to deformities, shallow orbits, and exophthalmos.
long neck and narrow shoulders.. Distorted cranial base impacts maxillary growth
and nasopharyngeal development.
 CLINICAL FEATURES:
 CLINICAL FEATURES:
 Large head, brachycephalic with prominent
frontal and parietal bossing, hypoplastic facial  Froglike facies, midface hypoplasia,
bones, and maxillary hypoplasia. exophthalmos, relative mandibular prognathism,
 Unerupted supernumerary teeth, delayed parrot-like nose, short upper lip, drooping lower
eruption of permanent teeth, hypoplastic enamel, lip.
taurodontia.  Severe maxillary hypoplasia, narrow maxillary
 Short stature, drooping shoulders, long neck, arch, high-arched palate, bilateral posterior
hypoplastic clavicles, potential kyphoscoliosis, lingual cross-bites, anterior open bite.
and pelvic defects.
 HISTOPATHOLOGY:
 HISTOPATHOLOGY:
 Obliterated sutures, compensatory cranial
 Delayed cementum formation, presence of deformities.
supernumerary teeth, hypoplastic enamel.
 DIFFERENTIAL DIAGNOSIS:
 DIFFERENTIAL DIAGNOSIS:
 Pfeiffer syndrome and Apert syndrome.
 Conditions to Consider: Osteogenesis
imperfecta, Marfan syndrome, other craniofacial  TREATMENT:
dysplasias.
  May include artificial sutures to manage The clinical