3. It is a chronic infectious disease
characterized by lesions of the peripheral
nerve, skin, and mucus
membrane of the URT(nasal mucosa).
World's oldest recorded disease
Every year January 27 is World Leprosy Day
3
5. M. leprae is discovered by Hansen from Norway in 1873
5
6. Leprosy develops slowly from 6 months up to
40 yrs
Results in skin lesions and deformities, most
often affecting the cooler places on the body
( for example: eyes, nose, earlobes, hands,
feet, and testicles) that can be very disfiguring.
6
7. Although human-to-
human transmission is
the primary source of
infection, two other
species can carry and
(rarely) transfer M.
leprae to humans:
chimpanzees and
nine-banded
armadillos.
7
8. The spread of leprosy is believed to be via nasal
discharge (Droplet infection).
Every 1 cc of nasal secretion contains 1- 2millions lepra bacilli
9. 1. Residence in an endemic area.
2. Poverty (malnutrition).
3. Contact with affected armadillo.
4. Immunity
9
10. The incubation period range from 3 -5 years.
Males appear to be twice common than females.
Bimodal age (10-14 years & 35-44 years).
Children are more susceptible to disease.
10
12. A typical lesion shows
asymmetrical hypopigmented,
sharply demarcated macules or
reddish plaques, which spreads at
the periphery and heals in the
centre.
Lepromin Skin Test is positive.
12
15. TUBERCULOID LEPROSY
M/E: Histologically TT
resemble tuberculosis.
Characterized by
tuberculoid granuloma,
made up of epitheloid cell
in the center surrounded by
abundant Langhans giant
cells, lymphocytes and foci
of little or non-caseating
necrosis.
Weak acid-fast bacilli.
15
16. Lepromatous leprosy involves:
◦ the skin,
◦ peripheral nerves,
◦ anterior chamber of the eye,
◦ upper airways (down to the larynx),
◦ testes,
◦ hands and feet.
The vital organs and CNS are rarely affected,
presumably because the core temperature is
too high for growth of M. leprae.
16
17. Lepromatous lesions contain large
aggregates of lipid-laden macrophages
(lepra cells), often filled with masses
(“globi”) of acid-fast bacilli.
Because of the abundant bacteria,
lepromatous leprosy is referred to as
“multibacillary”.
Lepromin skin test is negative.
17
18. Macular, papular, or nodular lesions form on the
face, ears, wrists, elbows, and knees.
With progression, the nodular lesions coalesce to
yield a distinctive leonine facies.
Skin smear shows high bacterial count.
18
Lepromatous Leprosy: Leonine Face
19.
20. M/E: Characterized by diffuse infiltration of foamy
macrophages in the dermis.
Lymphocytes are scanty and giant cells typically absent.
20
Lepromatous leprosy. Acid-fast bacilli
(“red snappers”) within macrophages
Lepromatous leprosy- the
dermis shows clear space.
21. 21
Leprosy. A,
Peripheral nerve.
Note the
inflammatory cell
infiltrates in the
endoneural and
epineural
compartments.
B, Cells within the
endoneurium contain
acid-fast positive
lepra bacilli
22. Tends to be unstable.
With time, an evolution to BT or BL may be
seen.
The lesions are many and may be extensive,
annular with some tendency towards
symmetrical distribution.
22
23. Numerous moderately well
defined, usually large & small
plaques, dome shaped lesions /
nodules.
Sometimes with a slightly
hypopigmented halo & a
tendency towards symmetrical
distribution.
Skin smears strongly positive.
23
24. Procedure to Lepromin Skin Test
A tiny sample of leprosy antigen is injected
under the skin, usually in the forearm.
The skin gets pushed up, forming a small bump.
This is an indication that the antigen has been
injected to the correct depth.
The site of the injection is marked, and is
examined for reaction,
• first after 3 days(early reaction-Fernandez
reaction:-redness and induration) and
• then again after 21 days(late reaction-
Mitsuda reaction:-nodule>5mm).
26. Type I
•Change in host CMI
•Seen in borderlines
•Skin and nerve lesions
Type II
•Antigen antibody
•Seen in LL & BL leprosy
•Skin, nerve & systemic
involvement
27. Seen in BT, BB & BL.
Sudden onset.
Eythematous &
oedematous changes in
old lesions.
Appearing of new lesions.
Tenderness & swelling of
peripheral nerves.
28. Type II Lepra Reaction- Erythema Nodosum Leprosum
(ENL)
Appearance of Erythema nodosum
leprosum (ENL)-like skin lesions-
Erythematous
Tender
Subcutaneous
Resolve in 7 to 10 days
Appear in crops
Occur any where
Associated with fever & joint pains
May be vesicular, pustular & may ulcerate
29. Skin Scrapings
Samples from the skin are obtained from
the edge of the lesion, which is smeared on
the slide and stained with Fite- Faraco
technique to demonstrate the bacilli.
Biopsy
Useful in classification & definitive diagnosis
29
30. Contractures, paralyses, and
autoamputation of fingers or toes may
ensue.
Facial nerve involvement can lead to
paralysis of the eyelids, with keratitis and
corneal ulcerations.
30
31.
32. Sexually acquired infection
Etiologic agent: Treponema pallidum
Disease progresses in stages
May become chronic without treatment
32
33. Etiologic agent:
Treponema pallidum
◦ Corkscrew-shaped, motile
microaerophilic bacterium
◦ Cannot be cultured in vitro
◦ Cannot be viewed by normal
light microscopy
33
Treponema pallidum on darkfield microscopy
Electron photomicrograph, 36,000 x.
34. 34
Penetration:
◦ T. pallidum enters the body via skin and mucous
membranes through abrasions during sexual
contact
◦ Also transmitted transplacentally
Dissemination:
◦ Travels via the lymphatic system to regional
lymph nodes and then throughout the body via
the blood stream
◦ Invasion of the CNS can occur during any stage of
syphilis
Pathogenesis
35.
36. Primary lesion or "chancre" develops at the
site of inoculation
Chancre:
◦ Typically painless, relatively avascular,
circumscribed, indurated, superficially
ulcerated lesion and has a clean base
◦ Progresses from macule to papule to
ulcer
◦ Highly infectious
◦ Heals spontaneously within 1 to 6 weeks
◦ 25% present with multiple lesions
Regional lymphadenopathy: classically
rubbery, painless, bilateral
Serologic tests for syphilis may not be
positive during early primary syphilis.
36
Clinical Manifestations
37. On histologic examination,
Treponemes are visible at the
surface of the ulcer with silver
stains (e.g., Warthin-Starry
stain) or immunofluorescence
techniques.
Chancre contains an intense
infiltrate of plasma cells, with
scattered macrophages and
lymphocytes and a proliferative
endarteritis.
37
38. Secondary lesions occur 3 to 6 weeks after the primary
chancre appears; may persist for weeks to months.
Primary and secondary stages may overlap.
Mucocutaneous lesions - most common.
Manifestations:
◦ Rash (75%-100%)
◦ Lymphadenopathy (50%-86%)
◦ Malaise
◦ Mucous patches (6%-30%)
◦ Condylomata lata (10%-20%)
◦ Alopecia (5%)
Serologic tests are usually highest in titre during this stage
38
Clinical Manifestations
39. Mucosal lesions (highly infectious):
30% develop mucous patch (slightly
raised, oval area covered by a gray
white membrane, a pink base that
does not bleed.
Skin rash: Diffuse, papulosquamous
lesions, may leave residual
pigmentation or depigmentation.
Red lesions in the mouth or vagina
contain the most organisms and are
the most infectious.
39
Clinical Manifestations
40. Most frequently involves the aorta; the CNS; and the
liver, bones, and testes.
The aortitis is caused by endarteritis of the vasa
vasorum of the proximal aorta.
Occlusion of the vasa vasorum results in scarring of the
media of the proximal aortic wall, causing a loss of
elasticity, followed by aneurysm, giving a tree bark
appearance.
There may be narrowing of the coronary artery ostia
caused by subintimal scarring with resulting myocardial
ischemia.
40
Clinical Manifestations
41. Syphilitic gummas are
white-gray and rubbery,
occur singly or multiply,
and vary in size from
microscopic lesions
resembling tubercles to
large tumor-like masses.
They occur in most
organs but particularly in
skin, subcutaneous
tissue, bone, and joints.
41
Clinical Manifestations
42. On histologic examination,
Gummas have centers of
coagulated, necrotic
material and margins
composed of plump,
palisading macrophages
and fibroblasts surrounded
by large numbers of
mononuclear leukocytes,
chiefly plasma cells.
Treponemes are scant in
gummas and are difficult to
demonstrate.
42
Trichrome stain of liver shows a
gumma (scar), stained blue,
caused by tertiary syphilis (the
hepatic lesion is also known as
hepar lobatum
43. Occurs when T. pallidum invades the CNS.
May occur at any stage of syphilis
Can be asymptomatic
Early neurosyphilis occurs a few months to a
few years after infection
◦ Clinical manifestations include acute
syphilitic meningitis, meningovascular
syphilis, ocular involvement
Late neurosyphilis occurs decades after
infection and is rarely seen
◦ Clinical manifestations include general
paresis, tabes dorsalis, ocular involvement
43
44. Occurs when T. pallidum is
transmitted from a pregnant
woman with syphilis to her fetus
May lead to stillbirth, neonatal
death, and infant disorders such as
deafness, neurologic impairment,
and bone deformities
Transmission to the fetus in
pregnancy can occur during any
stage of syphilis; risk is much
higher during primary and
secondary syphilis
Wide spectrum of severity exists;
only severe cases are clinically
apparent at birth
◦ Early lesions (most common):
Infants <2 years old; usually
inflammatory
◦ Late lesions: Children >2 years old;
tend to be immunologic and
destructive
44
46. 46
Principles
◦ Measure antibody directed against a cardiolipin-
lecithin-cholesterol antigen
◦ Not specific for T. pallidum
◦ Titers usually correlate with disease activity and
results are reported quantitatively
◦ May be reactive for life
Non treponemal tests include
◦ VDRL,
◦ Rapid Plasma Reagin test
Diagnosis
47. 47
Principles
◦ Measure antibody directed against T. pallidum
antigens
◦ Qualitative
◦ Usually reactive for life
Treponemal tests include
◦ TP-hemaglutination assay,
◦ Flourescent treponemal Ab test,
◦ Enzyme Immuno Assay
Diagnosis