Title: Epidemiology and Control of Zoonotic Infections
1Epidemiology and Control of Zoonotic Infections
Leishmaniasis
2History
- Cutaneous
- more than 650 years BC
- Avesina named it as KHeiroonie or Jeiroonie in
Ghanoon in 10th century AC(5th century after
Hejrat) - Razi explained it for the first time in 11th
century AC - 1952
- For the first time microorganism was isolated
from the spleen of soldires with visceral
leishmaniasis by Leishman in Dun Dum region near
Kalkate in India
3Importance
- A group of diseases with different clinical
presentations, outcomes complications - Estimated infected persons worldwide 12
millions - Persons living in regions at risk of getting
infection 350 millions - New cases each year 1.5 millions(500000 of them
visceral) - Endemic in 60-70 country
- CFR of visceral
- With Dx Rx 5 10
- Without Rx 100
- Cutaneous a cosmetic problem in endemic areas
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8Infectious Agent
- Genus leishmania
- Cutaneous
- Eastern Hemisphere( old world)
- L. tropica( leishmaniasis recidivans cutaneous
leisions ) L. major cause localized cutaneous
sometimes visceral in India middle East - L. aethiopica( localized diffuse cutaneous )
- Western Hemisphere( new world)
L.braziliensis(mucosal leision) L. mexicana
complexes - Visceral
- Eastern Hemisphere L. donovani complex( Kenya,
Sudan, India, China, Pakistan) , L. infantum(
Central Asia, middle East, Mediterranean region) - Western Hemisphere L. chagasi
- All 3 may cause cutaneous without concomitant
visceral , and post- kala-azar dermal
leishmaniasis
9Occurrence Cutaneous
- Pakistan, India, recently China, Middle East(
including Iran, Afghanistan), southern regions of
the former Soviet Union, sub-Saharan Africa,
Sudan, Kenya, Namibia, Central America, South
America( except Chile Uruguay), Mediterranean
littoral - Rural is more prevalent than urban
10Occurrence Visceral
- In rural regions of tropical sub-tropical
areas, mostly as scattered cases among infants,
children, adolescents but occasionally in
epidemic waves - India, Bangladesh, Pakistan, China, middle east(
including Turkey), Central south America( esp.
Brazil), Sudan, Kenya, Ethiopia, sub-Saharan
Africa, southern regions of the former Soviet
Union, Mediterranean basin - Use of antimalarial insecticides dog population
11Occurrence EMRO
- Public health problem
- Iran, Iraq, Saudi Arabian, Sudan, Syria, Tunisia
- Visceral( kala-azar)
- L. infantum, zoonoses, rural, reservoir
carnivore esp. dog - Cutaneous
- Wet, rural, zoonoses L. major, reservoir
rodents( esp. gerbils) - Iran, Iraq, Saudi Arabia, Pakistan, Syria,
Ordonez, Sudan - Dry, urban, anthroponotic L. tropica
12OccurrenceIran Cutaneous
- common in many parts
- 1366 incidence 14/ 100000 decreasing untill
1368.after that increasing the highest
incidence in 1371 91/ 100000 - Isfahan Hormozgan
- Imposed war, immigration, decreased use of
antimalarial insectisides - Urban
- Tehran, Mashad, Shiraz, neishabour, Kerman, Bam
- Mostly in face, no seasonality
- Rural
- Isfahan, Fars(south), Khorasan, Mazandaran,
Khoozestan, Ilam, Boushehr - lower upper extremity,
- seasonalitySandfly bite in summer, clinical
manifestation from the mid fall till mid winter
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1385-1376
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1386-1376
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1389-1376
20OccurrenceIran Visceral
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21Life Cycle
- As nonmotile obligate intracellular (in
macrophage) amastigote in vertebrate including
human - As motile fllagelated extracellular promastigote
invitro in phlebotomines(sand flies)
22Reservoir
- Cutaneous
- Urban Human, Dog( accidental)
- Rural Rodents(gerbils,rats)
- Visceral
- Indian Human
- Mediteranean( Iran) Canidae( Dog, Fox)(from
human to human is possible by sand fly) - Africa Rodents
23Mode of Transmission
- Through bite of female sand fly from the infected
zoonotic reservoir - After feeding on an infected mammalian host,
motile promastigote develop multiply in gut in
8-20 days(10) - Carnivore with eating the carcasses of infected
animals - Person to person, transfusion sexual reported
but is rare - Contact of eye mucosa or open wound with infected
materials - Transmission of cutaneous leishmaniasis can be
- Person to person
- Animal to animal
- Animal to human vice versa
24Vector Sand fly
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28Ph Sergenti
29Ph Sergenti
30Ph Papatasi
31Ph Papatasi
32Ph Papatasi
33Ph Papatasi
34Ph Papatasi
35Ph Papatasi
36Ph Papatasi
37Ph Papatasi
38Incubation Period
- Cutaneous( at least one wk)
- Rural 1-4 wks
- Urban 2-8 mo( even 1-2 yrs)
- Visceral
- 2-6 mo( several wks to several mo, even 10 days
to years)
39Period of Communicability
- Cutaneous not typically transmitted from person
to person - Infectious to sand fly as long as parasites
remain in lesions( without Rx a few mo to 2 yrs) - Visceral
- Infectious to sand fly as long as parasites
remain in the circulating blood or skin of the
mammalian reservoir - Infectivity for sand fly may persist even after
clinical recovery of patient
40Clinical presentationCutaneous
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41Ph Sergenti
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44Susceptibility Resistance
- Cutaneous
- Susceptibility is general
- Tropica, Major Lifelong immunity( not
essentially with cross-immunity) - Visceral
- Susceptibility is general
- Lasting homologus immunity
- Inapparent subclinical infections are common
- Malnutrition predispose to clinical dx
activation of inapparent infections( AIDS
reactivation of latent infection)
45Methods of Control Prevention
- Detection rapid Rx( esp if human is reservoir)
- Residual insecticide( periodic)
- Sand fly has a short flight range is highly
susceptible to systematic spraying ( interior
exterior of doorways) - Eastern Spraying of breeding sites such as
stone walls, animal houses rubbish heaps)
46- Insecticide impregnated bed nets are under trial
- Screening( size not more than 0.89 mm,10 -12
holes per linear cm) - Eastern Eliminate rubbish heaps other breeding
places - Western
- Dog control, destroy gerbils their burrows
- Avoid thickly forested areas esp. after sundown
- Use insect repellents protective clothing
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49Control of Patientcutaneous
- Isolation quarantine none
- Concurrent disinfection none
- Treatment
- Pentavalent antimonials
- Meglumine antimonate( Glucantime)
- Na stibogluconate(pentostam)
- Pentamidine
- Imidazoles ketoconazole, itraconazole
- Amphotericin B (mucosal)
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??? ???? 2 ? 3 - ?????? ???? ???????????? ? ????
51Control of PatientVisceral
- Quarantine none
- Isolation Blood body fluid precautions
- Concurrent disinfection none
- Treatment
- Pentavalent antimonials
- Meglumine antimonate( Glucantime)
- Na stibogluconate(pentostam)
- Pentamidine
- Amphotericin B