Post on 15-Jan-2016
One day WorkshopYUMS
|Tissue and Blood Protozoan diseases
Malaria & Leishmaniasis
Mohammad Amin Ghatee
Ph.D in medical Parasitology
MALARIA THE KILLER DISEASEMALARIA THE KILLER DISEASE
•
•The majority of victims are children and pregnant women. (one African child every 30 seconds)
• Sub-Saharan Africa bears 90 per cent of the burden.
• 500 million people suffer from malaria
•Over one million of people die each year.
Plasmodium species which infect humans
Plasmodium falciparum (tertian)
Plasmodium vivax (tertian)
Plasmodium malariae (quartian)
Plasmodium ovale (tertian)
Geographical distribution and incidence of malaria
Figure 23.10
Plasmodium species
• Plasmodium falciparum: Tropics. Accounts for 50% of all malaria cases. Most pathogenic.
• Plasmodium vivax: Tropics, subtropics, and some temperate regions.. About 43% of all malaria cases. Some Africans are refractory to infection because the lack the red cell receptor that the parasite use to enter.
• Plasmodium malariae: Tropics. About 7% of all malaria cases.
• Plasmodium ovale: West Africa. Rare.
HOSTSHOSTS
DEFINITIVE HOST:DEFINITIVE HOST: Anopheline female Mosquito (sexual Anopheline female Mosquito (sexual reproduction)reproduction)
INTERMEDIATE HOST:INTERMEDIATE HOST: Humans (asexual and sexual phases) Humans (asexual and sexual phases)
Malaria Life Cycle
Types of Infections
• Recrudescence– exacerbation of persistent undetectable parasitemia, due to
survival of erythrocytic forms, no exo-erythrocytic cycle (P.f., P.m.)
– Blood origin– Can be occurred along the life time
• Relapse– reactivation of hypnozoites forms of parasite in liver, separate
from previous infection with same species (P.v. and P.o.)– Tissue (liver) origin– Up to 3-5 years after primary infection
Erythrocytic phasestages of parasite in RBC
• Young trophozoites or ring form• Tropohozoite • forms merozoites• Schizogeny to forms merozoites releasing merozoites into
blood stream.
• Merozoites invade other RBCs and schizongeny is repeated• Parasite density increases until host’s immune response
slows it down• Merozoites may develop into gametocytes (gametogony),
the sexual forms of the parasite
Development in the mosquito
• Upon ingestion with a blood meal, both the micro and macrogametocyte rapidly mature
• Macrogamete is released from ruptured rbc
• Microgametocyte rapidly undergoes multiple nuclear divisions to form 8 gametes
• Exflagellation
Development in the mosquito: the ookinete
A mature A mature ookineteookinete. A number of organelles are shown. . A number of organelles are shown. The nucleus can be seen at the lower end of the organism. The nucleus can be seen at the lower end of the organism. There are abundant ribosomes in the area above the There are abundant ribosomes in the area above the nucleus and endoplasmic reditulum can also be seen. The nucleus and endoplasmic reditulum can also be seen. The zygote is surrounded by a three-layered pellicle. The apical zygote is surrounded by a three-layered pellicle. The apical complex at the upper end includes numerous rhoptries and complex at the upper end includes numerous rhoptries and micronemes (dark spots). micronemes (dark spots). Image from Sinden RE. Image from Sinden RE. "Malaria", Topics in Inernational Health,(1998) The WellcomeTrust, CABI Publishing, CAB International
Development in the mosquito
• Encysted ookinete transforms into oocycst
• 10-14 days of development • reductional nuclear
division, haploid again• multiplication to form
1000’s of sporozoites
THE OOCYSTTHE OOCYST
SEM which shows two oocysts on the outer wall of SEM which shows two oocysts on the outer wall of the midgut of a mosquito. These contain the midgut of a mosquito. These contain developing developing P. gallinaciumP. gallinacium sporozoites. sporozoites.Image from Guggehheim R."Malaria", Topics in Inernational Health,(1998) The WellcomeTrust, CABI Publishing, CAB International)
Anopheles gambiae, the deadliest malaria vector (top), and blue-colored Plasmodium oocysts, appearing from the mosquito’s gut. (MOSQUITO ENGINEERING:Building a Disease-Fighting Mosquito. Martin Enserink/Science 2000 290: 440-441. (in News Focus)
Schizogenic periodicity and fever patterns
• Schizogenic periodicity is length of asexual erythrocytic phase– 48 hours in P.f., P.v., and P.o. (tertian)– 72 hours in P.m. (quartian)
• Initially may not see characteristic fever pattern if schizogony not synchronous.
• With synchrony, periods of fever or febrile paroxsyms assume a more definite 3 (tertian)- or 4 (quartian)- day pattern.
Clinical presentation
• Early symptoms– Headache– Malaise– Fatigue– Nausea– Muscular pains– Slight diarrhea– Slight fever– Photophobia– Anorexia
• Could mistake for influenza or gastrointestinal infection
Paroxysm of malaria
• Malaria tertiana: 48h between fevers (P. vivax and ovale)
• Malaria quartana: 72h between fevers (P. malariae)
• Malaria tropica: irregular high fever (P. falciparum)
Malaria Paroxysm
Disease Severity Pv Po Pm Pf Paroxysm Severity
moderate to severe
mild mild to
moderate severe
Average (per mm3)
20,000 9,000 6,000 50,000-500,000
Maximum (per mm3)
50,000 30,000 20,000 2,500,000
Anemia ++ + ++ ++++ Duration
Disease Infection
3-8 w 5-8 y*
2-3 w 12-20 m*
3-24 w >20 y
2-3 w 6-17 m
Complications renal cerebral**
*true relapses ( recrudescence) due to dormant hypnozoite stage in liver **plus many other organs
Malaria the disease
Irritability, loss of reflexes, neurological symptoms similar to menigitis, coma20% fatality
Progressive severe dropof hematocrit, poor oxygenSupply for organs andtissues
Dwindling urine, high ureaLevel in serum
Cerebral malaria Severe anemia Renal failure
3 Severe manifestations
Knobs and cytoadherence • Cytoadhrence and rosetting
correlates with the presence of “knobs” (left column) on the surface of the infected RBC
• The right column shows a RBC infected with a knob-less strain which does not cause cerebral malaria
• Knobs are made up of parasite derived proteins
knobs knob-less
Cerebral Malaria PossiblePathophysiology
cytoadherence
cerebral ischemia
hypoxia, metabolic effects,
cytokines (eg, TNF-)
coma
death
Severe anaemia - pathogenesis• Erythrocyte destruction
during schizogony (destruction of both parasitized and nonparasitized erythrocytes)
• Erythrophagocytosis in spleen
• Immune mediated response
• Black water fever• Bone marrow suppression
Spleen
Other severe complications
• Pulmonary oedema
• Renal insufficiency (nephrotic syndrome)– P. malariae
• Haemolysis
• Thrombocytopaenia, DIC
• Superinfections (secondry infection)– Septicaemia
• Protective immunity to malaria is primarily a premunition.
• In highly endemic areas, infants are protected by maternal antibodies, and young children are at greatest risk after weaning.
Immunity and Resistance in malaria
Genetically resistance factors
• Sickle cell anemia, favism, and thalassemia
can cause resistance to infection by P. f
-Duffy blood groups and P. v
Modes of transmission
• 1. Natural or biological transmission
• 2. Accidental transmission:
blood transfusion
sharing of needles by IV drug users
3. Maternal transmission
Malaria Diagnosis
Clinical Diagnosis:• Symptoms: fever, chills,
headache, malaise, etc.• History of being in
endemic area• Splenomegaly and
anemia as disease progresses
Laboratory diagnosis:• Microscopic demonstration of parasite in blood smear (distinguish species)• thick film: more sensitive• thin film: species identification easier
• Fluorescent microscopy• antigen detection ‘dipstick’• Serology• Polymerase Chain Reaction
Malaria Diagnosis
1.Touch 3 drops of blood to a clean slide.
2.Spread the drops to make a 1 cm circle.
3.Touch a fresh drop of blood to the edge of another slide.
6.Wait for both to dry before fixing and staining.
5.Pull the drop of blood across the first slide in one motion.
4.Carry the drop of blood to the first slide and hold at 45degree angle.
Malaria Blood Smear
• Remains the gold standard for diagnosis• Giemsa stain• distinguishes between species and life cycle stages• parasitemia is quantifiable
• Requirements: equipment, training, reagents, supervision
• Simple, inexpensive yet labor-intensive• Accuracy depends on laboratorian skill
Interpreting Thick and Thin Films
• THICK FILM– lysed RBCs– larger volume– 0.25 μl blood/100 fields– blood elements more
concentrated– good screening test– positive or negative– parasite density– more difficult to diagnose
species
• THIN FILM– fixed RBCs, single layer
– smaller volume
– 0.005 μl blood/100 fields
– good species differentiation
– requires more time to read
– low density infections can be missed
Malaria Parasite Erythrocytic Stages
Ring form
TrophozoiteSchizont
Gametocytes
Plasmodium falciparum
Rings: double chromatin dots, multiple infections in same red cell
Gametocytes: mature (M)andimmature (I) forms
Trophozoites: compact
Schizonts: 16-24 merozoites(rarely seen in peripheral blood)
Infected erythrocytes: normal size, maurers cleft, discrimination of P. falciparum from other species is a important, because P. falciparum in blood of non-immune case is a medical emergency.
M I
Plasmodium vivax
Trophozoites: ameboid; deforms the erythrocyte
Gametocytes: round-oval Schizonts: 12-24 merozoites
Rings
Infected erythrocytes: enlarged up to 2X; deformed; (Schüffner’s dots))
Plasmodium ovaleInfected erythrocytes: moderately enlarged (11/4 X); fimbriated; oval; (Schüffner’s dots)
“malariae - like parasite in vivax - like erythrocyte”
Rings
Trophozoites: compact
Schizonts: 6-12 merozoites;(usually 8) dark pigment
Gametocytes: round-oval
Infected erythrocytes: size normal to decreased (3/4X), Zeimanns dots
Plasmodium malariae
Trophozoite:compact
Trophozoite:typical band form
Schizont:6-12 merozoites (usually 8);
coarse, dark pigment ; (“rosettes”)
Gametocyte:round; coarse,dark pigment
Malaria Serology – antibody detection
Antibodies to asexual parasites appear some days after invasion of RBCs and may persist for months
• Positive test indicates past infection
• Not useful for treatment decisions– Investigating congenital malaria, esp. if
mom’s smear is negative
Malaria Antigen Detection• Immunologic assays to detect specific antigens• Commercial kits now available as
immunochromatographic rapid diagnostic tests (RDTs), used with blood
• P. falciparum histidine-rich protein 2 (PfHRP-2)• parasite LDH (pLDH)
• Monoclonal and polyclonal antibodies used in antigen (Ag) capture test
• Species- and pan-specific Ab• Cross reactivity with rheumatoid factor reportedly
corrected
Detection of Plasmodium antigens
Polymerase Chain Reaction (PCR))
• Molecular technique to identify parasite genetic material
• Uses whole blood collected in anticoagulated tube (200 µl) or directly onto filter paper (5 µl)
• Definitive species-specific diagnosis now possible
Treatment
• Chloroquine
• Primaquine
• Quinine
• Artemisinins
• Blood schizonticides:
1-Rapid acting:
Chloroquine, Amodiaquine, Quinine, Quinidine, Mefloquine, Atovaquone, Artemisinin
2- Slow acting: Antifolates(Fansidar, proguanil) , Clindamycin, Tetracyclines, Proguanil
Tissue schizonticides: Primaquine , Proguanil
Gametocidal: Primaquine
Anti – relapsing: Primaquine
Selected Anti-Malarials
Chinchona the source of quinine
• Peruvian Indians appear to have been the first to know about the medicinal effects of quinine.
• They chewed Chinchona bark while working in the mines as forced laborers for the Spanish
Malaria Drug Therapy in Iran
First day: Chloroquine 600 mg (4 tab), 6 h later: 300 mg
Second day: Chloroquine 300 mg
Third day: Chloroquine 300 mg & Primaquine 45 mg (3 tab)
Plasmodium falciparum & Plasmodium malariae infections
Vaccine
• Radiated sporozoite
• Sporozoite recombinant proteins
• Spf66: synthethic polypeptides of merozoites
• RTS,S: recombinant HBV surface protein and parasite proteins