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1 CONTINUED FROM PART 1 1

2 LYNNE S. GARCIA, MS, CLS, FAAM CAPHLD 65 th Institute Future Challenges in Diagnostic Medical Parasitology SPONSOR: MEDICAL CHEMICAL CORPORATION 2

3 MALARIA PATIENT: LABORATORY ER Evening & night shifts (always a STAT request) Hematology - microbiology? (late shift responsibility) Finger stick to venipuncture (organism morphology changes) (parasites continue to grow in EDTA!!) Automated hematology instruments vs manual examination (test request format); low parasitemia Thick and/or thin blood films (prepare, read); controls Lack of technical expertise (generalist/specialist) Risk management issues (recognition of STAT!) 3

4 Parasitemia Light Microscopy % (5-20/µl) = Positive thick film % (100/µl) = Naïve patients may be symptomatic below this level; remember emergency room patients - travelers 0.2% (10,000/µl) = Level above which immune patients exhibit symptoms; 0.1% (5,000) = BinaxNOW (maximum sensitivity) 2% (100,000/µl) = Maximum parasitemia of P. vivax, P. ovale (young RBCs only) rarely exceeds 2% 2-5% (100, ,000/µl) = Hyperparasitemia, severe malaria, increased mortality 10% (500,000/µl) = Exchange transfusion, high mortality

5 BLOOD PARASITE STAINS Color Variations 5 Patient thick/thin blood films are own controls; WBCs look good = parasites look good.

6 NORMOCYTIC VS MACROCYTIC RBCS Plasmodium falciparum Normocytic Plasmodium vivax Macrocytic 6

7 EXTRACELLULAR FORMS Parasites and Platelets Babesia spp. Extracellular Forms 7 Make sure you know what platelets look like artifact situation. Actual parasites must have both nuclear and cytoplasmic colors.

8 Examination Possibilities RBCs Intraerythrocytic protozoa Plasmodium spp. Babesia spp. Extraerythrocytic protozoa Babesia spp. Trypanosoma spp. Extraerythrocytic helminth Microfilariae 8

9 Examination Possibilities WBCs 9 Within WBCs Leishmania donovani Toxoplasma gondii Outside of WBCs Toxoplasma gondii Trypanosoma spp. Top: Leishmania; Bottom: Toxoplasma

10 Plasmodium vivax 10

11 Plasmodium ovale P. ovale curtisi, P. ovale wallikeri 11

12 Plasmodium malariae 12

13 Plasmodium falciparum 13 Exflagellation can occur in any Plasmodium spp.

14 Plasmodium knowlesi Characteristics 24 hr (simian malaria); most rapid cycle of the 5 Tends to infect any RBC; heavy infection ; severe All sizes of RBCs; Duffy factor like P. vivax No Schüffner s dots (stippling); clumpy dots later on Delicate rings, may have two dots of chromatin/ring, appliqué or accolé forms; may have two rings/rbc Band form trophozoites commonly seen Gametocytes round, tend to fill the cell Early stages = P. falciparum; later stages = P. malariae 14

15 Plasmodium knowlesi Endemic Areas 15 Sarawak (Malaysian Borneo), Singapore, Thai-Myanmar border; Philippines, Yunnan Province in China; Finland, New York, Australia, Netherlands (travelers-endemic areas)

16 16

17 MIXED MALARIAL INFECTIONS More common than thought Thailand: 30% both P. falciparum, P. vivax Africa: P. falciparum, P. malariae (Malaysia/ P. knowlesi Gambian children: <1% to >60% mixed infections New Guinea: all four species (confirmed by PCR) Anopheles mosquitoes: can transmit two species at the same time 17 Difficult to detect Different parasite levels, low organism densities, confusion among morphologic criteria PCR becoming test of choice for ID to species level

18 ANTIGEN DETECTION TESTS External controls now available. TEST PRINCIPLE Detection of HRPII Antigen SPECIES IDENTIFIED P. falciparum, P. vivax BinaxNOW Alere Scarborough P. falciparum Sensitivity/Specificity 99.7% / 94.2%* P. vivax Sensitivity/Specificity 93.5% / 99.8% Maximum sensitivity - parasitemia >5,000 (parasites/µl) = 0.1% 18

19 Parasitemia Light Microscopy % (5-20/µl) = Positive thick film % (100/µl) = Naïve patients may be symptomatic below this level; remember emergency room patients - travelers 0.2% (10,000/µl) = Level above which immune patients exhibit symptoms; 0.1% (5,000) = BinaxNOW (maximum sensitivity) 2% (100,000/µl) = Maximum parasitemia of P. vivax, P. ovale (young RBCs only) rarely exceeds 2% 2-5% (100, ,000/µl) = Hyperparasitemia, severe malaria, increased mortality 10% (500,000/µl) = Exchange transfusion, high mortality

20 PLASMODIUM SPP. Report Comments Plasmodium spp. seen: Unable to rule out Plasmodium falciparum or Plasmodium knowlesi Plasmodium spp. not seen: One negative set of blood films will NOT rule out malaria; submit additional blood specimens every 4-6 hours. Plasmodium spp. seen, possible mixed infection: Unable to rule out Plasmodium falciparum or P. knowlesi NOTE: It is mandatory that the parasitemia be calculated and reported for every initial and subsequent positive set of malarial films the same method for determining parasitemia must be used for all blood film sets on that particular patient. 20

21 BABESIA SPP. Ixodes scapularis Babesia divergens: Europe Rare, but 42% mortality Babesia microti: US, parts of Europe, Japan Northeast, south to New Jersey; 5% mortality Most cases mild; more severe in immunosuppressed WA1, CA1, MO1 (Babesia divergens-like), states Very serious in splenectomized patients Related to canine pathogen, B. gibsoni WA1, CA5: Now Babesia duncani More pathogenic than B. microti 21

22 Other blood parasites: Babesia spp. 22 Artifacts Plasmodium falciparum

23 CUTANEOUS LEISHMANIASIS IN U.S. MILITARY PERSONNEL Afghanistan, Iraq, Kuwait: >1000 cases Cases isoenzyme analysis: L. major Consider cutaneous leishmaniasis skin lesions (Southwest/Central Asia) Almost all with CL infected in Iraq Decrease risks Improve living conditions, heighten awareness, protective measures (permethrin- treated clothes, bed nets; exposed skin, repellent 30-35% DEET, dusk to dawn, vector control) 23

24 CUTANEOUS LEISHMANIASIS : CLINICAL PRESENTATION 24

25 MUCOCUTANEOUS LEISHMANIASIS L. mexicana Complex Common throughout Mexico, Belize, Guatemala and southern United States (Arizona, Texas) Forest rodents (wood rats) are important hosts Prolonged exposure = chicleros live in forest collecting chewing gum latex (30% infected in first year), timber cutters, road builders, farm workers Two culture-positive and four PCR-pos rodents Leishmania-positive. Isolates extend geographic and ecologic range of enzootic leishmaniasis in the United States and represent a new host record. Now in Tucson, Arizona. 25

26 MUCOCUTANEOUS LEISHMANIASIS 26

27 CUTANEOUS LEISHMANIASIS: DIAGNOSIS 27 Organism isolation by smear or culture; histology Lesion sampling: dental broach, slit scrape method, aspiration of lesion edge (multiple samples required), biopsy Tissue sampling better than other smearing techniques; culture positive in 80% of cases LD bodies seen in about 30% of patients; many lymphocytes/plasma cells in wet ulcerative lesions; dry lesions = granulomas / fewer cells

28 AMERICAN TRYPANOSOMIASIS (No longer South American) Chagas Disease Trypanosoma cruzi Transmission infective organisms in feces of blood-sucking triatomid bugs (kissing bugs, reduviid bugs) Bug s feces contact site of bug bite or mucus membranes; transfusions, congenital infections Mexico, Central, South, and North America (Texas, California); rural areas; dogs, cats, opossums, rodents, armadillos important reservoir hosts 28

29 Spread of Triatomid Bugs 29

30 CONFIRMED BLOOD DONATIONS: CHAGAS DISEASE 30

31 TRYPANOSOMIASIS, AMERICAN CLINICAL DISEASE Initial infection often asymptomatic evidence years later as chronic form of disease; acute disease more common in children Unilateral periorbital edema (Romaña s sign) Local lesion followed by fever, lymphadenopathy, hepatosplenomegaly, myocarditis, meningoencephalitis Chronic disease = cardiomyopathy, congestive heart failure or arrhythmias; dilation of esophagus or colon; MEGASYNDROME 31

32 32

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