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Severe Plasmodium Falciparum Malaria: Utility of Exchange Transfusion

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Bay Area Mobile Apheresis Program (BAMAP) San Francisco, California Background Infections due to malaria estimated 1.0-2.5 million deaths/yr. – PowerPoint PPT presentation

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Title: Severe Plasmodium Falciparum Malaria: Utility of Exchange Transfusion


1
Severe Plasmodium Falciparum Malaria Utility
of Exchange Transfusion
  • JC Hofmann, MD SJ Smith, RN RM Rohe, RN DD
    Kiprov, MD
  • Division of Immunotherapy
  • California Pacific Medical Center
  • Bay Area Mobile Apheresis Program (BAMAP)
  • San Francisco, California

2
Background
  • Infections due to malaria ? estimated 1.0-2.5
    million deaths/yr.
  • Most malaria deaths due to plasmodium
    falciparum.
  • Non-immune travelers and children lt 5 y.o.
    susceptible to severe
  • infection.
  • Case fatality rate of imported falciparum
    malaria 0.6-3.8.
  • Progression from asymptomatic infection to
    death 36-48 hrs.
  • Among U.S. civilians who die of malaria ? dx
    missed in 40.
  • severe falciparum malaria ? altered
    consciousness, jaundice, severe normocytic
    anemia, oliguria, hypoglycemia, multiorgan
    failure, and parasitemia gt 5.

3
Treatment
  • Severe Falciparum Malaria
  • ICU management for close monitoring.
  • Blood smears Q 12 hrs. until parasitemia
    levels lt 1.
  • Antimalarial drugs
  • quinoline derivatives quinine, quinidine,
    chloroquine, mefloquine.
  • antimicrobials clindamycin, doxycycline,
    tetracycline.
  • antifolates sulfonamides, dapsone,
    pyrimethamine.
  • artemisinin derivatives artemisinin,
    artemether.

4
Adjunctive Treatment
  • RBC exchange transfusion (ET) recommended in
    falciparum infection
  • Parasitemia gt 10.
  • In coma, renal failure, or ARDS, regardless of
    parasitemia level.
  • ET removes parasitized RBCs, parasitic toxins,
    cytokines.
  • ET should be combined with drug therapy ?
    parasitemia lt 5.
  • Phillips et al (1990) ET not proven to
    enhance survival.
  • Riddle et al (2002) meta-analysis no
    greater survival rate with using ET compared to
    antimalarials alone.
  • No RCT has yet been performed.

5
Patients
  • 3 patients diagnosed with severe falciparum
    malaria in 11 months (referred for RBC exchange
    transfusion)
  • 44-68 y.o. and non- or partially-immunized
    travelers.
  • 67 patients were female.
  • visited rural sub-Saharan Africa in prior 30
    days.
  • experienced a 4-5 day h/o flu-like symptoms.
  • 33 patients had prior h/o falciparum malaria.

6
Patients
  • 3 patients diagnosed with severe falciparum
    malaria
  • presented with moderately severe hypotension,
    anemia, thrombocytopenia.
  • 67 patients experienced mental status
    abnormalities, renal insufficiency, hematuria,
    and cholestasis (1 patient had mild DIC).
  • 1 patient fulfilled criteria for cerebral
    malaria.

7
Treatment
  • IV quinidine (/- IV doxycycline) for 8-24 hrs.
    prior to receiving single RBC exchange
    transfusion (8-10 units of RBCs).
  • Premedication acetaminophen, diphenylhydramine,
    hydrocortisone.
  • Mean volume of RBCs exchanged 2777 ml
    (2500-3060 ml).
  • Average FCR (fraction cells remaining) 33
    (27-42).

8
Results
  • Significant ? level of parasitemia
  • Initial mean parasitemia 38 (10-90).
  • Mean parasitemia (prior to RBC exchange
    transfusion) 8 (5-15).
  • Mean parasitemia (6-12 hrs. after treatment)
    1.1 (0.3-2.0).
  • Dramatic improvement in clinical status
  • Significant resolution of fever, chills,
    hypotension, mental status abnormalities,
    nausea, and abdominal pain.
  • 67 patients able to tolerate oral quinine and
    doxycycline after single RBC exchange
    transfusion.

9
Table I Demographics Outcomes of Patients
with Severe Falciparum Malaria
Patient Demographics Clinical Progression Treatment Outcome
45 y.o. female ICU nurse PMH h/o severe RA on MTX infliximab. No prophylaxis 2 wks. in rural Mali, Africa. F/C, H/A, myalgias, LH ? exp. aphasia, seizures ? obtundation coma. hypotensive, ?plt, mild DIC hematuria, ecchymoses. received pRBC, FFP, plt. IV quinidine/IV doxycycline (48) (parasitemia ? 90 ? 5) 8U pRBC exch. transfusion (D3) (parasitemia 5 ? 0.3) FCR 30 D/c to home (d9) No neuro deficits. Back to work (d21)
44 y.o. African male PMH h/o prior f. malaria (2 yrs. ago) on prophylaxis. No prophylaxis 3 wks. in Cameron, Africa. fatigue, flu-like sxs X 5d ? somnolent, min. responsive hypotensive (on pressors). anemic ? received pRBC. PO quinine/PO doxycycline (6) ? IV quinine/IV doxycycline (6) (parasitemia 15 ? 10) 10U pRBC exch transfusion (D1) (parasitemia 10 ? lt 1.0) FCR 42 D/c to home (d7) No neuro deficits.
68 y.o. female scientist PMH h/o HTN, DM, hypothyroidism. Partial prophylaxis 4 days in rain forest (6 wk. in Nairobi, Kenya). F/C, flu-like sxs X 4d ? syncope X2, lethargic ? somnolent. anemic ? received pRBC. IV quinidine/IV doxycycline (24) (parasitemia 10 ? 9) 8U pRBC exch. transfusion (D2) (parasitemia 9 ? 2.0) FCR 27 D/c to home (d6) No neuro deficits.
10
Summary
  • In patients with severe plasmodium falciparum
    malaria, RBC exchange transfusion
  • is useful in removing parasitized RBCs,
    toxins, and cytokines.
  • should be instituted if parasitemia gt 10,
    and continued until parasitemia lt 5.0 .
  • may be life saving.
  • Adequate immunization is extremely important
    when traveling to endemic areas.

11
Parasite Density
  • 1) Calculate the of parasites per 200 WBC on a
    thick smear.
  • 2) Divide the total WBC count by 200.
  • 3) Multiply the parasites in 1) by the result
    in 2) parasites/uL.
  • 4) parasitemia parasites/uL divided by the
    WBC.
  • Ex thick smear 10 parasites/200 WBC and
    WBC8000/uL, 8000/200 40. 10 parasites X 40
    400 parasites/uL. Percent parasitemia 400/8000
    5.
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