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Zinc and Malaria

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Title: Zinc and Malaria


1
Zinc and Malaria
  • Davidson H. Hamer, M.D.
  • Division of Geographic Medicine and Infectious
    Diseases
  • Tufts-New England Medical Center,
  • Tufts University Friedman School of Nutrition
    Science and Policy, and
  • Center for International Health
  • Boston U. School of Public Health

2
Beneficial Effects of Zinc
  • Zinc supplementation beneficial for growth,
    especially stunted or underweight children
  • Zinc supplementation has been found to be
    effective for the prevention of
  • Acute and persistent diarrhea
  • Acute respiratory infections

3
Zinc and Malaria Background
  • Murine models have shown that zinc deficiency can
    exacerbate
  • Malaria parasitemia
  • Mortality
  • Lipid peroxidation during infection
  • Arif et al. Indian J Malariol 1987 Shankar FASEB
    J 1995
  • Papua New Guinea and Malawi
  • Associations between zinc status, anemia, and
    malaria suggest that zinc status is inversely
    correlated with P. falciparum malaria
  • Gibson et al. Am J Clin Nutr 1991 Gibson et al.
    AJCN 1998

4
Zinc and Prevention of Malaria
Placebo-Controlled Trials (1)
  • The Gambia
  • N 110 children aged 6 to 28 months
  • Twice weekly supplementation with 70 mg zinc
    reduced Pf malaria-attributable health center
    attendance by 30 (p.09) (impact greatest after
    the first month p0.054)
  • Bates et al. Brit J Nutr 199369243-55.
  • Papua New Guinea
  • N 274 children aged 6 to 60 months
  • Zinc gluconate (10 mg/d given 6 days/week) for a
    total of 46 weeks
  • Primary outcome number of slide-confirmed
    Pf-attributable clinic-based febrile episodes
  • Shankar AS et al. Am J Trop Med Hyg,
    200062663-9.

5
Summary of Effects of Zinc on Malaria Morbidity
in Papua New Guinea
  • 38 (95 CI 3 to 60, p0.034) reduction in
    Pf-attributable health center attendance
  • 69 (95 CI 27 to 86, p0.009) reduction in Pf
    attacks with parasitemia gt100,000/?L
  • No effect on P. vivax episodes
  • No consistent effects on parasite density,
    hemoglobin, spleen rates, or prevalence, and no
    evidence of age specificity
  • Shankar AS et al. Am J Trop Med Hyg,
    200062663-9.

6
Zinc and Prevention of Malaria Placebo-Controlled
Trials (2)
  • Burkina Faso
  • N 709 children between 6 to 31 months of age
  • Zinc sulfate (12.5 mg/day given 6 days/week)
    supplemented during the rainy season (about 6
    months)
  • Primary outcome clinical episodes of Pf malaria
    defined as axillary temperature ?37.5ºC and
    ?5,000 parasites/?L
  • Muller O et al. Brit Med J 20013221-6.

7
Burkina Faso Study Results
  • No difference in P. falciparum incidence, even
    when different parasitemia cutoff points were
    used
  • No difference in duration or severity of malaria
    episodes
  • Fewer children died in the Zn than in the P group
  • (5/341 vs. 12/344 p 0.1)
  • Serum zinc was significantly higher in the zinc
    group after 3 months of supplementation
  • 15.3 ?mol/L (Zn) vs. 12.4 ?mol/L (P)

8
Why Are There Conflicting Results?
  • Population studied in Burkina Faso had lower
    levels of subclinical zinc deficiency
  • Mean baseline plasma zinc concentration 77.0
    ?g/dL and was even higher after 3 months of
    supplementation (in contrast to deficiency cutoff
    point of 60 ?g/dL)
  • Duration of supplementation may have been too
    short in Burkina Faso (6 mo vs. 48 weeks in PNG)
  • Possible benefit seen in Burkina Faso in terms of
    malariometric indices (Pf prevalence and density
    of parasitemia)

9
Zinc Against Plasmodium (ZAP) Study
10
ZAP StudyMethods
  • Multicenter, randomized, double-blind,
    placebo-controlled clinical trial of children
    aged 6-59 months with
  • Axillary temperature ?37.5C
  • Blood smear with ? 2000/mm3 asexual forms of P.
    falciparum
  • Children were treated with standard antimalarial
    therapy plus zinc sulfate or placebo for 3 days
  • 20 mg/d of zinc for infants lt12 mo
  • 40 mg/d for children 12-60 mo

11
ResultsPrimary Outcomes
  • Zinc and placebo groups were similar at baseline
  • Zinc sulfate was well tolerated
  • Time to resolution of fever similar in the two
    groups
  • Zinc 24.2 and placebo 24.0 hours (p 0.37)
  • Proportion of children with reduction of
    parasitemia by ?75 was similar in the two groups
  • Zinc 73.4 and placebo 77.6 (p 0.11)
  • No differences between treatment groups after
    controlling for baseline plasma zinc, nutritional
    status, and parasitemia

12
ResultsSecondary Outcomes
  • No differences between the zinc and placebo
    groups in terms of
  • Proportion of children aparasitemic at 72 hours,
    days 7, 14, and 28
  • Hemoglobin levels at days 7, 14, and 28
  • Plasma zinc levels increased more in the zinc
    supplemented group than in the control group

13
Baseline Plasma Zinc Levels By Baseline
Parasitemia Quartile
200
150
Plasma Zinc (?g/dL)
100
50
0
1
2
3
4
Parasitemia Quartile
14
Discussion
  • Potential explanations for the lack of efficacy
    of zinc in the ZAP study include
  • Study population was not zinc deficient
  • Unlikely given low plasma zinc levels and high
    phytate diets common in these countries
  • Longer duration of supplementation may be needed
    to result in improvements in immune function
  • Too small a dose of zinc was used
  • However, higher doses may be harmful
  • High levels of chloroquine treatment failures

15
Future Studies of Zinc and Malaria
  • Determine whether there is a beneficial effect of
    zinc for the prevention of morbidity due to
    falciparum malaria
  • Evaluation of combinations of zinc with vitamin A
    or iron versus use of a multiple micronutrient
    supplement
  • To evaluate whether the beneficial effects of
    vitamin A and zinc are additive or synergistic
  • To determine whether the use of zinc helps to
    limit the increase in malaria parasitemia seen
    during iron replacement
  • To evaluate the impact on anemia and growth in
    children in malaria-endemic regions
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