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Review

Oral Zinc Supplementation for the Treatment of Acute Diarrhea in Children: A Systematic Review and Meta-Analysis

1
Department of International Health, Johns Hopkins Bloomberg School of Public Health, 615 N. Wolfe St, Baltimore, MD 21205, USA
2
Department of Health Policy and Management, School of Public Health, Peking University Health Science Centre, 38 Xueyuan Rd. in Haidian District, Beijing 10083, China
3
Centre for Population Health Sciences, University of Edinburgh Medical School, Teviot Place, Edinburgh, Scotland EH8 9AG, UK
*
Author to whom correspondence should be addressed.
Nutrients 2013, 5(11), 4715-4740; https://0-doi-org.brum.beds.ac.uk/10.3390/nu5114715
Submission received: 4 September 2013 / Revised: 9 October 2013 / Accepted: 4 November 2013 / Published: 21 November 2013
(This article belongs to the Special Issue Paediatric Nutrition)

Abstract

:
Evidence supporting the impact of therapeutic zinc supplementation on the duration and severity of diarrhea among children under five is largely derived from studies conducted in South Asia. China experiences a substantial portion of the global burden of diarrhea, but the impact of zinc treatment among children under five has not been well documented by previously published systematic reviews on the topic. We therefore conducted a systematic literature review, which included an exhaustive search of the Chinese literature, in an effort to update previously published estimates of the effect of therapeutic zinc. We conducted systematic literature searches in various databases, including the China National Knowledge Infrastructure (CNKI), and abstracted relevant data from studies meeting our inclusion and exclusion criteria. We used STATA 12.0 to pool select outcomes and to generate estimates of percentage difference and relative risk comparing outcomes between zinc and control groups. We identified 89 Chinese and 15 non-Chinese studies for the review, including studies in 10 countries from all WHO geographic regions, and analyzed a total of 18,822 diarrhea cases (9469 zinc and 9353 control). None of the included Chinese studies had previously been included in published pooled effect estimates. Chinese and non-Chinese studies reported the effect of therapeutic zinc supplementation on decreased episode duration, stool output, stool frequency, hospitalization duration and proportion of episodes lasting beyond three and seven days. Pooling Chinese and non-Chinese studies yielded an overall 26% (95% CI: 20%−32%) reduction in the estimated relative risk of diarrhea lasting beyond three days among zinc-treated children. Studies conducted in and outside China report reductions in morbidity as a result of oral therapeutic zinc supplementation for acute diarrhea among children under five years of age. The WHO recommendation for zinc treatment of diarrhea episodes should be supported in all low- and middle-income countries.

1. Introduction

In response to mounting evidence supporting the efficacy and effectiveness of therapeutic zinc supplementation for diarrhea among children under five years of age, the World Health Organization (WHO) and the United Nation’s Children Fund (UNICEF) issued a global recommendation in 2004, which advised zinc supplementation in addition to oral rehydration solution (ORS) for the treatment of all diarrhea episodes among children <5 years of age [1,2]. Systematic reviews have quantified the association between therapeutic zinc supplementation and a reduction in the duration and severity of childhood diarrhea episodes in low- and middle-income countries (LMICs) [1,3,4]. Many of the studies contributing to this body of evidence were conducted in South Asia [5,6,7], but literature stemming from East Asia has not been included in past reviews. In 2011, Zhang published a systematic review which identified 11 Chinese studies assessing zinc treatment for diarrhea and signified the need to update previous meta-analyses with literature published in languages other than English [8].
We sought to conduct an extensive search for studies of oral therapeutic zinc supplementation published in Chinese and any other language. We also aimed to combine evidence across regions in order to generate global estimates of the effect of oral therapeutic zinc supplementation on selected morbidity and mortality outcomes among children under five years of age.

2. Methods

We conducted a systematic literature search for studies published in any language between 1980 and November 2012 using the MeSH search terms “zinc” and “diarrhea” limited to “humans” in the following databases: Biosis, Cumulative Index to Nursing and Allied Health (CINAHL), Cochrane Central Register of Controlled Trials (CENTRAL), Embase, the WHO International Clinical Trials Registry Platform (ICTRP), Global Health, Latin American and Caribbean Health Sciences Literature (LILACS), PubMed, Scopus, Web of Science, IndMed, Egyptian Universities Library Consortium, Index Medicus for the Eastern Mediterranean Region (IMEMR), China National Knowledge Infrastructure (CNKI), WanFang, and Chinese BioMedical (CBM) database.
Titles and abstracts were reviewed by two independent reviewers, and complete manuscripts were obtained for further review of pertinent studies. Discrepancies were resolved in consultation with a third reviewer. We restricted inclusion to individually randomized controlled trials (RCTs) of children under five years of age with acute diarrhea, including dysentery, where diarrhea was defined as the passage of at least three loose or watery stools in a 24-h period. We excluded cluster RCTs, studies that exclusively enrolled a particular subgroup of children (e.g., HIV-infected children; preterm infants), and studies of persistent diarrhea. We included RCTs assessing oral zinc supplementation of any zinc salt in comparison to a control group receiving placebo supplement. For studies conducted in China, where placebo supplements may not have been readily available, we included trials in which cases received the same supportive therapy regardless of zinc allocation. For all studies, administration of minerals (excluding iron), vitamins, and supporting therapy beyond zinc were only considered acceptable if these were received by both the intervention and control groups. Studies that used supplements that included iron, zinc-fortified ORS, or zinc-fortified foods were excluded.
Included studies were reviewed for the following outcomes: diarrhea duration; the proportion of diarrhea episodes lasting >3 and >7 days; duration of hospitalization; duration of fever; duration of vomiting; proportion of cases vomiting; stool frequency (number per day); stool output (mL); and death from diarrhea or any cause. Two independent reviewers entered data into structured tables, and discrepancies were resolved in consultation with a third reviewer.
We conducted independent analyses for studies assessing diarrhea due to unspecified causes and those assessing specific pathogens (e.g., rotavirus) that were laboratory confirmed prior to enrollment. All data analyses were conducted in STATA 12.0 [9]. We fit Poisson and logistic regression models to continuous and binary outcomes, respectively, weighting all outcomes by sample size. These models generated pooled estimates and 95% confidence intervals lower bound by zero for all outcomes and upper bound by one for proportions.
For continuous outcomes, we calculated the overall percentage difference between the pooled estimates for the zinc and control groups. For binary outcomes, we calculated estimates of relative risk (RR) with placebo as the reference group and conducted random effects meta-analyses to combine RRs across studies [9].
We conducted hypothesis testing to assess the equivalence of pooled outcomes and of effect estimates by placebo and non-placebo controlled trials. To compare effect estimates, we tested the difference of mean percentage differences for continuous outcomes and the ratio of relative risks (RRR) for binary outcomes [10]. We subsequently pooled placebo and non-placebo controlled trials for outcomes with no statistically significant difference in effect size.
We assessed the association between the dose of oral zinc supplement and diarrhea duration by regressing the mean percentage difference in diarrhea duration comparing the zinc and control groups onto a categorical variable which indicated whether zinc dose was lower than, equal to, or greater than the WHO recommendation.
During the course of our analyses, we identified a zinc product called Licorzinc that appeared to be unique to China. To determine whether outcomes for Chinese studies were generalizable comparing Licorzinc to other better established zinc products, we conducted hypothesis testing to assess the equivalence of the mean percentage difference in episode duration between zinc and placebo. We also calculated the RRR to compare the RR of episodes lasting >3 days between studies using Licorzinc and other zinc products.
We plotted funnel plots to assess our primary outcomes for publication bias. We also employed the Child Health Epidemiology Reference Group (CHERG) grading system to assess the quality of evidence for each outcome on a four-point scale (“high”, “moderate”, “low”, “very low”) [11].

3. Results

The systematic literature search of the non-Chinese databases uncovered 4038 titles, and 15 were included after subsequent review of abstracts and full manuscripts for inclusion and exclusion criteria (Figure 1) [5,6,7,12,13,14,15,16,17,18,19,20,21,22,23]. Of the included studies, 13 were conducted in a hospital setting and two assessed episodes occurring in the community. Included studies were conducted in sites located within 10 countries: India (n = 6); Bangladesh (n = 5); Nepal (n = 1); Turkey (n = 1); Brazil (n = 1); Pakistan (n = 1); Ethiopia (n = 1); Yemen (n = 1); and Poland (n = 1). These studies enrolled a total of 3271 zinc-allocated and 3314 placebo-allocated diarrhea cases. The systematic literature search for Chinese studies resulted in 1520 titles, of which 89 were included (Figure 1) [24,25,26,27,28,29,30,31,32,33,34,35,36,37,38,39,40,41,42,43,44,45,46,47,48,49,50,51,52,53,54,55,56,57,58,59,60,61,62,63,64,65,66,67,68,69,70,71,72,73,74,75,76,77,78,79,80,81,82,83,84,85,86,87,88,89,90,91,92,93,94,95,96,97,98,99,100,101,102,103,104,105,106,107,108,109,110,111,112]. All included studies were conducted in a hospital setting, and 33 studies focused on diarrhea attributable to laboratory confirmed rotavirus. None of the included studies identified through the Chinese database were placebo-controlled; for Chinese studies, zinc and control groups received a range of supportive treatments, including fluid infusion, probiotics and antivirals. The total enrolment of included Chinese studies was 6198 zinc group and 6039 control group diarrhea cases. Table 1 describes the trial setting, sample size, and zinc intervention for all included studies.
Figure 1. Results of systematic literature search and review.
Figure 1. Results of systematic literature search and review.
Nutrients 05 04715 g001
Table 1. Characteristics of included studies.
Table 1. Characteristics of included studies.
Author [Reference]Year PublishedCountryTrial SettingSpecific Causative OrganismsAge Group (months)Sample SizeZinc SaltTablet or SyrupDaily Zinc DoseLength of Supplementation (days)
Zinc GroupControl Group
Al Sonboli [17]2003BrazilHospitalUnknown3–603737Not ListedTablet3–5 mos: 22.5 mg
6–60 mos: 45 mg
5
Bahl [7]2002IndiaCommunityUnknown6–35404401Zinc GluconateSyrup6–11 mos: 15 mg
12–35 mos: 30 mg
14
Brooks [16]2005BangladeshHospitalUnknown1–69193Zinc AcetateSyrup20 mgDuration of episode
Brooks [16]2005BangladeshHospitalUnknown1–69193Zinc AcetateSyrup5 mgDuration of episode
Dutta [23]2011IndiaHospitalUnknown6–244441Not ListedSyrup40 mg14
Elnemr [21]2007YemenHospitalUnknown3–248892Zinc AcetateSyrup20 mg14
Faruque [12]1999BangladeshHospitalUnknown6–24343341Zinc AcetateSyrup14.2 mg15
Fischer Walker [19]2006PakistanHospitalUnknown1–5281279Zinc SulfateTablet10 mg14
Fischer Walker [19]2006IndiaHospitalUnknown1–5186187Zinc SulfateTablet10 mg14
Fischer Walker [19]2006EthiopiaHospitalUnknown1–58790Zinc SulfateTablet10 mg14
Larson [18]2005BangladeshHospitalUnknown3–59267266Zinc SulfateTablet20 mg10
Patel [20]2009IndiaHospitalUnknown6–59264271Zinc SulfateSyrup20 mg14
Patro [22]2010PolandHospitalUnknown3–488179Zinc SulfateSyrup3–5 mos: 10 mg
6–48 mos: 20 mg
10
Polat [15]2003TurkeyHospitalUnknown2–295254Zinc SulfateSyrup20 mg10
Roy [13]1999BangladeshHospitalUnknown3–243235Zinc AcetateSyrup20 mg14
Sachdev [5]1988IndiaHospitalUnknown6–182525Zinc SulfateTablet40 mgNot Listed
Sazawal [6]1995IndiaHospitalUnknown6–35456481Zinc GluconateSyrup20 mgNot Listed
Strand [14]2002NepalCommunityUnknown6–35442449Not ListedSyrup6–11 mos: 15 mg
12–35 mos: 30 mg
From enrolment until 7 days after episode subsided
Zhao [24]2011ChinaHospitalUnknown4–364040LicorzincTablet4–5 mos: 10.8 mg
6–12 mos: 14.4 mg
13–36 mos: 21.6 mg
Not Listed
Zhang [25]2009ChinaHospitalRotavirus6–246060Zinc GluconateNot Listed20 mgDuration of episode
Lin [26]2010ChinaHospitalRotavirus1.5–365858Zinc GluconateSyrup1.5–5 mos: 10 mg
6–36 mos: 20 mg
Duration of episode
Zhou [27]2010ChinaHospitalRotavirus6–244240Zinc GluconateNot Listed20 mg14
Yang [28]2011ChinaHospitalUnknown3–364240Zinc GluconateTablet3–5 mos: 10 mg
6–36 mos: 20 mg
10–14
Liu [29]2010ChinaHospitalUnknown5–184040Zinc GluconateNot Listed5 mos: 10 mg
6–18 mos: 20 mg
10–14
Chen [30]2006ChinaHospitalRotavirus0–243030Zinc gluconateNot Listed10 mgNot Listed
Liu [31]2011ChinaHospitalUnknown6.8–229090Zinc GluconateTablet20 mgNot Listed
Liu [32]2009ChinaHospitalUnknown6–36112108Zinc GluconateTablet20 mg10
Fu [33]2010ChinaHospitalRotavirus2–2498102Zinc GluconateSyrup5 mgNot Listed
Zhou [34]2008ChinaHospitalUnknown2–484040LicorzincNot Listed2–5 mos: 7.5 mg
6–12 mos: 11.25 mg
13–48 mos: 18.75 mg
10–14
Chen [35]2008ChinaHospitalRotavirus4–486060LicorzincNot Listed4–5 mos: 7.2 mg
6–48 mos: 10.8 mg
Not Listed
Guan [36]2012ChinaHospitalRotavirus1.5–45.64545Licorzinc Not Listed1.5–5 mos: 7.5 mg
6–11 mos: 11.25 mg
12–45.6 mos: 18.75 mg
10–14
Wu [37]2010ChinaHospitalRotavirus4–134646LicorzincNot Listed4–5 mos: 10 mg
6–13 mos: 20 mg
Not Listed
Zhou [38]2010ChinaHospitalUnknown6–246560LicorzincTablet20 mgNot Listed
Luo [39]2009ChinaHospitalrotavirus6–365550LicorzincTablet18.75 mgNot Listed
Zhang [40]2010ChinaHospitalUnknown5–485050LicorzincNot ListedNot Listed *Not Listed
Ju [41]2007ChinaHospitalUnknown6–364038LicorzincTablet6–12 mos: 11–25 mg
13–36 mos: 15 mg
Not Listed
Wang [42]2012ChinaHospitalUnknown6–363030LicorzincTabletNot Listed *3
Hong [43]2009ChinaHospitalRotavirus3–60140120Zinc SulfateSyrup3–11 mos: 20 mg
12–36 mos: 30 mg
37–60 mos: 40 mg
Not Listed
Lin [44]1994ChinaHospitalUnknown0.5–244658Zinc SulfateSyrup10–14 mg/kg *Not Listed
Yan [45]2011ChinaHospitalUnknown5–367050Zinc SulfateSyrup5 mos: 50 mg
6–36 mos: 100 mg
Not Listed
He [46]1997ChinaHospitalUnknown6–365258Zinc GluconateNot Listed20 mgNot Listed
Wei [47]2011ChinaHospitalUnknown3–364442Zinc GluconateSyrup3–5 mos: 10 mg
6–36 mos: 20 mg
10–14
Yang [48]2012ChinaHospitalUnknown0–368080Zinc GluconateTablet0–5 mos: 10 mg
6–36 mos: 20 mg
10
Pu [49]2010ChinaHospitalRotavirus0–243834Zinc GluconateNot Listed0–5 mos: 10 mg
6–24 mos: 20 mg
Not Listed
Zhang [50]2011ChinaHospitalRotavirus3–365353Zinc GluconateNot Listed3–5 mos: 10 mg
6–36 mos: 20 mg
10
Sun [51]2008ChinaHospitalUnknown1.5–364545Zinc GluconateSyrup1.5–5 mos: 10 mg
6–36 mos: 20 mg
Not Listed
Zhang [52]2011ChinaHospitalUnknown3–369090Zinc GluconateSyrup3–5 mos: 10 mg
6–36 mos: 20 mg
Not Listed
Lin [53]2010ChinaHospitalRotavirus6–542820Zinc GluconateTablet6–54 mos: 20 mg14
Liu [54]2009ChinaHospitalUnknown3–369591Zinc GluconateNot Listed3–5 mos: 10 mg
6–36 mos: 20 mg
10–14
Qiao [55]2011ChinaHospitalUnknown6–367372Zinc GluconateTablet6–36 mos: 20 mg14
Zhang [56]2007ChinaHospitalUnknown0–248590Zinc GluconateNot Listed0–5 mos: 10 mg
6–24 mos: 20 mg
10
Zhao [57]2012ChinaHospitalUnknown0–247070Zinc GluconateSyrup0–5 mos: 10 mg
6–24 mos: 20 mg
10–14
Cai [58]2011ChinaHospitalUnknown0–248884Zinc GluconateNot Listed0–5 mos: 10 mg
6–24 mos: 20 mg
14
Zhang [59]2012ChinaHospitalRotavirus6–17120120Zinc GluconateTablet20 mg10–14
Qiao [60]2012ChinaHospitalUnknown0–248585Zinc GluconateNot Listed0–5 mos: 10 mg
6–24 mos: 20 mg
10
Zhong [61]2012ChinaHospitalRotavirus3–485050Zinc GluconateTablet 3–5 mos: 10 mg
6–48 mos: 20 mg
10
Wang [62]2011ChinaHospitalRotavirus0–246060Zinc GluconateNot Listed0–5 mos: 10 mg
6–24 mos: 20 mg
10
Yang [63]2008ChinaHospitalRotavirus0–36164168Zinc GluconateNot Listed0–5 mos: 10 mg
6–36 mos: 20 mg
10
Zhao [64]2012ChinaHospitalRotavirus6–366060Zinc GluconateSyrup35 mg10
Ma [65]2012ChinaHospitalRotavirus4–424141Zinc GluconateNot Listed20 mgNot Listed
Chen [66]2012ChinaHospitalRotavirus0–369393Zinc GluconateNot Listed0–5 mos: 10 mg
6–36 mos: 20 mg
10
Hu [67]2009ChinaHospitalRotavirus4–366060Zinc GluconateTablet4–5 mos: 10 mg
6–36 mos: 20 mg
10
Yuan [68]2011ChinaHospitalUnknown1–36100100Zinc GluconateTablet1–12 mos: 70 mg
13–36 mos: 140 mg
14
Tan [69]2011ChinaHospitalUnknown3–365035Zinc GluconateTablet3–5 mos: 10 mg
6–36 mos: 20 mg
10–14
Liu [70]2010ChinaHospitalUnknown0–368977Zinc GluconateSyrup0–5 mos: 10 mg
6–36 mos: 20 mg
10
Hu [71]2011ChinaHospitalUnknown3–60108100Zinc GluconateTablet3–5 mos: 10 mg
6–60 mos: 20 mg
14
Li [72]2008ChinaHospitalUnknown6–364038Zinc GluconateTablet6–12 mos: 7.5 mg
13–36 mos: 15 mg
3
Gao [73]2012ChinaHospitalUnknown3–367474Zinc GluconateNot Listed3–5 mos: 10 mg
6–36 mos: 20 mg
14
Wu [74]2011ChinaHospitalUnknown3–602020Zinc SulfateSyrup10 mg10
Wu [74]2011ChinaHospitalUnknown3–602020Zinc SulfateNot Listed10 mg10
Liu [75]2011ChinaHospitalUnknown3–605453Zinc GluconateTablet3–5 mos: 10 mg
6–60 mos: 20 mg
3–5
Chen [76]2010ChinaHospitalUnknown5–364220Zinc GluconateNot Listed5 mos: 10 mg
6–36 mos: 20 mg
10–14
Ma [77]2012ChinaHospitalUnknown2–366363Zinc GluconateNot Listed2–5 mos: 70 mg
6–36 mos: 140 mg
10–14
Lu [78]2012ChinaHospitalUnknown6–18120140Zinc GluconateNot Listed140 mg10–14
Ma [79]2012ChinaHospitalUnknown6–365852Zinc GluconateSyrup6–36 mos: 20 mg10
Ao [80]2012ChinaHospitalRotavirus0–248780Zinc GluconateSyrup0–5 mos: 10 mg
6–24 mos: 20 mg
Not Listed
Gu [81]2011ChinaHospitalUnknown3–605660Zinc GluconateSyrup3–5 mos: 10 mg
6–60 mos: 20 mg
10
Wen [82]2006ChinaHospitalUnknown0–243029Zinc GluconateNot Listed20 mg10–14
Wang [83]2011ChinaHospitalUnknown3–366060LicorzincNot Listed10–20 mg *Duration of episode
Liu [84]2012ChinaHospitalRotavirus8–309090LicorzincNot Listed8–30 mos: 20 mgNot Listed
Liu [85]2012ChinaHospitalUnknown3–60100100LicorzincTablet3–5 mos: 10 mg
6–60 mos: 20 mg
Not Listed
Tong [86]2011ChinaHospitalUnknown2–369898LicorzincNot Listed2–5 mos: 10 mg
6–36 mos: 20 mg
Not Listed
Qiu [87]2010ChinaHospitalRotavirus1–245352LicorzincTablet1–5 mos: 10 mg
6–24 mos: 20 mg
14
Kong [88]2011ChinaHospitalUnknown3–303535Zinc GluconateTablet3–5 mos: 10 mg
6–11 mos: 15 mg
12–30 mos: 20 mg
14
He [89]2007ChinaHospitalRotavirus5–226063Zinc GluconateNot Listed20 mgNot Listed
Kang [90]2010ChinaHospitalRotavirus6–369280Zinc GluconateTablet20 mg14
Su [91]2012ChinaHospitalRotavirus6–369797Zinc GluconateNot Listed20 mgNot Listed
Huang [92]2010ChinaHospitalRotavirus2–36100100Not ListedTablet2–5 mos: 10 mg
6–36 mos: 20 mg
Not Listed
Zhang [93]2006ChinaHospitalUnknown0–368363LicorzincSyrup0–5 mos: 10 mg
6–36 mos: 20 mg
10–14
Wang [94]2012ChinaHospitalUnknown4–306060Zinc GluconateSyrup10 mgNot Listed
Lin [95]2008ChinaHospitalUnknown0.5–346060Zinc GluconateTablet0.5–5 mos: 140 mg
6–34 mos: 280 mg
10–14
Yan [96]2011ChinaHospitalUnknown6–605757Zinc GluconateTablet20 mg10
Yu [97]2012ChinaHospitalUnknown0–364040Zinc GluconateTablet0–5 mos: 10 mg
6–36 mos: 20 mg
10–14
Zhang [98]2011ChinaHospitalRotavirus4–36128128Zinc GluconateSyrup4–5 mos: 10 mg
6–36 mos: 20 mg
14
Xu [99]2010ChinaHospitalRotavirus2–368483Zinc GluconateNot Listed2–5 mos: 10 mg
6–36 mos: 20 mg
14
Tan [100]2010ChinaHospitalUnknown3.5–605555Zinc GluconateSyrup3.5–5 mos: 10 mg
6–60 mos: 20 mg
10–14
Shen [101]2012ChinaHospitalRotavirus2.5–404642Zinc GluconateNot Listed2.5–5 mos: 10 mg
6–40 mos: 20 mg
Duration of episode
Wang [102]2010ChinaHospitalUnknown6–485251Zinc GluconateTablet20 mgNot Listed
Chen [103]2011ChinaHospitalUnknown1–365050Zinc GluconateTablet1–5 mos: 5 mg
6–36 mos: 10 mg
Not Listed
Meng [104]2012ChinaHospitalUnknown0–249090Zinc GluconateTablet0–5 mos: 2.5 mg
6–12 mos: 5 mg
13–24 mos: 10 mg
Not Listed
Zhong [105]2010ChinaHospitalUnknown1–246060Zinc GluconateTablet1–5 mos: 2.5 mg
6–12 mos: 5 mg
13–24 mos: 7.5 mg
5–7
Xie [106]2010ChinaHospitalRotavirus6–36128124Zinc GluconateTablet20 mgNot Listed
Fan [107]2012ChinaHospitalUnknown0–36163121Not ListedNot Listed0–5 mos: 10 mg
6–36 mos: 20 mg
10
Zhou [108]2012ChinaHospitalRotavirus6–247575Zinc GluconateSyrup20 mg10–14
Zhao [109]2008ChinaHospitalUnknown0–364443Zinc GluconateTablet0–5 mos: 10 mg
6–24 mos: 20 mg
Not Listed
Wan [110]2006ChinaHospitalUnknown6–362624Not ListedNot ListedNot ListedNot Listed
Yang [111]2012ChinaHospitalUnknown6–606060Not ListedNot Listed20 mgNot Listed
Luo [112]2012ChinaHospitalUnknown0–36168196Not ListedNot Listed0–5 mos: 10 mg
6–36 mos: 20 mg
Not Listed
* Study not included in dose analyses.
The results of the studies identified through non-Chinese databases are summarized in Table 2 and Table 3. Acute episodes were 4% (95% CI: 1%–8%) shorter in duration among children treated with zinc compared to those receiving placebo (Table 2). Among children hospitalized for diarrhea, the duration of hospitalization was reduced by 37% (95% CI: 21%–53%) comparing the zinc and control groups (Table 2). Stool frequency was decreased by 6% (95% CI: 2%–10%) among zinc-treated children. Zinc-treated children had a reduced relative risk (RR) of acute diarrhea lasting beyond three and seven days and an increased risk of vomiting (RR: 1.83; 95% CI: 1.40–2.39) (Table 3).
Table 2. Pooled means of select outcomes for non-Chinese studies.
Table 2. Pooled means of select outcomes for non-Chinese studies.
OutcomeStudy Sites 1Pooled Mean (95% CI) 2Percent Difference 3
NZinc GroupControl Group(%)
Duration of Episode (days)133.51 (3.43–3.60)3.67 (3.59–3.76)−4.4 (−7.8, −1.0)
Duration of Hospitalization (days)12.00 (1.99–2.01)3.17 (2.38–3.96)−36.9 (−52.6, −21.2)
Stool Output (mL)2391.2 (388.5–393.8)388.8 (386.2–391.5)0.6 (−0.3, 1.6)
Stool Frequency (Number per day)65.04 (4.88–5.19)5.36 (5.20–5.52)−6.0 (−9.9, −2.0)
1 Individual studies may contribute more than one study site (N) to each estimate; 2 Estimates for ≥2 study sites generated by Poisson regression model weighted by sample size; 3 Percent difference calculated by: 100 × ((Pooled Zinc Estimate − Pooled Control Estimate)/Pooled Control Estimate); 95% CI calculated by: Percent Difference ± 1.96 × {|(meanzinc/meancontrol)| × sqrt[(std errorzinc)2/(meanzinc)2 + (std errorcontrol)2/(meancontrol)2]} × 100.
Table 3. Pooled relative risk of select outcomes for non-Chinese studies.
Table 3. Pooled relative risk of select outcomes for non-Chinese studies.
OutcomeStudy Sites 1Pooled Estimate Percentage (95% CI) 2Pooled Relative Risk 3
NZinc GroupControl GroupRR (95% CI)
Episodes >3 days (%)329.7 (26.7–32.7)39.5 (36.3–42.7)0.78 (0.67–0.90)
Episodes >7 days (%)610.3 (8.9–11.7)14.9 (13.2–16.5)0.74 (0.55–0.99)
Vomiting (%)318.8 (16.0–21.6)9.4 (7.3–11.4)1.83 (1.40–2.39)
1 Individual studies may contribute more than one study site (N) to each estimate; 2 Estimates for ≥2 study sites generated by logistic regression model weighted by sample size; 3 Estimates for ≥2 studies generated by random effects meta-analysis.
Outcomes pooled across studies conducted in China showed reductions in the duration of diarrhea, hospitalization, fever, vomiting, stool output and stool frequency among zinc-treated children with acute diarrhea attributable to rotavirus and to non-specific causes (Table 4). The reduction in the duration of diarrhea was 37% (95% CI: 35%–39%) among non-specific episodes and 31% (95% CI: 29%–34%) among rotavirus episodes (Table 4). The RR of diarrhea lasting beyond three days was reduced among zinc-treated patients with non-specific (RR: 0.73; 95% CI: 0.66–0.79) and rotavirus (RR: 0.70; 95% CI: 0.63–0.78) diarrhea (Table 5; Figure 2 and Figure 3).
Table 4. Pooled means of select outcomes for Chinese studies.
Table 4. Pooled means of select outcomes for Chinese studies.
OutcomeSpecific Causative PathogensStudy Sites 1Pooled Mean
(95% CI) 2
Percent Difference 3
NZinc GroupControl Group(%)
Duration of Episode (days)Unknown402.96 (2.90–3.03)4.68 (4.60–4.77)−36.8 (−38.7, −34.8)
Rotavirus243.45 (3.36–3.54)5.01 (4.89–5.12)−31.1 (−33.5, −28.8)
Duration of Hospitalization (days)Unknown104.65 (4.50–4.80)6.43 (6.25–6.61)−27.7 (−30.8, −24.6)
Rotavirus24.15 (3.79–4.51)6.1 (5.66–6.54)−32.0 (−39.6, −24.3)
Duration of Fever (days)Unknown131.90 (1.80–1.99)2.81 (2.70–2.92)−32.4 (−36.5, −28.2)
Rotavirus41.96 (1.78–2.14)3.18 (2.95–3.41)−38.4 (−45.6, −31.2)
Duration of Vomiting (days)Unknown61.15 (1.05–1.25)1.53 (1.41–1.64)−24.8 (−33.3, −16.4)
Rotavirus31.84 (1.64–2.04)2.49 (2.26–2.72)−26.1 (−36.6, −15.6)
Stool Output (mL)Unknown140 (38.1–41.9)70 (68.0–72.0)−42.9 (−46.0, −39.7)
Rotavirus1278.4 (256.8–300.0)425.4 (382.1–468.7)−34.6 (−42.9, −26.2)
Stool Frequency (Number per day)Unknown14 (3.8–4.2)8 (7.6–8.4)−50.0 (−53.5, −46.5)
Rotavirus23.74 (3.30–4.18)4.27 (3.77–4.77)−12.4 (−27.0, 2.1)
1 Individual studies may contribute more than one study site (N) to each estimate; 2 Estimates for ≥2 study sites generated by Poisson regression model weighted by sample size; 3 Percent difference calculated by: 100 × ((Pooled Zinc Estimate − Pooled Control Estimate)/Pooled Control Estimate); 95% CI calculated by: Percent Difference ± 1.96 × {|(meanzinc/meancontrol)| × sqrt[(std errorzinc)2/(meanzinc)2 + (std errorcontrol)2/(meancontrol)2]} × 100.
Table 5. Pooled relative risk of select outcomes for Chinese studies.
Table 5. Pooled relative risk of select outcomes for Chinese studies.
OutcomeSpecific Causative PathogensStudy Sites 1Pooled Estimate Percentage (95% CI) 2Relative Risk 3
NZinc GroupControl GroupRR (95% CI)
Episodes >3 days (%)Unknown4431.4 (29.4–33.5)49.2 (46.6–51.8)0.73 (0.66–0.79)
Rotavirus2931.8 (29.5–34.1)50.3 (47.4–53.3)0.70 (0.63–0.78)
Episodes >7 days (%)Unknown126.9 (-)39.2 (-)0.75 (0.42–1.37)
1 Individual studies may contribute more than one study site (N) to each estimate; 2 Estimates for ≥2 study sites generated by Poisson regression model weighted by sample size; 3 Estimates for ≥2 studies generated by random effects meta-analysis.
We did not identify any studies reporting diarrhea-specific or all-cause mortality for inclusion in this review. Nor did we identify non-Chinese studies reporting duration of fever or vomiting, or Chinese studies reporting the proportion of children vomiting.
The mean episode duration and proportion of episodes lasting >3 days were not statistically significantly different comparing zinc-treated children in Chinese and non-Chinese studies. There was no statistically significant difference between the estimated relative risk of an episode lasting >3 days (RRR: 1.07; 95% CI: 0.90–1.27) comparing Chinese and non-Chinese studies; therefore, we pooled this outcome across regions (RR: 0.74; 95% CI: 0.68–0.80) (Figure 3). The percentage difference between the mean episode duration of zinc-treated and control group children was statistically significantly larger for Chinese compared to non-Chinese studies (p < 0.05), so this outcome was not pooled across regions. We did not have sufficient power to compare other commonly reported outcomes by region.
Figure 2. Forest plot for the effect of therapeutic zinc supplementation on Rotavirus diarrhea episodes >3 days.
Figure 2. Forest plot for the effect of therapeutic zinc supplementation on Rotavirus diarrhea episodes >3 days.
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Zinc dose was not associated with the mean percent difference in diarrhea duration comparing zinc and control children for non-Chinese (p = 0.50) or Chinese (p = 0.12) studies. Comparing Chinese studies that used Licorzinc to those that used other zinc supplements, there were no statistically significant differences in the mean percent difference in the duration of rotavirus episodes (p = 0.56), the RR of non-specific episodes lasting >3 days (RRR: 0.99; 95% CI: 0.72–1.35), or the RR of rotavirus episodes lasting >3 days (RRR: 0.93; 95% CI: 0.68–1.26). The percentage difference in the mean duration of non-specific episodes comparing zinc and control group children was statistically significantly higher for Licorzinc compared to “other zinc” studies (p = 0.01).
Our assessment of publication bias yielded largely symmetrical funnel plots for all outcomes.
Under the CHERG grading system, the studies included in this review were of moderate quality (Table 6) [11]. Effect estimates were largely consistent in directionality for all outcomes.
Figure 3. Forest plot for the effect of therapeutic zinc supplementation on non-specific diarrhea episodes lasting >3 days.
Figure 3. Forest plot for the effect of therapeutic zinc supplementation on non-specific diarrhea episodes lasting >3 days.
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Table 6. Quality assessment of studies measuring the association between therapeutic zinc supplementation and selected outcomes.
Table 6. Quality assessment of studies measuring the association between therapeutic zinc supplementation and selected outcomes.
Number of StudiesDesignLimitationsConsistencyDirectness
Generalizability to Population of InterestGeneralizability to Intervention of Interest
Diarrhea Duration (mean): Moderate outcome-specific quality 1
53 non-specific
24 Rotavirus
RCTChinese studies not placebo-controlled (−0.5)All but 4 studies showing decreased mean duration of diarrhea among zinc-treated children (+1)Mostly South Asia and China (−0.5)Generalizable
Diarrhea Duration (>3 days): Moderate outcome-specific quality 1
47 non-specific
29 Rotavirus
RCTChinese studies not placebo-controlled (−0.5)All studies showing decreased risk of diarrhea duration >3 days among zinc-treated children (+1)Mostly South Asia and China (−0.5)Generalizable
Diarrhea Duration (>7 days): Moderate outcome-specific quality 1
7 non-specificRCTChinese studies not placebo-controlled (−0.5)All but one study showing decreased risk of diarrhea duration >7 days among zinc-treated children (+1)Mostly South Asia and China (−0.5)Generalizable
Hospitalizations Duration: Moderate outcome-specific quality 1
11 non-specific
2 Rotavirus
RCTChinese studies not placebo-controlled (−0.5)All studies showing decreased mean duration of hospitalization among zinc-treated children (+1)Only one non-Chinese study (−0.5)Generalizable
Stool Output: Moderate outcome-specific quality 1
3 non-specific
1 Rotavirus
RCTChinese studies not placebo-controlled (−0.5)All but one study showing decreased stool output among zinc-treated children (+1)Only South Asia and China (−0.5)Generalizable
Stool Frequency: Moderate outcome-specific quality 1
7 non-specific
2 Rotavirus
RCTChinese studies not placebo-controlled (−0.5)All but three studies showing decreased stool frequency among zinc-treated children (+1)Mostly South Asia and China (−0.5)Generalizable
Vomiting: Moderate outcome-specific quality1
3 non-specificRCTNoneAll studies showing increased vomiting among zinc-treated children (+1)No Chinese studies (−0.5)Generalizable
Vomiting Duration: Moderate outcome-specific quality1
6 non-specific
3 Rotavirus
RCTChinese studies not placebo-controlled (−0.5)All but one study showing decreased duration of vomiting among zinc-treated children (+1)No non-Chinese studies (−0.5)Generalizable
Fever Duration: Moderate outcome-specific quality1
13 non-specific
4 Rotavirus
RCTChinese studies not placebo-controlled (−0.5)All studies showing decreased duration of fever among zinc-treated children (+1)No non-Chinese studies (−0.5)Generalizable
1 Quality assessment scoring based on previously published criteria [11].

4. Discussion

The findings of our systematic review confirm and highlight the benefits of therapeutic zinc supplementation for diarrhea among children under five years of age in low- and middle-income countries. The effects of zinc treatment, which include reductions in episode duration, stool output, stool frequency and length of hospitalization, were consistent across Chinese and non-Chinese studies and non-specific and rotavirus diarrhea. These results suggest that zinc therapy of diarrhea is largely beneficial and important in both low- and middle-income settings.
The results of the large number of Chinese trials in rotavirus diarrhea are a substantial addition to the global evidence base because there have been no non-Chinese trials. One study in India based on a post-hoc subgroup analysis suggested that zinc treatment was not beneficial for rotavirus diarrhea [113]; however, the evidence from China demonstrates that therapeutic zinc supplementation reduces the duration and severity of rotavirus episodes. As rotavirus is the predominant cause of severe acute diarrhea worldwide and most likely the leading cause of diarrhea mortality [114], zinc treatment of rotavirus diarrhea could potentially yield large reductions in hospitalizations and deaths.
In comparison to non-Chinese studies, the difference between the mean episode duration of zinc-treated and control group children was statistically significantly higher for Chinese studies (p < 0.05). It is possible that this difference resulted from lack of placebo-controlled groups and blinding among Chinese studies. However, estimates of the effects of therapeutic zinc supplementation on other outcomes were largely consistent across study locations and we were able to generate a pooled global effect size for the proportion of episodes >3days. The consistency of effect estimates between studies conducted in and outside China suggests that the lack of placebo-controlled groups in Chinese studies did not greatly bias the results.
Zinc dose did not affect the estimate of the effect of zinc supplementation on the duration of diarrhea for non-Chinese or Chinese studies. Although Licorzinc was associated with slightly greater reductions in the mean duration of non-specific diarrhea than other zinc products, zinc effect sizes were generally comparable across Chinese studies regardless of type of zinc preparation.
There is a dearth of literature meeting our inclusion criteria that assessed diarrhea-specific and all-cause mortality. Although a previous review published mortality effect estimates [4], the sole study reporting diarrhea-specific deaths was cluster-randomized and thus violated our inclusion criteria [115]. In addition, three studies of all-cause mortality were also excluded from our review; one was on persistent diarrhea [116], and two others were review papers [3,117].
Using previously published scoring criteria, the studies included in our review yielded pooled estimates of overall moderate quality [11]. The majority of studies contributing to this review were conducted in China and South Asia; however, studies conducted outside Asia were consistent in the directionality of effect estimates. The consistency and quality of all outcomes bolsters the evidence in support of oral zinc supplementation for the treatment of acute diarrhea among children under five in low- and middle-income countries.

5. Conclusions

Oral therapeutic zinc supplementation reduces the morbidity of acute diarrhea among children under five in and outside China. Global efforts should be made to support scale-up of the WHO recommended regimen of therapeutic zinc in all regions.

Authors’ Contributions

LML conducted the systematic review of non-Chinese studies, analysis and led the initial manuscript preparation. CLFW assisted with the analysis and the manuscript preparation. KC and WYJ conducted the systematic review of Chinese studies. REB conceptualized the idea and assisted with the interpretation of the analysis and the final manuscript preparation.

Acknowledgments

We would like to thank Wei-Ju Chen, Xun Luo and Wenze Zhang for reviewing and abstracting data from Chinese publications. Financial support for this review was provided by the Bill and Melinda Gates Foundation to the US Fund for UNICEF for the ongoing work of the Child Health Epidemiology Reference Group (CHERG).

Conflicts of Interest

The authors declare no conflict of interest.

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MDPI and ACS Style

Lamberti, L.M.; Walker, C.L.F.; Chan, K.Y.; Jian, W.-Y.; Black, R.E. Oral Zinc Supplementation for the Treatment of Acute Diarrhea in Children: A Systematic Review and Meta-Analysis. Nutrients 2013, 5, 4715-4740. https://0-doi-org.brum.beds.ac.uk/10.3390/nu5114715

AMA Style

Lamberti LM, Walker CLF, Chan KY, Jian W-Y, Black RE. Oral Zinc Supplementation for the Treatment of Acute Diarrhea in Children: A Systematic Review and Meta-Analysis. Nutrients. 2013; 5(11):4715-4740. https://0-doi-org.brum.beds.ac.uk/10.3390/nu5114715

Chicago/Turabian Style

Lamberti, Laura M., Christa L. Fischer Walker, Kit Y. Chan, Wei-Yan Jian, and Robert E. Black. 2013. "Oral Zinc Supplementation for the Treatment of Acute Diarrhea in Children: A Systematic Review and Meta-Analysis" Nutrients 5, no. 11: 4715-4740. https://0-doi-org.brum.beds.ac.uk/10.3390/nu5114715

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