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Poor vitamin D status and the risk of maternal depression: a dose–response meta-analysis of observational studies

Published online by Cambridge University Press:  18 December 2020

Quansheng Tan
Affiliation:
Human Resource Department, Jingmen No. 2 People’s Hospital, Jingmen, Hubei448000, China
Shuai Liu
Affiliation:
Department of Disease Control and Prevention, Health and Family Planning Commission of Wuhan Municipality, Wuhan, Hubei430030, China
Dajie Chen*
Affiliation:
Department of Social Medicine and Health Management, School of Public Health, Tongji Medical College, Huazhong University of Science and Technology, Wuhan, Hubei430030, China
*
*Corresponding author: Email [email protected]
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Abstract

Objective:

The association between 25-hydroxyvitamin D (25(OH)D) and maternal depression (MD) is deemed to be inconclusive. The current analysis aimed to quantify the relationship between 25(OH)D serum concentrations, the main indicator of vitamin D nutritional status, and MD.

Design:

Dose–response meta-analysis.

Setting:

A systematic search in PubMed, Embase and Web of Science from inception to June 2019.

Participants:

Relevant observational studies reporting risk estimates and 95 % CI of random effects for 25(OH)D concentration on MD were identified.

Results:

Twelve observational studies with thirteen independent reports involving 10 317 pregnant women were included. Compared with the lowest category of 25(OH)D, the pooled OR for the highest category of MD was 0·49 (95 % CI 0·35, 0·63); a high heterogeneity was observed (P = 0·001, I2 = 82·1 %). A non-linear association between 25(OH)D and MD was found (P for non-linearity = 0·001); the dose–response analysis indicated that the lowest pooled OR was at blood 25(OH)D concentrations of 90–110 nmol/l. Subgroup analyses suggested a stronger association between 25(OH)D and MD in summer time (OR 0·25, 95 % CI 0·08, 0·43) than in other seasons (OR 0·68, 95 % CI 0·52, 0·83) (P for interaction = 0·008). A visual inspection of funnel plot and Begg’s and Egger’s tests did not indicate any evidence of publication bias.

Conclusions:

Low circulating 25(OH)D is associated with MD, and our analysis suggests that they influence each other. Further randomised controlled trials would be needed to determine the direction of causation.

Type
Review Article
Copyright
© The Authors 2020

Depression is a common mental disorder and a leading cause of disability worldwide(1). It has been reported that 350 million people around the world are affected by depression, and as many as two-thirds of all persons who committed suicide may have had this condition(Reference Ledford2). Women of child-bearing age are more vulnerable to suffer from depression due to strong biological, physical and social changes they experience(Reference Marcus3). Approximately 15–30 % and 10–40 % of women experience depression during pregnancy and postpartum, respectively(Reference Marcus, Flynn and Blow4Reference Savitz, Stein and Ye7). Maternal depression (MD) (including antepartum depression and postpartum depression) is associated with adverse offspring development, such as preterm birth, low birth weight, intrauterine growth restriction, birth defects and low intelligence(Reference Grote, Bridge and Gavin8Reference Schneuer, Roberts and Guilbert10). During pregnancy, women need to provide nutrition for the growth and development of the fetus as well as for their own metabolic needs; hence, the demand for vitamins increases. However, due to reduced outdoor activities and sunlight exposure, pregnant women obtain less vitamin D from sun exposure, thereby making them susceptible to vitamin D deficiency. Over the past decades, the relationship between poor vitamin D status – as measured by serum concentration of the intermediary metabolite, 25-hydroxyvitamin D (25(OH)D) – and depression has been a research hotspot.

The aetiology of depression is not fully established; however, genetic, biological and environmental reasons, such as nutritional deficiency and inadequate sunlight exposure, are considered potential factors that could play a role in its pathophysiology(Reference Saveanu and Nemeroff11). Depression is associated with dysregulated hypothalamic–pituitary–adrenal axis function, overactivity of the sympatho-adrenal system and increased level of inflammatory markers(Reference Amini, Jafarirad and Amani12,Reference Cassidy-Bushrow, Peters and Johnson13) . Vitamin D, vitamin D receptors, vitamin D-activating enzyme 1α-hydroxylase and other vitamin D-related components play an important role in regulating neuronal function, neurotransmitter synthesis, inhibiting apoptosis and regulating neuron regeneration and differentiation(Reference Garcion, Wion-Barbot and Montero-Menei14Reference Fernandes de Abreu, Eyles and Feron16), which have been associated with cognitive impairment and depressive symptoms.

The most widely accepted indicator of vitamin D status is blood 25(OH)D concentrations, the intermediary metabolite of vitamin that circulates after dietary or vitamin D synthesised in the skin after sun exposure is hydroxylated in the liver. Some epidemiological studies were conducted to evaluate the association between serum 25(OH)D and MD. However, the results have been inconclusive. Some studies have found that 25(OH)D has a protective effect on MD and recommended vitamin D supplement use for pregnant women(Reference Accortt, Schetter and Peters17,Reference Williams, Romero and Clinton18) , while other studies did not report a uniform relationship(Reference Nielsen, Strom and Boyd19,Reference Gould, Anderson and Yelland20) . In addition, the association of serum 25(OH)D concentrations with optimal mental health remains unknown. We, therefore, performed a dose–response meta-analysis of observational studies to describe the epidemiological evidence on the relationship between 25(OH)D and MD, and explored supplemental doses of vitamin D required to achieve the lowest risk of MD.

Methods

Search strategy

We comprehensively conducted a literature search of PubMed, Embase and Web of Science from inception to June 2019 for studies addressing the associations between 25(OH)D and MD based on the Meta-analysis Of Observational Studies in Epidemiology guidelines(Reference Stroup, Berlin and Morton21). We used the following search terms without restriction: ‘antenatal’ or ‘prepartum’ or ‘prenatal’ or ‘prepartal’ or ‘peripartum’ or ‘perinatal’ or ‘postpartum’ or ‘postnatal’ or ‘puerperal’ or ‘puerperium’ or ‘pregnant’ or ‘pregnancy’ or ‘gravida’ or ‘gestation’ or ‘gestational’ or ‘maternal’ (Mesh) and ‘vitamin D’ or ‘25-hydroxyvitamin D’ or ‘25(OH)D’ or ‘cholecalciferol’ or ‘ergocalciferol’ or ‘ergosterol’ or ‘7-dehydrocholesterol’ (Mesh) and ‘depression’ or ‘depressive symptoms’ or ‘mood disorders’ or ‘mood disturbance’ or ‘mood symptoms’ or ‘mental disorders’ or ‘mental health’ or’ psychological disorders’. Additionally, we reviewed reference lists of retrieved articles to identify additional relevant studies.

Study selection

Two investigators (D.C. and Q.T.) independently screened all articles. Studies that met the following criteria were included: (i) the study design was observational; (ii) 25(OH)D concentrations were estimated and MD was the outcome variable; (iii) the study reported OR or relative risk with 95 % CI for the association between 25(OH)D and MD, or provided sufficient information to allow for their calculation. The studies were limited to English language; non-human studies, clinical trials, reviews, letters and commentaries were excluded. If study populations were reported more than once, we included the result with the longest follow-up time; any result in one study stratified by the season of 25(OH)D measurement was treated as separate reports. Any discrepancy was solved through discussion with the third reviewer (S.L.).

Definition of depression and 25-hydroxyvitamin D measurement

Our primary outcome for all studies was depression diagnosed by one of the following: (i) a clinical diagnosis; (ii) a diagnosis using a validated rating scale with an established cut-off point, such as the twenty-one-item Depression, Anxiety and Stress Scales, or Center for Epidemiological Studies Depression Scale, or Beck Depression Scale, or Edinburgh Postnatal Depression Scale. The cut-off point of the twenty-one-item Depression, Anxiety and Stress Scale, Center for Epidemiological Studies Depression Scale and Beck Depression Scale was 14, 16 and 17, respectively, while that of Edinburgh Postnatal Depression Scale was diverse in different studies, ranging from 6 to 13.

In two studies, cord blood sample was collected to analyse the concentrations of 25(OH)D; many studies showed that maternal 25(OH)D levels are highly correlated with cord blood 25(OH)D concentrations; mean cord blood 25(OH)D concentrations approximated half of maternal 25(OH)D levels(Reference Bouillon, Van Baelen and De Moor22,Reference Lamb, Lutenbacher and Wallston23) . So we converted 25(OH)D concentrations from cord blood to maternal blood with a conversion factor of 2(Reference Bouillon, Van Baelen and De Moor22,Reference Lamb, Lutenbacher and Wallston23) . Meanwhile, we converted 25(OH)D concentrations from ng/ml to nmol/l with a conversion factor of 2·5.

Data extraction

Data extraction was conducted independently by two authors (D.C. and Q.T.). Information such as name of first author, year of publication, study location, number of participants, number of cases, study design and characteristics of study population at baseline (age and race) was extracted from the included studies. In addition, the duration of follow-up for cohort study, methods of exposure measurements and outcome measurements, risk estimates and corresponding 95 % CI, and covariates adjusted in the statistical analysis were extracted. The most adjusted risk estimates were extracted when available. Interobserver agreement was assessed using Cohen’s κ. Any disagreements were resolved by discussion with the third author (S.L.).

Quality assessment

Quality assessment was independently performed by two reviewers (D.C. and Q.T.). For cohort and case–control studies, the Newcastle–Ottawa Scale was used(Reference Wells, Shea and O’Connell24), it is a nine-point scale allocating points based on the selection process, comparability and identification of exposures and outcomes in the cohort. Scores of 0–3, 4–6 and 7–9 denoted low, moderate and high quality of studies, respectively. For cross-sectional studies, the quality assessment guideline recommended by the Agency for Healthcare Research and Quality was applied(25). The quality of articles was evaluated based on established questions, which were scored as follows: 1 point if the item was considered in the study; otherwise 0 point was assigned.

Data synthesis and statistical analysis

In this meta-analysis, OR and relative risk were considered as the effect level of association between 25(OH)D and MD. OR was deemed equivalent to relative risk. Multivariable adjusted risk was pooled where such estimates were available; otherwise we pooled the unadjusted estimate. Since exposure categories (dichotomous, multichotomous) might be different in different studies, the highest concentration of 25(OH)D was defined as the exposure group and the lowest was the reference group. We used the study-specific OR for the highest v. lowest category of 25(OH)D concentration for the current meta-analysis. Overall pooled OR was calculated using a random-effects model, which considers both within- and between-study variations.

Statistical heterogeneity among the studies was estimated by the Cochran Q test, reported as I 2 statistic, where values of <50, 50–75, >75 % were considered as low, moderate and high degrees of heterogeneity, respectively(Reference Higgins and Thompson26). If heterogeneity was significant, the Mantel–Haenszel random-effect model was used to pool the results, and when heterogeneity was negligible, a fixed-effect model was performed. We conducted sensitivity analysis by sequential and combinatorial algorithms to evaluate the change in between-study heterogeneity as one or more studies were excluded from the calculations. Potential publication bias was evaluated using a funnel plot and with Begg’s and Egger’s tests.

Subgroup analyses were conducted to explore potential sources of study heterogeneity and examine the robustness of the primary results. These included study design (cohort study, case–control study, cross-sectional study), MD type (postpartum depression, antepartum depression) and methods of MD measurements (depression scale and clinical diagnoses). Additionally, latitude (low, middle, high), race of participants (Caucasian, Asian, mixed), season of 25(OH)D measurement (summer, winter, all) and adjustment for different confounders (age, education, parity, history of depression, BMI and smoking) underwent subgroup analysis.

Dose–response analysis was performed on articles that reported more than two quantitative categories of 25(OH)D. For studies that reported concentrations at separate ranges of 25(OH)D levels, we estimated the midpoint in each category by calculating the average of lower and upper bounds. Where the lower boundary of the lowest category was unavailable, half of the upper boundary of that category was considered the assigned median; if the upper boundary of the highest category was not provided, the midpoint of this category was set at 1·5 times that of the lower level. To evaluate for a potential non-linear dose–response association between 25(OH)D and risk of MD, we used a restricted cubic spline regression model with four knots at percentiles 5, 35, 65 and 95 % of the distribution. If the P value for non-linearity was against the null hypothesis that 25(OH)D of the second and third spline transformation was equal to zero, the non-linear dose–response relationship between 25(OH)D and risk of MD was statistically significant(Reference Orsini, Li and Wolk27). A trend curve of non-linear dose–response relationship was drawn. All analyses were performed with Stata statistical software (version 14.0). All tests were two-sided with a significance level of 0·05.

Result

Literature search and quality evaluation

We initially retrieved 405 articles from the Web of Science, 366 from PubMed and 331 from Embase. After removing duplicates, 489 articles were identified as potentially relevant. After reviewing the titles and abstracts, 465 studies were excluded based on ineligibility according to the inclusion criteria. The full text of the remaining twenty-four articles was retrieved for review and detailed evaluation; twelve studies(Reference Nielsen, Strom and Boyd19,Reference Gould, Anderson and Yelland20,Reference Brandenbarg, Vrijkotte and Goedhart28Reference Lin, Chen and Su37) with thirteen independent reports were finally included in the meta-analysis (Fig. 1). The average quality assessment score of all included cohort, case–control and cross-sectional studies was 7·0, 8·5 and 7·0, respectively, and all studies were of moderate or high quality (quality score ≥6) (Table 1). Interobserver agreement between reviewers for study inclusion was very high (κ = 0·97). In the dose–response analysis, two studies(Reference Fu, Liu and Tu33,Reference Zhou, Zhang and Tong35) were excluded because of no or having less than three categories of 25(OH)D concentrations. Finally, ten studies with eleven reports were included in the dose–response analysis of 25(OH)D concentrations with risk of MD.

Fig. 1 Flowchart showing the relevant observational studies of vitamin D in relation to maternal depression

Table 1 Characteristics of twelve studies and scores of quality assessment included in the meta-analysis

CES-D, Center for Epidemiological Studies Depression Scale; APD, antepartum depression; EPDS, Edinburgh Postnatal Depression Scale; DASS-21, twenty-one-item Depression, Anxiety and Stress Scales; PPD, postpartum depression.

Study characteristics

This analysis included seven cohort studies(Reference Gould, Anderson and Yelland20,Reference Brandenbarg, Vrijkotte and Goedhart28,Reference Gur, Gokduman and Turan30,Reference Robinson, Whitehouse and Newnham32,Reference Figueiredo, Trujillo and Freitas-Vilela34,Reference Zhou, Zhang and Tong35,Reference Lin, Chen and Su37) , two case–control studies(Reference Nielsen, Strom and Boyd19,Reference Abedi, Bovayri and Fakhri36) and three cross-sectional studies(Reference Cassidy-Bushrow, Peters and Johnson29,Reference Huang, Arnold and Qiu31,Reference Fu, Liu and Tu33) . All studies used were published within the last 8 years from 2012 to 2019. Sample sizes of these studies ranged from 120 to 4101, with a total of 10 317 subjects, and the number of depression cases ranged from 23 to 651, with a total of 2553. Study locations were as follows: three in China(Reference Fu, Liu and Tu33,Reference Zhou, Zhang and Tong35,Reference Lin, Chen and Su37) , one in Brazil(Reference Figueiredo, Trujillo and Freitas-Vilela34), two in Australia(Reference Gould, Anderson and Yelland20,Reference Robinson, Whitehouse and Newnham32) , one in Turkey(Reference Gur, Gokduman and Turan30), two in USA(Reference Cassidy-Bushrow, Peters and Johnson29,Reference Huang, Arnold and Qiu31) , one in Denmark(Reference Nielsen, Strom and Boyd19), one in The Netherlands(Reference Brandenbarg, Vrijkotte and Goedhart28) and one in Iran(Reference Abedi, Bovayri and Fakhri36). Methods of depression measurement used were one by clinical diagnosis(Reference Nielsen, Strom and Boyd19), one by the twenty-one-item Depression, Anxiety and Stress Scale(Reference Huang, Arnold and Qiu31), one by Beck Depression Scale(Reference Abedi, Bovayri and Fakhri36), three by Center for Epidemiological Studies Depression Scale(Reference Brandenbarg, Vrijkotte and Goedhart28,Reference Cassidy-Bushrow, Peters and Johnson29,Reference Zhou, Zhang and Tong35) and six by Edinburgh Postnatal Depression Scale(Reference Gould, Anderson and Yelland20,Reference Gur, Gokduman and Turan30,Reference Robinson, Whitehouse and Newnham32Reference Figueiredo, Trujillo and Freitas-Vilela34,Reference Lin, Chen and Su37) .

25-Hydroxyvitamin D and risk of maternal depression

Results of the random-effects meta-analysis combining the OR of MD in relation to 25(OH)D are shown in Fig. 2. Compared with the lowest category of 25(OH)D, the pooled OR of MD for the highest category was 0·49 (95 % CI 0·35, 0·63). A high heterogeneity was observed (P = 0·001, I 2 = 82·1 %). Compared with the lowest category of 25(OH)D, the pooled OR of antepartum depression and postpartum depression for the highest category was 0·51 (95 % CI 0·37, 0·65) and 0·48 (95 % CI 0·24, 0·72), respectively; a moderate heterogeneity was observed (P = 0·024, I 2 = 61·2 %) within the studies of antepartum depression, and a high heterogeneity was observed (P = 0·001, I 2 = 82·8 %) within the studies of postpartum depression.

Fig. 2 Association between 25(OH)D and risk of maternal depression (1, antepartum depression; 2, postpartum depression; ES, effect size)

Dose–response analysis of 25-hydroxyvitamin D with the risk of maternal depression

A total of ten studies with eleven reports were included in the dose–response analysis(Reference Nielsen, Strom and Boyd19,Reference Gould, Anderson and Yelland20,Reference Brandenbarg, Vrijkotte and Goedhart28Reference Robinson, Whitehouse and Newnham32,Reference Figueiredo, Trujillo and Freitas-Vilela34,Reference Abedi, Bovayri and Fakhri36,Reference Lin, Chen and Su37) . In the cubic spline model (Fig. 3), we found evidence suggesting a non-linear association of 25(OH)D with the risk of MD (P for non-linearity = 0·001). As vitamin D concentrations increased, the risk of MD rapidly decreased to the lowest and then rose slowly. The lowest pooled OR was at 25(OH)D concentrations of 90–110 nmol/l.

Fig. 3 Dose–response relation plots between 25(OH)D concentration and risk of maternal depression. , lb with ref; , ub with ref; , rr with ref; , rr_lin

Subgroup analyses

In most of the subgroup analyses, an association between 25(OH)D and risk of MD was identified. A subgroup analysis of 25(OH)D measurement by season showed that 25(OH)D was negatively associated with MD, irrespective of the season it was measured. The risk was more pronounced for 25(OH)D measured in summer (OR 0·25, 95 % CI 0·08, 0·43) than in other seasons (OR 0·68, 95 % CI 0·52, 0·83). Additionally, depression type, study design, depression measurement, 25(OH)D measurement, latitude, race, adjustment for age, education, parity, history of depression, BMI and smoking did not influence the OR summary (Table 2).

Table 2 Subgroup and meta-regression analysis of relative risk (RR) of maternal depression

APD, antepartum depression; PPD, postpartum depression; CES-D, Center for Epidemiological Studies Depression Scale; EPDS, Edinburgh Postnatal Depression Scale.

* P for heterogeneity within each subgroup.

P for heterogeneity between subgroups in the meta-regression analysis.

Sensitivity analyses

Sensitivity analyses were performed to check for the robustness of results and to find the potential origins of heterogeneity. After dropping out four studies identified by combinatorial algorithms, which were primary origins of heterogeneity, there was still a statistically significant negative association (OR 0·67, 95 % CI, 0·56, 0·80), and no heterogeneity was observed (P = 0·29, I 2 = 17·2 %). By sequential algorithms, we excluded any single report in turn and pooled the results of remaining reports; a pooled OR of MD ranging from 0·49 (95 % CI, 0·40, 0·51; P = 0·001) to 0·59 (95 % CI 0·47, 0·71; P = 0·001) was observed, which indicated the result was robust.

Publication bias

A visual inspection of the funnel plot did not suggest a substantial asymmetry (Fig. 4). Both the Begg’s rank correlation test (Z = 0·18, P = 0·855) and the Egger’s linear regression test (t = –0·09, P = 0·928) indicated no evidence of publication bias among the studies.

Fig. 4 Funnel plot of 25(OH)D and risk of maternal depression

Discussion

To our knowledge, this is the first review to use a dose–response meta-analytic approach to quantitatively summarise the evidence and systematically estimate the effect of vitamin D status on MD risk. Based on our systematic analysis, we interpreted the range of serum 25(OH)D concentrations associated with optimal mental health. In thirteen reports, 25(OH)D is shown to be significantly related to a decreased risk of MD. Specifically, the dose–response meta-analysis indicated that a high blood 25(OH)D concentrations has a protective effect on MD. Notably, when blood 25(OH)D concentrations increased to 90–100 nmol/l, the risk of MD was the lowest.

Two valuable and important findings were obtained from the current analyses. Firstly, we inferred that 25(OH)D and MD were both a causality and a consequence. Some studies have demonstrated that vitamin D, a potential neurosteroid, may play an important role in certain mental processes, and its deficiency could lead to an improper functioning of hormones that control mood. Conversely, depression may also be a risk factor for developing vitamin D deficiency because of staying indoors, consumption of less-nutritious diets and inadequate exercises. In the subgroup analysis by season, an inverse relationship between 25(OH)D concentrations and MD symptoms was found, and the association became stronger in summer months. If depression was caused by vitamin D deficiency (mainly due to inadequate sunlight exposure), then the association between 25(OH)D concentrations and contemporaneous MD symptoms would be expected to be stronger in summer months when the levels are strongly influenced by sunlight exposure(Reference Nanri, Mizoue and Matsushita38Reference Rabenberg, Harisch and Rieckmann40). This was clearly evident in the subgroup analysis by season. Regardless of the direction of causation, poor vitamin D status and depression are common among pregnant women, and although both appear to have substantial adverse health consequences, they are potentially reversible if enough attention can be paid to it.

Secondly, from our dose–response analysis, pregnant and lactating mothers may need to maintain blood 25(OH)D concentrations at about 90–100 nmol/l to reduce the risk of depression to the barest minimum. As Heaney has suggested(Reference Heaney and Armas41), an equivalence value of 2·5 nmol/l may be used to reflect an input of 2·5 µg/d; herein, 90–100 nmol/l reflects an input of 90–100 µg/d of vitamin D. Studies estimating diet records have found that intakes of food sources would supply no more than 5·0 µg/d of vitamin D. Even at peak summer, maximal solar synthesis could account for less than 17·5 µg/d(Reference Heaney and Armas41). In this regard, we inferred a need for about 67·5–77·5 µg/d of supplemental vitamin D from our dose–response analysis. The American Endocrine Society’s clinical practice guidelines suggest that pregnant and lactating women require at least 15·0 µg/d of supplemental vitamin D. It added that at least 37·5–50 µg/d of supplemental vitamin D may be needed to maintain a blood 25(OH)D level >75 nmol/l(Reference Holick, Binkley and Bischoff-Ferrari42). The recommended dose in the current dose–response analysis is higher than that prescribed by the American Endocrine Society; however, it is below the tolerable upper intake level and well within the safe range delineated by Hathcock et al.(Reference Hathcock, Shao and Vieth43).

Although poor vitamin D status may not be the only cause of depression, it is correlated with the aetiology and manifestation of depression. Therefore, vitamin D screening and intake of supplements could be an effective public health measure to reduce MD risk. To date, guidelines concerning vitamin D screening and supplements among pregnant women are conflicting. Clinical antenatal care guidelines in USA and Australia recommend screening for women only at an increased risk of vitamin D deficiency, including those with limited exposure to sunlight. In UK, pregnant women could obtain free vitamin D supplements from local health departments. However, similar policies are yet to be implemented in China and other developing countries(Reference Yun, Chen and He44). In conclusion, the evidence provided by the current meta-analysis shows that low 25(OH)D concentrations is implicated as not only a risk factor but also a consequence of MD, and supports the recommendation to scale-up vitamin D screening and use of supplements by pregnant women. Given the potential impact of season (sunlight exposure) on 25(OH)D concentrations, the dosage of supplement should be carefully estimated; in winter, pregnant women should moderately increase the dosage of vitamin D supplement.

The current study has several limitations. Firstly, twelve studies that measured 25(OH)D concentrations were selected independently of whether or not the assay used was standardised as currently recommended for accurate meta-analyses, and therefore the reported measurements might vary. Secondly, an association between 25(OH)D and MD derived from observational studies could just infer causality; further prospective studies and randomised controlled trials would be needed to confirm the causality. Another important limitation pertains to the observational study design; most employed a scale cut-off rather than a clinical depression diagnosis and used the unadjusted estimates as several important covariates, including life stress, social support and exercise, were missing. Lastly, 25(OH)D2 and 25(OH)D3 were not separately analysed in the dose–response analysis because 25(OH)D3 is the main part of 25(OH)D.

Acknowledgements

Acknowledgements: We express our appreciation and gratitude to all the authors of the original studies included in the current meta-analysis. Financial support: The present research was financially supported by ‘study on the effect of six sigma management on improving the quality of information on home page of medical records’ (2018YFYB010). Conflicts of interests: None. Authorship: D.C. performed study conception and design, literature search and data analysis. Q.T. performed literature search and drafting of manuscript. S.L. contributed to the literature search, data analysis and revised the article critically for important intellectual content. Ethics of human subject participation: None.

References

World Health Organization (2020) Depression. http://www.who.int/mediacentre/factsheets/fs369/en/ (accessed September 2020).Google Scholar
Ledford, H (2014) Medical research: if depression were cancer. Nature 515, 182184.CrossRefGoogle ScholarPubMed
Marcus, SM (2009) Depression during pregnancy: rates, risks and consequences–motherisk consequences – Motherisk Update 2008. Can J Clin Pharmacol 16, 1522.Google ScholarPubMed
Marcus, SM, Flynn, HA, Blow, FC et al. (2003) Depressive symptoms among pregnant women screened in obstetrics settings. J Women Health Gen-B 12, 373380.CrossRefGoogle ScholarPubMed
Robertson, E, Grace, S, Wallington, T et al. (2004) Antenatal risk factors for postpartum depression: a synthesis of recent literature. Gen Hosp Psychiatry 26, 289295.CrossRefGoogle ScholarPubMed
Field, T (2010) Postpartum depression effects on early interactions, parenting, and safety practices: a review. Infant Behav Dev 33, 16.CrossRefGoogle ScholarPubMed
Savitz, DA, Stein, CR, Ye, F et al. (2011) The epidemiology of hospitalized postpartum depression in New York State, 1995–2004. Ann Epidemiol 21, 399406.CrossRefGoogle ScholarPubMed
Grote, NK, Bridge, JA, Gavin, AR et al. (2010) A meta-analysis of depression during pregnancy and the risk of preterm birth, low birth weight, and intrauterine growth restriction. Arch Gen Psychiat 67, 10121024.CrossRefGoogle ScholarPubMed
Aghajafari, F, Nagulesapillai, T, Ronksley, PE et al. (2013) Association between maternal serum 25-hydroxyvitamin D level and pregnancy and neonatal outcomes: systematic review and meta-analysis of observational studies. BMJ 346, f1169.CrossRefGoogle ScholarPubMed
Schneuer, FJ, Roberts, CL, Guilbert, C et al. (2014) Effects of maternal serum 25-hydroxyvitamin D concentrations in the first trimester on subsequent pregnancy outcomes in an Australian population. Am J Clin Nutr 99, 287295.CrossRefGoogle Scholar
Saveanu, RV & Nemeroff, CB (2012) Etiology of depression: genetic and environmental factors. Psychiatr Clin North Am 35, 5171.10.1016/j.psc.2011.12.001CrossRefGoogle ScholarPubMed
Amini, S, Jafarirad, S & Amani, R (2019) Postpartum depression and vitamin D: a systematic review. Crit Rev Food Sci Nutr 59 15141520.CrossRefGoogle ScholarPubMed
Cassidy-Bushrow, AE, Peters, RM, Johnson, DA et al. (2012) Association of depressive symptoms with inflammatory biomarkers among pregnant African-American women. J Reprod Immunol 94, 202209.CrossRefGoogle ScholarPubMed
Garcion, E, Wion-Barbot, N, Montero-Menei, CN et al. (2002) New clues about vitamin D functions in the nervous system. Trends Endocrin Met 13, 100105.CrossRefGoogle ScholarPubMed
Bertone-Johnson, ER (2009) Vitamin D and the occurrence of depression: causal association or circumstantial evidence? Nutr Rev 67, 481492.CrossRefGoogle ScholarPubMed
Fernandes de Abreu, DA, Eyles, D & Feron, F (2009) Vitamin D, a neuro-immunomodulator: implications for neurodegenerative and autoimmune diseases. Psychoneuroendocrinology 34, Suppl. 1, S265S277.10.1016/j.psyneuen.2009.05.023CrossRefGoogle ScholarPubMed
Accortt, EE, Schetter, CD, Peters, RM et al. (2016) Lower prenatal vitamin D status and postpartum depressive symptomatology in African American women: preliminary evidence for moderation by inflammatory cytokines. Arch Womens Ment Health 19, 373383.10.1007/s00737-015-0585-1CrossRefGoogle ScholarPubMed
Williams, JA, Romero, VC, Clinton, CM et al. (2016) Vitamin D levels and perinatal depressive symptoms in women at risk: a secondary analysis of the mothers, omega-3, and mental health study. BMC Pregnancy Childbirth 16, 203.CrossRefGoogle ScholarPubMed
Nielsen, NO, Strom, M, Boyd, HA et al. (2013) Vitamin D status during pregnancy and the risk of subsequent postpartum depression: a case–control study. PLoS ONE 8, e80686.CrossRefGoogle ScholarPubMed
Gould, JF, Anderson, AJ, Yelland, LN et al. (2015) Association of cord blood vitamin D at delivery with postpartum depression in Australian women. Aust N Z J Obstet Gynaecol 55, 446452.CrossRefGoogle ScholarPubMed
Stroup, DF, Berlin, JA, Morton, SC et al. (2000) Meta-analysis of observational studies in epidemiology: a proposal for reporting. Meta-analysis Of Observational Studies in Epidemiology (MOOSE) group. JAMA 283, 20082012.CrossRefGoogle ScholarPubMed
Bouillon, R, Van Baelen, H & De Moor, P (1977) 25-Hydroxyvitamin D and its binding protein in maternal and cord serum. J Clin Endocrinol Metab 45, 679684.CrossRefGoogle ScholarPubMed
Lamb, AR, Lutenbacher, M, Wallston, KA et al. (2018) Vitamin D deficiency and depressive symptoms in the perinatal period. Arch Women Ment Health 21, 745755.CrossRefGoogle ScholarPubMed
Wells, GA, Shea, B, O’Connell, D et al. (2014) The Newcastle-Ottawa Scale (NOS) for Assessing the Quality of Non-Randomised Studies in Meta-Analyses. Ottawa, ON: Ottawa Health Research Institute.Google Scholar
Rockville (2004) Evidence Reports. https://www.ncbi.nlm.nih.gov/books/NBK35156/ (accessed September 2020).Google Scholar
Higgins, JP &Thompson, SG (2002) Quantifying heterogeneity in a meta-analysis. Stat Med 21, 15391558.CrossRefGoogle ScholarPubMed
Orsini, N, Li, RF, Wolk, A et al. (2012) Meta-analysis for linear and nonlinear dose-response relations: examples, an evaluation of approximations, and software. Am J Epidemiol 175, 6673.10.1093/aje/kwr265CrossRefGoogle Scholar
Brandenbarg, J, Vrijkotte, TGM, Goedhart, G et al. (2012) Maternal early-pregnancy vitamin D status is associated with maternal depressive symptoms in the Amsterdam born children and their development cohort. Psychosom Med 74, 751757.CrossRefGoogle ScholarPubMed
Cassidy-Bushrow, AE, Peters, RM, Johnson, DA et al. (2012) Vitamin D nutritional status and antenatal depressive symptoms in African American women. J Womens Health 21, 11891195.CrossRefGoogle ScholarPubMed
Gur, EB, Gokduman, A, Turan, GA et al. (2014) Mid-pregnancy vitamin D levels and postpartum depression. Eur J Obstet Gynecol Reprod Biol 179, 110116.CrossRefGoogle ScholarPubMed
Huang, JY, Arnold, D, Qiu, CF et al. (2014) Association of serum vitamin D with symptoms of depression and anxiety in early pregnancy. J Womens Health 23, 588595.CrossRefGoogle ScholarPubMed
Robinson, M, Whitehouse, AJO, Newnham, JP et al. (2014) Low maternal serum vitamin D during pregnancy and the risk for postpartum depression symptoms. Arch Women’s Ment Health 17, 213219.CrossRefGoogle ScholarPubMed
Fu, CW, Liu, JT, Tu, WJ et al. (2015) Association between serum 25-hydroxyvitamin D levels measured 24 hours after delivery and postpartum depression. BJOG 122, 16881694.CrossRefGoogle ScholarPubMed
Figueiredo, ACC, Trujillo, J, Freitas-Vilela, AA et al. (2017) Association between plasma concentrations of vitamin D metabolites and depressive symptoms throughout pregnancy in a prospective cohort of Brazilian women. J Psychiatr Res 95, 18.CrossRefGoogle Scholar
Zhou, QF, Zhang, MX, Tong, SL et al. (2017) Maternal depression attenuates newborn vitamin D concentrations in winter-spring: a prospective population-based study. Sci Rep 7, 1522.CrossRefGoogle ScholarPubMed
Abedi, P, Bovayri, M, Fakhri, A et al. (2018) The relationship between vitamin D and postpartum depression in reproductive-aged Iranian women. J Med Life 11, 286292.Google ScholarPubMed
Lin, YH, Chen, CM, Su, HM et al. (2019) Association between postpartum nutritional status and postpartum depression symptoms. Nutrients 11, 1204.CrossRefGoogle ScholarPubMed
Nanri, A, Mizoue, T, Matsushita, Y et al. (2009) Association between serum 25-hydroxyvitamin D and depressive symptoms in Japanese: analysis by survey season. Eur J Clin Nutr 63, 14441447.CrossRefGoogle ScholarPubMed
Stewart, R & Hirani, V (2010) Relationship between vitamin D levels and depressive symptoms in older residents from a national survey population. Psychosom Med 72, 608612.10.1097/PSY.0b013e3181e9bf15CrossRefGoogle ScholarPubMed
Rabenberg, M, Harisch, C, Rieckmann, N et al. (2016) Association between vitamin D and depressive symptoms varies by season: results from the German Health Interview and Examination Survey for Adults (DEGS1). J Affect Disord 204, 9298.CrossRefGoogle Scholar
Heaney, RP & Armas, LA (2015) Quantifying the vitamin D economy. Nutr Rev 73, 5167.CrossRefGoogle ScholarPubMed
Holick, MF, Binkley, NC, Bischoff-Ferrari, HA et al. (2011) Evaluation, treatment, and prevention of vitamin D deficiency: an endocrine society clinical practice guideline. J Clin Endocrinol Metab 96, 19111930.CrossRefGoogle ScholarPubMed
Hathcock, JN, Shao, A, Vieth, R et al. (2007) Risk assessment for vitamin D. Am J Clin Nutr 85, 618.CrossRefGoogle ScholarPubMed
Yun, C, Chen, J, He, Y et al. (2017) Vitamin D deficiency prevalence and risk factors among pregnant Chinese women. Public Health Nutr 20, 17461754.CrossRefGoogle ScholarPubMed
Sempos, CT, Heijboer, AC, Bikle, DD et al. (2018) Vitamin D assays and the definition of hypovitaminosis D: results from the First International Conference on Controversies in Vitamin D. Br J Clin Pharmacol 84, 21942207.CrossRefGoogle ScholarPubMed
Figure 0

Fig. 1 Flowchart showing the relevant observational studies of vitamin D in relation to maternal depression

Figure 1

Table 1 Characteristics of twelve studies and scores of quality assessment included in the meta-analysis

Figure 2

Fig. 2 Association between 25(OH)D and risk of maternal depression (1, antepartum depression; 2, postpartum depression; ES, effect size)

Figure 3

Fig. 3 Dose–response relation plots between 25(OH)D concentration and risk of maternal depression. , lb with ref; , ub with ref; , rr with ref; , rr_lin

Figure 4

Table 2 Subgroup and meta-regression analysis of relative risk (RR) of maternal depression

Figure 5

Fig. 4 Funnel plot of 25(OH)D and risk of maternal depression