- Research article
- Open access
- Published:
Risk of long-term renal disease in women with a history of preterm delivery: a population-based cohort study
BMC Medicine volume 18, Article number: 66 (2020)
Abstract
Background
Preterm delivery is an independent risk factor for maternal cardiovascular disease. Little is known about the association between preterm delivery and maternal renal function. This study aimed to examine whether women who experience preterm delivery are at increased risk of subsequent chronic kidney disease (CKD) and end-stage kidney disease (ESKD).
Methods
Using data from the Swedish Medical Birth Register, singleton live births from 1973 to 2012 were identified and linked to data from the Swedish Renal Register and National Patient Register (up to 2013). Gestational age at delivery was the main exposure and treated as a time-dependent variable. Primary outcomes were maternal CKD or ESKD. Cox proportional hazard regression models were used for analysis.
Results
The dataset included 1,943,716 women who had 3,760,429 singleton live births. The median follow-up was 20.6 (interquartile range 9.9–30.0) years. Overall, 162,918 women (8.4%) delivered at least 1 preterm infant (< 37 weeks). Women who had any preterm delivery (< 37 weeks) were at increased risk of CKD (adjusted hazard ratio (aHR) 1.39, 95% CI 1.32–1.45) and ESKD (aHR 2.22, 95% CI 1.90–2.58) compared with women who only delivered at term (≥ 37 weeks). Women who delivered an extremely preterm infant (< 28 weeks) were at increased risk of CKD (aHR 1.84, 95% CI 1.52–2.22) and ESKD (aHR 3.61, 95% CI 2.03–6.39). The highest risk of CKD and ESKD was in women who experienced preterm delivery + preeclampsia (vs. non-preeclamptic term deliveries, for CKD, aHR 2.81, 95% CI 2.46–3.20; for ESKD, aHR 6.70, 95% CI 4.70–9.56). However, spontaneous preterm delivery was also associated with increased risk of CKD (aHR 1.32, 95% CI 1.25–1.39) and ESKD (aHR 1.99, 95% CI 1.67–2.38) independent of preeclampsia or small for gestational age (SGA).
Conclusions
Women with history of preterm delivery are at increased risk of CKD and ESKD. The risk is higher among women who had very preterm or extremely preterm deliveries, or whose preterm delivery was medically indicated. Women who experience spontaneous preterm delivery are at increased risk of long-term renal disease independent of preeclampsia or SGA. Preterm delivery may act as a risk marker for adverse maternal renal outcomes.
Background
Chronic kidney disease (CKD) is a major cause of morbidity globally, with an estimated prevalence of 7–12% for stage 3 CKD or greater among women [1,2,3]. End-stage kidney disease (ESKD), although relatively rare, has a disproportionately high healthcare burden. Preterm delivery, before 37 weeks’ gestation, is recognised as a risk factor for maternal cardiovascular disease (CVD), independent of socio-demographic factors (e.g. age, ethnicity, education), obstetric history (e.g. preeclampsia, parity), and cardiometabolic factors (e.g. chronic hypertension, diabetes, body mass index (BMI)) [4,5,6]. Although cardiovascular guidelines suggest that pregnancy-related factors, including preterm delivery, should be considered markers of future CVD risk [7, 8], little is known about the association between preterm delivery and subsequent renal disease. This information could potentially provide opportunities for risk stratification and secondary prevention of CKD in women.
Existing research on preterm delivery and the risk of maternal CKD has been limited to groups with an increased baseline risk of renal disease [9, 10], or has failed to adjust for important confounders such as maternal smoking [11,12,13] and obesity [12, 13]. Cardiovascular risk is higher among women who experience very or extremely preterm deliveries (before 32 weeks’ gestation) [4], but it is uncertain whether a similar pattern exists for future risk of CKD. It is plausible that women with earlier preterm deliveries experience greater risk of CKD or ESKD relative to women who deliver closer to full term.
Most preterm deliveries occur spontaneously, but about 30% are iatrogenic and performed for obstetric reasons, typically maternal preeclampsia or intrauterine growth restriction (IUGR) [14]. Preeclampsia has been identified as a strong risk factor for ESKD [11, 13, 15], and women who experience IUGR or a small for gestational age (SGA) delivery may also be at increased risk of CKD [11, 16]. Thus, the risk of maternal CKD/ESKD may differ depending on whether women experience spontaneous or iatrogenic preterm deliveries.
We aimed to examine whether women who experience preterm delivery are at increased risk of CKD and ESKD, and whether this association differs by medical indication (i.e. spontaneous or iatrogenic preterm) or across categories of gestational age.
Methods
Study population
Data from the Swedish Medical Birth Register (MBR) (established 1973) were used to identify all women who had singleton live births between January 1, 1973, and December 31, 2012. Data from the Swedish National Patient Register (NPR) (established 1964) and Swedish Renal Register (SRR) (established 1991) were linked with the MBR using anonymised unique identification numbers. Data from the NPR and SRR were used to identify women who developed CKD or ESKD during follow-up, until December 31, 2013 (study end date). Data from the Swedish Death Register and Migration Register were also available until December 31, 2013, and used for censoring (Additional file 1. Supplementary Figure S1).
In order to reduce potential confounding from comorbid diseases, we identified women with pre-pregnancy CKD, ESKD, CVD, hypertension, diabetes (type 1 or 2), or systemic lupus erythematosus (SLE) from the MBR, and they were excluded from the study. We also excluded all women in the NPR who were admitted to hospital with these diagnoses before their index pregnancy. Three iterations of ICD coding were used to identify pre-existing diseases in the NPR: ICD-8 coding before 1986, ICD-9 coding from 1987 to 1996, and ICD-10 coding from 1997 to 2013. New hospital admissions and outpatient reviews for preeclampsia and gestational diabetes were also identified in the NPR using ICD codes, and used to supplement information in the MBR. The ICD codes are summarised in Additional file 2 (Supplementary Table S1).
We further excluded multiple pregnancies, stillbirths, and pregnancies with implausible dates of delivery from all analyses (Additional file 3. Supplementary Figure S2).
Preterm delivery
Maternal history of preterm delivery was the main exposure of interest. Gestational age at delivery was estimated based on second trimester ultrasound (around 17th week of pregnancy) where available, or the time from last menstrual period (LMP) to birth based on maternal report at first antenatal visit. LMP was used to estimate gestational age until 1982, but ultrasonography data became increasingly available in the MBR thereafter.
Five separate exposure variables were used to investigate the effects of gestational age, including preterm and early term delivery, on maternal CKD/ESKD risk. Each of these used different classifications of preterm delivery. For all models, time-dependent variables were used so that a woman could contribute pregnancies and person-time to both unexposed and exposed groups during follow-up. Women could contribute unexposed time if they never had a preterm delivery, or until their first preterm delivery occurred. For example, if a woman delivered at term (≥ 37 weeks) in the first pregnancy, and then had a preterm delivery (< 37 weeks) in the second pregnancy, she was considered unexposed between deliveries 1 and 2, and exposed from delivery 2 onwards irrespective of subsequent pregnancy outcomes.
For the main analysis (exposure 1), women were categorised according to any previous history of preterm delivery (ever, < 37 weeks). If women had more than one pregnancy, they were considered exposed from the date of their first preterm delivery onwards. For exposure 2, established definitions of term (≥ 37 weeks, reference group) vs. moderate (32–36 + 6 weeks)/very (28–31 + 6 weeks)/extremely (< 28 weeks) preterm were used. Maternal exposure status was always based on the earliest gestation of any previous delivery. For example, if a woman had three deliveries during follow-up, at 35 weeks, 27 weeks, and 39 weeks, respectively, she contributed exposed time to the moderate preterm category between deliveries 1 and 2, and contributed exposed time to the extremely preterm category thereafter (irrespective of her third delivery at term).
Next, for exposure 3, additional categories of early term deliveries (37–38 + 6 weeks) and post-term deliveries (≥ 42 weeks) were used together with the established categories of moderate/very/extremely preterm. The reference group for exposure 3 was those who delivered at “full term” (i.e. 39–41 + 6 weeks). Early term deliveries (37–38 + 6 weeks) were examined separately since they are associated with increased risk of adverse perinatal outcomes [17, 18], and they share common risk factors with preterm deliveries [19].
For exposure 4, preterm deliveries (< 37 weeks) were stratified by spontaneous or iatrogenic preterm, where those deliveries complicated by preeclampsia and/or SGA were assumed to be iatrogenic preterm. A series of dummy variables were included to represent non-overlapping scenarios: (i) preterm delivery alone (i.e. assumed spontaneous preterm), (ii) preterm delivery + preeclampsia, (iii) preterm delivery + SGA, and (iv) preterm delivery + preeclampsia + SGA (co-occurring). The definition of SGA in the MBR was a birth weight of 2 standard deviations (SD) below the sex-specific and gestational age distributions, according to Swedish weight-based growth standards [20].
Finally, for exposure 5, the analysis was restricted to all women in the dataset who only had two live births during the study period to examine differences in risk between none/one/two preterm deliveries (< 37 weeks).
Outcome variables
There were two main outcomes: maternal CKD and maternal ESKD. Outcome data were defined by a recorded diagnosis of CKD or ESKD in the SRR or based on a primary or secondary diagnosis of CKD or ESKD in the NPR (using ICD codes). The earliest date at which a woman appeared in either the SRR or the NPR was assumed to be her date of diagnosis for CKD/ESKD. Women who had renal disease due to an identifiable congenital or genetic cause were excluded (Additional file 2. Supplementary Table S1).
Covariates
The following covariates were adjusted for: maternal age, year of delivery, country of origin, education level, body mass index (BMI), smoking during pregnancy, gestational diabetes, preeclampsia, parity, and inter-pregnancy interval. Education level was available from the Swedish Education Register and was based on the mother’s highest level of educational achievement (proxy variable for socio-economic status). Smoking status was based on any reported smoking during pregnancy, either at first antenatal visit or at 30–32 weeks’ gestation. Maternal BMI was calculated based on weight and length (kg/m2) as recorded at first antenatal visit. There were large amounts of missing data for smoking status and BMI, and these variables were only available from 1982 onwards. Missing indicator variables were created to control for this. A sensitivity analysis was also undertaken where the dataset was restricted to births between 1982 and 2012 to check for comparability with the main results.
Maternal exposure to gestational diabetes was treated as a time-dependent covariate, where women were considered exposed from their date of first delivery with gestational diabetes. Preeclampsia was also considered a time-dependent covariate and was adjusted for in all models except when exposure 4 was used, since preterm preeclamptic deliveries were already considered as a separate group. Inter-pregnancy interval was defined as the date between a woman’s last live birth and her estimated date of conception for the next live birth (estimated by subtracting gestational age in days from the date of next live birth).
Statistical analysis
Data were set up for survival analysis, where entry date in the study was the date of each woman’s first live birth. The association between history of preterm delivery and risk of maternal CKD was estimated using the Kaplan-Meier method. Differences in survival curves were estimated using logrank tests. We used multivariable Cox proportional hazard regression models to estimate minimally adjusted and fully adjusted hazard ratios (aHRs) and 95% confidence intervals (CI) for the associations between preterm delivery and maternal renal disease. We followed women from date of entry until date of CKD/ESKD diagnosis, date of death, date of emigration, or study end date (31 December 2013), whichever came first. Log cumulative hazard plots were used to check the adequacy of each Cox regression model, and year of delivery was included in all minimally adjusted models to ensure the assumption of proportional hazards was met.
Two-sided P values were used, and P < 0.05 denoted statistical significance. All analyses were performed using Stata version 15 (StataCorp LLC).
Results
The study cohort consisted of 1,943,716 unique women who had 3,760,429 singleton pregnancies, followed up for a total of 42,341,527 person-years. The median follow-up was 20.6 years (interquartile range 9.9–30.0), and the maximum follow-up was 41.0 years. There were 162,918 women (8.4%) who experienced preterm delivery (< 37 weeks) at some point (Table 1). From 1973 to 2013, 18,001 women (0.9%) developed CKD, and 1268 (0.07%) developed ESKD.
History of any preterm or early term delivery
Tables 2 and 3 summarise the results of the main analyses for CKD and ESKD, respectively. Women who had at least one preterm delivery (< 37 weeks) (exposure 1) were at significantly increased risk of long-term CKD (aHR 1.39, 95% CI 1.32–1.45) and ESKD (aHR 2.22, 95% CI 1.90–2.58).
Figure 1 shows the differences in the Kaplan-Meier curves for CKD across categories of gestational age (moderate/very/extremely preterm delivery). Relative to those who delivered at term (≥ 37 weeks), women who had at least one extremely preterm delivery (< 28 weeks) were at higher risk of CKD (aHR 1.84, 95% CI 1.52–2.22) and ESKD (aHR 3.61, 95%CI 2.03–6.39), respectively (exposure 2, Tables 2 and 3).
The Kaplan-Meier survival curves for risk of chronic kidney disease among women by exposure to moderate, very, or extremely preterm delivery between 1973 and 2012 in Sweden
Women who experienced early term deliveries (37–38 + 6 weeks) were also at increased risk of CKD (aHR 1.19, 95% CI 1.15–1.24) and ESKD (aHR 1.50, 95% CI 1.31–1.73) compared to women who only had full term deliveries (39–41 + 6 weeks) (exposure 3, Tables 2 and 3).
History of spontaneous or iatrogenic preterm delivery
Figure 2 shows the differences in the Kaplan-Meier survival curves for CKD across categories of spontaneous vs. iatrogenic preterm delivery. Compared to women who delivered at term (≥ 37 weeks), the risk of CKD and ESKD was highest in those who experienced preterm delivery (< 37 weeks) complicated by preeclampsia (for CKD, aHR 2.81, 95% CI 2.46–3.20; for ESKD, aHR 6.70, 95% CI 4.70–9.56) (exposure 4, Tables 2 and 3). Importantly, spontaneous preterm delivery (< 37 weeks) was also associated with increased risk of both CKD (aHR 1.32, 95% CI 1.25–1.39) and ESKD (aHR 1.99, 95% CI 1.67–2.38) independent of all other factors (exposure 4, Tables 2 and 3).
The Kaplan-Meier survival curves for risk of chronic kidney disease among women by exposure to spontaneous or iatrogenic preterm delivery between 1973 and 2012 in Sweden
Sensitivity analysis
All analyses were repeated for deliveries occurring between 1982 and 2012, when data became available on maternal BMI and smoking. No meaningful differences were observed between preterm delivery and CKD in these analyses (Table 4). Stronger associations were observed between extremely preterm delivery (< 28 weeks) and ESKD (aHR 5.14, 95% CI 2.81–9.40), and for preterm delivery + SGA and ESKD (aHR 4.89, 95% CI 3.33–8.40), but these associations were based on relatively few ESKD outcomes. The 95% CIs did not differ significantly from the corresponding 95% CIs in the main analysis.
Discussion
Statement of principal findings
This study aimed to determine whether women who deliver preterm infants are at increased long-term risk of CKD and ESKD. The results suggest that preterm delivery may be considered as a marker of heightened risk of future CKD and ESKD in parous women, independently of causal mechanisms. This finding was consistent across various definitions of gestational age and was strongest in those with very/extremely preterm deliveries. Mothers exposed to early term delivery, at 37–38 + 6 weeks’ gestation, were also at increased risk of future renal disease relative to women who delivered at full term (39–41 + 6 weeks).
Women who experienced iatrogenic preterm delivery were at the highest risk of subsequent CKD or ESKD, and this may be largely driven by the effects of preeclampsia or SGA, or by the cumulative effect of preterm delivery in the context of these factors. However, our results suggest that women who had spontaneous preterm delivery were also at increased risk of CKD and ESKD irrespective of obstetric comorbidities or other factors. Given that the majority of preterm deliveries are spontaneous [14], it is relevant to consider whether these women should be informed of their heightened relative risk, and whether their history of preterm deliveries should be considered as part of their overall risk profile for chronic disease.
Interpretation
There is a small body of literature which has examined independent associations between preterm delivery and maternal renal disease [21]. Longitudinal studies from Canada, Israel, and Norway have each reported that preterm delivery increases the risk of maternal ESKD, but they have been limited by incomplete adjustment for confounders [11,12,13]. Other cohort studies have been restricted to women with pre-existing diabetes [9] or renal disease [10], and cannot be generalised to wider populations. Our study builds on existing research by controlling for a broader range of covariates, including maternal smoking, BMI, and inter-pregnancy interval, and by excluding women with pre-existing medical comorbidities, which may have otherwise increased the risk of CKD. Moreover, previous studies focused on ESKD [9,10,11, 13] or kidney-related hospitalisation [12] as their outcome variable. To our knowledge, the current study is the first to report the association between preterm delivery and maternal CKD.
Only one previous study on this topic stratified preterm deliveries according to whether they were spontaneous or iatrogenic [12]. Although spontaneous preterm delivery was independently associated with CKD and ESKD in our study, the results suggest that preeclampsia, and to a lesser extent SGA, has a greater impact on renal risk than preterm delivery. Preeclampsia has been reported to increase the risk of maternal CKD [22,23,24,25] and ESKD [11, 13, 15, 22] previously.
The mechanisms underlying the independent associations between spontaneous preterm delivery and maternal CKD/ESKD are uncertain. Intuitively, it seems plausible that this is a manifestation of subclinical predisposition to renal and cardiometabolic disease. Women with a history of preterm delivery are at higher risk of developing hypertension, diabetes, and hypercholesterolaemia [26], as well as CVD [4,5,6], and these factors may all increase the subsequent risk of CKD and ESKD. It is also possible that inflammatory processes associated with spontaneous preterm delivery increase the risk of endothelial dysfunction and subclinical vascular disease, which in turn increase the risk of subsequent CKD and ESKD [27, 28]. Women with spontaneous preterm deliveries are considered to have a pro-inflammatory phenotype [29]. They may have higher C-reactive protein (CRP) levels in pregnancy [28, 30], and CRP is a strong predictor of later CKD risk [31]. Thus, inflammatory factors may underlie a woman’s predisposition to deliver at earlier gestation and her later susceptibility to renal disease.
Strengths and weaknesses of the study
This study has several strengths. The use of a large national cohort of pregnant women with a 41-year follow-up period reduced the possibility of selection bias and provided statistical power to examine the effect of gestational age independently of a wide range of recognised risk factors for maternal renal disease. The size of our cohort allowed us to provide robust effect estimates for spontaneous and iatrogenic preterm delivery. Our data were retrieved from national registers with mandatory reporting, thereby excluding the possibility of recall bias. We used time-dependent covariates which allowed for changes in exposure status over time, and are more representative of women’s cumulative exposure to obstetric risks during their reproductive lifetime.
Gestational age was identified from the MBR based on maternal report of LMP in the 1970s and early 1980s, and using ultrasound estimation from 1982 onwards where available. LMP is a less accurate method of predicting a woman’s delivery date than ultrasonography [32]. It is possible that some term births may have been misclassified and included in earlier categories of preterm delivery. This may have led to underestimation of the observed risks, but is unlikely to have affected the overall results. When ultrasound dating is used, first trimester crown-rump length is regarded as the best parameter for determining gestational age, and should be used where possible [33,34,35,36]. In our study, the standard ultrasound method to date pregnancies was through combination of biparietal diameter and femoral length in the second trimester. Although this method has been validated previously [37], we cannot exclude the possibility of misclassification of some term or preterm births. Pregnancy dating guidelines in Sweden have been updated in recent years and recommend the use of first trimester ultrasound where possible [34], but evidence suggests ongoing variation in adherence to these guidelines [38].
Our study population was primarily Swedish/Caucasian, and this may limit generalisability of the findings. Black women have higher prevalence of preterm delivery than Caucasian women [39], and the causes of preterm delivery may vary by ethnicity or change over time.
The majority of cases of CKD and ESKD were identified using ICD-coded diagnoses in the NPR. There was no specific ICD-8 code for ESKD before 1986, and although some individuals may have been captured as CKD in the NPR, ESKD cases may have been underestimated as a result. Data collection was also less comprehensive in the NPR before national coverage was achieved in 1987, and outpatient diagnoses were only recorded from 2001 onwards [40]. The SRR only collected ESKD data from 1991 onwards, and CKD data from 2007 onwards; thus, we cannot exclude the possibility of immortal time bias in our study.
The SRR has almost complete coverage of ESKD cases in Sweden, but coverage of CKD cases is lower [41]. There was a relatively low prevalence of CKD among women in our study, possibly due to a combination of under-ascertainment of cases from the SRR and NPR, strict exclusion criteria, and the relative youth of the cohort involved. It is likely that a considerable number of women with renal disease were never diagnosed or ascertained by either the NPR or the SRR. However, an external review has reported high positive predictive values for most diagnoses recorded in the NPR, despite lower sensitivity levels [40]. Thus, it is likely that those who were diagnosed with CKD or ESKD in the dataset were valid diagnoses.
Most variables in the dataset had almost complete data, but there were large amounts of missing data on maternal BMI and smoking. Missing data can significantly affect prevalence estimates, but only have a slight impact on risk estimates assuming the lack of information is random [42]. In our dataset, the availability of data on maternal BMI and smoking varied by year of delivery, because these covariates were only collected from 1982 onwards. We used missing indicator variables, and adjusted for year of delivery in all models, to control for this. We also conducted sensitivity analyses restricted to pregnancies after 1982, and most results were not substantially different.
There was no suitable ICD-8 code available for gestational diabetes in the NPR. We could not ascertain those who may have been diagnosed before 1986, although this proportion is likely to be small. Finally, we excluded women on the basis of pre-existing comorbidities at baseline, including chronic hypertension. This information came from both the birth and hospital registers, but the NPR has low sensitivity for chronic hypertension. Thus, we cannot exclude the possibility of unmeasured confounding.
Implications
It is likely that the absolute risk of ESKD remains very low in women with a history of preterm delivery (with or without preeclampsia), despite the high relative risks observed in this study, since ESKD is a rare outcome. By contrast, modest increases in the risk of CKD in women exposed to spontaneous preterm deliveries or early term births may be important from a population perspective. Early term births (at 37–38 + 6 weeks) account for about 22% of all births in high-income countries [43], and the majority of preterm and early term births occur spontaneously [14, 44].
Obstetric history is easy to collect in the clinical setting, and it could be of potential use for renal risk stratification in women. Existing prediction models for CKD and ESKD have not taken obstetric factors into consideration [45]. Further research is warranted to elucidate whether incorporating history of spontaneous preterm delivery, and other relevant obstetric factors, adds incremental value or clinically relevant information to the overall risk of renal disease for women when other demographic and cardiometabolic risk factors have been accounted for.
Conclusions
Women with a history of preterm delivery are at increased risk of maternal CKD and ESKD. The risk of renal disease is highest among women who have experienced very or extremely preterm deliveries, and those whose preterm delivery is medically indicated. Women who experience spontaneous preterm delivery are at increased risk of renal disease independently of preeclampsia and SGA. Preterm delivery may act as an important risk marker of adverse renal outcomes in the years and decades following pregnancy irrespective of causal mechanisms.
Availability of data and materials
Data are from the Swedish Medical Birth Register, National Patient Register, and Swedish Renal Register. Data cannot be put into a public data repository due to Swedish confidentiality regulations for registry data. Details on the application procedures for data usage are available on the homepages of the respective registries: the Medical Birth Register (https://www.socialstyrelsen.se/en/statistics-and-data/registers/alla-register/the-swedish-medical-birth-register/), the National Patient Register (https://www.socialstyrelsen.se/en/statistics-and-data/registers/alla-register/the-national-patient-register/), and the Swedish Renal Register (https://www.medscinet.net/snr/).
Abbreviations
- aHR:
-
Adjusted hazard ratio
- BMI:
-
Body mass index
- CI:
-
Confidence interval
- CKD:
-
Chronic kidney disease
- CRP:
-
C-reactive protein
- CVD:
-
Cardiovascular disease
- ESRD:
-
End-stage renal disease
- ICD:
-
International Classification of Diseases
- IUGR:
-
Intrauterine growth restriction
- LMP:
-
Last menstrual period
- MBR:
-
Medical Birth Register
- NPR:
-
National Patient Register
- SGA:
-
Small for gestational age
- SRR:
-
Swedish Renal Register
References
Hill NR, Fatoba ST, Oke JL, Hirst JA, O'Callaghan CA, Lasserson DS, et al. Global prevalence of chronic kidney disease - a systematic review and meta-analysis. PLoS One. 2016;11(7):e0158765.
Ji E, Kim YS. Prevalence of chronic kidney disease defined by using CKD-EPI equation and albumin-to-creatinine ratio in the Korean adult population. Korean J Intern Med. 2016;31(6):1120–30.
Gasparini A, Evans M, Coresh J, Grams ME, Norin O, Qureshi AR, et al. Prevalence and recognition of chronic kidney disease in Stockholm healthcare. Nephrol Dial Transplant. 2016;31(12):2086–94.
Tanz LJ, Stuart JJ, Williams PL, Rimm EB, Missmer SA, Rexrode KM, et al. Preterm delivery and maternal cardiovascular disease in young and middle-aged adult women. Circulation. 2017;135(6):578–89.
Heida KY, Velthuis BK, Oudijk MA, Reitsma JB, Bots ML, Franx A, et al. Cardiovascular disease risk in women with a history of spontaneous preterm delivery: a systematic review and meta-analysis. Eur J Prev Cardiol. 2016;23(3):253–63.
Bonamy AK, Parikh NI, Cnattingius S, Ludvigsson JF, Ingelsson E. Birth characteristics and subsequent risks of maternal cardiovascular disease: effects of gestational age and fetal growth. Circulation. 2011;124(25):2839–46.
Mosca L, Benjamin EJ, Berra K, Bezanson JL, Dolor RJ, Lloyd-Jones DM, et al. Effectiveness-based guidelines for the prevention of cardiovascular disease in women--2011 update: a guideline from the American Heart Association. J Am Coll Cardiol. 2011;57(12):1404–23.
Whelton PK, Carey RM, Aronow WS, Casey DE, Collins KJ, Himmelfarb CD, et al. 2017 ACC/AHA/AAPA/ABC/ACPM/AGS/APhA/ASH/ ASPC/NMA/PCNA guideline for the prevention, detection, evaluation, and management of high blood pressure in adults: executive summary: a report of the American college of cardiology/American Heart Association task force on clinical practice guidelines. Hypertension. 2018;71(6):1269–324.
Sandvik MK, Iversen BM, Irgens LM, Skjaerven R, Leivestad T, Softeland E, et al. Are adverse pregnancy outcomes risk factors for development of end-stage renal disease in women with diabetes? Nephrol Dial Transplant. 2010;25(11):3600–7.
Vikse BE, Hallan S, Bostad L, Leivestad T, Iversen BM. Previous preeclampsia and risk for progression of biopsy-verified kidney disease to end-stage renal disease. Nephrol Dial Transplant. 2010;25(10):3289–96.
Dai L, Chen Y, Sun W, Liu S. Association between hypertensive disorders during pregnancy and the subsequent risk of end-stage renal disease: a population-based follow-up study. J Obstet Gynaecol Can. 2018;40(9):1129–38.
Pariente G, Kessous R, Sergienko R, Sheiner E. Is preterm delivery an independent risk factor for long-term maternal kidney disease? J Matern Fetal Neonatal Med. 2017;30(9):1102–7.
Vikse BE, Irgens LM, Leivestad T, Skjærven R, Iversen BM. Preeclampsia and the risk of end-stage renal disease. N Engl J Med. 2008;359(8):800–9.
Goldenberg RL, Culhane JF, Iams JD, Romero R. Epidemiology and causes of preterm birth. Lancet. 2008;371(9606):75–84.
Wu CC, Chen SH, Ho CH, Liang FW, Chu CC, Wang HY, et al. End-stage renal disease after hypertensive disorders in pregnancy. Am J Obstetr Gynecol. 2014;210(2):147.e1–8.
Almasi O, Pariente G, Kessous R, Sergienko R, Sheiner E. Association between delivery of small-for-gestational-age neonate and long-term maternal chronic kidney disease. J Mater Fetal Neonatal Med. 2016;29(17):2861–4.
Brown HK, Speechley KN, Macnab J, Natale R, Campbell MK. Neonatal morbidity associated with late preterm and early term birth: the roles of gestational age and biological determinants of preterm birth. Int J Epidemiol. 2014;43(3):802–14.
Kirby RS, Wingate MS. Late preterm birth and neonatal outcome: is 37 weeks’ gestation a threshold level or a road marker on the highway of perinatal risk? Birth. 2010;37(2):169–71.
Delnord M, Blondel B, Prunet C, Zeitlin J. Are risk factors for preterm and early-term live singleton birth the same? A population-based study in France. BMJ Open. 2018;8(1):e018745.
Marsal K, Persson PH, Larsen T, Lilja H, Selbing A, Sultan B. Intrauterine growth curves based on ultrasonically estimated foetal weights. Acta Paediatr. 1996;85(7):843–8.
Barrett PM, McCarthy FP, Kublickiene K, Evans M, Cormican S, Judge C, et al. Adverse pregnancy outcomes and long-term risk of maternal renal disease: a systematic review and meta-analysis protocol. BMJ Open. 2019;9(5):e027180.
Wang IK, Muo CH, Chang YC, Liang CC, Chang CT, Lin SY, et al. Association between hypertensive disorders during pregnancy and end-stage renal disease: a population-based study. CMAJ. 2013;185(3):207–13.
Männistö T, Mendola P, Vääräsmäki M, Järvelin MR, Hartikainen AL, Pouta A, et al. Elevated blood pressure in pregnancy and subsequent chronic disease risk. Circulation. 2013;127(6):681–90.
Ayansina D, Black C, Hall SJ, Marks A, Millar C, Prescott GJ, et al. Long term effects of gestational hypertension and pre-eclampsia on kidney function: record linkage study. Pregnancy Hypertens Int J Womens Cardiovasc Health. 2016;6(4):344–9.
Kristensen JH, Basit S, Wohlfahrt J, Damholt MB, Boyd HA. Pre-eclampsia and risk of later kidney disease: nationwide cohort study. BMJ. 2019;365:l1516.
Tanz LJ, Stuart JJ, Williams PL, Missmer SA, Rimm EB, James-Todd TM, et al. Preterm delivery and maternal cardiovascular disease risk factors: the Nurses’ Health Study II. J Women's Health. 2002;2018:578–89.
Blake GJ, Ridker PM. Novel clinical markers of vascular wall inflammation. Circ Res. 2001;89(9):763–71.
Pitiphat W, Gillman MW, Joshipura KJ, Williams PL, Douglass CW, Rich-Edwards JW. Plasma C-reactive protein in early pregnancy and preterm delivery. Am J Epidemiol. 2005;162(11):1108–13.
Sattar N. Do pregnancy complications and CVD share common antecedents? Atheroscler Suppl. 2004;5(2):3–7.
Moghaddam Banaem L, Mohamadi B, Asghari Jaafarabadi M, Aliyan MN. Maternal serum C-reactive protein in early pregnancy and occurrence of preterm premature rupture of membranes and preterm birth. J Obstet Gynaecol Res. 2012;38(5):780–6.
Kugler E, Cohen E, Goldberg E, Nardi Y, Levi A, Krause I, et al. C reactive protein and long-term risk for chronic kidney disease: a historical prospective study. J Nephrol. 2015;28(3):321–7.
Mongelli M, Wilcox M, Gardosi J. Estimating the date of confinement: ultrasonographic biometry versus certain menstrual dates. Am J Obstet Gynecol. 1996;174(1 Pt 1):278–81.
Butt K, Lim K, Diagnostic IC. Determination of gestational age by ultrasound. J Obstetr Gynaecol Can. 2014;36(2):171–81.
SFOG-råd. Fetometri UltraARG 2010. Svensk Förening för Obstetrik och Gynekologi; 2019.
Clinical Practice Guidelines. Pregnancy care 2019 edition. Canberra: Australian Government, Department of Health; 2018.
Committee Opinion No. 700 Summary: methods for estimating the due date. Obstetrics and gynecology. 2017;129(5):967–8.
Persson PH, Weldner BM. Reliability of ultrasound fetometry in estimating gestational age in the second trimester. Acta Obstet Gynecol Scand. 1986;65(5):481–3.
Kullinger M, Granfors M, Kieler H, Skalkidou A. Adherence to Swedish national pregnancy dating guidelines and management of discrepancies between pregnancy dating methods: a survey study. Reprod Health. 2019;16(1):95.
Hamilton BE, Martin JA, Osterman MJ, Curtin SC, Matthews TJ. Births: final data for 2014. Natl Vital Stat Rep. 2015;64(12):1–64.
Ludvigsson JF, Andersson E, Ekbom A, Feychting M, Kim JL, Reuterwall C, et al. External review and validation of the Swedish national inpatient register. BMC Public Health. 2011;11:450.
Rapporteringen till nationella kvalitetsregister och hälsodataregistren. Jämförelser av täckningsgrader 2014. Stockholm: Socialstyrelsen; 2014.
The Swedish Medical Birth Register. A summary of content and quality. Stockholm: Centre for Epidemiology. The National Board of Health and Welfare; 2003.
Delnord M, Mortensen L, Hindori-Mohangoo AD, Blondel B, Gissler M, Kramer MR, et al. International variations in the gestational age distribution of births: an ecological study in 34 high-income countries. Eur J Pub Health. 2018;28(2):303–9.
Delnord M, Zeitlin J. Epidemiology of late preterm and early term births - an international perspective. Semin Fetal Neonatal Med. 2019;24(1):3–10.
Collins GS, Omar O, Shanyinde M, Yu LM. A systematic review finds prediction models for chronic kidney disease were poorly reported and often developed using inappropriate methods. J Clin Epidemiol. 2013;66(3):268–77.
Acknowledgements
Not applicable
Funding
This work was performed within the Irish Clinical Academic Training (ICAT) Programme, supported by the Wellcome Trust and the Health Research Board (grant number 203930/B/16/Z), the Health Service Executive National Doctors Training and Planning, and the Health and Social Care, Research and Development Division, Northern Ireland. PMB is employed as an ICAT Fellow. KK is supported by the Swedish Research Council (grant numbers 2018-00932 and 2009-1068), the Stockholm County Council (ALF), and the Swedish Kidney Foundation (Njurfonden). The funders had no role in the study design, data collection and analysis, decision to publish, or preparation of the manuscript.
Author information
Authors and Affiliations
Contributions
PMB and ASK had full access to all of the data in the study and take responsibility for the integrity of the data and the accuracy of the data analysis. KK and ASK are joint senior authors. The corresponding author attests that all listed authors meet authorship criteria and that no others meeting the criteria have been omitted. PMB is the guarantor. All authors contributed to the study concept and design. PMB, FPM, ME, MK, PS, KK, and ASK contributed to the acquisition, analysis, or interpretation of data. PMB contributed to the drafting of the manuscript. All authors contributed to the critical revision of the manuscript for important intellectual content. PMB and ASK contributed to the statistical analysis. PMB, ASK, and KK obtained the funding. FPM, IJP, KK, and ASK contributed to the study supervision. All authors read and approved the final manuscript.
Corresponding author
Ethics declarations
Ethics approval and consent to participate
All data were anonymised and non-identifiable. Merging of individual datasets was possible using a unique serial number (lpnr) derived from each participant’s identification number before the research team received the data [40]. Ethical approval was granted by the Swedish Ethical Review Authority in Stockholm (Regionala Etikprovningsnamnden Stockholm) (Dnr 2012/397-31/1) and by the Social Research and Ethics Committee, University College Cork (2019-109).
Consent for publication
It was not necessary to gain consent from individual participants for publication since anonymised data fall outside the remit of the European Union General Data Protection Regulation and Health Research Regulations 2018 (Ireland).
Competing interests
The authors declare that they have no competing interests.
Additional information
Publisher’s Note
Springer Nature remains neutral with regard to jurisdictional claims in published maps and institutional affiliations.
Supplementary information
Additional file 1: Supplementary Figure S1.
Timeline of study design.
Additional file 2: Supplementary Table S1.
ICD codes used for disease definitions.
Additional file 3: Supplementary Figure S2.
Flow chart illustrating construction of study cohort.
Rights and permissions
Open Access This article is licensed under a Creative Commons Attribution 4.0 International License, which permits use, sharing, adaptation, distribution and reproduction in any medium or format, as long as you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons licence, and indicate if changes were made. The images or other third party material in this article are included in the article's Creative Commons licence, unless indicated otherwise in a credit line to the material. If material is not included in the article's Creative Commons licence and your intended use is not permitted by statutory regulation or exceeds the permitted use, you will need to obtain permission directly from the copyright holder. To view a copy of this licence, visit http://creativecommons.org/licenses/by/4.0/. The Creative Commons Public Domain Dedication waiver (http://creativecommons.org/publicdomain/zero/1.0/) applies to the data made available in this article, unless otherwise stated in a credit line to the data.
About this article
Cite this article
Barrett, P.M., McCarthy, F.P., Evans, M. et al. Risk of long-term renal disease in women with a history of preterm delivery: a population-based cohort study. BMC Med 18, 66 (2020). https://0-doi-org.brum.beds.ac.uk/10.1186/s12916-020-01534-9
Received:
Accepted:
Published:
DOI: https://0-doi-org.brum.beds.ac.uk/10.1186/s12916-020-01534-9