Predicting hypertensive disorders in pregnancy using multiple methods: Models with the placental growth factor parameter
Abstract
BACKGROUND:
Placental growth factor (PlGF), one of the biomarkers, has a certain predictive effect on hypertensive disorders in pregnancy (HDP).
OBJECTIVE:
To study the HDP prediction effect of different methods for variable selection and modeling for models containing PlGF.
METHODS:
For the model containing PlGF, the appropriate range of PlGF parameters needed to be selected. Step-logistic regression and lasso were used to compare the model effect of twice range selection. The PlGF model with good predictive effect and appropriate detecting gestational age was selected for the final prediction.
RESULTS:
The effect of the model containing PlGF tested at 15–16 weeks was better than the PlGF value without comprehensive screening. The sensitivity of both methods was over 92%. By comprehensive comparison, the final model of lasso method in this study was more effective.
CONCLUSIONS:
In this study, a variety of methods were used to screen models containing PlGF parameters. According to clinical needs and model effects, the optimal HDP prediction model with PlGF parameters in the second trimester of 15–26 weeks of pregnancy was finally selected.
1.Introduction
Hypertensive disorders in pregnancy (HDP) is an important risk factor for increasing neonatal and maternal morbidity and mortality [1, 2, 3]. Early prediction and treatment can be carried out through related risk factors [4]. Preeclampsia in HDP is one of the most serious pregnancy complications [5, 6]. Studies have shown that placental growth factor (PlGF) was related to the diagnosis of HDP [7]. Nguyen et al. studied the predictive value of Soluble fms-Like Tyrosine Kinase 1 (sFlt-1) and PlGF for women at high risk of preeclampsia [8]. Combining maternal risk factors, mean arterial pressure (MAP), PlGF, and uterine artery pulsatility index (UTPI) for related prediction accuracy was higher [9]. Bian et al. used sFlt-1/PlGF ratio to predict the risk of preeclampsia in Asian women [10]. PlGF combined with other angiogenesis markers, such as sFlt-1, also had a certain prognostic value for preeclampsia [11, 12]. There are also some controversies in related prediction research. Cnossen et al. found that the predictive value of uterine artery Doppler studies alone for early and late onset preeclampsia was very low [13]. No test could reliably predict preeclampsia, and further prospective studies were needed to prove the clinical utility of predictors [14].
A large number of foreign studies have confirmed the role of PlGF in predicting HDP. Such as using maternal factors plus biomarkers (PlGF, etc.) for prediction. But the associated clinical utility was unclear. For PlGF, one of biomarkers, the appropriate range of PlGF parameters included in the predictive model needed to be further selected. Moreover, variable screening methods were mostly based on the statistical indicator (P value), rather than comprehensive screening of risk factors. The data analysis method of this study mainly included two aspects: variable selection and model methods. Model parameters were screened based on the effects of various models containing PlGF, and several model methods were comprehensively selected to compare the prediction effects.
2.Materials and methods
2.1Subjects
The data source of this study: 1368 cases collected from July 2015 to December 2016 provided by the Obstetrics Department of Peking University People’s Hospital. After the pregnant women gave birth, according to the doctor’s final diagnosis, the subjects were divided into 186 HDP group and 1182 control (normal pregnancy) group.
Exclusion criteria for overall data: pregnant women with chronic hypertension combined with pregnancy or eclampsia; cases with incomplete factors or data; singular values.
2.2Classification of risk factors
The model parameters selected in this study were shown in Table 1.
Table 1
Classification of risk factors for HDP
| Category | Risk factors |
|---|---|
| Basic situation | Age, Gravidity, Parity, Height, Pre-BMI |
| Family history | Family history of hypertension |
| Diseases | GDM, Diabetes mellitus with pregnancy, Pregnancy with immune system disease |
| The situation of this pregnancy | SBP, DBP, MAP, GA-W |
| Biomarkers | PlGF |
Notes: Pre-BMI: Pre-pregnancy body mass index; Diseases: Existing or potential underlying medical diseases and pathological conditions; GDM: Gestational diabetes mellitus; SBP, DBP, MAP: Systolic blood pressure, Diastolic blood pressure, and Mean arterial pressure all at 11–13 weeks of pregnancy; GA-W: Weight gain during pregnancy.
2.3For PlGF parametric model
2.3.1Preliminary screening of PlGF parameters
In this study, we reviewed the cases where serum PlGF was mainly tested twice. The gestational week of the next test (mainly starting at 15 weeks) was greater than the previous one. Therefore, 211 cases of data were preliminarily selected. Among them, 37 cases were in the HDP group (pregnant women without chronic hypertension combined with pregnancy and eclampsia); 174 cases were in the control (normal pregnancy) group. The ratio of training set to test set was 7:3. In the training set, there were 28 cases in the HDP group and 119 cases in the control group. In the test set, there were 9 cases and 55 cases in the HDP group and control group, respectively.
About the parameters of PlGF: PlGF
2.3.2Selection of the appropriate model with PlGF parameter
The main biological function of PlGF is to promote the formation of placental blood vessels [10, 11]. PlGF is a kind of biomarker. Changes in serum PlGF of healthy pregnant women during pregnancy: PlGF levels are low at 5–15 weeks of gestation, and PlGF increases rapidly at 15–26 weeks, reaching a peak at 28–30 weeks of gestation.
And the main distribution of PlGF measured twice was also concentrated in 15–26 weeks. Combined with the variable screening and model effect of 2.3.1, the appropriate model with PlGF parameter could be selected. Finally, this study selected the serum PlGF test data at 15–26 weeks. The PlGF test for this study was a dry fluorescence immunoassay analyzer from Hebei Twente Biotechnology Development Co., Ltd. Table 2 showed the normal range of PlGF value provided by the company that tested PlGF in this study.
Table 2
Normal range of PlGF value
| Gestational weeks | PlGF value (pg/ml) |
|---|---|
| 5–15 weeks | 35 |
| 16–20 weeks | 60 |
| 100 | |
| Placental insufficiency raises the risk of preterm birth ( | High risk: |
According to Table 2, the data of serum PlGF in 15–26 weeks were specifically selected. When PlGF has multiple detection values at 15–26 weeks, it generally takes a relatively abnormal value. At 15 weeks, PlGF value
Finally, the results of this study selected data for a total of 922 cases. There were 85 cases in the HDP group (pregnant women without chronic hypertension combined with pregnancy and eclampsia) and 837 cases in the control (normal pregnancy) group. For the training set: 57 cases of HDP group, 588 cases of control group. For the test set: 28 cases of HDP group, 249 cases of control group. The ratio of the two data sets was 7:3.
2.4Data and statistical analysis
IBM SPSS statistics 23.0 software was used for data analysis. Step-logistic regression and lasso was used for model research in R studio (R version 4.0.1) Step-logistic regression and lasso are both regression methods in nature. Both of them have the function of automatic variable screening. The two regression methods are combined to carry out variable screening and modeling. The significance level alpha was set to 0.05. A 95% confidence interval was set in this study.
3.Results
In this study, the categories of predictive model parameters were derived from Table 1. For the model containing PlGF, the situation before the screening in 2.3.1 and after the screening in 2.3.2 was compared, as shown in Tables 3 and 4. Except for PlGF, all the other parameters (see Table 1) existed consistently before being included in the prediction model for automatic variable screening in 2.3.1 and 2.3.2.
Table 3
Comparison of the two models before screening
| Model-PlGF |
| AUC (95%CI) | Sensitivity | Specificity |
|---|---|---|---|---|
| Step-logistic regression | 0.062 | 0.695 (0.526–0.864) | 0.789 | 0.573 |
| Lasso | 0.008 | 0.776 (0.649–0.903) | 0.883 | 0.581 |
Notes:
Table 4
Comparison of two models for detecting PlGF in 15–26 weeks
| Model-PlGF (15–26 w) |
| AUC (95%CI) | Sensitivity | Specificity |
|---|---|---|---|---|
| Step-logistic regression | 0.000 | 0.798 (0.703–0.893) | 0.929 | 0.590 |
| Lasso | 0.000 | 0.807 (0.721–0.893) | 0.929 | 0.643 |
Notes:
For the models without PlGF screening in Table 3, the step-logistic regression test of PlGF
Table 5
Final model situation
| Model parameters | Coefficient |
|---|---|
| Pre-BMI | 0.07051 |
| Family history of hypertension | 0.39227 |
| Diabetes mellitus with pregnancy | 0.23397 |
| Pregnancy with immune system disease | 0.04001 |
| DBP | 0.00806 |
| MAP | 0.10351 |
| PlGF | |
| Constant |
Notes: Pre-BMI: Pre-pregnancy body mass index; DBP, MAP: Diastolic blood pressure and Mean arterial pressure both at 11–13 weeks of pregnancy.
4.Discussion
Some angiogenic factors (Soluble fms-Like Tyrosine Kinase 1 (sFlt-1), placental growth factor (PlGF), and Soluble endothelin) in the second trimester may be tools for predicting preeclampsia [14]. Numerous studies have demonstrated that sFlt-1 and PlGF can play a role in the prediction of early preeclampsia in the second trimester [15]. Knudsen et al. also affirmed the independent predictive effect of PlGF [16]. The levels of sFlt-1 and PlGF in pregnant women in Malaysia could be used as biochemical indicators of gestational hypertension [17]. As a predictive marker of preeclampsia, PlGF could simplify the clinical management of preeclampsia and reduced costs [18].
This study used maternal basic factors and PlGF, and also confirmed the predictive role of PlGF in the second trimester. Based on the quality and effect of the model, comprehensive variable screening and modeling analysis and prediction were carried out.
5.Conclusion
In addition to basic statistical analysis, this research had comprehensive advantages in variable selection and model building. Maternal factors and biomarker PlGF were combined to predict. Based on the model and clinical needs, a comprehensive screening analysis was carried out to select the optimal prediction model plan containing the PlGF parameter. Finally, the PlGF value of 15–26 weeks (the second trimester) was selected for model research containing the PlGF parameter. The PlGF test in step-logistic regression was statistically significant (
Acknowledgments
This research was supported by the National Key R&D Program of China (2019YFC0119700), Bill & Melinda Gates Foundation (OPP1148910), Beijing International Science and Technology Cooperation Base for Intelligent Physiological Measurement and Clinical Transformation, and the prospective multicenter study of placental growth factor combined with maternal factors in predicting the onset of hypertensive disorders in pregnancy.
Conflict of interest
None to report.
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