The REVAMP study: research exploring various aspects and mechanisms in preeclampsia: study protocol

We hypothesize that LCPUFA and one carbon metabolite status among Indian women play a causal role in the etiology of preeclampsia, mediated by changes in oxidative stress and growth factors which alter placental development.

Dietary folate and vitamin B₁₂ are considered as important nutritional constituents of the one carbon cycle for the supply of methyl groups for the remethylation of homocysteine to methionine which is then converted to SAM, a major methyl donor. Any alteration in the one carbon cycle leads to increased homocysteine levels which is associated with higher oxidative stress. Our studies have demonstrated that folate and vitamin B₁₂ are interlinked with DHA in the one carbon cycle. Alpha linolenic acid (ALA), an omega-3 fatty acid is the dietary precursor for the synthesis of LCPUFA such as DHA. Omega-3 fatty acids are extremely important during pregnancy as they are critical building blocks of fetal brain and retina. Any alteration in the conversion, transport, storage or utilization of fatty acids may reduce maternal LCPUFA levels, thereby reducing the levels of placental phospholipids containing these LCPUFA. Membrane phospholipids are the major methyl group acceptors, where the PE containing LCPUFA accepts methyl group from SAM to form PC containing LCPUFA. Reduced phospholipids may therefore divert the flux of methyl groups from SAM to DNA and histone thereby affecting DNA and histone methylation patterns. This may affect the gene expression patterns of various transcription factors and growth factors. In addition, reduced fatty acids are also known to affect the regulation of various transcription factors thereby affecting the expression of various growth factors involved in placental growth and development. This may lead to endothelial dysfunction thereby affecting the growth and development of the placenta and fetus, ultimately resulting into preeclampsia (Fig. 1).

The REVAMP study (Research Exploring Various Aspects and Mechanisms in Preeclampsia) proposes to examine the associations of maternal LCPUFA and one carbon micronutrient status in early gestation with clinical outcome in preeclampsia and to understand the underlying key biochemical and molecular mechanisms. It consists of 4 sub-projects:

The proposed study will answer the following questions:

The REVAMP study has been funded by the Indian Council of Medical Research (ICMR) as a Centre for Advanced Research Project - “Investigating mechanisms leading to preeclampsia” (5/7/1069/13-RCH dated 31-03-2017). The study is being carried out at the Interactive Research School for Health Affairs (IRSHA) in collaboration with Bharati Medical College and Hospital, Pune; Gupte Hospital and Research Centre, Pune; and Council of Scientific and Industrial Research-Centre for Cellular and Molecular Biology (CSIR-CCMB), Hyderabad. The current study is ongoing and the total duration of the study is five years i.e. from 31st March 2017 – 30th March 2022.

The study has been approved by the Institutional Ethics Committee, Bharati Vidyapeeth Deemed University (IEC/2015/37, dated 03.10.2015).

The ICMR Centre for Advanced Research Project was set up in March 2017. Patients coming to the outpatient departments of the Department of Obstetrics and Gynecology of Bharati Vidyapeeth Medical College and Hospital, Pune, and Gupte Hospital and Research Centre, Pune form the participants of the current study. Pregnant women attending the hospital for their first obstetric visit are informed about the study and their participation is solicited. Written consent is obtained from the women, including broad consent for further measurements of biochemical and molecular markers.

Our earlier preliminary study on erythrocyte fatty acid levels in women with preeclampsia (n = 58) and normotensive controls (n = 137) at 16–18 weeks of gestation showed a mean difference of 0.3 and standard deviation of 0.8 [49]. We aim to study 100 women with preeclampsia and 200 normotensive women, which will give 87% power to detect a difference of the same magnitude when alpha is kept at 0.05. If the standard error is increased by 10%, the power will become 80%. For every case of preeclampsia, 2 normotensive controls will be randomly chosen from all non-preeclampsia pregnancies. Considering the incidence of preeclampsia to be around 8–10%, we will enroll ~ 1000 pregnant women until we get 100 cases of preeclampsia with complete data collection.

All consenting participants are recruited at 11–14 weeks of gestation (visit 1 – V1), assigned a unique participant code, and subsequently followed across gestation at three time points viz. 18–22 weeks (visit 2 – V2), 26–28 weeks (visit 3 – V3) and at delivery. All data are recorded in a booklet that includes the various questionnaires, covering the following:

Figure 4 shows the collection of maternal blood, cord blood, and placental samples at different time points. Various biochemical and molecular measures to be estimated are summarized in the Fig. 4. The biochemical measures and the molecular measures such as gene expression and global DNA methylation are carried out at IRSHA, Pune. Gene specific methylation analysis will be carried out CSIR-CCMB, Hyderabad. Histopathological analysis on placental samples will be carried out at Department of Pathology, Bharati Vidyapeeth Medical College, Pune.

This project allows us to form a secure Indian Biobank consisting of the various biological samples collected under this project, and the associated data, and facilitate access to other investigators. External researchers can propose projects, and what the sample resource and/or data they require, and sharing will be carried out following approval by a scientific steering committee. The samples collected are stored at IRSHA, Bharati Vidyapeeth (Deemed to be University), Pune. Strict procedures are used to protect the confidentiality of the study participant’s data and samples. Memorandum of understanding (MOUs) will be undertaken as per Government of India rules and regulations.

Different aliquots for different fractions i.e. plasma, erythrocyte, lymphocytes, serum, and placenta are stored in different − 80 °C freezers. A stock record (manual and computerized) is maintained for each sample, including date of sample collection and processing, sample quantity, number of aliquots for each sample, position of each aliquot in the freezer, and end user details. Access to the freezer is restricted to authorized trained personnel only.

The laboratory staff will be blinded to the identity of the samples. Inter- and intra- observer/laboratory reliability assays have been performed. For example, inter-laboratory comparison for angiogenic factors was undertaken at All India Institute of Medical Sciences (AIIMS), Delhi and at IRSHA. An inter-laboratory comparison for fatty acid analysis by Gas Chromatography was carried out at three laboratories – IRSHA, AIIMS, Delhi and National Institute of Nutrition (NIN), Hyderabad. Color Doppler and USG assessments are validated on a sub-sample by an expert in the field.

All study participants’ information is stored in locked filing cabinets with limited access. Double data entry is performed to reduce errors. Data confidentiality is maintained and datasets are anonymized before any analysis. An experienced statistical consultant will help in selecting and implementing data analysis methods.

To initiate the project a series of meetings were held with the clinicians from both the participating hospitals. Subsequent meetings were held with clinicians to finalize various aspects related to sample collection and processing. Discussions were also held with the collaborators from CCMB to finalize issues related to sample processing for epigenetic work. Aspects related to information on participants’ family and personal history, SLI, physical activity, FFQ and 24 h dietary recall data, infant proforma, feeding practices, and child follow-up data were discussed and finalized with expert advisors.

A Scientific Advisory Committee has been formed which consists of clinicians, research scientists, and research experts viz. Professor Caroline HD Fall (University of Southampton, UK), Professor C. S. Yajnik (KEM Hospital, Pune), Dr. Anura Kurpad (St. John’s Medical College, Bangalore), Dr. K. Kumaran (MRC Lifecourse Epidemiology Unit, Southampton & Holdsworth Memorial Hospital, Mysore), Dr. Julian Crasta (St. John’s Medical College, Bangalore), Dr. Lakshmy Ramakrishnan (All India Institute of Medical Sciences, New Delhi), Dr. Arun Kinare (Bharati Medical College and Hospital, Pune), Dr. Suhas Otiv (KEM Hospital, Pune). A series of annual meetings are being held with the advisory committee to discuss scientific aspects and the monitoring of the progress made in this project. Reports are submitted to Indian Council of Medical Research (ICMR) and a face-to-face meeting is held each year.

The present study will be useful in:

Children born to mothers with preeclampsia are at an increased risk of developing cardiovascular disease, diabetes and neurodevelopmental disorders in later life. The proposed study will systematically and comprehensively investigate the key biochemical and molecular mechanisms contributing to preeclampsia. We expect to identify novel circulating proteins which predict the risk of developing preeclampsia. Identification of such factors may provide clues for therapeutic interventions. The study will furthermore give insights into novel epigenetic mechanisms in the placenta which may lead to impaired placentation and fetal growth in preeclampsia. This study will also help us to establish the correct reference baseline for vital nutrients like omega-3 fatty acids for the Indian population as, such data is long overdue. An improved understanding of these factors will help guide development of public health interventions to reduce and curtail the burden of non-communicable diseases (NCDs) in India.

The proposed comprehensive basic science, translational and public health oriented collaborative research plan between basic scientists and clinicians will help to understand the origin of preeclampsia in the mother and its metabolic consequences in their offspring. This research includes identifying biomarkers like growth factors in the plasma for the early prediction of risk for developing preeclampsia.