Communication between mother and fetus : Imprinting and endocrine adaptations to pregnancy
Lead Research Organisation:
Queen Mary University of London
Department Name: William Harvey Research Institute
Abstract
Context:
Pregnancy is associated with high rates of morbidity and mortality despite broad advances in healthcare over the last 50 years. In addition, as rates of obesity and diabetes increase in the general population, the outcomes of pregnancy have worsened and maternal and fetal health remains a significant public health issue. Underlying this is a lack understanding of how energy is diverted to the fetus from the mother during gestation, and how this goes wrong as a result of the interaction between altered maternal diet and genetic factors. In addition, there are few diagnostic tools available to detect when the energy supply to the fetus is compromised, and consequently paediatric clinicians have a paucity of information upon which to act to improve outcomes for pregnant women and their children.
Aims and objectives:
We propose to increase our basic knowledge about how the fetus gains resources from the mother during pregnancy. In late gestation, when the fetus is growing very rapidly, the mother must be able to deliver maximal resources. One way in which the mother's body knows to do this is because the placenta releases hormones into the maternal circulation that signal redistribution of maternal nutrients obtained from food. For example, during late gestation the mother becomes less likely to convert excess dietary glucose into stored fat, and instead the glucose is transported across the placenta to become fuel for fetal growth. We work on a signalling molecule called DLK1, which increases in concentration in maternal blood during pregnancy in mice. Others have found that this increase in maternal DLK1 also occurs during human pregnancy. We recently proved (using genetically modified mice that have a mutation in their Dlk1 gene) that this molecule must come from the fetus or the placenta. We propose to discover if DLK1 is a placental hormone, and if the human placenta is also a source of DLK1. In non-pregnant females the amount of DLK1 in the blood is low. We found that genetically modified mice that make high levels of DLK1 store less energy as fat, and use fats rather than glucose as an energy source. This is very similar to what happens in pregnancy when DLK1 is naturally high. We hypothesise is that the fetus uses DLK1 as a signal to instruct the mother to make more energy available for fetal growth. We will test this hypothesis, and aim to discover how this potentially novel hormone works.
DLK1 is encoded by a member of a group of genes that are regulated in an unusual way. Each gene in the genome is present in two copies, one inherited from the father and the other from the mother. In most circumstances both of these genes form the template for producing proteins. However, a group of ~100 genes in the mammalian genome are only expressed from one parental copy, and the other copy is silenced, the imprinted genes. Imprinted genes are known to encode molecules that have crucial functions in growth and development, as well as in metabolic processes during adulthood.
The maternal pituitary gland is known to change its size and hormone output during pregnancy. DLK1, and other imprinted products are expressed in the pituitary gland, and are regulated by pregnancy. We would like to understand if imprinted genes mediate maternal pituitary function during pregnancy, and how they are activated during this period. This is important because if the maternal pituitary gland does not adapt appropriately to pregnancy the growth and wellbeing of both mother and fetus are compromised.
Potential applications and benefits.
It is likely that maternal DLK1 levels differ between normal pregnancies and those where fetal growth is compromised such as in preeclampsia and intrauterine growth restriction. Our hope is that by understanding its source and function we could in the future use maternal DLK1 levels as a novel non-invasive marker of fetal well being, informing clinical practice to improve pregnancy outcomes
Pregnancy is associated with high rates of morbidity and mortality despite broad advances in healthcare over the last 50 years. In addition, as rates of obesity and diabetes increase in the general population, the outcomes of pregnancy have worsened and maternal and fetal health remains a significant public health issue. Underlying this is a lack understanding of how energy is diverted to the fetus from the mother during gestation, and how this goes wrong as a result of the interaction between altered maternal diet and genetic factors. In addition, there are few diagnostic tools available to detect when the energy supply to the fetus is compromised, and consequently paediatric clinicians have a paucity of information upon which to act to improve outcomes for pregnant women and their children.
Aims and objectives:
We propose to increase our basic knowledge about how the fetus gains resources from the mother during pregnancy. In late gestation, when the fetus is growing very rapidly, the mother must be able to deliver maximal resources. One way in which the mother's body knows to do this is because the placenta releases hormones into the maternal circulation that signal redistribution of maternal nutrients obtained from food. For example, during late gestation the mother becomes less likely to convert excess dietary glucose into stored fat, and instead the glucose is transported across the placenta to become fuel for fetal growth. We work on a signalling molecule called DLK1, which increases in concentration in maternal blood during pregnancy in mice. Others have found that this increase in maternal DLK1 also occurs during human pregnancy. We recently proved (using genetically modified mice that have a mutation in their Dlk1 gene) that this molecule must come from the fetus or the placenta. We propose to discover if DLK1 is a placental hormone, and if the human placenta is also a source of DLK1. In non-pregnant females the amount of DLK1 in the blood is low. We found that genetically modified mice that make high levels of DLK1 store less energy as fat, and use fats rather than glucose as an energy source. This is very similar to what happens in pregnancy when DLK1 is naturally high. We hypothesise is that the fetus uses DLK1 as a signal to instruct the mother to make more energy available for fetal growth. We will test this hypothesis, and aim to discover how this potentially novel hormone works.
DLK1 is encoded by a member of a group of genes that are regulated in an unusual way. Each gene in the genome is present in two copies, one inherited from the father and the other from the mother. In most circumstances both of these genes form the template for producing proteins. However, a group of ~100 genes in the mammalian genome are only expressed from one parental copy, and the other copy is silenced, the imprinted genes. Imprinted genes are known to encode molecules that have crucial functions in growth and development, as well as in metabolic processes during adulthood.
The maternal pituitary gland is known to change its size and hormone output during pregnancy. DLK1, and other imprinted products are expressed in the pituitary gland, and are regulated by pregnancy. We would like to understand if imprinted genes mediate maternal pituitary function during pregnancy, and how they are activated during this period. This is important because if the maternal pituitary gland does not adapt appropriately to pregnancy the growth and wellbeing of both mother and fetus are compromised.
Potential applications and benefits.
It is likely that maternal DLK1 levels differ between normal pregnancies and those where fetal growth is compromised such as in preeclampsia and intrauterine growth restriction. Our hope is that by understanding its source and function we could in the future use maternal DLK1 levels as a novel non-invasive marker of fetal well being, informing clinical practice to improve pregnancy outcomes
Technical Summary
Late gestation in mammals is accompanied by multiple adaptations of maternal energy homeostasis, to divert maternal resources towards the supply of glucose for the rapidly-growing fetus. These adaptations include a reduction in hepatic lipogenesis and adipose deposition. During pregnancy there is considerable remodelling of the anterior pituitary which causes an increase in somatolactotrophic cells. In addition, the placenta secretes placental lactogen and a pregnancy-specific version of growth hormone (GH). Since GH and its family members cause insulin resistance and inhibit hepatic lipogenesis, increased activity of the pituitary-placental axis is thought to modulate maternal adaptations in late pregnancy.
The product of the imprinted Delta-like homologue 1, DLK1, is a signalling molecule that reaches a high concentration in maternal serum from mid to late pregnancy in rodents and humans. We recently discovered that that the conceptus is the source, and that DLK1 may therefore be a novel endocrine signal from fetus to mother. Our studies with genetically-modified mice show that endocrine DLK1 acts to inhibit hepatic lipogenesis and increase beta oxidation in skeletal muscle. Moreover, elevated DLK1 causes an increase in pituitary GH secretion.
Using genetic models of altered Dlk1 gene dosage, we will test the hypothesis that DLK1 produced by the conceptus alters the activity of the pituitary-placental axis, modulating important metabolic changes in maternal resource allocation. Moreover, Dlk1 is a member of an imprinted gene network that we propose acts in the maternal pituitary gland during pregnancy. We wish to understand the regulation of this network.
Understanding the function of DLK1 and other imprinted genes in pregnancy has potential clinical value since failures of growth and timely development occur when maternal resource allocation is disrupted. Moreover, maternal serum DLK1 could be used as a non-invasive biomarker of poor pregnancy outcome.
The product of the imprinted Delta-like homologue 1, DLK1, is a signalling molecule that reaches a high concentration in maternal serum from mid to late pregnancy in rodents and humans. We recently discovered that that the conceptus is the source, and that DLK1 may therefore be a novel endocrine signal from fetus to mother. Our studies with genetically-modified mice show that endocrine DLK1 acts to inhibit hepatic lipogenesis and increase beta oxidation in skeletal muscle. Moreover, elevated DLK1 causes an increase in pituitary GH secretion.
Using genetic models of altered Dlk1 gene dosage, we will test the hypothesis that DLK1 produced by the conceptus alters the activity of the pituitary-placental axis, modulating important metabolic changes in maternal resource allocation. Moreover, Dlk1 is a member of an imprinted gene network that we propose acts in the maternal pituitary gland during pregnancy. We wish to understand the regulation of this network.
Understanding the function of DLK1 and other imprinted genes in pregnancy has potential clinical value since failures of growth and timely development occur when maternal resource allocation is disrupted. Moreover, maternal serum DLK1 could be used as a non-invasive biomarker of poor pregnancy outcome.
Planned Impact
We will seek to impact the wider community in 3 ways:
1) The outcome of this project will lead to greater understanding of how failures of energy allocation to the fetus bring about common complications of pregnancy such as intrauterine growth restriction and placental insufficiency. This understanding could ultimately lead to new diagnostic tests/interventions to treat these disorders. Production of such a test will also have value to the economy.
2) Disseminating basic research findings and technical skills to the medical/clinical training community.
3) Public dissemination of science. We will work with Games Design students at the University of East London to prototype a computer game on the theme of 'Maternal-Fetal Interaction'. A successful prototype will be publicised on the UEL Games website and potentially be pitched for further development to a public dissemination funding body such as the Wellcome Trust.
1) The outcome of this project will lead to greater understanding of how failures of energy allocation to the fetus bring about common complications of pregnancy such as intrauterine growth restriction and placental insufficiency. This understanding could ultimately lead to new diagnostic tests/interventions to treat these disorders. Production of such a test will also have value to the economy.
2) Disseminating basic research findings and technical skills to the medical/clinical training community.
3) Public dissemination of science. We will work with Games Design students at the University of East London to prototype a computer game on the theme of 'Maternal-Fetal Interaction'. A successful prototype will be publicised on the UEL Games website and potentially be pitched for further development to a public dissemination funding body such as the Wellcome Trust.
People |
ORCID iD |
| Marika Charalambous (Principal Investigator) |
Publications
Cassidy FC
(2018)
Genomic imprinting, growth and maternal-fetal interactions.
in The Journal of experimental biology
Cleaton MA
(2016)
Fetus-derived DLK1 is required for maternal metabolic adaptations to pregnancy and is associated with fetal growth restriction.
in Nature genetics
Furse S
(2021)
A pipeline for making 31P NMR accessible for small- and large-scale lipidomics studies
in Analytical and Bioanalytical Chemistry
Howard M
(2015)
Molecular basis of imprinting disorders affecting chromosome 14: lessons from murine models.
in Reproduction (Cambridge, England)
Macdougall C
(2018)
Visceral Adipose Tissue Immune Homeostasis Is Regulated by the Crosstalk between Adipocytes and Dendritic Cell Subsets
in Cell Metabolism
Macdougall Claire E.
(2018)
Visceral Adipose Tissue Immune Homeostasis Is Regulated by the Crosstalk between Adipocytes and Dendritic Cell Subsets
in CELL METABOLISM
Novoselova TV
(2018)
MRAP deficiency impairs adrenal progenitor cell differentiation and gland zonation.
in FASEB journal : official publication of the Federation of American Societies for Experimental Biology
Pedraza-Arevalo S
(2022)
Epigenetic and post-transcriptional regulation of somatostatin receptor subtype 5 (SST5 ) in pituitary and pancreatic neuroendocrine tumors.
in Molecular oncology
Scagliotti V
(2021)
Dynamic Expression of Imprinted Genes in the Developing and Postnatal Pituitary Gland.
in Genes
| Description | EQUIPMENT COMPETITION FOR MRC-FUNDED MID-CAREER RESEARCHERS IN UK UNIVERSITIES |
| Amount | £80,000 (GBP) |
| Funding ID | C0489 |
| Organisation | University of Western Australia |
| Department | Raine Medical Research Foundation |
| Sector | Academic/University |
| Country | Australia |
| Start | 03/2014 |
| End | 03/2015 |
| Description | Marie Curie Actions: WHRI Academy Fellowship |
| Amount | € 74,714 (EUR) |
| Organisation | William Harvey International Translational Research (WHRI) Academy |
| Sector | Public |
| Country | United Kingdom |
| Start | 04/2016 |
| End | 03/2018 |
| Description | QMUL School of Medicine funded PhD studentship |
| Amount | £84,000 (GBP) |
| Organisation | Queen Mary University of London |
| Sector | Academic/University |
| Country | United Kingdom |
| Start | 10/2014 |
| End | 09/2017 |
| Description | Society for Endocrinology Early Careers Grant |
| Amount | £10,000 (GBP) |
| Organisation | Society for Endocrinology |
| Sector | Charity/Non Profit |
| Country | United Kingdom |
| Start | 06/2016 |
| End | 05/2017 |
| Title | Refining the 'AdipoChaser' model for monitoring of adipose tissue development and turnover. |
| Description | We have adapted the murine in-vivo adipose tracing methodology from the Scherer lab (Wang, 2013) to include a fluorescent reporter. Our system provides significant advantages over the classical AdipoChaser: i) live cells labelled with membrane bound proteins can be readily counted, sorted by flow cytometry and cultured, ii) all cells are labelled (either red or green) so quantitative measures of cell proportion can be made, iii) and minimal tissue processing is required in order to visualise the cells. This method also represents an animal welfare refinement since multiple measurements can be made from a single animal, necessitating fewer animals to be used in the overall programme of work. |
| Type Of Material | Model of mechanisms or symptoms - mammalian in vivo |
| Provided To Others? | No |
| Impact | We have yet to publish any data resulting from this method. |
| Description | COST:Imprinting Disorders |
| Organisation | EU-T0 |
| Country | European Union (EU) |
| Sector | Public |
| PI Contribution | This is a training network. I have participated in the annual training meeting, the 'Imprinting School'. I have given lectures in 2014 and will do so in 2016. Members of my group presented their research in 2015. |
| Collaborator Contribution | The network paid for my attendance at their 'Imprinting School' at 2014-2016, and to an additional meeting in Naples in 2015 where I presented my work. My lab members received funds to attend the Imprinting School in 2015. |
| Impact | I converted my 2014 lecture into a review 'Molecular basis of imprinting disorders affecting chromosome 14: lessons from murine models.', published in Reproduction in May 2015. |
| Start Year | 2013 |
| Description | Pregnancy Outcome Prediction Study |
| Organisation | University of Cambridge |
| Country | United Kingdom |
| Sector | Academic/University |
| PI Contribution | We initiated this collaboration when data from our reseach indicated that there may be important clinical translation. We have performed experiments and guided the intellectual progress of this collaboration, which uses our experimental models to address clinically-relevant issues. |
| Collaborator Contribution | Our collaborators have established a unique clinical resource, an extremely well phenotyped large prospective cohort of pregnant women. Measurements were taken during pregnancy and after birth, and biological materials are available from these women. We have used these data and materials to generate experimental data that translates our primary findings into the clinical sphere.Our collaborators are experts in diagnosis and treatment of obstetric disorders - we benefit from their considerable expertise. |
| Impact | Our intial collaboration resulted in a paper published in Nature Genetics in 2017, Cleaton, et. al. With Profs Gordon Smith and Steven Charnock-Jones who led the POP study, I applied for further funding to follow up the initial finding of the 2017 paper. We were awarded a project grant by the MRC, MR/R022836/1, which commenced in August 2018. |
| Start Year | 2017 |
| Description | Barts and Queen Mary Science Festival |
| Form Of Engagement Activity | Participation in an activity, workshop or similar |
| Part Of Official Scheme? | No |
| Geographic Reach | Local |
| Primary Audience | Public/other audiences |
| Results and Impact | This year the QMUL Epigenetics Hub (including PhD students form my research group) took part in the Barts and Queen Mary Science Festival. The event is held annually and is aimed at anyone interested in science from children and teenagers to adults of any age. The 2015 event was opened by Professor Vernon Trafford and had over 400 attendees. The Epigenetics Hub stand was designed and manned by PhD students and Post-Doctoral Researchers representing each of the labs involved in the QMUL Epigenetics Hub. Topics introduced to attendees on the day covered the role of epigenetics in everything from cancer to learning behaviours and included kid-friendly explanations of the molecular mechanisms behind these phenomena. Our stand sparked lots of interest from attendees, and many felt that they left knowing a little more about this complex scientific area. |
| Year(s) Of Engagement Activity | 2015 |
| URL | http://www.blizard.qmul.ac.uk/research-groups/1247.html |
| Description | Widening Participation activity to Year 5 schoolchildren in the local area of QMUL |
| Form Of Engagement Activity | Participation in an activity, workshop or similar |
| Part Of Official Scheme? | No |
| Geographic Reach | Local |
| Primary Audience | Schools |
| Results and Impact | In 2015 MC planned and led a public engagement exercise in partnership with the QMUL Widening Participation (WP) outreach team. QMUL is committed to delivering continued outreach provision, which will motivate and inform students to consider higher education. We understand that in order to have maximum impact and truly inspire students, we must work with young people frequently and from an early age. The workshop was for 30 primary school children from Year 5, entitled 'How to be a biologist.' The objectives were 1) for the children to meet a scientist and to get a feeling for what doing science as a job is like, 2) To learn about some of the tools that we use in a biology lab, and 3) to do an experiment, including planning, conducting the experiment, displaying the results and interpreting them. The workshop was well received and will be repeated with refinements at subsequent QMUL WP events. Many of the children had never met a scientist before, and said after the workshop that they would consider going to university to study science. |
| Year(s) Of Engagement Activity | 2015 |