Obesity in Pregnancy May Up Risk of Heart Disease in Offspring
Being obese during pregnancy can impair the function of the fetus's heart later, reveals a new mice study.
The study, published in Journal of Physiology found that maternal obesity causes molecular changes in the heart of the fetus and alters the expression of genes related to nutrient metabolism, which greatly increases the offspring's risk of cardiac problems in later life.
‘Understanding the mechanisms involved can help develop new treatments that could help prevent later-life cardiometabolic illnesses early.’
This is the first study to show that the heart is �programmed' by the nutrients it receives in fetal life. Changes in the expression of genes alter how the heart normally metabolizes carbohydrates and fats. They shift the heart's nutrient preference further toward fat and away from sugar. As a result, the hearts of fetuses of obese female mice were larger, weighed more, had thicker walls and showed signs of inflammation. This impairs how efficiently the heart contracts and pumps blood around the body.
Research Using a Mouse Model
The researchers from the University of Colorado, US, used a mouse model that replicates human maternal physiology and placental nutrient transport in obese women.Female mice (n = 31) were fed a diet with a high-fat content together with a sugary drink, which is equivalent to a human regularly consuming a burger, chips and a fizzy drink (1,500 kcal). The female mice consumed this diet until they had developed obesity, putting on about 25% of their original body weight and 50 female mice were fed a controlled diet.
Mouse pups (n = 187) were studied in utero, as well as after birth at 3, 6, 9 and 24 months using imaging techniques, including echocardiography and positron emission tomography (PET) scans. Researchers have analyzed genes, proteins and mitochondria of the offspring.
The changes in offspring cardiac metabolism strongly depended on sex. The expression of 841 genes were altered in the hearts of female fetuses and 764 genes were altered in male fetuses, but less than 10% of genes were commonly altered in both sexes.
Interestingly,
although both male and female offspring from mothers with obesity had impaired cardiac function, there were differences in the progression between sexes;
males were impaired from the start, whereas females' cardiac function got progressively worse with age.
The sex-difference in the lasting impairments of cardiovascular health and function could be due to estrogen. Higher levels in young females may protect cardiovascular health, the protection diminishes as estrogen levels deplete as the females age. The molecular cause for the sex difference is not yet understood.
Lead author, Dr. Owen Vaughan, University of Colorado, US said: "Our research indicates a mechanism linking maternal obesity with cardiometabolic illness in the next generation. This is important because
obesity is increasing rapidly in the human population and affects almost one-third of women of childbearing age.
By improving our understanding of the mechanisms involved, this research paves the way for treatments that could be used in early life to prevent later-life cardiometabolic illnesses, which are costly for health services and affect many people's quality of life. For example, we could offer more tailored advice on nutrition to mothers or children based on their body mass index or sex, or develop new drugs that target metabolism in the heart of the fetus."
Mice have shorter pregnancies, more offspring and different diets than humans so further studies on human volunteers would be required to extrapolate the findings to women's health. Loss-of-function studies also need to be carried out to prove this mechanism linking maternal obesity and offspring heart function and pinpoint the exact molecules responsible.
Source: Eurekalert