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Đã xuất bản: 2021-06-02
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DOI: https://doi.org/10.52724/tcnk.v13i6.28
Số xuất bản
Tập 13 Số 6 (2020):
Chuyên mục
Tổng quan

FETAL ORIGIN OF ADULT DISEASE

Nguyen Cong Khanh1
1 Hội Nhi khoa Việt Nam

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Tóm tắt

“Fetal origins of adult disease”, often called the “Barker hypothesis” after a large proportion
data of Barker and colleagues in Southampton over the last decade, that adverse influences
early in development, and particularly during intrauterine life, can result in permanent changes
in structure, physiology, metabolism, which result in increased disease risk in adulthood. Many
further studies have provided evidence for the hypothesis that size at birth is related to the
risk of developing disease in later life. In particular, links are well established between reduced
birthweight and increased risk of coronary heart disease, diabetes, hypertension and stroke
in adulthood. The most widely accepted mechanisms thought to underlie these relationship
are those of altered fetal nutrition, genetic–epigenetic links, fetal programming and fetal
excess glucocorticoid exposure. It is suggested that the fetus makes physiological adaption in
response to changes in its environment to prepare itself for posnatal life. The “Fetal origin of
adult disease” hypothesis is attractive. It suggests that these diseases could be prevented by
improving maternal health and fetal development

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Từ khóa

Development origin of adult disease, Chronic diseases, Heart disease, Hypertension, Diabetes, Programming.

Tài liệu tham khảo

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