β-cell development and turnover during prenatal life in humans

β-cell development and turnover during prenatal life in humans

Introductionβ-cell regeneration is an area under active investigation for the future treatment of diabetes, but little is known about the patterns and dynamics of prenatal β-cell development in humans. In particular, the quantitative changes in β-cell mass in the developing pancreas have not been el...

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Published in:European journal of endocrinology Vol. 162; no. 3; pp. 559 - 568
Main Authors: Meier, Juris J, Köhler, Christina U, Alkhatib, Bacel, Sergi, Consolato, Junker, Theresa, Klein, Harald H, Schmidt, Wolfgang E, Fritsch, Helga
Format: Journal Article
Language:English
Published: Bristol BioScientifica 01-03-2010
European Society of Endocrinology
Subjects:
Apoptosis - physiology
Biological and medical sciences
Cell Differentiation - physiology
Cell Division - physiology
Cell Proliferation
Clinical Study
Endocrinopathies
Female
Fundamental and applied biological sciences. Psychology
Glucagon - metabolism
Humans
Immunohistochemistry
Insulin - metabolism
Insulin-Secreting Cells - cytology
Insulin-Secreting Cells - metabolism
Islets of Langerhans - embryology
Islets of Langerhans - metabolism
Male
Medical sciences
Microscopy, Fluorescence
Pancreas - embryology
Pancreas - metabolism
Vertebrates: endocrinology
Human
Cell proliferation
Prenatal
Langerhans islet
Turnover
β Cell
Endocrinology
Endocrine pancreas
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Summary:Introductionβ-cell regeneration is an area under active investigation for the future treatment of diabetes, but little is known about the patterns and dynamics of prenatal β-cell development in humans. In particular, the quantitative changes in β-cell mass in the developing pancreas have not been elucidated in detail. We addressed the following questions in prenatal humans: i) what is the timing of β-cell occurrence and islet growth? ii) What are the dynamics of β-cell replication and apoptosis?MethodsPancreatic tissue was obtained from 65 human embryos and foetuses aged between 8 weeks post conception (p.c.) and birth. Sections were stained for insulin, glucagon, Ki67 (proliferation marker), TUNEL (apoptosis marker) and CD31 (blood vessel marker), and morphometric analyses were performed.Resultsβ-cells were detected from gestational week 9 onward, whereas glucagon expression was detected already at week 8. The fractional β-cell area of the pancreas increased in a linear fashion until birth (r=0.60, P<0.001). The first endocrine cells were found within or adjacent to the primitive ductal epithelium. β-cell replication was readily detected in the newly forming islets already starting at week 9 p.c. (average frequency 2.8±0.4%). A small percentage of cells co-expressed insulin and glucagon during the early foetal period. There was a close relationship between the development of endocrine islets and blood vessels during all stages of prenatal pancreas development suggesting a possible interaction between both cell types. The frequency of β-cell apoptosis was relatively high throughout all ages (1.5±0.3%).Conclusionsβ-cell differentiation in humans occurs from week 9 p.c. onward. The first endocrine cells are closely associated with the ductal epithelium suggesting differentiation from precursor cells. High rates of β-cell replication suggest that this mechanism plays an important role in the prenatal expansion of β-cell mass.
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ISSN:0804-4643
1479-683X
DOI:10.1530/EJE-09-1053