β-cell replication is the primary mechanism subserving the postnatal expansion of β-cell mass in humans

JJ Meier, AE Butler, Y Saisho, T Monchamp… - Diabetes, 2008 - Am Diabetes Assoc
JJ Meier, AE Butler, Y Saisho, T Monchamp, R Galasso, A Bhushan, RA Rizza, PC Butler
Diabetes, 2008Am Diabetes Assoc
OBJECTIVE—Little is known about the capacity, mechanisms, or timing of growth in β-cell
mass in humans. We sought to establish if the predominant expansion of β-cell mass in
humans occurs in early childhood and if, as in rodents, this coincides with relatively
abundant β-cell replication. We also sought to establish if there is a secondary growth in β-
cell mass coincident with the accelerated somatic growth in adolescence. RESEARCH
DESIGN AND METHODS—To address these questions, pancreas volume was determined …
OBJECTIVE— Little is known about the capacity, mechanisms, or timing of growth in β-cell mass in humans. We sought to establish if the predominant expansion of β-cell mass in humans occurs in early childhood and if, as in rodents, this coincides with relatively abundant β-cell replication. We also sought to establish if there is a secondary growth in β-cell mass coincident with the accelerated somatic growth in adolescence.
RESEARCH DESIGN AND METHODS— To address these questions, pancreas volume was determined from abdominal computer tomographies in 135 children aged 4 weeks to 20 years, and morphometric analyses were performed in human pancreatic tissue obtained at autopsy from 46 children aged 2 weeks to 21 years.
RESULTS— We report that 1) β-cell mass expands by severalfold from birth to adulthood, 2) islets grow in size rather than in number during this transition, 3) the relative rate of β-cell growth is highest in infancy and gradually declines thereafter to adulthood with no secondary accelerated growth phase during adolescence, 4) β-cell mass (and presumably growth) is highly variable between individuals, and 5) a high rate of β-cell replication is coincident with the major postnatal expansion of β-cell mass.
CONCLUSIONS— These data imply that regulation of β-cell replication during infancy plays a major role in β-cell mass in adult humans.
Am Diabetes Assoc