Patel, AA;
Zhang, Y;
Fullerton, JN;
Boelen, L;
Rongvaux, A;
Maini, AA;
Bigley, V;
Flavell, RA;
Gilroy, DW;
Asquith, B;
et al.
Patel, AA; Zhang, Y; Fullerton, JN; Boelen, L; Rongvaux, A; Maini, AA; Bigley, V; Flavell, RA; Gilroy, DW; Asquith, B; Macallan, D; Yona, S
(2017)
The fate and lifespan of human monocyte subsets in steady state and systemic inflammation.
J Exp Med, 214 (7).
pp. 1913-1923.
ISSN 1540-9538
https://doi.org/10.1084/jem.20170355
SGUL Authors: Macallan, Derek Clive
Abstract
In humans, the monocyte pool comprises three subsets (classical, intermediate, and nonclassical) that circulate in dynamic equilibrium. The kinetics underlying their generation, differentiation, and disappearance are critical to understanding both steady-state homeostasis and inflammatory responses. Here, using human in vivo deuterium labeling, we demonstrate that classical monocytes emerge first from marrow, after a postmitotic interval of 1.6 d, and circulate for a day. Subsequent labeling of intermediate and nonclassical monocytes is consistent with a model of sequential transition. Intermediate and nonclassical monocytes have longer circulating lifespans (∼4 and ∼7 d, respectively). In a human experimental endotoxemia model, a transient but profound monocytopenia was observed; restoration of circulating monocytes was achieved by the early release of classical monocytes from bone marrow. The sequence of repopulation recapitulated the order of maturation in healthy homeostasis. This developmental relationship between monocyte subsets was verified by fate mapping grafted human classical monocytes into humanized mice, which were able to differentiate sequentially into intermediate and nonclassical cells.
Statistics
Item downloaded times since 11 Jul 2017.
Actions (login required)
|
Edit Item |