The sequential determination model of hematopoiesis

Geoffrey Brown; Philip Hughes; Robert Michell; Antonius G. Rolink; Rhodri Ceredig

doi:10.1016/j.it.2007.07.007

The sequential determination model of hematopoiesis

Geoffrey Brown, Philip Hughes, Robert Michell, Antonius G. Rolink, Rhodri Ceredig

Research output: Contribution to journal › Review article › peer-review

24 Citations (Scopus)

Abstract

Analysis of hematopoietic development has for decades been central to understanding lineage diversification. Some models consider hematopoietic commitment to be random, and branching lineage maps often include an early myeloid or lymphoid bifurcation. However, the existence of joint lymphoid or myeloid intermediate progenitors argues against both. One of us earlier proposed the sequential determination (SD) model, which features a limited and stepwise set of binary choices across the full hematopoietic spectrum. This model arose from observations that hematopoietic progenitors show preferences for particular associations of lineage potentials--indicating that these linked fates are neighbours developmentally. An updated SD model complemented by several recently recognized processes--spatiotemporal fluctuations in transcription factor concentrations, asymmetric cell division, and Notch signalling--still offers a sound summary of hematopoiesis.

Original language	English
Pages (from-to)	442-448
Number of pages	7
Journal	Trends in Immunology
Volume	28
Issue number	10
Early online date	7 Sept 2007
DOIs	https://doi.org/10.1016/j.it.2007.07.007
Publication status	Published - 1 Oct 2007

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title = "The sequential determination model of hematopoiesis",

abstract = "Analysis of hematopoietic development has for decades been central to understanding lineage diversification. Some models consider hematopoietic commitment to be random, and branching lineage maps often include an early myeloid or lymphoid bifurcation. However, the existence of joint lymphoid or myeloid intermediate progenitors argues against both. One of us earlier proposed the sequential determination (SD) model, which features a limited and stepwise set of binary choices across the full hematopoietic spectrum. This model arose from observations that hematopoietic progenitors show preferences for particular associations of lineage potentials--indicating that these linked fates are neighbours developmentally. An updated SD model complemented by several recently recognized processes--spatiotemporal fluctuations in transcription factor concentrations, asymmetric cell division, and Notch signalling--still offers a sound summary of hematopoiesis.",

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T1 - The sequential determination model of hematopoiesis

AU - Brown, Geoffrey

AU - Hughes, Philip

AU - Michell, Robert

AU - Rolink, Antonius G.

AU - Ceredig, Rhodri

PY - 2007/10/1

Y1 - 2007/10/1

N2 - Analysis of hematopoietic development has for decades been central to understanding lineage diversification. Some models consider hematopoietic commitment to be random, and branching lineage maps often include an early myeloid or lymphoid bifurcation. However, the existence of joint lymphoid or myeloid intermediate progenitors argues against both. One of us earlier proposed the sequential determination (SD) model, which features a limited and stepwise set of binary choices across the full hematopoietic spectrum. This model arose from observations that hematopoietic progenitors show preferences for particular associations of lineage potentials--indicating that these linked fates are neighbours developmentally. An updated SD model complemented by several recently recognized processes--spatiotemporal fluctuations in transcription factor concentrations, asymmetric cell division, and Notch signalling--still offers a sound summary of hematopoiesis.

AB - Analysis of hematopoietic development has for decades been central to understanding lineage diversification. Some models consider hematopoietic commitment to be random, and branching lineage maps often include an early myeloid or lymphoid bifurcation. However, the existence of joint lymphoid or myeloid intermediate progenitors argues against both. One of us earlier proposed the sequential determination (SD) model, which features a limited and stepwise set of binary choices across the full hematopoietic spectrum. This model arose from observations that hematopoietic progenitors show preferences for particular associations of lineage potentials--indicating that these linked fates are neighbours developmentally. An updated SD model complemented by several recently recognized processes--spatiotemporal fluctuations in transcription factor concentrations, asymmetric cell division, and Notch signalling--still offers a sound summary of hematopoiesis.

U2 - 10.1016/j.it.2007.07.007

DO - 10.1016/j.it.2007.07.007

M3 - Review article

C2 - 17825625

SN - 1471-4981

VL - 28

SP - 442

EP - 448

JO - Trends in Immunology

JF - Trends in Immunology

IS - 10

ER -

The sequential determination model of hematopoiesis

Abstract

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