Transcriptional Control of Dendritic Cell Development

Theresa L. Murphy, Gary E. Grajales-Reyes, Xiaodi Wu, Roxane Tussiwand, Carlos G. Briseño, Arifumi Iwata, Nicole M. Kretzer, Vivek Durai, Kenneth M. Murphy

Research output: Contribution to journalArticlepeer-review

240 Scopus citations

Abstract

The dendritic cells (DCs) of the immune system function in innate and adaptive responses by directing activity of various effector cells rather than serving as effectors themselves. DCs and closely related myeloid lineages share expression of many surface receptors, presenting a challenge in distinguishing their unique in vivo functions. Recent work has taken advantage of unique transcriptional programs to identify and manipulate murine DCs in vivo. This work has assigned several nonredundant in vivo functions to distinct DC lineages, consisting of plasmacytoid DCs and several subsets of classical DCs that promote different immune effector modules in response to pathogens. In parallel, a correspondence between human and murine DC subsets has emerged, underlying structural similarities for the DC lineages between these species. Recent work has begun to unravel the transcriptional circuitry that controls the development and diversification of DCs from common progenitors in the bone marrow.

Original languageEnglish
Pages (from-to)93-119
Number of pages27
JournalAnnual Review of Immunology
Volume34
DOIs
StatePublished - May 20 2016

Keywords

  • Common dendritic progenitor
  • Dendritic cell
  • Lineage commitment
  • Transcription factors

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