Use of Stem Cell Radiation Chimeras to Analyze How Domains of Specific Proteins Impact on Murine NK Cell Development In Vivo英文文献.pdfVIP
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Chapter 5
Use of Stem Cell Radiation Chimeras to Analyze How
Domains of Specific Proteins Impact on Murine NK Cell
Development In Vivo
Rebecca H. Lian and Vinay Kumar
Abstract
Although the use of mutant mice has been extremely useful in identifying those proteins and molecules
specifically required for the development of NK cells, the establishment of a well-defined protocol to
replicate in vitro the major steps corresponding to the process of NK cell differentiation and maturation
has enabled us to dissect the molecular events governing certain aspects of NK cell development. This
chapter describes a protocol that combines both the use of mutant mice and the in vitro bone marrow
(BM) culture system for examining the role of proteins and their putative signaling domains in NK cell
development. BM-derived Lin–c-kit+ stem cells expressing the protein of interest are first cultured for
6 days in a cocktail of cytokines that promote lymphoid development. The semi-differentiated cells are
then transplanted into mice to complete their development in vivo. While all hematopoietic lineages can
develop from these transplanted cells, we focus primarily on assessing the effect of the protein on the
production of NK cells, as well as the acquisition of Ly49 receptors. The most prevalent advantage of this
method is the ability to potentially link signaling regulators to known aspects of NK cell development.
Key Words: Stem cell chimeras, natural killer cells, Ly49, IL-15R.
1. Introduction
The biological importance of certain protein receptors or sig-
naling molecules is most often revealed through studies using
mutant mice (1). Likewise, in the process of identifying the neces-
sary components needed for natural kil
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