Genetic Modification of Dendritic Cells Through the Directed Differentiation of Embryonic Stem Cells
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Recent years have witnessed a progressive acceptance of the dual role played by dendritic cells (DC) in the initiation of
immune responses and their specific attenuation through the induction of immunological tolerance. Nevertheless, as terminally
differentiated cells of the myeloid lineage, DC share with macrophages an inherent resistance to genetic modification, greatly
restricting strategies available for studying their physiology and function. Consequently, little is known of the molecular
interactions provided by DC that underlie the critical decision between tolerance and immunity. Embryonic stem (ES) cells
are, by contrast, relatively amenable to genetic modification. Furthermore, their propensity for self-renewal, one of the
cardinal features of a stem cell, permits cloning at the single cell level and the rational design of ES cell lines, uniformly
expressing a desired, mutant phenotype. Here, we describe how another defining property of ES cells, their demonstrable pluripotency,
may be harnessed for their directed differentiation along the DC pathway, enabling the generation of limitless numbers of
DC faithfully expressing candidate genes of interest. The protocols we outline in this chapter may, therefore, offer new opportunities
for dissecting the biology of DC and the molecular basis of their unique properties.
Book Title: Immunological Tolerance: Methods and Protocols
Series: Methods in Molecular Biology | Volume: 380 | Pub. Date: Jun-08-2007 | Page Range: 59-72 | DOI: 10.1007/978-1-59745-395-0_4
Subject: Immunology
Key Words: Dendritic cell - embryonic stem cell - directed differentiation - tolerance - genetic modification
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