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rho gtpase expression in human myeloid cellsρgtpase人类髓细胞表达
Rho GTPase Expression in Human Myeloid Cells
1,2 1,2 3 1,2
Suzanne F. G. van Helden *, Eloise C. Anthony , Rob Dee , Peter L. Hordijk
1 Department of Molecular Cell Biology, Sanquin Research, Amsterdam, The Netherlands, 2 Landsteiner Laboratory, Academic Medical Centre, University of Amsterdam,
Amsterdam, The Netherlands, 3 Department of Immunocytology, Sanquin Diagnostics, Amsterdam, The Netherlands
Abstract
Myeloid cells are critical for innate immunity and the initiation of adaptive immunity. Strict regulation of the adhesive and
migratory behavior is essential for proper functioning of these cells. Rho GTPases are important regulators of adhesion and
migration; however, it is unknown which Rho GTPases are expressed in different myeloid cells. Here, we use a qPCR-based
approach to investigate Rho GTPase expression in myeloid cells. We found that the mRNAs encoding Cdc42, RhoQ, Rac1,
Rac2, RhoA and RhoC are the most abundant. In addition, RhoG, RhoB, RhoF and RhoV are expressed at low levels or only in
specific cell types. More differentiated cells along the monocyte-lineage display lower levels of Cdc42 and RhoV, while RhoC
mRNA is more abundant. In addition, the Rho GTPase expression profile changes during dendritic cell maturation with Rac1
being upregulated and Rac2 downregulated. Finally, GM-CSF stimulation, during macrophage and osteoclast differentiation,
leads to high expression of Rac2, while M-CSF induces high levels of RhoA, showing that these cytokines induce a distinct
pattern. Our data uncover cell type specific modulation of the Rho GTPase expression profile in hematopoietic stem cells
and in more differentiated cells of the myeloid lineage.
Citation: van Helden SFG, Anthony EC, Dee R, Hordijk PL
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