AI Article Synopsis

  • Previous studies highlighted GATA1's importance for mast cell differentiation, but the total loss of GATA1 in mast cells hadn't been studied until now.
  • The new research using Gata1 knockout mice showed that deleting GATA1 had little effect on the number and distribution of mast cells, though it did reduce tryptase expression.
  • In contrast, GATA2 was found to be more critical than GATA1 for regulating mast cell genes and maintaining specific mast cell populations.

Article Abstract

Although previous studies have shown that GATA1 is required for mast cell differentiation, the effects of the complete ablation of GATA1 in mast cells have not been examined. Using conditional Gata1 knockout mice (Gata1(-/y)), we demonstrate here that the complete ablation of GATA1 has a minimal effect on the number and distribution of peripheral tissue mast cells in adult mice. The Gata1(-/y) bone marrow cells were capable of differentiating into mast cells ex vivo. Microarray analyses showed that the repression of GATA1 in bone marrow mast cells (BMMCs) has a small impact on the mast cell-specific gene expression in most cases. Interestingly, however, the expression levels of mast cell tryptases in the mouse chromosome 17A3.3 were uniformly reduced in the GATA1 knockdown cells, and GATA1 was found to bind to a 500-bp region at the 5' end of this locus. Revealing a sharp contrast to that observed in the Gata1-null BMMCs, GATA2 deficiency resulted in a significant loss of the c-Kit(+) FcεRIα(+) mast cell fraction and a reduced expression of several mast cell-specific genes. Collectively, GATA2 plays a more important role than GATA1 in the regulation of most mast cell-specific genes, while GATA1 might play specific roles in mast cell functions.

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http://www.ncbi.nlm.nih.gov/pmc/articles/PMC4019035PMC
http://dx.doi.org/10.1128/MCB.01524-13DOI Listing

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