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Journal of Experimental Medicine, Vol 169, 1213-1231, Copyright © 1989 by Rockefeller University Press
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DJ Diamond, FB Nelson and EL Reinherz
Laboratory of Immunobiology, Dana-Farber Cancer Institute, Boston, Massachusetts.
We have characterized the sequence contribution of DNA 5' of a functionally rearranged TCR promoter (V beta 8.1) on its T lineage- specific expression through the use of the chloramphenicol acetyl- transferase (CAT) reporter gene. A 230-bp fragment located 570 bp upstream of the determined transcription start site of the V beta 8.1 promoter confers a T lineage specificity of expression to a heterologous promoter. The inability of the V beta 8.1 promoter and its associated elements to function in B cells suggests the existence of a mechanism to prevent inappropriate V beta gene expression in B cells. Of considerable interest is the fact that both a B cell-specific and a nontissue-specific enhancer element were incapable of stimulating significant expression of this promoter in B cells. We discuss the implication of these results on the process of rearrangement of both Ig and TCR genes, and the differentiation of the lymphoid system.
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