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Regulated activity of the IgH intron enhancer (E{micro}) in the T lymphocyte lineage
Authors:Cook  Graham P; Meyer  Kerstin B; Neuberger  Michael S; Pettersson  Sven
Institution:Laboratory of Molecular Biology, Medical Research Council Cambridge CB2 2QH, UK
1 Wellcome/CRC Institute of Cancer and Developmental Biology, and Department of Pathology, University of Cambridge Cambridge CB2 1QR, UK
2Present address Centre for Protein Engineering, Medical Research Centre Cambridge CB2 2QH, UK
3Present address: Center for Biotechnology, Karolinska Institute 14157 Huddinge, Sweden
Abstract:The activity of the IgH (Eµ) enhancer in the T lymphocytelineage has been investigated using both transgenic mice andtransfection studies. Thymocyte fractionation experiments indicatethat a transgene consisting of the bacterial chloramphenicolacetyl transferase (CAT) gene, linked to Eµ and the SV40early promoter (Eµ–CAT), is expressed only in thymocyteswith a mature medullary phenotype and not in immature cells.Transfection of this same construct into two thymoma cell linesrepresenting different stages of thymocyte development mimicsthe pattern of activity observed in vivo. Further transfectionexperiments suggest that this pattern of expression might beattributed to the differential activity of the E2E3 and octanucleotidemotifs of Eµ during development. In contrast, an Ig {lambda} transgene(linked to Eµ and an Ig V{lambda} promoter) is expressed in themajority of thymocytes. We envisage that the different patternsof expression of the two transgenes reflect interactions betweentheir respective promoters and the factors which are bound toEµ at different stages of thymocyte development. Althoughdiffering in their pattern of expression within the thymus,the two transgenes share the property of extinction in peripheralT lymphocytes. These results indicate that the expression ofEµ-linked transgenes in the thymus cannot simply be explainedby activation of the enhancer in a lymphoid progenitor cellprior to B/T lineage divergence. Rather, the enhancer (or componentsof it) must be independently activated (and inactivated) duringT lymphocyte development. Furthermore, this activity is consistentwith the developmental timing of Ig DH–JH rearrangementsin these cells.
Keywords:Ig enhancer  Ig gene  lymphocyte  thymus
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