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pubmed-article:7600290pubmed:abstractTextRecent experiments involving disruption of the Oct-2 gene have shown that this largely B cell-restricted transcription factor is not required in the early stages of B cell development. However, B cells that lack Oct-2 may be blocked from differentiation past the surface immunoglobulin-positive stage. To identify a possible function for Oct-2 in the late stage immunoglobulin-secreting cell, we have used the method of somatic cell fusion. When the immunoglobulin-producing myeloma MPC11 is fused to a T lymphoma, Oct-2 production ceases, as does the expression of immunoglobulin, J chain, and several other B cell-specific gene products. In the present study, we show that by preventing the loss of Oct-2 in the hybrid cells, we can preserve expression of all other tested B cell-specific genes. These results establish a central role for Oct-2 in maintaining the genetic program of the immunoglobulin-secreting plasmacyte.lld:pubmed
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pubmed-article:7600290pubmed:articleTitleConstitutively expressed Oct-2 prevents immunoglobulin gene silencing in myeloma x T cell hybrids.lld:pubmed
pubmed-article:7600290pubmed:affiliationDepartment of Biological Sciences, Hunter College, City University of New York, New York 10021, USA.lld:pubmed
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