The A-myb gene is preferentially expressed in tonsillar CD38+, CD39-, and sIgM- B lymphocytes and in Burkitt's lymphoma cell lines.

Abstract

Abstract The A-myb gene is structurally related to the c-mby proto-oncogene, a transcription factor involved in the regulation of hemopoietic proliferation and differentiation. Recent evidence has shown that A-myb also functions as a transcriptional activator. We have previously demonstrated that A-myb RNA is not expressed in most mature human leukocytes at rest or after mitogenic or functional activation. We show here, by using cell sorting, PCR, and Western analyses that A-myb is most highly expressed in the subsets of human tonsillar B lymphocytes with the phenotypes CD38+, CD39-, and SIgM-. The preferential expression of A-myb in these populations was seen at both the RNA and protein levels. CD38 was consistently best at separating high from low A-myb-expressing cells, whereas other markers (CD10, 22, 23, 77, 11a, and 49d) did not correlate with A-myb expression. The CD38+ population expressing the highest levels of A-myb was shown to contain mostly cycling cells inasmuch as more than 95% were in the late G1, S, G2, and M phases of the cell cycle. In addition, A-myb expression always correlated with the percentage of cells in S/G2/M in the populations sorted with either CD38, CD39, or sIgM. Small resting tonsillar B lymphocytes induced to proliferate in vitro by several different polyclonal B cell activators did not, however, express detectable levels of A-myb, although these cells were demonstrated to express CD38 and enter the S/G2/M phases of the cell cycle. These data suggest that A-myb is a marker of in vivo-activated but not in vitro-activated B lymphocytes. Finally, A-myb was also found to be highly expressed in five of seven Burkitt's lymphoma lines and in none of three EBV lymphoblastoid cell lines. This finding is in agreement with the phenotype of the normal B cells that express high levels of A-myb in vivo and suggests that A-myb may be specifically induced within germinal center B cells.

Keywords

BiologyMYBMolecular biologyCD38Cell cycleCD19PopulationCellGene expressionCell biologyGeneFlow cytometryGeneticsStem cellMedicine

Affiliated Institutions

Mario Negri Institute for Pharmacological Research IT

Related Publications

Somatic hypermutation in normal and transformed human B cells

Ulf Klien , Tina Goasens , Motthias Fischer +4 more

Summary: In the human, most IgM + IgD + as well as CD5* peripheral blood B cells express unmutated V genes and thus can be assigned to a pre‐germinal centre (GC) stage of develo...

1998 Immunological Reviews 337 citations

A specific monoclonal antibody (PG-B6) detects expression of the BCL-6 protein in germinal center B cells.

Leonardo Flenghi , B. H. Ye , Marco Fizzotti +7 more

The BCL-6 gene is frequently involved in translocations occurring at the 3q27 locus and is rearranged in approximately 30% of diffuse large cell lymphomas and in a small fractio...

1995 PubMed 97 citations

Isolation of a candidate human hematopoietic stem-cell population.

C Baum , I L Weissman , Atsushi Tsukamoto +2 more

We have identified a rare (0.05-0.1%) subset of human fetal bone marrow cells that contains multipotent hematopoietic precursors. The population of human precursor cells that ex...

1992 Proceedings of the National Academy o... 1079 citations

Role of Members of the Wnt Gene Family in Human Hematopoiesis

David Van Den Berg , Arun Sharma , E Bruno +1 more

Abstract The hematopoietic system is derived from ventral mesoderm. A number of genes that are important in mesoderm development have been identified including members of the tr...

1998 Blood 330 citations

Human embryonic stem cell–derived CD34+ cells: efficient production in the coculture with OP9 stromal cells and analysis of lymphohematopoietic potential

Maxim A. Vodyanik , Jack A. Bork , James A. Thomson +1 more

Abstract Embryonic stem (ES) cells have the potential to serve as an alternative source of hematopoietic precursors for transplantation and for the study of hematopoietic cell d...

2004 Blood 599 citations

Publication Info

Year: 1994
Type: article
Volume: 153
Issue: 2
Pages: 543-553
Citations: 30
Access: Closed

External Links

View on DOI.org

Social Impact

Altmetric

The A-myb gene is preferentially expressed in tonsillar CD38+, CD39-, and sIgM- B lymphocytes and in Burkitt's lymphoma cell lines.

PlumX Metrics

Social media, news, blog, policy document mentions

Citation Metrics

OpenAlex

Cite This

APA Style

                            
                                
                                    Josée Golay, 
                                
                                    Eugenio Erba, 
                                
                                    Sergio Bernasconi
                                
                                et al.
                            
                            (1994). 
                            The A-myb gene is preferentially expressed in tonsillar CD38+, CD39-, and sIgM- B lymphocytes and in Burkitt's lymphoma cell lines.. 
                            The Journal of Immunology
                            , 153
                            (2)
                            , 543-553.
                            https://doi.org/10.4049/jimmunol.153.2.543
                        

Identifiers

DOI: 10.4049/jimmunol.153.2.543