ABSTRACT
Memory B cells (MBCs) are essential for long-lived humoral immunity. However, the transcription factors (TFs) involved in MBC differentiation are poorly defined. Here, by single cell RNAseq analysis, we identified a population of germinal center (GC) B cells in the process of differentiating into MBCs. Using an inducible Crispr/Cas9 screening approach we identified the hematopoietically-expressed homeobox gene Hhex as a transcription factor regulating MBC differentiation. The co-repressor Tle3 was also identified in the screen and was found to interact with Hhex. Bcl6 directly repressed Hhex in GC B cells. Reciprocally, Hhex-deficient MBCs exhibited derepressed Bcl6 and reduced expression of Bcl6-repressed Bcl2. Overexpression of Bcl2 was able to rescue MBC differentiation in Hhex-deficient cells. We also identified Ski as an Hhex-induced transcription factor involved in MBC differentiation. These findings establish an important role for Hhex-Tle3 in regulating the transcriptional circuitry governing MBC differentiation.
Abbreviations
- GC
- germinal center
- MBC
- memory B cell
- TFH
- T follicular helper cell
- DEGs
- differentially expressed genes
- TF
- transcription factor
- scRNAseq
- single cell RNA sequencing
- FO
- follicular
- DZ
- dark zone
- LZ
- light zone
- FO
- follicular
- Sg
- single guide
- ChIP
- chromatin immunoprecipitation
- GST
- glutathione S-transferase
- HDAC
- histone deacetylase
- LCMV
- lymphocytic choriomeningitis virus
- MAPK
- mitogen activated protein kinase