Abstract
Follicular dendritic cells (FDCs) have been shown to play a crucial role in the positive selection of high-affinity B cells that are generated by somatic hypermutation in germinal center (GC). Because of technical difficulties in preparing and maintaining pure FDCs, a role for FDCs in this complicated process has not been fully elucidated. In this study, we established a cell line designated as pFL that retained major FDC phenotypes from a three-dimensional culture of mouse lymph node cells. pFL cells proliferated slowly in response to an agonistic anti-lymphotoxin beta receptor mAb and TNF-alpha. A more rapidly growing clone, named FL-Y, with similar requirements for growth was isolated from a long-term culture of pFL. Analysis of surface markers in these two cell lines by immunostaining, flow cytometry, and DNA microarray revealed the expression of genes, including those of CD21, FcgammaRIIB, lymphotoxin beta receptor, ICAM-1, VCAM-1, IL-6, and C4, which have been shown to be characteristic of FDCs. In addition, B cell-activating factor was expressed in these two cell lines. At the pFL or FL-Y:B cell ratio of 1:100, the cell lines markedly sustained B cell survival and Ab production during 2 wk of culture, while most B cells collapsed within 1 wk in the absence of the FDC-like cells. Interestingly, expression of typical GC markers, Fas and GL-7, was notably augmented in B cells that were cocultured with Th cells on these two cell lines. Thus, pFL and FL-Y cells may be useful for providing insight into the functional role for FDCs in GC.
Highlights
Normal development of Follicular dendritic cells (FDCs) has been shown to be essential for the establishment of proper segregation of T/B cell areas in secondary lymphoid organs and the formation of germinal center (GC) within the B cell follicle (8 –23)
Accumulating evidence suggests a pivotal role of FDCs in B cell differentiation and selection in GCs, molecular mechanisms underlying these complicated processes have not been fully elucidated
Primary FDCs prepared from lymphoid organs in irradiated mice have been used in many in vitro experiments reported to date
Summary
GC, germinal center; FDC, follicular dendritic cell; BAFF, B cell-activating factor; BMDC, bone marrow-derived DC; CGG, chicken ␥-globulin; Con A-sup, Con A-stimulated rat spleen cell culture; HS, horse serum; IC, immune complex; KLH, keyhole limpet hemocyanin; LN, lymph node; LT, lymphotoxin; NIP, 4-hydroxy-3-iodo-5-nitrophenylacetyl; NP, 4-hydroxy-3-nitrophenylacetyl; TNP, 2,4,6-trinitrophenyl. FDC-like human cell lines, including HK, have been established to overcome these problems (30 –33) These cell lines have been shown to retain a variety of FDC functions, some respects of them, including expression of surface markers, were different from those of primary FDCs. In previous in vitro experiments using primary FDCs that were isolated from murine lymphoid tissues, high FDC:B cell ratios, such as 1:3, have been used to observe augmenting effects of FDCs on the differentiation of B cells [25,26,27, 34]. We characterized pFL and FL-Y cells, focusing on their ability to support survival and differentiation of B cells in vitro
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