Genomics based analysis of interactions between developing B-lymphocytes and stromal cells reveal complex interactions and two-way communication

Zetterblad, Jenny; Qian, Hong; Zandi, Sasan; Månsson, Robert; Lagergren, Anna; Hansson, Frida; Bryder, David; Paulsson, Nils; Sigvardsson, Mikael

Genomics based analysis of interactions between developing B-lymphocytes and stromal cells reveal complex interactions and two-way communication

Mark

Zetterblad, Jenny ; Qian, Hong ; Zandi, Sasan ; Månsson, Robert ^LU ; Lagergren, Anna ^LU ; Hansson, Frida ; Bryder, David ^LU ; Paulsson, Nils and Sigvardsson, Mikael ^LU (2010) In BMC Genomics 11.

Abstract: Background: The use of functional genomics has largely increased our understanding of cell biology and promises to help the development of systems biology needed to understand the complex order of events that regulates cellular differentiation in vivo. One model system clearly dependent on the integration of extra and intra cellular signals is the development of B-lymphocytes from hematopoietic stem cells in the bone marrow. This developmental pathway involves several defined differentiation stages associated with specific expression of genes including surface markers that can be used for the prospective isolation of the progenitor cells directly from the bone marrow to allow for ex vivo gene expression analysis. The developmental process... (More); Background: The use of functional genomics has largely increased our understanding of cell biology and promises to help the development of systems biology needed to understand the complex order of events that regulates cellular differentiation in vivo. One model system clearly dependent on the integration of extra and intra cellular signals is the development of B-lymphocytes from hematopoietic stem cells in the bone marrow. This developmental pathway involves several defined differentiation stages associated with specific expression of genes including surface markers that can be used for the prospective isolation of the progenitor cells directly from the bone marrow to allow for ex vivo gene expression analysis. The developmental process can be simulated in vitro making it possible to dissect information about cell/cell communication as well as to address the relevance of communication pathways in a rather direct manner. Thus we believe that B-lymphocyte development represents a useful model system to take the first steps towards systems biology investigations in the bone marrow. Results: In order to identify extra cellular signals that promote B lymphocyte development we created a database with approximately 400 receptor ligand pairs and software matching gene expression data from two cell populations to obtain information about possible communication pathways. Using this database and gene expression data from NIH3T3 cells (unable to support B cell development), OP-9 cells (strongly supportive of B cell development), pro-B and pre-B cells as well as mature peripheral B-lineage cells, we were able to identify a set of potential stage and stromal cell restricted communication pathways. Functional analysis of some of these potential ways of communication allowed us to identify BMP-4 as a potent stimulator of B-cell development in vitro. Further, the analysis suggested that there existed possibilities for progenitor B cells to send signals to the stroma. The functional consequences of this were investigated by co-culture experiments revealing that the co-incubation of stromal cells with B cell progenitors altered both the morphology and the gene expression pattern in the stromal cells. Conclusions: We believe that this gene expression data analysis method allows for the identification of functionally relevant interactions and therefore could be applied to other data sets to unravel novel communication pathways. (Less)

Please use this url to cite or link to this publication: https://lup.lub.lu.se/record/1589768

author

Zetterblad, Jenny ; Qian, Hong ; Zandi, Sasan ; Månsson, Robert ^LU ; Lagergren, Anna ^LU ; Hansson, Frida ; Bryder, David ^LU ; Paulsson, Nils and Sigvardsson, Mikael ^LU

organization

publishing date

2010

type

Contribution to journal

publication status

published

subject

Genetics

in

BMC Genomics

volume

11

article number

108

publisher

BioMed Central (BMC)

external identifiers

wos:000275293200001
scopus:77649123428

ISSN

1471-2164

DOI

10.1186/1471-2164-11-108

language

English

LU publication?

yes

id

7ed52b88-f534-4e98-84cb-0c1fa0e016ec (old id 1589768)

date added to LUP

2016-04-01 12:58:53

date last changed

2022-01-27 08:40:25

@article{7ed52b88-f534-4e98-84cb-0c1fa0e016ec,
  abstract     = {{Background: The use of functional genomics has largely increased our understanding of cell biology and promises to help the development of systems biology needed to understand the complex order of events that regulates cellular differentiation in vivo. One model system clearly dependent on the integration of extra and intra cellular signals is the development of B-lymphocytes from hematopoietic stem cells in the bone marrow. This developmental pathway involves several defined differentiation stages associated with specific expression of genes including surface markers that can be used for the prospective isolation of the progenitor cells directly from the bone marrow to allow for ex vivo gene expression analysis. The developmental process can be simulated in vitro making it possible to dissect information about cell/cell communication as well as to address the relevance of communication pathways in a rather direct manner. Thus we believe that B-lymphocyte development represents a useful model system to take the first steps towards systems biology investigations in the bone marrow. Results: In order to identify extra cellular signals that promote B lymphocyte development we created a database with approximately 400 receptor ligand pairs and software matching gene expression data from two cell populations to obtain information about possible communication pathways. Using this database and gene expression data from NIH3T3 cells (unable to support B cell development), OP-9 cells (strongly supportive of B cell development), pro-B and pre-B cells as well as mature peripheral B-lineage cells, we were able to identify a set of potential stage and stromal cell restricted communication pathways. Functional analysis of some of these potential ways of communication allowed us to identify BMP-4 as a potent stimulator of B-cell development in vitro. Further, the analysis suggested that there existed possibilities for progenitor B cells to send signals to the stroma. The functional consequences of this were investigated by co-culture experiments revealing that the co-incubation of stromal cells with B cell progenitors altered both the morphology and the gene expression pattern in the stromal cells. Conclusions: We believe that this gene expression data analysis method allows for the identification of functionally relevant interactions and therefore could be applied to other data sets to unravel novel communication pathways.}},
  author       = {{Zetterblad, Jenny and Qian, Hong and Zandi, Sasan and Månsson, Robert and Lagergren, Anna and Hansson, Frida and Bryder, David and Paulsson, Nils and Sigvardsson, Mikael}},
  issn         = {{1471-2164}},
  language     = {{eng}},
  publisher    = {{BioMed Central (BMC)}},
  series       = {{BMC Genomics}},
  title        = {{Genomics based analysis of interactions between developing B-lymphocytes and stromal cells reveal complex interactions and two-way communication}},
  url          = {{http://dx.doi.org/10.1186/1471-2164-11-108}},
  doi          = {{10.1186/1471-2164-11-108}},
  volume       = {{11}},
  year         = {{2010}},
}

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Genomics based analysis of interactions between developing B-lymphocytes and stromal cells reveal complex interactions and two-way communication