Complementary signaling through flt3 and interleukin-7 receptor alpha is indispensable for fetal and adult B cell genesis.

Ewa Sitnicka; Cord Brakebusch; Inga-Lill Martensson; Marcus Svensson; William W Agace; Mikael Sigvardsson; Natalija Buza-Vidas; David Bryder; Corrado M Cilio; Henrik Ahlenius; Eugene Maraskovsky; Jacques J Peschon; Sten Eirik W Jacobsen

doi:10.1084/jem.20031152

Complementary signaling through flt3 and interleukin-7 receptor alpha is indispensable for fetal and adult B cell genesis.

Ewa Sitnicka, Cord Brakebusch, Inga-Lill Martensson, Marcus Svensson, William W Agace, Mikael Sigvardsson, Natalija Buza-Vidas, David Bryder, Corrado M Cilio, Henrik Ahlenius, Eugene Maraskovsky, Jacques J Peschon, Sten Eirik W Jacobsen

Nutritional Immunology

Research output: Contribution to journal › Journal article › Research › peer-review

137 Citations (Scopus)

Abstract

Extensive studies of mice deficient in one or several cytokine receptors have failed to support an indispensable role of cytokines in development of multiple blood cell lineages. Whereas B1 B cells and Igs are sustained at normal levels throughout life of mice deficient in IL-7, IL-7Ralpha, common cytokine receptor gamma chain, or flt3 ligand (FL), we report here that adult mice double deficient in IL-7Ralpha and FL completely lack visible LNs, conventional IgM+ B cells, IgA+ plasma cells, and B1 cells, and consequently produce no Igs. All stages of committed B cell progenitors are undetectable in FL-/- x IL-7Ralpha-/- BM that also lacks expression of the B cell commitment factor Pax5 and its direct target genes. Furthermore, in contrast to IL-7Ralpha-/- mice, FL-/- x IL-7Ralpha-/- mice also lack mature B cells and detectable committed B cell progenitors during fetal development. Thus, signaling through the cytokine tyrosine kinase receptor flt3 and IL-7Ralpha are indispensable for fetal and adult B cell development.

Original language	English
Journal	Journal of Experimental Medicine
Volume	198
Issue number	10
Pages (from-to)	1495-506
Number of pages	11
ISSN	0022-1007
DOIs	https://doi.org/10.1084/jem.20031152
Publication status	Published - 2003

Bibliographical note

Keywords: Animals; B-Lymphocytes; Cell Differentiation; Membrane Proteins; Mice; Mice, Knockout; Peyer's Patches; Receptors, Interleukin-7; Signal Transduction

Access to Document

10.1084/jem.20031152

Cite this

Sitnicka, E., Brakebusch, C., Martensson, I.-L., Svensson, M., Agace, W. W., Sigvardsson, M., Buza-Vidas, N., Bryder, D., Cilio, C. M., Ahlenius, H., Maraskovsky, E., Peschon, J. J., & Jacobsen, S. E. W. (2003). Complementary signaling through flt3 and interleukin-7 receptor alpha is indispensable for fetal and adult B cell genesis. Journal of Experimental Medicine, 198(10), 1495-506. https://doi.org/10.1084/jem.20031152

Sitnicka, E, Brakebusch, C, Martensson, I-L, Svensson, M, Agace, WW, Sigvardsson, M, Buza-Vidas, N, Bryder, D, Cilio, CM, Ahlenius, H, Maraskovsky, E, Peschon, JJ & Jacobsen, SEW 2003, 'Complementary signaling through flt3 and interleukin-7 receptor alpha is indispensable for fetal and adult B cell genesis.', Journal of Experimental Medicine, vol. 198, no. 10, pp. 1495-506. https://doi.org/10.1084/jem.20031152

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title = "Complementary signaling through flt3 and interleukin-7 receptor alpha is indispensable for fetal and adult B cell genesis.",

abstract = "Extensive studies of mice deficient in one or several cytokine receptors have failed to support an indispensable role of cytokines in development of multiple blood cell lineages. Whereas B1 B cells and Igs are sustained at normal levels throughout life of mice deficient in IL-7, IL-7Ralpha, common cytokine receptor gamma chain, or flt3 ligand (FL), we report here that adult mice double deficient in IL-7Ralpha and FL completely lack visible LNs, conventional IgM+ B cells, IgA+ plasma cells, and B1 cells, and consequently produce no Igs. All stages of committed B cell progenitors are undetectable in FL-/- x IL-7Ralpha-/- BM that also lacks expression of the B cell commitment factor Pax5 and its direct target genes. Furthermore, in contrast to IL-7Ralpha-/- mice, FL-/- x IL-7Ralpha-/- mice also lack mature B cells and detectable committed B cell progenitors during fetal development. Thus, signaling through the cytokine tyrosine kinase receptor flt3 and IL-7Ralpha are indispensable for fetal and adult B cell development.",

author = "Ewa Sitnicka and Cord Brakebusch and Inga-Lill Martensson and Marcus Svensson and Agace, {William W} and Mikael Sigvardsson and Natalija Buza-Vidas and David Bryder and Cilio, {Corrado M} and Henrik Ahlenius and Eugene Maraskovsky and Peschon, {Jacques J} and Jacobsen, {Sten Eirik W}",

note = "Keywords: Animals; B-Lymphocytes; Cell Differentiation; Membrane Proteins; Mice; Mice, Knockout; Peyer's Patches; Receptors, Interleukin-7; Signal Transduction",

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T1 - Complementary signaling through flt3 and interleukin-7 receptor alpha is indispensable for fetal and adult B cell genesis.

AU - Sitnicka, Ewa

AU - Brakebusch, Cord

AU - Martensson, Inga-Lill

AU - Svensson, Marcus

AU - Agace, William W

AU - Sigvardsson, Mikael

AU - Buza-Vidas, Natalija

AU - Bryder, David

AU - Cilio, Corrado M

AU - Ahlenius, Henrik

AU - Maraskovsky, Eugene

AU - Peschon, Jacques J

AU - Jacobsen, Sten Eirik W

N1 - Keywords: Animals; B-Lymphocytes; Cell Differentiation; Membrane Proteins; Mice; Mice, Knockout; Peyer's Patches; Receptors, Interleukin-7; Signal Transduction

PY - 2003

Y1 - 2003

N2 - Extensive studies of mice deficient in one or several cytokine receptors have failed to support an indispensable role of cytokines in development of multiple blood cell lineages. Whereas B1 B cells and Igs are sustained at normal levels throughout life of mice deficient in IL-7, IL-7Ralpha, common cytokine receptor gamma chain, or flt3 ligand (FL), we report here that adult mice double deficient in IL-7Ralpha and FL completely lack visible LNs, conventional IgM+ B cells, IgA+ plasma cells, and B1 cells, and consequently produce no Igs. All stages of committed B cell progenitors are undetectable in FL-/- x IL-7Ralpha-/- BM that also lacks expression of the B cell commitment factor Pax5 and its direct target genes. Furthermore, in contrast to IL-7Ralpha-/- mice, FL-/- x IL-7Ralpha-/- mice also lack mature B cells and detectable committed B cell progenitors during fetal development. Thus, signaling through the cytokine tyrosine kinase receptor flt3 and IL-7Ralpha are indispensable for fetal and adult B cell development.

AB - Extensive studies of mice deficient in one or several cytokine receptors have failed to support an indispensable role of cytokines in development of multiple blood cell lineages. Whereas B1 B cells and Igs are sustained at normal levels throughout life of mice deficient in IL-7, IL-7Ralpha, common cytokine receptor gamma chain, or flt3 ligand (FL), we report here that adult mice double deficient in IL-7Ralpha and FL completely lack visible LNs, conventional IgM+ B cells, IgA+ plasma cells, and B1 cells, and consequently produce no Igs. All stages of committed B cell progenitors are undetectable in FL-/- x IL-7Ralpha-/- BM that also lacks expression of the B cell commitment factor Pax5 and its direct target genes. Furthermore, in contrast to IL-7Ralpha-/- mice, FL-/- x IL-7Ralpha-/- mice also lack mature B cells and detectable committed B cell progenitors during fetal development. Thus, signaling through the cytokine tyrosine kinase receptor flt3 and IL-7Ralpha are indispensable for fetal and adult B cell development.

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DO - 10.1084/jem.20031152

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