Basal immunoglobulin signaling actively maintains developmental stage in immature B cells

Lina E. Tze; Brian R. Schram; Kong Peng Lam; Kristin A. Hogquist; Keli L. Hippen; Jiabin Liu; Susan A. Shinton; Kevin L. Otipoby; Peter R. Rodine; Amanda L. Vegoe; Manfred Kraus; Richard R. Hardy; Mark S. Schlissel; Klaus Rajewsky; Timothy W. Behrens

doi:10.1371/journal.pbio.0030082

Basal immunoglobulin signaling actively maintains developmental stage in immature B cells

Lina E. Tze, Brian R. Schram, Kong Peng Lam, Kristin A. Hogquist, Keli L. Hippen, Jiabin Liu, Susan A. Shinton, Kevin L. Otipoby, Peter R. Rodine, Amanda L. Vegoe, Manfred Kraus, Richard R. Hardy, Mark S. Schlissel, Klaus Rajewsky, Timothy W. Behrens

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Abstract

In developing B lymphocytes, a successful V(D)J heavy chain (HC) immunoglobulin (Ig) rearrangement establishes HC allelic exclusion and signals pro-B cells to advance in development to the pre-B stage. A subsequent functional light chain (LC) rearrangement then results in the surface expression of IgM at the immature B cell stage. Here we show that interruption of basal IgM signaling in immature B cells, either by the inducible deletion of surface Ig via Cre-mediated excision or by incubating cells with the tyrosine kinase inhibitor herbimycin A or the phosphatidylinositol 3-kinase inhibitor wortmannin, led to a striking "back-differentiation" of cells to an earlier stage in B cell development, characterized by the expression of pro-B cell genes. Cells undergoing this reversal in development also showed evidence of new LC gene rearrangements, suggesting an important role for basal Ig signaling in the maintenance of LC allelic exclusion. These studies identify a previously unappreciated level of plasticity in the B cell developmental program, and have important implications for our understanding of central tolerance mechanisms.

Original language	English (US)
Article number	e82
Pages (from-to)	463-475
Number of pages	13
Journal	PLoS Biology
Volume	3
Issue number	3
DOIs	https://doi.org/10.1371/journal.pbio.0030082
State	Published - Mar 2005

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Tze, L. E., Schram, B. R., Lam, K. P., Hogquist, K. A., Hippen, K. L., Liu, J., Shinton, S. A., Otipoby, K. L., Rodine, P. R., Vegoe, A. L., Kraus, M., Hardy, R. R., Schlissel, M. S., Rajewsky, K., & Behrens, T. W. (2005). Basal immunoglobulin signaling actively maintains developmental stage in immature B cells. PLoS Biology, 3(3), 463-475. Article e82. https://doi.org/10.1371/journal.pbio.0030082

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abstract = "In developing B lymphocytes, a successful V(D)J heavy chain (HC) immunoglobulin (Ig) rearrangement establishes HC allelic exclusion and signals pro-B cells to advance in development to the pre-B stage. A subsequent functional light chain (LC) rearrangement then results in the surface expression of IgM at the immature B cell stage. Here we show that interruption of basal IgM signaling in immature B cells, either by the inducible deletion of surface Ig via Cre-mediated excision or by incubating cells with the tyrosine kinase inhibitor herbimycin A or the phosphatidylinositol 3-kinase inhibitor wortmannin, led to a striking {"}back-differentiation{"} of cells to an earlier stage in B cell development, characterized by the expression of pro-B cell genes. Cells undergoing this reversal in development also showed evidence of new LC gene rearrangements, suggesting an important role for basal Ig signaling in the maintenance of LC allelic exclusion. These studies identify a previously unappreciated level of plasticity in the B cell developmental program, and have important implications for our understanding of central tolerance mechanisms.",

author = "Tze, {Lina E.} and Schram, {Brian R.} and Lam, {Kong Peng} and Hogquist, {Kristin A.} and Hippen, {Keli L.} and Jiabin Liu and Shinton, {Susan A.} and Otipoby, {Kevin L.} and Rodine, {Peter R.} and Vegoe, {Amanda L.} and Manfred Kraus and Hardy, {Richard R.} and Schlissel, {Mark S.} and Klaus Rajewsky and Behrens, {Timothy W.}",

year = "2005",

month = mar,

doi = "10.1371/journal.pbio.0030082",

language = "English (US)",

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AU - Tze, Lina E.

AU - Schram, Brian R.

AU - Lam, Kong Peng

AU - Hogquist, Kristin A.

AU - Hippen, Keli L.

AU - Liu, Jiabin

AU - Shinton, Susan A.

AU - Otipoby, Kevin L.

AU - Rodine, Peter R.

AU - Vegoe, Amanda L.

AU - Kraus, Manfred

AU - Hardy, Richard R.

AU - Schlissel, Mark S.

AU - Rajewsky, Klaus

AU - Behrens, Timothy W.

PY - 2005/3

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N2 - In developing B lymphocytes, a successful V(D)J heavy chain (HC) immunoglobulin (Ig) rearrangement establishes HC allelic exclusion and signals pro-B cells to advance in development to the pre-B stage. A subsequent functional light chain (LC) rearrangement then results in the surface expression of IgM at the immature B cell stage. Here we show that interruption of basal IgM signaling in immature B cells, either by the inducible deletion of surface Ig via Cre-mediated excision or by incubating cells with the tyrosine kinase inhibitor herbimycin A or the phosphatidylinositol 3-kinase inhibitor wortmannin, led to a striking "back-differentiation" of cells to an earlier stage in B cell development, characterized by the expression of pro-B cell genes. Cells undergoing this reversal in development also showed evidence of new LC gene rearrangements, suggesting an important role for basal Ig signaling in the maintenance of LC allelic exclusion. These studies identify a previously unappreciated level of plasticity in the B cell developmental program, and have important implications for our understanding of central tolerance mechanisms.

AB - In developing B lymphocytes, a successful V(D)J heavy chain (HC) immunoglobulin (Ig) rearrangement establishes HC allelic exclusion and signals pro-B cells to advance in development to the pre-B stage. A subsequent functional light chain (LC) rearrangement then results in the surface expression of IgM at the immature B cell stage. Here we show that interruption of basal IgM signaling in immature B cells, either by the inducible deletion of surface Ig via Cre-mediated excision or by incubating cells with the tyrosine kinase inhibitor herbimycin A or the phosphatidylinositol 3-kinase inhibitor wortmannin, led to a striking "back-differentiation" of cells to an earlier stage in B cell development, characterized by the expression of pro-B cell genes. Cells undergoing this reversal in development also showed evidence of new LC gene rearrangements, suggesting an important role for basal Ig signaling in the maintenance of LC allelic exclusion. These studies identify a previously unappreciated level of plasticity in the B cell developmental program, and have important implications for our understanding of central tolerance mechanisms.

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ER -

Basal immunoglobulin signaling actively maintains developmental stage in immature B cells

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