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Most Marginal Zone B Cells in Rat Express Germline Encoded Ig V sub(H) Genes and Are Ligand Selected
The present study was performed to analyze whether marginal zone B (MZ-B) cells in nondeliberately immunized adult rats are selected on basis of the specificity of their B cell receptor, and to determine to what extent memory B cells contribute to the MZ-B cell subset. To this end, the Ig PC7183 V s...
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Published in: | The Journal of immunology (1950) 2000-12, Vol.165 (11), p.6156-6169 |
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container_title | The Journal of immunology (1950) |
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creator | Dammers, P M Visser, A Popa, E R Nieuwenhuis, P Kroese, FGM |
description | The present study was performed to analyze whether marginal zone B (MZ-B) cells in nondeliberately immunized adult rats are selected on basis of the specificity of their B cell receptor, and to determine to what extent memory B cells contribute to the MZ-B cell subset. To this end, the Ig PC7183 V sub(H) gene repertoire was studied among V sub(H)DJ sub(H)- mu transcripts expressed in four sequential stages of B cell development, of two individual untreated adult rats. B cell subsets, i.e., pro/pre-B cells and newly formed B (NF-B) cells from bone marrow, and recirculating follicular B cells and MZ-B cells from spleen were sorted by flow cytometry. In addition, from one these rats, cells were microdissected from follicular and MZ areas of the spleen and productive PC7183 V sub(H) gene rearrangements were analyzed for the presence of somatic mutations. Sequence analysis reveals that most MZ-B cells in the adult rat, either defined by flow cytometry or by their anatomical location in the spleen, express germline encoded V sub(H) genes (naive MZ-B cells) and a minor fraction (about 20%) of the MZ-B cells carry somatic mutations (memory MZ-B cells). In addition, we show that naive MZ-B cells are a selected population of cells, both based on PC7183 V sub(H) gene repertoire and on the length of the Ig heavy (H) chain complementarity-determining region 3 (H-CDR3) region, i.e., PC7183 V sub(H)DJ sub(H)- mu transcripts of MZ-B cells carry significantly shorter H-CDR3 regions than other B cell subsets. |
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To this end, the Ig PC7183 V sub(H) gene repertoire was studied among V sub(H)DJ sub(H)- mu transcripts expressed in four sequential stages of B cell development, of two individual untreated adult rats. B cell subsets, i.e., pro/pre-B cells and newly formed B (NF-B) cells from bone marrow, and recirculating follicular B cells and MZ-B cells from spleen were sorted by flow cytometry. In addition, from one these rats, cells were microdissected from follicular and MZ areas of the spleen and productive PC7183 V sub(H) gene rearrangements were analyzed for the presence of somatic mutations. Sequence analysis reveals that most MZ-B cells in the adult rat, either defined by flow cytometry or by their anatomical location in the spleen, express germline encoded V sub(H) genes (naive MZ-B cells) and a minor fraction (about 20%) of the MZ-B cells carry somatic mutations (memory MZ-B cells). In addition, we show that naive MZ-B cells are a selected population of cells, both based on PC7183 V sub(H) gene repertoire and on the length of the Ig heavy (H) chain complementarity-determining region 3 (H-CDR3) region, i.e., PC7183 V sub(H)DJ sub(H)- mu transcripts of MZ-B cells carry significantly shorter H-CDR3 regions than other B cell subsets.</description><identifier>ISSN: 0022-1767</identifier><language>eng</language><subject>AB-cell receptor ; complementarity-determining region 3</subject><ispartof>The Journal of immunology (1950), 2000-12, Vol.165 (11), p.6156-6169</ispartof><lds50>peer_reviewed</lds50><woscitedreferencessubscribed>false</woscitedreferencessubscribed></display><links><openurl>$$Topenurl_article</openurl><openurlfulltext>$$Topenurlfull_article</openurlfulltext><thumbnail>$$Tsyndetics_thumb_exl</thumbnail><link.rule.ids>314,777,781</link.rule.ids></links><search><creatorcontrib>Dammers, P M</creatorcontrib><creatorcontrib>Visser, A</creatorcontrib><creatorcontrib>Popa, E R</creatorcontrib><creatorcontrib>Nieuwenhuis, P</creatorcontrib><creatorcontrib>Kroese, FGM</creatorcontrib><title>Most Marginal Zone B Cells in Rat Express Germline Encoded Ig V sub(H) Genes and Are Ligand Selected</title><title>The Journal of immunology (1950)</title><description>The present study was performed to analyze whether marginal zone B (MZ-B) cells in nondeliberately immunized adult rats are selected on basis of the specificity of their B cell receptor, and to determine to what extent memory B cells contribute to the MZ-B cell subset. 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To this end, the Ig PC7183 V sub(H) gene repertoire was studied among V sub(H)DJ sub(H)- mu transcripts expressed in four sequential stages of B cell development, of two individual untreated adult rats. B cell subsets, i.e., pro/pre-B cells and newly formed B (NF-B) cells from bone marrow, and recirculating follicular B cells and MZ-B cells from spleen were sorted by flow cytometry. In addition, from one these rats, cells were microdissected from follicular and MZ areas of the spleen and productive PC7183 V sub(H) gene rearrangements were analyzed for the presence of somatic mutations. Sequence analysis reveals that most MZ-B cells in the adult rat, either defined by flow cytometry or by their anatomical location in the spleen, express germline encoded V sub(H) genes (naive MZ-B cells) and a minor fraction (about 20%) of the MZ-B cells carry somatic mutations (memory MZ-B cells). In addition, we show that naive MZ-B cells are a selected population of cells, both based on PC7183 V sub(H) gene repertoire and on the length of the Ig heavy (H) chain complementarity-determining region 3 (H-CDR3) region, i.e., PC7183 V sub(H)DJ sub(H)- mu transcripts of MZ-B cells carry significantly shorter H-CDR3 regions than other B cell subsets.</abstract></addata></record> |
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subjects | AB-cell receptor complementarity-determining region 3 |
title | Most Marginal Zone B Cells in Rat Express Germline Encoded Ig V sub(H) Genes and Are Ligand Selected |
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