Differential Expression of IgM and IgD Discriminates Two Subpopulations of Human Circulating IgM+IgD+CD27+ B Cells That Differ Phenotypically, Functionally, and Genetically

Diana Bautista; Camilo Vásquez; Paola Ayala-Ramírez; Juan Téllez-Sosa; Ernestina Godoy-Lozano; Jesús Martínez-Barnetche; Manuel Franco; Juana Angel

doi:10.3389/fimmu.2020.00736

Differential Expression of IgM and IgD Discriminates Two Subpopulations of Human Circulating IgM⁺IgD⁺CD27⁺ B Cells That Differ Phenotypically, Functionally, and Genetically

Diana Bautista, Camilo Vásquez, Paola Ayala-Ramírez, Juan Téllez-Sosa, Ernestina Godoy-Lozano, Jesús Martínez-Barnetche, Manuel Franco, Juana Angel

Producción: Contribución a una revista › Artículo › revisión exhaustiva

31 Citas (Scopus)

Resumen

The origin and function of blood IgM⁺IgD⁺CD27⁺ B cells is controversial, and they are considered a heterogeneous population. Previous staining of circulating B cells of healthy donors with rotavirus fluorescent virus-like particles allowed us to differentiate two subsets of IgM⁺IgD⁺CD27⁺: IgM^hi and IgM^lo B cells. Here, we confirmed this finding and compared the phenotype, transcriptome, in vitro function, and Ig gene repertoire of these two subsets. Eleven markers phenotypically discriminated both subsets (CD1c, CD69, IL21R, CD27, MTG, CD45RB, CD5, CD184, CD23, BAFFR, and CD38) with the IgM^hi phenotypically resembling previously reported marginal zone B cells and the IgM^lo resembling both naïve and memory B cells. Transcriptomic analysis showed that both subpopulations clustered close to germinal center-experienced IgM only B cells with a Principal Component Analysis, but differed in expression of 78 genes. Moreover, IgM^hi B cells expressed genes characteristic of previously reported marginal zone B cells. After stimulation with CpG and cytokines, significantly (p < 0.05) higher frequencies (62.5%) of IgM^hi B cells proliferated, compared with IgM^lo B cells (35.37%), and differentiated to antibody secreting cells (14.22% for IgM^hi and 7.19% for IgM^lo). IgM^hi B cells had significantly (p < 0.0007) higher frequencies of mutations in IGHV and IGKV regions, IgM^lo B cells had higher usage of IGHJ6 genes (p < 0.0001), and both subsets differed in their HCDR3 properties. IgM^hi B cells shared most of their shared IGH clonotypes with IgM only memory B cells, and IgM^lo B cells with IgM^hi B cells. These results support the notion that differential expression of IgM and IgD discriminates two subpopulations of human circulating IgM⁺IgD⁺CD27⁺ B cells, with the IgM^hi B cells having similarities with previously described marginal zone B cells that passed through germinal centers, and the IgM^lo B cells being the least differentiated amongst the IgM⁺CD27⁺ subsets.

Idioma original	Inglés
Número de artículo	736
Publicación	Frontiers in Immunology
Volumen	11
DOI	https://doi.org/10.3389/fimmu.2020.00736
Estado	Publicada - 06 may. 2020

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Bautista, D., Vásquez, C., Ayala-Ramírez, P., Téllez-Sosa, J., Godoy-Lozano, E., Martínez-Barnetche, J., Franco, M., & Angel, J. (2020). Differential Expression of IgM and IgD Discriminates Two Subpopulations of Human Circulating IgM⁺IgD⁺CD27⁺ B Cells That Differ Phenotypically, Functionally, and Genetically. Frontiers in Immunology, 11, Artículo 736. https://doi.org/10.3389/fimmu.2020.00736

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title = "Differential Expression of IgM and IgD Discriminates Two Subpopulations of Human Circulating IgM+IgD+CD27+ B Cells That Differ Phenotypically, Functionally, and Genetically",

abstract = "The origin and function of blood IgM+IgD+CD27+ B cells is controversial, and they are considered a heterogeneous population. Previous staining of circulating B cells of healthy donors with rotavirus fluorescent virus-like particles allowed us to differentiate two subsets of IgM+IgD+CD27+: IgMhi and IgMlo B cells. Here, we confirmed this finding and compared the phenotype, transcriptome, in vitro function, and Ig gene repertoire of these two subsets. Eleven markers phenotypically discriminated both subsets (CD1c, CD69, IL21R, CD27, MTG, CD45RB, CD5, CD184, CD23, BAFFR, and CD38) with the IgMhi phenotypically resembling previously reported marginal zone B cells and the IgMlo resembling both na{\"i}ve and memory B cells. Transcriptomic analysis showed that both subpopulations clustered close to germinal center-experienced IgM only B cells with a Principal Component Analysis, but differed in expression of 78 genes. Moreover, IgMhi B cells expressed genes characteristic of previously reported marginal zone B cells. After stimulation with CpG and cytokines, significantly (p < 0.05) higher frequencies (62.5%) of IgMhi B cells proliferated, compared with IgMlo B cells (35.37%), and differentiated to antibody secreting cells (14.22% for IgMhi and 7.19% for IgMlo). IgMhi B cells had significantly (p < 0.0007) higher frequencies of mutations in IGHV and IGKV regions, IgMlo B cells had higher usage of IGHJ6 genes (p < 0.0001), and both subsets differed in their HCDR3 properties. IgMhi B cells shared most of their shared IGH clonotypes with IgM only memory B cells, and IgMlo B cells with IgMhi B cells. These results support the notion that differential expression of IgM and IgD discriminates two subpopulations of human circulating IgM+IgD+CD27+ B cells, with the IgMhi B cells having similarities with previously described marginal zone B cells that passed through germinal centers, and the IgMlo B cells being the least differentiated amongst the IgM+CD27+ subsets.",

keywords = "Ig gene repertoire, blood, cell proliferation, cell surface molecules, gene expression, human, marginal zone B cells, memory B cells",

author = "Diana Bautista and Camilo V{\'a}squez and Paola Ayala-Ram{\'i}rez and Juan T{\'e}llez-Sosa and Ernestina Godoy-Lozano and Jes{\'u}s Mart{\'i}nez-Barnetche and Manuel Franco and Juana Angel",

note = "Publisher Copyright: {\textcopyright} Copyright {\textcopyright} 2020 Bautista, V{\'a}squez, Ayala-Ram{\'i}rez, T{\'e}llez-Sosa, Godoy-Lozano, Mart{\'i}nez-Barnetche, Franco and Angel.",

year = "2020",

month = may,

day = "6",

doi = "10.3389/fimmu.2020.00736",

language = "English",

volume = "11",

journal = "Frontiers in Immunology",

issn = "1664-3224",

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}

Bautista, D, Vásquez, C, Ayala-Ramírez, P, Téllez-Sosa, J, Godoy-Lozano, E, Martínez-Barnetche, J, Franco, M & Angel, J 2020, 'Differential Expression of IgM and IgD Discriminates Two Subpopulations of Human Circulating IgM⁺IgD⁺CD27⁺ B Cells That Differ Phenotypically, Functionally, and Genetically', Frontiers in Immunology, vol. 11, 736. https://doi.org/10.3389/fimmu.2020.00736

Differential Expression of IgM and IgD Discriminates Two Subpopulations of Human Circulating IgM⁺IgD⁺CD27⁺ B Cells That Differ Phenotypically, Functionally, and Genetically. / Bautista, Diana; Vásquez, Camilo; Ayala-Ramírez, Paola et al.
En: Frontiers in Immunology, Vol. 11, 736, 06.05.2020.

Producción: Contribución a una revista › Artículo › revisión exhaustiva

TY - JOUR

T1 - Differential Expression of IgM and IgD Discriminates Two Subpopulations of Human Circulating IgM+IgD+CD27+ B Cells That Differ Phenotypically, Functionally, and Genetically

AU - Bautista, Diana

AU - Vásquez, Camilo

AU - Ayala-Ramírez, Paola

AU - Téllez-Sosa, Juan

AU - Godoy-Lozano, Ernestina

AU - Martínez-Barnetche, Jesús

AU - Franco, Manuel

AU - Angel, Juana

PY - 2020/5/6

Y1 - 2020/5/6

N2 - The origin and function of blood IgM+IgD+CD27+ B cells is controversial, and they are considered a heterogeneous population. Previous staining of circulating B cells of healthy donors with rotavirus fluorescent virus-like particles allowed us to differentiate two subsets of IgM+IgD+CD27+: IgMhi and IgMlo B cells. Here, we confirmed this finding and compared the phenotype, transcriptome, in vitro function, and Ig gene repertoire of these two subsets. Eleven markers phenotypically discriminated both subsets (CD1c, CD69, IL21R, CD27, MTG, CD45RB, CD5, CD184, CD23, BAFFR, and CD38) with the IgMhi phenotypically resembling previously reported marginal zone B cells and the IgMlo resembling both naïve and memory B cells. Transcriptomic analysis showed that both subpopulations clustered close to germinal center-experienced IgM only B cells with a Principal Component Analysis, but differed in expression of 78 genes. Moreover, IgMhi B cells expressed genes characteristic of previously reported marginal zone B cells. After stimulation with CpG and cytokines, significantly (p < 0.05) higher frequencies (62.5%) of IgMhi B cells proliferated, compared with IgMlo B cells (35.37%), and differentiated to antibody secreting cells (14.22% for IgMhi and 7.19% for IgMlo). IgMhi B cells had significantly (p < 0.0007) higher frequencies of mutations in IGHV and IGKV regions, IgMlo B cells had higher usage of IGHJ6 genes (p < 0.0001), and both subsets differed in their HCDR3 properties. IgMhi B cells shared most of their shared IGH clonotypes with IgM only memory B cells, and IgMlo B cells with IgMhi B cells. These results support the notion that differential expression of IgM and IgD discriminates two subpopulations of human circulating IgM+IgD+CD27+ B cells, with the IgMhi B cells having similarities with previously described marginal zone B cells that passed through germinal centers, and the IgMlo B cells being the least differentiated amongst the IgM+CD27+ subsets.

AB - The origin and function of blood IgM+IgD+CD27+ B cells is controversial, and they are considered a heterogeneous population. Previous staining of circulating B cells of healthy donors with rotavirus fluorescent virus-like particles allowed us to differentiate two subsets of IgM+IgD+CD27+: IgMhi and IgMlo B cells. Here, we confirmed this finding and compared the phenotype, transcriptome, in vitro function, and Ig gene repertoire of these two subsets. Eleven markers phenotypically discriminated both subsets (CD1c, CD69, IL21R, CD27, MTG, CD45RB, CD5, CD184, CD23, BAFFR, and CD38) with the IgMhi phenotypically resembling previously reported marginal zone B cells and the IgMlo resembling both naïve and memory B cells. Transcriptomic analysis showed that both subpopulations clustered close to germinal center-experienced IgM only B cells with a Principal Component Analysis, but differed in expression of 78 genes. Moreover, IgMhi B cells expressed genes characteristic of previously reported marginal zone B cells. After stimulation with CpG and cytokines, significantly (p < 0.05) higher frequencies (62.5%) of IgMhi B cells proliferated, compared with IgMlo B cells (35.37%), and differentiated to antibody secreting cells (14.22% for IgMhi and 7.19% for IgMlo). IgMhi B cells had significantly (p < 0.0007) higher frequencies of mutations in IGHV and IGKV regions, IgMlo B cells had higher usage of IGHJ6 genes (p < 0.0001), and both subsets differed in their HCDR3 properties. IgMhi B cells shared most of their shared IGH clonotypes with IgM only memory B cells, and IgMlo B cells with IgMhi B cells. These results support the notion that differential expression of IgM and IgD discriminates two subpopulations of human circulating IgM+IgD+CD27+ B cells, with the IgMhi B cells having similarities with previously described marginal zone B cells that passed through germinal centers, and the IgMlo B cells being the least differentiated amongst the IgM+CD27+ subsets.

KW - Ig gene repertoire

KW - blood

KW - cell proliferation

KW - cell surface molecules

KW - gene expression

KW - human

KW - marginal zone B cells

KW - memory B cells

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U2 - 10.3389/fimmu.2020.00736

DO - 10.3389/fimmu.2020.00736

M3 - Article

C2 - 32435242

AN - SCOPUS:85085158386

SN - 1664-3224

VL - 11

JO - Frontiers in Immunology

JF - Frontiers in Immunology

M1 - 736

ER -