Long-lived IgE plasma cells that reside in the spleen contribute to the persistence of the IgE response

Mariana C.G. Miranda-Waldetario; Edgar Gonzalez-Kozlova; Edenil C. Aguilar; Laura Xie; Kenneth B. Hoehn; Carlos J. Aranda; Yolanda Garcia-Carmona; Erica G.M. Ma; Emma S. Agudelo; Jamie Redes; Maria A. Curotto de Lafaille

doi:10.1016/j.immuni.2025.10.011

Long-lived IgE plasma cells that reside in the spleen contribute to the persistence of the IgE response

Mariana C.G. Miranda-Waldetario
, Edgar Gonzalez-Kozlova
, Edenil C. Aguilar
, Laura Xie
, Kenneth B. Hoehn
, Carlos J. Aranda
, Yolanda Garcia-Carmona
, Erica G.M. Ma
, Emma S. Agudelo
, Jamie Redes
, Maria A. Curotto de Lafaille

Research output: Contribution to journal › Article › peer-review

3 Scopus citations

Abstract

Expression of the IgE BCR is associated with increased B cell apoptosis, yet in persistent allergy, sustained production of IgE antibodies in the absence of allergen exposure suggests the existence of long-lived IgE plasma cells (PCs). Here we studied the development and localization of IgE PCs in mouse models of allergy. After immunization, IgE PCs underwent maturation in spleen and lymph nodes, acquiring a stable MHCII^loCD93⁺CD98^hiBCR^lo phenotype. Mature IgE PCs had a distinct transcriptional profile adapted to high protein synthesis, glycosylation, and survival and resisted BCR-crosslinking-induced apoptosis. Immunization induced a burst of short-lived IgE PC formation, followed by a reduced differentiation rate over time, compared with IgG1 PCs. Timestamping of PCs revealed long-lived IgE PCs that localize to the spleen, in addition to the bone marrow (BM). Thus, immune challenge can generate both short-lived and long-lived IgE PCs, with long-lived IgE PCs in spleen and BM contributing to allergy persistence.

Original language	English
Pages (from-to)	2717-2733.e7
Journal	Immunity
Volume	58
Issue number	11
DOIs	https://doi.org/10.1016/j.immuni.2025.10.011
State	Published - 11 Nov 2025

Keywords

IgE plasma cells
allergy persistence
long-lived plasma cells
spleen niche
timestamping

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Miranda-Waldetario, M. C. G., Gonzalez-Kozlova, E., Aguilar, E. C., Xie, L., Hoehn, K. B., Aranda, C. J., Garcia-Carmona, Y., Ma, E. G. M., Agudelo, E. S., Redes, J., & Curotto de Lafaille, M. A. (2025). Long-lived IgE plasma cells that reside in the spleen contribute to the persistence of the IgE response. Immunity, 58(11), 2717-2733.e7. https://doi.org/10.1016/j.immuni.2025.10.011

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title = "Long-lived IgE plasma cells that reside in the spleen contribute to the persistence of the IgE response",

abstract = "Expression of the IgE BCR is associated with increased B cell apoptosis, yet in persistent allergy, sustained production of IgE antibodies in the absence of allergen exposure suggests the existence of long-lived IgE plasma cells (PCs). Here we studied the development and localization of IgE PCs in mouse models of allergy. After immunization, IgE PCs underwent maturation in spleen and lymph nodes, acquiring a stable MHCIIloCD93+CD98hiBCRlo phenotype. Mature IgE PCs had a distinct transcriptional profile adapted to high protein synthesis, glycosylation, and survival and resisted BCR-crosslinking-induced apoptosis. Immunization induced a burst of short-lived IgE PC formation, followed by a reduced differentiation rate over time, compared with IgG1 PCs. Timestamping of PCs revealed long-lived IgE PCs that localize to the spleen, in addition to the bone marrow (BM). Thus, immune challenge can generate both short-lived and long-lived IgE PCs, with long-lived IgE PCs in spleen and BM contributing to allergy persistence.",

keywords = "IgE plasma cells, allergy persistence, long-lived plasma cells, spleen niche, timestamping",

author = "Miranda-Waldetario, \{Mariana C.G.\} and Edgar Gonzalez-Kozlova and Aguilar, \{Edenil C.\} and Laura Xie and Hoehn, \{Kenneth B.\} and Aranda, \{Carlos J.\} and Yolanda Garcia-Carmona and Ma, \{Erica G.M.\} and Agudelo, \{Emma S.\} and Jamie Redes and \{Curotto de Lafaille\}, \{Maria A.\}",

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year = "2025",

month = nov,

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doi = "10.1016/j.immuni.2025.10.011",

language = "English",

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AU - Miranda-Waldetario, Mariana C.G.

AU - Gonzalez-Kozlova, Edgar

AU - Aguilar, Edenil C.

AU - Xie, Laura

AU - Hoehn, Kenneth B.

AU - Aranda, Carlos J.

AU - Garcia-Carmona, Yolanda

AU - Ma, Erica G.M.

AU - Agudelo, Emma S.

AU - Redes, Jamie

AU - Curotto de Lafaille, Maria A.

PY - 2025/11/11

Y1 - 2025/11/11

N2 - Expression of the IgE BCR is associated with increased B cell apoptosis, yet in persistent allergy, sustained production of IgE antibodies in the absence of allergen exposure suggests the existence of long-lived IgE plasma cells (PCs). Here we studied the development and localization of IgE PCs in mouse models of allergy. After immunization, IgE PCs underwent maturation in spleen and lymph nodes, acquiring a stable MHCIIloCD93+CD98hiBCRlo phenotype. Mature IgE PCs had a distinct transcriptional profile adapted to high protein synthesis, glycosylation, and survival and resisted BCR-crosslinking-induced apoptosis. Immunization induced a burst of short-lived IgE PC formation, followed by a reduced differentiation rate over time, compared with IgG1 PCs. Timestamping of PCs revealed long-lived IgE PCs that localize to the spleen, in addition to the bone marrow (BM). Thus, immune challenge can generate both short-lived and long-lived IgE PCs, with long-lived IgE PCs in spleen and BM contributing to allergy persistence.

AB - Expression of the IgE BCR is associated with increased B cell apoptosis, yet in persistent allergy, sustained production of IgE antibodies in the absence of allergen exposure suggests the existence of long-lived IgE plasma cells (PCs). Here we studied the development and localization of IgE PCs in mouse models of allergy. After immunization, IgE PCs underwent maturation in spleen and lymph nodes, acquiring a stable MHCIIloCD93+CD98hiBCRlo phenotype. Mature IgE PCs had a distinct transcriptional profile adapted to high protein synthesis, glycosylation, and survival and resisted BCR-crosslinking-induced apoptosis. Immunization induced a burst of short-lived IgE PC formation, followed by a reduced differentiation rate over time, compared with IgG1 PCs. Timestamping of PCs revealed long-lived IgE PCs that localize to the spleen, in addition to the bone marrow (BM). Thus, immune challenge can generate both short-lived and long-lived IgE PCs, with long-lived IgE PCs in spleen and BM contributing to allergy persistence.

KW - IgE plasma cells

KW - allergy persistence

KW - long-lived plasma cells

KW - spleen niche

KW - timestamping

UR - https://www.scopus.com/pages/publications/105020804725

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DO - 10.1016/j.immuni.2025.10.011

M3 - Article

C2 - 41175873

AN - SCOPUS:105020804725

SN - 1074-7613

VL - 58

SP - 2717-2733.e7

JO - Immunity

JF - Immunity

IS - 11

ER -

Long-lived IgE plasma cells that reside in the spleen contribute to the persistence of the IgE response

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Keywords

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