Intraperitoneal Immunization with Cry1Ac Protoxin from <i>Bacillus thuringiensis</i> Provokes Upregulation of Fc‐Gamma‐II/and Fc‐Gamma‐III Receptors Associated with IgG in the Intestinal Epithelium of Mice

Moreno‐Fierros, Leticia; Verdı́n-Terán, S.Leticia; García‐Hernández, Ana Lilia

doi:10.1111/sji.12305

Cited by 6 publications

(4 citation statements)

References 44 publications

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“…This is surprising since FcG receptors have rarely been observed in non-haematopoietic cells 57 . To our knowledge, FcgrII expression has only been observed in mouse intestinal epithelial cells after immunization with bacterial neurotoxin 23 and by human nasal epithelial cells in response to bacteria-derived ligands 58 . We also note expression of the FCGR2A by our previously described thymic mTEC(II) epithelial population, which expresses low levels of tuft cell transcription factor POU2F3 (developmentcellatlas.ncl.ac.uk).…”

Section: Discussionmentioning

confidence: 94%

“…3K). Among these, only FCGR2A, which is activated in response to IgG and shown to be expressed by epithelial cells in immunized mice 23 , was specifically expressed by a fraction (2.75%) of tuft cells (Figure 2E). Using the mouse as a model, we confirmed expression of Fcgr3 (ortholog of FCGR2A) at protein level by approximately 5% of small intestinal tuft cells (Figure 2F & Supplementary Fig.…”

Section: Diversity Of Epithelial Cells In the Human Intestinal Tractmentioning

confidence: 99%

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Cells of the human intestinal tract mapped across space and time

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Kumasaka

King

et al. 2021

Preprint

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The cellular landscape of the human intestinal tract is dynamic throughout life, developing in utero and changing in response to functional requirements and environmental exposures. To comprehensively map cell lineages in the healthy developing, pediatric and adult human gut from ten distinct anatomical regions, as well as draining lymph nodes, we used single-cell RNA-seq and VDJ analysis of roughly one third of a million cells. This reveals the presence of BEST4+ absorptive cells throughout the human intestinal tract, demonstrating the existence of this cell type beyond the colon for the first time. Furthermore, we implicate IgG sensing as a novel function of intestinal tuft cells, and link these cells to the pathogenesis of inflammatory bowel disease. We define novel glial and neuronal cell populations in the developing enteric nervous system, and predict cell-type specific expression of Hirschsprung's disease-associated genes. Finally, using a systems approach, we identify key cell players across multiple cell lineages driving secondary lymphoid tissue formation in early human development. We show that these programs are adopted in inflammatory bowel disease to recruit and retain immune cells at the site of inflammation. These data provide an unprecedented catalogue of intestinal cells, and new insights into cellular programs in development, homeostasis and disease.

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Section: Discussionmentioning

confidence: 94%

Section: Diversity Of Epithelial Cells In the Human Intestinal Tractmentioning

confidence: 99%

Cells of the human intestinal tract mapped across space and time

Elmentaite

Kumasaka

King

et al. 2021

Preprint

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“…6i ). FCGR2A, which is activated in response to IgG and expressed by selected epithelial cells in immunized mice 21 , was specifically expressed by approximately 2.75% of tuft cells (Fig. 2f ).…”

Section: Diversity Of Intestinal Epithelial Cellsmentioning

confidence: 99%

Cells of the human intestinal tract mapped across space and time

Elmentaite

Kumasaka

Roberts

et al. 2021

Nature

372

349

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The cellular landscape of the human intestinal tract is dynamic throughout life, developing in utero and changing in response to functional requirements and environmental exposures. Here, to comprehensively map cell lineages, we use single-cell RNA sequencing and antigen receptor analysis of almost half a million cells from up to 5 anatomical regions in the developing and up to 11 distinct anatomical regions in the healthy paediatric and adult human gut. This reveals the existence of transcriptionally distinct BEST4 epithelial cells throughout the human intestinal tract. Furthermore, we implicate IgG sensing as a function of intestinal tuft cells. We describe neural cell populations in the developing enteric nervous system, and predict cell-type-specific expression of genes associated with Hirschsprung’s disease. Finally, using a systems approach, we identify key cell players that drive the formation of secondary lymphoid tissue in early human development. We show that these programs are adopted in inflammatory bowel disease to recruit and retain immune cells at the site of inflammation. This catalogue of intestinal cells will provide new insights into cellular programs in development, homeostasis and disease.

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“…In particular, an increased antibody response against an unrelated protein (i.e. ovalbumin) was observed (Vázquez-Padrón et al 1999 ; González-González et al 2015 ; Moreno-Fierros et al 2015 ). In contrast, the adjuvant effect of Cry1Ab on ovalbumin was not observed in BALB/c mice after airway exposure to extracts of MON810 pollen/leaf or trypsinized Cry1Ab (Andreassen et al 2015b ).…”

Section: Discussionmentioning

confidence: 99%

Humoral and cellular immune response in Wistar Han RCC rats fed two genetically modified maize MON810 varieties for 90 days (EU 7th Framework Programme project GRACE)

et al. 2018

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The genetically modified maize event MON810 expresses a Bacillus thuringiensis-derived gene, which encodes the insecticidal protein Cry1Ab to control some lepidopteran insect pests such as the European corn borer. It has been claimed that the immune system may be affected following the oral/intragastric administration of the MON810 maize in various different animal species. In the frame of the EU-funded project GRACE, two 90-day feeding trials, the so-called studies D and E, were performed to analyze the humoral and cellular immune responses of male and female Wistar Han RCC rats fed the MON810 maize. A MON810 maize variety of Monsanto was used in the study D and a MON810 maize variety of Pioneer Hi-Bred was used in the study E. The total as well as the maize protein- and Cry1Ab-serum-specific IgG, IgM, IgA and IgE levels, the proliferative activity of the lymphocytes, the phagocytic activity of the granulocytes and monocytes, the respiratory burst of the phagocytes, a phenotypic analysis of spleen, thymus and lymph node cells as well as the in vitro production of cytokines by spleen cells were analyzed. No specific Cry1Ab immune response was observed in MON810 rats, and anti-maize protein antibody responses were similar in MON810 and control rats. Single parameters were sporadically altered in rats fed the MON810 maize when compared to control rats, but these alterations are considered to be of no immunotoxicological significance.Electronic supplementary materialThe online version of this article (10.1007/s00204-018-2230-z) contains supplementary material, which is available to authorized users.

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Intraperitoneal Immunization with Cry1Ac Protoxin from Bacillus thuringiensis Provokes Upregulation of Fc‐Gamma‐II/and Fc‐Gamma‐III Receptors Associated with IgG in the Intestinal Epithelium of Mice

Cited by 6 publications

References 44 publications

Cells of the human intestinal tract mapped across space and time

Cells of the human intestinal tract mapped across space and time

Cells of the human intestinal tract mapped across space and time

Humoral and cellular immune response in Wistar Han RCC rats fed two genetically modified maize MON810 varieties for 90 days (EU 7th Framework Programme project GRACE)

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