An Immunologic Mode of Multigenerational Transmission Governs a Gut Treg Setpoint

Ramanan, Deepshika; Sefik, Esen; Galván-Peña, Silvia; Wu, Meng; Yang, Liang; Yang, Zhen; Kostic, Aleksandar D.; Golovkina, Tatyana V.; Kasper, Dennis L.; Mathis, Diane; Benoist, Christophe

doi:10.1016/j.cell.2020.04.030

Cited by 120 publications

(127 citation statements)

References 79 publications

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“…An additional limitation of our work is that we focused on the effect of desynchronization on the development of colonic pTregs, and the effects of desynchronization may extend well beyond this cellular population and effects of alterations in EGF exposure. Indeed, recent studies have found that breast milk IgA levels inversely correlate with colonic RORγt + Tregs in the offspring and that this is a phenotype transmissible across generations (68). Future work will attempt to correlate allergic outcomes with desynchronization in humans and examine the effects of desynchronization beyond EGF and this cellular population.…”

Section: Discussionmentioning

confidence: 98%

Synchronization of mothers and offspring promotes tolerance and limits allergy

Knoop¹,

McDonald²,

Coughlin³

et al. 2020

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Section: Discussionmentioning

confidence: 98%

Synchronization of mothers and offspring promotes tolerance and limits allergy

Knoop¹,

McDonald²,

Coughlin³

et al. 2020

JCI Insight

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“…This process is regulated by maternal ligands present in breastmilk and bacterial components of the maturing microbiota around weaning, most notably epidermal growth factor ( 17 , 32 ). Maternal antibodies IgA and IgG also present in breastmilk have been shown to promote tolerance, may protect from food allergy pathogenesis in early life, and may help regulate development of RORγt+ pTregs ( 22 , 36 , 37 ). Following weaning, dietary antigens are largely encountered by the immune system in the small intestine, and dietary antigen-specific pTregs developing post-weaning have a limited life span in absence of antigen exposure ( 38 , 39 ).…”

Section: Discussionmentioning

confidence: 99%

“…A population of Tregs expressing the transcription factor RORγt+ differentiate early in life in a process driven by the microbiota, and may have unique capacities to avoid immunopathologies and restrain Th2 responses ( 21 , 22 ). Intriguingly this population of Tregs are reduced in children with food allergies ( 23 ).…”

Section: Introductionmentioning

confidence: 99%

Regulatory T Cells Developing Peri-Weaning Are Continually Required to Restrain Th2 Systemic Responses Later in Life

et al. 2021

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Atopic disorders including allergic rhinitis, asthma, food allergy, and dermatitis, are increasingly prevalent in Western societies. These disorders are largely characterized by T helper type 2 (Th2) immune responses to environmental triggers, particularly inhaled and dietary allergens. Exposure to such stimuli during early childhood reduces the frequency of allergies in at-risk children. These allergic responses can be restrained by regulatory T cells (Tregs), particularly Tregs arising in the gut. The unique attributes of how early life exposure to diet and microbes shape the intestinal Treg population is a topic of significant interest. While imprinting during early life promotes the development of a balanced immune system and protects against immunopathology, it remains unclear if Tregs that develop in early life continue to restrain systemic inflammatory responses throughout adulthood. Here, an inducible deletion strategy was used to label Tregs at specified time points with a targeted mechanism to be deleted later. Deletion of the Tregs labeled peri-weaning at day of life 24, but not before weaning at day of life 14, resulted in increased circulating IgE and IL-13, and abrogated induction of tolerance towards new antigens. Thus, Tregs developing peri-weaning, but not before day of life 14 are continually required to restrain allergic responses into adulthood.

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“…It is perhaps because generalized suppression of adaptive immunity at mucosal sites through excessive pTreg generation could be dangerous, as contact with facultative pathogens are frequent and risk of infections are high. Setting the correct bar for RORγt+ Tregs and homeostasis with the developing microbiota needs to occur in childhood, and seems to also be imprinted from the mother to the next generation by a double-negative loop involving maternally transmitted IgA ( 67 , 68 ). While this mechanism ensures that the next generation benefits from a maternal experience on the correct bar for a beneficial host-microbiota equilibrium, microbial adaptations are still able to fine-tune the level of RORγt+ Tregs throughout life and offer therapeutic options.…”

Section: Discussionmentioning

confidence: 99%