Depleting CD103+ resident memory T cells in vivo reveals immunostimulatory functions in oral mucosa

J. Michael Stolley; Milcah C. Scott; Vineet Joag; Alexander J. Dale; Timothy S. Johnston; Flavia Saavedra; Noah V. Gavil; Sahar Lotfi-Emran; Andrew G. Soerens; Eyob Weyu; Mark J. Pierson; Mark C. Herzberg; Nu Zhang; Vaiva Vezys; David Masopust

doi:10.1084/jem.20221853

Depleting CD103⁺ resident memory T cells in vivo reveals immunostimulatory functions in oral mucosa

J. Michael Stolley, Milcah C. Scott, Vineet Joag, Alexander J. Dale, Timothy S. Johnston, Flavia Saavedra, Noah V. Gavil, Sahar Lotfi-Emran, Andrew G. Soerens, Eyob Weyu, Mark J. Pierson, Mark C. Herzberg, Nu Zhang, Vaiva Vezys, David Masopust

Department of Microbiology, Immunology & Molecular Genetics

Producción científica: Article › revisión exhaustiva

11 Citas (Scopus)

Resumen

The oral mucosa is a frontline for microbial exposure and juxtaposes several unique tissues and mechanical structures. Based on parabiotic surgery of mice receiving systemic viral infections or co-housing with microbially diverse pet shop mice, we report that the oral mucosa harbors CD8⁺ CD103⁺ resident memory T cells (T_RM), which locally survey tissues without recirculating. Oral antigen re-encounter during the effector phase of immune responses potentiated T_RM establishment within tongue, gums, palate, and cheek. Upon reactivation, oral T_RM triggered changes in somatosensory and innate immune gene expression. We developed in vivo methods for depleting CD103⁺ T_RM while sparing CD103^neg T_RM and recirculating cells. This revealed that CD103⁺ T_RM were responsible for inducing local gene expression changes. Oral T_RM putatively protected against local viral infection. This study provides methods for generating, assessing, and in vivo depleting oral T_RM, documents their distribution throughout the oral mucosa, and provides evidence that T_RM confer protection and trigger responses in oral physiology and innate immunity.

Idioma original	English (US)
Número de artículo	e20221853
Publicación	Journal of Experimental Medicine
Volumen	220
N.º	7
DOI	https://doi.org/10.1084/jem.20221853
Estado	Published - jul 3 2023

ASJC Scopus subject areas

Immunology and Allergy
Immunology

Acceder al documento

10.1084/jem.20221853

Otros archivos y enlaces

Citar esto

Michael Stolley, J., Scott, M. C., Joag, V., Dale, A. J., Johnston, T. S., Saavedra, F., Gavil, N. V., Lotfi-Emran, S., Soerens, A. G., Weyu, E., Pierson, M. J., Herzberg, M. C., Zhang, N., Vezys, V., & Masopust, D. (2023). Depleting CD103⁺ resident memory T cells in vivo reveals immunostimulatory functions in oral mucosa. Journal of Experimental Medicine, 220(7), Artículo e20221853. https://doi.org/10.1084/jem.20221853

Michael Stolley, J, Scott, MC, Joag, V, Dale, AJ, Johnston, TS, Saavedra, F, Gavil, NV, Lotfi-Emran, S, Soerens, AG, Weyu, E, Pierson, MJ, Herzberg, MC, Zhang, N, Vezys, V & Masopust, D 2023, 'Depleting CD103⁺ resident memory T cells in vivo reveals immunostimulatory functions in oral mucosa', Journal of Experimental Medicine, vol. 220, n.º 7, e20221853. https://doi.org/10.1084/jem.20221853

@article{ab9d65d7c09745c5bb8b2a9e0365da73,

title = "Depleting CD103+ resident memory T cells in vivo reveals immunostimulatory functions in oral mucosa",

abstract = "The oral mucosa is a frontline for microbial exposure and juxtaposes several unique tissues and mechanical structures. Based on parabiotic surgery of mice receiving systemic viral infections or co-housing with microbially diverse pet shop mice, we report that the oral mucosa harbors CD8+ CD103+ resident memory T cells (TRM), which locally survey tissues without recirculating. Oral antigen re-encounter during the effector phase of immune responses potentiated TRM establishment within tongue, gums, palate, and cheek. Upon reactivation, oral TRM triggered changes in somatosensory and innate immune gene expression. We developed in vivo methods for depleting CD103+ TRM while sparing CD103neg TRM and recirculating cells. This revealed that CD103+ TRM were responsible for inducing local gene expression changes. Oral TRM putatively protected against local viral infection. This study provides methods for generating, assessing, and in vivo depleting oral TRM, documents their distribution throughout the oral mucosa, and provides evidence that TRM confer protection and trigger responses in oral physiology and innate immunity.",

author = "{Michael Stolley}, J. and Scott, {Milcah C.} and Vineet Joag and Dale, {Alexander J.} and Johnston, {Timothy S.} and Flavia Saavedra and Gavil, {Noah V.} and Sahar Lotfi-Emran and Soerens, {Andrew G.} and Eyob Weyu and Pierson, {Mark J.} and Herzberg, {Mark C.} and Nu Zhang and Vaiva Vezys and David Masopust",

note = "Publisher Copyright: {\textcopyright} 2023 Stolley et al.",

year = "2023",

month = jul,

day = "3",

doi = "10.1084/jem.20221853",

language = "English (US)",

volume = "220",

journal = "Journal of Experimental Medicine",

issn = "0022-1007",

publisher = "Rockefeller University Press",

number = "7",

}

TY - JOUR

T1 - Depleting CD103+ resident memory T cells in vivo reveals immunostimulatory functions in oral mucosa

AU - Michael Stolley, J.

AU - Scott, Milcah C.

AU - Joag, Vineet

AU - Dale, Alexander J.

AU - Johnston, Timothy S.

AU - Saavedra, Flavia

AU - Gavil, Noah V.

AU - Lotfi-Emran, Sahar

AU - Soerens, Andrew G.

AU - Weyu, Eyob

AU - Pierson, Mark J.

AU - Herzberg, Mark C.

AU - Zhang, Nu

AU - Vezys, Vaiva

AU - Masopust, David

PY - 2023/7/3

Y1 - 2023/7/3

N2 - The oral mucosa is a frontline for microbial exposure and juxtaposes several unique tissues and mechanical structures. Based on parabiotic surgery of mice receiving systemic viral infections or co-housing with microbially diverse pet shop mice, we report that the oral mucosa harbors CD8+ CD103+ resident memory T cells (TRM), which locally survey tissues without recirculating. Oral antigen re-encounter during the effector phase of immune responses potentiated TRM establishment within tongue, gums, palate, and cheek. Upon reactivation, oral TRM triggered changes in somatosensory and innate immune gene expression. We developed in vivo methods for depleting CD103+ TRM while sparing CD103neg TRM and recirculating cells. This revealed that CD103+ TRM were responsible for inducing local gene expression changes. Oral TRM putatively protected against local viral infection. This study provides methods for generating, assessing, and in vivo depleting oral TRM, documents their distribution throughout the oral mucosa, and provides evidence that TRM confer protection and trigger responses in oral physiology and innate immunity.

AB - The oral mucosa is a frontline for microbial exposure and juxtaposes several unique tissues and mechanical structures. Based on parabiotic surgery of mice receiving systemic viral infections or co-housing with microbially diverse pet shop mice, we report that the oral mucosa harbors CD8+ CD103+ resident memory T cells (TRM), which locally survey tissues without recirculating. Oral antigen re-encounter during the effector phase of immune responses potentiated TRM establishment within tongue, gums, palate, and cheek. Upon reactivation, oral TRM triggered changes in somatosensory and innate immune gene expression. We developed in vivo methods for depleting CD103+ TRM while sparing CD103neg TRM and recirculating cells. This revealed that CD103+ TRM were responsible for inducing local gene expression changes. Oral TRM putatively protected against local viral infection. This study provides methods for generating, assessing, and in vivo depleting oral TRM, documents their distribution throughout the oral mucosa, and provides evidence that TRM confer protection and trigger responses in oral physiology and innate immunity.

UR - http://www.scopus.com/inward/record.url?scp=85153900814&partnerID=8YFLogxK

UR - http://www.scopus.com/inward/citedby.url?scp=85153900814&partnerID=8YFLogxK

U2 - 10.1084/jem.20221853

DO - 10.1084/jem.20221853

M3 - Article

C2 - 37097449

AN - SCOPUS:85153900814

SN - 0022-1007

VL - 220

JO - Journal of Experimental Medicine

JF - Journal of Experimental Medicine

IS - 7

M1 - e20221853

ER -