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159 results on '"McDonald, Keely G"'

2. Small Intestinal Goblet Cells Control Humoral Immune Responses and Mobilization During Enteric Infection.

Author

Kulkarni, Devesha H, primary, Talati, Khushi B, additional, Joyce, Elisabeth L, additional, Kousik, Hrishi, additional, Harris, Dalia L, additional, Floyd, Alexandra N, additional, Vavrinyuk, Vitaly, additional, Barrios, Bibiana, additional, Udayan, Sreeram, additional, McDonald, Keely G, additional, John, Vini, additional, Hsieh, Chyi-Song, additional, and Newberry, Rodney D, additional

Published
2024
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6. Intergenerational protective anti-gut commensal immunoglobulin G originates in early life.

Author

Rusconi, Brigida, Bard, Adina K., McDonough, Ryan, Kindsvogel, Angel M., Wang, Jacqueline D., Udayan, Sreeram, McDonald, Keely G., Newberry, Rodney D., and Tarr, Phillip I.

Subjects
IMMUNOGLOBULIN G, PLASMA cells, INTESTINAL infections, IMMUNOGLOBULINS, B cells
Abstract

Maternal immunoglobulins of the class G (IgGs) protect offspring from enteric infection, but when, where, and how these antibodies are physiologically generated and confer protection remains enigmatic. We found that circulating IgGs in adult mice preferentially bind early-life gut commensal bacteria over their own adult gut commensal bacteria. IgG-secreting plasma cells specific for early-life gut bacteria appear in the intestine soon after weaning, where they remain into adulthood. Manipulating exposure to gut bacteria or plasma cell development before, but not after, weaning reduced IgG-secreting plasma cells targeting early-life gut bacteria throughout life. Further, the development of this anti-gut commensal IgG response coincides with the early-life interval in which goblet cell--associated antigen passages (GAPs) are present in the colon. Offspring of dams "perturbed" by B cell ablation or reduced bacterial exposure in early life were more susceptible to enteric pathogen challenge. In contrast to current concepts, protective maternal IgGs targeted translocating gut commensals in the offspring, not the enteric pathogen. These early-life events affecting anti-commensal IgG production have intergenerational effects for protection of the offspring. [ABSTRACT FROM AUTHOR]

Published
2024
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7. Vancomycin-induced gut microbial dysbiosis alters enteric neuron–macrophage interactions during a critical period of postnatal development

Author

Schill, Ellen Merrick, primary, Joyce, Elisabeth L., additional, Floyd, Alexandria N., additional, Udayan, Sreeram, additional, Rusconi, Brigida, additional, Gaddipati, Shreya, additional, Barrios, Bibiana E., additional, John, Vini, additional, Kaye, Mitchell E., additional, Kulkarni, Devesha H., additional, Pauta, Jocelyn T., additional, McDonald, Keely G., additional, and Newberry, Rodney D., additional

Published
2023
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8. Gut microbiota induces weight gain and inflammation in the gut and adipose tissue independent of manipulations in diet, genetics, and immune development.

Author

Kulkarni, Devesha H., Rusconi, Brigida, Floyd, Alexandria N., Joyce, Elisabeth L., Talati, Khushi B., Kousik, Hrishi, Alleyne, Dereck, Harris, Dalia L., Garnica, Lorena, McDonough, Ryan, Bidani, Shay S., Kulkarni, Hrishikesh S., Newberry, Elizabeth P., McDonald, Keely G., and Newberry, Rodney D.

Published
2023
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14. Vancomycin-induced gut microbial dysbiosis alters enteric neuron--macrophage interactions during a critical period of postnatal development.

Author

Merrick Schill, Ellen, Joyce, Elisabeth L., Floyd, Alexandria N., Udayan, Sreeram, Rusconi, Brigida, Gaddipati, Shreya, Barrios, Bibiana E., John, Vini, Kaye, Mitchell E., Kulkarni, Devesha H., Pauta, Jocelyn T., McDonald, Keely G., and Newberry, Rodney D.

Subjects
NEONATAL sepsis, ENTERIC nervous system, PUERPERIUM, SUBMUCOUS plexus, MACROPHAGES, DYSBIOSIS, BONE marrow, NEURONS
Abstract

Vancomycin is a broad-spectrum antibiotic widely used in cases of suspected sepsis in premature neonates. While appropriate and potentially lifesaving in this setting, early-life antibiotic exposure alters the developing microbiome and is associated with an increased risk of deadly complications, including late-onset sepsis (LOS) and necrotizing enterocolitis (NEC). Recent studies show that neonatal vancomycin treatment disrupts postnatal enteric nervous system (ENS) development in mouse pups, which is in part dependent upon neuroimmune interactions. This suggests that early-life antibiotic exposure could disrupt these interactions in the neonatal gut. Notably, a subset of tissue-resident intestinal macrophages, muscularis macrophages, has been identified as important contributors to the development of postnatal ENS. We hypothesized that vancomycin-induced neonatal dysbiosis impacts postnatal ENS development through its effects on macrophages. Using a mouse model, we found that exposure to vancomycin in the first 10 days of life, but not in adult mice, resulted in an expansion of pro-inflammatory colonic macrophages by increasing the recruitment of bone-marrow-derived macrophages. Single-cell RNA sequencing of neonatal colonic macrophages revealed that early-life vancomycin exposure was associated with an increase in immature and inflammatory macrophages, consistent with an influx of circulating monocytes differentiating into macrophages. Lineage tracing confirmed that vancomycin significantly increased the non-yolk-sac-derived macrophage population. Consistent with these results, early-life vancomycin exposure did not expand CCR2-deficient mice. Collectively, these findings demonstrate that early-life vancomycin exposure alters macrophage number and phenotypes in distinct ways compared with vancomycin exposure in adult mice and results in altered ENS development. [ABSTRACT FROM AUTHOR]

Published
2023
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23. Notch2-dependent classical dendritic cells orchestrate intestinal immunity to attaching-and-effacing bacterial pathogens

Author

Satpathy, Ansuman T, Briseño, Carlos G, Lee, Jacob S, Ng, Dennis, Manieri, Nicholas A, KC, Wumesh, Wu, Xiaodi, Thomas, Stephanie R, Lee, Wan-Ling, Turkoz, Mustafa, McDonald, Keely G, Meredith, Matthew M, Song, Christina, Guidos, Cynthia J, Newberry, Rodney D, Ouyang, Wenjun, Murphy, Theresa L, Stappenbeck, Thaddeus S, Gommerman, Jennifer L, Nussenzweig, Michel C, Colonna, Marco, Kopan, Raphael, and Murphy, Kenneth M

Published
2013
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25. Murine astrovirus tropism for goblet cells and enterocytes facilitates an IFN-λ response in vivo and in enteroid cultures

Author

Ingle, Harshad, primary, Hassan, Ebrahim, additional, Gawron, Jana, additional, Mihi, Belgacem, additional, Li, Yuhao, additional, Kennedy, Elizabeth A., additional, Kalugotla, Gowri, additional, Makimaa, Heyde, additional, Lee, Sanghyun, additional, Desai, Pritesh, additional, McDonald, Keely G., additional, Diamond, Michael S., additional, Newberry, Rodney D., additional, Good, Misty, additional, and Baldridge, Megan T., additional

Published
2021
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26. Murine isolated lymphoid follicles contain follicular B lymphocytes with a mucosal phenotype

Author

Wang, Caihong, McDonald, Keely G., McDonough, Jacquelyn S., and Newberry, Rodney D.

Subjects
Lymphocytes -- Research, Immunoglobulin A -- Research, Biological sciences
Abstract

Isolated lymphoid follicles (ILFs) are organized intestinal lymphoid structures whose formation can be induced by luminal stimuli. ILFs have been demonstrated to act as inductive sites for the generation of immune responses directed toward luminal stimuli; however, the phenotype of the immune response initiated within ILFs has largely been uninvestigated. To gain a better understanding of the immune responses initiated within ILFs, we examined phenotypic and functional aspects of the largest cellular component of the routine ILF lymphocyte population, B lymphocytes. We observed that murine ILF B lymphocytes are composed of a relatively homogenous population of follicular B-2 B lymphocytes. Consistent with their proximity to multiple stimuli, ILF B lymphocytes displayed a more activated phenotype compared with their counterparts in the spleen and Peyer's patch (PP). ILF B lymphocytes also expressed higher levels of immunomodulatory B7 and CD28 family members B7X and programmed death-1 compared with their counterparts in the spleen and PP. ILF B lymphocytes preferentially differentiate into IgA-producing plasma cells and produce more IL-4 and IL-10 and less interferon-[gamma] compared with their counterparts in the spleen. Immunoglobulin repertoire analysis from individual ILFs demonstrated that ILFs contain a polyclonal population of B lymphocytes. These findings indicate that murine ILFs contain a polyclonal population of follicular B-2 B lymphocytes with a phenotype similar to PP B lymphocytes and that, in unchallenged animals, ILFs promote immune responses with a homeostatic phenotype. intestine; immunoglobulin A

Published
2006

29. Synchronization of mothers and offspring promotes tolerance and limits allergy

Author

Knoop, Kathryn A., primary, McDonald, Keely G., additional, Coughlin, Paige E., additional, Kulkarni, Devesha H., additional, Gustafsson, Jenny K., additional, Rusconi, Brigida, additional, John, Vini, additional, Ndao, I. Malick, additional, Beigelman, Avraham, additional, Good, Misty, additional, Warner, Barbara B., additional, Elson, Charles O., additional, Hsieh, Chyi-Song, additional, Hogan, Simon P., additional, Tarr, Phillip I., additional, and Newberry, Rodney D., additional

Published
2020
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31. CRTAM Protects Against Intestinal Dysbiosis During Pathogenic Parasitic Infection by Enabling Th17 Maturation

Author

Cervantes-Barragan, Luisa, primary, Cortez, Victor S., additional, Wang, Qiuling, additional, McDonald, Keely G., additional, Chai, Jiani N., additional, Di Luccia, Blanda, additional, Gilfillan, Susan, additional, Hsieh, Chyi-Song, additional, Newberry, Rodney D., additional, Sibley, L. David, additional, and Colonna, Marco, additional

Published
2019
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32. The tumor necrosis factor superfamily member RANKL suppresses effector cytokine production in group 3 innate lymphoid cells

Author

Bando, Jennifer, primary, Gilfillan, Susan, additional, Song, Christina, additional, McDonald, Keely G, additional, Huang, Stanley C-C, additional, Newberry, Rodney D, additional, Kobayashi, Yasuhiro, additional, Allan, David, additional, Carlyle, James R, additional, Cella, Marina, additional, and Colonna, Marco, additional

Published
2019
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33. Aging impacts isolated lymphoid follicle fevelopment and function

Author

Wang Caihong, Huang Conway, Leach Matthew R, McDonald Keely G, and Newberry Rodney D

Subjects
Immunologic diseases. Allergy, RC581-607, Geriatrics, RC952-954.6
Abstract

Abstract Background Immunosenescence is the age-related decline and dysfunction of protective immunity leading to a marked increase in the risk of infections, autoimmune disease, and cancer. The majority of studies have focused on immunosenescence in the systemic immune system; information concerning the effect of aging on intestinal immunity is limited. Isolated lymphoid follicles (ILFs) are newly appreciated dynamic intestinal lymphoid structures that arise from nascent lymphoid tissues, or cryptopatches (CP), in response to local inflammatory stimuli. ILFs promote "homeostatic" responses including the production of antigen-specific IgA, thus playing a key role in mucosal immune protection. ILF dysfunction with aging could contribute to immunosenescence of the mucosal system, and accordingly we examined phenotypic and functional aspects of ILFs from young (2 month old) and aged (2 year old) mice. Results We observed that aged mice have increased numbers of ILFs and increased numbers of structures corresponding to an early stage of CPs transforming into ILFs. The cellular composition of ILFs in aged mice is altered with a smaller B-lymphocyte population and an increased T-lymphocyte population. The ILF T-lymphocyte population is notable by the presence of CD4+ CD8αα+ T-lymphocytes, which are absent from the systemic compartment. The smaller B-lymphocyte population in ILFs from aged mice is directly correlated with decreased mRNA and protein expression of CCL20 and CXCL13, two chemokines that play crucial roles in recruiting B-lymphocytes into ILFs. Aged mice had elevated levels of serum and fecal immunoglobulins and despite the decreased B-lymphocyte population, ILFs from aged mice displayed increased IgA production. The immunoglobulin repertoire was skewed in aged mice, and ILFs demonstrated a repertoire usage similar to that of the systemic pool in both young and aged mice. Conclusions Here we observed that ILF development, cellular composition, and immunoglobulin production are altered with aging suggesting that ILF dysfunction contributes to mucosal immunosenescence.

Published
2011
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34. T Cells Developing Peri-Weaning Are Continually Required to Restrain Th2 Systemic Responses Later in Life.

Author

Knoop, Kathryn A., McDonald, Keely G., Hsieh, Chyi-Song, Tarr, Phillip I., and Newberry, Rodney D.

Subjects
T cells, SUPPRESSOR cells, ALLERGIC rhinitis, FOOD allergy, IMMUNE system
Abstract

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. [ABSTRACT FROM AUTHOR]

Published
2021
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36. The Tumor Necrosis Factor Superfamily Member RANKL Suppresses Effector Cytokine Production in Group 3 Innate Lymphoid Cells

Author

Bando, Jennifer K., primary, Gilfillan, Susan, additional, Song, Christina, additional, McDonald, Keely G., additional, Huang, Stanley C.-C., additional, Newberry, Rodney D., additional, Kobayashi, Yasuhiro, additional, Allan, David S.J., additional, Carlyle, James R., additional, Cella, Marina, additional, and Colonna, Marco, additional

Published
2018
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45. CRTAM controls residency of gut CD4+CD8+ T cells in the steady state and maintenance of gut CD4+ Th17 during parasitic infection

Author

Cortez, Victor S., primary, Cervantes-Barragan, Luisa, additional, Song, Christina, additional, Gilfillan, Susan, additional, McDonald, Keely G., additional, Tussiwand, Roxane, additional, Edelson, Brian T., additional, Murakami, Yoshinori, additional, Murphy, Kenneth M., additional, Newberry, Rodney D., additional, Sibley, L. David, additional, and Colonna, Marco, additional

Published
2014
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46. Goblet cell associated antigen passages are inhibited during Salmonella typhimuriuminfection to prevent pathogen dissemination and limit responses to dietary antigens

Author

Kulkarni, Devesha H., McDonald, Keely G., Knoop, Kathryn A., Gustafsson, Jenny K., Kozlowski, Konrad M., Hunstad, David A., Miller, Mark J., and Newberry, Rodney D.

Abstract

Dietary antigen acquisition by lamina propria (LP) dendritic cells (DCs) is crucial to induce oral tolerance and maintain homeostasis. However, encountering innocuous antigens during infection can lead to inflammatory responses, suggesting processes may limit steady-state luminal antigen capture during infection. We observed that goblet cell (GC) associated antigen passages (GAPs), a steady-state pathway delivering luminal antigens to LP-DCs, are inhibited during Salmonellainfection. GAP inhibition was mediated by IL-1β. Infection abrogated luminal antigen delivery and antigen-specific T cell proliferation in the mesenteric lymph node (MLN). Antigen-specific T cell proliferation to dietary antigen was restored by overriding GAP suppression; however, this did not restore regulatory T cell induction, but induced inflammatory T cell responses. Salmonellatranslocation to the MLN required GCs and correlated with GAPs. Genetic manipulations overriding GAP suppression, or antibiotics inducing colonic GAPs, but not antibiotics that do not, increased dissemination and worsened outcomes independent of luminal pathogen burden. Thus, steady-state sampling pathways are suppressed during infection to prevent responses to dietary antigens, limit pathogen entry, and lessen the disease. Moreover, antibiotics may worsen Salmonellainfection by means beyond blunting gut microbiota colonization resistance, providing new insight into how precedent antibiotic use aggravates enteric infection.

Published
2018
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48. AHR drives the development of gut ILC22 cells and postnatal lymphoid tissues via pathways dependent on and independent of Notch

Author

Lee, Jacob S, primary, Cella, Marina, additional, McDonald, Keely G, additional, Garlanda, Cecilia, additional, Kennedy, Gregory D, additional, Nukaya, Manabu, additional, Mantovani, Alberto, additional, Kopan, Raphael, additional, Bradfield, Christopher A, additional, Newberry, Rodney D, additional, and Colonna, Marco, additional

Published
2011
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