Your search keyword '"Lakeya C. Hardy"' showing total 6 results

1. Intestinal helminth infection impairs oral and parenteral vaccine efficacy

Author

LaKeya C. Hardy, Camille M. Kapita, Evelyn Campbell, Jason A. Hall, Joseph F. Urban, Yasmine Belkaid, Cathryn R. Nagler, and Onyinye I. Iweala

Abstract

The impact of endemic parasitic infection on vaccine efficacy is an important consideration for vaccine development and deployment. We have examined whether intestinal infection with the natural murine helminthHeligmosomoides polygyrus bakerialters antigen-specific antibody and cellular immune responses to oral and parenteral vaccination in mice. We found that oral vaccination of mice with a clinically relevant, live, attenuated, recombinantSalmonellavaccine that expresses chicken egg ovalbumin (Salmonella-OVA) disrupts ovalbumin-specific regulatory T cell networks in the gut associated lymphoid tissue and promotes T-effector responses to OVA. Chronic intestinal helminth infection significantly reduced Th1-skewed antibody responses to oral vaccination withSalmonella-OVA. Activated, adoptively-transferred, OVA-specific CD4+T cells accumulated in draining mesenteric lymph nodes (MLN) of vaccinated mice, irrespective of their helminth-infection status. However, helminth infection increased the frequencies of adoptively-transferred OVA-specific CD4+T cells producing IL-4 and IL-10 in the MLN. Chronic intestinal helminth infection also significantly reduced Th2-skewed antibody responses to parenteral vaccination with OVA adsorbed to alum. These findings suggest helminth-induced impairment of vaccine antibody responses may be driven by the development of IL-10-secreting CD4+T regulatory cells. They also underscore the potential need to treat parasitic infection before mass vaccination campaigns in helminth-endemic areas.

Published

2022

2. Targeting CD22 on memory B cells to induce tolerance to peanut allergens

Author

LaKeya C. Hardy, Johanna M. Smeekens, Dharmendra Raghuwanshi, Susmita Sarkar, Gour C. Daskhan, Stephen Rogers, Corwin Nycholat, Soheila Maleki, A. Wesley Burks, James C. Paulson, Matthew S. Macauley, and Michael D. Kulis

Subjects

Mice, Inbred C57BL, Mice, Arachis, Memory B Cells, Sialic Acid Binding Ig-like Lectin 2, Immunology, Immune Tolerance, Immunology and Allergy, Humans, Animals, Allergens, Article

Abstract

BACKGROUND: Circulating IgE and subsequent severe allergic reactions to peanut are sustained and propagated by recall of peanut allergen-specific memory B cells. OBJECTIVES: This study aimed to determine whether targeting mouse and human CD22 on peanut-specific memory B cells induces tolerance to peanut allergens. METHODS: Siglec-engaging tolerance-inducing antigenic liposomes (STALs) codisplaying peanut allergens (Ara h 1, Ara h 2, or Ara h 3) and high-affinity CD22 ligand (CD22L-STALs) were employed in various mouse models (BALB/cJ, C57BL/6, human CD22 transgenic, and NSG) of peanut allergy. To investigate memory B cells, a conferred memory model was used in which splenocytes from peanut-sensitized mice were transferred into naive animals. Reconstituted mice received either CD22L-STALs or an immunogenic liposome control, followed by a peanut allergen boost and later a challenge with individual peanut allergens. To assess the effects of CD22L-STALs on human B cells, PBMCs were injected into NSG mice, followed by administration of human CD22L-STALs (hCD22L-STALs) and later a whole peanut extract boost. Blood was collected to quantify WPE- and Ara h 1–, 2–, and 3–specific immunoglobulins. RESULTS: Mouse CD22L-STALs (mCD22L-STALs) significantly suppressed systemic memory to Ara h 1, Ara h 2, and Ara h 3 in BALB/cJ and C57BL/6 mice, as demonstrated by reduced allergen-specific IgE, IgG(1), and anaphylaxis on challenge. Importantly, 2 doses of mCD22L-STALs led to prolonged tolerance for at least 3 months. hCD22L-STALs displayed similar suppression in mice expressing human CD22 on B cells. Finally, human B cells were tolerized in vivo in NSG mice by hCD22L-STALs. CONCLUSIONS: Antigen-specific exploitation of CD22 on memory B cells can induce systemic immune tolerance.

Published

2022

3. Biomarkers in Food Allergy Immunotherapy

Author

Lakeya C. Hardy, Michael D. Kulis, and Johanna Smeekens

Subjects

Pulmonary and Respiratory Medicine, Allergy, medicine.medical_treatment, T-Lymphocytes, Immunology, Immunoglobulins, medicine.disease_cause, Immunoglobulin E, Allergen, Food allergy, Immunology and Allergy, Medicine, Humans, Skin Tests, biology, business.industry, Immunotherapy, medicine.disease, Slit, Basophils, Basophil activation, Desensitization, Immunologic, biology.protein, Biomarker (medicine), business, Biomarkers, Food Hypersensitivity

Abstract

Investigational allergen immunotherapies (AITs) including oral immunotherapy (OIT), sublingual immunotherapy (SLIT), and epicutaneous immunotherapy (EPIT) have proven to increase allergen thresholds required to elicit an allergic reaction in a majority of subjects. However, these studies lack consistent biomarkers to predict therapy outcomes. Here, we will review biomarkers that are currently being investigated for AIT. The mechanisms underlying the therapeutic benefit of AIT involve various cell types, including mast cells, basophils, T cells, and B cells. Skin prick and basophil activation tests assess effector cell sensitivity to allergen and are decreased in subjects on AIT. Allergen-specific IgE increases initially and decreases with continued therapy, while allergen-specific IgG and IgA increase throughout therapy. Allergen-induced regulatory T cells (Tregs) increase throughout therapy and were found to be associated with sustained unresponsiveness after OIT. Subjects on OIT and SLIT have decreased Th2 cytokine production during therapy. Although trends have been reported, a common limitation of these biomarkers is that none are able to reproducibly predict prognosis during AIT. Further studies are needed to expand the currently available biomarker repertoire to provide personalized approaches to AIT.

Published

2019

4. Antigenic Liposomes for Generation of Disease-specific Antibodies

Author

Dharmendra Raghuwanshi, Lakeya C. Hardy, Shiteng Duan, Johanna Smeekens, Mike Kulis, Kyle J. Bednar, and Matthew S. Macauley

Subjects

0301 basic medicine, Immunogen, Arachis, T-Lymphocytes, General Chemical Engineering, medicine.medical_treatment, Peanut allergy, General Biochemistry, Genetics and Molecular Biology, Mice, 03 medical and health sciences, 0302 clinical medicine, Antigen, Calcium flux, medicine, Animals, Humans, Peanut Hypersensitivity, Anaphylaxis, Immunology and Infection, General Immunology and Microbiology, biology, General Neuroscience, Reproducibility of Results, Allergens, Immunoglobulin E, medicine.disease, Vaccination, 030104 developmental biology, Immunization, Liposomes, Immunology, biology.protein, Nanoparticles, Female, Antibody, Adjuvant, Food Hypersensitivity, 030215 immunology

Abstract

Antibody responses provide critical protective immunity to a wide array of pathogens. There remains a high interest in generating robust antibodies for vaccination as well as understand how pathogenic antibody responses develop in allergies and autoimmune disease. Generating robust antigen-specific antibody responses is not always trivial. In mouse models, it often requires multiple rounds of immunizations with adjuvant that leads to a great deal of variability in the levels of induced antibodies. One example is in mouse models of peanut allergies where more robust and reproducible models that minimize mouse numbers and the use of adjuvant would be beneficial. Presented here is a highly reproducible mouse model of peanut allergy anaphylaxis. This new model relies on two key factors: (1) antigen-specific splenocytes are adoptively transferred from a peanut-sensitized mouse into a naïve recipient mouse, normalizing the number of antigen-specific memory B- and T-cells across a large number of mice; and (2) recipient mice are subsequently boosted with a strong multivalent immunogen in the form of liposomal nanoparticles displaying the major peanut allergen (Ara h 2). The major advantage of this model is its reproducibility, which ultimately lowers the number of animals used in each study, while minimizing the number of animals receiving multiple injections of adjuvant. The modular assembly of these immunogenic liposomes provides relatively facile adaptability to other allergic or autoimmune models that involve pathogenic antibodies.

Published

2018

5. Epigenetic Dysfunction in T cells is Associated with Enhanced Type-2 and Blunted Regulatory Immunity

Author

Shailesh K. Choudhary, Hsing-Hui Wang, Lakeya C. Hardy, Claire T. Addison, Maureen A. Su, Joseph F. Urban, Cathryn R. Nagler, Onyinye I. Iweala, Nikhil Milind, A. Wesley Burks, Kelly Orgel, Scott P. Commins, and Michael D. Kulis

Subjects

Immunity, Immunology, Immunology and Allergy, Epigenetics, Biology

Published

2019

6. Using Siglec-engaging Tolerance-inducing Antigenic Liposomes (STALs) to reduce memory B cell responses to the major peanut allergen Ara h 2

Author

Shiteng Duan, Michael D. Kulis, Kelly Orgel, James C. Paulson, Lakeya C. Hardy, Matthew S. Macauley, A. Wesley Burks, and Soheila J. Maleki

Subjects

Liposome, Allergen, Antigen, Chemistry, Immunology, medicine, Immunology and Allergy, SIGLEC, medicine.disease_cause, Memory B cell

Published

2018