Your search keyword '"Scott A Leddon"' showing total 17 results

1. The control of the specificity of CD4 T cells responses: thresholds, breakpoints and ceilings

Author

Andrea J Sant, Francisco A Chaves, Scott A Leddon, and Jacqueline eTung

Subjects

CD4 T cells, immunodominance, Immunoregulation, MHC, HLA-DM, Immunologic diseases. Allergy, RC581-607

Abstract

It has been known for over 25 years that CD4 T cell responses are restricted to a finite number of peptide epitopes within pathogens or protein vaccines. These selected peptide epitopes are termed immunodominant. Other peptides within the antigen that can bind to host MHC molecules and recruit CD4 T cells as single peptides are termed cryptic because they fail to induce responses when expressed in complex proteins or when in competition with other peptides during the immune response. In the last decade, our laboratory has evaluated the mechanisms that underlie the preferential specificity of CD4 T cells and have discovered that both intracellular events within antigen presenting cells, particular selective DM editing, and intercellular regulatory pathways, involving IFN-γ, indoleamine 2,3-dioxygenase and regulatory T cells, play a role in selecting the final peptide specificity of CD4 T cells. In this review, we summarize our findings, discuss the implications of this work on responses to pathogens and vaccines and speculate on the logic of these regulatory events.

Published

2013

2. The peptide specificity of the endogenous T follicular helper cell repertoire generated after protein immunization.

Author

Scott A Leddon and Andrea J Sant

Subjects

Medicine, Science

Abstract

T follicular helper (Tfh) cells potentiate high-affinity, class-switched antibody responses, the predominant correlate of protection from vaccines. Despite intense interest in understanding both the generation and effector functions of this lineage, little is known about the epitope specificity of Tfh cells generated during polyclonal responses. To date, studies of peptide-specific Tfh cells have relied on either the transfer of TcR transgenic cells or use of peptide:MHC class II tetramers and antibodies to stain TcR and follow limited peptide specificities. In order to comprehensively evaluate polyclonal responses generated from the natural endogenous TcR repertoire, we developed a sorting strategy to separate Tfh cells from non-Tfh cells and found that their epitope-specific responses could be tracked with cytokine-specific ELISPOT assays. The immunodominance hierarchies of Tfh and non-Tfh cells generated in response to immunization with several unrelated protein antigens were remarkably similar. Additionally, increasing the kinetic stability of peptide-MHC class II complexes enhanced the priming of both Tfh and conventional CD4 T cells. These findings may provide us with a strategy to rationally and selectively modulate epitope-specific Tfh responses. By understanding the parameters that control epitope-specific priming, vaccines may be tailored to enhance or focus Tfh responses to facilitate optimal B cell responses.

Published

2012

3. CXCL10+ peripheral activation niches couple preferred sites of Th1 entry with optimal APC encounter

Author

Hen Prizant, Nilesh Patil, Seble Negatu, Noor Bala, Alexander McGurk, Scott A. Leddon, Angela Hughson, Tristan D. McRae, Yu-Rong Gao, Alexandra M. Livingstone, Joanna R. Groom, Andrew D. Luster, and Deborah J. Fowell

Subjects

CD4 T cells, Th1, chemokine, CXCL10, CXCR3, inflammation, Biology (General), QH301-705.5

Abstract

Summary: Correct positioning of T cells within infected tissues is critical for T cell activation and pathogen control. Upon tissue entry, effector T cells must efficiently locate antigen-presenting cells (APC) for peripheral activation. We reveal that tissue entry and initial peripheral activation of Th1 effector T cells are tightly linked to perivascular positioning of chemokine-expressing APCs. Dermal inflammation induces tissue-wide de novo generation of discrete perivascular CXCL10+ cell clusters, enriched for CD11c+MHC-II+ monocyte-derived dendritic cells. These chemokine clusters are “hotspots” for both Th1 extravasation and activation in the inflamed skin. CXCR3-dependent Th1 localization to the cluster micro-environment prolongs T-APC interactions and boosts function. Both the frequency and range of these clusters are enhanced via a T helper 1 (Th1)-intrinsic, interferon-gamma (IFNγ)-dependent positive-feedback loop. Thus, the perivascular CXCL10+ clusters act as initial peripheral activation niches, optimizing controlled activation broadly throughout the tissue by coupling Th1 tissue entry with enhanced opportunities for Th1-APC encounter.

Published

2021

4. T cell activation niches—Optimizing T cell effector function in inflamed and infected tissues

Author

Deborah J. Fowell, Scott A Leddon, Noor Bala, Anastasia N Rup, Tiago J. Zilch, Evan M Carter, and Alexander McGurk

Subjects

Chemokine, Effector, T cell, T-Lymphocytes, Immunology, Germinal center, Antigen-Presenting Cells, Chemotaxis, Biology, Lymphocyte Activation, Article, Cell biology, medicine.anatomical_structure, Immune system, Cell Movement, medicine, T cell migration, biology.protein, Immunology and Allergy, Cytokines, Humans, Chemokines, Lymph node

Abstract

Successful immunity to infection, malignancy, and tissue damage requires the coordinated recruitment of numerous immune cell subsets to target tissues. Once within the target tissue, effector T cells rely on local chemotactic cues and structural cues from the tissue matrix to navigate the tissue, interact with antigen-presenting cells, and release effector cytokines. This highly dynamic process has been "caught on camera" in situ by intravital multiphoton imaging. Initial studies revealed a surprising randomness to the pattern of T cell migration through inflamed tissues, behavior thought to facilitate chance encounters with rare antigen-bearing cells. Subsequent tissue-wide visualization has uncovered a high degree of spatial preference when it comes to T cell activation. Here, we discuss the basic tenants of a successful effector T cell activation niche, taking cues from the dynamics of Tfh positioning in the lymph node germinal center. In peripheral tissues, steady-state microanatomical organization may direct the location of "pop-up" de novo activation niches, often observed as perivascular clusters, that support early effector T cell activation. These perivascular activation niches appear to be regulated by site-specific chemokines that coordinate the recruitment of dendritic cells and other innate cells for local T cell activation, survival, and optimized effector function.

Published

2021

5. CXCL10+ peripheral activation niches couple preferred sites of Th1 entry with optimal APC encounter

Author

Seble Negatu, Hen Prizant, Alexander McGurk, Noor Bala, Tristan D. McRae, Angela Hughson, Nilesh Patil, Joanna R Groom, Deborah J. Fowell, Scott A Leddon, Alexandra M. Livingstone, Yu-Rong Gao, and Andrew D. Luster

Subjects

Chemokine, Leukocyte migration, CXCR3, biology, Chemistry, Effector, QH301-705.5, CXCL10, Antigen presentation, chemokine, CD11c, Dendritic cell, General Biochemistry, Genetics and Molecular Biology, Cell biology, Th1, inflammation, biology.protein, CD4 T cells, Biology (General)

Abstract

Summary: Correct positioning of T cells within infected tissues is critical for T cell activation and pathogen control. Upon tissue entry, effector T cells must efficiently locate antigen-presenting cells (APC) for peripheral activation. We reveal that tissue entry and initial peripheral activation of Th1 effector T cells are tightly linked to perivascular positioning of chemokine-expressing APCs. Dermal inflammation induces tissue-wide de novo generation of discrete perivascular CXCL10+ cell clusters, enriched for CD11c+MHC-II+ monocyte-derived dendritic cells. These chemokine clusters are “hotspots” for both Th1 extravasation and activation in the inflamed skin. CXCR3-dependent Th1 localization to the cluster micro-environment prolongs T-APC interactions and boosts function. Both the frequency and range of these clusters are enhanced via a T helper 1 (Th1)-intrinsic, interferon-gamma (IFNγ)-dependent positive-feedback loop. Thus, the perivascular CXCL10+ clusters act as initial peripheral activation niches, optimizing controlled activation broadly throughout the tissue by coupling Th1 tissue entry with enhanced opportunities for Th1-APC encounter.

Published

2021

6. Pivotal role for α V integrins in sustained Tfh support of the germinal center response for long-lived plasma cell generation

Author

Deborah J. Fowell, Angela Hughson, James H. Miller, Scott A Leddon, Adam Lacy-Hulbert, and Dillon C. Schrock

Subjects

Multidisciplinary, biology, αv integrins, T cell, Integrin, Germinal center, Plasma cell, Cell biology, medicine.anatomical_structure, biology.protein, medicine, Antibody, Lymph node, B-cell activation

Abstract

CD4+ follicular helper T cells (Tfh) are essential for germinal center (GC) reactions in the lymph node that generate high-affinity, long-lived plasma cells (LLPCs). Temporal GC analysis suggests B memory cells (Bmem) are generated early, while LLPCs are generated late in the GC reaction. Distinct roles for Tfh at these temporally different stages are not yet clear. Tfh entry into the GC is highly dynamic and the signals that maintain Tfh within the GC for support of late LLPC production are poorly understood. The GC is marked by inflammation-induced presentation of specific ECM components. To determine if T cell recognition of these ECM components played a role in Tfh support of the GC, we immunized mice with a T cell-restricted deletion of the ECM-binding integrin αV (αV-CD4 cKO). T cell integrin αV deletion led to a striking defect in the number and size of the GCs following immunization with OVA protein in complete Freund's adjuvant. The GC defect was not due to integrin αV deficiency impeding Tfh generation or follicle entry or the ability of αV-CD4 cKO Tfh to contact and support B cell activation. Instead, integrin αV was essential for T cell-intrinsic accumulation within the GC. Altered Tfh positioning resulted in lower-affinity antibodies and a dramatic loss of LLPCs. Influenza A infection revealed that αV integrin was not required for Tfh support of Bmem but was essential for Tfh support of LLPCs. We highlight an αV integrin-ECM-guided mechanism of Tfh GC accumulation that selectively impacts GC output of LLPCs but not Bmem.

Published

2019

7. Hyperspectral multiphoton microscopy for

Author

Amanda J, Bares, Menansili A, Mejooli, Mitchell A, Pender, Scott A, Leddon, Steven, Tilley, Karen, Lin, Jingyuan, Dong, Minsoo, Kim, Deborah J, Fowell, Nozomi, Nishimura, and Chris B, Schaffer

Subjects

Article

Abstract

The insensitivity of multiphoton microscopy to optical scattering enables high-resolution, high-contrast imaging deep into tissue, including in live animals. Scattering does, however, severely limit the use of spectral dispersion techniques to improve spectral resolution. In practice, this limited spectral resolution together with the need for multiple excitation wavelengths to excite different fluorophores limits multiphoton microscopy to imaging a few, spectrally-distinct fluorescent labels at a time, restricting the complexity of biological processes that can be studied. Here, we demonstrate a hyperspectral multiphoton microscope that utilizes three different wavelength excitation sources together with multiplexed fluorescence emission detection using angle-tuned bandpass filters. This microscope maintains scattering insensitivity, while providing high enough spectral resolution on the emitted fluorescence and capitalizing on the wavelength-dependent nonlinear excitation of fluorescent dyes to enable clean separation of multiple, spectrally overlapping labels, in vivo. We demonstrated the utility of this instrument for spectral separation of closely-overlapped fluorophores in samples containing ten different colors of fluorescent beads, live cells expressing up to seven different fluorescent protein fusion constructs, and in multiple in vivo preparations in mouse cortex and inflamed skin with up to eight different cell types or tissue structures distinguished.

Published

2021

8. CXCL10+ peripheral activation niches couple preferred sites of Th1 entry with optimal APC encounter

Author

Nilesh Patil, Deborah J. Fowell, Hen Prizant, Seble Negatu, Scott A Leddon, Alexandra M. Livingstone, Tristan D. McRae, Andrew D. Luster, Alexander McGurk, Yu-Rong Gao, Angela Hughson, and Joanna R Groom

Subjects

Chemokine, biology, Chemistry, Effector, T cell, CD11c, Inflammation, Extravasation, Cell biology, medicine.anatomical_structure, medicine, biology.protein, CXCL10, medicine.symptom, Antigen-presenting cell

Abstract

SUMMARYCorrect positioning of T cells within infected tissues is critical for T cell activation and pathogen control. Upon tissue entry, effector T cells must efficiently locate antigen presenting cells (APC) for peripheral activation. We reveal that tissue entry and initial peripheral activation of Th1 effector T cells are tightly linked to perivascular positioning of chemokine-expressing APCs. Dermal inflammation induced tissue-wide de novo generation of discrete perivascular CXCL10+ cell clusters, enriched for CD11c+MHC-II+ monocyte-derived dendritic cells. These chemokine clusters were ‘hot spots’ for both Th1 extravasation and activation in the inflamed skin. CXCR3-dependent Th1 localization to the cluster micro-environment prolonged T-APC interactions and boosted function. Both the frequency and range of these clusters were enhanced via a Th1-intrinsic, IFNγ-dependent positive feedback loop. Thus, the perivascular CXCL10+ clusters act as initial peripheral activation niches, optimizing controlled activation broadly throughout the tissue by coupling Th1 tissue entry with enhanced opportunities for Th1-APC encounter.

Published

2020

9. The CD28 Transmembrane Domain Contains an Essential Dimerization Motif

Author

David Oleksyn, Ryan Kelly, Kristin Abramo, Scott A Leddon, James H. Miller, and Margaret M. Fettis

Subjects

lcsh:Immunologic diseases. Allergy, 0301 basic medicine, CD28, CD3 Complex, T cell, Amino Acid Motifs, Immunology, knock-in mice, Mice, Transgenic, chemical and pharmacologic phenomena, Ectopic Gene Expression, Mice, 03 medical and health sciences, 0302 clinical medicine, CD28 Antigens, medicine, Animals, Humans, Position-Specific Scoring Matrices, Immunology and Allergy, Glycophorin, Protein Interaction Domains and Motifs, Amino Acid Sequence, Protein Dimerization, Conserved Sequence, Original Research, biology, Chemistry, Cell Membrane, hemic and immune systems, transmembrane domain, Ligand (biochemistry), Transmembrane protein, Cell biology, Transmembrane domain, 030104 developmental biology, medicine.anatomical_structure, CRISPR, protein dimerization, FRET, biology.protein, Ectopic expression, Protein Multimerization, Signal transduction, lcsh:RC581-607, Signal Transduction, 030215 immunology

Abstract

CD28 plays a critical role in regulating immune responses both by enhancing effector T cell activation and differentiation and controlling the development and function of regulatory T cells. CD28 is expressed at the cell surface as a disulfide linked homodimer that is thought to bind ligand monovalently. How ligand binding triggers CD28 to induce intracellular signaling as well as the proximal signaling pathways that are induced are not well-understood. In addition, recent data suggest inside-out signaling initiated by the T cell antigen receptor can enhance CD28 ligand binding, possibly by inducing a rearrangement of the CD28 dimer interface to allow for bivalent binding. To understand how possible conformational changes during ligand-induced receptor triggering and inside-out signaling are mediated, we examined the CD28 transmembrane domain. We identified an evolutionarily conserved YxxxxT motif that is shared with CTLA-4 and resembles the transmembrane dimerization motif within CD3ζ. We show that the CD28 transmembrane domain can drive protein dimerization in a bacterial expression system at levels equivalent to the well-known glycophorin A transmembrane dimerization motif. In addition, ectopic expression of the CD28 transmembrane domain into monomeric human CD25 can drive dimerization in murine T cells as detected by an increase in FRET by flow cytometry. Mutation of the polar YxxxxT motif to hydrophobic leucine residues (Y145L/T150L) attenuated CD28 transmembrane mediated dimerization in both the bacterial and mammalian assays. Introduction of the Y145L/T150L mutation of the CD28 transmembrane dimerization motif into the endogenous CD28 locus by CRISPR resulted in a dramatic loss in CD28 cell surface expression. These data suggest that under physiological conditions the YxxxxT dimerization motif within the CD28 transmembrane domain plays a critical role in the assembly and/or expression of stable CD28 dimers at the cell surface.

Published

2020

10. CXCL10

Author

Hen, Prizant, Nilesh, Patil, Seble, Negatu, Noor, Bala, Alexander, McGurk, Scott A, Leddon, Angela, Hughson, Tristan D, McRae, Yu-Rong, Gao, Alexandra M, Livingstone, Joanna R, Groom, Andrew D, Luster, and Deborah J, Fowell

Subjects

Inflammation, Receptors, CXCR3, Histocompatibility Antigens Class II, Antigen-Presenting Cells, Ear, Mice, Transgenic, Th1 Cells, Lymphocyte Activation, Chemokine CXCL10, Interferon-gamma, Mice, Antigens, CD, Animals, Humans, Antigens, Cell Aggregation, Skin

Abstract

Correct positioning of T cells within infected tissues is critical for T cell activation and pathogen control. Upon tissue entry, effector T cells must efficiently locate antigen-presenting cells (APC) for peripheral activation. We reveal that tissue entry and initial peripheral activation of Th1 effector T cells are tightly linked to perivascular positioning of chemokine-expressing APCs. Dermal inflammation induces tissue-wide de novo generation of discrete perivascular CXCL10

Published

2020

11. Pivotal role for α

Author

Dillon C, Schrock, Scott A, Leddon, Angela, Hughson, Jim, Miller, Adam, Lacy-Hulbert, and Deborah J, Fowell

Subjects

Mice, Inbred C57BL, Mice, PNAS Plus, Plasma Cells, Animals, T-Lymphocytes, Helper-Inducer, Integrin alphaV, Germinal Center, Extracellular Matrix

Abstract

CD4+ follicular helper T cells (Tfh) are essential for germinal center (GC) reactions in the lymph node that generate high-affinity, long-lived plasma cells (LLPCs). Temporal GC analysis suggests B memory cells (Bmem) are generated early, while LLPCs are generated late in the GC reaction. Distinct roles for Tfh at these temporally different stages are not yet clear. Tfh entry into the GC is highly dynamic and the signals that maintain Tfh within the GC for support of late LLPC production are poorly understood. The GC is marked by inflammation-induced presentation of specific ECM components. To determine if T cell recognition of these ECM components played a role in Tfh support of the GC, we immunized mice with a T cell-restricted deletion of the ECM-binding integrin α(V) (α(V)-CD4 cKO). T cell integrin α(V) deletion led to a striking defect in the number and size of the GCs following immunization with OVA protein in complete Freund’s adjuvant. The GC defect was not due to integrin α(V) deficiency impeding Tfh generation or follicle entry or the ability of α(V)-CD4 cKO Tfh to contact and support B cell activation. Instead, integrin α(V) was essential for T cell-intrinsic accumulation within the GC. Altered Tfh positioning resulted in lower-affinity antibodies and a dramatic loss of LLPCs. Influenza A infection revealed that α(V) integrin was not required for Tfh support of Bmem but was essential for Tfh support of LLPCs. We highlight an α(V) integrin–ECM-guided mechanism of Tfh GC accumulation that selectively impacts GC output of LLPCs but not Bmem.

Published

2019

12. Hyperspectral multiphoton microscopy for in vivo visualization of spectrally-overlapped fluorescent labels

Author

Steven Tilley, Jingyuan Dong, Nozomi Nishimura, Chris B. Schaffer, Amanda J. Bares, Scott A Leddon, Menansili A. Mejooli, Minsoo Kim, and Deborah J. Fowell

Subjects

Materials science, Microscope, Scattering, Quantitative Biology::Tissues and Organs, Physics::Medical Physics, Second-harmonic generation, Hyperspectral imaging, Fluorescence, Quantitative Biology::Cell Behavior, law.invention, Visualization, In vivo, law, Computer Science::Computer Vision and Pattern Recognition, Preclinical imaging, Biomedical engineering

Abstract

We constructed a hyperspectral multiphoton microscope (HMM) that enabled high spectral-resolution imaging deep into scattering samples and used this instrument for in vivo visualization of the behavior of multiple cell types after an injury.

Published

2019

13. The Integrin LFA-1 Controls T Follicular Helper Cell Generation and Maintenance

Author

Michael Elliot, Mifong Tam, Ghislaine Fontes, Mary M. Stevenson, Alexandre P. Meli, Stuart G. Tangye, André Ballesteros-Tato, Scott A Leddon, Irah L. King, Danielle T. Avery, Deborah J. Fowell, and James H. Miller

Subjects

0301 basic medicine, Cellular differentiation, Immunology, Integrin, Cell, chemical and pharmacologic phenomena, Biology, Lymphocyte Activation, Article, Mice, 03 medical and health sciences, 0302 clinical medicine, medicine, Animals, Humans, Immunology and Allergy, Lymphocyte function-associated antigen 1, Cells, Cultured, Effector, Germinal center, Cell Differentiation, T-Lymphocytes, Helper-Inducer, Germinal Center, Acquired immune system, Lymphocyte Function-Associated Antigen-1, Immunity, Humoral, Cell biology, Mice, Inbred C57BL, 030104 developmental biology, Infectious Diseases, medicine.anatomical_structure, Humoral immunity, Proto-Oncogene Proteins c-bcl-6, biology.protein, 030215 immunology

Abstract

T follicular helper (Tfh) cells are a CD4+ T cell subset critical for long-lived humoral immunity. We hypothesized that integrins play a decisive role in Tfh cell biology. Here we show that Tfh cells expressed a highly active form of leukocyte function-associated antigen-1 (LFA-1) that was required for their survival within the germinal center niche. In addition, LFA-1 promoted expression of Bcl-6, a transcriptional repressor critical for Tfh cell differentiation, and inhibition of LFA-1 abolished Tfh cell generation and prevented protective humoral immunity to intestinal helminth infection. Furthermore, we demonstrated that expression of Talin-1, an adaptor protein that regulates LFA-1 affinity, dictated Tfh versus Th2 effector cell differentiation. Collectively, our results define unique functions for LFA-1 in the Tfh cell effector program and suggest that integrin activity is important in lineage decision-making events in the adaptive immune system.

Published

2016

14. Hyperspectral multiphoton microscopy for in vivo visualization of multiple, spectrally overlapped fluorescent labels

Author

Jingyuan Dong, Scott A Leddon, Nozomi Nishimura, Karen Lin, Chris B. Schaffer, Menansili A. Mejooli, Deborah J. Fowell, Mitchell A. Pender, Minsoo Kim, Amanda J. Bares, and Steven Tilley

Subjects

Materials science, Microscope, Scattering, business.industry, Hyperspectral imaging, Fluorescence, Atomic and Molecular Physics, and Optics, Light scattering, Electronic, Optical and Magnetic Materials, law.invention, Wavelength, Optics, law, Dispersion (optics), Spectral resolution, business

Abstract

The insensitivity of multiphoton microscopy to optical scattering enables high-resolution, high-contrast imaging deep into tissue, including in live animals. Scattering does, however, severely limit the use of spectral dispersion techniques to improve spectral resolution. In practice, this limited spectral resolution together with the need for multiple excitation wavelengths to excite different fluorophores limits multiphoton microscopy to imaging a few, spectrally distinct fluorescent labels at a time, restricting the complexity of biological processes that can be studied. Here, we demonstrate a hyperspectral multiphoton microscope that utilizes three different wavelength excitation sources together with multiplexed fluorescence emission detection using angle-tuned bandpass filters. This microscope maintains scattering insensitivity, while providing high enough spectral resolution on the emitted fluorescence and capitalizing on the wavelength-dependent nonlinear excitation of fluorescent dyes to enable clean separation of multiple, spectrally overlapping labels, in vivo. We demonstrated the utility of this instrument for spectral separation of closely overlapped fluorophores in samples containing 10 different colors of fluorescent beads, live cells expressing up to seven different fluorescent protein fusion constructs, and in multiple in vivo preparations in mouse cortex and inflamed skin, with up to eight different cell types or tissue structures distinguished.

Published

2020

15. Generation of MHC class II–peptide ligands for CD4 T-cell allorecognition of MHC class II molecules

Author

Scott A Leddon and Andrea J. Sant

Subjects

CD4-Positive T-Lymphocytes, Models, Molecular, CD74, Protein Conformation, Receptors, Antigen, T-Cell, chemical and pharmacologic phenomena, Biology, Ligands, Major histocompatibility complex, Article, Structure-Activity Relationship, MHC class I, Animals, Humans, Immunology and Allergy, Protein Interaction Domains and Motifs, Allorecognition, Genetics, Transplantation, MHC class II, Antigen processing, Histocompatibility Antigens Class II, Transporter associated with antigen processing, MHC restriction, Cell biology, biology.protein

Abstract

The molecular and cellular mechanisms that underlie allorecognition of MHC class II molecules have been the subject of much debate and experimentation in recent decades. In this review, we discuss several aspects of MHC class II structure, peptide acquisition and TcR-MHC-peptide interactions that have particular relevance to recognition of cells bearing allogeneic class II molecules.First, MHC polymorphism is heavily biased toward those amino acids that influence stable peptide binding by MHC class II. Second, the peptide repertoire presented by class II molecules is highly diverse and can be edited substantially by the molecular catalyst HLA-DM and by tissue-specific expression of HLA-DO, stress and cytokines. Third, T-cell receptor docking onto MHC peptide consistently involves substantial contacts with the bound peptide in the MHC class II molecule. Finally, there is increasing evidence that T-cell recognition of MHC is, in part, germline encoded through T-cell-receptor V region contacts with MHC class II alpha helices.Together, these conclusions support the view that allorecognition of MHC class II molecules is likely to parallel key aspects of conventional CD4 T-cell recognition, with allele-dependent variation in peptide representation accounting in large part for the high precursor frequency of alloreactive CD4 T cells.

Published

2010

16. The Control of the Specificity of CD4 T Cell Responses: Thresholds, Breakpoints, and Ceilings

Author

Scott A Leddon, Jacqueline Tung, Andrea J. Sant, and Francisco A. Chaves

Subjects

lcsh:Immunologic diseases. Allergy, Mini Review, Immunology, CD4 T cells, Immunodominance, HLA-DM, Biology, Major histocompatibility complex, Epitope, 03 medical and health sciences, 0302 clinical medicine, Immune system, Antigen, Immunology and Allergy, Antigen-presenting cell, 030304 developmental biology, Genetics, 0303 health sciences, immunodominance, Immunoregulation, MHC restriction, 3. Good health, biology.protein, MHC, lcsh:RC581-607, 030215 immunology

Abstract

It has been known for over 25 years that CD4 T cell responses are restricted to a finite number of peptide epitopes within pathogens or protein vaccines. These selected peptide epitopes are termed “immunodominant.” Other peptides within the antigen that can bind to host MHC molecules and recruit CD4 T cells as single peptides are termed “cryptic” because they fail to induce responses when expressed in complex proteins or when in competition with other peptides during the immune response. In the last decade, our laboratory has evaluated the mechanisms that underlie the preferential specificity of CD4 T cells and have discovered that both intracellular events within antigen presenting cells, particular selective DM editing, and intercellular regulatory pathways, involving IFN-γ, indoleamine 2,3-dioxygenase, and regulatory T cells, play a role in selecting the final peptide specificity of CD4 T cells. In this review, we summarize our findings, discuss the implications of this work on responses to pathogens and vaccines and speculate on the logic of these regulatory events.

Published

2013

17. The CD28 Transmembrane Domain Contains an Essential Dimerization Motif

Author

Scott A. Leddon, Margaret M. Fettis, Kristin Abramo, Ryan Kelly, David Oleksyn, and Jim Miller

Subjects

CD28, transmembrane domain, protein dimerization, FRET, CRISPR, knock-in mice, Immunologic diseases. Allergy, RC581-607

Abstract

CD28 plays a critical role in regulating immune responses both by enhancing effector T cell activation and differentiation and controlling the development and function of regulatory T cells. CD28 is expressed at the cell surface as a disulfide linked homodimer that is thought to bind ligand monovalently. How ligand binding triggers CD28 to induce intracellular signaling as well as the proximal signaling pathways that are induced are not well-understood. In addition, recent data suggest inside-out signaling initiated by the T cell antigen receptor can enhance CD28 ligand binding, possibly by inducing a rearrangement of the CD28 dimer interface to allow for bivalent binding. To understand how possible conformational changes during ligand-induced receptor triggering and inside-out signaling are mediated, we examined the CD28 transmembrane domain. We identified an evolutionarily conserved YxxxxT motif that is shared with CTLA-4 and resembles the transmembrane dimerization motif within CD3ζ. We show that the CD28 transmembrane domain can drive protein dimerization in a bacterial expression system at levels equivalent to the well-known glycophorin A transmembrane dimerization motif. In addition, ectopic expression of the CD28 transmembrane domain into monomeric human CD25 can drive dimerization in murine T cells as detected by an increase in FRET by flow cytometry. Mutation of the polar YxxxxT motif to hydrophobic leucine residues (Y145L/T150L) attenuated CD28 transmembrane mediated dimerization in both the bacterial and mammalian assays. Introduction of the Y145L/T150L mutation of the CD28 transmembrane dimerization motif into the endogenous CD28 locus by CRISPR resulted in a dramatic loss in CD28 cell surface expression. These data suggest that under physiological conditions the YxxxxT dimerization motif within the CD28 transmembrane domain plays a critical role in the assembly and/or expression of stable CD28 dimers at the cell surface.

Published

2020