Your search keyword '"Sia, Jonathan Kevin"' showing total 7 results

1. Mycobacterium tuberculosis impedes CD40-dependent notch signaling to restrict Th17 polarization during infection

Author

Enriquez, Ana Beatriz, Sia, Jonathan Kevin, Dkhar, Hedwin Kitdorlang, Goh, Shu Ling, Quezada, Melanie, Stallings, Kristina Larrieux, and Rengarajan, Jyothi

Published

2022

2. Innate Immune Defenses in Human Tuberculosis: An Overview of the Interactions between Mycobacterium tuberculosis and Innate Immune Cells

Author

Sia, Jonathan Kevin, Georgieva, Maria, and Rengarajan, Jyothi

Subjects

Article Subject, bacteria, chemical and pharmacologic phenomena, biochemical phenomena, metabolism, and nutrition, respiratory system, bacterial infections and mycoses

Abstract

Tuberculosis (TB) remains a serious global public health problem that results in up to 2 million deaths each year. TB is caused by the human pathogen, Mycobacterium tuberculosis (Mtb), which infects primarily innate immune cells patrolling the lung. Innate immune cells serve as barometers of the immune response against Mtb infection by determining the inflammatory milieu in the lungs and promoting the generation of adaptive immune responses. However, innate immune cells are also potential niches for bacterial replication and are readily manipulated by Mtb. Our understanding of the early interactions between Mtb and innate immune cells is limited, especially in the context of human infection. This review will focus on Mtb interactions with human macrophages, dendritic cells, neutrophils, and NK cells and detail evidence that Mtb modulation of these cells negatively impacts Mtb-specific immune responses. Furthermore, this review will emphasize important innate immune pathways uncovered through human immunogenetic studies. Insights into the human innate immune response to Mtb infection are necessary for providing a rational basis for the augmentation of immune responses against Mtb infection, especially with respect to the generation of effective anti-TB immunotherapeutics and vaccines.

Published

2015

3. Deletion of BCG Hip1 protease enhances dendritic cell and CD4 T cell responses.

Author

Bizzell, Erica, Sia, Jonathan Kevin, Quezada, Melanie, Enriquez, Ana, Georgieva, Maria, and Rengarajan, Jyothi

Subjects

T cells, DENDRITIC cells

Abstract

Abstract: Dendritic cells (DCs) play a key role in the generation of CD4 T cell responses to pathogens. Mycobacterium tuberculosis (Mtb) harbors immune evasion mechanisms that impair DC responses and prevent optimal CD4 T cell immunity. The vaccine strain Mycobacterium bovis Bacille Calmette‐Guérin (BCG) shares many of the immune evasion proteins utilized by Mtb, but the role of these proteins in DC and T cell responses elicited by BCG is poorly understood. We previously reported that the Mtb serine protease, Hip1, promotes sub‐optimal DC responses during infection. Here, we tested the hypothesis that BCG Hip1 modulates DC functions and prevents optimal antigen‐specific CD4 T cell responses that limit the immunogenicity of BCG. We generated a strain of BCG lacking hip1 (BCGΔhip1) and show that it has superior capacity to induce DC maturation and cytokine production compared with the parental BCG. Furthermore, BCGΔhip1‐infected DCs were more effective at driving the production of IFN‐γ and IL‐17 from antigen‐specific CD4 T cells in vitro. Mucosal transfer of BCGΔhip1‐infected DCs into mouse lungs induced robust CD4 T cell activation in vivo and generated antigen‐specific polyfunctional CD4 T cell responses in the lungs. Importantly, BCGΔhip1‐infected DCs enhanced control of pulmonary bacterial burden following Mtb aerosol challenge compared with the transfer of BCG‐infected DCs. These results reveal that BCG employs Hip1 to impair DC activation, leading to attenuated lung CD4 T cell responses with limited capacity to control Mtb burden after challenge. [ABSTRACT FROM AUTHOR]

Published

2018

4. Engaging the CD40-CD40L pathway augments T-helper cell responses and improves control of Mycobacterium tuberculosis infection.

Author

Sia, Jonathan Kevin, Bizzell, Erica, Madan-Lala, Ranjna, and Rengarajan, Jyothi

Subjects

*MYCOBACTERIUM tuberculosis, *TUBERCULOSIS prevention, *T helper cells, *DENDRITIC cells, *IMMUNE response

Abstract

Mycobacterium tuberculosis (Mtb) impairs dendritic cell (DC) functions and induces suboptimal antigen-specific CD4 T cell immune responses that are poorly protective. Mucosal T-helper cells producing IFN-γ (Th1) and IL-17 (Th17) are important for protecting against tuberculosis (TB), but the mechanisms by which DCs generate antigen-specific T-helper responses during Mtb infection are not well defined. We previously reported that Mtb impairs CD40 expression on DCs and restricts Th1 and Th17 responses. We now demonstrate that CD40-dependent costimulation is required to generate IL-17 responses to Mtb. CD40-deficient DCs were unable to induce antigen-specific IL-17 responses after Mtb infection despite the production of Th17-polarizing innate cytokines. Disrupting the interaction between CD40 on DCs and its ligand CD40L on antigen-specific CD4 T cells, genetically or via antibody blockade, significantly reduced antigen-specific IL-17 responses. Importantly, engaging CD40 on DCs with a multimeric CD40 agonist (CD40LT) enhanced antigen-specific IL-17 generation in ex vivo DC-T cell co-culture assays. Further, intratracheal instillation of Mtb-infected DCs treated with CD40LT significantly augmented antigen-specific Th17 responses in vivo in the lungs and lung-draining lymph nodes of mice. Finally, we show that boosting CD40-CD40L interactions promoted balanced Th1/Th17 responses in a setting of mucosal DC transfer, and conferred enhanced control of lung bacterial burdens following aerosol challenge with Mtb. Our results demonstrate that CD40 costimulation by DCs plays an important role in generating antigen-specific Th17 cells and targeting the CD40-CD40L pathway represents a novel strategy to improve adaptive immunity to TB. [ABSTRACT FROM AUTHOR]

Published

2017

5. Mycobacterium tuberculosis Impairs Dendritic Cell Functions through the Serine Hydrolase Hipl.

Author

Madan-Lala, Ranjna, Sia, Jonathan Kevin, King, Rebecca, Adekambi, Toidi, Monin, Leticia, Khader, Shabaana A., Pulendran, Bali, and Rengarajan, Jyothi

Subjects

*MYCOBACTERIUM tuberculosis, *MACROPHAGES, *DENDRITIC cells, *HYDROLASES, *INTERLEUKIN-12, *CD4 antigen

Abstract

Mycobacterium tuberculosis is a highly successful human pathogen that primarily resides in host phagocytes, such as macrophages and dendritic cells (DCs), and interferes with their functions. Although multiple strategies used by M. tuberculosis to modulate macrophage responses have been discovered, interactions between M. tuberculosis and DCs are less well understood. DCs are the primary APCs of the immune system and play a central role in linking innate and adaptive immune responses to microbial pathogens. In this study, we show that M. tuberculosis impairs DC cytokine secretion, maturation, and Ag presentation through the cell envelope-associated serine hydrolase, Hip1. Compared to wild-type, a hip1 mutant strain of M. tuberculosis induced enhanced levels of the key Th1-inducing cytokine IL-12, as well as other proinflammatory cytokines (IL-23, IL-6, TNF-α, IL-1β, and IL-18) in DCs via MyD88- and TLR2/9-dependent pathways, indicating that Hip1 restricts optimal DC inflammatory responses. Infection with the hip1 mutant also induced higher levels of MHC class II and costimulatory molecules CD40 and CD86, indicating that M. tuberculosis impairs DC maturation through Hip1. Further, we show that M. tuberculosis promotes suboptimal Ag presentation, as DCs infected with the hip1 mutant showed increased capacity to present Ag to OT-II- and early secreted antigenic target 6-specific transgenic CD4 T cells and enhanced Th1 and Th17 polarization. Overall, these data show that M. tuberculosis impairs DC functions and modulates the nature of Ag-specific T cell responses, with important implications for vaccination strategies. [ABSTRACT FROM AUTHOR]

Published

2014

6. Immunology of Mycobacterium tuberculosis Infections.

Author

Sia JK and Rengarajan J

Subjects

Adaptive Immunity, Animals, Granuloma diagnosis, Granuloma immunology, Granuloma microbiology, Humans, Immune Evasion, Immunity, Innate, Mycobacterium tuberculosis genetics, Mycobacterium tuberculosis immunology, Tuberculosis diagnosis, Mycobacterium tuberculosis physiology, Tuberculosis immunology, Tuberculosis microbiology

Abstract

Tuberculosis (TB) is a serious global public health challenge that results in significant morbidity and mortality worldwide. TB is caused by infection with the bacilli Mycobacterium tuberculosis ( M. tuberculosis ), which has evolved a wide variety of strategies in order to thrive within its host. Understanding the complex interactions between M. tuberculosis and host immunity can inform the rational design of better TB vaccines and therapeutics. This chapter covers innate and adaptive immunity against M. tuberculosis infection, including insights on bacterial immune evasion and subversion garnered from animal models of infection and human studies. In addition, this chapter discusses the immunology of the TB granuloma, TB diagnostics, and TB comorbidities. Finally, this chapter provides a broad overview of the current TB vaccine pipeline.

Published

2019

7. Mycobacterium tuberculosis GroEL2 Modulates Dendritic Cell Responses.

Author

Georgieva M, Sia JK, Bizzell E, Madan-Lala R, and Rengarajan J

Subjects

Animals, Cytokines metabolism, Disease Models, Animal, Mice, Inbred C57BL, Proteolysis, Tuberculosis microbiology, Chaperonin 60 metabolism, Dendritic Cells immunology, Host-Pathogen Interactions, Immune Evasion, Mycobacterium tuberculosis immunology, Tuberculosis pathology

Abstract

Mycobacterium tuberculosis successfully subverts the host immune response to promote disease progression. In addition to its known intracellular niche in macrophages, M. tuberculosis interferes with the functions of dendritic cells (DCs), which are the primary antigen-presenting cells of the immune system. We previously showed that M. tuberculosis dampens proinflammatory responses and impairs DC functions through the cell envelope-associated serine protease Hip1. Here we present data showing that M. tuberculosis GroEL2, a substrate of Hip1, modulates DC functions. The full-length GroEL2 protein elicited robust proinflammatory responses from DCs and promoted DC maturation and antigen presentation to T cells. In contrast, the cleaved form of GroEL2, which predominates in M. tuberculosis , was poorly immunostimulatory and was unable to promote DC maturation and antigen presentation. Moreover, DCs exposed to full-length, but not cleaved, GroEL2 induced strong antigen-specific gamma interferon (IFN-γ), interleukin-2 (IL-2), and IL-17A cytokine responses from CD4 + T cells. Moreover, the expression of cleaved GroEL2 in the hip1 mutant restored the robust T cell responses to wild-type levels, suggesting that proteolytic cleavage of GroEL2 allows M. tuberculosis to prevent optimal DC-T cell cross talk during M. tuberculosis infection., (Copyright © 2018 American Society for Microbiology.)

Published

2018