Toxoplasma Gondii Host Interactions: A Story of Immune Attack and Parasite Counterattack

Toxoplasma Gondii Host Interactions: A Story of Immune Attack and Parasite Counterattack
Author: Jeroen P. J. Saeij
Publisher: Frontiers Media SA
Total Pages: 233
Release: 2020-08-10
Genre:
ISBN: 2889634027

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Toxoplasma gondii is an obligate intracellular parasite that can infect all warm-blooded animals, including an estimated ~30% of humans. It can cause severe disease in immune-suppressed individuals and in fetuses as well as blinding chorioretinitis in adults and children. Toxoplasma-innate immune system interactions determine early parasite control and activation of the adaptive immune system by the host and are therefore critical in determining host survival during the acute phase of infection. However, induction of an exaggerated inflammatory response can also lead to pathology. Only the chronic tissue cyst form of Toxoplasma is orally infectious. It is therefore critical for the parasite’s survival during the chronic phase to escape immune responses at this stage as well. Toxoplasma exists as genetically divergent strains mostly depending on geography, with the most strain diversity being found in South America. The key to Toxoplasma’s successful co-option of the host are proteins secreted from its rhoptry and dense granule secretory organelles. Rhoptry proteins (ROPs) are secreted into the host cell cytoplasm upon invasion while dense granule proteins (GRAs) are secreted once the parasite establishes itself in its parasitophorous vacuole (PV). GRAs can localize to the PV, the PV membrane, or are secreted beyond the PVM into the host cytoplasm. Many ROPs and GRAs are involved in modulating host cell signaling pathways and evasion of host immune responses and play important roles in Toxoplasma virulence. Polymorphisms in Toxoplasma’s ROPs and GRAs, likely determine how well these effectors bind to the divergent substrates in different host species, which can explain Toxoplasma strain differences in virulence in a particular host species. By studying Toxoplasma we have not only started to unravel how the parasite modulates immune responses to enhance its survival, replication, and transmission but we have also learned a lot about the immune system. Many unique mechanisms of immunity have indeed been defined using Toxoplasma and this parasite has aided our understanding of tissue-specific immune responses in the brain and intestine. This Research Topic will give a comprehensive overview of Toxoplasma-host immune response interactions. Most Toxoplasma virulence determinants to date have been established in murine systems and it is unclear how the parasite interacts with other intermediate hosts and humans. In addition, the interactions of Toxoplasma with some of the most relevant cell types during infection, including dendritic cells, neurons, intestinal epithelial cells or vascular endothelial cells, remain poorly understood.

Toxoplasma gondii

Toxoplasma gondii
Author: Uwe Gross
Publisher: Springer Science & Business Media
Total Pages: 268
Release: 2012-12-06
Genre: Medical
ISBN: 3642510140

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For years, toxoplasmosis has been known as disease mostly affecting newborns. Since immunocompromised patients (AIDS) present a high risk of reactivation of chronic toxoplasmosis this parasitic disease has gained increasing interest. Besides presenting clinical and therapeutical concepts, this volume provides current knowledge about genetics and immunology of T. gondii and the interaction with its 'host'. Since in vivo and in vitro models of toxoplasmosis exist, and genetic manipulation has become possible, this protozoan parasite has recently been accepted as a model for understanding the pathogenesis and persistance of other intracellular parasites. The articles of the book compromise both reviewing current concepts and reporting on yet unpublished results of leading scientists in this field.

Elucidating Toxoplasma Gondii's Engagement with the Host

Elucidating Toxoplasma Gondii's Engagement with the Host
Author: Anjali Joshi Shastri
Publisher:
Total Pages:
Release: 2013
Genre:
ISBN:

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The ubiquitous parasite Toxoplasma gondii has developed an exquisite arsenal of effectors to support its intracellular lifestyle and its persistence within its diverse hosts. In order to survive and resist clearance, this obligate intracellular parasite must contend with the host immune response. Different strains of the parasite vary dramatically in their interaction with the immune system, and studying these strain differences has furthered our understanding of the spectrum of host-pathogen interactions and led to the identification of parasite effectors. The work described here dissects the interactions between different strains of the parasite and host macrophages: innate immune cells that paradoxically both serve as a niche for parasite replication and defend the host against parasite infection. Chapter 1 introduces Toxoplasma, the immune response to infection, and discusses the role of known parasite effectors. Experiments described in Chapter 2 identify a novel secreted parasite factor, GRA25, which modulates cytokine secretion in macrophages and controls parasite virulence in mice. In Chapter 3, high throughput methods are used to characterize the transcriptional and phosphorylation landscape of macrophages infected with different Toxoplasma strains. These analyses demonstrate that a secreted polymorphic tyrosine kinase, ROP16, directs murine macrophage polarization towards an alternatively activated phenotype. They also reveal that Toxoplasma parasites activate the Type I interferon response, a response classically associated with cytosolic pathogens. Chapter 4 describes work demonstrating that Toxoplasma strain-specifically modulates the innate immune response via secretion of a parasite factor, MAF1, which recruits host mitochondria to the parasitophorous vacuole. Finally, Chapter 5 discusses the future directions and implications of this work in the broader context of host-pathogen interactions.

The Role of Novel Toxoplasma Dense Granule Proteins in Establishing Infection and Modulating Host Interactions

The Role of Novel Toxoplasma Dense Granule Proteins in Establishing Infection and Modulating Host Interactions
Author: Amara Thind
Publisher:
Total Pages: 0
Release: 2023
Genre:
ISBN:

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Toxoplasma gondii is an obligate intracellular parasite that can infect any warm-blooded mammal, making it one of the most successful parasites in the world. It is estimated to infect approximately one-third of the global human population and can cause life threatening complications in immunocompromised individuals and congenitally infected neonates. During the acute infection, rapidly multiplying T. gondii tachyzoites must balance between avoiding clearance to ensure the infection and limiting parasite replication to avoid killing the host. While most tachyzoites are eliminated during the acute infection by the host's immune response, a fraction converts into slow growing bradyzoites that are encased by a cyst wall that constitute the chronic infection. These infectious tissue cysts remain largely undetected from the host's immune surveillance.The ability of T. gondii to survive intracellularly and establish a productive infection relies significantly on its capacity to regulate host cell functions. One way the parasite achieves this is through the secretion of dense granule proteins (GRAs) that are involved in remodeling the parasitophorous vacuole (PV), obtaining nutrients from the host, manipulating the host cell cycle, and modulating the immune response. Because of their diverse functions during infection, the goal of this work is to identify and characterize novel GRAs in the acute and chronic infection to better understand the array of effectors this parasite uses to colonize its mammalian hosts. This work first describes a proximity labeling experiment to identify several novel T. gondii GRAs, GRA55-59, that are expressed in bradyzoites. Deletion of these GRAs does not affect parasite fitness in vitro. Further characterization of GRA55 reveals that its deletion does not impact virulence during the acute infection but does reduce brain cyst burden in infected mice. This suggests that GRA55 is an important secreted protein for the establishment or maintenance of the chronic infection in mice. The next section identifies the dense granule protein GRA83 and reveals that this effector is secreted into the PV and plays a role in modulating a key element of the host's innate immune response. Disruption of GRA83 impacts proinflammatory cytokine production and increases T. gondii's virulence during the acute infection. This also results in a significantly higher brain cyst burden during the chronic infection in mice. Therefore, this effector functions in a pro-host manner to limit unrestricted parasite growth. Lastly, this work describes the novel secreted effector, GRA84, that is exported to the host cell nucleus. GRA84 is dependent on the aspartyl protease (ASP5) and the MYR translocon to traverse the PV barrier and reach the host cell nucleus. Disruption of GRA84 does not substantially impact in vitro parasite growth or the chronic infection in mice. Most interestingly, this work demonstrates that GRA84 is proteolytically cleaved for maturation in its N-terminus and that this processing event is essential its ability to translocate across the vacuolar membrane to reach its destination in the host nucleus. Together, this thesis identifies and characterizes an array of novel GRA proteins that regulate Toxoplasma infection, which is likely to aid in the development of new treatments or therapeutics that can ultimately clear this widespread human infection.

Unraveling Host and Parasite Pathways in Human Innate Immunity to Toxoplasma Gondii

Unraveling Host and Parasite Pathways in Human Innate Immunity to Toxoplasma Gondii
Author: Lanny Gov
Publisher:
Total Pages: 125
Release: 2014
Genre:
ISBN: 9781321448405

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Toxoplasma gondii is a pathogen of global importance. Innate immunity is critical for control of acute infection. In vivo mouse models have shown that monocytes are rapidly recruited to sites of T. gondii infection and MCP-1 and CCR2 knock-out mice that fail to do so succumb to infection, underscoring the importance of monocytes in host defense. However, the role of human monocytes in immunity to T. gondii and their specific interactions with T. gondii are not well understood. Human monocytes are actively infected by T. gondii and permissive to parasite replication. Infected human monocytes release interleukin-1beta (IL-1beta), a "master regulator" of inflammation that has been shown to be protective against T. gondii in vivo. However, the host and parasite factors regulating T. gondii-induced IL-1beta production in human monocytes were unknown. We found that T. gondii induces IL-1beta transcript, post-translational processing, and release from human monocytes. We demonstrate a role for host inflammasome components caspase-1 and ASC and the parasite protein GRA15 in the induction and release of IL-1beta. This work provides important mechanistic insight into the regulation of a key mediator of inflammation and is the first to identify a T. gondii factor that drives innate immune responses in human cells. Recently, there has been increasing appreciation for the heterogeneity of circulating monocytes. Three phenotypically and functionally distinct subpopulations have been defined in humans based on CD14 and CD16 expression. However, the interactions of specific monocyte subsets with T. gondii and their functional outcomes have not been elucidated. We found that T. gondii preferentially invades classical (CD14+CD16-) and intermediate (CD14+CD16+) monocytes and that these subsets are more permissive to intracellular parasite survival. All monocyte subsets were capable of phagocytosing and degrading Mycalolide B-treated parasites. T. gondii infection induces IL-1beta in all three monocyte subsets, but the resident monocytes (CD14loCD16+) showed an enhanced IL-1beta response. These data suggest that resident monocytes are less permissive to infection and may play a critical role in parasite control. Collectively, our work defines host and parasite pathways driving innate immunity and contributes to a better understanding of the role of human monocytes in parasite control.

Essential Immunology

Essential Immunology
Author: Ivan Maurice Roitt
Publisher:
Total Pages: 244
Release: 1971
Genre: Immunity
ISBN:

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Metabolic Interaction in Infection

Metabolic Interaction in Infection
Author: Ricardo Silvestre
Publisher: Springer
Total Pages: 478
Release: 2018-04-06
Genre: Science
ISBN: 3319749323

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This book focuses on host–pathogen interactions at the metabolic level. It explores the metabolic requirements of the infectious agents, the microbial metabolic pathways that are dedicated to circumvent host immune mechanisms as well as the molecular mechanisms by which pathogens hijack host cell metabolism for their own benefit. Finally, it provides insights on the possible clinical and immunotherapeutic applications, as well as on the available experimental and analytical methods. The contributions break new ground in understanding the metabolic crosstalk between host and pathogen.

Parasitology

Parasitology
Author: Eric Loker
Publisher: Garland Science
Total Pages: 577
Release: 2015-03-02
Genre: Medical
ISBN: 1317407725

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Parasitology: A Conceptual Approach focuses on the conceptual basis of parasitology, with the goal of providing students with an enriched view of parasites and their biology. Concentrating on concepts will enable readers to gain a broader perspective that will increase their ability to think critically about all kinds of parasitic associations. The interfaces between the study of parasitism and prominent biological disciplines such as biodiversity, immunology, ecology, evolution, conservation biology, and disease control are highlighted. Studying individual parasites is an essential part of parasitology so Parasitology: A Conceptual Approach contains an appendix which provides a concise overview of the biology of important human and veterinary parasites. End-of-chapter questions are provided, as is an instructor manual.

The Rapture of the Nerds

The Rapture of the Nerds
Author: Cory Doctorow
Publisher: Macmillan
Total Pages: 353
Release: 2012-09-04
Genre: Fiction
ISBN: 0765329107

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From the two defining personalities of post-cyberpunk SF, a brilliant collaboration to rival 1987's The Difference Engine by William Gibson and Bruce Sterling

The Emperor of All Maladies

The Emperor of All Maladies
Author: Siddhartha Mukherjee
Publisher: Simon and Schuster
Total Pages: 624
Release: 2011-08-09
Genre: Health & Fitness
ISBN: 1439170916

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Winner of the Pulitzer Prize and a documentary from Ken Burns on PBS, this New York Times bestseller is “an extraordinary achievement” (The New Yorker)—a magnificent, profoundly humane “biography” of cancer—from its first documented appearances thousands of years ago through the epic battles in the twentieth century to cure, control, and conquer it to a radical new understanding of its essence. Physician, researcher, and award-winning science writer, Siddhartha Mukherjee examines cancer with a cellular biologist’s precision, a historian’s perspective, and a biographer’s passion. The result is an astonishingly lucid and eloquent chronicle of a disease humans have lived with—and perished from—for more than five thousand years. The story of cancer is a story of human ingenuity, resilience, and perseverance, but also of hubris, paternalism, and misperception. Mukherjee recounts centuries of discoveries, setbacks, victories, and deaths, told through the eyes of his predecessors and peers, training their wits against an infinitely resourceful adversary that, just three decades ago, was thought to be easily vanquished in an all-out “war against cancer.” The book reads like a literary thriller with cancer as the protagonist. Riveting, urgent, and surprising, The Emperor of All Maladies provides a fascinating glimpse into the future of cancer treatments. It is an illuminating book that provides hope and clarity to those seeking to demystify cancer.