XB-ART-56392
Front Immunol
2018 Sep 12;9:2536. doi: 10.3389/fimmu.2018.02536.
Show Gene links
Show Anatomy links
Review of the Amphibian Immune Response to Chytridiomycosis, and Future Directions.
Grogan LF
,
Robert J
,
Berger L
,
Skerratt LF
,
Scheele BC
,
Castley JG
,
Newell DA
,
McCallum HI
.
???displayArticle.abstract???
The fungal skin disease, chytridiomycosis (caused by Batrachochytrium dendrobatidis and B. salamandrivorans), has caused amphibian declines and extinctions globally since its emergence. Characterizing the host immune response to chytridiomycosis has been a focus of study with the aim of disease mitigation. However, many aspects of the innate and adaptive arms of this response are still poorly understood, likely due to the wide range of species' responses to infection. In this paper we provide an overview of expected immunological responses (with inference based on amphibian and mammalian immunology), together with a synthesis of current knowledge about these responses for the amphibian-chytridiomycosis system. We structure our review around four key immune stages: (1) the naïve immunocompetent state, (2) immune defenses that are always present (constitutive defenses), (3) mechanisms for recognition of a pathogen threat and innate immune defenses, and (4) adaptive immune responses. We also evaluate the current hot topics of immunosuppression and immunopathology in chytridiomycosis, and discuss their respective roles in pathogenesis. Our synthesis reveals that susceptibility to chytridiomycosis is likely to be multifactorial. Susceptible amphibians appear to have ineffective constitutive and innate defenses, and a late-stage response characterized by immunopathology and Bd-induced suppression of lymphocyte responses. Overall, we identify substantial gaps in current knowledge, particularly concerning the entire innate immune response (mechanisms of initial pathogen detection and possible immunoevasion by Bd, degree of activation and efficacy of the innate immune response, the unexpected absence of innate leukocyte infiltration, and the cause and role of late-stage immunopathology in pathogenesis). There are also gaps concerning most of the adaptive immune system (the relative importance of B and T cell responses for pathogen clearance, the capacity and extent of immunological memory, and specific mechanisms of pathogen-induced immunosuppression). Improving our capacity for amphibian immunological research will require selection of an appropriate Bd-susceptible model species, the development of taxon-specific affinity reagents and cell lines for functional assays, and the application of a suite of conventional and emerging immunological methods. Despite current knowledge gaps, immunological research remains a promising avenue for amphibian conservation management.
???displayArticle.pubmedLink??? 30473694
???displayArticle.pmcLink??? PMC6237969
???displayArticle.link??? Front Immunol
???displayArticle.grants??? [+]
R24 AI059830 NIAID NIH HHS
???attribute.lit??? ???displayArticles.show???
|
|
|
Figure 1. Amphibian host immunity schematic, depicting a histological section through the skin and progressive infection stages with Bd. The inference of the main cellular components is based on mammalian immunology and an expected “normal” immune response (including the expected response to vaccination). (A) Normal skin: Layers of uninfected frog skin epidermis including, from deepest to most superficial, the basal lamina, stratum germinativum, stratum spinosum, stratum granulosum, stratum corneum and the superficial mucus layer. Two immune surveillance cells are illustrated within the epidermis, an immune dendritic cell (homologous to Langerhans cell), and a dendritic epidermal T cell (dETC). Within the dermis is a capillary with the nucleated red blood cells of amphibians. An example complement of naïve B and T lymphocytes are depicted waiting quiescent in the spleen, illustrated schematically as the lower band on the figure (please note that the spleen is a separate organ and does not lie adjacent to the dermis in living amphibians). (B) Early infection: Expected immune mechanisms upon initial exposure to Bd, assuming constitutive defenses (such as AMPs and bacteria) are insufficient. Zoospores are illustrated penetrating the mucus layer, and early thalli with zoosporangia developing are illustrated inside deeper host cells. In a normal immune response, pathogen recognition should lead to the infiltration of innate immune cells, illustrated here to include macrophages and granulocytes (such as neutrophils). (C) Intermediate infection: Expected response at an intermediate stage of infection includes the recognition of antigens by dendritic cells that then differentiate into antigen presenting cells and migrate to the spleen enabling antigen-specific selection of lymphocytes. Simultaneously, membrane-bound immunoglobulin on naïve B lymphocytes is exposed to extracellular Bd antigens (transported via the blood circulatory and lymphatic systems). With the assistance of T helper cells, these B cells are activated to respond to infection. (D) Late infection: The late adaptive response involves lymphocyte clonal expansion, differentiation into plasma cells and activated T cells (including cytotoxic and helper T cells), as well as the production of antibodies by plasma cells. (E) Recovery: If the frog is cleared of infection (perhaps by topical antifungals or heat), the skin might be expected to return to normal, however, a cohort of selected memory lymphocytes should remain. (F) Re-exposure: If the frog is then later re-exposed to Bd, the memory lymphocytes (produced during the previous clonal expansion) are then activated and induced to replicate and differentiate, leading to a much more rapid and effective adaptive immune response on re-exposure. This is the concept of immunization (vaccination). |
|
Figure 1. Amphibian host immunity schematic, depicting a histological section through the skin and progressive infection stages with Bd. The inference of the main cellular components is based on mammalian immunology and an expected “normal” immune response (including the expected response to vaccination). (A) Normal skin: Layers of uninfected frog skin epidermis including, from deepest to most superficial, the basal lamina, stratum germinativum, stratum spinosum, stratum granulosum, stratum corneum and the superficial mucus layer. Two immune surveillance cells are illustrated within the epidermis, an immune dendritic cell (homologous to Langerhans cell), and a dendritic epidermal T cell (dETC). Within the dermis is a capillary with the nucleated red blood cells of amphibians. An example complement of naïve B and T lymphocytes are depicted waiting quiescent in the spleen, illustrated schematically as the lower band on the figure (please note that the spleen is a separate organ and does not lie adjacent to the dermis in living amphibians). (B) Early infection: Expected immune mechanisms upon initial exposure to Bd, assuming constitutive defenses (such as AMPs and bacteria) are insufficient. Zoospores are illustrated penetrating the mucus layer, and early thalli with zoosporangia developing are illustrated inside deeper host cells. In a normal immune response, pathogen recognition should lead to the infiltration of innate immune cells, illustrated here to include macrophages and granulocytes (such as neutrophils). (C) Intermediate infection: Expected response at an intermediate stage of infection includes the recognition of antigens by dendritic cells that then differentiate into antigen presenting cells and migrate to the spleen enabling antigen-specific selection of lymphocytes. Simultaneously, membrane-bound immunoglobulin on naïve B lymphocytes is exposed to extracellular Bd antigens (transported via the blood circulatory and lymphatic systems). With the assistance of T helper cells, these B cells are activated to respond to infection. (D) Late infection: The late adaptive response involves lymphocyte clonal expansion, differentiation into plasma cells and activated T cells (including cytotoxic and helper T cells), as well as the production of antibodies by plasma cells. (E) Recovery: If the frog is cleared of infection (perhaps by topical antifungals or heat), the skin might be expected to return to normal, however, a cohort of selected memory lymphocytes should remain. (F) Re-exposure: If the frog is then later re-exposed to Bd, the memory lymphocytes (produced during the previous clonal expansion) are then activated and induced to replicate and differentiate, leading to a much more rapid and effective adaptive immune response on re-exposure. This is the concept of immunization (vaccination). |
References [+] :
Anil,
Impact of lysozyme and lactoferrin on oral Candida isolates exposed to polyene antimycotics and fluconazole.
2002, Pubmed
Anil, Impact of lysozyme and lactoferrin on oral Candida isolates exposed to polyene antimycotics and fluconazole. 2002, Pubmed
Antonovics, Transmission dynamics: critical questions and challenges. 2017, Pubmed
Bataille, Susceptibility of amphibians to chytridiomycosis is associated with MHC class II conformation. 2015, Pubmed
Bates, Amphibian chytridiomycosis outbreak dynamics are linked with host skin bacterial community structure. 2018, Pubmed
Becker, Towards a better understanding of the use of probiotics for preventing chytridiomycosis in Panamanian golden frogs. 2011, Pubmed
Becker, Composition of symbiotic bacteria predicts survival in Panamanian golden frogs infected with a lethal fungus. 2015, Pubmed
Bell, Screening bacterial metabolites for inhibitory effects against Batrachochytrium dendrobatidis using a spectrophotometric assay. 2013, Pubmed
Berger, Chytridiomycosis causes amphibian mortality associated with population declines in the rain forests of Australia and Central America. 1998, Pubmed
Berger, Effect of season and temperature on mortality in amphibians due to chytridiomycosis. 2004, Pubmed
Berger, Life cycle stages of the amphibian chytrid Batrachochytrium dendrobatidis. 2005, Pubmed
Berger, Distribution of Batrachochytrium dendrobatidis and pathology in the skin of green tree frogs Litoria caerulea with severe chytridiomycosis. 2005, Pubmed
Bletz, Mitigating amphibian chytridiomycosis with bioaugmentation: characteristics of effective probiotics and strategies for their selection and use. 2013, Pubmed
Bletz, Estimating Herd Immunity to Amphibian Chytridiomycosis in Madagascar Based on the Defensive Function of Amphibian Skin Bacteria. 2017, Pubmed
Boltaña, Behavioural fever is a synergic signal amplifying the innate immune response. 2013, Pubmed
Bouvet, Diversity of antibody-mediated immunity at the mucosal barrier. 1999, Pubmed
Brannelly, Epidermal cell death in frogs with chytridiomycosis. 2017, Pubmed
Carrillo-Farga, Langerhans-like cells in amphibian epidermis. 1990, Pubmed
Cashins, Prior infection does not improve survival against the amphibian disease Chytridiomycosis. 2013, Pubmed
Chai, Fungal strategies for overcoming host innate immune response. 2009, Pubmed
Clarke, The natural history of amphibian skin secretions, their normal functioning and potential medical applications. 1997, Pubmed
Colombo, Microbiota and mucosal immunity in amphibians. 2015, Pubmed , Xenbase
Conlon, Purification and characterization of antimicrobial peptides from the skin secretions of the carpenter frog Rana virgatipes (Ranidae, Aquarana). 2005, Pubmed
Conlon, The contribution of skin antimicrobial peptides to the system of innate immunity in anurans. 2011, Pubmed
Conlon, A family of brevinin-2 peptides with potent activity against Pseudomonas aeruginosa from the skin of the Hokkaido frog, Rana pirica. 2004, Pubmed
Cramp, First line of defence: the role of sloughing in the regulation of cutaneous microbes in frogs. 2014, Pubmed
Cunha, DAMP signaling in fungal infections and diseases. 2012, Pubmed
Daum, Hybrid advantage in skin peptide immune defenses of water frogs (Pelophylax esculentus) at risk from emerging pathogens. 2012, Pubmed
Dhabhar, Stress-induced changes in blood leukocyte distribution. Role of adrenal steroid hormones. 1996, Pubmed
Du Pasquier, Expression of MHC class II antigens during Xenopus development. 1990, Pubmed , Xenbase
Du Pasquier, The immune system of Xenopus. 1989, Pubmed , Xenbase
Du Pasquier, B-cell development in the amphibian Xenopus. 2000, Pubmed , Xenbase
Du Pasquier, Antibody diversity in lower vertebrates--why is it so restricted? 1982, Pubmed
Edholm, Evolution of innate-like T cells and their selection by MHC class I-like molecules. 2016, Pubmed , Xenbase
Edholm, Distinct MHC class I-like interacting invariant T cell lineage at the forefront of mycobacterial immunity uncovered in Xenopus. 2018, Pubmed , Xenbase
Edholm, Unusual evolutionary conservation and further species-specific adaptations of a large family of nonclassical MHC class Ib genes across different degrees of genome ploidy in the amphibian subfamily Xenopodinae. 2014, Pubmed , Xenbase
Ellison, Fighting a losing battle: vigorous immune response countered by pathogen suppression of host defenses in the chytridiomycosis-susceptible frog Atelopus zeteki. 2014, Pubmed
Ellison, More than skin deep: functional genomic basis for resistance to amphibian chytridiomycosis. 2014, Pubmed
Eskew, Gene expression differs in susceptible and resistant amphibians exposed to Batrachochytrium dendrobatidis. 2018, Pubmed
Fisher, Global emergence of Batrachochytrium dendrobatidis and amphibian chytridiomycosis in space, time, and host. 2009, Pubmed
Fites, Inhibition of local immune responses by the frog-killing fungus Batrachochytrium dendrobatidis. 2014, Pubmed , Xenbase
Fites, The invasive chytrid fungus of amphibians paralyzes lymphocyte responses. 2013, Pubmed , Xenbase
Fitzgerald, Mal (MyD88-adapter-like) is required for Toll-like receptor-4 signal transduction. 2001, Pubmed , Xenbase
Flajnik, Changes in the immune system during metamorphosis of Xenopus. 1987, Pubmed , Xenbase
Flajnik, Comparative analyses of immunoglobulin genes: surprises and portents. 2002, Pubmed
Flechas, Surviving chytridiomycosis: differential anti-Batrachochytrium dendrobatidis activity in bacterial isolates from three lowland species of Atelopus. 2012, Pubmed
Fonner, Effects of corticosterone on infection and disease in salamanders exposed to the amphibian fungal pathogen Batrachochytrium dendrobatidis. 2017, Pubmed
Fu, Major histocompatibility complex variation and the evolution of resistance to amphibian chytridiomycosis. 2017, Pubmed
Fujita, Primitive complement system--recognition and activation. 2004, Pubmed
Gabor, A non-invasive stress assay shows that tadpole populations infected with Batrachochytrium dendrobatidis have elevated corticosterone levels. 2013, Pubmed
Gabor, Elevated Corticosterone Levels and Changes in Amphibian Behavior Are Associated with Batrachochytrium dendrobatidis (Bd) Infection and Bd Lineage. 2015, Pubmed
Gabor, Are the adverse effects of stressors on amphibians mediated by their effects on stress hormones? 2018, Pubmed
Gantress, Development and characterization of a model system to study amphibian immune responses to iridoviruses. 2003, Pubmed , Xenbase
Garmyn, Waterfowl: potential environmental reservoirs of the chytrid fungus Batrachochytrium dendrobatidis. 2012, Pubmed
Goyos, Remarkable conservation of distinct nonclassical MHC class I lineages in divergent amphibian species. 2011, Pubmed , Xenbase
Graham, Non-invasive monitoring of glucocorticoid physiology within highland and lowland populations of native Australian Great Barred Frog (Mixophyes fasciolatus). 2013, Pubmed
Greenspan, Host invasion by Batrachochytrium dendrobatidis: fungal and epidermal ultrastructure in model anurans. 2012, Pubmed
Grogan, Evolution of resistance to chytridiomycosis is associated with a robust early immune response. 2018, Pubmed
Grogan, Endemicity of chytridiomycosis features pathogen overdispersion. 2016, Pubmed
Grogan, Chytridiomycosis causes catastrophic organism-wide metabolic dysregulation including profound failure of cellular energy pathways. 2018, Pubmed
Harris, Skin microbes on frogs prevent morbidity and mortality caused by a lethal skin fungus. 2009, Pubmed
Holden, Development of antimicrobial peptide defenses of southern leopard frogs, Rana sphenocephala, against the pathogenic chytrid fungus, Batrachochytrium dendrobatidis. 2015, Pubmed
Hsu, Mutation, selection, and memory in B lymphocytes of exothermic vertebrates. 1998, Pubmed , Xenbase
Ishii, Phylogenetic and expression analysis of amphibian Xenopus Toll-like receptors. 2007, Pubmed , Xenbase
Kindermann, Urinary corticosterone metabolites and chytridiomycosis disease prevalence in a free-living population of male Stony Creek frogs (Litoria wilcoxii). 2012, Pubmed
King, Pentadactylin: an antimicrobial peptide from the skin secretions of the South American bullfrog Leptodactylus pentadactylus. 2005, Pubmed
Kosch, Major histocompatibility complex selection dynamics in pathogen-infected túngara frog (Physalaemus pustulosus) populations. 2016, Pubmed
König, The diversity and evolution of anuran skin peptides. 2015, Pubmed
Lam, Motile zoospores of Batrachochytrium dendrobatidis move away from antifungal metabolites produced by amphibian skin bacteria. 2011, Pubmed
Li, B lymphocytes from early vertebrates have potent phagocytic and microbicidal abilities. 2006, Pubmed , Xenbase
Lips, Overview of chytrid emergence and impacts on amphibians. 2016, Pubmed , Xenbase
Luquet, Genetic erosion in wild populations makes resistance to a pathogen more costly. 2012, Pubmed
Mangoni, The synthesis of antimicrobial peptides in the skin of Rana esculenta is stimulated by microorganisms. 2001, Pubmed
Maniero, Generation of a long-lasting, protective, and neutralizing antibody response to the ranavirus FV3 by the frog Xenopus. 2006, Pubmed , Xenbase
Maniero, Phylogenetic conservation of gp96-mediated antigen-specific cellular immunity: new evidence from adoptive cell transfer in xenopus. 2004, Pubmed , Xenbase
Mao, Pathogenic fungus Microsporum canis activates the NLRP3 inflammasome. 2014, Pubmed
Marr, Localization and differential expression of activation-induced cytidine deaminase in the amphibian Xenopus upon antigen stimulation and during early development. 2007, Pubmed , Xenbase
Martel, Batrachochytrium salamandrivorans sp. nov. causes lethal chytridiomycosis in amphibians. 2013, Pubmed
Martel, Wildlife disease. Recent introduction of a chytrid fungus endangers Western Palearctic salamanders. 2014, Pubmed
McKnight, The compatibility of Xenopus antibody and homoiothermic complement. 1987, Pubmed , Xenbase
McMahon, Transition of chytrid fungus infection from mouthparts to hind limbs during amphibian metamorphosis. 2015, Pubmed
McMahon, Amphibians acquire resistance to live and dead fungus overcoming fungal immunosuppression. 2014, Pubmed
Mescher, Cells of cutaneous immunity in Xenopus: studies during larval development and limb regeneration. 2007, Pubmed , Xenbase
Meyer, Changes in cutaneous microbial abundance with sloughing: possible implications for infection and disease in amphibians. 2012, Pubmed
Meyer, How selection shapes variation of the human major histocompatibility complex: a review. 2001, Pubmed
Moss, Chemotaxis of the amphibian pathogen Batrachochytrium dendrobatidis and its response to a variety of attractants. 2008, Pubmed
Murphy, Temperature, hydric environment, and prior pathogen exposure alter the experimental severity of chytridiomycosis in boreal toads. 2011, Pubmed
Myers, Synergistic inhibition of the lethal fungal pathogen Batrachochytrium dendrobatidis: the combined effect of symbiotic bacterial metabolites and antimicrobial peptides of the frog Rana muscosa. 2012, Pubmed
Neely, "Double-duty" conventional dendritic cells in the amphibian Xenopus as the prototype for antigen presentation to B cells. 2018, Pubmed , Xenbase
Newell, Population recovery following decline in an endangered stream-breeding frog (Mixophyes fleayi) from subtropical Australia. 2013, Pubmed
Nichols, Experimental transmission of cutaneous chytridiomycosis in dendrobatid frogs. 2001, Pubmed
Nicolas, Peptides as weapons against microorganisms in the chemical defense system of vertebrates. 1995, Pubmed
O'Hanlon, Recent Asian origin of chytrid fungi causing global amphibian declines. 2018, Pubmed
Ohmer, Skin sloughing in susceptible and resistant amphibians regulates infection with a fungal pathogen. 2017, Pubmed
Ohta, IgD, like IgM, is a primordial immunoglobulin class perpetuated in most jawed vertebrates. 2006, Pubmed , Xenbase
Ostrovsky, Frog lysozyme. I. Its identification, occurrence as isozymes, and quantitative distribution in tissues of the leopard frog, Rana pipiens. 1976, Pubmed
Pask, Skin peptides protect juvenile leopard frogs (Rana pipiens) against chytridiomycosis. 2013, Pubmed
Patin, Pattern recognition receptors in fungal immunity. 2019, Pubmed
Pessier, Cutaneous chytridiomycosis in poison dart frogs (Dendrobates spp.) and White's tree frogs (Litoria caerulea). 1999, Pubmed
Peterson, Host stress response is important for the pathogenesis of the deadly amphibian disease, Chytridiomycosis, in Litoria caerulea. 2013, Pubmed
Phillott, Chytridiomycosis and seasonal mortality of tropical stream-associated frogs 15 years after introduction of Batrachochytrium dendrobatidis. 2013, Pubmed
Pilla-Moffett, Interferon-Inducible GTPases in Host Resistance, Inflammation and Disease. 2016, Pubmed
Piovia-Scott, Greater Species Richness of Bacterial Skin Symbionts Better Suppresses the Amphibian Fungal Pathogen Batrachochytrium Dendrobatidis. 2017, Pubmed
Plato, Pattern recognition receptors in antifungal immunity. 2015, Pubmed
Poorten, Comparative study of host response to chytridiomycosis in a susceptible and a resistant toad species. 2016, Pubmed
Price, A de novo Assembly of the Common Frog (Rana temporaria) Transcriptome and Comparison of Transcription Following Exposure to Ranavirus and Batrachochytrium dendrobatidis. 2015, Pubmed
Rachowicz, Transmission of Batrachochytrium dendrobatidis within and between amphibian life stages. 2004, Pubmed
Ramsey, Immune defenses against Batrachochytrium dendrobatidis, a fungus linked to global amphibian declines, in the South African clawed frog, Xenopus laevis. 2010, Pubmed , Xenbase
Rebollar, Using "Omics" and Integrated Multi-Omics Approaches to Guide Probiotic Selection to Mitigate Chytridiomycosis and Other Emerging Infectious Diseases. 2016, Pubmed
Rebollar, Skin bacterial diversity of Panamanian frogs is associated with host susceptibility and presence of Batrachochytrium dendrobatidis. 2016, Pubmed
Rebollar, Direct and Indirect Horizontal Transmission of the Antifungal Probiotic Bacterium Janthinobacterium lividum on Green Frog (Lithobates clamitans) Tadpoles. 2016, Pubmed
Reeve, Natural stressors and ranavirus susceptibility in larval wood frogs (Rana sylvatica). 2013, Pubmed
Ribas, Expression profiling the temperature-dependent amphibian response to infection by Batrachochytrium dendrobatidis. 2009, Pubmed , Xenbase
Richards-Zawacki, Thermoregulatory behaviour affects prevalence of chytrid fungal infection in a wild population of Panamanian golden frogs. 2010, Pubmed
Ricklin, Complement component C3 - The "Swiss Army Knife" of innate immunity and host defense. 2016, Pubmed
Robbins, Prevention of the spread of rabies to wildlife by oral vaccination of raccoons in Massachusetts. 1998, Pubmed
Robert, Minor histocompatibility antigen-specific MHC-restricted CD8 T cell responses elicited by heat shock proteins. 2002, Pubmed , Xenbase
Robert, Comparative and developmental study of the immune system in Xenopus. 2009, Pubmed , Xenbase
Robert, Frog's DCs have it all in one. 2018, Pubmed , Xenbase
Rollins-Smith, Immune defenses of Xenopus laevis against Batrachochytrium dendrobatidis. 2009, Pubmed , Xenbase
Rollins-Smith, Metamorphosis and the amphibian immune system. 1998, Pubmed
Rollins-Smith, The role of amphibian antimicrobial peptides in protection of amphibians from pathogens linked to global amphibian declines. 2009, Pubmed
Rollins-Smith, Amphibian immune defenses against chytridiomycosis: impacts of changing environments. 2011, Pubmed
Rollins-Smith, Antimicrobial peptide defenses of the mountain yellow-legged frog (Rana muscosa). 2006, Pubmed
Rollins-Smith, Amphibian immunity-stress, disease, and climate change. 2017, Pubmed , Xenbase
Rollins-Smith, Immunomodulatory metabolites released by the frog-killing fungus Batrachochytrium dendrobatidis. 2015, Pubmed , Xenbase
Rosenblum, Only skin deep: shared genetic response to the deadly chytrid fungus in susceptible frog species. 2012, Pubmed , Xenbase
Rosenblum, Genome-wide transcriptional response of Silurana (Xenopus) tropicalis to infection with the deadly chytrid fungus. 2009, Pubmed , Xenbase
Savage, Adaptive tolerance to a pathogenic fungus drives major histocompatibility complex evolution in natural amphibian populations. 2016, Pubmed
Savage, MHC genotypes associate with resistance to a frog-killing fungus. 2011, Pubmed
Scheele, High adult mortality in disease-challenged frog populations increases vulnerability to drought. 2016, Pubmed
Scheele, Interventions for reducing extinction risk in chytridiomycosis-threatened amphibians. 2014, Pubmed
Scheele, Reservoir-host amplification of disease impact in an endangered amphibian. 2017, Pubmed
Schwinger, Structural and mechanical aspects of the skin of Bufo marinus (Anura, Amphibia). 2001, Pubmed
Searle, Stress and chytridiomycosis: exogenous exposure to corticosterone does not alter amphibian susceptibility to a fungal pathogen. 2014, Pubmed
Speth, Complement and fungal pathogens: an update. 2008, Pubmed
Stice, Immunization is ineffective at preventing infection and mortality due to the amphibian chytrid fungus Batrachochytrium dendrobatidis. 2010, Pubmed
Takeuchi, Pattern recognition receptors and inflammation. 2010, Pubmed
Tam, Intracellular sensing of complement C3 activates cell autonomous immunity. 2014, Pubmed
Tatiersky, Effect of glucocorticoids on expression of cutaneous antimicrobial peptides in northern leopard frogs (Lithobates pipiens). 2015, Pubmed
Teacher, Evidence for directional selection at a novel major histocompatibility class I marker in wild common frogs (Rana temporaria) exposed to a viral pathogen (Ranavirus). 2009, Pubmed , Xenbase
Thekkiniath, A novel subtilisin-like serine protease of Batrachochytrium dendrobatidis is induced by thyroid hormone and degrades antimicrobial peptides. 2013, Pubmed
Van Rooij, Amphibian chytridiomycosis: a review with focus on fungus-host interactions. 2015, Pubmed
Van Rooij, Germ tube mediated invasion of Batrachochytrium dendrobatidis in amphibian skin is host dependent. 2012, Pubmed , Xenbase
Vas, Fundamental roles of the innate-like repertoire of natural antibodies in immune homeostasis. 2013, Pubmed
Venesky, Selecting for tolerance against pathogens and herbivores to enhance success of reintroduction and translocation. 2012, Pubmed
Venesky, Dietary protein restriction impairs growth, immunity, and disease resistance in southern leopard frog tadpoles. 2012, Pubmed
Voyles, Temperature alters reproductive life history patterns in Batrachochytrium dendrobatidis, a lethal pathogen associated with the global loss of amphibians. 2012, Pubmed
Voyles, Shifts in disease dynamics in a tropical amphibian assemblage are not due to pathogen attenuation. 2018, Pubmed
Voyles, Pathogenesis of chytridiomycosis, a cause of catastrophic amphibian declines. 2009, Pubmed
Walke, Harnessing the Microbiome to Prevent Fungal Infections: Lessons from Amphibians. 2016, Pubmed
Wilson, What limits affinity maturation of antibodies in Xenopus--the rate of somatic mutation or the ability to select mutants? 1992, Pubmed , Xenbase
Woodhams, Prodigiosin, Violacein, and Volatile Organic Compounds Produced by Widespread Cutaneous Bacteria of Amphibians Can Inhibit Two Batrachochytrium Fungal Pathogens. 2018, Pubmed
Woodhams, Chytridiomycosis and amphibian population declines continue to spread eastward in Panama. 2008, Pubmed
Woodhams, Predicted disease susceptibility in a Panamanian amphibian assemblage based on skin peptide defenses. 2006, Pubmed , Xenbase
Woodhams, Tolerance of fungal infection in European water frogs exposed to Batrachochytrium dendrobatidis after experimental reduction of innate immune defenses. 2012, Pubmed
Woodhams, Population trends associated with skin peptide defenses against chytridiomycosis in Australian frogs. 2006, Pubmed
Woodhams, Immune evasion or avoidance: fungal skin infection linked to reduced defence peptides in Australian green-eyed treefrogs, Litoria serrata. 2012, Pubmed
Woodhams, Life-history trade-offs influence disease in changing climates: strategies of an amphibian pathogen. 2008, Pubmed
Woods, Knocking on the right door and making a comfortable home: Histoplasma capsulatum intracellular pathogenesis. 2003, Pubmed
Woods, Human lysozyme has fungicidal activity against nasal fungi. 2011, Pubmed
Wu, Alpha-Ketoglutarate: Physiological Functions and Applications. 2016, Pubmed
Young, Defects in host immune function in tree frogs with chronic chytridiomycosis. 2014, Pubmed
Zhao, Identification of IgF, a hinge-region-containing Ig class, and IgD in Xenopus tropicalis. 2006, Pubmed , Xenbase
Zhao, Purification of a lysozyme from skin secretions of Bufo andrewsi. 2006, Pubmed