The document provides an overview of medical protozoa and fungi. It discusses the structures, life cycles, modes of transmission, and pathogenesis of protozoan parasites. Key protozoan groups covered include amoebas, flagellates, ciliates, and apicomplexans. The document also reviews fungal characteristics, morphologies such as yeasts and molds, dimorphism, reproductive cycles, and the polymorphic fungus Candida albicans.
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Infection and Immunity Exam 1: Study Guide
The document provides an overview of medical protozoa and fungi. It discusses the structures, life cycles, modes of transmission, and pathogenesis of protozoan parasites. Key protozoan groups covered include amoebas, flagellates, ciliates, and apicomplexans. The document also reviews fungal characteristics, morphologies such as yeasts and molds, dimorphism, reproductive cycles, and the polymorphic fungus Candida albicans.
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Infection and Immunity
Exam 1: Study Guide
Medical Protozoa: - Pathogenic protozoa o Plasmodium falciparum - Opportunistic parasites o Not normally pathogens o Become pathogenic due to impairment of host resistance o Clinical importance in the AIDS epidemic Cryptosporidium parvum - Basic Structures o Cytoplasm Ectoplasm: locomotion, ingestion Endoplasm: metabolism o Nuclear Vesicular or compact form o Locomotive organelle Pseudopodium, flagellum, cilia - Life Cycle Patterns o One stage Trophozoite Take food, mobile, multiply o Two-stage form Trophozoite and cyst Not mobile with cyst wall o Two-host form Mammals – mammals Mammals – insect vectors - Hosts for Parasites o Intermediate Eggs/early larva develop into next stage Larval or intermediate stages respectively o Trophozoite → Gametocyte o Definitive Larval stages mature into sexually mature adult parasites Gametocyte → Gametes → Zygote → Trophozoite o Reservoir Essential for survival of parasite Means of transmission to other organisms - Types of Vectors o Mechanical Transmits pathogen but not essential to its life cycle Housefly and E. coli o Biological Required for proper development of pathogen Anopheles mosquitoes and malaria - Parasite Pathogenesis o Exhibit wide range of pathogenic effects Typically do not have high virulence levels and may not replicate in host o Pathogenicity of parasites related to: Infectious dose of organism # of organisms acquired over time Chronic nature of most parasitic diseases Immunopathologic effects Invasion of host and attachment to host cells/tissues With damage thereof - Parasite Portals of Entry o Protozoan and helminthic infections almost always exogenous Entry into the host becomes critical event Most commonly used portals of entry: o Ingestion Contamination of food/water with human/animal waste Applicable to most parasitic organisms o Direct penetration Arthropod bites (typically protozoa) Transplacental penetration (limited) Organism-directed penetration (typically helminths) - Adherence and Replication of Parasites o Species and tissue tropisms usually important Nonspecific – mechanical process Specific – cell-surface molecules interact with adhesins on parasite’s surface A variety of cell-surface molecules useful to parasite o Glycoproteins (fibronectin, Duffy antigen, etc) o Complement receptors o Complement proteins - Cell and Tissue Damage from Parasites o Toxins produced not on same level as bacterial toxins o Damage results from: Degradative enzymes Proteases, phospholipases, etc Function as toxins Mechanical tissue damage Blockages o Intestinal, bile duct, blood or lymphatic vessels Migration through tissues Immunopathology Hypersensitivity Autoimmunity Carcinogenic effects from chronic inflammation Degradation of immunoglobulins by proteases - Groups of Medically Important Protozoa o Amoebas(Sarcodina) Amoeboid movement/pseudopodia Entamoeba, Acanthamoeba, and Naegleria o Flagellates (Mastigophora) Giardia, Trichomonas, Trypanosoma, and Leishmania o Ciliates (Ciliata) Balantidium coli o Apicomplexa (Sporozoans) Typically use TWO hosts Gliding motility Apical complex that facilitates entry into host cells Plasmodium, Toxoplasma, Pneumocystis, Cryptosporidium - Medically important Phyla and Organisms in the Kingdom Protozoa o Metamonada (flagellates) Giardia, Chilomastix o Parabasala (flagellates) Dientamoeba, Trichomonas o Euglenozoa (flagellates) Leishmania, Trypanosoma o Percolozoa (amoeba) Naegleria o Amoebozoa (amoebas) Acanthamoeba, Balamuthia, Entamoeba o Sporozoa (sporozoans/apicomplexans) Cryptosporidium, Cyclospora, Toxoplasma, Babesia, Plasmodium o Ciliophora (ciliates) Balantidium coli - General Characteristics of Protozoa o Single-cell eukaryotes o 2-100 μm in size o Motility important for classification/pathogenicity o Phagocytosis/pinocytosis OR simple diffusion (some cases) o Facultative anaerobes o Majority free-living and not pathogenic o Many can change surface antigens frequently Immunoevasive tactics - Reproduction in Protozoa o Asexual Simple binary fission Schizogony Nuclei repeatedly divide o Cytoplasm divides Nuclei separate Merogony if daughter cells merozoites Sporogony if daughter cells sporozoites Gametogony if daughter cells gametes o Sexual Syngamy Two cells fuse Conjugation - Protozoan Forms o Trophozoites Motile Feeding form Fragile Cannot live long outside body Rarely withstand stomach acid Noninfectious form mostly o Cysts (Diagnostic) Resting/dormant stage Infectious form Common in fecal-oral transmission Survive longer than trophozoites Survive exposure to stomach acid Protozoa without cyst form Transmitted by direct contact or arthropod vector only - Fungal Characteristics o Kingdom Fungi/Myceteae o Eukaryotic cells Cell wall: contains chitin and glucan Cell membrane: contains ergosterol o Lifestyles Saprobes, Symbionts, Commensal, Parasites o Most aerobic Facultative and strict anaerobes are possible as well o Produce primary and secondary metabolites Many extreme economic value o Very slow growth rates Generation times in hours (instead of minutes) - Fungal Morphologies o Yeasts Unicellular Budding or Fission reproduction Nuclear fission → two cells Budding → Ballistoconidia Pseudohyphae Germ tube → Pseudohyphae Important in pathogenic yeast (i.e. Candida albicans) o Molds Hyphae Grow by apical extension Coenocytic vs Septate o Septate = septum o Coenocytic = no septum o Septate hyphae with clamp connections Aerial vs Vegetative o The portion of the mycelium that anchors mold and absorbs nutrients is vegetative o Portion that produces asexual reproductive spores is aerial o Dimorphic Fungi Two morphologies In response to temperature or nutrient supply o Thermal dimorphism Typically yeast forms seen in human tissues Mold forms in the environment “Yeast beasts in body heat; bold mold in the cold” Blastomyces, Histoplasma, Coccidioides, and Sporothrix - Fungal Reproductive Life Cycles o Asexual and Sexual spores (majority) Anamorph = asexual spores Teleomorph = sexual spores o Rely mostly on anamorphic stage and minimize teleomorphic stage Asexual designations used in clinical setting Usually isolated from patient’s tissues Sexual stage is typically not seen clinically - Candida albicans: An exception to the rule o Polymorphic fungus can grow in several forms Primarily yeast, Pseudohyphae, and Hyphae o Pathogenicity: Ovoid-shaped budding yeast Important in spread of C. albicans Parallel-walled true hyphae More prevalent for infection Pseudohyphae Not well understood Intermediate form between yeast and hyphae - Lab Diagnosis of Fungal Disease o 10-20% KOH wet mount of skin scrapings Dissolves skin cells and leaves fungal cells Can be stained in same prep with fungal stains o India ink wet mount of CSF Detects capsule of Cryptococcus neoformans Not very sensitive (only about 50%) o Latex agglutination test for cryptococcal antigens more common Much more sensitive Particularly valuable for CSF from meningitis o Giemsa or Wright’s stain of blood Detection of intracellular Histoplasma capsulatum o Lactophenol cotton blue Quick and easy Stains chitin in fungal cell walls (Aspergillus sp.) o Calcofluor white Fluorescent stain Binds strongly to structures containing cellulose and chitin Cryptococcus neoformans o GMS (Gomori methenamine silver) Method of choice among silver stains for fungi o Fontana-Masson silver stain Specific stain for melanin Identification of dematiaceous fungi o Culture Time issues Temperature issues Growth media Tend to be more general purpose than bacterial growth media Sabouraud dextrose agar, potato dextrose agar, brain heart infusion agar with blood Antibacterial antibiotics frequently added to media to inhibit normal flora bacteria and environmental fungi that are possible contaminants o Gentamicin, chloramphenicol, cycloheximide - Fungal Pathogenesis o Only about 200 outright pathogens Mycoses o Many patients are at increased risk for opportunistic fungal infections: Immunocompromised patients Transplants AIDS Cancer chemotherapy Patients hospitalized with severe underlying conditions Diabetes Invasive procedures Severe burns o Few fungi considered primary pathogens Do not have necessary virulence factors NO endotoxin NO bacteria-like exotoxins o Fungi that qualify as primary pathogens have variety of virulence factors: Growth at 37oC Thermal dimorphism Immune response resistance Resistance to phagocytosis/survival inside phagocytes Alteration of cell wall composition Modulation of the host immune response o Dimorphism Yeast forms larger than conidia or hyphal fragments Harder to phagocytize Able to persist inside phagocytes Some hyphal fragments have cell walls with antiphagocytic properties o Modification of cell wall composition Removal of antigens needed for recognition by macrophages o Stimulation of the “wrong” kind of immune response Cell wall antigens that stimulate the TH2 response instead of TH1 TH2 is ineffective for immune control of (these particular) fungi o Usually makes infection worse - Resistance to antifungal agents o Develops slowly and generally uncommon o Resistance is NOT transmissible from cell to cell Unlike bacteria o Some of the same mechanisms are present as in bacteria Multidrug efflux pumps Target alterations Reduced drug target access - Antifungal Therapy o Good drug targets: Ergosterol and enzymes involved in production of its metabolic precursors Glucan-containing cell walls o Inhibition of protein synthesis Sordarins and Azasordarins o Cell wall inhibitors of: Glucan synthesis Echinocandins Chitin synthesis Nikkomycin o Cell membrane inhibitors of: Ergosterol synthesis Azoles Allylamines o Direct membrane damage Polyenes o Disruption of: Microtubules and inhibition of mitosis Griseofulvin o Inhibition of nucleic acid synthesis Flucytosine