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chapter 24 viruses associated with respiratory infections Department of pathogenic biology xie-shuixiang 1 ORTHOMYXOVIRUSES • pleomorphic • influenza types A,B,C • febrile, respiratory illness with systemic symptoms 2 ‘FLU’ • True influenza – influenza virus A or influenza virus B (or influenza virus C infections - much milder) • Febrile respiratory disease with systemic symptoms caused by a variety of other organisms often called ‘flu’ 3 THE IMPACT OF INFLUENZA PANDEMICS Deaths: 1918-19 Spanish flu 500,000 US 20,000,000 world 1957-58 Asian flu 70,000 US 1968-69 Hong Kong 34,000 US flu 4 INFLUENZA VIRUS 5 Composition of Influenza Virus 1.Core RNA: -ssRNA, 8 fragments NP (nucleoprotein) RNA dependent RNA polymerase 2. envelope M protein lipid envelope sipke hemagglutinin(HA) 5 neuraminidase(NA) 1 6 HA - hemagglutinin NA - neuraminidase helical nucleocapsid (RNA plus NP protein) lipid bilayer membrane polymerase complex M1 protein type A, B, C : NP, M1 protein sub-types: HA or NA protein 7 Nomenclature Host of origin geographical origin strain number parentheses antigenic description of HA and NA e.g. A/swine/Iowa/3/70(H1N1) A/Hong Kong/1/68(H3N2) 8 Functions of Hemagglutinin • HA causes agglutination of red blood cells. • Viruses bind to the mucous membrane cells by HA1 interacting with membrane receptor. • Virus’ envelope fuse with cell membrane by HA2 forming a fusion pore. 9 HA protein - attachment, fusion S S S S S S cell enzymes acid pH 10 11 Functions of Neuraminidase • NA help the virus to permeate mucin and escape from “non-specific”inhibitor. • NA can increase the number of free virus particles, hence more virus spread from the original site of infection. • NA is important in the final stages of release of the new virus particle from infected cells. 12 NA protein - neuraminidase 13 ANTIGENIC DRIFT • Minor changes in antigens due to gene mutation in influenza virus. • HA and NA accumulate mutations – RNA virus • immune response no longer protects fully • sporadic outbreaks, limited epidemics 14 15 ANTIGENIC SHIFT • Major changes in antigens due to gene reassortment in influenza virus. • “new” HA or NA proteins • pre-existing antibodies do not protect • may get pandemics 16 17 INFLUENZA A PANDEMICS Ryan et al., in Sherris Medical Microbiology 18 where do “new” HA and NA come from? • 15 types HA • 9 types NA – all circulate in birds • pigs – avian and human 19 where do “new” HA and NA come from? 20 why do we not have influenza B pandemics? • so far no shifts have been recorded • no animal reservoir known 21 TRANSMISSION • AEROSOL – 100,000 TO 1,000,000 VIRIONS PER DROPLET • 18-72 HR INCUBATION • SHEDDING 22 • DECREASED CLEARANCE • RISK BACTERIAL INFECTION • VIREMIA RARE 23 Lycke and Norrby Textbook of Medical Virology 1983 RECOVERY • INTERFERON - SIDE EFFECTS INCLUDE: – FEVER, MYALGIA, FATIGUE, MALAISE • CELL-MEDIATED IMMUNE RESPONSE • TISSUE REPAIR – CAN TAKE SOME TIME 24 INTERFERON 25 INTERFERON antiviral state antiviral state antiviral state antiviral state 26 INTERFERON antiviral state antiviral state antiviral state antiviral state 27 INTERFERON antiviral state antiviral state antiviral state antiviral state 28 PROTECTION AGAINST RE-INFECTION • IgG and IgA – IgG less efficient but lasts longer • antibodies to both HA and NA important – antibody to HA more important (can neutralize) 29 SYMPTOMS • FEVER • HEADACHE • MYALGIA • COUGH • RHINITIS • OCULAR SYMPTOMS 30 CLINICAL FINDINGS • SEVERITY – VERY YOUNG – ELDERLY – IMMUNOCOMPROMISED – HEART OR LUNG DISEASE 31 PULMONARY COMPLICATIONS • CROUP (YOUNG CHILDREN) • PRIMARY INFLUENZA VIRUS PNEUMONIA • SECONDARY BACTERIAL INFECTION – Streptococcus pneumoniae – Staphlyococcus aureus – Hemophilus influenzae 32 DIAGNOSIS • ISOLATION – NOSE, THROAT SWAB – TISSUE CULTURE OR EGGS • SEROLOGY • RAPID TESTS • provisional - clinical picture + outbreak 33 VACCINE • ‘BEST GUESS’ OF MAIN ANTIGENIC TYPES – CURRENTLY • type A - H1N1 • type A - H3N2 • type B • each year choose which variant of each subtype is the best to use for optimal protection 34 VACCINE • inactivated • egg grown • sub-unit vaccine for children • reassortant live vaccine approved 2003 – for healthy persons (those not at risk for complications from influenza infection) ages 5-49 years 35 live vaccine development adapted from 36 Treanor JJ Infect. Med. 15:714 TREATMENT - DRUGS • RIMANTADINE (M2) • AMANTADINE (M2) • type A only, needs to be given early • type A only, needs to be given early • ZANAMIVIR (NA) • types A and B, needs to be given early • OSELTAMIVIR (NA) • types A and B, needs to be given early 37 NA protein - neuraminidase . . . . . . . . . . .. ... . . . . 38 OTHER TREATMENT • REST, LIQUIDS, ANTI-FEBRILE AGENTS (NO ASPIRIN FOR AGES 6MTHS-18YRS) • BE AWARE OF COMPLICATIONS AND TREAT APPROPRIATELY 39 CORONA VIRUSES COLDS AND SARS 40 Severe acute respiratory syndrome (SARS) 41 SARS Coronavirus, SARS CoV • Severe Acute Respiratory Syndrome(SARS) • 2002/11 42 SARS symtom • Droplet or osculation • Latent period:2~12d,usually4~5d • Centralization in family and hospital apparently 43 Biological properties • 60-130nm,envelope with spikes • +ssRNA,29.7KB,14 ORF:RNA polymer- ase、 S、E、M、N • Vero cell--CPE • Infected quadrumana – typical SARS symptom 44 SARS Genome 45 Transmission and Epidemiology 46 Chinese SARS epidemiology 47 48 Diagnosis • Mainly depend on the clinic and epidemiologic data • Pathogen diagnosis – Isolation and identification of virus – RT-PCR – Immunofluorescence、ELISA • P3 laboratory • Pathogen diagnosis is immature 49 Prevention • SARS CoV比普通CoV抵抗力强,室温下痰、 粪便、尿中可稳定存活1~2d • 对温度敏感,37oC存活4d,56oC存活90m, 75oC30m • 对含氯消毒剂、过氧乙酸及UV均敏感, • WHO推荐中效以上的消毒剂,如过氧乙酸 50 51 52 53 54 Pathologic cytoarchitectural changes indicative of diffuse alveolar damage, as well as a multinucleated giant cell with no conspicuous viral inclusions. 55 56 Paramyxoviridae -ssRNA 57 measles (rubeola) Koplik's spots on mucosal membranes Maculopapular rash (extends from face to extremities) 58 Measles virus measles (rubeola) 59 SUB-ACUTE SCLEROSING PANENCEPHALITIS (SSPE) • • • • Very rarely (7 in 1,000,000 cases) 1-10 years after initial infection. progressive, fatal disease. defective forms of the virus in the brain 60 Lab Diagnosis Histopathology of measles pneumonia. Giant cells. 61 Prevention MMR • (mumps, measles, rubella) vaccine contains live, attenuated forms of all three of these viruses. 62 MUMPS VIRUS Mumps • British "to mump" - to • grimace or grin, from the appearance of the patient as a result of parotid gland swelling. (Note: Other agents can also cause parotitis). 63 • very contagious 64 RESPIRATORY SYNCYTIAL VIRUS spherical or pleomorphic enveloped viruses (100-350 nm) with single-stranded, negative sense linear RNA 65 • Upper respiratory infection (‘bad cold’) in older children and adults • Lower respiratory • Infection of cells results in syncytium formation infection- Bronchiolitis and/or pneumonia may occur after the upper respiratory infection • Severe infections occur in infants (2-6m) 66 Others 67 ADENOVIRUS • non-enveloped • linear double-stranded (ds) • • DNA Icosahedral capsid, capsomeres hexons; at the vertices are 12 pentons, from which a fiber with a terminal knob projects. This complex is toxic to cells causing rounding and death of cells through inhibition of protein synthesis. 68 • Eye • • • Epidemic Keratoconjunctivitis (EKC), acute follicular conjunctivitis, pharyngoconjunctival fever Respiratory system Common cold (rhinitis), pharyngitis (with or without fever), tonsillitis, bronchitis, pharyngoconjunctival fever, acute respiratory disease (LRI) Genitourinary Acute hemorrhagic cystitis Gastrointestinal Gastroenteritis. 69 RUBELLA cataracts Rash Congenital rubella 70 RUBELLA (GERMAN MEASLES) VIRUS • Togavirus • +ssRNA • Fetal damage • live vaccine (attenuated strain) 71