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Haemophilus, Brucella and Bordetella

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Title: Haemophilus, Brucella and Bordetella

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Haemophilus, Brucella and Bordetella
Dr. Brian OConnell
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Parvobacteria
Haemophilus influenzae Invasive disease - meningitis, bacteraemia, osteomyelitis Non-invasive disease respiratory tract.
Bordetella pertussis Whooping Cough
Brucella spp. Brucellosis
Yersinia spp. Diarrhoea and systemic disease
Pasteurella Wound infection after dog/cat bites
Francisella Tularaemia
Legionella Pneumonia
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Parvobacteria
Gram stain of Haemophilus influenzae
Gram stain of E. coli
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H. influenzae

Small, non-sporing, non-motile bacterium
Encapsulated strains isolated from cerebrospinal
fluid are gram-negative coccobacilli
Non encapsulated organisms from sputum are
pleomorphic
Requires preformed growth factors that are
present in blood, specifically
X factor (i.e., hemin from iron containing
pigments)
V factor (NAD or NADP).
Usually grown on chocolate blood agar

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Gram stain of H. influenzae from a CSF
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Gram stain of H. influenzae from sputum
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Epidemiology
Only found in humans
Normally found in the pharynx (conjunctiva,
genital tract)
Spread by airborne droplets or direct contact
with respiratory secretions
Both extra and intracellular pathogen

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Virulence and Immunity

Some strains are encapsulated with
polyribosylribitolphosphate (PRP)
Subdivides H. influenzae into groups a-f
Type B is a major virulence factor
95 percent of bloodstream and meningeal
Haemophilus infections in children are caused by
type B organisms
Encapsulated organisms penetrate the epithelium
of the nasopharynx and invade the blood
capillaries directly
Resist phagocytosis and complement-mediated lysis
in the the nonimmune host

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The age incidence of H. influenzae meningitis is
inversely proportional to the titre of
bactericidal antibody in the blood
Passively acquired from the mother or actively
formed
In children aged 2 months to 3 years, antibody
levels are minimal

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Relation of the age incidence of bacterial
meningitis caused by Haemophilus influenzae to
bactericidal antibody titres in the blood
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Clinical Manifestations- invasive disease

Hib
Bacteraemia
Meningitis
No particular features to distinguish HiB
meningitis from other causes
May be fulminant but usually presents with
several days of mild URTI followed by
deterioration
Mortality lt5 but neurologic sequelae are common
Septic arthritis
Previously common in children lt2 years
Single weight-bearing joint

Epiglottitis
Acute respiratory obstruction caused by
cellulitis of supraglottic tissues
Usually children aged between 2 and 7 but also
occasionally occurs in adults
Sore throat, fever, pooling of secretions,
restless, anxious, sitting in characteristic
position sitting up, tongue sticking out,
drooling, inspiratory stridor

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Epiglottitis in an adult
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Cellulitis
Reddish-blue hue, typically on cheek

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Haemophilus influenzae type b periorbital
cellulitis
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Clinical manifestations- mucosal disease

Non-typable H. influenzae
Otitis media
Sinusitis
Conjunctivitis
Exacerbations of COPD
Pneumonia
Especially in elderly with pre-existing lung
disease

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Laboratory Diagnosis

Gram stain
Pleomorphic gram-negative coccobacilli
Culture
Chocolate agar
Confirm by growth around X and V discs

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Treatment

Hib
Third-generation cephalosporin e.g. cefotaxime
until susceptibility confirmed
Between 5 and 20 of strains produce ?-lactamase
Non-typable strains
Amoxicillin, co-amoxyclav

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Prevention

HiB vaccine introduced in Ireland in 1992
Scheduled doses at 2, 4 and 6 months
Uptake gt90
Still about 40 cases/year
6 true vaccine failures (TVF) in 2004, 11 in
2005 (Fitzgerald et al. 2005)
Introduction of booster dose at 12-15 months in
2008

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Haemophilus influenzae Type B Disease by Age
Group 1987 to 2005
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One true vaccine failures in 2010.
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Bordetella pertussis

Gram-negative coccobacillus
Nutritionally fastidious, normally cultivated on
medium containing blood
Primarily a human pathogen
Other members of the genus Bordetella can cause
disease in animals
Causes Pertussis (Whooping cough)
Serious, highly communicable acute
tracheobronchitis

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Whooping cough - Epidemiology

Estimated 285,000 deaths in 2001 worldwide
Cases in Ireland
8296 cases in U.S.
Previously mainly in children
Now a number of reports of increasing pertussis
in adults because of the limited duration of
protection from pertussis vaccine

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Data from HPSC
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Virulence factors

4 important steps in development of disease
attachment, (2) evasion of host defenses, (3)
local damage, and (4) systemic manifestations
Filamentous Hemagglutinin (Fha)
ability to agglutinate RBCs
Binds to galactose on sulfated glycolipids (in
membranes of ciliated cells)
Antibodies to Fha protect against infection
Pertussis Toxin (PT)
may act as an adhesin and toxin
Two toxin subunits (S2 and S3) mediate adherence
Anti-Pt-antibody prevents colonization of
ciliated cells, protects vs infection

Adenylate cyclase toxin (ACT)
Mainly cell-associated, can be released
activated adenylate cyclase leads to impaired
white cell function
Tracheal cytotoxin (TCT)
Peptidoglycan fragment
Released by lysis
Kills ciliated cells
Stimulates release of IL-1 (produces fever)
Dermonecrotic toxin (DNT)
Causes smooth muscle contraction leading to
ischaemic necrosis

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Pathogenesis
Attachment to respiratory epithelium mediated by
FHA and possibly PT
Ciliostatsis and damage to epithelium mediated by
TCT
Inhibition of phagocytsosis mediated by ACT, PT
and DNT
Systemaic manifestations probably manifested by PT
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Clinical manifestationsPertussis (whooping
cough)

Spread by aerosol/direct contact
Early symptoms - nonspecific- seldom diagnosed
until paroxysmal stage- most contagious early
Stages- Incubation period 7-10 days- Catarrhal
stage
Symptoms like common cold, lasts 1-2 weeks
Paroxysmal stage
dry nonproductive cough, paroxysmal
excess mucus production, vomiting, convulsions,
cyanosis, paroxysms separated by inspiratory
whoop
Lasts 4-6 weeks

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Children who are too young to be fully
vaccinated and those who have not completed the
primary vaccination series are at highest risk
for severe illness
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Complications

Pneumonia
Either caused by B. pertussis or secondary
bacterial infection
Bronchiectasis
Neurological damage
Seizures in 1.4, encephalopathy 0.2 (seizures
and mental retardation)
Raised intrathoracic and intrabdominal pressure
leading to intracranial bleeds, conjunctival
haemorrhages, petichiae, pneumothorax, inguinal
hernia etc.

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Laboratory Diagnosis

Leucocytosis with absolute lymphocytosis at end
of catarrhal and beginning of paroxysmal stage
Culture pernasal swab early in course of
illness, plate on Bordet-Genou or charcoal medium
PCR
Serology

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Management and Prevention

effect of antimicrobial therapy on the severity
and duration of the illness is debated but
erythromycin x 14 days (clarythromycin and
azithromycin are alternatives) is recommended as
it may reduce the spread of disease
Antimicrobial prophylaxis (erythromycin x 14 d)
should be offered to all family members and other
close contacts
There is no evidence of any benefit from
chemoprophylaxis given more than 21 days from the
date of onset of the primary case.
Chemoprophylaxis should be considered if a case
has a household contact who is at greatest risk
from pertussis primarily young

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Vaccination

Whole-cell pertussis vaccination is associated
with rare serious events such as acute
encephalopathy, estimated to occur at 0.0-10.5
per million doses
1996 several new acellular pertussis vaccines
developed
multicomponent vaccines contain combinations of
pertussis toxoid, filamentous hemagglutinin,
pertactin, and the two types of fimbriae
fewer side effects than the whole cell vaccine
Protection declines with time (little protection
at 10 yrs)
Booster recommended at 11-14 yrs

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Pertussis in Ireland
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Brucella species

Gram-negative coccobacillus
Facultative intracellular parasites
Six species
B. abortus - cattle
B. suis - pigs
B. melitensis - goats
B. canis - dogs
B. ovis - sheep
B. neotomae - desert wood rats
Cause zoonoses worldwide
Ireland was declared free of brucellosis in
cattle on July 1st 2009

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B. abortus
Disease in cattle- causes abortion, mammary
infection (not mastitis)- transmission to humans
by ingestion (infected milk) or inhalation
(aborted material)
Disease in humans- long incubation period
(weeks, months)- malaise, chills, fever,
sweats- weakness, myalgia, headache- nervous
symptoms (psychoneurosis)- difficult to diagnose
due to vagueness of symptoms

B. melitensis
Primary hosts are sheep and goat
Disease in goat similar to B. abortus in
cattle
Early localization in mammary gland,
shedding in milk leads to human infection
Gastroenteritis- Malta/Mediterranean fever
potential agent of bioterrorism

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Pathogenesis

Ingestion.
Most common.
Inhalation.
Certain occupations e.g. laboratory workers,
abbattoir workers.
Enter the body through skin wounds.
Slaughterhouses or meat packing plants or for
veterinarians.
Laboratory
inhalation of aerosols (estimated infectious dose
of 10-100 organisms )
Common laboratory-acquired infection
Accounts for 10 of LAIs in US
11 of deaths associated with occupational
exposure

Intracellular pathogen and disseminated widely
(within macrophages or free) to lymph nodes
variable clinical presentation
Any system/tissue may be involved
Incubation period is highly variable
CDC recommend 6 months active surveillance
following exposure with antibody tests to check
for seroconversion

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Clinical manifestations

nonspecific and "flu-like," including fever,
sweats, malaise, anorexia, headache, myalgia, and
back pain, lymphadenopathy, splenomegaly
Endocarditis
Cutaneous manifestations may include ulcerations,
petechiae, purpura, and erythema nodosum
Mild leukopenia and relative lymphocytosis, along
with mild anemia and thrombocytopenia
Mild increase of liver function enzymes
Non-caseating epithelioid granulomas
indistinguishable from the ones seen in
sarcoidosis can be found in liver biopsy
meningoencephalitis, meningovascular involvement,
parenchymatous dysfunction, peripheral
neuropathy/radiculopathy (PNP), and various
degrees of behavioral abnormalities
Osteoarticular complications of brucellosis are
common

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Chronic brucellosis

? (gt1 year from illness onset), may include
chronic fatigue syndrome-like, depressive
episodes, and arthritis.

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Diagnosis

Isolation of Brucella sp. from a clinical
specimen
Need prolonged incubation (45 days recommended)
Bone marrow culture
Demonstration of a specific antibody response
(gt160 or 4-fold rise between acute and
convalescent phase)

Serologic tests
Serum agglutination test (SAT) or
microagglutination test
Most widely used
Not useful for following treatment as titres
remain high
ELISA
Most sensitive IgG and IgM
Brucellacapt
All antibodies detected by an inmmunocapture-agglu
tination technique
No single titre assay is always diagnostic
Consider titre of gt1160 as suspicious

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Treatment

World Health Organization (WHO)
doxycycline 100 mg b.i.d. rifampin 600-1200 mg
daily X 6 weeks or
doxycycline for 6 weeks and streptomycin 15 mg/kg
daily for 2-3 weeks

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Yersinia species

Y. pestis
Causes plague bubonic/pneumonic
Transmitted by flea bite, occasionally from
aeroslisation
periodic disease outbreaks in rodent populations,
hungry infected fleas that have lost their normal
hosts seek other sources of blood
Rat-borne epidemics continue to occur in some
developing countries, particularly in rural
areas.
Potential bioterrorist agent

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Yersinae pestis
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Yersinia pestis on blood agar
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Protective clothing worn in 14th century Europe
during the Black Death
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Xenopsylla cheopis - Oriental rat flea
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Clinical features

Bubonic plague
enlarged, tender lymph nodes, fever, chills and
prostration
Septicemic plague
fever, chills, prostration, abdominal pain, shock
and bleeding into skin and other organs
Pneumonic plague
fever, chills, cough and difficulty breathing
rapid shock and death if not treated early
TREATMENT
Streptomycin/gentamicin, ciprofloxacin,
doxycycline

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Plague axillary bubo (CDC Public Health Image
Library No2061)
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Plague inguinal bubo CDC Public Health Image
Library No2044
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Peripheral blood smear of septicaemic plague
showing bipolar staining bacilli
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Y. pseudotuberculosis
Y. enterocolitica
Both can cause abdominal symptoms
Occurs most often in young children. Fever,
abdominal pain, and diarrhoea, which is often
bloody
May mimic appendicitis
Eating contaminated food, especially raw or
undercooked pork
Outbreaks are described
Usually self-limited
Tetracyclines

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Pasteurella multocida