Brucella
Clinical Significance: Brucella melitensis
(sheep/goats) most important sources of brucellosis in humans
Identification of Brucella spp.:
CO2/H2S/Dyes Fuschin, Thionin/Serological Agglutination A, M, R- B. meitensis FT M B. abortus CH F A B. suis T AM B. canis T R B. ovis C T R B. neotomae H A
Clinical Significance: Brucella suis
affects both swine sexes infertility arbortion orchitis lesions of bones, joints
Molecular Biology Techniques: primers, probes
amplify/detect species-specific targets: 16S rRNA 23S rRNA 5S rRNA omp2
Brucellosis: infection in humans
male infertility arthritis endocarditis meningitis
BurR/BurS
(2)-component regulatory system: sensor kinase & response regulator modulates host cell cytoskeleton regulates expression of outer membrane proteins required for full virulence autophosphorylation BurR binds to regulatory region of DNA to turn on mode of operation
Molecular Biology Techniques: IS711
(PCR specific Assay) insertion sequence found in all Brucella occurs in variable numbers, and positions but in constant manner within a spp.
Molecular Biology Techniques: Phage-typing
10+ brucellaphage (narrow host range easily identifies genus, species) phage is associated w/ Brucella spp Phages (commercially available): Tb (Tbilisi) Fi ( Firenze) Wb (Weybridge) Iz (Izatnagar)
Brucella genomes sequenced:
2 circular chromosomes except B. suis biovar 3 (1 circular) all genomes similar (Seq., org., struct.) 0 plasmids/intact lysogenic phages
O-polysaccharide of S-LPS
2 main antigens: A, M (speciation & biotyping) 3 phenotypes: A+M- (B. abortus) A-M+ (B. melitensis) A+M+ (B. suis)
Transmission: Brucella
3 routes: ingestion (contaminated meats/dairy) direct contact (infected animals/products) inhalation (aerosolized organisms)
Brucellosis: human pathogenicity scale
B. melitensis > B. suis > B. arbortus > B. canis
Pathogenesis: Brucella BCV
BCV Brucella containing vacuole: survives w/in phagocytic/nonphagocytic cells interacts w/ early endosomes, late endosomes, lysosomes BCV fuses w/ the ER replicated BCV (rBCV)
Pathogenesis: Brucella rBCV
BCV fuses w/ the ER replicated BCV (rBCV): ER-derived BCVs are replication-permissive organelles after replication, bacteria exits host cell to reinfect adjacent cells
General Properties: Brucella morphology
Gram- coccobacilli, coccoid, rod-shaped no capsules singly, pairs, short chains, groups non-motile no spores
Pathogenesis: Brucella virulence factors
HSP60 heat-shock protein 60 (mediates attachment) CBG cyclic beta-1,2 glucan (early biogenesis BCV) VirB Type IV secretion apparatus BurR/BurS (2)-component regulatory system
General Properties: Brucella LPS
LPS (unconventional structure): low endotoxicity hidden from immune system recognition 2 types (sugars)- smooth-phase S-LPS (long o chain)(high virulence) rough-phase R-LPS (short o chain)(low virulence)(susceptible to complement)
Clinical Significance: names of the disease caused by Brucella spp.:
Most common term- Brucellosis Microbiologists: Sir David Bruce Bernard Bang Clinical presentation of the disease: undulant fever(humans) Sites of outbreaks: Mediterranean/Malta fever
Presumptive differentiation of Brucella spp. from similiar Gram negative organisms:
Oxidase/Motility/X, V factor- Brucella spp. +-- (Ox-pos) Acinetobact spp. --- Bordetella spp. ++- (Ox-pos, Motility) Haemophilus influenzae +-+ (Ox-pos, non-motile, X, V required) X, V factors preformed growth factors found in blood
Brucella species: R/S-LPS form type
Rough LPS form: B. canis (dogs) B. ovis (sheep) Smooth LPS form: B. melitensis (goats) 1st gene sequenced B. abortus (cattle) B. suis ( pigs) B. inopinata (humans)
General Properties: Brucella metabolism
STRICT Aerobes: chemoorganoheterotrophic respiratory metabolism (O2 as TEA) Catalase positive oxidase negative no acid prod. from carbohydrates gelatinase- negative VP negative Methyl red negative Indole negative most strains urease positive
VirB Type IV secretion apparatus
VirB Type IV secretion apparatus: General VirB, Specific VirB required for late survival events alows bacterial effectors to inject in host cell's cytosol subverts signaling pathways favors bacterial growth & pathogenesis
Clinical Significance: Brucellosis, source of infection
Zoonosis: infected animals consumption of milk/milk products Oral entry: raw milk /derivatives Direct contact: fingers common route of entry Inhalation: aerosol contamination of conjuctivae
Treatment: human Brucellosis
antibiotic combo: rifampin (prevents transcription, blocks reverse transcriptase) + tetracycline (inhibits translation) (+ streptomycin) prolonged treatment course: 4-6 wks. (Brucella is intracellular) no antibiotic resistance demonstrated
Clinical Significance: Bovine Brucellosis
caused by B. arbortus (cattle)
Laboratory Diagnosis: cultivation Brucella spp.
colonies small, non-hemolytic, non-pigmented- Agar: Brucella agar (specific; yeast, casein, animal tissue) blood agar (35-37ºC) chocolate MAC MacConkey agar Gram stain: not well retained in Brucella (Gram-) difficult in blood sample
Prevention, Control: Brucellosis
control of infection in livestock controls human brucellosis vaccination: animals RV51 vaccine
Pathogenesis: Brucella
facultative intracellular no classic virulence factors defeats both innate & adaptive immunity: lowers its stimulatory activity & toxicity for cells BCV Brucella containing vacuole
Brucellosis: infection B. melitensis
granulomas small major toxemia
Natural Habitats: Brucella
infected mammals/products not commensals not free-living Brucellosis: occupational disease (cattle, pigs, goats) common lab infection
Brucellosis: onset/ initial episode
influenza-like (fever) limb/back pain severe sweating, fatigue normal/reduced leukocyte count w/ lymphocytosis (high WBC) splenomegaly (enlarged spleen) patients may recover after 2-4 weeks/ suffer series of exacerbations
General Properties: Brucella cell wall
meso-DAP LPS (unconventional structure)
Brucella species: general
named according to host preference Most pathogenic: B. melitensis (goats) 1st gene sequenced B. abortus (cattle) B. suis ( pigs) B. inopinata (humans) Least pathogenic: B. canis (dogs) B. ovis (sheep) B. neotomae (desert wood rat)
Brucellosis: infection B. suis
necrosis abscesses (pus w/ infection)
Brucellosis: general
occupational exposure incubation period: 2-4 wks onset insidious/abrupt subclinical infection (asymptomatic carrier)
Clinical Significance: B. canis infection
occurs in dog handler
Brucella spp. deadly in daylight:
respond to blue wavelength replicate quickly LOVs signaling proteins (signal replication)
smooth vs. rough phase LPS
rough is mutant of smooth
Brucellosis: post-onset 4-8 wks; series of exacerbations
undulant fever (10 day intervals) anemia relapses (months) tissue lesions/ granulomas (inflammation)
Molecular Biology Techniques: other methods
whole-cell protein profile analysis by SDS-PAGE- PFGE RAPD-PCR RFLP-PCR MLVA MLST IS711 (PCR specific Assay) Multiplex-PCR AMOS-PCR ( uses 5 primers) Brucella-ladder PCR (uses 7 primers) Phage-typing
