Yersinia Pestis
Yersinia Pestis
MATERIAL SAFETY DATA SHEET – INFECTIOUS SUBSTANCES
SECTION I – INFECTIOUS AGENT
NAME: Yersinia pestis
SYNONYM OR CROSS REFERENCE: Plague, Peste, Bubonic plague
CHARACTERISTICS: Gram negative rod-ovoid 0.5-0.8 µm in width and 1-3 µm in length, bipolar staining (safety pin appearance), facultative intracellular, non-motile
SECTION II – HEALTH HAZARD
PATHOGENICITY: Zoonotic disease; bubonic plague with lymphadenitis in nodes receiving drainage from site of flea bite, occuring in lymph nodes and inguinal areas, fever, 50% case fatality if untreated; may progress to septicemic plague with dissemination by blood to meninges; secondary pneumonic plague with pneumonia, mediastinitis, and pleural effusion; untreated pneumonic and septicemic are fatal
EPIDEMIOLOGY: Wild rodent plague in North America, South America, Africa, Near and Middle East, Central and Southeast Asia, Indonesia; plague foci in USSR; urban plague controlled in most areas; human plague occurred recently in Africa; endemic in Burma and Vietnam; sporadic cases in North and South America following exposure to wild rodents or their fleas (no human-to-human transmission in USA since 1925)
HOST RANGE: Humans,> 200 mammalian species
INFECTIOUS DOSE: Unknown
MODE OF TRANSMISSION: Result of human intrusion into zoonotic (sylvatic) cycle or by entry of rodents or infected fleas into human’s habitat and bite of infected fleas; domestic pets can carry plague-infected fleas; contact of commensal rodents and their fleas with sylvatic rodents may result in epizootic and epidemic plague; handling of infected tissues; airborne droplets from humans or pets with plague pneumonia; careless manipulation of laboratory cultures; person-to-person transmission by human fleas
INCUBATION PERIOD: From 2 to 6 days; may be a few days longer in vaccinated individuals; for primary plague pneumonia, 1 to 6 days, usually short
COMMUNICABILITY: Fleas may remain infective for months; bubonic plague not usually transmitted directly from person-to-person; pneumonic plague may be highly communicable under appropriate climatic conditions (overcrowding facilitates transmission)
SECTION III – DISSEMINATION
RESERVOIR: Wild rodents (rats) are the natural reservoir; lagomorphs (rabbits, hares) and carnivores may be a source of infection to humans
ZOONOSIS: Yes – bites of fleas from an infected animal; contact or being bitten by an infected animal
VECTORS: Wild rodent fleas, especially the oriental rat flea (Xenopsylla cheopis); occasionlly by human fleas (Pulex irritans)
SECTION IV – VIABILITY
DRUG SUSCEPTIBILITY: Sensitive to streptomycin, tetracycline, chloramphenicol (for cases of plague meningitis), kanamycin (for neonates)
DRUG RESISTANCE: Generally not a concern; a multi-drug resistant strain (MDR) mediated by transferrable plasmid has been isolated
SUSCEPTIBILITY TO DISINFECTANTS: Susceptible to many disinfectants – 1% sodium hypochlorite, 70% ethanol, 2% glutaraldehyde, iodines, phenolics, formaldehyde
PHYSICAL INACTIVATION: Sensitive to moist heat (121° C for at least 15 min) and dry heat (160-170° C for at least 1 hour)
SURVIVAL OUTSIDE HOST: Blood – 100 days; human bodies – up to 270 days
SECTION V – MEDICAL
SURVEILLANCE: Monitor for symptoms; presumptive diagnosis by visualizing bipolar staining, ovoid, gram-negative organisms in sputum or material aspirated from bubo; FA and ELISA test; PHA using Fraction-1 antigen
FIRST AID/TREATMENT: Antibiotic therapy in early stages (8 to 24 hours after onset of pneumonic plague); secondary infection or suppurative bubo may require incision and drainage
IMMUNIZATION: Although field trials have not been conducted to determine the efficacy of licensed vaccines, experience has been favourable; immunization is recommended for personnel working regularly with culture of Y. pestis or infected rodents, boosters are required every 6 months if high risk continues; protection against pneumonic form is limited
PROPHYLAXIS: Chemoprophylaxis using tetracyclines or sulfonamides; for close contacts of pneumonic cases
SECTION VI – LABORATORY HAZARDS
LABORATORY-ACQUIRED INFECTIONS: 10 reported laboratory-acquired infections with 4 deaths
SOURCES/SPECIMENS: Bubo fluid, blood, sputum, CSF, feces, urine
PRIMARY HAZARDS: Direct contact with cultures and infectious materials from humans or rodents; infectious aerosols or droplets generated during manipulation of cultures and infected tissues and in the necropsy of rodents; accidental auto-inoculation; ingestion
SPECIAL HAZARDS: Bites by infected fleas collected from rodents
SECTION VII – RECOMMENDED PRECAUTIONS
CONTAINMENT REQUIREMENTS: Biosafety level 3 practices, containment equipment and facilites for all activities involving the handling of potentially infectious clinical materials and cultures
PROTECTIVE CLOTHING: Gloves should be worn when handling field-collected or infected laboratory rodents and when there is the likelihood of direct skin contact with infectious materials; gown with tight cuffs and ties in back should be worn when manipulating cultures and specimens; a mask should be worn when there is a risk of contact with aerosols
OTHER PRECAUTIONS: Special care should be taken to avoid the generation of aerosols during the necropsy of animals; necropsy should be conducted in a biological safety cabinet; insecticide treatment when collecting animals (living or dead) for testing
SECTION VIII – HANDLING INFORMATION
SPILLS: Allow aerosols to settle; wearing protective clothing, gently cover spill with paper towels and apply 1% sodium hypochlorite, starting at perimeter and working towards the centre; allow sufficient contact time (30 min) before clean up
DISPOSAL: Decontaminate before disposal; steam sterilization, incineration (animal carcasses)
STORAGE: In sealed containers that are appropriately labeled
SECTION IX – MISCELLANEOUS INFORMATION
Date prepared: January, 2001
Prepared by: Office of Laboratory Security, PHAC
Although the information, opinions and recommendations contained in this Material Safety Data Sheet are compiled from sources believed to be reliable, we accept no responsibility for the accuracy, sufficiency, or reliability or for any loss or injury resulting from the use of the information. Newly discovered hazards are frequent and this information may not be completely up to date.
Copyright © Health Canada, 2001
This MSDS / PSDS document, provided by Public Health Agency of Canada (PHAC), is offered here as a FREE public service to visitors of www.EHS.com. As outlined in this site’s Terms of Use, VelocityEHS is not responsible for the accuracy, content or any aspect of the information contained therein.
Copyright © Health Canada, 2001
This MSDS / PSDS document, provided by Public Health Agency of Canada (PHAC), is offered here as a FREE public service to visitors of www.EHS.com. As outlined in this site’s Terms of Use, VelocityEHS is not responsible for the accuracy, content or any aspect of the information contained therein.
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