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Plague

Central Department Of Microbiology, TU
Central Department Of Microbiology, TU

Emerging bacterial diseases- Plaque

Ciencias
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PLAGUE Name: Purshotam Kumar Sah Kanu Roll No.: MB 1318/075 Level: M.Sc Microbiology (3rd Sem) Central Department of Microbiology Tribhuvan University, Kirtipur Kathmandu, Nepal
Introduction • Plague, infectious disease caused by Yersinia pestis, a bacterium transmitted from rodents to humans by the bite of infected fleas, direct contact with infected fluids or tissue from a host inhalation of respiratory droplet. • The bacteria, the animal reservoir and the vector in a given area are collectively called a “plague natural focus”. • Plague is a fatal disease, which approximately more than 200 million people have been dead by this disease.
History • Plague recorded more than 2000 years ago. • Three pandemics: • 1st 542 AD; Justinian plague;100 million dead in 60 years from N. Africa. • 2nd 14th century; Black death; 25 million dead in Europe alone. • 3rd ended in 1990s; Burma to China(1894) and Hong kong to other continents including N. America via rat infected ships; 20 million dead in India alone. • By the end of the 19th century, the germ theory of disease had been put on a sound empirical basis by the work of the great European scientists Louis Pasteur, Joseph Lister, and Robert Koch.
• In 1894, during the epidemic in Hong Kong, the organism that causes plague was isolated independently by two bacteriologists, the Frenchman Alexandre Yersin, working for the Pasteur Institute, and the Japanese Kitasato Shibasaburo, a former associate of Koch. Both men found bacteria in fluid samples taken from plague victims, then injected them into animals and observed that the animals died quickly of plague. • Yersin named the new bacillus Pasteurella pestis, after his mentor, but in 1970 the bacterium was renamed Yersinia pestis, in honour of Yersin himself.
Epidemiology • Internationally, cases of plague are typically reported from developing countries in Africa and Asia. • From 1990-1995, 12, 998 cases worldwide were reported to the World Health Organization (WHO), particularly from countries such as India, Zaire, Peru, Malawi, and Mozambique. • In 2003,2118 cases were reported with 182 deaths worldwide. • 98.7 percent of cases and 98.9 percent of deaths were reported from Africa. • Australia is the only continent that has never report a case of plague. • In the United states, natural Y. pestis loci exist in primarily rural and uninhabited areas.
• 10-15 cases of plague on average are reported each year in the united states. • In the early twentieth century, plague epidemics accounted for about 10 million deaths in India. • As reported in National Geographic, mass graves of plague victims were discovered in an area of Venice called “Quarantine island.” • In recent years, and with the potential threat for bioterrorism, the centers for Disease control and Prevention (CDC) has specified Y. pestis as a Category A bioterrorism agent.
Plague in Nepal • It was first recorded only between 1960-1962, in Rupandehi and Mahottari districts with 150 cases. • Later, it was reported again in October 1967, in Nawra village of Bajhang. • It was reported that the plague was airborne and resulted in six cases of tonsillar plague, one case of primary pneumonic plague, and 17 cases of bubonic plague.
Causative Organism • The disease is caused by the Plague bacillus, rod shaped bacteria referred to as Yersinia pestis (family enterobacteriaceae). • It is a non-motile, pleomorphic, gram negative coccobacillus that is non sporulating. • It is facultative anaerobe. • It can infect human and animals via the oriental rat flea which called (Xenopsylla Cheopis). • It can reproduce inside cells, so even if phagocytosed they can still survive, because it produces an anti-phagocytic slime layer.
Pathogenesis • Colonization and growth of Y. pestis in the flea proventriculus (valve between oesophagus and midgut) blocks passage of food, which results in efficient transmission via flea bite. • Phospholipase D helps the bacteria to withstand antibacterial factors active in the flea midgut and haemin storage locus (hms) is required to colonize and for biofilm formation in the flea. • Y. pestis disseminates from the site of infection within macrophages and this requires a plasminogen activator. • Once phagocytized the disease progresses the same from bite or ingestion or inhalation.
• There are two stages of Y. pestis proliferation in the host. • Neutrophils kill the bacteria, but macrophages phagocytize them but do not kill them and there it grows intracellularly within spacious vacuoles. • In susceptible hosts, infected macrophages are carried to the lymph nodes --hence, buboes-- and the liver and spleen, where the bacteria cause the macrophages to lyse. • Then, the bacteria grow extracellularly. Extracellular growth requires plasmid encoded Type III secretion system and translocation of Yersinia outer protein (Yops). • Yops interfere with immune cell function and can cause immune cell death by apoptosis. LcrV (V antigen) has anti-inflammatory activity. • These virulence factors allow massive extracellular proliferation of the bacteria in affected tissues.
Infectious dose, Incubation, Colonization • In humans, the infectious dose of Y. pestis has been estimated to range from 100 organisms to 20,000 organisms. • The incubation period of the bubonic, septicemic, and pneumonic plague types ranges from 2-6 days. • Y. pestis colonizes macrophages, reaches lymph nodes, escapes the macrophages, and proliferates extracellularly. • Left untreated, Y. pestis is able to spread to the bloodstream and cause secondary infection as well as septicemic plague in rare cases. • Y. pestis is also able to colonize lung tissue as pneumonic plague.
Mode of transmission in humans • Air droplet • Direct physical contact • Indirect physical contact • Fecal-oral transmission • Vector borne transmission
Virulence factors • Plasminogen activator: facilitates the adhesion and invasion of the bacterium to the extracellular matrix of the host tissue. • Siderophores: Yersiniabactin(Ybt); organism capable of scavenging iron from human and of enhanced growth. • Anti-phagocytic antigens: Factor 1 (f1) and V antigen increases Y. pestis resistance to phagocytosis by macrophages. • Type III secretion system: Y.pestis utilizes a T3SS in order to evade host immune responses.
Clinical Features The symptoms of Y. pestis present in different ways: Bubonic plague oIt usually results from the bite of an infected flea or by introduction of contaminated fluid or tissue into an open wound. oAfter an incubation period of 2 -6 days, there is acute onset of symptoms such as fever, headache, chills and weakness. oIt is also common to see gastrointestinal symptoms like nausea and vomiting. oAbout 24hrs after start of these symptoms, swollen, extremely tender lymph nodes known as buboes, filled with multiplying Y. pestis appear. oThese buboes typically form from lymph nodes that were closet to the site of infection.
Septicemic Plague  When the bacteria enters the blood stream directly and multiply there, it’s known as septicemic plague.  It can either develop primarily, often through the introduction of contaminated fluid or tissue into an open wound or secondarily as a result of untreated bubonic plague.  There is a sudden onset of symptoms including fever, chills, nausea and vomiting.  Later on in the course of the disease purpura, a rash caused by bleeding into the skin and disseminated vascular coagulation can develop.  Tissue blackening and death specially in the fingers, toes and the nose is also seen.
Pneumonic Plague • It is a highly contagious form of the disease. Primary pneumonic plague develops when a person inhales infectious droplets emitted by a pneumonic plague sufferer. • Secondary pneumonic plague can develop when untreated bubonic or septicemic plague spreads to the lungs. • Symptoms include fever, headache, weakness and a developing pneumonia which includes symptoms of cough, chest pain and shortness of breathe. • As the disease progresses, hemorrhages, necrosis of the tissue and pulmonary abscesses are other common symptoms. • In the end stages of untreated pneumonic plague, Adult Respiratory Distress Syndrome (ARDS) and shock can sometimes be seen.
Diagnosis Specimen: Pus or fluid, Sputum, blood, throat swab or washings, skin swabs and scrapings are also collected. Microscopy: Gram staining, methylene blue and giemsa’s staining of sputum and aspirate from lymph node show bacilli with bipolar staining. Culture: Trypticase soy agar with 5% sheep blood and incubated for 24hrs at 28°C The colonies should be gray-white, translucent, little to no hemolysis and be non lactose fermenter. It should test positive for catalase, but negative for oxidase, urease and indole test. Serological test: antibodies to F1 antigen appear towards the end of first week of the illness and may be detected by passive haemagglutination, ELISA or complement fixation test.
Treatment • Streptomycin is the antibiotic of choice for treating Yersinia pestis infections. • Other possible antibiotics include gentamicin, chloramphenicol, tetracyclines, and fluoroquinolones. • The antibiotic levofloxacin has also been recently approved by the Food and Drug Administration as appropriate treatment. • Antibiotic dosages are typically administered for the full period of ten days or for three days after the fever has subsided. • It is also important to hospitalize and quarantine any suspected or confirmed cases of Yersinia pestis in order to provide effective treatment and prevent the spread of the disease if it develops into secondary pneumonic plague.
Prevention and control • Diminish the possibility of rodent infestation around homes by clearing away cluttered debris and apply flea control products for pets that roam freely in the open. • Means of prevention can also be applied in hospital settings where the possibility of transmission can be high. • Standardized procedures of handwashing and utilization of gowns, latex gloves, and protective devices should be followed to protect all body orifices from coming into contact with Y. pestis. • Restrictions of patients suspected with plague should be enacted to prevent the spread of disease to other individuals.
BIBLIOGRAPHY • Park K. (2015) Park’s Textbook of Preventive and Social medicine,23rd Edition. Bhanot, India. • https://www.cdc.gov/plague/transmission/index.html • https://www.who.int/news-room/fact-sheets/detail/plague • https://microbewiki.kenyon.edu/index.php/Yersinia_Pestis_(Pathogenesis) • https://english.onlinekhabar.com/history-of-epidemics-in-nepal-part-i-6-deadly- diseases-that-killed-hundreds.html • https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2427975/pdf/bullwho00199- 0004.pdf
Plague

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Plague

  • 1. PLAGUE Name: Purshotam Kumar Sah Kanu Roll No.: MB 1318/075 Level: M.Sc Microbiology (3rd Sem) Central Department of Microbiology Tribhuvan University, Kirtipur Kathmandu, Nepal
  • 2. Introduction • Plague, infectious disease caused by Yersinia pestis, a bacterium transmitted from rodents to humans by the bite of infected fleas, direct contact with infected fluids or tissue from a host inhalation of respiratory droplet. • The bacteria, the animal reservoir and the vector in a given area are collectively called a “plague natural focus”. • Plague is a fatal disease, which approximately more than 200 million people have been dead by this disease.
  • 3. History • Plague recorded more than 2000 years ago. • Three pandemics: • 1st 542 AD; Justinian plague;100 million dead in 60 years from N. Africa. • 2nd 14th century; Black death; 25 million dead in Europe alone. • 3rd ended in 1990s; Burma to China(1894) and Hong kong to other continents including N. America via rat infected ships; 20 million dead in India alone. • By the end of the 19th century, the germ theory of disease had been put on a sound empirical basis by the work of the great European scientists Louis Pasteur, Joseph Lister, and Robert Koch.
  • 4. • In 1894, during the epidemic in Hong Kong, the organism that causes plague was isolated independently by two bacteriologists, the Frenchman Alexandre Yersin, working for the Pasteur Institute, and the Japanese Kitasato Shibasaburo, a former associate of Koch. Both men found bacteria in fluid samples taken from plague victims, then injected them into animals and observed that the animals died quickly of plague. • Yersin named the new bacillus Pasteurella pestis, after his mentor, but in 1970 the bacterium was renamed Yersinia pestis, in honour of Yersin himself.
  • 5. Epidemiology • Internationally, cases of plague are typically reported from developing countries in Africa and Asia. • From 1990-1995, 12, 998 cases worldwide were reported to the World Health Organization (WHO), particularly from countries such as India, Zaire, Peru, Malawi, and Mozambique. • In 2003,2118 cases were reported with 182 deaths worldwide. • 98.7 percent of cases and 98.9 percent of deaths were reported from Africa. • Australia is the only continent that has never report a case of plague. • In the United states, natural Y. pestis loci exist in primarily rural and uninhabited areas.
  • 6. • 10-15 cases of plague on average are reported each year in the united states. • In the early twentieth century, plague epidemics accounted for about 10 million deaths in India. • As reported in National Geographic, mass graves of plague victims were discovered in an area of Venice called “Quarantine island.” • In recent years, and with the potential threat for bioterrorism, the centers for Disease control and Prevention (CDC) has specified Y. pestis as a Category A bioterrorism agent.
  • 7. Plague in Nepal • It was first recorded only between 1960-1962, in Rupandehi and Mahottari districts with 150 cases. • Later, it was reported again in October 1967, in Nawra village of Bajhang. • It was reported that the plague was airborne and resulted in six cases of tonsillar plague, one case of primary pneumonic plague, and 17 cases of bubonic plague.
  • 8. Causative Organism • The disease is caused by the Plague bacillus, rod shaped bacteria referred to as Yersinia pestis (family enterobacteriaceae). • It is a non-motile, pleomorphic, gram negative coccobacillus that is non sporulating. • It is facultative anaerobe. • It can infect human and animals via the oriental rat flea which called (Xenopsylla Cheopis). • It can reproduce inside cells, so even if phagocytosed they can still survive, because it produces an anti-phagocytic slime layer.
  • 9. Pathogenesis • Colonization and growth of Y. pestis in the flea proventriculus (valve between oesophagus and midgut) blocks passage of food, which results in efficient transmission via flea bite. • Phospholipase D helps the bacteria to withstand antibacterial factors active in the flea midgut and haemin storage locus (hms) is required to colonize and for biofilm formation in the flea. • Y. pestis disseminates from the site of infection within macrophages and this requires a plasminogen activator. • Once phagocytized the disease progresses the same from bite or ingestion or inhalation.
  • 10. • There are two stages of Y. pestis proliferation in the host. • Neutrophils kill the bacteria, but macrophages phagocytize them but do not kill them and there it grows intracellularly within spacious vacuoles. • In susceptible hosts, infected macrophages are carried to the lymph nodes --hence, buboes-- and the liver and spleen, where the bacteria cause the macrophages to lyse. • Then, the bacteria grow extracellularly. Extracellular growth requires plasmid encoded Type III secretion system and translocation of Yersinia outer protein (Yops). • Yops interfere with immune cell function and can cause immune cell death by apoptosis. LcrV (V antigen) has anti-inflammatory activity. • These virulence factors allow massive extracellular proliferation of the bacteria in affected tissues.
  • 11. Infectious dose, Incubation, Colonization • In humans, the infectious dose of Y. pestis has been estimated to range from 100 organisms to 20,000 organisms. • The incubation period of the bubonic, septicemic, and pneumonic plague types ranges from 2-6 days. • Y. pestis colonizes macrophages, reaches lymph nodes, escapes the macrophages, and proliferates extracellularly. • Left untreated, Y. pestis is able to spread to the bloodstream and cause secondary infection as well as septicemic plague in rare cases. • Y. pestis is also able to colonize lung tissue as pneumonic plague.
  • 12. Mode of transmission in humans • Air droplet • Direct physical contact • Indirect physical contact • Fecal-oral transmission • Vector borne transmission
  • 13. Virulence factors • Plasminogen activator: facilitates the adhesion and invasion of the bacterium to the extracellular matrix of the host tissue. • Siderophores: Yersiniabactin(Ybt); organism capable of scavenging iron from human and of enhanced growth. • Anti-phagocytic antigens: Factor 1 (f1) and V antigen increases Y. pestis resistance to phagocytosis by macrophages. • Type III secretion system: Y.pestis utilizes a T3SS in order to evade host immune responses.
  • 14. Clinical Features The symptoms of Y. pestis present in different ways: Bubonic plague oIt usually results from the bite of an infected flea or by introduction of contaminated fluid or tissue into an open wound. oAfter an incubation period of 2 -6 days, there is acute onset of symptoms such as fever, headache, chills and weakness. oIt is also common to see gastrointestinal symptoms like nausea and vomiting. oAbout 24hrs after start of these symptoms, swollen, extremely tender lymph nodes known as buboes, filled with multiplying Y. pestis appear. oThese buboes typically form from lymph nodes that were closet to the site of infection.
  • 15. Septicemic Plague  When the bacteria enters the blood stream directly and multiply there, it’s known as septicemic plague.  It can either develop primarily, often through the introduction of contaminated fluid or tissue into an open wound or secondarily as a result of untreated bubonic plague.  There is a sudden onset of symptoms including fever, chills, nausea and vomiting.  Later on in the course of the disease purpura, a rash caused by bleeding into the skin and disseminated vascular coagulation can develop.  Tissue blackening and death specially in the fingers, toes and the nose is also seen.
  • 16. Pneumonic Plague • It is a highly contagious form of the disease. Primary pneumonic plague develops when a person inhales infectious droplets emitted by a pneumonic plague sufferer. • Secondary pneumonic plague can develop when untreated bubonic or septicemic plague spreads to the lungs. • Symptoms include fever, headache, weakness and a developing pneumonia which includes symptoms of cough, chest pain and shortness of breathe. • As the disease progresses, hemorrhages, necrosis of the tissue and pulmonary abscesses are other common symptoms. • In the end stages of untreated pneumonic plague, Adult Respiratory Distress Syndrome (ARDS) and shock can sometimes be seen.
  • 17. Diagnosis Specimen: Pus or fluid, Sputum, blood, throat swab or washings, skin swabs and scrapings are also collected. Microscopy: Gram staining, methylene blue and giemsa’s staining of sputum and aspirate from lymph node show bacilli with bipolar staining. Culture: Trypticase soy agar with 5% sheep blood and incubated for 24hrs at 28°C The colonies should be gray-white, translucent, little to no hemolysis and be non lactose fermenter. It should test positive for catalase, but negative for oxidase, urease and indole test. Serological test: antibodies to F1 antigen appear towards the end of first week of the illness and may be detected by passive haemagglutination, ELISA or complement fixation test.
  • 18. Treatment • Streptomycin is the antibiotic of choice for treating Yersinia pestis infections. • Other possible antibiotics include gentamicin, chloramphenicol, tetracyclines, and fluoroquinolones. • The antibiotic levofloxacin has also been recently approved by the Food and Drug Administration as appropriate treatment. • Antibiotic dosages are typically administered for the full period of ten days or for three days after the fever has subsided. • It is also important to hospitalize and quarantine any suspected or confirmed cases of Yersinia pestis in order to provide effective treatment and prevent the spread of the disease if it develops into secondary pneumonic plague.
  • 19. Prevention and control • Diminish the possibility of rodent infestation around homes by clearing away cluttered debris and apply flea control products for pets that roam freely in the open. • Means of prevention can also be applied in hospital settings where the possibility of transmission can be high. • Standardized procedures of handwashing and utilization of gowns, latex gloves, and protective devices should be followed to protect all body orifices from coming into contact with Y. pestis. • Restrictions of patients suspected with plague should be enacted to prevent the spread of disease to other individuals.
  • 20. BIBLIOGRAPHY • Park K. (2015) Park’s Textbook of Preventive and Social medicine,23rd Edition. Bhanot, India. • https://www.cdc.gov/plague/transmission/index.html • https://www.who.int/news-room/fact-sheets/detail/plague • https://microbewiki.kenyon.edu/index.php/Yersinia_Pestis_(Pathogenesis) • https://english.onlinekhabar.com/history-of-epidemics-in-nepal-part-i-6-deadly- diseases-that-killed-hundreds.html • https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2427975/pdf/bullwho00199- 0004.pdf