CBRNE – Glanders and Melioidosis

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CBRNE – Glanders and Melioidosis

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Glanders and melioidosis are related diseases produced by bacteria of the Burkholderia species, which are gram-negative rods. The two diseases have similar symptoms and similar pathophysiologic consequences.

Burkholderia mallei (nonmotile, nonsporulating, obligate aerobic, gram-negative bacillus) is the causative agent of glanders, which is primarily a disease of animals such as horses, mules, and donkeys. [1]  Glanders has been only a rare and sporadic disease in humans, and no epidemics have been reported. In China during World War II, 30% of the tested horses were infected with glanders, but human cases were rare. The reason for the low transmission rate is not known. In the human population, Burkholderia mallei typically is found in persons with close and frequent contact with infected animals, such as veterinarians, animal caretakers, abattoir workers, and laboratory personnel. [2]

Melioidosis, also known as Whitmore disease, is caused by the bacterium Burkholderia pseudomallei (a motile, aerobic, non–spore-forming bacillus). [3]  It is clinically similar to glanders, although the epidemiology differs. The bacteria thrive in tropical climates. The disease is endemic in Southeast Asia and Australia, and is also found in the Middle East, India, and China (essentially tropical areas between latitudes 20 degrees north and south). [4, 5] Sporadic melioidosis cases have been reported in the United States (typically 0-5 cases per year, usually among immigrants and travelers). However, the worldwide incidence appears to be rising as a result of increased travel and epidemiological sophistication. Both humans and other susceptible animals may contract the disease.

Both organisms are considered potential biological warfare agents, especially in the aerosolized form. [6]  Because they are highly infectious by inhalation and resistant to routine antibiotics, both bacteria have been classified as category B priority pathogens by the National Institutes of Health and the Centers for Disease Control and Prevention (CDC). [7]

Patient education resources are available at First Aid and Injuries Center. Also, see patient education articles Biological Warfare and Personal Protective Equipment.

Glanders and melioidosis are of interest because of significant study for potential weaponization by the United States and other countries in the past. During World War I, glanders was believed to have been spread to infect large numbers of Russian horses and mules on the Eastern Front. The Japanese infected horses, civilians, and prisoners of war during World War II. The United States studied this agent as a possible biological warfare (BW) weapon in 1943-1944 but did not weaponize it. The former Soviet Union is believed to have been interested in glanders as a potential BW weapon, as well.

Glanders is caused by Burkholderia mallei (formerly Pseudomonas mallei). The bacteria exist only in infected susceptible hosts and are not found in water, soil, or plants. In nature, humans typically acquire glanders from equids via direct contact with broken skin or mucous membranes. While transmission through intact skin has been reported, it is not well documented. A secondary mode of transmission can be through inhalation of droplets from an infected equid or patient.

Once in the host, synthesis and release of certain toxins occur. Usually, the amount is insignificant, and no clinical disease process ensues. However, if a large quantity of the organism is incorporated, the amount of toxin is sufficient to cause specific symptoms. Antibiotics are of little use. The toxins include pyocyanin (blue-green pigment that interferes with the terminal electron transfer system), lecithinase (causes cell lysis by degrading lecithin in certain cell membranes), collagenase, lipase, and hemolysin.

Melioidosis is an infectious disease caused by B pseudomallei (formerly P pseudomallei). The organism is distributed widely in the soil and water of the tropics. It is spread to humans through direct contact with a contaminated source, especially during the rainy season. The disease usually occurs in the fourth and fifth decades of life, especially among those who have chronic comorbidities such as diabetes, alcoholism, immunosuppression, and renal failure. [5]

B pseudomallei is considered a good candidate as a bioweapon because it is easily available in the tropics, it is fairly easy to cultivate, it is sturdy, and it has a high potential to become bacteremic, thereby increasing morbidity and mortality. The incubation period in naturally acquired infections can vary from days to months to years. The incubation period after an aerosol attack is expected to be from 10-14 days.

Glanders and melioidosis produce similar clinical syndromes.

Bacteria enter the skin through a laceration or abrasion, and a local infection with ulceration develops. The incubation period is 1-5 days. Swollen lymph glands may develop. Bacteria that enter the host through mucous membranes can cause increased mucus production in the affected areas.

When bacteria are aerosolized and enter the respiratory tract via inhalation or hematogenous spread, pulmonary infections may develop. Pneumonia, pulmonary abscesses, and pleural effusions can occur. The incubation period is 10-14 days. With inhalational melioidosis, cutaneous abscesses may develop and take months to appear.

When bacteria is disseminated in the bloodstream in glanders, it is usually fatal within 7-10 days. The septicemia that develops affects multiple systems, and cutaneous, hepatic, and splenic involvement may occur. With melioidosis, bacteremia is observed with chronically ill patients (eg, patients with HIV, patients with diabetes). They develop respiratory distress, headaches, fever, diarrhea, pus-filled lesions on the skin, and abscesses throughout the body. Septicemia may be overwhelming, with a 90% fatality rate and death occurring within 24-48 hours.

The chronic form involves multiple abscesses, which may affect the liver, spleen, skin, or muscles. This form also is known as farcy in glanders disease. Melioidosis, in addition to this chronic form, can become reactive many years after the primary infection.

Glanders was eliminated from US domesticated animals in the 1940s. One human case of glanders in a laboratory worker occurred in 2000. This is the first human case reported in the United States since 1945. [8]

A few isolated cases of melioidosis have occurred in the United States. Confirmed cases range from 0-5 each year and occur among travelers, immigrants, and intravenous drug users. [9]  From 2008 to 2013, 37 confirmed cases of melioidosis in the United States and Puerto Rico were reported to the CDC’s Bacterial Special Pathogens Branch of human infections, including 34 human cases and three animal cases. Among individuals with a documented travel history, 64% of reported cases occurred in those with a travel history to endemic areas. During the study period, two incidents of occupational exposures were reported, and no human infections occurred. [10]

Glanders is endemic in Africa, Asia, the Middle East, Central America, and South America.

Melioidosis is endemic in Southeast Asia and northern Australia. In 2011, melioidosis was diagnosed in six individuals in a desert region of Australia over a 4-month period following unusual heavy rains and flooding. [11] Nevertheless, even in these zones, the diagnosis may be delayed. [12] Melioidosis has also been observed in the South Pacific, Africa, India, the Middle East, Central America, and South America. A case of young boy with laboratory-confirmed melioidosis was reported from Malawi in 2011, and the authors’ review of the literature indicates that the number of cases seems to be increasing in Africa. [13]

In India, melioidosis has acquired the status of a newly emerging infectious disease. [14] One study in India involving a series of patients with melioidosis revealed that skin and soft-tissue involvement (16%), liver abscess (16%), and bone and joint involvement (16%) were the most common presentations of this disease in patients with diabetes. Septicemia and major organ failure resulting in death was not uncommon. [15]

The mortality rate in the pulmonary form of glanders is 90-95% if untreated and 40% if treated. The mortality rate in the septicemic form of glanders is greater than 95% if untreated and 50% if treated. The mortality rate in the cutaneous form of glanders is 90-95% if it becomes systemic and if untreated but 50% if properly treated. For the chronic form of glanders, the mortality rate may be 50% despite treatment.

The risk for glanders infection is increased in veterinarians, horse handlers, equine butchers, slaughterhouse workers and laboratory workers exposed to infected animals or infected specimens. [16] ​ 

Melioidosis has had a reported mortality rate up to 90% if disseminated septicemia is present. In Australia, the mortality rate is 19%, whereas in Thailand it is 50%. It is most widespread in Thailand, where in one hospital, it was responsible for 19% of community-acquired sepsis and 40% of deaths from community-acquired septicemia. [17]  

Although healthy people may get melioidosis, the major risk factors are [18] :

Possible complications of these diseases include the following:

Spickler AR. Glanders. Center for Food Security and Public Health. Available at http://www.cfsph.iastate.edu/DiseaseInfo/disease.php?name=glanders. Accessed: January 17, 2019.

Van Zandt KE1, Greer MT, Gelhaus HC. Glanders: an overview of infection in humans. Orphanet J Rare Dis. 2013. 8:131-138. [Medline]. [Full Text].

Spickler AR. Melioidosis. Center for Food Security & Public Health. Available at http://www.cfsph.iastate.edu/DiseaseInfo/disease.php?name=melioidosis. Accessed: January 17, 2019.

Paul Vijay Kingsley, Mark Leader, Nandika Suranjith Nagodawithana, Meghan Tipre, and Nalini Sathiakumar. Melioidosis in Malaysia: A Review of Case Reports. PLoS Negl Trop Dis. 2016. 10:e0005182. [Medline]. [Full Text].

Ramar Perumal Samy, Bradley G. Stiles, Gautam Sethi, and Lina H. K. Lim. Melioidosis: Clinical impact and public health threat in the tropics. PLoS Negl Trop Dis. 2017. 11:e0004738. [Medline]. [Full Text].

USAMRIID. Bacterial Agents. USAMRIID’s Medical Management of Biological Casualties Handbook. 8th Edition. Fort Detrick, MD: US Army Medical Research Institute of Infectious Diseases; 2014. 51-58. [Full Text].

Bondi SK, Goldberg JB. Strategies toward vaccines against Burkholderia mallei and Burkholderia pseudomallei. Expert Rev Vaccines. 2008 Nov. 7(9):1357-65. [Medline].

Centers for Disease Control and Prevention. Laboratory-acquired human glanders–Maryland, May 2000. MMWR Morb Mortal Wkly Rep. 2000 Jun 23. 49(24):532-5. [Medline].

Duplessis C, Maguire JD. Melioidosis masquerading as community-acquired pneumonia: a case report demonstrating efficacy of intrapleural fibrinolytic therapy. J Travel Med. 2009 Jan-Feb. 16(1):74-7. [Medline].

Benoit TJ, Blaney DD, Gee JE, Elrod MG, Hoffmaster AR, Doker TJ, et al. Melioidosis Cases and Selected Reports of Occupational Exposures to Burkholderia pseudomallei – United States, 2008-2013. MMWR Surveill Summ. 2015 Jul 3. 64 Suppl 5:1-9. [Medline]. [Full Text].

Yip TW, Hewagama S, Mayo M, Price EP, Sarovich DS, Bastian I, et al. Endemic melioidosis in residents of desert region after atypically intense rainfall in central Australia, 2011. Emerg Infect Dis. 2015 Jun. 21 (6):1038-40. [Medline].

Overtoom R, Khieu V, Hem S, Cavailler P, Te V, Chan S, et al. A first report of pulmonary melioidosis in Cambodia. Trans R Soc Trop Med Hyg. 2008 Dec. 102 Suppl 1:S21-5. [Medline].

Katangwe T, Purcell J, Bar-Zeev N, et al. Human melioidosis, Malawi, 2011. Emerg Infect Dis. 2013 Jun. 19(6):981-4. [Medline]. [Full Text].

Valsalan R, Seshadri S, Pandit VR. Melioidosis masquerading as enteric fever. Trans R Soc Trop Med Hyg. 2008 Dec. 102 Suppl 1:S117-8. [Medline].

Mukhopadhyay C, Chawla K, Krishna S, Nagalakshmi N, Rao SP, Bairy I. Emergence of Burkholderia pseudomallei and pandrug-resistant non-fermenters from southern Karnataka, India. Trans R Soc Trop Med Hyg. 2008 Dec. 102 Suppl 1:S12-7. [Medline].

Centers for Disease Control and Prevention. Glanders. CDC.gov. Available at https://www.cdc.gov/glanders/index.html. October 20, 2017; Accessed: March 15, 2018.

Montgomery S. Burkholderia pseudomallei (melioidosis) Attack. Ciottone GR, Anderson PD, Auf Der Heide E, Darling RG, Jacoby I, Noji E, Suner S, eds. Disaster Medicine. 3rd ed. Philadelphia, PA: Mosby/Elsevier; 2006. chap 115; 650-652.

Centers for Disease Control and Prevention. Melioidosis. CDC.gov. Available at https://www.cdc.gov/melioidosis/index.html. August 8, 2017; Accessed: March 15, 2018.

Muttarak M, Peh WC, Euathrongchit J, Lin SE, Tan AG, Lerttumnongtum P, et al. Spectrum of imaging findings in melioidosis. Br J Radiol. 2008 Dec 19. [Medline].

Estes DM, Dow SW, Schweizer HP, Torres AG. Present and future therapeutic strategies for melioidosis and glanders. Expert Rev Anti Infect Ther. 2010 Mar. 8(3):325-38. [Medline]. [Full Text].

Goodyear A, Kellihan L, Bielefeldt-Ohmann H, Troyer R, Propst K, Dow S. Protection From Pneumonic Burkholderia Infection by Inhalational Immunotherapy. Infect Immun. 2009 Jan 29. [Medline].

Titball RW, Burtnick MN, Bancroft GJ, Brett P. Burkholderia pseudomallei and Burkholderia mallei vaccines: Are we close to clinical trials?. Vaccine. 2017 Oct 20. 35 (44):5981-5989. [Medline].

Johnson MM, Ainslie KM. Vaccines for the Prevention of Melioidosis and Glanders. Curr Trop Med Rep. 2017 Sep. 4 (3):136-145. [Medline].

Lowe CW, Satterfield BA, Nelson DB, Thiriot JD, Heder MJ, March JK, et al. A Quadruplex Real-Time PCR Assay for the Rapid Detection and Differentiation of the Most Relevant Members of the B. pseudomallei Complex: B. mallei, B. pseudomallei, and B. thailandensis. PLoS One. 2016. 11 (10):e0164006. [Medline]. [Full Text].

Paul P Rega, MD, FACEP Assistant Professor, Department of Public Health and Preventive Medicine, Assistant Professor, Emergency Medicine Residency Program, Department of Emergency Medicine, The University of Toledo College of Medicine; Director of Emergency Medicine Education and Disaster Management, OMNI Health Services

Paul P Rega, MD, FACEP is a member of the following medical societies: American College of Emergency Physicians

Disclosure: Nothing to disclose.

Francisco Talavera, PharmD, PhD Adjunct Assistant Professor, University of Nebraska Medical Center College of Pharmacy; Editor-in-Chief, Medscape Drug Reference

Disclosure: Received salary from Medscape for employment. for: Medscape.

Duane C Caneva, MD, MSc Senior Medical Advisor to Customs and Border Protection, Department of Homeland Security (DHS) Office of Health Affairs; Federal Co-Chair, Health, Medical, Responder Safety Subgroup, Interagency Board (IAB)

Disclosure: Nothing to disclose.

Jerry L Mothershead, MD Medical Readiness Consultant, Medical Readiness and Response Group, Battelle Memorial Institute; Advisor, Technical Advisory Committee, Emergency Management Strategic Healthcare Group, Veteran’s Health Administration; Adjunct Associate Professor, Department of Military and Emergency Medicine, Uniformed Services University of the Health Sciences

Jerry L Mothershead, MD is a member of the following medical societies: American College of Emergency Physicians, National Association of EMS Physicians

Disclosure: Nothing to disclose.

The authors and editors of Medscape Reference gratefully acknowledge the contributions of previous authors, Dahna Batts, MD, Alan H Hall, MD, and Thomas W McGovern, MD, to the development and writing of this article.

CBRNE – Glanders and Melioidosis

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