Coccidioidomycosis
Coccidioidomycosis | |
---|---|
Histopathological changes in a case of coccidioidomycosis of the lung showing a large fibrocaseous nodule. | |
Classification and external resources | |
Specialty | Infectious disease |
ICD-10 | B38 |
ICD-9-CM | 114 |
MedlinePlus | 001322 |
eMedicine | med/103 ped/423 |
MeSH | D003047 |
Coccidioidomycosis (/kɒkˌsɪdiɔɪdoʊmaɪˈkoʊsɪs/, kok-sid-ee-oy-doh-my-KOH-sis), commonly known as cocci,[1] "valley fever",[1] as well as "California fever",[2] "desert rheumatism",[2] and "San Joaquin Valley fever",[2] is a mammalian fungal disease caused by Coccidioides immitis or Coccidioides posadasii.[3] It is endemic in certain parts of Arizona, California, Nevada, New Mexico, Texas, Utah, and northern Mexico.[4]
C. immitis is a dimorphic saprophytic fungus that grows as a mycelium in the soil and produces a spherule form in the host organism. It resides in the soil in certain parts of the southwestern United States, most notably in California and Arizona.[1] It is also commonly found in northern Mexico, and parts of Central and South America.[1] C. immitis is dormant during long dry spells, then develops as a mold with long filaments that break off into airborne spores when it rains. The spores, known as arthroconidia, are swept into the air by disruption of the soil, such as during construction, farming, or an earthquake.[5]
Coccidioidomycosis is a common cause of community acquired pneumonia in the endemic areas of the United States.[1] Infections usually occur due to inhalation of the arthroconidial spores after soil disruption.[1] The disease is not contagious.[1] In some cases the infection may recur or be permanent.
Signs and symptoms
An estimated 60% of people infected with the fungi responsible for coccidioidomycosis have minimal to no symptoms, while 40% will have a range of possible clinical symptoms.[1][6] Of those who do develop symptoms, the primary infection is most often respiratory, with symptoms resembling bronchitis or pneumonia that resolve over a matter of a few weeks. In endemic regions, coccidioidomycosis is responsible for 20% of case of community acquired pneumonia.[6] Notable coccidioidomycosis signs and symptoms include a profound feeling of tiredness, fever, cough, headaches, rash, muscle pain, and joint pain.[1] Fatigue can persist for many months after initial infection.[6] The classic triad of coccidioidomycosis known as "desert rheumatism" includes the combination of fever, joint pains, and erythema nodosum.[1]
3% to 5% of infected individuals do not recover from the initial acute infection and develop a chronic infection. This can take the form of chronic lung infection or widespread disseminated infection (affecting the tissues lining the brain, soft tissues, joints, and bone). Chronic infection is responsible for most of the morbidity and mortality. Chronic fibrocavitary disease is manifested by cough, sputum, fevers, night sweats and weight loss.[6] Vertebral disease can cause osteomyelitis and meningitis which may occur months to years after initial infection. Severe lung disease may develop in HIV-infected persons.[7]
Types
After Coccidioides infection, Coccidioidomycosis begins with Valley fever, which is its initial acute form. If left untreated, it can progress to the chronic form and then to disseminated Coccidioidomycosis. Therefore, Coccidioidomycosis may be divided into the following types:[8]
- Acute coccidioidomycosis, sometimes described in literature as primary pulmonary coccidioidomycosis
- Chronic coccidioidomycosis
- Disseminated coccidioidomycosis, which includes primary cutaneous coccidioidomycosis
Complications
Serious complications may occur in patients with weakened immune systems, including severe pneumonia with respiratory failure and bronchopleural fistulas requiring resection, lung nodules, and possible disseminated form, where the infection spreads throughout the body.[6] The disseminated form of Coccidioidomycosis can devastate the body, causing skin ulcers, abscesses, bone lesions, swollen joints with severe pain, heart inflammation, urinary tract problems, and inflammation of the brain's lining, which can lead to death.[9]
Cause
It must rain first to start the cycle of initial growth of the fungus underneath the soil.[10] In soil (and in agar media), coccidioides exists in filament form. It forms hyphae in both horizontal and vertical directions. Over a prolonged dry period, cells within hyphae degenerate to form alternating barrel-shaped cells (arthroconidia). Arthroconidia are light-weight and carried by air currents. This happens when the soil is disturbed often by clearing trees, construction and farming. As the population grows, so have all these industries causing a potential cascade effect. The more land you clear, the more arid the soil, the riper the environment for coccidioides.[11] These spores can be easily inhaled without the person knowing. On arriving in alveoli, they enlarge in size and internal septations are developed. This division of cells is made possible by the optimal temperature inside the body.[12] These septations are called spherules. Septations develop and form endospores, which are smaller pieces. Rupture of spherules release these endospores, which in turn repeat the cycle and spread the infection locally. Nodules can form in lungs surrounding these spherules. When they rupture, they release their contents into bronchi, forming thin-walled cavities. These cavities can result in symptoms like characteristic chest pain, coughing up blood, and persistent cough. In individuals with a weakened immune system, the infection can spread through the blood. On rare occasion it can enter the body through a break in the skin causing infection.[12]
Diagnosis
Coccidioidomycosis diagnosis relies on a combination of an infected person's signs and symptoms, findings on radiographic imaging, and laboratory results.[1] The disease is commonly misdiagnosed as bacterial community-acquired pneumonia.[1] The fungal infection can be demonstrated by microscopic detection of diagnostic cells in body fluids, exudates, sputum and biopsy-tissue by methods of Papanicolaou or Grocott's methenamine silver staining. These stains can demonstrate spherules and surrounding inflammation.
With specific nucleotide primers, C.immitis DNA can be amplified by polymerase chain reaction (PCR). It can also be detected in culture by morphological identification or by using molecular probes that hybridize with C.immitis RNA. C. immitis and C. posadasii cannot be distinguished on cytology or by symptoms, but only by DNA PCR.
An indirect demonstration of fungal infection can be achieved also by serologic analysis detecting fungal antigen or host IgM or IgG antibody produced against the fungus. The available tests include the tube-precipitin (TP) assays, complement fixation assays, and enzyme immunoassays. TP antibody is not found in cerebrospinal fluid (CSF). TP antibody is specific and is used as confirmatory test, while ELISA is sensitive and thus used for screening.
If the meninges are affected, CSF will show abnormally low glucose levels in CSF, a decreased level of protein in the CSF, and lymphocytic pleocytosis. Rarely, CSF eosinophilia is present.
Imaging
Chest x-rays rarely demonstrate nodules or cavities in the lungs but these images commonly demonstrate lung opacification, pleural effusions, or enlargement of lymph nodes associated with the lungs.[1] Computed tomography scans of the chest are better able to detect these changes than chest x-rays.[1]
Treatment
Significant disease develops in less than 5% of those infected and typically occurs in those with a weakened immune system.[13] Mild asymptomatic cases often do not require any treatment and the symptoms will go away within a few months. Those with severe symptoms may warrant anti-fungal therapy, which usually requires 3–6 months of treatment.[14] There is a lack of prospective studies that examine optimal anti-fungal therapy for coccidioidomycosis.
On the whole, oral fluconazole and intravenous amphotericin B are used in progressive or disseminated disease, or in immunocompromised individuals.[13] Amphotericin B used to be the only available treatment,[15] although now there are alternatives, including itraconazole or ketoconazole may be used for milder disease.[16] Fluconazole is the preferred medication for coccidioidal meningitis, due to its penetration into CSF.[3] Intrathecal or intraventricular amphotericin B therapy is used if infection persists after fluconazole treatment.[13] Itraconazole is used for cases that involve treatment of infected person's bones and joints. The antifungal medications posaconazole and voriconazole have also been used to treat coccidioidomycosis. Because the symptoms of valley fever are similar to the common flu and other respiratory diseases, it is important for public health professionals to be aware of the rise of valley fever and the specifics of diagnosis. Greyhounds often get valley fever as well, and their treatment regimen involves 6–12 months of Ketoconazole, to be taken with food.[17]
Prevention
Preventing valley fever is challenging because it’s hard to avoid breathing in the fungus should it be present, however, the Public Health impact of the disease is essential to understand in areas where the fungi are endemic. Enhancing surveillance of Coccidiodomycosis is key to preparedness in the medical field in addition to improving diagnostics for early infections.[15] Currently there are no completely effective preventive measures available for people who live or travel through Valley fever endemic areas. Recommended preventive measures include avoiding airborne dust or dirt, but this does not guarantee protection against infection. People in certain occupations may be advised to wear face masks.[18] The use of air filtration indoors is also a method to use, in addition to keeping skin injuries clean and covered to avoid skin infection.
In 1998-2011, there were 111,117 cases of coccidioidomycosis in the U.S. that were logged into the National Notifiable Diseases Surveillance System (NNDSS).[19] Since many U.S. states do not require reporting of coccidioidomycosis, the actual numbers can be higher. The United States' Centers for Disease Control and Prevention (CDC) called the disease a "silent epidemic" and acknowledged that there is no proven anticoccidioidal vaccine available.[20] Studies done in the past show that the cost benefit of a vaccine is most notable among infants, teens, and immigrant adults, with negative cost results among all senior demographics.[21]
Raising both surveillance and awareness of the disease while medical researchers are developing a human vaccine can positively contribute towards prevention efforts.[22][23] Research demonstrates that patients from endemic areas who are aware of the disease are most likely to request diagnostic testing for coccidioidomycosis.[24] Presently, Meridian Bioscience manufactures the so-called EIA test to diagnose the Valley fever, which however is known for producing a fair quantity of false positives. Currently, recommended prevention measures can include type-of-exposure-based respirator protection for persons engaged in agriculture, construction and others working outdoors in the endemic areas.[25][26] Dust control measures such as planting grass and wetting the soil, and also limiting exposure to dust storms are advisable for residential areas in endemic regions.[27]
Epidemiology
Coccidioidomycosis is endemic to the western hemisphere between 40°N and 40°S. The ecological niches are characterized by hot summers and mild winters with an annual rainfall of 10–50 cm.[28] The species are found in alkaline sandy soil, typically 10–30 cm below the surface. In harmony with the mycelium life cycle, incidence increases with periods of dryness after a rainy season; this phenomenon, termed "grow and blow", refers to growth of the fungus in wet weather, producing spores which are spread by the wind during succeeding dry weather. While the majority of cases are observed in the endemic region, cases reported outside the area are generally visitors, who contact the infection and return to their native areas before becoming symptomatic.
North America
In the United States, C. Immitis is endemic to southern and central California with the highest presence in the San Joaquin Valley. C. posadassi is most prevalent in Arizona although it can be found in a wider region spanning from Utah, New Mexico, Texas, and Nevada. An estimated 150,000 infections occur annually, with 25,000 new infections occurring every year. The incidence of coccidioidomycosis in the United States in 2011 (42.6 per 100,000) was almost ten times higher than the incidence reported in 1998 (5.3 per 100,000). In area where it is most prevalent, the infection rate is 2-4%.[29]
Incidence varies widely across the west and southwest. In Arizona, for instance, in 2007, there were 3,450 cases in Maricopa County, which in 2007 had an estimated population of 3,880,181[30] for an incidence of approximately 1 in 1,125.[31] In contrast, though southern New Mexico is considered an endemic region, there were 35 cases in the entire state in 2008, and 23 in 2007,[31] in a region that had an estimated 2008 population of 1,984,356[32] for an incidence of approximately 1 in 56,695.
Infection rates vary greatly by county, and although population density is important, so are other factors that have not been proven yet. Greater construction activity may disturb spores in the soil. In addition, the effect of altitude on fungi growth and morphology has not been studied, and altitude can range from sea level to 10,000 feet or higher across California, Arizona, Texas and New Mexico.
In California from 2000 to 2007, there were 16,970 reported cases (5.9 per 100,000 people) and 752 deaths of the 8,657 people hospitalized. The highest incidence was in the San Joaquin Valley with 76% of the 16,970 cases (12,855) occurring in the area.[33] Following the 1994 Northridge earthquake, there was a sudden increase of cases in the areas affected by the quake, at a pace of over 10 times baseline.[34]
There was an outbreak in the summer of 2001 in Colorado, away from where the disease was considered endemic. A group of archeologists visited Dinosaur National Monument, and eight members of the crew, along with two National Park Service workers were diagnosed with Valley fever.[35]
California state prisons, beginning in 1919, have been particularly affected by Coccidioidomycosis. In 2005 and 2006, the Pleasant Valley State Prison near Coalinga and Avenal State Prison near Avenal on the western side of the San Joaquin Valley had the highest incidence in 2005, of at least 3,000 per 100,000.[36] The receiver appointed in Plata v. Schwarzenegger issued an order in May 2013 requiring relocation of vulnerable populations in those prisons.[37] The incidence rate has been increasing, with rates as high as 7% during 2006-2010. The cost of care and treatment is $23 million in California prisons. A lawsuit was filed against the state in 2014 on behalf of 58 inmates stating that the Avenal and Pleasant valley state prisons did not take preventative steps to prevent infections.[38]
Risk factors
There are several populations that have a higher risk for contracting coccidioidomycosis and developing the advanced disseminated version of the disease. Populations with exposure to the airborne arthroconidia working in agriculture and construction have a higher risk. Outbreaks have also been linked to earthquakes, windstorms and military training exercises where the ground is disturbed.[39] Historically an infection is more likely to occur in males than females, although this could be attributed to occupation rather than gender specific. Women who are pregnant and immediately postpartum are at a high risk of infection and dissemination. There is also an association between stage of pregnancy and severity of the disease, with third trimester women being more likely to develop dissemination. Presumably this is related to highly elevated hormonal levels, which stimulate growth and maturation of spherules and subsequent release of endospores.[40] Ethnic populations are more susceptible to disseminated coccioidomycosis. The risk of dissemination is 175 times greater in Filipinos and 10 times greater in African Americans than non-Hispanic whites.[41] Individuals with a weakened immune system are also more susceptible to the disease. In particular, individuals with HIV and diseases that impair T-cell function. Individuals with pre-existing conditions such as diabetes are also at a higher risk. Age also has an impact on the severity of the disease, with more than one third of deaths being in the 65-84 age group.[42]
Other animals
An animal infected with valley fever cannot transmit the disease to other animals. In dogs, the most common symptom of coccidioidomycosis is a chronic cough which can be dry or moist. Other symptoms include fever (in approximately 50% of cases), weight loss, anorexia, lethargy, and depression. The disease can disseminate throughout the dog's body, most commonly causing osteomyelitis (infection of the bone marrow) which leads to lameness. Dissemination can cause other symptoms, depending on which organs are infected. If the fungus infects the heart or pericardium, it can cause heart failure and death.[43]
In cats, symptoms may include skin lesions, fever, and loss of appetite, with skin lesions being the most common.[44]
Other species in which Valley fever has been found include livestock such as cattle and horses; llamas; marine mammals, including sea otters; zoo animals such as monkeys and apes, kangaroos, tigers, etc.; and wildlife native to the geographic area where the fungus is found, such as cougars, skunks, and javelinas.[45]
History
The first case of what was later named Coccidioidomycosis was described in 1892 in Buenos Aires by Alejandro Posadas, a medical intern at the Hospital de Clínicas "José de San Martín".[46] Posados established an infectious character of the disease after being able to transfer it in laboratory conditions to lab animals.[47] In the U.S., E. Rixford, a physician from a San Francisco hospital, and T. C. Gilchrist, a pathologist at Johns Hopkins Medical School, became early pioneers of clinical studies of the infection.[48] They decided that the causative organism was a Coccidia-type protozoan and named it Coccidioides immitis (resembling Coccidia, not mild).
During the next several decades it became clear that the etiological agent of the disease that was at first called Coccidioides infection and later Coccidioidomycosis[49] was a fungal pathogen, and Coccidioidomycosis was also distinguished from Histoplasmosis and Blastomycosis. Further, C. immitis was identified as the culprit of respiratory disorders previously called San Joaquin fever, Desert fever, and Valley fever, and a serum precipitin test was developed by Charles E. Smith that was able to detect an acute form of the infection. In retrospect, Smith played a major role in both medical research and raising awareness about Coccidioidomycosis,[50] especially when he became dean of the School of Public Health at the University of California at Berkeley in 1951.
C. immitis was considered by the United States during the 1950s and 1960s as a potential biological weapon.[51] The explored strain was designated with the military symbol OC, and initial expectations were for its employment as a human incapacitant. Medical research suggested that OC might have had some lethal effects on the populace, and C. immitis started to be classified by the authorities as a threat to public health. However, C. immitis was never weaponized, and most of the military research in the mid-1960s was concentrated on developing a human vaccine. Currently, it is not on the U.S. Department of Health and Human Services' (HHS)[52] or Centers for Disease Control and Prevention's[53] list of select agents and toxins.
In 2002, Coccidioides posadasii was identified as genetically distinct from C. immitis despite their morphologic similarities and can also cause coccidioidomycosis.[54]
Research
As of 2013, there is no vaccine available to prevent disease from infection with Coccidioides immitis or Coccidioides posadasii, but efforts to develop such a vaccine are underway.[55]
Additional images
See also
- Coccidioides
- Coccidioides immitis
- Coccidioides posadasii
- Zygomycosis
- Medical geology
- List of cutaneous conditions
- Thunderhead, a 1998 novel by Douglas Preston and Lincoln Child which uses the fungus and illness as a central plot point.
References
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- 1 2 3 Rapini, Ronald P.; Bolognia, Jean L.; Jorizzo, Joseph L. (2007). Dermatology: 2-Volume Set. St. Louis: Mosby. ISBN 1-4160-2999-0.
- 1 2 Nguyen C, Barker BM, Hoover S, Nix DE, Ampel NM, Frelinger JA, Orbach MJ, Galgiani JN (July 2013). "Recent advances in our understanding of the environmental, epidemiological, immunological, and clinical dimensions of coccidioidomycosis". Clin Microbiol Rev 26 (3): 505–25. doi:10.1128/CMR.00005-13. PMC 3719491. PMID 23824371.
- ↑ Hector R, Laniado-Laborin R (2005). "Coccidioidomycosis—A Fungal Disease of the Americas". PLoS Med 2 (1): e2. doi:10.1371/journal.pmed.0020002. PMC 545195. PMID 15696207.
- ↑ Schneider E, Hajjeh RA, Spiegel RA; et al. (1997). "A coccidioidomycosis outbreak following the Northridge, Calif, earthquake". JAMA 277 (11): 904–8. doi:10.1001/jama.277.11.904. PMID 9062329.
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- ↑ Ampel N (2005). "Coccidioidomycosis in persons infected with HIV type 1". Clin Infect Dis 41 (8): 1174–8. doi:10.1086/444502. PMID 16163637.
- ↑ James, William D.; Berger, Timothy G.; et al. (2006). Andrews' Diseases of the Skin: clinical Dermatology. Saunders Elsevier. ISBN 0-7216-2921-0.
- ↑ Galgiani J. N. Coccidioidomycosis. In: Cecil, Russell L., Lee Goldman, and D. A. Ausiello. Cecil Medicine. Philadelphia: Saunders Elsevier, 2007.
- ↑ Kolivras, K. & Comrie, A. (2003). "Modeling valley fever (coccidioidomycosis) incidence on the basis of climate conditions." International Journal of Biometeorology, 47,(2); 87-101.
- ↑ "Mayo Clinic". Valley Fever. Mayo Clinic. May 27, 2015. Retrieved September 30, 2015.
- 1 2 "CDC". Fungal diseases: valley fever. CDC. July 20, 2015. Retrieved September 30, 2015.
- 1 2 3 Welsh O., Vera-Cabrera L., Rendon A. (November–December 2012). "Coccidioidomycosis". Clinics in dermatology 30 (6): 573–591. doi:10.1016/j.clindermatol.2012.01.003. PMID 23068145.
- ↑ Galgiani, John N., Ampel, Neil M. , Blair, Janis E.; et al. "Coccidioidomycosis" (PDF). Practice Guidelines for the Treatment of Coccidioidomycosis. Infectious Diseases Society of America. Retrieved 10 July 2013.
- 1 2 Hector, Richard F.; Rutherford, George W.; Tsang, Clarisse A.; Erhart, Laura M.; McCotter, Orion; Anderson, Shoana M.; Komatsu, Kenneth; Tabnak, Farzaneh; Vugia, Duc J. (2011-04-01). "The Public Health Impact of Coccidioidomycosis in Arizona and California". International Journal of Environmental Research and Public Health 8 (4): 1150–1173. doi:10.3390/ijerph8041150. ISSN 1661-7827. PMC 3118883. PMID 21695034.
- ↑ Barron MA and Madinger NE (November 18, 2008). "Opportunistic Fungal Infections, Part 3: Cryptococcosis, Histoplasmosis, Coccidioidomycosis, and Emerging Mould Infections". Infections in Medicine.
- ↑ Rubensohn, Mark; Stack, Suzanne (2003-02-01). "Coccidiomycosis in a dog". The Canadian Veterinary Journal 44 (2): 159–160. ISSN 0008-5286. PMC 340059. PMID 12650050.
- ↑ "Risk factors". Valley Fever Center for Excellence.
- ↑ "Increase in Reported Coccidioidomycosis—United States, 1998–2011". Morbidity and Mortality Weekly Report (MMWR). Centers for Disease Control and Prevention. Retrieved 6 July 2013.
- ↑ "Valley Fever: Awareness is Key". CDC Features. Centers for Disease Control and Prevention. Retrieved 6 July 2013.
- ↑ Barnato, A. E.; Sanders, G. D.; Owens, D. K. (2001-01-01). "Cost-effectiveness of a potential vaccine for Coccidioides immitis.". Emerging Infectious Diseases 7 (5): 797–806. doi:10.3201/eid0705.010005. ISSN 1080-6040. PMC 2631863. PMID 11747691.
- ↑ Cole G.T., Xue J.M., Okeke C.N., at al. (June 2004). "A vaccine against coccidioidomycosis is justified and attainable". Medical mycology 42 (3): 189–216. doi:10.1080/13693780410001687349. PMID 15283234.
- ↑ "Valley Fever Vaccine Project" (PDF). Archived from the original (PDF) on February 1, 2014. Retrieved 11 July 2013.
- ↑ Tsang C.A., Anderson S.M., Imholte S.B.; et al. (2010). "Enhanced surveillance of coccidioidomycosis, Arizona, USA, 2007–2008". Emerging Infectious Diseases 16 (11): 1738–44. doi:10.3201/eid1611.100475.
- ↑ Das R., McNary J., Fitzsimmons K.; et al. (May 2012). "Occupational coccidioidomycosis in California: outbreak investigation, respirator recommendations, and surveillance findings". Journal of occupational and environmental medicine 54 (5): 564–571. doi:10.1097/JOM.0b013e3182480556. PMID 22504958.
- ↑ "Coccidioidomycosis (Valley Fever)". Health Information: Diseases & Conditions. California Department of Public Health. Retrieved 11 July 2013.
- ↑ "Coccidioidomycosis: Prevention" (PDF). Acute Communicable Disease Control Annual Morbidity Reports, Los Angeles County, 2002-2010. Retrieved 12 July 2013.
- ↑ Brown, Jennifer. "Coccidioidomycosis: epidemiology". NCBI. Retrieved June 25, 2013.
- ↑ Hospenthal, Duane. "Coccidioidomycosis". Medscape. Retrieved 2015-10-18.
- ↑ U.S. Census Bureau, State & County QuickFacts
- 1 2 "Number of Reported Cases of Selected Notifiable Diseases by Category for each County, Arizona, 2007" (PDF). Arizona Department of Health Services. Retrieved 10 July 2013.
- ↑ New Mexico Intercensal Population Estimates from the U.S. Census Bureau
- ↑ "Increase in Coccidioidomycosis: California, 2000-2007". Morbidity and Mortality Weekly Report (MMWR) 58 (5): 105–109. February 13, 2009.
- ↑ "Coccidioidmycosis Outbreak". USGS Landslide Hazards Program. Archived from the original on 2014-02-02.
- ↑ "Coccidioidomycosis in Workers at an Archeologic Site ---Dinosaur National Monument, Utah, June--July 2001". Morbidity and Mortality Weekly Report (MMWR), 50(45), p. 1005-1008. Centers for Disease Control and Prevention (CDC). November 16, 2001. Retrieved 10 July 2013.
- ↑ Pappagianis, Demosthenes; Coccidioidomycosis Serology Laboratory (September 2007). "Coccidioidomycosis in California State Correctional Institutions". Annals of the New York Academy of Sciences 1111: 103–11. doi:10.1196/annals.1406.011. PMID 17332089.
- ↑ Rachel Cook; Rebecca Plevin (May 7, 2013). "Some Prison Inmates to Be Moved Out of Valley Fever Hot Spots". Voice of OC. Retrieved May 9, 2013.
- ↑ "CDC Says Calif. Inmates Should Be Tested for Valley Fever Immunity". California HealthLine.
- ↑ Brown, Jennifer. "Coccidioidomycosis: epidemiology". National Center for Biotechnology Information.
- ↑ Shehab, Ziad M. (2010). "Coccidioidomycosis". Advances in Pediatrics. doi:10.1016/j.yapd.2010.08.008.
- ↑ Hospenthal, Duane. "Coccidioidomycosis". Medscape.
- ↑ Cook, Rachel. "Just One Breath: More People Dying from Valley Fever – Especially Those With Chronic Disease, Study Shows". Reporting on Health.
- ↑ Graupmann-Kuzma, Angela; Valentine, Beth A.; Shubitz, Lisa F.; Dial, Sharon M.; Watrous, Barbara; Tornquist, Susan J. (2008-09-01). "Coccidioidomycosis in Dogs and Cats: A Review". Journal of the American Animal Hospital Association 44 (5): 226–235. doi:10.5326/0440226. ISSN 0587-2871.
- ↑ Greene, Russell T.; Troy, Gregory C. (1995-03-01). "Coccidioidomycosis in 48 Cats: A Retrospective Study (1984–1993)". Journal of Veterinary Internal Medicine 9 (2): 86–91. doi:10.1111/j.1939-1676.1995.tb03277.x. ISSN 1939-1676.
- ↑ "Valley Fever Center for Excellence: Valley Fever in Other Animal Species". University of Arizona.
- ↑ Posadas A. Un nuevo caso de micosis fungoidea con posrospemias. Annales Cir. Med. Argent. (1892), Volume 15, p. 585-597.
- ↑ Hirschmann, Jan V. (2007). "The Early History of Coccidioidomycosis: 1892–1945". Clinical Infectious Diseases 44 (9): 1202–1207. doi:10.1086/513202. PMID 17407039.
- ↑ Rixford E., Gilchrist T. C. Two cases of protozoan (coccidioidal) infection of the skin and other organs. Johns Hopkins Hosp Rep 1896; 10:209-268.
- ↑ Dickson, EC; Gifford, MA (1 November 1938). "Coccidioides infection (coccidioidomycosis). ii. The primary type of infection". Archives of Internal Medicine 62 (5): 853–71. doi:10.1001/archinte.1938.00180160132011.
- ↑ Smith, CE (Jun 1940). "Epidemiology of Acute Coccidioidomycosis with Erythema Nodosum ("San Joaquin" or "Valley Fever").". American journal of public health and the nation's health 30 (6): 600–11. doi:10.2105/AJPH.30.6.600. PMC 1530901. PMID 18015234.
- ↑ Ciottone, Gregory R. Disaster Medicine. Philadelphia, PA: Mosby Elsevier, 2006, pp. 726-128.
- ↑ "HHS select agents and toxins" (PDF). Code of Federal Regulations (CFR), Title 42 - Public Health. Office of the Federal Register. Archived from the original (PDF) on October 20, 2013. Retrieved 11 July 2013.
- ↑ "Select Agents and Toxins List" (PDF). CDC. December 4, 2012. Archived from the original (PDF) on February 28, 2013. Retrieved 11 July 2013.
- ↑ Fisher, M. C., Koenig, G. L., White, T. J., & Taylor, J. W (2002). "Molecular and phenotypic description of Coccidioides posadasii sp. nov., previously recognized as the non-California population of Coccidioides immitis" (PDF). Mycologia 94 (1): 73–84. doi:10.2307/3761847. PMID 21156479.
- ↑ Yoon HJ, Clemons KV (July 2013). "Vaccines against Coccidioides". The Korean journal of internal medicine 28 (4): 403–7. doi:10.3904/kjim.2013.28.4.403. PMC 3712146. PMID 23864796.
External links
Wikimedia Commons has media related to Coccidioidomycosis. |
- U.S. Centers for Disease Control and Prevention page on Coccidioidomycosis
- Medline Plus Entry for Coccidioidomycosis
- Radiology of Lesions in Valley Fever
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