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Paracoccidioidomycosis

February 15, 2024

Paracoccidioidomycosis (PCM), also known as South American blastomycosis, is a fungal infection that can occur as a mouth and skin type, lymphangitic type, multi-organ involvement type (particularly lungs), or mixed type.[1][6] If there are mouth ulcers or skin lesions, the disease is likely to be widespread.[1] There may be no symptoms, or it may present with fever, sepsis, weight loss, large glands, or a large liver and spleen.[4][7]

Paracoccidioidomycosis
Other namesSouth American blastomycosis,[1] Brazilian blastomycosis,[2] Lutz-Splendore-de Almeida disease,[3]
Paracoccidioides histopathology
SpecialtyInfectious disease
SymptomsFever, sepsis, weight loss, large glands, large liver and spleen,[4] mouth ulcers, skin lesions.[5]
TypesMucocutaneous, lymphatic, multi-organ[1]
CausesParacoccidioides brasiliensis[4]
Diagnostic methodSampling of blood, sputum, or skin[4]
Differential diagnosisTuberculosis, leukaemia, lymphoma[4]
TreatmentAntifungal medication[6]
MedicationItraconazole, amphotericin B,[6] trimethoprim/sulfamethoxazole[7]
Deaths200 deaths per year in Brazil[1]

The cause is fungi in the genus Paracoccidioides, including Paracoccidioides brasiliensis and Paracoccidioides lutzii,[8] acquired by breathing in fungal spores.[6]

Diagnosis is by sampling of blood, sputum, or skin.[4] The disease can appear similar to tuberculosis, leukaemia, and lymphoma[4] Treatment is with antifungals; itraconazole.[1][7] For severe disease, treatment is with amphotericin B followed by itraconazole, or trimethoprim/sulfamethoxazole as an alternative.[1][7]

It is endemic to Central and South America,[9] and is considered a type of neglected tropical disease.[8] In Brazil, the disease causes around 200 deaths per year.[1]

Signs and symptoms edit

 
Lesions due to Paracoccidioidomycosis on the face of a Brazilian child

Asymptomatic lung infection is common, with fewer than 5% of infected individuals developing clinical disease.[10]

It can occur as a mouth and skin type, lymphangitic type, multi-organ involvement type (particularly lungs), or mixed type.[1][6] If there are mouth ulcers or skin lesions, the disease is likely to be widespread.[1] There may be no symptoms, or it may present with fever, sepsis, weight loss, large glands, or a large liver and spleen.[4][7]

Two presentations are known, firstly the acute or subacute form, which predominantly affects children and young adults,[11] and the chronic form, predominantly affecting adult men.[12] Most cases are infected before age 20, although symptoms may present many years later.[13]

Juvenile (acute/subacute) form edit

The juvenile, acute form is characterised by symptoms, such as fever, weight loss and feeling unwell together with enlarged lymph nodes and enlargement of the liver and spleen.[14][15][16] This form is most often disseminated, with symptoms manifesting depending on the organs involved.[14] Skin and mucous membrane lesions are often present,[17] and bone involvement may occur in severe cases.[14] This acute, severe presentation may mimic tuberculosis, lymphoma or leukaemia.[17]

Adult (chronic) form edit

The chronic form presents months to years after the initial infection occurs and most frequently presents with dry cough and shortness of breath.[10] Other symptoms include excess salivation, difficulty swallowing, and difficulties with voice control.[14] Upper respiratory tract mucosal lesions may be present, as well as increased mucus production and coughing up blood.[18] Both pulmonary and extrapulmonary involvement is common.[14]

Up to 70% of cases have mucosal involvement, with lesions often found in the mouth, oropharynx, larynx, and palate. Classic lesions are superficial painful granular ulcers, with small spots of bleeding.[15]

Cause edit

Paracoccidioidomycosis is caused by two species of fungi that can exist as a mold or yeast depending on temperature, P. brasiliensis and P. lutzii.[19] In protected soil environments, near water sources, that are disturbed either naturally or by human activity, P. brasiliensis has been epidemiologically observed (although not isolated).[20] A known animal carrier is the armadillo.[13] In the natural environment, the fungi are found as filamentous structures, and they develop infectious spores known as conidia.[13]

Human to human transmission has never been proven.[21]

Mechanism edit

Primary infection, although poorly understood due to lack of data, is thought to occur through inhalation of the conidia through the respiratory tract, after inhaling fungal conidia produced by the mycelial form of P. brasiliensis.[14][21] This occurs predominantly in childhood and young adulthood, after exposure to agricultural activity.[13] Infection may occur through direct skin inoculation, although this is rare.[15]

After inhalation into the alveoli, there is rapid multiplication of the organism in the lung tissue, sometimes spreading via the venous and lymphatic systems.[14] Approximately 2% of people develop clinical features after the initial asymptomatic infection.[15]

The type of immune response determines the clinical manifestation of the infection, with children and HIV co-infected individuals most commonly developing the acute/subacute disseminated disease.[14] Most of those infected develop a Type 1 T-cell (Th1) mediated immune response, resulting in fibrosing alveolitis and compact granuloma formation that control fungal replication, and latent or asymptomatic infection.[13][14] It then is thought to remain dormant in residual lung lesions and mediastinal lymph nodes.[21] A deficient Th1 cell response results in the severe forms of the disease. In these individuals, granulomas do not form, and the affected person develops Th2 and Th9 responses, resulting in activation of B lymphocytes, high levels of circulating antibodies, eosinophilia, and hypergammaglobulinemia.[13]

Lung involvement subsequently occurs after a dormant phase, manifesting in upper respiratory tract symptoms, and lung infiltrates on imaging.[15] The commonest, chronic form, is almost certainly a reactivation of the disease,[15] and may develop into progressive scarring of the lungs (pulmonary fibrosis).[22]

It can cause disease in those with normal immune function, although immunosuppression increases the aggressiveness of the fungus. It rarely causes disease in fertile-age women, probably due to a protective effect of estradiol.[23]

Diagnosis edit

More than 90% of cases can be diagnoses with direct histological examination of tissue, such as sputum, bronchial lavage fluid, exudates and biopsies. Histopathological study with Gomori methenamine silver (GMS) stain or hematoxylin and eosin (H&E) stain revealing large yeast cells with translucent cell walls with multiple buds.[14]

In the juvenile form, lung abnormalities are shown in high-resolution CT scans of the lungs, whereas in the chronic form plain X-rays may show interstitial and alveolar infiltrates in the central and lower lung fields.[14]

Culture of P. brasiliensis takes between 20 and 30 days, requiring multiple samples and culture media. Initial culture can occur at room temperature, however after growth is noted, confirmation occurs by incubating at to 36-37 degrees to transform the fungus into yeast cells.[14]

Antibody detection is useful both for acute diagnosis and monitoring. Gel immunodiffusion is commonly used in endemic areas, diagnoses 95% of cases with high specificity.[14] Complement fixation allows for a measure of severity of cases by quantifying the antibody level, and is thus useful for monitoring treatment response. It is however only sensitive for 85% of cases, and cross-reacts with H. capsulatum.[14]

Differential diagnosis edit

The disease can appear similar to tuberculosis, leukaemia, and lymphoma[4]

Treatment edit

Both P. brasiliensis and P. lutzii are in-vitro susceptible to most antifungal agents, unlike other systemic fungal infections. Mild and moderate forms are treated with itraconazole for 9 to 18 months, as this has been shown to be more effective, has a shorter treatment duration and is more tolerated.[citation needed] Acidic beverages have been shown to reduce absorption of itraconazole.[13] Co-trimoxazole is a second line agent, and is preferred for those with brain involvement, and during pregnancy.[13] For severe cases, intravenous treatment with amphotericin B is indicated, for an average of 2 to 4 weeks.[13]Prednisolone prescribed at the same time may reduce inflammation during treatment.[13] Patients should be treated until stabilisation of symptoms, and increase in body weight. Advice in regards to nutritional support, as well as smoking and alcohol intake should be provided. Adrenal insufficiency, if found, is treated with corticosteroids.[24] Clinical criteria for cure includes the absence or healing of lesions, stabilisation of body weight, negative as well as negative autoantibody tests.[13] There is insufficient data to support the benefits of above drugs to treat the disease.[25]

Epidemiology edit

Paracoccidioidomycosis is endemic in rural areas of Latin America, from southern Mexico to Argentina, and is also found in Brazil, Colombia, Venezuela, Ecuador and Paraguay.[13][15] An epidemic outbreak has never been observed.[13] It has the highest prevalence of all systemic mycoses (fungal infections) in the area.[12] As many as 75% of people in endemic areas have been estimated to be infected with the asymptomatic form (up to 10 million people), with 2% developing clinically significant disease.[12] Morbidity and mortality is strongly associated with patient's socioeconomic background,[12] with most adult patients being male agricultural workers.[26] Other risk factors include smoking, alcohol use, HIV co-infection or other immunosuppression.[21] 80% of reported cases are in Brazil, in the southeast, midwest, and south, spreading in the 1990s to the Amazon area. Most of the remaining infections are in Argentina, Colombia and Venezuela.[21] Most epidemiological reports have focused on P. brasliensis, with P. lutzii epidemiology poorly understood as of 2015.[21]

Rising cases have been linked to agriculturalization and deforestation in Brazil, urbanisation to peripheral city areas with poor infrastructure, as well as increased soil and air humidity.[13][21] One Brazilian indigenous tribe, the Surui, after changing from subsistence agriculture to coffee farming showed higher infection rates than surrounding tribes.[21]

There have also been reports in non-endemic areas with the rise of eco-tourism, in the United States, Europe and Japan.[15] All reported cases were returned travellers from endemic regions.[21]

History edit

Lutz-Splendore-de Almeida disease[3] is named for the physicians Adolfo Lutz,[27] Alfonso Splendor (1871–1953), an Italo-Brazilian parasitologist[28] and Floriano Paulo de Almeida (1898–1977), a Brazilian pathologist specializing in Pathologic Mycology (Study of Infectious Fungi),[29][30] who first characterized the disease in Brazil in the early 20th century.

See also edit

References edit

  1. ^ a b c d e f g h i j James, William D.; Elston, Dirk; Treat, James R.; Rosenbach, Misha A.; Neuhaus, Isaac (2019). "13. Diseases resulting from fungi and yeasts". Andrews' Diseases of the Skin: Clinical Dermatology (13th ed.). Elsevier. pp. 313–314. ISBN 978-0-323-54753-6.
  2. ^ Rapini, Ronald P.; Bolognia, Jean L.; Jorizzo, Joseph L. (2007), Dermatology: 2-Volume Set, St. Louis: Mosby, ISBN 978-1-4160-2999-1
  3. ^ a b Lutz-Splendore-de Almeida disease at Who Named It?
  4. ^ a b c d e f g h i "ICD-11 - ICD-11 for Mortality and Morbidity Statistics". icd.who.int. Retrieved 26 June 2021.
  5. ^ Johnstone, Ronald B. (2017). "25. Mycoses and Algal infections". Weedon's Skin Pathology Essentials (2nd ed.). Elsevier. p. 451. ISBN 978-0-7020-6830-0.
  6. ^ a b c d e Barlow, Gavin; Irving, Irving; moss, Peter J. (2020). "20. Infectious diseases". In Feather, Adam; Randall, David; Waterhouse, Mona (eds.). Kumar and Clark's Clinical Medicine (10th ed.). Elsevier. p. 561. ISBN 978-0-7020-7870-5.
  7. ^ a b c d e Proia, Laurie (2020). "28. The dimorphic mycoses". In Spec, Andrej; Escota, Gerome V.; Chrisler, Courtney; Davies, Bethany (eds.). Comprehensive Review of Infectious Diseases. Elsevier. pp. 419–420. ISBN 978-0-323-56866-1.
  8. ^ a b Queiroz-Telles, Flavio; Fahal, Ahmed Hassan; Falci, Diego R; Caceres, Diego H; Chiller, Tom; Pasqualotto, Alessandro C (November 2017). "Neglected endemic mycoses". The Lancet Infectious Diseases. 17 (11): e367–e377. doi:10.1016/S1473-3099(17)30306-7. PMID 28774696.(subscription required)
  9. ^ Marques, Silvio Alencar (October 2013). "Paracoccidioidomycosis: epidemiological, clinical, diagnostic and treatment up-dating". Anais Brasileiros de Dermatologia. 88 (5): 700–711. doi:10.1590/abd1806-4841.20132463. ISSN 0365-0596. PMC 3798345. PMID 24173174.
  10. ^ a b Queiroz-Telles, Flavio; Escuissato, Dante (December 2011). "Pulmonary Paracoccidioidomycosis". Seminars in Respiratory and Critical Care Medicine. 32 (6): 764–774. doi:10.1055/s-0031-1295724. ISSN 1069-3424. PMID 22167404. S2CID 260319905.
  11. ^ Brummer, E; Castaneda, E; Restrepo, A (April 1993). "Paracoccidioidomycosis: an update". Clinical Microbiology Reviews. 6 (2): 89–117. doi:10.1128/CMR.6.2.89. ISSN 0893-8512. PMC 358272. PMID 8472249.
  12. ^ a b c d Travassos, Luiz R; Taborda, Carlos P; Colombo, Arnaldo L (April 2008). "Treatment options for paracoccidioidomycosis and new strategies investigated". Expert Review of Anti-infective Therapy. 6 (2): 251–262. doi:10.1586/14787210.6.2.251. ISSN 1478-7210. PMID 18380607. S2CID 41184245.
  13. ^ a b c d e f g h i j k l m n Shikanai-Yasuda, Maria Aparecida; Mendes, Rinaldo Pôncio; Colombo, Arnaldo Lopes; Queiroz-Telles, Flávio de; Kono, Adriana Satie Gonçalves; Paniago, Anamaria M. M; Nathan, André; Valle, Antonio Carlos Francisconi do; Bagagli, Eduardo (2017-07-12). "Brazilian guidelines for the clinical management of paracoccidioidomycosis". Revista da Sociedade Brasileira de Medicina Tropical. 50 (5): 715–740. doi:10.1590/0037-8682-0230-2017. hdl:11449/163455. ISSN 1678-9849. PMID 28746570.
  14. ^ a b c d e f g h i j k l m n Restrepo, Angela M.; Tobón Orozco, Angela Maria; Gómez, Beatriz L.; Benard, Gil (2015), Hospenthal, Duane R.; Rinaldi, Michael G. (eds.), "Paracoccidioidomycosis", Diagnosis and Treatment of Fungal Infections, Infectious Disease, Springer International Publishing, pp. 225–236, doi:10.1007/978-3-319-13090-3_19, ISBN 9783319130903, S2CID 243500706
  15. ^ a b c d e f g h Marques, SA (Nov–Dec 2012). "Paracoccidioidomycosis". Clinics in Dermatology. 30 (6): 610–5. doi:10.1016/j.clindermatol.2012.01.006. PMID 23068148.
  16. ^ F. Franco, Marcello; Del Negro, Gildo; Lacaz, Carlos da Silva; Restrepo-Moreno, Angela (1994). Paracoccidioidomycosis. Boca Raton: CRC Press. ISBN 9780849348686. OCLC 28421361.
  17. ^ a b Ferreira, Marcelo Simão (2009-12-01). "Paracoccidioidomycosis". Paediatric Respiratory Reviews. 10 (4): 161–165. doi:10.1016/j.prrv.2009.08.001. ISSN 1526-0542. PMID 19879504.
  18. ^ RESTREPO, ANGELA; TOBÓN, ANGELA MARÍA (2010), "Paracoccidioides brasiliensis", Mandell, Douglas, and Bennett's Principles and Practice of Infectious Diseases, Elsevier, pp. 3357–3363, doi:10.1016/b978-0-443-06839-3.00268-x, ISBN 9780443068393
  19. ^ Salgado-Salazar, Catalina; Jones, Leandro R.; Restrepo, Ángela; McEwen, Juan G. (2010-11-10). "The human fungal pathogen Paracoccidioides brasiliensis (Onygenales: Ajellomycetaceae) is a complex of two species: phylogenetic evidence from five mitochondrial markers". Cladistics. 26 (2010): 613–624. doi:10.1111/j.1096-0031.2010.00307.x. hdl:11336/84231. ISSN 1096-0031. PMID 34879597. S2CID 84410217.
  20. ^ Felipe, Maria S. S.; Bagagli, Eduardo; Nino-Vega, Gustavo; Theodoro, Raquel C.; Teixeira, Marcus M. (2014-10-30). "Paracoccidioides Species Complex: Ecology, Phylogeny, Sexual Reproduction, and Virulence". PLOS Pathogens. 10 (10): e1004397. doi:10.1371/journal.ppat.1004397. ISSN 1553-7374. PMC 4214758. PMID 25357210.
  21. ^ a b c d e f g h i Martinez, Roberto (September 2015). "Epidemiology of Paracoccidioidomycosis". Revista do Instituto de Medicina Tropical de São Paulo. 57 (suppl 19): 11–20. doi:10.1590/S0036-46652015000700004. ISSN 0036-4665. PMC 4711199. PMID 26465364.
  22. ^ Kasper, Dennis L.; Fauci, Anthony S.; Hauser, Stephen L.; Longo, Dan L.; Larry Jameson, J.; Loscalzo, Joseph (2018-02-06). "Superficial Mycoses and Less Common Systemic Mycoses". Harrison's principles of internal medicine. Jameson, J. Larry,, Kasper, Dennis L.,, Fauci, Anthony S., 1940-, Hauser, Stephen L.,, Longo, Dan L. (Dan Louis), 1949-, Loscalzo, Joseph (Twentieth ed.). New York. ISBN 9781259644047. OCLC 990065894.{{cite book}}: CS1 maint: location missing publisher (link)
  23. ^ Severo LC, Roesch EW, Oliveira EA, Rocha MM, Londero AT (June 1998), "Paracoccidioidomycosis in women", Rev Iberoam Micol, 15 (2): 88–9, PMID 17655417.
  24. ^ Shikanai-Yasuda, Maria Aparecida (September 2015). "Paracoccidioidomycosis Treatment". Revista do Instituto de Medicina Tropical de São Paulo. 57 (Suppl 19): 31–37. doi:10.1590/S0036-46652015000700007. PMC 4711189. PMID 26465367.
  25. ^ da Mota Menezes, Valfredo; Soares, Bernardo GO; Fontes, Cor Jesus Fernandes (2006-04-19). Cochrane Infectious Diseases Group (ed.). "Drugs for treating paracoccidioidomycosis". Cochrane Database of Systematic Reviews. 2006 (2): CD004967. doi:10.1002/14651858.CD004967.pub2. PMC 6532700. PMID 16625617.
  26. ^ Restrepo, Angela; Tobón, Angela M.; Agudelo, Carlos A. (2008), "Paracoccidioidomycosis", Diagnosis and Treatment of Human Mycoses, Infectious Disease, Humana Press, pp. 331–342, doi:10.1007/978-1-59745-325-7_18, ISBN 9781588298225
  27. ^ Lutz A (1908), "Uma mycose pseudococcidioidica localizada no boca e observada no Brasil. Contribuicao ao conhecimento das hypoblastomycoses americanas.", Imprensa Médica (in Portuguese), Rio de Janeiro, 16: 151–163
  28. ^ Splendore A (1912), "Zimonematosi con localizzazione nella cavita della bocca osservata nel Brasile", Bulletin de la Société de pathologie exotique (in French), Paris, 5: 313–319
  29. ^ De Almeida FP (1928), "Lesoes cutaneas da blastomicose en cabaios experimentalmente infeetados", Anais da Faculdade de Medicina de Universidade de São Paulo (in Portuguese), 3: 59–64
  30. ^ de Almeida FP, da Silva Lacaz C (1942), "Micoses broco-pulmonares", Comp. Melhoramentos (in Portuguese), São Paulo: 98 pages

External links edit

February 15, 2024
paracoccidioidomycosis, also, known, south, american, blastomycosis, fungal, infection, that, occur, mouth, skin, type, lymphangitic, type, multi, organ, involvement, type, particularly, lungs, mixed, type, there, mouth, ulcers, skin, lesions, disease, likely,. Paracoccidioidomycosis PCM also known as South American blastomycosis is a fungal infection that can occur as a mouth and skin type lymphangitic type multi organ involvement type particularly lungs or mixed type 1 6 If there are mouth ulcers or skin lesions the disease is likely to be widespread 1 There may be no symptoms or it may present with fever sepsis weight loss large glands or a large liver and spleen 4 7 ParacoccidioidomycosisOther namesSouth American blastomycosis 1 Brazilian blastomycosis 2 Lutz Splendore de Almeida disease 3 Paracoccidioides histopathologySpecialtyInfectious diseaseSymptomsFever sepsis weight loss large glands large liver and spleen 4 mouth ulcers skin lesions 5 TypesMucocutaneous lymphatic multi organ 1 CausesParacoccidioides brasiliensis 4 Diagnostic methodSampling of blood sputum or skin 4 Differential diagnosisTuberculosis leukaemia lymphoma 4 TreatmentAntifungal medication 6 MedicationItraconazole amphotericin B 6 trimethoprim sulfamethoxazole 7 Deaths200 deaths per year in Brazil 1 The cause is fungi in the genus Paracoccidioides including Paracoccidioides brasiliensis and Paracoccidioides lutzii 8 acquired by breathing in fungal spores 6 Diagnosis is by sampling of blood sputum or skin 4 The disease can appear similar to tuberculosis leukaemia and lymphoma 4 Treatment is with antifungals itraconazole 1 7 For severe disease treatment is with amphotericin B followed by itraconazole or trimethoprim sulfamethoxazole as an alternative 1 7 It is endemic to Central and South America 9 and is considered a type of neglected tropical disease 8 In Brazil the disease causes around 200 deaths per year 1 Contents 1 Signs and symptoms 1 1 Juvenile acute subacute form 1 2 Adult chronic form 2 Cause 3 Mechanism 4 Diagnosis 4 1 Differential diagnosis 5 Treatment 6 Epidemiology 7 History 8 See also 9 References 10 External linksSigns and symptoms edit nbsp Lesions due to Paracoccidioidomycosis on the face of a Brazilian childAsymptomatic lung infection is common with fewer than 5 of infected individuals developing clinical disease 10 It can occur as a mouth and skin type lymphangitic type multi organ involvement type particularly lungs or mixed type 1 6 If there are mouth ulcers or skin lesions the disease is likely to be widespread 1 There may be no symptoms or it may present with fever sepsis weight loss large glands or a large liver and spleen 4 7 Two presentations are known firstly the acute or subacute form which predominantly affects children and young adults 11 and the chronic form predominantly affecting adult men 12 Most cases are infected before age 20 although symptoms may present many years later 13 Juvenile acute subacute form edit The juvenile acute form is characterised by symptoms such as fever weight loss and feeling unwell together with enlarged lymph nodes and enlargement of the liver and spleen 14 15 16 This form is most often disseminated with symptoms manifesting depending on the organs involved 14 Skin and mucous membrane lesions are often present 17 and bone involvement may occur in severe cases 14 This acute severe presentation may mimic tuberculosis lymphoma or leukaemia 17 Adult chronic form edit The chronic form presents months to years after the initial infection occurs and most frequently presents with dry cough and shortness of breath 10 Other symptoms include excess salivation difficulty swallowing and difficulties with voice control 14 Upper respiratory tract mucosal lesions may be present as well as increased mucus production and coughing up blood 18 Both pulmonary and extrapulmonary involvement is common 14 Up to 70 of cases have mucosal involvement with lesions often found in the mouth oropharynx larynx and palate Classic lesions are superficial painful granular ulcers with small spots of bleeding 15 Cause editParacoccidioidomycosis is caused by two species of fungi that can exist as a mold or yeast depending on temperature P brasiliensis and P lutzii 19 In protected soil environments near water sources that are disturbed either naturally or by human activity P brasiliensis has been epidemiologically observed although not isolated 20 A known animal carrier is the armadillo 13 In the natural environment the fungi are found as filamentous structures and they develop infectious spores known as conidia 13 Human to human transmission has never been proven 21 Mechanism editPrimary infection although poorly understood due to lack of data is thought to occur through inhalation of the conidia through the respiratory tract after inhaling fungal conidia produced by the mycelial form of P brasiliensis 14 21 This occurs predominantly in childhood and young adulthood after exposure to agricultural activity 13 Infection may occur through direct skin inoculation although this is rare 15 After inhalation into the alveoli there is rapid multiplication of the organism in the lung tissue sometimes spreading via the venous and lymphatic systems 14 Approximately 2 of people develop clinical features after the initial asymptomatic infection 15 The type of immune response determines the clinical manifestation of the infection with children and HIV co infected individuals most commonly developing the acute subacute disseminated disease 14 Most of those infected develop a Type 1 T cell Th1 mediated immune response resulting in fibrosing alveolitis and compact granuloma formation that control fungal replication and latent or asymptomatic infection 13 14 It then is thought to remain dormant in residual lung lesions and mediastinal lymph nodes 21 A deficient Th1 cell response results in the severe forms of the disease In these individuals granulomas do not form and the affected person develops Th2 and Th9 responses resulting in activation of B lymphocytes high levels of circulating antibodies eosinophilia and hypergammaglobulinemia 13 Lung involvement subsequently occurs after a dormant phase manifesting in upper respiratory tract symptoms and lung infiltrates on imaging 15 The commonest chronic form is almost certainly a reactivation of the disease 15 and may develop into progressive scarring of the lungs pulmonary fibrosis 22 It can cause disease in those with normal immune function although immunosuppression increases the aggressiveness of the fungus It rarely causes disease in fertile age women probably due to a protective effect of estradiol 23 Diagnosis editMore than 90 of cases can be diagnoses with direct histological examination of tissue such as sputum bronchial lavage fluid exudates and biopsies Histopathological study with Gomori methenamine silver GMS stain or hematoxylin and eosin H amp E stain revealing large yeast cells with translucent cell walls with multiple buds 14 In the juvenile form lung abnormalities are shown in high resolution CT scans of the lungs whereas in the chronic form plain X rays may show interstitial and alveolar infiltrates in the central and lower lung fields 14 Culture of P brasiliensis takes between 20 and 30 days requiring multiple samples and culture media Initial culture can occur at room temperature however after growth is noted confirmation occurs by incubating at to 36 37 degrees to transform the fungus into yeast cells 14 Antibody detection is useful both for acute diagnosis and monitoring Gel immunodiffusion is commonly used in endemic areas diagnoses 95 of cases with high specificity 14 Complement fixation allows for a measure of severity of cases by quantifying the antibody level and is thus useful for monitoring treatment response It is however only sensitive for 85 of cases and cross reacts with H capsulatum 14 Differential diagnosis edit The disease can appear similar to tuberculosis leukaemia and lymphoma 4 Treatment editBoth P brasiliensis and P lutzii are in vitro susceptible to most antifungal agents unlike other systemic fungal infections Mild and moderate forms are treated with itraconazole for 9 to 18 months as this has been shown to be more effective has a shorter treatment duration and is more tolerated citation needed Acidic beverages have been shown to reduce absorption of itraconazole 13 Co trimoxazole is a second line agent and is preferred for those with brain involvement and during pregnancy 13 For severe cases intravenous treatment with amphotericin B is indicated for an average of 2 to 4 weeks 13 Prednisolone prescribed at the same time may reduce inflammation during treatment 13 Patients should be treated until stabilisation of symptoms and increase in body weight Advice in regards to nutritional support as well as smoking and alcohol intake should be provided Adrenal insufficiency if found is treated with corticosteroids 24 Clinical criteria for cure includes the absence or healing of lesions stabilisation of body weight negative as well as negative autoantibody tests 13 There is insufficient data to support the benefits of above drugs to treat the disease 25 Epidemiology editParacoccidioidomycosis is endemic in rural areas of Latin America from southern Mexico to Argentina and is also found in Brazil Colombia Venezuela Ecuador and Paraguay 13 15 An epidemic outbreak has never been observed 13 It has the highest prevalence of all systemic mycoses fungal infections in the area 12 As many as 75 of people in endemic areas have been estimated to be infected with the asymptomatic form up to 10 million people with 2 developing clinically significant disease 12 Morbidity and mortality is strongly associated with patient s socioeconomic background 12 with most adult patients being male agricultural workers 26 Other risk factors include smoking alcohol use HIV co infection or other immunosuppression 21 80 of reported cases are in Brazil in the southeast midwest and south spreading in the 1990s to the Amazon area Most of the remaining infections are in Argentina Colombia and Venezuela 21 Most epidemiological reports have focused on P brasliensis with P lutzii epidemiology poorly understood as of 2015 21 Rising cases have been linked to agriculturalization and deforestation in Brazil urbanisation to peripheral city areas with poor infrastructure as well as increased soil and air humidity 13 21 One Brazilian indigenous tribe the Surui after changing from subsistence agriculture to coffee farming showed higher infection rates than surrounding tribes 21 There have also been reports in non endemic areas with the rise of eco tourism in the United States Europe and Japan 15 All reported cases were returned travellers from endemic regions 21 History editLutz Splendore de Almeida disease 3 is named for the physicians Adolfo Lutz 27 Alfonso Splendor 1871 1953 an Italo Brazilian parasitologist 28 and Floriano Paulo de Almeida 1898 1977 a Brazilian pathologist specializing in Pathologic Mycology Study of Infectious Fungi 29 30 who first characterized the disease in Brazil in the early 20th century See also editNorth American blastomycosisReferences edit a b c d e f g h i j James William D Elston Dirk Treat James R Rosenbach Misha A Neuhaus Isaac 2019 13 Diseases resulting from fungi and yeasts Andrews Diseases of the Skin Clinical Dermatology 13th ed Elsevier pp 313 314 ISBN 978 0 323 54753 6 Rapini Ronald P Bolognia Jean L Jorizzo Joseph L 2007 Dermatology 2 Volume Set St Louis Mosby ISBN 978 1 4160 2999 1 a b Lutz Splendore de Almeida disease at Who Named It a b c d e f g h i ICD 11 ICD 11 for Mortality and Morbidity Statistics icd who int Retrieved 26 June 2021 Johnstone Ronald B 2017 25 Mycoses and Algal infections Weedon s Skin Pathology Essentials 2nd ed Elsevier p 451 ISBN 978 0 7020 6830 0 a b c d e Barlow Gavin Irving Irving moss Peter J 2020 20 Infectious diseases In Feather Adam Randall David Waterhouse Mona eds Kumar and Clark s Clinical Medicine 10th ed Elsevier p 561 ISBN 978 0 7020 7870 5 a b c d e Proia Laurie 2020 28 The dimorphic mycoses In Spec Andrej Escota Gerome V Chrisler Courtney Davies Bethany eds Comprehensive Review of Infectious Diseases Elsevier pp 419 420 ISBN 978 0 323 56866 1 a b Queiroz Telles Flavio Fahal Ahmed Hassan Falci Diego R Caceres Diego H Chiller Tom Pasqualotto Alessandro C November 2017 Neglected endemic mycoses The Lancet Infectious Diseases 17 11 e367 e377 doi 10 1016 S1473 3099 17 30306 7 PMID 28774696 subscription required Marques Silvio Alencar October 2013 Paracoccidioidomycosis epidemiological clinical diagnostic and treatment up dating Anais Brasileiros de Dermatologia 88 5 700 711 doi 10 1590 abd1806 4841 20132463 ISSN 0365 0596 PMC 3798345 PMID 24173174 a b Queiroz Telles Flavio Escuissato Dante December 2011 Pulmonary Paracoccidioidomycosis Seminars in Respiratory and Critical Care Medicine 32 6 764 774 doi 10 1055 s 0031 1295724 ISSN 1069 3424 PMID 22167404 S2CID 260319905 Brummer E Castaneda E Restrepo A April 1993 Paracoccidioidomycosis an update Clinical Microbiology Reviews 6 2 89 117 doi 10 1128 CMR 6 2 89 ISSN 0893 8512 PMC 358272 PMID 8472249 a b c d Travassos Luiz R Taborda Carlos P Colombo Arnaldo L April 2008 Treatment options for paracoccidioidomycosis and new strategies investigated Expert Review of Anti infective Therapy 6 2 251 262 doi 10 1586 14787210 6 2 251 ISSN 1478 7210 PMID 18380607 S2CID 41184245 a b c d e f g h i j k l m n Shikanai Yasuda Maria Aparecida Mendes Rinaldo Poncio Colombo Arnaldo Lopes Queiroz Telles Flavio de Kono Adriana Satie Goncalves Paniago Anamaria M M Nathan Andre Valle Antonio Carlos Francisconi do Bagagli Eduardo 2017 07 12 Brazilian guidelines for the clinical management of paracoccidioidomycosis Revista da Sociedade Brasileira de Medicina Tropical 50 5 715 740 doi 10 1590 0037 8682 0230 2017 hdl 11449 163455 ISSN 1678 9849 PMID 28746570 a b c d e f g h i j k l m n Restrepo Angela M Tobon Orozco Angela Maria Gomez Beatriz L Benard Gil 2015 Hospenthal Duane R Rinaldi Michael G eds Paracoccidioidomycosis Diagnosis and Treatment of Fungal Infections Infectious Disease Springer International Publishing pp 225 236 doi 10 1007 978 3 319 13090 3 19 ISBN 9783319130903 S2CID 243500706 a b c d e f g h Marques SA Nov Dec 2012 Paracoccidioidomycosis Clinics in Dermatology 30 6 610 5 doi 10 1016 j clindermatol 2012 01 006 PMID 23068148 F Franco Marcello Del Negro Gildo Lacaz Carlos da Silva Restrepo Moreno Angela 1994 Paracoccidioidomycosis Boca Raton CRC Press ISBN 9780849348686 OCLC 28421361 a b Ferreira Marcelo Simao 2009 12 01 Paracoccidioidomycosis Paediatric Respiratory Reviews 10 4 161 165 doi 10 1016 j prrv 2009 08 001 ISSN 1526 0542 PMID 19879504 RESTREPO ANGELA TOBoN ANGELA MARIA 2010 Paracoccidioides brasiliensis Mandell Douglas and Bennett s Principles and Practice of Infectious Diseases Elsevier pp 3357 3363 doi 10 1016 b978 0 443 06839 3 00268 x ISBN 9780443068393 Salgado Salazar Catalina Jones Leandro R Restrepo Angela McEwen Juan G 2010 11 10 The human fungal pathogen Paracoccidioides brasiliensis Onygenales Ajellomycetaceae is a complex of two species phylogenetic evidence from five mitochondrial markers Cladistics 26 2010 613 624 doi 10 1111 j 1096 0031 2010 00307 x hdl 11336 84231 ISSN 1096 0031 PMID 34879597 S2CID 84410217 Felipe Maria S S Bagagli Eduardo Nino Vega Gustavo Theodoro Raquel C Teixeira Marcus M 2014 10 30 Paracoccidioides Species Complex Ecology Phylogeny Sexual Reproduction and Virulence PLOS Pathogens 10 10 e1004397 doi 10 1371 journal ppat 1004397 ISSN 1553 7374 PMC 4214758 PMID 25357210 a b c d e f g h i Martinez Roberto September 2015 Epidemiology of Paracoccidioidomycosis Revista do Instituto de Medicina Tropical de Sao Paulo 57 suppl 19 11 20 doi 10 1590 S0036 46652015000700004 ISSN 0036 4665 PMC 4711199 PMID 26465364 Kasper Dennis L Fauci Anthony S Hauser Stephen L Longo Dan L Larry Jameson J Loscalzo Joseph 2018 02 06 Superficial Mycoses and Less Common Systemic Mycoses Harrison s principles of internal medicine Jameson J Larry Kasper Dennis L Fauci Anthony S 1940 Hauser Stephen L Longo Dan L Dan Louis 1949 Loscalzo Joseph Twentieth ed New York ISBN 9781259644047 OCLC 990065894 a href Template Cite book html title Template Cite book cite book a CS1 maint location missing publisher link Severo LC Roesch EW Oliveira EA Rocha MM Londero AT June 1998 Paracoccidioidomycosis in women Rev Iberoam Micol 15 2 88 9 PMID 17655417 Shikanai Yasuda Maria Aparecida September 2015 Paracoccidioidomycosis Treatment Revista do Instituto de Medicina Tropical de Sao Paulo 57 Suppl 19 31 37 doi 10 1590 S0036 46652015000700007 PMC 4711189 PMID 26465367 da Mota Menezes Valfredo Soares Bernardo GO Fontes Cor Jesus Fernandes 2006 04 19 Cochrane Infectious Diseases Group ed Drugs for treating paracoccidioidomycosis Cochrane Database of Systematic Reviews 2006 2 CD004967 doi 10 1002 14651858 CD004967 pub2 PMC 6532700 PMID 16625617 Restrepo Angela Tobon Angela M Agudelo Carlos A 2008 Paracoccidioidomycosis Diagnosis and Treatment of Human Mycoses Infectious Disease Humana Press pp 331 342 doi 10 1007 978 1 59745 325 7 18 ISBN 9781588298225 Lutz A 1908 Uma mycose pseudococcidioidica localizada no boca e observada no Brasil Contribuicao ao conhecimento das hypoblastomycoses americanas Imprensa Medica in Portuguese Rio de Janeiro 16 151 163 Splendore A 1912 Zimonematosi con localizzazione nella cavita della bocca osservata nel Brasile Bulletin de la Societe de pathologie exotique in French Paris 5 313 319 De Almeida FP 1928 Lesoes cutaneas da blastomicose en cabaios experimentalmente infeetados Anais da Faculdade de Medicina de Universidade de Sao Paulo in Portuguese 3 59 64 de Almeida FP da Silva Lacaz C 1942 Micoses broco pulmonares Comp Melhoramentos in Portuguese Sao Paulo 98 pagesExternal links edit Retrieved from https en wikipedia org w index php title Paracoccidioidomycosis amp oldid 1195808039, wikipedia, wiki, book, books, library,

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