Pneumocystis pneumonia

From Wikipedia, the free encyclopedia

Pneumocystis pneumonia (PCP) is a form of pneumonia caused by the yeast-like fungal microorganism Pneumocystis jirovecii (Jirovecii is pronounced "yee row vet zee eye"). The causal agent was originally described as a protozoan and spelled P. jiroveci and prior to then was formerly classified as a form of Pneumocystis carinii, a name still in common usage.[1][2] These names are discussed below. As a result, Pneumocystis pneumonia (PCP) has also been known as Pneumocystis jiroveci[i] pneumonia and as Pneumocystis carinii pneumonia, as is also explained below.[3][4][5]

Pneumocystis jirovecii pneumonia
Classification & external resources
Pneumocystis jirovecii cysts from bronchoalveolar lavage, stained with Toluidin blue O stain
ICD-10 B20.6
ICD-9 136.3
DiseasesDB 10160
MedlinePlus 000671
eMedicine med/1850 

It is relatively rare in people with normal immune systems but common among people with weakened immune systems, such as premature or severely malnourished children, the elderly, and especially AIDS patients, in whom it is most commonly observed today.[6] PCP can also develop in patients who are taking immunosuppressant medications (e.g., patients who have undergone solid organ transplantation) and in patients who have undergone bone marrow transplantation.

The organism is distributed worldwide[7][1].


Contents

[edit] Symptoms

Symptoms of PCP include fever, non-productive cough, shortness of breath (especially on exertion), weight loss and night sweats. There is usually not a large amount of sputum with PCP unless the patient has an additional bacterial infection. The fungus can invade other visceral organs, such as the liver, spleen and kidney, but only in a minority of cases.

X-ray of Pneumocystis jirovecii pneumonia There is increased white (opacity) in the lower lungs on both sides, characteristic of Pneumocystis pneumonia
X-ray of Pneumocystis jirovecii pneumonia There is increased white (opacity) in the lower lungs on both sides, characteristic of Pneumocystis pneumonia

[edit] Pathophysiology

The risk of pneumonia due to Pneumocystis jirovecii increases when CD4 levels are less than 200 cells/mm3. In these immunosuppressed individuals the manifestations of the infection are highly variable.[8] The disease attacks the interstitial, fibrous tissue of the lungs, with marked thickening of the alveolar septa and alveoli and leading to significant hypoxia which can be fatal if not treated aggressively; ergo, LDH levels increase and gas exchange is compromised. Oxygen is less able to diffuse into the blood, leading to hypoxia. Hypoxia, along with high arterial carbon dioxide (CO2) levels, stimulates ventilation, thereby causing dyspnea.

[edit] Diagnosis

The clinical diagnosis can be confirmed by the characteristic appearance of the chest x-ray which shows widespread pulmonary infiltrates, and an arterial oxygen level (pO2) strikingly lower than would be expected from symptoms. The diagnosis can be definitively confirmed by pathologic identification of the causative organism in induced sputum or bronchial washings obtained by bronchoscopy with coloration by toluidine blue or immunofluorescence assay, which will show characteristic cysts [2].

Pneumocystis infection can also be diagnosed by immunofluorescent or histochemical staining of the specimen, and more recently by molecular analysis of PCR products comparing DNA samples. Notably, simple molecular detection of Pneumocystis jirovecii in lung fluids does not mean that a person has Pneumocystis pneumonia or infection by HIV. The fungus appears to be present in healthy individuals also in the general population.[9]


[edit] Life-cycle

The complete life-cycles of any of the species of Pneumocystis are not known, but presumably all resemble the others in the genus. The terminology follows zoological terms, rather than mycological terms, reflecting the initial misdetermination as a protozoan parasite. All stages are found in lungs and because they cannot be cultured, direct observation of living Pneumocystis is difficult. The trophozoite stage is the vegetative state. It is single-celled and appears amoeboid (multilobed) and closely associated with host cells. Globular cysts eventually form that have a thicker wall. Within these ascus-like cysts, eight spores form which are released through rupture of the cyst wall. The cysts often collapse forming crescent-shaped bodies visible in stained tissue. It is not known for certain if meiosis takes place within the cysts, or what the genetic status is of the various cell types- see DPDx life-cycle diagram.


[edit] PCP and AIDS

Because PCP rarely occurs without AIDS, it can be one of the first clues to a new AIDS diagnosis, though it does not generally occur unless the CD4 count is less than 200/mm³. An unusual rise in PCP cases in North America, noticed when physicians began requesting large quantities of the rarely used antibiotic pentamidine, was the first clue to the existence of AIDS in the early 1980s.

Prior to the development of more effective treatments, PCP was a common and rapid cause of death in AIDS patients. Much of the incidence of PCP has been reduced by instituting a standard practice of using oral trimethoprim/sulfamethoxazole to prevent the disease in people with CD4 counts less than 200/mm³. In populations that do not have access to preventative treatment, PCP continues to be a major cause of death in AIDS.

In immunocompromised patients (e.g., cancer patients on chemotherapy, or AIDS patients with a CD4+ T-cell count below 200/μl), prophylaxis with regular pentamidine inhalations or sulfamethoxazole/trimethoprim (co-trimoxazole or TMP-SMX) may be necessary to prevent PCP.

[edit] Treatment

Antipneumocystic medication is used with concomitant steroids in order to avoid inflammation, which causes an exacerbation of symptoms about four days after treatment begins if steroids are not used. By far the most commonly used medication is a combination of trimethoprim and sulfamethoxazole (co-trimoxazole, with the tradenames Bactrim, Septrin, or Septra), but some patients are unable to tolerate this treatment due to allergies. Other medications that are used, alone or in combination, include pentamidine, trimetrexate, dapsone, atovaquone, primaquine, and clindamycin. Treatment is usually for a period of about 21 days.

Pentamidine is less often used as its major limitation is the high frequency of side effects. These include acute pancreatitis, renal failure, hepatotoxicity, leukopenia, rash, fever and hypoglycaemia.

[edit] Nomenclature

Wikipedia:How to read a taxobox
How to read a taxobox
Pneumocystis
P. jirovecii cysts in tissue
P. jirovecii cysts in tissue
Scientific classification
Kingdom: Fungi
Subkingdom: Dikarya
Phylum: Ascomycota
Subphylum: Taphrinomycotina
Class: Pneumocystidomycetes
Order: Pneumocystidales
Family: Pneumocystidaceae
Genus: Pneumocystis
(Delanoë & Delanoë 1912)
Species

P. carinii
P. jirovecii
P. murina
P. oryctolagi
P. wakefieldiae

The name P. jirovecii, to distinguish the organism found in humans from physiological variants of Pneumocystis found in other animals, was first proposed in 1976, in honor of Otto Jirovec, who described Pneumocystis pneumonia in humans in 1952. After DNA analysis showed significant differences in the human variant, the proposal was made again in 1999 and has come into common use; P. carinii still describes the species found in rats[1] and that name is typified by an isolate from rats.[2] The International Code of Botanical Nomenclature (ICBN) requires that the name to be spelled jirovecii rather than jiroveci. The latter spelling originated when Pneumocystis was believed to be a protozoan, rather than a fungus, and therefore was spelled using the International Code of Zoological Nomenclature; both spellings are commonly used. A change in the ICBN in 2005 now recognizes the validity of the 1976 publication, making the 1999 proposal redundant, and cites Pneumocystis and P. jirovecii as examples of the change in ICBN Article 45, Ex 8. The name P. jirovecii is typified (both lectotypified and epitypified) by samples from human autopsies dating from the 1960's.[2]

The term PCP, which was widely used by practitioners and patients, has been retained for convenience, with the rationale that it now stands for the more general Pneumocystis pneumonia rather than Pneumocystis carinii pneumonia.

[edit] History

The earliest report of this genus appears to have been that of Carlos Chagas in 1909[10] who discovered it in experimental animals but confused it with part of the life-cycle of Trypanosoma cruzi (causal agent of Chagas Disease) and later called both organisms 'Schizotrypanum cruzi' a form of trypanosome infecting humans[11] The rediscovery of Pneumocystis cysts was reported by Antonio Carini in 1910 also in Brazil.[12] The genus was again discovered in 1912 by Delanoë and Delanoë this time at the Pasteur Institute in Paris, France who found it in rats and who proposed the genus and species name Pneumocystis carinii after Carini.[13]

Pneumocystis was redescribed as a human pathogen in 1942 by two Dutch investigators, van der Meer and Brug who found it in three new cases: a 3-month-old infant with congenital heart disease and in 2 of 104 autopsy cases - a 4-month-old infant and a 21-year-old adult.[14] There being only one described species in the genus, they considered the human parasite to be P. carinii. Nine years later (1951) Dr. Josef Vanek at Karls-Universität in Prague, Czechoslovakia showed in a study of lung sections from sixteen children that the organism labelled "P. carinii" was the causative agent of pneumonia in these children.[15] The following year (1952) Jírovec reported "P. carinii" as the cause of interstitial pneumonia in neonates.[16][17][18] Following the realization that Pneumocystis from humans could not infect experimental animals such as rats, and that the rat form of Pneumocystis differed physiologically and had different antigenic properties, Frenkel[19] was the first to recognize the human pathogen as a distinct species. He named it Pneumocystis jirovecii (see nomenclature above). There has been controversy over the relabeling of P. carinii in humans as P. jirovecii,[20][2] which is why both names still appear in publications. However, only the name P. jirovecii is used exclusively for the human pathogen, whereas the name P. carinii has had a broader application to many species.[21] Frenkel and those before him, believed that all Pneumocystis were protozoans, but soon afterwards evidence began accumulating that Pneumocystis was a fungal genus. Recent studies show it to be an unusual, in some ways a primitive genus of Ascomycota, related to a group of yeasts.[22] Every tested primate, including humans, appears to have their own type of Pneumocystis that is incapable of cross-infecting other host species and has co-evolved with each mammal species.[23] Currently only 5 species have been formally named: P. jirovecii from humans, P. carinii as originally named from rats, P. murina from mice,[24] P. wakefieldiae[25][26] also from rats, and P. oryctolagi from rabbits.[27]

Historical and even recent reports of P. carinii from humans are based upon older classifications (still used by many, or those still debating the recognition of distinct species in the genus Pneumocystis) which does not mean that the true P. carinii from rats actually infects humans. In an intermediate classification system, the various taxa in different mammals have been called formae speciales or forms. For example the human "form" was called Pneumocystis carinii f. [or f. sp.] hominis, while the original rat infecting form was called Pneumocystis carinii f. [or f. sp.] carinii. This terminology is still used by some researchers. The species of Pneumocystis species originally seen by Chagas have not yet been named as distinct species.[2] Many other undescribed species presumably exist and those that have been detected in many mammals are only known from molecular sample detection from lung tissue or fluids, rather than by direct physical observation.[28] As of yet, they are cryptic taxa.

[edit] Pneumocystis Genome Project

Pneumocystis species cannot be grown in culture. Therefore, there is a limitation to the availability of the human disease causing agent, P. jirovecii. Hence, investigation of the whole genome of a Pneumocystis is largely based upon true P. carinii available from experimental rats which can be maintained with infections. The project is described in the site linked here. Genetic material of other species, such as P. jirovecii can be compared to the genome of P. carinii. Pneumocystis Genome Project

[edit] References

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  2. ^ a b c d e Redhead SA, Cushion MT, Frenkel JK, Stringer JR (2006). "Pneumocystis and Trypanosoma cruzi: nomenclature and typifications". J Eukaryot Microbiol 53 (1): 2-11. PMID 16441572. 
  3. ^ Cushion MT . (1998). "Chapter 34. Pneumocystis carinii. In: Collier, L., Balows, A. & Sussman, M. (ed.), Topley and Wilson's Microbiology and Microbial Infections 9th ed. Arnold and Oxford Press, New York.": 645-683. 
  4. ^ Cushion MT (1998). "Taxonomy, genetic organization, and life cycle of Pneumocystis carinii". Semin. Respir. Infect 13 (4): 304-312. 
  5. ^ Cushion MT (2004). "Pneumocystis: unraveling the cloak of obscurity". Trends Microbiol 12 (5): 243-249. 
  6. ^ Ryan KJ; Ray CG (editors) (2004). Sherris Medical Microbiology, 4th ed., McGraw Hill. ISBN 0838585299. 
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  9. ^ Medrano FJ et al (2005). "Pneumocystis jirovecii in General Population". Emerg Infect Dis 11 (2): 245-250. PMID 15752442. 
  10. ^ Chagas C (1909). "Neue Trypanosomen". Vorläufige Mitteilung. Arch. Schiff. Tropenhyg. 13: 120-122. 
  11. ^ Chagas C (1909). "Nova tripanozomiase humana: Estudos sobre a morfolojia e o ciclo evolutivo do Schizotrypanum cruzi n. gen., n. sp., ajente etiolojico de nova entidade morbida do homem". Mem Inst Oswaldo Cruz 1 (2): 159-218. 
  12. ^ Carini A. (1910). "Formas des eschizogonia do Trypanosoma lewisi.". Soc Med Cir São Paulo 38 (8): –. 
  13. ^ Delanoë P, Delanoë M. (1912). "Sur les rapports des kystes de Carini du poumon des rats avec le Trypanosoma lewisi.". Comptes rendus de l’Academie des sciences. 155: 658–61. 
  14. ^ van der Meer MG, Brug SL. (1942). "Infection à Pneumocystis chez l’homme et chez les animaux.". Amer Soc Belge Méd Trop 22: 301–9. 
  15. ^ Vanek J. (1951). "Atypicka (interstitiálni) pneumonie detí vyvolaná Pneumocystis carinii (Atypical interstitial pneumonia of infants produced by Pneumocystis carinii).". Casop lék cesk 90: 1121–4. 
  16. ^ Jírovec O. (1952). "Pneumocystis carinii puvodce t. zv intertitialnich plasmocelularnich pneumonii kojencw (Pneumocystis carinii, the cause of interstitial plasmacellular pneumonia in neonates)". P Csl. Hyg epid mikrob 1: 141. 
  17. ^ Vanek J, Jírovec O, Lukes J. (1953). "Interstitial plasma cell pneumonia in infants.". Ann Paediatrici 180: 1–21. 
  18. ^ Gajdusek DC (1957). "Pneumocystis carinii; etiologic agent of interstitial plasma cell pneumonia of premature and young infants.". Pediatrics 19: 543–65. 
  19. ^ Frenkel JK (1976). "Pneumocystis jiroveci n. sp. from man: morphology, physiology, and immunology in relation to pathology". Natl Cancer Inst Monogr 43: 13-27. PMID 828240. 
  20. ^ Gigliotti F (2005). "Pneumocystis carinii: has the name really been changed?". Clin Infect Dis 41 (12): 1752-5. PMID 16288399. 
  21. ^ Hawksworth DL (2007). "Responsibility in naming pathogens: the case of Pneumocystis jirovecii, the causal agent of pneumocystis pneumonia". Lancet Infect. Dis. 7(1): 3-5. PMID 17182335. 
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  24. ^ Keely S, Fischer J, Cushion M, Stringer J (2004). "Phylogenetic identification of Pneumocystis murina sp. nov., a new species in laboratory mice". Microbiology 150 (Pt 5): 1153-65. PMID 15133075. 
  25. ^ Cushion MT, Keely SP, Stringer JR (2004). "Molecular and phenotypic description of Pneumocystis wakefieldiae sp. nov., a new species in rats". Mycologia 96: 429-438. 
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  27. ^ Dei-Cas E et al (2006). "Pneumocystis oryctolagi sp. nov., an uncultured fungus causing pneumonia in rabbits at weaning: review of current knowledge, and description of a new taxon on genotypic, phylogenetic and phenotypic bases". FEMS Micriobiol. Rev. 30(6): 853-871. PMID 17064284. 
  28. ^ Demanche C et al (2001). "Phylogeny of ‘’Pneumocystis carinii’’ from 18 primate species confirms host specificity and suggests coevolution". J. Clinical Microbiol. 39 (6): 2126-2133. PMID 11376046.