Angiostrongylus cantonensis
Angiostrongylus cantonensis | |
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Adult female worm of Angiostrongylus cantonensis with characteristic barber-pole appearance (anterior end of worm is to the top). Scale bar is 1 mm. | |
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Species: | A. cantonensis
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Binomial name | |
Angiostrongylus cantonensis (Chen, 1935)[1]
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Angiostrongylus cantonensis is a parasitic nematode (roundworm) that causes angiostrongyliasis, the most common cause of eosinophilic meningitis in Southeast Asia and the Pacific Basin.[2] The nematode commonly resides in the pulmonary arteries of rats, giving it the common name rat lungworm. Snails are the primary intermediate hosts, where larvae develop until they are infectious.
Humans are incidental hosts of this roundworm, and may become infected through ingestion of larvae in raw or undercooked snails or other vectors, or from contaminated water and vegetables.[3] The larvae are then transported via the blood to the central nervous system, where they are the most common cause of eosinophilic meningitis, a serious condition that can lead to death or permanent brain and nerve damage.[4] Angiostrongyliasis is an infection of increasing public health importance, as globalization contributes to the geographic spread of the disease.[5]
History
First described by the renowned Chinese parasitologist Hsin-Tao Chen (1904–1977) in 1935, after examining Cantonese rat specimens,[1] the nematode Angiostrongylus cantonensis was identified in the cerebrospinal fluid of a patient with eosinophilic meningitis by Nomura and Lim in Taiwan in 1944. They noted that raw food eaten by the patient may have been contaminated by rats. In 1955, Mackerass and Sanders identified the lifecycle of the worm in rats, defining snails and slugs as the intermediate hosts and noting the path of transmission through the blood, brain, and lungs in rats.[citation needed]
Infectious agent
A. cantonensis is a helminth of the phylum Nematoda, order Strongylida, and superfamily Metastrongyloidea. Nematodes are roundworms characterized by a tough outer cuticle, unsegmented bodies, and a fully developed gastrointestinal tract. The order Strongylida includes hookworms and lungworms. Metastrongyloidea are characterized as 2-cm-long,[6] slender, threadlike worms that reside in the lungs of the definitive host.[7] Angiostrongylus costaricensis is a closely related worm that causes intestinal angiostrongyliasis in Central and South America.
Epidemiology and pathogenesis
Following World War II, A. cantonensis spread throughout Southeast Asia and Western Pacific Islands, including Australia, Melanesia, Micronesia, and Polynesia. Cases were soon reported in New Caledonia, the Philippines, Rarotonga, Saipan, Sumatra, Taiwan, and Tahiti. In the 1960s, even more cases were reported from the region from locations such as Cambodia, Guam, Hawaii, Java, Thailand, Sarawak, Vietnam, and the New Hebrides (Vanuatu).[8]
In 1961, an epidemiological study of eosinophilic meningitis in humans was conducted by Rosen, Laigret, and Bories, who hypothesized that the parasite causing these infections was carried by fish. However, Alicata noted that raw fish was consumed by large numbers of people in Hawaii without apparent consequences, and patients presenting with meningitis symptoms had a history of eating raw snails or prawns in the weeks before presenting with symptoms. This observation, along with epidemiology and autopsy of infected brains, confirmed A. cantonensis infection in humans as the cause of the majority of eosinophilic meningitis cases in Southeast Asia and the Pacific Islands.[9]
Since then, cases of A. cantonensis infestations have appeared in American Samoa, Australia, Hong Kong, Bombay, Fiji, Hawaii, Honshu, India, Kyushu, New Britain, Okinawa, Ryukyu Islands, Western Samoa, and most recently mainland China. Other sporadic occurrences of the parasite in its rat hosts have been reported in Cuba, Egypt, Louisiana, Madagascar, Nigeria, New Orleans, and Puerto Rico.[8]
In 2013, A. cantonensis was confirmed present in Florida, USA, where its range and prevalence are expanding.[10] In 2018, a case was found in a New Yorker, who had visited Hawaii.[11]
In recent years, the parasite has been shown to be proliferating at an alarming rate due to modern food consumption trends and global transportation of food products. Scientists are calling for a more thorough study of the epidemiology of A. cantonensis, stricter food safety policies, and the increase of knowledge on how to properly consume products commonly infested by the parasite such as snails and slugs that act as intermediate hosts or those that act as paratenic hosts such as fish, frogs, or freshwater prawns.[12][13][14] Ingestion of food items that can be contaminated by the mucus excretions of intermediate or paratenic hosts, such as snails and slugs or by the feces of rats that act as definitive hosts, can lead to infection of A. cantonensis.[15] The most common route of infection of A. cantonesis in humans is by ingestion of either intermediate or paratenic hosts of the larvae.[16] Unwashed fruits and vegetables, especially romaine lettuce, can be contaminated with snail and slug mucus or can result in accidental ingestion of these intermediate and paratenic hosts. These items need to be properly washed and handled to prevent accidental ingestion of A. cantonensis larvae or the larvae-containing hosts.[17] The best mechanism of prevention of A. cantonesis outbreak is to institute an aggressive control of snail and slug population, proper cooking of intermediate and paratenic hosts such as fish, freshwater prawn, frogs, mollusks, and snails along with proper food handling techniques.[18] The common prevention techniques for diarrheal illness is very effective in preventing A. cantonensis infection.[19] Not much is known about why it targets the brain in humans, but a chemical induced chemotaxis has been implicated recently. Acetylcholine has been previously reported to enhance motility of this worm via nicotinic acetylcholine receptors.[20] Experimental assays in animal model are needed to validate a chemical induced chemotaxis by use of anticholinergic drugs to prevent cerebral infection following infections by A. cantonesis.[21]
Hosts
Intermediate hosts of larvae of for A. cantonensis include:
- Land snails: Thelidomus aspera from Jamaica,[22][23] Pleurodonte sp. from Jamaica, Sagda sp. from Jamaica, Poteria sp. from Jamaica,[23] Achatina fulica,[24][25][26][27] Satsuma mercatoria, Acusta despecta,[26][27] Bradybaena brevispira,[24] Bradybaena circulus[26] Bradybaena ravida, Bradybaena similaris, Plectotropis appanata[24] and Parmarion martensi from Okinawa[26] and from Hawaii,[28] Camaena cicatricosa, Trichochloritis rufopila, Trichochloritis hungerfordianus and Cyclophorus spp.[27]
- Freshwater snails: Pila spp.,[25] Pomacea canaliculata,[24][25] Cipangopaludina chinensis, Bellamya aeruginosa and Bellamya quadrata[24]
- Slugs: Limax maximus,[29] Limax flavus[24] Deroceras laeve,[24][30] Deroceras reticulatum,[30] Veronicella alte,[26] =? Laevicaulis alte,[24][30] Sarasinula plebeia,[30][31] Vaginulus yuxjsjs,[24] Lehmannia valentiana,[26] Phiolomycus bilineatus, Macrochlamys loana, Meghimatium bilineatum[24] and probably other species of slugs.
Definitive host of A. cantonensis include wild rodents, especially the brown rat (Rattus norvegicus) and the black rat (Rattus rattus).[22]
Paratenic hosts of A. cantonensis include: predatory land flatworm Platydemus manokwari and amphibians Bufo asiaticus, Rana catesbeiana, Rhacophorus leucomystax and Rana limnocharis.[26]
In 2004, a captive yellow-tailed black cockatoo (Calyptorhynchus funereus) and two free-living tawny frogmouths (Podargus strigoides) suffering neurological symptoms were shown to have the parasite. They were the first avian hosts discovered for the organism.[32]
Pathogenesis of human angiostrongylosis
The presence of parasitic worms burrowed in the neural tissue of the human central nervous system will cause obvious complications. All of the following will result in damage to the CNS:[citation needed]
- Direct mechanical damage to neural tissue from the worms' motion
- Toxic byproducts such as nitrogenous waste
- Antigens released by dead and living parasites
Eosinophilic meningitis
Although the clinical disease caused by Angiostrongylus invasion into the central nervous system is commonly referred to as "eosinophilic meningitis", the actual pathophysiology is of a meningoencephalitis with invasion not just of the meninges, or superficial lining of the brain, but also deeper brain tissue. Initial invasion through the lining of the brain, the meninges, may cause a typical inflammation of the meninges and a classic meningitis picture of headache, stiff neck and often fever. The parasites subsequently invade deeper into the brain tissue, causing specific localizing neurologic symptoms depending on where in the brain parenchyma they migrate. Neurologic findings and symptoms wax and wane as initial damage is done by the physical in-migration of the worms and secondary damage is done by the inflammatory response to the presence of dead and dying worms. This inflammation can lead in the short term to paralysis, bladder dysfunction, visual disturbance and coma and in the long term to permanent nerve damage, mental retardation, nerve damage, permanent brain damage or death.[33]
Eosinophilic meningitis is commonly defined by the increased number of eosinophils in the cerebrospinal fluid (CSF). In most cases, eosinophil levels rise to 10 or more eosinophils per μl in the cerebrospinal fluid, accounting for at least 10% of the total CSF leukocyte (white blood cell) count.[34] The chemical analysis of the CSF typically resembles the findings in "aseptic meningitis" with slightly elevated protein levels, normal glucose levels and negative bacterial cultures. Presence of a significantly decreased glucose on CSF analysis is an indicator of severe meningoencephalitis and may indicate a poor medical outcome. Initial CSF analysis early in the disease process may occasionally show no increase of eosinophils only to have classical increases in eosinophils in subsequent spinal fluid analysis. Caution should be advised in using eosinophilic meningitis as the only criterion for diagnosing angiostrongylus infestation in someone with classic symptoms as the disease evolves with the migration of the worms into the central nervous system.[citation needed]
Eosinophils are specialized white blood cells of the granulocytic cell line which contain granules in their cytoplasm. These granules contain proteins that are toxic to parasites. When these granules degranulate, or break down, chemicals are released that combat parasites such as A. cantonensis. Eosinophils, which are located throughout the body, are guided to sites of inflammation by chemokines when the body is infested with parasites such as A. cantonensis. Once at the site of inflammation, Type 2 cytokines are released from helper T cells, which communicate with the eosinophils, signaling them to activate. Once activated, eosinophils can begin the process of degranulation, releasing their toxic proteins in the fight against the foreign parasite.[citation needed]
Clinical signs and symptoms
According to a group case study, the most common symptoms in mild eosinophilic meningitis tend to be headache (with 100% of people in the study suffering from this symptom), photophobia or visual disturbance (92%), neck stiffness (83%), fatigue (83%), hyperesthesias (75%), vomiting (67%) and paresthesias (50%).[35][19] Incubation period is often 3 weeks, but can be 3–36 days[8] and even 80 days.[36]
Possible clinical signs and symptoms of mild and severe eosinophilic meningitis are:
- Fever is often minor or absent but the presence of high fever suggests severe disease[35]
- headaches - progressive and severe,[35] a bitemporal character in the frontal or occipital lobe[8]
- Meningismus - neck stiffness[35]
- Photophobia - sensitivity to light[35]
- Muscle weakness and fatigue[8][36]
- Nausea with or without vomiting[8][35]
- Paresthesias - tingling, prickling, or numbing of skin; may last for several weeks or months[8]
- Hyperesthesia - severe sensitivity to touch; may last for several weeks or months[35]
- Radiculitis - pain irradiated along certain areas of skin[35]
- Bladder dysfunction with urinary retention[37]
- Constipation[37]
- Brudziński’s sign[36]
- Vertigo
- Blindness
- Paralysis localized to one area; e.g. paralysis of extraocular muscles and facial palsy[36]
- General paralysis (flaccid)[8] often ascending in nature starting with the feet and progressing upwards to involve the entire body
- Coma[35]
- Death[35]
Treatment
The severity and clinical course of Angiostrongylus disease depends significantly on the ingested load of third-stage larvae,[38] creating great variability from case to case, making clinical trials difficult to design, and effectiveness of treatments difficult to discern. Typical conservative medical management including analgesics and sedatives provide minimal relief for the headaches and hyperesthesias. Removing cerebrospinal fluid at regular 3- to 7-day intervals is the only proven method of significantly reducing intracranial pressure and can be used for symptomatic treatment of headaches.[39] This process may be repeated until improvement is shown.[34] There is growing evidence of moderate quality that suggests corticosteroid therapy using prednisolone[40] or dexamethasone[41] has beneficial effect in treating the CNS symptoms related to A. cantonensis infections.[42][43] Although early research did not show treatment with antihelminthic agents (parasite killing drugs) like thiobendazole or albendazole effective in improving the clinical course of the illness,[44][35] a number or recent studies out of Thailand and China show that the combination of glucocorticoids and antihelminthics are safe and decrease the duration of headaches and the number of patients who had significant headache.[41][40][45][46] Although the addition of antihelminthic agents for management of A. cantonensis infection has a theoretic risk of precipitating a neurologic crisis by releasing an overwhelming load of antigens though simultaneous death of the larvae,[39] no study has shown this to exist in the clinical setting.[47][41][46][40] Additionally, the failure to kill parasites before they attempt to migrate out of the CNS increases the risk of mechanical damage by migrating larvae. Although combination therapy using albendazole and prednisolone has no significant advantage compared to treatment using prednisolone alone in mild cases,[48] the treatment with antihelminthics is demonstrably safe and may have significant benefit for patients with high parasite loads at risk for permanent disability or death.[33] Further studies to better define treatment regimens for mild, moderate, and severe disease would be extremely useful, but have not yet been performed due to the technical difficulties mentioned above.
Diagnosis
The diagnosis of disease caused by A. cantonensis infestation is often difficult and relies heavily on the history of a likely ingestion of a commonly infested host and the presence of typical features of the disease. The presumptive diagnosis is particularly strong when eosinophilic meningoencephalitis can be confirmed. The diagnosis of eosinophilic meningitis can be arrived at through detection of elevated cranial pressure and increased numbers of eosinophils. The diagnosis of the cause of eosinophilic meningitis and the presence of A. cantonensis is remarkably more difficult. A spinal tap, or a sample of CSF, must be taken to search for A. cantonensis worms or larvae. A. cantonensis is undetectable in the CSF of more than half of the infected individuals. Current methods of detecting specific antigens associated with A. cantonensis are also unreliable. Consequently, alternative approaches to detect antigen-antibody reactions are being explored, such as Immuno-PCR.[49] A rapid dot-blot ELISA test is also available for quick, effective and economical on-site diagnosis of A. cantonensis.[50]
References
- ^ a b Chen, H.-T. (1935). "Un nouveau nématode pulmonaire, Pulmonema cantonensis, n. g., n. sp". Annales de Parasitologie Humaine et Comparée. 13 (4): 312–317. doi:10.1051/parasite/1935134312.
- ^ Baheti NN, Sreedharan M, Krishnamoorthy T, Nair MD, Radhakrishnan K (March 2008). "Neurological picture. Eosinophilic meningitis and an ocular worm in a patient from Kerala, south India". Journal of Neurology, Neurosurgery, and Psychiatry. 79 (3): 271. doi:10.1136/jnnp.2007.122093. PMC 3106000. PMID 18281446.
- ^ Magill, Alan J.; Strickland, G. Thomas; Maguire, James H.; Ryan, Edward T.; Solomon, Tom (2012). Hunter's tropical medicine and emerging infectious disease (9th ed.). London: Elsevier Health Sciences. ISBN 9781455740437. OCLC 861539914.
- ^ Li H, Xu F, Gu JB, Chen XG (October 2008). "A severe eosinophilic meningoencephalitis caused by infection of Angiostrongylus cantonensis". The American Journal of Tropical Medicine and Hygiene. 79 (4): 568–70. PMID 18840746.
- ^ Eamsobhana, P. (December 2014). "Eosinophilic meningitis caused by Angiostrongylus cantonensis--a neglected disease with escalating importance". Tropical Biomedicine. 31 (4): 569–578. ISSN 0127-5720. PMID 25776582.
- ^ Canada, Public Health Agency of. "Pathogen Safety Data Sheet: Infectious Substances – Angiostrongylus cantonensis - Canada.ca". www.phac-aspc.gc.ca. Archived from the original on 2017-07-14. Retrieved 2018-04-13.
{{cite web}}
: Unknown parameter|dead-url=
ignored (|url-status=
suggested) (help) - ^ "Helminth Taxonomy - Phylum Nematoda". Schistosomiasis Research Group. Archived from the original on April 13, 2009. Retrieved 26 February 2009.
{{cite web}}
: Unknown parameter|dead-url=
ignored (|url-status=
suggested) (help) - ^ a b c d e f g h "EOSINOPHILIC MENINGITIS" (PDF). louisiana.gov. 2018-03-09. Archived from the original (PDF) on 2010-06-15.
{{cite web}}
: Cite has empty unknown parameter:|dead-url=
(help) - ^ Alicata, J.E. (1991). "The discovery of Angiostrongylus cantonensis as a cause of human eosinophilic meningitis". Parasitology Today. 7 (6): 151–153. doi:10.1016/0169-4758(91)90285-v.
- ^ Iwanowicz DD, Sanders LR, Schill WB, Xayavong MV, da Silva AJ, Qvarnstrom Y, Smith T (July 2015). "Spread of the Rat Lungworm (Angiostrongylus cantonensis) in Giant African Land Snails (Lissachatina fulica) in Florida, USA". Journal of Wildlife Diseases. 51 (3): 749–53. doi:10.7589/2014-06-160. PMID 25973628.
- ^ "New York teen contracts rat lungworm during Hawaii vacation". NY Daily News. Archived from the original on 2018-04-13. Retrieved 2018-04-13.
{{cite news}}
: Unknown parameter|dead-url=
ignored (|url-status=
suggested) (help) - ^ Lv S, Zhang Y, Steinmann P, Zhou XN (January 2008). "Emerging angiostrongyliasis in Mainland China". Emerging Infectious Diseases. 14 (1): 161–4. doi:10.3201/eid1401.061529. PMC 2600175. PMID 18258099.
- ^ Alicata, Joseph E. (1967). "Effect of Freezing and Boiling on the Infectivity of Third-Stage Larvae of Angiostrongylus cantonensis Present in Land Snails and Freshwater Prawns". The Journal of Parasitology. 53 (5): 1064–1066. doi:10.2307/3276839. JSTOR 3276839.
- ^ Ash, Lawrence R. (1968). "The Occurrence of Angiostrongylus cantonensis in Frogs of New Caledonia with Observations on Paratenic Hosts of Metastrongyles". The Journal of Parasitology. 54 (3): 432–436. doi:10.2307/3277060. JSTOR 3277060.
- ^ Richards CS, Merritt JW (April 1967). "Studies on Angiostrongylus cantonensis in molluscan intermediate hosts". The Journal of Parasitology. 53 (2): 382–8. doi:10.2307/3276595. JSTOR 3276595. PMID 6022396.
- ^ Campbell BG, Little MD (May 1988). "The finding of Angiostrongylus cantonensis in rats in New Orleans". The American Journal of Tropical Medicine and Hygiene. 38 (3): 568–73. PMID 3275136.
- ^ Yeung NW, Hayes KA, Cowie RH (June 2013). "Effects of washing produce contaminated with the snail and slug hosts of Angiostrongylus cantonensis with three common household solutions". Hawai'i Journal of Medicine & Public Health. 72 (6 Suppl 2): 83–6. PMC 3689494. PMID 23901391.
- ^ Cowie RH (June 2013). "Pathways for transmission of angiostrongyliasis and the risk of disease associated with them". Hawai'i Journal of Medicine & Public Health. 72 (6 Suppl 2): 70–4. PMC 3689478. PMID 23901388.
- ^ a b Slom TJ, Cortese MM, Gerber SI, Jones RC, Holtz TH, Lopez AS, Zambrano CH, Sufit RL, Sakolvaree Y, Chaicumpa W, Herwaldt BL, Johnson S (February 2002). "An outbreak of eosinophilic meningitis caused by Angiostrongylus cantonensis in travelers returning from the Caribbean". The New England Journal of Medicine. 346 (9): 668–75. doi:10.1056/NEJMoa012462. PMID 11870244.
- ^ Mentz MB, Graeff-Teixeira C (July 2003). "Drug trials for treatment of human angiostrongyliasis". Revista do Instituto de Medicina Tropical de Sao Paulo. 45 (4): 179–84. PMID 14502343.
- ^ Baig AM (December 2017). "Is There a Cholinergic Survival Incentive for Neurotropic Parasites in the Brain?". ACS Chemical Neuroscience. 8 (12): 2574–2577. doi:10.1021/acschemneuro.7b00370. PMID 28985043.
- ^ a b Lindo JF, Waugh C, Hall J, Cunningham-Myrie C, Ashley D, Eberhard ML, Sullivan JJ, Bishop HS, Robinson DG, Holtz T, Robinson RD (March 2002). "Enzootic Angiostrongylus cantonensis in rats and snails after an outbreak of human eosinophilic meningitis, JAMAica". Emerging Infectious Diseases. 8 (3): 324–6. doi:10.3201/eid0803.010316. PMC 2732477. PMID 11927033.
- ^ a b Barth JD, Jansen H, Kromhout D, Reiber JH, Birkenhager JC, Arntzenius AC (November 1987). "Progression and regression of human coronary atherosclerosis. The role of lipoproteins, lipases and thyroid hormones in coronary lesion growth". Atherosclerosis. 68 (1–2): 51–8. PMC 3689483. PMID 3689483.
- ^ a b c d e f g h i j Lv S, Zhang Y, Steinmann P, Zhou XN (January 2008). "Emerging angiostrongyliasis in Mainland China". Emerging Infectious Diseases. 14 (1): 161–4. doi:10.3201/eid1401.061529. PMC 2600175. PMID 18258099.
- ^ a b c Lv S, Zhang Y, Chen SR, Wang LB, Fang W, Chen F, Jiang JY, Li YL, Du ZW, Zhou XN (September 2009). Graeff-Teixeira C (ed.). "Human angiostrongyliasis outbreak in Dali, China". PLoS Neglected Tropical Diseases. 3 (9): e520. doi:10.1371/journal.pntd.0000520. PMC 2739427. PMID 19771154.
{{cite journal}}
: CS1 maint: unflagged free DOI (link) - ^ a b c d e f g Asato R, Taira K, Nakamura M, Kudaka J, Itokazu K, Kawanaka M (2004). "Changing Epidemiology of Angiostrongyliasis Cantonensis in Okinawa Prefecture, Japan" (PDF). Japanese Journal of Infectious Diseases. 57: 184–186.
- ^ a b c "MEMORANDUM FOR 18 MDG/SGPM" (PDF). "Land snail infection rates for the human parasitic nematode, Angiostrongylus cantonensis (rat lung worm) with notes on snail and parasite biology and distribution on Kadena AB, Okinawa Japan. Consultative Letter, IERA-DO-BR-CL-2001-0049.". Department of the Air Force. 20 June 2001. Archived from the original (PDF) on 2011-08-11.
{{cite web}}
: Unknown parameter|dead-url=
ignored (|url-status=
suggested) (help)CS1 maint: others (link) - ^ Hollingsworth, R. G.; Kaneta, R.; Sullivan, J. J.; Bishop, H. S.; Qvarnstrom, Y.; Da Silva, A. J.; Robinson, D. G. (2007). "Distribution of Parmarion cf. Martensi (Pulmonata: Helicarionidae), a New Semi-Slug Pest on Hawai'i Island, and Its Potential as a Vector for Human Angiostrongyliasis1" (PDF). Pacific Science (Submitted manuscript). 61 (4): 457–467. doi:10.2984/1534-6188(2007)61[457:DOPCMP]2.0.CO;2. hdl:10125/22629.
{{cite journal}}
: Unknown parameter|name-list-format=
ignored (|name-list-style=
suggested) (help). - ^ Senanayake SN, Pryor DS, Walker J, Konecny P (October 2003). "First report of human angiostrongyliasis acquired in Sydney". The Medical Journal of Australia. 179 (8): 430–1. PMID 14558868.
- ^ a b c d Högger C. H. (update 25 March 2003). "Antagonists of Slugs and Snails. A Bibliography of Sources and a List of Citations grouped according to Taxon of the Antagonists". in web Archive.
- ^ "Christoph Högger - Antagonists of Slugs and Snails". homepage.sunrise.ch/mysunrise/choegger. 2007-12-14. Archived from the original on 2008-05-24. Retrieved 2018-03-09.
{{cite web}}
: Cite has empty unknown parameter:|dead-url=
(help) - ^ Monks DJ, Carlisle MS, Carrigan M, Rose K, Spratt D, Gallagher A, Prociv P (2005). "Angiostrongylus cantonensis as a Cause of Cerebrospinal Disease in a Yellow-tailed Black Cockatoo (Calyptorhynchus funereus) and Two Tawny Frogmouths (Podargus strigoides)". Journal of Avian Medicine and Surgery. 19 (4): 289–293. doi:10.1647/2004-024.1.
- ^ a b Wang QP, Lai DH, Zhu XQ, Chen XG, Lun ZR (October 2008). "Human angiostrongyliasis". The Lancet. Infectious Diseases. 8 (10): 621–30. doi:10.1016/S1473-3099(08)70229-9. PMID 18922484.
- ^ a b "EOSINOPHILIC MENINGITIS". Revised 28 February 2006, accessed 1 June 2011.
- ^ a b c d e f g h i j k Murphy GS, Johnson S (June 2013). "Clinical aspects of eosinophilic meningitis and meningoencephalitis caused by Angiostrongylus cantonensis, the rat lungworm". Hawai'i Journal of Medicine & Public Health. 72 (6 Suppl 2): 35–40. PMC 3689484. PMID 23901382.
- ^ a b c d Tseng YT, Tsai HC, Sy CL, Lee SS, Wann SR, Wang YH, Chen JK, Wu KS, Chen YS (October 2011). "Clinical manifestations of eosinophilic meningitis caused by Angiostrongylus cantonensis: 18 years' experience in a medical center in southern Taiwan". Journal of Microbiology, Immunology, and Infection = Wei Mian Yu Gan Ran Za Zhi. 44 (5): 382–9. doi:10.1016/j.jmii.2011.01.034. PMID 21524976.
- ^ a b Maretić T, Perović M, Vince A, Lukas D, Dekumyoy P, Begovac J (June 2009). "Meningitis and radiculomyelitis caused by Angiostrongylus cantonensis". Emerging Infectious Diseases. 15 (6): 996–8. doi:10.3201/eid1506.081263. PMC 2727321. PMID 19523323.
- ^ Tsai HC, Liu YC, Kunin CM, Lee SS, Chen YS, Lin HH, Tsai TH, Lin WR, Huang CK, Yen MY, Yen CM (August 2001). "Eosinophilic meningitis caused by Angiostrongylus cantonensis: report of 17 cases". The American Journal of Medicine. 111 (2): 109–14. doi:10.1016/S0002-9343(01)00766-5. PMID 11498063.
- ^ a b Slom TJ, Cortese MM, Gerber SI, Jones RC, Holtz TH, Lopez AS, Zambrano CH, Sufit RL, Sakolvaree Y, Chaicumpa W, Herwaldt BL, Johnson S (February 2002). "An outbreak of eosinophilic meningitis caused by Angiostrongylus cantonensis in travelers returning from the Caribbean". The New England Journal of Medicine. 346 (9): 668–75. doi:10.1056/nejmoa012462. PMID 11870244.
- ^ a b c Chotmongkol, V (2006). "Treatment of eosinophilic meningitis with a combination of prednisolone and mebendazole". Am J Trop Med Hyg. 74: 1122–1124.
- ^ a b c Tsai, TH (2001). "An outbreak of meningitis caused by Angiostrongylus cantonensis in Kaohsiung". J Microbiol Immunol Infect. 34: 50–56.
- ^ Chotmongkol V, Sawanyawisuth K, Thavornpitak Y (September 2000). "Corticosteroid treatment of eosinophilic meningitis". Clinical Infectious Diseases. 31 (3): 660–2. doi:10.1086/314036. PMID 11017811.
- ^ Thanaviratananich S, Thanaviratananich S, Ngamjarus C (February 2015). "Corticosteroids for parasitic eosinophilic meningitis". The Cochrane Database of Systematic Reviews (2): CD009088. doi:10.1002/14651858.CD009088.pub3. PMID 25687750.
- ^ Kliks MM, Kroenke K, Hardman JM (November 1982). "Eosinophilic radiculomyeloencephalitis: an angiostrongyliasis outbreak in American Samoa related to ingestion of Achatina fulica snails". The American Journal of Tropical Medicine and Hygiene. 31 (6): 1114–22. doi:10.4269/ajtmh.1982.31.1114. PMID 7149098.
- ^ Jitpimolmard S, Sawanyawisuth K, Morakote N, Vejjajiva A, Puntumetakul M, Sanchaisuriya K, Tassaneeyakul W, Tassaneeyakul W, Korwanich N (May 2007). "Albendazole therapy for eosinophilic meningitis caused by Angiostrongylus cantonensis". Parasitology Research. 100 (6): 1293–6. doi:10.1007/s00436-006-0405-7. PMID 17177056.
- ^ a b Chotmongkol, V (2004). "Treatment of eosinophilic meningitis with a combination of albendazole and corticosteroid". Southeast Asian J Trop Med Public Health. 35: 172–74.
- ^ Chotmongkol V, Sawanyawisuth K, Thavornpitak Y (September 2000). "Corticosteroid treatment of eosinophilic meningitis". Clinical Infectious Diseases. 31 (3): 660–2. doi:10.1086/314036. PMID 11017811.
- ^ Chotmongkol, Verajit; Kittimongkolma, Suvicha; Niwattayakul, Kanigar; Intapan, Pewpan M.; Thavornpitak, Yupa (2009-09-01). "Comparison of Prednisolone Plus Albendazole with Prednisolone Alone for Treatment of Patients with Eosinophilic Meningitis". The American Journal of Tropical Medicine and Hygiene. 81 (3): 443–445. doi:10.4269/ajtmh.2009.81.443. ISSN 0002-9637.
- ^ Chye SM, Lin SR, Chen YL, Chung LY, Yen CM (January 2004). "Immuno-PCR for detection of antigen to Angiostrongylus cantonensis circulating fifth-stage worms". Clinical Chemistry. 50 (1): 51–7. doi:10.1373/clinchem.2003.020867. PMID 14709636.
- ^ Eamsobhana P, Yong HS (July 2009). "Immunological diagnosis of human angiostrongyliasis due to Angiostrongylus cantonensis (Nematoda: Angiostrongylidae)". International Journal of Infectious Diseases. 13 (4): 425–31. doi:10.1016/j.ijid.2008.09.021. PMID 19117782.
External links
"Angiostrongylus". CDC.gov. Centers for Disease Control and Prevention. 2015-12-28. Retrieved 2017-04-04.
- "DPDx - Angiostrongyliasis". CDC. 2016-10-17. Retrieved 2017-04-04. Tabs for Parasite Biology, Image Gallery, Laboratory Diagnosis, and Treatment Information.
- Angiostrongylus+cantonensis at the U.S. National Library of Medicine Medical Subject Headings (MeSH)
- Sydney Morning Herald story of human infection, Example of Angiostrongylus cantonensis human infection: Hard to swallow: slug-eating dare causes rare disease
- Angiostronglyus cantonensis on the UF / IFAS Featured Creatures website.