Wikipedia preview

出典(authority):フリー百科事典『ウィキペディア（Wikipedia）』「2016/04/22 09:27:18」(JST)

wiki en

Cysticercosis is a tissue infection caused by the young form of the pork tapeworm.^[1]^[2] People may have little or no symptoms for years.^[3]^[4] In some cases, particularly in Asia, solid lumps of between one and two centimetres may develop under the skin.^[2] After months or years these lumps can become painful and swollen and then resolve.^[4]^[3] A specific form called neurocysticercosis which affects the brain can give neurological symptoms. In developing countries this is one of the most common causes of seizures.^[4]

Cysticercosis is usually acquired by eating food or drinking water that has tapeworm eggs in it. Among foods, uncooked vegetables are the major source.^[2] The tapeworm eggs are present in the feces of a person infected with the adult worms, a condition known as taeniasis.^[4]^[5] Taeniasis, in the strict sense, is a different disease and is due to eating cysts in poorly cooked pork.^[2] People who live with someone with the tapeworm have a greater risk of getting cysticercosis.^[5] The diagnosis can be made by aspiration of a cyst.^[4] Taking pictures of the brain with computer tomography (CT) or magnetic resonance imaging (MRI) are most useful for the diagnosis of disease in the brain. An increased number of a type of white blood cell, called eosinophils, in the cerebral spinal fluid and blood is also an indicator.^[4]

Infection can be effectively prevented by personal hygiene and sanitation: this includes cooking pork well, proper toilets and sanitary practices, and improved access to clean water. Treating those with taeniasis is important to prevent spread.^[2] Treating the disease when it does not involve the nervous system may not be required.^[4] Treatment of those with neurocysticercosis may be with the medications praziquantel or albendazole. These may be required for long periods of time. Steroids, for anti-inflammation during treatment, and anti-seizure medications may also be required. Surgery is sometimes done to remove the cysts.^[2]

The pork tapeworm is particularly common in Asia, Sub-Saharan Africa, and Latin America.^[4] In some areas it is believed that up to 25% of people are affected.^[4] In the developed world it is very uncommon.^[6] Worldwide as of 2010 it caused about 1,200 deaths, up from 700 in 1990.^[7] Cysticercosis also affects pigs and cows but rarely causes symptoms as most do not live long enough.^[2] The disease has occurred in humans throughout history.^[6] It is one of the neglected tropical diseases.^[8]

1 Signs and symptoms
- 1.1 Muscles
- 1.2 Nervous system
- 1.3 Eyes
- 1.4 Skin
2 Cause
3 Diagnosis
- 3.1 Serological
- 3.2 Neurocysticercosis
  - 3.2.1 Imaging
  - 3.2.2 CSF
4 Prevention
- 4.1 Pigs
- 4.2 Limitations
- 4.3 Vaccines
  - 4.3.1 S3PVAC vaccine
- 4.4 Other
5 Management
- 5.1 Neurocysticercosis
- 5.2 Eyes
- 5.3 Skin
6 Epidemiology
- 6.1 Regions
- 6.2 Infection estimates
- 6.3 Deaths
7 History
8 Society and culture
9 References

Signs and symptoms

Muscles

Cysticerci can develop in any voluntary muscles in humans. Invasion of muscle by cysticerci can cause myositis, with fever, eosinophilia, and muscular pseudohypertrophy, which initiates with muscle swelling and later progress to atrophy and fibrosis. In most cases, it is asymptomatic since the cysticerci die and become calcified.^[9]

Nervous system

The term neurocysticercosis is generally accepted to refer to cysts in the parenchyma of the brain. It presents with seizures and, less commonly, headaches.^[10] Cysticerca in brain parenchyma are usually 5–20 mm in diameter. In subarachnoid space and fissures, lesions may be as large as 6 cm in diameter and lobulated. They may be numerous and life threatening.^[11]

Cysts located within the ventricles of the brain can block the outflow of cerebrospinal fluid and present with symptoms of increased intracranial pressure.^[12]

Racemose neurocysticercosis refers to cysts in the subarachnoid space. These can occasionally grow into large lobulated masses causing pressure on surrounding structures.^[13]

Neurocysticercosis involving the spinal cord, most commonly presenting as back pain and radiculopathy.^[14]

Eyes

In some cases, cysticerci may be found in the globe, extraocular muscles, and under the conjunctiva (subconjunctiva). Depending on the location, they may cause visual difficulties that fluctuate with eye position, retinal edema, hemorrhage, a decreased vision or even a visual loss.^[9]

Skin

Subcutaneous cysts are in the form of firm, mobile nodules, occurring mainly on the trunk and extremities.^[15] Subcutaneous nodules are sometimes painful.

Cause

Life cycle of Taenia solium

The cause of human cysticercosis is the egg form of Taenia solium (often abbreviated as T. solium and also called pork tapeworm), which is transmitted through the oral-fecal route. Eggs are accidentally ingested from contaminated water or vegetables. The eggs enter the intestine where they develop into larvae. The larvae enter bloodstream and invade host tissues, where they further develop into larvae called cysticerci. The cysticercus larva completes development in about 2 months. It is semitransparent, opalescent white, and elongate oval in shape and may reach a length of 0.6 to 1.8 cm.^[9]

Diagnosis

The traditional method of demonstrating either tapeworm eggs or proglottids in stool samples diagnoses only taeniasis, carriage of the tapeworm stage of the life cycle.^[5] Only a small minority of patients with cysticercosis will harbor a tapeworm, rendering stool studies ineffective for diagnosis.^[16] Ophthalmic cysticercosis can be diagnosed by visualizing parasite in eye by fundoscopy.

In cases of human cysticercosis, diagnosis is a sensitive problem and requires biopsy of the infected tissue or sophisticated instruments.^[17] Taenia solium eggs and proglottids found in feces, ELISA, or polyacrylamide gel electrophoresis diagnose only taeniasis and not cysticercosis. Radiological tests, such as X-ray, CT scans which demonstrate "ring-enhancing brain lesions", and MRIs, can also be used to detect diseases. X-rays are used to identify calcified larvae in the subcutaneous and muscle tissues, and CT scans and MRIs are used to find lesions in the brain.^[18]^[19]

Serological

Antibodies to cysticerci can be demonstrated in serum by EITB (Enzyme Linked Immunotransfer Blot) assay and in CSF by ELISA. An immunoblot assay using lentil-lectin (agglutinin from Lens culinaris) is highly sensitive and specific. However, Individuals with intracranial lesions and calcifications may be seronegative. In the CDC’s immunoblot assay, cysticercosis-specific antibodies can react with structural glycoprotein antigens from the larval cysts of Taenia solium.^[5] However, this is mainly a research tool not widely available in clinical practice and nearly unobtainable in resource limited settings.

Neurocysticercosis

The diagnosis of neurocysticercosis is mainly clinical, based on a compatible presentation of symptoms and findings of imaging studies.

Imaging

Neuroimaging with CT or MRI is the most useful method of diagnosis. CT scan shows both calcified and uncalcified cysts, as well as distinguishing active and inactive cysts. Cystic lesions can show ring enhancement and focal enhancing lesions. Some cystic lesions, especially the ones in ventricles and subarachnoid space may not be visible on CT scan, since the cyst fluid is isodense with cerebrospinal fluid (CSF). Thus diagnosis of extraparenchymal cysts usually relies on signs like hydrocephalus or enhanced basilar meninges. In such cases CT scan with intraventricular contrast or MRI can be used. MRI is more sensitive in detection of intraventricular cysts.^[20]^[21]

CSF

CSF findings include pleocytosis, elevated protein levels and depressed glucose levels; but these may not be always present.

Prevention

Cysticercosis is considered as “tools-ready disease” according to WHO.^[22] International Task Force for Disease Eradication in 1992 reported that cysticercosis is potentially eradicable.^[23] It is feasible because there are no animal reservoirs besides humans and pigs. The only source of Taenia solium infection for pigs is from humans, a definite host. Theoretically, breaking the life cycle seems easy by doing intervention strategies from various stages in the life cycle.^[24]

For example,

Massive chemotherapy of infected individuals, improving sanitation, and educating people are all major ways to discontinue the cycle, in which eggs from human feces are transmitted to other humans and/or pigs.
Cooking of pork or freezing it and inspecting meat are effective means to cease the life cycle
The management of pigs by treating them or vaccinating them is another possibility to intervene
The separation of pigs from human faeces by confining them in enclosed piggeries. In Western European countries post World War 2 the pig industry developed rapidly and most pigs were housed.^{[citation needed]} This was the main reason for pig cysticercosis largely being eliminated from the region. This of course is not a quick answer to the problem in developing countries.

Pigs

The intervention strategies to eradicate cysticercosis includes surveillance of pigs in foci of transmission and massive chemotherapy treatment of humans.^[23] In reality, control of T. solium by a single intervention, for instance, by treating only human population will not work because the existing infected pigs can still carry on the cycle. The proposed strategy for eradication is to do multilateral intervention by treating both human and porcine populations.^[25] It is feasible because treatment pigs with oxfendazole have been shown to be effective and once treated, they are protected from further infections for at least 3 months.^[26]

Limitations

Even with the concurrent treatment of humans and pigs, complete elimination is hard to achieve. In one study conducted in 12 villages in Peru, both humans and porcine were treated with praziquantel and oxfendazole, with the coverage of more than 75% in humans and 90% in pigs^[27] The result shows a decreased in prevalence and incidence in the intervention area; however the effect did not completely eliminate T. solium. The possible reason includes the incomplete coverage and re-infection.^[28] Even though T. solium could be eliminated through mass treatment of human and porcine population, it is not sustainable.^[25] Moreover, both tapeworm carriers of humans and pigs tend to spread the disease from endemic to non-endemic areas resulting in periodic outbreaks of cysticercosis or outbreaks in new areas.^[29]^[30]

Vaccines

Given the fact that pigs are part of a life cycle, vaccination of pigs is another feasible intervention to eliminate cysticercosis. Research studies have been focusing on vaccine against cestode parasites, since many immune cell types are found to be capable of destroying cysticercus.^[31] Many vaccine candidates are extracted from antigens of different cestodes such as Taenia solium, T. crassiceps, T. saginata, T. ovis and target oncospheres and/or cysticerci. In 1983, Molinari et al. reported the first vaccine candidate against porcine cysticercosis using antigen from cysticercus cellulosae drawn out from naturally infected.^[32] Recently, vaccines extracted from genetically engineered 45W-4B antigens have been successfully tested to pigs in an experimental condition.^[33] This type of vaccine can protect against cysticercosis in both Chinese and Mexican type of T. solium. However, it has not been tested in endemic field conditions, which is important because the realistic condition in the field differ greatly from experimental condition, and this can result in a great difference in the chances of infection and immune reaction.^[31]

Even though vaccines have been successfully generated, the feasibility of its production and usage in rural free ranging pigs still remains a challenge. If a vaccine is to be injected, the burden of work and the cost of vaccine administration to pigs will remain high and unrealistic.^[31] The incentives of using vaccines by pig owners will decrease if the vaccine administration to pigs takes time by injecting every single pig in their livestock. A hypothetical oral vaccine is proposed to be more effective in this case as it can be easily delivered to the pigs by food.^[31]

S3PVAC vaccine

The vaccine constituted by 3 peptide synthetically produced (S3Pvac) has proven its efficacy in natural conditions of transmission.^[34] The S3PVAC vaccine so far, can be considered as the best vaccine candidate to be used in endemic areas such as Mexico (20). S3Pvac consists of three protective peptides: KETc12, KETc1 and GK1, whose sequences belong to native antigens that are present in the different developmental stages of T. solium and other cestode parasites.^[31]^[35]

Non-infected pigs from rural villages in Mexico were vaccinated with S3Pvac and the vaccine reduced 98% the number of cysticerci and 50% the number of prevalence.^[34]^[36] The diagnostic method involves necropsy and tongue inspection of pigs. The natural challenge conditions used in the study proved the efficacy of the S3Pvac vaccine in transmission control of T. solium in Mexico.^[31] The S3Pvac vaccine is owned by the National Autonomous University of Mexico and the method of high scale production of the vaccine has already been developed.^[31] The validation of the vaccine in agreement with the Secretary of Animal Health in Mexico is currently in the process of completion.^[37] It is also hoped that the vaccine will be well-accepted by pig owners because they also lose their income if pigs are infected cysticercosis.^[37] Vaccination of pigs against cysticercosis, if succeeded, can potentially have a great impact on transmission control since there is no chance of re-infection once pigs receive vaccination.

Other

Cysticercosis can also be prevented by routine inspection of meat and condemnation of measly meat by the local government.^[38] However, in areas where food is scarce, cyst-infected meat might be considered as wasted since pork can provide high quality protein.^[39] At times, infected pigs are consumed within the locality or sold at low prices to traffickers who take the uninspected pigs at urban areas for sale.^[40]

Due to these limitations, cysticercosis has not been eliminated in any endemic areas.

Management

Neurocysticercosis

Asymptomatic cysts, such as those discovered incidentally on neuroimaging done for another reason, may never lead to symptomatic disease and in many cases do not require therapy. Calcified cysts have already died and involuted. Further antiparasitic therapy will be of no benefit.

Neurocysticercosis may present as hydrocephalus and acute onset seizures, thus the immediate therapy is emergent reduction of intracranial pressure and anticonvulsant medications. Once the seizures have been brought under control, antihelminthic treatments may be undertaken. The decision to treat with antiparasitic therapy is complex and based on the stage and number of cysts present, their location, and the persons specific symptoms.^[41]

Adult Taenia solium are easily treated with niclosamide, and is most commonly used in taeniasis. However cysticercosis is a complex disease and requires careful medication. Praziquantel (PZQ) is the drug of choice. In neurocysticercosis praziquantel is widely used.^[42] Albendazole appears to be more effective and a safe drug for neurocysticercosis.^[43]^[44] In complicated situation a combination of praziquantel, albendazole and steroid (such as corticosteroids to reduces the inflammation) is recommended.^[45] In the brain the cysts can be usually found on the surface. Most cases of brain cysts are found by accident, during diagnosis for other ailments. Surgical removals are the only option of complete removal even if treated successfully with medications.^[18]

Antiparasitic treatment should be given in combination with corticosteroids and anticonvulsants to reduce inflammation surrounding the cysts and lower the risk of seizures. When corticosteroids are given in combination with praziquantel, cimetidine is also given, as corticosteroids decrease action of praziquantel by enhancing its first pass metabolism. Albendazole is generally preferable over praziquantel due to its lower cost and fewer drug interactions.^[43]

Surgical intervention is much more likely to be needed in cases of intraventricular, racemose, or spinal neurocysticercosis. Treatments includes direct excision of ventricular cysts, shunting procedures, and removal of cysts via endoscopy.

Eyes

In eye disease, surgical removal is necessary for cysts within the eye itself as treating intraocular lesions with anthelmintics will elicit an inflammatory reaction causing irreversible damage to structural components. Cysts outside the globe can be treated with anthelmintics and steroids. Treatment recommendations for subcutaneous cysticercosis includes surgery, praziquantel and albendazole.^[15]

Skin

In general, subcutaneous disease does not need specific therapy. Painful or bothersome cysts can be surgically removed.

Epidemiology

Regions

Taenia solium is found worldwide, but is more common where pork is part of the diet. Cysticercosis is most prevalent where humans live in close contact with pigs. Therefore, high prevalences are reported in Mexico, Latin America, West Africa, Russia, India, Pakistan, North-East China, and Southeast Asia.^[46] In Europe it is most widespread among Slavic people.^[18]^[47]

The frequency has decreased in developed countries owing to stricter meat inspection, better hygiene and better sanitation of facilities.

Infection estimates

In Latin America, an estimated 75 million persons live in endemic areas and 400,000 people have symptomatic disease.^[48] Some studies suggest that the prevalence of cysticercosis in Mexico is between 3.1 and 3.9 percent. Other studies have found the seroprevalence in areas of Guatemala, Bolivia, and Peru as high as 20 percent in humans, and 37 percent in pigs.^[49] In Ethiopia, Kenya and the Democratic Republic of Congo around 10% of the population is infected, in Madagascar 16%. The distribution of cysticercosis coincides with the distribution of T. solium.^[50] Cysticercosis is the most common cause of symptomatic epilepsy worldwide.^[51]

Prevalence rates in the United States have shown immigrants from Mexico, Central and South America, and Southeast Asia account for most of the domestic cases of cysticercosis.^[52]

In 1990 and 1991, four unrelated members of an Orthodox Jewish community in New York City developed recurrent seizures and brain lesions, which were found to have been caused by T. solium. All of the families had housekeepers from Latin American countries and were suspected to be source of the infections.^[53]^[54]

Deaths

Worldwide as of 2010 it caused about 1,200 deaths, up from 700 in 1990.^[7]

In US during 1990–2002, 221 cysticercosis deaths were identified. Mortality rates were highest for Latinos and men. The mean age at death was 40.5 years (range 2–88). Most patients, 84.6%, were foreign born, and 62% had emigrated from Mexico. The 33 US-born persons who died of cysticercosis represented 15% of all cysticercosis-related deaths. The cysticercosis mortality rate was highest in California, which accounted for 60% of all cysticercosis deaths.^[55]

History

Scolex (head) of Taenia solium

The earliest reference to tapeworms were found in the works of ancient Egyptians that date back to almost 2000 BC.^[56] The description of measled pork in the History of Animals written by Aristotle (384–322 BC) showed that the infection of pork with tapeworm was known to ancient Greeks at that time.^[56] It was also known to Jewish^[57] and later to early Muslim physicians and has been proposed as one of the reasons for pork being forbidden by Jewish and Islamic dietary laws.^[58] Recent examination of evolutionary histories of hosts and parasites and DNA evidence show that over 10,000 years ago, ancestors of modern humans in Africa became exposed to tapeworm when they scavenged for food or preyed on antelopes and bovids, and later passed the infection on to domestic animals such as pigs.^[59]

Cysticercosis was described by Johannes Udalric Rumler in 1555; however, the connection between tapeworms and cysticercosis had not been recognized at that time.^[60] Around 1850, Friedrich Küchenmeister fed pork containing cysticerci of T. solium to humans awaiting execution in a prison, and after they had been executed, he recovered the developing and adult tapeworms in their intestines.^[56]^[60] By the middle of the 19th century, it was established that cysticercosis was caused by the ingestion of the eggs of T. solium.^[61]

Society and culture

The first patient on the television show House (in the pilot episode) had cysticercosis.
In the crossover of the series Grey's Anatomy (season 5, episode 15) and Private Practice (season 2), Archer Montgomery, brother of Addison Forbes Montgomery, suffered from neurocysticercosis. He was cured via the surgical removal of the cysts by his former brother-in-law Derek Shepherd.

References

^ Roberts, Larry S.; Janovy, Jr., John (2009). Gerald D. Schmidt & Larry S. Roberts' Foundations of Parasitology (8 ed.). Boston: McGraw-Hill Higher Education. pp. 348–351. ISBN 978-0-07-302827-9.
^ ^a ^b ^c ^d ^e ^f ^g "Taeniasis/Cysticercosis Fact sheet N°376". World Health Organization. February 2013. Retrieved 18 March 2014.
^ ^a ^b García HH, Evans CA, Nash TE, et al. (October 2002). "Current consensus guidelines for treatment of neurocysticercosis". Clin. Microbiol. Rev. 15 (4): 747–56. doi:10.1128/CMR.15.4.747-756.2002. PMC: 126865. PMID 12364377.
^ ^a ^b ^c ^d ^e ^f ^g ^h ⁱ García HH, Gonzalez AE, Evans CA, Gilman RH (August 2003). "Taenia solium cysticercosis". Lancet 362 (9383): 547–56. doi:10.1016/S0140-6736(03)14117-7. PMC: 3103219. PMID 12932389.
^ ^a ^b ^c ^d "CDC - Cysticercosis".
^ ^a ^b Bobes RJ, Fragoso G, Fleury A, et al. (April 2014). "Evolution, molecular epidemiology and perspectives on the research of taeniid parasites with special emphasis on Taenia solium". Infect. Genet. Evol. 23: 150–60. doi:10.1016/j.meegid.2014.02.005. PMID 24560729.
^ ^a ^b Lozano R, Naghavi M, Foreman K, et al. (December 2012). "Global and regional mortality from 235 causes of death for 20 age groups in 1990 and 2010: a systematic analysis for the Global Burden of Disease Study 2010". Lancet 380 (9859): 2095–128. doi:10.1016/S0140-6736(12)61728-0. PMID 23245604.
^ "Neglected Tropical Diseases". cdc.gov. June 6, 2011. Retrieved 28 November 2014.
^ ^a ^b ^c Markell, E.K.; John, D.T.; Krotoski, W.A. (1999). Markell and Voge's medical parasitology (8th ed.). Saunders. ISBN 978-0-7216-7634-0.
^ Kerstein AH, Massey AD (2010). "Neurocysticercosis". Kansas Journal of Medicine 3 (4): 52–4.
^ Fleury, A; Dessein, A; Preux, PM; Dumas, M; Tapia, G; Larralde, C; Sciutto, E (July 2004). "Symptomatic human neurocysticercosis--age, sex and exposure factors relating with disease heterogeneity.". Journal of neurology 251 (7): 830–7. PMID 15258785.
^ Suri A, Goel RK, Ahmad FU, Vellimana AK, Sharma BS, Mahapatra AK (January 2008). "Transventricular, transaqueductal scope-in-scope endoscopic excision of fourth ventricular neurocysticercosis: a series of 13 cases and a review". J Neurosurg Pediatr 1 (1): 35–9. doi:10.3171/PED-08/01/035. PMID 18352801.
^ Hauptman JS, Hinrichs C, Mele C, Lee HJ (April 2005). "Radiologic manifestations of intraventricular and subarachnoid racemose neurocysticercosis". Emerg Radiol 11 (3): 153–7. doi:10.1007/s10140-004-0383-y. PMID 16028320.
^ Jang JW, Lee JK, Lee JH, Seo BR, Kim SH. (Mar 2010). "Recurrent primary spinal subarachnoid neurocysticercosis.". Spine 35 (5): E172–5. doi:10.1097/BRS.0b013e3181b9d8b6. PMID 20118838.
^ ^a ^b Wortman PD (August 1991). "Subcutaneous cysticercosis". J. Am. Acad. Dermatol. 25 (2 Pt 2): 409–14. doi:10.1016/0190-9622(91)70217-p. PMID 1894783.
^ HH Garcia, R Araoz, RH Gilman, J Valdez, AE Gonzalez, C Gavidia, ML Bravo, and VC Tsang (1998). "Increased prevalence of cysticercosis and taeniasis among professional fried pork vendors and the general population of a village in the Peruvian highlands. Cysticercosis Working Group in Peru". Am. J. Trop. Med. Hyg. 59 (6): 902–905. PMID 9886197.
^ Richards F, Jr; Schantz, PM (1991). "Laboratory diagnosis of cysticercosis.". Clinics in Laboratory Medicine 11 (4): 1011–28. PMID 1802519.
^ ^a ^b ^c Gutierrez, Yezid (2000). "26. Cysticercosis, Coenurosis, Sparganosis and proliferating Cestode larvae". Diagnostic Pathology of Parasitic Infections with Clinical Correlations (2nd ed.). Oxford University Press. pp. 635–652. ISBN 978-0-19-512143-8.
^ Webbe, G. (1994). "Human cysticercosis: Parasitology, pathology, clinical manifestations and available treatment". Pharmacology & Therapeutics 64 (1): 175–200. doi:10.1016/0163-7258(94)90038-8. PMID 7846114.
^ Robbani, I; Razdan, S; Pandita, KK (2004). "Diagnosis of intraventricular cysticercosis by magnetic resonance imaging: improved detection with three-dimensional spoiled gradient recalled echo sequences.\". Australasian Radiology 48 (2): 237–9. doi:10.1111/j.1440-1673.2004.01279.x. PMID 15230764.
^ Lucato, L.T.; Guedes, M.S.; Sato, J.R.; Bacheschi, L.A.; Machado, L.R.; Leite, C.C. (1 September 2007). "The Role of Conventional MR Imaging Sequences in the Evaluation of Neurocysticercosis: Impact on Characterization of the Scolex and Lesion Burden". American Journal of Neuroradiology 28 (8): 1501–1504. doi:10.3174/ajnr.A0623.
^ "Global Plan to Combat Neglected Tropical Diseases 2008–2015" (PDF). World Health Organization. 2007. Box 1. Selected neglected tropical diseases and zoonoses to be addressed within the Global Plan. p. 2.
^ ^a ^b "Update: International Task Force for Disease Eradication, 1992". MMWR Morb. Mortal. Wkly. Rep. 41 (37): 691, 697–8. September 1992. PMID 1518501.
^ Schantz, P. "Eradication of T. solium Cysticercosis" International Conference on Emerging Infectious Diseases 2002. CDC.ftp://ftp.cdc.gov/pub/infectious_diseases/iceid/2002/pdf/schantz.pdf
^ ^a ^b Gonzalez AE, García HH, Gilman RH, Tsang VC (June 2003). "Control of Taenia solium". Acta Trop. 87 (1): 103–9. doi:10.1016/S0001-706X(03)00025-1. PMID 12781384.
^ Gonzalez AE, Gavidia C, Falcon N, et al. (July 2001). "Protection of pigs with cysticercosis from further infections after treatment with oxfendazole". Am. J. Trop. Med. Hyg. 65 (1): 15–8. PMID 11504400.
^ Garcia, H.H., 2002. "Effectiveness of an interventional control program for human and porcine Taenia solium cysticercosis in field conditions." In: International Health. Johns Hopkins University, Baltimore, p. 250.
^ Gilman, R.H.; Garcia, H.H.; Gonzalez, A.E.; Dunleavy, M.; Verastegui, M. (1999). "Short cuts to development: methods to control the transmission of cysticercosis in developing countries". In García, H.H.; Martínez, M. Taenia solium taeniasis/cysticercosis. Lima: Editorial Universo. pp. 313–326. ISBN 9972910202.
^ Margono SS, Subahar R, Hamid A, et al. (2001). "Cysticercosis in Indonesia: epidemiological aspects". Southeast Asian J. Trop. Med. Public Health 32 (Suppl 2): 79–84. PMID 12041608.
^ Wandra T, Subahar R, Simanjuntak GM, et al. (2000). "Resurgence of cases of epileptic seizures and burns associated with cysticercosis in Assologaima, Jayawijaya, Irian Jaya, Indonesia, 1991–95". Trans. R. Soc. Trop. Med. Hyg. 94 (1): 46–50. doi:10.1016/s0035-9203(00)90433-4. PMID 10748897.
^ ^a ^b ^c ^d ^e ^f ^g Sciutto E, Fragoso G, de Aluja AS, Hernández M, Rosas G, Larralde C (2008). "Vaccines against cysticercosis". Curr Top Med Chem 8 (5): 415–23. doi:10.2174/156802608783790839. PMID 18393905.
^ Molinari JL, Meza R, Suárez B, Palacios S, Tato P, Retana A (June 1983). "Taenia solium: immunity in hogs to the Cysticercus". Exp. Parasitol. 55 (3): 340–57. doi:10.1016/0014-4894(83)90031-0. PMID 6852171.
^ Luo X, Zheng Y, Hou J, Zhang S, Cai X (February 2009). "Protection against Asiatic Taenia solium induced by a recombinant 45W-4B protein". Clin. Vaccine Immunol. 16 (2): 230–2. doi:10.1128/CVI.00367-08. PMC: 2643551. PMID 19091992.
^ ^a ^b Huerta M, De Aluja AS, Fragoso G, Toledo A, Villalobos N, Hernandez M, Gevorkian G, Acero G, Diaz A, et al. (2001). "Synthetic peptide vaccine against Taenia solium pig cysticercosis: successful vaccination in a controlled field trial in rural Mexico". Vaccine 20 (1–2): 262–6. doi:10.1016/S0264-410X(01)00249-3. PMID 11567772.
^ http://www-lab.biomedicas.unam.mx/cistimex/s1.html#capitulo6
^ Sciutto E, Morales J, Martinez JJ, Toledo A, Villalobos MN, Cruz-Revilla C, Meneses G, Hernandez M, Diaz A, et al. (2007). "Further evaluation of the synthetic peptide vaccine S3Pvac against Taenia solium cysticercosis in pigs in an endemic town of Mexico". Parasitology 134 (Pt 1): 129–33. doi:10.1017/S0031182006001132. PMID 16948875.
^ ^a ^b E-mail interview with Edda Sciutto. Feb 26 2009.
^ http://www.cwgesa.org/CWGESA%20Action%20Plan/CWGESA%20Action%20Plan.aspx
^ CWGESA. 5th General Assembly of the Cysticercosis Working Group in Eastern and Southern Africa. 2007. CIRADhttp://pigtrop.cirad.fr/sp/recursos/publications/procedimientos/5th_general_assembly_of_the_cysticercosis_working_group_in_eastern_and_southern_africa
^ Morales J, Martínez JJ, Garcia-Castella J, et al. (March 2006). "Taenia solium: the complex interactions, of biological, social, geographical and commercial factors, involved in the transmission dynamics of pig cysticercosis in highly endemic areas". Ann Trop Med Parasitol 100 (2): 123–35. doi:10.1179/136485906x86275. PMID 16492360.
^ White AC (May 2009). "New developments in the management of neurocysticercosis". J. Infect. Dis. 199 (9): 1261–2. doi:10.1086/597758. PMID 19358667.
^ Pawlowski ZS (2006). "Role of chemotherapy of taeniasis in prevention of neurocysticercosis". Parasitol. Int. 55 (Suppl): S105–9. doi:10.1016/j.parint.2005.11.017. PMID 16356763.
^ ^a ^b Matthaiou DK, Panos G, Adamidi ES, Falagas ME. (2008). Carabin, Hélène, ed. "Albendazole versus Praziquantel in the Treatment of Neurocysticercosis: A Meta-analysis of Comparative Trials". PLOS Neglected Tropical Diseases 2 (3): e194. doi:10.1371/journal.pntd.0000194. PMC: 2265431. PMID 18335068.
^ Garcia HH, Pretell EJ, Gilman RH, Martinez SM, Moulton LH, Del Brutto OH, Herrera G, Evans CA, Gonzalez AE, Cysticercosis Working Group in Peru. (2004). "A trial of antiparasitic treatment to reduce the rate of seizures due to cerebral cysticercosis". N Engl J Med. 350 (3): 249–258. doi:10.1056/NEJMoa031294. PMID 14724304.
^ "Taeniasis/Cysticercosis". World Health Organization. Retrieved 6 February 2014.
^ Reeder, P.E.S. Palmer, M.M. (2001). Imaging of Tropical Diseases : With Epidemiological, Pathological, and Clinical Correlation (2 (revised) ed.). Heidelberg, Germany: Springer-Verlag. pp. 641–642. ISBN 978-3-540-56028-9.
^ Hansen, NJ; Hagelskjaer, LH; Christensen, T (1992). "Neurocysticercosis: a short review and presentation of a Scandinavian case.". Scandinavian Journal of Infectious Diseases 24 (3): 255–62. doi:10.3109/00365549209061330. PMID 1509231.
^ Bern C, Garcia HH, Evans C, et al. (November 1999). "Magnitude of the disease burden from neurocysticercosis in a developing country". Clin. Infect. Dis. 29 (5): 1203–9. doi:10.1086/313470. PMC: 2913118. PMID 10524964.
^ Yeh J, Sheffield JS (April 2008). "Cysticercosis: A Zebra in the Neighborhood". Virtual Mentor 10 (4): 220–3. doi:10.1001/virtualmentor.2008.10.4.cprl1-0804.
^ "Taeniasis/Cysticercosis". Zoonoses. World Health Organization.
^ "Relationship between epilepsy and tropical diseases. Commission on Tropical Diseases of the International League Against Epilepsy". Epilepsia 35 (1): 89–93. 1994. doi:10.1111/j.1528-1157.1994.tb02916.x. PMID 8112262.
^ Flisser A. (May 1988). "Neurocysticercosis in Mexico". Parasitology Today 4 (5): 131–137. doi:10.1016/0169-4758(88)90187-1. PMID 15463066.
^ Dworkin, Mark S. (2010). Outbreak Investigations Around the World: Case Studies in Infectious Disease. Jones and Bartlett Publishers. pp. 192–196. ISBN 978-0-7637-5143-2. Retrieved August 9, 2011.
^ Schantz, Peter M.; Moore, Anne C.; et al. (September 3, 1992). "Neurocysticercosis in an Orthodox Jewish Community in New York City". New England Journal of Medicine 327 (10): 692–695. doi:10.1056/NEJM199209033271004.
^ Sorvillo FJ, DeGiorgio C, Waterman SH (February 2007). "Deaths from cysticercosis, United States". Emerging Infect. Dis. 13 (2): 230–5. doi:10.3201/eid1302.060527. PMC: 2725874. PMID 17479884.
^ ^a ^b ^c Wadia, N.H.; Singh, G. (2002). "Taenia Solium: A Historical Note". In Singh, G.; Prabhakar, S. Taenia Solium Cysticercosis: From Basic to Clinical Science. CABI Publishing. pp. 157–168. ISBN 0851996280.
^ Ancient Hebrew Medicine<http://www.healthguidance.org/entry/6309/1/Ancient-Hebrew-Medicine.html>
^ del Brutto, O.H.; Sotelo, J.; Román, G.C. (1998). Neurocysticercosis. Taylor and Francis. p. 3. ISBN 90-265-1513-8.
^ Becker H (May 2001). "Out of Africa: The Origins of the Tapeworms". Agricultural Research Magazine (US Department of Agriculture) 49 (5).
^ ^a ^b Cox FE (October 2002). "History of human parasitology". Clin. Microbiol. Rev. 15 (4): 595–612. doi:10.1128/CMR.15.4.595-612.2002. PMC: 126866. PMID 12364371.
^ Küchenmeister, F. The Cysticercus cellulosus transformed within the organism of man into Taenia solium. Lancet 1861 i:39.

"Taenia solium". NCBI Taxonomy Browser. 6204.

UpToDate Contents

全文を閲覧するには購読必要です。 To read the full text you will need to subscribe.

1. 嚢虫症の臨床症状および診断 clinical manifestations and diagnosis of cysticercosis
2. 嚢虫症の治療 treatment of cysticercosis
3. 嚢虫症の疫学、感染、および予防 epidemiology transmission and prevention of cysticercosis
4. 腸管条虫 intestinal tapeworms
5. 駆虫薬療法 anthelminthic therapies

English Journal

A mouse air pouch model for evaluating the immune response to Taenia crassiceps infection.

Gaspar EB1, Sakai YI2, De Gaspari E3.Author information 1Embrapa South Animal Husbandry & Sheep, Bagé, RS, Brazil.2Department of Pathology, Adolfo Lutz Institute, São Paulo, SP, Brazil.3Department of Immunology, Adolfo Lutz Institute, São Paulo, SP, Brazil. Electronic address: egaspari@ial.sp.gov.br.AbstractThe experimental system of Taenia crassiceps cysticerci infection in BALB/c mice is considered to be the most representative model of cysticercosis. In our work, mice were sacrificed 7 and 30days after infection, and pouch fluid was collected to determine the number of accumulated cells and the concentrations of IFNγ, IL-2, IL-4, IL-6, IL-10 and nitric oxide. The injection of 50 nonbudding cysticerci into normal mouse dorsal air pouches induced a high level of IFNγ and nitric oxide production relative to the parasite load. The air pouch provides a convenient cavity that allows studying the cellular immunological aspects of the T. crassiceps parasite. The nonbudding cysticerci recovered from the air pouches contained cells that can reconstitute complete cysts in the peritoneal cavity of mice. In conclusion, these results demonstrate that the air pouch model is an alternative tool for the evaluation of the immune characteristics of T. crassiceps infection.
Experimental parasitology.Exp Parasitol.2014 Feb;137:66-73. doi: 10.1016/j.exppara.2013.12.005. Epub 2013 Dec 28.
The experimental system of Taenia crassiceps cysticerci infection in BALB/c mice is considered to be the most representative model of cysticercosis. In our work, mice were sacrificed 7 and 30days after infection, and pouch fluid was collected to determine the number of accumulated cells and the conc
PMID 24378477

Historic of therapeutic efficacy of albendazol sulphoxide administered in different routes, dosages and treatment schemes, against Taenia saginata cysticercus in cattle experimentally infected.

Lopes WD1, Cruz BC2, Soares VE3, Nunes JL4, Teixeira WF2, Maciel WG2, Buzzulini C2, Pereira JC2, Felippelli G2, Soccol VT5, de Oliveira GP2, da Costa AJ2.Author information 1Faculdade de Ciências Agrárias e Veterinárias, UNESP/CPPAR, Via de Acesso Prof. Paulo Donatto Castellani, s/n CEP 14884-900, Jaboticabal, São Paulo, Brazil. Electronic address: wdzlopes@fcav.unesp.br.2Faculdade de Ciências Agrárias e Veterinárias, UNESP/CPPAR, Via de Acesso Prof. Paulo Donatto Castellani, s/n CEP 14884-900, Jaboticabal, São Paulo, Brazil.3Faculdade de Ciências Agrárias e Veterinárias, UNESP/CPPAR, Via de Acesso Prof. Paulo Donatto Castellani, s/n CEP 14884-900, Jaboticabal, São Paulo, Brazil; Universidade Camilo Castelo Branco - UNICASTELO. Av. Hilário da Silva Passos, 950. Parqui universitário - Descalvado-SP, CEP13690-970, Brazil.4Faculdade de Ciências Agrárias e Veterinárias, UNESP/CPPAR, Via de Acesso Prof. Paulo Donatto Castellani, s/n CEP 14884-900, Jaboticabal, São Paulo, Brazil; Centro Universitário Barão de Mauá. Rua Laguna, 241 - Jardim Paulista, Ribeirão Preto-SP, CEP 1409-180, Brazil.5Universidade Federal do Paraná. Rua Quinze de Novembro, Curitiba-PR, CEP 80060-000, Brazil.AbstractThe present study aimed to notify the history of albendazole sulphoxide (ALB-SO) and albendazole (ALBZ) efficacy against Taenia saginata cysticercus (Cysticercus bovis) parasitizing experimentally infected bovines. A total of 11 efficacy trials were performed between the years of 2002 and 2010. In order to perform these trials, animals were individually inoculated with 2×10(4) eggs of T. saginata in each study's day zero (D0). For every trial, a positive control group (untreated infected animals) and a negative control group (animals that were neither infected nor treated) were used. ALB-SO or ALB were administered in the different dosages, in different days of treatments. In a last study with this formulation, this active principle was administered orally, mixed with the mineral supplement, on the 60th DPI, in a dosage of 30mg/kg. In all trials, on the 100th DPI, all animals were euthanized and submitted to the sequenced slicing of 26 anatomical segments (fragments of approximately five millimeters) for the survey of T. saginata cysticercus. With the obtained results it is possible to verify that in the first trials, conducted in 2002, ALB-SO reached, independently of dosage and treatment scheme, efficacies superior to 98% (arithmetic means). The trials conducted in 2005 (2.5mg/kg on the 30th, 60th, and 90th DPI) obtained values of efficacy all inferior to 60%. In 2008, the trials with 2.5 and 7.7mg/kg demonstrated efficacy values inferior to 40%, for both dosages and treatment schemes (30th/60th/90th DPI and 60th DPI). When this formulation was administered orally on the dosage of 30mg/kg on the 60th DPI, the efficacy against T. saginata cysticercus reached 88.28%. ALB administered orally showed efficacy values of 0.0%, 29.88% and 28.64% in the dosages of 5, 10 and 15mg/kg, respectively, using the treatment schemes described above for each dosage. Based on the results of these trials, conducted in an eight year period (2002-2010) using the sequenced slicing method for evaluating the efficacy of the aforementioned formulations against T. saginata cysticercus, it is possible to observe that, amongst the few molecules used in the chemotherapic treatment against T. saginata larvae, ALB-SO, administered in varied routes, dosages and treatment schemes, the studies conducted in 2008, 2009, and 2010, have a low therapeutic efficacy against C. bovis in Brazil, while ALBZ had insignificant efficacy values against T. saginata larvae parasitizing experimentally infected bovines. However, future studies using molecular biology will be necessary to assess whether the difference on the efficacy of the ALB-SO can be related to strain or another specific factor.
Experimental parasitology.Exp Parasitol.2014 Feb;137:14-20. doi: 10.1016/j.exppara.2013.11.007. Epub 2013 Dec 2.
The present study aimed to notify the history of albendazole sulphoxide (ALB-SO) and albendazole (ALBZ) efficacy against Taenia saginata cysticercus (Cysticercus bovis) parasitizing experimentally infected bovines. A total of 11 efficacy trials were performed between the years of 2002 and 2010. In o
PMID 24309372

Case 202: extensive unilateral widening of virchow-robin spaces.

Mölzer G, Robinson S.Author information From the Diagnose Zentrum Urania, Laurenzerberg 2, A-1010 Vienna, Austria.AbstractHistory A 57-year-old woman was referred to our institute in 2010 by a neurologist for a follow-up brain magnetic resonance (MR) examination. She had not experienced any acute change in symptoms, but unspecific unilateral hyperintensities in her left cerebral hemisphere had been noted at a previous MR examination in 2004. Since 2001, she had been repeatedly seen in neurology departments for recurrent episodes of clumsiness of her left hand and frequent headaches. Her other medical history was unremarkable, as were the findings of a neurologic examination. She was not born prematurely, she was not hypertensive, and she had not shown signs or symptoms suggestive of immune incompetence or autoimmune disease. There was no history of meningitis or encephalitis. A source for embolic foci could not be established. Serology indicated no previous cysticercosis infection. Her laboratory test results were normal. Since no other underlying cause had been previously considered, a radiologist from another institute postulated that her left hemispheric hyperintensities could be seen as a rudimentary expression of tuberous sclerosis lacking the classic clinical triad. The MR examination in our institution was performed to rule out progression. The resulting images were compared with those obtained in 2004.
Radiology.Radiology.2014 Feb;270(2):623-6. doi: 10.1148/radiol.13110419.
History A 57-year-old woman was referred to our institute in 2010 by a neurologist for a follow-up brain magnetic resonance (MR) examination. She had not experienced any acute change in symptoms, but unspecific unilateral hyperintensities in her left cerebral hemisphere had been noted at a previous
PMID 24471396

Japanese Journal

Neurocysticercosis with Diplopia Responds Well to Albendazole

Internal Medicine 55(9), 1219-1222, 2016
NAID 130005149588

The present situation and towards the prevention and control of neurocysticercosis on the tropical island, Bali, Indonesia

Parasites and Vectors 8, 2015-03-07
NAID 120005758428

The present situation and towards the prevention and control of neurocysticercosis on the tropicalisland, Bali, Indonesia

Parasites and Vectors (8), 1-11, 2015-03
NAID 120005553885

Related Pictures

★リンクテーブル★

リンク元	「顧みられない熱帯病」「有鉤嚢虫症」「嚢虫症」「有鈎嚢虫」

「顧みられない熱帯病」

Cysticercosis
	Magnetic resonance image in a person with neurocysticercosis showing many cysts within the brain.
Classification and external resources
Specialty	Infectious disease
ICD-10	B69
ICD-9-CM	123.1
DiseasesDB	3341
MedlinePlus	000627
eMedicine	emerg/119 med/494 ped/537
MeSH	D003551
	[edit on Wikidata]

　　[★]

英: neglected tropical diseases, NTDs

neglected tropical diseases

ブルーリ潰瘍 Buruli ulcer (マイコバクテリウム・ウルセランス感染症 Mycobacterium ulcerans infection)
シャーガス病 Chagas disease
デング熱 Dengue/severe Dengue
メジナ虫症 dracunculiasis (ギニア虫症 guinea-worm disease)
包虫症 echinococcosis
食物媒介吸虫類感染症 foodborne trematodiases
アフリカトリパノソーマ human african trypanosomiasis (睡眠病 sleeping sickness)
リーシュマニア症 leishmaniasis
ハンセン病 leprosy
リンパ系フィラリア症 lymphatic filariasis(象皮症 elephantiasis)　・・・　糸状虫性象皮症
オンコセルカ症 onchocerciasis (河盲症 river blindness)
狂犬病 rabies
住血吸虫症 schistosomiasis
土壌伝播寄生虫症 soil transmitted helminthiases
条虫症 taeniasis/嚢尾虫症 cysticercosis
トラコーマ trachoma
イチゴ腫 yaws (トレポネーマ感染症 endemic treponematoses)

other 'neglected' conditions

足菌腫 mycetoma 菌腫
ポドコニオシス非糸状虫性象皮症 podoconiosis
疥癬 scabies
蛇咬傷 snakebite
糞線虫症 strongyloidiasis

参考

http://www.who.int/neglected_diseases/diseases/en/

「有鉤嚢虫症」

　　[★]

英: cysticercosis
関: 嚢虫症

[show details]

有鉤嚢虫症 : 約 28,300 件
有鈎嚢虫症 : 約 59 件
有鉤嚢虫 : 約 50,700 件
有鈎嚢虫 : 約 132,000 件

「嚢虫症」

　　[★]

英: cysticercosis
同: 幼条虫症 metacestodiasis
関: 有鉤嚢虫症、人体有鉤嚢虫症、有鉤条虫

「有鈎嚢虫」

　　[★]

関: 有鉤嚢虫症有鈎嚢虫症 cysticercosis

[1] Roberts, Larry S.; Janovy, Jr., John (2009). Gerald D. Schmidt & Larry S. Roberts' Foundations of Parasitology (8 ed.). Boston: McGraw-Hill Higher Education. pp. 348–351. ISBN 978-0-07-302827-9.

[WHO2013-2] ^ ^a ^b ^c ^d ^e ^f ^g "Taeniasis/Cysticercosis Fact sheet N°376". World Health Organization. February 2013. Retrieved 18 March 2014.

[Gar2002-3] García HH, Evans CA, Nash TE, et al. (October 2002). "Current consensus guidelines for treatment of neurocysticercosis". Clin. Microbiol. Rev. 15 (4): 747–56. doi:10.1128/CMR.15.4.747-756.2002. PMC: 126865. PMID 12364377.

[Garcia03-4] ^ ^a ^b ^c ^d ^e ^f ^g ^h ⁱ García HH, Gonzalez AE, Evans CA, Gilman RH (August 2003). "Taenia solium cysticercosis". Lancet 362 (9383): 547–56. doi:10.1016/S0140-6736(03)14117-7. PMC: 3103219. PMID 12932389.

[CDC-5] "CDC - Cysticercosis".

[Bob2014-6] Bobes RJ, Fragoso G, Fleury A, et al. (April 2014). "Evolution, molecular epidemiology and perspectives on the research of taeniid parasites with special emphasis on Taenia solium". Infect. Genet. Evol. 23: 150–60. doi:10.1016/j.meegid.2014.02.005. PMID 24560729.

[Loz2012-7] Lozano R, Naghavi M, Foreman K, et al. (December 2012). "Global and regional mortality from 235 causes of death for 20 age groups in 1990 and 2010: a systematic analysis for the Global Burden of Disease Study 2010". Lancet 380 (9859): 2095–128. doi:10.1016/S0140-6736(12)61728-0. PMID 23245604.

[8] "Neglected Tropical Diseases". cdc.gov. June 6, 2011. Retrieved 28 November 2014.

[test-9] Markell, E.K.; John, D.T.; Krotoski, W.A. (1999). Markell and Voge's medical parasitology (8th ed.). Saunders. ISBN 978-0-7216-7634-0.

[pmid19836788-10] Kerstein AH, Massey AD (2010). "Neurocysticercosis". Kansas Journal of Medicine 3 (4): 52–4.

[11] Fleury, A; Dessein, A; Preux, PM; Dumas, M; Tapia, G; Larralde, C; Sciutto, E (July 2004). "Symptomatic human neurocysticercosis--age, sex and exposure factors relating with disease heterogeneity.". Journal of neurology 251 (7): 830–7. PMID 15258785.

[12] Suri A, Goel RK, Ahmad FU, Vellimana AK, Sharma BS, Mahapatra AK (January 2008). "Transventricular, transaqueductal scope-in-scope endoscopic excision of fourth ventricular neurocysticercosis: a series of 13 cases and a review". J Neurosurg Pediatr 1 (1): 35–9. doi:10.3171/PED-08/01/035. PMID 18352801.

[13] Hauptman JS, Hinrichs C, Mele C, Lee HJ (April 2005). "Radiologic manifestations of intraventricular and subarachnoid racemose neurocysticercosis". Emerg Radiol 11 (3): 153–7. doi:10.1007/s10140-004-0383-y. PMID 16028320.

[14] Jang JW, Lee JK, Lee JH, Seo BR, Kim SH. (Mar 2010). "Recurrent primary spinal subarachnoid neurocysticercosis.". Spine 35 (5): E172–5. doi:10.1097/BRS.0b013e3181b9d8b6. PMID 20118838.

[eight-15] Wortman PD (August 1991). "Subcutaneous cysticercosis". J. Am. Acad. Dermatol. 25 (2 Pt 2): 409–14. doi:10.1016/0190-9622(91)70217-p. PMID 1894783.

[pmid9886197-16] HH Garcia, R Araoz, RH Gilman, J Valdez, AE Gonzalez, C Gavidia, ML Bravo, and VC Tsang (1998). "Increased prevalence of cysticercosis and taeniasis among professional fried pork vendors and the general population of a village in the Peruvian highlands. Cysticercosis Working Group in Peru". Am. J. Trop. Med. Hyg. 59 (6): 902–905. PMID 9886197.

[17] Richards F, Jr; Schantz, PM (1991). "Laboratory diagnosis of cysticercosis.". Clinics in Laboratory Medicine 11 (4): 1011–28. PMID 1802519.

[gut-18] Gutierrez, Yezid (2000). "26. Cysticercosis, Coenurosis, Sparganosis and proliferating Cestode larvae". Diagnostic Pathology of Parasitic Infections with Clinical Correlations (2nd ed.). Oxford University Press. pp. 635–652. ISBN 978-0-19-512143-8.

[19] Webbe, G. (1994). "Human cysticercosis: Parasitology, pathology, clinical manifestations and available treatment". Pharmacology & Therapeutics 64 (1): 175–200. doi:10.1016/0163-7258(94)90038-8. PMID 7846114.

[20] Robbani, I; Razdan, S; Pandita, KK (2004). "Diagnosis of intraventricular cysticercosis by magnetic resonance imaging: improved detection with three-dimensional spoiled gradient recalled echo sequences.\". Australasian Radiology 48 (2): 237–9. doi:10.1111/j.1440-1673.2004.01279.x. PMID 15230764.

[21] Lucato, L.T.; Guedes, M.S.; Sato, J.R.; Bacheschi, L.A.; Machado, L.R.; Leite, C.C. (1 September 2007). "The Role of Conventional MR Imaging Sequences in the Evaluation of Neurocysticercosis: Impact on Characterization of the Scolex and Lesion Burden". American Journal of Neuroradiology 28 (8): 1501–1504. doi:10.3174/ajnr.A0623.

[22] "Global Plan to Combat Neglected Tropical Diseases 2008–2015" (PDF). World Health Organization. 2007. Box 1. Selected neglected tropical diseases and zoonoses to be addressed within the Global Plan. p. 2.

[TaskForce92-23] "Update: International Task Force for Disease Eradication, 1992". MMWR Morb. Mortal. Wkly. Rep. 41 (37): 691, 697–8. September 1992. PMID 1518501.

[eleven-24] Schantz, P. "Eradication of T. solium Cysticercosis" International Conference on Emerging Infectious Diseases 2002. CDC.ftp://ftp.cdc.gov/pub/infectious_diseases/iceid/2002/pdf/schantz.pdf

[Gonzalez03-25] Gonzalez AE, García HH, Gilman RH, Tsang VC (June 2003). "Control of Taenia solium". Acta Trop. 87 (1): 103–9. doi:10.1016/S0001-706X(03)00025-1. PMID 12781384.

[fifteen-26] Gonzalez AE, Gavidia C, Falcon N, et al. (July 2001). "Protection of pigs with cysticercosis from further infections after treatment with oxfendazole". Am. J. Trop. Med. Hyg. 65 (1): 15–8. PMID 11504400.

[27] Garcia, H.H., 2002. "Effectiveness of an interventional control program for human and porcine Taenia solium cysticercosis in field conditions." In: International Health. Johns Hopkins University, Baltimore, p. 250.

[28] Gilman, R.H.; Garcia, H.H.; Gonzalez, A.E.; Dunleavy, M.; Verastegui, M. (1999). "Short cuts to development: methods to control the transmission of cysticercosis in developing countries". In García, H.H.; Martínez, M. Taenia solium taeniasis/cysticercosis. Lima: Editorial Universo. pp. 313–326. ISBN 9972910202.

[29] Margono SS, Subahar R, Hamid A, et al. (2001). "Cysticercosis in Indonesia: epidemiological aspects". Southeast Asian J. Trop. Med. Public Health 32 (Suppl 2): 79–84. PMID 12041608.

[30] Wandra T, Subahar R, Simanjuntak GM, et al. (2000). "Resurgence of cases of epileptic seizures and burns associated with cysticercosis in Assologaima, Jayawijaya, Irian Jaya, Indonesia, 1991–95". Trans. R. Soc. Trop. Med. Hyg. 94 (1): 46–50. doi:10.1016/s0035-9203(00)90433-4. PMID 10748897.

[twenty-31] ^ ^a ^b ^c ^d ^e ^f ^g Sciutto E, Fragoso G, de Aluja AS, Hernández M, Rosas G, Larralde C (2008). "Vaccines against cysticercosis". Curr Top Med Chem 8 (5): 415–23. doi:10.2174/156802608783790839. PMID 18393905.

[32] Molinari JL, Meza R, Suárez B, Palacios S, Tato P, Retana A (June 1983). "Taenia solium: immunity in hogs to the Cysticercus". Exp. Parasitol. 55 (3): 340–57. doi:10.1016/0014-4894(83)90031-0. PMID 6852171.

[33] Luo X, Zheng Y, Hou J, Zhang S, Cai X (February 2009). "Protection against Asiatic Taenia solium induced by a recombinant 45W-4B protein". Clin. Vaccine Immunol. 16 (2): 230–2. doi:10.1128/CVI.00367-08. PMC: 2643551. PMID 19091992.

[Huerta_M_2001-34] Huerta M, De Aluja AS, Fragoso G, Toledo A, Villalobos N, Hernandez M, Gevorkian G, Acero G, Diaz A, et al. (2001). "Synthetic peptide vaccine against Taenia solium pig cysticercosis: successful vaccination in a controlled field trial in rural Mexico". Vaccine 20 (1–2): 262–6. doi:10.1016/S0264-410X(01)00249-3. PMID 11567772.

[35] ttp://www-lab.biomedicas.unam.mx/cistimex/s1.html#capitulo6

[36] Sciutto E, Morales J, Martinez JJ, Toledo A, Villalobos MN, Cruz-Revilla C, Meneses G, Hernandez M, Diaz A, et al. (2007). "Further evaluation of the synthetic peptide vaccine S3Pvac against Taenia solium cysticercosis in pigs in an endemic town of Mexico". Parasitology 134 (Pt 1): 129–33. doi:10.1017/S0031182006001132. PMID 16948875.

[twenty_seven-37] E-mail interview with Edda Sciutto. Feb 26 2009.

[38] ttp://www.cwgesa.org/CWGESA%20Action%20Plan/CWGESA%20Action%20Plan.aspx

[39] CWGESA. 5th General Assembly of the Cysticercosis Working Group in Eastern and Southern Africa. 2007. CIRADhttp://pigtrop.cirad.fr/sp/recursos/publications/procedimientos/5th_general_assembly_of_the_cysticercosis_working_group_in_eastern_and_southern_africa

[40] Morales J, Martínez JJ, Garcia-Castella J, et al. (March 2006). "Taenia solium: the complex interactions, of biological, social, geographical and commercial factors, involved in the transmission dynamics of pig cysticercosis in highly endemic areas". Ann Trop Med Parasitol 100 (2): 123–35. doi:10.1179/136485906x86275. PMID 16492360.

[41] White AC (May 2009). "New developments in the management of neurocysticercosis". J. Infect. Dis. 199 (9): 1261–2. doi:10.1086/597758. PMID 19358667.

[42] Pawlowski ZS (2006). "Role of chemotherapy of taeniasis in prevention of neurocysticercosis". Parasitol. Int. 55 (Suppl): S105–9. doi:10.1016/j.parint.2005.11.017. PMID 16356763.

[Matthaiou08-43] Matthaiou DK, Panos G, Adamidi ES, Falagas ME. (2008). Carabin, Hélène, ed. "Albendazole versus Praziquantel in the Treatment of Neurocysticercosis: A Meta-analysis of Comparative Trials". PLOS Neglected Tropical Diseases 2 (3): e194. doi:10.1371/journal.pntd.0000194. PMC: 2265431. PMID 18335068.

[44] Garcia HH, Pretell EJ, Gilman RH, Martinez SM, Moulton LH, Del Brutto OH, Herrera G, Evans CA, Gonzalez AE, Cysticercosis Working Group in Peru. (2004). "A trial of antiparasitic treatment to reduce the rate of seizures due to cerebral cysticercosis". N Engl J Med. 350 (3): 249–258. doi:10.1056/NEJMoa031294. PMID 14724304.

[45] "Taeniasis/Cysticercosis". World Health Organization. Retrieved 6 February 2014.

[46] Reeder, P.E.S. Palmer, M.M. (2001). Imaging of Tropical Diseases : With Epidemiological, Pathological, and Clinical Correlation (2 (revised) ed.). Heidelberg, Germany: Springer-Verlag. pp. 641–642. ISBN 978-3-540-56028-9.

[47] Hansen, NJ; Hagelskjaer, LH; Christensen, T (1992). "Neurocysticercosis: a short review and presentation of a Scandinavian case.". Scandinavian Journal of Infectious Diseases 24 (3): 255–62. doi:10.3109/00365549209061330. PMID 1509231.

[48] Bern C, Garcia HH, Evans C, et al. (November 1999). "Magnitude of the disease burden from neurocysticercosis in a developing country". Clin. Infect. Dis. 29 (5): 1203–9. doi:10.1086/313470. PMC: 2913118. PMID 10524964.

[49] Yeh J, Sheffield JS (April 2008). "Cysticercosis: A Zebra in the Neighborhood". Virtual Mentor 10 (4): 220–3. doi:10.1001/virtualmentor.2008.10.4.cprl1-0804.

[50] "Taeniasis/Cysticercosis". Zoonoses. World Health Organization.

[51] "Relationship between epilepsy and tropical diseases. Commission on Tropical Diseases of the International League Against Epilepsy". Epilepsia 35 (1): 89–93. 1994. doi:10.1111/j.1528-1157.1994.tb02916.x. PMID 8112262.

[52] Flisser A. (May 1988). "Neurocysticercosis in Mexico". Parasitology Today 4 (5): 131–137. doi:10.1016/0169-4758(88)90187-1. PMID 15463066.

[53] Dworkin, Mark S. (2010). Outbreak Investigations Around the World: Case Studies in Infectious Disease. Jones and Bartlett Publishers. pp. 192–196. ISBN 978-0-7637-5143-2. Retrieved August 9, 2011.

[54] Schantz, Peter M.; Moore, Anne C.; et al. (September 3, 1992). "Neurocysticercosis in an Orthodox Jewish Community in New York City". New England Journal of Medicine 327 (10): 692–695. doi:10.1056/NEJM199209033271004.

[55] Sorvillo FJ, DeGiorgio C, Waterman SH (February 2007). "Deaths from cysticercosis, United States". Emerging Infect. Dis. 13 (2): 230–5. doi:10.3201/eid1302.060527. PMC: 2725874. PMID 17479884.

[four-56] Wadia, N.H.; Singh, G. (2002). "Taenia Solium: A Historical Note". In Singh, G.; Prabhakar, S. Taenia Solium Cysticercosis: From Basic to Clinical Science. CABI Publishing. pp. 157–168. ISBN 0851996280.

[57] Ancient Hebrew Medicine<http://www.healthguidance.org/entry/6309/1/Ancient-Hebrew-Medicine.html>

[58] Brutto, O.H.; Sotelo, J.; Román, G.C. (1998). Neurocysticercosis. Taylor and Francis. p. 3. ISBN 90-265-1513-8.

[seven-59] Becker H (May 2001). "Out of Africa: The Origins of the Tapeworms". Agricultural Research Magazine (US Department of Agriculture) 49 (5).

[Cox02-60] Cox FE (October 2002). "History of human parasitology". Clin. Microbiol. Rev. 15 (4): 595–612. doi:10.1128/CMR.15.4.595-612.2002. PMC: 126866. PMID 12364371.

[six-61] Küchenmeister, F. The Cysticercus cellulosus transformed within the organism of man into Taenia solium. Lancet 1861 i:39.

匿名

検索

案内

cysticercosis

Wikipedia preview

wiki en

Contents

Signs and symptoms

Muscles

Nervous system

Eyes

Skin

Cause

Diagnosis

Serological

Neurocysticercosis

Imaging

CSF

Prevention

Pigs

Limitations

Vaccines

S3PVAC vaccine

Other

Management

Neurocysticercosis

Eyes

Skin

Epidemiology

Regions

Infection estimates

Deaths

History

Society and culture

References

UpToDate Contents

English Journal

Japanese Journal

Related Links

Related Pictures

★リンクテーブル★

「顧みられない熱帯病」

neglected tropical diseases

other 'neglected' conditions

参考

「有鉤嚢虫症」

「嚢虫症」

「有鈎嚢虫」