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Parasitic Infestations
Basim Asmar, M.D.
Wayne State University School of Medicine Children’s Hospital of Michigan Division of Infectious Diseases
Parasitic Infestations
Parasitic diseases: Caused by protozoa or helminths Parasitic protozoa & helminths : Referred to as animal parasites to distinguish them from bacteria, fungi & viruses Endoparasitic protozoa: A diverse group of >10,000 eukayotic unicellular animals Endoparasitic helminths of humans: Two phyla – (1) Platyheminths (flatworms) (2) Nematoda (round-worms)
Intestinal Parasitic Infestations Protozoa Giardia lamblia (Giardiasis)
• A flagellated protozoan • Infects the duodenum and upper part of the small
intestine
• Infection is often asymptometic but can be associated
with a variety of intestinal manifestations
Giardia lamblia
Giardia lamblia
Giardia lamblia - Life Cycle
• Infection occurs by the ingestion of • In the small intestine, excystation releases trophozoites that multiply by longitudinal binary fission. • The trophozoites remain in the lumen of the proximal small bowel where they can be free or attached to the mucosa by a ventral sucking disk. • Encystation occurs when the parasites transit toward the colon, and cysts are the stage found in normal (non diarrheal) feces. • The cysts are hardy, can survive several months in cold water, and are responsible for transmission. • Because the cysts are infectious when passed in the stool or shortly afterward, person-to-person transmission is possible. • While animals are infected with Giardia, their importance as a reservoir is unclear.
Giardia lamblia
In wet mounts, cysts show the typical ovoid ellipsoid shape measuring from 8-19 mm (range 11-14 mm)
Giardia trophozoite
(Trichrome stain x 1000)
Giardia lamblia
• 10-25 cysts sufficient to initiate infection • Colonization
may result in morphologic damage to normal microvilli or subtotal atrophy
– Disaccharidase deficiencies (usually lactase) – Malabsorption affecting protein & fat-soluble vitamines – Decreased intestinal absorption of antibiotics
Giardia lamblia
• Cysts viable for 3 months in water at 4
o C
• Freezing does not eliminate infectivity
completely
• Heating, drying and sea water are likely
to do so
• Human milk is lethal to Giardia trophozoites
through the action of fatty acids
• Duodenal fluid is also lethal to Giardia • Survival in hostile environment is attributed to
the protective effect of human mucus
Giardia lamblia
• Anti-Giardia IgG is found in >80% of patients during
symptomatic infection
• Anti-Giardia IgG tends to persist, thus limiting
usefulness in distinguishing current from past infection
• Serum anti-Giardia IgM antibodies increase early in
infection and decrease rapidly after 2-3 weeks
• Human milk protection against Giardia correlates
with anti-Giardia serum IgA
Giardiasis
Epidemiology
• Occurs worldwide • Age-specific prevalence: – Highest in children 0-5 years – Followed by 31-40 years old • Most cases reported in late summer and early fall • Transmission is common in certain high risk populations: – Children and employees in DCC’s – Consumers of contaminated water – Travelers to certain areas of the world – Those exposed to domestic and wild animals (dogs, cats, cattle deer,
and beaver)
Giardiasis
Epidemiology
• Major risk for hikers:
Drinking untreated mountain stream water
• Person-to-person spread:
Frequent in areas of low hygienic
• Person-to-person spread occurs in: – Childcare centers – Families of children with diarrhea
Symptom
Giardiasis
Clinical Manifestations Percent
Diarrhea Malaise. Weakness Abdominal distension Flatulance Abdominal cramps Nausea Foul-smelling, greasy stools Anorexia Weight loss Vomiting Fever Constipation 64-100 72-97 42-97 35-97 44-81 14-79 15-79 41-73 53-73 14-35 0-28 0-17
Giardiasis
Clinical Manifestations
• Symptoms vary with age • Profuse watery stools
greasy, foul smelling, buoyant
• Blood, mucus & fecal leukocyte are absent • Varying degrees of malabsorption can occur • Abnormal stool patterns can alternate with constipation
and normal bowel movements
• Infrequent associations: reactive arthritis, urticaria
Giardiasis
Clinical Manifestations
• Asymptomatic carriers in USA:
3%-7% (up to 20% in southern regions)
• Prevalence studies in DCC children <36 months: 21% • Asymptomatic infection is well tolerated • Testing of case contacts/treatment of asymptomatically
infected individuals is NOT indicated routinely
• Humoral immunodeficienies (hypo-, agammaglobulinemia)
predispose to chronic symptomatic giardiasis
Giardiasis
Diagnosis
Definitive Diagnosis: Detection of trophzoites, cysts or antigens in stool or duodenal fluid
• Stool specimens:
Examined within 1 hour after being passed or should be stored in vials containing polyvinyl alcohol (PVA) or 10% formalin
– Trophozoites are more likely to be found in unformed stools
(rapid transit time)
– Cysts, but not trophozoites, are stable outside the GI tract
• Duodenal Specimens:
Aspirate/Biopsy
Trophozoites can be seen on direct wet mount
Giardiasis
Diagnosis Microscopy: Diagnostic: 70% of patients with single exam 85% with a second exam Antigen Detection: (Polyclonal antisera or monoclonal antibodies) EIA: 87%-100% sensitivity / 100% specificity DFA: 100% sensitivity/specificity Giardiasis is NOT associated with eosinophilia
Giardiasis
Treatment
Oral Antimicrobial Therapy for Giardiasis Agent Pediatric Dose Adult Dose Metronidazole 15 mg/k/d divided in 3 doses X 5d 250 mg tid X 5d (Flagyl) Furazolidone 6 mg/k/d divided in 3-4 doses X 10d 100 mg tid X 10d (Furoxone) Albendazole 400 mg/day X 5d 400 mg/day X 5d (Albenza) Quinacrine 6 mg/k/d divided in 3 doses X 5d 100 mg tid X 5d (Atabrine) Nitazoxanide 12-47 mo: 100 mg bid X 3d N/A (Alinia) 4-11 yrs: 200 mg bid X 3d (100 mg/5 ml)
Giardiasis
Prevention
• Strict hand washing after contact with feces • Purification of public water supplies • Chlorination • Sedimentation • Filtration • Avoid swallowing: recreational water, water from
shallow wells, lakes, rivers, streams, ponds & springs
• Travelers to endemic areas: avoid drinking untreated
water & uncooked foods that have been grown, washed
• Purification of drinking water: Heating (55
o C X 5 min)
Cryptosporidium parvum
• Human disease caused by Cryptosporidiun was first
described in 1976
• The AIDS epidemic fueled interest in cryptosporidiosis • Improved detection of oocysts in feces
immunocompromised hosts
infection is common cause of diarrhea in immunocompetent &
• 2- to 6-um coccidian parasite that infects the
epithelial cells lining the digestive and respiratory tract of vertebrates (fish, reptiles, and mamals, & humans)
Life cycle of Cryptosporidium parvum
• • • •
Sporulated oocysts, containing 4 sporozoites, are excreted by the infected host through feces (1). Transmission of Cryptosporidium parvum occurs mainly through contact with contaminated water (e.g., drinking or recreational water) (2). Occasionally food sources, such as chicken salad, may serve as vehicles for transmission. Many outbreaks in the United States have occurred in waterparks, community swimming pools, and day care centers. Zoonotic and anthroponotic transmission of C. parvum occur through exposure to infected animals or exposure to water contaminated by feces of infected animals . Following ingestion (and possibly inhalation) by a suitable host (3), excystation occurs (a). The sporozoites are released and parasitize epithelial cells (b,c) of the gastrointestinal tract or other tissues such as the respiratory tract. In these cells, the parasites undergo asexual multiplication (schizogony or merogony) (d, e, f) and then sexual multiplication (gametogony) producing microgamonts (male) (g) and macrogamonts (female) (h). Upon fertilization of the macrogamonts by the microgametes (i), oocysts (j, k) develop that sporulate in the infected host. Two different types of oocysts are produced, the thick-walled, which is commonly excreted from the host (j), and the thin-walled oocyst (k), which is primarily involved in autoinfection.
Oocysts are infective upon excretion, thus permitting direct& immediate fecal-oral transmission.
Cryptosporidium parvum
Cryptosporidium parvum
Epidemiology
Crptosporidiosis is associated with diarrheal illness worldwide Transmission to humans:
– Close association with infected animals (calves,
rodents, puppies, kittens)
– Person-to-person (DCC, Traveler’s diarrhea) – Environmentally contaminated water
~130 oocysts can cause infection in immunocompetent
Cryptosporidium parvum
Epidemiology
• Outbreaks have been associated with contaminated
community water supplies
• Waterborne outbreak in Milwaukee, WI (1985):
403,000 cases of diarrhea 4400 were hospitalized Total cost: $96.2 million
• Swimming pool water & water from decorative fountains
have been linked with outbreaks of crptosporodiosis
Cryptosporidiosis Epidemiology
• More prevalent in underdeveloped countries & in
children <2 years of age
• Most cases are not recognized • Infection rates surveys in selected populations:
– Developed countries: 0.6%-20% – Underdeveloped countries: up to 32%
• Difference is due to:
– Poor sanitation, lack of clean water, crowded living
conditions, close association with animals
Cryptosporidiosis Clinical Manifestations
• Incubation period: 2-14 days • Diarrhea: Profuse watery diarrhea + mucus
Rarely contains WBC’s or RBC’s
• Crampy abdominal pain, nausea, vomiting (50%) • Fever is uncommon • Infection may be asymptomtic, self-limited or
protracted
Cryptosporidiosis Clinical Manifestations
• Severity is linked with immunosuppression • Most immunocompetent hosts: self-limited illness (10-14 days) • Immunocompromised (HIV, malignancy): prolonged debilitating
disease
• Oocysts shedding: up to 2 weeks after clinical improvement • Biliary tract disease may occur in immunocompromised hosts (15%): – Fever – RUQ pain – N,V,D – Jaundice & elevated LFT’s can occur
Cryptosporidiosis Laboratory Diagnosis
• Identification of oocysts in – (1) stools or – (2) along epithelial surface of biopsy tissue • Highest concentration in jejunum • Histology: villous atrophy, blunting, epithelial flattening • Stool specimens for oocysts identification: – Put in fixative (to prevent infection in lab workers) – 3 specimens in immunocompetent – 2 specimens in immunocompromised – Auramine & rhodamine stain – most sensitive/expensive – Acid fast stain – commonly used – Not detected by routine O & P
Cryptosporidiosis
Cryptosporidia are usually identified in stool specimens by a modified acid-fast stain.
The left panel shows numerous red staining oocysts.
In more difficult cases, a biopsy of small bowel or colon leads to the diagnosis.
In the right panel, numerous basophilic cryptosporidia stud the surface of the enterocytes. Note the lack of inflammation.
Cryptosporidiosis
–
Small spherical organisms (red arrow) attached to the brush border of absorptive intestinal epithelial cells
Oocysts of Cryptosporidium visualized with Acid-fast stain
Oocysts of Cryptosporidium parvum
Cryptosporidiosis Treatment
• In most immunocompetent:
Self-limited; no therapy except adequate hydration
• In severe cases/immunocompromised hosts:
A variety of agents have been used without consistent results
• Until recently the mainstay of treatment was
supportive care
• Newly effective/FDA-approved agent:
Nitazoxanide (Alinia): 12-47 mo: 100 mg bid X 3d 4-11 yrs: 200 mg bid X 3d (Concentration: 100 mg/5 ml)
Cryptosporidiosis Prevention
• Hand washing: prevent person-to-person transmission • Enteric precautions for hospitalized patients • Cohort infected patients in hospital • Immunocompromised hosts should take special
precautions around animals
• Avoid swallowing recreational water • Avoid drinking water from shallow wells, lakes, rivers,
streams, ponds and springs
Amebiasis
Entamoeba histolytica
• Pseudopod-forming, non-flagellated protzoa • Most invasive parasite of the Entamoeba group • Only member that causes:
Amebic colitis & liver abscess
• Life Cycle consists of:
(1) Infectious cyst (2) Invasive trophzoite Trophozoites adhere to colonic mucin and epithelial cells
kill host epithelial & immune cells
tissue destruction
Amebiasis
Entamoeba histolytica trophozoite Entamoeba histolytica
mature cyst
Amebiasis
Cysts are passed in feces(1). Infection by Entamoeba histolytica occurs by ingestion of mature cysts in fecally contaminated food, water, or hands (2).
Excystation occurs in the small intestine(3)
trophozoites released
(4). Trophozoites multiply by binary fission and produce cysts (5)
migrate to the large intestine passed in the feces.
Cysts (protected by their cell walls) can survive days to weeks in the external environment and are responsible for transmission.
In many cases, trophozoites remain confined to the intestinal lumen (noninvasive infection) of individuals who are asymptomatic carriers, passing cysts in their stool.
In some patients trophozoites invade the intestinal mucosa (intestinal disease), or, through the bloodstream, extraintestinal sites such as the liver, brain, and lungs (extraintestinal disease), with resultant pathologic manifestations.
Invasive and noninvasive forms represent two separate species (E. histolytica & E. dispar respectively), however not all persons infected with E. histolytica will have invasive disease. These two species are morphologically indistinguishable.
Transmission can also occur through fecal exposure during sexual contact (cysts, & also trophozoites could prove infective).
Trophozoites of Entamoeba histolytica (Trichrome stain).
Two diagnostic characteristics: Two of the trophozoites have ingested erythrocytes, and the nuclei have typically a small, centrally located karyosome, as well as thin, uniform peripheral chromatin.
Entamoeba histolytica
Epidemiology
• Disease more severe in:
The very young Elderly Pregnant women
• Worldwide: 40-50 million symptomatic infections/year
100,000 deaths annually
• In Dhaka, Bangladesh, 50% of children have serologic evidence of
E. histolytica infection by 5 years
• Groups at increased risk of amebiasis in developed nations: – Immigrants from endemic areas – Long-term visitors to endemic areas – Institutionalized individuals
Entamoeba histolytica
Clinical Manifestations
Amebic colitis Sign or Symptom Symptoms > 1 wk Most patients Diarrhea % of Patients Affected 94-100 Dysentery Abdominal pain Weight loss Fever >38 o C Heme (+) stool 94-100 12-80 44 10 100 Immigrant from or traveler to endemic area >50 Prevalence (male/female) 50/50
Entamoeba histolytica
Clinical Manifestations
Amebic colitis Patients with chronic, non-dysenteric intestinal amebiasis may complain for months to years of abdominal pain, flatulence, intermittent diarrhea, mucus in the stools, and weight loss Chronic non-dysenteric intestinal amebiasis has been mistakinly diagnosed as ulcerative colitis
Amebic Colitis: Severe dysentery with multiple ulcers in the large bowel, and a bloody diarrhea
Entamoeba histolytica trophozoites in section of intestine (H&E)
Entamoeba histolytica
Clinical Manifestations
Acute Fulminant or Necrotizing Colitis
• Unusual (about 0.5% of cases) • A complication that occurs more frequently in patients
inappropriately treated with corticosteroid
• Abdominal pain, distension, and rebound tenderness are
present in most patients
• Indications for surgery: – Failure of response to anti-amebic drugs after intestinal
perforation/abscess formation
– Persistence of abdominal distention after institution of anti-
amebic Rx
– Toxic megacolon
Histopathology of a typical flask-shaped ulcer of intestinal amebiasis
Entamoeba histolytica
Clinical Manifestations
ascending colon amebiasis
Ameboma
• Segmented mass of granulation tissue in the cecum or • Occurs in 0.5% to 1.5% of patients with intestinal • Tender palpable abdominal mass • Concuurent amebic dysentery present in 2/3 of patients • “Apple-core” lesions on barium enema study • Lesions resolve with anti-amebic chemotherapy • Intestinal constriction occurs in the colon in <1% of
patients
Entamoeba histolytica
Clinical Manifestations
Amebic Liver Abscess
• Develops in about 10% of patients with invasive E.
histolytica infections
• Few patients have concurrent dysentery – most report
dysentery within the preceding year
• Occurs in any age group • Patients with a more chronic illness (2-12 weeks of
symptoms) commonly present with hepatomegaly and weight loss
Entamoeba histolytica
Clinical Manifestations
Amebic Liver Abscess Sign or Symptom Fever % of Patients Affected Symptoms > 4 wks 21-51 85-90 Abdominal tenderness 84-90 Hepatomegaly Jaundice 6-10 Diarrhea Immigrant from or traveler 30-50 20-33 Weight loss 33-50 Cough 10-30 to endemic area >50 Prevalence (male/female) 50/50 in children; 90/10 in adults
Gross pathology of liver containing amebic abscess
Gross pathology of amebic abscess of liver. Tube of "chocolate" pus from abscess
.
Entamoeba histolytica
Laboratory Findings and Diagnosis
• Differential Diagnosis of Amebic Dysentery
:
– IBD – Ischemic colitis – Other infectious causes of bloody diarrhea • Diagnostic Tests: – EIA is best for specific diagnosis of amebiasis
(Sensitivity & specificity of assay on stool >95%)
– Colonoscopy remains important to evaluate for other causes – Serology for antibodies: IHA – Positive in: 88% amebic dysentery, 70-80% liver abscess,
50% of general population
Entamoeba histolytica
Laboratory Findings and Diagnosis
• Differential Diagnosis of Amebic Liver Abscess
:
– Pyogenic abscess – Echinococcal cyst – Hepatoma • Diagnostic Tests: – Ultrasonography – CT – MRI
None differentiate amebic from pyogenic abscess Diagnosis is frequently a diagnosis of exclusion IHA: Acutely, E. Histolytica antibody can be detected in serum in 70-80% of cases EIA: Can detect E. histolytica antigen in serum in ~96% of patients with abscess
Amebic liver abscesses
Amebic liver abscesses
Entamoeba histolytica Treatment
Asymptometic amebiais: Luminal agent (paromomycin, diloxanide furate, or iodohydroxyquin) Amebic Colitis: Metronidazole & a luminal agent Amebic Liver Absces: Metronidazole & a luminal agent
Entamoeba histolytica
Prevention
Prevention of E. hisolytca transmission requires disruption of the fecal-oral spraed of amebic cysts Individuals should be advised regarding:
• Risk of traveling to endemic areas • Safeguards to prevent ingesting colonic organisms
Because humans and primates are the only known reservoirs of E. histolytica, a successful vaccine Could potentially eliminate this disease
Intestinal Nematodes Round Worms
• The most common parasitic infections in humans;
affect one quarter of the world population
• Remain a major cause of physical growth delay,
cognitive delay, and malnutrition throughout the world
• In certain endemic populations, children are
disproportionately affected
• Being increasingly encountered in the developed world.
In the USA, groups at increased risk include: international travelers, recent immigrants, refugees, and international adoptees
Ascaris lumbricoides
• The most common helminthic infection in humans • 1.2 billion infected worldwide • 51 million children are currently estimated to be
infected
• Commonly affects children living in economically
disadvantaged communities
• Ascariasis still occurs frequently in the USA as an
imported infection in recent immigrants from Latin America and Asia & internationally adopted children
• Young children seem to be affected more severely
than adults (larger worm burden, parasite-induced malnutrition)
Ascaris lumbricoides
Adult worms live in the lumen of the small intestine (1). A female may produce approximately 200,000 eggs per day, which are passed with the feces (2) . Unfertilized eggs may be ingested but are not infective. Fertile eggs embryonate and become infective after 18 days to several weeks(3) , depending on the environmental conditions (optimum: moist, warm, shaded soil).
After infective eggs are swallowed (4) , the larvae hatch (5), invade the intestinal mucosa, and are carried via the portal, then systemic circulation to the lungs (6) .
The larvae mature further in the lungs (10 to 14 days), penetrate the alveolar walls, ascend the bronchial tree to the throat (7), and are swallowed . Upon reaching the small intestine, they develop into adult worms (1) . Between 2 and 3 months are required from ingestion of the infective eggs to oviposition by the adult female. Adult worms can live 1 to 2 years.CDC
Ascaris lumbricoides
Clinical Manifestations
• Larvae migration through the lung parenchyma
mechanical and immune-mediated damage:
– Pulmonary microhemorrhages – Inflammation & exudation of fluid – Pulmonary infiltrates – Cough, dyspnea, wheeezing, mild hemoptysis (Loffler
pneumonia)
• Adult ascaris worms in the small bowel – Epigastric pain – Diffuse abdominal discomfort • Heavy infestation
intestinal obstruction
• Chronic infection
malnutrition due partly to malabsorption (proteins, fat & vitamin A)
Ascaris lumbricoides
Ascaris lumbricoides Laboratory Findings/Diagnosis
• Diagnosis is established by stool examination for
characteristic ova. Each adult female produces so many eggs that a single stool specimen is adequate
• Migration of larvae through the lungs is assocaited
with peripheral eosinophilia and pulmonary infiltrates on chest radiograph
• In endemic areas, any child presenting with signs
suggestive of intestinal obstruction should be evaluated for Ascariasis
Characteristic fertilized egg : Bile stained, mammillated thick external layer, unembryonated (55-75 um x 35-50 um)
Ascaris lumbricoides
Characteristic unfertilized egg : elongated & larger than fertile egg, thin shelled (85-95 um x 43-47 um)
Ascaris lumbricoides Treatment
• Mebendazole (100 mg twice daily X 3 days) or • Albendazole (400 mg as a single dose)
(The above are not generally given to children < 1 yr)
• Pyrantel pamoate (11 mg/kg up to 1 gm/day, X 3 days) • In cases of partial bowel obstruction caused by
Ascaris: alternative therapy with piperazine citrate, which paralyzes the worms may abrogate the need of surgical intervention
Ascaris lumbricoides Prevention
• Elimination of contact with soil contaminated by egg-
containing feces. In tropical areas, poor sanitation is responsible for infection rates approaching 100%
• Diagnosis, effective treatment, improved sanitation
practices
• In endemic areas (infection rate is >50%),
antihelmenthic agents administration to school-age children has been recommended as part of a targeted deworming program
• Sustained economic growth is most effective means of
long-term parasite control
Hookworms
• Approximately 1 billion people harbor
hookworms in their gastrointestinal tract
• A leading cause of iron deficiency anemia in the
developing world
• Children are particularly vulnerable to the
morbid effects of hookworms infections (often because dietary intake fails to compensate for intestinal losses of iron and serum proteins)
The two most common hookworms that infect humans:
(1) Ancylostoma duodenale
(2) Necator americanus
Adult females:10-13 mm (A. duodenale), 9-11 mm (N. americanus) Adult males: 8-11 mm (A. duodenale), 7-9 mm (N. americanus).
A smaller group of hookworms infecting animals can invade and parasitize humans (A. ceylanicum) or can penetrate the human skin (causing cutaneous larva migrans), but do not develop any further (A. braziliense,
Uncinaria stenocephala).
Life Cycle: A. duodenale & N. americanus Eggs are passed in the stool (1), and under favorable conditions (moisture, warmth, shade), larvae hatch in 1 to 2 days.
The released rhabditiform larvae grow in 5 to 10 days (and two molts) they larvae that are infective (3).
These infective larvae can survive 3-4 host, the larvae penetrate the skin and heart and then to the lungs. They ascend the bronchial tree to the The larvae reach the small intestine, where they reside and mature into adults. loss by the host (5). Most adult worms longevity records can reach years.
several
Geographic distribution of Ancylostoma duodenale
Geographic distribution of Necator americanus
Hookworms
• In the bowel, adults attach by their mouth to the
intestinal mucosa and begin to feed
• Equipped with teeth, cutting plates or both, powerful
esophageal muscles, and hydrolytic enzymes, the hookworm digests the plug of tissue within its buccal capsule
• Potent anticoagulants and inhibitors of platelet function
are released and cause profound bleeding from lacerated capillaries in the lamina propria
• Adult worms mate in the small intestine, and the
females deposit fertilized eggs in the lumen
Hookworms
• The heads of these worms look like some
monster out of a horror movie
• The mouth parts of these nematodes are
designed to bite onto the lining of the intestine, abrade the surface and suck the patients blood
• Horrific as this sounds many people who
are infected show no outward symptoms of disease
• The presence and severity of the disease
depends on the number of worms per individual, the nutritional state of the patient and the species of hookworm (A. duodenale suck greater volumes of blood than N. americanus and so it requires fewer worms to produce disease).
Necator americanus Ancylostoma duodenale
Anterior: Note the ventral teeth in the buccal capsule of A.duodenale.
N. americanus
has ventral cutting plates.
Male Posterior: The copulatory bursa is used by the males for grasping the female during mating.Females lack a copulatory bursa.
Hookworms Clinical Manifestations
• Skin penetration by third stage larvae
pruritic dermatitis called ground itch (localized to site of hookworm entry)
an intensely
• Adult hookworms in intestine: – Nonspecific GI tract symptoms – Blood loss secondary is proportional to worm burden and
develops 10-20 weeks after infection
– A. duodenale infection is usually associated with greater loss
than occurs with N. amricanus
– Hookworm anemia results when blood loss exceeds the host’s
iron reserve and dietary intake
– Occasionally, severe hookworm anemia leads to heart failure
Hookworms Laboratory Findings and Ddiagnosiss
• Characteristic rash of ground itch occurs on any skin surface and
can be erythematous, papular, or vesicular
• Intense prtutitis can lead to scratching, excoriation, and
secondary bacterial infection
• In contrast to Ascaris, pulmonary symptoms are usually not severe • Intestinal hookworm infection is detected by identifying the
characteistic egg in feces
• The eggs of Ancylostoma & Necator amerianus are similar under
light microscope & cannot be easily distinguished by morphology
Ancylostoma duodenale &
Necator americanus
Although the adult form of these intestinal nematodes can be distinguished, the diagnostic form in humans, the ova, are essentially identical. The ova are oval and measure about 60 X 40 µm. There is typically a clear space between the embryo and the thin shell.
This is unstained wet-prep.
Hookworms Treatment
• Mebendazole (100 mg twice daily X 3 days) or • Albendazole (400 mg as a single dose) • Mebendazole is poorly absorbed and may not eradicate
developmentally arrested Ancylostoma larvae residing in extraintestinal issues. Therefore periodic follow up stool examination may be necesessary
• Alternate Treatment:
Pyrantel pamoate (11 mg/kg up to 1 gm/day, X 3 days)
• Re-infection in endemic areas occur so commonly that the effect
of single course of treatment is of questionable benefit
• Iron supplementaion reverses mild to modertae hookworm anemis
Hookworms Prevention
• No evidence of naturally acquired resistance • Children in endemic areas are constantly exposed to infective
third-stage larvae
• Interest in development of a vaccines aimed at preventing
hookworm infection/disease in children in the developing world
• Most promising vaccine candidates: family of proteins called
ASP’s (Ancylostoma–secreted proteins) which are secreted by the infective larval stage
• Immunization with recombinant hookworm ASP has been shown to
prevent tissue migration in a murine model of ancylostomiasis
Tapeworms Taenia saginata and Taenia solium
Segmented worms, called tape worms, cause human illness in either of two stages in their life cycle: (1) Adult stage: Cause gastrointestinal symptomatology (2) Larval stage: Causes signs and symptoms referable to enlarging larval cysts in a variety of tissues Humans are the only definitive hosts for T. saginata (the beef tapeworm) and T. solium (the pork tapeworm
)
Life cycle of Taenia saginata and Taenia solium Humans are the only definitive hosts for Taenia saginata and Taenia solium. Eggs or gravid proglottids are passed with feces (1); eggs can survive for days to months in the environment Cattle (T. saginata) and pigs (T. solium) become infected by ingesting vegetation contaminated with eggs or gravid proglottids (2). In the animal's intestine, the oncospheres hatch(3), invade the intestinal wall, and migrate to the striated muscles, where they develop into cysticerci. A cysticercus can survive for several years in the animal Humans become infected by ingesting raw or undercooked infected meat (4). In the human intestine, the cysticercus develops over 2 months into an adult tapeworm, which can survive for years.
The adult tapeworms attach to the small intestine by their scolex(5) and reside in the small intestine (6). Length of adult worms is usually <5 m for T. saginata (may reach up to 25 m) and 2 - 7 m for T. solium. The adults produce proglottids which mature, become gravid, detach from the tapeworm, and migrate to the anus or are passed in the stool (~6 per day T. saginata adults usually have 1,000 to 2,000 proglottids, while T. solium adults have an average of 1,000 proglottids. The eggs contained in the gravid proglottids are released after the proglottids are passed with the feces. T. saginata may produce up to 100,000 and T. solium may produce 50,000 eggs per proglottid respectively. CDC
Taenia saginata - The Beef Tapeworm
Taenia solium - The Pork Tapeworm
Taenia saginata
&
Taenia solium
Epidemiology
T. saginata:
Widespread in cattle breeding areas of the world. Prevalence >10% in some independent states of the former Soviet Union, in Near East, and in central and eastern Africa.
Lower rates in Europe, Southeast Asia, & South America
T. solium:
Prevalent in Mexico, Central and South America, Africa, Southeast Asia,and the Philippines Infections in USA and Canada are found in immigrants from areas where taeniasis is endemic, and in travelers who consume undercooked meats in endemic areas
Taenia saginata
&
Taenia solium
Clinical Manifestations
Cysticercosis occurs in humans after the ingestion of T. solium eggs Embryonic metacestode migrates from the intestine and can lodge in a number of tissue sites such as the brain, muscle, and eyes with proclivity for the brain The clinical course largely depends on the endurance of the parasite inside the tissue and on the ensuing inflammation In the brain parenchyma, the intruding cysticercus might be destroyed within a few days by host immune mechanisms or remain viable in the brain for > 10 years
Taenia saginata
&
Taenia solium
Clinical Manifestations
Cysticercosis can affect humans at any age Most common during the 3 rd and 4 th decades of life About 10% occur in children In infants initial signs of cysticecosis in infants is generalized seizure CT with contast or T 2 -weighted MRI
isolated cystic lesion in the brain parenchyma Typically the lesion disappears spontaneously 2-3 months later, but in some
granuloma
cacification (permanent sequela) Isolated lesion is most common; some children have two-several cysts Cystcercotic encephalitis is a severe form of CNS cystcercosis that occasionally occurs in children, particularly adolescent girls
Taenia saginata
&
Taenia solium
Clinical Manifestations
In adults neurocysticercosis is quite different: Multiple brain cysticerci, variable immune response, chronic inflammation, chronic persistence of many active cysts, vasculitis and protean clinical picture Epilepsy occurs in 50% of cases; intracranial hypertension in 30% Occular Cysticercosis: Subretinal area or vitreous chamber Muscular cystcercosis: Rare in both children and adults; usually benign course
• • •
Taenia saginata
&
Taenia solium
Laboratory Findings/Diagnosis
CT and MRI are the most relaible tools for the diagnosis of neurcysticercosis Serologic tests are unreliable (cross reactivity with antigens of other parasites) Serology is highly specific for CNS inection when tests are performed on CSF
• • • •
Taenia saginata
&
Taenia solium Treatment
Intestinal T. solium infection: Praziquantel - (5-10 mg/kg once) Neurocysticercosis: Albendazole - 15 mg/kg/day (maximum, 800 mg/day) divided into two doses X 8 days Two months later, if repeat imaging studies show cysts: Praziquantel in a total dose of 75mg/kg divided in three doses for 15 days. Repeat imaging studies in two months