Antiparasites

Question 1

Antamebics

Answer 1

• Luminal: Act on parasite in bowel lumen
• Systemic: Active both in intestinal wall and liver
• Mixed: Active against both luminal & systemic disease
  
  • metro & tinidazole

Question 2

Metronidazole

Answer 2

• Amebicide of choice for treating invasive amebiasis
• Patients should receive a luminal amebicide in addition after treatment with metronidazole

Other Clinical Applications

• Giardia lamblia
• Trichomonas vaginalis
• Anaerobic cocci
• Anaerobic Gram-negative bacilli
• Combination regimens for H.pylori eradication

MOA

• Once absorbed, metronidazole is non-enzymatically reduced by reacting with reduced ferredoxin
• This reduction causes the production of cytotoxic compounds
• The cytotoxic compounds bind to proteins & DNA, resulting in unstable molecules and cell death

PK

• Oral
• Well distributed (inc. vaginal & seminal fluids, saliva, breast milk & CSF)
• Undergoes hepatic oxidation & glucuronidation (CYP P450’s)

Question 3

Metro - Adverse

Answer 3

• GI distress
• Disulfiram-like reaction (avoid alcohol intake) • Unpleasant metallic taste
• Oral moniliasis
• Dark coloration of urine
• Leukopenia, dizziness, ataxia.
• Safety in pregnancy NOT established

Question 4

Tinidazole

Answer 4

• 2nd generation nitroimidazole
• Similar to metronidazole but better tolerated and has shorter treatment course

Clinical Applications

• Amebiasis
• Amebic liver abscess
• Giardiasis
• Trichomoniasis

Question 5

Tinidazole - Adverse

Answer 5

Same as metronidazole but reports indicate shorter duration of effects with tinidazole

Question 6

Luminal antiamebics

Answer 6

• Diloxanide furoate
• Iodoquinol
• Paromomycin

Question 7

Diloaxanide furoate

Answer 7

• Used as sole agent for treatment of asymptomatic amebiasis
• Converted in gut to diloxanide freebase active form
• Adverse Effects: Mild (GI distress)
• Not currently available in US – however remains luminal amebicide of choice

Question 8

Iodoquinol

Answer 8

• Orally active against luminal trophozoite and cyst forms of E.histolytica
• Used as an alternative to diloxanide furoate for mild- severe infections

Question 9

Iodoquinol - Adverse

Answer 9

• Rash, diarrhea, dose-related peripheral neuropathy
• Long term use should be avoided (due to risk of optic neuritis)

Question 10

Paromomycin including Adverse

Answer 10

• Aminoglycoside antibiotic
• Effective only against luminal forms of E.histolytica and tapeworm
• Sometimes used with tetracyclines for mild intestinal disease
• Alternative agent for cryptosporidiosis in AIDS patient
• Amebicidal (causes cell membranes to leak)
• Interferes with bacterial protein synthesis (binds to 30S ribosomal subunits)
• Reduces intestinal flora population

Adverse Effects

• GI distress & diarrhea
• Systemic absorption may lead to headaches, dizziness, rashes and arthralgia

Question 11

Systemic antiamebics

Answer 11

• Chloroquine
• Emetine
• Dehydroemetine
• Useful for treating liver abscesses or intestinal wall infections

Question 12

Chloroquine

Answer 12

• Used in combination with metronidazole & diloxanide furoate
• **Indication: **severe intestinal infection w E. Histolytica
• MOA: Eliminates trophozoites in liver abscesses

Question 13

Emetine and Dihydroemetine

Answer 13

• Backup drugs for treatment of severe intestinal or hepatic amebiasis
• Used in combination with a luminal agent
• MOA: Inhibit protein synthesis by blocking ribosomal movement along messenger RNA

PK

• IM or SC
• Concentrate in liver (persists for 1 month)
• Slowly metabolized & eliminated

Question 14

Emetine and Dihydroemetine - Adverse

Answer 14

• Pain at site of injection
• Transient nausea
• Cardiotoxicity
• Neuromuscular weakness
• Dizziness
• Rash

Question 15

Amebiasis Rx

Answer 15

• Asymptomatic, intestinal infection: Diloxanide furoate
• Mild-moderate intestinal infection: Metronidazole + diloxanide furoate
• Severe intestinal infection: metro or tinidazole + diloxanide furoate
• Hepatic abscess & other extraintestinal disease: Metronidazole or tinidazole + diloxanide furoate

Question 16

Antihelminthics durgs

Answer 16

• Nematode
• Trematode
• Cestode
• In most cases broad spectrum agents cure or control most human worm infections
• Some systemic infections only respond partially to antihelminthic drugs (cysticercosis, echinococcosis, filariasis, trichinosis)
• Antihelminthic drugs can act either:
• locally (to expel worms from GI tract) or,
• systemically (to eradicate adult helminths or developmental forms)

Question 17

Benzimidazoles

Answer 17

• Albendazole
• Mebendazole
• Thiabendazole

Question 18

Albendazole

Answer 18

Used in the treatment of cestodal infestations, such as cysticercosis (Taenia solium larvae) and hydatid disease (Echinococcus granulosis)

MOA

• Inhibits microtubule synthesis & glucose uptake
• ATP production is decreased resulting in worm immobilization and death

PK

• Oral (erratically absorbed, enhanced by high-fat meal)
• Extensive first-pass metabolism, including rapid sulfoxidation to active metabolite

Question 19

Albendazole - Adverse

Answer 19

• Short course therapy (1-3 days) = mild & transient (headache, nausea)
• Hydatid treatment (3 months) = risk of hepatotoxicity, agranulocytosis or pancytopenia
• Treatment is associated with inflammatory responses to dying parasites in CNS (headache, vomiting, hyperthermia, convulsions, mental changes)
• Contraindicated in pregnancy & children < 2y (FDA Category C)

Question 20

Mebendazole

Answer 20

Drug of choice in the treatment of infections by (will treat most infections):

• Whipworm (Trichuris trichiura)
• Pin worm (Enterobius vermicularis)
• Hookworms (Necator americanus & Ancylostoma duodenale)
• Roundworm (Ascariasis lumbricoides)

MOA

• Inhibits formation of helminth microtubules
• Irreversibly blocks glucose uptake
• Affected parasites are expelled with feces

Pharmacokinetics

• Oral (chewable) – nearly insoluble in aqueous solution, take with high-fat meal
• Undergoes first-pass metabolism to inactive compounds

Question 21

Mebendazole - Adverse

Answer 21

• Abdominal pain, diarrhea, headache, dizziness
• Contraindicated in pregnancy (FDA Category C)
• Use with caution in children < 2
• Use with caution in patients with cirrhosis

Question 22

Thiabendazole

Answer 22

Effective in treatment of strongyloidiasis caused by Strongyloides stercoralis (threadworm), cutaneous larva migrans, and early stages of trichinosis

MOA: Affects microtubular aggregation

Pharmacokinetics

• Oral
• Nearly insoluble in H20

Question 23

Thiabendazole - Adverse

Answer 23

• More toxic than other benzimidazoles
• Dizziness, anorexia, nausea, vomiting
• CNS disturbances (dizziness -> seizures)
• Cases of erythema multiforme & Stevens-Johnson reported
• Contraindicated in pregnancy (FDA Category C)
• Should not be used in presence of liver or kidney disease

Question 24

Ivermectin

Answer 24

Drug of choice for the treatment of onchocerciasis (Onchocerca volvulus), cutaneous larva migrans & strongyloides

MOA

• GABA agonist
• Cl- influx increases leading to hyperpolarization of nerve /muscle cell. Death occurs due to paralysis of parasite

Pharmacokinetics: Oral (does not cross BBB)

Question 25

Ivermectin - Adverse

Answer 25

• Mazotti-like reactions with onchoceriasis (fever, dizziness, somnolence, hypotension)
• Contraindicated in pregnancy (FDA Category C)
• Contraindicated in meningitis (may cross BBB)
• Best to avoid concomitant use of ivermectin & other drugs that enhance GABAergic activity (eg, barbiturates, benzodiazepines)

Question 26

Piperazine

Answer 26

Alternative drug for treatment of pinworm & roundworm infections

MOA

• GABA agonist
• Expulsion of worm occurs by peristalsis

Contraindications: Patients with seizure disorders

Question 27

Pyrantel Pamoate including Adverse

Answer 27

Effective in treatment of infections by roundworms, pinworms and hookworms

MOA: Acts as a depolarizing, neuromuscular-blocker (causes persistent activation of parasite’s nicotinic receptors by release of acetylcholine & inhibition of cholinesterase)

PK: Poorly absorbed orally (exerts effects in intestinal tract)

**Adverse: **Mild (nausea, vomiting, diarrhea)

Question 28

Diethylcarbamazine

Answer 28

DOC for treatment of lymphatic filariasis, loiasis & tropical eosinophilia.

MOA: Immobilizes microfilariae & renders them susceptible to host defense mechanisms

**PK: **Oral (rapidly absorbed with meals)

Question 29

Diethylcarbamazine - Adverse

Answer 29

• Most AE thought to be due to host responses following damage/death of parasite
• Fever, malaise, rash, myalgias, arthralgias, headache
• Leukocytosis (common)
• Antihistamines or steroids can be coadministered

Question 30

Doxycycline - MOA

Answer 30

• Tetracycline antibiotic.
• Macrofilaricidal activity against Wuchereria bancrofti.
• Also active against onchocerciasis
• MOA: Acts indirectly by killing Wolbachia (intracellular bacterial symbiont of filarial parasites)

Question 31

Praziquantal

Answer 31

DOC for all forms of schistosomiasis & most trematode & cestode infections

Cysticercosis – albendazole is drug of choice (praziquantel has similar efficacy)

MOA: Increases permeability of cell membrane to calcium, causing contracture & paralysis of worm musculature, resulting in detachment of suckers from blood vessel walls.

**PK: **

• Oral
• Extensive first-pass metabolism (CYPs)
• Inactive metabolites excreted via urine & bile

Question 32

Praziquantal - Adverse

Answer 32

• Drowsiness, dizziness, malaise, anorexia & GI upsets
• Drug interactions (CYP P450)
• Contraindicated in pregnancy & nursing mothers (FDA Category B)
• Contraindicated for treatment of ocular cysticercosis (destruction of organism may damage eye)

Question 33

Bithionol

Answer 33

• Drug of choice for fasciolosis (sheep liver fluke)
• Alternative drug for pulmonary paragonimiasis
• MOA: Inhibition of helminth’s electron transport chain (probably)

Question 34

Niclosamide

Answer 34

• 2nd line drug for treatment of most cestode infections
• Use is uncommon due to excellent efficacy of praziquantel
• No longer available in US

MOA

• Inhibition of the parasite’s mitochondrial phosphorylation of ADP. Anaerobic metabolism may also be inhibited
• Drug is lethal for cestode’s scolex & segments of cestodes but not for the ova

PK

• Laxative is admin. prior to niclosamide (oral) to purge bowel of all dead segments in order to preclude digestions & liberation of ova (may lead to cysticercosis)
• Alcohol should be avoided within 1 day of dose
• Safety has not been established in pregnancy or children <2