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Transcript
Antiprotozoal and Antihilmintic
Drugs
General Pharmacology
M212
Dr. Laila M. Matalqah
Protozoal Infection
 Protozoal diseases are less easily treated than bacterial
infections:
Unicellular protozoal cells have metabolic processes closer to
human cells than bacteria.
Many of antiprotozoal drugs cause serious toxic effects and most of
them are not safe I n pregnancy.
Protozoal diseases, such as:
 Malaria,
 Amebiasis,
Leishmaniasis,
Trypanosomiasis,
Trichomoniasis,
Giardiasis
Antiamebic Drugs
 Mixed amebicides : both systemic and luminal
 Metronidazole
 Tinidazole
 Luminal amebicides
–



treatment of the asymptomatic colonization state.
Iodoquinol,
Paromomycin
diloxanide furoate
 systemic amebicides
– These drugs are useful for treating liver abscesses and intestinal wall
infections caused by amebas
 Chloroquine
 Emetine
 Dehydroemetine

Life cycle of Entameaba histolytica and the sites of action of
amebicidal drugs
Mixed amebicide



Metronidazole
MOA: Releases in the parasites toxic superoxide
or hydroxyl radical forming reduced cytotoxic
compounds that bind to proteins and DNA,
resulting in cell death.
Metronidazole is Drug of choice (DOC) for
amebic infection and for infections caused by:



Giardia lamblia
Trichomonas vaginalis
Anaerobic cocci, gram+ve bacilli and “C.difficile” that
cause Pseudomemberanous colitis
Metronidazole (cont.)

It kills the trophozoites and less effective
against the cyst
Most effective against the invasive amebae
 Less effective against the luminal amebae
SO
• it is usually administered with a luminal amebicide,
such as iodoquinol or paromomycin

Luminal Amebicides
Iodoquinol
*Paromomycin *diloxanide furoate
• They have a direct amebicidal effect to the
trophozoites and cyst forms.
• Used in: asymptomatic cyst carriers and in intestinal
amebiasis.
• Amebae feed on intestinal Flora so tetracycline is
added to luminal amebicides to decrease major food
source.
• Side effects
• iodoquinol include rash, diarrhea, and dose-related
peripheral neuropathy, including a rare optic neuritis.
Systemic Amebicides
• *Chloroquine :useful for treating liver abscesses,
and intestinal wall trophozoites
** Usually used with metronidazole and
diloxanide furoate to treat and prevent liver
abscess – orally for 25 days
*** Other uses: Antimalaial and anti-inflammatory
in arthritis.
Systemic Amebicides
2. Emetine and Dihydroemetine
•
•
•
•
•
•
They inhibit protein synthesis
Direct amebicidal on invasive amebae in tissue.
Given IM.
Its half-life in plasma is 5 days
They should not be taken for more than 5 days
ADRs:
– GIT upset very common (N&V).
– Cardiotoxicity: arrhythmia and CHF
– Neuromuscular weakness ,dizziness and skin rash.
Summary
Malaria
• Malaria is an acute infectious disease caused by four
species of the protozoal genus Plasmodium: P.
malariae, P. falciparum,P. ovale and P. Vivex
• Life cycle: Anopheles mosquito injects -Plasmodium sporozoites into the bloodstream - to
the liver form merozoites invades a red blood cell,
becoming a trophozoite - released merozoites from
RBCs can become gametocytes – to the insect
becoming sporozoites again……and so on
Life cycle of malaria parasite
and the sites of action of antimalarial drugs
Antimalarial Drugs
• No drug against sporozoites is available.(?)
a: They remain in the blood for a very short
time.
b: They have very low metabolic rate , “not
easily destroyed by drugs”
1:Drugs Against Exoerythrocytic Form
• Primaquine (8-aminoquinoline)
•
•
•
•
“Tissue schizonticide”
MOA: oxidative agent???
Also has gametocidal effect prevent transmission.
Primaquine is the only agent that can lead to radical
cures of the P. vivax and P. ovale malarias, which may
remain in the liver in the exoerythrocytic form after the
erythrocytic form of the disease is eliminated
• Well absorbed orally.
• Side effects: May cause hemolytic anemia in G6PD
deficiency ,decrease WBC and hemoglobinemia.
• C/I in pregnancy
2:Drugs Against Erythrocytic Form
• “Blood schizonticides”
•  Clinical cure or suppression of signs and
symptoms
1. Chloroquine:
• MOA: binds to heme, increased pH, result in oxidative damage to
the membranes, leading to lysis of both the parasite and the red
blood cell.
• DOC in the treatment of erythrocytic P. falciparum malaria
• Also has gametocidal effect prevent transmission.




Very well absorbed orally.
4 days of therapy to cure the disease.
Mainly metabolized by the liver.
The rest is eliminated unchanged in urine
Chloroquine(cont.)
• Start with 1.0 gm, after 6h give ½ gm then
½ gm for 2 days.
Side effects:
Blurring of vision,
Yellow discoloration of skin and nails
Alopecia.
BM depression.
• Other uses:
– Amebic hepatitis
– Giardiasis.
– rheumatoid arthritis.
2:Drugs Against Erythrocytic Form
2: Quinine:
• Blood schizonticidal and gametocidal.
• Taken orally
• It is reserved for severe infection and for malarial strains
that are resistant to other agents such as chloroquine.
 Stimulate uterine contraction C/I in pregnancy
abortion
 Given if a positive Coombs test for hemolytic anemia
ADRs:
• Cinchonism: a syndrome causing nausea, vomiting,
tinnitus, and vertigo
• Slight deafness,
• Haemolysis
2:Drugs Against Erythrocytic Form
3: Mefloquine
• Similar to chloroquine.
• Less toxic.
• Effective in most cases of chlorquine resistant malaria.
• ECG abnormalities and cardiac arrest are possible if
mefloquine is taken concurrently with quinine or
quinidine.
4: Artemisnin
• Useful in Treatment of severe, multidrug resistant
malaria.
• IV, orally and rectally
• High doses neurotoxicity & prolonged QT
3. Blood schizonticide and
sporontocide
Pyrimethamine “Antifolate”
• inhibits plasmodial dihydrofolate reductase (DFR)
• They have tissue and blood schizonticidal effect
clinical and radical cure.
ADRs: megaloplastic anemia.
• Combination: Pyrimethamine + sulphadoxine=
Fansidar®
for : P. malariae and Toxoplasma gondii.
Other Protozoa
 Trichomoniasis and Giardiasis
 Metronidazole &Tinadizole
 Toxoplasmosis
 Pyrimethamine-sulphadoxine (Fansidar®)
 Co-trimoxazole
 Azithromycin
 Leishmaniasis
 Na- stebogluconate .
Antihelmintic Drugs(AHDs)
Drugs that kill or remove intestinal parasites
 Vermicide – to kill.
 Vermifuge – affect the worm in such away,
they can be expelled by peristalsis or by
purgatives (laxatives).
 Purgation may be needed as MgSO4 or NaSO4,
C/I intestinal obstruction and pregnancy.
 AHDs are C/I in pregnancy teratogenicity
Helminths (Worms)
• Three major groups:
 Nematods :Round worm -Ascaris.
Hook worm
Pin worm
Whip worm
Thread worm
 Trematodes: (Flat worm):
Schistosoma.mansoni (Schistosomiasis)

Cestodes (Tape worms):
Taenia Saginata (Taeniasis), Taenia solium
(cysticercosis)
Antihelemintic Drugs
Antihelemintic Drugs
For Nematodes
1. Mebendazole
• MOA: acts by binding to and interfering with the assembly of
the parasites’ microtubules and also by decreasing glucose
uptake
• C/I in pregnancy
2. Pyrantel pamoate.
•
MOA: It is depolarizing NM blocker, the paralyzed worm is
then expelled from the host’s intestinal tract.
• along with mebendazole, is effective in the treatment of
infections caused by roundworms, pinworms, and
hookworms
Antihelemintic Drugs(cont.)
• For Trematodes
• Praziquantel
• MOA: Increase Ca+2 permeability contracture
and paralysis.
• DOC in all forms of schistosomiasis and other
trematode infections
• SE:
• drowsiness, dizziness, malaise, and anorexia as
GIT upsets
• C/I: pregnancy and nursing mother
Antihelemintic Drugs(cont.)
• For Cestodes
 Niclosamide
• MOA: inhibition of the parasite’s mitochondrial
phosphorylation of ADP to form of ATP.
• A laxative is administered prior to oral
administration of niclosamide, to purge the bowel
of all dead segments and so preclude digestion
and liberation of the ova, which may lead to
cysticercosis.