- Paromomycin sulfate (Humatin):
- Overview:
- Classification:
aminoglycoside-- related to
neomycin, streptomycin, &
kanamycin (Kantrex)
- Luminal amebicide
{no significant absorption from
the gastrointestinal tract}
- Direct &
indirect gametocidal activity
{indirect secondary to bowel
bacteria inhibition}
- Clinical Uses:
- monotherapy:
alternative for asymptomatic
amebiasis
- For mild/moderate
disease: paromomycin (Humatin) in
combination with tissue
amebicide, e.g. metronidazole (Flagyl)
- Pharmacokinetics:
- Minimal
absorption/small amount absorbed
slowly excreted by glomerular
filtration
- Cautions:
- In patients with
renal insufficiency-- toxic
levels may be achieved
- Prolonged use at
non-therapeutic levels can cause
bacterial/yeast superinfections.
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Leishmania
- Overview:-Leishmaniasis
- Characteristics-of idea
diseases (cutaneous, visceral,
mucocutaneous) caused by protozoal
parasites classified in the genus Leishmania.
- Causal
Agents:
- "Leishmaniasis is an
infection caused by obligate
intracellular protozoa transmitted
by sandflies, belonging to the genus Leishmania.
- Several species
are found in different
geographical areas and cause
different clinical
manifestations.
- While the taxonomy
is still not definitive, a
generally accepted classification
recognizes 12 species.
- These include a L.
donovani complex with 3
species (L. donovani, L.
infantum, L. chagasi);
a L. mexicana complex
with 2 species (L. mexicana
and L. amazonensis); L.
tropica; L. major; L.
aethiopica; and a group of
the subgenus Viannia
with 4 species (L. (V.)
braziliensis, L. (V.)
guyanensis, L. (V.)
panamensis, and L. (V.)
peruviana.
- The different
species are morphologically
undistinguishable, but can be
differentiated on the basis of
their isoenzymes, antigens, and
nucleic acids composition."
 Life
Cycle
- Clinical Characteristics:Leishmaniasis
-
"Human leishmanial
infections can result in 3 main forms of
disease.
- The factors
determining the form of disease
include leishmanial species,
geographic location, and immune
response of the host.
- Cutaneous
leishmaniasis is characterized by
one or more cutaneous lesions on
areas where sandflies have fed.
- Ulcerative lesions
appear that resolve spontaneously
over a period of weeks to months,
but can recur.
- Mucosal
leishmaniasis is caused
principally by members of the
subgenus Viannia and is
found in Central and South
America. This form of
leishmaniasis results in
nasopharyngeal lesions that can
be severe.
- Visceral
leishmaniasis (kala-azar) is
caused primarily by the L.
donovani complex and to a
lesser extent by L. tropica
in the Old World, and by L.
amazonensis in the New
World.
- Its
clinical manifestations
include fever,
hepatosplenomegaly,
weakness and progressive
emaciation which can
result in death if
untreated. Some
patients develop post
kala azar dermal leishmaniasis.
- Visceral leishmaniasis is
becoming an important
opportunistic infection
in areas where it
coexists with HIV."- CDC: http://www.dpd.cdc.gov/DPDx/HTML/Leishmaniasis.htm
- Laboratory Diagnosis:leishmaniasis
- Pharmacological
Management: Leishmaniasis
- Drug of
choice --sodium antimony gluconate
(Sodium stibogluconate (Pentostam))
- Preferred Route of
Administration -- IV for large
volumes
- Side effects
develop with drug accumulation
- most
common:Gastrointestinal
symptoms, fever, rash.
- Uncommon:
cardiac, renal, liver
damage; hemolytic anemia
- Alternative drugs:
- pentamidine (Pentam)
- Amphotericin B
(Fungizone, Amphotec) {may be
associated with severe side
effects}
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