Pages that link to "Q28484622"

← Imipramine is an orally active drug against both antimony sensitive and resistant Leishmania donovani clinical isolates in experimental infection (Q28484622)

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The following pages link to Imipramine is an orally active drug against both antimony sensitive and resistant Leishmania donovani clinical isolates in experimental infection (Q28484622):

Displaying 16 items.

Recent developments in drug discovery for leishmaniasis and human African trypanosomiasis (Q27011766) (← links)
Combination of liposomal CpG oligodeoxynucleotide 2006 and miltefosine induces strong cell-mediated immunity during experimental visceral leishmaniasis (Q27341915) (← links)
A screen-and-treat strategy targeting visceral leishmaniasis in HIV-infected individuals in endemic East African countries: the way forward? (Q28541690) (← links)
The Use of Gene Ontology Term and KEGG Pathway Enrichment for Analysis of Drug Half-Life (Q28552953) (← links)
Imipramine alters the sterol profile in Leishmania amazonensis and increases its sensitivity to miconazole. (Q35977108) (← links)
Vaccination against a virus-encoded cytokine significantly restricts viral challenge (Q37252720) (← links)
Treatment failure in leishmaniasis: drug-resistance or another (epi-) phenotype? (Q38209866) (← links)
Drug delivery: lessons to be learnt from Leishmania studies (Q38254087) (← links)
Investigational drugs for visceral leishmaniasis (Q38269581) (← links)
Repurposing as a strategy for the discovery of new anti-leishmanials: the-state-of-the-art (Q38939544) (← links)
Simple colorimetric trypanothione reductase-based assay for high-throughput screening of drugs against Leishmania intracellular amastigotes (Q39067203) (← links)
Miltefosine Resistant Field Isolate From Indian Kala-Azar Patient Shows Similar Phenotype in Experimental Infection (Q40067217) (← links)
Cholesterol-lowering drug, in combination with chromium chloride, induces early apoptotic signals in intracellular L. donovani amastigotes, leading to death (Q49866040) (← links)
In vitro screening of known drugs identified by scaffold hopping techniques shows promising leishmanicidal activity for suramin and netilmicin. (Q55240622) (← links)
Ketanserin, an antidepressant, exerts its antileishmanial action via inhibition of 3-hydroxy-3-methylglutaryl coenzyme A reductase (HMGR) enzyme of Leishmania donovani (Q87673902) (← links)
In vivo experiments demonstrate the potent antileishmanial efficacy of repurposed suramin in visceral leishmaniasis (Q99633688) (← links)

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