Inxight Drugs

Search results for "WHO ESSENTIAL MEDICINES LIST" in comments (approximate match)

Showing 1 - 10 of 311 results

NIFURTIMOX

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M84I3K7C2O

Status:

US Approved Rx (2020)

First approved in 2020

Class (Stereo):

CHEMICAL (RACEMIC)

Targets:

Conditions:

Nifurtimox is a nitrofuran derivative used as a primary agent in the treatment of American trypanosomiasis (Chagas' disease) caused by Trypanosoma cruzi, especially in the acute, early stage of the disease. The efficacy of nifurtimox in the treatment...

TRICLABENDAZOLE

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4784C8E03O

Status:

US Approved Rx (2019)

First approved in 2019

Class (Stereo):

CHEMICAL (ACHIRAL)

Targets:

Conditions:

Triclabendazole, (brand name Avomec, Egaten, etc) is a member of the benzimidazole family of anthelmintics used to treat liver flukes, specifically fascioliasis and paragonimiasis. Triclabendazole used routinely since 1983 in veterinary practice for ...

MILTEFOSINE

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53EY29W7EC

Status:

US Approved Rx (2014)

First approved in 2014

Class (Stereo):

CHEMICAL (ACHIRAL)

Targets:

Conditions:

Miltefosine is an anti-leishmanial agent. It is an alkyl phospholipids compound, was originally intended for breast cancer and other solid tumors. However, it could not be developed as an oral agent because of dose-limiting gastro-intestinal toxicity...

BENZNIDAZOLE

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YC42NRJ1ZD

Status:

US Approved Rx (2017)

First approved in 2011

Class (Stereo):

CHEMICAL (ACHIRAL)

Targets:

Conditions:

Benznidazole is an antiparasitic medication used in first-line treatment of Chagas disease. Benznidazole is a nitroimidazole antiparasitic with good activity against acute infection with Trypanosoma cruzi, commonly referred to as Chagas disease. Like...

other nitroimidazoles, benznidazole's main mechanism of action is to generate radical species which can damage the parasite's DNA or cellular machinery. Under anaerobic conditions, the nitro group of nitroimidazoles is believed to be reduced by the pyruvate:ferredoxin oxidoreductase complex to create a reactive nitro radical species. The nitro radical can then either engage in other redox reactions directly or spontaneously give rise to a nitrite ion and imidazole radical instead. In mammals, the principal mediators of electron transport are NAD+/NADH and NADP+/NADPH, which have a more positive reduction potential and so will not reduce nitroimidazoles to the radical form. This limits the spectrum of activity of nitroimidazoles so that host cells and DNA are not also damaged. This mechanism has been well-established for 5-nitroimidazoles such as metronidazole, but it is unclear if the same mechanism can be expanded to 2-nitroimidazoles (including benznidazole). In the presence of oxygen, by contrast, any radical nitro compounds produced will be rapidly oxidized by molecular oxygen, yielding the original nitroimidazole compound and a superoxide anion in a process known as "futile cycling". In these cases, the generation of superoxide is believed to give rise to other reactive oxygen species. The degree of toxicity or mutagenicity produced by these oxygen radicals depends on cells' ability to detoxify superoxide radicals and other reactive oxygen species. In mammals, these radicals can be converted safely to hydrogen peroxide, meaning benznidazole has very limited direct toxicity to human cells. In Trypanosoma species, however, there is a reduced capacity to detoxify these radicals, which results in damage to the parasite's cellular machinery. Benznidazole has a significant activity during the acute phase of Chagas disease, with a therapeutical success rate up to 80%. Its curative capabilities during the chronic phase are, however, limited. Some studies have found parasitologic cure (a complete elimination of T. cruzi from the body) in pediatric and young patients during the early stage of the chronic phase, but overall failure rate in chronically infected individuals is typically above 80%. However, some studies indicate treatment with benznidazole during the chronic phase, even if incapable of producing parasitologic cure, because it reduces electrocardiographic changes and a delays worsening of the clinical condition of the patient. Side effects tend to be common and occur more frequently with increased age. The most common adverse reactions associated with benznidazole are allergic dermatitis and peripheral neuropathy. It is reported that up to 30% of people will experience dermatitis when starting treatment. Benznidazole may cause photosensitization of the skin, resulting in rashes. Rashes usually appear within the first 2 weeks of treatment and resolve over time. In rare instances, skin hypersensitivity can result in exfoliative skin eruptions, edema, and fever. Peripheral neuropathy may occur later on in the treatment course and is dose-dependent. Other adverse reactions include anorexia, weight loss, nausea, vomiting, insomnia, and dyslexia, and bone marrow suppression. Gastrointestinal symptoms usually occur during the initial stages of treatment and resolves over time. Bone marrow suppression has been linked to the cumulative dose exposure.

ATAZANAVIR

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QZU4H47A3S

Status:

US Approved Rx (2020)

First approved in 2003

Class (Stereo):

CHEMICAL (ABSOLUTE)

Targets:

Conditions:

Atazanavir is the first once-daily protease inhibitor for the treatment of human immunodeficiency virus type 1 infection and should be used only in combination therapy, as part of a highly active antiretroviral therapy (HAART) regimen. In addition to...

EMTRICITABINE

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G70B4ETF4S

Status:

US Approved Rx (2023)

First approved in 2003

Class (Stereo):

CHEMICAL (ABSOLUTE)

Targets:

Conditions:

Emtricitabine was discovered by Emory researchers Dr. Dennis C. Liotta, Dr. Raymond F. Schinazi and Dr. Woo-Baeg Choi and licensed to Triangle Pharmaceuticals by Emory University in 1996. Triangle was acquired by Gilead in 2003. Emtricitabine, market...

MIFEPRISTONE

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320T6RNW1F

Status:

US Approved Rx (2019)

First approved in 2000

Class (Stereo):

CHEMICAL (ABSOLUTE)

Targets:

Conditions:

Mifepristone is a synthetic steroid with antiprogestational effects indicated for the medical termination of intrauterine pregnancy through 49 days' pregnancy. Doses of 1 mg/kg or greater of mifepristone have been shown to antagonize the endometrial ...

LOPINAVIR

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2494G1JF75

Status:

US Approved Rx (2021)

First approved in 2000

Class (Stereo):

CHEMICAL (ABSOLUTE)

Targets:

Conditions:

Lopinavir (ABT-378) is an antiretroviral of the protease inhibitor class. It is used against HIV infections as a fixed-dose combination with another protease inhibitor, ritonavir, under the trade names Kaletra.

ABACAVIR

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WR2TIP26VS

Status:

US Approved Rx (2017)

First approved in 1998

Class (Stereo):

CHEMICAL (ABSOLUTE)

Targets:

Conditions:

Abacavir is a nucleoside reverse transcriptase inhibitor used for treatment of HIV infection (either alone or in combination with other antiviral drugs). It was shown that abacavir exerts its antiviral activity through its active metabolite, carbovir...

EFAVIRENZ

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JE6H2O27P8

Status:

US Approved Rx (2018)

First approved in 1998

Class (Stereo):

CHEMICAL (ABSOLUTE)

Targets:

Conditions:

Efavirenz (brand names Sustiva® and Stocrin®) is a non-nucleoside reverse transcriptase inhibitor (NNRTI) and is used as part of highly active antiretroviral therapy (HAART) for the treatment of a human immunodeficiency virus (HIV) type 1. For HIV in...

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Condition

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Substance Form

Search results for "WHO ESSENTIAL MEDICINES LIST" in comments (approximate match)

NIFURTIMOX

M84I3K7C2O

TRICLABENDAZOLE

4784C8E03O

MILTEFOSINE

53EY29W7EC

BENZNIDAZOLE

YC42NRJ1ZD

ATAZANAVIR

QZU4H47A3S

EMTRICITABINE

G70B4ETF4S

MIFEPRISTONE

320T6RNW1F

LOPINAVIR

2494G1JF75

ABACAVIR

WR2TIP26VS

EFAVIRENZ

JE6H2O27P8