Inxight Drugs

Showing 21 - 30 of 1,076 results

Status:

US Approved Rx (2017)

First approved in 2006

Class (Stereo):

CHEMICAL (ABSOLUTE)

Targets:

Conditions:

Decitabine was first synthesized by Pliml and Sorm in the Institute of Organic Chemistry, Czechoslovak Academy of Sciences in 1964. Later, the drug was approved by FDA for the treatment of myelodysplastic syndromes in patients with cancer. Upon admin...

TIGECYCLINE

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70JE2N95KR

Status:

US Approved Rx (2015)

First approved in 2005

Class (Stereo):

CHEMICAL (ABSOLUTE)

Targets:

Conditions:

Tigecycline (INN) is an antibiotic used to treat a number of bacterial infections. It is a first in class glycylcycline that is administered intravenously. For the treatment of infections caused by susceptible strains of the designated microorganisms...

NELARABINE

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60158CV180

Status:

US Approved Rx (2024)

First approved in 2005

Class (Stereo):

CHEMICAL (ABSOLUTE)

Targets:

Conditions:

Arranon is a nucleoside metabolic inhibitor indicated for the treatment of patients with T-cell acute lymphoblastic leukemia and T-cell lymphoblastic lymphoma. It is a purine nucleoside analog converted to its corresponding arabinosylguanine nucleoti...

Clofarabine triphosphate

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YPJ8ZV99ZP

Status:

US Approved Rx (2019)

First approved in 2004

Class (Stereo):

CHEMICAL (ABSOLUTE)

Targets:

Conditions:

Clofarabine is a anti-cancer drug which was approved by FDA for the treatment of pediatric patients with relapsed or refractory acute lymphoblastic leukemia. After crossing the cell membrane the drug is rapidly metabolized by deoxycytidine kinase to ...

TINIDAZOLE

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033KF7V46H

Status:

US Approved Rx (2004)

First approved in 2004

Class (Stereo):

CHEMICAL (ACHIRAL)

Targets:

Conditions:

Tinidazole is a synthetic antiprotozoal agent, formally known as 1-[2-(ethylsulfonyl)ethyl]-2-methyl-5-nitroimidazole and a second-generation 2-methyl-5-nitroimidazole. Tinidazole is a prodrug and antiprotozoal agent. The nitro group of tinidazole is...

Azacitidine

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M801H13NRU

Status:

US Approved Rx (2013)

First approved in 2004

Class (Stereo):

CHEMICAL (ABSOLUTE)

Targets:

Conditions:

Azacitidine (Vidaza; Pharmion), an inhibitor of DNA methylation, was approved by the US FDA for the treatment of myelodysplastic syndromes in May 2004. It is the first drug to be approved by the FDA for treating this rare family of bone-marrow disord...

PREGABALIN

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55JG375S6M

Status:

US Approved Rx (2010)

First approved in 2004

Class (Stereo):

CHEMICAL (ABSOLUTE)

Targets:

Conditions:

Pregabalin, marketed under the brand name Lyrica among others. LYRICA is indicated for: Neuropathic pain associated with diabetic peripheral neuropathy (DPN) Postherpetic neuralgia (PHN); Adjunctive therapy for adult patients with partial onset seizu...

DAPTOMYCIN

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NWQ5N31VKK

Status:

US Approved Rx (2018)

First approved in 2003

Class (Stereo):

CHEMICAL (ABSOLUTE)

Targets:

Conditions:

Daptomycin is a lipopeptide antibiotic used in the treatment of systemic and life-threatening infections caused by Gram-positive organisms. Daptomycin has a distinct mechanism of action, disrupting multiple aspects of bacterial cell membrane function...

PIMECROLIMUS

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7KYV510875

Status:

US Approved Rx (2019)

First approved in 2001

Class (Stereo):

CHEMICAL (ABSOLUTE)

Targets:

Conditions:

Pimecrolimus, an ascomycin macrolactam derivative, is an inhibitor of T-cell and mast-cell activation, developed and launched by Novartis for the potential treatment of psoriasis and allergic, irritant and atopic dermatitis. The topical formulation h...

Sirolimus

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W36ZG6FT64

Status:

US Approved Rx (2019)

First approved in 1999

Class (Stereo):

CHEMICAL (ABSOLUTE)

Targets:

Conditions:

Sirolimus is the USAN-assigned generic name for the natural product rapamycin. Sirolimus is produced by a strain of Streptomyces hygroscopicus, isolated from a soil sample collected from Rapa Nui commonly known as Easter Island. Although sirolimus wa...

s isolated as an antifungal agent with potent anticandida activity, subsequent studies revealed impressive antitumor and immunosuppressive activities. Sirolimus demonstrates activity against several murine tumors, such as B16 43 melanocarcinoma, Colon 26 tumor, EM ependymoblastoma, and mammary and colon 38 solid tumors. Demonstration of the potent immunosuppressive activity of sirolimus in animal models of organ transplantation led to clinical trials and subsequent approval by regulatory authorities for prophylaxis of renal graft rejection. Interest in sirolimus as an immunosuppressive therapy in organ transplantation derives from its unique mechanism of action, its unique side-effect profile, and its ability to synergize with other immunosuppressive agents. It is used in medicine to prevent organ transplant rejection and to treat lymphangioleiomyomatosis. Sirolimus inhibits T-lymphocyte activation and proliferation that occurs in response to antigenic and cytokine (Interleukin [IL]-2, IL-4, and IL-15) stimulation by a mechanism that is distinct from that of other immunosuppressants. Sirolimus also inhibits antibody production. In cells, sirolimus binds to the immunophilin, FK Binding Protein-12 (FKBP-12), to generate an immunosuppressive complex. This complex blocks the activation of the cell-cycle-specific kinase, TOR. The downstream events that follow the inactivation of TOR result in the blockage of cell-cycle progression at the juncture of G1 and S phase. Rapamycin/FKBP12 efficiently inhibit some, but not all, functions of mTOR and hence much interest has been placed in the development of drugs that target the kinase activity of mTOR directly. Studies in experimental models show that sirolimus prolongs allograft (kidney, heart, skin, islet, small bowel, pancreatico-duodenal, and bone marrow) survival in mice, rats, pigs, and/or primates. Sirolimus reverses acute rejection of heart and kidney allografts in rats and prolongs the graft survival in presensitized rats. In some studies, the immunosuppressive effect of sirolimus lasts up to 6 months after discontinuation of therapy. This tolerization effect is alloantigen-specific. In rodent models of autoimmune disease, sirolimus suppresses immune-mediated events associated with systemic lupus erythematosus, collagen-induced arthritis, autoimmune type I diabetes, autoimmune myocarditis, experimental allergic encephalomyelitis, graft-versus-host disease, and autoimmune uveoretinitis. Lymphangioleiomyomatosis involves lung tissue infiltration with smooth muscle-like cells that harbor inactivating mutations of the tuberous sclerosis complex (TSC) gene (LAM cells). Loss of TSC gene function activates the mTOR signaling pathway, resulting in cellular proliferation and release of lymphangiogenic growth factors. Sirolimus inhibits the activated mTOR pathway and thus the proliferation of LAM cells.

Development Status

Primary Target

Highest Phase

Approval Year

Condition

Treatment Modality

CNS Activity

Originator

Substance Class

INN Stem

Code System

Protein Type

ATC Level 1

ATC Level 2

ATC Level 3

ATC Level 4

Substance Form

Decitabine

776B62CQ27

TIGECYCLINE

70JE2N95KR

NELARABINE

60158CV180

Clofarabine triphosphate

YPJ8ZV99ZP

TINIDAZOLE

033KF7V46H

Azacitidine

M801H13NRU

PREGABALIN

55JG375S6M

DAPTOMYCIN

NWQ5N31VKK

PIMECROLIMUS

7KYV510875

Sirolimus

W36ZG6FT64