Zanamivir: from drug design to the clinic

Elliott, Michael J.

doi:10.1098/rstb.2001.1021

Cited by 35 publications

(27 citation statements)

References 41 publications

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“…Recently, NA has become a 'hot' target in anti-influenza fields and newly discovered drugs, zanamivir (Relenza ® ) [56] and oseltamivir (Tamiflu ® ) [57], are all the NAIs. So in this article we will mainly discuss NA of the influenza virus.…”

Section: The General Structure Of Influenza Virusmentioning

confidence: 99%

Structure and Functions of Influenza Virus Neuraminidase

Gong¹,

Xu²,

Zhang

2007

CMC

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Influenza is a disease that deeply affects millions of people every year. There has not been any drug effective against all strains. Neuraminidase (NA) is the major surface glycoprotein of the influenza virus, which possesses critical enzymatic activity and has been considered as a suitable target for designing agents against influenza viruses. Here we review the structure and functions of this enzyme and touch upon the structure-activity relationship (SAR) of existing influenza neuraminidase inhibitors (NAIs).

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Section: The General Structure Of Influenza Virusmentioning

confidence: 99%

Structure and Functions of Influenza Virus Neuraminidase

Gong¹,

Xu²,

Zhang

2007

CMC

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“…4-Deoxy-4-guanidino-Neu5Ac2en 5 was selected by Glaxo in 1990 as a lead drug candidate against influenza virus infection, and progressed under the generic name zanamivir (reviewed in [130,131]). Zanamivir was granted regula tory approval by the Food and Drug Administration (FDA) in the United States in 1999, under the tradename Relenza, as the first sialidase-targeting drug for the treatment of influenza.…”

Section: Efficacy Against Virus Replicationmentioning

confidence: 99%

Development of Influenza Virus Sialidase Inhibitors

Pascolutti

Thomson

Itzstein

2016

Methods and Principles in Medicinal Chemistry

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“…Influenza is a highly contagious respiratory tract infection that is caused by influenza type A and B viruses (Elliott, 2001). Influenza can cause serious morbidity and increased mortality, particularly in the elderly or the immunocompromised and those with underlying diseases such as chronic obstructive pulmonary disease, cardiovascular disease, and diabetes (Dunn and Goa, 1999; Freund et al ., 1999; Elliott, 2001; Colman, 2005).…”

Section: Introductionmentioning

confidence: 99%

“…Influenza can cause serious morbidity and increased mortality, particularly in the elderly or the immunocompromised and those with underlying diseases such as chronic obstructive pulmonary disease, cardiovascular disease, and diabetes (Dunn and Goa, 1999; Freund et al ., 1999; Elliott, 2001; Colman, 2005). Neuraminidase inhibitors, oseltamivir and zanamivir (ZMR), are considered to be the drug of choice in the treatment of influenza principally due to their low toxicity and high efficacy (Freund et al ., 1999; Boonyapiwat et al ., 2011; Gupta et al ., 2011).…”

Section: Introductionmentioning

confidence: 99%

“…1) is available as a dry powder formulation for oral inhalation applied using Diskhaler™ (a dry powder inhaler) due to its poor oral bioavailability (2%; range 1 to 5%) in human (Dunn and Goa, 1999; Caballero et al ., 2000; Elliott, 2001; Colman, 2005). The major drawback with this route of administration is lack of patient compliance, and therapy is not recommended in patients with chronic represpiratory conditions such as asthma, COPD, etc.…”

Section: Introductionmentioning

confidence: 99%

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Zanamivir Oral Delivery: Enhanced Plasma and Lung Bioavailability in Rats

Shanmugam

Sohn

et al. 2013

Biomolecules and Therapeutics

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The objective of this study was to enhance the oral bioavailability (BA) of zanamivir (ZMR) by increasing its intestinal permeability using permeation enhancers (PE). Four different classes of PEs (Labrasol®, sodium cholate, sodium caprate, hydroxypropyl β-cyclodextrin) were investigated for their ability to enhance the permeation of ZMR across Caco-2 cell monolayers. The flux and Papp of ZMR in the presence of sodium caprate (SC) was significantly higher than other PEs in comparison to control, and was selected for further investigation. All concentrations of SC (10-200 mM) demonstrated enhanced flux of ZMR in comparison to control. The highest flux (13 folds higher than control) was achieved for the formulation with highest SC concentration (200 mM). The relative BA of ZMR formulation containing SC (PO-SC) in plasma at a dose of 10 mg/kg following oral administration in rats was 317.65% in comparison to control formulation (PO-C). Besides, the AUC0-24 h of ZMR in the lungs following oral administration of PO-SC was 125.22 ± 27.25 ng hr ml-1 with a Cmax of 156.00 ± 24.00 ng/ml reached at 0.50±0.00 h. But, there was no ZMR detected in the lungs following administration of control formulation (PO-C). The findings of this study indicated that the oral formulation PO-SC containing ZMR and SC was able to enhance the BA of ZMR in plasma to an appropriate amount that would make ZMR available in lungs at a concentration higher (>10 ng/ml) than the IC50 concentration of influenza virus (0.64-7.9 ng/ml) to exert its therapeutic effect.

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Zanamivir: from drug design to the clinic

Cited by 35 publications

References 41 publications

Structure and Functions of Influenza Virus Neuraminidase

Structure and Functions of Influenza Virus Neuraminidase

Development of Influenza Virus Sialidase Inhibitors

Zanamivir Oral Delivery: Enhanced Plasma and Lung Bioavailability in Rats

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