139110-80-8

Basic information

• Product Name: ZANAMIVIR HYDRATE
• Synonyms: ZANAMIVIR HYDRATE;ZANAMIVIR(FORR&DONLY);4-Guanidino-2,4-dideoxy-2,3-dehydro-N-acetylneuraminic acid;4-Guanidino-Neu5Ac2en;D-glycero-D-galacto-Non-2-enonic acid, 5-(acetylamino)-4-[(aminoiminomethyl)amino]-2,6-anhydro-3,4,5-trideoxy- (9CI);GANA;GANA (inhibitor);GG 167
• CAS NO: 139110-80-8
• Molecular Formula: C₁₂H₂₀N₄O₇
• Molecular Weight: 332.31
• EINECS: 1592732-453-0
• Product Categories: Anti-viral Compounds;Anti-virals;Intermediates & Fine Chemicals;Pharmaceuticals;Inhibitors
• Mol File: 139110-80-8.mol
• Article Data: 14

Chemical Properties

• Melting Point: 2560C (dec.)
• Appearance: white to beige/
• Density: 1.75 g/cm³
• Storage Temp.: -20°C Freezer
• Solubility: H2O: soluble10mg/mL, clear
• PKA: 3.82±0.70(Predicted)
• CAS DataBase Reference: ZANAMIVIR HYDRATE(CAS DataBase Reference)
• NIST Chemistry Reference: ZANAMIVIR HYDRATE(139110-80-8)
• EPA Substance Registry System: ZANAMIVIR HYDRATE(139110-80-8)

Safety Data

• Hazard Codes: Xn
• Statements: 22-36/37/38
• Safety Statements: 26
• WGK Germany: 3
• RTECS: RA9451000
• Hazardous Substances Data: 139110-80-8(Hazardous Substances Data)

Usage

Description

Zanamivir was launched as Relenza in Australia for treatment of human influenza A and B virus infections. Zanamivir (4-guanidino-Neu5Ac2en) can be obtained by several similar ways, for instance in seven step synthesis starting from N-acetyI-D-neuraminic acid. Mechanistically, Zanamivir is a potent and specific inhibitor of neuraminidase (or sialidase), a key viral surface glycohydrolase essential for viral replication and disease progression by catalyzing the cleavage of terminal sialic acid residues from the glycoprotein. The in vitro activity of Zanamivir against a wide variety of influenza A and B strains was demonstrated in different model systems; its activity against clinically relevant isolates of influenza virus, with IC50 values ranging from 0.005 to 15 pM was superior to those of amantadine and rimantadine.

Chemical Properties

Colorless Crystalline Solid

Originator

Biota Scientific Management (Australia)

Uses

Different sources of media describe the Uses of 139110-80-8 differently. You can refer to the following data:
1. Influenza viral neuraminidase inhibitor; structural analog of the sialic acid. Antiviral
2. antineoplastic, anti-metabolite
3. ZANAMIVIR HYDRATE is a sialic acid analog that inhibits neuraminidase release of newly replicated influenza virus particles. It has been shown to selectively inhibit the growth of influenza A and B viruses in plaque reduction assays with IC50 values ranging from 5 to 14 nM and to directly inhibit influenza A and B virus neuraminidases with IC50 values ranging from 0.6 to 7.9 nM in vitro. The efficacy and tolerabilbity of zanamivir has also been established in clinical trial.[Cayman Chemical]

Indications

Zanamivir (Relenza) is a neuraminidase inhibitor with activity against influenza A and B strains. Like oseltamivir, zanamivir is a reversible competitive antagonist of viral neuraminidase. It inhibits the release of progeny virus, causes viral aggregation at the cell surface, and impairs viral movement through respiratory secretions. Resistant variants with hemagglutinin and/or neuraminidase mutations have been produced in vivo; however, clinical resistance to zanamivir is quite rare at present.

Manufacturing Process

The 1st method of preparation of zanamivir:5-(Acetylamino)-4-amino-2,6-anhydro-3,4,5-trideoxy-D-glycero-D-galacto- non-2-enonic acid (3 g, 10.35 mmol) was suspended in methanol (37.5 ml) and sodium acetate (1.89 g, 23.1 mmol) was added, causing a "caking" of the suspension and making stirring difficult. To this at 21°C with exclusion of moisture was added a solution of cyanogen bromide (1.14 g, 10.8 mmol) in methanol (150 ml), in a dropwise manner. Stirring gradually became easier, until a readily stirrable suspension was obtained. Addition was complete in 3.5 hours. The mixture was then stirred at 21°C with exclusion of moisture for 44 hours. The small amount of remaining solid was filtered off and solvent evaporated in vacuo to an orange-brown foam. The foam was taken up in methanol (125 ml) and with rapid stirring at 21°C was treated dropwise with propan-2-ol (130 ml). The precipitate was filtered off, washed with iso- PrOH/MeOH (3:2), and combined filtrate and washings evaporated to give the 5-(acetylamino)-4-cyanoamino-2,6-anhydro-3,4,5-trideoxy-D-glycero-D- galacto-non-2-enonic acid as a pale yellow foam (3.48 g).5-(Acetylamino)-4-cyanoamino-2,6-anhydro-3,4,5-trideoxy-D-glycero-D- galacto-non-2-enonic acid (500 mg, 1.59 mmol) was dissolved in dried (over 3 A mol. sieves) methanol (20 ml) and anhydrous hydrazine (0.5 ml, 15.9 mmol) was added. This was then stirred at 21°C for 18 hours. The white precipitate was filtered off, washed with methanol and air-dried (0.172 g, 31%). The solid was taken up in water (3.2 ml) and with warming and swirling, propan-2-ol (8.1 ml) was added. The cystallised material was filtered off, air-dried then dried under high vacuum to give D-glycero-D-galacto-non- 2-enonic acid, 5-(acetylamino)-4-(aminoiminomethyl)amino)-2,6-anhydro- 3,4,5-trideoxy as a white solid (0.127 g,); >97% purity; M.P. >180°C.The 2nd method of preparation of zanamivir:5-(Acetylamino)-4-cyanoamino-2,6-anhydro-3,4,5-trideoxy-D-glycero-D- galacto-non-2-enopyranosonic acid (500 mg, 1.585 mmol) was dissolved in dried (over 3 A mol. sieves) methanol (12 ml) and methylamine (33 wt. % solution in ethanol, 1.93 ml, 15.85 mmol) was added. This was stirred at 21°C for 18 hours. The precipitate was filtered off and air dried to a white solid (127 mg, 23%). This was recrystalIised from water (1.4 ml) and propan- 2-ol (6.9 ml). The product was filtered off and dried under high vacuum to give the title compound as a white solid (56 mg, 10.2%). Concentration of mother liquors gave a further 21.3 mg (4%) of D-glycero-D-galacto-non-2- enonic acid, 5-(acetylamino)-4-(aminoiminomethyl)amino)-2,6-anhydro-3,4,5- trideoxy-; 97.7% purity; M.P. >180°C.

Brand name

Relenza (GlaxoSmithKline).

Therapeutic Function

Antiviral

Acquired resistance

Resistance is presently uncommon, including strains resistant to oseltamivir. In clinical trials the frequency was no more than 1% of exposed patients.

General Description

Zanamivir is identical to 2-deoxy-2,3-dehydro-N-acetylneuraminic acid except that itpossesses a guanidino group at position 4 instead of a hydroxylgroup. At positions 119 and 227 of the receptor site,there exist glutamic acid residues. Zanamivir has beenshown to form a salt bridge with the guanidine and Glu-119and a charge transfer interaction with Glu-227. These interactionsincrease the interaction strength with the enzymeand create an excellent competitive inhibitor and an effectiveantiviral agent for influenza types A and B.Human studies have shown that zanamivir is effectivewhen administered before or after exposure to the influenzavirus. If administered before exposure to the virus, the drugreduced viral propagation, infectivity, and disease symptoms.If administered after exposure, the drug reduces propagation,viral titer, and illness. Zanamivir is marketed as a dry powderfor oral inhalation. It is used in adolescents and adults who have been exposed and are symptomatic for not more than 2days. Zanamivir is also indicated for prophylactically treatingfamily members of a person who has developed influenza.

Pharmaceutical Applications

A synthetic neuraminidase inhibitor formulated for administration by inhalation.

Biochem/physiol Actions

Zanamivir is an influenza viral neuraminidase inhibitor.

Pharmacology

Zanamivir is generally well tolerated. Bronchospasm and impaired lung function have been reported in some patients taking this medication, but many of these individuals had serious underlying pulmonary disease. Zanamivir should be discontinued if an individual develops bronchospasm or breathing difficulties; treatment and hospitalization may be required. Allergic reactions, including angioedema, have been rarely reported. The efficacy of zanamivir depends upon the proper use of the inhaler device.

Pharmacokinetics

Oral bioavailability is poor. After inhalation local respiratory mucosal concentrations greatly exceed those that are inhibitory for influenza A and B replication. The median concentrations in the sputum exceed 1 mg/L 6 h after inhalation and remain detectable for 24 h.

Clinical Use

Different sources of media describe the Clinical Use of 139110-80-8 differently. You can refer to the following data:
1. Treatment of influenza A and B infections in patients over 7 years of age, and prophylaxis of patients ??5 years of age
2. Zanamivir is indicated for treatment of uncomplicated acute influenza A and B virus in patients aged 7 and older.Treatment should be initiated no later than 2 days after the onset of symptoms. Zanamivir shortens the duration of illness by 1 to 1.5 days. It is also an effective prophylaxis against influenza; however, the FDA has not approved this indication at the time of publication.

Side effects

Different sources of media describe the Side effects of 139110-80-8 differently. You can refer to the following data:
1. Most adverse effects are related to the respiratory tree. These include rhinorrhea and, rarely, bronchospasm. Nausea and vomiting have been reported at low incidence.
2. Zanamivir is contraindicated in individuals with severe or decompensated chronic obstructive lung disease or asthma because it has not been shown to be effective in these individuals and can cause serious adverse pulmonary reactions. Individuals with mild to moderate asthma may have a decline in lung function when taking zanamivir. The safety and efficacy of this medication have not been determined in individuals with severe renal insufficiency. No clinically significant drug interactions have been reported. Zanamivir does not decrease the effectiveness of the influenza vaccine.

Drug interactions

Potentially hazardous interactions with other drugs None known

Metabolism

Zanamirvir is effective when administered via the nasal, intraperitoneal, and intravenous (IV) routes, but it is inactive when given orally. Animal studies have shown 68% recovery of the drug in the urine following intraperitoneal administration, 43% urinary recovery following nasal administration, and only 3% urinary recovery following oral administration. Human data gave results similar to those obtained in animal models. Human efficacy studies with nasal drops or sprays demonstrated that the drug was effective when administered before and after exposure to influenza A or B virus. When given before viral inoculation, the drug reduced viral shedding, infection, and symptoms. When administered beginning at either 26 or 32 hours after inoculation, there was a reduction in shedding, viral titer, and fever.

references

[1] elliott m. zanamivir: from drug design to the clinic. philos trans r soc lond b biol sci, 2001, 356(1416): 1885-93.

InChI:InChI=1/C12H20N4O7.H2O/c1-4(18)15-8-5(16-12(13)14)2-7(11(21)22)23-10(8)9(20)6(19)3-17;/h2,5-6,8-10,17,19-20H,3H2,1H3,(H,15,18)(H,21,22)(H4,13,14,16);1H2/t5-,6+,8+,9+,10+;/m0./s1

Upstream product

• 19342-33-7 N-acetyl neuraminic acid 
• 166197-22-4 1H-pyrazolecarboxamidine hydrochloride 
• 130525-62-1 5-acetamido-4-amino-2,6-anhydro-3,4,5-trideoxy-D-glycero-D-galacto-non-2-enonic acid 
• 4023-02-3 1H-pyrazole-1-carboximidamide hydrochloride 
• 108740-39-2 (1S,2R)-1-((2R,3R,4S,6R)-3-acetamido-4,6-diacetoxy-6-(methoxycarbonyl)tetrahydro-2H-pyran-2-yl)propane-1,2,3-triyl triacetate 
• 139110-70-6 5-acetamido-7,8,9-tri-O-acetyl-2,6-anhydro-4-amino-3,4,5-trideoxy-D-glycero-D-galacto-non-2-enonic acid methyl ester 

Relevant articles and documents

Organocatalytic and scalable synthesis of the anti-influenza drugs zanamivir, laninamivir, and CS-8958

Zanamivir, laninamivir, and CS-8958 are three neuraminidase inhibitors that have been clinically used to combat influenza. We report herein a novel organocatalytic route for preparing these agents. Only 13 steps are needed for the assembly of zanamivir and laninamivir from inexpensive d-araboascorbic acid by this synthetic route, which relies heavily on a thiourea-catalyzed enantioselective Michael addition of acetone to tert-butyl (2-nitrovinyl)carbamate and an anti-selective Henry reaction of the resulting Michael adduct with an aldehyde prepared from d-araboascorbic acid. The synthetic procedures are scalable, as evident from the preparation of more than 3.5 g of zanamivir.

Preparation method of zanamivir intermediate and preparation method of zanamivir

The invention relates to a preparation method of a zanamivir intermediate, namely an acetylation protected amino compound, and a preparation method of zanamivir. The preparation method of the zanamivir, provided by the invention, comprises the following steps: performing cyclization by taking sialic acid as a raw material and through group protection to produce a cyclization substance, treating the cyclization substance by a metal amino substance at one step to obtain the acetylation protected amino compound, and removing a hydroxyl protective agent acetic acid ester and removing guanidyl from imipyrozole reaction to obtain the zanamivir, wherein the process of treating the cyclization substance by the metal amino substance at one step to obtain the acetylation protected amino compound is great substantial breakthrough in preparation of the zanamivir, the synthesis steps are greatly shortened and the process operation is simplified. Ring opening is conducted by the cheap metal amino substance instead of expensive trimethylsilyl azid, so that the cost is reduced and the safety of the production process is guaranteed. According to thepreparation method of the zanamivir, provided by the invention, the total mass yield can reach 50 percent or above and is greatly increased as compared with that in the prior art.

Chemical insight into the emergence of influenza virus strains that are resistant to Relenza

A reagent panel containing ten 4-substituted 4-nitrophenyl α-d-sialosides and a second panel of the corresponding sialic acid glycals were synthesized and used to probe the inhibition mechanism for two neuraminidases, the N2 enzyme from influenza type A virus and the enzyme from Micromonospora viridifaciens. For the viral enzyme the logarithm of the inhibition constant (Ki) correlated with neither the logarithm of the catalytic efficiency (kcat/Km) nor catalytic proficiency (kcat/Kmkun). These linear free energy relationship data support the notion that these inhibitors, which include the therapeutic agent Relenza, are not transition state mimics for the enzyme-catalyzed hydrolysis reaction. Moreover, for the influenza enzyme, a correlation (slope, 0.80 ± 0.08) is observed between the logarithms of the inhibition (Ki) and Michaelis (Km) constants. We conclude that the free energy for Relenza binding to the influenza enzyme mimics the enzyme-substrate interactions at the Michaelis complex. Thus, an influenza mutational response to a 4-substituted sialic acid glycal inhibitor can weaken the interactions between the inhibitor and the viral neuraminidase without a concomitant decrease in free energy of binding for the substrate at the enzyme-catalyzed hydrolysis transition state. The current findings make it clear that new structural motifs and/or substitution patterns need to be developed in the search for a bona fide influenza viral neuraminidase transition state analogue inhibitor.