2587-00-0

Basic information

• Product Name: 2,6-DICHLOROPYRIDINE N-OXIDE
• Synonyms: 2,6-DICHLOROPYRIDINE N-OXIDE;AURORA KA-6496;AURORA KA-3003;2,6-Dichloropyridine-N-oxide,98%;2,6-dichloro-2,3-dihydropyridin-3-one;NSC 136569;2,6-Dichloropyridine N-oxide 98%;2,6-dichloro-1-oxidopyridin-1-ium
• CAS NO: 2587-00-0
• Molecular Formula: C₅H₃Cl₂NO
• Molecular Weight: 163.99
• Product Categories: Heterocyclic Compounds;Nucleotides and Nucleosides;Bases & Related Reagents;Nucleotides;C5Heterocyclic Building Blocks;Halogenated Heterocycles;Heterocyclic Building Blocks;Pyridines;Building Blocks;C5;C5 to C6;Chemical Synthesis;Halogenated Heterocycles;Heterocyclic Building Blocks;Heterocycle-Pyridine series
• Mol File: 2587-00-0.mol

Chemical Properties

• Melting Point: 138-142 °C(lit.)
• Boiling Point: 344.2 °C at 760 mmHg
• Flash Point: 162 °C
• Appearance: White to creamish or light yellow/Powder or Crystals
• Density: 1.47 g/cm³
• Storage Temp.: under inert gas (nitrogen or Argon) at 2-8°C
• Solubility: Chloroform
• PKA: -2.26±0.10(Predicted)
• CAS DataBase Reference: 2,6-DICHLOROPYRIDINE N-OXIDE(CAS DataBase Reference)
• NIST Chemistry Reference: 2,6-DICHLOROPYRIDINE N-OXIDE(2587-00-0)
• EPA Substance Registry System: 2,6-DICHLOROPYRIDINE N-OXIDE(2587-00-0)

Safety Data

• Hazard Codes: Xn
• Statements: 36/37/38-20/21/22
• Safety Statements: 36/37/39-26-22
• RIDADR: UN2811
• WGK Germany: 3
• HazardClass: 6.1
• Hazardous Substances Data: 2587-00-0(Hazardous Substances Data)

Usage

Uses

Used in Organic Synthesis:
2,6-DICHLOROPYRIDINE N-OXIDE is used as a synthetic intermediate for the development of various organic compounds. Its chemical structure, featuring two chlorine atoms at the 2nd and 6th positions of the pyridine ring and an oxide group, makes it a versatile and reactive molecule that can be further modified or functionalized to produce a wide range of products.
Used in Pharmaceutical Industry:
In the pharmaceutical industry, 2,6-DICHLOROPYRIDINE N-OXIDE is used as a key component in the synthesis of certain pharmaceuticals. Its unique properties allow it to be incorporated into the molecular structures of drugs, potentially enhancing their efficacy, stability, or other desirable characteristics.
Used in Chemical Research:
2,6-DICHLOROPYRIDINE N-OXIDE also finds application in chemical research, where it may be employed to study reaction mechanisms, explore new synthetic routes, or investigate the properties of novel compounds. Its reactivity and structural features make it an interesting subject for scientific inquiry and experimentation.
Used in Agrochemicals:
In the agrochemical sector, 2,6-DICHLOROPYRIDINE N-OXIDE may be utilized in the development of new pesticides, herbicides, or other products designed to protect crops and enhance agricultural productivity. Its chemical properties can be harnessed to create molecules with specific biological activities, targeting pests or weeds without harming the crops themselves.
Overall, 2,6-DICHLOROPYRIDINE N-OXIDE is a versatile compound with a range of applications across different industries, primarily due to its utility in organic synthesis and its potential for further modification and functionalization.

InChI:InChI=1/C5H4Cl2NO/c6-4-2-1-3-5(7)8(4)9/h1-4H/q+1

Synthetic route

2,6-dichloropyridine (2402-78-0) → 2,6-dichloropyridine N-oxide (2587-00-0)

Conditions	Yield
With dihydrogen peroxide; trifluoroacetic acid at 80℃; for 2h; Reagent/catalyst; Temperature;	90.15%
With dihydrogen peroxide; trifluoroacetic acid In water at 0℃; for 6.5h; Reflux;	87.6%
With dihydrogen peroxide; trifluoroacetic acid In water for 6.5h; Reflux;	87.6%

2,6-dichloropyridine (2402-78-0) + dihydrogen peroxide (7722-84-1) → 2,6-dichloropyridine N-oxide (2587-00-0)

Conditions	Yield
With trifluoroacetic acid

2,6-dichloropyridine N-oxide (2587-00-0) → 2,6-dichloropyridine (2402-78-0)

Conditions	Yield
With 2-methyl-but-2-ene; trans-dioxo(5,10,15,20-tetramesitylporphirinato)ruthenium(VI) In benzene at 30℃; for 15h;	94%
With (4,4′-di-tert-butyl-2,2′-bipyridine)bis[(2-pyridinyl)phenyl]iridium(III) hexafluorophosphate; di-tert-butyl 1,4-dihydro-2,6-dimethyl-3,5-pyridine-dicarboxylate In acetonitrile at 20℃; for 0.75h; Inert atmosphere; Irradiation; chemoselective reaction;	92%
With ammonium formate; silica gel; zinc In methanol at 20℃; for 0.166667h; chemoselective reaction;	88%

2,6-dichloropyridine N-oxide (2587-00-0) + octanol (111-87-5) → 1-hydroxy-6-(octyloxy)pyridine-2(1H)-one (162912-64-3)

Conditions	Yield
With sodium hydroxide In water at 20 - 120℃; pH=3.5 - 4.0; Reflux;	90.6%

2,6-dichloropyridine N-oxide (2587-00-0) → 2,4,6-trichloropyridine (16063-69-7)

Conditions	Yield
With trichlorophosphate for 4h; Reflux;	85%
With trichlorophosphate for 4h; Reflux;	85%
With trichlorophosphate for 4h; Reflux;	85%

2,6-dichloropyridine N-oxide (2587-00-0) → C5H4BCl2NO3 (1415388-29-2)

Conditions	Yield
With (1,5-cyclooctadiene)(methoxy)iridium(I) dimer; bis(pinacol)diborane; 4,4'-di-tert-butyl-2,2'-bipyridine	85%

2,6-dichloropyridine N-oxide (2587-00-0) + allyl (4-bromophenyl)sulfide (6334-55-0) + phenylacetylene (536-74-3) → 2-(4-bromophenylthio)-1-phenylpent-4-en-1-one

Conditions	Yield
With Mor-DaIPhos-AuCl; sodium tetrakis[(3,5-di-trifluoromethyl)phenyl]borate In 1,2-dichloro-ethane at 60℃; for 20h;	77%

2,6-dichloropyridine N-oxide (2587-00-0) → 2-chloropyridine (109-09-1) + 2,6-dichloropyridine (2402-78-0)

Conditions	Yield
With copper(l) iodide; zinc In ethanol at 55 - 60℃; for 3h;	A n/a B 75%

2,6-dichloropyridine N-oxide (2587-00-0) + [(N,N’-bis(2,6-diisopropylphenyl)imidazol-2-ylidene)Ge{CH(SiMe3)2}][(3,5-(CF3)2C6H3)4] → C32H12BF24(1-)*C39H58Cl2GeN3O2Si2(1+)

Conditions	Yield
In fluorobenzene at 20℃; for 0.0833333h; Inert atmosphere;	73%

1-allylsulfanyl-4-chloro-benzene (15446-14-7) + 2,6-dichloropyridine N-oxide (2587-00-0) + phenylacetylene (536-74-3) → 2-(4-chlorophenylthio)-1-phenylpent-4-en-1-one

Conditions	Yield
With Mor-DaIPhos-AuCl; sodium tetrakis[(3,5-di-trifluoromethyl)phenyl]borate In 1,2-dichloro-ethane at 60℃; for 8h;	70%

2,6-dichloropyridine N-oxide (2587-00-0) → 2,6-dichloro-4-nitro-pyridine (25194-01-8)

Conditions	Yield
Stage #1: 2,6-dichloropyridine N-oxide With sulfuric acid; nitric acid In water at 148 - 156℃; for 1h; Stage #2: With ammonia In water pH=6;	66.4%
Stage #1: 2,6-dichloropyridine N-oxide With sulfuric acid; nitric acid at 148 - 156℃; for 1h; Stage #2: With ammonia In water at 20℃; pH=6;	66.4%
With sulfuric acid; nitric acid for 15h; Heating;	25%
With sulfuric acid; nitric acid at 160℃;

2,6-dichloropyridine N-oxide (2587-00-0) → 2-amino-6-chloropyridine N-oxide

Conditions	Yield
With ammonia In methanol at 105℃; for 26h;	55%

2,6-dichloropyridine N-oxide (2587-00-0) + 2-ethyl-7-mercapto-8-methyl-4H-chromen-4-one (1362586-97-7) → 7-(6-chloropyridin-2-ylthio)-2-ethyl-8-methyl-4H-chromen-4-one N-oxide (1362586-28-4)

Conditions	Yield
With pyridine at 20℃; for 2h;	53%
With pyridine for 2h; Reflux;	53%

2,6-dichloropyridine N-oxide (2587-00-0) + 2-ethyl-7-mercapto-4H-chromen-4-one (1337971-33-1) → 7-(6-chloropyridin-2-ylthio)-2-ethyl-4H-chromen-4-one N-oxide (1362586-25-1)

Conditions	Yield
With pyridine at 20℃; for 2h;	51%

2-(trifluoromethoxy)biphenylyl-2'-diazonium hexafluoroantimonate + 2,6-dichloropyridine N-oxide (2587-00-0) → N-trifluoromethoxy-2,6-dichloropyridinium hexafluoroantimonate

Conditions	Yield
In dichloromethane at 42℃; for 3.5h; Sealed tube; Inert atmosphere;	51%

2,6-dichloropyridine N-oxide (2587-00-0) + 7-mercapto-4-methyl-2H-chromen-2-one (137215-27-1) → 7-(6-chloropyridin-2-ylthio)-4-methyl-2H-chromen-2-one N-oxide (1141172-55-5)

Conditions	Yield
With pyridine at 20℃; for 2h;	48%
With pyridine for 2h; Reflux;	48%

2,6-dichloropyridine N-oxide (2587-00-0) + tert-butylmagnesium chloride (677-22-5) → 2-(tert-butyl)-6-chloropyridine 1-oxide

Conditions	Yield
With copper(l) iodide In tetrahydrofuran at 0 - 20℃; Inert atmosphere;	45%

2,6-dichloropyridine N-oxide (2587-00-0) → 2-Chloropyridinyl 6-disulfide (72917-33-0)

Conditions	Yield
With thiourea In ethanol for 2h; Heating;	40%

Togni's reagent (887144-97-0) + 2,6-dichloropyridine N-oxide (2587-00-0) + trimethylsilyl bis(trifluoromethanesulfonyl)imide (82113-66-4) → 2,6-dichloro-N-(trifluoromethoxy)pyridinium triflimide

Conditions	Yield
Stage #1: 2,6-dichloropyridine N-oxide; trimethylsilyl bis(trifluoromethanesulfonyl)imide In dichloromethane at 20℃; Schlenk technique; Inert atmosphere; Glovebox; Stage #2: Togni's reagent In dichloromethane at 20℃; for 12h; Schlenk technique; Inert atmosphere; Glovebox;	39%

2,6-dichloropyridine N-oxide (2587-00-0) → 2-hydroxylamino-6-chloropyridine 1-oxide (72647-13-3)

Conditions	Yield
With hydroxylamine In ethanol for 144h; Ambient temperature;	24%

2,6-dichloropyridine N-oxide (2587-00-0) + C32H50FeN4 (1433221-40-9) → C64H100Fe2N8O (1433221-44-3)

Conditions	Yield
In benzene at -78 - 20℃; for 8h; Inert atmosphere;	18%

2,6-dichloropyridine N-oxide (2587-00-0) + isopropylamine (75-31-0) → (6-chloro-1-oxy-pyridin-2-yl)-isopropyl-amine (59618-29-0)

Conditions	Yield
In hexane; dimethyl sulfoxide	15.01%

piperidine (110-89-4) + 2,6-dichloropyridine N-oxide (2587-00-0) → 6'-chloro-3,4,5,6-tetrahydro-2H-[1,2']bipyridinyl 1'-oxide (59618-35-8)

Conditions	Yield
In hexane; benzene	12.9%

2,6-dichloropyridine N-oxide (2587-00-0) + 3-Chlorostyrene (2039-85-2) → 2,6-dichloropyridine (2402-78-0) + (R)-meta-chlorostyrene oxide (20697-04-5, 53631-04-2, 115648-90-3, 62600-71-9) + (S)-3-chlorostyrene oxide (115648-90-3)

Conditions	Yield
chiral ruthenium porphyrin complex catalyst In toluene at -10℃; for 48h; Title compound not separated from byproducts.;

4-vinylbenzyl chloride (1073-67-2) + 2,6-dichloropyridine N-oxide (2587-00-0) → 2,6-dichloropyridine (2402-78-0) + (R)-2-(4-chlorophenyl)oxirane (2788-86-5, 53649-47-1, 97466-49-4, 21019-51-2) + (2S)-2-(4-chlorophenyl)oxirane (2788-86-5, 21019-51-2, 53649-47-1, 97466-49-4)

Conditions	Yield
chiral ruthenium porphyrin complex catalyst In toluene at -10℃; for 48h; Title compound not separated from byproducts.;

1-propenylbenzene (873-66-5) + 2,6-dichloropyridine N-oxide (2587-00-0) → 2,6-dichloropyridine (2402-78-0) + (1S,2S)-(-)-1-phenyl-1-propene oxide (4518-66-5) + (+)-(R,R)-β-methylstyrene oxide (14212-54-5)

Conditions	Yield
chiral ruthenium porphyrin complex catalyst In toluene at -10℃; for 48h; Title compound not separated from byproducts.;

styrene (292638-84-7) + 2,6-dichloropyridine N-oxide (2587-00-0) → 2,6-dichloropyridine (2402-78-0) + (R)-Styrene oxide (20780-53-4) + (S)-styrene oxide (20780-54-5)

Conditions	Yield
chiral ruthenium porphyrin complex catalyst In toluene at -10℃; for 48h; Title compound not separated from byproducts.;

2,6-dichloropyridine N-oxide (2587-00-0) → 8-chloro-3-deazaadenine

Conditions	Yield
Multi-step reaction with 10 steps 1: HNO3; H2SO4 / 160 °C 2: AcOH; Fe / Heating 3: HNO3; H2SO4 / 20 °C 4: H2SO4 / 100 °C 5: 51 percent / Fe / 2 h / Heating 6: aq. NaOH / Heating 7: 96 percent / Ac2O / 4.5 h / Heating 8: 49 percent / ammonia / methanol / 90 h / 160 °C 9: 72 percent / NaOH; H2 / Pd/C / H2O / 20 h / 1758.3 Torr 10: 31 percent / t-butyl hypochlorite / dimethylsulfoxide / 144 h / 20 °C
Multi-step reaction with 10 steps 1: HNO3; H2SO4 / 160 °C 2: AcOH; Fe / Heating 3: HNO3; H2SO4 / 20 °C 4: H2SO4 / 100 °C 5: 51 percent / Fe / 2 h / Heating 6: aq. NaOH / Heating 7: 96 percent / Ac2O / 4.5 h / Heating 8: 49 percent / ammonia / methanol / 90 h / 160 °C 9: 72 percent / NaOH; H2 / Pd/C / H2O / 20 h / 1758.3 Torr 10: HCl; mCPBA / N,N-dimethyl-acetamide / 0.42 h / 20 °C
Multi-step reaction with 9 steps 1: HNO3; H2SO4 / 160 °C 2: AcOH; Fe / Heating 3: HNO3; H2SO4 / 20 °C 4: H2SO4 / 100 °C 5: 94 percent / Fe; H2O; HCl / ethanol / 16 h / 95 °C 6: 96 percent / Ac2O / 4.5 h / Heating 7: 49 percent / ammonia / methanol / 90 h / 160 °C 8: 72 percent / NaOH; H2 / Pd/C / H2O / 20 h / 1758.3 Torr 9: 31 percent / t-butyl hypochlorite / dimethylsulfoxide / 144 h / 20 °C
Multi-step reaction with 9 steps 1: HNO3; H2SO4 / 160 °C 2: AcOH; Fe / Heating 3: HNO3; H2SO4 / 20 °C 4: H2SO4 / 100 °C 5: 94 percent / Fe; H2O; HCl / ethanol / 16 h / 95 °C 6: 96 percent / Ac2O / 4.5 h / Heating 7: 49 percent / ammonia / methanol / 90 h / 160 °C 8: 72 percent / NaOH; H2 / Pd/C / H2O / 20 h / 1758.3 Torr 9: HCl; mCPBA / N,N-dimethyl-acetamide / 0.42 h / 20 °C

2,6-dichloropyridine N-oxide (2587-00-0) → 3-chloro-3-deazaadenine

Conditions	Yield
Multi-step reaction with 10 steps 1: HNO3; H2SO4 / 160 °C 2: AcOH; Fe / Heating 3: HNO3; H2SO4 / 20 °C 4: H2SO4 / 100 °C 5: 51 percent / Fe / 2 h / Heating 6: aq. NaOH / Heating 7: 96 percent / Ac2O / 4.5 h / Heating 8: 49 percent / ammonia / methanol / 90 h / 160 °C 9: 72 percent / NaOH; H2 / Pd/C / H2O / 20 h / 1758.3 Torr 10: 6.2 percent / HCl; mCPBA / N,N-dimethyl-acetamide / 0.42 h / 20 °C
Multi-step reaction with 9 steps 1: HNO3; H2SO4 / 160 °C 2: AcOH; Fe / Heating 3: HNO3; H2SO4 / 20 °C 4: H2SO4 / 100 °C 5: 94 percent / Fe; H2O; HCl / ethanol / 16 h / 95 °C 6: 96 percent / Ac2O / 4.5 h / Heating 7: 49 percent / ammonia / methanol / 90 h / 160 °C 8: 72 percent / NaOH; H2 / Pd/C / H2O / 20 h / 1758.3 Torr 9: 6.2 percent / HCl; mCPBA / N,N-dimethyl-acetamide / 0.42 h / 20 °C

Upstream product

• 2402-78-0 2,6-dichloropyridine 
• 7722-84-1 dihydrogen peroxide 

Downstream Products

• 2402-78-0 2,6-dichloropyridine 
• 16063-69-7 2,4,6-trichloropyridine 
• 25194-01-8 4-nitro-2,6-dichloro-pyridine 
• 109-09-1 2-chloropyridine 
• 20697-04-5 (R)-meta-chlorostyrene oxide 
• 115648-90-3 (S)-3-chlorostyrene oxide 
• 2788-86-5 (R)-2-(4-chlorophenyl)oxirane 
• 2788-86-5 (2S)-2-(4-chlorophenyl)oxirane 
• 4518-66-5 (1S,2S)-(-)-1-phenyl-1-propene oxide 
• 14212-54-5 (+)-(R,R)-β-methylstyrene oxide 
• 20780-53-4 (R)-Styrene oxide 
• 20780-54-5 (S)-styrene oxide 
• 668268-64-2 8-chloro-3-deazaadenine 
• 668268-69-7 3-chloro-3-deazaadenine 

Relevant articles and documents

The discovery of novel diarylpyri(mi)dine derivatives with high level activity against a wide variety of HIV-1 strains as well as against HIV-2

By means of structure-based molecular hybridization strategy, a series of novel diarylpyri(mi)dine derivatives targeting the entrance channel of HIV-1 reverse transcriptase (RT) were designed, synthesized and evaluated as potent non-nucleoside reverse transcriptase inhibitors (NNRTIs). Encouragingly, all the tested compounds showed good activities against wild-type (WT) HIV-1 (IIIB) with EC50 in the range of 1.36 nM–29 nM, which is much better than those of nevirapine (NVP, EC50 = 125.42 nM) and azidothymidine (AZT, EC50 = 11.36 nM). Remarkably, these compounds also displayed effective activity against the most of the single and double-mutated HIV-1 strains with low EC50 values, which is comparable to the control drugs. Besides, these compounds were also exhibited favorable enzymatic inhibitory activity. Moreover, preliminary structure-activity relationships (SARs) and molecular modeling study were investigated and discussed in detail. Unexpectedly, four diarylpyrimidines yielded moderate anti-HIV-2 activities. To our knowledge, this is rarely reported that diarylpyrimidine-based NNRTIs have potent activity against both HIV-1 and HIV-2 in cell culture.

Regioselective Reaction of Heterocyclic N-Oxides, an Acyl Chloride, and Cyclic Thioethers

Treatment of electron deficient pyridine N-oxides with 4-nitrobenzoyl chloride and a cyclic thioether in the presence of triethylamine leads to the corresponding 2-functionalized product in up to a 74% isolated yield. The transformation can also be accomplished with alternative nitrogen containing heterocycles, including quinolines, pyrimidines, and pyrazines. To expand the scope of the transformation, diisopropyl ether can be used as the reaction medium to allow for the use of solid thioether substrates.

Green catalyst induction 2,6-dichloro-pyridine-N-oxide synthesis (by machine translation)

The invention discloses a production method for 2,6-dichloropyridine-N-oxide. The production method is characterized in that a novel green catalyst (heteropoly acid) is disclosed according to the synergy effect theory, is prepared by performing oxygen atom coordination bridging on heterotoms and polyatoms according to a certain structure, has the advantages of unique acidity, quasi-liquid behaviors, multifunction (acid, oxidation and photocatalysis) and the like, and can be used for controllably synthesizing the 2,6-dichloropyridine-N-oxide, and successfully realizing the high-content and high-yield synthesis and mass production of the 2,6-dichloropyridine-N-oxide. According to the production method, 2,6-dichloropyridine is used as a raw material, and reaction is accelerated by virtue of high efficiency and multifunction of the heteropoly acid; a synthesis method is simple, high in efficiency, environmentally friendly and suitable for industrial production, and the purity and yield of a product can reach more than 98 percent and 85 percent respectively.

Efficient synthesis of 4-amino-2,6-dichloropyridine and its derivatives

A facile synthetic route to an important intermediate 4-amino-2,6-dichloropyridine was developed. Oxidation of 2,6-dichloropyridine as a starting material gave pyridine N-oxide derivative which was subjected to nitration followed by reduction. Subsequent nitration of the product and nucleophilic displacement reaction were carried out to afford fully substituted energetic pyridine derivatives. Most of the synthetic reactions proceeded under mild conditions.

Synthesis and evaluation of novel imidazo[4,5-: C] pyridine derivatives as antimycobacterial agents against Mycobacterium tuberculosis

The current study involves the synthesis of novel imidazo[4,5-c]pyridine derivatives (IPD) containing amide/urea/sulfonamide. The synthesized compounds were evaluated for in vitro and in vivo antimycobacterial activities against Mycobacterium tuberculosis. The pharmacological activities were determined by the objective to better understand their structure-activity relationship (SAR) for their in vitro antimycobacterial activity against M. tuberculosis. Some synthesized compounds showed significant activity against M. tuberculosis based on the agar dilution method. Among the forty-one compounds screened, compounds 21, 22 and 23 were found to be the most active compounds against M. tuberculosis. In the in vivo animal model, 21, 22 and 23 decreased the bacterial load in lung and spleen tissues at the dose of 50 mg kg-1 body weight.

Stereo- and Regioselective Alkyne Hydrometallation with Gold(III) Hydrides

The hydroauration of internal and terminal alkynes by gold(III) hydride complexes [(C^N^C)AuH] was found to be mediated by radicals and proceeds by an unexpected binuclear outer-sphere mechanism to cleanly form trans-insertion products. Radical precursors such as azobisisobutyronitrile lead to a drastic rate enhancement. DFT calculations support the proposed radical mechanism, with very low activation barriers, and rule out mononuclear mechanistic alternatives. These alkyne hydroaurations are highly regio- and stereospecific for the formation of Z-vinyl isomers, with Z/E ratios of >99:1 in most cases.

Design, synthesis and anti-HIV evaluation of novel diarylpyridine derivatives targeting the entrance channel of NNRTI binding pocket

The development of novel NNRTIs with activity against variants of HIV-1RT is crucial for overcoming treatment failure. In the present study, a series of novel 6-substituted diarylpyridine derivatives targeting the entrance channel of the NNIBP of RT were designed through a molecular hybridization strategy. Encouragingly, these new diarylpyridine derivatives were found to be active against wild-type (WT) HIV-1 with an EC50 values ranging from 0.035 μM to 1.99 μM. Nearly half of them exhibited more potent inhibitory activities in cellular assays than the control drug nevirapine (NVP). Notably, three most promising compounds If (EC50 = 35 nM), Ia (EC50 = 43 nM) and IIa (EC50 = 41 nM) showed high potency against WT and were comparable to the reference drug delavirdine (DLV) (EC50 = 33 nM). Moreover, compounds Ib, IIb and IIh displayed effective activity against the most common clinically observed single and double-mutated HIV-1 strains in micromolar concentrations. In particular, the inhibition of IIb against the K103N mutation (EC50 = 49 nM), which confers resistance to a wide variety of NNRTIs, was about 140 times more effective than NVP (EC50 = 6.78 μM), 50 times more than DLV (EC50 = 2.48 μM) and about 3 times more than EFV (EC50 = 0.12 μM), indicating that the newly designed compounds have great potential to be further developed as new anti-HIV-1 agents. Preliminary structure-activity relationships (SARs) and molecular modeling of the new diarylpyridine derivatives were discussed in detail.

Structural optimization of pyridine-type DAPY derivatives to exploit the tolerant regions of the NNRTI binding pocket

Based on the crystallographic studies of diarylpyrimidines (DAPYs), we embarked on incorporating the hydrophilic piperidyl or morpholinyl group into the known DAPY derivatives bearing the pyridine moiety as a core structure, with the double aim to exploit additional interactions with the HIV-1 NNRTI binding pocket (NNIBP), as well as to improve the compound solubility. The antiviral evaluation result show that the most potent compounds I-8b2, I-8b3, I-8b4 and I-8c3 exhibited anti-HIV-1 (IIIB) strain activity ranging from 7.4 nM to 9.4 nM (SI = 168-1283), superior to FDA-approved drugs of nevirapine (NVP), lamivudine (3TC) and delavirdine (DLV), and comparable to etravirine (ETV), zidovudine (AZT) and efavirenz (EFV). Additionally, compounds I-8c2 and I-8c3 showed moderate activity against NNRTI resistant strains baring mutations K103N and Y181C with EC50 values of 6.2 mM and 6.8 mM, respectively. Preliminary structure-activity relationships (SARs), reverse transcriptase inhibition efficacy and molecular modeling of selected compounds are also presented. These outcomes support our design hypothesis and demonstrate that the piperidyl group modified pyridine-typed DAPY derivatives are highly potent NNRTIs with improved water solubility.

6-substitute diaryl pyridine derivative and preparing method and application thereof

The invention discloses a 6-substitute diaryl pyridine derivative and a preparing method and application thereof. The compound has a structure shown in a formula I. The invention further relates to a drug composition containing the compound with the structure in the formula I and provides application of the compound to preparation of anti-HIV drugs.

Discovery of 2-pyridone derivatives as potent HIV-1 NNRTIs using molecular hybridization based on crystallographic overlays

Based on crystallographic overlays of the known inhibitors TMC125 and R221239 complexed in RT, we designed a novel series of 4-phenoxy-6-(phenylamino) pyridin-2(1H)-one derivatives as HIV NNRTIs by molecular hybridization approach. The biological testing results indicated that 2-pyridone scaffold of these inhibitors was indispensable for their anti-HIV-1 activity, and substitution of halogen at the 3-position of the 2-pyridone ring would decrease the anti-HIV activity. Four most potent compounds had anti-HIV-1 IIIB activities at low micromolar concentrations (EC50 = 0.15-0.84 μM), comparable to that of nevirapine and delavidine. Some compounds were selected to test their anti-HIV-1 RT inhibitory action and to perform molecular modeling studies to predict the binding mode of these 2-pyridone derivatives.