CN1546457A - Preparation of o-nitrobenzaldehyde by biomimetic catalysis oxidation of o-nitrotoluene with oxygen - Google Patents
Preparation of o-nitrobenzaldehyde by biomimetic catalysis oxidation of o-nitrotoluene with oxygen Download PDFInfo
- Publication number
- CN1546457A CN1546457A CNA2003101214781A CN200310121478A CN1546457A CN 1546457 A CN1546457 A CN 1546457A CN A2003101214781 A CNA2003101214781 A CN A2003101214781A CN 200310121478 A CN200310121478 A CN 200310121478A CN 1546457 A CN1546457 A CN 1546457A
- Authority
- CN
- China
- Prior art keywords
- ortho nitro
- general formula
- ortho
- oxygen
- benzaldehyde
- Prior art date
- Legal status (The legal status is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the status listed.)
- Granted
Links
Abstract
The invention relates to a process for preparing aromatic aldehydes, in particular a process for preparing o-nitrobenzaldehyde through bionic catalytic oxidation of ortho-methylnitro benzene, wherein metallic phthalocyanine, single nuclear metalloporphyrin or mu-oxy-double nuclear metalloporphyrin having the similar structure as the biological enzymes are selected as the catalyst for the disclosed process, whose dose is 0.2-1.0% weight of ortho-methylnitro benzene, and methyl alcohol is used as solvent, 0.8-3.0 MPa oxygen is let into 3.0-6.0 mol/L strong alkaline methyl alcohol solution, the reaction temperature is controlled between 25 deg. C to 60 deg. C, the reaction time being 6-48 hrs.
Description
Technical field
The present invention relates to a kind of preparation method of aromatic aldehyde, specifically, relate to the method that a kind of bionically catalyzing and oxidizing Ortho Nitro Toluene prepares Ortho Nitro Benzaldehyde.
Background technology
The preparation method of Ortho Nitro Benzaldehyde mainly contains phenyl aldehyde method, Ortho Nitro Toluene oxidation style, Ortho Nitro Toluene pendant methyl chloro hydrolysis method and ortho-nitrophenyl formyl chloride method at present, and these methods have all adopted the polystep reaction method.The shortcoming of multistep processes is the equipment cost height that reacts used, complex operation, time-consuming; And need of reaction carried out under sour environment more, and be bigger to the corrosion of equipment.In addition, above-mentioned reaction adopts metallic compound to carry out oxidation mostly, and environment has been caused serious pollution.CN1111615A discloses and has a kind ofly made catalyzer with manganese salt, alkoxyalkyl amine is made solvent, carry out the method for preparing Ortho Nitro Benzaldehyde of oxidation in the presence of highly basic with pure oxygen or air, the shortcoming of this method has been to use the metal salt catalyst and the expensive alkoxyalkyl amine solvent of contaminate environment.
Summary of the invention
The invention provides that a kind of technology is simple, cost is low and environment amenable bionically catalyzing and oxidizing Ortho Nitro Toluene prepares the method for Ortho Nitro Benzaldehyde.
The technical solution adopted in the present invention is: be raw material with the Ortho Nitro Toluene, select any in the μ-oxygen dinuclear metalloporphyrin of the monokaryon metalloporphyrin of metal phthalocyanine, general formula (II), (III) structure of general formula (I) structure or general formula (IV) structure for use as catalyzer, in the formula, M
1, M
2, M
3, M
4, M
5Be transition metal atoms, M
1=Fe, Co, Cu, Zn, M
2=Fe, Mn, Co, Cu, Zn, M
3=Fe, Mn, Co, M
4And M
5Can be identical, also can be different, when identical, M
4=M
5=Fe, Mn, Co, not simultaneously, M
4=Fe, M
5=Mn or M
4=Fe, M
5=Co, R can be that carboxyl also can be a hydrogen, R
1, R
2Can be hydrogen, halogen, nitro, hydroxyl, alkoxyl group, dentate X are chlorine, and catalyst consumption is 0.2~1.0% of an Ortho Nitro Toluene weight, with methyl alcohol is solvent, in 3.0~6.0mol/L strong basicity methanol solution, feed the oxygen of 0.8~3.0MPa, control reaction temperature is 25~60 ℃, reaction times 6~48h obtains the Ortho Nitro Benzaldehyde crude product.After adopting ordinary method to separate, purify, obtain the Ortho Nitro Benzaldehyde elaboration.
Preferably have the monokaryon metalloporphyrin of general formula (III) structure or the μ-oxygen-dinuclear metalloporphyrin of general formula (IV) structure and make catalyzer.
Be preferably M in the general formula (III) especially
3=Mn or Fe, R
1=NO
2Or Cl, R
2=H, the monokaryon metalloporphyrin of X=Cl; M in the general formula (IV)
4=M
5=Fe or Mn or Co, M
4And M
5Not not simultaneously, M
4=Fe, M
5=Mn, R
1=NO
2Or Cl, R
2μ-oxygen of=H-dinuclear metalloporphyrin.
The starting point concentration of Ortho Nitro Toluene is 0.6~1.0mol/L.
General formula (I)
General formula (II)
General formula (III)
General formula (IV)
The used catalyzer of the present invention is metal phthalocyanine class and metal porphyrins, its structure and biological enzyme are similar, and biological enzyme has important effect to regulating vital movement in vivo, as hemoglobinase, cytochrome C, cytochrome P-450 and hydrogen peroxide biological enzyme etc., can be at highly selective transmission under the mild conditions, activation oxygen molecule, and organism such as catalyzed oxidation carbohydrate.The present invention just with metal phthalocyanine class and metal porphyrins as the agent of simulation biological enzyme, realized that (25~60 ℃) oxygen catalytic oxidation Ortho Nitro Toluene prepares Ortho Nitro Benzaldehyde under mild conditions.Because catalyst levels is little, temperature of reaction and reaction pressure are lower, and therefore, oxidation depth is easy to control.Structure and suitable adjusting process parameter by selecting catalyst can optionally obtain the oxidation products Ortho Nitro Benzaldehyde.Experimental results show that: these catalyzer all have good catalytic performance to the reaction that the dioxygen oxidation Ortho Nitro Toluene prepares Ortho Nitro Benzaldehyde.In addition, the recyclable utilization of catalyzer reduces reaction cost.
The present invention carries out under alkaline condition, and is less to the corrosion of equipment.Preferred sodium hydroxide of used highly basic or potassium hydroxide.In this reaction, highly basic plays promotor, makes the methyl activation of nitrotoluene, forms the very strong carbanion of reactive behavior, has improved reactive behavior.But alkaline concentration can not be too high, and too high meeting makes the carbanion concentration of generation excessive, and side reaction increases, and alkali concn is excessive, makes the aldehyde of generation change into acid easily; But can not be too low, too low then with raw material effect excessively a little less than, the reaction just can't carry out.So the alkaline amount ranges is controlled at 3.0~6.0mol/L, preferred 4.0~5.0mol/L.
The present invention uses methyl alcohol to make solvent, and is cheap and easy to get, reduced preparation cost.
The present invention uses oxygen as oxygenant, cleaning, pollution-free and cost is low.The pressure range of oxygen is controlled at 0.8~3.0MPa.
The present invention adopts single stage method to make Ortho Nitro Benzaldehyde, simple, the easy row of operation.
The technology of separation, purification Ortho Nitro Benzaldehyde need not to adopt the bisulfite adduct extracting method of cost height, contaminate environment from the reaction mixture that the present invention obtains, but adopts ordinary methods such as filtration, extraction, and step is easy, and is easy to operate.
Embodiment
Embodiment 1
Get 7mg cobalt phthalocyanine (be R=H in the general formula (I), M
1=Co), 3.5g Ortho Nitro Toluene and 5.6g sodium hydroxide in the 200ml autoclave of packing into, add 30ml methyl alcohol, and feeding pressure is the oxygen of 2.5MPa, and temperature control reacts 12h down for 40 ℃ in water-bath.Reacted mixed solution is removed catalyzer through suction filtration earlier, adds 30ml distilled water then, adds the dilute hydrochloric acid neutralization, filters, and the back of purifying is detected with high pressure liquid chromatographic analysis, and the yield of Ortho Nitro Benzaldehyde is 15.6%, and the product purity after the purification is 98.5%.
Embodiment 2
Get the 15mg iron-phthalocyanine (be R=H in the general formula (I), M
1=Fe), 2.5g Ortho Nitro Toluene and 3.6g sodium hydroxide in the autoclave of packing into, add 30ml methyl alcohol, and oxygen pressure is 3.0MPa, and temperature control is 40 ℃ in the water-bath, reaction 18h.Treatment step implements 1 with example, and products obtained therefrom detects with high pressure liquid chromatographic analysis, and the yield of Ortho Nitro Benzaldehyde is 13.5%, and the product purity after the purification is 99.0%.
Embodiment 3
Get the 14mg copper phthalocyanine (be R=H in the general formula (I), M
1=Cu), 3.5g Ortho Nitro Toluene and 6.4g sodium hydroxide in the autoclave of packing into, add 30ml methyl alcohol, and oxygen pressure is 1.0MPa, and temperature control is 25 ℃ in the water-bath, reaction 48h.Treatment step is with embodiment 1, and products obtained therefrom detects with high pressure liquid chromatographic analysis, and the yield of Ortho Nitro Benzaldehyde is 18.4%, and the product purity after the purification is 99.2%.
Embodiment 4
Get 41mg zinc phthalocyanine (be R=H in the general formula (I), M
1=Zn), 4.1g Ortho Nitro Toluene and 7.2g sodium hydroxide in the autoclave of packing into, add 30ml methyl alcohol, and reaction pressure is 2.0MPa, and temperature control is 30 ℃ in the water-bath, reaction 24h.Treatment step is with embodiment 1, and products obtained therefrom detects with high pressure liquid chromatographic analysis, and the yield of Ortho Nitro Benzaldehyde is 20.1%, and the product purity after the purification is 99.0%.
Embodiment 5
Get 7mg tetracarboxylic cobalt phthalocyanine (be R=COOH in the general formula (I), M
1=Co), 3.5g Ortho Nitro Toluene and 7.8g potassium hydroxide in the autoclave of packing into, add 30ml methyl alcohol, and oxygen pressure is 2.0MPa, and temperature control is 60 ℃ in the water-bath, reaction 6h.Treatment step is with embodiment 1, and products obtained therefrom detects with high pressure liquid chromatographic analysis, and the yield of Ortho Nitro Benzaldehyde is 11.6%, and the product purity after the purification is 98.8%.
Embodiment 6
Get 15mg tetracarboxylic iron-phthalocyanine (be R=COOH in the general formula (I), M
1=Fe), 2.5g Ortho Nitro Toluene and 5.0g potassium hydroxide in the autoclave of packing into, add 30ml methyl alcohol, and oxygen pressure is 0.8MPa, and temperature control is 45 ℃ in the water-bath, reaction 18h.Treatment step is with embodiment 1, and products obtained therefrom detects with high pressure liquid chromatographic analysis, and the yield of Ortho Nitro Benzaldehyde is 18.4%, the product purity 99.5% after the purification.
Embodiment 7
Get 14mg tetracarboxylic copper phthalocyanine (be R=COOH in the general formula (I), M
1=Cu), 3.5g Ortho Nitro Toluene and 6.4g sodium hydroxide in the autoclave of packing into, add 30ml methyl alcohol, and oxygen pressure is 1.0MPa, and temperature control is 25 ℃ in the water-bath, reaction 30h.Treatment step is with embodiment 1, and products obtained therefrom detects with high pressure liquid chromatographic analysis, and the yield of Ortho Nitro Benzaldehyde is 17.6%, and the product purity after the purification is 99.4%.
Embodiment 8
Get 41mg tetracarboxylic zinc phthalocyanine (be R=COOH in the general formula (I), M
1=Zn), 4.1g Ortho Nitro Toluene and 10.1g potassium hydroxide in the autoclave of packing into, add 30ml methyl alcohol, and oxygen pressure is 2.0MPa, and temperature control is 30 ℃ in the water-bath, reaction 24h.Treatment step is with embodiment 1, and products obtained therefrom detects with high pressure liquid chromatographic analysis, and the yield of Ortho Nitro Benzaldehyde is 19.8%, and the product purity after the purification is 98.5%.
Embodiment 9
Getting 6mg four-(rubigan) manganoporphyrin (is R in the general formula (II)
1=H, R
2=Cl, M
2=Mn), 0.82g Ortho Nitro Toluene and 1.2g sodium hydroxide in the 200ml autoclave of packing into, add 10ml methyl alcohol, and feeding pressure is the oxygen of 1.0MPa, and temperature control is 45 ℃ in the water-bath, reaction 12h.Reacted mixed solution is removed catalyzer through suction filtration earlier, adds 10ml distilled water then, adds the dilute hydrochloric acid neutralization, filters.Products obtained therefrom detects with high pressure liquid chromatographic analysis, and the yield of Ortho Nitro Benzaldehyde is 13.5%, and the product purity after the purification is 98.9%.
Embodiment 10
Getting 2mg four-(rubigan) zinc protoporphyrin (is R in the general formula (II)
1=H, R
2=Cl, M
2=Zn), 1.17g Ortho Nitro Toluene and 2.0g sodium hydroxide in the autoclave of packing into, add 10ml methyl alcohol, and oxygen pressure is 2.0MPa, and temperature control is 30 ℃ in the water-bath, reaction 24h.Treatment step is with implementing 9, and products obtained therefrom detects with high pressure liquid chromatographic analysis, and the yield of Ortho Nitro Benzaldehyde is 19.7%, and the product purity after the purification is 99.0%.
Embodiment 11
Getting 5mg four-(rubigan) iron porphyrin (is R in the general formula (II)
1=H, R
2=Cl, M
2=Fe), 1.17g Ortho Nitro Toluene and 2.4g sodium hydroxide in the autoclave of packing into, add 10ml methyl alcohol, and oxygen pressure is 0.8MPa, and temperature control is 25 ℃ in the water-bath, reaction 48h.Treatment step is with implementing 9, and products obtained therefrom detects with high pressure liquid chromatographic analysis, and the yield of Ortho Nitro Benzaldehyde is 22.3%, and the product purity after the purification is 99.3%.
Embodiment 12
Getting 14mg four-(rubigan) cobalt porphyrin (is R in the general formula (II)
1=H, R
2=Cl, M
2=Co), 1.37g Ortho Nitro Toluene and 1.8g sodium hydroxide in the autoclave of packing into, add 10ml methyl alcohol, and oxygen pressure is 2.5MPa, 35 ℃ of water-bath temperature controls, reaction 18h.Treatment step is with implementing 9, and products obtained therefrom detects with high pressure liquid chromatographic analysis, and the yield of Ortho Nitro Benzaldehyde is 17.8%, and the product purity after the purification is 99.5%.
Embodiment 13
Getting 14mg four-(rubigan) copper porphyrin (is R in the general formula (II)
1=H, R
2=Cl, M
2=Cu),, 1.37g Ortho Nitro Toluene and 3.4g potassium hydroxide in the autoclave of packing into, add 10ml methyl alcohol, and oxygen pressure is 2.5MPa, and temperature control is 60 ℃ in the water-bath, reaction 6h.Treatment step is with implementing 9, and products obtained therefrom detects with high pressure liquid chromatographic analysis, and the yield of Ortho Nitro Benzaldehyde is 12.4%, and the product purity after the purification is 99.5%.
Embodiment 14
Getting 6mg four-(Chloro-O-Phenyl) manganoporphyrin (is R in the general formula (II)
1=Cl, R
2=H, M
2=Mn), 0.82g Ortho Nitro Toluene and 1.2g sodium hydroxide in the autoclave of packing into, add 10ml methyl alcohol, oxygen pressure 1.0MPa, and temperature control is 40 ℃ in the water-bath, reaction 30h.Treatment step is with implementing 9, and products obtained therefrom detects with high pressure liquid chromatographic analysis, and the yield of Ortho Nitro Benzaldehyde is 28.6%, and the product purity after the purification surpasses 99.0%.
Embodiment 15
Getting 2mg four-(Chloro-O-Phenyl) zinc protoporphyrin (is R in the general formula (II)
1=Cl, R
2=H, M
2=Zn), 1.17g Ortho Nitro Toluene and 2.8g potassium hydroxide in the autoclave of packing into, add 10ml methyl alcohol, and oxygen pressure is 2.0MPa, and temperature control is 30 ℃ in the water-bath, reaction 24h.Treatment step is with implementing 9, and products obtained therefrom detects with high pressure liquid chromatographic analysis, and the yield of Ortho Nitro Benzaldehyde is 24.1%, and the product purity after the purification is 99.0%.
Embodiment 16
Getting 5mg four-(Chloro-O-Phenyl) iron porphyrin (is R in the general formula (II)
1=Cl, R
2=H, M
2=Fe), 1.17g Ortho Nitro Toluene and 2.4g sodium hydroxide in the autoclave of packing into, add 10ml methyl alcohol, and oxygen pressure is 0.8MPa, and temperature control is 25 ℃ in the water-bath, reaction 48h.Treatment step is with implementing 9, and products obtained therefrom detects with high pressure liquid chromatographic analysis, and the yield of Ortho Nitro Benzaldehyde is 24.4%, and the product purity after the purification is 98.5%.
Embodiment 17
Getting 14mg four-(Chloro-O-Phenyl) cobalt porphyrin (is R in the general formula (II)
1=Cl, R
2=H, M
2=Co), 1.37g Ortho Nitro Toluene and 2.5g potassium hydroxide in the autoclave of packing into, add 10ml methyl alcohol, and oxygen pressure is 2.5MPa, and temperature control is 35 ℃ in the water-bath, reaction 18h.Treatment step is with implementing 9, and products obtained therefrom detects with high pressure liquid chromatographic analysis, and the yield of Ortho Nitro Benzaldehyde is 23.2%, and the product purity after the purification is 98.7%.
Embodiment 18
Getting 14mg four-(Chloro-O-Phenyl) copper porphyrin (is R in the general formula (II)
1=Cl, R
2=H, M
2=Cu), 1.37g Ortho Nitro Toluene and 3.4g potassium hydroxide in the autoclave of packing into, add 10ml methyl alcohol, and oxygen pressure is 2.5MPa, and temperature control is 60 ℃ in the water-bath, reaction 6h.Treatment step is with implementing 9, and products obtained therefrom detects with high pressure liquid chromatographic analysis, and the yield of Ortho Nitro Benzaldehyde is 12.4%, and the product purity after the purification is 99.1%.
Embodiment 19
Getting 2mg four-(ortho-nitrophenyl base) manganoporphyrin (is R in the general formula (II)
1=NO
2, R
2=H, M
2=Mn), 1.17g Ortho Nitro Toluene and 2.4g sodium hydroxide in the autoclave of packing into, add 10ml methyl alcohol, oxygen pressure 1.0MPa, and temperature control is 30 ℃ in the water-bath, reaction 24h.Treatment step is with implementing 9, and products obtained therefrom detects with high pressure liquid chromatographic analysis, and the yield of Ortho Nitro Benzaldehyde is 27.9%, and the product purity after the purification is 99.0%.
Embodiment 20
Getting 2mg four-(p-nitrophenyl) manganoporphyrin (is R in the general formula (II)
1=H, R
2=NO
2, M
2=Mn), 1.17g Ortho Nitro Toluene and 2.4g sodium hydroxide in the autoclave of packing into, add 10ml methyl alcohol, oxygen pressure 1.0MPa, and temperature control is 30 ℃ in the water-bath, reaction 24h.Treatment step is with implementing 9, and products obtained therefrom detects with high pressure liquid chromatographic analysis, and the yield of Ortho Nitro Benzaldehyde is 25.1%, and the product purity after the purification is 98.6%.
Embodiment 21
Getting 14mg four-(o-methoxyphenyl) cobalt porphyrin (is R in the general formula (II)
1=OCH
3, R
2=H, M
2=Co), 1.37g Ortho Nitro Toluene and 2.5g potassium hydroxide in the autoclave of packing into, add 10ml methyl alcohol, and oxygen pressure is 2.5MPa, and temperature control is 35 ℃ in the water-bath, reaction 18h.Treatment step is with implementing 9, and products obtained therefrom detects with high pressure liquid chromatographic analysis, and the yield of Ortho Nitro Benzaldehyde is 21.7%, and the product purity after the purification is 99.2%.
Embodiment 22
Getting 14mg four-(o-methoxyphenyl) zinc protoporphyrin (is R in the general formula (II)
1=OCH
3, R
2=H, M
2=Zn), 1.37g Ortho Nitro Toluene and 2.5g potassium hydroxide in the autoclave of packing into, add 10ml methyl alcohol, and oxygen pressure is 2.5MPa, and temperature control is 35 ℃ in the water-bath, reaction 18h.Treatment step is with implementing 9, and products obtained therefrom detects with high pressure liquid chromatographic analysis, and the yield of Ortho Nitro Benzaldehyde is 18.6%, and the product purity after the purification is 99.2%.
Embodiment 23
Getting 14mg four-(p-methoxyphenyl) cobalt porphyrin (is R in the general formula (II)
1=H, R
2=OCH
3, M
2=Co), 1.37g Ortho Nitro Toluene and 2.5g sodium hydroxide in the autoclave of packing into, add 10ml methyl alcohol, and oxygen pressure is 2.5MPa, and temperature control is 35 ℃ in the water-bath, reaction 18h.Treatment step is with implementing 9, and products obtained therefrom detects with high pressure liquid chromatographic analysis, and the yield of Ortho Nitro Benzaldehyde is 20.5%, and the product purity after the purification is 99.4%.
Embodiment 24
Getting 6mg four-(o-hydroxy-phenyl) iron porphyrin (is R in the general formula (II)
1=OH, R
2=H, M
2=Fe), 0.82g Ortho Nitro Toluene and 1.7g potassium hydroxide in the autoclave of packing into, add 10ml methyl alcohol, oxygen pressure 1.0MPa, and temperature control is 40 ℃ in the water-bath, reaction 30h.Treatment step is with implementing 9, and products obtained therefrom detects with high pressure liquid chromatographic analysis, and the yield of Ortho Nitro Benzaldehyde is 23.4%, and the product purity after the purification surpasses 98.6%.
Embodiment 25
Getting 6mg four-(p-hydroxybenzene) copper porphyrin (is R in the general formula (II)
1=H, R
2=OH, M
2=Cu), 0.82g Ortho Nitro Toluene and 1.2g sodium hydroxide in the autoclave of packing into, add 10ml methyl alcohol, oxygen pressure 1.0MPa, and temperature control is 40 ℃ in the water-bath, reaction 30h.Treatment step is with implementing 9, and products obtained therefrom detects with high pressure liquid chromatographic analysis, and the yield of Ortho Nitro Benzaldehyde is 15.9%, and the product purity after the purification surpasses 99.3%.
Embodiment 26
Getting 6mg four-(p-hydroxybenzene) manganoporphyrin (is R in the general formula (II)
1=H, R
2=OH, M
2=Mn), 0.82g Ortho Nitro Toluene and 1.2g sodium hydroxide in the autoclave of packing into, add 10ml methyl alcohol, oxygen pressure 1.0MPa, and temperature control is 40 ℃ in the water-bath, reaction 30h.Treatment step is with implementing 9, and products obtained therefrom detects with high pressure liquid chromatographic analysis, and the yield of Ortho Nitro Benzaldehyde is 22.1%, and the product purity after the purification surpasses 98.6%.
Embodiment 27
Getting 6mg chlorination four-(Chloro-O-Phenyl) iron porphyrin (is R in the general formula (III)
1=Cl, R
2=H, M
3=Fe, X=Cl), 0.82g Ortho Nitro Toluene and 1.2g sodium hydroxide in the autoclave of packing into, add 10ml methyl alcohol, oxygen pressure 1.0MPa, temperature control is 40 ℃ in the water-bath, reaction 30h.Treatment step is with implementing 9, and products obtained therefrom detects with high pressure liquid chromatographic analysis, and the yield of Ortho Nitro Benzaldehyde is 27.6%, the product purity 99.7% after the purification.
Embodiment 28
Getting 6mg chlorination four-(ortho-nitrophenyl base) iron porphyrin (is R in the general formula (III)
1=NO
2, R
2=H, M
3=Fe, X=Cl), 0.82g Ortho Nitro Toluene and 1.7g potassium hydroxide in the autoclave of packing into, add 10ml methyl alcohol, oxygen pressure 1.0MPa, temperature control is 40 ℃ in the water-bath, reaction 30h.Treatment step is with implementing 9, and products obtained therefrom detects with high pressure liquid chromatographic analysis, and the yield of Ortho Nitro Benzaldehyde is 24.8%, the product purity 99.7% after the purification.
Embodiment 29
Getting 6mg chlorination four-(p-nitrophenyl) iron porphyrin (is R in the general formula (III)
1=H, R
2=NO
2, M
3=Fe, X=Cl), 0.82g Ortho Nitro Toluene and 1.7g potassium hydroxide in the autoclave of packing into, add 10ml methyl alcohol, oxygen pressure 1.0MPa, temperature control is 40 ℃ in the water-bath, reaction 30h.Treatment step is with implementing 9, and products obtained therefrom detects with high pressure liquid chromatographic analysis, and the yield of Ortho Nitro Benzaldehyde is 24.6%, and the product purity after the purification is 99.5%.
Embodiment 30
Getting 2mg chlorination four-(Chloro-O-Phenyl) manganoporphyrin (is R in the general formula (III)
1=Cl, R
2=H, M
3=Mn, X=Cl), 1.17g Ortho Nitro Toluene and 2.4g sodium hydroxide in the autoclave of packing into, add 10ml methyl alcohol, oxygen pressure 1.0MPa, temperature control is 30 ℃ in the water-bath, reaction 24h.Treatment step is with implementing 9, and products obtained therefrom detects with high pressure liquid chromatographic analysis, and the yield of Ortho Nitro Benzaldehyde is 29.1%, and the product purity after the purification is 99.0%.
Embodiment 31
Getting 2mg chlorination four-(ortho-nitrophenyl base) manganoporphyrin (is R in the general formula (III)
1=NO
2, R
2=H, M
3=Mn, X=Cl), 1.17g Ortho Nitro Toluene and 2.4g sodium hydroxide in the autoclave of packing into, add 10ml methyl alcohol, oxygen pressure 1.0MPa, temperature control is 30 ℃ in the water-bath, reaction 24h.Treatment step is with implementing 9, and products obtained therefrom detects with high pressure liquid chromatographic analysis, and the yield of Ortho Nitro Benzaldehyde is 28.7%, and the product purity after the purification is 99.0%.
Embodiment 32
Getting 2mg chlorination four-(p-nitrophenyl) manganoporphyrin (is R in the general formula (III)
1=H, R
2=NO
2, M
3=Mn, X=Cl), 1.17g Ortho Nitro Toluene and 2.4g sodium hydroxide in the autoclave of packing into, add 10ml methyl alcohol, oxygen pressure 1.0MPa, temperature control is 30 ℃ in the water-bath, reaction 24h.Treatment step is with implementing 9, and products obtained therefrom detects with high pressure liquid chromatographic analysis, and the yield of Ortho Nitro Benzaldehyde is 26.4%, and the product purity after the purification is 99.4%.
Embodiment 33
Getting 6mg μ-oxygen-double-core four-(Chloro-O-Phenyl) manganoporphyrin (is R in the general formula (IV)
1=Cl, R
2=H, M
4=M
5=Mn), 0.82g Ortho Nitro Toluene and 1.2g sodium hydroxide in the autoclave of packing into, add 10ml methyl alcohol, oxygen pressure 0.8MPa, and temperature control is 40 ℃ in the water-bath, reaction 30h.Treatment step is with implementing 9, and products obtained therefrom detects with high pressure liquid chromatographic analysis, and the yield of Ortho Nitro Benzaldehyde is 29.7%, and the product purity after the purification is 99.5%.
Embodiment 34
Getting 6mg μ-oxygen-double-core four-(ortho-nitrophenyl base) manganoporphyrin (is R in the general formula (IV)
1=NO
2, R
2=H, M
4=M
5=Mn), 0.82g Ortho Nitro Toluene and 1.7g potassium hydroxide in the autoclave of packing into, add 10ml methyl alcohol, oxygen pressure 0.8MPa, and temperature control is 40 ℃ in the water-bath, reaction 30h.Treatment step is with implementing 9, and products obtained therefrom detects with high pressure liquid chromatographic analysis, and the yield of Ortho Nitro Benzaldehyde is 29.2%, and the product purity after the purification is 98.7%.
Embodiment 35
Getting 14mg μ-oxygen-double-core four-(Chloro-O-Phenyl) cobalt porphyrin (is R in the general formula (IV)
1=Cl, R
2=H, M
4=M
5=Co), 1.37g Ortho Nitro Toluene and 2.5g potassium hydroxide in the autoclave of packing into, add 10ml methyl alcohol, and oxygen pressure is 2.5MPa, and temperature control is 35 ℃ in the water-bath, reaction 18h.Treatment step is with implementing 9, and products obtained therefrom detects with high pressure liquid chromatographic analysis, and the yield of Ortho Nitro Benzaldehyde is 25.8%, and the product purity after the purification is 99.5%.
Embodiment 36
Getting 14mg μ-oxygen-double-core four-(ortho-nitrophenyl base) cobalt porphyrin (is R in the general formula (IV)
1=NO
2, R
2=H, M
4=M
5=Co), 1.37g Ortho Nitro Toluene and 2.5g potassium hydroxide in the autoclave of packing into, add 10ml methyl alcohol, and oxygen pressure is 2.5MPa, and temperature control is 35 ℃ in the water-bath, reaction 18h.Treatment step is with implementing 9, and products obtained therefrom detects with high pressure liquid chromatographic analysis, and the yield of Ortho Nitro Benzaldehyde is 25.4%, and the product purity after the purification is 98.7%.
Embodiment 37
Getting 5mg μ-oxygen-double-core four-(Chloro-O-Phenyl) iron porphyrin (is R in the general formula (IV)
1=Cl, R
2=H, M
4=M
5=Fe), 1.17g Ortho Nitro Toluene and 2.4g sodium hydroxide in the autoclave of packing into, add 10ml methyl alcohol, and oxygen pressure is 0.8MPa, and temperature control is 25 ℃ in the water-bath, reaction 48h.Treatment step is with implementing 9, and products obtained therefrom detects with high pressure liquid chromatographic analysis, and the yield of Ortho Nitro Benzaldehyde is 27.1%, and the product purity after the purification is 98.7%.
Embodiment 38
Getting 2mg μ-oxygen-double-core four-(ortho-nitrophenyl base) iron porphyrin (is R in the general formula (IV)
1=NO
2, R
2=H, M
4=M
5=Fe), 1.17g Ortho Nitro Toluene and 1.8g sodium hydroxide in the autoclave of packing into, add 10ml methyl alcohol, oxygen pressure 3.0MPa, and temperature control is 60 ℃ in the water-bath, reaction 6h.Treatment step is with implementing 9, and products obtained therefrom detects with high pressure liquid chromatographic analysis, and the yield of Ortho Nitro Benzaldehyde is 9.7%, and the product purity after the purification is 99.0%.
Embodiment 39
Getting 2mg μ-oxygen-double-core four-(ortho-nitrophenyl base) iron porphyrin (is R in the general formula (IV)
1=NO
2, R
2=H, M
4=M
5=Fe), 1.17g Ortho Nitro Toluene and 2.4g sodium hydroxide in the autoclave of packing into, add 10ml methyl alcohol, oxygen pressure 1.0MPa, and temperature control is 30 ℃ in the water-bath, reaction 24h.Treatment step is with implementing 9, and products obtained therefrom detects with high pressure liquid chromatographic analysis, and the yield of Ortho Nitro Benzaldehyde is 25.9%, and the product purity after the purification is 99.0%.
Embodiment 40
Getting 2mg μ-oxygen-double-core four-(p-nitrophenyl) iron porphyrin (is R in the general formula (IV)
1=H, R
2=NO
2, M
4=M
5=Fe), 1.17g Ortho Nitro Toluene and 1.7g potassium hydroxide in the autoclave of packing into, add 10ml methyl alcohol, oxygen pressure 2.0MPa, and temperature control is 30 ℃ in the water-bath, reaction 12h.Treatment step is with implementing 9, and products obtained therefrom detects with high pressure liquid chromatographic analysis, and the yield of Ortho Nitro Benzaldehyde is 14.9%, and the product purity after the purification is 99.3%.
Embodiment 41
Getting 2mg μ-oxygen-double-core four-(p-nitrophenyl) iron porphyrin (is R in the general formula (IV)
1=H, R
2=NO
2, M
4=M
5=Fe), 1.17g Ortho Nitro Toluene and 2.4g sodium hydroxide in the autoclave of packing into, add 10ml methyl alcohol, oxygen pressure 1.0MPa, and temperature control is 30 ℃ in the water-bath, reaction 24h.Treatment step is with implementing 9, and products obtained therefrom detects with high pressure liquid chromatographic analysis, and the yield of Ortho Nitro Benzaldehyde is 24.7%, and the product purity after the purification is 99.0%.
Embodiment 42
Getting 4mg μ-oxygen-double-core four-(Chloro-O-Phenyl) iron-manganoporphyrin (is R in the general formula (IV)
1=Cl, R
2=H, M
4=Fe, M
5=Mn), 1.4g Ortho Nitro Toluene and 3.4g potassium hydroxide in the autoclave of packing into, add 10ml methyl alcohol, oxygen pressure 2.0MPa, and temperature control is 30 ℃ in the water-bath, reaction 18h.Treatment step is with implementing 9, and products obtained therefrom detects with high pressure liquid chromatographic analysis, and the yield of Ortho Nitro Benzaldehyde is 24.5%, and the product purity after the purification is 98.5%.
Embodiment 43
Getting 2mg μ-oxygen-double-core four-(Chloro-O-Phenyl) iron-manganoporphyrin (is R in the general formula (IV)
1=Cl, R
2=H, M
4=Fe, M
5=Mn), 1.17g Ortho Nitro Toluene and 2.4g sodium hydroxide in the autoclave of packing into, add 10ml methyl alcohol, oxygen pressure 1.0MPa, and temperature control is 30 ℃ in the water-bath, reaction 24h.Treatment step is with implementing 9, and products obtained therefrom detects with high pressure liquid chromatographic analysis, and the yield of Ortho Nitro Benzaldehyde is 33.4%, and the product purity after the purification is 99.0%.
Embodiment 44
Getting 14mg μ-oxygen-double-core four-(ortho-nitrophenyl base) iron-manganoporphyrin (is R in the general formula (IV)
1=NO
2, R
2=H, M
4=Fe, M
5=Mn), 1.17g Ortho Nitro Toluene and 3.4g potassium hydroxide in the autoclave of packing into, add 10ml methyl alcohol, oxygen pressure 1.0MPa, and temperature control is 30 ℃ in the water-bath, reaction 24h.Treatment step is with implementing 9, and products obtained therefrom detects with high pressure liquid chromatographic analysis, and the yield of Ortho Nitro Benzaldehyde is 30.4%, and the product purity after the purification is 99.0%.
Embodiment 45
Getting 14mg μ-oxygen-double-core four-(Chloro-O-Phenyl) iron-cobalt porphyrin (is R in the general formula (IV)
1=Cl, R
2=H, M
4=Fe, M
5=Co), 1.37g Ortho Nitro Toluene and 2.5g potassium hydroxide in the autoclave of packing into, add 10ml methyl alcohol, and oxygen pressure is 2.5MPa, and temperature control is 35 ℃ in the water-bath, reaction 18h.Treatment step is with implementing 9, and products obtained therefrom detects with high pressure liquid chromatographic analysis, and the yield of Ortho Nitro Benzaldehyde is 24.9%, and the product purity after the purification is 99.5%.
Embodiment 46
Getting 14mg μ-oxygen-double-core four-(ortho-nitrophenyl base) iron-cobalt porphyrin (is R in the general formula (IV)
1=NO
2, R
2=H, M
4=Fe, M
5=Co), 1.37g Ortho Nitro Toluene and 2.5g potassium hydroxide in the autoclave of packing into, add 10ml methyl alcohol, and oxygen pressure is 2.5MPa, and temperature control is 35 ℃ in the water-bath, reaction 18h.Treatment step is with implementing 9, and products obtained therefrom detects with high pressure liquid chromatographic analysis, and the yield of Ortho Nitro Benzaldehyde is 23.1%, and the product purity after the purification is 98.7%.
Claims (6)
1, a kind of bionically catalyzing and oxidizing Ortho Nitro Toluene prepares the method for Ortho Nitro Benzaldehyde, it is characterized in that with the Ortho Nitro Toluene being raw material, select any in the μ-oxygen-dinuclear metalloporphyrin of the monokaryon metalloporphyrin of metal phthalocyanine, general formula (II), (III) structure of general formula (I) structure or general formula (IV) structure for use as catalyzer, in the formula, M
1, M
2, M
3, M
4, M
5Be transition metal atoms, M
1=Fe, Co, Cu, Zn, M
2=Fe, Mn, Co, Cu, Zn, M
3=Fe, Mn, Co, M
4And M
5Can be identical, also can be different, when identical, M
4=M
5=Fe, Mn, Co, not simultaneously, M
4=Fe, M
5=Mn or M
4=Fe, M
5=Co, R can be that carboxyl also can be a hydrogen, R
1, R
2Can be hydrogen, halogen, nitro, hydroxyl, alkoxyl group, dentate X are chlorine, catalyst consumption is 0.2~1.0% of an Ortho Nitro Toluene weight, is solvent with methyl alcohol, in 3.0~6.0mol/L strong basicity methanol solution, feed the oxygen of 0.8~3.0MPa, control reaction temperature is 25~60 ℃, and reaction times 6~48h obtains the Ortho Nitro Benzaldehyde crude product, after adopting ordinary method to separate, purify, obtain the Ortho Nitro Benzaldehyde elaboration.
General formula (I)
General formula (II)
General formula (III)
General formula (IV)
2, bionically catalyzing and oxidizing Ortho Nitro Toluene according to claim 1 prepares the method for Ortho Nitro Benzaldehyde, it is characterized in that preferably having the monokaryon metalloporphyrin of general formula (III) structure or the μ-oxygen-dinuclear metalloporphyrin of general formula (IV) structure is made catalyzer.
3, bionically catalyzing and oxidizing Ortho Nitro Toluene according to claim 1 and 2 prepares the method for Ortho Nitro Benzaldehyde, it is characterized in that described catalyzer is preferably M in the general formula (III) especially
3=Mn or Fe, R
1=NO
2Or Cl, R
2=H, the monokaryon metalloporphyrin of X=Cl; M in the general formula (IV)
4=M
5=Fe or Mn or Co, M
4And M
5Not not simultaneously, M
4=Fe, M
5=Mn, R
1=NO
2Or Cl, R
2μ-oxygen of=H-dinuclear metalloporphyrin.
4, bionically catalyzing and oxidizing Ortho Nitro Toluene according to claim 1 prepares the method for Ortho Nitro Benzaldehyde, it is characterized in that described Ortho Nitro Toluene starting point concentration is 0.6~1.0mol/L.
5, bionically catalyzing and oxidizing Ortho Nitro Toluene according to claim 1 prepares the method for Ortho Nitro Benzaldehyde, it is characterized in that described highly basic is sodium hydroxide or potassium hydroxide.
6, the bionically catalyzing and oxidizing Ortho Nitro Toluene prepares the method for Ortho Nitro Benzaldehyde according to claim 1 or 5, it is characterized in that the preferred 4.0~5.0mol/L of described strong base concentrations.
Priority Applications (1)
| Application Number | Priority Date | Filing Date | Title |
|---|---|---|---|
| CN 200310121478 CN1243717C (en) | 2003-12-18 | 2003-12-18 | Preparation of o-nitrobenzaldehyde by biomimetic catalysis oxidation of o-nitrotoluene with oxygen |
Applications Claiming Priority (1)
| Application Number | Priority Date | Filing Date | Title |
|---|---|---|---|
| CN 200310121478 CN1243717C (en) | 2003-12-18 | 2003-12-18 | Preparation of o-nitrobenzaldehyde by biomimetic catalysis oxidation of o-nitrotoluene with oxygen |
Publications (2)
| Publication Number | Publication Date |
|---|---|
| CN1546457A true CN1546457A (en) | 2004-11-17 |
| CN1243717C CN1243717C (en) | 2006-03-01 |
Family
ID=34338459
Family Applications (1)
| Application Number | Title | Priority Date | Filing Date |
|---|---|---|---|
| CN 200310121478 Expired - Fee Related CN1243717C (en) | 2003-12-18 | 2003-12-18 | Preparation of o-nitrobenzaldehyde by biomimetic catalysis oxidation of o-nitrotoluene with oxygen |
Country Status (1)
| Country | Link |
|---|---|
| CN (1) | CN1243717C (en) |
Cited By (5)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| CN100395228C (en) * | 2006-10-27 | 2008-06-18 | 北京工业大学 | Process for preparing ortho-nitro benzoic acid by bionically catalystic ally oxidizing ortho-nitro toluene with oyxgen |
| CN102070382A (en) * | 2011-01-19 | 2011-05-25 | 山东瀛洋香精香料有限公司 | Method for preparing benzaldehyde or substituted benzaldehyde by catalytically oxidizing methylbenzene or substituted methylbenzene |
| CN104402675A (en) * | 2014-11-20 | 2015-03-11 | 中山大学惠州研究院 | Method for preparing tert butyl alcohol through biomimetic catalysis iso-butane oxidation |
| CN104591990A (en) * | 2014-12-25 | 2015-05-06 | 北京工业大学 | Method for preparing p-hydroxyacetophenone by catalytically oxidizing paraethyl phenol with metalloporphyrin-metal salt composite catalyst |
| CN110907405A (en) * | 2019-11-26 | 2020-03-24 | 桂林理工大学 | Method for determining trace hydrogen peroxide based on tetra-carboxyl nickel phthalocyanine |
-
2003
- 2003-12-18 CN CN 200310121478 patent/CN1243717C/en not_active Expired - Fee Related
Cited By (7)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| CN100395228C (en) * | 2006-10-27 | 2008-06-18 | 北京工业大学 | Process for preparing ortho-nitro benzoic acid by bionically catalystic ally oxidizing ortho-nitro toluene with oyxgen |
| CN102070382A (en) * | 2011-01-19 | 2011-05-25 | 山东瀛洋香精香料有限公司 | Method for preparing benzaldehyde or substituted benzaldehyde by catalytically oxidizing methylbenzene or substituted methylbenzene |
| CN102070382B (en) * | 2011-01-19 | 2014-04-16 | 山东瀛洋香精香料有限公司 | Method for preparing benzaldehyde or substituted benzaldehyde by catalytically oxidizing methylbenzene or substituted methylbenzene |
| CN104402675A (en) * | 2014-11-20 | 2015-03-11 | 中山大学惠州研究院 | Method for preparing tert butyl alcohol through biomimetic catalysis iso-butane oxidation |
| CN104402675B (en) * | 2014-11-20 | 2016-11-30 | 中山大学惠州研究院 | A kind of method that bionic catalysis oxidation of isobutane prepares the tert-butyl alcohol |
| CN104591990A (en) * | 2014-12-25 | 2015-05-06 | 北京工业大学 | Method for preparing p-hydroxyacetophenone by catalytically oxidizing paraethyl phenol with metalloporphyrin-metal salt composite catalyst |
| CN110907405A (en) * | 2019-11-26 | 2020-03-24 | 桂林理工大学 | Method for determining trace hydrogen peroxide based on tetra-carboxyl nickel phthalocyanine |
Also Published As
| Publication number | Publication date |
|---|---|
| CN1243717C (en) | 2006-03-01 |
Similar Documents
| Publication | Publication Date | Title |
|---|---|---|
| CN1931824A (en) | Process and catalyst for preparing unsaturated carboxylate continuously from unsaturated aldehyde | |
| CN1032784A (en) | Produce the method for N-phosphonomethylglycine | |
| CN101037431A (en) | Method for synthesizing cricoid carbonate by addition reaction of carbon dioxide and epoxy compound ring | |
| CN1054838C (en) | Process to prepare amino carboxylic acid salts | |
| CN1103860A (en) | Process for producing highly purified benzendicarboxylic acid isomers | |
| CN1070167C (en) | Method for the preparation of carboxylic acids or corresponding esters in the presence of a soluble iridium and iodide-based catalyst | |
| CN101066926A (en) | Prepn process of 3-trifluoro methyl benzoate | |
| CN1915983A (en) | Method for preparing epoxy compound by oxidating olefin or cycloolefine through bionic catalysis oxygen | |
| CN1243717C (en) | Preparation of o-nitrobenzaldehyde by biomimetic catalysis oxidation of o-nitrotoluene with oxygen | |
| CN1662302A (en) | Metallic copper catalyst for polyfluoroalkylethyl iodide production and process for producing polyfluoroalkylethyl iodide | |
| CN1231449C (en) | Method of preparing adipinic acid using bionic catalytic oxggen to oxidize cyclohexane | |
| CN1138744C (en) | Method for producing optically active chrysanthemic acid | |
| CN1271040C (en) | Preparation of o-nitrobenzaldehyde by biomimetic catalysis oxidation of o-nitrotoluene with oxygen | |
| CN1918094A (en) | Method for producing optically active alcohols or carboxylic acids | |
| CN86107833A (en) | Zinc oxide catalytic agent for synthesizing of acetic acid ethylene | |
| CN1066054A (en) | The method of preparing hexadiacid by hydro-carboxylation of pentenoic acid | |
| CN1672791A (en) | Double active species catalyst and its application | |
| CN1134314A (en) | Solid basic catalyst, process for producing the same and process for producing carbonyl compound derivative using the same | |
| CN1198789C (en) | Process for preparing 4-nitroso-aniline from urea and nitrobenzene | |
| CN101065387A (en) | Composition containing phosphorylcholine and preparing method thereof | |
| CN1724525A (en) | Gamma-butyrolactone derivative and its preparation method | |
| CN1136180C (en) | Preparation of aryl methyl ketone | |
| CN1090618C (en) | Process for production of pyridinecarboxylic acids | |
| CN1231451C (en) | Process to enable recemation of optical rotatary vinyl substituted cyclopropane carboxylic compound | |
| CN1094489C (en) | Process for producing pyrazine compounds |
Legal Events
| Date | Code | Title | Description |
|---|---|---|---|
| C06 | Publication | ||
| PB01 | Publication | ||
| C10 | Entry into substantive examination | ||
| SE01 | Entry into force of request for substantive examination | ||
| C14 | Grant of patent or utility model | ||
| GR01 | Patent grant | ||
| CF01 | Termination of patent right due to non-payment of annual fee | ||
| CF01 | Termination of patent right due to non-payment of annual fee |
Granted publication date: 20060301 Termination date: 20191218 |