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    5.sunil Article

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    Baru Chandrasekhar Rao
    Indo American Journal of Pharmaceutical Sciences (IAJPS) is an international, peer-reviewed, multidisciplinary monthly journal, devoted to pharmaceutical sciences. The aim of IAJPS is to increase the impact of pharmaceutical research both in academia and industry, with strong emphasis on quality and originality. IAJPS publishes Original Research Articles, Short Communications, Review Articles in all areas of pharmaceutical sciences from the discovery of a drug up to clinical evaluation. Topics covered are: Pharmaceutics, Bio Pharmaceutics and Pharmacokinetics, Novel Drug Delivery System, Pharmaceutical chemistry including medicinal and analytical chemistry; Pharmacognosy including herbal products standardization and Phytochemistry; Pharmacology, Bio Technology: Allied sciences including drug regulatory affairs, Pharmaceutical Marketing, Pharmaceutical Microbiology, Pharmaceutical biochemistry, Pharmaceutical Education and Hospital Pharmacy

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    5.sunil Article

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    Baru Chandrasekhar Rao
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    Indo American Journal of Pharmaceutical Sciences (IAJPS) is an international, peer-reviewed, multidisciplinary monthly journal, devoted to pharmaceutical sciences. The aim of IAJPS is to increase the impact of pharmaceutical research both in academia and industry, with strong emphasis on quality and originality. IAJPS publishes Original Research Articles, Short Communications, Review Articles in all areas of pharmaceutical sciences from the discovery of a drug up to clinical evaluation. Topics covered are: Pharmaceutics, Bio Pharmaceutics and Pharmacokinetics, Novel Drug Delivery System, Pharmaceutical chemistry including medicinal and analytical chemistry; Pharmacognosy including herbal products standardization and Phytochemistry; Pharmacology, Bio Technology: Allied sciences including drug regulatory affairs, Pharmaceutical Marketing, Pharmaceutical Microbiology, Pharmaceutical biochemistry, Pharmaceutical Education and Hospital Pharmacy

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    Indo American Journal of Pharmaceutical Sciences (IAJPS) is an international, peer-reviewed, multidisciplinary monthly journal, devoted to pharmaceutical sciences. The aim of IAJPS is to increase the impact of pharmaceutical research both in academia and industry, with strong emphasis on quality and originality. IAJPS publishes Original Research Articles, Short Communications, Review Articles in all areas of pharmaceutical sciences from the discovery of a drug up to clinical evaluation. Topics covered are: Pharmaceutics, Bio Pharmaceutics and Pharmacokinetics, Novel Drug Delivery System, Pharmaceutical chemistry including medicinal and analytical chemistry; Pharmacognosy including herbal products standardization and Phytochemistry; Pharmacology, Bio Technology: Allied sciences including drug regulatory affairs, Pharmaceutical Marketing, Pharmaceutical Microbiology, Pharmaceutical biochemistry, Pharmaceutical Education and Hospital Pharmacy

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    © All Rights Reserved
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    55 views6 pages

    5.sunil Article

    Uploaded by

    Baru Chandrasekhar Rao
    Indo American Journal of Pharmaceutical Sciences (IAJPS) is an international, peer-reviewed, multidisciplinary monthly journal, devoted to pharmaceutical sciences. The aim of IAJPS is to increase the impact of pharmaceutical research both in academia and industry, with strong emphasis on quality and originality. IAJPS publishes Original Research Articles, Short Communications, Review Articles in all areas of pharmaceutical sciences from the discovery of a drug up to clinical evaluation. Topics covered are: Pharmaceutics, Bio Pharmaceutics and Pharmacokinetics, Novel Drug Delivery System, Pharmaceutical chemistry including medicinal and analytical chemistry; Pharmacognosy including herbal products standardization and Phytochemistry; Pharmacology, Bio Technology: Allied sciences including drug regulatory affairs, Pharmaceutical Marketing, Pharmaceutical Microbiology, Pharmaceutical biochemistry, Pharmaceutical Education and Hospital Pharmacy

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    IAJPS 2016, 3 (7), 728-733

    S.S.Thakare and S.P.Kakad

    CODEN (USA): IAJPBB

    ISSN 2349-7750

    ISSN: 2349-7750

    INDO AMERICAN JOURNAL OF

    PHARMACEUTICAL SCIENCES

    Available online at: http://www.iajps.com

    Research Article

    SELECTIVE SYNTHESIS OF 2-CHLORO-N-ALKYL-7NITROQUINAZOLIN-4-AMINES DERIVATIVES FROM 2, 4


    DICHLORO 7 NITRO QUINAZOLINE BY CONTROL REACTION
    CONDITIONS
    Dr. S. S. Thakare*, Mr. S. P. Kakad
    Post graduate Teaching Department of Chemistry, Shri Shivaji Science College, Amravati,

    Maharashtra 444603.
    Graphical abstract:
    Cl
    N
    N

    O2N

    NH

    Cl

    R-NH2
    TEA, THF,
    0C-rt, 3h

    N
    O2N

    Cl

    Abstract:
    A method is presented for the synthesis of selective derivatization of quinazoline by controlling the temperature and
    solvent concentration, 2,4-dichloro-7-nitroquinazoline reacted with different amines to form the selective 2-chloro-Nalkyl-7-nitroquinazolin-4-amines by chloro amine reaction, The products have been characterized through the usual
    chemical transformations, IR, NMR and mass spectral analyses.
    Keywords: Quinazoline derivative, 5, 6 dichloride 7-nitro quinazoline, chloro amine coupling, dihydroxy compound.

    Corresponding author:
    Dr. S. S. Thakare,
    Post graduate Teaching Department of Chemistry,
    Shri Shivaji Science College, Amravati, Maharashtra 444603.
    Email id: skakad1@gmail.com

    QR code

    Please cite this article in press as S.S.Thakare and S.P.Kakad, Selective Synthesis of 2-Chloro-N-Alkyl-7Nitroquinazolin-4-Amines Derivatives from 2, 4 Dichloro 7 Nitro Quinazoline By Control Reaction Conditions,
    Indo Am. J. P. Sci, 2016; 3(7).

    www.iajps.com

    Page 728

    IAJPS 2016, 3 (7), 728-733

    S.S.Thakare and S.P.Kakad

    INTRODUCTION:
    Quinazoline represent a fundamental and abundant
    class of nitrogen containing heterocyclic,
    quinazoline derivatives are of special importance
    because of their versatile biological and
    pharmacological activities and the researcher have
    all ready determined many therapeutic activity of
    quinazoline including antitumor, antiplsmodial [15] , anti microbial [6-7], anti cancer [8-9],
    antitubecular activity [10]. In recent journal have
    reported the quinazoline has anti-inflammatory
    [11] activity and many compounds that contain the
    quinazoline motif possess a wide range of
    remarkable biological and medicinal activities as
    anti hypertensive [12], some article has reported
    quinazoline has anti hypertension and antioxidation activity [13], recently in journal has
    reported ant malarial activity of quinazoline
    derivatives [16] and in next journal has reported the
    quinazoline showed anti fungal and anti diabetes
    activity [14-15] . Quinazoline derivatives showed
    the different biological activity and also potential
    application in field of biology, pesticide and
    medicine quinazoline is a heterocyclic compound
    with unique place in field of medicinal chemistry
    [16-18]. Medicinal chemistry is concerned with
    discovery, development synthesis in laboratory and
    identifies action of physical and chemical methods.
    Here most of activity of directed to new natural or
    synthetic organic compounds. Inorganic

    ISSN 2349-7750

    compounds continue to be important in therapy that


    is trace element in nuatritional therapy, antacids
    and radiopharmaceutical.
    Quinazoline (1, 3-diazanaphthalene) was prepared
    by garbrial in 1903 although the first derivative was
    synthesized by griess. The name was proposed by
    widdege, other names such as phenmiazine, benzo1, 3-diazine and 5,6- benzopyrimidine has
    occasionally been used .
    MATERIALS AND METHODS:
    4-nitro antharnilic acid ordered from the
    Spectrochem Pvt. ltd, POCl3 also from spectrochem
    inda.pvt ltd., all amine purchased from different
    companies, spectrochem, Avra chemical pvt. ltd.
    chemical pvt.Ltd. SD fine chemicals, all melting
    points are uncorrected and were measured using an
    electro- thermal apparatus. 1H NMR spectra were
    recorded on Brucker Avance II 400 NMR
    spectrometer using DMSO-d6 and CDCl3 as solvent
    and tetramethylsilane as internal standard and
    chemical shifts being reported in parts per million
    () relative to TMS. Mass spectra were obtained
    using Waters Micromass Q-Tof Micro instrument at
    70 eV. Analytical thin-layer chromatography (TLC)
    was performed on Silica Gel 60F254 (Merck,
    Germany). The spots were visualized by exposure
    to UV light and I2vapors.

    Scheme:

    O
    OH
    NH2

    O2 N

    OH

    Cl
    POCl3,TEA

    Urea,190C
    5h

    O2 N

    OH
    110 C,12 h

    O2 N

    Cl

    NH 2

    SM
    R
    R-NH2
    4a-m
    DIPEA, THF,
    rt, 3h
    Where,
    3a : Cyclopropyl amine
    3b : t-Butyl amine
    3c : p-Anisidine
    3d : 2-Amino thizole
    3e : 2-Amino pyrazine,

    www.iajps.com

    O2 N

    Cl

    3f : Ethyl amine
    3g : Morpholine
    3h : Piperidine 3i
    : p-Toludine 3j :
    Aniline

    3k : m-Toludine
    3l : Imidazole
    3m : Methyl amine 3n
    : n Propyl amine 3o :
    4 Nitro aniline
    3p : 4-Amino pyridine

    Page 729

    IAJPS 2016, 3 (7), 728-733

    S.S.Thakare and S.P.Kakad

    Part A: Synthesis of scaffold up to Dichloro


    quinazoline
    First two steps we consider as scaffold synthesis,
    in the first step as scheme started from 4 nitro
    anthranilic acid and urea to form 7nitroquinazoline-2,4-diol in the in the second step
    2,4 7 dichloro-7 nitro-quinazoline has synthesized
    by using POCl3, scaffold synthesis played
    important role for synthesis of whole scheme. We
    have synthesized the 2,4-dichloroquinazoline as
    per procedure reported in some journals[20-23]
    Step-1: Synthesis of 7-nitroquinazoline-2,4-diol
    4-nitro anthranilc acid (10 g, 1 eq, 54.94 mmol)
    was mixed with urea (9.89 g , 3 eq, 164.8 mmol) in
    nitrogen atmosphere, mixed material was heated at
    120 C, reaction mass become dark brown liquid,
    stirred the reaction mass for 30 min at 120. Further
    heated the reaction mass at 180C for 4-5 hrs,
    reaction mass became brown colored solid,
    Progress of reaction monitored by TLC, it showed
    complete conversion. Cooled the reaction mixture
    up to room temperature, the methanol was added
    into the reaction mixture and heated the reaction
    mixture 50-55 C, maintained the reaction mixture
    3 hrs at 50-55C, cooled it to 30-35C, filtered the
    reaction mass at 30-35C, washed the solid by
    methanol. Suck dried the solid under vacuum to
    afforded light yellow colored solid (10.2 g) yield
    .90.26 %, same material used for next step.
    Properties of compound -1: Melting Point: 214 C
    Mass: (M-1): 206
    Step-2:
    synthesis of 2, 4-dichloro-7nitroquinazoline
    Synthesis of 2,4 dichloro 7 nitro quinazoline
    synthesized from 2, 4 hydroxy 7 nitro quinazoline (5
    g, 1 eq, 24.15 mmol ) charged into RBF under
    nitrogen atm. TEA (10.16 mL, 3 eq, 72.45 mmol )
    was added into it at room temperature POCl3 (
    22.95 g , 5 eq, 120.77 mmol) added to it portion
    wise. (Some slight exotherm observed if starting
    compound contains moisture) stirred the reaction
    mixture for 20 min at 30 C. Cooled the reaction
    mixture at 0 to 10 C. Charged triethyl amine via
    addition funnel drop wise. Heated the reaction
    mixture up to 60C and after that up to 110C.
    Maintained the reaction mixture for 7-8 hrs at 110C
    (Oil temp) progress of reaction monitored by TLC,
    Reaction mixture becomes dark brown colour turbid
    solution, TLC showed complete conversion of
    starting compound. Cooled the reaction mass up to
    rt. Pored the reaction mixture into wet ice slowly
    and portion wise sudden exotherm observed.
    (Temperature should not be exceed than 30 C)
    filtered the reaction mixture under vacuum.
    Unloaded the solid from Buckner funnel, transferred

    www.iajps.com

    ISSN 2349-7750

    the brown solid to next RBF added the ethyl acetate


    into it. Stirred the turbid material for 30 min. filtered
    the solid and again stirred with ethyl acetate until
    TLC showing dichloro compound. Total organic
    was collected washed with saturated bicarbonate
    solution, distilled out the organic layer. Crude
    compound was purified by column chromatography
    by using 100-200 mish size silica and 01 ethyl
    acetate in petroleum ether. Afforded 7 g of pure
    material same material used for next step.
    Properties of compound -2: Light yellow colour.
    Melting Point: 131C
    Mass (M+1): 244.02
    Step-3:
    synthesis
    of
    2-chloro-N-alkyl-7nitroquinazolin-4-amine
    7nitroquinazoline-2, 4-dichloro quinazoline
    (3 g, 1 eq, 12.29 mmol) dissolved in THF (15 vol),
    stirred the reaction mass for 30 min at 25 to 30C,
    TEA ( 5.17 mL, 3eq, 36.68 mmol ) was added into it
    at room temperature, Prepared cyclopropyl amine
    solution (0.56 mL,0.8 eq, 9.83 mmol ) in THF (10
    Vol) at 0C, stirred the reaction mass at room
    temperature for 1-3 hrs, Reaction of some
    derivatives completed with 2 hrs, but with others
    reaction completed within 3 hrs. TLC showed the
    complete consumption of starting compound,
    charged ethyl acetate (5 vol) to reaction mass
    prepared 1 M HCL (5 vol), solution to reaction
    mass, confirmed the pH, if required pH should be
    acidic, washed the reaction mass by 1 M HCL (2
    vol), total aqueous layer was collected washed the
    by ethyl acetate layer, combined organic layers and
    washed with brine solution. distilled out the organic
    layer under vacuum and finally poured the crude
    compound was purified by column chromatography
    using 100-200 silica and 20 ethyl acetate in
    petroleum ether used as mobile phase to afforded
    pure product, but few compounds have purified by
    triturating with organic solvent and remaining by
    recrystallization afforded pure 2-chloro-N-alkyl-7nitroquinolin-4-amines . The entire target compound
    was confirmed by 1H NMR, LCMS, IR. TLC: (TLC
    solvent system 20% ethyl acetate in petroleum ether)
    TLC Stain: Ninhydrin
    RESULT AND DISCUSSION:
    In the result and discussion, while synthesizing 16
    derivatives it is observed that experiment in the
    higher temperature the formation of disubstituted
    derivatives in more percentage and reaction in
    minimum dilution of solvent also helped to form
    disubstituted product. Compound 3a to 3c scheme
    went smoothly but the reaction on compound 3d and
    3e was critical, reaction taken longer time and
    product were polar compared to other. Reaction
    with Aliphatic primary amines was preceded fast

    Page 730

    IAJPS 2016, 3 (7), 728-733

    S.S.Thakare and S.P.Kakad

    compared to aromatic amines which has taken


    longer time. All the compounds have repsentative
    colour.
    Compound 3p has unique quality of material and

    ISSN 2349-7750

    very polar in nature. Compound 3h and 3m afford


    less yield and critical to isolate the pure material,
    colour of compound little dark than other
    derivatives.

    List of Compounds:
    Sr. No

    1.

    Amines

    Comp 3

    Time

    Yield (%)

    Colour

    1
    2
    3
    4

    Cyclopropyl amine
    tert-Butyl amine
    p-Anisidine
    2 Amino thiozole

    C3H7N
    C4H11N
    C7H9NO
    C3H4N2S

    3a
    3b
    3c
    3d

    2h
    3h
    3h
    3h

    87
    91
    88
    90

    Light yellow
    Light yellow
    Light brown
    Dark brown

    5
    6
    7
    8
    9
    10
    11
    12
    13

    2 Amino pyrazine
    Ethyl amine
    Morpholine
    Piperidine
    p-Toludine
    Aniline
    m- Toludine
    1H-Imidazole
    methyl amine

    C4H5N3
    C2H7N
    C4H9NO
    C4H10N2
    C7H9N
    C6H7N
    C7H9N
    C3H4N2
    CH5N

    3e
    3f
    3g
    3h
    3i
    3j
    3k
    3l
    3m

    2h
    2h
    3h
    2.h
    3h
    3h
    2.5 h
    3h
    2.5 h

    91
    95
    85
    98
    87
    91
    91
    82
    85

    Dark brown
    Yellow
    Dark yellow
    Light brown
    Yellow
    Light yellow
    Yellow
    Light brown
    Yellow

    14
    15
    16

    n-propyl amine
    4-niroaniline
    4-amino pyridine

    C3H9N
    C6H6N2O2
    C5H6N2

    3n
    3o
    3p

    3h
    3h
    2h

    84
    90
    85

    Yellow
    Dark yellow
    Light brown

    N-tert-butyl-2-chloro-7-nitroquinazolin-4-amine: (compound 3a)

    o 1
    Yellow solid, mp 155-158 C. H NMR ppm (DMSO): 8.91 (s, 1H ) 8.54-8.50 (dd, 1H ), 8.06- 8.08 (d, 1H),
    -1
    4.10 (exchangeable, 1H ), 1.10 (s, 9H), I R (cm ) : 3414, 3196, 3087, 1538, 1345, 1243, 1046, 894, 820,
    ,
    778 MS (m/z), 281.06 (M+1) 283.06(M+3) Anal.Calcd.for
    C12H13ClN4O2: C 64.28, H 4.79 N, 16.66; O, 14.27

    2.

    2-chloro-7-nitro-N-p-tolylquinazolin-4-amine :(compound 3i)

    o 1
    Dark yellow solid, mp 163-166 C. H NMR (DMSO): 8.95 (s, 1H ) 8.57-8.54 (dd, 1H ), 8.10-8.08 (d, 1H)
    -1
    6.78-6.76 ( d,1H, Ar-H), 6.34-6.36 ( d,1H, Ar-H), 4.10 (exchangeable, 1H), 2.20 (s, 3H), I R (cm ) : 3410,
    ,
    3194, 3080, 1542, 1348, 3840, 1310, 1048, 896, 824, 782 MS (m/z), 281.06 (M+1) 283.06(M+3)

    3.

    2-chloro-7-nitro-N-phenylquinazolin-4-amine : (compound 3j)

    o 1
    Dark yellow solid, mp 168-171 C. H NMR ppm (DMSO): 8.97 (s, 1H ) 8.62-8.58 (dd, 1H), 8.14-8.12 (d,
    -1
    1H) 7.02-6.98 ( d, 1H, Ar-H), 6.62-6.58 (m,1H), 6.44-6.42 (d,1H), 4.10(exchangeable, 1H), I R (cm ) : 3422,
    3200, 3060,3038, 1532, 1346, 1310, 1220, 1042, 824,
    ,
    782 MS (m/z), 301.04 (M+1), 303.04 (M+3),

    www.iajps.com

    Page 731

    IAJPS 2016, 3 (7), 728-733

    S.S.Thakare and S.P.Kakad

    CONCLUSION:
    In conclusion, we would like to emphasize that
    synthesized 16 quinazoline derivatives selectively
    by control reaction condition, up to 1 to 5%
    disubstituted compounds also formed with desire
    product, it is concluded that disubstituted
    compound formed in high reaction temperature and
    low dilution, on the basis of bond dissociation
    energy and reactivity of pyrimidine desire target
    compounds synthesized after three steps, synthesis
    on basis of wield range biological activated of
    quinazoline derivatives in pharmaceutical sciences,
    our library synthesis of above sixteen derivatives
    could be help to synthesis biological active
    quinazoline derivatives and upcoming research on
    quinazoline, all the above derivatives afforded in
    good percentage of yield . Compound 3d and 3 e
    were tough to synthesis and afforded low yield,
    then compound 3c, 3f, 3 k formed in clean on TLC
    with better yield compare to other and our
    quinazoline derivatives synthesis could help the
    design the new quinazoline drug in drug discovery.
    ACKNOWLEDGEMENT:
    Author would like to thanks to Principle of Shri
    Shivaji Sciences College of Amravati to providing
    needful facility and freedom to execute experiment
    in the laboratory, no any financially support for this
    study.
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    ISSN 2349-7750

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