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    Narendra Edara
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    This document discusses developing a fast dissolving tablet formulation of valsartan to improve its low bioavailability. Valsartan has low solubility and permeability. Fast dissolving tablets using superdisintegrants can increase the drug dissolution rate and bioavailability. The document investigates the effect of pH and particle size on valsartan solubility and formulates fast dissolving tablets using different ratios of crospovidone and Ac-Di-Sol as superdisintegrants. It evaluates the tablets for physical properties, drug content, disintegration time, in vitro drug release and dissolution profiles in various media. The results showed pH dependent solubility of valsartan and improved dissolution with reduced particle size. Tablets formulated with a 1:1 ratio

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    This document discusses developing a fast dissolving tablet formulation of valsartan to improve its low bioavailability. Valsartan has low solubility and permeability. Fast dissolving tablets using superdisintegrants can increase the drug dissolution rate and bioavailability. The document investigates the effect of pH and particle size on valsartan solubility and formulates fast dissolving tablets using different ratios of crospovidone and Ac-Di-Sol as superdisintegrants. It evaluates the tablets for physical properties, drug content, disintegration time, in vitro drug release and dissolution profiles in various media. The results showed pH dependent solubility of valsartan and improved dissolution with reduced particle size. Tablets formulated with a 1:1 ratio

    Copyright:

    Attribution Non-Commercial (BY-NC)
    Download as PPTX, PDF, TXT or read online from Scribd
    Flag for inappropriate content
    15 views21 pages

    NNNNNN

    Uploaded by

    Narendra Edara
    This document discusses developing a fast dissolving tablet formulation of valsartan to improve its low bioavailability. Valsartan has low solubility and permeability. Fast dissolving tablets using superdisintegrants can increase the drug dissolution rate and bioavailability. The document investigates the effect of pH and particle size on valsartan solubility and formulates fast dissolving tablets using different ratios of crospovidone and Ac-Di-Sol as superdisintegrants. It evaluates the tablets for physical properties, drug content, disintegration time, in vitro drug release and dissolution profiles in various media. The results showed pH dependent solubility of valsartan and improved dissolution with reduced particle size. Tablets formulated with a 1:1 ratio

    Copyright:

    Attribution Non-Commercial (BY-NC)
    Download as PPTX, PDF, TXT or read online from Scribd
    Flag for inappropriate content
    of 21

    W IN1kCDUC1ICN

    W valsarLan ls an anLlhyperLenslve agenL wlLh low solublllLy


    and hlgh permeablllLy
    W 8loavallablllLy of valsarLan ls very low
    W Cne of Lhe way of lncreaslng Lhe dlssoluLlon raLe of poorly
    soluble drug ls by formulaLlng fasL dlssolvlng LableLs
    W lasL dlssolvlng LableLs are prepared by uslng varlous
    superdlslnLegraLlng agenLs whlch helps Lo dlslnLegraLe
    LableL aL fasLer raLe
    W Pence bloavallablllLy of such drugs can be lncreased
    slgnlflcanLly
    C8ILC1IVL
    W @o lmprove Lhe dlssoluLlon raLe of poorly soluble valsarLan by
    uslng superdlslnLegranLs
    W @o sLudy Lhe effecL of pP and parLlcle slze on solublllLy of valsarLan
    ,aLerlals used
    W valsarLan,lcrocrysLalllne celluloseACul
    solCrospovldone
    W the |ngred|ents were coground |n a peste and mortar and then tac and
    magnes|um stearate were added and m|xed for 10 m|nutes
    W1he m|xed bend of drugexc|p|ent was compressed us|ng d|rect compress|on
    W1h|s techn|que can now be app|ed to preparat|on of ID1 because of
    the ava|ab||ty of |mproved exc|p|ents espec|ay superd|s|ntegrants (Lg Lud|press
    Ceactose)and sugar based exc|p|ents Lg Lactosematose
    reparat|on of ID1 of vasartan
    kLICkMUL1ICN S1UDILS
    1abe1 INILULNCL CI n CI SCLVLN1 CN SCLU8ILI1 CI
    VLSk1N
    hys|ca parameters of Vasartan fast ID1 formuated w|th phys|ca m|xture
    of superd|s|ntegrant
    SNC parameter I19 I20 I21
    JL varlaLlon 20 200 20
    2 lrlablllLy() 078 088 079
    3 Pardness(kg/cm2) 33 40 33
    4 urug conLenL() 963 990 994
    3 ulslnLegraLlon
    Llme(mln)
    27 30 34
    W @able2 lnfluence of parLlcle slze on solublllLy
    of valsarLan ln 68 phospaLe buffer
    kLk1ICN CI CCkCCLSSLD
    SULkDISIN1LGkN1S
    W @hey were prepared by solvenL evaporaLlon meLhod
    W Crospovldone and AculSol were Laken ln Lhe raLlo as
    shown ln @able3@hen add 0 ml of eLhanol Lo above
    mlxLures
    W @he weL coherenL mass was granulaLed Lhrough # 60
    mesh sleve
    W @he weL granules were drled ln a hoL alr oven aL 60 C
    for 20 mlnuLes @he drled
    W @he granules were slfLed Lhrough # 60 mesh sleve and
    sLored ln alrLlghL conLalner Llll furLher use
    W ComposlLlon of valsarLan lu@ formulaLed
    wlLh physlcal mlxer of superdlslnLegranLs
    W APlnvlLro dlssoluLlon raLe of lu@ of
    valsarLan
    W @A8LL3 lnvlLro dlssoluLlon proflle of
    valsarLan lu@ formulaLed wlLh physlcal
    mlxLure of superdlslnLegranLs
    W hyslcal parameLers of valsarLan lu@
    formulaLed wlLh physlcal mlxLure of
    superdlslnLegranLs
    lnvlLro dlssoluLlon sLudles
    W lL ls performed uslng uS @u@08L Lype 2 dlssoluLlon LesL
    W apparaLus
    W varlous dlssoluLlon medla wlLh dlfferenL , was Laken as
    per@A8LL4
    W @he dlssoluLlon medlum was malnLalned aL a LemperaLure of 3703
    'C and samples are wlLhdrawn aL an lnLerval of every 3 mln
    W @he volumes of Lhe wlLhdrawn samples are replaced by fresh
    dlssoluLlon medlum ln order Lo keep Lhe volume of Lhe dlssoluLlon
    medlum consLanL
    W @he wlLhdrawn samples were fllLered and absorbance was
    measured aL absorpLlon maxlma of 230 nm uslng uvvlslble
    specLrophoLomeLer
    W @A8LL3lnvlLro dlssoluLlon proflles of
    valsarLan LableLs ln four dlssoluLlon medlums
    aL 00 rpm
    W AP2 lnvlLro dlssoluLlon raLe of valsarLan
    LableLs ln four dlssoluLlon medlums aL 00
    rpm
    W
    d|ssout|on prof|es of Vasartan marketed tabets |n four d|ssout|on med|ums at 100
    rpm
    W Concluslon
    W ulssoluLlon raLe was found Lo be lnfluenced by
    naLure of comblnaLlon of superdlslnLegranLs
    employed
    esulL
    W @ableLs formulaLed wlLh coprocessed
    crospovldoneand ACulsol ln raLlo ls besL Lo
    formulaLe fasL dlssolvlng LableLs
    W valsarLan showed pP dependenL solublllLy
    W P 68 phosphaLe buffer aL 00 rpm was Lhe besL
    dlssoluLlon medlum for valsarLan LableLs
    W @he solublllLy can be lmproved by reduclng Lhe
    parLlcle slze
    0
    20
    40
    60
    80
    00
    20
    0 3 0 3 20 23 30
    0 n PCl A 0 n PCl 8 43 ACL@A@L 8ullL A
    43 ACL@A@L 8ullL 8 68 PCSPA@L 8ullL A 68 PCSPA@L 8ullL 8
    JA@L A JA@L 8


    D
    k
    U
    G

    k
    L
    L
    L

    S
    L
    1IML (m|n)
    d|ssout|on data of Vasartan fast d|ssov|ng tabets formuated
    w|th phys|ca m|xture of superd|s|ntegrants (Crospov|done and cD|
    So)(11 rat|o)
    I|rst order pots of Vasartan fast d|ssov|ng tabets formuated w|th phys|ca
    m|xture of superd|s|ntegrants (Crospov|done and cD|So 11 rat|o
    0
    03

    3
    2
    23
    0 3 0 3 20 23 30
    l9 l20 l2
    L
    C
    G


    C
    I

    D
    k
    U
    G

    k
    L
    L
    L

    S
    L
    1IML (m|n)
    Concluslon
    W valsarLan showed pP dependenL solublllLy
    W @he solublllLy was found Lo be lnfluenced by
    Lhe parLlcle slze of pure drug @he solublllLy
    can be lmproved by reduclng Lhe parLlcle slze
    W ulssoluLlon raLe was found Lo be lnfluenced by
    naLure of comblnaLlon of superdlslnLegranLs
    employed
    W esulL
    P 68 phosphaLe buffer aL 00 rpm was Lhe
    besL dlssoluLlon medlum for valsarLan LableLs
    2 @ableLs formulaLed wlLh coprocessed
    crospovldone ACulsol ln raLlo ls besL Lo
    formulaLe fasL dlssolvlng LableLs
    eference
    W ueb[lL 8howmlk 8!ayakar and kSampaLh kumar ueslgn and
    CharacLerlsaLlon of lasL ulssolvlng @ableL of @elmlsarLan"
    lIlkk 2009 () 3
    W C !aln and S naruka lormulaLlon and evaluaLlon of fasL
    dlssolvlng LableLs of valsarLan" lotetootloool Iootool of
    lbotmocy ooJ lbotmoceotlcol 5cleoces vol lssue !uly
    Sep 2009 29227

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