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"Vaksinasi merupakan upaya kesehatan preventif terhadap penularan penyakit infeksi, terutama oleh bakteri dan virus. Vaksin hepatitis B yang tersedia di pasar berbentuk suspensi cair yang sensitif terhadap panas. Penelitian dilakukan untuk menghasilkan formula vaksin hepatitis B yang dapat dikelola di luar sistem rantai dingin. Optimisasi pada alat pengering menunjukkan bahwa formula vaksin cair dapat dikeringkan dan dimonitor untuk menghasilkan serbuk vaksin yang berkualitas. Teknik pengeringan yang digunakan meliputi : spray drying, freeze drying dan vacuum drying. Formula vaksin yang disiapkan sebanyak 6 sampel dengan kode A sampai F yang merefleksikan komposisi bahan pengisi dan teknik pengeringan. Serbuk vaksin dikarakterisasi secara fisik, kimia dan potensi antigenik serta dilakukan uji stabilitas dipercepat.Hasil penelitian menunjukkan bahwa teknik pengeringan berpengaruh terhadap penurunan pH dan potensi antigenik vaksin. Kombinasi trehalosa dan mannitol tidak memberikan perbedaan yang signifikan terhadap pH dan potensi relatif vaksin kering. Vaksin yang dikeringkan secara freeze drying dengan komposisi trehalosa: mannitol 7:3 menunjukkan potensi relatif secara in vitro sebesar 97,78 dan in vivo 35,6 serta berpotensi untuk dikelola di luar sistem rantai dingin.

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Vaccination is a preventive health measure against the transmission of infectious diseases, especially by bacteria and viruses. Hepatitis B vaccines are available in the market in the form of liquid suspensions that is heat sensitive. The study was conducted to produce the hepatitis B vaccine formula which can be managed out of the cold chain system. Optimization of the drying instrument indicates that liquid vaccine formula can be dried and monitored to produce quality vaccines powder. Drying techniques used include spray drying, freeze drying and vacuum drying. Vaccine formulas were prepared as much as 6 samples with codes A through F, which reflects the composition of fillers and drying techniques. The powder vaccine was characterized by physical, chemical and antigenic potential as well as an accelerated stability test.

The results showed that the drying technique affecting the decrease of pH and the potential of antigenic vaccine. The combination of trehalose and mannitol did not provide a significant difference to the pH and the relative potency of dried vaccine. The vaccine which was dried by freeze drying with the composition of trehalose mannitol 7 3 showed the relative potency in vitro at 97,78 and in vivo at 35,6 and has an opportunity to be managed out of the cold chain system."

"Plastik merupakan bahan yang banyak digunakan dalam peralatan keseharaian. Penambahan zat tertentu pada alat berbahan plastik ini diketahui dapat menambah kualitas, yaitu lebih elastis, kuat dan tahan lama. Salah satu bahan aditif yang biasa digunakan yaitu ftalat. Senyawa ftalat dapat berpotensi menghasilkan terjadinya DNA adduct. Penelitian ini mempelajari mengenai pembentukan 8-OHdG akibat paparan senyawa ftalat dan logam Cu (II) secara in vitro dan in vivo pada tikus (Rattus novergicus). Pembentukan 8-OHdG dianalisa secara in vitro dengan menggunakan HPLC, dengan variasi pH, waktu inkubasi dan perbandingan konsentrasi. Sedangkan secara in vivo pada tikus, sampel darah dianalisa menggunakan ELISA Kit dan sampel urin menggunakan instrumen LC-MS/MS. Secara umum, konsentrasi 8-OHdG paling besar pada sampel 2-dG diinkubasi dengan kombinasi larutan H₂O₂, ftalat, dan Cu (II). Pada studi in vitro dengan variasi pH menunjukkan konsentrasi 8-OHdG yang lebih tinggi pada pH 7,4; pada variasi waktu inkubasi lebih besar kosentrasi 8-OHdG pada 32 jam; dan pada variasi konsentrasi lebih besar pada perbandingan 1:20. Hasil studi in vivo menggunakan ELISA Kit, konsentrasi 8-OHdG yang terbentuk menunjukkan nilai paling besar pada sampel darah kelompok tikus terpapar ftalat kombinasi Cu (II) yaitu 5,26 ppb; kelompok tikus terpapar ftalat sebesar 4,29 ppb; dan kelompok tikus kontrol (tanpa paparan) sebesar 2,58 ppb. Sedangkan uji in vivo menggunakan LC-MS/MS pada sampel urin tikus juga menunjukkan konsentrasi 8-OHdG paling besar pada tikus kelompok ftalat kombinasi Cu (II) sebesar 174,1 ppb; dan tikus kelompok ftalat sebesar 156,5 ppb.

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Plastic is a material that is widely used in everyday appliances. The addition of certain substances to plastic tools is known to add quality, namely more elastic, strong and durable. One of the additives commonly used is phthalate. Phthalate compounds can potentially produce DNA adducts. This research studies the formation of 8-OHdG due to exposure to phthalate compounds and Cu (II) metal in vitro and in vivo in rats (Rattus novergicus). The formation of 8-OHdG was analyzed in vitro using HPLC, with variations in pH, incubation time and concentration ratio. While in vivo in rats, blood samples were analyzed using ELISA Kit and urine samples using LC-MS/MS instrument. In general, the concentration of 8-OHdG was greatest in 2-dG samples incubated with a combination of H2O2, phthalate, and Cu (II) solutions. In vitro studies with variations in pH showed higher concentrations of 8-OHdG at pH 7.4; at variations in incubation time the concentration of 8-OHdG was greater at 32 hours; and at variations in concentration greater at a ratio of 1:20. The results of the In vivo study using ELISA Kit, the concentration of 8-OHdG formed showed the greatest value in the blood samples of the rat group exposed to phthalate combined with Cu (II), which was 5.26 ppb; the rat group exposed to phthalate was 4.29 ppb; and the control rat group (without exposure) was 2.58 ppb. While the In vivo test using LC-MS/MS on rat urine samples also showed the highest concentration of 8-OHdG in rats of the Cu (II) phthalate combination group at 174.1 ppb; and rats of the phthalate group at 156.5 ppb."

"Peningkatan DNA adduct yaitu 8-OHdG dipengaruhi oleh adanya xenobiotik yang bersifat toksik dan karsinogenik. Xenobiotik yang digunakan pada penelitian ini adalah paraquat diklorida sebagaimana diketahui paraquat diklorida merupakan pestisida golongan II berdasarkan WHO yang memikili efek berbahaya karena dapat menyebabkan mutasi gen sehingga berdampak karsinogenik. Penambahan ion logam Cu(II) dan Ni(II) sebagai media yang dapat berekasi dengan hidrogen peroksida untuk mengahasilkan reaksi Fenton. Rekasi fenton akan menghasilkan hidroksil radikal yang dapat menyebabkan peningkatan stress oksidatif sehingga menghasilkan rekatif oksigen spesies (ROS) yang berakibat pada mutasi DNA.Pada penelitian ini baik secara in vitro maupun in vivo diperoleh hasil bahwa dengan penambahan dua ion logam, Cu(II) dan Ni(II), menghasilkan efek yang supresif, artinya nilai konsentrasi 8-OHdG yang diperoleh lebih kecil dibandingkan dengan nilai masing-masing logam. Hal itu disebabkan ion logam Ni(II) akan menekan oksidasi DNA sehingga oksidasi DNA dengan ion logam Cu(II) akan terganggu. 8-OHdG terbanyak diperoleh dengan pencampuran paraquat diklorida dan ion logam Cu(II). Kajian in viro ini menggunakan kondisi inkubasi pada suhu 370C mewakili kondisi tubuh dan pH 7,4 serta 8,4 dengan waktu inkubasi 24 jam dan 6 jam. Diperoleh untuk kadar 8-OHdG dari ion logam Cu(II) dan paraquat diklorida sebesar 101,48 ppb dan 134,60 ppb. Sedangkan nilai kadar urin dan serum dari proses in vivo hari 14 dan 28 adalah 6,76 ppb& 3,48 ppb dan 1,22 ppb dan 0,76 ppb.

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Increased DNA adduct, which is 8-OHdG is influenced by the presence of xenobiotics which are toxic and carcinogenic. Xenobiotics used in this study are paraquat dichloride, known as paraquat dichloride, a group II pesticide based on WHO which has a dangerous effect because it can cause gene mutations, so it has a carcinogenic impact. Adding Cu(II) and Ni(II) metal ions as a medium can reject hydrogen peroxide to produce Fenton reactions. Fenton's reaction will produce radical hydroxyl, which can cause an increase in oxidative stress to have oxygen species (ROS), resulting in DNA mutations.

In this study, both in vitro and in vivo obtained the result that the addition of two metals, Cu(II) and Ni(II) ions, produced a suppressive effect, meaning that the 8-OHdG concentration value obtained was smaller than the respective values metal. That is because Ni(II) metal ions will suppress DNA oxidation, so DNA oxidation with Cu(II) metal will be disrupted. 8-OHdG is obtained by mixing paraquat dichloride and Cu(II). In vitro study uses incubation conditions at 370C, representing the condition of the body and pH of 7.4 and 8.4 with an incubation time of 24 hours and 6 hours. They obtained 8-OHdG levels of Cu(II) metal ions and paraquat dichloride of 101.48 ppb and 134.60 ppb. While the concentration of urine and serum from in Vivo process days 14 and 28 is 6.76 ppb & 3.48 ppb and 1.22 ppb and 0.76 ppb."

"Latar Belakang: Infeksi virus dengue (DENV) masih endemis di Indonesia dan di banyak negara tropis. Hingga saat ini belum ada antivirus terhadap DENV. Penelitian ini bertujuan untuk mendapatkan antivirus dari tanaman Cassia alata Linn (CA) terhadap DENV-2 secara in vitro, in vivo, dan in silico.Metode: Penelitian ini dilakukan dilakukan di Laboratorium LIPI dan Departemen Mikrobiologi FKUI, 2017-2019. Penelitian in vitro menggunakan DENV serotipe 2 strain New Guinea C (NGC) dan sel Huh 7it-1. DENV diberi perlakuan ekstrak CA dan fraksi dan senyawa murni hasil isolasi dengan bebagai dan konsentrasi untuk menentukan nilai IC₅₀ dan CC₅₀. Penentuan nilai IC₅₀ dan CC₅₀ melalui uji fokus dan MTT secara berurutan. Selanjutnya dilakukan percobaan untuk menentukan mekanisme penghambatan pada tahapan reseptor, pre, post dan pre/post infeksi dari ektrak CA dan fraksinya. Uji efikasi ekstrak CA in vivo dilakukan pada model mencit Balb/c dengan melakukan pengukuran titer virus dengue, jumlah trombosit, leukosit, IL-6 dan IL-10 yang dilanjutkan dengan uji  toksisitas akut  ekstrak CA.  Dilakukan juga uji in silico untuk mengetahui interaksi antara senyawa dengan  protein DENVmenggunakan software Autodock 1.5.6.Hasil: Uji in vitro menunjukkan nilai IC₅₀ ekstrak CA, fraksi heksan, etil asetat, butanol, dan air berturut-turut adalah 0,026; 0,004; 0,0013; 4,6; dan 2,5 mg/ml dengan nilai CC₅₀ berturut-turut adalah 208,9; 47,46; 57,2; 753,8; 311,33 mg/ml. Hasil uji mekanisme pada dosis 10 mg/ml, ekstrak CA, fraksi heksan dan etil asetat menunjukkan hambatan pada tahapan reseptor, pre, post dan pre/post infeksi yang lebih baik dibandingkan fraksi butanol dan etil asetat. Ekstrak CA dapat menghambat keempat mekanisme di atas dengan nilai >95%. Fraksi heksan dan etil asetat menghambat 100% pada post dan pre/post infeksi. Hasil uji in vivo dengan pemberian ekstrak 1 hari setelah infeksi menunjukkan bahwa ekstrak CA dosis 0,2; 0,4; 1 g/kg bb menurunkan titer virus DENV-2 dan menaikkan hitung trombosit  secara bermakna dibandingkan dengan kelompok DENV-2 tanpa ekstrak . Ekstrak CA tidak  memberikan efek terhadap jumlah leukosit dan kadar sitokin IL-6 dan IL-10. LD₅₀ semu ekstrak CA > 15 g/kg bb. Aloe-emodin diisolasi dari ekstrak CA dengan metode kolom kromaografi. IC₅₀ senyawa kaempferol, emodin dan aloe-emodin  terhadap DENV-2 berturut-turut adalah  22,24; 42,47; 7,51 mg/ml, dan CC₅₀ terhadap Huh7-it 1 berturut-turut 68,28; 74,19; 68,28 mg/ml. Uji in silico  ketiga senyawa menunjukkan bahwa mekanisme penghambatan ekstrak CA yang paling stabil adalah terhadap protein NS5 (IL9K4) dimana diperoleh tingkat energi bebas (DG) terendah.Kesimpulan: Ekstrak CA menghambat DENV-2 secara in vitro dan in vivo. Selain menurunkan titer virus dengue, ekstrak CA juga  meningkatkan hitung trombosit, dengan mekanisme penghambatan in vitro >95% pada tahap pre, post, pre/post dan reseptor. Mekanisme penghambatan fraksi heksan dan EA terbaik pada post dan pre/post infeksi sebesar 100%. Ikatan paling stabil senyawa yang terdapat didalam ekstrak CA adalah ikatan dengan protein NS5.

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Background: Dengue virus infection (DENV) is still endemic in Indonesia and in many tropical countries. Until now there is no anti viral available against dengue virus. This study aimed to investigate the antiviral effects of Cassia alata Linn (CA) leaves on DENV in vitro, in vivo, and in silico.Methods: This research was carried out at Laboratories of LIPI, Department of Microbiology  FMUI, 2017-2019. In vitro tests of CA extract,fractions and isolated compound were carried out to determine the IC₅₀, CC₅₀  and the inhibition mechanism  at receptor, pre, post and pre/post infection stages. In vivo efficacy  of CA extract was tested in mice Balb/c model. Dengue virus titers, platelet, leukocytes and IL-6 and IL-10 in bloods were measured. Acute oral toxicity test was carried out to determine the LD₅₀ of CA extract.  Isolation of compounds was carried out  from CA extract. In silico test was carried out to know interaction test compound with DENV protein using Autodock 1.5.6 software.Results: The results of the in vitro test showed that  the IC₅₀ of CA extract, hexane, ethyl acetate, butanol, and water fraction  against DENV-2 were 0.026; 0,004; 0.0013; 4.6; and 2.5 mg/ml and the CC₅₀ to Huh 7 it-1 were 208.9; 47.46; 57.2; 753,8; 311.33 mg/ ml, respectively. The results of the  mechanism study showed that at a dose of 10 mg/ml, CA extract, the hexane and ethyl acetate fractions  inhibited DENV-2 at the receptor stage, pre, post and pre/post infection which were better than the butanol and ethyl acetate fractions. CA extract inhibited the four mechanisms above by more than 95%.  Hexane and ethyl acetate fractions inhibited DENV-2 100% at post and pre-post infection stages. In vivo test showed that  the administration of CA extract at doses of 0.2; 0.4; 1 g/kg bw 1 day after DENV-2 infection  significantly reduced virus titers and increased platelet counts compared to DENV-2 infected group only. CA extract did not affect the number of leukocytes and  cytokines of IL-6 and IL-10 back to normal which had been altered in  the DENV-2 group. LD₅₀ of CA extract was more than 15 g/kg bw. Aloe-emodin was isolated from CA extract used column chromatography. The IC₅₀ of  kaempferol, emodin and aloe emodin to Huh7-it 1, respectively were 22.24; 42,47; 7.51 mg ml, and the CC₅₀ respectively were 68.28; 74,19; 68.28 mg/ml. In silico study of the three compounds showed that the most stable inhibition mechanism of CA extract was on protein NS5 (IL9K4) which had the lowest free energy (DG) level.Conclusion: CA extracts have high inhibitory activity against DENV-2 in vitro and in vivo. In addition to reducing dengue virus titers, CA extract also increased platelet count, with in vitro inhibition mechanism >95% at the pre, post, pre/post and receptor stages. Hexane and ethyl acetate fractions inhibit DENV-2 100% at post and pre/post infections. The most stable bond of the compounds contained in CA extract is the bond with NS5 protein."

"Penelitian daun sirih hijau sebagai antibakteri penyakit mastitis sapi perah telah dilakukan. Penelitian bertujuan daun sirih dapat sebagai pengganti antibiotik terhadap penyakit mastitis. Sebanyak 144 sampel susu mastitis dikoleksi dari daerah peternakan dataran rendah 250 m dpl, menengah 450 m dpl dan tinggi 720 m dpl. Bakteri diidentifikasi, diisolasi dan diuji daya antibakteri menggunakan ekstrak daun sirih konsentrasi 6,25; 12,5; 25 dan 50 b/v secara in vitro. Hasil yang diperoleh menunjukkan efektivitas ekstrak daun sirih konsentrasi 50 dibandingkan antibiotika komersial Lactaclox adalah berturut-turut 63,94; 66,23 dan 80,89 di dataran rendah, menengah dan tinggi. Secara in vivo, ekstrak daun sirih signifikan dapat menurunkan jumlah bakteri P.

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Research an antibacterial green betel leaf of dairy cow against mastitis diseases have carried out. The aims of the study to examine the ability of extract leaf medicinal plant against bacterial mastitis at dairy farm in three level of altitudes lower 250 m, moderate 450 m and high land 720 m. Four concentrations of extract leaf were 6.25 12.5 25 , and 50 b v which be done in vitro. The results revealed that the effectiveness extract leaf high at 50 compare to the commercial antibiotics were 63.94 66.23 and 80.89 at low, moderate and high altitude, respectively. Moreover, in vivo study was resulted significantly different P."

"Gabapentin, an anticonvulsant drug is used in the treatment of epilepsy, which has small dose therapeutic in blood plasma. Therapeutic drug monitoring (TDM) needs sensitive and specific analytical method.The aim of this study was to obtaine optimized method for analytical gabapentine in plasma (in vitro) with High Performance Liquid Chromatography - fluorescence and validation the method. The method involves derivatization of the primary amine group of gabapentin with dansyl chloride produce flurescence agent and could be analyzed with high performance liquid chromatography-fluorescence.In this research was used column Lichrosphere C18 ,10 μm, 250 x 10 μm, reverse phase with mobile phase 50 mmol/L sodium dihydrogen phosphate in 50 % acetonitrile. Flow rate of 1.7 mL/minutes, and fluorometric detection ( excitation and emission wavelength ; 318 nm and 510 nm ). For the range concentration of 0.1 ? 10 μg/mL have correlation coefficients of the calibration curves (r) is 0.9982 with a lower limit of quantification of gabapentin in 30 ng/mL. The results of validation method fulfilled for the given criterias."

"Senyawa turunan eugenol diduga dapat menginhibisi Bcl-2 pada sel kanker kolorektal HT29. Penelitian ini bertujuan untuk memperoleh senyawa baru turunan eugenol yang dapat menghambat sel kanker kolorektal HT29 secara in vitro dan menurunkan ekspresi Bcl-2 pada mencit yang mengalami pre-klamsia terhadap kolon secara in vivo. Penelitian ini diawali dengan melakukan desain senyawa turunan secara in silico. Hasil senyawa hit disintesis di laboratorium. Uji secara in vitro, uji apoptosis dan uji in vivo dilakukan berturut-turut pada hasil senyawa sintesis. Hasil in silico, dari skrining secara farmakofor dengan rancangan acak lengkap menggunakan 220 senyawa desain. Berdasarkan fitur farmakofor dengan cut off 5 fitur dihasilkan 23 senyawa. Hasil skrining farmakofor dilakukan docking menghasilkan delapan senyawa yaitu senyawa 4 rsquo;- 2-kloro-3-hidroksipropil -2 rsquo;-metoksifenil 2-hidroksibenzoat 57, 4 rsquo;- 2-kloro-3-hidroksi-propil -2 rsquo;-hidroksifenil 2-hidroksibenzoat 167, S -4 rsquo;- 2,3-dihidroksipropil -2 rsquo;-metoksifenil 2-hidroksibenzoat 59, R -4 rsquo;- 2,3-dihidroksipropil -2 rsquo;-metoksifenil 2-hidroksibenzoat 60, 4 rsquo;-alil-2 rsquo;-metoksifenil 4-amino-2-hidroksibenzoat 71, 4 rsquo;-alil-2 rsquo;-hidroksifenil 4-amino-2-hidroksibenzoat 181, 4 rsquo;-alil-2 rsquo;-metoksifenil 3,4,5-trihidroksibenzoat 86 dan 4 rsquo;-alil-2 rsquo;-metoksifenil 3,5-diihidroksi-4-metoksibenzoat 91 dengan energi ikatan lebih negatif dari standar. Delapan senyawa hasil skrining disintesis melalui reaksi esterifikasi, adisi halogen, hidroksilasi dan demetilasi. Hasil sintesis diuji aktivitas penghambatannya secara in vitro terhadap sel HT29 kanker kolon. Aktivitas penghambatan terhadap sel HT29 menunjukkan nilai IC50 antara 82.98 g/mL - 8.455 g/mL. Nilai IC50 tersebut lebih negatif dibandingkan senyawa penuntun eugenol. Hubungan Kuantitatif Struktur Aktivitas terhadap sel line HT29 menghasilkan persamaan Log 1/IC50 = -0.865-0.210 LogP 2 1.264 logP -0.994CMR n=10; r=0.706; SE:0.21; F=0.497, sig=7.86 . Persamaan menunjukkan variabel log P dan CMR berpengaruh terhadap IC50. Sifat hidrofobisitas log P lebih berperan dibandingkan dengan sifat sterik CMR . Hasil uji in vivo terhadap mencit Mus musculus menunjukkan senyawa turunan 59 memiliki nilai HE dan IHK mendekati kontrol positif. Peningkatan dosis pemberian menyebabkan peningkatan degradasi Bcl-2 pada jaringan mendekati kontrol normal. Hasil penelitian menunjukkan bahwa senyawa baru turunan eugenol 59 yang diperoleh dapat menghambat kanker kolorektal secara in vitro dan in vivo.

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Compounds derived from eugenol are thought to inhibit Bcl 2 in HT29 colorectal cancer cells. The aim of this study was to obtain new compounds of eugenol derivatives that could inhibit in HT29 cell invitro test and decrease of Bcl 2 expression in mice pre clammed on colon with invivo test. This research begins by designing in silico derivative compounds. The result of the hit compound is synthesized in the laboratory. In vitro tests, apoptotic test and in vivo test were performed successively on the result of the synthesis compound. In silico yield, from a complete randomized pharmacophore screening using 220 design compounds. Based on the pharmacophore features with cut off 5 features produced 23 compounds. The results of pharmacophore screening conducted docking which yielded eight compounds of compound 4 rsquo 2 chloro 3 hydroxypropyl 2 rsquo metohoxyphenyl 2 hydroxybenzoat 57, 4 rsquo 2 chloro 3 hidroxy propyl 2 rsquo hydroxyphenyl 2 hydroxybenzoat 167, S 4 rsquo 2,3 dihydroxypropyl 2 rsquo methoxyphenyl 2 hydroxybenzoat 59, R 4 rsquo 2,3 dihydroxypropyl 2 rsquo methoxyphenyl 2 hydroxybenzoat 60, 4 rsquo allyl 2 rsquo methoxyphenyl 4 amino 2 hydroxybenzoat 71, 4 rsquo allyl 2 rsquo hydroxyphenyl 4 amino 2 hydroxybenzoat 181, 4 rsquo allyl 2 rsquo methoxyphenyl 3,4,5 trihydroxybenzoat 86 dan 4 rsquo allyl 2 rsquo methoxyphenyl 3,5 dihydroxy 4 methoxybenzoat 91 with energy binding more negative than standard. The eight compounds of the screening are synthesized by esterification reaction, addition with halogen, hydroxylation. And demetylation The synthesis results were tested in vitro inhibitory activity against HT29 colon cancer cells. The inhibitory activity against HT29 cells shows an IC50 value between 82.98 g mL 8,455 g mL. The value of IC50 is better than the eugenol guiding compound. Quantitative Relation of Structure Activity against cell line HT29 with equation Log 1 IC50 0.865 0.210 LogP 2 1.264 logP 0.994CMR n 10 r 0.706 SE 0.21 F 0.497, sig 7.86 . This equation showed that log P and CMR have effect with IC50. Hydrophobicity log P more of effect compared than steric parameters CMR . In vivo test of Mus musculus that showed compound derivative 59 based on HE and IHK values approaching positive control. Increased dosage of administration leads to an increase in Bcl 2 degradation in tissues near normal control. The results showed that the new compound derived eugenol 59 obtained can inhibit colorectal cancer in vitro and in vivo."

"Sistem penghantaran obat transdermal saat ini banyak digunakan sebagai alternatif terhadap terapi konvensional (oral) untuk menghindari masalah seperti efek samping, metabolisme lintas pertama, dan kurangnya kepatuhan pasien.Penelitian ini bertujuan untuk mengembangkan sediaan hidrogel transdermal yang mengandung natrium diklofenak serta mengevaluasi penetrasi perkutan secara in vitro dan in vivo. Matriks sediaan hidrogel dibuat dari eksipien sambungsilang-6 dari koproses amilosa dan xanthan gum (CL6-Ko-A-XG). Hidrogel yang dibuat diuji penetrasinya secara in vitro melewati kulit tikus dengan menggunakan metode sel difusi Franz. Selanjutnya, dilakukan uji penetrasi secara in vivo menggunakan tikus Sprague-Dawley jantan (n=6) selama 12 jam. Analisis kadar natrium diklofenak dalam plasma tikus dilakukan dengan menggunakan kromatografi cair kinerja tinggi (KCKT). Berdasarkan hasil uji penetrasi secara in vitro, diperoleh jumlah kumulatif natrium diklofenak yang terpenetrasi 5890 ± 0,8 μg/cm2 dan fluks pada kondisi tunak 528 ± 72,5 μg/cm2/jam. Selanjutnya, dari hasil uji penetrasi in vivo diperoleh nilai area di bawah kurva (AUC0-t) natrium diklofenak yakni 47,94 ± 16,5 μg/mL jam. Maka, dapat disimpulkan bahwa hidrogel yang terbuat dari eksipien CL6-Ko-A-XG dapat menghantarkan natrium diklofenak hingga sirkulasi sistemik d.

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Transdermal drug delivery system can be an alternative to conventional (oral) therapy in order to avoid problems such as side effects, first pass metabolism, and poor patient compliance. The purpose of this study was to develop transdermal hydrogels containing diclofenac sodium and evaluate the in vitro and in vivo percutaneous penetration. The hydrogels matrices were prepared from 6-crosslinked of co-processed amylose-xanthan gum (CL6-Ko-A-XG). The hydrogels were subjected to in vitro penetration through rat skin using Franz diffusion cell. Furthermore, in vivo penetration study was carried out in male Sprague-Dawley rats (n=6) during 12 hours. In vivo drug plasma concentrations were determined using high performance liquid chromatography (HPLC). Based on the results of the in vitro study, the cumulative amount of diclofenac sodium penetrated was 5890 ± 0.8 μg/cm2 and flux at steady state condition was 528 ± 72.5 μg/cm2 hour. Moreover, the results of in vivo study showed that the area under curve (AUC0-t) was 47.94 ± 16.5 μg/mL hr. In conclusions, hydrogels which were formulated using CL6-Ko-A-XG could deliver diclofenac sodium into systemic circulation. According to the results, CL6-Ko-A-XG has a potential to be developed as matrices in transdermal system."

"This reference work presents the basic principles of angiogenesis induction, including the roles of signaling factors such as hypoxia-inducible factors, biophysical stimulation and angiogenic cells. The book also covers lymphogenesis induction. Both the established fundamentals in the field as well as new trends in the vascularization of engineered tissues are discussed. These include pre-vascularization strategies using preparation of channeled scaffolds and preparation of decellularized blood vessel trees, approaches to inducing formation of microvasculature and approaches to inducing the growth of vascular networks. The authors expand on these concepts with current studies of dual-level approaches to engineer vascularized tissue composites. The book concludes with a discussion of current clinical approaches and the use of vascular grafts in the context of providing clinical practice with new tissue engineering strategies."