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Valentino Ryu Yudianto
Abstrak :
Pendahuluan: Pengobatan Kolitis Ulseratif (KU) hingga saat ini masih dilakukan dengan cara pemberian obat-obatan antiinflamasi, seperti 5-aminosalicylic acid (5-ASA), hingga pembedahan. Selain pengobatan konvensional, dikembangkan pula pengobatan alternatif yang memanfaatkan bahan-bahan dari alam seperti elagitanin. Elagitanin danderivatnya, yakni asam elagat, dapat ditemukan dalam jumlah yang banyak pada kulit buah delima dan diduga memiliki efek antiinflamasi yang bermanfaat untuk terapi alternatif kolitis. Oleh karena itu, penelitian ini hendak menelusuri lebih lanjut pengaruh ekstrak etanol kulit buah delima terhadap ekspresi NF-kB sebagai penanda inflamasi. Metode: Desain penelitian yang digunakan dalam penelitian ini adalah eksperimental. Penelitian ini menggunakan organ kolon mencit yang telah diberikan perlakuan di penelitian dan dikelompokkan ke dalam 6 kelompok sebagai berikut: kelompok tanpa perlakuan (KTP), kontrol negatif (KN) yang diberikan DSS2%, kontrol positif 1 (KP1) yang diberikan DSS2% dan aspirin 43 mg/kgBB/hari, kontrol positif 2 (KP2) yang diberikan DSS2% dan asam elagat 26 mg/kgBB/hari, serta kelompok dosis 1 (KD1) dan 2 (KD2) yang diberikan DSS2% dan ekstrak kulit delima dalam dosis 240 mg/kgBB/hari dan 480 mg/kgBB/hari. Hasil dan Pembahasan: Rerata H Score untuk KTP adalah 129,0946; untuk KN adalah 200.3989; untuk KP1 adalah 165,5808; untuk KP2 adalah 159,0553; untuk KD1 adalah 186,1655; dan untuk KD2 adalah 141,0696. Uji One Way ANOVA menunjukkan hasil yang signifikan. Uji posthoc Tukey menunjukkan perbedaan yang bermakna antara KD2 dan KN. Kesimpulan: Pemberian ekstrak etanol kulit delima dengan dosis 480 mg/kgBB/hari dapat menurunkan ekspresi NF-kB pada epitel kolon mencit yang diinduksi DSS. ......Introduction: Up until now, Ulcerative Colitis (UC) treatment is mainly done conservatively by using antiinflammatory drugs, such as 5-aminosalicylic acid (5-ASA), or surgery. In addition to convensional treatment, alternative treatment that uses natural ingredient, such as elagitanin, is now under development. Elagitanin and its derivative, ellagic acid, can be found abundantly in pomegranate peel, and are expected to own an antiinflammatory property that can be considered to be an alternative choice for UC treatment. Therefore, this study is conducted with the intention of acknowledging the effect of pomegranate peel ethanol extract on NF-κB expression in mice’s colon tissue induced with DSS. Method: Study design used in this study is experimental. This study used the colonic tissue that was already prepared by the previous researcher and is divided into 6 groups: group without intervention (KTP), negative control (KN) with the administration of DSS 2%, positive control 1 (KP1) with the administration of DSS 2% and aspirin 43 mg/kgBW/day, positive control 2 (KP2) in which the mice are given DSS 2% and ellagic acid 26 mg/kgBW/day, and finally dose 1 and dose 2 group (KD1 and KD2) with the administration of DSS 2% and pomegranate peel extract with dose of 240 mg/kgBW/day and 480 mg/kgBW/day. Result and Discussion: Mean H Score for KTP is 129,0946; for KN is 200.3989; for KP1 is 165,5808; for KP2 is 159,0553; for KD1 is 186,1655; and for KD2 is 141,0696. Analysis using One Way ANOVA test shows a signicant result. Posthoc Tukey test shows a significant difference between KD2 and KN. Conclusion: pomegranate peel ethanol extract with dose of 480 mg/kgBW/day can decrease the NF-κB expression in mice’s colon epithelium induced with DSS.
Depok: Fakultas Kedokteran Universitas Indonesia, 2020
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Afra Intan Nurlaili
Abstrak :
ABSTRAK Insidensi kolitis ulseratif di Indonesia mulai meningkat. Sedangkan etiologi penyakit tersebut masih belum jelas sehingga pengobatan saat ini masih bersifat simptomatik, jangka panjang, dan menimbulkan banyak efek samping. Tujuan dari penelitian ini adalah untuk membuktikan efek antiinflamasi ekstrak daun Ficus deltoidea pada kolon mencit yang diinduksi dekstran sodium sulfat (DSS). Penelitian dilakukan dengan menggunakan 24 sampel materi biologik tersimpan dari penelitian sebelumnya yang dibagi menjadi empat kelompok: kontrol negatif (DSS), kontrol positif (aspirin), ekstrak daun Ficus deltoidea dosis 25 mg, dan ekstrak daun Ficus deltoidea dosis 50 mg. Preparat histologis jaringan kolon diwarnai dengan pewarnaan hematoksilin-eosin (HE) dan diamati pada perbesaran 400x. Terdapat peningkatan sel goblet secara signifikan (p < 0,001) pada kelompok ekstrak daun Ficus deltoidea dosis 50 mg dibandingkan dengan kelompok kontrol negatif. Namun tidak terdapat perbedaan bermakna pada parameter fokus inflamasi dan angiogenesis.
ABSTRACT The incidence of ulcerative colitis in Indonesia is increasing. While its etiology is still unknown, the current treatment is still symptomatic, long term, and causes many side effects. The purpose of this study is to confirm that Ficus deltoidea leaf extract has an antiinflammatory effect on DSS-induced mice colon. This study was conducted using 24 stored tissue samples from previous study which are divided into four groups: negative control (DSS), positive control (aspirin), Ficus deltoidea leaf extract at a dose of 25 mg, and Ficus deltoidea leaf extract at a dose of 50 mg. Colon tissue histology sample is stained with hematoxylin-eosin (HE) staining and examined on magnification of 400x. There is a significant increase number of goblet cells (p < 0,001) on the Ficus deltoidea leaf extract group at a dose of 50 mg compared to negative control group. However, there is no significant effect of Ficus deltoidea leaf extract on inflammation focus and angiogenesis.
Depok: Fakultas Kedokteran Universitas Indonesia , 2019
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Sonya Aprella Diva
Abstrak :
[Buah manggis (Garcinia mangostana Linn) merupakan salah satu buah tropis dari Asia Tenggara seperti Indonesia dan kulitnya biasanya digunakan sebagai obat tradisional untuk mengatasi inflamasi dan mikroorganisme. Selain itu, kulit buah manggis juga diperkirakan dapat digunakan sebagai antikanker. Tujuan dari penelitian ini adalah mengetahui pengaruh ekstrak etanol kulit buah manggis terhadap viabilitas sel Raji secara in vitro melalui uji sitotoksisitas. Ekstrak etanol kulit buah manggis didapatkan melalui proses maserasi dan evaporasi dengan rotary evaporator. Ekstrak dibagi menjadi beberapa konsentrasi, yaitu 6,25 μg/ml, 12,5 μg/ml, 25 μg/ml, 50 μg/ml, 100 μg/ml, 200 μg/ml, 400 μg/ml, dan 800 μg/ml, kemudian diujikan ke sel Raji dan diinkubasi selama 48 jam. Uji sitotoksisitas yang digunakan adalah metode MTT-assay. Sifat sitotoksisitas ekstrak tersebut ditentukan oleh nilai IC50, lalu uji kemaknaan yang digunakan adalah Kruskal-Wallis. Hasil analisis menunjukkan nilai IC50 sebesar 3,07 μg/ml (p = 0,02). Kesimpulan dari penelitian ini adalah ekstrak etanol kulit buah manggis bersifat sitotoksik kuat terhadap viabilitas sel Raji dan ditemukan adanya perbedaan bermakna antar kelompok. Hasil uji Post Hoc memperlihatkan terdapat perbedaan bermakna antara kelompok kontrol dan kelompok perlakuan dengan konsentrasi 6,25 μg/ml dengan kelompok perlakuan lain.;Mangosteen (Garcinia mangostana Linn) is one of tropical fruit from south east Asia such as Indonesia and its pericarp usually used as traditional medicine for anti-inflammatory and anti-microorganism. Mangosteen pericarp is also expected can be used as anticancer. The aim of this study was to determine the in vitro cytotoxicity of mangosteen pericarp ethanol extract on viability of Raji cells. The extract was obtained by maceration and evaporation process with rotary evaporator. The extract was divided into several concentration, such as 6.25 μg/ml, 12.5 μg/ml, 25 μg/ml, 50 μg/ml, 100 μg/ml, 200 μg/ml, 400 μg/ml, and 800 μg/ml, then it was tested with Raji cells and incubated during 48 hours. The cytotoxic effect against Raji cells is evaluated by MTT-assay. The cytotoxicity level of the extract is determined by IC50 value, then the significance test is used Kruskal-Wallis. The result of analysis showed that IC50 value was 3.07 μg/ml (p = 0.02). The conclusion of this research were the mangosteen pericarp ethanol extract has high cytotoxicity for viability Raji cells and there was a significant difference between groups. Post Hoc test result showed there were significant difference between control and 6.25 μg/ml group which compared with other groups;Mangosteen (Garcinia mangostana Linn) is one of tropical fruit from south east Asia such as Indonesia and its pericarp usually used as traditional medicine for anti-inflammatory and anti-microorganism. Mangosteen pericarp is also expected can be used as anticancer. The aim of this study was to determine the in vitro cytotoxicity of mangosteen pericarp ethanol extract on viability of Raji cells. The extract was obtained by maceration and evaporation process with rotary evaporator. The extract was divided into several concentration, such as 6.25 μg/ml, 12.5 μg/ml, 25 μg/ml, 50 μg/ml, 100 μg/ml, 200 μg/ml, 400 μg/ml, and 800 μg/ml, then it was tested with Raji cells and incubated during 48 hours. The cytotoxic effect against Raji cells is evaluated by MTT-assay. The cytotoxicity level of the extract is determined by IC50 value, then the significance test is used Kruskal-Wallis. The result of analysis showed that IC50 value was 3.07 μg/ml (p = 0.02). The conclusion of this research were the mangosteen pericarp ethanol extract has high cytotoxicity for viability Raji cells and there was a significant difference between groups. Post Hoc test result showed there were significant difference between control and 6.25 μg/ml group which compared with other groups, Mangosteen (Garcinia mangostana Linn) is one of tropical fruit from south east Asia such as Indonesia and its pericarp usually used as traditional medicine for anti-inflammatory and anti-microorganism. Mangosteen pericarp is also expected can be used as anticancer. The aim of this study was to determine the in vitro cytotoxicity of mangosteen pericarp ethanol extract on viability of Raji cells. The extract was obtained by maceration and evaporation process with rotary evaporator. The extract was divided into several concentration, such as 6.25 μg/ml, 12.5 μg/ml, 25 μg/ml, 50 μg/ml, 100 μg/ml, 200 μg/ml, 400 μg/ml, and 800 μg/ml, then it was tested with Raji cells and incubated during 48 hours. The cytotoxic effect against Raji cells is evaluated by MTT-assay. The cytotoxicity level of the extract is determined by IC50 value, then the significance test is used Kruskal-Wallis. The result of analysis showed that IC50 value was 3.07 μg/ml (p = 0.02). The conclusion of this research were the mangosteen pericarp ethanol extract has high cytotoxicity for viability Raji cells and there was a significant difference between groups. Post Hoc test result showed there were significant difference between control and 6.25 μg/ml group which compared with other groups]
[, ], 2015
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Jihan Bennovry
Abstrak :
[Buah Manggis (Garcinia mangostana L.) merupakan buah yang banyak tumbuh di negara tropis, di antaranya Indonesia dan Thailand. Bagian kulit (pericarp) Manggis memiliki banyak khasiat, salah satunya sebagai antikanker. Berdasarkan hal tersebut, dilakukan uji sitotoksisitas untuk melihat efek ekstrak kulit buah Manggis terhadap viabilitas sel leukemia MT-2. Untuk membuat ekstrak, pelarut yang digunakan adalah etanol 99%. Ekstrak etanol kulit buah Manggis dibuat dengan menggunakan alat rotary evaporator. Konsentrasi ekstrak dibagi menjadi delapan yakni, 6,25 μg/ml, 12,5 μg/ml, 25 μg/ml, 50 μg/ml, 100 μg/ml, 200 μg/ml, 400 μg/ml, dan 800 μg/ml. Penambahan DMSO dan media kultur digunakan sebagai kontrol. Ekstrak dan kontrol diberikan kepada sel leukemia MT-2 dan dilakukan uji sitotoksisitas dengan menggunakan metode MTT-Assay. Hasil uji sitotoksisitas berupa kepadatan sel yang dinyatakan dengan Optical Density (OD). Data ini diolah sehingga menghasilkan IC50. Nilai IC50 yang didapatkan adalah 1,72 μg/ml yang tergolong sitotoksik kuat. Data penelitian dianalisis menggunakan uji Kruskal-Wallis, dilanjutkan dengan uji post hoc Mann Whitney dan didapatkan hasil perbedaan bermakna pada kelompok kontrol dan kelompok perlakuan dengan konsentrasi 6,25 μg/ml, 12,5 μg/ml, 25 μg/ml, dan 50 μg/ml.;Mangosteen (Garcinia mangostana L.). is a fruit which grows in tropical countries, includes Indonesia and Thailand. Its peel or pericarp has a lot of benefits. One of the benefits is as anticancer. To test the effectiveness of the peel as anticancer, cytotoxicity test should be done. The previous researches haven?t done the test on leukemia MT-2 cells, so this research did this test on leukemia MT-2 cells to know the effect of mangosteen pericarp ethanol extract to the viability of this cancer cell. This research used ethanol 99% for the solvent. Mangosteen pericarp ethanol extract was made by using rotary evaporator. The extract was adjusted into eight concentrations, which are 6.25 μg/ml, 12.5 μg/ml, 25 μg/ml, 50 μg/ml, 100 μg/ml, 200 μg/ml, 400 μg/ml, and 800 μg/ml. DMSO and culture media were used for the control. Both the extract and the control were given to the leukemia MT-2 cells and were tested for cytotoxicity test. MTT-Assay method was used for the cytotoxicity test. The result of cytotoxicity test is called Optical Density (OD) or the density of the cancer cells which are still ?alive?. This data was processing so that the IC50 can be valued. The IC50 value from this experiment is 1.72 μg/ml which is a very strong cytotoxicity. For data analysis, this research used Kruskal-Wallis Test and was continued by using Post hoc Mann-Whitney Test. From Post hoc Mann-Whitney Test, there are the significant differences between several concentrations. The significant differences can be seen on control group and tested group with concentration 6.25 μg/ml, 12.5 μg/ml, 25 μg/ml, and 50 μg/ml;Mangosteen (Garcinia mangostana L.). is a fruit which grows in tropical countries, includes Indonesia and Thailand. Its peel or pericarp has a lot of benefits. One of the benefits is as anticancer. To test the effectiveness of the peel as anticancer, cytotoxicity test should be done. The previous researches haven?t done the test on leukemia MT-2 cells, so this research did this test on leukemia MT-2 cells to know the effect of mangosteen pericarp ethanol extract to the viability of this cancer cell. This research used ethanol 99% for the solvent. Mangosteen pericarp ethanol extract was made by using rotary evaporator. The extract was adjusted into eight concentrations, which are 6.25 μg/ml, 12.5 μg/ml, 25 μg/ml, 50 μg/ml, 100 μg/ml, 200 μg/ml, 400 μg/ml, and 800 μg/ml. DMSO and culture media were used for the control. Both the extract and the control were given to the leukemia MT-2 cells and were tested for cytotoxicity test. MTT-Assay method was used for the cytotoxicity test. The result of cytotoxicity test is called Optical Density (OD) or the density of the cancer cells which are still ?alive?. This data was processing so that the IC50 can be valued. The IC50 value from this experiment is 1.72 μg/ml which is a very strong cytotoxicity. For data analysis, this research used Kruskal-Wallis Test and was continued by using Post hoc Mann-Whitney Test. From Post hoc Mann-Whitney Test, there are the significant differences between several concentrations. The significant differences can be seen on control group and tested group with concentration 6.25 μg/ml, 12.5 μg/ml, 25 μg/ml, and 50 μg/ml, Mangosteen (Garcinia mangostana L.). is a fruit which grows in tropical countries, includes Indonesia and Thailand. Its peel or pericarp has a lot of benefits. One of the benefits is as anticancer. To test the effectiveness of the peel as anticancer, cytotoxicity test should be done. The previous researches haven’t done the test on leukemia MT-2 cells, so this research did this test on leukemia MT-2 cells to know the effect of mangosteen pericarp ethanol extract to the viability of this cancer cell. This research used ethanol 99% for the solvent. Mangosteen pericarp ethanol extract was made by using rotary evaporator. The extract was adjusted into eight concentrations, which are 6.25 μg/ml, 12.5 μg/ml, 25 μg/ml, 50 μg/ml, 100 μg/ml, 200 μg/ml, 400 μg/ml, and 800 μg/ml. DMSO and culture media were used for the control. Both the extract and the control were given to the leukemia MT-2 cells and were tested for cytotoxicity test. MTT-Assay method was used for the cytotoxicity test. The result of cytotoxicity test is called Optical Density (OD) or the density of the cancer cells which are still ‘alive’. This data was processing so that the IC50 can be valued. The IC50 value from this experiment is 1.72 μg/ml which is a very strong cytotoxicity. For data analysis, this research used Kruskal-Wallis Test and was continued by using Post hoc Mann-Whitney Test. From Post hoc Mann-Whitney Test, there are the significant differences between several concentrations. The significant differences can be seen on control group and tested group with concentration 6.25 μg/ml, 12.5 μg/ml, 25 μg/ml, and 50 μg/ml]
[, ], 2015
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Michelle Cancera Angelita
Abstrak :
[Angka kejadian penyakit mieloma multipel kecil, yaitu 0,8% di dunia dan 0,6% di Asia Tenggara dari seluruh kasus kanker yang ada. Namun, penyakit ini terjadi secara asimtomatik sehingga sulit didiagnosis, belum dapat disembuhkan, dan mudah mempengaruhi organ dalam tubuh. Kulit buah manggis yang jarang dimanfaatkan diketahui mengandung senyawa xanton (polifenolat) yang memiliki aktivitas antikanker. Penelitian in vitro menggunakan sel jalur p3x63ag8 untuk menemukan ada tidaknya efek sitotoksisitas ekstrak etanol kulit buah manggis serta IC50. Sel dibagi menjadi 9 kelompok, yaitu 1 kelompok kontrol dan 8 kelompok perlakuan dengan konsentrasi 6,25 μg/ml, 12,5 μg/ml, 25 μg/ml, 50 μg/ml, 100 μg/ml, 200 μg/ml, 400 μg/ml, dan 800 μg/ml. Data diambil dengan metode MTT assay dan hasilnya berupa nilai optical density. Setelah inkubasi 48 jam menggunakan ekstrak etanol kulit buah manggis, hasil persamaan garis diketahui IC50 nya adalah 5,41 μg/ml. Analisis statistik dengan Kruskal Wallis menghasilkan adanya perbedaan efek sitotoksik pada konsentrasi yang berbeda . Uji Post Hoc didapatkan perbedaan bermakna antara kelompok kontrol dan kelompok perlakuan 6,25 μg/ml dengan kelompok perlakuan lain.;Multiple myeloma disease has small incidence, namely 0,8% in the world and 0,6% in Southeast Asia of all cancer cases. However, the diasease occurs in asymptomatic that so difficult to be diagnosed, can not be cured, and affects many organs. The mangosteen pericarp which rarely used evidently contain xanthone (polifenolat) compound which have anticancer activity. Research in in vitro manner using cell lines p3x63ag8 to discover the presence of cytotoxicity effect of mangosteen pericarp ethanol extract and the IC50. Cells was divided into 9 groups, 1 control group and 8 treatment groups (consentrations: 6,25 μg/ml, 12,5 μg/ml, 25 μg/ml, 50 μg/ml, 100 μg/ml, 200 μg/ml, 400 μg/ml, and 800 μg/ml). Data taken by MTT assay method and the result is optical density value. After 48-hours incubation period and the result in line equation, found that IC50 was 5.41 ug / ml. Statistical analysis with Kruskal Wallis declared differences in the cytotoxic effects of different concentrations.Post Hoc test found significant difference beetwen the control group and the treatment group of 6.25 ug / ml just than other groups;Multiple myeloma disease has small incidence, namely 0,8% in the world and 0,6% in Southeast Asia of all cancer cases. However, the diasease occurs in asymptomatic that so difficult to be diagnosed, can not be cured, and affects many organs. The mangosteen pericarp which rarely used evidently contain xanthone (polifenolat) compound which have anticancer activity. Research in in vitro manner using cell lines p3x63ag8 to discover the presence of cytotoxicity effect of mangosteen pericarp ethanol extract and the IC50. Cells was divided into 9 groups, 1 control group and 8 treatment groups (consentrations: 6,25 μg/ml, 12,5 μg/ml, 25 μg/ml, 50 μg/ml, 100 μg/ml, 200 μg/ml, 400 μg/ml, and 800 μg/ml). Data taken by MTT assay method and the result is optical density value. After 48-hours incubation period and the result in line equation, found that IC50 was 5.41 ug / ml. Statistical analysis with Kruskal Wallis declared differences in the cytotoxic effects of different concentrations.Post Hoc test found significant difference beetwen the control group and the treatment group of 6.25 ug / ml just than other groups, Multiple myeloma disease has small incidence, namely 0,8% in the world and 0,6% in Southeast Asia of all cancer cases. However, the diasease occurs in asymptomatic that so difficult to be diagnosed, can not be cured, and affects many organs. The mangosteen pericarp which rarely used evidently contain xanthone (polifenolat) compound which have anticancer activity. Research in in vitro manner using cell lines p3x63ag8 to discover the presence of cytotoxicity effect of mangosteen pericarp ethanol extract and the IC50. Cells was divided into 9 groups, 1 control group and 8 treatment groups (consentrations: 6,25 μg/ml, 12,5 μg/ml, 25 μg/ml, 50 μg/ml, 100 μg/ml, 200 μg/ml, 400 μg/ml, and 800 μg/ml). Data taken by MTT assay method and the result is optical density value. After 48-hours incubation period and the result in line equation, found that IC50 was 5.41 ug / ml. Statistical analysis with Kruskal Wallis declared differences in the cytotoxic effects of different concentrations.Post Hoc test found significant difference beetwen the control group and the treatment group of 6.25 ug / ml just than other groups]
[;Fakultas Kedokteran Universitas Indonesia, Fakultas Kedokteran Universitas Indonesia], 2015
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Moch Yasin Friansyah
Abstrak :
[Kanker merupakan salah satu penyebab kematian utama di dunia, termasuk Indonesia. Berbagai penelitian dilakukan untuk mencari alternatif terapi kanker. Kulit manggis dipercaya mempunyai kandungan senyawa yang bersifat sitotoksik terhadap sel kanker. Penelitian ini bertujuan untuk mengetahui efek sitotoksisitas ekstrak etanol kulit manggis terhadap sel limfoma Hodgkin. Ekstrak yang digunakan berasal dari proses ekstraksi kulit manggis dengan pelarut etanol menggunakan Vaccum Rotary Evaporator pada tekanan 1 atm dengan suhu 60o C. Ekstrak kulit manggis diberikan dalam 8 konsentrasi berbeda yaitu 6,25 μg/ml, 12,5 μg/ml, 25 μg/ml, 50 μg/ml, 100 μg/ml, 200 μg/ml, 400 μg/ml, dan 800 μg/ml. Sitotoksisitas dinilai dengan uji MTT-assay untuk mendapat nilai IC50. Hasil penelitian menunjukkan bahwa ekstrak etanol kulit manggis mempunyai efek sitotoksik terhadap sel limfoma Hodgkin dengan nilai IC50 sebesar 5.6 μg/ml. Uji kemaknaan menggunakan uji Kruskal-Wallis menunjukkan nilai p = 0.008 (p ≤ 0.05). Kesimpulan dari penelitian ini yaitu ekstrak etanol kulit manggis mempunyai efek sitotoksik kuat terhadap sel Limfoma Hodgkin.;Cancer is one of the leading cause of death in the world, including Indonesia. Various studies have been done to seek alternative cancer therapy. Mangosteen pericarp is believed to have substance that are cytotoxic to cancer cells. The purpose of this study is to determine the in vitro cytotoxicity of mangosteen pericarp ethanol extract on Hodgkin Lymphoma cells. The extract used in this study is obtained from the mangosteen pericarp extraction using Vacuum Rotary Evaporator at a pressure of 1 atm and temperature of 60o C. Mangosteen pericarp extract is given in eight different concentration of 6.25 ug / ml, 12.5 pg / ml, 25 mg / ml, 50 pg / ml, 100 pg / ml, 200 mg / mL, 400 mg / ml, and 800 ug / ml. Cytotoxicity was assessed using MTT-assay test to obtain IC50 values. The results showed that ethanol extract of mangosteen pericarp has a cytotoxic effect on Hodgkin lymphoma cells with IC50 value of 5.6 ug / ml. The data were analyzed using Kruskal-Wallis test and had a p value of 0.008 (p ≤ 0.05). The conclusion of this study is that ethanol extract of mangosteen pericarp has a strong cytotoxic effect on Hodgkin lymphoma cells, Cancer is one of the leading cause of death in the world, including Indonesia. Various studies have been done to seek alternative cancer therapy. Mangosteen pericarp is believed to have substance that are cytotoxic to cancer cells. The purpose of this study is to determine the in vitro cytotoxicity of mangosteen pericarp ethanol extract on Hodgkin Lymphoma cells. The extract used in this study is obtained from the mangosteen pericarp extraction using Vacuum Rotary Evaporator at a pressure of 1 atm and temperature of 60o C. Mangosteen pericarp extract is given in eight different concentration of 6.25 ug / ml, 12.5 pg / ml, 25 mg / ml, 50 pg / ml, 100 pg / ml, 200 mg / mL, 400 mg / ml, and 800 ug / ml. Cytotoxicity was assessed using MTT-assay test to obtain IC50 values. The results showed that ethanol extract of mangosteen pericarp has a cytotoxic effect on Hodgkin lymphoma cells with IC50 value of 5.6 ug / ml. The data were analyzed using Kruskal-Wallis test and had a p value of 0.008 (p ≤ 0.05). The conclusion of this study is that ethanol extract of mangosteen pericarp has a strong cytotoxic effect on Hodgkin lymphoma cells]
[, Fakultas Kedokteran Universitas Indonesia], 2015
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Paulus Anthony Halim
Abstrak :
Latar belakang: Azoxymethane AOM dan dextran sodium sulfate DSS adalah senyawa kimia yang sering digunakan untuk menginduksi kanker kolorektal pada tikus. Penelitian sebelumnya menunjukkan bahwa azoxymethane dan DSS juga menyebabkan nefrotoksisitas. Omega 3 yang ditemukan pada minyak ikan diketahui memiliki efek protektif pada ginjal. Namun, omega 3 minyak ikan kaya masih sangat kurang dimanfaatkan di Indonesia. Untuk mempelajari fitur histopatologi ginjal pada tikus yang diinduksi AOM DSS setelah pemberian omega 3 minyak ikan kaya. Metode: Mencit eksperimental yang telah diinduksi menggunakan AOM 10 mg kg dan DSS 2 selama 2 minggu dialokasikan secara acak ke dalam 4 kelompok sebagai berikut. Kelompok Kontrol tikus tidak menerima minyak ikan, tikus Kelompok Dosis Rendah menerima 1,5 mg minyak ikan, tikus kelompok Dosis Menengah menerima 3 mg minyak ikan, tikus Kelompok Dosis Tinggi menerima 6 minyak ikan mg hari. Minyak ikan kaya omega 3 diberikan selama 12 minggu. Pemeriksaan patologi dilakukan untuk menilai degenerasi tubular dan kongesti vaskular. Hasil: Gambaran histopatologis yang ditemukan di ginjal adalah peradangan, degenerasi tubular, nekrosis, dan kongesti vaskular. Persentase 3 tubular degenerasi berat pada kelompok yang diberi minyak zaitun kaya omega 3 rendah, menengah, dan tinggi lebih rendah sebesar 17,5, 25, dan 37,5 masing-masing dibandingkan dengan kelompok kontrol. Pemberian omega 3 minyak ikan kaya menunjukkan persentase yang lebih sedikit dari tingkat kongesti 2 pembuluh darah moderat dibandingkan dengan kelompok kontrol namun, peningkatan dosis omega 3 minyak ikan kaya tidak menunjukkan persentase yang berbeda dari kemacetan pembuluh darah moderat di antara kelompok-kelompok. Kesimpulan: Hasil menunjukkan efek omega 3 minyak ikan kaya untuk mencegah nefrotoksisitas pada tikus yang diinduksi oleh azoxymethane dan DSS. ......Background: Azoxymethane AOM and dextran sodium sulfate DSS are chemical compounds frequently used to induce colorectal cancer in mice. Previous studies have shown that azoxymethane and DSS also cause nephrotoxicity. Omega 3 found on fish oil is known to have protective effect on kidney. However, omega 3 rich fish oil is still very underutilized in Indonesia.Aim To study the histopathologic features of kidney on mice induced AOM DSS after the administration of omega 3 rich fish oil. Method: The experimental mice that had been induced using AOM 10 mg kg and DSS 2 for 2 weeks were allocated randomly into 4 groups as follows Control Group mice recieved no fish oil, Low Dose Group mice recieved 1.5 mg day fish oil, Medium Dose Group mice recieved 3 mg day fish oil, High Dose Group mice recieved 6 mg day fish oil. The omega 3 rich fish oil were given for 12 weeks. Pathology examination was done to grade tubular degeneration and vascular congestion. Result: The histopathologic features found in the kidney were inflammation, tubular degeneration, necrosis, and vascular congestion. The percentage of severe 3 tubular degeneration on groups given low, medium, and high dose omega 3 rich olive oil were lower by 17.5 , 25 , and 37,5 respectively compared to control group. The administration of omega 3 rich fish oil showed less percentage of moderate 2 vascular congestion degree compared to control group however, increasing dose of omega 3 rich fish oil did not show different percentages of moderate vascular congestion among groups. Conclusion: The result indicates the effect of omega 3 rich fish oil on preventing nephrotoxicity in mice induced by azoxymethane and DSS.
Jakarta: Fakultas Kedokteran Universitas Indonesia, 2017
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Harits Adi Putra
Abstrak :
Inflamasi lambung (gastritis) merupakan salah satu penyakit dengan prevalensi yang cukup tinggi di Indonesia. Inflamasi tersebut dapat terjadi akibat proses infeksi atau noninfeksi. Jika tidak ditangani dengan baik, dapat terjadi komplikasi ulkus, perforasi, dan perdarahan lambung. Terapi farmakologi untuk gastritis belum cukup efektif karena terdapat risiko efek samping dan interaksi obat. Hal tersebut mendorong berbagai penelitian untuk menelusuri potensi zat lain sebagai antiinflamasi. Ekstrak kulit delima diketahui mengandung asam elagat dan elagitanin yang telah terbukti mampu menghambat inflamasi di sejumlah organ. Belum terdapat studi mengenai efek ekstrak kulit delima terhadap inflamasi di lambung, khususnya delima yang tumbuh di Indonesia. Penelitian dilakukan dengan menggunakan 25 mencit yang terbagi menjadi lima kelompok. Mencit pada kelompok Kontrol Negatif, Dosis-1 (diberikan ekstrak 240 mg/KgBB), Dosis-2 (diberikan ekstrak 480 mg/KgBB), dan Kontrol Positif (diberikan asam elagat 26 mg/KgBB) diinduksi dengan DSS 2% sebanyak tiga siklus. Gambaran histopatologi (pewarnaan hematoxylin-eosin) mukosa lambung diamati pada sepuluh lapang pandang tiap preparat. Uji statistik menyatakan terdapat pengaruh signifikan ekstrak kulit delima terhadap infiltrasi sel radang (p= 0,001) dengan dosis 480 mg/KgBB, hiperplasia (p= 0,002) dengan dosis 240 mg/KgBB dan 480 mg/KgBB, serta displasia (p= 0,002) dengan dosis 480 mg/KgBB. Namun, tidak terdapat pengaruh signifikan ekstrak kulit delima terhadap angiogenesis (p= 0,114). Efek ekstrak kulit delima terjadi karena kandungan asam elagat dan elagitanin yang menghambat jalur inflamasi NF-κB sehingga terjadi penurunan ekspresi sitokin dan mediator inflamasi. Penelitian lebih lanjut untuk mengetahui dosis optimal, toksisitas, dan uji klinis dibutuhkan untuk memastikan efikasi serta keamanan suplementasi ekstrak kulit delima. ......Gastric inflammation (gastritis) is one of the most prevalent disease in Indonesia. The etiologies are infection and noninfection factors. If not treated adequately, there can be complications, such as gastric ulcer, perforation, and bleeding. However, pharmacological treatments for gastritis have some risks of side effects and drug interactions. Many studies are conducted to discover potential of another substances as anti-inflammatory agents which have less side effects and drug interactions. Pomegranate peel extract contains ellagic acid and ellagitannin which have been proven to inhibit inflammation in some organs. Nevertheless, there has been no study proving its efficacy in inhibiting gastric inflammation. This research used 25 mice which are divided into five groups. Mice in four groups consists of Negative Control, Dosage-1 (given the extract at a dose 240 mg/KgBW), Dosage-2 (given the extract at a dose of 480 mg/KgBW), and Positive Control (given ellagic acid at a dose of 26 mg/KgBW) were induced by DSS 2% in three cycles. Histopathological preparations were observed in ten microscopic fields (each slides) to examine the dependent variables. There are significant differences in the amount of leukocyte infiltration (p= 0,001) at a dose of 240 mg/KgBW, hyperplasia (p= 0,002) at doses of 240 mg/KgBW and 480 mg/KgBW, and dysplasia (p = 0,002) at a dose of 240 mg/KgBW. However, there is no significant effect of pomegranate peel extract to the amount of angiogenesis (p= 0,114). It has anti-inflammatory effect because of the ellagic acid and ellagitannin contents inhibit the NF-κB inflammatory pathway which down regulate the inflammatory cytokines and mediators expressions. Further researches to discover the optimal dose, toxicity, and clinical trials are necessary to ensure the efficacy and safety of pomegranate peel extract supplementation.
Jakarta: Fakultas Kedokteran Universitas Indonesia, 2018
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Vannessa Karenina
Abstrak :
Latar belakang : Kanker kolorektal merupakan salah satu kanker dengan peningkatan insidensi yang paling pesat dalam dekade terakhir. Peningkatan terbesar diperkirakan akan terjadi di negara berkembang akibat perubahan gaya hidup. Pilihan tata laksana kanker kolorektal yang ada saat ini, seperti pembedahan, terapi radiasi, dan kemoterapi, diketahui belum mampu memberikan efek yang diinginkan. Dengan mempertimbangkan ketersediaan, harga, dan efek toksik, kedelai merupakan salah satu bahan pangan yang berpotensi menjadi terapi adjuvan. Hal ini dikarenakan zat aktif yang terkandung dalam kedelai, yaitu protein lunasin, diketahui memiliki efek antiinflamasi dan antikanker yang bermanfaat pada kasus kanker kolorektal. Metode : Sebanyak 30 ekor mencit Swiss Webster dipisahkan menjadi enam kelompok. Lima dari enam kelompok mencit diinduksi dengan azoksimetan (AOM) dan dekstran sodium sulfat (DSS). Ekstrak kedelai kaya lunasin dengan dosis 250 mg/kgBB, 300 mg/kgBB, dan 350 mg/kgBB diberikan pada tiga kelompok mencit selama 6 minggu. Pewarnaan imunohistokimia terhadap COX-2 kemudian dilakukan pada jaringan kolon distal mencit yang telah dikorbankan, lalu diamati di bawah mikroskop. Hasil interpretasi ekspresi COX-2 dinyatakan dalam bentuk optical density score (ODS). Hasil : Terdapat perbedaan yang signifikan antara kelompok negatif dengan kelompok intervensi ekstrak kedelai kaya lunasin pada dosis 300 mg/kgBB (p=0,047) dan 350 mg/kgBB (p=0,016). Kesimpulan : Pemberian ekstrak kedelai kaya lunasin menghambat ekspresi COX-2 pada sel epitel kripta kolon distal mencit yang diinduksi AOM dan DSS. ......Background : Colorectal cancer is one of the fastest growing incidences of cancer in the past decade. The highest increase is expected to occur in developing countries due to lifestyle changes. The choice of colorectal cancer management currently available, such as surgery, radiation therapy, and chemotherapy, is known to have not been able to give the desired effect. Taking into account the availability, price and toxic effects, soybeans are one of the food ingredients that have the potential to become adjuvant therapy. This is because the active substance contained in soybeans, namely lunasin protein, is known to have anti-inflammatory and anticancer effects that are beneficial in colorectal cancer cases. Method : A total of 30 Swiss Webster mice were separated into six groups. Five of the six groups of mice were induced with azoximethane (AOM) and dextran sodium sulfate (DSS). Extracts of lunasin-rich soybean with a dose of 250 mg / kgBB, 300 mg / kgBW, and 350 mg / kgBB were given to three groups of mice for 6 weeks. Immunohistochemical staining of COX-2 was then carried out on the distal colon tissue of mice that had been sacrificed, then observed under a microscope. The results of interpretation of COX-2 expression are stated in the form of optical density score (ODS). Result : There was a significant difference between the negative group and the intervention group of lunasin-rich soybean extract at a dose of 300 mg/kgBW (p = 0.047) and 350 mg/kgBW (p = 0.016). Conclusion : Administration of lunasin-rich soy extracts inhibit COX-2 expression in cryptic epithelial cells of distal colon of mice induced by AOM and DSS.
Jakarta: Fakultas Kedokteran Universitas Indonesia, 2018
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Renata Tamara
Abstrak :
Kanker kolorektal menyumbang 9,7% dari seluruh kasus kanker dan kejadiannya berhubungan dengan inflamasi kronik. Oleh karena terapi kanker saat ini masih memiliki banyak kekurangan, peptida dalam makanan semakin banyak diteliti karena murah, mudah didapat, toksisitas rendah, dan berpotensi mencegah kanker. Riset dilakukan untuk mengetahui apakah lunasin dari kacang kedelai dapat menurunkan ekspresi sitokin proinflamasi TNF-I±  pada epitel kolon. Sebanyak 30 ekor mencit Swiss Webster dibagi ke dalam enam kelompok secara acak. Satu kelompok normal, sementara lima kelompok lainnya diinduksi karsinogenesis dengan azoxymethane dan dextran sodium sulfate, kemudian ada yang dibiarkan (kontrol negatif), diberi aspirin (kontrol positif), dan ekstrak kedelai kaya lunasin dalam tiga dosis berbeda (250, 300, dan 350 mg/kgBB) selama 4 minggu. Jaringan kolon distal diambil untuk diwarnai imunohistokimia dan diamati di bawah mikroskop cahaya pada pembesaran 400x untuk menghitung sel epitel berdasarkan intensitas warnanya. Indeks dihitung berdasarkan optical density score. Ekstrak kedelai kaya lunasin dapat menurunkan ekspresi TNF-I±. Perbedaan antara kontrol negatif dengan ekstrak bermakna pada dosis 300 mg/kgBB (p=0,016) dan 350 mg/kgBB (p=0,009), tetapi tidak bermakna dengan dosis 250 mg/kgBB (p=0,754). Penelitian ini menunjukkan penurunan ekspresi TNF-I± signifikan pada dosis ekstrak kedelai 300 mg/kgBB atau lebih. ......Colorectal cancer contributes to 9.7% of all cancer and its pathogenesis is related to chronic inflammation. Because of there are some lacks in current cancer therapy, peptide in food becomes popular among researchers because it is cheap, easy to get, low toxicity, and a promising cancer preventing agent. This research aimed to investigate whether lunasin from soybean can reduce the expression of pro-inflammatory cytokine TNF-I± in colonic epithelial cell. 30 Swiss Webster mice randomly allocated to six groups. One group was normal and five groups were induced carcinogenesis using azoxymethane (AOM) and dextran sodium sulfate (DSS), then was given nothing (negative control), aspirin (positive control), and lunasin-rich soybean extract in three different doses (250, 300, and 350 mg/kgBW) for four weeks. Distal colon tissue was immunohistochemically stained and then observed under light microscope with 400X magnification to count epithelial cell based on its colour. Index was calculated using optical density score. Lunasin-rich soybean extract can decrease expression of TNF-I±. There are statistically significant between negative control and dose 300 mg/kgBW (p=0.016) and 350 mg/kgBW (p=0.009), yet not significant with dose 250 mg/kgBW (p=0.754). This research shows that reduction of TNF-I± expression is significant with dose 300 mg/kgBW or higher.
Jakarta: Fakultas Kedokteran Universitas Indonesia, 2018
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