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Abstrak :
Salah satu obat antikanker yang sekarang paling efektif digunakan sebagai kemoterapi kanker ovarium adalah cisplatin. Namun, cisplatin memiliki banyak efek samping pada berbagai organ, salah satunya hepar. Hepatotoksisitas akibat cisplatin menyebabkan terbatasnya dosis kemoterapi cisplatin. Salah satu faktor kunci patofisiologi kerusakan akut hepar adalah inflamasi. Kurkumin merupakan senyawa alami yang memiliki sifat antiinflamasi tetapi bioavailabilitasnya rendah. Untuk itu, diformulasikan nanokurkumin untuk meningkatkan bioavailabilitasnya. Meskipun begitu, efek kurkumin dan nanokurkumin dalam memodulasi jalur inflamasi hepatotoksisitas akibat cisplatin pada kanker ovarium belum diamati. Penelitian ini bertujuan untuk membandingkan pengaruh kurkumin dan nanokurkumin sebagai ko-kemoterapi terhadap hepatotoksisitas cisplatin dalam jalur inflamasi. Penelitian in vivo dilakukan pada tikus Wistar betina yang diinduksi DMBA untuk mendapatkan model kanker ovarium. Kemudian, tikus-tikus diberi perlakuan terapi dengan cisplatin secara intraperitoneal (4 mg/kgBB/minggu) dan kombinasinya dengan kurkumin (100 mg/kgBB/hari) dan nanokurkumin (100 mg/kgBB/hari) per oral. Tikus-tikus tersebut dibagi menjadi kelompok: tikus normal, model kanker ovarium saja, terapi cisplatin, terapi cisplatin + kurkumin, dan terapi cisplatin + nanokurkumin. Setelah 1 bulan, tikus di-sacrifice dan organ hepar disimpan beku. Ekspresi mRNA relatif NF-κB dan IL-1β serta kadar protein IL-6 diukur dengan metode qt RT-PCR dan ELISA secara berurutan. Data hasil pengukuran IL-6 dan data hasil transformasi logaritma NF-κB dan IL-1β dianalisis menggunakan uji one-way ANOVA, menggunakan perangkat lunak SPSS20. Tidak terdapat perbedaan signifikan secara statistik antar kelompok perlakuan dalam mRNA NF-κB (p=0,503), mRNA IL-1β (p=0,237), dan protein IL-6 (p=0,157). Tidak ada perbedaan yang signifikan antara kurkumin dan nanokurkumin dalam memodulasi jalur inflamasi hepatotoksisitas cisplatin pada model kanker ovarium tikus. ...... Up to now, one of the most effective anticancer drug as ovarian cancer chemotherapy is cisplatin. Nevertheless, cisplatin has many side effects on several organs, one of which is liver. Cisplatin-induced hepatotoxicity causes limited cisplatin chemotherapy dose. One of the pathophysiological key factor of acute liver injury is inflamation. Curcumin is natural compound which has antiinflamation properties but the bioavailability is low. To overcome it, nanocurcumin is made to increase its bioavailability. Nonetheless, curcumin and nanocurcumin effect on modulating inflammatory pathway toward cisplatin-induced hepatotoxicity in ovarian cancer rat model has not been observed. This study aims to compare the effect of curcumin and nanocurcumin as co-chemotherapy toward cisplatin-induced hepatotoxicity in inflammatory pathway. An in vivo study was done on female Wistar rats induced by DMBA to achieve ovarian cancer model. Then, rats was treated with cisplatin intraperitoneally (4 mg/kgBW/week) and the combination with per oral curcumin (100 mg/kgBW/day) and nanocurcumin (100 mg/kgBW/day). Those rats were divided into groups, which are normal rat, only ovarian cancer model, cisplatin therapy, cisplatin + curcumin therapy, and cisplatin + nanocurcumin therapy. After 1 month, rats are sacrificed and liver organs are stored frozen. mRNA relative expression of NF-κB and IL-1β as well as protein level of IL-6 was measured using qt RT-PCR and ELISA method, respectively. The result data from the measurement of IL-6 and the data from logarithmic transformation of NF-κB and IL-1β was analysed using one-way ANOVA test using SPSS20 software. There is no significant differences between groups in mRNA NF-κB (p=0.503), mRNA IL-1β (p=0.237), and protein IL-6 (p=0.157). There is no significant differences between curcumin and nanocurcumin in modulating inflammatory pathway of cisplatin-induced hepatotoxicity in ovarian cancer rat model.

Abstrak :
Latar belakang : Cisplatin adalah pilihan utama dalam penatalaksanaan kanker ovrium secara farmakologi. Namun, disisi lain cisplatin dapat menyebabkan kerusakan ginjal. Kerusakan ginjal akibat Cisplatin salah satunya terjadi karena perubahan aktivitas sistem endotelin ginjal sebagai pengatur hemodinamik ginjal. Secara teori kerusakan ini dapat dikurangi dengan pemberian ko-kemoterapi cisplatin yang memiliki sifat renoprotektif. Salah satu agen renoprotektif adalah Kurkumin. Salah satu manfaat kurkumin dapat mengurangi kerusakan ginjal karena bersifat renoprotektif. Penelitian ini bertujuan untuk mengetahui efek pemberian kurkumin sebagai ko-kemoterapi cisplatin terhadap ekspresi reseptor endothelin B (ETBR) dan gambaran hitopatologi pada ginjal tikus model kanker ovarium. Metode: Dua puluh empat tikus Wistar betina (150-200 gram) berusia 5 minggu dikelompokan menjadi empat kelompok: Normal (N), Kanker Ovarium tanpa pemberian obat (Ca), Cisplatin (Cis) adalah kelompok tikus kanker ovarium yang mendapat terapi cisplatin 4mg/KgBB selama tiga minggu, Cisplatin+Kurkumin (Cis+Cur) adalah kelompok tikus kanker ovarium yang diberi cisplatin 4mg/KgBB+ curcumin 100mg/KgBB selama tiga minggu. Setelah memasuki minggu ke-24, tikus dikorbankan dan diambil jaringan ginjal untuk dilakukan pengamatan secara histologi dan molekular. Hasil: gambaran histologi ginjal menunjukan perubahan struktur abrnomal. Akan tetapi perubahan struktur menuju kerusakan ginjal pada penelitian ini tidak signifikan. Selanjutnya, pengamatan ekspresi ETBR didapati ekspresi tertinggi pada kelompok tikus normal (N) dan terendah pada kelompok tikus dengan pemberian Cisplatin dan Kurkumin (Cis+Cur) dengan nilai p pada uji ANOVA Satu Arah sebesar 0.087 (signifikan jika p<0,05). Kesimpulan: pemberian kurkumin sebagai ko-kemoterapi cisplatin pada tikus model kanker ovarium tidak menyebabkan perubahan struktur histologi yang bermakna dan tidak menyebabkan peningkatan ekspresi ETBR yang signifikan. ......Background: Cisplatin is the main choice in pharmacological treatment of ovarian cancer. However, cisplatin can cause kidney damage. One of the causes of kidney damage due to cisplatin occurs due to changes in the activity of the renal endothelin system as a renal hemodynamic regulator. In theory, this damage can be reduced by giving cisplatin co-chemotherapy which has renoprotective properties. One of the renoprotective agents is curcumin. One of the benefits of curcumin is to reduce kidney damage because it is renoprotective. This study aims to determine the effect of curcumin administration as co-chemotherapy of cisplatin on endothelin B receptor expression (ETBR) and the histopathological description of ovarian cancer model rats. Methods: Twenty-four female Wistar rats (150-200 grams) aged 5 weeks were grouped into four groups: Normal (N), Ovarian Cancer without drug administration (Ca), Cisplatin (Cis) is a group of ovarian cancer mice receiving 4mg/KgBB cisplatin therapy for three weeks, Cisplatin + Curcumin (Cis + Cur) is a group of ovarian cancer mice that were given cisplatin 4mg / KgBB + curcumin 100mg / KgBB for three weeks. After entering the 24th week, the rats were sacrificed and kidney tissue was taken for histological and molecular observation. Result: The histology of the kidneys showed an abnormal structural change. However, the structural changes leading to kidney damage in this study were not significant. Furthermore, observations of ETBR expression found the highest expression in the normal (N) group of rats and the lowest in the group of rats given Cisplatin and Curcumin (Cis + Cur) with a p value in the One Way ANOVA test of 0.087 (significant if p <0.05). Conclusion: giving curcumin as co-chemotherapy of cisplatin in ovarian cancer model mice did not cause significant changes in histological structure and did not cause a significant increase in ETBR expression

Abstrak :
Latar belakang: Terdapat peningkatan 80% ekspresi reseptor endothelin A dan 40% ekspresi endothelin B pada kanker ovarium. Peningkatan ekspresi reseptor endothelin A terbukti berperan dalam menyebabkan progresifitas dan metastasi kanker ovarium. REB berperan sebagai klirens endothelin-1 dan meningkatkan proses apoptosis. Cisplatin sebagai lini pertama pengobatan kanker ovarium memiliki efek samping dan berisiko mengembangkan kanker ovarium resistensi cisplatin. Kurkumin sebagai salah satu bahan alami terbukti memiliki potensi sebagai antikanker dan dapat meingkatkan efikasi cisplatin. Tujuan: penelitian ini adalah untuk melihat efektifitas kombinasi kurkumin dan cisplatin sebagai tatalaksana alternatif kanker ovarium dilihat dari ekspresi relatif mRNA reseptor endothelin A dan reseptor endothelin B. Metode: Homogenasi jaringan ovarium tersimpan yang dilanjutkan dengan sentrifugasi. Cairan supernatan diambil untuk dilakukan purifikasi. RNA yang terfurifikasi diubah menjadi cDNA. Selanjutnya, analisis dilakukan menggunakan mesin qRT-PCR, dengan metode Livak-Schmittgen 2(-Ct). Hasil: Ekspresi mRNA reseptor endothelin B pada kelompok normal (7,376±1,407), DMBA +Cis (1,701±1,096), DMBA+Cis+Cur (7,391±2,261), DMBA (0,649±0,221), dengan p<0,05. Hasil bermakna pada kelompok DMBA dan DMBA+Cis+Kur dengan p=0,014. Ekspresi mRNA reseptor endothelin A pada kelompok normal (0,698±0,366), DMBA+Cis (5,311±2,737), DMBA+Cis+Kur (7,502±2,476), DMBA (10,970±3,883), dengan p<0,05. Namun antar kelompok DMBA dan kelompok DMBA+Cis+Kur atau DMBA+Cis tidak ditemukan hasil bermakna p>0,05. Simpulan: Kombinasi kurkumin dan cisplatin yang diberikan pada tikus model kanker ovarium yang diinduksi DMBA, dapat memengaruhi jalur reseptor endothelin melalui peningkatan ekspresi relatif mRNA reseptor endothelin B, dan kecendrungan penurunan ekspresi reseptor endothelin A. ......Background: There was an 80% increase in endothelin A receptor expression and 40% endothelin B expression in ovarian cancer. Increased expression of endothelin A receptors has been shown to play a role in causing progression and metastasis of ovarian cancer. REB acts as endothelin-1 clearance and increases the apoptotic process. Cisplatin as the first line of ovarian cancer treatment has side effects and the risk of developing cisplatin- resistant ovarian cancer. Curcumin as a natural ingredient is proven to have potential as an anticancer and can increase the efficacy of cisplatin. The purpose of this study was to determine the effectiveness of the combination of curcumin and cisplatin as an alternative treatment for ovarian cancer in terms of the relative expression of endothelin A and endothelin B receptor mRNAs. Methods: Homogenation of stored ovarian tissue followed by centrifugation. The supernatant fluid is taken for purification. The purified RNA is converted into cDNA. Furthermore, the analysis was performed using a qRT- PCR machine, with the Livak-Schmittgen methode 2(-Ct). Results: The expression of mRNA endothelin B receptor in normal (7.376 ± 1.407), DMBA + Cis (1.701 ± 1.096), DMBA + Cis + Cur (7.391 ± 2.261), DMBA (0.649 ± 0.221) groups, with p <0.05. The results were significant in the DMBA and DMBA + Cis + Kur groups with p = 0.014. The expression of endothelin A receptor mRNA in normal (0.698 ± 0.366), DMBA + Cis (5.311 ± 2.737), DMBA + Cis + Kur (7.502 ± 2.476), DMBA (10.970 ± 3.883) groups, with p <0.05. However, between the DMBA group and the DMBA + Cis + Kur or DMBA + Cis group there were no significant results found with p> 0.05. Conclusion: The combination of curcumin and cisplatin given to DMBA-induced ovarian cancer model mice can affect the endothelin receptor pathway through an increase in the relative expression of endothelin B receptor mRNA, and a tendency to decrease the expression of endothelin A receptors.

Abstrak :
30 years after its discovery as an antitumor agent, cisplatin represents today one of the most successful drugs in chemotherapy. This book is intended to reminisce this event, to take inventory, and to point out new lines of development in this field. Divided in 6 sections and 22 chapters, the book provides an up-to-date account on topics such as - the chemistry and biochemistry of cisplatin, - the clinical status of Pt anticancer drugs, - the impact of cisplatin on inorganic and coordination chemistry, - new developments in drug design, testing and delivery. It also includes a chapter describing the historical development of the discovery of cisplatin. The book addresses the problem of mutagenicity of Pt drugs and raises the question of the possible relevance of the minor DNA adducts, e.g. of interstrand cross-links, and the possible use of trans-(NH3)2Pt(II)-modified oligonucleotides in antisense and antigene strategies. The final section of the book is concerned with new developments such as novel di- and trinuclear Pt(II) drugs with DNA binding properties different from those of cisplatin, with orally active Pt(IV) drugs which are presently in clinical studies, and with attempts to modify combinatorial chemistry in such a way that it may become applicable to fast screening of Pt antitumor drugs. The potential of including computational methods in solving questions of Pt-DNA interactions is critically dealt with in the concluding chapter.