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"Latar belakang: Mortalitas yang tinggi pada kanker ovarium utamanya disebabkan oleh progresi, kemoresistensi, dan rekurensinya. Diketahui progresivitas dan kemoresistensi kanker ovarium dipengaruhi oleh aksis endothelin, yang melibatkan endothelin-1 dan reseptor endothelin melalui proses epithelial-to-mesenchymal transition (EMT), sehingga menargetkan aksis ini merupakan prospek yang menjanjikan dalam pengembangan agen sensitisasi yang efektif. Kurkumin, senyawa herbal yang banyak di Indonesia, berpotensi menjadi agen ko-kemoterapi kanker ovarium, namun mekanismenya masih belum banyak diketahui. Penelitian sebelumnya menemukan bahwa kurkumin mampu menekan jalur endothelin di beberapa galur sel. Tujuan: Penelitian eksperimental dilakukan untuk menganalisis aktivitas kurkumin sebagai agen ko-kemoterapi cisplatin dalam memodulasi aksis endothelin pada sel SKOV3. Metode: Sampel terbagi menjadi tiga kelompok, yaitu kelompok kontrol (hanya diberikan vehicle), kelompok cisplatin 3,75 μM, serta kelompok kurkumin 5 μM dan cisplatin 3,75 μM. Sel diinkubasi selama 48 jam setelah pemberian perlakuan. Setelah 48 jam, dilakukan pemeriksaan ekspresi mRNA endothelin-1, reseptor endothelin A, dan reseptor endothelin B menggunakan metode qRT-PCR. Hasil: Terdapat penurunan signifikan ekspresi mRNA endothelin-1 pada sel SKOV3 yang diberikan kurkumin bersama cisplatin (0,55±0,32; p=0,005) dibandingkan dengan kelompok kontrol (3,35±2,80). Tidak ditemukan perbedaan dalam ekspresi mRNA reseptor endothelin A dan B yang signifikan antar kelompok. Kesimpulan: Kurkumin sebagai agen ko-kemoterapi cisplatin mampu memodulasi aksis endothelin melalui penekanan ekspresi mRNA endothelin-1, namun tidak melalui penekanan ekspresi mRNA reseptor endothelin A maupun B.

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Background: The high mortality of ovarian cancer is mainly attributed to its progression, chemoresistance to cisplatin, and recurrence. This progression and chemoresistance is mediated by the endothelin axis, which involves endothelin-1 and endothelin receptors through epithelial-to-mesenchymal transition (EMT) process, so targeting this axis is a promising prospect in developing an effective chemosensitizer. According to previous studies, curcumin, a ubiquitous herbal compound in Indonesia, has the potential to be a co-chemotherapeutic agent in ovarian cancer, but its mechanism in cancer progression is still unknown. Previous studies show that curcumin has the ability to modulate endothelin axis in non cancer cells.

Objective: To analyze the activity of curcumin as a co-chemotherapeutic agent with cisplatin in modulating endothelin axis in SKOV3 cells.

Methods: Sample is divided into three groups: control group (only given vehicle), cisplatin 3,75 μM group, and curcumin 5 μM and cisplatin 3,75 μM group. Cells are then incubated for 48 hours. After 48 hours, expression of endothelin-1, endothelin receptor A, and endothelin receptor B mRNAs are measured by qRT-PCR.

Results: There is a significant decrease in endothelin-1 mRNA expression in SKOV3 cells treated with curcumin and cisplatin (0,55±0,32; p=0,005) compared to control group (3,35±2,80). There is no significant difference of endothelin receptor A and B mRNA expression between each group.

Conclusion: Curcumin as a co-chemotherapeutic agent with cisplatin potentially modulates endothelin axis through repression of endothelin-1 mRNA expression, but not endothelin receptor mRNA A or B expression."

"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.

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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."