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"Latar belakang: Temulawak adalah tanaman obat asli Indonesia yang mengandung zat aktif xanthorrhizol dan memiliki efek antifungal. Dengan membentuk biofilm, Candida albicans menjadi virulen dan semakin virulen ketika mencapai fase maturasi. Tujuan: Mengetahui potensi ekstrak etanol temulawak dalam menghambat biofilm C. albicans isolat klinis dan C. albicans ATCC 10231 pada fase maturasi. Metode: Pemaparan ekstrak etanol temulawak berbagai konsentrasi pada biofilm C. albicans dimulai pada 1.5 jam setelah inkubasi dan dilanjutkan selama 48 jam. MTT assay digunakan untuk mengukur persentase viabilitas sel C. albicans pada biofilm yang kemudian dikonversi menjadi persentase inhibisi biofilm oleh ekstrak temulawak. Hasil: Terhadap C. albicans isolat klinis, Kadar Hambat Minimum KHM dan Kadar Bunuh Minimum KBM ekstrak etanol temulawak adalah 15 dan 30, sedangkan terhadap C. albicans ATCC 10231 adalah 20 dan 35. Nilai Kadar Hambat Biofilm Minimum KHBM50 ekstrak etanol temulawak adalah 35 terhadap C. albican isolat klinis dan 40 terhadap C. albicans ATCC 10231. Dibutuhkan konsentrasi ekstrak etanol temulawak yang lebih tinggi untuk menghambat C. albicans ATCC 10231 daripada untuk menghambat C. albicans isolat klinis. Kesimpulan: Baik terhadap C. albicans isolat klinis maupun C. albicans ATCC 10231, ekstrak etanol temulawak berpotensi menghambat biofilm C. albicans fase maturasi.

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Background: Javanese turmeric is an Indonesian medicinal plant which contains xanthorrhizol had been reported to have antifungal effect. By forming biofilms, C. albicans becomes virulent and more virulent as it reaches the maturation phase.

Objective: To investigate the capability of Javanese turmeric ethanol extract in inhibiting the formation of maturation phase C. albicans biofilm both of clinical isolate and ATCC 10231.

Methods: The Exposure of various concentrations of Javanese turmeric ethanol extract to C. albicans biofilm started at 1.5 hours after incubation and continued for 48 hours. MTT assay was used to measure the percentage viability of C. albicans cells on the biofilm which was then converted into the percentage of biofilm inhibition.

Results: Against C. albicans clinical isolate, Minimum Inhibition Concentration MIC and Minimum Fungicidal Concentration MFC of javanese turmeric ethanol extract was 15 and 30 whereas against C. albicans ATCC 10231 was 20 and 35. Minimum Biofilm Inhibition Concentration MBIC50 of javanese turmeric ethanol extract was 35 against C. albicans clinical isolate and 40 against C. albicans ATCC 10231 biofilm. Higher concentration of the extract was required to inhibit C. albicans ATCC 10231 compared to the concentration to inhibit C. albicans clinical isolate.

Conclusion: Both against C. albicans clinical isolat and C. albicans ATCC 10231, javanese turmeric ethanol extract has potential in inhibiting mature phase of C. albicans biofilm."

"Temu Putih (Curcuma zedoaria) adalah tanaman dari famili Zingiberaceae yang berasal dari Himalaya, India. Penelitian sebelumnya pada rimpang temu putih menunjukkan bahwa tanaman ini mengandung metabolit sekunder dari golongan alkaloid, fenolik, dan terpenoid yang diketahui memiliki aktivitas antibakteri. Tujuan penelitian ini adalah mengisolasi metabolit sekunder dari ekstrak metanol rimpang kunyit putih dan menguji aktivitas antibakterinya terhadap bakteri penyebab jerawat yaitu Propionibacterium acnes dan Staphylococcus epidermidis. Pada penelitian ini diperoleh hasil maserasi ekstrak rimpang kunyit putih dengan rendemen 3,68%. Ekstrak metanol kemudian dipartisi dan persentase rendemen ekstrak etil asetat adalah 47,06%. Ekstrak partisi etil asetat selanjutnya difraksinasi menggunakan berbagai teknik kromatografi seperti kromatografi cair vakum (KCV), kromatografi kolom (KK), kromatografi radial (KR), dan kromatografi lapis tipis preparatif (KLT). Senyawa hasil isolasi kemudian dikarakterisasi menggunakan instrumen FTIR, UV-Vis, dan LC-MS/MS. Dari penelitian ini berhasil diisolasi tiga senyawa golongan fenolik, yaitu dimethoxycurcumin (A), 3,5,7-trihydroxy-4'-methoxyflavon (B), dan 7-methoxyumarin (C). Uji aktivitas antibakteri terhadap bakteri penyebab jerawat dilakukan dengan metode difusi cakram dengan kontrol positif klindamisin dan kontrol negatif DMSO. Berdasarkan hasil uji aktivitas, baik ekstrak kasar metanol, ekstrak etil asetat terpartisi, maupun senyawa hasil isolasi tidak memiliki aktivitas antibakteri terhadap bakteri P. acnes dan S. epidermidis. Berdasarkan hasil penelitian, kandungan metabolit sekunder rimpang kunyit putih tidak cukup potensial sebagai antibakteri terhadap bakteri P. acnes dan S. acnes.Temu Putih (Curcuma zedoaria) is a plant from the Zingiberaceae family originating from the Himalayas, India. Previous research on temu putih rhizome showed that this plant contains secondary metabolites from the alkaloid, phenolic, and terpenoid groups which are known to have antibacterial activity. The purpose of this study was to isolate secondary metabolites from methanol extract of white turmeric rhizome and to test its antibacterial activity against acne-causing bacteria, namely Propionibacterium acnes and Staphylococcus epidermidis. In this study, the results of maceration of white turmeric rhizome extract were obtained with a yield of 3.68%. The methanol extract was then partitioned and the percentage yield of the ethyl acetate extract was 47.06%. The ethyl acetate partition extract was further fractionated using various chromatographic techniques such as vacuum liquid chromatography (KCV), column chromatography (KK), radial chromatography (KR), and preparative thin layer chromatography (TLC). The isolated compounds were then characterized using FTIR, UV-Vis, and LC-MS/MS instruments. From this study, three phenolic compounds were isolated, namely dimethoxycurcumin (A), 3,5,7-trihydroxy-4'-methoxyflavone (B), and 7-methoxyumarin (C). Antibacterial activity test against acne-causing bacteria was carried out by disc diffusion method with positive control of clindamycin and negative control of DMSO. Based on the activity test results, both the crude methanol extract, the partitioned ethyl acetate extract, and the isolated compound did not have antibacterial activity against P. acnes and S. epidermidis bacteria. Based on the results of the study, the secondary metabolite content of white turmeric rhizome is not enough potential as an antibacterial against P. acnes and S. acnes bacteria."