Malaria merupakan penyakit yang disebabkan oleh infeksi Plasmodium. Pengobatan malaria dengan obat konvensional (klorokuin dan sulfadoksin pirimetamin) mengalami resistensi sehingga perlu dilakukan eksplorasi dalam pengobatan malaria (Harijanto, 2011). Ekstrak etanolik Dumortiera hirsuta mengandung senyawa bioaktif (alkaloid, terpenoid, flavonoid, dan saponin) dan bioaktivitas terhadap penurunan tingkat parasitemia Plasmodium berghei pada mencit (Fathoni, 2013). Berdasarkan hal tersebut, dilakukan penelitian untuk mempelajari apakah ekstrak etanolik D. hirsuta berpengaruh terhadap struktur mikroanatomis hepar dan ren mencit yang diinfeksi P. berghei. 27 ekor mencit (Mus musculus L.) jantan berumur 2-3 bulan dibagi atas 4 kelompok kontrol dan 5 kelompok perlakuan (n = 3). Kelompok kontrol dibagi atas perlakuan DMSO 3% per oral, ekstrak etanolik D. hirsuta 300 mg/kg BB, diinfeksi P. berghei, dan diinfeksi P. berghei dan klorokuin. Kelompok perlakuan diinfeksi P. Berghei, dan diberi ekstrak etanolik D. hirsuta per oral dosis 100; 200; 300; 400; 500 mg/kg BB. Uji antiplasmodium dilakukan dengan metode Peter’s Supressive Test. Hasil penelitian menunjukkan bahwa pemberian ekstrak etanolik D. hirsuta pada mencit yang diinfeksi P. berghei memberikan pengaruh bervariasi terhadap perubahan struktur mikroanatomis hepar dan ren sesuai dosis yang diberikan. Berdasarkan tingkat kerusakan organ hepar dan ren mencit, diketahui bahwa semakin tinggi dosis ekstrak etanolik D. hirsuta yang diberikan, kerusakan yang ditimbulkan semakin berat. Simpulan dari penelitian ini adalah pemberian ekstrak etanolik D. hirsuta berpengaruh terhadap struktur mikroanatomis hepar dan ren mencit yang diinfeksi P. berghei. Dosis ekstrak etanolik D. hirsuta yang aman digunakan adalah dosis di bawah 300 mg/kg BB berdasarkan perubahan struktur mikroanatomis hepar dan ren mencit yang diinfeksi P. berghei.

Malaria is the disease caused by Plasmodium. Malaria’s medicinal treatment by conventional drugs (chloroquin and sulfodoxin-pirimetamin) have been resistance, and the new way of medical treatment for malaria is needed. Ethanolic extract of Dumortiera hirsuta contains bioactive compounds (alkaloid, terpenoid, flavonoid, and saponin) and has bioactivity to decrease level of parasitemia caused by Plasmodium berghei in mice. This research was conducted to study whether ethanolic extract of D. hirsuta affect on microanatomical structure of liver and kidney mice infected by P. berghei. Twenty seven of male mices (Mus musculus L.) at the age of 2-3 months were divided into 4 control groups and 5 treatment groups (n = 3). The control groups were divided as DMSO 3%, ethanolic extract of D. hirsuta (300 mg/kg BW), infected by P. berghei, and infected by P. berghei and given a Chloroquin groups. The treatment groups were infected by P. berghei and given ethanolic extract of D. hirsuta at the doses of 100; 200; 300; 400; and 500 mg/kg BW. Test of antiplasmodium was analyzed Peter’s Supressive Test. Based on descriptive observation, various dosage of ethanolic extract of D. hirsuta could affect on microanatomical structures of liver and kidney of mices infected by P. berghei with various changes. Based on the level of damage of microanatomical structure of liver and kidney, the higher dosage of ethanolic extract of D. hirsuta given to mice, the worse damage of liver and kidney structures could be. Conclusion of this research was ethanolic extract of D. hirsuta could affect the microanatomical structures of liver and kidney of mices infected by P. berghei. Based on the level of damage of hepar and ren structures in mice infected with P. berghei, the limited dosage of ethanolic extract of D. hirsuta allowed for drugs was under 300 mg/kg BW

Kata Kunci : Plasmodium, Dumortiera hirsuta, hepar, ren, Mus musculus