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Minggu, 11 Desember 2011

Tugas-Tugas MAPRO 22

Bagi teman-teman yang ingin mengunduh tugas-tugas kita silahkan klik aja dibawah ini....

Etika profesi
Farmasi Industri
Biofarmasetika
QA RS B.Nanik
PBL Herbal
PBL Terapi


Semoga bermanfaat untuk kita semua....Semangat.....

Minggu, 04 Desember 2011

Brosur kegiatan


Foto-Foto Kegiatan


BAB II LAPORAN PELAKSANAAN PROGRAM PROMOSI KESEHATAN

BAB II
LAPORAN PELAKSANAAN
PROGRAM PROMOSI KESEHATAN
Berikut ini dilaporkan kegiatan promosi kesehatan yang sudah dilaksankan oleh setiap anggota kelompok.
  1. Wahyu Irna Wati dan Winda Abdulrahman
  • Tempat : Rumah Bapak Agus Maryono, Jeruk Legi RT 21/RW 35 No. 504 Banguntapan, Bantul, Yogyakarta
  • Hari / Tanggal : Kamis, 17 November 2011
  • Waktu : 20.00-20.30 WIB
  • Kontak person : Thaufa Nugroho
  • No Tlp. : 08975872633
  • Materi : Swamedikasi dan Pengenalan Obat yang dapat digunakan, Swamedikasi Influenza, Salesma, Rhinitis Alergi
  • Dosen Pendamping : Farida, M.Si, Apt

BAB III EVALUASI DAN REKOMENDASI

BAB III
EVALUASI DAN REKOMENDASI
  1. Evaluasi
Evaluasi keberhasilan program promosi kesehatan yang telah dilaksanakan dapat dilakukan dengan beberapa cara, seperti dengan tanya jawab langsung dengan masyarakat yang terkait atau menggunakan kuisioner.

BAB I LAPORAN HASIL ANALISA KESEHATAN DAN RENCANA PROGRAM PROMOSI KESEHATAN


I. Gambaran Lokasi Praktek
  1. Gambaran Demografi dan Geografi
Secara geografis, Kecamatan Banguntapan merupakan kecamatan yang terletak di sisi Timur wilayah Kota Yogyakarta. Batas-batas wilayahnya, di sebelah utara berbatasan dengan kecamatan Depok,Sleman ; sebelah timur dengan kecamatan Piyungan, Bantul ; sebelah selatan dengan kecamatan Pleret,Bantul ; dan sebelah barat berbatasan dengan kecamatan Sewon, Kabupaten Bantul. Luas wilayah kecamatan Banguntapan 28,48 km2 dengan jumlah penduduk sebanyak 91.355 jiwa.

Laporan PROMKES


LAPORAN PELAKSANAAN
PROGRAM PROMOSI KESEHATAN
KELOMPOK “KUNIR ASEM”


Laporan ini dalam rangka pembelajaran praktikum KIE (Komunikasi Informasi dan Edukasi) Promosi Kesehatan di Masyarakat sekaligus sebagai bagian dari persyaratan menyelesaikan kegiatan praktikum KIE






Disusun Oleh Kelompok V:


Rita Chandra Irawaty (11762041)
Rina Saputri (11762042)
Siti khairatun Hisan (11762047)
Tri Muji S. (11762048)
Tofan Pranoto (11762049)
Wahyu Irna Wati (11762052)
Welinda Dyah Ayu (11762053)
Winda Abdulrahman (11762054)


Lokasi Promosi Kesehatan : Kecamatan Banguntapan, Bantul.
Diajukan Kepada : Farida, M.Si, Apt

Rabu, 26 Oktober 2011

Afiafit X-tra


komposisi :
- Ganoderma lucidum
- Eurycoma longifolia 
- Pimpinella pruacen     
- Nigella sativa semen   
- Zingiber officinale     
- Piper retrofractum     
- Tribulus terrestris   
  

Selasa, 25 Oktober 2011

MERIT®

Komposisi :
1. Guazumae Folium
2. Rhei Radix
3. Granati Fructus

Khasiat : pelangsing
1. Guazumae Folium
Zat aktif :
Secara umum, zat utama yang terkandung dari seluruh bagian tanaman adalah tanin dan musilago. Kandungan lainnya yaitu resin, flavonoid, karotenoid, asam fenolat, zat pahit, karbohidrat, kafein, terpen, juga senyawa – senyawa lain seperti sterol, beta-sitosterol, friedelin-3-alfa-asetat, friedelin -3-beta-ol,alkoloida serta karbohidrat dan minyak lemak.

Zat yang berkhasiat pelangsing :
Tanin yang banyak terkandung di bagian daun, mampu mengurangi penyerapan makanan dengan cara mengendapkan mukosa protein yang ada dalam permukaan usus. Sementara itu, musilago yang berbentuk lendir bersifat sebagai pelicin. Dengan adanya musilago, absorbsi usus terhadap makanan dapat dikurangi. Hal ini yang yang menjadi alasan banyaknya daun jati belanda yang dimanfaatkan sebagai obat susut perut dan pelangsing. Dalam perkembangannya, daun jati belanda juga banyak dimanfaatkan untuk mengatasi penyakit kolesterol.

Struktur tannin















 Struktur musilago






















2. Rhei Radix
Zat aktif (menurut Kathi J. Kemper) :
Anthranoids, khususnya anthraquinone glycosides : rhein (sennosides A dan B), aloe-emodin, physcion
Oxalic acid
Tannins (5% - 10%): gallotannin, catechin, procyanidin
Lainya : pectin, phenolic carboxylic acids

Zat aktif yang berkhasiat pelangsing :
Rhein (sennosides A dan B). Zat ini memiliki efek laksatif sehingga membantu dalam penurunan berat badan.
Sennoside A & B (C42H38O20)


















Evidence Base :
Regionally differential effects of sennoside A on spontaneous contractions of colon in mice.
Kobayashi M, Yamaguchi T, Odaka T, Nakamura T, Tsuchiya S, Yokosuka O, Yano S.
Department of Medicine and Clinical Oncology, Graduate School of Medicine, Chiba University, Chiba, Japan. rinko_kobayashi@yahoo.co.jp
Abstract
Sennosides, the most popular irritant laxatives, cause purgative actions in the intestine through biotransformation to rhein anthrone; however, the underlying mechanisms remain unclear. The purpose of this study was to define colonic motor actions of sennoside A with special reference to purgative action. Mice received a single oral dose of 30 mg/kg sennoside A, and the colon was removed about 6 hr later. Contractions of longitudinal and circular muscles were recorded using an isometric force transducer and a pressure transducer, respectively. In longitudinal muscle preparations, spontaneous contractions were augmented in distal colon compared to control. In circular muscle preparations, contractions were reduced in the proximal colon, but increased in the distal colon. Particularly in the proximal colon, the frequency of high-amplitude contraction was reduced. In the control group, non-adrenergic, non-cholinergic treatment decreased the amplitude of contractions in the proximal colon, but not in the distal colon. In the sennoside A group, non-adrenergic, non-cholinergic treatment only slightly depressed the amplitude of contractions in the proximal and distal colon. To confirm a causal relationship between luminal prostaglandin level and purgative action of sennoside A, the mice were treated with indomethacin. Significant changes induced by sennoside A were attenuated by indomethacin treatment. The present study indicates that spontaneous motility is inhibited by sennoside A in the proximal colon, but accelerated in the distal colon, and that effects are associated with luminal prostanoid level and only partially with cholinergic nerve mediation.

Efek toksisitas dari senyawa sennosides A dan B :
Cytotoxicity of rhein, the active metabolite of sennoside laxatives, is reduced by multidrug resistance-associated protein 1.
van Gorkom BA, Timmer-Bosscha H, de Jong S, van der Kolk DM, Kleibeuker JH, de Vries EG.
Department of Gastroenterology, University Hospital, PO Box 30.001, 9700 RB Groningen, The Netherlands.
Abstract
Anthranoid laxatives, belonging to the anthraquinones as do anthracyclines, possibly increase colorectal cancer risk. Anthracyclines interfere with topoisomerase II, intercalate DNA and are substrates for P-glycoprotein and multidrug resistance-associated protein 1. P-glycoprotein and multidrug resistance-associated protein 1 protect colonic epithelial cells against xenobiotics. The aim of this study was to analyse the interference of anthranoids with these natural defence mechanisms and the direct cytotoxicity of anthranoids in cancer cell lines expressing these mechanisms in varying combinations. A cytotoxicity profile of rhein, aloe emodin and danthron was established in related cell lines exhibiting different levels of topoisomerases, multidrug resistance-associated protein 1 and P-glycoprotein. Interaction of rhein with multidrug resistance-associated protein 1 was studied by carboxy fluorescein efflux and direct cytotoxicity by apoptosis induction. Rhein was less cytotoxic in the multidrug resistance-associated protein 1 overexpressing GLC4/ADR cell line compared to GLC4. Multidrug resistance-associated protein 1 inhibition with MK571 increased rhein cytotoxicity. Carboxy fluorescein efflux was blocked by rhein. No P-glycoprotein dependent rhein efflux was observed, nor was topoisomerase II responsible for reduced toxicity. Rhein induced apoptosis but did not intercalate DNA. Aloe emodin and danthron were no substrates for MDR mechanisms. Rhein is a substrate for multidrug resistance-associated protein 1 and induces apoptosis. It could therefore render the colonic epithelium sensitive to cytotoxic agents, apart from being toxic in itself.