INSULIN DAN ANTI DIABETIK ORAL Dr. dr. NURDIANA, M.Kes LAB. FARMAKOLOGI FK UNIBRAW MALANG

1. INSULIN DAN ANTI DIABETIK ORAL Dr. dr. NURDIANA, M.Kes LAB. FARMAKOLOGI FK UNIBRAW MALANG

2. PANKREAS 1 juta pulau langerhans memproduksi hormon (lihat tabel) SEL B PANKREAS SINTESIS oleh DNA ATAU RNA INSULIN BM : 5808 2 RANTAI : RANTAI A RANTAI B lihat gambar RANTAI DISULFIDA PROINSULIN RANTAI TUNGGAL, PANJANG DIPROSES DALAM GOLGI APPARATUS MENJADI INSULIN (HIDROLISA), SEGMEN SISANYA C-PEPTIDA INSULIN DISEKRESI SETARA DENGAN STIMULAN/ SECRETAGOGUES

4. STRUKTUR PROINSULIN MANUSIA

5. SEKRESI INSULIN Insulin dilepas dari sel B pankreas : Low basal rate : tanpa stimuli dari luar Much higher stimulated rate : ada stimuli dari luar terutama glukosa stimuli lain  mannose, asam amino : leucine,arginin, rangs vagus EFEK FISIOLOGI INSULIN MENURUNKAN KADAR GULA DARAH Interaksi glukosa-insulin neg feed back mengatur agar kadar gula darah segera kembali normal

6. FARMAKODINAMIK INSULIN INSULIN AGONIS INSULIN SIRKULASI  BERIKATAN DENGAN RESEPTOR PADA MEMBRAN SEL , MENGHASILKAN RESPON BIOLOGIS YANG SESUAI SIFAT KOMPLEKS IKATAN. TARGET TISSUE TERUTAMA : HATI, OTOT, JARINGAN LEMAK INSULIN BERIKATAN DG RESEPTOR DG SPESIFISITAS DAN AFINITAS TINGGI (picomolar). FARMAKOKINETIK INSULIN INSULIN TIDAK DIBERIKAN PERORAL KARENA DIRUSAK OLEH PEPTIDASE DI G.I.T. , SEHINGGA DIBERIKAN SC, IM, IV, NASAL SPRAY DAN IMPLANTABLE PUMP INSULIN  ABSORBSI  DARAH  CAIRAN EKSTRASEL  DISTRB HALF LIFE : ORG SEHAT, CEPAT, DL BEBERAPA MENIT DM, LBH LBT, KARENA BERIKATAN DG ANTIBODI METAB : LIVER, OTOT DAN GINJAL EKSKRESI : METABOLIT, FRAKSI KECIL YG T’BERUBAH  GINJAL

7. Efek fisiologis Insulin metab. glukosa • transport aktif glukosa utk masuk ke dl sel • * meningkatkan penggunaan glukosa oleh jar. tbh • * meningkatkan glikogenesis di otot dan hati • * oksidasi KH utk enersi di otot bergaris • Meningkatkan sintesis lemak di di jar lemak • glukoneogenesis , glikogenolisis • peningkatan sintesis protein dan as. nukleat pertumbh • oksidasi lemak utk enersi ketosis • insulin proses anabolik • glukosa produksi enersi • disimpan (storage)

8. Insulin hati otot Jar.lemak

9. Fluktuasi kadar glukosa dalam serum dipengaruhi faktor-faktor : • Glkogenolisis/glukoneogenesis • Penggunaan glukosa oleh sel perifer • Jumlah reseptor insulin pada sel • Kadar antibodi insulin • Hormon yg mempengaruhi metab. Glukosa : insulin, glucagon, cortison, epinefrin dan GH • Insulin, vit C, chromium me metab glukosa. Exercise me penggn glukosa • KONDISI PATOLOGIS • Ggn sekresi insulin : meningkat : reactive hypoglycemia, insulinoma • menurun : defisiensi insulin  DM • DM  bisa disebabkan antibodi yg menghalangi kerja insulin atau kurangnya • reseptor insulin, kemampuan jar menggunakan glukosa (obesitas)

10. Sifat preparat insulin • A. Tipe dan lama kerja • Ultra short acting, very rapid onset, short duration • Short acting, rapid onset of action • Intermediate-acting • Long – acting, slow onset of action • tabel

12. Degradasi insulin • - dilakukan oleh hati dan ginjal, membersihkan insulin dari sirkulasi • Cara hidrolisis ikatan disulfid antara rantai A dan B melalui kerja insulinase • (glutathione insulin transhidrogenase) proteolysis • Insulin endogen hati : 60 % • ginjal 35-40 % • Insulin eksogen, sebaliknya • Circulating insulin half life 3-5’ • Pengukuran insulin • RIA picomolar, berdasarkan reaksi dg antibodi • bisa mengukur insulin sapi, babi dan manusia • basal insulin value, 5 – 15 U/ml (30-90 mol/L)pada manusia, kadar puncak 60-90 U/ml (360-540 mol/L), pada saat makan.

13. TERAPI INSULIN • DIABETES TIPE 1 INSULIN DEPENDENT GROUP • DIABETES TIPE 2TDK BTH INSULIN UTK SURVIVAL, TP UTK OPTIMAL HEALTH • “GLYCEMIC CONTROL” PADA DM • DM TIPE 1 COMPREHENSIVE SELF-MANAGEMENT TRAINING, DIMULAI SESUDAH PUBERTAS • UMUR 7 TH , TDK BOLEH KONTROL KETAT, KARENA HIPOGLIKEMI DPTBRAIN DAMAGE • KOMPLIKASI TERAPI INSULIN • HIPOGLIKEMI  PENYEBAB : TERLAMBAT MAKAN • AKTIVITAS FISIK TDK SESUAI • DOSIS INSULIN > UTK KEPERLUAN • MENDADAK

14. ORANG TUA DG DMMENDPT “LONG ACTING INSULIN” -AUTONOMIC WARNING : SIMP : Takikardi, palpitasi,sweating, tremor SIGNAL P.SIMP : Nausea, lapar -KEGGL FS CNS : Mental confusion, bizzare behaviour, coma TERAPI HIPOGLIKEMIA Berikan glukosa  * mild hipoglycemia, sadar, dpt menelan : makanan manis * more severe, stupor  20-50 ml gluc 50 % i.v glucagon 1 mg s.c atau i.m. B. IMMUNOPATHOLOGY OF INSULIN THERAPY Insulin antibodi  IgA, IgD, IgE, IgG dan IgM 2 gangguan immunitas pd DM dg terapi insulin : 1 Alergi insulin : urtikaria , syok anafilaktik,nodul ditempat suntikan makin murni insulin, alergi

15. 2. Immune insulin resistance : • a. Tx insulin : low titer IgG anti insulin antibodies • b. a+ terapi insulin kurang murni +jar kurang sensitif insulinIgG • antiinsulin antibodies • kebutuhan insulin > 200 U/hari • LIPODISTROPI PADA TEMPAT INJEKSI • Sudah berkurang karena insulin babi dan manusia yang murni, pH netral. • Sekarang terjadi hipertropi lemak s.c bl disuntik berulang ditempat yg sama •  liposuction

17. Type 2 diabetes: the role of insulin resistance and -cell failure Insulin resistance Hyperinsulinaemia Increasing insulin resistance -cell failure + Impaired glucose tolerance Type 2 diabetes Adapted from: Reaven GM. Diabetes 1988;37:1595–1607 and Beck-Nielsen H, Groop LC. J Clin Invest 1994;94:1714–1721

18. OAD (oral anti diabetic)

19. INSULIN SECRETAGOGUES 1. SULFONYLUREA : GENERASI 1 : CHLORPROPAMIDE, TOLBUTAMIDE, TOLAZAMIDE GENERASI 2 : GLYBURIDE, GLIPIZIDE, GLIMEPIRIDE kelebihan generasi 2 : efek samping dan interaksi obat lbh sedikit hati-hati pada pasien dg penderita peny.jantung dan orang tua  hipoglikemia 2. MEGLITINIDE : REPAGLINIDE onset of action cepat, peak conc.1 jam, duration of act 5-8 jam kontrol gula darah postprandial 3. D-PHENYLALANINE DERIVATIVE : NATEGLINIDE digunakan sebelum makan, masa kerja pendek (<4jam). tdk perlu titrasi dosis, insiden hipoglikemi rendah

20. Sulphonylureas • 1st generation : chlorpropamid • 2nd generation : gliclazide, glipizide gliburid, glibenklamid • 3nd generation : glimepiride Others : Meglitinide : Repaglinide  utk DM tipe 2 yg alergi sulfonylurea Nateglinide Stimulate beta cells to release insulin (assumes there is residual beta cell activity) • Side effects: hypoglycaemia, weight gain, GI disturbances, headache

21. EFEK SAMPING Sulfonilurea-nausea, vomiting -jaundice -agranulositosis, anemia aplastik -teratogenik -toksik : Hipoglikemi

22. Sulfonylureas: Mechanism of Action 1 Intestine: glucose absorption 2 Muscle and adipose tissue:glucose uptake Insulin resistance Blood glucose 4 Liver: hepaticglucose output Insulinresistance • Pancreas: insulin secretionSulfonylureas • insulin secretion DeFronzo RA. Diabetes. 1988;37:667-687. Lebovitz HE. In Joslin's Diabetes Mellitus. 1994:508-529

23. C Meglitinides: Mechanism of Action 2 Muscle and adipose tissue:glucose uptake 1 Intestine: glucose absorption Insulin resistance Blood glucose 4 Liver: hepatic glucose output Insulinresistance 3 Pancreas: insulin secretion Meglitinides Insulin secretion Wolffenbuttel BHR. Eur J Clin Pharmacol. 1993;45:113-116.

24. Biguanides Metformin Drug of choice in obese patients only Monotherapy or adjunct Decreases gluconeogenesis Increases peripheral uptake of glucose in to cells  Basal & post prandial glucose levels Weight neutral Increased insulin sensitivity Beneficial effect on plasma lipid profile

25. Metformin: Mechanism of Action 2 Muscle and adipose tissue:glucose uptakeMetformin glucose utilization 1 Intestine: glucose absorption Insulin resistance Blood glucose 4 Liver: hepatic glucose output Metformin HGO Insulinresistance 3 Pancreas: insulin secretion DeFronzo RA et al. J Clin Endocrinol Metab. 1991;73:1294-1301.

26. Metformin cont’d • Side effects • Nausea, vomiting, diarrhoea, abdominal discomfort

27. a-Glucosidase Inhibitors :Mechanism of Action 1 Intestine: glucose absorptionAcarbose glucose absorption secondaryto digestion of carbohydrate 2 Muscle and adipose tissue: glucose uptake Insulin resistance Blood glucose 4 Liver: hepaticglucose output Insulinresistance 3 Pancreas: insulin secretion Amatruda JM. In: Diabetes Mellitus. 1996.

28. Alpha glucosidase inhibitors • Acarbose • monotherapy or adjunct • Inhibits intestinal enzyme, specific activity on sucrase, delaying digestion of starch and sucrose into absorbable monosaccharides such as glucose • Safe • Weight neutral

29. Acarbose cont’d • Side effects: • GI intolerance • flatulence, diarrhoea, abdominal distension & pain

30. Thiazolidinediones: Mechanism of Action Muscle and adipose tissue: Thiazolidinediones insulin resistance glucose uptake Intestine: glucose absorption Liver: hepatic glucose output Thiazolidinediones HGO Blood glucose Pancreas: insulin secretion Improve b-cell function Whitcomb RW et al. In: Diabetes Mellitus. 1996.Cavaghan MK et al. J Clin Invest. 1997;100:530-537.Ehrmann DA et al. J Clin Endocrinol Metab. 1997;82:2108-2116.

31. The PPAR Family(Peroxisome proliferator-activated receptor) Fibrates Thiazolidinediones Fatty acids Ligand PPAR-a PPAR-g PPAR-d Receptor Effect on: Lipoproteinexpression Peroxisomeproliferation Lipidsynthesis Carbohydratemetabolism Saltiel AR, Olefsky JM. Diabetes. 1996;45:1661-1669.

32. Thiazolidinediones • Counteract insulin resistance • Bind to PPAR-gamma (receptor), forming a complex promoting transcription of genes sensitive to insulin. • Receptors are present in skeletal muscle, adipose tissue &liver, thereby promoting uptake of fatty acids &glucose at these sites

33. Thiazolidinedionescont’d • Pioglitazone, rosiglitazone • Adjunct with either metformin or SU

34. Thiazolidinediones • ? Alternative to insulin • Side effects: • oedema, weight gain, GI disturbances, headache, dizziness

35. Sites of Action by Therapeutic Options PANCREAS LIVER Therapy: Biguanides Thiazolidinediones Therapy: Sulfonylureas Meglitinides Insulin DECREASED INSULIN SECRETION INCREASED GLUCOSE PRODUCTION HYPERGLYCEMIA DECREASED PERIPHERAL GLUCOSE UPTAKE INTESTINE ADIPOSE TISSUE INCREASE GLUCOSE ABSORPTION Therapy: Alpha-glucosidase inhibitors Therapy: Thiazolidinediones (Biguanides) MUSCLE Adapted from Sonnenberg and Kotchen Curr Opin Nephrol Hypertens 1998;7(5):551-555.

36. EFEK SAMPING Sulfonilurea-nausea, vomiting -jaundice -agranulositosis, anemia aplastik -teratogenik -toksik : Hipoglikemi Biguanid :-asidosis laktat -nausea, diare -menghambat absorpsi vit.B12 Thiazolidindione -jarang hipoglikemi -udema, anemia ringan Glukosidase inhibitor: -flatulen, diare, nyeri abdomen

37. TAHAPAN TERAPI DIABETES MELITUS Diagnosis Health education Diet, exercise, weight control Oral agent monotherapy SU, metformin, meglitinide, thiazolidinedione, acarbose Oral agent combination therapy (2 different classes) Insulin + oral agent Insulin

38. Stepwise management of type 2 diabetes Insulin ± oral agents Oral combination Oral monotherapy Diet & exercise