Abstrak

HDAC merupakan penentu dalam peristiwa epigenetic sehingga harus dihambat.Penghambat menggunakan molekul kecil,dengan memperhatikan jarak ikatandan posisi ikatan.Guna mendapatkan penghambat yang baik maka diharapkan molekulkecil tersebut mampu berikatan dengan membentuk formasi Pi stacking,sehinggaenergi yang terpakai menjadi kecil.Metoda yang digunakan adalah doking dengan autodok vina dengan grid.Hasil penelitian menunjukan ikatan pi stacking terbentuk antara molekul Dietilsinamamid dengan Arginin,Leisin dll.Sehingga dapat menjadi kandidat penghambatyang baik.Kesimpulan Dietilsinamamide dapat membentuk posisi Pi stacking dengan HDAC

 

Kata Kunci: Pi stacking, HDAC inhibitor, in-silico

 

Abstract

HDAC is a determinant in epigenetic events that should be blocked . Using a small molecule inhibitor , with due regard to the bond distances and bond positions . In order to get a good inhibitor it is expected that the small molecule is able to bind to the formation pi stacking , so that the energy that used to be small . The methods used are docking with Davina autodok the grid. The results showed the bond between molecules pi stacking terbentu Dietilsinamamid with Arginine, Leisin etc. So that can be a good candidate inhibitor. Conclusion Dietilsinamamide can form pi stacking position with HDAC

 

Keywords: Pi stacking , HDAC inhibitors , in-silico

Cheng, HL; Gu, Y; Mostoslavsky, R; Saito, S et al. (2003), “Developmental defects and p53 hyperacetylation in Sir2 homolog (SIRT1)-deficient miceâ€, Proc Natl Acad Sci, Vol.100, 10794-10799.

Ruijter, AJM; Van Gennip, AH; Caron, HN; Kemp, S et al. (2003), “Histone deacetylases (HDACs): characterization of the classical HDAC familyâ€, Biochem J, Vol. 370,737–749.

Finnin, MS; Donigian, JR; Cohen, A; Richon, VM et al. (1999), “Structures of a histone deacetylase homologue bound to the TSA and SAHA inhibitorsâ€, Nature, Vol.401, 188,3.

Haberland M, Montgomery RL, Olson EN (2009). “The many roles of histone deacetylases in development and physiology: implications for disease and therapy. “ Nat Rev Genet, 10,32-42.

Gui CY, Ngo L, Xu WS, et al (2004). “Histone deacetylase (HDAC) inhibitor activation of p21WAF1 involves changes in promoter-associated proteins, including HDAC1.â€Proc Natl Acad Sci USA, 101, 1241–6.

Takai N, Narahara H (2010a). “Histone Deacetylase Inhibitor Therapy In Epithelial Ovarian Cancer.â€J Oncol.

Takai N, Narahara H (2010b). “Preclinical Studies Of Chemotherapy Using Histone Deacetylase Inhibitors In Endometrial Cancer.â€Obstet Gynecol Int

Anton, VB; Sujith, VW and Mary Kay HP (2007), “Structural requirements of HDAC inhibitors: SAHA analogs functionalized adjacent to the hydroxamic acidâ€, Bioorganic Chemistry and Organic letters, Vol.17, 2216-2219.

Miller, TA; Witter, DJ; Belvedere, S et al(2003), “Histone deacetylase inhibitorsâ€, J MedChem, Vol.46, 5097 – 5116.

Yoshida, M; Kijima, M; Akita, M; Beppu, T (1990), “Potent and specific inhibition of Mammalian histone deacetylase both in vivo and in vitro by trichostatin Aâ€, J Biol chem, Vol. 265, 17174 – 17179.

Kumar, Ranjit. (2005)Research Methodology-A Step-by-Step Guide forBeginners,(2nd.ed.). Singapore, Pearson Education.

Difai Wang (2009).“Computational Studies on the Histone Deacetylases and the Design of Selective Histone Deacetylase Inhibitors.†Curr Top Med Chem. 2009 ; 9(3): 241–256.

James Folzman. (1993). “Biostatistics: Experimental Design and Statistical Inference.â€Oxford University Press, USA; 1th edition.