Sains Malaysiana 40(11)(2011): 1247–1253

 

Differential Protein Expression in Senescent Human Skin Fibroblasts and Stress

Induced Premature Senescence (SIPS) Fibroblasts

(Perbezaan Pengekspresan Protein dalam Fibroblas Kulit Manusia Senesen dan Fibroblas

Senesen Pramatang Teraruh Tekanan)

 

Goon Jo Aan*, Haryati Ahmad Hairi, Suzana Makpol & Wan Zurinah Wan Ngah

Jabatan Biokimia, Fakulti Perubatan, Universiti Kebangsaan Malaysia, 50300 Kuala Lumpur, Malaysia

 

Mariati Abdul Rahman

Jabatan Biologi Mulut Klinikal, Fakulti Pergigian, Universiti Kebangsaan Malaysia

50300 Kuala Lumpur, Malaysia

 

Saiful Anuar Karsani

Institut Sains Biologi, Fakulti Sains, Universiti Malaya, 50603 Kuala Lumpur, Malaysia

 

Received: 28 April 2010 / Accepted: 22 February 2011

 

ABSTRACT

 

Replicative senescence of human diploid fibroblasts (HDFs) occurs when cells lose their capacity to proliferate and enter a phase of irreversible growth arrest. Stress-induced premature senescence (SIPS) on the other hand is caused by subcytotoxic concentrations of various oxidants which trigger accelerated cellular senescence. In this study, a SIPS model was established by exposing human diploid fibroblasts (HDFs) to 20 μM H2O2 for two weeks. A proteomic comparison between young, senescent and SIPS cells was done using two dimensional gel electrophoresis (2DGE) to elucidate the changes in protein expression associated with cellular aging. Our analysis showed that 28 protein spots were differentially expressed in senescent cells whereas 10 protein spots were differentially expressed in SIPS as compared to young cells. Three similar protein spots were differentially expressed in both senescent and SIPS cells when compared to the young cells. These results indicate that a difference in protein expression exists between senescent cells and SIPS cells compared to young cells.

 

Keywords: Fibroblast; senescent cells; SIPS; two dimensional gel electrophoresis (2DGE)

 

ABSTRAK

Senesen replikatif fibroblas diploid manusia berlaku apabila sel hilang kapasiti untuk berproliferasi dan memasuki fasa pertumbuhan terencat secara tidak berbalik. Senesen pramatang teraruh tekanan (SIPS) pula berpunca daripada kepekatan subsitotoksik pelbagai oksidan yang boleh mengaruh senesen sel. Dalam kajian ini, model SIPS telah dihasilkan dengan mendedahkan fibroblas diploid manusia kepada 20 μM H2O2 selama dua minggu. Suatu perbandingan proteomik antara sel muda, sel tua dan model SIPS telah dilakukan dengan menggunakan elektroforesis gel dua dimensi (2DGE) untuk menunjukkan perubahan dalam pengekspresan protein berkaitan dengan penuaan selular. Keputusan menunjukkan 28 titik protein yang diekspreskan secara berbeza dalam sel senesen manakala SIPS menunjukkan 10 titik protein yang diekspreskan secara berbeza berbanding dengan sel muda. Tiga titik protein yang sama diekspreskan secara berbeza dalam kedua-dua sel senesen dan SIPS berbanding sel muda. Keputusan ini menunjukkan bahawa terdapat perbezaan dalam ekspresi protein antara sel senesen dan sel SIPS berbanding dengan sel muda.

 

Kata kunci: Elektroforesis gel dua dimensi; fibroblas; sel senesen; SIPS

 

REFERENCES

 

Bagnato, C., Thumar, J., Mayya, V., Hwang, S., Zebroski, H., Claffey, K.P., Haudenschild, C., Eng, J.K., Lundgren, D.H. & Han, D.K. 2007. Proteomics analysis of human coronary atherosclerotic plague. A feasibility study of direct tissue proteomics by liquid chromatography and randem mass spectrometry. Molecular and Cellular Proteomics 6.6. 1088-1102.

Bradford, M.M. 1976. A dye binding assay for protein. Analytical Biochemistry 72: 248-254.

Boraldi, F., Bini, L., Liberatori, S., Armini, A., Pallini, V., Tiozzo, R., Pasqualironchetti, I. & Quaglino, D. 2003. Proteome analysis of dermal fibroblasts cultured in vitro from human healthy subjects of different ages. Proteomics 3: 917-929.

Borlon, C., Debacq-Chainiaux, F., Hinrichs C., Scharffetter-Kochanek, K., Toussaint, O. & Wlaschek, M. 2007. The gene expression profile of psoralen plus UVA-induced premature senescence in skin fibroblasts resembles a combined DNA-damage and stress-induced cellular senescence response phenotype. Experimental Gerontology 42: 911-923.

Brack, C, Lithgow G.J., Osiewacs, H.D. & Toissaint, O. 2000. Molecular & Cellular Gerontology. EMBO Journal 19: 1929-1934.

Chen, Q.M., Tu, V.C. & Liu, J. 2000. Measurements of hydrogen peroxide induced premature senescence: senescence-associated β galactosidase and DNA synthesis index in human diploid fibroblasts with down-regulated p53 or Rb. Biogerontology 1: 335-339

Deaton, C.M. & Marlin, D.J. 2003. Exercise-associated oxidative stress. Clinical Techniquesin Equine Practice 2(3): 278-291.

de Magalhaes, J.P., Chainiaux, F., de Longueville, F., Mainfroid, V., Migeot, V., Marcq, L., Remacle, J., Salmon, M. & Toussaint, O. 2004. Gene expression and regulation in H2O2-induced premature senescence of human foreskin fibroblasts expressing or not telomerase. Experimental Gerontology 39: 1379-1389.

Dierick, J.F., Eliaters, F., Remacle, J., Raes, M., Fey, S.J., Larsen, P.M. & Toussaint, O. 2002a. Stress-induced premature senescence and replicative senescence are different phenotypes, proteomic evidence. Biochemical Pharmacology 64: 1011-1017.

Dierick, J.F., Kalume, D.E., Wenders, F., Salmon, M., Dieu, M., Ress, M., Roepstorff, P. & Toissaint, O. 2002b. Identification of 30 protein species involved in replicative senescence and stress-induced premature senescence. FEBS Letters 531: 499-504.

Dimri, G.P., Lee, X., Basile, G., Acosta, M., Scott, G., Roskelley, C., Medrano, E.E., Linskens, M., Rubelj, I., Pereira-Smith, O., Peacocke, M. & Campisi, J. 1995. A biomarker that identifies senescent human cells in culture and in aging skin in vivo. Proceedings of the National Academy of Sciences USA 92: 9363-9367.

Duan, J., Duan, J., Zhang, Z. & Tong, T. 2005. Irreversible cellular senescence induced by prolonged exposure to hydrogen peroxide involves DNA-damage-and-repair genes and telomere shortening. The International Journal of Biochemistry & Cell Biology 37: 1407-1420.

Frippiat, C., Remacle, J. & Toussaint, O. 2003. Down-regulation and decreased activity of cyclin-dependent kinase 2 in H2O2 –induced premature senescence. The International Journal of Biochemistry & Cell Biology 35: 246-254.

Gork, A. 2004. 2-D Electrophoresis. Principles and Methods. Handbooks from GE Healthcare. Sweden

Grune, T., Reinheckel, T. & Davies, K.J. 2003. Degradation of oxidized proteins in mammalian cells. The Federation of American Societies for Experimental Biology Journal 11: 526-534.

Hayflick, L. & Moorhead, P.S. 1961. The serial cultivation of human diploid cell strains. Experimental Cell Research. 25: 585-621

Harman, D. 1956. Aging: A theory based on free radical and radiation chemistry. The Journal of Gerontology. 11: 298-300.

Puricelli, L., Iori, E., Milioni, R., Arrigoni, G., James, P., Vedoyato, M. & Tessari, P. 2006. Proteome analysis of cultured fibroblasts from type 1 diabetic patients and normal subjects. The Journal of Clinical Endocrinology & Metabolism 91(9): 3507-3514.

Toussaint, O., Medrano, E.E. & von Zglinicki, T. 2000. Stress-induced premature senescence (SIPS) of human diploid fibroblasts and melanocytes. Experimental Gerontology 35: 927-945.

Toussaint, O., Raed, M., & Remackle, J. 1999. Ageing as a multi-step process characterized by a lowering of entropy production leading the cell to a sequence of defined stages. Mechanisms of Ageing and Development 61: 45-54.

Toussaint, O., Remacle, J., Dierick, J.F., Pascal, T., Frippiat, C., Royer, V. & Chainiaux, F. 2002. Approach of evolutionary theories of ageing, stress, senescence-like phenotypes, caloric restriction and hormesis from the view point of far-equilibrium thermodynamics. Mechanisms of Ageing and Development 123: 937-946.

Zhang, J., Keene, C.D., Pan, C., Montine, S.K. & Montine, T.J. 2008. Proteomics of human neurodegenerative diseases. Journal of Neuropathology & Experimental Neurology 67(10): 923-932.

 

*Corresponding author; email: joaan@medic.ukm.my

 

 

 

 

 

 

 

 
previous