 |
 |
 |
 |
 |
 |
Sains Malaysiana 48(1)(2019): 121–127
http://dx.doi.org/10.17576/jsm-2019-4801-14
Cytotoxicity,
Proliferation and Migration Rate Assessments of Human Dermal Fibroblast Adult
Cells using Zingiber zerumbet Extract
(Penilaian
Kesitotoksikan, Proliferasi dan Kadar Migrasi Sel Dewasa Fibroblas
Derma Manusia menggunakan Ekstrak Zingiber zerumbet)
MAZLYZAM ABDUL LATIF1, FARAH WAHIDA IBRAHIM1, SITI AISYAH ARSHAD1, CHUA KIEN HUI2, NURUL FARHANA JUFRI1 & ASMAH HAMID1*
1Programme of
Biomedical Science, Centre of Health & Applied Sciences, Faculty of Health
Sciences, Universiti Kebangsaan Malaysia, Jalan Raja Muda Abdul Aziz, 50300
Kuala Lumpur, Federal Territory, Malaysia
2Department of
Physiology, Faculty of Medicine, Universiti Kebangsaan Malaysia, Jalan Yaacob
Latif, Bandar Tun Razak, 56000 Cheras, Kuala Lumpur, Federal Territory, Malaysia
Received: 30 March 2018/Accepted: 8 August 2018
ABSTRACT
Zingiber zerumbet is a plant that is traditionally consumed in
many countries, including Malaysia due to its therapeutic properties.
Previously it has been proven to inhibit migration and proliferation of cancer
cells. However, its effects on normal cells are still unknown and would be the
main focus of this study. The cytotoxicity along with proliferation and migration
activities were evaluated against human dermal fibroblast adult cell line (HDF-a)
using MTT [3-(4,5-dimethylthiazol-2-yl)-2,5-diphenyltetrazolium],
proliferation and scratch assays. The cytotoxicity effect was determined
following 24 h of treatment by ethyl acetate Z. zerumbet extracts while
proliferation assay was conducted at different concentrations (500, 750, 1000,
1250 and 1500 μg/mL) at 24, 48 and 72 h. The cell migration rate was
determined by scratch assay in 6-well culture plate using 10 μL pipette
tip following 80% confluency at optimum concentration (750 μg/mL) of Z.
zerumbet at different time points. Migration rate was scored at every 24 h
using digital camera connected to the inverted microscope. The results from
cytotoxicity test showed no IC50 values were observed for Z.
zerumbet extract as compared to the positive control (menadione).
Proliferation assay exhibited highest cell viability (137%) at 750 μg/mL.
The rate of cell migration increased following treatment with Z. zerumbet extract
after 48 h. However, the result was not significantly different when compared
to the control. In conclusion, Z. zerumbet ethyl acetate extract is able
to induce cell proliferation and potentially promoting migration rate of wound
healing in in-vitro model.
Keywords: Dermal; fibrolast; migration; proliferation; wound
healing; Zingiber zerumbet
ABSTRAK
Zingiber zerumbet merupakan tumbuhan ubatan tradisi yang digunakan
di kebanyakan negara termasuk Malaysia disebabkan kesan teraputiknya.
Kajian terdahulu telah membuktikan ia dapat menghalang migrasi dan
proliferasi sel kanser. Namun, kesan pada sel normal masih belum
diketahui dan menjadi fokus kajian ini. Kesan kesitotoksikan serta
aktiviti proliferasi dan migrasi terhadap sel dewasa derma fibroblas
manusia (HDF-a)
dikaji menggunakan asai MTT [3-(4,5-dimetiltiazol-2-il)-2,5-difeniltetrazolium],
proliferasi dan calaran. Kesan kesitotoksikan ditentukan selepas
rawatan selama 24 jam ekstrak etil asetat Z. zerumbet dan
asai proliferasi ditentukan pada kepekatan berbeza (500, 750, 1000,
1250 dan 1500 μg/mL) pada 24, 48 dan 72 jam. Kadar migrasi
sel ditentukan dengan asai calaran pada jangka waktu berbeza dalam
piring kultur 6 telaga menggunakan hujung tip pipet 10 μL selepas
sel mencapai 80% konfluensi pada kepekatan optimum (750 μg/mL)
Z. zerumbet. Kadar migrasi sel ditentukan setiap 24 jam menggunakan
kamera digital yang disambung pada mikroskop. Keputusan daripada
ujian kesitotoksikan menunjukkan tiada nilai IC50 diperhatikan pada ekstrak Z. zerumbet
apabila dibandingkan dengan kawalan positif (menadion). Asai
proliferasi menunjukkan keviabelan sel yang tinggi (137%) pada kepekatan
750 μg/mL. Kadar migrasi sel meningkat selepas 48 jam rawatan
dengan ekstrak Z. zerumbet. Namun, keputusan menunjukkan
tiada perbezaan signifikan apabila dibandingkan dengan kawalan.
Kesimpulannya, ekstrak etil asetat Z. zerumbet merangsang
proliferasi dan kadar migrasi sel melalui model penyembuhan luka
in vitro.
Kata kunci: Derma; fibrolas;
migrasi; proliferasi; penyembuhan luka; Zingiber zerumbet REFERENCES
Chien, T.Y., Chen,
L.G., Lee, C.J., Lee, F.Y. & Wang, C.C. 2008. Anti-inflammatory
constituents of Zingiber zerumbet. Food Chemistry 110(3):
584-589.
Davis, S.C. & Perez, R. 2009. Cosmeceuticals and natural
products: Wound healing. Clinics in Dermatology 27(5): 502-506.
Demma, J., Engidawork, E. & Hellman, B. 2009. Potential
genotoxicity of plant extracts used in Ethiopian traditional medicine. Journal
of Ethnopharmacol. 122(1): 136-142.
Dorai, A.A. 2012. Wound care with traditional, complementary
and alternative medicine. Indian Journal of Plastic Surgery 45(2):
418-424.
D’souza, K.M., Malhotra, R., Philip, J.L., Staron, M.L.,
Theccanat, T., Jeevanandam, V. & Akhter, S.A. 2011. G protein-coupled
receptor kinase-2 is a novel regulator of collagen synthesis in adult human
cardiac fibroblasts. The Journal of Biological Chemistry 286(17):
15507-15516.
Greg, D. 2005. Wound Pharmacology Sawma, Monash
University. Presented at SAWMA Education Night.
Hadjikakou, S.K. & Hadjiliadis, N. 2009.
Antiproliferative and anti-tumor activity of organotin compounds. Coordination
Chemistry Reviews 253(1): 235-249.
Hamid, A., Ibrahim, F.W., Ming, T.H., Nasrom, M.N., Eusoff,
N., Husain, K. & Latif, M.A. 2018. Zingiber zerumbet L. (Smith)
extract alleviates the ethanol-induced brain damage via its antioxidant
activity. BMC Complementary and Alternative Medicine 18(1): 101.
Hamid, A., Rajab, N.F., Shen, T.S. & Nasrom, M.N. 2017.
Cytotoxic and genotoxic effects of zerumbone on Wehi 7.2 wild type murine
thymoma cells. Journal of Agricultural Science 9(13): 1-13.
Harishkumar, M., Masatoshi, Y., Hiroshi, S., Tsuyomu, I.
& Masugi, M. 2013. Revealing the mechanism of in vitro wound healing
properties of Citrus tamurana extract. Biomed. Research International 2013: 963457.
How, F.N.F., Crouse, K.A., Tahir, M., Tarafder, M.T.H. &
Cowley, A.R. 2008. Synthesis, characterization and biological studies of
s-benzyl-b-n-(benzoyl) dithiocarbazate and its metal complexes. Polyhedron 27:
3325-3329.
Howell-Jones, R.S., Wilson, M.J., Hill, K.E., Howard, A.J.,
Price, P.E. & Thomas, D.W. 2005. A review of the microbiology, antibiotic
usage and resistance in chronic skin wounds. Journal of Antimicrobial Chemotherapy 55(2): 143-149.
Kon, K. & Rai, M. 2014. Chapter 11-Natural remedies for
the treatment of wounds and wound infection. In Microbiology for Surgical
Infections. Amsterdam: Academic Press. pp. 187-203.
Kulac, M., Aktas, C., Tulubas, F., Uygur, R., Kanter, M.,
Erboga, M., Ceber, M., Topcu, B. & Ozen, O.A. 2013. The effects of topical
treatment with curcumin on burn wound healing in rats. Journal of Molecular
Histology 44(1): 83-90.
Latif, M.A., Zaki, M.Z., Leng, T.M., Rahman, N.H., Arshad,
S.A. & Hamid, A. 2015. Alocasia denudata Engler treatment enhance
open wound healing activities in Wistar rat’s skin. Journal of
Ethnopharmacology 176: 258-267.
Lodish, H., Berk, A. & Lawrence, Z.S. 2000. Integrating
cells into tissues. In Molecular Cell Biology. 4th ed. New York:
Freeman.
Mosmann, T. 1983. Rapid colorimetric assay for cellular
growth and survival: Application to proliferation and cytotoxicity assays. Journal
of Immunological Methods 65(1-2): 55-63.
Nhareet, S.M. & Nur, S.M.H. 2003. Anti-inflammatory
property of ethanol and water extracts of Zingiber zerumbet. Indian Journal
of Pharmacology 35: 181-182.
Pari, L. & Amarnath Satheesh, M. 2004. Antidiabetic
activity of Boerhaavia diffusa L.: Effect on hepatic key enzymes in
experimental diabetes. Journal of Ethnopharmacol. 91(1): 109-113.
Rahman, N.S.A., Salleh, L.M., Yaakob, H. & Majid, F.A.A.
2013. Cells migration potential of Quercus infectoria aqueous extract
evidenced in human skin fibroblast scratch assay method. Regenerative
Research 2(2): 43-47.
Raina, R., Parwez, S., Verma, P.K. & Pankaj, N.K. 2008.
Medicinal plants and their role in wound healing. VetScan 3(21): 1-7.
Rhee, S. 2009. Fibroblasts in three dimensional matrices:
Cell migration and matrix remodeling. Experimental & Molecular Medicine 41(12):
858-865.
Robson, M.C. 1997. The role of growth factors in the healing
of chronic wounds. Wound Repair and Regeneration 5(1): 12-17.
Ruslay, S. 2006. LC-MS/MS Profiling and Characterization
of Active Components from Medicinal Gingers. Serdang: Universiti Putra
Malaysia.
Singh, C.B., Chanu, S.B.,
Lenin, Kh., Swapana, N., Cantrell, C. & Ross, S.A. 2014. Chemical
composition and biological activity of the essential oil of rhizome of Zingiber zerumbet (L.) Smith. Journal of Pharmacognosy and Phytochemistry 3(3): 130-133.
Sinno, H. & Prakash, S. 2013. Complements and the wound
healing cascade: An updated review. Plastic Surgery International 2013:
7.
Sulaiman,
M.R., Perimal, E.K., Akhtar, M.N., Mohamad, A.S., Khalid, M.H., Tasrip, N.A.,
Mokhtar, F., Zakaria, Z.A., Lajis, N.H. & Israf,
D.A. 2010. Anti-inflammatory effect of zerumbone on acute and chronic
inflammation models in mice. Fitoterapia 81(7): 855-858.
Tan, S.P., McLoughlin,
P., O'Sullivan, L., Prieto, M.L., Gardiner, G.E., Lawlor, P.G. &
Hughes, H. 2013. Development of a novel antimicrobial seaweed extract-based
hydrogel wound dressing. International Journal of Pharmaceutics
456(1): 10-20. WHO. 2017. Noncommunicable Diseases. http://www.who.int/
mediacentre/factsheets/fs355/en/. Accessed on 29 March 2018.
Wong, V.W. & Crawford, J.D. 2013. Vasculogenic cytokines
in wound healing. BioMed. Research International 2013: 11.
Yan, H., Ren, M.Y., Wang, Z.X., Feng, S.J., Li, S., Cheng,
Y., Hu, C.X., Gao, S.Q. & Zhang, G.Q. 2017. Zerumbone inhibits melanoma
cell proliferation and migration by altering mitochondrial functions. Oncology
Letters 13(4): 2397-2402.
Yob, N.J., Jofrry, S.M., Affandi, M.M., Teh, L.K., Salleh,
M.Z. & Zakaria, Z.A. 2011. Zingiber zerumbet (L.) smith: A review of
its ethnomedicinal, chemical, and pharmacological uses. Evidence-Based
Complementary Alternative Medicine 2011: 543216.
*Corresponding author; email: asmah0901@ukm.edu.my
|
|||
|
