THE EFFICACY OF 200 ÎœG/KGBW/IP HEAT SHOCK PROTEIN-70 IN REDUCTION OF CYT C, BAX, AND CASPASE 3 EXPRESSION, AND MORTALITY IN MICE MODEL WITH MULTIPLE ORGAN DYSFUNCTION SYNDROME

Authors

  • Igl Sukamto Department of Anesthesiology, Dr. Moewardi Hospital, Faculty of Medicine, Doctoral Program in Medicine, Universitas Sebelas Maret, Surakarta, Central Java, Indonesia.
  • Suroto Suroto Department of Neurology, Dr. Moewardi/Faculty of Medicine, Universitas Sebelas Maret, Surakarta, Indonesia.
  • Ambar Mudigdo Department of Anatomic Pathology, Dr. Moewardi/Faculty of Medicine, Universitas Sebelas Maret, Surakarta, Indonesia.
  • Bambang Purwanto Department of Internal Medicine, Dr. Moewardi/Faculty of Medicine, Universitas Sebelas Maret, Surakarta, Indonesia.

DOI:

https://doi.org/10.22159/ajpcr.2018.v11i11.29541

Keywords:

Sepsis, Multiple organ dysfunction syndrome, Apoptosis, Heat shock protein 70

Abstract

Objective: Heat shock protein 70 (HSP70) decreases Cyt expression c, Bax, and Caspase 3 in apoptosis multiple organ dysfunction syndrome (MODS), thus inhibiting death. This study aimed to analyze the efficacy of HSP70 200 μg/KgBB/ip to decrease Cyt c, Bax, and Caspase 3 expression, to reduce mortality, and to increase survival rate, in the MOD alveolar lung epithelial of 78-h sepsis model.

Methods: This was a post-test only quasi-experiment conducted at Inter-University Central Laboratory of Gadjah Mada University, Yogyakarta, and the Anatomy Pathology Laboratory, Faculty of Medicine, Universitas Sebelas Maret, Surakarta. The study used a type of Balb/c mice, male, aged of 6–8 weeks, body weight of 25–33 g. Sepsis induction used LIG SIGMA L2880-10MG Lot #025M4040V from Escherichia coli 055:B5 purified by phenol extraction. Medication to reduce mortality used HSP70 Lot #L16020515 and then continued with 400× immunohistochemistry (IHC) examination. A sample of 30 mice were divided into three groups: (1) Control group without 78 h treatment, (2) lipopolysaccharide (LPS) group with a dose of 0.25 mg/kgBW/ip 78 h, and (3) HSP70 group with a dose of 200 μg/kgBB/ip after LPS injection 0.25 mg/kgBW/ip 78 h. The outcome variables included expression of Cyt, Bax, Caspase 3, and mortality in mice model with multiple organ dysfunction syndrome. The data were analyzed by Kruskal–Wallis and continued by Mann–Whitney U-test.

Results: Administration of HSP70 200 mg/KgBW/ip after LPS 0.25 mg/kgBW/ip significantly decreased Cyt c expression (p=0.014), Bax (p=0.004), and Caspase 3 (p=0.015) in 78 h pulmonary alveolar cells, reduced mortality rate, and increased the number of survivors. Expressions of Cyt c, Bax, and Caspase 3 of IHC 400× magnification had a near-normal image change.

Conclusion: There is a decrease of Cyt c, Bax, and Caspase 3 expression in the MOD alveolar lung epithelial cells of the 78-h sepsis model mice, a decrease of mortality rate, and an increase of survival rate, and the image of IHC is almost normal.

Downloads

Download data is not yet available.

References

Guntur HA. Imunologi, Diagnosis dan Penatalaksanaan Sepsis. In: Steroid Dosis Rendah Dalam Penatalaksanaan Sepsis. Surakarta: UNS Press; 2011. p. 1-45.

Singer M. The role of mitochondrial dysfunction in sepsis-induced multi-organ failure. Virulence 2014;5:66-72.

Chouhan S, Hansa J, Pradhan S. Early diagnosis of sepsis through sepsis markers and sepsis index through flow cytometry technology. Asian J Pharm Clin Res 2017;10:145-8.

Babu M, Menon VP, Devi U. Epidemiology and outcome among severe sepsis and septic shock patients in a South Indian tertiary care hospital. Int J Pharm Pharm Sci 2017;9:256-9.

Foroutan B, Razavianzadeh N, Anderson D. Overcoming chemoresistance in non-hodgkin lymphoma preliminary studies of apoptosis and necrosis by P-glycoprotein reversal agents. Int J Pharm Pharm Sci 2015;7:382-8.

Green DR. Means to an End: Apoptosis and Other Cell Death Mechanisms. Spring Harbor (N.Y.): Cold Spring Harbor Laboratory Press; 2011.

Kalogeris T, Baines CP, Krenz M, Korthuis RJ. Cell biology of ischemia/reperfusion injury. Int Rev Cell Mol Biol 2012;298:229-317.

Martinvalet D, Zhu P, Lieberman J. Granzyme A induces caspase-independent mitochondrial damage, a required first step for apoptosis. Immunity 2005;22:355-70.

Elmore S. Apoptosis: A review of programmed cell death. Toxicol Pathol 2007;35l:495-516.

Hariharan S, Subramanian S, Pooja C, Renukadevi G, Hashik M. Heat shock proteins - A mini review. Int J Pharm Pharm Anal 2014;1:65-73.

Choudhury S, Bae S, Ke Q, Lee JY, Kim J, Kang PM, et al. Mitochondria to nucleus translocation of AIF in mice lacking hsp70 during ischemia/ reperfusion. Basic Res Cardiol 2011;106:397-407.

Brunet M, Didelot C, Rerole AL, de Thonel A, Garrido C. Hsp70 and Hsp27 as Pharmacological Targets in Apoptosis Modulation for Cancer Therapy. In: Calderwood SK, Sherman MK, Ciocca DR, editors. Heat Shock Proteins in Cancer. Netherlands: Springer; 2007. p. 209-30.

Xu J, Vanderlick TK, Beales PA. Lytic and non-lytic permeabilization of cardiolipin-containing lipid bilayers induced by cytochrome C. PLoS One 2013;8:e69492.

Wu CC, Bratton SB. Regulation of the intrinsic apoptosis pathway by reactive oxygen species. Antioxid Redox Signal 2013;19:546-58.

Jiang X, Jiang H, Shen Z, Wang X. Activation of mitochondrial protease OMA1 by bax and bak promotes cytochrome c release during apoptosis. Proc Natl Acad Sci U S A 2014;111:14782-7.

Evans CG, Chang L, Gestwicki JE. Heat shock protein 70 (hsp70) as an emerging drug target. J Med Chem 2010;53:4585-602.

Kustanova GA, Murashev AN, Karpov VL, Margulis BA, Guzhova IV, Prokhorenko IR, et al. Exogenous heat shock protein 70 mediates sepsis manifestations and decreases the mortality rate in rats. Cell Stress Chaperones 2006;11:276-86.

Aschkenasy G, Bromberg Z, Raj N, Deutschman CS, Weiss YG. Enhanced hsp70 expression protects against acute lung injury by modulating apoptotic pathways. PLoS One 2011;6:e26956.

Sharma D, Masison DC. Hsp70 structure, function, regulation and influence on yeast prions. Protein Pept Lett 2009;16:571-81.

Mazzei L, Docherty NG, Manucha W. Mediators and mechanisms of heat shock protein 70 based cytoprotection in obstructive nephropathy. Cell Stress Chaperones 2015;20:893-906.

Markwart R, Condotta SA, Requardt RP, Borken F, Schubert K, Weigel C, et al. Immunosuppression after sepsis: Systemic inflammation and sepsis induce a loss of naïve T-cells but no enduring cell-autonomous defects in T-cell function. PLoS One 2014;9:e115094.

Zhao J, Wei J, Weathington N, Jacko AM, Huang H, Tsung A, et al. Lysophosphatidic acid receptor 1 antagonist ki16425 blunts abdominal and systemic inflammation in a mouse model of peritoneal sepsis. Transl Res 2015;166:80-8.

Fodor RÅž, Georgescu AM, Cioc AD, Grigorescu BL, Cotoi OS, Fodor P, et al. Time- and dose-dependent severity of lung injury in a rat model of sepsis. Rom J Morphol Embryol 2015;56:1329-37.

Kumar S, Deepak P, Acharya A. HSP70 modulates the enhanced production of reactive intermediate metabolites and a proinflammatory cytokine TNFα expression in a t cell lymphoma. Eur J Inflamm 2006;4:157-69.

Published

07-11-2018

How to Cite

Sukamto, I., S. Suroto, A. Mudigdo, and B. Purwanto. “THE EFFICACY OF 200 ÎœG/KGBW/IP HEAT SHOCK PROTEIN-70 IN REDUCTION OF CYT C, BAX, AND CASPASE 3 EXPRESSION, AND MORTALITY IN MICE MODEL WITH MULTIPLE ORGAN DYSFUNCTION SYNDROME”. Asian Journal of Pharmaceutical and Clinical Research, vol. 11, no. 11, Nov. 2018, pp. 482-4, doi:10.22159/ajpcr.2018.v11i11.29541.

Issue

Vol 11 Issue 11 November 2018

Section

Original Article(s)

The publication is licensed under CC By and is open access. Copyright is with author and allowed to retain publishing rights without restrictions.

Crossref
Scopus
Google Scholar
Europe PMC