Immediately transcripted genes in various hepatic ischemia models
- Authors
- Choi, Kang Kook; Cho, Jin A.; Kim, Se Hoon; Lee, Sang Woo; Min, Seon Ok; Kim, Kyung Sik
- Issue Date
- Nov-2012
- Publisher
- KOREAN SURGICAL SOCIETY
- Keywords
- Reperfusion injury; Ischemic preconditioning; Necrosis; Apoptosis; Microarray analysis
- Citation
- JOURNAL OF THE KOREAN SURGICAL SOCIETY, v.83, no.5, pp.298 - 306
- Journal Title
- JOURNAL OF THE KOREAN SURGICAL SOCIETY
- Volume
- 83
- Number
- 5
- Start Page
- 298
- End Page
- 306
- URI
- https://scholarworks.bwise.kr/gachon/handle/2020.sw.gachon/16031
- DOI
- 10.4174/jkss.2012.83.5.298
- ISSN
- 2233-7903
- Abstract
- Purpose: To elucidate the characteristic gene transcription profiles among various hepatic ischemia conditions, immediately transcribed genes and the degree of ischemic injury were compared among total ischemia (TI), intermittent clamping (IC), and ischemic preconditioning (IPC). Methods: Sprague-Dawley rats were equally divided into control (C, sham-operated), TI (ischemia for 90 minutes), IC (ischemia for 15 minutes and reperfusion for 5 minutes, repeated six times), and IPC (ischemia for 15 minutes, reperfusion for 5 minutes, and ischemia again for 90 minutes) groups. A cDNA microarray analysis was performed using hepatic tissues obtained by partial hepatectomy after occluding hepatic inflow. Results: The cDNA microarray revealed the following: interleukin (IL)-1 beta expression was 2-fold greater in the TI group than in the C group. In the IC group, IL-1 alpha/beta expression increased by 2.5-fold, and Na+/K+ ATPase 1 beta expression decreased by 2.4-fold. In the IPC group, interferon regulatory factor-1, osteoprotegerin, and retinoblastoma-1 expression increased by approximately 2-fold compared to that in the C group, but the expression of Na+/K+ ATPase beta 1 decreased 3-fold. Conclusion: The current findings revealed characteristic gene expression profiles under various ischemic conditions. However, additional studies are needed to clarify the mechanism of protection against IPC.
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