|
|
|
| Changes of the expression of signaling pathway of PI3K/Akt/GSK3β and endoplasmic reticulum stress in the formation of deep tissue injury of pressure ulcer in rats |
| 1.Department of Nursing, Dongyang Hospital Affiliated to Wenzhou Medical University, Jinhua, 322100; |
|
| Cite this article: |
|
CUI Feifei1,ZHANG Jufang1,WU Haiying1, et al. Changes of the expression of signaling pathway of PI3K/Akt/GSK3β and endoplasmic reticulum stress in the formation of deep tissue injury of pressure ulcer in rats[J]. JOURNAL OF WEZHOU MEDICAL UNIVERSITY, 2014, 44(8): 555-560.
|
|
|
|
Abstract Objective: To explore changes of the expression of signaling pathway of PI3K/Akt/GSK3β and expressions of ER chaperones in the deep tissue injury of pressure ulcer in rats. Methods: Fifty-four male Sprague-Dawley rats were divided into normal group and compressed groups (1 cycle, 3 cycles, 6 cycles, and 9 cycles group), natural recovery group as 1 day group, 3 days group, 5 days group and 7 days group according to the random number table, with six rats in each group. Muscle tissues underneath compression region and the same region normal group tissue were collected for analysis. Haematoxylin and eosin staining was carried out to examine the tissue histology; the expression of caspase-3 was assayed by immunohistochemical staining (Vectastain avidin-biotin complex, ABC); during different stages (experimental group and natual recovery group) the dynamic change of the ER chaperone such as GRP78, CHOP, caspase-12 and Akt, GSK3β, p-Akt, p-GSK3β in compressed muscle tissue were assayed by Western blot. Results: Under the light microscope of HE staining, the compressed muscle tissue of the experiment group showed a gradual degradation in the pathological changes, in recovery group, there were still signs of the pathlogical phenomenon; The immunohistochemical analysis indicated that the protein abundance of caspase-3 was elevated in the experiment group and natural recovery group compared with the control group, the detected immunoreactivity were generally distributed in cytoplasm. According to our immunoblot analysis, the protein expression of GRP78, CHOP, caspase-12 displayed a general ascending trend during different cycle; the protein expression of p-Akt showed first increased and then decreased; the protein expression of p-GSK3β offered first increased and then decreased with the time going, in recovery group p-GSK3β expression appeared first decreased and then increased with time going. Conclusion: The reasons of deep layer ulcers hard to heal may be related to muscle injury of the surrounding tissue; ERS and PI3K/Akt/GSK3β signaling pathway may involved in the procedure of deep ulcers.
|
|
Received: 26 March 2014
|
| |
|
Corresponding Authors:
2.Nursing School of Wenzhou Medical University, Wenzhou, 325035
|
| About author:: 姜丽萍,教授,博士生导师,Email:jlp@wzmc.edu.cn。 |
|
|
|
[1] Bouten CV, Oomens CW, Baaijens FP, et al. The etiology of
pressure ulcers: skin deep or muscle bound?[J]. Arch Phys
Med Rehabil, 2003, 84(4): 616-619.
[2] Black J, Baharestani MM, CuddiganJ, et al. National Pres-
sure Ulcer Advisory Panel’s updated pressure ulcer staging
system[J]. Adv Skin Wound Care, 2007, 20(5): 269-274.
[3] Stratos I, Li Z, Rotter R, et al. Inhibition of caspase mediat-
ed apoptosis restores muscle function after crush injury in
rat skeletal muscle[J]. Apoptosis, 2012, 17(3): 269-277.
[4] Wu QL, Shen T, Shao LL, et al. Ischemic postcondition-
ing mediates cardioprotection via PI3K/GSK-3beta/beta-
catenin signaling pathway in ischemic rat myocardium[J].
Shock, 2012, 38(2): 165-169.
[5] National Pressure Ulcer Advisory Panel. Resources: Ed-
ucation and Clinical Resources: NPUAP Pressure Ulcer
Stages/Categories[EB/OL]. 2007. http://www.npuap.org/re-
sources/educational-and-clinical-resources/npuap-pressure-
ulcer-stages Categories/.
[6] 王艳艳, 张纯瑜, 姜丽萍, 等. 压疮早期动物模型制备及评
价[J]. 护理学杂志, 2010, 25(14): 1-5.
[7] 臧爽, 翟秀岩. 压疮大鼠骨骼肌组织形态学变化研究[J].
中国血液流变学杂志, 2009, 19(2): 192-194.
[8] Liu H, Miller E, van de Water B, et al. Endoplasmic reticu-
lum stress proteins block oxidant induced Ca2+ increases and
cell death[J]. J Biol Chem, 1998, 273(21): 12858-12862.
[9] Zhang PL, Lun M, Teng J, et al. Preinduced molecular chap-
erones in the endnoplasmic reticulum protect cardiomyo-
cytes from lethal injury[J]. Ann Clin Lab Sci, 2004, 34(4):
449-457.
[10] 崔飞飞, 代彦丽, 张龙, 等. 凋亡因子caspase-12在压疮早期
损伤中的作用[J]. 护理研究, 2013, 27(3A): 665-667.
[11] 崔飞飞, 潘莹莹, 张龙, 等. 内质网分子伴侣蛋白在压疮局
部缺血性损伤中的表达[J]. 中国应用生理学杂志, 2013,
29(3): 309-311.
[12] 左群, 张卫群, 于新凯. 骨骼肌损伤与修复中内质网应激
蛋白的表达变化[J]. 中国康复医学杂志, 2012, 27(3): 201-
205.
[13] FujioY, Nguyen T, Wencker D, et al. Akt promotes survival
of cardiomyocytes in vitro and protects against ischemia-
reperfusion injury in mouse heart[J]. Circulation, 2000,
101(6): 660-667.
[14] Mozaffari MS, Liu JY, Schaffer SW. Effect of pressure over-
load on cardioprotection via PI3K-Akt: comparison of post-
conditioning, insulin, and pressure unloading[J]. Am J Hy-
pertens, 2010, 23(6): 668-674. |
| [1] |
. [J]. JOURNAL OF WEZHOU MEDICAL UNIVERSITY, 2022, 52(8): 0-. |
|
|
|
|
