Human amniotic epithelial stem cells attenuate mice liver ischemia-reperfusion injury by regulating M1/M2 macrophage polarization

doi:10.3877/cma.j.issn.1674-3903.2023.01.005

Abstract

Abstract:

Objective

To investigate the protective effect and mechanism of human amnion epithelial stem cells (hAECs) against liver ischemia-reperfusion injury (IRI) in mice.

Methods

Ten C57BL/6 mice were randomly divided into the control group (IRI+ PBS group) and the experimental group (IRI+ hAECs group), with 5 mice in each group. The IRI+ PBS group was injected with PBS (100 μL) via the dorsal vein of the penis, and the IRI+ hAECs group was injected with hAECs (1×10⁵ pieces) via the dorsal vein of the penis. At 0.5 h after injection, ischemia at normal temperature for 1.5 h and reperfusion for 6 h. HE staining was used to observe the pathological changes of mouse liver tissue. Biochemical analysis was used to measure serum ALT, AST and lactate dehydrogenase (LDH) levels. Immunohistochemical staining was used to observe the infiltration of macrophages (F4/80) and M1 (CD68) and M2 (CD206) macrophages. At the same time, the apoptosis-related factors B-lymphoma-2 (BCL-2), BCL-2-related X protein (BAX), cysteinyl aspartate-specific protease (Caspase)-3 and Caspase-7, and the inflammatory factors IL-6, IL-23, TNF-α and IL-β mRNA relative expressions were also compared. Data of continuous variables conforming to normal distribution were compared by independent sample t test. P<0.05 was considered statistically significant.

Results

Compared with the IRI + PBS group, the pathological damage of the liver tissue was significantly improved in the IRI + hAECs group. The expression levels of serum ALT, AST and LDH in the IRI+ hAECs group were (1 456±20), (1 375±49) and (2 435±147) U/L, respectively, and those in the IRI+ PBS group were (3 919±48), (3 142±145) and (3 499±147) U/L, the differences were statistically significant (t=47.13, 11.53 and 4.53, all P<0.05). The mRNA expression levels of BCL-2, BAX, Caspase-3 and Caspase-7 in the IRI + hAECs group were (0.20±0.05), (0.19±0.09), (0.46±0.13) and (0.27±0.03), respectively; they were all lower than those in the IRI + PBS group (1.01±0.16), (1.02±0.28), (1.01±0.17) and (1.00±0.11), and the differences were statistically significant (t=8.45, 4.88, 4.39 and 10.79, all P<0.05). Immunohistochemical staining showed that macrophage infiltration was lower in the IRI+ hAECs group. The mRNA levels of IL-6, IL-23, TNF-α and IL-β in the IRI+ hAECs group were (0.38±0.04), (0.33±0.05), (0.43±0.08) and (0.12±0.04), respectively; they were all lower than those in the IRI+ PBS group (1.10±0.11), (1.00±0.05), (1.00±0.02) and (1.10±0.06), and the differences were statistically significant (t=11.27, 16.37, 12.96 and 22.34, all P<0.05). The expression of M1 macrophages cells was significantly decreased in the IRI+ hAECs group, and the proportion of M2 macrophages cells was increased.

Conclusion

hAECs protect mice from liver IRI by attenuating inflammatory responses by modulating the polarization of M1/M2 macrophages.

Key words: Human amniotic epithelial stem cells, Ischemia-reperfusion injury, Macrophage polarization, Inflammatory response

Wenzhi Shu, Mengfan Yang, Binhua Pan, Renyi Su, Zuyuan Lin, Modan Yang, Zhensheng Zhang, Yisu Song, Zhengyan Lu, Shusen Zheng, Xiao Xu, Xuyong Wei. Human amniotic epithelial stem cells attenuate mice liver ischemia-reperfusion injury by regulating M1/M2 macrophage polarization[J]. Chinese Journal of Transplantation(Electronic Edition), 2023, 17(01): 36-41.

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URL: https://zhyzzz.cma-cmc.com.cn/EN/10.3877/cma.j.issn.1674-3903.2023.01.005

https://zhyzzz.cma-cmc.com.cn/EN/Y2023/V17/I01/36

Figures/Tables 6

References 16

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基因名称	序列
TNF-α	正向：GGTGCCTATGTCTCAGCCTCTT
	反向：GCCATAGAACTGATGAGAGGGAG
IL-1β	正向：TGGACCTTCCAGGATGAGGACA
	反向：GTTCATCTCGGAGCCTGTAGTG
IL-23	正向：CATGCTAGCCTGGAACGCACAT
	反向：ACTGGCTGTTGTCCTTGAGTCC
Caspase-7	正向：CCGTCCACAATGACTGCTCTTG
	反向：CCCGTAAATCAGGTCCTCTTCC
Caspase-3	正向：GGAGTCTGACTGGAAAGCCGAA
	反向：CTTCTGGCAAGCCATCTCCTCA
BCL-2	正向：CCTGTGGATGACTGAGTACCTG
	反向：AGCCAGGAGAAATCAAACAGAGG
BAX	正向：AGGATGCGTCCACCAAGAAGCT
	反向：TCCGTGTCCACGTCAGCAATCA
IL-6	正向：TACCACTTCACAAGTCGGAGGC
	反向：CTGCAAGTGCATCATCGTTGTTC
GAPDH	正向：CATCACTGCCACCCAGAAGACTG
	反向：ATGCCAGTGAGCTTCCCGTTCAG

基因名称	序列
TNF-α	正向：GGTGCCTATGTCTCAGCCTCTT
	反向：GCCATAGAACTGATGAGAGGGAG
IL-1β	正向：TGGACCTTCCAGGATGAGGACA
	反向：GTTCATCTCGGAGCCTGTAGTG
IL-23	正向：CATGCTAGCCTGGAACGCACAT
	反向：ACTGGCTGTTGTCCTTGAGTCC
Caspase-7	正向：CCGTCCACAATGACTGCTCTTG
	反向：CCCGTAAATCAGGTCCTCTTCC
Caspase-3	正向：GGAGTCTGACTGGAAAGCCGAA
	反向：CTTCTGGCAAGCCATCTCCTCA
BCL-2	正向：CCTGTGGATGACTGAGTACCTG
	反向：AGCCAGGAGAAATCAAACAGAGG
BAX	正向：AGGATGCGTCCACCAAGAAGCT
	反向：TCCGTGTCCACGTCAGCAATCA
IL-6	正向：TACCACTTCACAAGTCGGAGGC
	反向：CTGCAAGTGCATCATCGTTGTTC
GAPDH	正向：CATCACTGCCACCCAGAAGACTG
	反向：ATGCCAGTGAGCTTCCCGTTCAG

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