黄芪甲苷对顺铂所致小鼠肝损伤的抑制作用及其机制

doi:10.13481/j.1671-587X.20250211

Abstract

Abstract:

Objective To investigate the inhibitory effect of astragaloside Ⅳ（AS-Ⅳ） on cisplatin（CDDP）-induced liver injury in the mice，and to elucidate its possible mechanism. Methods Forty male C57BL/6 mice with body weights of 18-22 g were randomly divided into control group，model group，AS-Ⅳ group and adenosine 5'-monophosphate-activated protein kinase （AMPK） inhibitor （Compound C）+ AS-Ⅳ group. The mice in control group and model group were gavaged with the same volume of normal saline，and the drug was administered continuously for 9 d. The mice in AS-Ⅳ group and Compound C+AS-Ⅳ group were given AS-Ⅳ aqueous solution（150 mg·kg^-1·d^-1）， respectively. On the 6th day of experiment，the mice in Compound C+AS-Ⅳ group were intraperitoneally injected with Compound C （20 mg·kg^-1）， and on the 7th day，except for control group，the mice in other groups were intraperitoneally injected with 20 mg·kg^-1 CDDP to establish the mouse liver injury models，and the mice were sacrificed 48 h later. Serum and liver tissues were collected，and the levels of aspartate aminotransferase （AST） and alanine aminotransferase （ALT） in the serum of the mice，as well as the activities of superoxide dismutase（SOD） and catalase （CAT） and the levels of malondialdehyde（MDA） in the liver tissue of the mice in various groups were detected by kits. The pathomorphology of liver tissue of the mice in various groups were detected by HE staining. The expression levels of glutathione peroxidase 4 （GPX4）， ferritin heavy chain 1 （FTH1） and ferroptosis inhibitory protein 1 （FSP1） proteins in liver tissue of the mice in various groups were detected by immunohistochemical staining， and the expression levels of nuclear factor-E2-related factor 2 （Nrf2）， heme oxygenase-1 （HO-1） and AMPK proteins in liver tissue of the mice in various groups were detected by Western blotting method. Results Compared with control group， the levels of AST and ALT in serum of the mice in model group were increased （P<0.01）， the activities of SOD and CAT in the liver tissue were significantly decreased （P<0.01）， and the MDA level was increased （P<0.01）； compared with model group，the levels of AST and ALT in serum of the mice in AS-Ⅳ group were decreased （P<0.01）， the MDA level in the liver tissue was decreased （P<0.01）， and the activities of SOD and CAT were increased （P<0.01）； compared with AS-Ⅳ group （P<0.01）， the levels of AST and ALT in serum of the mice in Compound C+AS-Ⅳ group were increased （P<0.01）， the level of MDA in liver tissue was increased （P<0.05）， and the activities SOD and CAT were decreased（P<0.01）. The HE staining results showed that compared with control group， the liver damage degree of the mice in model group was enhanced，the hepatocyte arrangement was disordered， and some hepatocyte edema were increased； compared with model group， the liver morphology of the mice in AS-Ⅳ group returned to normal； compared with AS-Ⅳ group， the hepatocyte arrangement of the mice in Compound C+AS-Ⅳ group was disordered and the edges were blurred. The immunohistochemistry results showed that compared with control group， the expression levels of GPX4， FTH1 and FSP1 proteins in liver tissue of the mice in model group were decreased （P<0.05）； compared with model group， the expression levels of GPX4， FTH1 and FSP1 proteins in liver tissue of the mice in AS-Ⅳ group were increased （P<0.05）； compared with AS-Ⅳ group， the expression levels of GPX4， FTH1 and FSP1 proteins in liver tissue of the mice in Compound C+AS-Ⅳ group were decreased （P<0.05 or P<0.01）. The Western blotting results showed that compared with control group，the expression levels of Nrf2， HO-1 and AMPK proteins in liver tissue of the mice in model group were decreased （P<0.01）； compared with model group，the expression levels of Nrf2， HO-1 and AMPK proteins in liver tissue of the mice in AS-Ⅳ group were increased （P<0.01）； compared with AS-Ⅳ group，the expression levels of Nrf2， HO-1 and AMPK proteins in liver tissue of the mice in Compound C+AS-Ⅳ group were decreased （P<0.01）. Conclusion AS-Ⅳ can alleviate the CDDP-induced liver injury，and its mechanism may be related to the regulation of AMPK/Nrf2/HO-1 signal pathway and ferroptosis by AS-Ⅳ.

Key words: Astragaloside Ⅳ, Cisplatin, Liver injury, Ferroptosis, Adenosine 5'-monophosphate-activated protein kinase

CLC Number:

Kaiqi NIU,He CHANG,Guangfu LYU,Pengyu ZHENG,Xueting CHI,Jia ZHOU,Yuchen WANG,Xiaowei HUANG. Inhibitory effect of astragaloside Ⅳ on cisplatin-induced liver injury in mice and its mechanism[J].Journal of Jilin University(Medicine Edition), 2025, 51(2): 370-377.

Figures/Tables 6

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References 28

1	LIU Y， CHEN L， HE X，et al. Enhancement of therapeutic effectiveness by combining liposomal honokiol with cisplatin in ovarian carcinoma［J］. Int J Gynecol Cancer，2008，18（4）： 652-659.
2	SHAFFEI IEL， ABDEL-LATIF G A， FARAG D B，et al. Ameliorative effect of betanin on experimental cisplatin-induced liver injury； the novel impact of miRNA-34a on the SIRT1/PGC-1α signaling pathway［J］. J Biochem Mol Toxicol，2021，35（6）： 1-14.
3	HE Z Q， SHEN P， FENG L J，et al. Cadmium induces liver dysfunction and ferroptosis through the endoplasmic stress-ferritinophagy axis［J］. Ecotoxicol Environ Saf，2022，245： 114123.
4	张明娇，朱杰夫，吴雄飞. 顺铂诱导的肾损伤中的细胞死亡［J］. 生物技术进展， 2023， 13（5）： 718-724.
5	SU W T， GAO W C， ZHANG R，et al. TAK1 deficiency promotes liver injury and tumorigenesis via ferroptosis and macrophage cGAS-STING signalling［J］. JHEP Rep， 2023， 5（5）： 100695.
6	WANG X， CHEN X X， ZHOU W Q，et al. Ferroptosis is essential for diabetic cardiomyopathy and is prevented by sulforaphane via AMPK/NRF2 pathways［J］. Acta Pharm Sin B，2022，12（2）： 708-722.
7	WANG E Y， WANG L， DING R，et al. Astragaloside Ⅳ acts through multi-scale mechanisms to effectively reduce diabetic nephropathy［J］. Pharmacol Res，2020，157： 104831.
8	SONG M T， RUAN J， ZHANG R Y，et al. Astragaloside Ⅳ ameliorates neuroinflammation-induced depressive-like behaviors in mice via the PPARγ/NF-κB/NLRP3 inflammasome axis［J］. Acta Pharmacol Sin， 2018， 39（10）： 1559-1570.
9	RIESWIJK L， LIZARRAGA D， BRAUERS K J J，et al. Characterisation of cisplatin-induced transcriptomics responses in primary mouse hepatocytes，HepG2 cells and mouse embryonic stem cells shows conservation of regulating transcription factor networks［J］. Mutagenesis，2014， 29（1）： 17-26.
10	WANG L， DONG X L， QIN X M， et al. Investigating the inter-individual variability of Astragali Radix against cisplatin-induced liver injury via 16S rRNA gene sequencing and LC/MS-based metabolomics［J］. Phytomedicine， 2022， 101： 154107.
11	徐源，黄存东，李竹青，等. 黄芪甲苷对糖尿病大鼠肝损伤保护作用及其机制研究［J］. 安徽医科大学学报，2017， 52（12）： 1823-1829.
12	王文哲，魏星宇，于冬冬，等. 针灸调控TNF-α/TLR4/NF-κB改善顺铂小鼠肝损伤的作用机制［J］. 世界科学技术-中医药现代化，2023，25（3）： 1055-1060.
13	WANG Y， HU P C， GAO F F， et al. The protective effect of curcumin on hepatotoxicity and ultrastructural damage induced by cisplatin［J］. Ultrastruct Pathol，2014， 38（5）： 358-362.
14	HAMZEH M， HOSSEINIMEHR S J， KHALATBARY A R， et al. Atorvastatin mitigates cyclophosphamide-induced hepatotoxicity via suppression of oxidative stress and apoptosis in rat model［J］. Res Pharm Sci， 2018， 13（5）： 440-449.
15	张静，马翠丽，王志国. 黄芪甲苷对大鼠心肌局部缺血再灌注损伤的改善作用及其对PI3K/Akt/mTOR信号通路的影响［J］. 吉林大学学报（医学版）， 2014， 40（5）： 991-996，1130.
16	赵芳，王洪新，鲁美丽，等. 黄芪甲苷对慢性间歇性缺氧诱导血管内皮功能障碍的保护作用［J］. 中成药，2022， 44（10）： 3145-3150.
17	GOYAL Y， KOUL A， RANAWAT P. Ellagic acid ameliorates cisplatin induced hepatotoxicity in colon carcinogenesis［J］. Environ Toxicol，2019，34（7）： 804-813.
18	ZHU J， SUN R P， SUN K Q， et al. The deubiquitinase USP11 ameliorates intervertebral disc degeneration by regulating oxidative stress-induced ferroptosis via deubiquitinating and stabilizing Sirt3［J］. Redox Biol，2023， 62： 102707.
19	BASIT F， VAN OPPEN L M， SCHÖCKEL L， et al. Mitochondrial complex I inhibition triggers a mitophagy-dependent ROS increase leading to necroptosis and ferroptosis in melanoma cells［J］. Cell Death Dis， 2017， 8（3）： e2716.
20	LI J， JIA B W， CHENG Y， et al. Targeting molecular mediators of ferroptosis and oxidative stress for neurological disorders［J］. Oxid Med Cell Longev， 2022，2022： 3999083.
21	沈惟钰，吴艳，卞涛. 铁死亡抑制蛋白1在铁死亡相关疾病中的研究进展［J］. 安徽医药， 2023， 27（3）： 425-428.
22	YU Y， YAN Y， NIU F L， et al. Ferroptosis： a cell death connecting oxidative stress， inflammation and cardiovascular diseases［J］. Cell Death Discov， 2021， 7（1）： 193.
23	周云洁，常红波，王新洲. 龙牙楤木总皂苷通过调控AMPK/Nrf2信号抑制缺氧/复氧诱导的心肌细胞铁死亡［J］. 中药材， 2023， 46（12）： 3091-3096.
24	石雨鹭，康权，岳小涵，等. LETM1对骨肉瘤细胞恶性生物学行为的作用及其机制［J］. 解放军医学杂志， 2024， 49（10）： 1163-1173.
25	XU W T， ZHAO T T， XIAO H Y. The implication of oxidative stress and AMPK-Nrf2 antioxidative signaling in pneumonia pathogenesis［J］. Front Endocrinol （Lausanne）， 2020， 11： 400.
26	LEE H， ZANDKARIMI F， ZHANG Y L， et al. Energy-stress-mediated AMPK activation inhibits ferroptosis［J］. Nat Cell Biol， 2020， 22（2）： 225-234.
27	LU Q Y， YANG L J， XIAO J J， et al. Empagliflozin attenuates the renal tubular ferroptosis in diabetic kidney disease through AMPK/NRF2 pathway［J］. Free Radic Biol Med， 2023， 195： 89-102.
28	任东根，龚婷，王丽娟，等. 川麦冬多糖的结构特征及对过度运动小鼠肝损伤的改善作用［J］. 食品与发酵工业， 2024， 50（2）： 213-223.

Group	AST	ALT
Control	105.27±6.76	58.35±3.76
Model	327.78±15.90^*	135.23±7.63^*
AS-Ⅳ	154.80±12.25^△	91.12±6.67^△
Compound C+AS-Ⅳ	226.69±18.21^#	108.43±7.86^#

Group	SOD[λ_B/(U·mg^-1）]	CAT[λ_B/(U·mg^-1）]	MDA[m_B/(μmol·g^-1）]
Control	448.55±13.01	25.43±1.23	4.08±0.38
Model	184.64±6.63^*	12.36±1.27^*	7.73±1.42^*
AS-Ⅳ	316.23±9.65^△	17.85±0.88^△	3.37±0.98^△
Compound C +AS-Ⅳ	233.29±5.48^##	15.21±0.35^##	6.53±0.64^##

Group	GPX4	FTH1	FSP1
Control	41.24±1.56	21.27±1.44	24.89±1.66
Model	26.57±1.87^*	6.52±0.65^*	13.19±1.34^*
AS-Ⅳ	30.20±1.98^△	16.05±1.72^△	15.36±1.47^△
Compound C+AS-Ⅳ	24.96±1.88^#	12.36±0.56^#	13.87±1.29^##

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Inhibitory effect of astragaloside Ⅳ on cisplatin-induced liver injury in mice and its mechanism

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