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Research Article | | Peer-Reviewed

Study on the Effect of Rhubarb and Its Active Components on Pyroptosis in DKD by Regulating STAT3/Caspase-11 Axis

Yanwen Mao Minghao Zhang Zijuan Zhang Xiaowei Zhang Wenhui Rong Juan Zhang Mengmeng Yang Jiangyan Xu*
Published in American Journal of Clinical and Experimental Medicine (Volume 12, Issue 3)
Received: 5 July 2024     Accepted: 22 July 2024     Published: 29 July 2024
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Abstract

Rhubarb has been found to have a certain protective effect on improving the kidney function. However, the specific mechanism is still unclear. In this study, network pharmacology, molecular docking spontaneous binding technology and molecular biology experiments were used to verify the mechanism of rhubarb and its active ingredients in the treatment of DKD. A total of 10 active compounds and 121 (larger than average) target proteins were collected. The target proteins with higher degree value were screened by PPI according to degree value as follows: AKT1, STAT3, EGFR, NFKB1, SRC, etc. GO and KEGG enrichment analysis suggest that rhubarb therapy for DKD mainly involves Pathways in cancer, Prostate cancer, Proteoglycans in cancer, Chemokine signaling pathway, PI3K-Akt signaling pathway, PD-L1 expression and PD-1 checkpoint pathway in cancer, EGFR tyrosine kinase inhibitor resistance signaling pathway and so on. Furthermore, molecular docking results suggest that hydrogen bonding, salt bridge and hydrophobic interactions contribute to spontaneous binding of the compound to the target protein. Experimental verification shows that rhubarb and aloe emodin affect the mechanism of pyroptosis in diabetic kidney disease by regulating STAT3/Caspase11 axis. In conclusion, this study comprehensively elaborated the active compounds, potential targets and molecular experimental mechanisms of rhubarb to provide the basic experimental theory for clinical treatment of DKD.

Published in American Journal of Clinical and Experimental Medicine (Volume 12, Issue 3)
DOI 10.11648/j.ajcem.20241203.12
Page(s) 28-44
Creative Commons

This is an Open Access article, distributed under the terms of the Creative Commons Attribution 4.0 International License (http://creativecommons.org/licenses/by/4.0/), which permits unrestricted use, distribution and reproduction in any medium or format, provided the original work is properly cited.

Copyright

Copyright © The Author(s), 2024. Published by Science Publishing Group
Previous article
Keywords

Network Pharmacology, Rhubarb, SATA3, Pyroptosis, DKD

1. Introduction
As early as 1764, Cotunnius reported for the first time that persistent diabetes had a certain impact on the kidney. In 1877, Armanni and Epstein first discovered the specific pathological damage of the kidney under the microscope of DKD. In 1983, Mogensen CE conducted the staging of DKD, which has been used as a reference for clinical diagnosis and treatment. DKD is one of the most common microvascular complications induced by chronic hyperglycemia in diabetes mellitus and has a high disability rate. In recent years, the incidence of diabetes has increased year by year, and the disease has become the main cause of chronic kidney disease and end-stage renal disease. The risk factors of diabetic nephropathy include age, hyperglycemia, hypertension, obesity, hyperlipidemia and so on. Its pathogenesis is complex. Studies have been conducted, including abnormal renal hemodynamics, inflammation, oxidative stress, and disorders of glucose and lipid metabolism, all of which are involved in the occurrence and development of the disease. The pathological manifestations began with the increase of kidney volume at the initial stage, followed by glomerular basement membrane thickening and mesangial matrix increase as the disease progressed, and the disease further progressed to massive fibrinogen deposition, glomerular sclerosis, Kimnel-Steil-Wilson (K-W) nodules formation, and finally irreversible damage. Clinical DKD patients often have entered the stage IV or even the terminal stage of diabetic nephropathy when the disease is found
[1-3]
.
At present, the treatment of DKD in modern medicine mainly includes basic treatment such as controlling blood sugar and blood pressure, regulating lipid metabolism, etc. The lack of effective specific treatment methods has brought huge mental and economic burden to patients and their families, and seriously affected their quality of life. Traditional Chinese medicine (TCM) is a mature traditional medicine that has been continuously fighting against diseases in life practice for thousands of years in China, and has significant advantages in the treatment of DKD
[4-6]
.
According to the main clinical manifestations of DKD, Chinese medicine classified it into the categories of "kidney elimination", "Xiaothirst", "edema" and "turbidity-urine", and emphasized that the disease location was mainly in the kidney, and its pathological nature was the original deficiency, which was the deficiency of Qi and blood, Yin and Yang and the five viscera, and the standard was the deficiency of water dampness, blood stasis and turbidity-phlegm
[7-9]
. Many ancient books record that rhubarb is the essential medicine for purging and invading accumulation, which was first recorded in Shennong's Herbal Classic. Alias General, Huang Liang, Fire ginseng, etc. Smell bitter cold, non-toxic, the main blood stasis, Blood blocking cold and heat, breaking the accumulation of mass, Drink vegetarian food, cleanse the stomach, Push the old to the new, easing intestines and stomach, Regulating the medium to transform food, Peace and five viscera. The main effects are diarrhea and accumulation, cooling and detoxification, Expelling stasis through menstruation, removing dampness and withdrawing yellow. It is recorded in "Medicine Zhongshen Xilu": "Rhubarb taste bitter, fragrant, cool, can enter the blood, break all blood stasis." Because the pathogenesis of DKD is kidney collateral stasis, and rhubarb has the function of clearing blood stasis and dredging meridians, rhubarb has a better effect on targeted treatment of DKD. At present, there are only four kinds of rhubarb products recorded in the Pharmacopoeia of the People's Republic of China (Part I) (referred to as the "Chinese Pharmacopoeia"), namely, raw rhubarb, cooked rhubarb, wine rhubarb and rhubarb charcoal. Raw rhubarb has strong catharsis; Cooked rhubarb purging slow, can purging fire detoxification; Wine rhubarb good clear upper jiao blood heat poison; Rhubarb charcoal is used to cool blood and remove stasis. Other studies have found that among the four kinds of rhubarb products, wine rhubarb has the strongest effect on promoting blood circulation and removing blood stasis, while cooked rhubarb is slightly weaker. Raw rhubarb has certain effect on promoting blood circulation and removing blood stasis, while charcoal rhubarb has no effect on promoting blood circulation and removing blood stasis
[10-13]
.
Yishentongluo formula is one of the classic Chinese medicine compounds used for DKD treatment, which consists of 7 kinds of medicines: Salvia miltiorrhiza, Astragalus, Fructus Corni, Rhubarb, cooked Rehmannia, dragon's blood, Euonymus alatus. Previous studies by our research group have found that Yishentongluo can improve DKD through multiple signaling pathways and multiple targets, but its mechanism of action has not been fully clarified
[14]
. Rhubarb is a supplementary drug in Yishentongluo prescription. This study intends to further explore the role and possible mechanism of rhubarb and its active components in DKD through network pharmacology and molecular experiments on the basis of our previous research group. Working flow chart of rhubarb for DKD (Figure 1).
Figure 1. To study the working flow of rhubarb intervention mechanism for DKD.
2. Materials and Methods
2.1. Animal Experiment Verification
Experimental animals: clean Wild type (WT) control mouse, male, body weight (20±5); db/db mouse, male, weight (40±10)g. Purchased from Jiangsu Zhichaokang Biotechnology Co, LTD, Lot number: [SCXK(Su)2018-0008].
2.2. Cell Transfection
Mouse renal tubular epithelial cells (mRTEC) cells were purchased from Guangzhou Genio Biological Co.LTD. Transfection was performed when the cell fusion reached 50-60%. Successively add: DMEM culture solution (no serum, no double antibody), PEI, plasmid, prompt separation, mix, and stand in a sterile environment for 20min; Incubate in a 5% CO2 incubator at 37°C for 4-6h; After 4-6h, discard the transfer solution, add DMEM culture solution (no serum, no double antibody) to the labeled 6-well plate or petri dish, respectively, and incubate in the incubator (37°C, 5% CO2) overnight (generally 24h). On the next day, 6-well plates or petri dishes were taken out, the culture medium was discarded, washed with PBS for 3 times, and culture medium containing different treatments prepared according to the needs of the groups was added to them respectively, and incubated in the incubator (37°C, 5% CO2) for 48h. The cells were divided into the following groups: normal glucose control group (NG), high glucose control group (HG), normal glucose STAT3 no-load and plasmid treatment group, and high glucose STAT3 no-load and plasmid treatment group.
2.3. Materials and Reagents
Rhubarb (Chang Zhongjing Pharmacy, Henan, Lot No.: 220902), aloe-emodin (MCE), mouse anti-STAT3 (Abcam), rabbit anti-phospho-STAT3 (CST), Mouse-anti-IL-1β ELISA (Elabscience), Mouse-anti-IL-18 ELISA (Elabscience), Rabbit-anti-CollagenIII (Sigma), Mouse-anti-E-cadherin (Proteintech), Mouse-anti-Caspase-11 (Santa Cruz), Rabbit-anti-GSDMD (Abcam), STAT3 plasmid (Shanghai Yi Le biological Company), Urinary microalbumin assay kit, Total cholesterol assay kit, Triglyceride determination kit, Creatinine test kit.
2.4. Database Screening of Main Components and Gene Targets of Rhubarb
The active components of Rhubarb extract were screened using TCMSP according to oral bioavailability (OB) ≥ 30% and drug-likeness (DL) ≥ 0.18. Then the Swiss Target Prediction database was used to query and screen out all the gene targets corresponding to the active components of Rhubarb extract, and the target protein was corrected as the gene name by UniProt database after the repeated targets were removed.
2.5. Obtain Dkd Related Gene Targets
On Gene Cards (https://www.genecards.org/) and OMIM (http://www.omim.org) DKD related gene targets are retrieved with the keyword "Diabetic Kidney Disease, DKD" in the database. After collection, repeats are removed, and the intersection targets between rhubarb active ingredients and diseases are obtained through Venn diagram.
2.6. Construction of Protein-Protein Interaction Network
The protein-protein interaction (PPI) between potential targets of rhubarb active ingredients and DKD targets was analyzed through the STRING database, and the protein-protein interaction relationship network was constructed. The relevant parameters are set to: Species is set to Human species, reliability >0.40, and the rest are default values. Delete the discrete target and download the TSV file to import Cytoscape software to map the PPI network. Then the core active ingredients and targets of rhubarb extract for DKD were screened according to the node color depth and Degree.
2.7. Go and Kegg Pathway Enrichment Analysis
The core targets were imported into the DAVID (https://david.ncifcrf.gov/) database for GO and KEGG enrichment analysis. The species "Homo sapiens" was set, and the screening criteria was P<0.01. Then enrichment results through microscopic letter platform (http://www.bioinformatics.com.cn) for the main biological processes and metabolic pathways for visualization, analysis the main biological processes involved and signaling pathway and action mechanism of the rhubarb treatment DKD.
2.8. Construct a "Compound - Target - Pathway" Network Diagram
Construct an "active Compound - Target - pathway" network including active compounds, potential targets and pathways of Rhubarb using Cytoscape software. The color depth of the node is designed according to the degree value.
2.9. Molecular Docking
Download the MOL2 format of two-dimensional structure of core components from TCMSP or Pub Chem database, and then download the PDB format of core targets from PDB (https://www.rcsb.org) database. Auto Dock Tools were used to dewater and hydrogenate the downloaded target protein receptors and ligand small molecules, and then exported and saved as pdbqt file. Docking parameters and docking range were set, and molecular docking of active ingredients and key targets was performed with Auto Dock Vina. The lowest binding energy conformation was saved, the corresponding visualization results were displayed using Pymol software, and the binding energy heat map was constructed using Weisenxin platform software.
2.10. Molecular Experimental
Total cholesterol and triglyceride detection: mixed according to the instructions, incubated at 37°C/10min at 510nm wavelength, and the absorbance value of each hole was determined by enzymolysis. TNF-α, IL-18, IL-1β, creatinine and mouse urinary microalbumin were measured according to the instructions.
The animal protein samples were quantitatively analyzed according to the instructions of the BCA assay kit, and then the proteins were denatured, followed by electrophoresis, membrane transfer, sealing, and primary antibody incubation overnight. The next day, the second antibody was incubated, and finally the development and exposure were performed. The grayscale value of each strip was obtained using Quantity one software (β-actin as the internal parameter), and the relative expression of the target protein was calculated. Western Blot exposure strip gray value processing software Image Lab 4.0 and Quantity one software, data statistical analysis software SPSS21.0, statistical chart making software GraphPad Prism7.0. Statistical data were expressed as mean ± standard deviation ( ), paired T-test was used for comparison between two groups, and one-way analysis of variance was used for comparison between multiple groups. P <0.05 indicated statistically significant differences.
3. Results
3.1. Compounds And Targets of Rhubarb
TCMSP database was used to screen the active ingredients in Rhubarb extract, and the active ingredients were screened according to OB≥30% and DL≥ 0.18 (Table 1). The Swiss Target Prediction database was used to screen all gene targets corresponding to the active components of Rhubarb extract. 13,763 DKD-related Gene targets were obtained from the Gene Cards and OMIM databases, and a total of 343 intersection targets were obtained with the active ingredients of drugs. In view of the fact that a large number of intersection targets was not conducive to the prediction and analysis of subsequent results, the follow-up study was finally conducted with 121 targets greater than the average value (Table 2).
Table 1. TheMolID, OB and DL of compounds in DKD.

MOL ID

Molecule Name

OB (%)

DL

MOL002235

EUPATIN

50.8

0.41

MOL002259

Physciondiglucoside

41.65

0.63

MOL002268

rhein

47.07

0.28

MOL002281

Toralactone

46.46

0.24

MOL002288

Emodin-1-O-beta-D-glucopyranoside

44.81

0.8

MOL002293

Sennoside D_qt

61.06

0.61

MOL002297

Daucosterol_qt

35.89

0.7

MOL000358

beta-sitosterol

36.91

0.75

MOL000471

aloe-emodin

83.38

0.24

MOL000096

(-)-catechin

49.68

0.24
Table 2. Potential targets of Rhubarb and DKD.

No.

Target

No.

Target

No.

Target

No.

Target

No.

Target

1

AKT1

26

ABL1

51

SLC2A1

76

HDAC2

101

CCR1

2

STAT3

27

CDK2

52

CYP3A4

77

DRD2

102

PLK1

3

EGFR

28

SYK

53

PRKCD

78

NOS2

103

CDC25C

4

NFKB1

29

PDGFRB

54

PTPN6

79

PDPK1

104

PTGS1

5

SRC

30

CDK1

55

LGALS3

80

CYP19A1

105

ALOX5

6

ESR1

31

LYN

56

HMGCR

81

TYMS

106

ACHE

7

HSP90AA1

32

PIK3CB

57

CTSS

82

OPRM1

107

GRM5

8

MMP9

33

AR

58

KEAP1

83

RET

108

F2

9

GSK3B

34

ACE

59

PTK2B

84

PRKCZ

109

CYP1B1

10

MTOR

35

ABCB1

60

FLT3

85

IDO1

110

SLC6A3

11

PTGS2

36

NOS3

61

ZAP70

86

XDH

111

SLC6A4

12

CXCR4

37

PTK2

62

MMP3

87

CDK5

112

G6PD

13

TLR4

38

PRKACA

63

AXL

88

PLAT

113

HTR2A

14

PIK3CA

39

NFE2L2

64

SHH

89

CTSD

114

HPRT1

15

KDR

40

NR3C1

65

ALK

90

CHUK

115

CFTR

16

STAT1

41

ABCG2

66

TOP2A

91

GSTP1

116

CYP17A1

17

IGF1R

42

CDK6

67

MAPT

92

DHFR

117

KDM1A

18

MMP2

43

PIK3CD

68

ARG1

93

PPARD

118

GRK5

19

APP

44

PIK3CG

69

PLG

94

CDC25A

119

GRIN1

20

PIK3R1

45

CTSB

70

CCNE1

95

PSMB9

120

ACACA

21

CASP8

46

MPO

71

ROCK1

96

ELANE

121

CYSLTR2

22

PTPN11

47

SERPINE1

72

PTPN1

97

CYP2C19

23

EZH2

48

PDGFRA

73

NOX4

98

BACE1

24

ITGB1

49

CHEK1

74

MAOA

99

CSNK2A1

25

MET

50

ESR2

75

INSR

100

CXCR1
3.2. "Active ingredient-target protein" Network
A Venn diagram of DKD and rhubarb targets was made on the Weishengxinxin visual analysis platform. There were 343 intersection targets between DKD and Rhubarb in total (Figure 2A). The "Active ingredient - target protein" network was constructed using string database and Cytoscape software based on a larger than average 121 target sites (Figure 2B-C).
3.3. Go Functional Enrichment Results
The common intersection target genes were imported into the DAVID database, and then mapped through the Weishengxinxin visual analysis platform, and the functional enrichment results of GO and KEGG were obtained. The GO enrichment results showed that the Biological Progress (BP) of rhubarb in treating DKD mainly included: protein phosphorylation, positive regulation of protein kinase B signaling, protein autophosphorylation, transmembrane receptor protein tyrosine kinase signaling pathway, peptidyl-tyrosine phosphorylation, etc. The enrichment of Cell components (CC) involved mainly concentrated on: cytoplasm, membrane raft, plasma membrane, macromolecular complex, cytosol, etc. protein serine/threonine/tyrosine kinase activity, ATP binding, protein kinase activity, protein tyrosine kinase activity, enzyme binding, etc. The results suggest that DKD is involved in multiple gene functions, and rhubarb may play a role in treating DKD by regulating these biological processes (Figure 3A-D).
Figure 2. Active ingredients and targets of Rhubarb. (A) Venn diagram showing intersection targets of rhubarb and DKD. (B) string diagram shows the network results of protein-to-protein interactions. (C) "Active ingredient-target protein" network diagram. The color gradient from the inner ring to the outer ring varies according to the degree value, and the edge indicates the interaction between proteins.
Figure 3. GO enrichment analysis results. (A) Biological processes (BP). (B) Bubble map of cell composition (CC). (C) Molecular function bubble diagram (MF). The color and size of each bubble is based on the P-value and the number of genes, respectively. (D) GO enrichment analysis. In the first ten enrichment diagrams, green, orange, and purple represent enrichment analysis biological processes, cell components, and molecular functions.
3.4. KEGG Functional Enrichment Results
Analysis of KEGG enrichment results showed signal Pathways (the top 20 signal pathways were selected): including Pathways in cancer, Prostate cancer, Proteoglycans in cancer, Chemokine signaling pathway, PI3K-Akt signaling pathway, etc. It is suggested that rhubarb may achieve therapeutic effects on DKD through these pathways (Figure 4A-B). Network and type files were prepared respectively for pharmaceutical chemical components, higher-than-average intersection targets, and KEGG enriched results, and were uploaded to Cytoscape software to construct the "component-target-pathway" network diagram (Figure 4C). The visual analysis platform of Weishengxin was used to draw the Sankey diagram, and the results showed that one Target gene corresponded to multiple channels, and one channel corresponded to multiple Target genes (Figure 4D). The results of KEGG enrichment showed that cancer signaling pathway ranked first, involving a variety of pathways, such as Jak-STAT signaling pathway, PI3K-Akt signaling pathway, Wnt signaling pathway, VEGF signaling pathway, and mTOR signaling pathway, which affect cell proliferation, apoptosis, and gene damage, etc. (Figure 5).
Figure 4. KEGG enrichment results and "component-target-pathway" network diagram. (A) Bubble maps of the top 20 pathways of KEGG enrichment analysis. (B) Classification of the top 20 pathways. (C) The "ingredient-target-pathway" network diagram involved in the mechanism of rhubarb treatment of DKD: the purple circle, the blue quadrilateral and the green V-shaped represent the active drug ingredients, targets and pathways enriched in Rhubarb, respectively. (D) KEGG's Sankey result graph quantifies the linear flow ratio of incoming/outgoing data for the same node.
Figure 5. The distribution of key targets in Pathway in cancer signaling pathway.
3.5. Molecular Docking
According to the results of PPI analysis, AKT1, STAT3, EGFR, NFκB1, SRC with a higher degree were selected to combine with EUPATIN, Physciondiglucoside, rhein, Toralactone, the main active ingredient of rhubarb. Emodin-1-O-beta-D-glucopyranoside, Sennoside D, Daucosterol, beta-sitosterol, aloe-emodin, (-) -Catechin were sequentially simulated for molecular docking. The results of molecular docking indicate the binding activity between the receptor and the ligand in terms of the binding energy. The smaller the binding energy, the higher the affinity between the receptor and ligand, and the greater the possibility of interaction. Binding energy <−5.0kJ/mol indicates high binding activity, and binding energy <−7.0 kJ/mol indicates strong binding activity. Visualization analysis was performed by Pymol software, and the binding sites were analyzed by PLIP website. According to the selected compounds and target proteins sorted by degree, we focused on aloe-emodin and STAT3. STAT3 and aloe-emodin were combined through hydrophobic interaction, hydrogen bonding and salt bridge, and the binding energy of -7.5 indicated strong binding activity. According to the degree values obtained in PPI, the binding ability of the first 5 core proteins and the active ingredients was predicted, and the heat map was drawn according to the binding energy score (Figure 6A-B).
Figure 6. Molecular docking (A) Heat map of binding energy score of active ingredient and target protein (B) The results of molecular docking between AE and STAT3.
3.6. Detection of Renal Function Indicators
After gavage of rhubarb (3g•kg-1) and AE (10mg/kg), the overall state of the mice was better than that of the db/db group, with no death and decreased BG, and the MAU, CRE and UACR of the mice were decreased (Figure 7A-D), T-CHO and TG were decreased. Both IL-18 and IL-1β were decreased (Figure 7E-H). The difference was statistically significant (P<0.05).
Figure 7. Biochemical index detection (A) Mouse blood glucose statistics (B) Urine microalbumin test results (C) CRE test results (D) UACR ratio test results. Results of T-CHO (E), TG (F), IL-1β (G) and IL-18 (H) in mouse.
3.7. Western Blot and Co-immunoprecipitation
Compared with WT group, the expressions of P-STAT3, STAT3, Caspase-11 and GSDMD-N in kidney tissues in db/db group have been significantly increased, while the expressions of Collagen-III and α-SMA in db/db group have been significantly increased, and the expression of E-cadherin protein in db/db group has been decreased. After Rhubarb and AE intervention, the expression of E-cadherin protein increased, and the other indexes decreased. The difference was statistically significant (P<0.05), while GSDMD-FL did not change (Figure 8A-D). Verification of the interaction between STAT3 and Caspase-11: Co-immunoprecipitation results indicated that there was a protein-protein interaction between STAT3 and Caspase-11 (Figure 8E).
Figure 8. Western blot test results The expression of pyroptosis (A-B) and fibrosis indexes (C-D) was detected in vivo, and the interaction between STAT3 and Caspase-11 was detected by co-immunoprecipitation (E).
3.8. Cell Experiment
After knocking down STAT3, the indicators of pyroptosis and fibrosis were detected. The results showed that the protein of each group was collected for Western blot detection. The results showed that the expressions of Caspase-11 and GSDMD-N decreased significantly after STAT3 knockdown, The expression of Collagen-Ⅲ and α-SMA protein has been down-regulated, while the expression of E-cadherin protein has been recovered, The difference was statistically significant, P<0.05 (Figure 9A-D). After STAT3 overexpression, Western blot analysis of the indicators of pyroptosis and fibrosis showed that: The expressions of Caspase-11 and GSDMD-N increased significantly after overexpression of STAT3. The expression of Collagen-Ⅲ and α-SMA protein was up-regulated, The expression of E-cadherin protein was significantly decreased, and the difference was statistically significant, P<0.05 (Figure 9E-H).
Figure 9. Effects of STAT3 knockdown on pyroptosis (A-B) and fibrosis indexes (C-D). Effects of STAT3 overexpression on pyroptosis (E-F) and fibrosis indexes (G-H).
4. Discussion
DKD is a common complication of diabetes, its pathogenesis is very complex, modern medical treatment can not effectively control the progress of the disease. TCM (TCM), which has been passed down for thousands of years, is safe and effective in treating diabetes through multi-target and multi-factor treatment. Diabetes belongs to the category of "the dispersion-thirst disease" in TCM. The lesion of viscera involves many parts such as lung, stomach and kidney. The physiological functions of kidney include human growth, development, excretion and reproduction. The effect of rhubarb is mainly for purging and attacking accumulation, clearing heat and purging fire, detoxifying, promoting blood circulation and removing blood stasis. Rhubarb has a good purging effect and has a good effect in the treatment of DKD
[15, 16].
Network pharmacology is to search and screen the active ingredients of drugs on the pharmacology database and analysis platform of TCM system. The target genes corresponding to effective chemical components were intersected with disease-related genes. The corresponding signaling pathway was obtained by intersecting target proteins, and the network model of "active ingredient-target-signaling pathway" was established to show the result of the effective active ingredient against the disease through the possible pathway. Thus, the interaction between drug ingredients and disease can be clarified. Compared with the traditional pharmacological experiments, the multi-pathway regulation of the signal pathway can improve the therapeutic effect of drugs and reduce the side effects of drugs.
In this study, 10 active ingredients of Rhubarb were collected by network pharmacology method. The PPI network was constructed by STRING database and Cytoscape software, and AKT1, STAT3, EGFR, NFKB1 and SRC were selected as core targets. According to molecular docking verification, most of the above core targets and the main active components of rhubarb have good binding ability and stable conformation through molecular docking simulation in sequence, and it is speculated that the above core targets are the key targets for rhubarb to interfere with DKD.
Aloe emodin (Rhabarberone), a major active ingredient in Rhubarb, has anti-tumor activity and induces apoptosis by playing an anti-proliferative role. Studies have found that AE can affect the development of some diseases by regulating pyroptosis. But the specific role of AE in DKD is unclear
[17-19]
. Studies have shown that STAT3 can affect the progression of disease by regulating the pyroptosis of cells
[20-22]
. Other studies have shown that STAT3 can interfere with the process of DKD in kidney diseases regardless of whether it is an upstream regulatory factor or a downstream target protein
[23-26]
.
In summary, in the process of DKD, is there a mechanism by which AE affects pyroptosis in DKD by regulating STAT3? The results of molecular docking showed that STAT3 and AE were combined through hydrophobic interaction, hydrogen bonding and salt bridge, and the binding activity was very strong. It is suggested that AE may combine with STAT3 to achieve the purpose of DKD treatment. Interestingly, after the AE intervention of rhubarb and one of its active ingredients. we found that the changes in the indicators were basically the same. Therefore, the potential drug effects of AE on DKD need to be further explored.
5. Conclusions
In conclusion, the intersection targets of rhubarb active compounds and DKD were identified by network pharmacology in this study. After analyzing the results of PPI database and molecular docking technology, this study focused on STAT3 protein and active component AE. Subsequently, molecular biology experiments were used to further verify the relationship between the two, and the final results showed that rhubarb and AE affected the mechanism of pyroptosis in DKD by regulating the STAT3/Caspase-11 axis. This provides a basic experimental basis for exploring the potential effect of rhubarb in the treatment of DKD and the clinical treatment of DKD.
Abbreviations

DKD

Diabetic Kidney Disease

TCM

Traditional Chinese Medicine

AE

Aloe emodin
Author Contributions
Yanwen Mao: Project administration, Writing – review &editing
Minghao Zhang: Writing – revising &editing
Zijuan Zhang: Methodology
Xiaowei Zhang: Methodology
Wenhui Rong: Visualization
Juan Zhang: Investigation
Mengmeng Yang: Software
Jiangyan Xu: Supervision, Project administration
Funding
This work is supported by Name of Funder:
National Key R&D Program of China (No.2020YFE0201800)
Henan Provincial Key Research and Development Program (No.221111520300)
Henan provincial science and technology research and development program joint fund (No.232301420093)
Sponsored by Program for Science&Technology Innovation Talents in Universities of Henan Province (No.24HASTIT072)
Data Availability Statement
The data supporting the outcome of this research work has been reported in this manuscript.
Conflicts of Interest
The authors declare no conflicts of interest.
References
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    Mao, Y., Zhang, M., Zhang, Z., Zhang, X., Rong, W., et al. (2024). Study on the Effect of Rhubarb and Its Active Components on Pyroptosis in DKD by Regulating STAT3/Caspase-11 Axis. American Journal of Clinical and Experimental Medicine, 12(3), 28-44. https://doi.org/10.11648/j.ajcem.20241203.12

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    ACS Style

    Mao, Y.; Zhang, M.; Zhang, Z.; Zhang, X.; Rong, W., et al. Study on the Effect of Rhubarb and Its Active Components on Pyroptosis in DKD by Regulating STAT3/Caspase-11 Axis. Am. J. Clin. Exp. Med. 2024, 12(3), 28-44. doi: 10.11648/j.ajcem.20241203.12

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    AMA Style

    Mao Y, Zhang M, Zhang Z, Zhang X, Rong W, et al. Study on the Effect of Rhubarb and Its Active Components on Pyroptosis in DKD by Regulating STAT3/Caspase-11 Axis. Am J Clin Exp Med. 2024;12(3):28-44. doi: 10.11648/j.ajcem.20241203.12

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  • @article{10.11648/j.ajcem.20241203.12,
  author = {Yanwen Mao and Minghao Zhang and Zijuan Zhang and Xiaowei Zhang and Wenhui Rong and Juan Zhang and Mengmeng Yang and Jiangyan Xu},
  title = {Study on the Effect of Rhubarb and Its Active Components on Pyroptosis in DKD by Regulating STAT3/Caspase-11 Axis
},
  journal = {American Journal of Clinical and Experimental Medicine},
  volume = {12},
  number = {3},
  pages = {28-44},
  doi = {10.11648/j.ajcem.20241203.12},
  url = {https://doi.org/10.11648/j.ajcem.20241203.12},
  eprint = {https://article.sciencepublishinggroup.com/pdf/10.11648.j.ajcem.20241203.12},
  abstract = {Rhubarb has been found to have a certain protective effect on improving the kidney function. However, the specific mechanism is still unclear. In this study, network pharmacology, molecular docking spontaneous binding technology and molecular biology experiments were used to verify the mechanism of rhubarb and its active ingredients in the treatment of DKD. A total of 10 active compounds and 121 (larger than average) target proteins were collected. The target proteins with higher degree value were screened by PPI according to degree value as follows: AKT1, STAT3, EGFR, NFKB1, SRC, etc. GO and KEGG enrichment analysis suggest that rhubarb therapy for DKD mainly involves Pathways in cancer, Prostate cancer, Proteoglycans in cancer, Chemokine signaling pathway, PI3K-Akt signaling pathway, PD-L1 expression and PD-1 checkpoint pathway in cancer, EGFR tyrosine kinase inhibitor resistance signaling pathway and so on. Furthermore, molecular docking results suggest that hydrogen bonding, salt bridge and hydrophobic interactions contribute to spontaneous binding of the compound to the target protein. Experimental verification shows that rhubarb and aloe emodin affect the mechanism of pyroptosis in diabetic kidney disease by regulating STAT3/Caspase11 axis. In conclusion, this study comprehensively elaborated the active compounds, potential targets and molecular experimental mechanisms of rhubarb to provide the basic experimental theory for clinical treatment of DKD.
},
 year = {2024}
}

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  • TY  - JOUR
T1  - Study on the Effect of Rhubarb and Its Active Components on Pyroptosis in DKD by Regulating STAT3/Caspase-11 Axis

AU  - Yanwen Mao
AU  - Minghao Zhang
AU  - Zijuan Zhang
AU  - Xiaowei Zhang
AU  - Wenhui Rong
AU  - Juan Zhang
AU  - Mengmeng Yang
AU  - Jiangyan Xu
Y1  - 2024/07/29
PY  - 2024
N1  - https://doi.org/10.11648/j.ajcem.20241203.12
DO  - 10.11648/j.ajcem.20241203.12
T2  - American Journal of Clinical and Experimental Medicine
JF  - American Journal of Clinical and Experimental Medicine
JO  - American Journal of Clinical and Experimental Medicine
SP  - 28
EP  - 44
PB  - Science Publishing Group
SN  - 2330-8133
UR  - https://doi.org/10.11648/j.ajcem.20241203.12
AB  - Rhubarb has been found to have a certain protective effect on improving the kidney function. However, the specific mechanism is still unclear. In this study, network pharmacology, molecular docking spontaneous binding technology and molecular biology experiments were used to verify the mechanism of rhubarb and its active ingredients in the treatment of DKD. A total of 10 active compounds and 121 (larger than average) target proteins were collected. The target proteins with higher degree value were screened by PPI according to degree value as follows: AKT1, STAT3, EGFR, NFKB1, SRC, etc. GO and KEGG enrichment analysis suggest that rhubarb therapy for DKD mainly involves Pathways in cancer, Prostate cancer, Proteoglycans in cancer, Chemokine signaling pathway, PI3K-Akt signaling pathway, PD-L1 expression and PD-1 checkpoint pathway in cancer, EGFR tyrosine kinase inhibitor resistance signaling pathway and so on. Furthermore, molecular docking results suggest that hydrogen bonding, salt bridge and hydrophobic interactions contribute to spontaneous binding of the compound to the target protein. Experimental verification shows that rhubarb and aloe emodin affect the mechanism of pyroptosis in diabetic kidney disease by regulating STAT3/Caspase11 axis. In conclusion, this study comprehensively elaborated the active compounds, potential targets and molecular experimental mechanisms of rhubarb to provide the basic experimental theory for clinical treatment of DKD.

VL  - 12
IS  - 3
ER  -

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Author Information

  • Yanwen Mao

    Academy of Medical, Henan University of Chinese Medicine, Zhengzhou, China

    Biography: Yanwen Mao is a lecturer at Henan University of TCM.She received her Doctor of Medicine degree in 2021. In recent years, he has published a number of SCI articles and presided over and participated in a number of national and provincial scientific research cooperation projects. She is currently the director of the General Practice Branch of China Information Society of TCM.

    Research Fields: Pathogenesis of chronic kidney disease and traditional Chinese medicine prevention and treatment; Neurodegenerative diseases and traditional Chinese medicine prevention and treatment

    http://orcid.org/0009-0005-2036-9109

  • Minghao Zhang

    Academy of Medical, Henan University of Chinese Medicine, Zhengzhou, China

    Research Fields: Pathogenesis of chronic kidney disease and traditional Chinese medicine prevention and treatment; Neurodegenerative diseases and traditional Chinese medicine prevention and treatment

    http://orcid.org/0009-0001-6550-546X

  • Zijuan Zhang

    Academy of Medical, Henan University of Chinese Medicine, Zhengzhou, China

    Research Fields: Neurodegenerative diseases and traditional Chinese medicine prevention and treatment

    http://orcid.org/0000-0001-7047-4795

  • Xiaowei Zhang

    Academy of Chinese Medical Sciences, Henan University of Chinese Medicine, Zhengzhou, China

    Research Fields: Pathogenesis of chronic kidney disease and traditional Chinese medicine prevention and treatment

    http://orcid.org/0009-0001-3936-8297

  • Wenhui Rong

    Academy of Medical, Henan University of Chinese Medicine, Zhengzhou, China

    Research Fields: Cardiovascular system disease and traditional Chinese medicine prevention and treatment

    http://orcid.org/0009-0000-9006-7193

  • Juan Zhang

    Academy of Medical, Henan University of Chinese Medicine, Zhengzhou, China

    Research Fields: Pathogenesis and prevention of liver fibrosis with traditional Chinese medicine

    http://orcid.org/0009-0004-2336-6491

  • Mengmeng Yang

    School of Management, Henan University of Chinese Medicine, Zhengzhou, China

    Research Fields: Chronic lung diseases and traditional Chinese medicine prevention and treatment

    http://orcid.org/0009-0001-6154-0030

  • Jiangyan Xu

    Henan Engineering Research Center for Prevention and Treatment of Major Chronic Diseases with Chinese Medicine, Henan University of Chinese Medicine, Zhengzhou, China

    Research Fields: Pathogenesis of chronic kidney disease and traditional Chinese medicine prevention and treatment; Neurodegenerative diseases and traditional Chinese medicine prevention and treatment; Cardiovascular system disease and traditional Chinese medicine prevention and treatment

    Contact Email

    http://orcid.org/0000-0002-8723-1463

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  • Abstract
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  • Document Sections

    1. 1. Introduction
    2. 2. Materials and Methods
    3. 3. Results
    4. 4. Discussion
    5. 5. Conclusions
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  • Abbreviations
  • Author Contributions
  • Funding
  • Data Availability Statement
  • Conflicts of Interest
  • References
  • Cite This Article
  • Author Information

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