Network pharmacology and experimental validation of asiaticoside protecting against diabetic kidney disease by regulating 11β-hydroxysteroid dehydrogenase type 2

doi:10.19852/j.cnki.jtcm.2026.03.008

Journal of Traditional Chinese Medicine ›› 2026, Vol. 46 ›› Issue (3): 641-651.DOI: 10.19852/j.cnki.jtcm.2026.03.008

• Original Articles • Previous Articles Next Articles

Network pharmacology and experimental validation of asiaticoside protecting against diabetic kidney disease by regulating 11β-hydroxysteroid dehydrogenase type 2

ZHU Qin¹, BI Peng¹, ZENG Jiali¹, ZHANG Yang¹, HU Lidan², CAO Zhongkai², ZHU Jingyu¹, JIN Qinyang³()

¹ Department of Nephrology (Key Laboratory of Zhejiang Province, Management of Kidney Disease), Hangzhou Traditional Chinese Medicine Hospital Affiliated to Zhejiang Chinese Medical University, Hangzhou 310007, China
² the Children’s Hospital, Zhejiang University School of Medicine, National Clinical Research Center for Child Health, Hangzhou 310052, China
³ Geriatric Medicine Center, Department of Geriatric Medicine, Zhejiang Provincial People's Hospital (Affiliated People's Hospital), Hangzhou Medical College, Hangzhou 310014, China

Received:2024-12-22 Accepted:2025-07-05 Online:2026-06-15 Published:2026-06-08
Contact: JIN Qinyang, Geriatric Medicine Center, Department of Geriatric Medicine, Zhejiang Provincial People's Hospital (Affiliated People's Hospital), Hangzhou Medical College, Hangzhou 310014, China. jqy119@163.com, Telephone: +86-13777877613
About author:First author contact:
ZHU Qin and BI Peng are co-first authors and contributed equally to this work
Supported by:
National Natural Science Foundation of China for Young Scholars: Study on the Mechanism of Compound Centella Asiatica Mediate 24-dehydrocholesterol Reductase (DHCR24)/Liver X Receptor (LXR) Signaling Axis to Regulate Macrophage Activation and Alleviate Microinflammation in Diabetic Kidney Disease(82205008);Medical Scientific Research Foundation of Zhejiang Province, China: Mechanistic Study of Asiaticoside in Regulating Macrophage Innate Immune Response in Diabetic Kidney Disease by Maintaining Cholesterol Homeostasis via the DHCR24/Desmosterol/ LXR Signaling Axis(2023RC242);Zhejiang Traditional Medicine and Technology Program, China: Research on the Construction of a Knowledge Graph for the Academic Thoughts and Clinical Experience of Famous Traditional Chinese Medicine Practitioner Chen Hongyu in Diagnosing and Treating Diabetic Kidney Disease(2023ZF137);Hangzhou Science and Technology Bureau project: Precise Diagnosis of Prostate Malignancies Using Artificial Intelligence(20231203A12);Special key research project of the Affiliated Hospital of Zhejiang University of Traditional Chinese Medicine: Study on Clinical Auxiliary Decision-Making Model for Professor Wang Yongjun in Diagnosis and Treatment of Diabetic Kidney Disease Based on Graph Convolutional Neural Network(2022FSYYZZ14)

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Abstract

Abstract:

OBJECTIVE: To explore the protective effects and mechanisms of Asiaticoside (AC) against diabetic kidney disease (DKD) through network pharmacology combined with in vitro and in vivoexperiments.

METHODS: Based on network pharmacology and RNA sequencing (RNA-Seq) analyses, combined with molecular docking, the core targets and signaling pathways of AC in the treatment of DKD were predicted and screened. Subsequently, the therapeutic effect of AC on DKD was validated in db/db mice and SV40-MES-13 cells, and its molecular mechanism was evaluated.

RESULTS: Network pharmacology and protein-protein interaction analyses identified 11-beta hydroxysteroid dehydrogenase type 2 (HSD11B2) as a potential key target for AC treatment of DKD. Molecular docking indicated strong affinity between AC derivative and HSD11B2. RNA-Seq analysis showed that AC significantly regulated steroid metabolism under diabetic conditions. In db/db mice, AC reduced urinary protein excretion, improved renal morphology, and protected renal function. AC also dose-dependently inhibited excessive proliferation of SV40-MES-13 cells in a high-glucose environment. Further validation showed that AC upregulated Hsd11b2 mRNA expression and HSD11B2 protein levels.

CONCLUSION: AC may alleviate DKD-related pathological processes by regulating Hsd11b2 gene expression and HSD11B2 protein levels.

Key words: diabetic kidney disease, asiaticoside, hydroxysteroid 11-beta dehydrogenase 2, network pharmacology, RNA-sequencing, molecular docking

ZHU Qin, BI Peng, ZENG Jiali, ZHANG Yang, HU Lidan, CAO Zhongkai, ZHU Jingyu, JIN Qinyang. Network pharmacology and experimental validation of asiaticoside protecting against diabetic kidney disease by regulating 11β-hydroxysteroid dehydrogenase type 2[J]. Journal of Traditional Chinese Medicine, 2026, 46(3): 641-651.

Figures/Tables 5

Table 1 Common targets of GO biologic processes

Term ID	Term description	Matching proteins in network (labels)	FDR
GO:0048545	Response to steroid hormone	NR3C1, CASP3, HSD11B2, ANXA1, ATP1A3, ATP1A1	3.32E-05
GO:0033993	Response to lipid	NR3C1, CASP3, HSD11B2, NFKB2, ANXA1, ATP1A3, ATP1A1	9.37E-05
GO:0051384	Response to glucocorticoid	NR3C1, CASP3, HSD11B2, ANXA1	0.0024
GO:0071383	Cellular response to steroid hormone stimulus	NR3C1, ANXA1, ATP1A3, ATP1A1	0.0024
GO:1901700	Response to oxygen-containing compound	NR3C1, CASP3, HSD11B2, NFKB2, ANXA1, ATP1A3, ATP1A1	0.0024
GO:0071407	Cellular response to organic cyclic compound	NR3C1, CASP3, ANXA1, ATP1A3, ATP1A1	0.0036
GO:1903416	Response to glycoside	ATP1A3, ATP1A1	0.0069

Figure 1 High-dose AC intervention alleviates the deterioration of biochemical parameters induced by DKD A: body weight; B: FBG; C: Scr; D: BUN; E: 24-h urinary protein in the 6 groups. Mice were randomly divided into six groups (n = 5 per group) and treated via oral gavage once daily for 12 weeks: control group (db/m), model group (db/db), low-dose AC group (5 g/kg), medium-dose AC group (15 g/kg), high-dose AC group (45 g/kg), and positive control group (valsartan, 5 mg/kg). All compounds were prepared as 0.2 mL suspensions for daily oral administration. AC: asiaticoside; DKD: diabetic kidney disease; FBG: fasting blood glucose; Scr: serum creatinine; BUN: blood urea nitrogen; LD: low-dose; MD: medium-dose; HD: high-dose. Differences among groups were assessed using one-way analysis of variance and the Bonferroni test. Data are presented as mean ± standard deviation (n = 5). aP < 0.01, bP < 0.05, compared with the db/m group; cP < 0.01, eP < 0.05, compared with the db/db group; dP < 0.01 compared with the AC (LD) group.

Figure 2 High-dose AC intervention ameliorated the abnormal pathological changes caused by DKD A: PAS staining and TEM; A1: db/m group; A2: db/m group; A3: db/db group; A4: db/db group; A5: AC (LD) group; A6: AC (LD) group; A7: AC (MD) group; A8: AC (MD) group; A9: AC (HD) group; A10: AC (HD) group; A11: Val group; A12: Val group; B: mesangial matrix areas; C: foot process effacement rate. Mice were randomly divided into six groups and treated via oral gavage once daily for 12 weeks: control group (db/m), model group (db/db), low-dose AC group (5 g/kg), medium-dose AC group (15 g/kg), high-dose AC group (45 g/kg), and positive control group (valsartan, 5 mg/kg). All compounds were prepared as 0.2 mL suspensions for daily oral administration. AC: asiaticoside; DKD: diabetic kidney disease; PAS: periodic acid-schiff; TEM: transmission electron microscope; FPR: foot process effacement; LD: low-dose; MD: medium-dose; HD: high-dose. Differences among groups were assessed using one-way analysis of variance and the Bonferroni test. Data are presented as mean ± standard deviation (n = 5). aP < 0.01 compared with the db/m group; bP < 0.01 compared with the db/db group; cP < 0.05, dP < 0.01 compared with the AC (LD) group.

Figure 3 High-dose AC treatment showed significant inhibition of cell proliferation in vitro A: SV40-MES-13 cells were exposed to normal- or high-glucose conditions at 48 h at different concentrations of AC treatment (200 × with 15 × zoom); A1: NG; A2: HG; A3: HG + LD; A4: HG + MD; A5: HG + HD; B: inhibition rates of SV40-MES-13 cell proliferation in various groups were assayed by CCK8. NG: normal glucose, 5 mmol/L; HG: high glucose, 30 mmol/L; LD: low dose AC, 0.1 mmol/L; MD: medium dose AC, 1 mmol/L; HD: high dose AC, 10 mmol/L. AC: asiaticoside; LD: low-dose; MD: medium-dose; HD: high-dose: HG: high glucose. Differences among groups were assessed using one-way analysis of variance and the Bonferroni test. Data are presented as mean ± standard deviation (n = 5). aP < 0.01, compared with NG; bP < 0.01, compared with HG.

Figure 4 High-dose AC intervention protected against DKD mice by upregulating HSD11B2 A: the levels of HSD11B2 protein in mice with or without DKD as well as the intervention of high-dose AC revealed from Western blot; A1: representative western blot bands of HSD11B2 in each group; A2: representative western blot bands of Vinculin in each group; A3: quantitative analysis of HSD11B2 protein expression normalized to Vinculin; B: IHC-stained sites and relevant statistical analysis of HSD11B2 protein in kidney tissues; B1: db/m group; B2: db/db group; B3: AC (HD) group; C: HSD11B2-stain-positive area; D: ELISA results of HSD11B2 protein in the 3 groups; E: mRNA level of the expression of Hsd11b2 in the 3 groups. Mice were randomly divided into six groups and treated via oral gavage once daily for 12 weeks: control group (db/m), model group (db/db), low-dose AC group (5 g/kg), medium-dose AC group (15 g/kg), high-dose AC group (45 g/kg), and positive control group (valsartan, 5 mg/kg). All compounds were prepared as 0.2 mL suspensions for daily oral administration. AC: asiaticoside; DKD: diabetic kidney disease; ELISA: enzyme-linked immunosorbent assay; HSD11B2: 11-beta hydroxysteroid dehydrogenase type 2; IHC: immunohistochemistry. Black arrows indicate the distal convoluted tubules with positive staining. Differences among groups were assessed using one-way analysis of variance and the Bonferroni test. Data are presented as mean ± standard deviation (n = 5). aP < 0.01, compared with the db/m group; bP < 0.01, cP < 0.05,compared with the db/db group; dP < 0.01, AC (HD) compared with db/m group.

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