Qizhi Jiangtang capsule (芪蛭降糖胶囊) activates podocyte autophagy in diabetic kidney disease by inhibiting phosphatidylinositol 3-kinase/protein kinase B/mammalian target of rapamycin pathways

doi:10.19852/j.cnki.jtcm.20230428.001

Abstract

Abstract:

OBJECTIVE: To investigate the therapeutic action and mechanism of the Qizhi Jiangtang capsule (芪蛭降糖胶囊, QZJT) on diabetic kidney disease (DKD) treatment.

METHODS: This experiment used db/db mice and podocytes (MPC5) to develop DKD model. Evaluation of the effect of the QZJT on db/db mice by testing urine and blood biochemical parameters (24-h urinary albumin, serum creatinine, blood urine nitrogen), pathological kidney injury, and podocyte integrity. Moreover, autophagosomes in podocytes of DKD mice and cultured podocytes were detected using electron microscopy. Additionally, Western blotting was applied to detect the expression of podocyte marker protein (podocin), autophagy-associated proteins, and phosphatidylinositol 3-kinase/protein kinase B/mammalian target of rapamycin (PI3K/AKT/mTOR) signaling pathway changes in vivo and in vitro.

RESULTS: QZJT significantly reduced urine protein, blood nitrogen urea, and serum creatinine and showed histological restoration of renal tissues. QZJT also significantly improved the down-regulation of podocin and foot fusion and effacement in db/db mice. QZJT increased autophagic vesicles in mice and cultured podocytes. QZJT also upregulated microtubule-associated protein 1 light chain 3-II (LC3-II) / (LC3-I) and Beclin-1 and downregulated phosphorylated-PI3K (p-PI3K), p-AKT, and p-mTOR in db/db mice and MPC5 cells. However, autophagy inhibitor 3-methyladenine partially alleviated the above effects in MPC5 cells.

CONCLUSIONS: These results showed that the QZJT can enhance podocyte autophagy and ameliorate podocyte injury in DKD by inhibiting the PI3K/AKT/mTOR signaling pathway.

Key words: diabetic kidney disease, podocytes, autophagy, AKT, Qizhi Jiangtang capsule

GUO Zhaoan, SUN Lina, LIU Yingying, LI Ruifeng, LIU Chong, DIAO Ke, SHI Jing, SUN Jun. Qizhi Jiangtang capsule (芪蛭降糖胶囊) activates podocyte autophagy in diabetic kidney disease by inhibiting phosphatidylinositol 3-kinase/protein kinase B/mammalian target of rapamycin pathways[J]. Journal of Traditional Chinese Medicine, 2023, 43(4): 667-675.

Figures/Tables 5

Table 1 Effects of QZJT on Urine protein, Scr and BUN in db/db mice ($\bar{x}±s$)

Group	n	Urine protein (mg/24 h)	Scr(μmol/L)	BUN (mmol/L)
db/m	10	80.5±11.9	52.3±10.3	5.6±1.4
db/db	10	153.7±11.2^a	131.8±13.2^a	12.4±1.2^a
db/db+RAP	10	126.6±9.5^b	89.4±12.8^b	7.5±1.1^b
db/db+QZJT	10	129.7±6.1^b	79.2±16.8^b	8.3±1.2^b

Figure 1 QZJT improves pathological damage and podocyte injury in db/db mice Renal tissues were observed by staining with PAS (A1-A4), and Masson (B1-B4) and photographed by a light microscope (× 400 magnification) in db/m, db/db, db/db + RAP, db/db + QZJT group, respectively. C1-C4: representative fields of podocyte foot processes under electron microscopy (scale bars: 5 μm) in db/m, db/db, db/db+RAP, db/db + QZJT group, respectively. D: Western blot of nephrin and podocin expression in the four groups. E: relative band intensities were used in order to quantify nephrin expression levels. F: relative band intensities were used in order to quantify podocin protein expression levels. Eight-week-old db/db mice were treated with or without QZJT or rapamycin. Db/m (control group group, n = 10), db/db (diabetic kidney disease group, n = 10), db/db+RAP (rapamycin (5 mg·kg-1·d-1), n = 10), db/db + QZJT group (QZJT 3.9 g/kg, n = 10). QZJT: Qizhi Jiangtang capsule; RAP: rapamycin; GAPDH: glyceraldehyde-3-phosphate dehydrogenase; PAS: periodic acid-Schiff; Masson: Masson's trichrome staining; EM: electron microscopy. Student t-test and one-way analysis of variance were used for comparison analysis. aP < 0.01, the db/db group vs the db/m group, bP < 0.05, the db/db group vs the db/db + RAP group or db/db + QZJT group, cP < 0.05, the db/db group vs the db/m group.

Figure 2 QZJT treatment induces podocyte autophagy in db/db mice A: autophagic vesicles (autophagosomes, arrows) of podocytes in the four groups were detected by transmission electron microscopy. Scale bar: 1 μm; B: the number of autophagic vesicles was detected by transmission electron microscopy in 10-15 randomly selected electron micrographs from the four groups; C, D: Western blot of LC3I, LC3II, beclin-1 expression in db/m, db/db, db/db + RAP, db/db + QZJT. E: quantitative analysis of LC3II/LC3I protein levels. Eight-week-old db/db mice were treated with or without QZJT or rapamycin. F: quantitative analysis of beclin-1 protein levels.Eight-week-old db/db mice were treated with or without QZJT or rapamycin. Db/m (control group group, n = 10), db/db (diabetic kidney disease group, n = 10), db/db + RAP (rapamycin (5 mg·kg-1·d-1), n = 10), db/db + QZJT group (QZJT 3.9 g/kg, n = 10). QZJT: Qizhi Jiangtang capsule; HG: high glucose; NG: normal glucose; RAP: rapamycin; LC3: light chain 3; AV: autophagic vacuole. Student t-test and one-way analysis of variance were used for comparison analysis. aP < 0.05, bP < 0.01, the db/db group vs the db/m group; cP < 0.05, the db/db group vs the db/db + RAP group or db/db + QZJT group.

Figure 3 QZJT treatment plays a protective role in podocytes exposed to HG by regulating autophagy A: representative western blotting images of nephrin and synaptopodin in NG, HG, HG + QZJT, HG + QZJT + 3MA groups; B: representative Western blotting images of LC3 II, LC3 I and beclin-1 in the four groups; C: quantitative analysis of nephrin expression levels; D: quantitative analysis of synaptopodin expression levels; E: quantitative analysis of LC3II/LC3I protein levels; F: quantitative analysis of beclin-1 protein levels; G1: autophagic vesicles (autophagosomes, arrows) of podocytes in NG group were detected by transmission electron microscopy; G2: autophagic vesicles (autophagosomes, arrows) of podocytes in HG group were detected by transmission electron microscopy; G3: autophagic vesicles (autophagosomes, arrows) of podocytes in HG + QZJT group were detected by transmission electron microscopy; G4: autophagic vesicles (autophagosomes, arrows) of podocytes in HG + QZJT + 3MA group were detected by transmission electron microscopy; H: the number of autophagic vesicles was detected by transmission electron microscopy in 10-15 randomly selected electron micrographs from each group. The differentiated podocytes were incubated with normal glucose (NG, 5.5 mM) or high glucose (HG, 35 mM). The cells in the QZJT groups were preconditioned with 10% drug-containing serum for 2 h, then cultured in high glucose for 48 h (HG + QZJT). The cells in the QZJT + 3MA group were pre-treated with 5 mM of 3MA for 1 h before QZJT treatment, then cultured in high glucose for 48 h (HG + QZJT + 3MA). QZJT: Qizhi Jiangtang capsule; HG: high glucose; NG: normal glucose; LC3: light chain 3; AV: autophagic vacuole; 3MA: 3 methyladenine. Student t-test and one-way analysis of variance were used for comparison analysis. aP < 0.01, the HG group vs the NG group; bP < 0.05, cP < 0.01, the HG group vs the HG + QZJT group or HG + QZJT + 3MA group; dP < 0.05, the HG group vs the NG group.

Figure 4 Effect of QZJT on PI3K/AKT pathway in db/db mice and HG-induced podocytes A: representative western blotting images of p-PI3K, p-AKT and p-mTOR in the four groups of mice; B: quantitative analysis of p-PI3K expression levels in the four groups of mice; C: quantitative analysis of p-AKT expression levels in the four groups of mice; D: quantitative analysis of p-mTOR expression levels in the four groups of mice. Eight-week-old db/db mice were treated with or without QZJT or rapamycin. Db/m (control group group, n = 10), db/db (diabetic kidney disease group, n = 10), db/db + RAP (rapamycin (5 mg·kg-1·d-1), n = 10), db/db + QZJT group (QZJT 3.9 g/kg, n = 10). QZJT: Qizhi Jiangtang capsule; HG: high glucose; NG: normal glucose; RAP: rapamycin; p-PI3K: phosphorylated phosphatidylinositol 3-kinase; p-AKT: phosphorylated protein kinase B; p-MTOR: phosphorylated mammalian target of rapamycin. Student t-test and one-way analysis of variance were used for comparison analysis. aP < 0.01, the db/db group vs the db/m group, bP < 0.01, cP < 0.05, the db/db group vs the db/db + RAP group or db/db + QZJT group; E: representative western blotting images of p-PI3K, p-AKT and p-mTOR in NG, HG, HG + QZJT, HG + QZJT + 3MA groups. F: relative band intensities were used in order to quantify protein p-PI3K expression levels; G: relative band intensities were used in order to quantify protein p-AKT expression levels; H: relative band intensities were used in order to quantify protein p-mTOR expression levels.The differentiated podocytes were incubated with normal glucose (NG, 5.5 mM) or high glucose (HG, 35 mM). The cells in the QZJT groups were preconditioned with 10% drug-containing serum for 2 h, then cultured in high glucose for 48 h (HG + QZJT). The cells in the QZJT + 3MA group were pre-treated with 5 mM of 3MA for 1 h before QZJT treatment, then cultured in high glucose for 48 h (HG + QZJT + 3MA). 3MA: 3 methyladenine. Student t-test and one-way analysis of variance were used for comparison analysis. dP < 0.01, eP < 0.05, the HG group vs the NG group; fP < 0.01, the HG group vs the HG + QZJT group or HG + QZJT + 3MA group.

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