Astragalus mongholicus bunge and panax notoginseng formula (A&P) improves renal fibrosis in UUO mice via inhibiting the long non-coding RNA A330074K22Rik and downregulating ferroptosis signaling.

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Author(s): Zhong, Xia¹ (AUTHOR); Huang, Yue^2,3 (AUTHOR); Jia, Jian¹ (AUTHOR); Liu, Jian² (AUTHOR); Su, Hongwei^1,4 (AUTHOR); Hu, Qiongdan² (AUTHOR) ; Tan, Ruizhi¹ (AUTHOR) ; Wang, Li¹ (AUTHOR)
Source:
BMC Complementary Medicine & Therapies. 7/19/2024, Vol. 24 Issue 1, p1-15. 15p.
Subject Terms:
*Ureter surgery; *Astragalus (Plants); *Chinese medicine; *Combination drug therapy; *In vitro studies; *Epithelial cells; *Small interfering RNA; *Ureteric obstruction; *Herbal medicine; *Plasmids; *Polymerase chain reaction; *Cellular signal transduction; *In vivo studies; *Electroporation; *Reverse transcriptase polymerase chain reaction; *Descriptive statistics; *Fibrosis; *RNA; *Mice; *Chronic kidney failure; *Immunohistochemistry; *Gene expression; *Messenger RNA; *Cell death; *Animal experimentation; *Molecular structure; *Dosage forms of drugs; *Western immunoblotting; *Kidney diseases; *Ginseng; *Data analysis software; *Comparative studies; *Transforming growth factors-beta; *Drug synergism

Additional Information
- Abstract:
  Background: Chronic kidney disease (CKD) and its associated end-stage renal disease (ESRD) are significant health problems that pose a threat to human well-being. Renal fibrosis is a common feature and ultimate pathological outcome of various CKD leading to ESRD. The Astragalus mongholicus Bunge and Panax notoginseng formula (A&P) is a refined compound formulated by our research group, which has been clinically administered for over a decade and has demonstrated the ability to improve the inflammatory state of various acute or chronic kidney diseases. However, the underlying mechanism by which A&P ameliorates renal fibrosis remains unclear. Methods: We established a mouse model by surgically ligating the unilateral ureter to induce renal injury in vivo. And we utilized renal in situ electroporation of a plasmid with low LncRNA A33 expression to establish the unilateral ureteral obstruction(UUO)mouse model. In vitro, we stimulated primary tubular epithelial cells(pTEC) injury using TGF-β1, siRNA-A33, and pcDNA3.1-A33 plasmids were transfected into pTECs to respectively knockdown and overexpress LncRNA A33, and both in vitro and in vivo models were intervened with A&P. Results: The results demonstrated that A&P effectively alleviated renal fibrosis in mice. Subsequent findings indicated high expression of LncRNA A33 in the kidneys of UUO mice and TGF-β1-induced renal tubular cells. In situ, renal electroporation of a plasmid with reduced LncRNA A33 expression revealed that inhibiting LncRNA A33 significantly improved renal fibrosis in UUO mice. Moreover, A&P effectively suppressed LncRNA A33 expression both in vitro and in vivo. Subsequent downregulation of LncRNA A33 in renal tubular epithelial cells resulted in the downregulation of numerous fibrotic markers, a significant inhibition of LncRNA A33, and a notable reduction in downstream ferroptosis signaling. Cell experiments demonstrated that A&P improved renal fibrosis in UUO mice by inhibiting LncRNA A33 and downregulating ferroptosis signaling. Conclusion: Through the inhibition of LncRNA A33 and subsequent downregulation of ferroptosis signaling, A&P showed potential as a therapeutic approach for improving renal fibrosis in UUO mice, providing a potential treatment avenue for CKD. [ABSTRACT FROM AUTHOR]

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Astragalus mongholicus bunge and panax notoginseng formula (A&P) improves renal fibrosis in UUO mice via inhibiting the long non-coding RNA A330074K22Rik and downregulating ferroptosis signaling.

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