4.7 Article

Dissection of Targeting Molecular Mechanisms of Aristolochic Acid-induced Nephrotoxicity via a Combined Deconvolution Strategy of Chemoproteomics and Metabolomics

INTERNATIONAL JOURNAL OF BIOLOGICAL SCIENCES (2022)

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Journal

INTERNATIONAL JOURNAL OF BIOLOGICAL SCIENCES
Volume 18, Issue 5, Pages 2003-2017

Publisher

IVYSPRING INT PUBL
DOI: 10.7150/ijbs.69618

Keywords

Aristolochic acid nephropathy; chemical proteomics; mitochondrial dysfunction; apoptosis; metabolism

Categories

Biochemistry & Molecular Biology Biology

Funding

  1. National Key Research and Development Program of China [2020YFA0908000]
  2. Innovation Team and Talents Cultivation Program of National Administration of Traditional Chinese Medicine [ZYYCXTD-C-202002]
  3. National Natural Science Foundation of China [82074098, 81903588]
  4. CACMS Innovation Fund [CI2021A05101]
  5. Fundamental Research Funds for the Central public welfare research institutes [ZZ14YQ-050, ZZ14-YQ-051, ZZ14-ND-010, ZZ15-ND-10, ZZ14-FL-002, ZZ15-YQ-063]

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This study reveals the targeting molecular mechanisms of AA-induced nephrotoxicity. Key enzymes involved in metabolic processes and mitochondrial respiration were found to be directly bound by AA, disrupting metabolic biosynthesis processes and impairing mitochondrial functions. This ultimately leads to renal cell apoptosis and the development of aristolochic acid nephropathy.
Aristolochic acid (AA), mainly derived from herbal Aristolochia and Asarum plants, was listed as a human carcinogen class I in 2002. Aristolochic acid nephropathy (AAN) is a rapidly progressive tubulointerstitial nephritis and urothelial cancer caused by AA. However, the targeting molecular mechanisms of AAs-induced nephrotoxicity are largely unclear. This study aims to dissect targeting molecular mechanisms of AA-induced nephrotoxicity. Activity-based protein profiling (ABPP) in combination with cellular thermal shift assay (CETSA) was performed to identify the AAs binding target proteins. Our data indicated that several key enzymes in the metabolic process and mitochondrial respiration including IDH2 and MDH2 (Krebs cycle), PKM and LDH (aerobic respiration), FASN (fatty acid beta-oxidation), HK2 (glucose metabolism), and ATP synthase were identified as directly binding targets of AAs. Metabolomics and oxygen consumption rate (OCR) experiments further confirmed that AAs targeting proteins disrupted metabolic biosynthesis processes and impaired mitochondrial functions. Ultimately, AAs induced renal cells apoptosis by disturbing various biological processes. Cumulatively, AAs may directly bind to key proteins involved in the metabolic process and mitochondrial homeostasis, and finally induce aristolochic acid nephropathy. Our findings provide novel insight into underlying mechanisms of AAs-induced kidney toxicity, which may help to develop therapeutic strategies for AAN.

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