4.6 Article

Src-mediated Tyr353 phosphorylation of IP3R1 promotes its stability and causes apoptosis in palmitic acid-treated hepatocytes

EXPERIMENTAL CELL RESEARCH (2021)

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Journal

EXPERIMENTAL CELL RESEARCH
Volume 399, Issue 2, Pages -

Publisher

ELSEVIER INC
DOI: 10.1016/j.yexcr.2020.112438

Keywords

Apoptosis; IP3R1; src kinase; NAFLD

Categories

Oncology Cell Biology

Funding

  1. National Key R&D Program of China [2018YFC1312700]
  2. National Natural Science Foundation of China [81970510, 31971084]
  3. talent project of chongqing [CQYC2019050790]
  4. Science and Technology Research Program of Chongqing Municipal Education Commission [KJQN201900438]
  5. 111 Project of China [D20028]

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This study revealed that palmitic acid induces hepatocyte apoptosis through promoting the phosphorylation and stability of IP3R1 via the activation of the src pathway, leading to mitochondrial dysfunction and Ca2+ overload in hepatic cells. The inhibition of the src/IP3R1 pathway may offer a potential therapeutic approach for the treatment of NAFLD.
Palmitic acid (PA)-induced hepatocyte apoptosis is critical for the progression of nonalcoholic fatty liver disease (NAFLD). Inositol 1,4,5-trisphosphate receptor type 1 (IP3R1) is an intracellular Ca2+-release channel and is involved in PA-induced hepatocyte apoptosis. While the expression of IP3R1 is elevated in patients with NAFLD and in hepatocytes treated with PA, it remains unclear how PA promotes the expression of IP3R1. In present study, our results showed that PA induced mitochondrial dysfunction and apoptosis, which is accompanied with the increase of the IP3R1 expression in hepatic cells. The inhibition of IP3R1 expression using siRNA ameliorated the PA-induced mitochondrial dysfunction. Furthermore, PA enhanced the stability of the IP3R1 protein instead of an increase in its mRNA levels. PA also promoted the phosphorylation of IP3R1 at the Tyr353 site and increased the phosphorylation of src in hepatic cells. Moreover, an inhibitor of src kinase (SU6656) significantly reduced the Tyr353 phosphorylation of IP3R1 and decreased its stability. In addition, SU6656 improved mitochondrial function and reduced apoptosis in hepatocytes. Conclusion: PA promotes the Tyr353 phosphorylation of IP3R1 by activating the src pathway and increasing the protein stability of IP3R1, which consequently results in mitochondrial Ca2+ overload and mitochondrial dysfunction in hepatic cells. Our results also suggested that inhibition of the src/IP3R1 pathway, such as by SU6656, may be a novel potential therapeutic approach for the treatment of NAFLD.

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