4.7 Article

MYC drives autophagy to adapt to stress in Penaeus vannamei

期刊

FISH & SHELLFISH IMMUNOLOGY
卷 126, 期 -, 页码 187-196

出版社

ACADEMIC PRESS LTD- ELSEVIER SCIENCE LTD
DOI: 10.1016/j.fsi.2022.05.020

关键词

PvMYC; Autophagy; Low temperature; Penaeus vannamei

资金

  1. National Natural Sci-ence Foundation of China [32101247, 31971417]
  2. Nat-ural Science Foundation of Guangdong Province, China [2019A1515011442]

向作者/读者索取更多资源

In this study, a novel transcription factor MYC gene was identified from Penaeus vannamei. The expression of PvMYC was constitutive in all detected tissues and highly expressed in hepatopancreas. PvMYC was up-regulated significantly and responded to low temperature stress. Overexpression of PvMYC negatively regulated autophagy, while silencing PvMYC increased autophagic activity under low temperature stress. These findings suggest that PvMYC plays a vital role in the cold adaptation mechanism of P. vannamei by negatively regulating autophagy.
MYC pmto-oncogene (MYC), a first oncogenic nuclear transcription factor isolated from the human genome, belongs to the helix loop helix/leucine zipper protein family (bHLHzip). MYC plays an important part in the process of various physiological and biochemical of vertebrate, such as cell growth, proliferation, cycle, and autophagy. However, its molecular regulation mechanism and function in invertebrates are still unclear. In this study, a novel transcription factor MYC gene was screened, cloned, and characterized from Penaeus vannamei. The open reading frame of PvMYC was 1593bp, encode a polypeptide of 530 amino acids with molecular weight of 58.5 kDa, and a theoretical PI of 5.75. The results of tissue distribution showed that PvMYC was constitutively expressed in all detected tissues, and highest expression in hepatopancreas. The expression level of PvMYC up-regulated significantly and responded to low temperature stress by nuclear ectopic after low temperature stress. Overexpression of PvMYC in shrimp hemocytes negatively regulated the expression of Beclin-1 and reduced the conversion from LC3I to LC3II, yet p62 was decreased significantly. Meanwhile, RAPA eliminated the inhibition of autophagy caused by overexpression of PvMYC. ROS levels and autophagy flux showed the similar trend under low temperature stress after silencing PvMYC. The expression levels of Beclin-1, key ATG gene and LC3II increased significantly, while p62 decreased significantly under the same conditions. In addition, the Total hemocyte count (THC) decreased sharply, and accelerated the injury of hepatopancreas under low temperature stress after silencing PvMYC. Collectively, these results suggest that PvMYC has vital role in the cold adaptation mechanism of P. vannamei by negatively regulating autophagy.

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