4.5 Article

Transcriptional study reveals a potential leptin-dependent gene regulatory network in zebrafish brain

期刊

FISH PHYSIOLOGY AND BIOCHEMISTRY
卷 47, 期 4, 页码 1283-1298

出版社

SPRINGER
DOI: 10.1007/s10695-021-00967-0

关键词

Leptin receptor; Zebrafish; Gene expression; Gene regulatory network; Feeding; Brain

资金

  1. Uppsala University
  2. Carl Trygger Foundation for scientific research [CTS 16:413, CTS 19:805]

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The study investigated the regulatory connections between leptin and downstream genes mediating its appetite-regulating effects in teleost fish. Using a loss of function leptin receptor mutant in zebrafish, a potential gene expression network comprising several anorexigenic genes was identified. The findings suggest a potentially conserved regulatory connection between leptin and sp3a, acting as a transcriptional driver of a downstream gene network in the zebrafish brain.
The signal mediated by leptin hormone and its receptor is a major regulator of body weight, food intake and metabolism. In mammals and many teleost fish species, leptin has an anorexigenic role and inhibits food intake by influencing the appetite centres in the hypothalamus. However, the regulatory connections between leptin and downstream genes mediating its appetite-regulating effects are still not fully explored in teleost fish. In this study, we used a loss of function leptin receptor zebrafish mutant and real-time quantitative PCR to assess brain expression patterns of several previously identified anorexigenic genes downstream of leptin signal under different feeding conditions (normal feeding, 7-day fasting, 2 and 6-h refeeding). These downstream factors include members of cart genes, crhb and gnrh2, as well as selected genes co-expressed with them based on a zebrafish co-expression database. Here, we found a potential gene expression network (GRN) comprising the abovementioned genes by a stepwise approach of identifying co-expression modules and predicting their upstream regulators. Among the transcription factors (TFs) predicted as potential upstream regulators of this GRN, we found expression pattern of sp3a to be correlated with transcriptional changes of the downstream gene network. Interestingly, the expression and transcriptional activity of Sp3 orthologous gene in mammals have already been implicated to be under the influence of leptin signal. These findings suggest a potentially conserved regulatory connection between leptin and sp3a, which is predicted to act as a transcriptional driver of a downstream gene network in the zebrafish brain.

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