Essential Role of Syntaxin-Binding Protein-1 in the Regulation of Glucagon-Like Peptide-1 Secretion

Mar 7, 2020Endocrinology

Key Role of Syntaxin-Binding Protein-1 in Controlling Glucagon-Like Peptide-1 Release

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Abstract

Stxbp1 is identified as a circadian regulated exocytotic protein essential for secretion in intestinal L-cells.

  • Stxbp1 is highly enriched in L-cells and expressed in a subpopulation of these cells in both mouse and human intestines.
  • Circadian patterns of Stxbp1 transcripts and protein were observed in mGLUTag L-cells.
  • Increased interaction between the core clock protein BMAL1 and Stxbp1 occurred at the peak of the circadian cycle.
  • Stxbp1 was recruited to the cytosol and plasma membrane shortly after L-cell stimulation.
  • Loss of Stxbp1 resulted in reduced GLP-1 secretion at the peak time of circadian release and impaired secretion in ex vivo conditions.

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Key numbers

74.9%
Reduction in Secretion
Compared to GIP-stimulated control cells after Stxbp1 knockdown.
50.1%
Impairment of Response
In L-cell knockout mice following an oral glucose load.
4 hours
Circadian Peak Expression
Stxbp1 levels peak at 12 hours post-synchronization.

Full Text

What this is

  • This research investigates the role of Syntaxin-Binding Protein-1 (Stxbp1) in regulating glucagon-like peptide-1 () secretion.
  • Stxbp1 is shown to be highly enriched in intestinal L-cells and exhibits circadian expression patterns.
  • Loss of Stxbp1 impairs secretion both in vitro and in vivo, indicating its essential role in this process.

Essence

  • Stxbp1 is crucial for secretion in intestinal L-cells, with its expression regulated by circadian rhythms. Loss of Stxbp1 significantly reduces secretion.

Key takeaways

  • Stxbp1 is enriched in L-cells and shows circadian expression patterns. It peaks at the same time as secretion, indicating a regulatory role.
  • Knockdown of Stxbp1 in L-cells leads to a 74.9% reduction in GIP-stimulated secretion, demonstrating its essential role in this process.
  • In vivo studies show that L-cell knockout of Stxbp1 results in a 50.1% impairment of response to an oral glucose load, affecting secretion dynamics.

Caveats

  • The study did not observe significant changes in plasma insulin or blood glucose levels despite impaired secretion, suggesting compensatory mechanisms may be at play.
  • Stxbp1's role in glucagon secretion remains unclear, as no significant differences were found in glucagon levels between knockout and control mice.

Definitions

  • GLP-1: Glucagon-like peptide-1, an incretin hormone that stimulates insulin secretion.
  • SNARE proteins: A family of proteins involved in the fusion of vesicles with target membranes, crucial for neurotransmitter and hormone release.
  • Circadian rhythm: Biological processes that display an endogenous oscillation of about 24 hours, influencing various physiological functions.

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