Transcriptomics

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A systemic role of macrophage-derived BMP2/4 homolog Dpp in controlling sterol hormone synthesis under dietary stress


ABSTRACT: High-caloric diets, prevalent in Western societies, are characterized by their affordability, yet they hinder overall development and compromise adult physiological performance. Unfortunately, children consuming diets rich in sugar are prone to developing insulin resistance, chronic low-grade inflammation, and delayed developmental transitions, such as puberty, which collectively lead to adverse systemic outcomes. In metazoans, these critical developmental transitions are tightly regulated by steroid hormones. These deleterious effects underscore the vital role of nutritional sensing organs in orchestrating inter-organ communication, which is indispensable for maintaining physiological and metabolic homeostasis. For instance, macrophages are capable of detecting metabolic perturbations and subsequently secreting growth factors to restore equilibrium. Whereas macrophages have been shown to modulate steroid hormone synthesis in Drosophila melanogaster under conditions of inanition, it remains unclear whether high-sugar diets (HSDs) influence macrophage behavior and steroid hormone synthesis. Using Drosophila melanogaster, we report that macrophage-derived Decapentaplegic (Dpp) mediates the biosynthesis of the steroid hormone ecdysone during HSD consumption, thereby impacting development and growth. Mechanistically, macrophage-derived Dpp interacts with Thickveins (Tkv) in the prothoracic gland, leading to the activation of the BMP pathway. This activation subsequently downregulates ecdysone synthesis (the only sterol hormone in flies), ultimately extending developmental time to ensure adult viability.

ORGANISM(S): Drosophila melanogaster

PROVIDER: GSE303750 | GEO | 2026/06/11

REPOSITORIES: GEO

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