Dual role for Headcase in hemocyte progenitor fate determination in Drosophila melanogaster

Kharrat, Bayan and Gábor, Erika and Virag, Nikolett and Sinka, Rita and Jankovics, Ferenc and Kristó, Ildikó and Vilmos, Péter and Csordás, Gábor and Honti, Viktor (2024) Dual role for Headcase in hemocyte progenitor fate determination in Drosophila melanogaster. PLOS GENETICS, 20 (10). No. e1011448. ISSN 1553-7390

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Official URL: https://doi.org/10.1371/journal.pgen.1011448

Abstract

The hematopoietic organ of the Drosophila larva, the lymph gland, is a simplified representation of mammalian hematopoietic compartments, with the presence of hemocyte progenitors in the medullary zone (MZ), differentiated hemocytes in the cortical zone (CZ), and a hematopoietic niche called the posterior signaling centre (PSC) that orchestrates progenitor differentiation. Our previous work has demonstrated that the imaginal cell factor Headcase (Hdc, Heca) is required in the hematopoietic niche to control the differentiation of hemocyte progenitors. However, the downstream mechanisms of Hdc-mediated hematopoietic control remained unknown. Here we show that Hdc exerts this function by negatively regulating the insulin/mTOR signaling in the niche. When Hdc is depleted in the PSC, the overactivation of this pathway triggers reactive oxygen species (ROS) accumulation and, in turn, the differentiation of effector lamellocytes non-cell-autonomously. Although overactivation of insulin/mTOR signaling normally leads to an increase in the size of the hematopoietic niche, this effect is concealed by cell death caused by hdc loss-of-function. Moreover, we describe here that hdc silencing in progenitors causes cell-autonomous ROS elevation and JNK pathway activation, resulting in decreased MZ size and differentiation of lamellocytes. Similarly to the PSC niche, knocking down hdc in the MZ also leads to caspase activation. Notably, depleting Hdc in the progenitors triggers proliferation, an opposing effect to what is observed in the niche. These findings further our understanding of how progenitor maintenance in the larval lymph gland is controlled autonomously and non-cell-autonomously, and point towards new mechanisms potentially regulating HSC maintenance across vertebrates.

Item Type:	Article
Additional Information:	Funding Agency and Grant Number: National Research, Development and Innovation Office [OTKA K-131484]; National Laboratory of Biotechnology [2022-2.1.1-NL-2022-00008] Funding text: This work was supported by the National Research, Development and Innovation Office OTKA K-131484 (VH) and the 2022-2.1.1-NL-2022-00008 (National Laboratory of Biotechnology) grants. BK received a salary from the 2022-2.1.1-NL-2022-00008 (National Laboratory of Biotechnology) grant. The funders had no role in study design, data collection and analysis, decision to publish, or preparation of the manuscript.
Uncontrolled Keywords:	PROTEIN; CELL; PROLIFERATION; INSULIN; MAINTENANCE; LINEAGES; COMPARTMENTS; Hematopoietic progenitors; Oxidative stress;
Subjects:	Q Science / természettudomány > QH Natural history / természetrajz > QH301 Biology / biológia
SWORD Depositor:	MTMT SWORD
Depositing User:	MTMT SWORD
Date Deposited:	14 Apr 2025 09:00
Last Modified:	14 Apr 2025 09:00
URI:	https://real.mtak.hu/id/eprint/217740

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