Transcription repressor-mediated control of engulfment receptor expression in Drosophila phagocytes

Transcription repressor-mediated control of engulfment receptor expression in Drosophila phagocytes

We previously reported that Drosophila phagocytes enhance their phagocytic activity after apoptotic cell engulfment accompanied by the activation of the transcription repressor Tailless and an increase in the levels of engulfment receptors. We herein investigated the underlying mechanisms. We found...

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Bibliographic Details
Published in:Experimental cell research Vol. 381; no. 1; pp. 10 - 17
Main Authors: Nonaka, Saori, Sono, Mai, Hoshi, Chiharu, Kanetani, Takuto, Nakayama, Hiroshi, Dohmae, Naoshi, Nakanishi, Yoshinobu
Format: Journal Article
Language:English
Published: United States Elsevier Inc 01-08-2019
Subjects:
Apoptosis
Drosophila
Gene regulation
Phagocytosis
Transcription repressor
Transcription repressor
Drosophila
Gene regulation
Phagocytosis
Apoptosis
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Summary:We previously reported that Drosophila phagocytes enhance their phagocytic activity after apoptotic cell engulfment accompanied by the activation of the transcription repressor Tailless and an increase in the levels of engulfment receptors. We herein investigated the underlying mechanisms. We found that Tailless phosphorylation levels decreased in Drosophila phagocytes following the stimulation with apoptotic cells. Anticipating the involvement of another transcription repressor, we examined the possible involvement of Krüppel, a bibliographically identified repressor whose expression is controlled by Tailless. The level of Krüppel in phagocytes decreased after the stimulation in a Tailless-dependent manner. The RNAi knockdown of Krüppel abrogated increases in the levels of engulfment receptors and phagocytic activity in stimulated phagocytes. The binding of Krüppel to the 5′-upstream regions of genes coding for engulfment receptors was demonstrated. These results suggest the following pathway: Tailless is activated by de-phosphorylation; Krüppel expression is inhibited by Tailless; the transcription of engulfment receptors-encoding genes is augmented due to a decrease of inhibition by Krüppel; and finally phagocytic activity is enhanced. [Display omitted] •Drosophila phagocytes are activated upon the engulfment of apoptotic cells.•This activation is due to the increased expression of engulfment receptor-encoding genes.•The transcription of engulfment receptor genes is enhanced through a release from transcription repression by Krüppel.•Krüppel transcription is inhibited by Tailless activated in phagocytes after apoptotic cell engulfment.•The activation of Tailless seems to be due to de-phosphorylation at a Thr residue.
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ISSN:0014-4827
1090-2422
DOI:10.1016/j.yexcr.2019.04.032