A hormone receptor pathway cell-autonomously delays neuron morphological aging by suppressing endocytosis

Richardson, Claire E. and Yee, Callista and Shen, Kang and Ceriani, Maria Fernanda (2019) A hormone receptor pathway cell-autonomously delays neuron morphological aging by suppressing endocytosis. PLOS Biology, 17 (10). e3000452. ISSN 1545-7885

[thumbnail of file (1).pdf] Text
file (1).pdf - Published Version

Download (2MB)

Abstract

Neurons have a lifespan that parallels that of the organism and are largely irreplaceable. Their unusually long lifespan predisposes neurons to neurodegenerative disease. We sought to identify physiological mechanisms that delay neuron aging in Caenorhabditis elegans by asking how neuron morphological aging is arrested in the long-lived, alternate organismal state, the dauer diapause. We find that a hormone signaling pathway, the abnormal DAuer Formation (DAF) 12 nuclear hormone receptor (NHR) pathway, functions cell-intrinsically in the dauer diapause to arrest neuron morphological aging, and that same pathway can be cell-autonomously manipulated during normal organismal aging to delay neuron morphological aging. This delayed aging is mediated by suppressing constitutive endocytosis, which alters the subcellular localization of the actin regulator T cell lymphoma Invasion And Metastasis 1 (TIAM-1), thereby decreasing age-dependent neurite growth. Intriguingly, we show that suppressed endocytosis appears to be a general feature of cells in diapause, suggestive that this may be a mechanism to halt the growth and other age-related programs supported by most endosome recycling.

Item Type: Article
Subjects: Pustakas > Biological Science
Depositing User: Unnamed user with email support@pustakas.com
Date Deposited: 27 Jan 2023 08:06
Last Modified: 09 Feb 2024 04:09
URI: http://archive.pcbmb.org/id/eprint/59

Actions (login required)

View Item
View Item